UNITED STATES
SECURITIES AND EXCHANGE COMMISSION
Washington, D.C. 20549
FORM 10-K
(Mark One)
|
x
|
Annual Report Pursuant to Section 13 or 15(d) of the
Securities Exchange Act of 1934
|
For the fiscal year ended December 31,
2016
|
¨
|
Transition Report under Section 13 or 15(d) of the Securities
Exchange Act of 1934
|
For the transition period from to
Commission File Number: 001-37720
INNOCOLL
HOLDINGS PUBLIC LIMITED COMPANY
(Exact name of registrant as specified
in its charter)
Ireland
|
|
N/A
|
(State or other jurisdiction of
incorporation or organization)
|
|
(I.R.S. Employer Identification No.)
|
Unit 9, Block D
Monksland Business Park
Monksland, Athlone
Ireland
|
|
N/A
|
(Address of principal executive offices)
|
|
(Zip Code)
|
Registrant’s telephone number, including
area code:
+353 (0) 90 648 6834
Securities registered pursuant to Section
12(b) of the Act:
Title of Each Class:
|
|
Name of Each Exchange on Which Registered:
|
Ordinary Shares, $0.01 par value per share
|
|
NASDAQ Global Market
|
Securities registered pursuant to Section
12(g) of the Act: None
Indicate
by check mark if the registrant is a well-known seasoned issuer, as defined in Rule 405 of the Securities Act.
Yes
¨
No
x
Indicate by check mark if the registrant is not required to
file reports pursuant to Section 13 or 15(d) of the Act.
Yes
¨
No
x
Indicate by check mark whether the registrant (1) has filed
all reports required to be filed by Section 13 or 15(d) of the Securities Exchange Act of 1934 during the preceding 12 months
(or for such shorter period that the registrant was required to file such reports), and (2) has been subject to such filing requirements
for the past 90 days.
Yes
x
No
¨
Indicate by check mark whether the registrant has submitted
electronically and posted on its corporate Web site, if any, every Interactive Data file required to be submitted and posted pursuant
to Rule 405 of Regulation S-T (§232.405 of this chapter) during the preceding 12 months (or for such shorter period that
the registrant was required to submit and post such files).
Yes
x
No
¨
Indicate by check mark if disclosure of delinquent filers pursuant
to Item 405 of Regulation S-K is not contained herein, and will not be contained, to the best of registrant’s knowledge,
in definitive proxy or information statements incorporated by reference in Part III of this Form 10-K or any amendment to this
Form 10-K.
x
Indicate by check mark whether the registrant is a large accelerated
filer, an accelerated filer, a non-accelerated filer, or a smaller reporting company. See the definitions of “large accelerated
filer,” “accelerated filer” and “smaller reporting company” in Rule 12b-2 of the Exchange Act. (Check
one):
¨
Large Accelerated Filer
|
x
Accelerated Filer
|
¨
Non-Accelerated Filer
|
¨
Smaller Reporting Company
|
Indicate by check mark whether the registrant is a shell company
(as defined in Rule 12b-2 of the Act).
Yes
¨
No
x
The aggregate market value of voting and non-voting common
equity held by non-affiliates of the registrant was approximately $112.0 million based upon the closing price of the common equity
on the NASDAQ Global Market on the last business day of the registrant’s most recently completed second fiscal quarter (June
30, 2016). In determining this amount, the registrant has assumed solely for this purpose that all of its directors, executive
officers and persons beneficially owning 10% or more of the outstanding ordinary shares of the registrant may be considered to
be affiliates. This assumption shall not be deemed conclusive as to affiliate status for this or any other purpose.
The number of Ordinary Shares, $0.01 par value per share, of
the registrant outstanding as of March 13, 2017 was 29,748,239.
INNOCOLL HOLDINGS PUBLIC LIMITED COMPANY
TABLE OF CONTENTS
In this annual report, unless the context otherwise indicates,
Innocoll Holdings plc, a public limited company formed under Irish law, is referred to as Innocoll. Innocoll, together with its
direct and indirect wholly owned subsidiaries as of the time relevant to the applicable reference, are collectively referred to
as the Innocoll Group. Innocoll and its current direct and indirect wholly owned subsidiaries are collectively referred to as
“we,” “us,” “our,” “Innocoll” or the “Company.”
Special Note Regarding Forward-Looking Statements.
This annual report on Form 10-K contains forward-looking
statements within the meaning of Section 27A of the Securities Act of 1933, as amended, and Section 21E of the Securities Exchange
Act of 1934, as amended, or the Exchange Act. This information may involve known and unknown risks, uncertainties and other factors
that are difficult to predict and may cause our actual results, performance or achievements to be materially different from future
results, performance or achievements expressed or implied by any forward-looking statements. These risks, uncertainties and other
factors include, but are not limited to, risks associated with the following:
|
·
|
our
plans to develop and manufacture XaraColl and our other product candidates;
|
|
·
|
the
results of clinical trials and non-clinical studies, including new studies that may
be required by the U.S. Food and Drug Administration, for XaraColl and our other
product candidates;
|
|
·
|
the
timing of, and our ability to obtain, regulatory approval of XaraColl and our other product
candidates;
|
|
·
|
our
ability to submit a revised New Drug Application for XaraColl in a timely manner;
|
|
·
|
our
ability to identify additional financing to allow us to continue our operations and pursue
our product development programs;
|
|
·
|
the
timing of our anticipated launches of XaraColl and our other product candidates;
|
|
·
|
the
rate and degree of market acceptance of XaraColl and our other product candidates;
|
|
·
|
the
size and growth of the potential markets for XaraColl and our other product candidates
and our ability to serve those markets;
|
|
·
|
the
regulatory framework and approval process we may become subject to in the event the FDA
classifies XaraColl or any other of our products as a drug/device combination;
|
|
·
|
our
manufacturing and marketing capabilities;
|
|
·
|
the
timing of, and our ability to obtain, regulatory approvals for the expansion of our manufacturing
facility;
|
|
·
|
regulatory
developments in the United States and foreign countries;
|
|
·
|
our
ability to obtain and maintain the scope, duration and protection of our intellectual
property rights;
|
|
·
|
statements
concerning our corporate and tax domiciles and potential changes to them, including potential
tax charges;
|
|
·
|
the
accuracy of our estimates regarding expenses and capital requirements;
|
|
·
|
fluctuations
in interest rates and currency exchange rates;
|
|
·
|
the
accuracy of our assessments regarding pending litigation and our ability to successfully
defend against any such claims;
|
|
·
|
the
loss of key scientific or management personnel; and
|
|
·
|
our
ability to regain compliance with, and thereafter continue to satisfy, the listing requirements
of the NASDAQ Global Market or any other national securities exchange upon which our
securities may be listed,
|
as well as risks detailed under the caption “Risk
Factors” in this annual report on Form 10-K and in our other reports filed with the U.S. Securities and Exchange Commission,
or the SEC, from time to time hereafter.
Forward-looking statements describe management’s current
expectations regarding our future plans, strategies and objectives and are generally identifiable by use of the words “may,”
“will,” “should,” “could,” “expect,” “anticipate,” “estimate,”
“believe,” “intend,” “project,” “potential” or “plan” or the negative
of these words or other variations on these words or comparable terminology. Such statements include, but are not limited to,
statements relating to:
|
·
|
XaraColl
and our other product candidates;
|
|
·
|
clinical
trials and non-clinical studies for XaraColl and our other product candidates;
|
|
·
|
potential
regulatory approvals;
|
|
·
|
future
product advancements; and
|
|
·
|
anticipated
financial or operational results.
|
Forward-looking statements are based on assumptions that
may be incorrect, and we cannot assure you that the projections included in the forward-looking statements will come to pass.
We have based the forward-looking statements included in
this annual report on Form 10-K on information available to us on the date of this annual report, and we assume no obligation
to update any such forward-looking statements, other than as required by law. Although we undertake no obligation to revise or
update any forward-looking statements, whether as a result of new information, future events or otherwise, you are advised to
consult any additional disclosures that we may make directly to you or through reports that we, in the future, may file with the
SEC, including annual reports on Form 10-K, quarterly reports on Form 10-Q and current reports on Form 8-K.
All forward-looking statements included herein are expressly
qualified in their entirety by the cautionary statements contained or referred to elsewhere in this annual report. Unless otherwise
indicated, the information in this annual report is as of December 31, 2016.
PART I
Item 1. Business.
Overview
We are a global, commercial stage specialty
pharmaceutical and medical device company with late stage development programs targeting areas of significant unmet medical need.
We utilize our proprietary collagen-based technology platform to develop our biodegradable and fully bioresorbable products and
product candidates which can be broken down by the body without the need for surgical removal or applied topically. Using our
proprietary processes at our manufacturing facility, we derive and purify bovine and equine collagen and then utilize our technology
platform to incorporate the purified collagen into our topical and implantable products. These products combine proven therapeutics,
including small molecules and biologics, with highly customized drug release profiles, localized drug delivery and superior handling
properties. Innocoll will use code names to refer to its products in development and we expect to seek brand name approval for
the names we currently use to refer to our products, which names may change in the future.
Our lead product candidate is XaraColl®
for the treatment of post-operative pain. We initiated our Phase 3 trials for XaraColl in the third quarter of 2015. We received
data from those Phase 3 efficacy trials for XaraColl in the second quarter of 2016 submitted a New Drug Application (“NDA”)
with the U.S. Food and Drug Administration (“FDA”) in October 2016 and we received a Refusal to File Letter from the
FDA in December 2016. CollaGUARD, which prevents post-surgical adhesions, has been approved in 12 countries in Asia, the Middle
East and Latin America, and we commenced steps required for approval in the United States, including the provision of additional
information required by the FDA, in the second quarter of 2016. In 2016, we generated $4.4 million of sales from four marketed
products: (i) CollaGUARD, which utilizes our CollaFilm® technology, a transparent, bioresorbable collagen film for the prevention
of post-operative adhesions in multiple surgical applications, including digestive, colorectal, gynecological and urological surgeries;
(ii) Collatamp® Gentamicin Surgical Implant, or CollatampG, which utilizes our CollaRx® sponge technology, indicated for
the treatment or prevention of post-operative infection; (iii) Septocoll®, a bioresorbable, dual-action collagen sponge, indicated
for the treatment or prevention of post-operative infection, which we manufacture and supply to Biomet Orthopedics Switzerland
GmbH, or Biomet; and (iv) RegenePro, a bioresorbable collagen sponge for dental applications which we manufacture and supply to
Biomet 3i. We utilize our proprietary collagen-based technology platform to develop our biodegradable and bioresorbable products
and product candidates. We manufacture our products in our own commercial scale facility. We have strategic partnerships in place
with large international healthcare companies, such as Takeda, EUSA Pharma and Biomet, which market certain of our approved products
in their applicable territory within Asia, Australia, Canada, Europe, Latin America, the Middle East, and the United States.
Summaries of Our Product Candidates
XaraColl (INL-001)
Our first lead product candidate, XaraColl,
is an implantable, bioresorbable collagen matrix that we designed to provide sustained post-operative pain relief through controlled
delivery of bupivacaine at the surgical site. The current standard of care for the treatment of post-operative pain relies heavily
on the use of opioids supplemented by other classes of pain medications, the combination of which is known as multi-modal pain
therapy. However, 75% of patients receiving standard treatments still report inadequate post-operative pain relief and many patients
report adverse events from these medications. Opioid-related adverse events, such as nausea, constipation and respiratory depression,
which are potentially severe, may require additional medications or treatments and prolong a patient’s hospital stay, thereby
increasing overall treatment costs significantly. Additionally, opioids are highly addictive and induce drug resistance and tolerance.
Given the negative side effects and costs associated with opioid use in particular, there is increasing focus from hospitals,
payors and regulators on treatments that reduce opioid use in the treatment of post-operative pain.
In 2016, Innocoll conducted 10 market research
studies in the U.S. with 556 hospital decision makers including 484 surgeons, 27 pain specialists, and 45 Pharmacy & Therapeutic
(P&T) members. The objectives of this research were to assess the potential market opportunity for XaraColl. Our findings
indicated an interest in the broad use of non-opioid based long-acting local anesthetics. The XaraColl profile was seen
as favorable by participants both due to its opioid reduction data, pain reductions on top of normal care and the consistency
of results across two large studies. In
addition, participating surgeons were curious
to learn more about our matrix drug-delivery format, viewing our delivery system as novel and targeted. XaraColl clinical
investigators found the matrix very easy to use, with little instruction required. When shown the Phase 3 clinical trial
results and a hypothetical hernia label, 272 surgeon survey respondents projected use of XaraColl across a broad array of soft
tissue surgeries, as well as in orthopedic procedures, although we will only be able to market XaraColl for those indications
that it is approved for. Respondents indicated that P&T acceptance will likely hinge on price and on strong demand from
surgeons.
XaraColl has been studied in one Phase
1, four Phase 2 and two pivotal Phase 3 clinical trials. Findings from the two identical multicenter, double-blind, placebo-controlled
Phase 3 studies demonstrated the effectiveness of locally placed INL-001 in reducing both pain intensity and the need for
opioid rescue medication after surgery, as well as the reproducibility of the treatment effects. In each study, subjects
treated with INL-001 had statistically significantly less pain from Time 0 through the first 24 hours (SPI24; p≤0.0004; primary
endpoint) and through 48 hours (SPI48; p=0.0033) in the combined analysis compared with subjects treated with placebo.
These reductions in pain intensity were coupled with less total opioid rescue medication usage in the INL-001 group compared with
the placebo group. A key secondary endpoint in the pivotal Phase 3 clinical trials was the sum of pain intensity over 48 hours
(SPI48), and the pooled data of the two studies were statistically significant for this endpoint (p=0.0033). Study-2 achieved a
statistically significant result (p=0.0270), and Study-1 trended toward, but did not achieve statistical significance (p=0.0568).
Another key secondary endpoint was the sum of pain intensity over 72 hours (SPI72). The pooled data of the two pivotal Phase 3
clinical studies for this endpoint were statistically significant, although neither individual study achieved statistical significance
for SPI72.
On the basis of the positive data from our
Phase 3 clinical program, we submitted an NDA for XaraColl at the beginning of the fourth quarter of 2016 and subsequently received
a Refusal to File Letter on December 23, 2016 from the FDA. In February 2017, our representatives attended a Type-A meeting with
representatives of the FDA to review potential pathways forward following our receipt of the Refusal to File Letter and to review
a proposed plan for proceeding with additional studies that would allow us to file a revised NDA for XaraColl. During the meeting,
we proposed a plan designed to allow us to submit a revised NDA to the FDA by the latter part of 2017. We proposed conducting
an additional short-term pharmacokinetic study and several short-term non-clinical studies. Under current practice before the
FDA, we received limited feedback during the meeting and we expect to receive shortly from the representatives of the FDA formal
written meeting minutes of our Type-A meeting, which will serve as the official record of the response of the FDA to our proposal
during the meeting. If the FDA concurs with our plan, we will commence the additional studies, and if the results are positive,
we would submit a revised NDA to the FDA soon after the completion of the studies. However, if the FDA suggests that studies beyond
those that we proposed would be necessary, or if the results of the studies that we proposed are not positive, we would not likely
be able to submit our revised NDA for an extended period of time, if at all.
We intend to continue to build commercial
capabilities in the U.S. to effectively support our brands, including XaraColl, in the U.S. In Europe, we plan to work with the
European Medicines Agency, or EMA, to finalize our regulatory pathway based on Scientific Advice received from the EMA in late
October 2015. We will, however, continue to evaluate the benefits of select partnerships or co-promotion alternatives if we believe
it is in the best interest of shareholders, and the success of our brands, now or into the future.
Cogenzia (INL-002)
Cogenzia (which was previously our second
lead product candidate), is a topically applied, bioresorbable collagen sponge for the treatment of Diabetic Foot Infections (DFIs).
Cogenzia is designed to release a high dose of gentamicin directly at the site of DFIs. The clinical development programs (COACT
1 and 2) for Cogenzia were completed in the fourth quarter 2016. Cogenzia and the placebo collagen-matrix were well-tolerated
in both studies. Incidence of overall adverse events was similar across all three treatment arms in the two Phase 3 studies.
However, COACT 1 and 2 both failed to meet their primary end point of clinical cure of infection after 28 days versus either placebo
plus Standard Of Care (SOC) or SOC alone.
While there were trends toward clinical
response (clinical cure plus improvement) in the Cogenzia arm and the placebo collagen-matrix arm, neither study achieved statistical
significance on the primary endpoint of clinical cure after 28 days. While Innocoll continued to analyse sub populations
of patients within the studies, the full dataset confirmed that the addition of gentamicin delivered topically through Cogenzia,
in conjunction with SOC, does not confer sufficient additional clinical benefit over the placebo collagen matrix, administered
with SOC, or SOC alone, in patients with moderate to severe diabetic foot ulcer infections.
Cogenzia has previously been approved in
Argentina, Australia, Canada, Jordan, Mexico, Russia and Saudi Arabia. We have filed five patent applications for Cogenzia in
Australia, Canada, Europe, Japan and the United States,
all of which are currently in the examination
phase. If and when our patents are issued, we expect patent protection for Cogenzia in the United States and Europe to expire
at the earliest in 2031.
The clinical development programs (COACT
1 and 2) for Cogenzia were discontinued in the fourth quarter of 2016 following the failure of these Phase 3 trials to meet their
primary end point of clinical cure of infection after 28 days versus either placebo plus SOC or SOC alone.
CollaGUARD (INL-003)
CollaGUARD is our translucent, bioresorbable
collagen film for the prevention of post-operative adhesions in multiple surgical applications, including digestive, colorectal,
gynecological and urological surgeries. The global market for anti-adhesion products is difficult to accurately measure, but it
was estimated at approximately $1.0 billion in 2014. We believe that CollaGUARD’s unique combination of features for optimal
handling, ease-of-use, hemostatic properties and anti-adhesion performance sets it apart from its competitors. Unlike other competitive
products, CollaGUARD can be used in both open and laparoscopic procedures. CollaGUARD is highly robust and can withstand suturing
or stapling if required during a procedure and is fully biodegradable and is designed to be safely and completely resorbed over
approximately three to five weeks post implantation. CollaGUARD is also translucent which allows for constant visibility of the
surgical field. In addition, CollaGUARD is highly stable at room temperature and has up to a five-year shelf life.
CollaGUARD is regulated as a Class III
device in the United States and we expect it will require a single pivotal clinical trial to support premarket approval, or PMA,
by the FDA. In the first quarter of 2015, we initiated a second pilot efficacy study in patients undergoing gynecological laparoscopic
adhesiolysis. However, we decided to terminate the second pilot efficacy study in favor of a planned pilot efficacy study in patients
undergoing myomectomy via open laparotomy to be performed in the U.S. under an Investigational Device Exemption, or IDE. We anticipate
that data from this pilot study will help us to finalize the design of the U.S. pivotal study protocol. In the fourth quarter
of 2015, we completed a pilot clinical study for CollaGUARD, run in the Netherlands, in patients undergoing intrauterine adhesiolysis
via operative hysteroscopy. A clinical study report for this study confirmed the ease of use and safety profile for CollaGUARD
in this patient population. We held our pre-IDE submission meeting with the FDA in the first quarter of 2016, in which we agreed
on a non-clinical development plan that will be completed and reported prior to our filing a full IDE package, which we expect
to file in the second half of 2017 with the Pilot (Feasibility) Clinical Study to be initiated after approval. CollaGUARD
has been approved in 12 countries in Asia, Latin America and the Middle East and we have launched the product in certain of these
territories through our established distribution partners, such as Takeda, which launched and distributed CollaGUARD in Russia
in 2014 and received approval in the first quarter of 2015 for the product in Belarus, Ukraine and Kazakhstan.
The initial European CE certificate for
CollaGUARD was valid from October 7, 2011 to July 26, 2015. In accordance with normal practice for device recertification, we
compiled an updated Design Dossier and submitted this to our European Notified Body (TÜV SÜD, Munich, Germany) in December
2014. As part of our application for recertification, we included an updated literature-based Clinical Evaluation Report and a
Post Market Clinical Follow-up (or PMCF) Plan, which rationalized the objectives of our ongoing clinical investigations in accordance
with the current 2012 European Guideline for PMCF studies. However, prior to the expiration of the original certificate, the Notified
Body requested that we revise our PMCF plan to additionally include a direct clinical comparison of CollaGUARD’s performance
and safety compared to another CE-certified adhesion barrier. In March 2016, we met with the Notified Body to seek clarification.
At the meeting, TÜV SÜD agreed that current European medical device regulations do not specifically require that our
PMCF plan include such a clinical comparison, and agreed with our proposal for an updated PMCF based on the pilot clinical study
in open myomectomy patients, as was agreed with FDA at the pre-IDE meeting. Provided TÜV SÜD determines that the clinical
data from the U.S. pilot study are supportive, then recertification would be possible at that time based on an updated Technical
Dossier and Clinical Evaluation. Until a new CE-certificate has been issued, we will not supply CollaGUARD to our marketing partners
for sale in Europe or other affected territories.
We submitted a family of patent applications
aimed at protecting CollaGUARD on an international basis, including Australia, Canada, Eurasia, Europe, Japan, Mexico, and the
United States, which are currently in the examination phase. If issued, these patents are expected to expire at the earliest in
2033 in the United States.
Our Products
Our current late-stage product candidate
pipeline is summarized in the table below, including expected milestones:
*References to all events in the table
denote expected timing of the events. Timing is subject to possible change. Any FDA Approval is subject to positive pivotal trial
results as well as other FDA determinations on various matters.
XaraColl
XaraColl is an implantable, bioresorbable
collagen matrix designed to provide sustained post-operative pain relief through the controlled local delivery of bupivacaine
at the surgical site, thereby reducing the need for systemic opioids in the treatment of post-operative pain. Bupivacaine is a
local anesthetic that blocks propagation of nerve signals via sodium channel antagonism. We designed XaraColl to:
|
·
|
provide an
initial rapid burst of bupivacaine followed by slower, sustained release that delivers
effective analgesia up to a 72 hour period, the crucial timeframe that impacts a patient’s
quality and duration of recovery;
|
|
·
|
provide safe
and effective pain relief as part of a multi-modal therapy;
|
|
·
|
reduce opioid
use and related adverse events;
|
|
·
|
target both
the incisional and deep visceral pain components associated with moderate and major surgery;
|
|
·
|
reduce patient
costs, including those associated with length of hospital stay;
|
|
·
|
be used in
both open and laparoscopic surgery; and
|
|
·
|
be easily positioned
at different layers within the surgical wound.
|
XaraColl was developed using our proven
and commercialized collagen sponge matrix technology, CollaRx. XaraColl is an intraoperative implant that is fully bioresorbable
and delivers the local anesthetic, bupivacaine, directly to the surgical site. We designed XaraColl to provide post-operative
analgesia for up to 72 hours after surgery. By placing XaraColl directly in contact with the traumatized tissue surfaces, surgeons
can sustain an effective drug concentration at both the visceral and incisional sites of surgical wound pain.
Post-operative Pain Market Overview
There are approximately 46 million inpatient
and 53 million outpatient surgeries performed in the United States each year. Traditionally, the standard of care for the treatment
of post-operative pain relied heavily on the use of opioids supplemented by other classes of pain medications and delivery mechanisms,
including non-steroidal anti-inflammatory drugs, or NSAIDs, acetaminophen and wound infiltration with local anesthetics, the combination
of which is known as multi-modal pain therapy. However, 75% of patients receiving standard treatments still report inadequate
post-operative pain relief and many patients report adverse events from these medications. Unrelieved acute pain can lead to longer
post-operative recovery time, delayed ambulation, higher incidence of surgery related complications, increased intensive care
unit and hospital length of stays, hospital readmission, progression from acute to chronic pain and reduced levels of daily functioning.
The table below summarizes the properties of various options available for the treatment of post-operative pain.
Properties of
Post-operative Pain Management
Treatment
|
|
Administration
|
|
Duration
of Action
|
|
Reported
Adverse Events
|
Opioids
|
|
Constant infusion / Multiple administrations
|
|
4-6 hours
|
|
Sedation, dizziness, nausea, vomiting, constipation,
physical dependence, tolerance and respiratory depression
|
PCA and Elastomeric Bag Systems
|
|
Constant infusion / Multiple administrations
|
|
Dependent on device settings and duration of
use
|
|
May introduce catheter-related issues such as
infection
|
NSAIDs
|
|
Multiple administrations
|
|
4-6 hours
|
|
Increased risk of bleeding and gastrointestinal
and renal complications
|
Acetaminophen
|
|
Multiple administrations
|
|
6-8 hours
|
|
Liver toxicity
|
Local Anesthetics
|
|
Single
|
|
≤8 hours
|
|
Mild
|
Injectable Suspensions
|
|
Single
|
|
Up to 24 hours (per label)
|
|
Mild
|
XaraColl
|
|
Single
|
|
Intended up to 48-72 hours
|
|
Mild
|
|
·
|
Opioids
.
Opioids, such as morphine, are the mainstay of post-operative pain management, but are
associated with a variety of unwanted and potentially severe side effects, leading healthcare
practitioners to seek opioid-sparing strategies for their patients. Opioid side effects
include sedation, nausea, vomiting, urinary retention, headache, itching, constipation,
cognitive impairment, respiratory depression and death. Most importantly, opioids are
highly addictive and induce drug resistance and tolerance. These side effects may require
additional medications or treatments and may prolong a patient’s stay in the post-anesthesia
care unit and the hospital or ambulatory surgery center, thereby increasing overall treatment
costs significantly.
|
|
·
|
PCA and Elastomeric
Bag Systems
. Opioids are often administered intravenously through patient-controlled
analgesia, or PCA, systems in the immediate post-operative period. PCA post-operative
pain management for three days can cost up to $500, excluding the costs of treating opioid
complications. In an attempt to reduce opioid consumption, many hospitals employ elastomeric
bag systems designed to deliver bupivacaine to the surgical area through a catheter over
a period of time. This effectively extends the duration of bupivacaine in the post-operative
site, but has significant shortcomings. PCA systems and elastomeric bag systems are clumsy
and difficult to use, which may delay patient ambulation and introduce catheter-related
issues, including infection. In addition, PCA systems and elastomeric bags require significant
additional hospital resources to implement and monitor.
|
|
·
|
NSAIDs
. NSAIDs
are considered to be useful alternatives to opioids for acute pain relief because they
do not produce respiratory depression or constipation. Despite these advantages, the
use of injectable NSAIDs, such as ketorolac and ibuprofen, is severely limited in the
post-operative period because they increase the risk of bleeding and gastrointestinal
and renal complications.
|
|
·
|
Acetaminophen
.
Oral and suppository formulations of acetaminophen have long been used to manage pain,
including pain in a post-operative setting. Recently, the FDA approved an IV formulation
of acetaminophen, Ofirmev, for the management of post-operative pain to avoid the slow
onset of the analgesic effects after oral delivery. Acetaminophen is considered not only
a viable alternative to NSAIDs, but also can be combined with NSAIDs for an additive
effect. However, in any formulation, acetaminophen increases the risk of liver damage
or failure which limits the ability to administer it at high dosages or over an extended
period of time.
|
|
·
|
Local Anesthetics
.
Treatment of post-operative pain typically begins at the end of surgery, with local anesthetics,
such as bupivacaine, administered by local infiltration. Though this infiltration provides
a base platform for the treatment of post-operative pain for the patient, efficacy of
conventional bupivacaine and other available local anesthetics is limited, lasting approximately
eight hours or less. As local infiltration is not practical after the surgery is complete,
and as surgical pain is greatest in the first few days after surgery, additional therapeutics
are required to manage post-operative pain.
|
|
·
|
Injectable Suspensions
.
Exparel®, a liposomal injection of bupivacaine, indicated for administration in the
surgical site to produce post-operative analgesia, was commercially launched in the United
States in 2012. Exparel has demonstrated significant reduction in pain intensity up to
72 hours post-surgery, based on Pacira Pharmaceuticals, Inc.’s hemorrhoidectomy data.
However, between 24 and 72 hours after administration, as per its label, Exparel showed
minimal to no difference on mean pain intensity when compared to placebo. Exparel should
be stored under refrigerated conditions and has a reported shelf life of 30 days when
stored at room temperature in sealed (unopened) vials.
|
|
·
|
XaraColl’s
Approach
. Given the negative side effects and the costs associated with opioid use
in particular, there is an increasing focus from hospitals, payors and regulators on
treatments that reduce opioid use for the treatment of post-operative pain. We believe
that XaraColl, in combination with NSAIDs, acetaminophen and/or local anesthetics, has
the potential to become a cornerstone in the treatment of post-operative pain, focusing
on opioid reduction or elimination.
|
XaraColl (INL-001) Clinical Data
XaraColl has been studied in one Phase
1 and four completed Phase 2 clinical trials enrolling 184 patients, including 103 patients in two Phase 2 trials in hernia repair
at doses of 100 mg and 200 mg of bupivacaine. Results from
both trials demonstrated that XaraColl reduces
both pain intensity and opioid consumption with the 200 mg dose resulting in an overall greater combined effect at 48 hours.
Phase 1 Trials
We conducted an open-label, single site,
Phase 1 pharmacokinetic and safety trial in 12 women undergoing total abdominal hysterectomy for a non-cancerous condition. Pharmacokinetic
trials study the interactions of a drug and the body in terms of its absorption, distribution, metabolism and excretion. Three
XaraColl 50 mg sponges (150 mg total dose) were implanted; the first over the vaginal vault, the second along the line of peritoneal
closure, and the third along the line of rectal sheath closure. Serum samples were obtained through 96 hours for pharmacokinetic
analysis and safety was assessed through 30 days. Patients were maintained on a non-opioid oral analgesic regimen according to
institutional standards through 96 hours and also given access to intravenous morphine via PCA during the first 24 hours. Pain
intensity was assessed at regular intervals using a 100 mm visual analog scale. XaraColl exhibited a biphasic and sustained release
pharmacokinetic profile with an early peak typically observed within the first 2 hours followed by a second, generally higher
peak up to 24 hours later. The individual maximum serum concentrations ranged from 0.14 to 0.44 μg/ml (mean 0.22 μg/ml),
which are well below the accepted neuro- and cardio-toxicity thresholds for bupivacaine. Patient use of PCA morphine for breakthrough
pain compared favorably with institutional experience and pain scores were generally low. XaraColl was considered safe and well
tolerated at a dose of 150 mg.
Phase 2 Clinical Trials in Open Hernia Repair
We conducted two independent, multicenter,
double-blind, placebo-controlled trials to evaluate the efficacy and safety of XaraColl in men undergoing unilateral inguinal
hernia repair by open laparotomy. Our primary and secondary efficacy endpoints in the trials included (i) SPI and (ii) the total
consumption of opioid analgesia, or TOpA (mg of IV morphine equivalent), each analyzed at 24, 48 and 72 hours after surgery, respectively.
In the first trial, we randomized 53 patients
to receive either two XaraColl 50 mg sponges for a total dosage of 100 mg bupivacaine (24 patients) or two placebo sponges (29
patients). In all cases, one sponge was placed beneath the hernia repair mesh and the second placed below the laparotomy incision.
During patient recovery, immediate post-operative pain was treated with intravenous morphine at incremental doses of 1 to 2 mg,
as needed to achieve pain control. Once patients could tolerate oral medication, they were provided with opioid tablets as rescue
analgesia and instructed to take only if necessary for breakthrough pain. Patients assessed their post-operative pain intensity
after aggravated movement (cough) on a 0 to 100 mm visual analogue scale at regular intervals through 72 hours. Their use of supplementary
opioid medication was also recorded. Safety was assessed through 30 days. XaraColl-treated patients in this first trial reported
significantly less pain through 24 hours (44% reduction; p = 0.001), 48 hours (37% reduction; p = 0.012) and 72 hours (34% reduction;
p = 0.030). They also took less opioid medication through each time point (25%, 16% and 17% reduction, respectively), although
these reductions were not statistically significant (p = 0.123, 0.359, and 0.396, respectively).
Based on the safety and efficacy results
we observed at the 100 mg dose, we conducted a second multicenter, double-blind, placebo-controlled hernia repair trial, implanting
two XaraColl 100 mg sponges for a total dosage of 200 mg. We enrolled 50 patients, 25 randomized to each group, and performed
the same efficacy analyses as the first trial. In this second trial, XaraColl-treated patients took significantly less opioid
medication through 24 hours (44% reduction; p = 0.004) and 48 hours (36% reduction; p = 0.042), with a trend towards statistical
significance at 72 hours (31% reduction; p = 0.094). Of the patients that received XaraColl, 16% did not require any opioid rescue
analgesia, compared to 0% in the control group. Although XaraColl-treated patients in the 200 mg also reported less pain (22%,
18%, and 19% reduction through 24, 48, and 72 hours, respectively) these results were not statistically significant. These results
are in contrast to the pain intensity results achieved in the 100 mg trial where statistical significance was demonstrated for
this parameter.
Results from the efficacy analyses are
presented in the table below. p-values of less than or equal to 0.05, representing a less than a 5% probability that the observed
difference occurred by chance alone, were considered statistically significant and p-values larger than 0.05, but less than or
equal to 0.10, were considered a statistical trend.
Efficacy of XaraColl
in Open Hernia Repair
Observed Treatment
Effect vs. Placebo Control
Summed Pain Intensity (SPI)
|
|
100
mg trial (n = 53)
|
|
|
200
mg trial (n = 50)
|
|
Efficacy Endpoint
|
|
Mean
reduction
|
|
|
p-value
|
|
|
Mean
reduction
|
|
|
p-value
|
|
24 hours
|
|
|
44
|
%
|
|
|
0.001
|
*
|
|
|
22
|
%
|
|
|
0.080
|
**
|
48 hours
|
|
|
37
|
%
|
|
|
0.012
|
*
|
|
|
18
|
%
|
|
|
0.178
|
|
72 hours
|
|
|
34
|
%
|
|
|
0.030
|
*
|
|
|
19
|
%
|
|
|
0.184
|
|
Total Use of Opioid Analgesia (TOpA)
|
|
100
mg trial (n = 53)
|
|
|
200
mg trial (n = 50)
|
|
Efficacy Endpoint
|
|
Mean
reduction
|
|
|
p-value
|
|
|
Mean
reduction
|
|
|
p-value
|
|
24 hours
|
|
|
25
|
%
|
|
|
0.123
|
|
|
|
44
|
%
|
|
|
0.004
|
*
|
48 hours
|
|
|
16
|
%
|
|
|
0.359
|
|
|
|
36
|
%
|
|
|
0.042
|
*
|
72 hours
|
|
|
17
|
%
|
|
|
0.396
|
|
|
|
31
|
%
|
|
|
0.094
|
**
|
*
statistically significant
**
statistical trend
Patients experiencing an opioid-related
adverse event in the United States had a 55% longer hospital stay than those without such events, a 47% higher hospitalization
cost, a 36% increased risk of 30-day readmission and a 3.4 times greater risk of in-patient mortality in 2013. We also observed
that at the higher 200 mg dose, 16% (4/25) of patients did not require any opioid rescue analgesia throughout the 72 hours, compared
to 0% in the corresponding placebo control group. Accompanying the significantly reduced use of rescue analgesia, we also observed
a 52% reduction in the number of patients who reported any adverse event commonly associated with consumption of opioids. In addition,
there was an increase of 102% in time until patients first used rescue medication following discharge from the post-anesthesia
care unit. Furthermore, we found that nausea events reported by XaraColl-treated patients were generally less severe and of shorter
duration, while more patients in the control group received antiemetic medication for nausea. We believed that increasing the
dosage of XaraColl from 200 mg to 300 mg in Phase 3, would result in a higher number of patients avoiding taking opioid medication
than was observed in Phase 2 as well as a further reduction in opioid-related adverse events.
In both trials, XaraColl was generally
considered safe and well tolerated. Most adverse events reported by patients were considered mild and none were considered related
to XaraColl. The most commonly reported adverse events included headache, rash and gastrointestinal effects such as nausea and
constipation.
Phase 2 Clinical Trial in Open Gynecological Surgery
In 2008, for the purpose of comparing the
clinical performance of XaraColl with the then-leading, commercially-available product, we designed and conducted a randomized,
multicenter trial to compare the efficacy of XaraColl with ON-Q. Prior studies had reported reduced use of opioid analgesia in
patients fitted with ON-Q. However, the device is expensive, requires subsequent removal of the indwelling catheter by nursing/hospital
staff and is relatively cumbersome.
In our trial, we randomized 27 women undergoing
total abdominal hysterectomy or similar open gynecological surgery to receive either three XaraColl 50 mg implants (150 mg total
dose divided between the vaginal vault, the peritoneal incision, and along the rectal sheath), or ON-Q (900 mg bupivacaine continuously
perfused post-operatively over 72 hours). Following surgery, patients had access to intravenous morphine via a PCA pump as rescue
analgesia for the first 24 hours and to oral opioid medication thereafter. Cumulative use of opioid analgesia was compared across
treatment groups through 24, 48, 72, and 96 hours after surgery, as described in the table below.
Performance of Three XaraColl 50mg
Implants (150 mg) vs. ON-Q Painbuster
900 mg Continuous Perfusion
|
|
Mean
Total Use of Opioid Analgesia
(TOpA; mg IV morphine equivalent)
|
|
|
|
|
|
|
|
Time Post-operative
|
|
On-Q
900 mg
(n=13)
|
|
|
XaraColl
150
mg
(n=14)
|
|
|
Mean
reduction
|
|
|
p-value
|
|
24 hours
|
|
|
67.0
|
|
|
|
46.9
|
|
|
|
30
|
%
|
|
|
0.067
|
*
|
48 hours
|
|
|
74.9
|
|
|
|
55.4
|
|
|
|
26
|
%
|
|
|
0.100
|
*
|
72 hours
|
|
|
85.4
|
|
|
|
62.0
|
|
|
|
27
|
%
|
|
|
0.089
|
*
|
96 hours
|
|
|
90.8
|
|
|
|
67.9
|
|
|
|
25
|
%
|
|
|
0.129
|
|
*depicts a statistical trend if < 0.1.
Despite delivering only one-sixth (17%)
of the total ON-Q bupivacaine dosage, we demonstrated that XaraColl was potentially more effective in providing post-operative
analgesia than continuous bupivacaine infusion over 72 hours, with statistical trends towards reduced opioid consumption in favor
of XaraColl through 24, 48 and 72 hours. We believe that by implanting XaraColl at different depths within the surgical wound,
we may target delivery of anesthetic to the major sites of surgical trauma more efficiently than is possible with continuous infusion
via an indwelling catheter.
Phase 3 Pharmoacokinetic & Safety Trials
In the second half of 2014, we commenced
a multicenter, blinded, randomized, single dose study in the United States in subjects scheduled for elective inguinal hernioplasty
via open laparotomy. The objectives of this study were to determine the pharmacokinetics and relative bioavailability, and to
evaluate the safety of XaraColl 200 mg and XaraColl 300 mg as compared to the bupivacaine 150 mg infiltrate containing epinephrine.
All subjects had measurable bupivacaine plasma concentrations 30 minutes after sponge implantation or infiltration. Mean bupivacaine
plasma concentrations were comparable between the XaraColl 200 mg group and the bupivacaine 150 mg infiltration group through
the first 24 hours after study drug administration. From approximately 25 hours after dosing through the end of
the 96-hour observation period, mean bupivacaine
plasma concentrations were higher in the XaraColl 200 mg group compared with the bupivacaine 150 mg infiltration group suggesting
the availability of more drug over the observation period in the XaraColl group compared with the bupivacaine 150 mg infiltration
group.
Mean bupivacaine plasma concentrations
were higher in the XaraColl 300 mg group compared with the XaraColl 200 mg and the bupivacaine 150 mg infiltration group throughout
the 96-hour observation period. Mean plasma concentrations in the XaraColl 300 mg group peaked at 3 hours, and bupivacaine concentrations
in this group were sustained above the peak level attained in both the bupivacaine 150 mg infiltration and XaraColl 200 mg groups
from 1 hour through 24 hours after implantation/administration of study drug. At 72 hours and 96 hours, mean plasma concentrations
of bupivacaine in the XaraColl 300 mg were nearly double that of the XaraColl 200 mg group. The highest individual bupivacaine
plasma concentration in this study was 777 ng/mL for a subject in the XaraColl 300 mg group. This concentration is 2.5 times lower
than the threshold concentration that has been associated with signs and symptoms of bupivacaine toxicity (2000 ng/mL). Areas
under the plasma concentration time curve (AUC) were dose proportional for XaraColl 200 mg and XaraColl 300 mg relative to the
bupivacaine 150 mg infiltration. The relative maximum concentrations (Cmax) for XaraColl 200 mg and XaraColl 300 mg were approximately
80% of the Cmax for the bupivacaine 150 mg infiltrate. The mean elimination half-life was approximately twice as long for the
Xaracoll groups compared to the bupivacaine infiltrate. These findings suggest slower release of bupivacaine over time from the
XaraColl bupivacaine sponges compared with the bupivacaine infiltrate.
XaraColl was well tolerated. No adverse
event was considered related to study drug and no adverse event met the criteria for serious. No subject was discontinued due
to an adverse event. No signs or symptoms of bupivacaine toxicity were observed in any patient.
The FDA has reviewed the data from this
study and agreed with Innocoll’s decision to proceed with the evaluation of the single 300mg dose of XaraColl in the subsequent
Phase 3 program.
Pivotal Phase 3 Clinical Trials
In May 2016, we received
data from our pivotal Phase 3 clinical trials for XaraColl. Our MATRIX Phase 3 studies had identical designs and were randomized,
placebo-controlled, double-blinded trials to investigate the safety and efficacy of XaraColl for the treatment of postoperative
pain following open hernia repair with mesh. These trials were undertaken in the United States at 22 sites and 25 sites, respectively.
The MATRIX-1 study enrolled 305 patients and the MATRIX-2 study enrolled 319 patients aged 18 and older and sum of pain intensity
data was evaluated based on a modified intent to treat population (MITT), including all randomized patients who received any dose
of XaraColl or placebo and who had at least one numerical rating pain intensity score prior to discharge. Patients with a unilateral
inguinal hernia undergoing open hernioplasty with mesh placement were treated in one of the two arms per study with either three
100 mg XaraColl matrices for a total dose of 300 mg of bupivacaine hydrochloride, or three placebo matrices. The matrices were
placed at the site of the hernia repair in order to provide local levels of bupivacaine directly at the location of surgical trauma.
Patients received background medication of 650 mg of acetaminophen administered three times daily, with access to opioids, as needed.
The primary efficacy endpoint in both Phase 3 studies was SPI24 (the time-weighted sum of pain intensity) over 24 hours comparing
the XaraColl matrix to placebo. Additional endpoints were SPI at 48 and 72 hours, as well as total opioid use at 24, 48 and 72
hours and time to first opioid use. Safety was evaluated through the collection of adverse events through 30 days postoperatively.
XaraColl showed consistency
across both studies in treatment effect for pain reduction and opioid reduction. The primary efficacy endpoint, the sum of pain
intensity over 24 hours comparing XaraColl to placebo, met statistical significance in both the MATRIX-1 (p=0.0004) and MATRIX-2
(p<0.0001) studies. These highly statistically significant results make XaraColl the first long-acting, opioid-sparing, local
analgesic to meet primary endpoints of Phase 3 clinical trials in hernia repair, a highly painful and commonly performed surgery.
The p-value is a measure of probability that the difference between the placebo group and the XaraColl group is due to chance (e.g.,
p = 0.01 means that there is a 1% (0.01 = 1.0%) chance that the difference between the placebo group and the XaraColl group is
the result of random chance as opposed to the XaraColl treatment). A p-value less than or equal to 0.05 (0.05 = 5%) is commonly
used as a criterion for statistical significance, with p-values of less than or equal to 0.001 considered highly statistically
significant (a less than one in a thousand chance of being the result of random chance).
A key secondary endpoint in the MATRIX
trials was the sum of pain intensity over 48 hours (SPI48). The pooled data of the two MATRIX studies were statistically significant
for this endpoint (p=0.0033). MATRIX-2 achieved a statistically significant result (p=0.0270), and MATRIX-1 trended toward, but
did not achieve statistical significance (p=0.0568). Another key secondary endpoint was the sum of pain intensity over 72 hours
(SPI72). The pooled data of the two MATRIX studies for this endpoint were statistically significant, although neither individual
study achieved statistical significance for SPI72.
The MATRIX trials also looked
at multiple opioid-sparing secondary endpoints such as total use of opioid rescue medication use at 24, 48 and 72 hours and time
to first opioid use. Both trials also demonstrated that XaraColl reduced the total use of opioid rescue pain medication through
24 hours post hernia repair, as both results were highly statistically significant. Both trials demonstrated with statistical significance
that XaraColl increases the time prior to the first use of opioids.
The incidence of overall
adverse events reported in the XaraColl treatment group was similar to the placebo treatment group in both trials, and the incidence
of discontinuation was very low and balanced across the treatment arms and across both studies. There were no XaraColl-related
serious adverse events. Opioid-related adverse events (nausea, vomiting and constipation) were higher in the placebo arms of both
trials.
Plans for Resubmission of NDA
On the basis of the positive data from
our Phase 3 clinical program, we submitted an NDA for XaraColl at the beginning of the fourth quarter of 2016 and subsequently
received a Refusal to File letter on December 23, 2016 from the FDA. In February 2017, our representatives attended a Type-A meeting
with representatives of the FDA to review potential pathways forward following our receipt of the Refusal to File Letter and to
review a proposed plan for proceeding with additional studies that would allow us to file a revised NDA for XaraColl. During the
meeting, we proposed a plan designed to allow us to submit a revised NDA to the FDA by the latter part of 2017. We proposed conducting
an additional short-term pharmacokinetic study and several short-term non-clinical studies. Under current practice before the
FDA, we received limited feedback during the meeting and we expect to receive shortly from the representatives of the FDA formal
written meeting minutes of our Type-A meeting, which will serve as the official record of the response of the FDA to our proposal
during the meeting. If the FDA concurs with our plan, we will commence the additional studies, and if the results are positive,
we would submit a revised NDA to the FDA soon after the completion of the studies. However, if the FDA suggests that studies beyond
those that we proposed would be necessary, or if the results of the studies that we proposed are not positive, we would not likely
be able to submit our revised NDA for an extended period of time, if at all.
Cogenzia (INL-002)
Cogenzia, is a topically applied, bioresorbable
collagen sponge for the treatment of DFIs. We designed Cogenzia to release a high dose of gentamicin directly at the site of DFIs.
After surgical debridement to remove any necrotic tissues, the Cogenzia sponge is applied daily to the DFI and covered with a
secondary wound dressing. Cogenzia is highly flexible and will take the shape of the wound bed, minimizing exudate build-up. A
high local concentration of gentamicin would penetrate the wound directly, delivering an optimal concentration of drug precisely
where it is needed with minimal systemic absorption. The type-1 collagen in Cogenzia, manufactured using our proprietary technologies,
is a natural and well-established biocompatible material that can help stimulate the growth of new tissue in the wound bed and
accelerate the natural process of wound healing.
Gentamicin is typically delivered systemically
which limits maximum possible dosage levels due to its adverse effects and toxicity risks on patients at higher dosage levels.
Therefore, it has historically only been used to treat Gram negative bacteria. However, gentamicin’s antibacterial efficacy
is concentration dependent, and at higher dose levels has been shown to provide broad spectrum coverage of both Gram positive
and Gram negative bacteria including methicillin-resistant Staphylococcus aureus, or MRSA, all of which may be present in DFIs.
The chart below compares published information
of the estimated gentamicin concentration levels achievable by delivering gentamicin locally with Cogenzia compared to the peak
safe serum levels obtained from systemic delivery. In a published study by Stemberger et al., it was demonstrated that gentamicin
begins to achieve broad spectrum microbial coverage at 16 μg/ml and reaches complete broad spectrum coverage at concentrations
of >512 μg/ml, both of
which exceed the maximum safe peak serum
level of gentamicin when delivered systemically (10-12 μg/ml). According to a publication by Dr. Benjamin Lipsky et al., Cogenzia
is expected to deliver local concentrations of gentamicin of approximately 1000 μg/ml, which exceeds the concentration required
to achieve broad spectrum coverage facilitating eradication of pathogens present at the infected wound site.
Comparison of Achievable
Local vs. Systemic Concentrations of Gentamicin
Preliminary data suggested that Cogenzia
is able to deliver a higher dose of gentamicin locally at the infection site than can be achieved by systemic delivery, providing
broad spectrum coverage of bacteria safely without the side effects and toxicity risks associated with systemic delivery at higher
dosage levels, while minimizing the risk of resistance. There are currently no topical agents approved for the treatment of DFIs.
We believe this topical route of administration, in combination with systemic antibiotic therapy, has the potential to become
the standard of care first line treatment of all types of DFIs, including mild, moderate and severe infections.
We filed an IND for Cogenzia in November
2006. The clinical protocols for our Phase 3 registration trials were agreed upon with the FDA under an SPA, and have also been
accepted by the EMA under the Scientific Advice procedure. We initiated the Cogenzia Phase 3 clinical program in both the United
States, Australia and Europe during 2016.
Cogenzia Clinical Data
Phase 2 Clinical Trial in Diabetic Foot Infections
In our multicenter, randomized, placebo-controlled
Phase 2 trial involving 36 patients, Cogenzia (50 mg or 200 mg) was applied daily for up to 28 days in combination with systemic
antibiotic therapy for the treatment of moderately-infected diabetic foot ulcers, with the control group receiving systemic therapy
alone. Patients were treated for at least 7 days and continued treatment until the investigator determined that all signs and
symptoms of infection had resolved, up to a maximum of 28 days. A final test-of-cure and safety assessment for each patient was
performed 2 weeks after completion of treatment. The investigator performed clinical assessments at regular study visits while
the patient was undergoing antibiotic therapy (i.e., days 3, 7, 10, 14, 21, and 28) and again at the final two-week follow-up
visit. The primary efficacy endpoint for this trial was the percentage of patients with a clinical outcome of “clinical
cure” (defined as the complete resolution or elimination of infection) at the study visit on day 7 of treatment. This study
visit was selected as the primary endpoint because statistical calculations suggested that we would need a substantially larger
sample size to test for treatment superiority at the later study visits. Our primary endpoint of clinical cure at 7 days after
treatment, however, was not achieved. At the final test-of-cure visit approximately two weeks after completion of treatment, however,
all evaluable patients in the treatment group achieved clinical cure. Nevertheless, since 100% of the patients who received Cogenzia
and who completed the trial achieved a clinical cure, the trial results demonstrated a statistically significant improvement in
cure rate at the final test-of-cure visit, despite the relatively small sample size. Below is a summary of the data from this
trial based on the modified intent-to-treat, or mITT, population, modified to include only patients who had been randomized to
the Cogenzia and control arms and not earlier terminated from the study for failure to comply with the study inclusion criteria.
Patients with Clinical Outcome of
Clinical Cure at Final Test-of-Cure
Modified Intent-to-Treat Population (mITT)
|
|
Cogenzia
(n=22)
|
|
|
Control
(n=10)
|
|
|
p-value
|
|
Completed subjects (n=32)
|
|
|
22
|
|
|
|
100.0
|
%
|
|
|
7
|
|
|
|
70.0
|
%
|
|
|
—
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
Cogenzia
(n=26)
|
|
|
Control
(n=10)
|
|
|
p-value
|
|
All subjects (n=36)
|
|
|
22
|
|
|
|
84.6
|
%
|
|
|
7
|
|
|
|
70.0
|
%
|
|
|
0.024
|
*
|
*
statistically significant
Based on the mITT population, a significantly
higher proportion of patients reached clinical cure than did the control group (100% versus 70.0%, p = 0.024). Accordingly, clinical
cure at test-of-cure, measured approximately 10 to 14 days after the last dose of treatment has been administered, has been set
as the primary endpoint of the Phase 3 trials for Cogenzia, as accepted by the FDA under our SPA as well as by the EMA.
Secondary endpoints of the trial included
the percentage of patients with pathogen eradication at each time point, and time to eradication of baseline pathogens. Importantly,
the Cogenzia group demonstrated a statistically significant higher rate of baseline pathogen eradication at all study visits (p
≤
0.038) and a significantly reduced time to pathogen eradication
(p < 0.001), as shown in the table below.
Baseline Pathogen Persistence
By achieving a complete eradication of
all pathogens at the wound site at study visits on day 28, as demonstrated by microbiological testing, the use of Cogenzia in
DFIs prepares the underlying wound for healing. Since diabetic foot ulcers generally cannot heal in the presence of infection,
a pathogen free wound site provides patients an unmatched opportunity to achieve a complete healing of the ulcer, thereby substantially
reducing the risk for both reinfection and potential amputation. Treatment by current systemic antibiotic therapy frequently leads
to wounds that ostensibly appear to be free of infection but still prove to have a high level of residual pathogens. It is clinically
meaningful that in our Phase 2 trial, Cogenzia achieved both a 100% clinical cure and 100% eradication of all pathogens at the
wound site, thereby potentially providing practitioners with a high degree of comfort that a wound which appears to be free of
infection is in fact free of infection. This important outcome, we believe, offers the potential for Cogenzia to become the recognized
standard of care for the treatment of DFI’s. As the risk of reinfection for patients treated by systemic antibiotic therapy
alone is high, this often results in further courses of antibiotic treatment, along with the potential for hospitalization where
IV antibiotics are administered. We believe the use of Cogenzia in combination with systemic antibiotic therapy can be much more
effective at eradicating the infecting pathogens than systemic antibiotic therapy alone, providing for an overall improved patient
outcome at substantially lower costs than those incurred if hospitalization is required.
Our Phase 2 trial also demonstrated that
Cogenzia was safe, well tolerated and conducive to ulcer healing. The proportion of patients experiencing any adverse event was
similar for the treatment (28.9%) and control (27.8%) groups. The most common adverse events occurring in at least two patients
per group were infected skin ulcer, tinea pedis and increased blood creatinine level. There were no clinically or statistically
significant changes in laboratory tests values or vital signs. Most adverse events were mild or moderate, but there were six serious
adverse events, including five in the Cogenzia treatment group (hypoglycemia, renal failure, cellulitis, tendon rupture and wound
hemorrhage), all of which resolved, and one in the control group. Only one patient in the treatment group experienced an adverse
event (moderate renal failure) that was considered definitely or probably related to the trial and resolved by the final visit.
One clinically improved patient was withdrawn from the trial due to an adverse event (hypoglycemia) that was unrelated to Cogenzia.
United States and European Registration Trials
We conducted two identical, randomized,
placebo-controlled, blinded trials, enrolling over 500 patients each, under our SPA with the FDA, in patients with moderate to
severe DFIs. Our trial protocols agreed to with the FDA in the SPA, and subsequently reaffirmed in 2014, have also been accepted
by the EMA under the Scientific Advice procedure. Each trial consisted of three arms, (1) Cogenzia, (2) placebo collagen
matrix or (3) no collagen matrix. In each arm, Cogenzia was used as adjuvant therapy in combination with a systemic antibiotic.
Patients were treated for up to a maximum of 28 days and the investigator stopped the trial treatment if a patient
achieved clinical cure on or after day 14. The primary endpoint was clinical cure at the test-of-cure visit approximately
10 days after the last dose of treatment was administered with co-primary endpoints, including (i) Cogenzia compared to
placebo and a systemic antibiotic, and (ii) Cogenzia compared to a systemic antibiotic alone. Follow-up visits with enrolled patients
are scheduled to occur at 10, 30, 60 and 90 days after the last dose of treatment was administered to assess ulcer closure
and re-infection. Planned secondary endpoints included (1) clinical cure time (percentage of patients at each visit), (2)
positive clinical response (percentage of patients at each visit), (3) pathogen eradication time (percentage of patients at each
visit), (4) microbiological outcomes, (5) surgical intervention, or (6) amputation and re-infection. We commenced the trials in
the first quarter of 2015.
Discontinuation
While there were trends toward clinical
response (clinical cure plus improvement) in the Cogenzia arm and the placebo collagen-matrix arm, neither study achieved statistical
significance on their shared primary endpoint of clinical cure after 28 days. While Innocoll continued to analyze sub populations
of patients within the studies, the full dataset confirmed that the addition of gentamicin delivered topically through Cogenzia,
in conjunction with SOC, does not confer sufficient additional clinical benefit over the placebo collagen matrix, administered
with SOC, or SOC alone, in moderate to severe diabetic foot ulcer infections. There was a suggestion that Cogenzia may be more
beneficial in more severely infected ulcers with difficult to treat pathogens as the underlying causative organisms. The sample
size of this sub population was, however, too small even in the pooled data to draw any definitive conclusions.
Cogenzia and the placebo collagen-matrix
were well-tolerated in both studies. Incidence of overall adverse events was similar across all three treatment arms in
the two Phase 3 studies.
This clinical development program (COACT
program) for Cogenzia was discontinued in the fourth quarter 2016 following the failure of these Phase 3 trials to meet their
primary end point of clinical cure of infection after 28 days versus either placebo plus SOC or SOC alone.
CollaGUARD
CollaGUARD is our translucent, bioresorbable
collagen film for the prevention of post-operative adhesions in multiple surgical applications, including digestive, general,
colorectal, gynecological and urological surgeries, in both open and laparoscopic approaches. It is approved in 12 countries outside
of the United States for the prevention of post-operative adhesions and may be used in patients undergoing laparotomy or laparoscopic
surgeries. When tested in vivo, CollaGUARD increased the probability of remaining adhesion-free by more than six fold (p 0.001)
and significantly reduced the extent and severity of adhesions (p 0.001) versus no anti-adhesion product. CollaGUARD has been
designed and engineered with a unique combination of features for optimal handling, ease-of-use, hemostatic properties and anti-adhesion
performance. The film, which is applied directly to tissue surfaces, is translucent allowing constant visibility of the surgical
field. It is highly stable at room temperature, does not require any special storage or advanced preparation before use and has
up to a five-year shelf life.
The product is non-tacky, non-sticky and
can be easily rolled for insertion through a trocar when implanted laproscopically. CollaGUARD is also fully biodegradable and
is designed to be safely and completely resorbed over approximately three to five weeks post implantation. CollaGUARD is available
in a wide variety of sizes up to 30 x 20 cm and may be cut and sutured if required and, therefore, can be used easily across a
broad range of surgeries. CollaGUARD is regulated as a Class III device in the United States and we expect it will require a single
pivotal clinical trial for PMA by the FDA. In the first quarter of 2015, we initiated a second pilot efficacy study in patients
undergoing gynecological laparoscopic adhesiolysis. However, we decided to terminate the second pilot efficacy study in favor
of a planned pilot efficacy study in patients undergoing myomectomy via open laparotomy to be performed in the U.S. under an IDE.
We anticipate that data from this pilot study will help us to finalize the design of the U.S. pivotal study protocol. In the fourth
quarter of 2015, we completed a pilot clinical study for CollaGUARD, run in the Netherlands, in patients undergoing intrauterine
adhesiolysis via operative hysteroscopy. A clinical study report for this study confirmed the ease of use and safety for CollaGUARD
in this patient population. We held our pre-IDE submission meeting with the FDA in the first quarter of 2016, in which we agreed
on a non-clinical development plan. Based on subsequent discussions with the FDA, we will be required to complete additional non-clinical
studies. We intend to resubmit the IDE to the FDA in the second half of 2017, assuming we have sufficient funding to do so. We
submitted a family of patent applications aimed at protecting CollaGUARD on an international basis, including Australia, Canada,
Eurasia, Europe, Japan, Mexico, and the United States, which is currently in the examination phase. If issued, these patents are
expected to expire in 2033 or later in the United States.
Surgical Adhesion Market
Adhesions are fibrous bands of scar tissue
that abnormally bind together two anatomic surfaces, and can develop naturally after surgery as part of the healing process. Post-surgical
adhesions occur in almost 95% of patients who have had multiple laparotomies. Complications associated with post-operative adhesions
can be severe, including chronic abdominal pain, bowl-obstruction, infertility in women, and joint immobilization, among others.
Adhesions can also make second surgeries more complicated and even dangerous, depending on their extent and severity, as surgeons
may have difficulties reaching and separating tissues, the median abdominal opening time increases threefold for repeat surgery
patients, and increased surgical procedure and re-entry time means increased costs and increased risk of infection to the patient.
Adhesions cause over 40% of all intestinal obstructions and 60% to 70% of small bowel obstructions. Approximately 35% of patients
who underwent open abdominal or pelvic surgery were readmitted due to adhesion-related problems. In the United States alone, there
are approximately 350,000 hospitalizations and $2.3 billion spent annually on surgery to remove adhesions formed following gynecologic
or abdominal surgeries. According to Global Industry Analysts Inc., the global market for anti-adhesion products was estimated
to be $1.3 billion in 2014. The market is mainly driven by increasing surgeon attention towards anti-adhesion products along with
the development of new products addressing unmet requirements. The current products available on the market include four basic
formulations: gels, films, sprays and liquids. Polymeric film is the most widely used anti-adhesion device to separate as well
as isolate wounded tissues following a surgical procedure. However, existing products have a number of disadvantages including
poor handling properties, limited efficacy, limitations to applicable surgical settings (i.e., open
or laparoscopic procedures) and strict product
warnings and contraindications. We believe that CollaGUARD has the ability to address these unmet needs and become a “best-in-class”
product.
Although the leading products that compete
with CollaGUARD are approved for use in open surgery, only one is approved for use laparoscopically. Accordingly, we believe CollaGUARD
offers significant advantages over anti-adhesion products currently on the market, such as Sanofi’s Seprafilm®, Baxter’s
Adept®, Ethicon’s Interceed® and Mast Biosurgery’s Surgiwrap®. Each of these products has one or more
of the following limitations or contraindications:
|
·
|
tacky, has
to be kept in packaging until placed into the surgical site;
|
|
·
|
must be brought
to temperature, limit to amount used;
|
|
·
|
cannot be overlapped
on itself or other organs;
|
|
·
|
must be sutured
in place;
|
|
·
|
cannot be used
laparoscopically;
|
|
·
|
leak potential
if wrapped around intestinal anastomosis;
|
|
·
|
reports of
pulmonary edema / effusion and arrhythmia; or
|
|
·
|
risk of damage
by excessive activity, requiring removal.
|
CollaGUARD Pre-Clinical Data
CollaGUARD is regulated as a Class III
device in the United States. In our pre-clinical animal trial with CollaGUARD, we have studied the performance, primary and secondary
endpoints and safety of CollaGUARD in rats. This method is a well-established and well-recognized surrogate for human testing
and was used to support regulatory approval in Europe and many other countries outside of the United States. The trial was conducted
in two stages, comparing the safety and performance of CollaGUARD in stage 1 to an untreated control group and in stage 2 to Prevadh®,
a commercially available collagen-based adhesion product approved in Europe. Prevadh, which also consists of collagen among other
component materials, was deemed to be the closest comparison to CollaGUARD among marketed products. In the first trial stage,
CollaGUARD demonstrated superiority over the control group in both the prevalence and severity of adhesions which was significantly
lower compared to the control group (p < 0.001). In stage 2 of this trial, we demonstrated equivalent outcomes in the prevalence
(p = 0.625) and severity (p = 0.317) of adhesions between CollaGUARD and Prevadh.
Percentage of
Rats Adhesion Free Following
Abdominal Abradement
CollaGUARD United States Trial
Because CollaGUARD is regulated as a Class
III device in the United States, we expect that it will require a single pivotal clinical trial for PMA by the FDA. We held our
pre-IDE submission meeting with the FDA in the first quarter of 2016, in which we agreed on a non-clinical development plan that
will be completed and reported prior to our filing a full IDE package, which we expect to file in the second half of 2017,
with the Pilot (Feasibility) Clinical Study to be initiated immediately after approval.
CollaGUARD Commercialization Strategy
CollaGUARD has been approved in 12 countries
within Asia, Latin America and the Middle East and we are preparing for launch in many of these countries through our established
distribution arrangements, in place with 18 partners. One of our most significant distribution arrangements is with Takeda, which
launched and distributed CollaGUARD in Russia in 2014 and planned to add additional territories in 2015. A second important partnership
for CollaGUARD is with Pioneer, to whom we have granted rights to the product in China and several ASEAN countries. Pioneer is
in the pre-launch phase for the product in a number of these countries. Further launches with partners in other Asian countries,
the Middle East and Europe were planned throughout 2015.
Subject to receipt of adequate funding, we plan to commercialize
CollaGUARD in the United States. Since surgeons represent the primary physician audience for both Xaracoll and CollaGUARD, the
same hospital formulary decision makers would be critical purchasers of both products. This complementary customer base will allow
us to aggregate a single point of sale for both XaraColl and CollaGUARD, and utilize the same sales team to effect these sales,
thereby enhancing the efficiency of our potential commercial sales footprint.
Recertification of CollaGUARD in Europe
The initial European CE certificate for
CollaGUARD was valid from October 7, 2011 to July 26, 2015. In accordance with normal practice for device recertification, we
compiled an updated Design Dossier and submitted this to our European Notified Body (TÜV SÜD, Munich, Germany) in December
2014. As part of our application for recertification, we included an updated literature-based Clinical Evaluation Report and a
Post Market Clinical Follow-up (PMCF) Plan, which rationalized the objectives of our ongoing clinical investigations in accordance
with the current 2012 European Guideline for PMCF studies. However, prior to the expiration of the original certificate, the Notified
Body requested that we revise our PMCF plan to additionally include a direct clinical comparison of CollaGUARD’s performance
and safety compared to another CE-certified adhesion barrier. We do not believe that current European medical device regulations
specifically require that our PMCF plan includes such a clinical comparison. In March 2016, we met with the Notified Body to seek
clarification. At the meeting, TÜV SÜD agreed that current European medical device regulations do not specifically require
that our PMCF plan includes such a clinical comparison, and agreed with our proposal for an updated PMCF based on the pilot clinical
study in open myomectomy patients, as was agreed with FDA at the pre-IDE meeting. Provided TÜV SÜD determines that the
clinical data from the U.S. pilot study are supportive, then recertification would be possible at that time based on an updated
Technical Dossier and Clinical Evaluation. Until a new CE-certificate has been issued, we will not supply CollaGUARD to our marketing
partners for sale in Europe or other affected territories. Accordingly, no such sales have been assumed in our financial forecasts.
Other Products
In addition to our lead product candidates,
we have the following additional products approved or commercialized:
Marketed and Partnered Products
|
|
|
|
Product
|
Indication
|
Region (Partner)
|
|
|
|
COLLATAMP®G*
|
Surgical Infections
|
Ex-US (EUSA)
|
REGENEPRO®**
|
Dental Wounds
|
US (Biomet 3i)
Ex-US (Biomet 3i)
|
ZORPREVA®***
|
Surgical Hemostat
|
Ex-US (Pioneer)
|
SEPTOCOLL®E****
|
Surgical Infections
|
Ex-US (Biomet)
|
COLLAGUARD®*****
|
Surgical Adhesion Prevention
|
Ex-US (various partners)
|
*COLLATAMP®G is a registered trademark
of EUSA/Jazz Pharmaceuticals
**REGENEPRO® is a registered trademark
of Biomet 3i
***ZORPREVA® is a registered trademark
of Innocoll Pharmaceuticals Ltd.
****SEPTOCOLL®E is a registered trademark
of Biomet Deutschland GmbH
*****COLLAGUARD® is a registered trademark
of Innocoll Pharmaceuticals Ltd.
In addition to our late-stage product candidates
described above, we develop and manufacture a range of additional biodegradable surgical implants and topically applied pharmaceutical
products and medical devices using our proprietary collagen-based technologies. We produce our products and product candidates,
such as CollatampG surgical implant, RegenePro and Septocoll, in a range of topical and implantable forms, including sponges,
films, membranes and gels, compatible with a variety of therapeutics, including hydrophobic and hydrophilic active ingredients
and small
molecules and biologics. A number of our
products have been marketed for several years. For example, our CollatampG Gentamicin Surgical Implant, a perioperative surgical
implant comprised of a lyophilized collagen matrix impregnated with a broad spectrum antibiotic is currently approved for sale
in 62 countries across Africa, Asia, Europe, Latin America and the Middle East. EUSA Pharma acquired the rights to distribute
CollatampG in all worldwide markets, excluding the United States. In addition, we have an exclusive License and Distribution Agreement
with Biomet 3i for our range of CollaCare Dental products, branded RegenePro, covering all global territories outside of China
and ASEAN, for which we have partnered with China Pioneer Pharma Holdings Ltd. Biomet 3i launched RegenePro in July 2014 in the
United States and, having recently received approvals in the European Union, also has plans for a European launch. We also supply
Septocoll, a surgical implant, to Biomet which markets the product in Europe and the Middle East. These agreements with our partner
are exclusive manufacturing and supply arrangements (see below “— Commercial Partners and Agreements”) pursuant
to which we exclusively supply, and the partner is required to exclusively purchase, the products for the respective territories.
The majority of our agreements contain minimum or specified purchase requirements and in addition, pursuant to our agreement with
Takeda, we receive payments upon achievement of certain regulatory milestones.
Our Collagen Based Technology Platform
All of our products and product candidates
are based on our proprietary collagen technology platform, which includes CollaRx, a lyophilized sponge which is the basis of
our XaraColl product and CollaFilm, a film cast membrane which is the basis of CollaGUARD. We utilize highly purified biocompatible,
biodegradable and fully bioresorbable type-1 bovine and equine collagen. Type 1 collagen is the primary fibril-forming collagen
in bone, dermis tendons and ligaments and is the most abundant protein in the human body. Our collagen plays an integral role
in the repair and replacement of both soft and hard tissue by providing an extracellular scaffold, stimulating certain growth
factors and promoting tissue healing. We perform the extraction and purification of collagen from either bovine or equine Achilles
tendons using a proprietary process at our manufacturing facility. The purified collagen is then incorporated into our technology
platform, to create topical and implantable products that combine proven therapeutics with improved localized drug delivery and
superior handling properties. Our proprietary processes and technologies also enable us to finely control the texture, consistency,
drug elution dynamics, resorption time and other physical characteristics of the finished product. These characteristics provide
meaningful differentiation of our products leading to superior performance and an overall improved user experience, because they:
|
·
|
can be applied
to a topical wound, surgically implanted, or injected into a subcutaneous tissue defect
or joint;
|
|
·
|
are fully biocompatible,
bioresorbable and biodegradable;
|
|
·
|
are suitable
for a wide range of active ingredients (hydrophilic, lipophilic and macromolecules),
including combinations thereof;
|
|
·
|
allow for versatile
drug loading capability from micrograms to grams of single or multiple active ingredients;
|
|
·
|
provide for
a rate of drug release that can be controlled by formulation and process variations;
|
|
·
|
utilize ready-to-use
formats for ease of administration - no need for any mixing in the operating theatre;
and
|
|
·
|
allow certain
of our surgical products to be implanted using laparoscopy and are easily manipulated
according to the site of application.
|
Our technologies have been fully scaled
up and in some cases commercialized and our manufacturing processes are well controlled and cost efficient.
Manufacturing
Our wholly-owned subsidiary, Syntacoll
GmbH, located in Saal, Germany, is our commercial-scale manufacturing division which exclusively produces both clinical and commercial
supply for all our products on a global basis. We believe our ability to manufacture our products allows us to control more effectively
the quality and cost of manufacturing, which will enable us to achieve higher operating margins. We have a fully integrated and
reliable manufacturing process in Saal, beginning with the extraction and purification of the type-1 collagen (from bovine and
equine Achilles tendons), which is further processed using one of our proprietary technologies to produce final finished products
in the forms of matrices, films, powders, liquids, and gels. We have qualified multiple sources for bovine and equine tendons,
and conduct a rigorous quality control process on the raw materials, locally at our Saal facility. These raw materials are readily
available to us from multiple sources at stable pricing. Several of our products, including CollaGUARD, CollatampG, Septocoll
and RegenePro, are marketed in countries around the world. Our proprietary technologies have been fully validated. Syntacoll was
established in Germany in 1975 and has been manufacturing commercial products based on collagen technology since 1985. Our manufacturing
staff is highly qualified and experienced due to Syntacoll’s long history of producing collagen-based products. Our manufacturing
facility has been approved in Germany for compliance with current Good Manufacturing Practice, or cGMP, but has not yet been
inspected by the FDA for cGMP compliance. Our manufacturing facility is ISO 13485 certified in Europe and Canada. In our 30
years of producing collagen-based products, we have not experienced any significant quality issues or recalls. We believe we currently
have adequate production capability to support our current production needs and planned trials and commercialization efforts for
XaraColl. In addition, we have substantially completed our capacity expansion build-out of our production facility to significantly
increase capacity
.
Once completed and approved, we anticipate that our production capacity will be sufficient to meet currently
forecasted market demand for all our current and late-stage pipeline product candidates.
Intellectual Property and Exclusivity
In the ordinary course of our business,
we seek to protect our products, product candidates and technology through a combination of patents, trademarks, processes, proprietary
know-how, regulatory exclusivity and contractual restrictions on disclosure.
Our knowledge base and expertise in collagen-based
drug delivery and the related trade secrets play an important role in protecting our collagen-based products, product candidates
and technology and provide protection apart from patents and regulatory exclusivity. The scale-up and commercial manufacture of
XaraColl and the use of our technology platform involve processes and in-process and release analytical techniques that we believe
are unique to us. We have developed the manufacturing processes which we employ in our manufacturing facility for over twenty
years, and they include all aspects of the sourcing, extraction and purification of raw source collagen, formulation and cost
effective processing of collagen to exhibit the characteristics that are necessary for the effective release of precisely specified
amounts of drug product over measured periods of time.
We also employ a strategy of filing patent
applications, where possible, to seek patent protection for certain aspects of our compositions, formulations, and processes.
We are continually evaluating and refining our patent prosecution strategy and evaluating the defensive strength of our patent
position.
Patents and Patent Applications
XaraColl
. A U.S. patent directed
to XaraColl and entitled “Drug delivery device for providing local analgesia, local anesthesia or nerve blockade”
was issued in October 2011 with claims directed to products comprising any amino amide and/or amino ester anesthetic in a collagen
matrix intended for the provision of local analgesia or anesthesia over about 24 hours or longer. Its earliest filing date is
March 28, 2007. The corresponding European application was issued as a patent in May 2016, and the corresponding Japanese application
was issued as a patent in September 2013, while the corresponding application in Ireland was issued as a patent in October 2011.
In March 2015, we submitted a petition
to reissue the U.S. patent directed to XaraColl, mainly for the purposes of submitting prior art references identified in the
corresponding European application. We did not submit these prior art references to the U.S. Patent and Trademark Office during
the prosecution of the U.S. patent. In addition, this reissue process will allow us to pursue additional claims, e.g., claims
within the scope of the originally issued claims but more tailored to our currently proposed XaraColl product. However, there
can be no assurance that any or all of the originally
issued claims will be reissued. It is also
uncertain whether any or all of the additional claims we have included in the petition will be granted. We anticipate the conclusion
of the reissue process before we launch XaraColl in the United States, and if the reissued claims are substantially the same as
the originally issued claims, there will be no intervening rights by others during the reissue period. We will be unable to enforce
the XaraColl U.S. patent unless and until the U.S. patent is reissued.
There can be no assurance that a patent
will reissue from the petition, or that any such patent will be enforceable and will not be challenged, invalidated or circumvented.
Notwithstanding the application for reissuance, we will continue to rely upon our proprietary know-how, techniques, expertise
and the decades of collective experience of our team relating to the development and manufacturing of collagen matrix products,
as well as the rigorous regulatory barriers applicable to the development, manufacture, distribution and marketing of potential
competing products. See “Item 1A. Risk Factors―Risks Related to Our Intellectual Property—Because we have filed
a petition for reissuance of our U.S. XaraColl patent, we will be unable to enforce it unless and until the U.S. patent is reissued.”
Cogenzia
. We have filed patent applications
in each of the United States, Europe, Canada, and Australia specifically related to Cogenzia with an earliest filing date of April
11, 2011. These applications are entitled “Methods for treating bacterial infection” and directed to the local treatment
of bacterial infections with an aminogylcoside antibiotic dispersed in a collagen matrix when used in combination with systemic
administration of other antibacterial agents. If and when issued, we expect patent protection for Cogenzia in the United States
and Europe to expire at the earliest in 2031.
CollaGUARD
(US Market). We have
also filed patent applications in each of the United States, Europe, Canada, Australia, Japan, Mexico, and Eurasia entitled “A
modified collagen” with an earliest filing date January 9, 2012, which is directed to an improved process for manufacturing
the next generation of CollaGUARD, e.g., CollaGUARD currently being developed for the U.S. These patent applications are also
directed to the current manufacturing process for XaraColl. If and when issued, these patents are expected to expire in 2033 or
later in the United States.
CollaPress Technology. Our proprietary
CollaPress technology is described in the issued European patent entitled “Novel collagen-based material with improved properties
for use in human and veterinary medicine and the method of manufacturing such,” which expires on March 9, 2020. It has been
nationalized and maintained in 6 European countries: France, Germany, Italy, Spain, Sweden and the United Kingdom. The patent
is directed to collagen membranes with improved mechanical and fluid-absorption properties which may be produced by thermal compression.
The technology patent is currently utilized in our ProColl™ wound management device and may also be used for the development
of other proprietary, bioresorbable tissue reinforcement implants and/or as implantable delivery systems for biologically active
substances such as hemostatic agents, growth factors, cytokines and drugs.
Trade Secrets and Proprietary Information
Trade secrets play an important role in
protecting our collagen-based products, product candidates and technology and provide protection beyond patents and regulatory
exclusivity. The scale-up and commercial manufacture of XaraColl and the use of our technology platform involve processes and
in-process and release analytical techniques that we believe are unique to us. We seek to protect our proprietary information,
including our trade secrets and proprietary know-how, by requiring our employees, consultants and other advisors to execute proprietary
information and confidentiality agreements upon the commencement of their employment or engagement. These agreements generally
provide that all confidential information developed or made known during the course of the relationship with us be kept confidential
and not be disclosed to third parties except in specific circumstances. In the case of our employees, the agreements also typically
provide that all inventions resulting from work performed for us, utilizing our property or relating to our business and conceived
or completed during employment shall be our exclusive property to the extent permitted by law. Where appropriate, agreements we
obtain with our consultants also typically contain similar assignment of invention obligations. Further, we require confidentiality
agreements from entities that receive our confidential data or materials.
Competition
The pharmaceutical and biotechnology industry
is characterized by intense competition and rapid and significant innovation and change. Our competitors may be able to develop
other drugs, drug/device combinations or products that are able to achieve similar or better results than our product candidates
or marketed products. Our competitors include organizations such as major multinational pharmaceutical companies, established
biotechnology companies, specialty pharmaceutical companies and generic drug companies. Many of our competitors have greater financial
and other resources than we have, such as more commercial resources, larger research and development staffs and more extensive
marketing and manufacturing facilities and organizations. Smaller or early-stage companies may also prove to be significant competitors,
particularly through collaborative arrangements with large, established companies. Our competitors may succeed in developing,
acquiring or licensing on an exclusive basis technologies and products that are more effective or less costly than XaraColl, CollaGUARD,
or any other products that we are currently selling through partners or developing or that we may develop, which could render
our products obsolete and noncompetitive. We expect any products that we develop and commercialize to compete on the basis of,
among other things, efficacy, safety, convenience of administration and delivery, price and the availability of reimbursement
from government and other third-party payers. We also expect to face competition in our efforts to identify appropriate collaborators
or partners to help commercialize our product candidates in our target commercial markets.
XaraColl Competition
We anticipate that, if approved by the
FDA for these indications, XaraColl would be used in conjunction with other pain medications, such as acetaminophen and NSAIDs
as part of an advanced multi-modal approach. We believe that XaraColl will primarily be competing with Pacira Pharmaceutical’s
Exparel, a liposome injection of bupivacaine, an amide local anesthetic, indicated for single-dose infiltration into the surgical
site to produce post-operative analgesia. Both Exparel and XaraColl are focused on opioid reduction or elimination as part of
a multi-modal approach to pain relief. In addition, XaraColl will be competing with currently marketed
bupivacaine and opioid analgesics such as morphine, as well as elastomeric bag/catheter devices intended to provide bupivacaine
over several days, which have been marketed by I-FLOW Corporation (now Halyard Health) since 2004.
CollaGUARD Competition
CollaGUARD competes with a number of anti-adhesion
products such as Sanofi’s SEPRAFILM, Baxter’s ADEPT, Ethicon’s INTERCEED and Mast Biosurgery’s SURGIWRAP,
which have been on the market for many years and have established market share. We believe that CollaGUARD has superior handling
properties when compared with competitors and, if and when approved, may include fewer warning and contraindications on the product
label. ADEPT is contraindicated for use in procedures with laparotomy incisions and INTERCEED has a black box warning for laparoscopic
use.
Commercial Partners and Agreements
EUSA Pharmaceuticals
In August 2007, we entered into a Manufacture
and Supply Agreement with EUSA Pharma (Europe) Limited, or EUSA, which was subsequently amended and restated in April 2010. Under
this agreement, we agreed to supply to EUSA its total supply of any Gentamicin-Collagen Implant product owned or commercialized
by EUSA in finished packaged form for commercial supply. We are supplying EUSA with CollatampG under this agreement. In addition,
the parties agreed that EUSA will own and retain all rights to the development data with respect to the product in all countries
worldwide, except for the United States and its territories and possessions and Innocoll will have an exclusive, fully-paid perpetual
license to use the development data with respect to the product in the United States and its territories and possessions. The
agreement has a 10-year term, starting from its original execution date, with automatic renewal for five additional years, unless
written notice of non-renewal is received by either party to the other at least three years prior to the expiration of the term
of the renewal term. In addition, either party may terminate for breach.
Under another agreement with EUSA, dated
April 27, 2010, we are obligated to pay EUSA a royalty on sales of XaraColl in the United States of 5% per year, not to exceed
$6.5 million in total for all years, and 10% of sales outside the United States, not to exceed $2.5 million in total for all years.
Such payments would accelerate under certain circumstances, including if we enter into a third-party agreement covering the development
and commercialization of XaraColl. Prior to the discontinuation of our Cogenzia program, we also agreed to pay a royalty equal
to 10% per year of sales of Cogenzia outside of the United States not to exceed $1.8 million in total for all years, also subject
to acceleration if we enter into a third-party agreement.
Takeda
In August 2013, we entered into a 15-year
License and Supply Agreement with Takeda GmbH, an affiliate of Takeda Pharmaceutical Company Limited, or Takeda, as expanded on
March 24, 2014, pursuant to which we granted Takeda an exclusive license to distribute, promote and sell CollaGUARD Adhesion Barrier
in Armenia, Azerbaijan, Belarus, Canada, Georgia, Kazakhstan, Kyrgyzstan, Mexico, Moldova, Mongolia, Russian Federation, Tajikistan,
Turkmenistan, Ukraine and Uzbekistan for all current and future approved indications of CollaGUARD. Takeda is obligated to launch
the product in the various jurisdictions in its territory, following regulatory approval, where required. Pursuant to the agreement,
Takeda is also required to make a milestone payment upon achievement of regulatory approval in Canada. In addition, we are Takeda’s
sole supplier for CollaGUARD and Takeda is required to purchase an initial quantity of product from us. We have also agreed on
certain annual minimum purchase order requirements and parameters for pricing for future supplies of products. The agreement has
a 15-year term, following the first commercial sale of the products in the various countries in the Takeda territory on a country-by-country
basis, with automatic renewal for five additional years, unless terminated by either party with 12 months advance notice. In addition,
we and Takeda have the right to terminate the agreement for breach and Takeda has the right to terminate the agreement with respect
to Canada only in the event the Canadian marketing authorization is different from the indications granted in the European Union
with severe restrictions that threaten Takeda’s forecasts in Canada.
Biomet Orthopedics
In June 2004, our subsidiary, Innocoll
Technologies Limited, entered into a Manufacturing and Supply Agreement with Biomet Orthopedics Switzerland GmbH, or Biomet Orthopedics,
which was subsequently amended several times, most recently in March 2013. Pursuant to the agreement, we have agreed to exclusively
supply to Biomet Orthopedics and Biomet Orthopedics has agreed to exclusively purchase Septocoll® and Septocoll E®, our
bioresorbable, dual-action collagen sponge product, from us. The agreement provides that all know-how, manufacturing and technical
data, instructions, specifications and experiences as well as all test methods developed in connection with the products, as specified,
are owned by Biomet Orthopedics and we receive a limited royalty-free license to the same for the term of the agreement. Biomet
Orthopedics also supplies us with gentamicin pursuant to the agreement. The agreement automatically terminates on December 31,
2018 and may be terminated by either party for cause prior to that date. We have also agreed on certain annual minimum purchase
order requirements and parameters for pricing for future supplies of products and Biomet Orthopedics has paid to us certain advances
for future supplies of products through the current end of the term.
Biomet 3i, LLC
In April 2013, we entered into an Exclusive
Distribution Agreement with Biomet 3i, pursuant to which we granted Biomet 3i the exclusive right to distribute and sell our RegenePro
range of products in all countries, republics, states, and areas of the world with the exception of Brunei Darussalam, Cambodia,
Hong Kong, Indonesia, Laos, Macau, Malaysia, Myanmar, Philippines, Singapore, Taiwan, Thailand, The People’s Republic of
China and Vietnam. Pursuant to the agreement, Biomet 3i has agreed to not sell or distribute any competitive products in the Biomet
3i territory and to purchase certain minimum amounts of product. The agreement has a 15-year term, can be terminated by either
party during the first two years of the term with six months’ notice and during the remainder of the term with 18 months’
notice. The agreement can also be terminated by either party for breach.
Pioneer Pharma Co. Ltd.
In October 2011, we entered into a Licensing,
Manufacturing and Supply Agreement with Pioneer Pharma Co Ltd., or Pioneer, pursuant to which we granted Pioneer the exclusive
right to distribute and sell CollaGUARD in The
People’s Republic of China, including
the territories of Hong Kong, Macau and Taiwan for adhesion barrier and any other indication approved by EU regulatory authorities
and the FDA. In August 2012, we expanded the territory in which Pioneer has the right to distribute and sell CollaGUARD to include
Brunei Darussalam, Cambodia, Indonesia, Laos, Malaysia, Myanmar, Singapore and Vietnam. Pioneer has agreed not to enter into similar
arrangements for competitive products in its territory. The agreement provides that Pioneer is responsible for compiling, submitting
and maintaining the product’s registration and associated costs in its territory and is required to place agreed-upon minimum
purchase orders within a certain time period after the product gains marketing approval in the Pioneer territory. In addition,
Pioneer is required to make certain scheduled payments which are creditable against future supply of product. The agreement has
a ten-year term and can be terminated by either party for breach.
Government Regulation
Government authorities in the United States
(at the federal, state and local level) and in other countries extensively regulate, among other things, the research, development,
testing, manufacturing, quality control, approval, labeling, packaging, storage, record-keeping, promotion, advertising, distribution,
post-approval monitoring and reporting, marketing and export and import of drug and medical device products such as those we are
developing. Sometimes FDA will apply both drug and medical device controls to the same product when it has both drug and device
components. XaraColl and our other combination product candidates, and CollaGUARD and our other medical device
product candidates or products only marketed in certain countries must be approved or cleared by the FDA before they may be legally
marketed in the United States and by the appropriate foreign regulatory agency before they may be legally marketed in foreign
countries.
United States Drug Development and Review
Drug Development Process
In the United States, the FDA regulates
drugs or drug/device combinations, such as XaraColl, under the Federal Food, Drug, and Cosmetic Act, or FDCA, and implementing
regulations. Drugs are also subject to other federal, state and local statutes and regulations. The process of obtaining regulatory
approvals and the subsequent compliance with appropriate federal, state, local and foreign statutes and regulations require the
expenditure of substantial time and financial resources. Failure to comply with the applicable U.S. requirements at any time during
the product development process, approval process or after approval may subject an applicant to administrative or judicial sanctions.
FDA sanctions could include, among other actions, refusal to approve pending applications, withdrawal of an approval, a clinical
hold, warning and notice of violation letters, product recalls or withdrawals from the market, product seizures, total or partial
suspension of production or distribution injunctions, unfavorable inspections, fines, refusals of government contracts, restitution,
disgorgement or civil or criminal penalties. Any agency or judicial enforcement action could have a material adverse effect on
us. The process required by the FDA before a drug may be marketed in the United States generally involves the following:
|
·
|
Completion
of extensive nonclinical, or preclinical, laboratory trials, preclinical animal trials
and formulation trials in accordance with applicable regulations, including the FDA’s
Good Laboratory Practice, or GLP, regulations;
|
|
·
|
Submission
to the FDA of an IND which must become effective before human clinical trials may begin;
|
|
·
|
Performance
of adequate and well-controlled human clinical trials in accordance with applicable regulations,
including cGCP, regulations to establish the safety and efficacy of the proposed drug
for its proposed indication;
|
|
·
|
Submission
to the FDA of an NDA for a new drug product;
|
|
·
|
A determination
by the FDA within 60 days of its receipt of an NDA to accept the NDA for filing and review;
|
|
·
|
Satisfactory
completion of an FDA inspection of the manufacturing facility or facilities where the
drug is produced to assess compliance with the FDA’s cGMP, regulations to assure
that the facilities, methods and controls are adequate to preserve the drug’s identity,
strength, quality and purity;
|
|
·
|
Potential FDA
audit of the preclinical and/or clinical trial sites that generated the study data in
support of the NDA; and
|
|
·
|
FDA review
and approval of the NDA.
|
Before testing any compounds with potential
therapeutic value in humans, the drug candidate enters the preclinical trial stage. Preclinical trials include laboratory evaluations
of product chemistry, toxicity and formulation, as well as animal trials to assess the potential safety and activity of the drug
candidate. The conduct of the preclinical trials must comply with federal regulations and requirements including GLP. The sponsor
must submit the results of the preclinical trials, together with manufacturing information, analytical data, any available clinical
data or literature and a proposed clinical protocol, to the FDA as part of the IND. An IND is a request for authorization from
the FDA to administer an investigational drug product to humans. The central focus of an IND submission is on the general investigational
plan and the protocol(s) for human trials. The IND automatically becomes effective 30 days after receipt by the FDA, unless the
FDA raises concerns or questions regarding the proposed clinical trials and places the IND on clinical hold within that 30-day
time period. In such a case, the IND sponsor and the FDA must resolve any outstanding concerns before the clinical trial can begin.
The FDA may also impose clinical holds on a drug candidate at any time before or during clinical trials due to safety concerns,
noncompliance with IND requirements, and other deficiencies. Accordingly, we cannot be sure that submission of an IND will result
in the FDA allowing clinical trials to begin, or that, once begun, issues will not arise that suspend or terminate such trial.
Clinical trials involve the administration
of the drug candidate to healthy volunteers or patients under the supervision of qualified investigators, generally physicians
not employed by or under the trial sponsor’s control, in accordance with GCP, which include the requirement that all research
subjects provide their informed consent for their participation in any clinical trial. Clinical trials are conducted under protocols
detailing, among other things, the objectives of the clinical trial, dosing procedures, subject selection and exclusion criteria,
and the parameters to be used to monitor subject safety and assess efficacy. Each protocol, and any subsequent amendments to the
protocol, must be submitted to the FDA as part of the IND. Further, each clinical trial must be reviewed and approved by an independent
institutional review board, or IRB, at or servicing each institution at which the clinical trial will be conducted. An IRB is
charged with protecting the welfare and rights of trial participants and considers issues such as whether the risks to individuals
participating in the clinical trials are minimized and are reasonable in relation to anticipated benefits. The IRB also approves
the informed consent form that must be provided to each clinical trial subject or his or her legal representative and must monitor
the clinical trial until completed. There are also requirements governing the reporting of ongoing clinical trials and completed
clinical trial results to public registries.
Human clinical trials are typically conducted
in three sequential phases that may overlap or be combined:
|
·
|
Phase 1
.
The drug is initially introduced into healthy human subjects and tested for safety, dosage
tolerance, absorption, metabolism and pharmacologic action of the drug in human distribution
and excretion, the side effects associated with increasing dosages, and if possible,
to gain early evidence of effectiveness. In the case of some products for severe or life-threatening
diseases, especially when the product may be too inherently toxic to ethically administer
to healthy volunteers, the initial human trial is often conducted in patients.
|
|
·
|
Phase 2
.
The drug is evaluated in a limited patient population to identify possible adverse effects
and safety risks, to preliminarily evaluate the effectiveness of the drug for a specific
indication or indications in patients with the disease or condition under study and to
determine dosage tolerance, optimal dosage and dosing schedule. Phase 2 trials are sometimes
further divided into Phase 2a and Phase 2b trials. Phase 2a trials are typically smaller
and shorter in duration, and generally consist of patient exposure-response trials which
focus on proving the hypothesized mechanism of action. Phase 2b trials are typically
higher enrolling and longer in duration, and generally consist of patient dose-
|
ranging trials which focus on finding
the optimum dosage at which the drug shows clinical benefit with minimal side effects.
|
·
|
Phase 3
.
Clinical trials are undertaken after preliminary evidence suggesting effectiveness has
been obtained and are intended to further evaluate dosage, clinical efficacy and safety
in an expanded patient population at geographically dispersed clinical trial sites. These
clinical trials are intended to establish the overall benefit/risk ratio of the product
and provide an adequate basis for product approval. Generally, two adequate and well-controlled
Phase 3 clinical trials are required by the FDA for approval of an NDA. Phase 3 clinical
trials usually involve several hundred to several thousand participants.
|
Post-approval trials, or Phase 4 clinical
trials, may be conducted after initial marketing approval. These trials are used to gain additional experience from the treatment
of patients in the intended therapeutic indication. In certain instances, the FDA may mandate the performance of Phase 4 trials.
The FDCA permits the FDA and an IND sponsor
to agree in writing on the design and size of clinical trials intended to form the primary basis of a claim of effectiveness in
an NDA. This process is known as a Special Protocol Assessment, or SPA. An SPA agreement may not be changed by the sponsor or
the FDA after the trial begins except with the written agreement of the sponsor and the FDA, or if the FDA determines that a substantial
scientific issue essential to determining the safety or effectiveness of the drug was identified after the trial began. For certain
types of protocols, including carcinogenicity protocols, stability protocols, and Phase 3 protocols for clinical trials that will
form the primary basis of an efficacy claim, the FDA has agreed under its performance goals associated with the Prescription Drug
User Fee Act, or PDUFA, to provide a written response on most protocols within 45 days of receipt. However, the FDA does not always
meet its PDUFA goals, and additional FDA questions and resolution of issues leading up to an SPA agreement may result in the overall
SPA process being much longer, if an agreement is reached at all.
Progress reports detailing the results
of the clinical trials must be submitted at least annually to the FDA and written IND safety reports must be submitted to the
FDA and the investigators for serious and unexpected adverse events or any finding from trials in laboratory animals that suggests
a significant risk for human subjects. Phase 1, Phase 2 and Phase 3 clinical trials may fail to be completed successfully within
any specified period, if at all. The FDA, the IRB, or the sponsor may suspend or terminate a clinical trial at any time on various
grounds, including a finding that the research subjects or patients are being exposed to an unacceptable health risk. An IRB can
suspend or terminate approval of a clinical trial at its institution if, among other things, the clinical trial is not being conducted
in accordance with the IRB’s requirements or if the drug has been associated with unexpected serious harm to patients. Additionally,
some clinical trials are overseen by an independent group of qualified experts organized by the clinical trial sponsor, known
as a data safety monitoring board or data monitoring committee. This group provides authorization for whether or not a trial may
move forward at designated checkpoints based on access to certain data from the trial. We may also suspend or terminate a clinical
trial based on evolving business objectives and/or competitive climate.
Concurrent with clinical trials, companies
usually complete additional animal trials and must also develop additional information about the chemistry and physical characteristics
of the drug as well as finalize a process for manufacturing the product in commercial quantities in accordance with cGMP requirements.
The manufacturing process must be capable of consistently producing quality batches of the drug candidate and, among other things,
must develop methods for testing the identity, strength, quality and purity of the final drug. Additionally, appropriate packaging
must be selected and tested and stability trials must be conducted to demonstrate that the drug candidate does not undergo unacceptable
deterioration over its shelf life. Labeling of the product must also be developed.
FDA Review and Approval Processes
The results of product development, preclinical
trials and clinical trials, along with descriptions of the manufacturing process, analytical tests conducted on the chemistry
of the drug, proposed labeling and other relevant information are submitted to the FDA as part of an NDA requesting approval to
market the product.
The NDA includes both negative or ambiguous
results of preclinical and clinical trials as well as positive findings. Data may come from company-sponsored clinical trials
intended to test the safety and effectiveness of a use of
a product, or from a number of alternative
sources, including trials initiated by investigators. To support marketing approval, the data submitted must be sufficient in
quality and quantity to establish the safety and effectiveness of the investigational drug product to the satisfaction of the
FDA. The submission of an NDA is subject to the payment of substantial user fees; a waiver of such fees may be obtained under
certain limited circumstances.
For XaraColl, we submitted an NDA under
Section 505(b)(2) of the FDCA, which allows us to submit an NDA as an application that contains full reports of investigations
of safety and effectiveness in which at least some of the information required for approval comes from studies not conducted by
or for the 505(b)(2) applicant, but instead from published literature reports and/or the FDA’s findings of safety and/or
effectiveness for one or more approved drugs, and for which the 505(b)(2) applicant has not obtained a right of reference or use.
In February 2017, our representatives attended a Type-A meeting with representatives of the FDA to review potential pathways
forward following our receipt of the Refusal to File Letter and to review a proposed plan for proceeding with additional studies
that would allow us to file a revised NDA for XaraColl. During the meeting, we proposed a plan designed to allow us to submit
a revised NDA to the FDA by the latter part of 2017. We proposed conducting an additional short-term pharmacokinetic study and
several short-term non-clinical studies. Under current practice before the FDA, we received limited feedback during the meeting
and we expect to receive shortly from the representatives of the FDA formal written meeting minutes of our Type-A meeting, which
will serve as the official record of the response of the FDA to our proposal during the meeting. If the FDA concurs with our plan,
we will commence the additional studies, and if the results are positive, we would submit a revised NDA to the FDA soon after
the completion of the studies. However, if the FDA suggests that studies beyond those that we proposed would be necessary, or
if the results of the studies that we proposed are not positive, we would not likely be able to submit our revised NDA for an
extended period of time, if at all.
In addition, under the Pediatric Research
Equity Act, or PREA, an NDA or supplement to an NDA for any new active ingredient, indication, dosage form, or route of administration
must contain data to assess the safety and effectiveness of the drug for the claimed indications in all relevant pediatric subpopulations
and to support dosing and administration for each pediatric subpopulation for which the product is safe and effective. The FDA
may grant deferrals for submission of data or full or partial waivers. Unless otherwise required by regulation, PREA does not
apply to any drug for an indication for which orphan designation has been granted. However, if only one indication for a product
has orphan designation, a pediatric assessment may still be required for any applications to market that same product for the
non-orphan indication(s).
The FDA reviews all NDAs submitted before
it accepts them for filing and may request additional information rather than accepting an NDA for filing. The FDA must make a
decision on accepting an NDA for filing within 60 days of receipt. Once the submission is accepted for filing, the FDA begins
an in-depth review of the NDA. Under the goals and policies agreed to by the FDA under PDUFA, the FDA has ten months from the
60-day filing date in which to complete its initial review of a standard NDA and respond to the applicant, and six months for
a priority NDA. The FDA does not always meet its PDUFA goal dates for standard and priority NDAs, and the review process is often
significantly extended by FDA requests for additional information or clarification.
After the NDA submission is accepted for
filing, the FDA reviews the NDA to determine, among other things, whether the proposed product is safe and effective for its intended
use, and whether the product is being manufactured in accordance with cGMP to assure and preserve the product’s identity,
strength, quality and purity. The FDA may refer applications for novel drug or biological products or drug or biological products
which present difficult questions of safety or efficacy to an advisory committee, typically a panel that includes clinicians and
other experts, for review, evaluation and a recommendation as to whether the application should be approved and under what conditions.
The FDA is not bound by the recommendations of an advisory committee, but it considers such recommendations carefully when making
decisions.
Before approving an NDA, the FDA will inspect
the facilities at which the product is manufactured. The FDA will not approve the product unless it determines that the manufacturing
processes and facilities are in compliance with cGMP requirements and adequate to assure consistent production of the product
within required specifications. Additionally, before approving an NDA, the FDA may inspect one or more clinical sites to assure
compliance with cGCP requirements. After the FDA evaluates the application, manufacturing process and manufacturing facilities
and other relevant information, it may issue an approval letter or a Complete Response Letter. An approval letter authorizes commercial
marketing of the drug with specific prescribing information for specific indications under specific conditions of use set out
in the approved labeling. A Complete Response Letter indicates that the review cycle of the
application is complete and the application
is not ready for approval. A Complete Response Letter usually describes all of the specific deficiencies in the NDA identified
by the FDA. The Complete Response Letter may require additional clinical data and/or an additional pivotal Phase 3 clinical trial(s),
and/or other significant and time-consuming requirements related to clinical trials, preclinical trials or manufacturing. If a
Complete Response Letter is issued, the applicant may either resubmit the NDA, addressing all of the deficiencies identified in
the letter or withdraw the application. Even if such data and information is submitted, the FDA may ultimately decide that the
NDA does not satisfy the criteria for approval. Data obtained from clinical trials are not always conclusive and the FDA may interpret
data differently than we interpret the same data.
If the FDA approves the NDA, the drug’s
approved labeling will be limited to specific diseases, dosages and indications and will include certain contraindications, warnings
and/or precautions. The FDA may condition the approval of the NDA on changes to the proposed labeling, development of adequate
controls and specifications or a commitment to conduct one or more post-market trials or clinical trials. For example, the FDA
may require post-approval studies which involve clinical trials designed to further assess a drug’s safety and effectiveness
and may require testing and surveillance programs to monitor the safety of approved products that have been commercialized. The
FDA may also determine that a risk evaluation and mitigation strategy, or REMS, is necessary to assure the safe use of the drug.
If the FDA concludes a REMS is needed, the sponsor of the NDA must submit a proposed REMS; the FDA will not approve the NDA without
an approved REMS, if required. A REMS could include medication guides, physician or patient communication plans, or other elements
to assure safe use, such as restricted distribution methods, patient registries and other risk minimization tools. Following approval
of an NDA with a REMS, the sponsor is responsible for marketing the drug in compliance with the REMS and must submit periodic
REMS assessments to the FDA. Any of these limitations could restrict the commercial value of the product.
Expedited Development and Review Programs
The FDA has several overlapping programs
that are intended to expedite or facilitate the process for reviewing new drug products that meet certain criteria. Specifically,
new drugs are eligible for Fast Track designation if they are intended to treat a serious or life-threatening disease or condition
and demonstrate the potential to address unmet medical needs for the disease or condition. This designation is a key provision
of the Generating Antibiotic Incentives Now Act, or GAIN Act, approved by Congress in 2012 to increase the incentives for drug
manufacturers to produce new antibiotics for serious and hard-to-treat bacterial and fungal infections. Qualified Infectious Disease
Product (QIDP) designation for a drug adds an additional five years of market exclusivity, which means that the company that brings
the drug into commercial use is protected from generic competitors for that period. A priority review designation means that the
FDA’s goal is to take action on an application within 6 months, compared to 10 months under standard review.
Any product submitted to the FDA for approval,
including a product with a Fast Track designation, may also be eligible for other types of FDA programs intended to expedite development
and review, such as priority review and accelerated approval. A product is eligible for priority review if it has the potential
to provide safe and effective therapy where no satisfactory alternative therapy exists or a significant improvement in the treatment,
diagnosis or prevention of a disease compared to marketed products. The FDA will attempt to direct additional resources to the
evaluation of an application for a new drug designated for priority review in an effort to facilitate the review. Additionally,
a product may be eligible for accelerated approval. Drug products studied for their safety and effectiveness in treating serious
or life-threatening diseases or conditions may receive accelerated approval upon a determination that the product has an effect
on a surrogate endpoint that is reasonably likely to predict clinical benefit, or on a clinical endpoint that can be measured
earlier than irreversible morbidity or mortality, that is reasonably likely to predict an effect on irreversible morbidity or
mortality or other clinical benefit, taking into account the severity, rarity, or prevalence of the condition and the availability
or lack of alternative treatments. As a condition of approval, the FDA may require that a sponsor of a drug or biological product
receiving accelerated approval perform adequate and well-controlled post-marketing clinical trials. In addition, the FDA currently
requires as a condition for accelerated approval pre-approval of promotional materials, which could adversely impact the timing
of the commercial launch of the product.
The FDA may also expedite the approval
of a designated breakthrough therapy, which is a drug that is intended, alone or in combination with one or more other drugs,
to treat a serious or life-threatening disease or condition and preliminary clinical evidence indicates that the drug may demonstrate
substantial improvement over existing therapies on one or more clinically significant endpoints, such as substantial treatment
effects observed early in clinical development. The sponsor of a breakthrough therapy may request the FDA to designate the drug
as a breakthrough
therapy at the time of, or any time after,
the submission of an IND for the drug. If FDA designates a drug as a breakthrough therapy, it must take actions appropriate to
expedite the development and review of the application, which may include holding meetings with the sponsor and the review team
throughout the development of the drug; providing timely advice to, and interactive communication with, the sponsor regarding
the development of the drug to ensure that the development program to gather the nonclinical and clinical data necessary for approval
is as efficient as practicable; involving senior managers and experienced review staff, as appropriate, in a collaborative, cross-disciplinary
review; assigning a cross-disciplinary project lead for the FDA review team to facilitate an efficient review of the development
program and to serve as a scientific liaison between the review team and the sponsor; and taking steps to ensure that the design
of the clinical trials is as efficient as practicable, when scientifically appropriate, such as by minimizing the number of patients
exposed to a potentially less efficacious treatment.
Fast Track designation, priority review
and breakthrough therapy designation do not change the standards for approval but may expedite the development or approval process.
Post-Approval Requirements for Approved Drugs
Any drug products for which we receive
FDA approvals are subject to continuing regulation by the FDA, including, among other things, record-keeping requirements, reporting
of adverse experiences with the product, providing the FDA with updated safety and efficacy information, product sampling and
distribution requirements, and complying with FDA promotion and advertising requirements, which include, among other requirements,
standards for direct-to-consumer advertising, restrictions on promoting drugs for uses or in patient populations that are not
described in the drug’s approved labeling (known as “off-label use”), limitations on industry sponsored scientific
and educational activities, and requirements for promotional activities involving the internet. Although physicians may prescribe
legally available drugs for off-label uses, manufacturers may not market or promote such off-label uses.
In addition, quality control and manufacturing
procedures must continue to conform to applicable manufacturing requirements after approval. We are relying exclusively on our
facility in Saal, Germany, for the production of clinical and commercial quantities of our products in accordance with cGMP regulations,
which is cGMP approved in Germany, but has not yet been cGMP approved by the FDA. cGMP regulations require among
other things, quality control and quality assurance as well as the corresponding maintenance of records and documentation and
the obligation to investigate and correct any deviations from cGMP. Drug manufacturers and other entities involved in the manufacture
and distribution of approved drugs are required to register their establishments with the FDA and certain state agencies, and
are subject to periodic unannounced inspections by the FDA and certain state agencies for compliance with cGMP and other laws.
Accordingly, manufacturers must continue to expend time, money and effort in the area of production and quality control to maintain
cGMP compliance. Discovery of problems with a product after approval may result in restrictions on a product, manufacturer or
holder of an approved NDA, including, among other things, recall or withdrawal of the product from the market. In addition, changes
to the manufacturing process are strictly regulated, and depending on the significance of the change, may require prior FDA approval
before being implemented and development of and submission of data to support the change. Other types of changes to the approved
product, such as adding new indications and additional labeling claims, are also subject to further FDA review and approval, as
well as, possibly, the development and submission of data to support the change.
The FDA also may require post-approval,
sometimes referred to as Phase 4, trials and surveillance to monitor the effects of an approved product or place conditions on
an approval that could restrict the distribution or use of the product. Discovery of previously unknown problems with a product
or the failure to comply with applicable FDA requirements can have negative consequences, including adverse publicity, judicial
or administrative enforcement, warning letters from the FDA, mandated corrective advertising or communications with doctors, and
civil or criminal penalties, among others. Newly discovered or developed safety or effectiveness data may require changes to a
product’s approved labeling, including the addition of new warnings and contraindications, and also may require the implementation
of other risk management measures, such as a REMS. Also, new government requirements, including those resulting from new legislation,
may be established, or the FDA’s policies may change, which could delay or prevent regulatory approval of our products under
development.
United States Premarket Clearance and Approval Requirements
for Medical Devices
Unless an exemption applies, each medical
device, such as CollaGUARD or our other device products or product candidates, we wish to distribute commercially in the United
States will require either prior premarket notification (510(k)) clearance or prior approval of a PMA application from the FDA.
The FDA classifies medical devices into one of three classes. Devices deemed to pose low to moderate risk are placed in either
class I or II, which, absent an exemption, generally requires the manufacturer to file with the FDA a 510(k) submission requesting
permission for commercial distribution. This process is known as 510(k) clearance. Some devices which are not substantially equivalent
to a predicate device can undergo the de novo review process for purposes of marketing authorization. Some low-risk devices are
exempt from this requirement. Devices deemed by the FDA to pose the greatest risk, such as life-sustaining, life-supporting or
certain implantable devices, or devices deemed not substantially equivalent to a previously cleared 510(k) device, or devices
not authorized for marketing through the de novo review process, are placed in class III, requiring approval of a PMA application.
CollaGUARD is a Class III device requiring premarket approval. Both premarket clearance and PMA applications are subject to the
payment of user fees, paid at the time of submission for FDA review. The FDA can also impose restrictions on the sale, distribution
or use of devices at the time of their clearance or approval, or subsequent to marketing.
510(k) Clearance Pathway
To obtain 510(k) clearance, we must file
a 510(k) submission demonstrating that the proposed device is substantially equivalent to a previously cleared 510(k) device or
a device that was in commercial distribution before May 28, 1976 for which the FDA has not yet called for the submission of PMA
applications. The FDA’s 510(k) clearance pathway usually takes from three to 12 months from the date the application is
completed and filed, but it can take significantly longer and clearance is never assured. Although many 510(k) submissions are
cleared without clinical data, in some cases, the FDA requires significant clinical data to support substantial equivalence. In
reviewing a 510(k) submission, the FDA may request additional information, including clinical data, which may significantly prolong
the review process. After a device receives 510(k) clearance, any modification that could significantly affect its safety or effectiveness,
or that would constitute a new or major change in its intended use, will require a new 510(k) clearance or, depending on the modification,
could require de novo review or a PMA application. The FDA requires each manufacturer to make this determination initially, but
the FDA can review any such decision and can disagree with a manufacturer’s determination. If the FDA disagrees with a manufacturer’s
determination that a new 510(k) submission is not required for the modification of an existing device, the FDA can require the
manufacturer to cease marketing and/or recall the modified device until 510(k) clearance, successful de novo review or approval
of a PMA application is obtained. If the FDA requires us to seek 510(k) clearance, de novo review or approval of a PMA application
for any modifications to a previously cleared product, we may be required to cease marketing or recall the modified device until
we obtain FDA marketing authorization. In addition, in these circumstances, we may be subject to significant regulatory fines
or penalties for failure to submit for marketing authorization.
Premarket Approval Pathway
Some devices which are not substantially
equivalent to a predicate device can undergo the de novo review process for purposes of marketing authorization. A PMA application
must be submitted if the device is not exempt, cannot be cleared through the 510(k) process and cannot be authorized through the
de novo review process, which will be the case for CollaGUARD. The PMA application process is generally more costly and time consuming
than the 510(k) premarket clearance process and requires proof of the safety and effectiveness of the device to the FDA’s
satisfaction. Accordingly, a PMA application must be supported by extensive data including, but not limited to, technical information
regarding device design and development, pre-clinical and clinical trials, manufacturing data and labeling to support the FDA’s
determination that the device is safe and effective for its intended use. After a PMA application is deemed complete, the FDA
will accept the application for filing and begin an in-depth review of the submitted information. By statute, the FDA has 180
days to review the “accepted application,” although, generally, review of the application takes between one and three
years, but may take significantly longer. During this review period, the FDA may request additional information or clarification
of information already provided. Also during the review period, an advisory panel of experts from outside the FDA may be convened
to review and evaluate the application and provide recommendations to the FDA as to the approvability of the device. In addition,
the FDA will conduct a preapproval inspection of the manufacturing facility to ensure compliance with Quality System Regulation,
or QSR, which requires elaborate design development, testing, production control, documentation and other quality
assurance procedures and measures upon the
design, manufacturing and distribution process. The FDA may approve a PMA application with post-approval conditions intended to
ensure the safety and effectiveness of the device including, among other things, restrictions on labeling, promotion, sale and
distribution, collection of long-term follow-up data from patients in the clinical trial that supported approval, or new post-approval
studies. Failure to comply with the conditions of approval can result in materially adverse enforcement action, including the
loss or withdrawal of the approval. PMA supplements are required for modifications that could affect device safety or effectiveness,
including, for example, certain types of modifications to the device’s indication for use, manufacturing process, labeling
and design. PMA supplements often require submission of the same type of information as an original PMA application, except that
the supplement is limited to information needed to support any changes to the device covered by the original PMA application,
and may not require as extensive clinical data or the convening of an advisory panel.
Clinical Trials
A clinical trial is almost always required
to support a PMA application and may be required for 510(k) premarket clearance. We expect that CollaGUARD, as a Class III device,
will require a single pivotal trial for PMA approval. In the United States, absent certain limited exceptions, human clinical
trials intended to support product clearance or approval require an IDE application which the FDA reviews. Some types of trials
deemed to present “non-significant risk” are deemed to have an approved IDE once certain requirements are addressed
and IRB approval is obtained. If the device presents a “significant risk” to human health, as defined by FDA regulations,
the sponsor must submit an IDE application to the FDA and obtain IDE approval prior to commencing the human clinical trials. The
IDE application must be supported by appropriate data, such as animal and laboratory trial results, showing that it is safe to
evaluate the device in humans and that the trial protocol is scientifically sound. The IDE application must be approved in advance
by the FDA for a specified number of subjects, unless the product is deemed a non-significant risk device and eligible for more
abbreviated IDE requirements. Clinical trials for a significant risk device may begin once the IDE application is approved by
the FDA and the responsible institutional review boards at the clinical trial sites. There can be no assurance that submission
of an IDE will result in the ability to commence clinical trials. Additionally, after a trial begins, the FDA may place it on
hold or terminate it if, among other reasons, it concludes that the clinical subjects are exposed to unacceptable health risks
that outweigh the benefits of participation in the trial. During a trial, we are required to comply with the FDA’s IDE requirements
for investigator selection, trial monitoring, reporting, record keeping and prohibitions on the promotion or commercialization
of investigational devices or making safety or efficacy claims for them, among other things. We are also responsible for the appropriate
labeling and distribution of investigational devices. Our clinical trials must be conducted in accordance with FDA regulations
and federal and state regulations concerning human subject protection, including informed consent and healthcare privacy. The
investigators must also obtain patient informed consent, rigorously follow the investigational plan and trial protocol, control
the disposition of investigational devices and comply with all reporting and recordkeeping requirements, among other things. The
FDA’s grant of permission to proceed with clinical trials does not constitute a binding commitment that the FDA will consider
the trial design adequate to support commercial marketing clearance or approval. In addition, there can be no assurance that the
data generated during a clinical trial will meet chosen safety and effectiveness endpoints or otherwise produce results that will
lead the FDA to grant marketing clearance or approval. Similarly, in Europe, the clinical trial must be approved by the local
ethics committee and in some cases, including trials of high-risk devices, by the Ministry of Health in the applicable country.
Pervasive and Continuing FDA Regulation for Medical
Devices
After a device is placed on the market,
regardless of its classification or premarket pathway, numerous regulatory requirements apply. These include, but are not limited
to:
|
·
|
establishing
establishment registration and device listings with the FDA;
|
|
·
|
Quality System
Regulation, or QSR, which requires manufacturers, including third-party manufacturers
and certain other parties, to follow stringent design, testing, process control, documentation,
CAPA, complaint handling and other quality assurance procedures, as applicable;
|
|
·
|
labeling statutes
and regulations, which prohibit the promotion of products for uncleared or unapproved,
or off-label, uses and impose other restrictions on labeling;
|
|
·
|
clearance,
approval or authorization of product modifications, e.g., that could affect (or for 510(k)
devices, significantly affect) safety or effectiveness or that would constitute a change
(or for 510(k) devices, a major change) in intended use;
|
|
·
|
medical device
reporting regulations, which require that manufacturers report to the FDA if an event
reasonably suggests that their device may have caused or contributed to a death or serious
injury or malfunctioned in a way that would likely cause or contribute to a death or
serious injury if the malfunction of the same or a similar device of the manufacturer
were to recur;
|
|
·
|
corrections
and removals reporting regulations, which require that manufacturers report to the FDA
field corrections and product removals if undertaken to reduce a risk to health posed
by the device or to remedy a violation of the FDCA, that may present a risk to health.
In addition, FDA may order a mandatory recall if there is a reasonable probability that
the device would cause serious adverse health consequences or death; and
|
|
·
|
post-approval
restrictions or conditions, including requirements to conduct post-market surveillance
studies to establish additional safety or efficacy data.
|
The FDA has broad post-market and regulatory
enforcement powers. The agency may conduct announced and unannounced inspections to determine compliance with the QSR and other
regulations, and these inspections may include the manufacturing facilities of subcontractors. Failure by us or our suppliers
to comply with applicable regulatory requirements can result in enforcement action by the FDA or other regulatory authorities,
which may result in sanctions and related consequences including, but not limited to:
|
·
|
operating restrictions,
partial suspension or total shutdown of production;
|
|
·
|
refusal of
or delay in granting our requests for 510(k) clearance or premarket approval of new products
or modified products;
|
|
·
|
withdrawing
510(k) clearance or premarket approvals that are already granted;
|
|
·
|
refusal to
grant export approval for our products;
|
|
·
|
criminal prosecution;
and
|
|
·
|
unanticipated
expenditures to address or defend such actions.
|
We are subject to announced and unannounced
device inspections by FDA and other regulatory agencies overseeing the implementation and adherence of applicable local, state
and federal statutes and regulations.
Health Care
Affordable Care Act
|
·
|
In March 2010, the
Patient Protection and Affordable Care Act, as amended by the Health Care and Education
Reconciliation Act of 2010, or collectively, the Affordable Care Act, was enacted, which
includes measures that have or will significantly change the way health care is financed
by both governmental and private insurers. Among the provisions of the Affordable Care
Act of greatest importance to the pharmaceutical industry are the following:
|
|
·
|
The Medicaid Drug
Rebate Program requires pharmaceutical manufacturers to enter into and have in effect
a national rebate agreement with the Secretary of the Department of Health and Human
Services as a condition for states to receive federal matching funds for the manufacturer’s
outpatient drugs furnished to Medicaid patients. Effective in 2010, the Affordable Care
Act made several changes to the Medicaid Drug Rebate Program, including increasing pharmaceutical
manufacturers’ rebate liability by raising the minimum basic Medicaid rebate on
most branded prescription drugs and biologic agents from 15.1% of average manufacturer
price (AMP) to 23.1% of AMP and adding a new rebate calculation for “line extensions”
(i.e., new formulations, such as extended release
|
formulations) of solid oral dosage
forms of branded products, as well as potentially impacting their rebate liability by modifying the statutory definition of AMP.
The Affordable Care Act also expanded the universe of Medicaid utilization subject to drug rebates by requiring pharmaceutical
manufacturers to pay rebates on Medicaid managed care utilization as of 2010. Per a ruling by the U.S. Supreme Court in 2012,
states have the option to expand their Medicaid programs which in turn expands the population eligible for Medicaid drug benefits.
The Centers for Medicare and Medicaid Services, or CMS, has proposed to expand Medicaid rebate liability to the territories of
the United States as well. In addition, the Affordable Care Act provides for the public availability of retail survey prices and
certain weighted average AMPs under the Medicaid program. The implementation of this requirement by the CMS may also provide for
the public availability of pharmacy acquisition of cost data, which could negatively impact our sales.
|
·
|
In order for a pharmaceutical
product to receive federal reimbursement under the Medicare Part B and Medicaid programs
or to be sold directly to U.S. government agencies, the manufacturer must extend discounts
to entities eligible to participate in the 340B drug pricing program. The required 340B
discount on a given product is calculated based on the AMP and Medicaid rebate amounts
reported by the manufacturer. Effective in 2010, the Affordable Care Act expanded the
types of entities eligible to receive discounted 340B pricing, although, under the current
state of the law, with the exception of children’s hospitals, these newly eligible
entities will not be eligible to receive discounted 340B pricing on orphan drugs when
used for the orphan indication. In July 2013, the Health Resources and Services Administration
(HRSA) issued a final rule allowing the newly eligible entities to access discounted
orphan drugs if used for non-orphan indications. While the final rule was vacated by
a federal court ruling, HRSA has stated it will continue to allow discounts for orphan
drugs when used for any indication other than for orphan indications. In addition, as
340B drug pricing is determined based on AMP and Medicaid rebate data, the revisions
to the Medicaid rebate formula and AMP definition described above could cause the required
340B discount to increase.
|
|
·
|
Effective in 2011,
the Affordable Care Act imposed a requirement on manufacturers of branded drugs and biologic
agents to provide a 50% discount off the negotiated price of branded drugs dispensed
to Medicare Part D patients in the coverage gap (i.e., “donut hole”).
|
|
·
|
Effective in 2011,
the Affordable Care Act imposed an annual, nondeductible fee on any entity that manufactures
or imports certain branded prescription drugs and biologic agents, apportioned among
these entities according to their market share in certain government healthcare programs,
although this fee would not apply to sales of certain products approved exclusively for
orphan indications.
|
|
·
|
The Affordable Care
Act required pharmaceutical manufacturers to track certain financial arrangements with
physicians and teaching hospitals, including any “transfer of value” made
or distributed to such entities, as well as any ownership or investment interests held
by physicians and their immediate family members. Manufacturers were required to begin
tracking this information in 2013 and to report this information to CMS by March 2014.
|
|
·
|
As of 2010, a new
Patient-Centered Outcomes Research Institute was established pursuant to the Affordable
Care Actor oversee, identify priorities in, and conduct comparative clinical effectiveness
research, along with funding for such research. The research conducted by the Patient-Centered
Outcomes Research Institute may affect the market for certain pharmaceutical products.
|
|
·
|
The Affordable Care
Act created the Independent Payment Advisory Board, IPAB, which, beginning in 2014, will
have authority to recommend certain changes to the Medicare program to reduce expenditures
by the program that could result in reduced payments for prescription drugs. Under certain
circumstances, these recommendations will become law unless Congress enacts legislation
that will achieve the same or greater Medicare cost savings. IPAB recommendations are
only required when Medicare spending exceeds a target growth rate established by the
Affordable Care Act. Members of the IPAB have still not been appointed and Medicare cost
growth is below the threshold that would require IPAB recommendations.
|
|
·
|
The Affordable Care
Act established the Center for Medicare and Medicaid Innovation within CMS to test innovative
payment and service delivery models to lower Medicare and Medicaid spending, potentially
including
|
prescription drug spending. Funding
has been allocated to support the mission of the Center for Medicare and Medicaid Innovation from 2011 to 2019.
|
·
|
In January 2017,
Congress voted to adopt a budget resolution for fiscal year 2017, or the Budget Resolution,
that authorizes the implementation of legislation that would repeal portions of the Affordable
Care Act. The Budget Resolution is not a law, but it is widely viewed as the first step
toward the passage of legislation that would repeal certain aspects of the Affordable
Care Act. Further, on January 20, 2017, President Trump signed an Executive Order directing
federal agencies with authorities and responsibilities under the Affordable Care Act
to waive, defer, grant exemptions from, or delay the implementation of any provision
of the Affordable Care Act that would impose a fiscal or regulatory burden on states,
individuals, healthcare providers, health insurers, or manufacturers of pharmaceuticals
or medical devices. Congress also could consider subsequent legislation to replace elements
of the Affordable Care Act that are repealed. We will continue to evaluate the effect
that the Affordable Care Act and any future measures to repeal or replace the Affordable
Care Act have on our business.
|
Pediatric Exclusivity
Pediatric exclusivity is another type of
regulatory market exclusivity in the United States. Pediatric exclusivity, if granted, adds six months to any existing exclusivity
period or patent term. This six-month exclusivity may be granted by FDA based on the completion of a pediatric trial in accordance
with a “Written Request” for such as outlined in §505A(d)(2) of the FDCA. Recently, the Food and Drug Administration
Safety and Innovation Act, or FDASIA, amended the FDCA. FDASIA requires that a sponsor who is planning to submit a marketing application
for a drug or biological product that includes a new active ingredient, new indication, new dosage form, new dosing regimen or
new route of administration submit an initial Pediatric Study Plan, or PSP, ideally within sixty days of an end-of-phase 2 meeting
or as may be agreed between the sponsor and FDA but no later than 210 days before submission of the NDA or supplement. The initial
PSP must include an outline of the pediatric study or studies that the sponsor plans to conduct, including study objectives and
design, age groups, relevant endpoints and statistical approach, or a justification for not including such detailed information,
and any request for a deferral of pediatric assessments or a full or partial waiver of the requirement to provide data from pediatric
studies along with supporting information. FDA and the sponsor must reach agreement on the PSP. A sponsor can submit amendments
to an agreed-upon initial PSP at any time if changes to the pediatric plan need to be considered based on data collected from
nonclinical studies, early phase clinical trials, and/or other clinical development programs.
United States Patent Term Restoration and Marketing
Exclusivity
Depending upon the timing, duration and
specifics of the FDA approval of the use of our drug or device candidates, some of our U.S. patents or patents issuing based on
our pending and future patent applications may be eligible for limited patent term extension under the Drug Price Competition
and Patent Term Restoration Act of 1984, commonly referred to as the Hatch-Waxman Amendments. The Hatch-Waxman Amendments permit
a patent restoration term of up to five years as compensation for patent term lost during product development and the FDA regulatory
review process. However, patent term restoration cannot extend the remaining term of a patent beyond a total of 14 years from
the product’s approval date. The patent term restoration period is generally one-half the time between the effective date
of an IND or IDE and the submission date of an NDA or PMA, respectively, plus the time between the submission date of an NDA or
PMA and the approval of that application. Only one patent applicable to an approved drug or device is eligible for the extension
and the application for the extension must be submitted prior to the expiration of the patent. The U.S. Patent and Trademark Office,
in consultation with the FDA, reviews and approves the application for any patent term extension or restoration. In the future,
we may intend to apply for restoration of patent term for one of our currently owned or licensed patents to add patent life beyond
its current expiration date, depending on the expected length of the clinical trials and other factors involved in the filing
of the relevant NDA.
Market exclusivity provisions under the
FDCA can also delay the submission or the approval of certain competing marketing applications. The FDCA provides a five-year
period of non-patent marketing exclusivity within the United States to the first applicant to obtain approval of an NDA for a
new chemical entity. A drug is a new chemical entity if the FDA has not previously approved any other new drug containing the
same active moiety, which is the molecule or ion responsible for the action of the drug substance. During the exclusivity period,
the FDA may not accept for review an abbreviated new drug application, or ANDA, or a 505(b)(2) NDA submitted by another company
for another drug based on the same active moiety, regardless of whether the drug is intended for the same indication as
the original innovative drug or for another
indication, where the applicant does not own or have a legal right of reference to all the data required for approval. However,
an application may be submitted after four years if it contains a certification of patent invalidity or non-infringement to one
of the patents listed with the FDA by the innovator NDA holder. The FDCA also provides three years of marketing exclusivity for
an NDA or supplement to an existing NDA if new clinical investigations, other than bioavailability studies, that were conducted
or sponsored by the applicant are deemed by the FDA to be essential to the approval of the application, for example, clinical
investigations to support new indications, dosages or strengths of an existing drug. This three-year exclusivity covers only the
modification for which the drug received approval on the basis of the new clinical investigations and does not prohibit the FDA
from approving ANDAs for drugs containing the active agent for the original indication or condition of use. Five-year and three-year
exclusivity will not delay the submission or approval of any full NDA. However, an applicant submitting a full NDA would be required
to conduct or obtain a right of reference to all of the preclinical and clinical trials necessary to demonstrate safety and effectiveness.
An applicant submitting an ANDA would be required to demonstrate bioequivalency in patients comparing their candidate product
to our product. Establishment of bioequivalency in patients can be a costly and challenging undertaking.
Other types of non-patent marketing exclusivity
include orphan drug exclusivity under the Orphan Drug Act, which may offer a seven-year period of marketing exclusivity as described
above, and pediatric exclusivity under the Best Pharmaceuticals for Children Act, which may add six months to existing exclusivity
periods and patent terms. This six-month pediatric exclusivity may be granted based on the voluntary completion of a pediatric
trial in accordance with an FDA-issued “Written Request” for such a trial.
Non-United States Government Regulation
In addition to regulations in the United
States, we will be subject to a variety of regulations in other jurisdictions governing, among other things, clinical trials and
any commercial sales, promotion and distribution of our products. Whether or not we obtain FDA approval for a product, we must
obtain the requisite approvals from regulatory authorities in foreign countries prior to the commencement of clinical trials or
marketing of the product in those countries. We, or our local partners, have also filed marketing authorization applications for
CollaGUARD in Argentina, Australia, Canada, Hong Kong, Mexico, Belarus, Kazakhstan and Taiwan. We obtained a CE Mark for CollaGUARD
in the EU in October 2011 and have received approval for CollaGUARD in India, Israel, the Philippines, the Russian Federation,
Saudi Arabia, Singapore, Thailand and Vietnam and require no further registration of approval to market CollaGUARD in New Zealand.
Non-United States Government Regulation Applicable
to Drugs
Certain countries outside of the United
States have a similar process that requires the submission of a clinical trial application much like an IND prior to the commencement
of human clinical trials. If we fail to comply with applicable foreign regulatory requirements, we may be subject in those countries
to, among other things, fines, suspension or withdrawal of regulatory approvals, product recalls, seizure of products, operating
restrictions and criminal prosecution.
In the EEA (which is comprised of the 28
Member States of the European Union plus Iceland, Liechtenstein and Norway), for example, medicinal products can only be commercialized
after obtaining a Marketing Authorization, or MA. There are two types of marketing authorizations:
|
·
|
The Community
MA, which is issued by the European Commission through the Centralized Procedure, based
on the opinion of the EMA Committee for Medicinal Products for Human Use (CHMP), and
which is valid throughout the entire territory of the EEA. The Centralized Procedure
is mandatory for certain types of products, such as biotechnology medicinal products,
advanced-therapy medicines, orphan medicinal products, and medicinal products containing
a new active substance indicated for the treatment of AIDS, cancer, neurodegenerative
disorders, diabetes, auto-immune and viral diseases. The Centralized Procedure is optional
for products containing a new active substance not yet authorized in the EEA, or for
products that constitute a significant therapeutic, scientific or technical innovation
or which are in the interest of public health in the European Union.
|
|
·
|
National MAs,
which are issued by the competent authorities of the Member States of the EEA and only
cover their respective territory, are available for products not falling within the mandatory
scope of the Centralized Procedure. Where a product has already been authorized for marketing
in a Member State of the EEA (the Reference Member State, or RMS), this National MA can
be recognized in other Member States (the Concerned Member States, or CMS) through the
Mutual Recognition Procedure. If the product has not received a National MA in any Member
State at the time of application, it can be approved simultaneously in various Member
States through the Decentralized Procedure. Under the Decentralized Procedure, an identical
dossier is submitted to the competent authorities of each of the Member States in which
the MA is sought, one of which is selected by the applicant as the RMS. The competent
authority of the RMS prepares a draft assessment report, a draft summary of the product
characteristics, or SPC, and a draft of the labeling and package leaflet, which are sent
to the CMS for their approval. If the CMS raise no objections, based on a potential serious
risk to public health, to the assessment, SPC, labeling, or packaging proposed by the
RMS, the product is subsequently granted a national MA in all the Member States (i.e.,
in the RMS and the CMS). If one or more CMS raise objections based on a potential serious
risk to public health, the application is referred to the Coordination group for mutual
recognition and decentralized procedure for human medicinal products (the CMDh), which
is composed of representatives of the EEA Member States. If a consensus cannot be reached
within the CMDh the matters is referred for arbitration to the CHMP, which can reach
a final decision binding on all EEA Member States. A similar process applies to disputes
between the RMS and the CMS in the Mutual Recognition Procedure.
|
As with FDA approval, we may not be able
to secure regulatory approvals in Europe in a timely manner, if at all. Additionally, as in the United States, post-approval regulatory
requirements, such as those regarding product manufacture, marketing, or distribution, would apply to any product that is approved
in Europe, and failure to comply with such obligations could have a material adverse effect on our ability to successfully commercialize
any product.
With respect to the conduct of clinical
trials in the European Union a clinical trial application, or CTA, must be submitted to each country’s national health authority
and an independent ethics committee, much like the FDA and IRB requirements in the United States, respectively. Generally, once
the CTA is approved in accordance with a country’s requirements, clinical trials may proceed.
In addition to regulations in Europe and
the United States, we will be subject to a variety of foreign regulations governing clinical trials and commercial distribution
of any future products. For other countries outside of the European Union, such as countries in Eastern Europe, Latin America
or Asia, the requirements governing the conduct of clinical trials, product licensing, pricing and reimbursement vary from country
to country. In all cases, again, the clinical trials are conducted in accordance with cGCP and the applicable regulatory requirements
and the ethical principles that have their origin in the Declaration of Helsinki.
Non-United States Government Regulation Applicable
to Medical Devices
The
advertising and promotion of our products in the EEA is subject to the provisions of the Medical Devices Directive (Directive
93/42), Directive 2006/114/EC concerning misleading and comparative advertising , and Directive 2005/29/EC on unfair commercial
practices , as well as other national legislation in the EEA countries governing the advertising and promotion of medical devices.
The European Commission has submitted a Proposal for a Regulation of the European Parliament and the Council on medical devices,
amending Directive 2001/83/EC, Regulation (EC) No 178/2002 and Regulation (EC) No 1223/2009, to replace, inter alia, Directive
93/42/EEC and to amend regulations regarding medical devices in the European Union, which could result in changes in the regulatory
requirements for medical devices in Europe. Whilst the proposed amending legislation is before the European Parliament, it has
not yet been adopted. Final form adoption is expected by both the European Parliament and the Council during 2017.
In
Germany, the advertising and promotion of our products can also be subject to restrictions provided by the German Act Against
Unfair Competition (Gesetz gegen den unlauteren Wettbewerb) and the law on the advertising of medicines (Heilmittelwerbegesetz),
criminal law, and some codices of conduct with regard to medical products and medical devices among others. These laws may limit
or restrict the advertising and promotion of our products to the general public and may impose limitations on our promotional
activities with healthcare professionals.
In
Ireland, the advertising and promotion of medicinal products to either healthcare professionals or the general public alike are
governed by a combination of legislation including consumer protection laws, advertising of human medicinal product laws, competition
and criminal laws and various codes of conduct, including in relation to advertising standards. The HPRA is the body responsible
for monitoring the advertising of medicinal products and the enforcement of the relevant regulations.
Sales of medical devices are subject to
foreign government regulations, which vary substantially from country to country. In order to market our products outside the
United States, we must obtain regulatory approvals or CE Certificates of Conformity and comply with extensive safety and quality
regulations. The time required to obtain approval by a foreign country or to obtain a CE Certificate of Conformity may be longer
or shorter than that required for FDA clearance or approval, and the requirements may differ. In the EEA, we are required to obtain
Certificates of Conformity before drawing up an EC Declaration of Conformity and affixing the CE Mark of conformity to our medical
devices. Many other countries, such as Australia, India, New Zealand, Pakistan and Sri Lanka, accept CE Certificates of Conformity
or FDA clearance or approval although others, such as Brazil, Canada and Japan require separate regulatory filings.
Reimbursement
Sales of our products will depend, in part,
on the extent to which our products will be covered by third-party payors, such as government health care programs, statutory
health insurances, commercial insurance and managed healthcare organizations. These third-party payors are increasingly reducing
reimbursements for medical products and services. In addition, the U.S. government, state legislatures and foreign governments
have continued implementing cost-containment programs, including price controls, competitive bidding program, restrictions on
reimbursement and requirements for substitution of generic products. Adoption of price controls and cost-containment measures,
and adoption of more restrictive policies in jurisdictions with existing controls and measures, could further limit our net revenue
and results. Decreases in third-party reimbursement for our product candidates or a decision by a third-party payor to not cover
our product candidates could reduce physician usage of our products once approved and have a material adverse effect on our sales,
results of operations and financial condition.
Fraud and Abuse Laws
We will also be subject to several healthcare
regulation and enforcement by the federal government and the states and foreign governments in which we will conduct our business
once our products are approved. The laws that may affect our ability to operate include:
|
·
|
the federal
healthcare programs’ Anti-Kickback Law, which prohibits, among other things, persons
from knowingly and willfully soliciting, receiving, offering or paying remuneration,
directly or indirectly, in exchange for or to induce either the referral of an individual
for, or the purchase, order or recommendation of, any good or service for which payment
may be made under federal healthcare programs such as the Medicare and Medicaid programs;
|
|
·
|
federal false
claims laws which prohibit, among other things, individuals or entities from knowingly
presenting, or causing to be presented, claims for payment from Medicare, Medicaid, or
other third-party payors that are false or fraudulent;
|
|
·
|
federal criminal
laws that prohibit executing a scheme to defraud any healthcare benefit program or making
false statements relating to healthcare matters;
|
|
·
|
federal Civil
Monetary Penalties Law that prohibits various forms of fraud and abuse involving the
Medicare and Medicaid programs;
|
|
·
|
state law equivalents
of each of the above federal laws, such as anti-kickback and false claims laws which
may apply to items or services reimbursed by any third-party payor, including commercial
insurers;
|
|
·
|
for Europe,
directive 2006/114/EC concerning misleading and comparative advertising, and Directive
2005/29/EC on unfair commercial practices, as well as other national legislation in the
European Union governing the advertising and promotion of medical devices; and
|
|
·
|
in Germany
the advertising and promotion of our products can be subject to restrictions provided
by the German Act Against Unfair Competition protecting against commercial practices
which unacceptably harass a market participants.
|
Healthcare Privacy and Security Laws
We may be subject to, or our marketing
activities may be limited by the federal Health Insurance Portability and Accountability Act of 1996, HIPAA, and its implementing
regulations, which established uniform standards for certain “covered entities” (healthcare providers, health plans
and healthcare clearinghouses) governing the conduct of certain electronic healthcare transactions and protecting the security
and privacy of protected health information. The American Recovery and Reinvestment Act of 2009, commonly referred to as the economic
stimulus package, included sweeping expansion of HIPAA’s privacy and security standards called the Health Information Technology
for Economic and Clinical Health Act, or HITECH, which became effective on February 17, 2010. Among other things, the new law
makes HIPAA’s privacy and security standards directly applicable to “business associates,” independent contractors
or agents of covered entities that receive or obtain protected health information in connection with providing a service on behalf
of a covered entity. HITECH also increased the civil and criminal penalties that may be imposed against covered entities, business
associates and possibly other persons, and gave state attorneys general new authority to file civil actions for damages or injunctions
in federal courts to enforce the federal HIPAA laws and seek attorney’s fees and costs associated with pursuing federal
civil actions.
In Europe and Germany, we may be subject
to strict data protection regulations, in particular with regard to health data of individuals, which are categorized as “special
categories of personal data” pursuant to Section 3 subsection 9 German Federal Data Protection Act (Bundesdatenschutzgesetz).
“Personal data” refers to any information relating to an identified or identifiable natural person (data subject);
an identifiable person is one who can be identified, directly or indirectly, in particular by reference to an identification number
or to one or more factors specific to his physical, physiological, mental, economic, cultural or social identity. The special
categories of data such as health data may only be processed if the data subject consented to such processing or if (i) this is
necessary in order to protect vital interests of the data subject or of a third-party, in so far as the data subject is unable
to provide consent for physical or legal reasons; (ii) the data concerned have evidently been made public by the data subject;
(iii) this is necessary in order to assert, exercise or defend legal claims and there is no reason to assume that the data subject
has an overriding legitimate interest in excluding such collection, processing or use; or (iv) this is necessary for the purposes
of scientific research, where the scientific interest in carrying out the research project substantially outweighs the data subject’s
interest in excluding collection, processing and use and the purpose of the research cannot be achieved in any other way or would
otherwise necessitate disproportionate effort. Therefore, we may be subject to and our marketing activities may be limited by
the regulations regarding the data protection of individuals (e.g., according to the Directive 95/46/EC of the European Parliament
and of the Council of 24 October 1995 on the protection of individuals with regard to the processing of personal data and on the
free movement of such data as well as to the German Federal Data Protection Act). These regulations could also restrict the transfer
of data from Germany/Europe to the United States. The general transfer of personal data outside of Europe is prohibited according
to Section 4b subsection 2 sentence 2 German Federal Data Protection Act (implementing Art. 25 subsection 1 of the Directive 95/46/EC)
if the data importer cannot guarantee an appropriate standard of data protection. A transfer of personal data to a non-EU member
state (third country) is allowed only if the third country guarantees a reasonable standard of protection. Currently the United
States is not regarded to be a country with an appropriate level of data protection meaning that further contractual arrangements
have to be adopted to permit the international transfer of personal data to the United States. The EU General Data Protection
Regulation (Regulation (EU) 2016/679) (“GDPR”) entered into force on 24 May 2016 and, following a two year transition
period, will apply from 25 May 2018, replacing the existing data protection framework under the EU Data Protection Directive.
The GDPR aims to make businesses more accountable for data privacy compliance and offers individuals extra rights and more control
over their personal data. The new rules will have significant impacts for all organisations handling personal data, including
us. As well as strengthening the EU data protection rules, the GDPR significantly increases the scope and nature of administrative
fines for non-compliance, providing for fines of up to €20 million or 4% of total worldwide annual turnover (whichever is
greater) in the event of non-compliance.
Corporate History
Our original legal predecessor was incorporated
in Delaware under the name Innocoll, Inc. in December 1997 and renamed Innocoll Holdings, Inc. in May 2004. In July 2013, we re-domiciled
Innocoll Holdings, Inc. from the United States to Germany pursuant to a contribution in-kind and share-for-share exchange into
the newly formed Innocoll GmbH, a German limited liability company.
Pursuant to a notarial deed entered into
between the shareholders of Innocoll Holdings, Inc. and Innocoll GmbH in July 2013, the holders of ordinary shares, preferred
shares and warrants to purchase ordinary shares of Innocoll Holdings, Inc. contributed their shares and warrants by way of a contribution
in kind to Innocoll GmbH in exchange for ordinary shares, preferred shares and options to purchase ordinary shares of Innocoll
GmbH and as a result thereof, Innocoll Holdings, Inc. became Innocoll GmbH’s wholly-owned subsidiary. Innocoll Holdings,
Inc. was subsequently liquidated and its assets, consisting of subsidiary companies Innocoll Pharmaceuticals Ltd., Innocoll Technologies
Ltd., both Irish companies, and Innocoll, Inc., a Delaware corporation, were distributed to Innocoll GmbH.
Pursuant to a notarial deed entered into
on June 16, 2014, all shareholders of Innocoll GmbH agreed to amend and restate its articles of association and cancel and terminate
all preference, redemption and cumulative dividend rights of the preferred shares (other than with respect to the series E shares
regarding certain anti-dilution rights) in exchange for ordinary shares of Innocoll GmbH. On July 3, 2014, Innocoll GmbH transformed
into a German stock corporation (Aktiengesellschaft or AG) in accordance with the provisions of the German Reorganization Act
(Umwandlungsgesetz), and all shares of Innocoll GmbH became ordinary shares of Innocoll AG. Innocoll AG is registered in the commercial
register of Regensburg, Germany under the number HRB 14298.
On July 30, 2014, Innocoll AG sold 6,500,000
ADSs of Innocoll Germany representing 490,567 ordinary shares of Innocoll Germany in our initial public offering at a price of
$9.00 per ADS of Innocoll Germany, thereby raising $54.4 million after deducting underwriting discounts and commissions. On August
20, 2014, the underwriters in our initial public offering partially exercised their overallotment option to purchase an additional
186,984 ADSs of Innocoll Germany, representing 14,112 ordinary shares of Innocoll Germany, at a public offering price of $9.00
per ADS of Innocoll Germany. The sale of the overallotment option by our underwriters occurred on September 12, 2014, at which
we raised additional net proceeds of approximately $1.57 million, after deducting underwriting discounts and commissions. The
ADSs of Innocoll Germany sold in the initial public offering represented new shares of Innocoll Germany issued in a capital increase
resolved by our shareholders for the purposes of the initial public offering on July 18, 2014.
On March 16, 2016, Innocoll AG, a German
stock corporation, with American Depository Shares, or ADSs, listed on the Nasdaq Global Market, merged with Innocoll Holdings
plc, a public limited company formed under Irish law, by way of a European cross-border merger with Innocoll Ireland being the
surviving company. Prior to the Merger Innocoll Holdings plc was a dormant company with minimal legally required share capital
and related debtor on the statement of financial position. Upon the effectiveness of the Merger, we terminated Innocoll Germany’s
ADS facility and each cancelled ADS effectively became an entitlement to receive one ordinary share of Innocoll Ireland. Holders
of Innocoll Germany ordinary shares received 13.25 ordinary shares of Innocoll Ireland in respect of each share held of Innocoll
Germany. Simultaneous with this transaction, Innocoll Ireland listed its ordinary shares on the Nasdaq Global Market under the
symbol “INNL”, which we previously used for Innocoll Germany’s ADSs. The Merger effectively resulted in Innocoll
Ireland becoming the publicly-traded parent of the Innocoll group of companies carrying on the same business as that conducted
by Innocoll Germany prior to the Merger.
We are managed and controlled in Ireland
and became an Irish tax resident as of January 1, 2014. Our principal executive offices are located at Unit 9, Block D, Monksland
Business Park, Monksland, Athlone, Ireland, and our telephone number is +353 (0) 90 648 6834. Our website address is www.innocoll.com.
Information contained on our website is not incorporated by reference into this annual report, and you should not consider information
contained on our website to be part of this annual report or in deciding whether to purchase our ordinary shares. Our agent for
service of process in the United States is Anthony Zook, 3803 West Chester Pike, Newtown Square, PA 19073. XaraColl®, Cogenzia®,
CollaGUARD®, our localized drug delivery technologies trademarked as CollaRx®, CollaFilm®, CollaPress™ and LiquiColl™,
the Innocoll logo and other trademarks or service marks of Innocoll appearing in this annual report are our property. This annual
report contains additional trade names, trademarks and service marks of other companies.
Employees
As of March 13, 2017, we had approximately
120 employees, of which 105 are full-time.
Research and Development
Our research and development expenses were
approximately $38.7 million, $29.8 million and $4.3 million for the years ended December 31, 2016, 2015, and 2014, respectively.
Segment and Geographic Information
We operate in one segment, the manufacture
and sale of collagen-based pharmaceutical products. Total revenues from external customers for the years ended December 31, 2016,
2015, and 2014 were $4.4 million, $2.9 million, and $6.0 million, respectively. Net loss for the years ended December 31, 2016,
2015, and 2014 was $57.0 million, $50.9 million, and $23.5 million, respectively. Total assets at December 31, 2016 and
2015 were $42.0 million and $52.8 million, respectively.
Information regarding our geographic revenues
and identifiable assets attributable to each of our geographic areas of operations for the last three fiscal years is presented
in “Item 8. Financial Statements and Supplementary Data― Note 5. Segment Reporting.”
Significant Customers
The majority of product revenue in 2016, $4.2
million, relates to sales of CollatampG and Septocoll and is split between two customers, EUSA Pharma and Biomet. For
the year ended December 31, 2016, the split was 87% and 10%, respectively. Revenues from EUSA Pharma represent approximately
$3.8 million of the Company’s consolidated revenues.
Available Information
Innocoll is required to file annual, quarterly
and special reports, proxy statements and other information with the SEC. Investors may read and copy any document that Innocoll
files at the SEC’s Public Reference Room at 100 F Street, N.E., Washington, DC 20549. Investors may obtain information on
the operation of the Public Reference Room by calling the SEC at 1-800-SEC-0330. In addition, the SEC maintains an Internet site
at http://www.sec.gov that contains reports, proxy and information statements and other information regarding issuers that file
electronically with the SEC, from which investors can electronically access Innocoll’s SEC filings.
Our Internet website is www.innocoll.com.
We make available free of charge in the “Investors” section of our website our Annual Reports on Form 10-K, Quarterly
Reports on Form 10-Q, Current Reports on Form 8-K, reports filed pursuant to Section 16 and amendments to those reports as soon
as reasonably practicable after we electronically file or furnish such materials to the SEC. In addition, we have posted the charters
for our Audit Committee, Compensation Committee and Nominating and Corporate Governance Committee under the heading “Corporate
Governance” in the Investor Relations section of our website. These charters and principles are not incorporated in this
report by reference. We will also provide a copy of these documents free of charge to shareholders upon request.
Item 1A. Risk Factors.
If any of the risks and uncertainties
set forth below actually materialize, our business, financial condition and/or results of operations could be materially and adversely
affected, the trading price of our ordinary shares could decline and a shareholder could lose all or part of his or her investment.
The risks and uncertainties set forth below are not the only ones we face. Additional risks and uncertainties not presently known
to us or that we currently consider immaterial may also impair our business operations.
Risks Related to Our Financial Position and Capital Requirements
We have a history of operating losses and anticipate
that we will continue to incur operating losses in the future and may never sustain profitability.
We have incurred operating losses in each
year since inception because our research and development and general and administrative expenses exceeded our revenue. Our operating
loss for the years ended December 31, 2014, 2015 and 2016 was $21.3 million, $52.0 million and $66.8 million, respectively. As
of December 31, 2016, we had an accumulated deficit of $223.1 million and our current assets exceeded our current liabilities
by $9.6 million.
Our ability to become profitable depends
on our ability to develop and commercialize our lead product candidate, XaraColl. Our lead product candidate is not yet approved
for commercial sale in the United States or Europe, and we do not know when, or if, we will generate significant revenues from
its sale in the future. In December 2016, we received a Refusal to File Letter from the FDA relating to our NDA for the product.
We will be required to conduct additional studies, that may not be successful. We do not know when we can resubmit our NDA, or
when and if we can receive FDA approval to market XaraColl. Our other late-stage product candidate, CollaGUARD, is approved
for commercial sale in 12 countries, but not yet approved for commercial sale in the United States or Europe and we do not know when, or
if, we will generate significant revenue from its sale in the United States in the future. We do not anticipate
generating revenue from sales of XaraColl until at least the end of 2018 assuming that the FDA agrees with the proposals we presented
at our Type-A meeting, and we will never generate revenue from XaraColl if we do not obtain regulatory approval. While we have
products approved or commercialized and available for sale in certain markets, including CollatampG, RegenePro and Septocoll,
our revenues to date from these products have been limited.
Even if we do generate product sales, we
may never achieve or sustain profitability. We anticipate that our operating losses will substantially increase over the next
several years as we execute our plan to expand our research, development and commercialization activities, including the clinical
development and planned commercialization of our product candidates, and incur the additional costs of operating as a public company.
In addition, if we obtain regulatory approval of our product candidates, we may incur significant sales and marketing expenses.
Because of the numerous risks and uncertainties associated with developing pharmaceutical products, we are unable to predict the
extent of any future losses or when we will become profitable, if ever.
We need additional funding to support our operations
and capital expenditures, which may not be available to us. Our continued operating losses and limited capital raise substantial
doubt about our ability to continue as a going concern.
As of December 31, 2016, we had
an accumulated deficit of $223.1 million and cash and cash equivalents of $15.8 million. We anticipate that expenditures
during the next twelve months necessary to advance our current operations, including plans to conduct further studies to
enable us to submit a revised NDA for XaraColl and to develop and commercialize CollaGUARD will be greater than the amount of
our current cash and cash equivalents. This assessment is based on current estimates and assumptions regarding our
clinical programs and business needs. Our working capital requirements could vary depending on a variety of circumstances,
including, for example, if we are required to conduct additional tests not currently contemplated. These matters, among
others, raise substantial doubt about our ability to continue as a going concern. Based on the foregoing, we currently do not
have sufficient working capital to meet our needs through the next 12 months, from the date of approval of the financial
statements, unless we can successfully obtain additional funding through debt or equity transactions. Our financial
statements include an opinion of our auditors that our loss for the year of $57.0 million and accumulated loss of $223.1
million at December 31, 2016 raise substantial doubt about our ability to continue as an ongoing concern. Our ability to
successfully raise sufficient funds through the sale of equity securities or the identification of strategic alliances, when
needed, is subject to many risks and uncertainties and even if we are successful, future equity issuances would result in
dilution to our existing stockholders. In addition, to the extent that we might seek to raise capital through the
identification of strategic alliances, we may be required to license or transfer rights to our technologies to other parties
that we might otherwise desire to retain.
When we elect to raise additional funds
or additional funds are required, we may raise such funds from time to time through public or private equity offerings, debt financings,
corporate collaboration and licensing arrangements or other financing alternatives. Additional equity or debt financing or corporate
collaboration and licensing arrangements may not be available on acceptable terms, if at all. If we are unable to raise additional
capital in sufficient amounts or on terms acceptable to us, we will be prevented from pursuing acquisition, licensing, development
and commercialization efforts and our ability to generate revenues and achieve or sustain profitability will be substantially
harmed.
We
are currently exploring additional sources of capital; however, we do not know whether additional funding will be available on
acceptable terms, or at all, especially given the economic conditions that currently prevail. Furthermore, any additional equity
funding will likely result in significant dilution to existing stockholders, and, if we incur additional debt financing in the
future, a substantial portion of our operating cash flow may be dedicated to the payment of principal and interest on such indebtedness,
thus limiting funds available for our business activities. In addition, to the extent that we might seek to raise capital through
the identification of strategic alliances, we may be
required
to license or transfer rights to our technologies to other parties that we might otherwise desire to retain. If adequate funds
are not available, it would have a material adverse effect on our business, financial condition and/or results of operations and
could cause us to be required to cease operations.
If we fail to obtain additional financing, we may
be unable to complete the development and commercialization of our product candidates.
Our operations have consumed substantial
amounts of cash since inception. We expect to continue to spend substantial amounts to continue the clinical development of our
product candidates, including our Phase 3 clinical trials. If our product candidates are approved, we will require significant
additional funds in order to launch and commercialize such product candidates in the United States and potentially in the EU.
As of December 31, 2016, we had cash and cash equivalents of $15.8 million. Finally, we had trade and other payables of
$13.5 million and deferred income of $1.8 million (representing products to be delivered for which payment has already been received)
as of December 31, 2016.
Our rate of expenses will continue to increase
as we advance our commercialization efforts for XaraColl and CollaGUARD. As a result, we will be required to seek additional sources
of capital during the next six months and restrict certain of our expenditures to conserve capital and extend our
resources. Our need for additional capital will depend significantly on the level and timing of regulatory approval and product
sales, as well as the extent to which we choose to establish collaboration, co-promotion, distribution or other similar agreements
for our products and product candidates. Moreover, changing circumstances may cause us to spend cash significantly faster than
we currently anticipate, and we may need to spend more cash than currently expected because of circumstances beyond our control.
We expect to continue to incur substantial additional operating losses as we seek regulatory approval for and commercialize XaraColl
and CollaGUARD and develop and seek regulatory approval for our other product candidates. If we obtain FDA approval for our products,
we will incur significant sales, marketing and manufacturing expenses. In addition, we expect to incur additional expenses to
add operational, financial and information systems and personnel, including personnel to support our planned product commercialization
and expanded manufacturing efforts for Xaracoll and CollaGUARD in the United States. We also expect to incur significant costs
to continue to comply with corporate governance, internal controls and similar requirements applicable to us as a public company.
Our future funding requirements, both near-
and long-term, will depend on many factors, including, but not limited to:
|
·
|
the initiation,
progress, timing, costs and results of clinical trials and non-clinical studies for our
product candidates, particularly XaraColl, and the PMA application for CollaGUARD;
|
|
·
|
the clinical
development plans we establish for these product candidates;
|
|
·
|
the number
and characteristics of product candidates that we develop and seek regulatory approval
for;
|
|
·
|
the outcome,
timing and cost of regulatory approvals by the FDA and comparable foreign regulatory
authorities, including the potential for the FDA or comparable foreign regulatory authorities
to require that we perform more studies than those that we currently expect;
|
|
·
|
the cost of
filing, prosecuting, defending and enforcing any patent claims and other intellectual
property rights;
|
|
·
|
the effects
of competing technological and market developments;
|
|
·
|
the timing
of, and our ability to obtain, regulatory approvals for the expansion of our manufacturing
facility;
|
|
·
|
the cost and
timing of completion of commercial-scale manufacturing activities; and
|
|
·
|
the cost of
establishing sales, marketing and distribution capabilities for any product candidates
for which we may receive regulatory approval in regions where we choose to commercialize
our products on our own.
|
We cannot be certain that additional funding
will be available on acceptable terms, or at all. If we are unable to raise additional capital in sufficient amounts or on terms
acceptable to us, we may have to significantly delay, scale back or discontinue the development or commercialization of our product
candidates or other research and development initiatives. We also could be required to seek collaborators for our product candidates
at an earlier stage than would otherwise be desirable or on terms that are less favorable than might otherwise be available or
relinquish or license on unfavorable terms our rights to our product candidates in markets in which we would otherwise seek to
pursue development or commercialization ourselves.
Any of the above events could significantly
harm our business, prospects, financial condition and results of operations and cause the price of our securities to decline.
Our existing and any future indebtedness could
adversely affect our ability to operate our business.
Innocoll Germany and our wholly-owned subsidiary,
Innocoll Pharmaceuticals Limited, or Innocoll Pharmaceuticals, entered into a Finance Contract with the European Investment Bank,
or EIB, in March 2015 whereby the EIB has committed to lend to Innocoll Pharmaceuticals up to €25 million. We have drawn
down the entirety of the €25 million loan commitment. We could in the future incur additional debt obligations beyond our
borrowings from the EIB. The EIB loan, our existing loan obligations, together with other similar obligations that we may incur
in the future, could have significant adverse consequences, including:
|
·
|
requiring us
to dedicate a portion of our cash resources to pay for the principal and interest accrued
over the five year period of the loan that is payable at the end of the period,
which may limit available resource to fund working capital, capital expenditures, product
development and other general expenses;
|
|
·
|
increasing
our vulnerability to adverse changes in general economic, industry and market conditions;
|
|
·
|
subjecting
us to restrictive covenants that may reduce our ability to take certain corporate actions
or obtain further debt or equity financing and could take up management time dealing
with any consents required from lenders or other financing sources;
|
|
·
|
limiting our
flexibility in planning for, or reacting to, changes in our business and the industry
in which we compete; and
|
|
·
|
placing us
at a competitive disadvantage compared to our competitors that have less debt or better
debt servicing options.
|
We may not have sufficient funds, and may
be unable to arrange for additional financing, to pay the amounts due under our existing loan obligations. Failure to make payments
or comply with other covenants under our existing debt could result in an event of default and acceleration of amounts due. Under
our agreement with the EIB the occurrence of an event which would in the reasonable opinion of EIB have a material adverse effect
on our business, operations, property or condition (financial or otherwise) or prospects compared with our condition at the date
of the EIB facility agreement is an event of default. If an event of default occurs and the lender accelerates the amounts due,
we may not be able to make accelerated payments, and the lender could seek to enforce security interests in the collateral securing
such indebtedness, such as the shares in and assets of Innocoll Pharmaceuticals Limited, which include all of our assets. In addition,
the covenants under our existing debt, and the pledge of our assets as collateral, could limit our ability to obtain additional
debt financing.
We are exposed to foreign currency exchange rate fluctuations.
As of June 30, 2016, we no longer met the
requirements to qualify as a foreign private issuer under the Exchange Act. As a result, we began reporting as a domestic registrant
as of January 1, 2017. We are now required
under current SEC rules to prepare our consolidated financial
statements in accordance with U.S. GAAP, rather than International Financial Reporting Standards or IFRS, and to present our financial
information in U.S. dollars instead of euros. The functional currency of the Company is the U.S. dollar. If we incur portions
of our expenses and derive revenues in currencies other than the U.S. dollar, we may be exposed to foreign currency exchange risk.
For example, in 2016, 99% of our revenues were generated and approximately 24% of our costs were incurred in euros. Foreign exchange
risk exposure may also arise from intra-company transactions and financing with subsidiaries that have a functional currency different
than the U.S. dollar.
Transactions in currencies other than the
functional currency of the Company entities are recorded at the exchange rates prevailing at the dates of the related transactions.
Foreign exchange gains and losses resulting from the settlement of such transactions, as well as from the translation at year-end
exchange rates of monetary assets and liabilities denominated in foreign currencies, are recognized in the consolidated statements
of operations and comprehensive loss. At each balance sheet date, monetary assets and liabilities that are denominated in foreign
currencies are translated to the respective functional currencies of the Company’s entities at the rates prevailing on the
relevant balance sheet date.
The resulting translation adjustments are
included in equity under the caption “Accumulated Currency Translation Adjustment” in the consolidated statement
of changes in (deficit)/equity.
We do not currently engage in currency
swaps or other currency hedging transactions. There can be no assurance that we will be successful in managing our foreign currency
exchange rate risk. We cannot predict the impact of foreign currency fluctuations, and foreign currency fluctuations in the future
may adversely affect our financial condition, results of operations and cash flows.
Risks Related to the Clinical Development and Regulatory
Approval of Our Product Candidates
Our business depends substantially on the success
of our lead product candidate, XaraColl, which is still in development. If we are unable to successfully develop and subsequently
commercialize XaraColl, or experience significant delays in doing so, our business will be materially harmed.
We have invested a significant portion
of our efforts and financial resources in the development of XaraColl, our lead product candidate, which has not yet been approved
for commercial sale in the United States or in Europe and Cogenzia, which we have abandoned. There remains a significant
risk that we will fail to successfully develop XaraColl. In February 2017, our representatives attended a Type-A meeting with
representatives of the FDA to review potential pathways forward following our receipt of the Refusal to File Letter and to review
a proposed plan for proceeding with additional studies that would allow us to file a revised NDA for XaraColl. During the meeting,
we proposed a plan designed to allow us to submit a revised NDA to the FDA by the latter part of 2017. We proposed conducting
an additional short-term pharmacokinetic study and several short-term non-clinical studies. Under current practice before the
FDA, we received limited feedback during the meeting and we expect to receive shortly from the representatives of the FDA formal
written meeting minutes of our Type-A meeting, which will serve as the official record of the response of the FDA to our proposal
during the meeting. If the FDA concurs with our plan, we will commence the additional studies, and if the results are positive,
we would submit a revised NDA to the FDA soon after the completion of the studies. However, if the FDA suggests that studies beyond
those that we proposed would be necessary, or if the results of the studies that we proposed are not positive, we would not likely
be able to submit our revised NDA for an extended period of time, if at all.
The success of, and our ability to generate
future revenues from, our product candidates will depend on several factors, including:
|
·
|
successful
completion of clinical trials and non-clinical studies;
|
|
·
|
receipt of
U.S. and/or foreign regulatory approvals for our product candidates from applicable regulatory
authorities;
|
|
·
|
maintaining
regulatory compliance for our manufacturing facility;
|
|
·
|
manufacturing
sufficient commercial quantities in acceptable quality and at acceptable costs;
|
|
·
|
achieving meaningful
commercial sales of our product candidates, if and when approved;
|
|
·
|
obtaining reimbursement
from third-party payors for product candidates, if and when approved;
|
|
·
|
sourcing sufficient
quantities of raw materials used to manufacture our products;
|
|
·
|
successfully
competing with other products;
|
|
·
|
continued acceptable
safety and effectiveness profiles for our product candidates following regulatory approval,
if and when received;
|
|
·
|
pursuing clinical
development of our product candidates for additional indications.
|
|
·
|
the
regulatory framework and approval process we may become subject to in the event the FDA
classifies XaraColl or any of our other product candidiates as a drug/device combination;
|
|
·
|
obtaining and
maintaining patent and trade secret protection and regulatory exclusivity; and
|
|
·
|
protecting
our intellectual property rights.
|
If we do not achieve one or more of these
factors in a timely manner, or at all, we could experience significant delays or an inability to successfully commercialize our
product candidates, which would materially harm our business and we may not be able to earn sufficient revenues and cash flows
to continue our operations.
We may not receive a general indication of postoperative
analgesia for XaraColl, which would have an adverse effect on our ability to market XaraColl for use in surgical procedures other
than those studied in our Phase 3 trials and could adversely affect our business and financial results.
We may not receive a general indication
of postoperative analgesia for XaraColl, which would have an adverse effect on our ability to market XaraColl for use in surgical
procedures other than those studied in our Phase 3 trials and could adversely affect our business and financial results.
The FDA strictly regulates marketing, labeling,
advertising and promotion of prescription drugs. These regulations include standards and restrictions for direct-to-consumer advertising,
industry-sponsored scientific and educational activities, promotional activities involving the Internet and off-label promotion.
The FDA generally does not allow drugs to be promoted for “Off-label” uses—that is, uses that are not described
in the product’s labeling and that differ from those that were approved by the FDA. In addition to the FDA approval required
for new formulations, any new indication for an approved product also requires FDA approval.
If we are not able to obtain FDA approval
for a label including any desired future indications for XaraColl outside of open hernioplasty or for efficacy beyond the initial
24 hour post-operative period, our ability to effectively market and sell XaraColl may be limited, and our business may be adversely
affected. Our goal for XaraColl is to ultimately seek an indication for administration into the surgical site to produce post-surgical
analgesia. Prior to conducting our Phase 3 trials for XaraColl, the FDA advised us that an indication for postoperative analgesia
following laparotomy for inguinal herniorrhaphy with mesh may be more appropriate than a general indication for postoperative
analgesia until it is known whether location, wound size, or other factors affect efficacy or safety. The FDA also recommended
that we evaluate the safety and efficacy for XaraColl following other surgical procedures including open herniorrhaphy without
mesh, unless there are specific reasons not to evaluate other clinical settings. Subsequent to providing this advice, it was reported
that the FDA and Pacira Pharmaceuticals, Inc., a specialty pharmaceutical company, settled ongoing litigation concerning the label
indication of Pacira’s Exparel product (bupivacaine liposome injectable suspension). The FDA confirmed that Exparel has
always been approved for “administration into the surgical site to produce postsurgical analgesia” for use in a variety
of surgeries not limited to those studied in its pivotal trials. Although we are not aware of the details of the discussions between
FDA and Pacira leading up to the reported settlement, we intend to use a similar justification to attempt to support a broad post-surgical
analgesia indication for XaraColl.
While physicians in the United States
may choose, and are generally permitted to prescribe drugs for uses that are not described in the product’s labeling,
and for uses that differ from those tested in clinical studies and approved by the regulatory authorities, our ability to
promote our products is narrowly limited to those indications that are specifically approved by the FDA.
“Off-label” uses are common across medical specialties and may constitute an appropriate treatment for some
patients in varied circumstances. Regulatory authorities in the United States generally do not regulate the behavior of
physicians in their choice of treatments. Regulatory authorities do, however, restrict communications by pharmaceutical
companies on the subject of off-label use. Although recent court decisions suggest that certain off-label promotional
activities may be protected under the First Amendment, the scope of any such protection is unclear. Moreover, while we intend
to promote our products consistent with what we believe to be the approved indication for our drugs, the FDA may disagree. If
the FDA determines that our promotional activities fail to comply with the FDA’s regulations or guidelines, we may be
subject to warnings from, or enforcement action by, the agency. In addition, our failure to follow FDA rules and guidelines
relating to promotion and advertising may cause the FDA to issue warning letters or untitled letters, bring an enforcement
action against us, suspend or withdraw an approved product from the market, request a recall or institute fines or civil
fines, or could result in disgorgement of money, operating restrictions, injunctions or criminal prosecution, any of which
could harm our reputation and our business.
Clinical drug development is expensive and involves
uncertain outcomes, and results of earlier studies and trials may not be predictive of future trial results. If our clinical trials
for XaraColl are unsuccessful, or significantly delayed, we could be required to abandon development and our business will be
materially harmed
.
Clinical testing is expensive and can take
many years to complete, and its outcome is inherently uncertain. Failure can occur at any time during the clinical trial process.
In February 2017, our representatives attended a Type-A meeting with representatives of the FDA to review potential pathways
forward following our receipt of the Refusal to File Letter and to review a proposed plan for proceeding with additional studies
that would allow us to file a revised NDA for XaraColl. During the meeting, we proposed a plan designed to allow us to submit
a revised NDA to the FDA by the latter part of 2017. We proposed conducting an additional short-term pharmacokinetic study and
several short-term non-clinical studies. Under current practice before the FDA, we received limited feedback during the meeting
and we expect to receive shortly from the representatives of the FDA formal written meeting minutes of our Type-A meeting, which
will serve as the official record of the response of the FDA to our proposal during the meeting. If the FDA concurs with our plan,
we will commence the additional studies, and if the results are positive, we would submit a revised NDA to the FDA soon after
the completion of the studies. However, if the FDA suggests that studies beyond those that we proposed would be necessary, or
if the results of the studies that we proposed are not positive, we would not likely be able to submit our revised NDA for an
extended period of time, if at all.
Furthermore, despite encouraging earlier
trial results for Cogenzia, our Phase 3 study failed to meet its primary endpoints and the program was discontinued. We cannot
provide assurances that following additional studies, the same will not happen for XaraColl or any of our other product candidates.
In some instances, there can be significant
variability in safety and/or efficacy results between different trials of the same product candidate due to numerous factors,
including changes in or adherence to trial protocols, differences in the size and type of patient populations and the dropout
rates among clinical trial participants. Our future clinical trial results, therefore, may not demonstrate efficacy and safety
sufficient to obtain regulatory approval for our product candidates.
Flaws in the design of a clinical trial
may not become apparent until the clinical trial is well under way. We have limited experience in designing clinical trials and
may be unable to design and execute a clinical trial to support regulatory approval. In addition, clinical trials often reveal
that it is not practical or feasible to continue development efforts.
We may voluntarily suspend or terminate
our clinical trials if at any time we believe that they present an unacceptable risk to participants. Further, regulatory agencies,
institutional review boards or data safety monitoring boards may at any time order the temporary or permanent discontinuation
of our clinical trials or request that we cease using certain investigators in the clinical trials if they believe that the clinical
trials are not being conducted in accordance with applicable regulatory requirements or that they present an unacceptable safety
risk to participants.
If the results of our clinical trials for
our current product candidates or clinical trials for any future product candidates do not achieve their primary efficacy endpoints
or raise unexpected safety issues, the prospects for approval of our product candidates will be materially adversely affected.
Moreover, preclinical and clinical data are often susceptible to varying interpretations and analyses and many companies that
believed their product candidates performed satisfactorily in preclinical studies and clinical trials have failed to achieve similar
results in later clinical trials, or have ultimately failed to obtain regulatory approval of their product candidates. Many products
that initially showed promise in clinical trials or earlier stage testing have later been found to cause undesirable or unexpected
adverse effects that have prevented their further development.
In addition, we may experience numerous
unforeseen events that could cause our clinical trials to be delayed, suspended or terminated, or which could delay or prevent
our ability to receive regulatory approval or commercialize our product candidates, including:
|
·
|
delay or failure
in reaching agreement with the FDA or comparable foreign regulatory authorities on trial
designs that we are able to execute;
|
|
·
|
the number
of patients required for clinical trials of our product candidates may be larger than
we anticipate, enrollment in these clinical trials may be slower than we anticipate or
participants may drop out of these clinical trials at a higher rate than we anticipate;
|
|
·
|
clinical trials
of our product candidates may produce negative, inconclusive or inconsistent results,
and we may decide, or regulators may require us, to conduct additional clinical trials
or implement a clinical hold;
|
|
·
|
we may elect
or be required to suspend or terminate clinical trials of our product candidates, including
based on a finding that the participants are being exposed to unacceptable health risks;
|
|
·
|
regulators
or institutional review boards may not authorize us or our investigators to commence
or continue a clinical trial, or conduct or continue a clinical trial at a prospective
trial site;
|
|
·
|
our third-party
contractors may fail to comply with regulatory requirements or meet their contractual
obligations to us in a timely manner, or at all;
|
|
·
|
we may have
delays in reaching or fail to reach agreement on acceptable clinical trial contracts
or clinical trial protocols with prospective trial sites;
|
|
·
|
the cost of
clinical trials of our product candidates may be greater than we anticipate;
|
|
·
|
changes in
government regulation or administrative actions;
|
|
·
|
the supply
or quality of our product candidates or other materials necessary to conduct clinical
trials of our product candidates may be insufficient or inadequate; and
|
|
·
|
our product
candidates may have undesirable adverse effects or other unexpected characteristics.
|
Patient enrollment, a significant factor
in the timing of clinical trials, is affected by many factors including the size and nature of the patient population, the proximity
of subjects to clinical sites, the eligibility criteria for the trial, the design of the clinical trial, ability to obtain and
maintain patient consents, risk that enrolled subjects will drop out before completion, competing clinical trials and clinicians’
and patients’ perceptions of the potential advantages of the drug being studied in relation to other available therapies,
including any new drugs that may be approved for the indications we are investigating.
If we experience delays in the completion
of, or termination of, any clinical trial of our product candidates, the commercial prospects of our product candidates will be
materially harmed, and our ability to generate product revenues from any of these product candidates will cease or be delayed.
In addition, any termination of, or delays in completing,
our clinical trials will increase our costs,
slow down our product candidate development and approval process and jeopardize our ability to commence product sales and generate
revenues. Any of these occurrences may significantly harm our business, financial condition and prospects. In addition, many of
the factors that cause, or lead to a delay in the commencement or completion of or early termination of, clinical trials may also
ultimately lead to the denial of regulatory approval of our product candidates.
We may not receive a general indication of postoperative
analgesia for XaraColl, which would have an adverse effect on our ability to market XaraColl for use in surgical procedures other
than those studied in our Phase 3 trials and could adversely affect our business and financial results.
The FDA strictly regulates marketing, labeling,
advertising and promotion of prescription drugs. These regulations include standards and restrictions for direct-to-consumer advertising,
industry-sponsored scientific and educational activities, promotional activities involving the Internet and off-label promotion.
The FDA generally does not allow drugs to be promoted for “Off-label” uses — that is, uses that
are not described in the product’s labeling and that differ from those that were approved by the FDA. In addition to the
FDA approval required for new formulations, any new indication for an approved product also requires FDA approval.
If we are not able to obtain FDA approval
for any desired future indications for XaraColl outside of open hernioplasty, our ability to effectively market and sell XaraColl
may be limited, and our business may be adversely affected.
While physicians in the United States may
choose, and are generally permitted to prescribe drugs for uses that are not described in the product’s labeling, and for
uses that differ from those tested in clinical studies and approved by the regulatory authorities, our ability to promote our
products is narrowly limited to those indications that are specifically approved by the FDA. “Off-label” uses are
common across medical specialties and may constitute an appropriate treatment for some patients in varied circumstances. Regulatory
authorities in the United States generally do not regulate the behavior of physicians in their choice of treatments. Regulatory
authorities do, however, restrict communications by pharmaceutical companies on the subject of off-label use. Although recent
court decisions suggest that certain off-label promotional activities may be protected under the First Amendment, the scope of
any such protection is unclear. Moreover, while we intend to promote our products consistent with what we believe to be the approved
indication for our drugs, the FDA may disagree. If the FDA determines that our promotional activities fail to comply with the
FDA’s regulations or guidelines, we may be subject to warnings from, or enforcement action by, these authorities. In addition,
our failure to follow FDA rules and guidelines relating to promotion and advertising may cause the FDA to issue warning letters
or untitled letters, bring an enforcement action against us, suspend or withdraw an approved product from the market, require
a recall or institute fines or civil fines, or could result in disgorgement of money, operating restrictions, injunctions or criminal
prosecution, any of which could harm our reputation and our business.
If our drug/device combination product candidates,
such as XaraColl, receive regulatory approval, we will be subject to ongoing regulatory requirements and we may face future development,
manufacturing and regulatory difficulties.
Our drug/device combination product candidates,
such as XaraColl, if approved, will be subject to ongoing regulatory requirements for labeling, packaging, storage, advertising,
promotion, sampling, record-keeping, submission of safety and other post-market approval information, importation and exportation.
In addition, approved products, manufacturers and manufacturers’ facilities are required to comply with extensive FDA and
European Medicines Agency, or EMA, requirements and the requirements of other similar agencies, including ensuring that quality
control and manufacturing procedures conform to cGMP requirements.
Accordingly, we will be required to expend
time, money and effort in all areas of regulatory compliance, including manufacturing, production and quality control. We will
also be required to report certain adverse reactions and production problems, if any, to the FDA and EMA and other similar agencies
and to comply with certain requirements concerning advertising and promotion for our potential products.
If a regulatory agency discovers previously
unknown problems with a product, such as adverse events of unanticipated severity or frequency, or problems with the facility
where the product is manufactured, or disagrees with
the promotion, marketing or labeling of a
product, it may impose restrictions on that product or us, including requiring withdrawal of the product from the market. If our
potential products fail to comply with applicable regulatory requirements, a regulatory agency may, among other actions:
|
·
|
issue warning
letters or untitled letters;
|
|
·
|
require product
recalls;
|
|
·
|
mandate modifications
to promotional materials or require us to provide corrective information to healthcare
practitioners;
|
|
·
|
require us
or our potential future collaborators to enter into a consent decree or permanent injunction;
|
|
·
|
impose other
administrative or judicial civil or criminal actions, including monetary or other penalties,
or pursue criminal prosecution;
|
|
·
|
withdraw regulatory
approval;
|
|
·
|
refuse to approve
pending applications or supplements to approved applications filed by us or by our potential
future collaborators;
|
|
·
|
impose restrictions
on operations, including costly new manufacturing requirements; or
|
|
·
|
seize or detain
products.
|
Risks Related to Our Business and Strategy
If we fail to manufacture XaraColl, CollaGUARD
or our other marketed products and product candidates in sufficient quantities and at acceptable quality and cost levels, or to
fully comply with cGMP or other applicable manufacturing regulations, we may face a bar to, or delays in, the commercialization
of our products, breach obligations to our licensing partners or be unable to meet market demand, and lose potential revenues.
The manufacture of our products based on
our collagen-based technology platform, including XaraColl, requires significant expertise and capital investment. Currently,
we are manufacturing all commercial and clinical supply for all of our marketed products and product candidates in our sole facility
in Saal, Germany without the benefit of any redundant or backup facilities. Also, substantially all of our inventory of raw material
and finished goods is held at this location. We take precautions to safeguard our facility, including acquiring insurance, employing
back-up generators, adopting health and safety protocols and utilizing off-site storage of computer data. However, vandalism,
terrorism or a natural or other disaster, such as a fire or flood, could damage or destroy our manufacturing equipment or our
inventory of raw material or finished goods, cause substantial delays in our operations, result in the loss of key information,
and cause us to incur additional expenses. Our insurance may not cover our losses in any particular case. In addition, regardless
of the level of insurance coverage, damage to our facilities may have a material adverse effect on our business, financial condition
and operating results. In addition, our competitors have substantially greater financial, technical and other resources, such
as a larger staff and experienced manufacturing organizations.
We must comply with federal, state and
foreign regulations, including FDA regulations governing cGMP enforced by the FDA through its facilities inspection program and
by similar regulatory authorities in other jurisdictions where we do business. These requirements include, among other things,
quality control, quality assurance and the maintenance of records and documentation. For our medical device products, we are required
to comply with the FDA’s Quality System Regulation, or QSR, which covers the methods and documentation of the design, testing,
production, control, quality assurance, labeling, packaging, sterilization, storage and shipping of our medical device products.
Our facility has not yet been inspected
by the FDA for cGMP compliance. If we do not successfully achieve cGMP compliance for our facility in a timely manner, commercialization
of our products could be prohibited or significantly delayed. Even after cGMP compliance has been achieved, the FDA or similar
foreign regulatory
authorities at any time may implement new
standards, or change their interpretation and enforcement of existing standards for manufacture, packaging, testing of or other
activities related to our products. For our marketed medical device products, the FDA audits compliance with the QSR through periodic
announced and unannounced inspections of manufacturing and other facilities. The FDA may conduct inspections or audits at any
time. Similar audit rights exist in Europe and other foreign jurisdictions. Any failure to comply with applicable cGMP, QSR and
other regulations may result in fines and civil penalties, suspension of production, product seizure or recall, imposition of
a consent decree, or withdrawal of product approval, and would limit the availability of our product. Any manufacturing defect
or error discovered after products have been produced and distributed also could result in significant consequences, including
adverse health consequences, injury or death to patients, costly recall procedures, re-stocking costs, damage to our reputation
and potential for product liability claims. If we are required to find a new manufacturer or supplier, the process would likely
require prior FDA and/or equivalent foreign regulatory authority approval, and would be very time consuming. An inability to continue
manufacturing adequate supplies of our products at our facility in Saal, Germany, could result in a disruption in the supply of
our products. We have licensed the commercial rights in specified foreign territories to market and sell our products. Under those
licenses, we have obligations to manufacture commercial product for our commercial partners. If we are unable to fill the orders
placed with us by our commercial partners in a timely manner, we may potentially lose revenue and be in breach of our licensing
obligations under agreements with them.
We have not obtained regulatory approval for any
of our late-stage product candidates in the United States, so we cannot yet generate any revenues from the sales of these products
in the United States.
Our late-stage product candidates, XaraColl
and CollaGUARD, have not yet been approved for commercial sale in the United States. We cannot commercialize product candidates
in the United States without first obtaining regulatory approval from the FDA to market each product. Before obtaining regulatory
approvals for the commercial sale of any product candidate for a target indication, we must demonstrate in non-clinical, or preclinical,
studies and clinical trials, and, with respect to approval in the United States, to the satisfaction of the FDA, that the product
candidate is safe and effective for use under the labeled conditions for use and that the manufacturing facilities, processes
and controls are adequate. We expect to submit a revised NDA for XaraColl following our receipt of the minutes from our Type-A
meeting with the FDA, provided that the FDA concurs with our plan to commence the additional studies proposed by
our management, and if the results of those studies are positive. However, if the FDA suggests that studies beyond those that
we proposed would be necessary, or if the results of the studies that we proposed are not positive, we would not likely be able
to submit our revised NDA for an extended period of time, if at all.
An NDA must include extensive preclinical
and clinical data and supporting information to establish the product candidate’s safety and effectiveness for each desired
indication. The NDA must also include significant information regarding the chemistry, manufacturing and controls for the product
and its components, and draft labeling. Obtaining approval of an NDA is a lengthy, expensive and uncertain process, and approval
may not be obtained. If we submit an NDA to the FDA, the FDA must decide whether to accept or reject the submission for filing.
We cannot be certain that any of our submissions will be accepted for filing and review by the FDA, or that the FDA will approve
the application if it accepts it.
Regulatory authorities outside of the United
States, such as in Europe and in emerging markets, also have requirements for approval of products for commercial sale with which
we must comply prior to marketing in those areas. Regulatory requirements can vary widely from country to country and could delay
or prevent the introduction of our product candidates. Clinical trials conducted in one country may not be accepted by regulatory
authorities in other countries, and obtaining regulatory approval in one country does not mean that regulatory approval will be
obtained in any other country. Approval processes vary among countries and can involve additional product testing and validation
and additional administrative review periods. Seeking foreign regulatory approval could require additional non-clinical studies
or clinical trials, which could be costly and time consuming. The foreign regulatory approval process may include all of the risks
associated with obtaining FDA approval, and potentially may include additional risks.
The process to develop, obtain regulatory
approval for, and commercialize product candidates is long, complex and costly both inside and outside of the United States, and
approval is not guaranteed. Even if we successfully obtain approval from the regulatory authorities for our product candidates,
any approval might significantly limit the approved indications for use, or require that precautions, contraindications or warnings
be included on the product labeling that
limit its commercialization, or limit its
commercialization through a Risk Evaluation and Mitigation Strategy, or REMS, that restricts who may prescribe or dispense the
product or imposes other significant limits to assure safe use, or require expensive and time-consuming post-approval clinical
studies or surveillance as conditions of approval. Following any approval for commercial sale of our product candidates, certain
changes to the product, such as changes in manufacturing processes and additional labeling claims, will be subject to additional
regulatory review and approval. In addition, regulatory approval for any of our product candidates may be withdrawn. If we are
unable to obtain regulatory approval for our product candidates in one or more jurisdictions, or if any approval we do obtain
contains significant limitations, our target market will be reduced and our ability to realize the full market potential of our
product candidates will be harmed. Furthermore, we may not be able to obtain sufficient funding or generate sufficient revenue
and cash flows to continue the development of any other product candidate in the future.
If we fail to develop and commercialize additional
product candidates, we may be unable to grow our business.
If we decide to pursue the development
and commercialization of any additional product candidates, we may be required to invest significant resources to acquire or in-license
the rights to such product candidates or to conduct product discovery activities. In addition, any other product candidates will
require additional, time-consuming development efforts prior to commercial sale, including preclinical studies, extensive clinical
trials and approval by the FDA and applicable foreign regulatory authorities. All product candidates are prone to the risk of
failure that is inherent in therapeutic product development, including the possibility that the product candidate will not be
shown to be sufficiently safe and/or effective for approval by regulatory authorities. In addition, we cannot assure you that
we will be able to acquire, discover or develop any additional product candidates, or that any additional product candidates we
may develop will be approved, manufactured or produced economically; successfully commercialized; or widely accepted in the marketplace
or be more effective than other commercially available alternatives. Research programs to identify new product candidates require
substantial technical, financial and human resources whether or not we ultimately identify any candidates. If we are unable to
develop or commercialize additional product candidates, our business and prospects will suffer.
We have engaged in only limited sales of our products
to date, 87% of which are to one customer for the year ended December 31, 2016.
While we are a global, commercial-stage,
specialty pharmaceutical and medical device company, with late-stage development programs targeting areas of significant unmet
medical needs, we have engaged in only limited sales of our products to date with approximately 87% of our sales being generated
by one customer in the year ended December 31, 2016. Our products may never gain significant acceptance in the marketplace and,
therefore, never generate substantial revenue or profits for the company. We must establish a market for our products and build
that market through marketing campaigns to increase awareness of, and consumer confidence in, our products. If we are unable to
expand our current customer base and obtain market acceptance of our products, our operations could be disrupted and our business
may be materially adversely affected. Even if we achieve profitability, we may not be able to sustain or increase profitability.
We face significant competition from other pharmaceutical
and medical device companies and our operating results will suffer if we fail to compete effectively.
The pharmaceutical and medical device industry
is characterized by intense competition and rapid innovation. Although we believe that we hold a leading position in our understanding
of collagen-based therapeutic products, our competitors may be able to develop other products that are able to achieve similar
or better results. Our potential competitors include established and emerging pharmaceutical and biotechnology companies and universities
and other research institutions. Many of our competitors have substantially greater financial, technical and other resources,
such as larger research and development staff and experienced marketing and manufacturing organizations and well-established sales
forces. Smaller or early-stage companies may also prove to be significant competitors, particularly through collaborative arrangements
with large, established companies. Mergers and acquisitions in the pharmaceutical and biotechnology industries may result in even
more resources being concentrated in our competitors. Competition may increase further as a result of advances in the commercial
applicability of technologies and greater availability of capital for investment in these industries. Our competitors may succeed
in developing, acquiring or licensing on an exclusive basis products that are more effective or less costly than our product candidates.
We believe the key
competitive factors that will affect the
development and commercial success of our product candidates are efficacy, safety and tolerability profile, reliability, price
and reimbursement.
We anticipate that XaraColl will compete
in the United States with currently marketed bupivacaine and opioid analgesics such as morphine, as well as elastomeric bag/catheter
devices intended to provide bupivacaine over several days, which have been marketed by I-FLOW Corporation (owned by Halyard Health)
since 2004; and Pacira Pharmaceutical’s Exparel, a liposomal injection of bupivacaine, indicated for single-dose infiltration
into the surgical site to produce postsurgical analgesia. Once approved in the United States, CollaGUARD will compete with a number
of well-accepted adhesion barriers marketed in the United States and elsewhere by well-established companies, including Sanofi’s
Seprafilm®, Baxter’s Adept®, Ethicon’s Interceed® and Mast Biosurgery’s Surgiwrap®.
The financial performance of our medical device
products, such as CollaGUARD, may be adversely affected by medical device tax provisions in the healthcare reform laws in the
United States.
The Patient Protection and Affordable Care
Act, as amended by the Health Care and Education Reconciliation Act of 2010, or collectively, the Affordable Care Act, imposes,
among other things, an annual excise tax of 2.3% on any entity that manufactures or imports medical devices offered for sale in
the United States beginning with tax year 2013. Under these provisions, the Congressional Research Service predicts that the total
cost to the medical device industry may be up to $20 billion over the next decade. We do not believe that CollaGUARD is currently
subject to this tax based on the retail exemption under applicable Treasury Regulations. However, the availability of this exemption
is subject to interpretation by the IRS, and the IRS may disagree with our analysis. In addition, future products that we manufacture,
produce or import may be subject to this tax. The financial impact this tax may have on our business is unclear and there can
be no assurance that our business will not be materially adversely affected by it.
Since its enactment, there have been
judicial and Congressional challenges to numerous provisions of the Affordable Care Act. In January 2017, Congress voted to adopt
a budget resolution for fiscal year 2017, or the Budget Resolution, that authorizes the implementation of legislation that would
repeal portions of the Affordable Care Act. The Budget Resolution is not a law, but it is widely viewed as the first step toward
the passage of legislation that would repeal certain aspects of the Affordable Care Act. Further, on January 20, 2017, President
Trump signed an Executive Order directing federal agencies with authorities and responsibilities under the Affordable Care Act
to waive, defer, grant exemptions from, or delay the implementation of any provision of the Affordable Care Act that would impose
a fiscal or regulatory burden on states, individuals, healthcare providers, health insurers, or manufacturers of pharmaceuticals
or medical devices. Congress also could consider subsequent legislation to replace elements of the Affordable Care Act that are
repealed. We will continue to evaluate the effect that the Affordable Care Act and any future measures to repeal or replace the
Affordable Care Act have on our business.
If we face allegations of noncompliance with the
law and encounter sanctions, our reputation, revenues and liquidity may suffer, and our products could be subject to restrictions
or withdrawal from the market.
Any government investigation of alleged
violations of law could require us to expend significant time and resources in response and could generate negative publicity.
Any failure to comply with ongoing regulatory requirements may significantly and adversely affect our ability to commercialize
and generate revenues from our products. If regulatory sanctions are applied or if regulatory approval is withdrawn, the value
of our company and our operating results will be adversely affected. Additionally, if we are unable to generate revenues from
our product sales, our potential for achieving profitability will be diminished and the capital necessary to fund our operations
will be increased.
Even if we obtain regulatory approval for our product
candidates, the products may not gain market acceptance among hospitals, physicians, health care payors, patients and others in
the medical community.
Even if we obtain regulatory approval for
any of our product candidates that we may develop or acquire in the future, the product may not gain market acceptance among hospitals,
physicians, health care payors, patients and others in the medical community. Market acceptance of any of our product candidates
for which we receive approval depends on a number of factors, including:
|
·
|
the clinical
indications for which they are approved;
|
|
·
|
the product
labeling, including warnings, precautions, side effects, and contraindications that the
FDA approves;
|
|
·
|
the potential
and perceived advantages of our product candidates over alternative products;
|
|
·
|
relative convenience
and ease of administration;
|
|
·
|
the effectiveness
of our sales and marketing efforts;
|
|
·
|
acceptance
by major operators of hospitals, physicians and patients of the product candidate as
a safe and effective treatment;
|
|
·
|
the prevalence
and severity of any side effects;
|
|
·
|
product labeling
or product insert requirements of the FDA or other regulatory authorities;
|
|
·
|
any REMS that
the FDA might require;
|
|
·
|
the timing
of market introduction of our product candidates as well as competitive products;
|
|
·
|
the cost of
treatment in relation to alternative products; and
|
|
·
|
the availability
of adequate reimbursement and pricing by third-party payors and government authorities.
|
If our product candidates are approved but fail
to achieve market acceptance among physicians, patients, payors, or others in the medical community, we will not be able to generate
significant revenues, which would have a material adverse effect on our business, prospects, financial condition and results of
operations.
If our product candidates are approved,
and with respect to our already approved products, we may be subject to healthcare laws, regulation and enforcement. Our failure
to comply with those laws could have a material adverse effect on our results of operations and financial conditions.
Although we currently do not have any of
our lead products on the market in the United States and several other key jurisdictions, if our lead-product candidates are approved,
once we begin commercializing our product candidates, we may be subject to additional healthcare regulation and enforcement by
the U.S. federal government and by authorities in the states and foreign jurisdictions in which we conduct our business. In certain
jurisdictions outside of the United States where we currently market certain of our products, we are already subject to such regulation
and enforcement. Such laws include, without limitation, state and federal anti-kickback, false claims, privacy, security, “sunshine,”
and trade regulation and advertising laws and regulations. If our operations are found to be in violation of any of such laws
or any other governmental regulations that apply to us, we may be subject to penalties, including, but not limited to, civil and
criminal penalties, damages, fines, the curtailment or restructuring of our operations, the exclusion from participation in federal
and state healthcare programs and imprisonment, any of which could adversely affect our ability to operate our business and our
financial results.
A recall of our drug or medical device products,
or the discovery of serious safety issues with our drug or medical device products, could have a significant negative impact on
us.
The FDA and other relevant regulatory agencies
have the authority to require or request the recall of commercialized products in the event of material deficiencies or defects
in design or manufacture or in the event that a product poses an unacceptable risk to health. Manufacturers may, under their own
initiative, recall a product. A government-mandated or voluntary recall by us or one of our distributors could occur as a result
of an unacceptable risk to health, component failures, manufacturing errors, design or labeling defects or other deficiencies
and issues. Recalls of any of our products would divert managerial and financial resources and have an adverse effect on our reputation,
financial condition and operating results, which could impair our ability to produce our products in a cost-effective and timely
manner.
Further, under the FDA’s medical
device reporting, or MDR, regulations, we are required to report to the FDA any event which reasonably suggests that our product
may have caused or contributed to a death or serious injury or in which our product malfunctioned and, if the malfunction of the
same or similar device marketed by us were to recur, would likely cause or contribute to death or serious injury. The FDA also
requires reporting of serious, life-threatening, unexpected and other adverse drug experiences and the submission of periodic
safety reports and other information. Product malfunctions or other adverse event reports may result in a voluntary or involuntary
product recall and other adverse actions, which could divert managerial and financial resources, impair our ability to manufacture
our products
in a cost-effective and timely manner and
have an adverse effect on our reputation, financial condition and operating results. Similar reporting requirements exist in Europe
and other jurisdictions.
Any adverse event involving our products
could result in future voluntary corrective actions, such as recalls or customer notifications, or regulatory agency action, which
could include inspection, mandatory recall or other enforcement action. Any corrective action, whether voluntary or involuntary,
will require the dedication of our time and capital, distract management from operating our business and may harm our reputation
and financial results.
Our medical device products, such as CollaGUARD,
are subject to extensive governmental regulation, and failure to comply with applicable requirements could cause our business
to suffer.
The medical device industry is regulated
extensively by governmental authorities, principally the FDA and corresponding state and foreign governmental agencies. The regulations
are very complex and are subject to rapid change and varying interpretations. Regulatory restrictions or changes could limit our
ability to carry on or expand our operations or result in higher than anticipated costs or lower than anticipated sales. The FDA
and other United States or foreign governmental agencies regulate numerous elements of our business, including:
|
·
|
product design
and development;
|
|
·
|
pre-clinical
and clinical testing and trials;
|
|
·
|
establishment
registration and product listing;
|
|
·
|
pre-market
clearance, approval or other authorization;
|
|
·
|
advertising
and promotion;
|
|
·
|
marketing,
manufacturing, sales and distribution;
|
|
·
|
adverse event
reporting;
|
|
·
|
servicing and
post-market surveillance; and
|
|
·
|
recalls and
field safety corrective actions.
|
Before we can market or sell a new regulated
product or a significant modification to an existing product in the United States, we must obtain either marketing clearance under
Section 510(k) of the Federal Food, Drug and Cosmetic Act, or FDCA, de novo review marketing authorization, or approval of a premarket
approval application, or PMA, from the FDA, unless an exemption from premarket clearance and approval applies. In the 510(k) clearance
process, the FDA must determine that a proposed device is “substantially equivalent” to a device legally on the market,
known as a “predicate” device, with respect to intended use, technology and safety and effectiveness, in order to
clear the proposed device for marketing. Clinical data are sometimes required to support substantial equivalence. Some products
which are not substantially equivalent to a predicate device can undergo the de novo review process for purposes of marketing
authorization. The PMA pathway requires an applicant to demonstrate the safety and effectiveness of the device based on extensive
clinical data. The PMA process is typically required for devices that are deemed to pose the greatest risk, such as life-sustaining,
life-supporting or certain implantable devices. Products that are approved through a PMA application generally need FDA approval
before they can be modified. Similarly, some modifications made to products cleared through a 510(k) premarket notification submission
or de novo review process may require a new submission, including possibly with clinical data. Before we can offer our device
products to any of the 31 nations within the EU and the European Free Trade Association, we must first satisfy the requirements
for CE Mark clearance, a conformity mark that signifies a product has met all criteria of the relevant EU directives, especially
in the areas of safety and
performance. The process of obtaining regulatory
clearances or approvals to market a medical device can be costly and time-consuming, and we may not be able to obtain these clearances
or approvals on a timely basis, or at all for our proposed products. The initial European CE certificate for CollaGUARD was valid
from October 7, 2011 to July 26, 2015.
The FDA can delay, limit or deny clearance,
approval or authorization of a device for many reasons, including:
|
·
|
our inability
to demonstrate that our products are safe and effective for their intended uses;
|
|
·
|
the data from
our clinical trials may not be sufficient to support clearance or approval; and
|
|
·
|
the manufacturing
process or facilities we use may not meet applicable requirements.
|
In addition, the FDA and other regulatory
authorities may change their respective clearance and approval policies, adopt additional regulations or revise existing regulations,
or take other actions which may prevent or delay approval or clearance of our products under development or impact our ability
to modify our currently cleared or approved products on a timely basis.
Any delay in, or failure to receive or
maintain, clearance, approval or authorization for our products under development could prevent us from generating revenue from
these products or achieving profitability. Additionally, the FDA and comparable foreign regulatory authorities have broad enforcement
powers. Regulatory enforcement or inquiries, or other increased scrutiny of us, could dissuade some customers from using our products
and adversely affect our reputation and the perceived safety and efficacy of our products.
Failure to comply with applicable regulations
could jeopardize our ability to sell our products and result in enforcement actions such as fines, civil penalties, injunctions,
warning letters, recalls of products, delays in the introduction of products into the market, refusal of the FDA or other regulators
to grant future clearances or approvals, and the suspension or withdrawal of existing approvals by the FDA or other regulators.
Any of these sanctions could result in higher than anticipated costs or lower than anticipated sales and have a material adverse
effect on our reputation, business, financial condition and operating results.
Furthermore, we may evaluate international
expansion opportunities in the future for our medical device products. As we expand our operations outside of the United States
and Europe, we are, and will become, subject to various additional regulatory and legal requirements under the applicable laws
and regulations of the international markets we enter. These additional regulatory requirements may involve significant costs
and expenditures and, if we are not able comply with any such requirements, our international expansion and business could be
significantly harmed.
Modifications to our medical device products, such
as CollaGUARD in Europe, may require reclassifications, new CE marking processes or may require us to cease marketing or recall
the modified products until new CE marking is obtained.
The initial European CE certificate for
CollaGUARD was valid from October 7, 2011 to July 26, 2015. In accordance with normal practice for device recertification, we
compiled an updated Design Dossier and submitted this to our European Notified Body (TÜV SÜD, Munich, Germany) in December
2014. As part of our application for recertification, we included an updated literature-based Clinical Evaluation Report and a
Post Market Clinical Follow-up (PMCF) Plan, which rationalized the objectives of our ongoing clinical investigations in accordance
with the current 2012 European Guideline for PMCF studies. However, prior to the expiration of the original certificate, the Notified
Body requested that we revise our PMCF plan to additionally include a direct clinical comparison of CollaGUARD’s performance
and safety compared to another CE-certified adhesion barrier. We do not believe that current European medical device regulations
specifically require that our PMCF plan includes such a clinical comparison. In March 2016, we met with the Notified Body to seek
clarification. At the meeting, TÜV SÜD agreed that current European medical device regulations do not specifically require
that our PMCF plan includes such a clinical comparison, and agreed with our proposal for an updated PMCF based on the pilot clinical
study in open myomectomy patients, as was agreed with FDA at the pre-IDE meeting. Provided TÜV SÜD determines that the
clinical data from the U.S. pilot study are supportive, then recertification would be possible at that time based on an updated
Technical Dossier and Clinical
Evaluation. Until a new CE-certificate has
been issued, we will not supply CollaGUARD to our marketing partners for sale in Europe or other affected territories. Accordingly,
no such sales have been assumed in our financial forecasts.
We are highly dependent on our key personnel, and
if we are not successful in attracting and retaining highly qualified personnel, we may be unable to successfully implement our
business strategy.
Our ability to compete in the highly competitive
pharmaceuticals industry depends upon our ability to attract and retain highly qualified managerial, scientific and medical personnel.
We are highly dependent on our management, scientific, medical and operations personnel. The loss of the services of any of our
executive officers or other key employees and our inability to find suitable replacements could potentially harm our business,
prospects, financial condition or results of operations.
Despite our efforts to retain valuable
employees, members of our management, scientific and development teams may terminate their employment with us on short notice
or no notice. Although we have employment agreements with our key employees, these employment agreements provide for at-will employment,
which means that any of our employees could leave our employment at any time, with or without notice. We do not maintain “key
man” insurance policies on the lives of these individuals or the lives of any of our other employees. Our success also depends
on our ability to continue to attract, retain and motivate highly skilled junior, mid-level and senior managers as well as junior,
mid-level and senior scientific and medical personnel.
Many of the other biotechnology and pharmaceutical
companies that we compete against for qualified personnel have greater financial and other resources, different risk profiles
and a longer history in the industry than we do. They may also provide more diverse opportunities and better chances for career
advancement. Some of these characteristics may be more appealing to high quality candidates than what we can offer. If we are
unable to continue to attract and retain high quality personnel, our ability to advance the development of our product candidates,
obtain regulatory approval and commercialize our product candidates will be limited.
Our employees may engage in misconduct or other
improper activities, including noncompliance with regulatory standards and requirements.
We are exposed to the risk of employee
fraud or other misconduct. Misconduct by employees could include intentional failures to: (i) comply with FDA regulations, (ii)
provide accurate information to the FDA, (iii) comply with manufacturing standards we have established, (iv) comply with federal
and state healthcare fraud and abuse laws and regulations, (v) report financial information or data accurately or (vi) disclose
unauthorized activities to us. In particular, sales, marketing and business arrangements in the healthcare industry are subject
to extensive laws and regulations intended to prevent fraud, kickbacks, self-dealing and other abusive practices in the United
States and in jurisdictions outside of the United States where we conduct our business. These laws and regulations may restrict
or prohibit a wide range of pricing, discounting, marketing and promotion, sales commission, customer incentive programs and other
business arrangements. Employee misconduct could also involve the improper use of information obtained in the course of clinical
trials, which could result in regulatory sanctions and serious harm to our reputation. We have adopted a code of business conduct
and ethics and are training our employees to abide by it, but it is not always possible to identify and deter employee misconduct,
and the precautions we take to detect and prevent this activity may not be effective in controlling unknown or unmanaged risks
or losses or in protecting us from governmental investigations or other actions or lawsuits stemming from a failure to be in compliance
with such laws or regulations. If any such actions are instituted against us, and we are not successful in defending ourselves
or asserting our rights, those actions could have a significant impact on our business, including the imposition of significant
fines or other sanctions.
We will need to grow the size of our organization
and we may experience difficulties in managing this growth.
As of March 13, 2017, we, together
with our subsidiaries, had approximately 120 total employees, 105 of whom are full-time. As our development and
commercialization plans and strategies develop, and as we continue operating as a public company, we expect to need additional
managerial, operational, sales, marketing, financial and other personnel. Future growth would impose significant added responsibilities
on members of management, including:
|
·
|
identifying,
recruiting, integrating, maintaining and motivating additional employees;
|
|
·
|
managing our
internal development efforts effectively, including the clinical and FDA review process
for our product candidates, while complying with our contractual obligations to contractors
and other third parties; and
|
|
·
|
improving our
operational, financial and management controls, reporting systems and procedures.
|
Our future financial performance and our
ability to commercialize our product candidates will depend, in part, on our ability to effectively manage any future growth,
and our management may also have to divert a disproportionate amount of its attention away from day-to-day activities in order
to devote a substantial amount of time to managing these growth activities. To date, we have used the services of outside vendors
to perform tasks including clinical trial management, statistics and analysis and regulatory affairs. Our growth strategy may
also entail expanding our group of contractors or consultants to implement these tasks going forward. Because we rely on numerous
consultants, effectively outsourcing many key functions of our business, we will need to be able to effectively manage these consultants
to ensure that they successfully carry out their contractual obligations and meet expected deadlines. However, if we are unable
to effectively manage our outsourced activities or if the quality or accuracy of the services provided by consultants is compromised
for any reason, our clinical trials may be extended, delayed or terminated, and we may not be able to obtain regulatory approval
for our product candidates or otherwise advance our business. There can be no assurance that we will be able to manage our existing
consultants or find other competent outside contractors and consultants on economically reasonable terms, or at all. If we are
not able to effectively expand our organization by hiring new employees and expanding our groups of consultants and contractors,
we may not be able to successfully implement the tasks necessary to further develop and commercialize our product candidates that
we develop and, accordingly, may not achieve our research, development and commercialization goals. Our ability to expand our
organization will be severely limited by our financial condition and we will be required to identify additional capital to engage
in significant expansion.
Certain of our employees and patents are subject
to foreign laws.
A majority of our employees work in Germany
and are subject to German employment law. Ideas, developments, discoveries and inventions made by such employees and consultants
are subject to the provisions of the German Act on Employees’ Inventions (Gesetz über Arbeitnehmererfindungen), which
regulates the ownership of, and compensation for, inventions made by employees. We face the risk that disputes can occur between
us and our employees or ex-employees pertaining to alleged non-adherence to the provisions of this act that may be costly to defend
and take up our management’s time and efforts whether we prevail or fail in such dispute. In addition, under the German
Act on Employees’ Inventions, certain employees retained rights to patents they invented or co-invented prior to 2009. Although
most of these employees have subsequently assigned their interest in these patents to us, to the extent permitted by law, there
is a risk that the compensation we provided to them may be deemed to be insufficient and we may be required under German law to
increase the compensation due to such employees for the use of the patents. In those cases where employees have not assigned their
interests to us, we may need to pay compensation for the use of those patents. If we are required to pay additional compensation
or face other disputes under the German Act on Employees’ Inventions, our results of operations could be adversely affected.
We believe that our success depends, in
part, upon our ability to protect our intellectual property throughout the world. However, the laws of some foreign countries,
including Germany and Ireland, may not be as comprehensive as those of the United States and may not be sufficient to protect
our proprietary rights abroad. In addition, we generally do not pursue patent protection outside the United States and certain
other key jurisdictions because of cost and confidentiality concerns. Accordingly, our international competitors could obtain
foreign patent protection for, and market overseas, products and technologies for which we are seeking patent protection in the
United States.
A variety of risks associated with marketing our
product candidates internationally could materially adversely affect our business.
We, or our licensing partners, plan to
seek regulatory approval for our product candidates outside of the United States and, accordingly, we expect that we will be subject
to additional risks related to operating in foreign countries if we obtain the necessary approvals, including:
|
·
|
differing regulatory
requirements in foreign countries;
|
|
·
|
faced with
high or higher local prices, opts to import goods from a foreign market (with low or
lower prices) rather than buying them locally;
|
|
·
|
unexpected
changes in tariffs, trade barriers, price and exchange controls and other regulatory
requirements;
|
|
·
|
economic weakness,
including inflation, or political instability in particular foreign economies and markets;
|
|
·
|
compliance
with tax, employment, immigration and labor laws for employees living or traveling abroad;
|
|
·
|
foreign taxes,
including withholding of payroll taxes;
|
|
·
|
foreign currency
fluctuations, which could result in increased operating expenses and reduced revenues,
and other obligations incident to doing business in another country;
|
|
·
|
difficulties
staffing and managing foreign operations;
|
|
·
|
workforce uncertainty
in countries where labor unrest is more common than in the United States;
|
|
·
|
potential liability
under the Foreign Corrupt Practices Act of 1977 or comparable foreign regulations;
|
|
·
|
challenges
enforcing our contractual and intellectual property rights, especially in those foreign
countries that do not respect and protect intellectual property rights to the same extent
as the United States;
|
|
·
|
production
shortages resulting from any events affecting raw material supply or manufacturing capabilities
abroad; and
|
|
·
|
business interruptions
resulting from geo-political actions, including war and terrorism.
|
These and other risks associated with our,
or our licensing partners’ international operations may materially adversely affect our ability to attain or maintain profitable
operations.
Coverage and reimbursement may be limited or unavailable
in certain market segments for our product candidates, which could make it difficult for us to sell our product candidates profitably.
Government authorities and third-party
payors, such as private health insurers and health maintenance organizations, or, in some jurisdictions, statutory health insurances,
decide which products they will cover and the amount of reimbursement. Reimbursement by a third-party payor may depend upon a
number of factors, including the third-party payor’s determination that use of a product is:
|
·
|
a covered benefit
under its health plan;
|
|
·
|
safe, effective
and medically necessary;
|
|
·
|
appropriate
for the specific patient;
|
|
·
|
neither experimental
nor investigational.
|
Obtaining coverage and reimbursement approval
for a product from a government or other third-party payor is a time-consuming and costly process that could require us to provide
to the payor supporting scientific, clinical and cost-effectiveness data for the use of our products. We may not be able to provide
data sufficient to gain acceptance with respect to coverage and reimbursement. If reimbursement of our future products is unavailable
or limited in scope or amount, or if pricing is set at unsatisfactory levels, we may be unable to achieve or sustain profitability.
We are approved to market certain of our
products in selected foreign jurisdictions and further intend to seek approval to market our product candidates in both the United
States and in selected foreign jurisdictions. If we obtain approval in one or more foreign jurisdictions for our product candidates,
we will be subject to rules and regulations in those jurisdictions. In some foreign countries, particularly those in the European
Union, the pricing of prescription pharmaceuticals is subject to governmental control. In these countries, pricing negotiations
with governmental authorities can take considerable time after obtaining marketing approval for a product candidate. In addition,
market acceptance and sales of our product candidates will depend significantly on the availability of adequate coverage and reimbursement
from third-party payors for our product candidates and may be affected by existing and future health care reform measures.
In both the United States and certain foreign
jurisdictions, there have been a number of legislative and regulatory changes to the health care system that could impact our
ability to sell our products profitably. In particular, the Medicare Prescription Drug, Improvement, and Modernization Act of
2003 revised the payment methodology for many products under Medicare in the United States, which has resulted in lower rates
of reimbursement. In 2010, the Patient Protection and Affordable Care Act, as amended by the Health Care and Education Reconciliation
Act of 2010, or collectively, the Affordable Care Act, was enacted. This expansion in the government’s role in the U.S.
healthcare industry may further lower rates of reimbursement for pharmaceutical products.
Other legislative changes have been proposed
and adopted in the United States since the Affordable Care Act was enacted. On August 2, 2011, the Budget Control Act of 2011,
among other things, created measures for spending reductions by Congress. A Joint Select Committee on Deficit Reduction, tasked
with recommending a targeted deficit reduction of at least $1.2 trillion for the years 2012 through 2021, was unable to reach
required goals, thereby triggering the legislation’s automatic reduction to several government programs. This includes aggregate
reductions of Medicare payments to providers up to 2% per fiscal year. On January 2, 2013, President Obama signed into law the
American Taxpayer Relief Act of 2012, or the ATRA, which delayed for another two months the budget cuts mandated by these sequestration
provisions of the Budget Control Act of 2011. On March 1, 2013, the President signed an executive order implementing sequestration,
and on April 1, 2013, the 2% Medicare payment reductions went into effect. The ATRA also, among other things, reduced Medicare
payments to several providers, including hospitals, imaging centers and cancer treatment centers, and increased the statute of
limitations period for the government to recover overpayments to providers from three to five years. In January 2017, Congress
voted to adopt a budget resolution for fiscal year 2017, or the Budget Resolution, that authorizes the implementation of legislation
that would repeal portions of the Affordable Care Act. The Budget Resolution is not a law, but it is widely viewed as the first
step toward the passage of legislation that would repeal certain aspects of the Affordable Care Act. Further, on January 20, 2017,
President Trump signed an Executive Order directing federal agencies with authorities and responsibilities under the Affordable
Care Act to waive, defer, grant exemptions from, or delay the implementation of any provision of the Affordable Care Act that
would impose a fiscal or regulatory burden on states, individuals, healthcare providers, health insurers, or manufacturers of
pharmaceuticals or medical devices. Congress also could consider subsequent legislation to replace elements of the Affordable
Care Act that are repealed. We will continue to evaluate the effect that the Affordable Care Act and any future measures to repeal
or replace the Affordable Care Act have on our business.
In Europe, the European Commission has
submitted a Proposal for a Regulation of the European Parliament and the Council on medical devices, amending Directive 2001/83/EC,
Regulation (EC) No 178/2002 and Regulation (EC) No 1223/2009, to replace, inter alia, Directive 93/42/EEC and to amend regulations
regarding medical devices in the European Union, which could result in changes in the regulatory requirements for medical devices
in Europe.
There have been, and likely will continue
to be, legislative and regulatory proposals at the federal and state levels directed at broadening the availability of healthcare
and containing or lowering the cost of healthcare. We cannot predict the initiatives that may be adopted in the future. The continuing
efforts of governments, insurance companies, managed care organizations and other payors of healthcare services to contain or
reduce costs of healthcare and/or impose price controls may adversely affect:
|
·
|
the demand
for our product candidates, if we obtain regulatory approvals;
|
|
·
|
our ability
to set a price that we believe is fair for our products;
|
|
·
|
our ability
to generate revenues and achieve or maintain profitability; and
|
|
·
|
the level of
taxes that we are required to pay.
|
Any reduction in reimbursement from Medicare
or other government programs may result in a similar reduction in payments from private payors, which may adversely affect our
future profitability.
The impact of recent health care reform
efforts with respect to the Affordable Care Act is currently unknown, and may adversely affect our business model.
Since its enactment, there have been judicial
and Congressional challenges to numerous provisions of the Affordable Care Act. In January 2017, Congress voted to adopt a budget
resolution for fiscal year 2017, or the Budget Resolution, that authorizes the implementation of legislation that would repeal
portions of the Affordable Care Act. The Budget Resolution is not a law, but it is widely viewed as the first step toward the
passage of legislation that would repeal certain aspects of the Affordable Care Act. Further, on January 20, 2017, President Trump
signed an Executive Order directing federal agencies with authorities and responsibilities under the Affordable Care Act to waive,
defer, grant exemptions from, or delay the implementation of any provision of the Affordable Care Act that would impose a fiscal
or regulatory burden on states, individuals, healthcare providers, health insurers, or manufacturers of pharmaceuticals or medical
devices. Congress also could consider subsequent legislation to replace elements of the Affordable Care Act that are repealed.
We will continue to evaluate the effect that the Affordable Care Act and any future measures to repeal or replace the Affordable
Care Act have on our business.
Our business and operations would suffer in the
event of system failures.
Despite the implementation of security
measures, our internal computer systems and those of our current and future clinical research organizations, or CROs and other
contractors and consultants are vulnerable to damage from computer viruses, unauthorized access, natural disasters, terrorism,
war and telecommunication and electrical failures. While we have not experienced any such material system failure, accident or
security breach to date, if such an event were to occur and cause interruptions in our operations, it could result in a material
disruption of our development programs and our business operations. For example, the loss of clinical trial data from completed
or future clinical trials could result in delays in our regulatory approval efforts and significantly increase our costs to recover
or reproduce the data. To the extent that any disruption or security breach were to result in a loss of, or damage to, our data
or applications, or inappropriate disclosure of confidential or proprietary information, we could incur liability and the further
development and commercialization of our product candidates could be delayed.
If product liability lawsuits are brought against
us, we may incur substantial liabilities and may be required to limit commercialization of our product candidates.
We face an inherent risk of product liability
as a result of the clinical testing of our product candidates and will face an even greater risk if we commercialize our product
candidates or our already commercialized products on a larger scale. For example, we may be sued if our product candidates allegedly
cause injury or are found to be otherwise unsuitable during clinical testing, manufacturing, marketing or sale. Any such product
liability claims may include allegations of defects in manufacturing; defects in design; a failure to warn of dangers inherent
in the product, negligence, strict liability; and a breach of warranties. Claims could also be asserted under state consumer protection
acts. In Europe, medical products and medical devices may, under certain circumstances, be subject to no-fault liability. If we
cannot successfully defend ourselves against product liability claims, we may incur substantial liabilities or be required to
limit commercialization of our product candidates. Even a successful defense would require significant financial and management
resources. Regardless of the merits or eventual outcome, liability claims may result in:
|
·
|
costs to defend
litigation and other proceedings;
|
|
·
|
a diversion
of management’s time and our resources;
|
|
·
|
decreased demand
for our product candidates;
|
|
·
|
injury to our
reputation;
|
|
·
|
withdrawal
of clinical trial participants;
|
|
·
|
initiation
of investigations by regulators;
|
|
·
|
product recalls,
withdrawals or labeling, marketing or promotional restrictions;
|
|
·
|
substantial
monetary awards to trial participants or patients;
|
|
·
|
exhaustion
of any available insurance and our capital resources;
|
|
·
|
the inability
to commercialize our product candidates; and
|
|
·
|
a decline in
our share price.
|
Our inability to obtain and retain sufficient
product liability insurance at an acceptable cost to protect against potential product liability claims could prevent or inhibit
the commercialization of products we develop. We currently do not carry product liability insurance covering our clinical trials.
If we determine that it is necessary to procure product liability coverage due to the commercial launch of our lead product candidates
after approval, we may be unable to obtain such coverage on acceptable terms, or at all. Until we obtain product liability insurance,
we will have to pay any amounts awarded by a court or negotiated in a settlement, and we may not have, or be able to obtain, sufficient
capital to pay such amounts.
Our business could be adversely affected by animal
rights activists.
Our business activities have involved animal
testing, including preclinical testing for XaraColl and CollaGUARD. Animal testing has been the subject of controversy and adverse
publicity. Some organizations and individuals have attempted to stop animal testing by pressing for legislation and regulation
in these areas. To the extent that the activities of such groups are successful, our business could be adversely affected.
Our international operations pose currency risks,
which may adversely affect our operating results and net income.
Our operating results may be affected by
volatility in currency exchange rates and our ability to effectively manage our currency transaction risks. In general, we conduct
our business, earn revenues and incur costs in the local currency of the countries in which we operate. In 2016, 99% of our revenues
were generated and approximately 24% of our costs were incurred in euros. As we execute our strategy to expand internationally,
our exposure to currency risks will increase. We do not manage our foreign currency exposure in a manner that would eliminate
the effects of changes in foreign exchange rates. Therefore, changes in exchange rates between these foreign currencies and the
euro will affect our revenues, cost of goods sold, and operating margins, and could result in exchange losses in any given reporting
period.
We incur currency transaction risks whenever
we enter into either a purchase or a sale transaction using a different currency from the currency in which we report revenues.
In such cases we may suffer an exchange loss because we do not currently engage in currency swaps or other currency hedging strategies
to address this risk.
Given the volatility of exchange rates,
we can give no assurance that we will be able to effectively manage our currency transaction risks or that any volatility in currency
exchange rates will not have an adverse effect on our results of operations.
Failure to comply with the U.S. Foreign Corrupt
Practices Act or other applicable anti-corruption legislation could result in fines, criminal penalties and an adverse effect
on our business.
We operate in a number of countries throughout
the world, including countries known to have a reputation for corruption. We are committed to doing business in accordance with
applicable anti-corruption laws. We are subject, however, to the risk that our officers, directors, employees, agents and collaborators
may take action determined to be in
violation of such anti-corruption laws, including
the U.S. Foreign Corrupt Practices Act of 1977, the U.K. Bribery Act 2010 and the European Union Anti-Corruption Act, as well
as trade sanctions administered by the Office of Foreign Assets Control and the U.S. Department of Commerce. Any such violation
could result in substantial fines, sanctions, civil and/or criminal penalties or curtailment of operations in certain jurisdictions,
and might adversely affect our results of operations. In addition, actual or alleged violations could damage our reputation and
ability to do business.
Global economic, political and social conditions
have adversely impacted our sales and may continue to do so.
The uncertain direction and relative strength
of the global economy, difficulties in the financial services sector and credit markets, continuing geopolitical uncertainties
and other macroeconomic factors all affect spending behavior of potential end-users of our products. The prospects for economic
growth in Europe, the United States and other countries remain uncertain and may cause end-users to further delay or reduce technology
purchases. In particular, a substantial portion of our sales are made to customers in countries in Europe, which is experiencing
a significant economic crisis. If global economic conditions remain volatile for a prolonged period or if European economies experience
further disruptions, our results of operations could be adversely affected. The global financial crisis affecting the banking
system and financial markets has resulted in a tightening of credit markets, lower levels of liquidity in many financial markets
and extreme volatility in fixed income, credit, currency and equity markets. These conditions may make it more difficult for our
end-users to obtain financing.
Risks Related to Our Dependence on Third Parties
We rely on third parties to conduct our clinical
trials. If these third parties do not successfully carry out their contractual duties or meet expected deadlines, we may not be
able to obtain regulatory approval for or commercialize our product candidates and our business could be substantially harmed.
We have engaged third-party CROs in connection
with our Phase 3 clinical trials for our product candidates and will continue to engage such CROs in the future. We rely heavily
on these parties for execution of our clinical trials, and we control only certain aspects of their activities. Nevertheless,
we are responsible for ensuring that each of our studies is conducted in accordance with applicable protocol, legal, regulatory
and scientific standards, and our reliance on our CROs does not relieve us of our regulatory responsibilities. We and our CROs
are required to comply with current Good Clinical Practices, or cGCP requirements, which are a collection of regulations enforced
by the FDA or comparable foreign regulatory authorities for product candidates in clinical development in order to protect the
health, safety and welfare of patients and assume the integrity of clinical data. cGCP are also intended to protect the health,
safety and welfare of study subjects through requirements such as informed consent. Regulatory authorities enforce these cGCPs
through periodic inspections of trial sponsors, principal investigators and trial sites. If we or any of these CROs fail to comply
with applicable cGCP regulations, the clinical data generated in our clinical trials may be deemed unreliable and the FDA or comparable
foreign regulatory authorities may require us to perform additional clinical trials before approving our marketing applications.
We cannot assure you that, upon inspection, such regulatory authorities will determine that any of our clinical trials comply
with the cGCP regulations. In addition, for drugs, our clinical trials must be conducted with products produced under cGMP regulations
and will require a large number of test subjects. For our devices, clinical trials must use product manufactured in compliance
with design controls under the QSR. Our failure or any failure by our CROs to comply with these regulations or to recruit a sufficient
number of patients may require us to repeat clinical trials, which would delay the regulatory approval process. Moreover, we may
be implicated if any of our CROs violate federal or state fraud and abuse or false claims laws and regulations, or healthcare
privacy and security laws.
The CROs are not employed directly by us
and, except for remedies available to us under our agreements with such CROs, we cannot control whether they devote sufficient
time and resources to our ongoing preclinical, clinical and nonclinical programs. These CROs may also have relationships with
other commercial entities, including our competitors, for whom they may also be conducting clinical studies or other product development
activities, which could affect their performance on our behalf. If CROs do not successfully carry out their contractual duties
or obligations or meet expected deadlines, if they need to be replaced or if the quality or accuracy of the clinical data they
obtain is compromised due to the failure to adhere to our clinical protocols or regulatory requirements or for other reasons,
our clinical trials may be extended, delayed or terminated and we may not be able to complete development of, obtain regulatory
approval for or successfully commercialize our product candidates. As a result, our financial results
and the commercial prospects for our product
candidates would be harmed, our costs could increase and our ability to generate revenues could be delayed.
Switching or adding CROs involves substantial
cost and requires extensive management time and focus. In addition, there is a natural transition period when a new CRO commences
work. As a result, delays may occur, which can materially impact our ability to meet our desired clinical development timelines.
Although we plan to carefully manage our relationships with our CROs, there can be no assurance that we will not encounter challenges
or delays in the future or that these delays or challenges will not have a material adverse impact on our business, prospects,
financial condition and results of operations.
We rely on third parties for the supply of specified
raw materials and equipment.
We rely on third parties for the timely
supply of specified raw materials and equipment for the manufacture of our collagen-based products. Although we actively manage
these third-party relationships to provide continuity and quality, some events which are beyond our control could result in the
complete or partial failure of these goods and services. Any such failure could have a material adverse effect on our financial
condition and operations.
If we are unable to establish effective marketing
and sales capabilities or enter into agreements with third parties to market and sell our products, we may be unable to generate
revenues from this product candidate.
In order to commercialize our products,
we must build our marketing, sales and distribution capabilities. The establishment, development and training of our sales force
and related compliance plans to market our products is expensive and time consuming and can potentially delay the commercial launch
of our products. In the event we are not successful in developing our marketing and sales infrastructure, we may not be able to
successfully commercialize our products, which would limit our ability to generate product revenues.
We currently license the commercialization rights
for some of our marketed products outside of the United States, which exposes us to additional risks of conducting business in
international markets.
The non-U.S. markets are an important component
of existing commercialization strategy for our existing marketed products as well as part of our growth strategy for Xaracoll
and CollaGUARD. We have entered into commercial supply agreements for our main commercialized products pursuant to which we exclusively
supply and our partners exclusively purchase the products from us in their respective territories outside of the United States
or worldwide. For CollaGUARD, we have entered into supply agreements with partners, the most significant of which are with Takeda
Pharmaceutical Company Limited, or Takeda, for 15 countries including Canada, Mexico and countries in the Commonwealth of Independent
States, or CIS, where distribution of the product is subject to obtaining local marketing approvals, and Pioneer Pharma Co. Ltd.,
or Pioneer, for nine Asian countries, including China and its territories. For CollatampG, we have entered into an exclusive supply
agreement with EUSA Pharma for all territories outside of the United States and for Septocoll, we have entered into an agreement
with Biomet Orthopedics for global supply of the product. We are also manufacturing RegenePro, a bioresorbable collagen sponge
for dental applications, which we supply to Biomet 3i. Our agreements require us to timely supply products that meet the agreed
quality standards and require our customers to purchase products from us, in some cases in specified minimum quantities. If we
fail to maintain these agreements and agreements with other partners or to enter into new distribution arrangements with selling
parties, or if these parties are not successful, our revenue-generating growth potential will be adversely affected. Moreover,
international business relationships subject us to additional risks that may materially adversely affect our ability to attain
or sustain profitable operations, including:
|
·
|
efforts to
enter into distribution or licensing arrangements with third parties in connection with
our international sales, marketing and distribution efforts may increase our expenses
or divert our management’s attention from the development of product candidates;
|
|
·
|
changes in
a specific country’s or region’s political and cultural climate or economic
condition;
|
|
·
|
differing requirements
for regulatory approvals and marketing internationally;
|
|
·
|
difficulty
of effective enforcement of contractual provisions in local jurisdictions;
|
|
·
|
potentially
reduced protection for intellectual property rights;
|
|
·
|
potential third-party
patent rights in countries outside of the United States;
|
|
·
|
unexpected
changes in tariffs, trade barriers and regulatory requirements;
|
|
·
|
economic weakness,
including inflation, or political instability, particularly in non-U.S. economies and
markets, including several countries in Europe;
|
|
·
|
compliance
with tax, employment, immigration and labor laws for employees traveling abroad;
|
|
·
|
the effects
of applicable foreign tax structures and potentially adverse tax consequences;
|
|
·
|
foreign currency
fluctuations, which could result in increased operating expenses and reduced revenue
and other obligations incidental to doing business in another country;
|
|
·
|
workforce uncertainty
in countries where labor unrest is more common than in the United States;
|
|
·
|
the potential
for so-called parallel importing, which is what happens when a local seller, faced with
high or higher local prices, opts to import goods from a foreign market (with low or
lower prices) rather than buying them locally;
|
|
·
|
failure of
our employees and contracted third parties to comply with Office of Foreign Asset Control
rules and regulations and the Foreign Corrupt Practices Act;
|
|
·
|
production
shortages resulting from any events affecting raw material supply or manufacturing capabilities
abroad; and
|
|
·
|
business interruptions
resulting from geo-political actions, including war and terrorism, or natural disasters,
including earthquakes, volcanoes, typhoons, floods, hurricanes and fires.
|
These and other risks may materially adversely
affect our ability to attain or sustain revenue from international markets.
We may form or seek strategic alliances in the
future and we may not realize the benefits of such alliances.
We may form or seek strategic alliances,
create joint ventures or collaborations or enter into licensing arrangements with third parties that we believe will complement
or augment our development and commercialization efforts with respect to our product candidates and any future products that we
may develop. Any of these relationships may require us to incur non-recurring and other charges, increase our near- and long-term
expenditures, issue securities that dilute our existing shareholders or disrupt our management and business. In addition, we face
significant competition in seeking appropriate strategic partners and the negotiation process is time-consuming and complex. Moreover,
we may not be successful in our efforts to establish a strategic partnership or other alternative arrangements for our product
candidates because they may be deemed to be at too early of a stage of development for collaborative effort and third parties
may not view our product candidates as having the requisite potential to demonstrate safety and efficacy. If we license products
or businesses, we may not be able to realize the benefit of such transactions if we are unable to successfully integrate them
with our existing operations and company culture and vice versa. We cannot be certain that, following a strategic transaction
or license, we will achieve the revenues or specific net income that justifies such transaction. Any delays in entering into new
strategic partnership agreements related to our product candidates could delay the development and commercialization of our product
candidates in certain geographies for certain indications, which would harm our business prospects, financial condition and results
of operations.
Risks Related to Our Intellectual Property
If our efforts to protect the proprietary nature
of the intellectual property related to our technologies are not adequate, we may not be able to compete effectively in our market.
We rely upon a combination of patents,
trade secret protection and confidentiality agreements to protect the intellectual property related to our technologies. Any disclosure
to or misappropriation by third parties of our confidential proprietary information could enable competitors to quickly duplicate
or surpass our technological achievements, thus eroding our competitive position in our market.
In addition, the patent applications that
we own or that we may license may fail to result in issued patents in the United States or in other foreign countries. Even if
the patents do successfully issue, third parties may challenge the validity, enforceability or scope thereof, which may result
in such patents being narrowed, invalidated or held unenforceable. Furthermore, even if they are unchallenged, our patents and
patent applications may not adequately protect our intellectual property or prevent others from designing around our claims. If
the breadth or strength of protection provided by the issued patents and patent applications we hold with respect to our product
candidates is threatened, it could dissuade companies from collaborating with us to develop, and threaten our ability to commercialize,
our product candidates. Further, if we encounter delays in our clinical trials, the period of time during which we could market
our product candidates under patent protection would be reduced. Since patent applications in the United States and most other
countries are confidential for a period of time after filing, we cannot be certain that we were the first to file any patent application
related to our product candidates. Furthermore, for applications in which all claims are entitled to a priority date before March
16, 2013, an interference proceeding can be provoked by a third-party or instituted by the United States Patent and Trademark
Office, or U.S. PTO, to determine who was the first to invent any of the subject matter covered by the patent claims of our applications.
For applications containing a claim not entitled to priority before March 16, 2013, there is greater level of uncertainty in the
patent law with the passage of the America Invents Act (2012) which brings into effect significant changes to the U.S. patent
laws that are yet untried and untested, and which introduces new procedures for challenging pending patent applications and issued
patents. A primary change under this reform is creating a “first to file” system in the U.S. This will require us
to be cognizant going forward of the time from invention to filing of a patent application.
In addition to the protection afforded
by patents, we seek to rely on trade secret protection and confidentiality agreements to protect proprietary know-how that is
not patentable, processes for which patents are difficult to enforce and any other elements of our product discovery and development
processes that involve proprietary know-how, information or technology that is not covered by patents. Although we require all
of our employees to assign their inventions to us to the extent permitted by law, and require all of our employees, consultants,
advisors and any third parties who have access to our proprietary know-how, information or technology to enter into confidentiality
agreements, we cannot be certain that our trade secrets and other confidential proprietary information will not be disclosed or
that competitors will not otherwise gain access to our trade secrets or independently develop substantially equivalent information
and techniques. Furthermore, the laws of some foreign countries do not protect proprietary rights to the same extent or in the
same manner as the laws of the United States. As a result, we may encounter significant problems in protecting and defending our
intellectual property both in the United States and abroad. If we are unable to prevent unauthorized material disclosure of our
intellectual property to third parties, we will not be able to establish or maintain a competitive advantage in our market, which
could materially adversely affect our business, operating results and financial condition.
Because we have filed a petition for reissuance
of our U.S. XaraColl patent, we will be unable to enforce it unless and until the U.S. patent is reissued.
We recently submitted a petition to reissue
the U.S. patent directed to XaraColl, mainly for the purposes of submitting prior art references identified in the corresponding
European application. We did not submit these prior art references to the U.S. Patent and Trademark Office during the prosecution
of the U.S. patent. In addition, this reissue process will allow us to pursue additional claims, e.g., claims within the scope
of the originally issued claims but more tailored to our currently proposed XaraColl product. Although we do not believe these
prior art references should have any substantial impact on the originally issued claims, especially with respect to the coverage
of the proposed XaraColl products, there can be no assurance that any or all of the originally issued claims will be reissued.
It is also uncertain whether any or all of the additional claims we have included in the petition will be granted. We anticipate
the
conclusion of the reissue process before
we launch XaraColl in the United States, and if the reissued claims are substantially the same as the originally issued claims,
there will be no intervening rights by others during the reissue period. We will be unable to enforce the XaraColl U.S. patent
unless and until the U.S. patent is reissued.
There can be no assurance that a patent
will reissue from the petition, or that any such patent will be enforceable and will not be challenged, invalidated or circumvented.
Nevertheless, we will continue to rely upon our proprietary know-how, techniques, expertise and the decades of collective experience
of our team relating to the development and manufacturing of collagen matrix products, as well as the rigorous regulatory barriers
applicable to the development, manufacture, distribution and marketing of potential competing products. See “Item 1. Business
— Intellectual Property and Exclusivity” for further information.
Third-party claims of intellectual property infringement
may prevent or delay our product discovery and development efforts.
Our commercial success depends in part
on our avoiding infringement of the patents and proprietary rights of third parties. There is a substantial amount of litigation
involving patents and other intellectual property rights in the biotechnology and pharmaceutical industries, as well as administrative
proceedings for challenging patents, including interference and reexamination proceedings before the U.S. PTO or oppositions and
other comparable proceedings in foreign jurisdictions. Recently, following U.S. patent reform, new procedures including inter
partes review and post grant review have been implemented. As stated above, this reform is untried and untested and will bring
uncertainty to the possibility of challenge to our patents in the future. Numerous U.S. and foreign issued patents and pending
patent applications, which are owned by third parties, exist in the fields in which we are developing our product candidates.
As the biotechnology and pharmaceutical industries expand and more patents are issued, the risk increases that our product candidates
may give rise to claims of infringement of the patent rights of others.
Third parties may assert that we are employing
their proprietary technology without authorization. There may be third-party patents of which we are currently unaware with claims
to materials, formulations, methods of manufacture or methods for treatment related to the use or manufacture of our product candidates.
Because patent applications can take many years to issue, there may be currently pending patent applications which may later result
in issued patents that our product candidates may infringe. In addition, third parties may obtain patents in the future and claim
that use of our technologies infringes upon these patents. If any third-party patent is held by a court of competent jurisdiction
to cover the manufacturing process of our product candidates, any molecules formed during the manufacturing process or any final
product itself, the holders of any such patents may be able to block our ability to commercialize the product candidate unless
we obtained a license under the applicable patents, or until such patents expire or they are finally determined to be held invalid
or unenforceable. Similarly, if any third-party patent is held by a court of competent jurisdiction to cover aspects of our formulations,
processes for manufacture or methods of use product candidates, including combination therapy or patient selection methods, the
holders of any such patent may be able to block our ability to develop and commercialize the product candidate unless we obtained
a license or until such patent expires or is finally determined to be held invalid or unenforceable. In either case, such a license
may not be available on commercially reasonable terms or at all. If we are unable to obtain a necessary license to a third-party
patent on commercially reasonable terms, or at all, our ability to commercialize our product candidates may be impaired or delayed,
which could in turn significantly harm our business.
Parties making claims against us may seek
and obtain injunctive or other equitable relief, which could effectively block our ability to further develop and commercialize
our product candidates. Defense of these claims, regardless of their merit, would involve substantial litigation expense and would
be a substantial diversion of employee resources from our business. In the event of a successful claim of infringement against
us, we may have to pay substantial damages, including treble damages and attorneys’ fees for willful infringement, obtain
one or more licenses from third parties, pay royalties or redesign our infringing products, which may be impossible or require
substantial time and monetary expenditure. We cannot predict whether any such license would be available at all or whether it
would be available on commercially reasonable terms. Furthermore, even in the absence of litigation, we may need to obtain licenses
from third parties to advance our research or allow commercialization of our product candidates. We may fail to obtain any of
these licenses at a reasonable cost or on reasonable terms, if at all. In that event, we would be unable to further develop and
commercialize our product candidates, which could harm our business significantly.
We may be involved in lawsuits to protect or enforce
our patents, which could be expensive, time-consuming and unsuccessful.
Competitors may infringe our patents. To
counter infringement or unauthorized use, we may be required to file infringement claims, which can be expensive and time-consuming.
In addition, in an infringement proceeding, a court may decide that one or more of our patents is not valid or is unenforceable,
or may refuse to stop the other party from using the technology at issue on the grounds that our patents do not cover the technology
in question. An adverse result in any litigation or defense proceedings could put one or more of our patents at risk of being
invalidated, held unenforceable, or interpreted narrowly and could put our patent applications at risk of not issuing. Defense
of these claims, regardless of their merit, would involve substantial litigation expense and would be a substantial diversion
of employee resources from our business. In the event of a successful claim of infringement against us, we may have to pay substantial
damages, including treble damages and attorneys’ fees for willful infringement, obtain one or more licenses from third parties,
pay royalties or redesign our infringing products, which may be impossible or require substantial time and monetary expenditure.
Interference proceedings provoked by third
parties or brought by the U.S. PTO may be necessary to determine the priority of inventions with respect to our patents or patent
applications. An unfavorable outcome could require us to cease using the related technology or to attempt to license rights to
it from the prevailing party. Our business could be harmed if the prevailing party does not offer us a license on commercially
reasonable terms. Litigation or interference proceedings may fail and, even if successful, may result in substantial costs and
distract our management and other employees. We may not be able to prevent misappropriation of our trade secrets or confidential
information, particularly in countries where the laws may not protect those rights as fully as in the United States.
Furthermore, because of the substantial
amount of discovery required in connection with intellectual property litigation, there is a risk that some of our confidential
information could be compromised by disclosure during this type of litigation. In addition, there could be public announcements
of the results of hearings, motions or other interim proceedings or developments. If securities analysts or investors perceive
these results to be negative, it could have a substantial adverse effect on the price of our securities.
Obtaining and maintaining our patent protection
depends on compliance with various procedures, document submission requests, fee payments and other requirements imposed by governmental
patent agencies, and our patent protection could be reduced or eliminated for noncompliance with these requirements.
Periodic maintenance fees on any issued
patent are due to be paid to the U.S. PTO and foreign patent agencies in several stages over the lifetime of the patent. The U.S.
PTO and various foreign governmental patent agencies require compliance with a number of procedural, documentary, fee payment
and other similar provisions during the patent application process. While an inadvertent lapse can in many cases be cured by payment
of a late fee or by other means in accordance with the applicable rules, there are situations in which noncompliance can result
in abandonment or lapse of the patent or patent application, resulting in partial or complete loss of patent rights in the relevant
jurisdiction. Noncompliance events that could result in abandonment or lapse of a patent or patent application include, but are
not limited to, failure to respond to official actions within prescribed time limits, non-payment of fees and failure to properly
legalize and submit formal documents. In such an event, our competitors might be able to enter the market, which would have a
material adverse effect on our business.
We may be subject to claims that our employees,
consultants or independent contractors have wrongfully used or disclosed confidential information of third parties.
We have received confidential and proprietary
information from third parties. In addition, we employ individuals who were previously employed at other biotechnology or pharmaceutical
companies. We may be subject to claims that we or our employees, consultants or independent contractors have inadvertently or
otherwise used or disclosed confidential information of these third parties or our employees’ former employers. Litigation
may be necessary to defend against these claims. Even if we are successful in defending against these claims, litigation could
result in substantial cost and be a distraction to our management and employees.
We may not be able to protect our intellectual
property rights throughout the world.
Filing, prosecuting and defending patents
on all of our product candidates throughout the world would be prohibitively expensive. Competitors may use our technologies in
jurisdictions where we have not obtained patent protection to develop their own products and further, may export otherwise infringing
products to territories where we have patent protection, but where enforcement is not as strong as that in the United States.
These products may compete with our products in jurisdictions where we do not have any issued patents and our patent claims or
other intellectual property rights may not be effective or sufficient to prevent them from so competing.
Many companies have encountered significant
problems in protecting and defending intellectual property rights in foreign jurisdictions. The legal systems of certain countries,
particularly certain developing countries, do not favor the enforcement of patents and other intellectual property protection,
particularly those relating to biopharmaceuticals, which could make it difficult for us to stop the infringement of our patents
or marketing of competing products in violation of our proprietary rights generally. Proceedings to enforce our patent rights
in foreign jurisdictions could result in substantial cost and divert our efforts and attention from other aspects of our business.
Our trade secrets are difficult to protect.
Confidentiality agreements with employees
and others may not adequately prevent disclosure of our trade secrets and other proprietary information and may not adequately
protect our intellectual property.
Our success depends upon the skills, knowledge
and experience of our scientific and technical personnel, our consultants and advisors as well as our partners, licensors and
contractors. Because we operate in a highly competitive technical field of drug development, we rely in part on trade secrets
to protect our proprietary technology and processes. However, trade secrets are difficult to protect. We enter into confidentiality
agreements with our corporate partners, employees, consultants, sponsored researchers and other advisors. These agreements generally
require that the receiving party keep confidential and not disclose to third parties all confidential information developed by
the receiving party or made known to the receiving party by us during the course of the receiving party’s relationship with
us. Our agreements also provide that any inventions made based solely upon our technology are our exclusive property, and we enter
into assignment agreements that are recorded in patent, trademark and copyright offices around the world to perfect our rights.
These confidentiality and assignment agreements
may be breached and may not effectively assign intellectual property rights to us. Our trade secrets also could be independently
discovered by competitors, in which case we would not be able to prevent use of such trade secrets by our competitors. The enforcement
of a claim alleging that a party illegally obtained and was using our trade secrets could be difficult, expensive and time consuming
and the outcome would be unpredictable. In addition, courts outside the United States may be less willing to protect trade secrets.
The failure to obtain or maintain meaningful trade secret protection could adversely affect our competitive position.
Risks Related to Ownership of our Securities
There has been limited trading volume for our securities.
Even though our ordinary shares have been
listed on the NASDAQ Global Market, there has been limited liquidity in the market for our securities, which could make it more
difficult for holders to sell our ordinary shares.
Our failure to meet the continued
listing requirements of the NASDAQ could result in a delisting of our common stock.
Our ordinary shares
are listed on the NASDAQ Global Market, which imposes, among other requirements, a minimum stockholders’ equity
requirement. On February 15, 2017, we received a notice from NASDAQ of non-compliance with its continuing listing rules indicating
that for 30 consecutive business days beginning on December 30, 2016, our ordinary shares had not maintained a minimum closing
bid price of $1.00 (“Minimum Bid Price Requirement”) per share as required by Nasdaq Listing Rule 5450(a)(1).
In accordance with Nasdaq Listing Rule 5810(c)(3)(A), we have been provided a period of 180 calendar days from the date of the
notification, or until August 14, 2017 (the “Compliance Period”), in which to regain compliance with the Minimum Bid
Price Requirement. In order to regain compliance with the Minimum Bid Price Requirement, the closing bid price of our ordinary
shares must be at
least $1.00 per share for a minimum of
ten consecutive business days during the Compliance Period. In the event that we do not regain compliance within the Compliance
Period, we may be eligible to seek an additional 180-calendar day compliance period if we elect to transfer the listing of our
ordinary shares to The Nasdaq Capital Market, meet the continued listing requirement for market value of publicly held shares
and all other initial listing standards for The Nasdaq Capital Market, with the exception of the Minimum Bid Price Requirement,
and provide written notice to Nasdaq of our intent to cure the deficiency during this second compliance period, by effecting a
reverse stock split, if necessary.
The delisting of our
common stock from NASDAQ may make it more difficult for us to raise capital on favorable terms in the future. Such a delisting
would likely have a negative effect on the price of our ordinary shares and would impair your ability to sell or purchase our
ordinary shares when you wish to do so. Further, if we were unable to maintain a NASDAQ listing, our ordinary shares would cease
to be recognized as covered securities and we would be subject to regulation in each state in which we offer our securities.
There can be no assurance that we will
successfully maintain our listing or regain compliance with the Minimum Bid Price Requirement. Moreover, there is no assurance
that any actions that we take to restore our compliance with NASDAQ’s listing requirements would stabilize the market price or
improve the liquidity of our ordinary shares, prevent our ordinary shares from remaining below the NASDAQ minimum bid price required
for continued listing or prevent future non-compliance with NASDAQ’s listing requirements.
There
can be no assurance that an active trading market for our ordinary shares will be sustained.
In addition, the stock market generally
has experienced extreme price and volume fluctuations that have often been unrelated or disproportionate to the operating performance
of listed companies. Broad market and industry factors may negatively affect the market price of our ordinary shares, regardless
of our actual operating performance. The market price and liquidity of the market for our ordinary shares that will prevail in
the market may be higher or lower than the price you pay and may be significantly affected by numerous factors, some of which
are beyond our control.
The price of our securities may be volatile, and
you could lose all or part of your investment.
The trading price of our ordinary shares
is likely to be highly volatile and could be subject to wide fluctuations in response to various factors, some of which are beyond
our control, including limited trading volume. In addition to the factors discussed in this “Risk Factors” section
and elsewhere in this annual report, these factors include:
|
·
|
adverse results
or delays in clinical trials;
|
|
·
|
actual or anticipated
variations in our operating results and our financial position;
|
|
·
|
otherwise provide
to the public and the publication of research reports about us or our industry;
|
|
·
|
adverse regulatory
decisions or changes in laws or regulations;
|
|
·
|
introduction
of new products or services offered by us or our competitors;
|
|
·
|
our inability
to obtain adequate product supply;
|
|
·
|
our inability
to establish collaborations, if needed;
|
|
·
|
our failure
to commercialize our product candidates;
|
|
·
|
departures
of key scientific or management personnel;
|
|
·
|
our ability
to successfully manage our growth and enter new markets;
|
|
·
|
disputes or
other developments relating to proprietary rights, including patents, litigation matters
and our ability to obtain patent protection for our technologies;
|
|
·
|
significant
lawsuits, including patent or shareholder litigation; and
|
|
·
|
other events
or factors, many of which are beyond our control.
|
In addition, the stock market in general,
and the NASDAQ Global Market and pharmaceutical companies in particular, have experienced extreme price and volume fluctuations
that have often been unrelated or disproportionate to the operating performance of these companies. Broad market and industry
factors may negatively affect the market price of our ordinary shares, regardless of our actual operating performance. If the
market price of our ordinary shares does not exceed your purchase price, you may not realize any return on your investment in
us and may lose some or all of your investment. In the past, securities class action litigation has often been brought against
a company following a decline in the market price of its securities. This risk is especially relevant for us because pharmaceutical
companies have experienced significant share price volatility in recent years.
We are no longer a foreign private issuer and are now
required to report as a domestic registrant, which could result in significant additional cost and expense.
As of June 30, 2016, we no longer met the
requirements to qualify as a foreign private issuer under the Exchange Act. As a result, we began reporting as a domestic registrant
as of January 1, 2017. The regulatory and compliance costs to us under U.S. securities laws as a U.S. domestic issuer may be significantly
more than costs we incurred as a foreign private issuer. As of January 1, 2017, we are required to file periodic reports including
annual reports on Form 10-K, quarterly reports on Form 10-Q and registration statements on U.S. domestic issuer forms with the
SEC, which are more detailed and extensive in certain respects than the forms available to a foreign private issuer. We are also
required under current SEC rules to prepare our consolidated financial statements in accordance with U.S. GAAP, rather than IFRS,
and to present our financial information in U.S. dollars instead of euros. In addition, we lost our ability to rely upon exemptions
from certain corporate governance requirements on U.S. stock exchanges that are available to foreign private issuers. We are now
also subject to the Exchange Act rules regulating disclosure obligations and procedural requirements related to the solicitation
of proxies, consents and authorizations applicable to a security registered under the Exchange Act, including the U.S. proxy rules
under Section 14 of the Exchange Act. Our officers and directors are also now subject to the reporting and “short-swing”
profit recovery provisions of Section 16 of the Exchange Act and related rules with respect to their purchases and sales of our
securities.
Our principal shareholders and management own a
significant percentage of our ordinary shares and will be able to exert significant control over matters subject to shareholder
approval.
Our executive officers, directors, board
members, 10% shareholders and their affiliates owned approximately 41.5% of our voting shares as of March 13, 2017.
Therefore, these shareholders, as a group, will have the ability to influence us through their ownership position. These shareholders
may be able to determine, or significantly influence, all matters requiring shareholder approval. For example, these shareholders
may be able to control elections of directors, amendments of our organizational documents, or approval of any merger, sale of
assets, or other major corporate transaction. This may prevent or discourage unsolicited acquisition proposals or offers for our
shares that you may feel are in your best interest as one of our shareholders. Our board members and their affiliates beneficially
owned approximately 9.0% of our outstanding ordinary shares as of March 13, 2017, after giving effect to the exercise of
all outstanding options to purchase ordinary shares. See “Item 12. Security Ownership of Certain Beneficial Owners and Management
and Related Stockholder Matters.”
We are an emerging growth company, and we cannot
be certain that the reduced reporting requirements applicable to emerging growth companies will make our securities less attractive
to investors.
We are an emerging growth company, as defined
in the Jumpstart Our Business Startups Act of 2012, or the JOBS Act. For as long as we continue to be an emerging growth company,
we may take advantage of exemptions from various reporting requirements that are applicable to other public companies that are
not emerging growth companies,
including not being required to comply with
the auditor attestation requirements of Section 404 of the Sarbanes-Oxley Act of 2002, or the Sarbanes-Oxley Act, reduced disclosure
obligations regarding executive compensation in this annual report and our periodic reports and proxy statements and exemptions
from the requirements of holding nonbinding advisory votes on executive compensation and shareholder approval of any golden parachute
payments not previously approved. We could be an emerging growth company through December 31, 2019, the last day of our fiscal
year following the fifth anniversary of the 2014 date of the first sale of Innocoll Germany’s ADSs in our initial public
offering, although circumstances could cause us to lose that status earlier, including if the market value of our ordinary shares
held by non-affiliates exceeds $700.0 million as of any June 30 before that time or if we have total annual gross revenue of $1.0
billion or more during any fiscal year before that time, in which cases we would no longer be an emerging growth company as of
the following December 31 or, if we issue more than $1.0 billion in non-convertible debt during any three-year period before that
time, we would cease to be an emerging growth company immediately. We cannot predict if investors will find our securities less
attractive because we may rely on these exemptions. If some investors find our securities less attractive as a result, there may
be a less active trading market for our ordinary shares and our share price may be more volatile.
Under the JOBS Act, an emerging growth
company can delay the adoption of certain accounting standards until those standards would otherwise apply to private companies.
Innocoll AG prepared its financial statements in accordance with International Financial Reporting Standards, or IFRS, as issued
by the International Accounting Standards Board, or IASB, which do not have separate provisions for publicly traded and private
companies. However, as Innocoll Holdings plc has transitioned its financial statements to be prepared in accordance with U.S.
GAAP, as an emerging growth company, we may be able to take advantage of the benefits of this extended transition period.
We have no present intention to pay dividends on
our ordinary shares in the foreseeable future and, consequently, your only opportunity to achieve a return on your investment
during that time is if the price of our ordinary shares appreciates.
We have no present intention to pay dividends
on our ordinary shares in the foreseeable future. In addition, for so long as our loan obligations under the financing contract
with EIB are outstanding, our ability to pay dividends is limited to certain circumstances. Any recommendation by our board to
pay dividends will depend on many factors, including our financial condition, results of operations, legal requirements and other
factors. In addition, if we issue securities at an equivalent value below $7.00 per ordinary share of Innocoll Ireland (based
on conversion to U.S. dollars at an exchange rate of $1.0663 per euro, the official exchange rate quoted as of March 13,
2017 by the European Central Bank), we may be required to adjust the exercise price of certain outstanding options pursuant to
our obligations under the 2014 Option Agreement (for more details on the 2014 Option Agreement, see “Item 7. Management’s
Discussion and Analysis of Financial Condition and Results of Operations―Liquidity and Capital Resources—2014 Option
Agreement”). Accordingly, if the price of our ordinary shares declines in the foreseeable future, you will incur a loss
on your investment, without the likelihood that this loss will be offset in part or at all by potential future cash dividends.
Raising additional capital may cause additional
dilution of the percentage ownership of our shareholders, restrict our operations, require us to relinquish rights to our technologies,
products or product candidates and could cause our share price to fall.
We expect that significant additional capital
may be needed in the future to continue our planned operations, including conducting clinical trials, commercialization efforts,
expanding our manufacturing facility, expanded research and development activities and costs associated with operating a public
company. To raise capital, we may sell ordinary shares, convertible securities or other equity securities in one or more transactions
at prices and in a manner we determine from time to time. If we sell ordinary shares, convertible securities or other equity securities,
investors may be materially diluted by subsequent sales. Such sales may also result in material dilution to our existing shareholders,
and new investors could gain rights, preferences and privileges senior to the holders of our ordinary shares. The incurrence of
indebtedness could result in increased fixed payment obligations and could involve certain restrictive covenants, such as limitations
on our ability to incur additional debt and other operating restrictions that could adversely impact our ability to conduct our
business. In addition, if we issue securities at an equivalent value below $7.00 per ordinary share of Innocoll Ireland (based
on conversion to U.S. dollars at an exchange rate of $1.0663 per euro, the official exchange rate quoted as of
March 13, 2017 by the European Central Bank), we may be required to adjust the exercise price of certain outstanding options
pursuant to our obligations under the 2014 Option Agreement (for more
details on the 2014 Option Agreement, see
“Item 7. Management’s Discussion and Analysis of Financial Condition and Results of Operations―Liquidity and
Capital Resources—2014 Option Agreement”). If we raise additional funds through strategic partnerships and alliances
and licensing arrangements with third parties, we may have to relinquish valuable rights to our technologies, products or product
candidates, or grant licenses on terms unfavorable to us.
Substantial future sales of our securities in the
public market, or the perception that these sales could occur, could cause the price of our securities to decline.
Additional sales of our securities in the
public market, or the perception that these sales could occur, could cause the market price of our securities to decline. As of
March 13, 2017, we had 29,748,239 ordinary shares outstanding, including an aggregate of up to 911,982 ordinary shares
registered pursuant to an effective resale registration statement that may be offered by the selling shareholders identified therein.
To the extent additional ordinary shares are sold into the market, the market price of our ordinary shares could decline.
Unstable market and economic conditions may have
serious adverse consequences on our business, financial condition and share price.
As widely reported, global credit and financial
markets have experienced extreme disruptions in the past several years, including severely diminished liquidity and credit availability,
declines in consumer confidence, declines in economic growth, increases in unemployment rates and uncertainty about economic stability.
There can be no assurance that further deterioration in credit and financial markets and confidence in economic conditions will
not occur. Our general business strategy may be adversely affected by any such economic downturn, volatile business environment
or continued unpredictable and unstable market conditions. If the current equity and credit markets deteriorate, or do not improve,
it may make any necessary debt or equity financing more difficult, more costly, and more dilutive. Failure to secure any necessary
financing in a timely manner and on favorable terms could have a material adverse effect on our growth strategy, financial performance
and share price and could require us to delay or abandon clinical development plans. In addition, there is a risk that one or
more of our current service providers, manufacturers and other partners may not survive these difficult economic times, which
could directly affect our ability to attain our operating goals on schedule and on budget.
At December 31, 2016, we had approximately
$15.8 million of cash, cash equivalents and short-term investments. While we are not aware of any downgrades, material losses,
or other significant deterioration in the fair value of our cash equivalents since December 31, 2016, no assurance can be given
that further deterioration of the global credit and financial markets would not negatively impact our current portfolio of cash
equivalents or marketable securities or our ability to meet our financing objectives. Furthermore, our share price may decline
due in part to the volatility of the stock market and the general economic downturn.
We and certain of our officers are currently subject
to securities class action litigation, and could be subject to additional securities class action litigation in the future.
We and certain of our officers have
been named as defendants in two securities class action lawsuits. Neither complaint has been served, although the plaintiffs have
requested the defendants to waive service of summons pursuant to Federal Rule of Civil Procedure 4. The complaints in both actions
allege that we and certain of our executive officers violated Section 10(b) of the Exchange Act and Rule 10b-5 promulgated thereunder
by making materially false or misleading statements and omissions relating to the development of Xaracoll and/or related requests
for regulatory approval. The complaints also allege that the defendant officers violated Section 20(a) of the Exchange Act. While
we believe that we have substantial legal and factual defenses to the claims in the class actions and intend to vigorously defend
the case, these lawsuits could divert our management's and board's attention from other business matters, the outcome of the pending
litigation is difficult to predict and quantify, and the defense against the underlying claims will likely be costly. The ultimate
resolution of this matter could result in payments of monetary damages or other costs, materially and adversely affect our business,
financial condition, results of operations and cash flows, or adversely affect our reputation, and consequently, could negatively
impact the price of our ordinary shares.
We have insurance policies related to
the risks associated with our business, including directors' and officers' liability insurance policies. However, there is no
assurance that our insurance coverage will be sufficient or that our insurance carriers will cover all claims in that litigation.
If we are not successful in our defense of the claims asserted in the putative action and those claims are not covered by insurance
or exceed our insurance coverage, we may have to pay damage awards, indemnify our officers from damage awards that may be entered
against them and pay the costs and expenses incurred in defense of, or in any settlement of, such claims.
In addition, there is the potential
for additional shareholder litigation with similar claims against us, and we could be materially and adversely affected by such
matters. Even if such claims are not successful, these lawsuits or other future similar actions, or other regulatory inquiries
or investigations, may result in substantial costs and have a significant adverse impact on our reputation and divert management’s
attention and resources, which could have a material adverse effect on our business, operating results or financial condition.
If securities or industry analysts do not publish
research, or publish inaccurate or unfavorable research, about our business, our share price and trading volume could decline.
The trading market for our ordinary shares
will depend in part on the research and reports that securities or industry analysts publish about us or our business. Securities
and industry analysts do not currently, and may never,
publish research on our company. If no securities
or industry analysts commence coverage of our company, the trading price for our shares would likely be negatively impacted. In
the event securities or industry analysts initiate coverage, if one or more of the analysts who covers us downgrades our shares
or publishes inaccurate or unfavorable research about our business, our share price may decline. If one or more of these analysts
ceases coverage of our company or fails to publish reports on us regularly, demand for our shares could decrease, which might
cause our share price and trading volume to decline.
We may qualify as a passive foreign investment company,
or “PFIC,” which could result in adverse U.S. federal income tax consequences to U.S. investors.
The treatment of U.S. holders (as defined
under U.S. federal income tax law) of Innocoll Ireland ordinary shares could be subject to material adverse tax consequences as
described herein if, at any relevant time, Innocoll Germany or Innocoll Ireland were a PFIC. In general, if you are a U.S. holder,
Innocoll Germany and/or Innocoll Ireland will be a PFIC with respect to you if for any taxable year in which you held ADSs or
ordinary shares of Innocoll Germany or ordinary shares of Innocoll Ireland: (i) at least 75% of the gross income of Innocoll Germany
or Innocoll Ireland, as applicable, for the taxable year is passive income or (ii) at least 50% of the value, determined on the
basis of a quarterly average (looking through certain corporate subsidiaries), of the assets of Innocoll Germany or Innocoll Ireland,
as applicable, is attributable to assets that produce or are held for the production of passive income. Passive income generally
includes dividends, interest, rents and royalties (other than certain rents and royalties derived in the active conduct of a trade
or business), annuities and gains from the disposition of assets that produce passive income.
We believe that Innocoll Germany should
not be treated as having been a PFIC in any prior taxable year and should not be treated as a PFIC in the taxable year in which
the Merger occurred. In addition, we believe that Innocoll Ireland should not be treated as a PFIC immediately after the Merger.
However, the tests for determining PFIC status are applied annually, and it is difficult to accurately predict future income and
assets relevant to this determination. Accordingly, we cannot assure U.S. holders that Innocoll Germany and Innocoll Ireland will
not be or become a PFIC. Moreover, the determination of PFIC status depends, in part, on the application of complex U.S. federal
income tax rules, which are subject to differing interpretations. As a result, whether Innocoll Germany or Innocoll Ireland is
or will be a PFIC for any relevant taxable year cannot be predicted with certainty, and there can be no assurance that the IRS
will not challenge our determination concerning our PFIC status.
If Innocoll Germany prior to the consummation of the Merger, and Innocoll Ireland, after the consummation
of the Merger, were to be treated as a PFIC, except as otherwise provided by certain election regimes, a U.S. holder would be
subject to special adverse tax rules with respect to (i) “excess distributions” received on our ADS or ordinary shares
of Innocoll Germany, and ordinary shares of Innocoll Ireland, as the case may be, and (ii) any gain recognized upon a sale or
other disposition (including a pledge) of ADSs or ordinary shares of Innocoll Germany or ordinary shares of Innocoll Ireland,
as the case may be. We urge U.S. holders to consult their own tax advisors regarding the possible application of the PFIC rules,
including any election regimes.
Exchange rate fluctuations may reduce the amount
of U.S. dollars you receive in respect of any dividends or other distributions we may pay in the future in connection with your
ordinary shares.
Under Irish law, dividends and distributions
may only be made from distributable reserves. Distributable reserves, broadly, means the accumulated realized profits of a company
less accumulated realized losses of the company on a standalone basis. In addition, no distribution or dividend may be made unless
the net assets of Innocoll Ireland are equal to, or in excess of, the aggregate of Innocoll Irelands’s called up share capital
plus undistributable reserves and the distribution does not reduce Innocoll Ireland’s net assets below such aggregate. Undistributable
reserves include Innocoll Ireland’s undenominated capital and the amount by which Innocoll Ireland’s accumulated unrealized
profits, so far as not previously utilized by any capitalization, exceed Innocoll Ireland’s accumulated unrealized losses,
so far as not previously written off in a reduction or reorganization of capital. The determination as to whether or not Innocoll
Ireland has sufficient distributable reserves to fund a dividend must be made by reference to “relevant entity financial
statements” of Innocoll Ireland being either the last set of unconsolidated annual audited financial statements or unaudited
financial statements prepared in accordance with the Irish Companies Act, which give a “true and fair view” of Innocoll
Ireland’s unconsolidated financial position and accord with accepted accounting practice.
Exchange rate fluctuations may affect the
amount in U.S. dollars that our shareholders receive upon the payment of cash dividends or other distributions we declare and
pay in euro, if any. Such fluctuations could adversely affect the value of our ordinary shares and, in turn, the U.S. dollar proceeds
that holders receive from the sale of our ordinary shares.
U.S. investors may have difficulty enforcing civil
liabilities against our company or members of our board and the experts named in this annual report.
The members of our board and certain of
the experts named in this annual report are non-residents of the United States, and all or a substantial portion of the assets
of such persons are located outside the United States. As a result, it may not be possible, or may be very difficult, to serve
process on such persons or us in the United States or to enforce judgments obtained in U.S. courts against them or us based on
civil liability provisions of the securities laws of the United States. In addition, it may not be possible to enforce court judgments
obtained in the United States against us in Ireland based on the civil liability provisions of the U.S. federal or state securities
laws. We have been advised by William Fry, our Irish counsel, that the United States currently does not have a treaty with Ireland
providing for the reciprocal recognition and enforcement of judgments in civil and commercial matters.
The following requirements must be met
before a judgment of a U.S. court will be deemed to be enforceable in Ireland: the judgment must be for a definite sum; the judgment
must be final and conclusive; and the judgment must be provided by a court of competent jurisdiction.
An Irish court will also exercise its right
to refuse enforcement if the U.S. judgment was obtained by fraud, if the judgment violates Irish public policy, if the judgment
is in breach of natural justice or if it is irreconcilable with an earlier foreign judgment. There is some uncertainty as to whether
the courts of Ireland would recognize or enforce judgments of U.S. courts obtained against us or our directors or officers based
on the civil liabilities provisions of the U.S. federal or state securities laws or hear actions against us or those persons based
on those laws. Therefore, a final judgment for the payment of money rendered by any U.S. federal or state court based on civil
liability, whether or not based solely on U.S. federal or state securities laws, would not automatically be enforceable in Ireland.
We will continue to incur significant increased
costs as a result of operating as a company whose securities are publicly traded in the United States, and our management will
continue to be required to devote substantial time to new compliance initiatives.
As a company whose securities commenced
trading in the United States in July 2014, we will continue to incur significant legal, accounting, insurance and other expenses
that we did not previously incur. In addition, the Sarbanes-Oxley Act, the Dodd-Frank Wall Street Reform and Consumer Protection
Act and related rules implemented by the SEC and the NASDAQ Global Market have imposed various requirements on public companies,
including requiring establishment and maintenance of effective disclosure and financial controls. These costs will increase at
the time we are no longer an emerging growth company eligible to rely on exemptions under the JOBS Act from certain disclosure
and governance requirements. Our management and other personnel will need to devote a substantial amount of time to these compliance
initiatives. Moreover, these rules and regulations will increase our legal and financial compliance costs and will make some activities
more time-consuming and costly. These laws and regulations could also make it more difficult and expensive for us to attract and
retain qualified persons to serve on our board or its committees or on our management board. Furthermore, if we are unable to
satisfy our obligations as a public company, we could be subject to delisting of our ordinary shares, fines, sanctions and other
regulatory action and potentially civil litigation.
If we fail to maintain an effective system of internal
control over financial reporting in the future, we may not be able to accurately report our financial condition, results of operations
or cash flows, which may adversely affect investor confidence in us.
The Sarbanes-Oxley Act requires, among
other things, that we maintain effective internal controls over financial reporting and disclosure controls and procedures. In
particular, we are required, beginning with our fiscal year ending December 31, 2015, under Section 404 of the Sarbanes-Oxley
Act, to perform system and process evaluations and testing of our internal controls over financial reporting to allow management
to report on the effectiveness of our internal control over financial reporting. This assessment will need to include disclosure
of any material weaknesses in our internal control over financial reporting identified by our management. A material weakness
is a control deficiency,
or combination of control deficiencies, in
internal control over financial reporting that results in more than a reasonable possibility that a material misstatement of annual
or interim financial statements will not be prevented or detected on a timely basis. Section 404 of the Sarbanes-Oxley Act also
generally requires an attestation from our independent registered public accounting firm on the effectiveness of our internal
control over financial reporting. However, for as long as we remain an emerging growth company as defined in the JOBS Act, we
intend to take advantage of the exemption permitting us not to comply with the independent registered public accounting firm attestation
requirement. At the time when we are no longer an emerging growth company, our independent registered public accounting firm may
issue a report that is adverse in the event it is not satisfied with the level at which our controls are documented, designed
or operating. Our remediation efforts may not enable us to avoid a material weakness in the future.
Our compliance with Section 404 caused
us to incur substantial accounting expenses and expend significant management efforts. We may not always be able to complete our
evaluation, testing and any required remediation in a timely fashion. During the evaluation and testing process, if we identify
one or more material weaknesses in our internal control over financial reporting, we will be unable to assert that our internal
control over financial reporting is effective. We cannot assure you that there will not be material weaknesses or significant
deficiencies in our internal control over financial reporting in the future. Any failure to maintain internal control over financial
reporting could severely inhibit our ability to accurately report our financial condition, results of operations or cash flows.
If we are unable to conclude that our internal control over financial reporting is effective, or if our independent registered
public accounting firm determines we have a material weakness or significant deficiency in our internal control over financial
reporting, we could lose investor confidence in the accuracy and completeness of our financial reports, the market price of the
ordinary shares could decline, and we could be subject to sanctions or investigations by the NASDAQ Global Market, the SEC or
other regulatory authorities. Failure to remedy any material weakness in our internal control over financial reporting, or to
implement or maintain other effective control systems required of public companies, could also restrict our future access to the
capital markets.
In order to satisfy our obligations as a public
company, we may need to hire qualified accounting and financial personnel with appropriate public company experience.
As a newly public company, we will need
to establish and maintain effective disclosure and financial controls and make changes in our corporate governance practices.
We may need to hire additional accounting and financial personnel with appropriate public company experience and technical accounting
knowledge, and it may be difficult to recruit and retain such personnel. Even if we are able to hire appropriate personnel, our
existing operating expenses and operations will be impacted by the direct costs of their employment and the indirect consequences
related to the diversion of management resources from research and development efforts.
Item 1B. Unresolved Staff Comments.
None.
Item 2. Properties.
Our manufacturing facility is located
on a site in Saal, Germany and consists of two production facilities, which occupy a total of approximately 30,000 square feet,
and an office building of approximately 6,500 square feet. We have leased the facilities pursuant to lease agreement dated April
2009 for a 10-year term, which is subject to additional five-year renewal options. Activities in this facility include the manufacture
of all our products and product candidates and quality control testing, product storage, development of analytical methods, research
and development, the coordination of clinical and regulatory functions, and general administrative functions. We have also leased
space in Saal, Germany, including a workshop building, for a 15-year term, which is subject to additional five-year renewal options.
This property will be used as an office, a laboratory, a warehouse, and for the production of pharmaceutical products and products
under the German Medical Device Act. The monthly rent is €15,494.50 plus the statutory Value Added Tax (“V.A.T.”)
applicable from time to time. With the current V.A.T. of 19%, equaling €2,943.96, the gross rent is €18,438.46. We expect
to complete a capacity expansion build-out of our production facility to approximately 50,000 square feet to expand its production
capacity to support commercial production of XaraColl, and the expanded facility is expected to be fully operational by the second
half of 2017. Once completed and approved, we anticipate that our production capacity will be sufficient to meet currently forecasted
market demand (including those marketed and sold through our partners) for all our current and late-stage pipeline product candidates.
We believe that once our factory
expansion program has been completed, our facility will be
adequate to meet our current needs, and that suitable additional alternative spaces will be available in the future on commercially
reasonable terms, if required
Our corporate headquarters are located
in Athlone, Ireland, where we lease an office. We have leased approximately 6,824 square feet of property in Newton Square, PA
in the U.S. for a corporate office pursuant to a lease agreement dated October 2015 for a three-year term. The monthly rent charged
in the first year under the lease is $15,069.67, which amount shall annually be increased over the three-year term. This lease
replaced a previous lease of different property in Newton Square, PA for 2,606 square feet.
Item 3. Legal Proceedings.
We and certain of our officers are subject
to two securities class action lawsuits, which may require significant management and board time and attention and significant
legal expenses and may result in an unfavorable outcome, which could have a material adverse effect on our business, financial
condition, results of operations and cash flows.
We and certain of our executive officers
have been named as defendants in a securities class action lawsuit initially filed in the United States District Court for the
Eastern District of Pennsylvania on January 24, 2017, captioned Anthony Pepicelli v. Innocoll Holdings Public Limited Company,
Anthony P. Zook, Jose Carmona and Lesley Russel, civil action no. 2:17-cv-00341-GEKP. We and certain of our executive officers
also have been named as defendants in a securities class action lawsuit initially filed in the United States District Court for
the Eastern District of Pennsylvania on February 16, 2017, captioned Jianmin Huang v. Innocoll Holdings Public Limited Company,
Anthony P. Zook, Jose Carmona and Lesley Russel, civil action no. 2:17-cv-00740-GEKP. Neither complaint has been served, although
the plaintiffs have requested the defendants to waive service of summons pursuant to Federal Rule of Civil Procedure 4. The complaints
in both actions allege that we and certain of our executive officers violated Section 10(b) of the Exchange Act and Rule 10b-5
promulgated thereunder by making materially false or misleading statements and omissions relating to the development of Xaracoll
and/or related requests for regulatory approval. The complaints also allege that the defendant officers violated Section 20(a)
of the Exchange Act. While we believe that we have substantial legal and factual defenses to the claims in the class actions and
intend to vigorously defend the case, these lawsuits could divert our management’s and board’s attention from other
business matters, the outcome of the pending litigation is difficult to predict and quantify, and the defense against the underlying
claims will likely be costly. The ultimate resolution of this matter could result in payments of monetary damages or other costs,
materially and adversely affect our business, financial condition, results of operations and cash flows, or adversely affect our
reputation, and consequently, could negatively impact the price of our ordinary shares.
We have insurance policies related to the
risks associated with our business, including directors’ and officers’ liability insurance policies. However, there is no assurance
that our insurance coverage will be sufficient or that our insurance carriers will cover all claims in that litigation. If we
are not successful in our defense of the claims asserted in the putative action and those claims are not covered by insurance
or exceed our insurance coverage, we may have to pay damage awards, indemnify our officers from damage awards that may be entered
against them and pay the costs and expenses incurred in defense of, or in any settlement of, such claims.
In addition, there is the potential for
additional shareholder litigation against us, and we could be materially and adversely affected by such matters.
Item 4. Mine Safety Disclosures.
Not applicable.
PART II
Item 5. Market for Registrant’s Common Equity, Related
Stockholder Matters and Issuer Purchases of Equity Securities.
Market
Our ordinary shares trade on the NASDAQ
Global Market under the symbol “INNL”. Historically, Innocoll Germany’s ADSs represented 1/13.25 of one ordinary
share of Innocoll AG. Innocoll Germany’s ADSs were listed on the NASDAQ Global Market from July 25, 2014 to March 15, 2016.
Upon the effectiveness of the Merger, we terminated Innocoll Germany’s ADS facility, each cancelled ADS was effectively
exchanged for one ordinary share of Innocoll Ireland and holders of Innocoll Germany ordinary shares received 13.25 ordinary shares
of Innocoll Ireland in exchange for each share held of Innocoll Germany. Simultaneous with this transaction, Innocoll Ireland
listed its ordinary shares on the NASDAQ Global Market under the symbol “INNL”, which we previously used for Innocoll
Germany’s ADSs. Our ordinary shares, par value $0.01 per share, have been listed on the NASDAQ Global Market since March
16, 2016.
The following table sets forth for the
periods indicated the reported high and low sale prices of Innocoll Germany’s ADSs through March 15, 2016, and Innocoll
Ireland’s ordinary shares from March 16, 2016, each on the NASDAQ Global Market.
Fiscal Year 2016
|
|
High
|
|
|
Low
|
|
|
|
|
|
|
|
|
4th Quarter ended December 31
|
|
$
|
6.51
|
|
|
$
|
0.59
|
|
3rd Quarter ended September 30
|
|
$
|
6.50
|
|
|
$
|
4.65
|
|
2nd Quarter ended June 30
|
|
$
|
12.94
|
|
|
$
|
4.57
|
|
1st Quarter ended March 31
|
|
$
|
9.35
|
|
|
$
|
6.01
|
|
|
|
|
|
|
|
|
|
|
Fiscal Year 2015
|
|
High
|
|
|
Low
|
|
|
|
|
|
|
|
|
4
th
Quarter ended December 31
|
|
$
|
13.72
|
|
|
$
|
6.30
|
|
3
rd
Quarter ended September 30
|
|
$
|
15.19
|
|
|
$
|
10.98
|
|
2
nd
Quarter ended June 30
|
|
$
|
16.46
|
|
|
$
|
6.98
|
|
1
st
Quarter ended March 31
|
|
$
|
8.98
|
|
|
$
|
6.00
|
|
Holders
As of March 13, 2017, we had 13 record
holders of our ordinary shares. The number of record holders is based on the actual number of holders registered on the books
of our transfer agent and does not reflect holders of shares in “street name” or persons, partnerships, associations,
corporations or other entities identified in security position listings maintained by depository trust companies.
Dividends
Neither we nor our legal predecessors,
Innocoll AG or Innocoll GmbH, have ever declared or paid any cash dividends on our ordinary shares, and we have no present intention
of declaring or paying any dividends in the foreseeable future. In addition, for so long as our loan obligations under the financing
contract with EIB are outstanding, our ability to pay dividends is limited to certain circumstances (for more details on the financing
contract with EIB, see “Item 7. Management’s Discussion and Analysis of Financial Condition and Results of Operations―Liquidity
and Capital Resources―Financing Activity—EIB Loan”). Any recommendation by our board to pay dividends, subject
to compliance with applicable law and any contractual provisions that restrict or limit our ability to pay dividends, including
under agreements for indebtedness that we may incur, will depend on many factors, including our financial condition, results of
operations, legal requirements, capital requirements, business prospects and other factors that our board deems relevant. We make
no assurances that we will ever pay dividends, cash or otherwise.
Irish Restrictions on Import and Export of Capital
The Financial Transfers Act 1992 provides
that the Irish Minister for Finance can make provision for the restriction of financial transfers between Ireland and other countries.
For the purposes of this Act, “financial transfers” include all transfers which would be movements of capital or payments
within the meaning of the treaties governing the European Communities if they had been made between Member States of the Communities.
This Act has been used by the Minister for Finance to implement European Council Directives, which provide for the restriction
of financial transfers to certain countries, organizations and people including the Al-Qaeda network and the Taliban, Afghanistan,
Belarus, Burma (Myanmar), Democratic People’s Republic of Korea, Democratic Republic of Congo, Egypt, Eritrea, Iran, Iraq,
Ivory Coast, Lebanon, Liberia, Libya, Republic of Guinea, Somalia, Sudan, Syria, Tunisia, Yugoslavia (Slobodan Milosevic and associated
persons and certain persons indicted by the International Criminal Tribunal for the former Yugoslavia who are still at large)
and Zimbabwe, and terrorist groups and persons listed under Council Implementing Regulation (EU) No. 1169/2012 (as amended).
Irish Taxes Applicable to U.S. Holders
Dividend withholding tax
Distributions made by Innocoll will generally
be subject to Irish dividend withholding tax (“DWT”) at the standard rate of income tax (currently 20 percent) unless
an exemption applies. For DWT purposes, a dividend includes any distribution made by Innocoll to its shareholders, including cash
dividends, non-cash dividends and additional stock or units taken in lieu of a cash dividend. Innocoll Ireland is responsible
for withholding DWT at source and forwarding the relevant payment to the Irish Revenue Commissioners.
Dividends paid to U.S. residents will not
be subject to Irish DWT provided that:
|
·
|
in
the case of a beneficial owner, the address of the beneficial owner in the records of
his or her broker is in the United States and this information is provided by the broker
to the Company’s qualifying intermediary; or
|
|
·
|
in
the case of a record owner, the record owner has provided to the Company’s transfer
agent a valid Irish DWT form showing a U.S. address to the transfer agent at least seven
business days before the record date for the first dividend payment to which they are
entitled.
|
Irish income tax may also arise with respect
to dividends paid on Innocoll’s ordinary shares. A U.S. resident who meets one of the exemptions from DWT described above
and who does not hold Innocoll shares through a branch or agency in Ireland through which a trade is carried on generally will
not have any Irish income tax or universal social charge liability on a dividend paid by Innocoll. In addition, if a U.S. shareholder
is subject to DWT, the withholding payment generally discharges any Irish income tax or universal social charge liability, provided
the shareholder furnishes to the Irish Revenue Commissioners a statement of the DWT imposed.
While the U.S./Ireland Double Tax Treaty
contains provisions regarding withholding, due to the wide scope of the exemptions from DWT available under Irish domestic law,
it would generally be unnecessary for a U.S. resident shareholder to rely on the treaty provisions.
Irish Tax on Chargeable Gains
The rate of tax on chargeable gains (where
applicable) in Ireland is currently 33%. Innocoll shareholders that are not resident or ordinarily resident in Ireland for Irish
tax purposes and do not hold their shares in connection with a trade carried on by such holder in Ireland through a branch or
agency will not be liable for Irish tax on chargeable gains realized on a subsequent disposal of their Innocoll ordinary shares
provided at the time of disposal: (i) the Innocoll ordinary shares are quoted on a recognized stock exchange; or (ii) the Innocoll
ordinary shares do not derive the greater part of their value from land, buildings, minerals, or mineral or exploration rights
in Ireland.
Innocoll shareholders that are resident
or ordinarily resident in Ireland for Irish tax purposes or shareholders that hold their shares in connection with a trade carried
on by such holder in Ireland through a branch or agency will, subject to the availability of exemptions and reliefs, be within
the charge to Irish tax on chargeable gains arising on a subsequent disposal of their Innocoll ordinary shares.
A holder of Innocoll ordinary shares who
is an individual and who is temporarily non-resident in Ireland may, under Irish anti-avoidance legislation, be liable to Irish
tax on any chargeable gain realized on a disposal during the period in which such individual is non-resident.
Capital Acquisitions Tax
Irish capital acquisitions tax (“CAT”)
comprises principally of gift tax and inheritance tax. CAT could apply to a gift or inheritance of Innocoll ordinary shares irrespective
of the place of residence, ordinary residence or domicile of the deceased or donor of the shares (collectively referred to as
the “donor”) or the successor or donee of the shares (collectively referred to as the “donee”). This is
because Innocoll ordinary shares are regarded as property situated in Ireland as the share register of Innocoll must be held in
Ireland. The person who receives the gift or inheritance has primary liability for CAT. However there are certain circumstances
where another person such as an agent or personal representative may become accountable for the CAT.
CAT is currently levied at a rate of 33%
above certain tax-free thresholds. The appropriate tax-free threshold is dependent upon (1) the relationship between the donor
and the donee and (2) the aggregation of the values of previous gifts and inheritances received by the donee from persons within
the same group threshold. Gifts and inheritances passing between spouses are exempt from CAT. Shareholders should consult their
own tax advisor as to whether CAT is creditable or deductible in computing any domestic tax liabilities.
Stamp Duty
The rate of stamp duty (where applicable)
on transfers of shares of Irish incorporated companies is 1% of the price paid or the market value of the shares acquired, whichever
is greater. Where Irish stamp duty arises it is generally a liability of the transferee.
Irish stamp duty may, depending on the manner
in which the Innocoll ordinary shares are held, be payable in respect of transfers of Innocoll ordinary shares.
Shares Held Through the Depository Trust Company (“DTC”)
A transfer of Innocoll ordinary shares effected
by means of the transfer of book-entry interests in DTC will not be subject to Irish stamp duty.
Shares Held Outside of DTC or Transferred Into or Out of
DTC
A transfer of Innocoll ordinary shares where
any party to the transfer holds such shares outside of DTC may be subject to Irish stamp duty.
Shareholders wishing to transfer their shares
into (or out of) DTC may do so without giving rise to Irish stamp duty, provided:
|
·
|
there
is no change in the ultimate beneficial ownership of such shares as a result of the transfer;
and
|
|
·
|
the
transfer into (or out of) DTC is not on a sale or in contemplation of a sale.
|
Recent Sales of Unregistered Securities
None.
Use of Proceeds
Not applicable.
Purchases of Equity Securities
Not applicable.
Item 6. Selected Financial Data.
You should read the following selected consolidated
financial data together with our consolidated financial statements and the related notes included in this annual report on Form
10-K and the “Management’s Discussion and Analysis of Financial Condition and Results of Operations” section
of this annual report.
We have derived the consolidated statement of operations
data for the years ended December 31, 2016, 2015 and 2014 and the consolidated balance sheet data as of December 31, 2016 and
2015 from our audited consolidated financial statements, which are included elsewhere in this annual report on Form 10-K. The
Company has omitted to present the consolidated statement of operations data for the years ended December 31, 2013 and 2012
and the balance sheet data as of December 31, 2014, 2013 and 2012, since this information was originally presented under IFRS
filed previously and to provide the information under US GAAP would cause unreasonable effort or expense.
|
|
Year ended and
as at December 31,
|
|
(in U.S.$000’s, except per
share amounts)
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Statement of Operations Data
|
|
|
|
|
|
|
|
|
|
|
|
|
Revenues
|
|
$
|
4,372
|
|
|
$
|
2,870
|
|
|
$
|
5,974
|
|
Loss from operating activities – continuing operations
|
|
|
(66,784)
|
|
|
|
(52,022)
|
|
|
|
(21,313)
|
|
Loss before income tax
|
|
|
(56,783)
|
|
|
|
(50,449)
|
|
|
|
(23,269)
|
|
Loss for the year – all attributable to equity holders of the company
|
|
|
(56,954)
|
|
|
|
(50,856)
|
|
|
|
(23,471)
|
|
Loss per share:
|
|
|
|
|
|
|
|
|
|
|
|
|
Basic & diluted
|
|
$
|
(2.12)
|
|
|
$
|
(2.28)
|
|
|
$
|
(2.41)
|
|
Balance Sheet Data
|
|
|
|
|
|
|
|
|
|
|
|
|
Total assets
|
|
$
|
42,002
|
|
|
$
|
52,760
|
|
|
|
|
|
Total current liabilities
|
|
|
15,368
|
|
|
|
16,650
|
|
|
|
|
|
Long-term debt
|
|
|
29,830
|
|
|
|
28,210
|
|
|
|
|
|
Stockholders’ equity
|
|
|
(3,196)
|
|
|
|
7,900
|
|
|
|
|
|
Item 7. Management’s Discussion and Analysis of Financial
Condition and Results of Operations.
The following discussion should be read
in conjunction with our consolidated financial statements, which present our results of operations for the years ended December
31, 2016, 2015 and 2014, as well as our balance sheets at December 31, 2016 and 2015, contained elsewhere in this annual report
on Form 10-K. Some of the information contained in this discussion and analysis or set forth elsewhere in this annual report,
including information with respect to our plans and strategy for our business and related financing, includes forward-looking
statements that involve risks and uncertainties. You should review the “Special Note Regarding Forward Looking Statements”
and “Risk Factors” sections of this annual report for a discussion of important factors that could cause actual results
to differ materially from the results described in or implied by the forward-looking statements contained in the following discussion
and analysis.
Overview
We are a global, commercial stage, specialty
pharmaceutical and medical device company, with late-stage development programs targeting areas of significant unmet medical need.
We were incorporated in Delaware under the name Innocoll, Inc. in December 1997 and renamed Innocoll Holdings, Inc. in May 2004.
Since 2004, our research and business development has been led and coordinated by our Irish subsidiaries. These Irish entities
own our intellectual property and will be subject to Irish corporate tax on their future profits after the utilization of their
tax losses. The applicable Irish corporate tax rate is 12.5%. In July 2013, we re-domiciled Innocoll Holdings, Inc. from the United
States to Germany pursuant to a contribution-in-kind and share for share exchange into Innocoll GmbH, a German limited liability
company, as a result of which Innocoll Holdings, Inc. became Innocoll GmbH’s wholly-owned subsidiary. On July 3, 2014, Innocoll
GmbH transformed into a German stock corporation, “Innocoll AG.” Innocoll AG was effectively managed and controlled
from Ireland and had, therefore, become tax resident in Ireland under the terms of the Ireland-Germany double tax treaty with
effect as of January 1, 2014. On March 16, 2016, Innocoll AG merged with Innocoll Holdings plc, a public limited company formed
under Irish law, by way of a European cross-border merger with Innocoll Ireland being the surviving company. Prior to the Merger
Innocoll Holdings plc was a dormant company with minimal legally required share capital and related debtor on the statement of
financial position. The Merger effectively resulted in Innocoll Ireland becoming the publicly-traded parent of the Innocoll group
of companies carrying on the same business as that conducted by Innocoll Germany prior to the Merger. Accordingly, the consolidated
information presented herein refers to Innocoll Holdings, Inc., as the “company,” and with its direct and indirect
subsidiaries, collectively, as the “group,” for the period from January 1, 2012 until July 24, 2013 and to Innocoll
AG, as the “company,” and with its direct and indirect subsidiaries, collectively, as the “group,” for
the period from July 25, 2013 until March 15, 2016 and to Innocoll Holdings plc, as the “company”, and with
its direct and indirect subsidiaries, collectively, as the “group”, for the period from March 16, 2016 until
December 31, 2016. Except where indicated to the contrary, or the context suggests otherwise, all share and per share information:
(i) not presented in the financial statements or financial statement data refers to ordinary shares of Innocoll Holdings plc,
and (ii) included in the financial statements and financial statement data for Innocoll AG refers to ordinary shares of Innocoll
Germany prior to the Merger. Innocoll Ireland, together with its direct and indirect wholly owned subsidiaries as of the time
relevant to the applicable reference, are collectively referred to as the Innocoll Group. Innocoll and its current direct and
indirect wholly owned subsidiaries are collectively referred to as “we,” “us,” “our,” “Innocoll”
or the “Company.”
As of December 31, 2016, we had four marketed
products: (i) CollaGUARD, which utilizes our CollaFilm® technology, a transparent, bioresorbable collagen film for the prevention
of post-operative adhesions in multiple surgical applications, including digestive, colorectal, gynecological and urological surgeries;
(ii) Collatamp Gentamicin Surgical Implant, or CollatampG, which utilizes our CollaRx® sponge technology indicated for the
treatment or prevention of post-operative infection; (iii) Septocoll®, a bioresorbable, dual-action collagen sponge, indicated
for the treatment or prevention of post-operative infection, which we manufacture and supply to Biomet Orthopedics Switzerland
GmbH, or Biomet; and (iv) RegenePro, a bioresorbable collagen sponge for dental applications which we manufacture and supply
to Biomet 3i.
All of our marketed products are currently
sold by commercial partners. CollatampG has been marketed outside of the United States since 1985, and is currently approved for
sale in 62 countries across Africa, Asia, Europe, Latin America and the Middle East. EUSA Pharma has rights to distribute CollatampG
in all worldwide markets, excluding the United States. We have been supplying Septocoll to Biomet since 2001, for distribution
to markets in
Europe and the Middle East. CollaGUARD has been approved in
12 countries within Asia, Europe, Latin America and the Middle East. RegenePro was launched by Biomet 3i in the United States
in July 2014.
From 2004 to 2016, we incurred significant
operating losses including a total of $121.2 million spent on research and development in relation to our products and product
candidates. Our operating losses were $66.8 million, $52.0 million and $21.3 million for the years ended December 31, 2016,
2015 and 2014, respectively. We do not expect that our currently marketed products alone will generate revenue that is sufficient
for us to achieve profitability because we expect to continue to incur significant expenses as we advance the development of XaraColl,
CollaGUARD and our other product candidates, seek FDA and other regulatory approval for our product candidates that successfully
complete clinical trials and develop our sales force and marketing capabilities to prepare for the commercial launch of our product
candidates. We also expect to incur additional expenses expanding our operational, financial and management information systems
and personnel, including personnel to support our product development efforts and our obligations as a public reporting company.
For us to become and remain profitable, we believe that we must succeed in commercializing XaraColl, CollaGUARD or other product
candidates with significant market potential.
For further information regarding our business
and operations, see “Item 1. Business.”
Transition to U.S. GAAP and Change in Reporting Currency
As of June 30, 2016, we no longer met
the requirements to qualify as a foreign private issuer under the Exchange Act. As a result, we began reporting as a domestic
registrant as of January 1, 2017 and we are now required under current SEC rules to prepare our financial statements in
accordance with U.S. GAAP, rather than IFRS, and to present our financial information in U.S. dollars instead of euros. The
transition from consolidated financial statements under IFRS to U.S. GAAP has impacted the results, presentation and
disclosures of our consolidated balance sheets and consolidated statements of shareholders (deficit)/equity as of December
31, 2015 and January 1, 2014 and consolidated statements of operations and comprehensive loss, and our consolidated
statements of cash flows (effects of exchange rate changes on cash and cash equivalents) for the years ended December 31, 2015
and 2014. The functional currency of the Company is the U.S. dollar. If we incur portions of our expenses and derive
revenues in currencies other than the U.S. dollar, we may be exposed to foreign currency exchange risk. Foreign exchange risk
exposure may also arise from intra-company transactions and financing with subsidiaries that have a functional currency
different than the U.S. dollar.
Transactions in currencies other than the
functional currency of the Company entities are recorded at the exchange rates prevailing at the dates of the related transactions.
Foreign exchange gains and losses resulting from the settlement of such transactions, as well as from the translation at year-end
exchange rates of monetary assets and liabilities denominated in foreign currencies, are recognized in the consolidated statements
of operations and comprehensive loss. At each balance sheet date, monetary assets and liabilities that are denominated in foreign
currencies are translated to the respective functional currencies of the Company’s entities at the rates prevailing on the
relevant balance sheet date.
The resulting translation adjustments are
included in equity under the caption “Currency Translation Adjustment” in the consolidated statement of changes in
(deficit)/equity.
Foreign Exchange
A substantial portion of our net sales
is denominated in Euros. As a result, changes in the relative values of U.S. Dollars and Euros affect our reported levels of net
sales and profitability as the results are translated into U.S. Dollars for reporting purposes. In particular, decreases in the
value of the U.S. Dollar relative to the value of the positively impact our levels of revenue and profitability because the
translation of a certain number of Euros into U.S. Dollars for financial reporting purposes will represent more U.S. Dollars than
it would have prior to the relative decrease in the value of the U.S. Dollar. Conversely, a decline in the value of the Euro will
result in a lower number of U.S. Dollars for financial reporting purposes.
During the year ended December 31,
2016, we conducted business in several foreign currencies. The following table provides the average exchange rate for the year
ended December 31, 2016 and the year ended December 31, 2015 of the U.S. Dollar against the foreign currency in
which we conduct the largest portion of our operations.
Currency
|
|
Average
exchange rate of the
U.S. Dollar in the year
December 31, 2016
|
|
Average
exchange rate of the
U.S. Dollar in the year
December 31, 2015
|
Euro
|
|
$1.11
= 1 Euro
|
|
$1.11
= 1 Euro
|
For
the year ended December 31, 2016, approximately
99
% of our
sales, and 24% of our costs were incurred, in Euros.
To mitigate the risk of transactions in
which a sale is made in one currency and associated costs are denominated in a different currency, we may in the future utilize
forward currency contracts in certain circumstances to lock in exchange rates with the objective that the gain or loss on the
forward contracts will approximate the loss or gain that results from the transaction or transactions being hedged. We may also
determine whether to enter into hedging arrangements in the future based upon the size of the underlying transaction or transactions,
an assessment of the risk of adverse movements in the applicable currencies and the availability of a cost effective hedge strategy.
As we currently do not engage in hedging, changes in the relative value of currencies can affect our profitability.
Financial Operations Overview
Revenues
In the years ended December 31, 2016, 2015
and 2014, our revenue was derived primarily from the supply of CollaGUARD, CollatampG and Septocoll, our products manufactured
by us and sold by our commercial partners. Supply revenue is derived from a contractual supply price paid to us by our commercial
partners. In the case of some of our distribution agreements, including for the sale of CollatampG, the supply price is a contractually
agreed percentage of the net sales price received by our distribution partner, which is net of discounts, returns, and allowances
incurred. In this case, revenue is recognized in two parts: the first amount is recognized for the manufacture and sale of the
product at the point of sale, and the final amount is added or deducted when the product is sold by the distributor based upon
the net sale price achieved.
Accordingly, the primary factors that determine
our revenues derived from our products are:
|
·
|
the level of
orders submitted by our commercial partners;
|
|
·
|
the level of
prescription and institutional demand for our products;
|
|
·
|
the amount
of gross-to-net sales adjustments realized by our commercial partners.
|
The following table sets forth a summary
of our revenues by product for the years ended December 31, 2016, 2015 and 2014. The reasons for the increase in revenues in the
years ended December 31, 2016 as compared to December 31, 2015 and the decrease in revenues in the year ended December 31, 2015
are more fully described in “—Results of Operations”:
|
|
Year
Ended
December
31,
|
|
|
Increase/
|
|
|
%
Increase/
|
|
|
Year
Ended December 31,
|
|
|
Increase/
|
|
|
%
Increase/
|
|
|
|
2016
|
|
|
2015
|
|
|
(Decrease)
|
|
|
(Decrease)
|
|
|
2015
|
|
|
2014
|
|
|
(Decrease)
|
|
|
(Decrease)
|
|
|
|
(USD in thousands)
|
|
|
|
|
|
|
|
|
(USD in thousands)
|
|
|
|
|
|
|
|
CollaGUARD
|
|
$
|
118
|
|
|
$
|
3
|
|
|
$
|
115
|
|
|
|
3,833.3
|
%
|
|
$
|
3
|
|
|
$
|
464
|
|
|
$
|
(461
|
)
|
|
|
(99.4
|
)%
|
CollatampG
|
|
|
3,785
|
|
|
|
2,491
|
|
|
|
1,294
|
|
|
|
52.0
|
%
|
|
|
2,491
|
|
|
|
4,733
|
|
|
|
(2,242
|
)
|
|
|
(47.4
|
)%
|
Septocoll
|
|
|
429
|
|
|
|
329
|
|
|
|
100
|
|
|
|
30.4
|
%
|
|
|
329
|
|
|
|
685
|
|
|
|
(356
|
)
|
|
|
(52.0
|
)%
|
Other
(1)
|
|
|
40
|
|
|
|
47
|
|
|
|
(7
|
)
|
|
|
(14.9
|
)%
|
|
|
47
|
|
|
|
92
|
|
|
|
(45
|
)
|
|
|
(48.9
|
)%
|
Total
|
|
$
|
4,372
|
|
|
$
|
2,870
|
|
|
$
|
1,502
|
|
|
|
52.3
|
%
|
|
$
|
2,870
|
|
|
$
|
5,974
|
|
|
$
|
(3,104
|
)
|
|
|
(52.0
|
)%
|
Cost of Sales
Cost of sales consists of the costs associated
with producing our products for our commercial partners. In particular, our cost of sales includes:
|
·
|
manufacturing
overhead and fixed costs associated with running our manufacturing facilities in Saal,
Germany, including salaries and related costs of personnel involved with our manufacturing
activities;
|
|
·
|
packaging,
testing, freight and shipping; and
|
|
·
|
the cost of
raw materials and active pharmaceutical ingredients.
|
All overhead costs associated with operating
the manufacturing facility are included in the standard cost of our products as indirect costs and charged to cost of revenue
based on sales volume.
Gross margins from supply revenue were
(60%), (86%) and (24%) for the years ended December 31, 2016, 2015 and 2014, respectively. Our negative margin is primarily due
to absorbing full indirect costs into the standard cost of our products. The amount of indirect costs included in cost of sales
was $2.3 million, $1.6 million and $2.9 million for the years ended December 31, 2016, 2015 and 2014, respectively. Excluding
these indirect costs, gross margins from supply revenue were (7%), (30%) and 25% for the years ended December 31, 2016, 2015 and
2014, respectively.
As we increase production with the launch
of new products, our indirect costs included in cost of sales will remain relatively fixed and therefore will decrease as a proportion
of sales. Our direct costs consist primarily of labor associated with our batch production processes, quality control and manual
packaging. In our expanded facility we will produce larger batch sizes and further automate our production and packaging processes,
resulting in decreased labor costs per unit produced. Accordingly, our gross margins are expected to increase significantly with
growth in product sales and expanded production capacity.
Research and Development Expenses
Our research and development expenses consist
of expenses incurred in developing, testing, manufacturing and seeking regulatory approval of our product candidates, including:
|
·
|
expenses associated
with regulatory submissions, clinical trials and manufacturing, including additional
expenses to prepare for the commercial manufacture of XaraColl and CollaGUARD, such as
the hiring and training of additional personnel;
|
|
·
|
payments to
third-party contract research organizations, contract laboratories and independent contractors;
|
|
·
|
payments made
to regulatory consultants;
|
|
·
|
payments made
to third-party investigators who perform clinical research on our behalf and clinical
sites where such testing is conducted;
|
|
·
|
personnel related
expenses, such as salaries, benefits, travel and other related expenses, including share-based
compensation;
|
|
·
|
expenses incurred
to maintain regulatory licenses, patents and trademarks; and
|
|
·
|
facility, maintenance,
and allocated rent, utilities, and depreciation and amortization, and other related expenses.
|
Clinical trial expenses for our product
candidates are a significant component of our research and development expenses. Product candidates in late-stage clinical development,
such as XaraColl and CollaGUARD, generally have higher research and development expenses than those in earlier stages of development,
primarily due to the increased size and duration of the clinical trials. We coordinate clinical trials through a number of contracted
investigational sites and recognize the associated expense based on a number of factors, including actual and estimated subject
enrollment and visits, direct pass-through costs and other clinical site fees.
From January 1, 2004 through December 31,
2016, we incurred research and development expenses of $121.2 million net of contributions and collaboration agreements with third
parties. We incurred average research and development expenses of $38.7 million, $29.8 million and $4.3 million for the years
ended December 31, 2016, 2015 and 2014, respectively, because substantially all of our Phase 3 clinical trials for Cogenzia and
Xaracoll occurred from the fourth quarter of 2014 to the fourth quarter of 2016.
General and Administrative Expenses
General and administrative expenses consist
primarily of salaries, benefits and other related costs, including share-based compensation, for personnel serving in our executive,
finance, business development, clinical and regulatory and administrative functions. Our general and administrative expenses also
include facility and related costs not included in research and development expenses and cost of revenues, professional fees for
legal, consulting, tax and accounting services, insurance, depreciation and general corporate expenses.
We incurred general and administrative
expenses of $25.4 million, $19.7 million and $15.6 million for the years ended December 31, 2016, 2015 and 2014, respectively.
General and administrative expenses in the year ended December 31, 2016 included $8.5 million in non-cash charges for share-based
compensation, compared to $4.0 million of such charges in the corresponding period in 2015 and $6.9 million in 2014. Excluding
share-based compensation, our general and administrative expenses for the year ended December 31, 2016 were $16.9 million, compared
to $15.8 million and $8.7 million for the years ended December 31, 2015 and 2014, respectively. The increase in general and administrative
expenses, excluding share-based compensation, was primarily due to our continued infrastructure build-out to support clinical
programs, initiation of our pre-commercialization investment and expenses related to our re-domiciliation to Ireland.
Other Income/(Expense)
Other income/(expense) consists of
fair value gains/(losses) on warrants outstanding and foreign exchange gains. Other income in the year ended December 31,
2016 consisted primarily of fair value gains on warrants outstanding and foreign exchange gains. Other income for the year
ended December 31, 2015 consisted primarily of foreign exchange gains partially offset by fair value losses on
warrants outstanding. Other expense for the year ended December 31, 2014 consisted primarily of fair value losses on
warrants outstanding partially offset by foreign exchange gains. We incurred other income/(expense) of $12.2 million, $1.6
million and ($2.0) million for the years ended December 31, 2016, 2015 and 2014 respectively.
Loss
per Share
The weighted-average number of Innocoll
Holdings plc ordinary shares (denominator – basic) was 26,867,343 at December 31, 2016, 22,328,908 at December 31, 2015
and 9,744,255 at December 31, 2014. The weighted-average number of historic ordinary shares for December 31, 2015 and December
31, 2014 have been adjusted for the effects of
the re-domicile of our then parent company. The weighted-average
number of ordinary shares of Innocoll Holdings plc outstanding during the period and for all periods presented is adjusted for
events, other than the conversion of potential ordinary shares of Innocoll Holdings plc, that have resulted in a change of the
number of ordinary shares of Innocoll Holdings plc outstanding without a corresponding change in resources.
|
|
For
the Year Ended December 31,
|
|
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
|
|
(in thousands, except for per
share data)
|
|
Numerator:
|
|
|
|
|
|
|
|
|
|
|
|
|
Net loss – basic & diluted
|
|
$
|
(56,954
|
)
|
|
$
|
(50,856
|
)
|
|
$
|
(23,471
|
)
|
Denominator - number of shares:
|
|
|
|
|
|
|
|
|
|
|
|
|
Weighted-average shares outstanding – basic & diluted
|
|
|
26,867,343
|
|
|
|
22,328,908
|
|
|
|
9,744,255
|
|
Loss per share:
|
|
|
|
|
|
|
|
|
|
|
|
|
Basic & diluted
|
|
|
(2.12
|
)
|
|
|
(2.28
|
)
|
|
|
(2.41
|
)
|
The basic & diluted loss per share
of Innocoll Holdings plc for the year ended December 31, 2016 was (S2.12) (2015: ($2.28) and 2014: $2.83). For the purpose of
calculating diluted loss per share for 2016, 2015 and 2014 the potentially exercisable instruments in issue would have the effect
of being antidilutive and, as such, the diluted loss per share is the same as the basic loss per share for those periods.
Critical Accounting Policies and Use of Estimates
We have based our management’s discussion
and analysis of financial condition and results of operations on our financial statements that have been prepared in accordance
with U.S. generally accepted accounting principles (GAAP) . The preparation of these financial statements requires us to make
estimates that affect the reported amounts of assets and liabilities and the disclosure of contingent assets and liabilities at
the date of the financial statements as well as the reported revenues and expenses during the reporting periods. On an ongoing
basis, we evaluate our estimates and judgments. We base our estimates on historical experience and on various other factors we
believe to be appropriate under the circumstances. Actual results may differ from these estimates under different assumptions
or conditions.
While our significant accounting policies
are more fully discussed in note 1 to our consolidated financial statements included in this annual report, we believe that the
following accounting policies are critical to the process of making significant judgments and estimates in the preparation of
our financial statements. We have reviewed these critical accounting policies and estimates with the audit committee of our board:
Revenue recognition
Significant management judgments and estimates must be made
and used in connection with the recognition of revenue in each accounting period. Material differences in the amount of revenue
in any given period may arise if these judgments or estimates prove to be incorrect or if management’s estimates change
on the basis of development of the business or market conditions. To date there have been no material differences arising from
these judgments and estimates.
Revenue from products is generally recorded as of the date
of shipment, consistent with our typical shipment terms. Where the shipment terms do not permit revenue to be recognized as of
the date of shipment, revenue is recognized when the group has satisfied all of its obligations to the customer in accordance
with the shipping terms. Revenue is recognized to the extent that it is probable that economic benefit will flow to the group,
that the risks and rewards of ownership have passed to the buyer and the revenue can be measured. No revenue is recognized if
there is uncertainty regarding recovery of the consideration due at the outset of the transaction or the possible return of goods.
Revenue is recognized from milestone payments received under
collaboration agreements when earned, provided that the milestone event is substantive, its achievability was not reasonably assured
at the inception of the agreement, the group has no further performance obligations relating to the event, and collectability
is reasonably assured. If these
criteria are not met, the group recognizes milestone payments
ratably over the remaining period of their performance obligations under the collaboration agreement.
Share-Based Payments
Share-based compensation expense related
to share-based awards granted to employees is measured at the date of grant based on the estimated fair value of the award, net
of estimated forfeitures. The charge to comprehensive income in relation to share based payments in the years ending December
31, 2016, 2015 and 2014 were $8.5 million, $4.0 million and $6.9 million, respectively. With respect to any future share-based
awards, the company plans to re-evaluate each of the fair value assumptions, and revise them as appropriate, on an ongoing basis.
We have granted restricted share, phantom share and option awards to members of our historic supervisory and management boards,
and employees as follows:
January/March 2014 Grants
Under the 2014 restricted share awards,
Innocoll GmbH granted to members of its advisory board, management board and group employees a total of 47,840 restricted shares
and 63,256 phantom shares. The total restricted shares and phantom shares represented 12.2% of the diluted share capital of Innocoll
GmbH at the time of grant, excluding issued and outstanding options to acquire ordinary shares. Innocoll Germany further created
an authorized capital of 22,724 ordinary shares as part of its Authorized Capital II with the intention to grant options to acquire
ordinary shares to certain members of Innocoll Germany’s advisory board, management board and employees, and these options
were subsequently granted in December 2014 (see “—Management Options”). The restricted shares were issued in
exchange for payment of nominal value of €47,840. The phantom shares may be either settled in cash or a new issue of shares,
at our option, on the date on which the repurchase right lapses. For purposes of valuing the share-based payment in relation to
the restricted share and phantom share grants, management performed the valuation with the assistance of a well-recognized independent
third-party valuation consultant, which valued all classes of shares fully diluted for the issue of the restricted shares and
phantom shares and options, on a pro-forma basis. The share-based payments will be recognized over a one-year period.
May 2014 Grants
Pursuant to a notarial deed entered into
on May 22, 2014, Innocoll GmbH granted to new and existing members of its supervisory board, management board and group employees
a total of 43,596 restricted shares, 9,113 phantom shares and 869 unrestricted shares to a former member of our supervisory board
(the “May 2014 Grant”). The total restricted shares and phantom shares issued pursuant to the May 2014 grant represented
5.1% of the diluted share capital of Innocoll GmbH at the time of grant, excluding issued and outstanding options to acquire ordinary
shares. Innocoll Germany further created an authorized capital of 2,060 ordinary shares as part of its Authorized Capital II with
the intention to grant options to acquire ordinary shares to certain members of Innocoll Germany’s advisory board, management
board and employees which options were subsequently granted in December 2014 (see “—Management Options”). The
restricted shares were issued in exchange for payment of nominal value of €43,596. The phantom shares may be either settled
in cash or a new issue of shares, at our option, on the date in which the repurchase right lapses. The May 2014 Grant occurred
simultaneously with a new issue of series E preferred shares. The series E preferred shares were purchased in an arms-length transaction
by existing investors, new supervisory board members who also received restricted stock grants, and three new investors who are
partners of one of the existing shareholders. The pricing of the series E preferred shares at €112.52 per share was based
upon our managing directors’ and our advisory board’s estimate, with the assistance of a third-party specialist, who
concluded that the price of Innocoll Germany’s ADS in an anticipated initial public offering would be at least equal to
such price or higher. To obtain the series E financing, it was necessary to give the investors anti-dilution rights in the event
the initial public offering would be priced at a discount to the expected valuation. As a result of the initial public offering
price of Innocoll Germany’s ADSs of $9.00 per ADS, and the anti-dilution rights granted to the series E preferred
investors, such investors have been issued additional shares of Innocoll Germany at €1.00 per share, as a result of which
their weighted-average purchase price is equal to €73.76 per share, a 16.7% discount to the effective value per ordinary
share of Innocoll Germany in our initial public offering. There were no significant valuation events at the company between
the May 2014 Grant date and date of our initial public offering in July 2014. Therefore, we have used the Series E preferred share
adjusted weighted-average purchase price of €73.76 per
share as the value for the share-based payment charge arising
out of the May 2014 Grant. The share-based payments will be recognized over a one to three year period as set out above.
July 2014, January 2015 Amendments and Restatements
In July 2014, after the transformation
of Innocoll GmbH into Innocoll AG, each of the restricted shares and phantom share awards issued in January 2014 and May 2014
were combined and applied to ordinary shares of Innocoll AG pursuant to amended and restated award agreements entered into with
Innocoll AG. In January 2015, the phantom share award agreements were each amended and restated to provide for the definition
of Exit Event triggering the lapse of the repurchase right by us to be extended to any trading day within the period beginning
on the third trading day after the publication of our quarterly reports for the fourth quarter 2014, and the ending on the trading
day immediately preceding the first trading day that is two weeks prior to the end of the first quarter 2015, which may be designated
by the company’s management board in its sole discretion. There was no impact to the 2014 or 2015 financial statements as
a result of this transaction.
Restricted Stock and Phantom Stock Valuations
The estimated fair market value of the
shares issued pursuant to, and underlying the January 2014 grant and May 2014 grant, was determined at the grant date by our historic
supervisory board and was deemed appropriate for the valuation of the grants pursuant to ASC 718.
The estimated fair value of the shares
as of each grant date are based on numerous objective and subjective factors, combined with management’s judgment, including
the following:
|
·
|
the assistance
of a well-recognized independent third-party valuation consultant in valuing our ordinary
shares and series A through D-2 preferred shares, originally issued as of June 30, 2013
in connection with the re-domicile of our parent company, and updated as of December
31, 2013;
|
|
·
|
the estimated
likelihood of achieving a liquidity event for our shares, such as an initial public offering
or an acquisition of our company, given prevailing market conditions and other contingencies
affecting the probability or potential timing of such an event;
|
|
·
|
the prices
at which we sold series D preferred shares in arms-length transactions in October 2013
and November 2013 and the terms of the series D preferred shares relative to the terms
of our series A, series B, series C and series D-2 preferred shares and ordinary shares;
|
|
·
|
the price at
which we sold our shares of series E preferred shares in an arms-length transaction in
May 2014 and the terms of the series E preferred shares relative to the terms of our
series A, series B, series C, series D and series D-2 preferred shares and ordinary shares,
as well as the near term probability that all preferred shares would be converted into
ordinary shares pursuant to our planned transformation into Innocoll AG in connection
with our initial public offering;
|
|
·
|
the subsequent
issue of anti-dilution shares to holders of series E preferred and ordinary shares as
result of the initial public offering price of Innocoll Germany ADS of $9.00 per ADS;
and
|
|
·
|
the fact that,
at the time of the restricted share and phantom share grants, our shares were illiquid
securities of a private company.
|
Management performed the valuation of our
ordinary shares and series A through D-2 preferred shares in the January/March 2014 grant with the assistance of a well-recognized
independent third-party valuation consultant.
Valuation Approaches
Management, with the assistance of an independent
third-party valuation consultant, considered several valuation approaches as follows: (1) Cost Approach; (2) Market Approach (including
both the Guideline Public
Company (“GPC”) method and the Guideline Merged
and Acquired Company (“GMAC”) method); (3) Income Approach; (4) Current Value Method; (5) Probability Weighted Expected
Return Method; (6) Option-Pricing Method; and (7) Back-Solve Method.
Management, with the assistance of an independent
third-party valuation consultant, relied upon the income approach to determine the range of fair market value of equity of our
company. Because our value is attributable to our business operations, rather than the assets we hold, management, with the assistance
of the independent third-party valuation consultant, did not rely upon the cost approach in its conclusion of the range of the
fair market value of our equity. Management, with the assistance of the independent third-party valuation consultant, also did
not believe that the multiples of established publicly-traded companies provided reliable indicators of value given that we are
relatively early-stage; therefore, they considered, but ultimately did not rely on the GPC method. They also considered, but ultimately
did not rely on the GMAC method due to the lack of comparable transactions. As a corroborative approach, they utilized the Back-Solve
Method to estimate our implied equity value as derived from the Option-Pricing Method, based on the most recent round of financing
of the series D preferred shares.
Factors contributing to differences between grant date estimated
fair values and the initial public offering price
We believe that the following factors,
along with those set forth above with respect to each of the grants, explain the difference between the grant date estimated fair
values of our shares on those grant dates and the initial public offering price of $9.00 per ADS of Innocoll Germany.
|
·
|
In January
2014, we knew the initial public offering was a possibility but we were also considering
other funding alternatives including the licensing of our products. As an independent
third-party valuation was produced in connection with the re-domicile of our parent company
in June 2013, updated to December 2013, it was determined that this valuation was a more
reasonable estimate of the value than any potential initial public offering price which
was far from certain and a potential liquidity event more distant.
|
|
·
|
The U.S. markets
affecting companies in our industry experienced a significant increase in activities
with accompanying increased market multiples and valuations.
|
|
·
|
In March 2014,
the board determined to proceed with the initial public offering, and the underwriters
were subsequently consulted as to the terms of the series E preferred financing, and
advised that the valuation and anti-dilution terms reflected a reasonable discount to
the expected initial public offering price.
|
|
·
|
Simultaneous
with the May 2014 grant, we added to our historic supervisory board three prominent and
experienced pharmaceutical and business executives: Jonathan Symonds, CBE, David R. Brennan
and Shumeet Banerji, Ph.D. This significantly enhanced the value and profile of our company
from an investor perspective and was instrumental in bringing new investors into the
series E preferred funding round.
|
|
·
|
In June 2014,
our pipeline product Cogenzia for the treatment of diabetic foot infections was approved
in Canada, which was earlier than expected.
|
|
·
|
Subsequent
to the confidential submission of our registration statement to the U.S. Securities and
Exchange Commission on March 26, 2014, we engaged in discussions with potential investors
in reliance on Section 5(d) of the Securities Act of 1933, as amended. In connection
with such testing the waters meetings, we received positive feedback from potential investors
which caused management to increase its expectations regarding the anticipated price
range of an initial public offering of Innocoll Germany’s ordinary shares.
|
|
·
|
The ADSs of
Innocoll Germany issued in the initial public offering were freely tradable in a public
market, whereas the estimated fair value of the shares as of all of grant dates described
above represents a contemporaneous estimate of the fair value of shares that were then
illiquid, might never
|
become liquid and, even if an initial public offering
were successfully completed, would remain illiquid at least until the expiration of the 180-day lockup period following the initial
public offering. This illiquidity also accounts for a substantial difference between the estimated fair values of the shares from
January 2014 and the initial public offering price.
|
·
|
The holders
of preferred shares enjoyed substantial economic rights and preferences over the holders
of Innocoll Germany’s ordinary shares, including the right to receive dividends
prior to any dividends declared or paid on any shares of Innocoll Germany’s ordinary
shares and liquidation payments in preference to holders of ordinary shares. The initial
public offering price was determined after the conversion of all of our convertible preferred
shares prior to the completion of our initial public offering. The corresponding elimination
of the preferences and rights enjoyed by the holders of such preferred shares results
in a higher valuation.
|
|
·
|
The successful
completion of an initial public offering would strengthen our balance sheet, provide
access to public equity and debt markets and provide a “currency” of publicly
tradable securities to enable us to make strategic acquisitions as our historic supervisory
board may deem appropriate, providing enhanced operational flexibility.
|
Management Options
In December 2014, the company entered into
option agreements with members of its management board and group employees which memorialized options previously promised to them
as consideration for past services. Pursuant to the terms of the Management Option Agreements, the members of the management board
and group employees have the right to subscribe for 24,784 ordinary shares of Innocoll Germany at an exercise price of $119.25
per ordinary share of Innocoll Germany (equivalent to $9.00 per ADS of Innocoll Germany), which rights are exercisable through
June 15, 2019, subject to certain black-out periods and which price is subject to adjustment in accordance with the Merger. Throughout
2015, the company entered into option agreements with members of its management board and group employees. Pursuant to the terms
of the Management Option Agreements, the members of the management board and group employees have the right to subscribe for 86,144
ordinary shares of Innocoll Germany at exercise prices ranging from $99.38 to $195.70 per ordinary share of Innocoll Germany (equivalent
to from $7.50 to $14.77 per ADS of Innocoll Germany), which rights are exercisable for a ten year period from date of grant, subject
to certain black-out periods and which price is subject to adjustment in accordance with the Merger. In January, 2014, the company
created an authorized capital to cover, among other issuances, the required share issuances under the Management Option Agreements.
On June 15, 2019, any unexercised options expire pursuant to the terms of the Management Option Agreements, unless the shareholders
approve the creation of a new authorized capital for an additional five-year period.
Throughout 2016 the company entered into
option agreements with members of it’s board and group employees. Pursuant to the terms of the Option Agreements the members
of the board and group employees have the right to subscribe for an aggregate of 1,372,359 ordinary shares on Innocoll
Holdings plc at exercise prices ranging from $5.40 to $8.80 per ordinary share of Innocoll Holdings plc which rights are exercisable
for a ten year period from date of grant, subject to certain black-out periods.
The share based payments cost of the options
was calculated using a Black Scholes model. The following input assumptions were used to value the options:
|
|
For the Year-Ended December 31,
|
|
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Expected stock option life (years)
|
|
|
9.36
|
|
|
|
8.74
|
|
|
|
4.52
|
|
Expected volatility
|
|
|
66.52
|
%
|
|
|
66.77
|
%
|
|
|
69.68
|
%
|
Risk-free interest rate
|
|
|
1.92
|
%
|
|
|
2.03
|
%
|
|
|
1.66
|
%
|
Exercise price
|
|
$
|
9.46
|
|
|
$
|
10.65
|
|
|
$
|
9.00
|
|
Valuation of financial instruments
The group issued financial instruments
during the relevant accounting periods and had financial instruments in issue at both accounting period ends. In conformity with
U.S. GAAP, the group initially measured these financial instruments at their fair value and thereafter at fair
value through the profit or loss if designated as such upon initial recognition. In order to value these various instruments,
the group (and the experts engaged by the group to provide such valuations where applicable) made assumptions and estimates concerning
variables such as future cashflows, discount rates, expected volatility, risk free rate and type of valuation models used. The
assumptions of future outcomes, and other sources of estimation uncertainty concerning the determination of key inputs to the
valuation models, are based on management’s (and relevant experts’) best assessment using the knowledge available,
their historical experiences as well as other factors that are considered to be relevant. The estimates and assumptions are reviewed
on an ongoing basis.
Taxation
Given the global nature of the business
and the multiple taxing jurisdictions in which the group operates, the determination of the group’s provision for income
taxes requires significant judgments and estimates, the ultimate tax outcome of which may not be certain. Although estimates are
believed to be reasonable, the final outcome of these matters may be different than those reflected in the historical income tax
provisions and accruals. Such differences could have a material effect on the income tax provision and results in the period during
which such determination is made.
Deferred tax assets and liabilities are
determined using enacted tax rates for the effects of net operating losses and temporary differences between the book and tax
bases of assets and liabilities. In assessing the reliability of deferred tax assets, management considers whether it is more
likely than not that some portion or all of the deferred tax assets will not be realized. The ultimate realization of deferred
tax assets is dependent upon the generation of future taxable income during the periods in which those temporary differences become
deductible. While management considers the scheduled reversal of deferred tax liabilities, and projected future taxable income
in making this assessment, there can be no assurance that these deferred tax assets may be realizable.
In addition, the group may also be subject
to audits in the multiple taxing jurisdictions in which it operates. These audits can involve complex issues which may require
an extended period of time for resolution. Management believes that adequate provisions for income taxes have been made in the
financial statements.
Allowance for slow-moving and obsolete inventory
The group evaluates the realizability of
their inventory on a case-by-case basis and makes adjustments to the inventory provision based on their estimates of expected
losses. The group writes off any inventory that is approaching its “use-by” date and for which no further re-processing
can be performed. The group also considers recent trends in revenues for various inventory items and instances where the realizable
value of inventory is likely to be less than its carrying value. Due to the fact that the allowance is calculated on the basis
of the actual inventory on hand at the particular balance sheet date, there were no material changes in estimates made during
the years ended December 31, 2016, 2015 or 2014 which would have had an impact on the carrying values of inventory during those
periods.
Trade receivables
The group evaluates customer accounts with
past-due outstanding balances or specific accounts for which it has information that the customer may be unable to meet its financial
obligations. Based upon a review of these accounts and management’s analysis and judgment, the group estimates the future
cash flows expected to be recovered from these receivables. The amount of the impairment on doubtful receivables is measured individually
and recorded as a specific allowance against that customer’s receivable balance to the amount expected to be recovered.
The allowance is re-evaluated and adjusted periodically as additional information is received.
Contingencies
Contingencies are recognized and measured
on the basis of the estimate and probability of future outflows of resources embodying benefits, as well as on the basis of experiential
values and the circumstances known at the end of the reporting period. Assumptions also are made as to the probabilities whether
and within what ranges the provisions may be used. The assessment of whether a present obligation exists is generally based on
assessment of internal experts. Estimates can change on the basis of new information and the actual charges may affect the performance
and financial position of the group.
JOBS Act
As a company with less than $1.0 billion
in revenues for our fiscal year ended December 31, 2016, we qualify as an “emerging growth company” as defined
in Section 2(a) of the U.S. Securities Act of 1933, as amended, or the Securities Act, as modified by the Jumpstart Our Business
Startups Act, or the JOBS Act, which was enacted in 2012. An emerging growth company may take advantage of exemptions from various
reporting requirements that are applicable to other public companies that are not emerging growth companies, including, but not
limited to:
|
·
|
not being required
to comply with the auditor attestation requirements of Section 404 of the Sarbanes-Oxley
Act of 2002, or the Sarbanes-Oxley Act;
|
|
·
|
reduced disclosure
obligations regarding executive compensation; and
|
|
·
|
not being required
to comply with any requirement that may be adopted by the Public Company Accounting Oversight
Board regarding mandatory audit firm rotation or a supplement to the auditor’s
report providing additional information about the audit and the financial statements.
|
We may choose to take advantage of some
or all of the available exemptions and have taken advantage of some of these exemptions in this annual report. Accordingly, the
information contained herein may be different from the information you receive from other public companies in which you hold shares.
We do not know if some investors will find our ordinary shares less attractive as a result of our utilization of these or other
exemptions. The result may be a less active trading market for our ordinary shares and increased volatility in the price of our
ordinary shares.
In addition, Section 107 of the JOBS
Act provides that an emerging growth company can take advantage of the extended transition period provided in Section
7(a)(2)(B) of the Securities Act for complying with new or revised accounting standards. In other words, an emerging growth
company can delay the adoption of certain accounting standards until those standards would otherwise apply to private
companies. Innocoll intends to take advantage of this extended transition period.
We will remain an emerging growth company
until the earliest of (a) the last day of our fiscal year during which we had total annual gross revenues of at least $1.0 billion;
(b) December 31, 2019, the last day of our fiscal year following the fifth anniversary of the date of the first sale of Innocoll
Germany’s ADSs in our 2014 initial public offering; (c) the date on which we have, during the previous three-year period,
issued more than $1.0 billion in non-convertible debt; or (d) the date on which we are deemed to be a “large accelerated
filer” under the Securities Exchange Act of 1934, as amended, or the Exchange Act, which would occur if the market value
of our shares that are held by non-affiliates exceeds $700 million as of the last business day of our most recently completed
second fiscal quarter and we have been publicly reporting for at least 12 months. Once we cease to be an emerging growth company,
we will not be entitled to the exemptions provided to emerging growth companies in the JOBS Act.
Results of Operations
Comparison of Years Ended December 31, 2016 and 2015
|
|
Year
Ended December 31,
|
|
|
Increase/
|
|
|
%Increase/
|
|
|
|
2016
|
|
|
2015
|
|
|
(Decrease)
|
|
|
(Decrease)
|
|
|
|
(in thousands)
|
|
|
|
|
Revenue
|
|
$
|
4,372
|
|
|
$
|
2,870
|
|
|
$
|
1,502
|
|
|
|
52.3
|
%
|
Cost of sales
|
|
|
(6,986
|
)
|
|
|
(5,328
|
)
|
|
|
1,658
|
|
|
|
31.1
|
%
|
Research and development expenses
|
|
|
(38,715
|
)
|
|
|
(29,821
|
)
|
|
|
8,894
|
|
|
|
29.8
|
%
|
General and administrative expenses
|
|
|
(25,446
|
)
|
|
|
(19,743
|
)
|
|
|
5,703
|
|
|
|
28.9
|
%
|
Loss on disposal of property, plant & equipment expense
|
|
|
(8
|
)
|
|
|
-
|
|
|
|
8
|
|
|
|
100.0
|
%
|
Other operating expenses
|
|
|
(1
|
)
|
|
|
-
|
|
|
|
1
|
|
|
|
100.0
|
%
|
Interest income
|
|
|
35
|
|
|
|
232
|
|
|
|
(197
|
)
|
|
|
(84.9
|
)%
|
Interest expense
|
|
|
(2,221
|
)
|
|
|
(223
|
)
|
|
|
1,998
|
|
|
|
896.0
|
%
|
Other income
|
|
|
12,187
|
|
|
|
1,564
|
|
|
|
10,623
|
|
|
|
679.2
|
%
|
Revenue
. Revenues for the year ended
December 31, 2016 were 52.3% higher at $4.4 million, compared to $2.9 million for year ended December 31, 2015. This increase
was primarily due to an increase in sales to EUSA Pharma of CollatampG, our gentamicin implant for the treatment and prevention
of post-surgical infection, of $1.3 million, or 52.0%. Revenue from the sales of Septocoll increased 30.4%.
Cost of Sales
. Cost of sales
of $7.0 million in the year ended December 31, 2016 increased by $1.7 million, or 31.1%, compared to $5.3 million in the year
ended December 31, 2015. Gross margins from supply revenue were (60)% and (86)% for the year ended December 31, 2016 and
2015, respectively. All overhead costs associated with operating our manufacturing facility are included in the standard cost
of our products as indirect costs and charged to cost of sales based on sales volume. Excluding such indirect costs, gross
margins from supply revenue were (7)% and (30%) for the years ended December 31, 2016 and 2015 respectively.
Research and Development (R&D) Expenses
.
R&D expenses were $38.7 million for the year ended December 2016 as compared to $29.8 million for the year ended December
31, 2015, a 29.8% increase. R&D expenses in each year consisted of external clinical research costs as well as costs of internal
research and development personnel and internal laboratory costs at our Saal, Germany facility. In the year ended December 31,
2016, external clinical research costs were $34.8 million in the year ended December 31, 2016 compared to $26.4 million external
clinical research costs in the year ended December 31, 2015, the increase was primarily due to ramp-up and completion of both
our Phase 3 XaraColl efficacy trials and our Phase 3 Cogenzia efficacy trials. From January 1, 2004 through December 31,
2016, we incurred research and development expenses of $121.2 million net of contributions and collaboration agreements with third
parties.
General and Administrative
(G&A) Expenses
. G&A expenses were $25.4 million for the year ended December 31, 2016 as compared to $19.7 million
for the year ended December 31, 2015, an increase of 28.9%. G&A expenses in the year ended December 31, 2016 included $8.5
million in non-cash charges for share-based compensation, compared to $4.0 million of such charges in the corresponding period
in 2015. Excluding such charges for share-based compensation, G&A expenses were $16.9 million for the year ended December
31, 2016 as compared to $15.8 million for the year ended December 31, 2015. The increase in G&A, excluding share-based compensation,
was primarily due to $2.2 million of one-off expenses related to the re-domiciliation of the company to Ireland, our continued
infrastructure to support clinical programs, and some pre-commercialization investment.
Interest Expense
: Interest
expense was $2.2 million in the year ended December 31, 2016 compared to $0.2 million in the year ended December 31,
2015, an 896.0% increase. Interest expense in the year ended December 31, 2016 and 2015 consisted primarily of
non-cash interest charges.
Other Income:
Other income
was $12.2 million in the year ended December 31, 2016 compared to $1.6 million in the year ended December 31, 2015, a
679.2% increase. Other income in the year ended December 31, 2016 consisted primarily of fair value gain on warrants
outstanding and foreign exchange gains. Other income in the year ended December 31, 2015 consisted primarily of foreign
exchange gains partially offset by fair value loss on warrants outstanding.
Comparison of Years Ended December 31, 2015 and 2014
|
|
Year
Ended December 31,
|
|
|
Increase/
|
|
|
%Increase/
|
|
|
|
2015
|
|
|
2014
|
|
|
(Decrease)
|
|
|
(Decrease)
|
|
|
|
(in thousands)
|
|
|
|
|
Revenue
|
|
$
|
2,870
|
|
|
$
|
5,974
|
|
|
$
|
(3,104
|
)
|
|
|
(52.0
|
)%
|
Cost of sales
|
|
|
(5,328
|
)
|
|
|
(7,404
|
)
|
|
|
(2,076
|
)
|
|
|
(28.0
|
)%
|
Research and development expenses
|
|
|
(29,821
|
)
|
|
|
(4,320
|
)
|
|
|
25,501
|
|
|
|
590.3
|
%
|
General and administrative expenses
|
|
|
(19,743
|
)
|
|
|
(15,611
|
)
|
|
|
4,132
|
|
|
|
26.5
|
%
|
Profit on disposal of property, plant & equipment expense
|
|
|
-
|
|
|
|
100
|
|
|
|
(100
|
)
|
|
|
(100.0
|
)%
|
Other operating expenses
|
|
|
-
|
|
|
|
(52
|
)
|
|
|
52
|
|
|
|
100.0
|
%
|
Interest income
|
|
|
232
|
|
|
|
87
|
|
|
|
145
|
|
|
|
166.7
|
%
|
Interest expense
|
|
|
(223
|
)
|
|
|
-
|
|
|
|
223
|
|
|
|
100.0
|
%
|
Other income/(expense)
|
|
|
1,564
|
|
|
|
(2,043
|
)
|
|
|
3,607
|
|
|
|
176.6
|
%
|
Revenue
. Revenues for the year
ended December 31, 2015 were 52.0% lower at $2.9 million, compared to $6.0 million for year ended December 31, 2014. This decrease
was primarily due to a decrease in sales to Jazz Pharmaceuticals/EUSA Pharma of CollatampG, our gentamicin implant for the treatment
and prevention of post-surgical infection, of $2.2 million, or 47%, and a decrease in CollaGUARD sales of $0.5 million, or 99%,
primarily due to partners having purchased sufficient product in 2014 for 2015. CollaGUARD revenues in the year ended December
31, 2015 were net of a $0.0 million charge for free stock due to be shipped per the terms of our distribution partner agreements,
leaving a CollaGUARD free stock credit outstanding of $0.1 million as of December 31, 2015. Revenue from the sales of Septocoll
decreased 52.0%, which was net of $0.2 million of free stock shipped under an agreement with our distribution partner during the
year ended December 31, 2013, leaving a Septocoll free stock credit outstanding of $0.0 million as of December 31, 2015. Biomet
end user Septocoll sales based on volume of units shipped decreased by 12.8% in the year ended December 31, 2015 compared to the
year ended December 31, 2014.
Cost of Sales
. Cost of sales of
$5.3 million in the year ended December 31, 2015 decreased by $2.1 million, or 28.0%, compared to $7.4 million in the year ended
December 31, 2014. Gross margins from supply revenue were (86%) and (24%) for the year ended December 31, 2015 and 2014, respectively.
All overhead costs associated with operating our manufacturing facility are included in the standard cost of our products as indirect
costs and charged to cost of sales based on sales volume. Excluding such indirect costs, gross margins from supply revenue were
(30%) and 25% for the years ended December 31, 2015 and 2014 respectively.
Research and Development (R&D)
Expenses
. R&D expenses were $29.8 million for the year ended December 2015 as compared to $4.3 million for the year ended
December 31, 2014, a 590.3% increase. R&D expenses in each year consisted of external clinical research costs as well as costs
of internal research and development personnel and internal laboratory costs at our Saal, Germany facility. In the year ended
December 31, 2015, external clinical research costs were $26.4 million in the year ended December 31, 2015 compared to $1.9 million
external clinical research costs in the year ended December 31, 2014, the increase was primarily due to the completion of our
pivotal pharmacokinetics and safety study of XaraColl and the initiation and running of our Phase 3 Cogenzia and Xaracoll efficacy
trials.
General and Administrative (G&A)
Expenses
. G&A expenses were $19.7 million for the year ended December 31, 2015 as compared to $15.6 million for the year
ended December 31, 2014, an increase of 26.5%. G&A expenses in the year ended December 31, 2015 included $4.0 million in non-cash
charges for share-based compensation, compared to $6.9 million of such charges in the corresponding period in 2014. Excluding
such charges for share-based compensation, G&A expenses were $15.7 million for the year ended December 31, 2015 as compared
to $8.7 million for the year ended December 31, 2014. The increase in G&A, excluding share-based compensation, was primarily
due to our continued infrastructure build-out to support clinical programs, initiation of our pre-commercialization investment
and expenses related to our re-domiciliation to Ireland.
Interest Expense
: Interest expense
was $0.2 million in the year ended December 31, 2015 compared to zero in the year ended December 31, 2014, a 100%
increase. Interest expense in the year ended December 31, 2015 consisted primarily of $0.2 million in non-cash interest
charges.
Other Income/(Expense):
Other income was $1.6 million in the year ended December 31, 2015 compared to other expense of $2.0 million in the year ended
December 31, 2014, a 176.6% increase. Other income in the year ended December 31, 2015 consisted primarily of foreign
exchange gains partially offset by fair value loss on warrants outstanding. Other expense in the year ended December 31, 2014
consisted primarily of fair value loss on warrants outstanding partially offset by foreign exchange gains.
Liquidity and Capital Resources
Since 2004, we have devoted a substantial
portion of our cash resources to research and development and general and administrative activities primarily related to the development
of our products, including XaraColl, Cogenzia and CollaGUARD. We have financed our operations primarily with the proceeds of the
sale of preferred shares and convertible notes, supply revenue and collaborative licensing and development revenue, our initial
public offering in 2014, our April 2015 and June 2016 follow-on public offerings as well as €25 million loan from the EIB.
We may not be able to generate revenues from the sale of XaraColl until the end of 2018, if at all. We have incurred losses and
generated negative cash flows from operations since 2004. As of December 31, 2016, we had an accumulated deficit of $223.1 million
and cash and cash equivalents of $15.8 million. As at December 31, 2016, Innocoll Pharmaceuticals Ltd. had Irish tax losses of
$181.1 million which can be carried forward to shelter future Irish trading profits indefinitely. There is no limitation on the
use of losses in any particular year (i.e. no minimum tax payment rule). Irish law imposes certain limitations on the application
of net operating loss carryforwards and no assurance can be given that these tax losses will be available to the full extent in
the future.
The following table summarizes our cash
flows from operating, investing and financing activities for the years ended December 31, 2016, 2015 and 2014:
|
|
Year
Ended December 31,
|
|
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
|
|
|
|
|
(in thousands)
|
|
|
|
|
Consolidated Statement of Cash Flows Data:
|
|
|
|
|
|
|
|
|
|
|
|
|
Net cash provided by (used in):
|
|
|
|
|
|
|
|
|
|
|
|
|
Operating activities
|
|
$
|
(62,471
|
)
|
|
$
|
(42,811
|
)
|
|
$
|
(16,785
|
)
|
Investing activities
|
|
|
(12,618
|
)
|
|
|
(3,260
|
)
|
|
|
(1,108
|
)
|
Financing activities
|
|
|
48,659
|
|
|
|
33,059
|
|
|
|
69,292
|
|
Effect of foreign exchange rate changes
|
|
|
9
|
|
|
|
(184
|
)
|
|
|
270
|
|
Net (decrease)/increase in cash and cash equivalents
|
|
|
(26,421
|
)
|
|
|
(13,196
|
)
|
|
|
51,669
|
|
Operating Capital and Capital Expenditure Requirements for
the Next 12 Months
As of December 31, 2016, we had an accumulated
deficit of $223.1 million and cash and cash equivalents of $15.8 million. We anticipate that expenditures during the next twelve
months necessary to advance our current operations, including plans to conduct further studies to enable us to submit a revised
NDA for XaraColl and to develop and commercialize CollaGUARD will be greater than the amount of our current cash and cash equivalents.
This assessment is based on current estimates and assumptions regarding our clinical programs and business needs. Our working
capital requirements could vary depending on a variety of circumstances, including, for example, if we are required to conduct
additional tests not currently contemplated. These matters, among others, raise substantial doubt about our ability to continue
as a going concern. Based on the foregoing, we currently do not have sufficient working capital to meet our needs through the
next 12 months, unless we can successfully obtain additional funding through debt or equity transactions. Our financial statements
include an opinion of our auditors that our continued operating losses and limited capital raise substantial doubt about our ability
to continue as an ongoing concern. Our ability to successfully raise sufficient funds through the sale of equity securities or
the identification of strategic alliances, when needed, is subject to many risks and uncertainties and even if we are successful,
future equity issuances would result in dilution to our existing stockholders. In addition, to the extent that we might seek to
raise capital through the identification of strategic alliances, we may be required to license or transfer rights to our technologies
to other parties that we might otherwise desire to retain. Our risk factors are described under the heading “Risk Factors”
in Part I Item 1A and elsewhere in our Annual Report on Form 10-K and in other reports we file with the SEC.
Operating Activities
For the years ended December 31, 2016,
2015 and 2014, our net cash used in operating activities was $62.5 million, $42.8 million, and $16.8 million, respectively.
The increase in net cash used in operating activities in the year ended December 31, 2016 resulted primarily from an increase
in both research & development expenses and general & administrative expenses together with an increase in trade and other
receivables and an increase in inventory. The increase in net cash used in operating activities in the year ended December 31,
2015 resulted primarily from an increase in both research & development expenses and general & administrative expenses
together with an increase in trade and other receivables and an increase in inventory.
Investing Activities
For the years ended December 31, 2016,
2015 and 2014, our net cash used in investing activities was $12.6 million, $3.3 million, and $1.1 million, respectively. The
net cash used in investing activities in the years ended December 31, 2016, 2015 and 2014 was primarily for the purchases of plant
and machinery at our Saal, Germany facility.
Financing Activities
Our net cash provided by financing activities
was $48.7 million for the year ended December 31, 2016 compared to $33.1 million for the year ended December 31, 2015.
The cash provided by financing activities for the year ended December 31, 2016 was primarily the result of the issuance of ordinary
shares in our June 2016 follow-on public offering for net proceeds $37.0 million and the drawdown of $11.2 million in loans from
the European Investment Bank. Our net cash provided by financing activities was $33.1 million for the year ended December
31, 2015 compared to $69.3 million for the year ended December 31, 2014. The cash provided by financing activities for the year
ended December 31, 2015 was primarily the result of the issuance of ordinary shares in our April 2015 follow-on public offering
for net proceeds $16.7 million and the drawdown of $16.3 million in loans from the European Investment Bank, compared to $69.3
million for the year ended December 31, 2014, primarily the result of the issuance of ADS in our initial public offering for net
proceeds of $57.7 million, and the 2014 pre-IPO equity financings for net proceeds for $11.6 million On July 3, 2014, all shares
of Innocoll GmbH became ordinary shares of Innocoll AG.
Innocoll GmbH 2014 Equity Financings
In May 2014, we issued 77,924 series E
preferred shares to certain existing shareholders, three new members of our historic supervisory board and three new investors
who are partners of one of the existing shareholders for approximately $12.1 million. We also issued 44,465 restricted and unrestricted
shares as described under “Financial Operations Overview—Valuation of financial instruments—May 2014 Grants.”
In June 2014, we issued 32,977 new ordinary shares of Innocoll GmbH for $5.1 million to certain existing shareholders under the
same terms and conditions and having the same anti-dilution rights as the series E preferred shares. Given that the price of Innocoll
Germany’s ADS at our initial public offering in July 2014 was $9.00 per ADS of Innocoll Germany (or €88.52 per ordinary
share) in February 2015 we issued 58,953 of our ordinary shares to such holders as a result of these anti-dilution provisions
after such issuance was approved at our shareholder meeting on December 4, 2014.
2014 Option Agreement
In January 2014, Innocoll Germany’s
predecessor, Innocoll GmbH, entered into an option agreement, as amended on March 20, 2014 with its then-existing shareholders,
including certain officers, directors and affiliates in their capacity as shareholders. The option agreement covers all options
issued by Innocoll GmbH in connection with its re-domicile and the 2013 equity financing described above under “—Re-Domicile
of Parent Company,” and “—Innocoll GmbH 2013 and 2014 Equity Financings,” respectively. Pursuant to the
2014 Option Agreement, these shareholders and Kinabalu Financial Products L.L.P. received the right, at any time and from time
to time, to purchase up to an aggregate of 205,199 shares of Innocoll GmbH in the aggregate, with an exercise price of
€100 per share (subject to adjustment) and a contractual life of 10 years. In connection with Innocoll Germany’s transformation
into a stock corporation, all options under the original 2014 option agreement were cancelled and replaced by a new option agreement
on substantially similar terms pursuant to which beneficiaries were entitled to purchase up to 205,199 ordinary shares of Innocoll
AG in the aggregate at the same initial exercise price of €100 per share (as so replaced, the “2014 Option
Agreement”), which obligations have been assumed by Innocoll Ireland. The 2014 Option Agreement provides that if we issue
or sell or are deemed to have issued or sold any of our ordinary shares without consideration or for a consideration per share
less than the exercise price in effect immediately prior to the time of such issue or sale, the exercise price is reduced to a
price equal to the price per share at which such shares are issued or sold or deemed issued or sold, subject to certain limited
exceptions for share option, share purchase or similar plan or arrangement for the benefit of our or our subsidiaries’ employees,
officers, consultants or directors, pre-existing options, securities issued as consideration for any acquisition by the us or
our subsidiaries, or securities issued to banks, equipment lessors or other financial institutions, or to real property lessors,
pursuant to a debt financing, equipment leasing or real property leasing transaction which is approved by the management board.
As a result of the $9.00 per ADSs price of Innocoll Germany’s initial public offering, the exercise price was adjusted to
€88.52 per ordinary share of Innocoll Germany, which price is subject to further adjustment if we issue securities at an
equivalent value below this price, or $7.42 per ordinary share of Innocoll Ireland (based on conversion to U.S. dollars at an
exchange rate of $1.1109 per euro, the official exchange rate quoted as of March 15, 2016 by the European Central Bank)
through June 15, 2019, on which date any unexercised options expire pursuant to the terms of the 2014 Option Agreement, unless
our shareholders approve an additional five-year period.
Innocoll GmbH Conversion of Preferred Shares into Ordinary
Shares of Innocoll GmbH and Subsequent Transformation into Innocoll AG
Pursuant to a notarial deed entered into
on June 16, 2014, the shareholders of Innocoll GmbH agreed to amend and terminate all preference, redemption and cumulative dividend
rights by converting all preferred shares into ordinary shares of Innocoll GmbH (other than, with respect to the holders of series
E preferred shares, who retained the anti-dilution right referred to above). On July 3, 2014, subsequent to the recapitalization,
Innocoll GmbH transformed into a German stock corporation (Aktiengesellschaft or AG) in accordance with the provisions of the
German Reorganization Act (Umwandlungsgesetz). In connection therewith, all 1,004,523 outstanding ordinary shares of Innocoll
GmbH became 1,004,523 ordinary shares of Innocoll AG. Accordingly, although we changed our legal form, there was no change in
our identity. The following table summarizes the capitalization of Innocoll GmbH before, and giving effect to, its recapitalization
and the conversion of all preferred shares into ordinary shares prior to its transformation into Innocoll AG:
Share Class (in order of preferences)
|
|
Shares
Pre-Conversion
|
|
|
Exchange Ratio
|
|
Ordinary
Shares
Upon
Conversion
of
Preferred
Shares
|
|
|
%
|
|
Series E preferred shares
|
|
|
90,286
|
|
|
1:1
|
|
|
90,286
|
|
|
|
7.0
|
%
|
Series D-2 preferred shares
|
|
|
24,981
|
|
|
1.88:1
|
|
|
47,025
|
|
|
|
3.7
|
%
|
Series D preferred shares
|
|
|
201,744
|
|
|
1.88:1
|
|
|
379,771
|
|
|
|
29.6
|
%
|
Series C preferred shares
|
|
|
240,611
|
|
|
0.67:1
|
|
|
160,203
|
|
|
|
12.5
|
%
|
Series A preferred shares
|
|
|
376,827
|
|
|
0.67:1
|
|
|
250,898
|
|
|
|
19.6
|
%
|
Series B preferred shares
|
|
|
63,352
|
|
|
1.83:1
|
|
|
115,733
|
|
|
|
9.0
|
%
|
Ordinary Shares Pre-Conversion
|
|
|
46,115
|
|
|
0:1
|
|
|
-
|
|
|
|
0
|
%
|
Ordinary Shares
|
|
|
32,977
|
|
|
1:1
|
|
|
32,977
|
|
|
|
2.6
|
%
|
Outstanding options
|
|
|
205,199
|
|
|
1:1
|
|
|
205,199
|
|
|
|
16.0
|
%
|
Total
|
|
|
1,282,092
|
|
|
|
|
|
1,282,092
|
|
|
|
100.0
|
%
|
Initial Public Offering
On July 30, 2014, Innocoll Germany sold
6,500,000 ADSs representing 490,567 ordinary shares of Innocoll Germany in its initial public offering at a price of $9.00 per
ADS of Innocoll Germany, thereby raising $54.4 million after deducting underwriting discounts and commissions. On August 20, 2014,
the underwriters in our initial public offering partially exercised their overallotment option to purchase an additional 186,984
ADSs of Innocoll Germany, representing 14,112 ordinary shares of Innocoll Germany, at a public offering price of $9.00 per ADS
of Innocoll Germany. The sale of the overallotment option by our underwriters occurred on September 12, 2014, at which the company
raised additional net proceeds of approximately $1.57 million, after deducting underwriting discounts and commissions. The Innocoll
Germany ADSs we sold in the initial public offering represented new ordinary shares of Innocoll Germany issued in a capital increase
resolved by our shareholders for the purposes of the initial public offering on July 30, 2014.
EIB Loan
On March 27, 2015, we approved the execution
of the Finance Contract between Innocoll Pharmaceuticals Limited and the European Investment Bank (“EIB”) for a loan
of up to $27.6 million.
The loan terms specify that the amounts
drawn will be used to finance up to 50% of certain research and development and capital expenditures forecast to be made by us
over a three year period from 2015 through 2017. The first $16.3 million of the loan commitment may be drawn at any time up to
fifteen months from the date of the Finance Contract. The remaining $11.2 million may be drawn at any time up to eighteen months
from the date of the Finance Contract subject to the delivery of clinical data, certified by our board, confirming to the satisfaction
of EIB that the primary clinical endpoints for either Cogenzia or XaraColl Phase 3 trials have been achieved and therefore that
it can be concluded the Phase 3 clinical trial has successfully been completed. The loan bears interest at a fixed rate of 12%
per annum, compounded annually. There are no cash payments of interest required during the term of the loan, interest on the outstanding
loan balance accrues daily, and is payable only on the maturity date or prepayment date of the loan, whichever is earlier. The
maturity date of each tranche is three to five years from the draw down date, as may be determined by us in each draw down request.
The principal of the loan is payable on the maturity date or the prepayment date, whichever is earlier. Where a prepayment is
made by us will incur a prepayment indemnity of 1%, 0.75%, 0.5% or 0.25% of the principal amount to be repaid within one year,
two years, three years or four years from date of drawdown, respectively. There is no prepayment indemnity for prepayment after
the fourth year.
The loan contains an expenditure covenant
requiring us to spend at least 75% of our forecast research and development, and capital expenditures during the period from 2015
to 2020 as set out in a business plan agreed to with the EIB. If, upon completion of the project, it is determined that the total
principal amount of the loan drawn by us exceeds 50% of the total cost of the project, EIB may cancel the undisbursed portion
of the loan and demand prepayment of the loan up to the amount by which the loan, excluding accrued interest, exceeds 50% of the
total cost of the project.
On December 18, 2015 we drew down the first
tranche of $16.3 million.
On June 17, 2016, we drew down the second
and final tranche of $11.3 million.
The security on the Finance Contract includes
a guarantee from us on 100% of the outstanding principal, interest, expense, commission, indemnity and other sum owed by our subsidiary,
Innocoll Pharmaceuticals Limited, together with a fixed charge over all the shares in Innocoll Pharmaceuticals Limited and a floating
charge over all the assets of Innocoll Pharmaceuticals Limited. As of December 31, 2016 no violations of the covenants occurred.
Follow-on Public Offerings
On April 30, 2015, Innocoll Germany sold
1,999,690 ADSs of Innocoll Germany representing 150,920 ordinary shares of Innocoll Germany in our follow-on public offering at
a price of $9.00 per ADS of Innocoll Germany, thereby raising $16.9 million after deducting underwriting discounts and commissions.
These ADSs represented new ordinary shares of Innocoll Germany issued in a capital increase resolved by our shareholders for such
purposes.
On June 22, 2016, we sold 5,725,000 ordinary
shares in a follow-on public offering at a price of $7.00 per share, thereby raising gross proceeds of $40 million before deducting
underwriting discounts and commissions and offering expenses.
Future Capital Requirements
As of December 31, 2016, we had an accumulated
deficit of $223.1 million and cash and cash equivalents of $15.8 million. We anticipate that expenditures during the next twelve
months necessary to advance our current operations, including plans to conduct further studies to enable us to submit a revised
NDA for XaraColl and to develop and commercialize CollaGUARD will be greater than the amount of our current cash and cash equivalents.
This assessment is based on current estimates and assumptions regarding our clinical programs and business needs. Our working
capital requirements could vary depending on a variety of circumstances, including, for example, if we are required to conduct
additional tests not currently contemplated. These matters, among others, raise substantial doubt about our ability to continue
as a going concern. Based on the foregoing, we currently do not have sufficient working capital to meet our needs through the
next 12 months, unless we can successfully obtain additional funding through debt or equity transactions. Our financial statements
include an opinion of our auditors that our continued operating losses and limited capital raise substantial doubt about our ability
to continue as an ongoing concern. Our ability to successfully raise sufficient funds through the sale of equity securities or
the identification of strategic alliances, when needed, is subject to many risks and uncertainties and even if we are successful,
future equity issuances would result in dilution to our existing stockholders. In addition, to the extent that we might seek to
raise capital through the identification of strategic alliances, we may be required to license or transfer rights to our technologies
to other parties that we might otherwise desire to retain. Our risk factors are described under the heading “Risk Factors”
in Part I Item 1A and elsewhere in our Annual Report on Form 10-K and in other reports we file with the SEC.
We expect to continue to incur substantial
additional operating losses as we seek regulatory approval for and commercialize XaraColl and CollaGUARD and develop and seek
regulatory approval for our other product candidates. If we obtain FDA approval for our products, we will incur significant sales,
marketing and manufacturing expenses. In addition, we expect to incur additional expenses to add operational, financial and information
systems and personnel, including personnel to support our planned product commercialization and expanded manufacturing efforts
for Xaracoll and CollaGUARD in the United States. We also expect to incur significant costs to continue to comply with corporate
governance, internal controls and similar requirements applicable to us as a public company.
Our future use of operating cash and capital
requirements will depend on many forward-looking factors, including the following:
|
·
|
our ability
to successfully complete additional short-term clinical studies and non-clinical studies
for Xaracoll in support of a proposed revised NDA to the FDA;
|
|
·
|
the timing
and outcome of the FDA’s review of the proposed revised NDA for XaraColl and the
PMA application for CollaGUARD;
|
|
·
|
the extent
to which the FDA may require us to perform additional clinical trials for XaraColl and
CollaGUARD;
|
|
·
|
the costs of
our commercialization activities for Xaracoll and CollaGUARD in the U.S., if approved
by the FDA;
|
|
·
|
the cost and
timing of purchasing manufacturing and other capital equipment for XaraColl, CollaGUARD
and our other products and product candidates;
|
|
·
|
the scope,
progress, results and costs of development for additional indications for XaraColl and
CollaGUARD and for our other product candidates;
|
|
·
|
the cost, timing
and outcome of regulatory review of our other product candidates;
|
|
·
|
the cost, timing
and outcome of regulatory review of our proposed expansion of our manufacturing facility;
|
|
·
|
the extent
to which we acquire or invest in products, businesses and technologies;
|
|
·
|
the extent
to which we choose to establish collaboration, co-promotion, distribution or other similar
agreements for our product candidates; and
|
|
·
|
the costs of
preparing, submitting and prosecuting patent applications and maintaining, enforcing
and defending intellectual property claims.
|
To the extent that our capital resources
are insufficient to meet our future operating and capital requirements, we will need to finance our cash needs through public
or private equity offerings, debt financings, corporate collaboration and licensing arrangements or other financing alternatives.
Additional equity or debt financing or corporate collaboration and licensing arrangements may not be available on acceptable terms,
if at all.
If we raise additional funds by issuing
equity securities, our shareholders will experience dilution. Debt financing, if available, would result in increased fixed payment
obligations and may involve agreements that include covenants limiting or restricting our ability to take specific actions, such
as incurring additional debt, making capital expenditures or declaring dividends. Any debt financing or additional equity that
we raise may contain terms, such as liquidation and other preferences, that are not favorable to us or our shareholders. If we
raise additional funds through collaboration and licensing arrangements with third parties, it may be necessary to relinquish
valuable rights to our technologies, future revenue streams or product candidates or to grant licenses on terms that may not be
favorable to us.
Contractual Obligations
As of December 31, 2016, future minimum payments
due under our contractual obligations are as follows (in million):
|
|
Payments Due by
Period (Including Interest on Debt)
|
|
($ in millions)
|
|
Total
|
|
|
2016
|
|
|
2017-2018
|
|
|
2019-2020
|
|
|
Thereafter
|
|
Long-term debt, including current portion
|
|
|
26,169
|
|
|
|
-
|
|
|
|
-
|
|
|
|
26,169
|
|
|
|
-
|
|
Interest payments on long-term debt obligations
|
|
|
2,779
|
|
|
|
-
|
|
|
|
-
|
|
|
|
2,779
|
|
|
|
-
|
|
Operating lease obligations
|
|
|
4,084
|
|
|
|
677
|
|
|
|
1,005
|
|
|
|
485
|
|
|
|
1,917
|
|
Total
|
|
|
33,032
|
|
|
|
677
|
|
|
|
1,005
|
|
|
|
29,433
|
|
|
|
1,917
|
|
Item 7A. Quantitative and Qualitative Disclosures about
Market Risk.
We are exposed to various risks in relation
to financial instruments including credit risk, liquidity risk and currency risk. Our risk management is coordinated by our managing
directors. We do not engage in the trading of financial assets for speculative purposes. The most significant financial risks
to which we are exposed include the following:
Credit risk
Our sales are currently concentrated with
two customers and accordingly we are exposed to the possibility of loss arising from customer default. We are addressing this
risk by monitoring our commercial relationships with these customers and by seeking to develop additional products for sale and
entering into new partnerships.
Liquidity risk
We have been dependent on our shareholders
to fund our operations. As described in Note 2 of our financial statements, our ability to continue as a going concern is dependent
on our ability to raise additional finance by way of debt and/or equity offerings to enable us to fund our clinical trial programs.
Currency risk
We are subject to currency risk, as our
income and expenditures are denominated in U.S. dollar and euro. As such we are exposed to exchange rate fluctuations between
the U.S. dollar and the euro. We aim to match foreign currency cash inflows with foreign cash outflows where possible. We do not
hedge this exposure. A 10% movement in the U.S. dollar versus euro exchange rate at December 31, 2016 would have the effect of
increasing/decreasing net liabilities by approximately $0.2 million. As we incur clinical trial expenses in the United States
in U.S. dollars, raise funds through licensing and collaboration revenue in U.S. dollars and commence sales of our products in
the United States, we expect to have significant increases in cash balances, revenues and research and development costs denominated
in U.S. dollars, while the majority of our cost of sales and operating costs are expected to remain denominated in euro. Accordingly,
our exposure to exchange rates between the U.S. dollar and the euro has increased significantly commencing in 2014 compared to
2013. Between January 2014 and December 2016, the exchange rate between the U.S. dollar and the euro ranged between $1.3953 per
euro and $1.0364 per euro.
Item 8. Financial Statements and Supplementary Data.
Our financial statements and supplementary
data required to be filed pursuant to this Item 8 appear in a separate section of this report beginning on page F-1.
Item 9. Changes In and Disagreements with Accountants
on Accounting and Financial Disclosure.
None.
Item 9A. Controls and Procedures.
Disclosure Controls and Procedures
We maintain disclosure controls and procedures
designed to ensure that information required to be disclosed in the reports that we file or submit under the Securities Exchange
Act of 1934, as amended, is recorded, processed, summarized and reported within the time periods specified in the SEC’s rules
and forms, and that such information is accumulated and communicated to our management, including our Chief Executive Officer
and Chief Financial Officer, as appropriate, to allow timely decisions regarding required disclosure.
Our management has evaluated, with the
participation of our Chief Executive Officer and our Chief Financial Officer, the effectiveness of our disclosure controls and
procedures, as defined in Rules 13a-15(e) and 15d-15(e) under the Securities Exchange Act of 1934, as of December 31, 2016. Based
upon this evaluation, our Chief Executive Officer and our Chief Financial Officer have concluded that our disclosure controls
and procedures were effective as of December 31, 2016.
Management’s Annual Report on Internal Control Over
Financial Reporting
Our management is responsible for establishing
and maintaining adequate internal control over financial reporting for the Company. Internal control over financial reporting
is defined in Rules 13a-15(f) and 15d-15(f) promulgated under the Securities Exchange Act of 1934.
Our management, with the participation
of our Chief Executive Officer and our Chief Financial Officer, assessed the effectiveness of the Company’s internal control
over financial reporting as of December 31, 2016. In making this assessment, our management used the criteria set forth by the
Committee of Sponsoring Organizations of the Treadway Commission, or COSO, in “Internal Control-Integrated Framework (2013
Framework).” Based on this
assessment, management concluded that, as
of December 31, 2016, the Company’s internal control over financial reporting was effective at the reasonable assurance
level.
This annual report does not include an
attestation report of our independent registered public accounting firm on our internal control over financial reporting due to
the exemption provided by SEC rules for emerging growth companies.
Changes in Internal Control Over Financial Reporting
There was no change in our internal control
over financial reporting during our most recently completed fiscal quarter that has materially affected, or is reasonably likely
to materially affect, our internal control over financial reporting.
Item 9B. Other Information.
None.
Part III
Item 10. Directors, Executive Officers
and Corporate Governance.
The information required by this Item will
be set forth in the Company’s proxy statement or an amendment to this annual report on Form 10-K, in either case, to be
filed with the Securities and Exchange Commission within 120 days after the Company’s fiscal year end and is incorporated
herein by reference.
Our board of directors has adopted a code
of business conduct and ethics that applies to all officers, directors and employees, which is available under the Investor Relations—Corporate
Governance section of our website at www.innocoll.com. We intend to satisfy the disclosure requirement under Item 5.05 of Form
8-K regarding amendment to, or waiver from, a provision of our code of business conduct and ethics by posting such information
on the website address and location specified above.
Item 11. Executive Compensation.
The information
required by this Item will be set forth in the Company’s proxy statement or an amendment to this annual report on Form 10-K,
in either case, to be filed with the Securities and Exchange Commission within 120 days after the Company’s fiscal year
end and is incorporated herein by reference.
Item 12. Security Ownership of Certain Beneficial Owners
and Management and Related Stockholder Matters.
The information required by this Item will
be set forth in the Company’s proxy statement or an amendment to this annual report on Form 10-K, in either case, to be
filed with the Securities and Exchange Commission within 120 days after the Company’s fiscal year end and is incorporated
herein by reference.
Item 13. Certain Relationships and Related Transactions,
and Director Independence.
The information required by this Item will
be set forth in the Company’s proxy statement or an amendment to this annual report on Form 10-K, in either case, to be
filed with the Securities and Exchange Commission within 120 days after the Company’s fiscal year end and is incorporated
herein by reference.
Item 14. Principal Accounting Fees and Services.
The information required by this Item will
be set forth in the Company’s proxy statement or an amendment to this annual report on Form 10-K, in either case, to be
filed with the Securities and Exchange Commission within 120 days after the Company’s fiscal year end and is incorporated
herein by reference.
Part IV
Item 15. Exhibits and Financial Statement Schedules.
Financial Statements
Reference is made to the Index to the Consolidated
Financial Statements beginning on page F-1 of this report.
Financial Statement Schedules
Required information is included in the
footnotes to the financial statements.
Exhibits
See the Exhibit Index immediately following
the financial statements to this Annual Report on Form 10-K.
Financial Statements and Schedules of Subsidiaries and
Affiliates
None.
Item 16. Form 10-K Summary.
None.
SIGNATURES
Pursuant to the requirements of Section
13 or 15(d) of the Securities Exchange Act of 1934, the registrant has duly caused this report to be signed on its behalf by the
undersigned, thereunto duly authorized.
|
INNOCOLL HOLDINGS PLC
|
|
|
|
|
By:
|
/s/ Anthony P. Zook
|
|
|
Anthony P. Zook
|
|
|
Chief Executive Officer
|
Dated:
March 16, 2017
POWER OF ATTORNEY
We, the undersigned officers and directors
of Innocoll Holdings plc, hereby severally constitute and appoint Anthony P. Zook and Jose Carmona, and each one of them individually,
to sign for us and in our names in the capacities indicated below, any and all amendments to the report on Form 10-K filed herewith,
and to file the same, with all exhibits thereto and other documents in connection therewith, in each case, with the Securities
and Exchange Commission, and generally to do all such things in our names and on our behalf in our capacities consistent with
the provisions of the Securities Exchange Act of 1934, as amended, and all requirements of the Securities and Exchange Commission.
Pursuant to the requirements of the Securities
Exchange Act of 1934, this report has been signed below by the following persons on behalf of the registrant in the capacities
and on the dates indicated.
Signature
|
|
Title
|
|
Date
|
|
|
|
|
|
/s/ Anthony P. Zook
|
|
Chief Executive Officer and Director
|
|
March 16, 2017
|
Anthony P. Zook
|
|
(Principal Executive Officer)
|
|
|
|
|
|
|
|
/s/ Jose Carmona
|
|
Chief Financial Officer
|
|
March 16, 2017
|
Jose Carmona
|
|
(Principal Financial Officer and Principal Accounting Officer)
|
|
|
|
|
|
|
|
/s/ Jonathan Symonds
|
|
Chairman of the Board
|
|
March 16, 2017
|
Jonathan Symonds, CBE
|
|
|
|
|
|
|
|
|
|
/s/ Shumeet Banerji
|
|
Vice Chairman of the Board
|
|
March 16, 2017
|
Shumeet Banerji, Ph.D.
|
|
|
|
|
|
|
|
|
|
/s/ A. James Culverwell
|
|
Director
|
|
March 16, 2017
|
A. James Culverwell
|
|
|
|
|
|
|
|
|
|
/s/ David R. Brennan
|
|
Director
|
|
March 16, 2017
|
David R. Brennan
|
|
|
|
|
|
|
|
|
|
/s/ Rolf D. Schmidt
|
|
Director
|
|
March 16, 2017
|
Rolf D. Schmidt
|
|
|
|
|
|
|
|
|
|
/s/ Joseph Wiley M.D.
|
|
Director
|
|
March 16, 2017
|
Joseph Wiley M.D.
|
|
|
|
|
PART IV
Item 15(a)(1). Financial Statements
Report of Independent Registered Public Accounting Firm
To the Board of Directors and Shareholders
of Innocoll Holdings plc
We have audited the accompanying consolidated balance sheets
of Innocoll Holdings plc (an Irish public limited company) and subsidiaries (“the Company”) as of December 31, 2016
and 2015, and the related consolidated statements of operations and comprehensive loss, changes in shareholders’ (deficit)/equity,
and cash flows for each of the three years in the period ended December 31, 2016. These financial statements are the responsibility
of the Company’s management. Our responsibility is to express an opinion on these financial statements based on our audits.
We conducted our audits in accordance with the standards of
the Public Company Accounting Oversight Board (United States). Those standards require that we plan and perform the audit to obtain
reasonable assurance about whether the financial statements are free of material misstatement. We were not engaged to perform
an audit of the Company’s internal control over financial reporting. Our audits included consideration of internal control
over financial reporting as a basis for designing audit procedures that are appropriate in the circumstances, but not for the
purpose of expressing an opinion on the effectiveness of the Company’s internal control over financial reporting. Accordingly,
we express no such opinion. An audit also includes examining, on a test basis, evidence supporting the amounts and disclosures
in the financial statements, assessing the accounting principles used and significant estimates made by management, as well as
evaluating the overall financial statement presentation. We believe that our audits provide a reasonable basis for our opinion.
In our opinion, the consolidated financial statements referred
to above present fairly, in all material respects, the financial position of Innocoll Holdings plc and subsidiaries as of December
31, 2016 and 2015, and the results of their operations and their cash flows for each of the three years in the period ended December
31, 2016, in conformity with accounting principles generally accepted in the United States of America (U.S. GAAP).
The accompanying consolidated financial statements have
been prepared assuming that the Company will continue as a going concern. The Company incurred a loss of $57.0 million
during the year and had an accumulated loss of $223.1 million at the year ended December 31, 2016. These conditions,
along with other matters as set forth in Note 2, raise substantial doubt about the Company’s ability to continue as a
going concern. Management’s plan in regard to these matters is described in Note 2. The consolidated financial
statements do not include any adjustments that might result from the outcome of this uncertainty.
As discussed in Note 3 to the consolidated financial statements,
the Company transitioned to U.S. GAAP as of January 1, 2016 and applied U.S. GAAP retrospectively for all periods presented.
As discussed in Note 1 to the consolidated financial statements,
the functional currency of the Company changed from Euro to U.S. Dollar. The change in functional currency was applied prospectively
effective January 1, 2016. On the same date, the Company changed its
reporting currency from Euro to U.S. Dollar. The change in reporting currency was applied retrospectively for all periods presented.
The selected quarterly financial data in Note 22 contains
information that we did not audit. Accordingly, we do not express an opinion on that data. The Company was not required to file
quarterly reports on Form 10-Q for the year ended December 31, 2016; accordingly, the Company did not engage us to review the
data in accordance with the standards of the Public Company Accounting Oversight Board (United States).
Grant Thornton
/s/ Grant Thornton
Dublin, Ireland
March 16, 2017
INNOCOLL HOLDINGS PLC
CONSOLIDATED STATEMENTS OF OPERATIONS
AND COMPREHENSIVE LOSS
for the years ended December 31, 2016,
2015 and 2014
Thousands of Dollars (except per
share data)
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Revenue
|
|
$
|
4,372
|
|
|
$
|
2,870
|
|
|
$
|
5,974
|
|
Cost of sales
|
|
|
(6,986
|
)
|
|
|
(5,328
|
)
|
|
|
(7,404
|
)
|
Gross loss
|
|
|
(2,614
|
)
|
|
|
(2,458
|
)
|
|
|
(1,430
|
)
|
Research and development expenses
|
|
|
(38,715
|
)
|
|
|
(29,821
|
)
|
|
|
(4,320
|
)
|
General and administrative expenses
|
|
|
(25,446
|
)
|
|
|
(19,743
|
)
|
|
|
(15,611
|
)
|
(Loss)/gain on disposals of property, plant & equipment
|
|
|
(8
|
)
|
|
|
-
|
|
|
|
100
|
|
Other operating expenses
|
|
|
(1
|
)
|
|
|
-
|
|
|
|
(52
|
)
|
Loss from operating activities
|
|
|
(66,784
|
)
|
|
|
(52,022
|
)
|
|
|
(21,313
|
)
|
Interest income
|
|
|
35
|
|
|
|
232
|
|
|
|
87
|
|
Interest expense
|
|
|
(2,221
|
)
|
|
|
(223
|
)
|
|
|
-
|
|
Other income/(expense)
|
|
|
12,187
|
|
|
|
1,564
|
|
|
|
(2,043
|
)
|
Loss before income tax
|
|
|
(56,783
|
)
|
|
|
(50,449
|
)
|
|
|
(23,269
|
)
|
Income tax expense
|
|
|
(171
|
)
|
|
|
(407
|
)
|
|
|
(202
|
)
|
Net loss
|
|
$
|
(56,954
|
)
|
|
$
|
(50,856
|
)
|
|
$
|
(23,471
|
)
|
Other comprehensive loss:
|
|
|
|
|
|
|
|
|
|
|
|
|
Preferred shares dividend
|
|
|
-
|
|
|
|
-
|
|
|
|
(4,069
|
)
|
Currency translation adjustment
|
|
|
(108
|
)
|
|
|
(4,460
|
)
|
|
|
(3,847
|
)
|
Total comprehensive loss
|
|
$
|
(57,062
|
)
|
|
$
|
(55,316
|
)
|
|
$
|
(31,387
|
)
|
Net loss per share:
|
|
|
|
|
|
|
|
|
|
|
|
|
Basic and diluted (Note 9)
|
|
$
|
(2.12
|
)
|
|
$
|
(2.28
|
)
|
|
$
|
(2.41
|
)
|
See accompanying notes to consolidated
financial statements.
INNOCOLL HOLDINGS PLC
CONSOLIDATED
BALANCE SHEETS
|
|
As
of December 31,
|
|
Thousands of Dollars (except share
and per share data)
|
|
2016
|
|
|
2015
|
|
Assets
|
|
|
|
|
|
|
|
|
Current assets:
|
|
|
|
|
|
|
|
|
Cash and cash equivalents
|
|
$
|
15,765
|
|
|
$
|
42,186
|
|
Trade and other receivables, net
|
|
|
1,350
|
|
|
|
945
|
|
Prepaid expenses
|
|
|
5,486
|
|
|
|
3,622
|
|
Inventories
|
|
|
2,403
|
|
|
|
1,808
|
|
Total current assets
|
|
|
25,004
|
|
|
|
48,561
|
|
Property, plant and equipment, net
|
|
|
16,698
|
|
|
|
4,199
|
|
Deferred income tax assets
|
|
|
125
|
|
|
|
-
|
|
Restricted cash
|
|
|
175
|
|
|
|
-
|
|
Total assets
|
|
$
|
42,002
|
|
|
$
|
52,760
|
|
Liabilities and Equity
|
|
|
|
|
|
|
|
|
Current liabilities:
|
|
|
|
|
|
|
|
|
Trade payables and accrued expenses
|
|
$
|
13,505
|
|
|
$
|
14,411
|
|
Deferred revenue
|
|
|
1,827
|
|
|
|
2,219
|
|
Current taxes payable
|
|
|
36
|
|
|
|
20
|
|
Total current liabilities
|
|
|
15,368
|
|
|
|
16,650
|
|
Interest bearing loans and borrowings
|
|
|
28,948
|
|
|
|
16,400
|
|
Warrant liability
|
|
|
854
|
|
|
|
11,498
|
|
Deferred income tax liabilities
|
|
|
-
|
|
|
|
263
|
|
Defined benefit pension liability
|
|
|
28
|
|
|
|
49
|
|
Total liabilities
|
|
|
45,198
|
|
|
|
44,860
|
|
Commitments and contingencies (note 18)
|
|
|
|
|
|
|
|
|
Equity:
|
|
|
|
|
|
|
|
|
Common shares, par value (note 19), authorized: 1,025,100,000 shares (2,875,848 shares in 2015), issued: 29,773,239 shares (1,785,009 shares in 2015), outstanding: 29,748,239 shares (1,785,009 shares in 2015)
|
|
|
324
|
|
|
|
1,943
|
|
Additional paid-in capital
|
|
|
220,965
|
|
|
|
173,353
|
|
Treasury shares, at cost, 25,000 shares as of December 31, 2016 and zero shares as of December 31, 2015
|
|
|
(27
|
)
|
|
|
-
|
|
Accumulated currency translation adjustment
|
|
|
(1,352
|
)
|
|
|
(1,244
|
)
|
Accumulated loss
|
|
|
(223,106
|
)
|
|
|
(166,152
|
)
|
Total shareholders’ (deficit)/equity
|
|
|
(3,196
|
)
|
|
|
7,900
|
|
Total liabilities and equity
|
|
$
|
42,002
|
|
|
$
|
52,760
|
|
See accompanying notes to consolidated
financial statements.
INNOCOLL HOLDINGS PLC
CONSOLIDATED
STATEMENTS OF SHAREHOLDERS (DEFICIT)/EQUITY
|
|
Temporary equity
|
|
|
Permanent equity
|
|
|
Preferred shares
|
|
|
Common shares
|
|
|
|
|
|
|
|
|
Treasury shares
|
|
|
|
|
|
|
|
|
|
Number
|
|
|
Amount
|
|
|
Number
|
|
|
Amount
|
|
|
Additional
paid-in capital
|
|
|
Accumulated
currency
translation
adjustment
|
|
|
Number
|
|
|
Amount
|
|
|
Accumulated
loss
|
|
|
Total
|
|
Balance as of January 1, 2014
|
|
|
762
|
|
|
$
|
102,677
|
|
|
|
39
|
|
|
$
|
54
|
|
|
$
|
9,672
|
|
|
$
|
1
|
|
|
|
-
|
|
|
$
|
-
|
|
|
$
|
(118,674
|
)
|
|
$
|
(108,947
|
)
|
Net loss
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
(23,471
|
)
|
|
|
(23,471
|
)
|
Currency translation adjustment
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
(3,847
|
)
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
(3,847
|
)
|
Issuance of convertible debt
|
|
|
78
|
|
|
|
11,916
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
Preferred shares dividend
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
(4,069
|
)
|
|
|
(4,069
|
)
|
Share-based compensation
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
6,926
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
6,926
|
|
Conversion of preferred into common shares
|
|
|
(840
|
)
|
|
|
(114,593
|
)
|
|
|
840
|
|
|
|
1,138
|
|
|
|
113,455
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
114,593
|
|
Issue of common shares net of issue costs
|
|
|
-
|
|
|
|
-
|
|
|
|
624
|
|
|
|
828
|
|
|
|
59,914
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
60,742
|
|
Balance as of December 31, 2014
|
|
|
-
|
|
|
$
|
-
|
|
|
|
1,503
|
|
|
$
|
2,020
|
|
|
$
|
189,967
|
|
|
$
|
(3,846
|
)
|
|
|
-
|
|
|
$
|
-
|
|
|
$
|
(146,214
|
)
|
|
$
|
41,927
|
|
Balance as of January 1, 2015
|
|
|
-
|
|
|
$
|
-
|
|
|
|
1,503
|
|
|
$
|
2,020
|
|
|
$
|
189,967
|
|
|
$
|
(3,846
|
)
|
|
|
-
|
|
|
$
|
-
|
|
|
$
|
(146,214
|
)
|
|
$
|
41,927
|
|
Net loss
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
(50,856
|
)
|
|
|
(50,856
|
)
|
Currency translation adjustment
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
(4,460
|
)
|
|
|
-
|
|
|
|
-
|
|
|
|
|
|
|
|
(4,460
|
)
|
Change in functional currency*
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
(389
|
)
|
|
|
(37,591
|
)
|
|
|
7,062
|
|
|
|
-
|
|
|
|
-
|
|
|
|
30,918
|
|
|
|
-
|
|
Share-based compensation
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
3,982
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
3,982
|
|
Fair value movement on warrants exercised in the period
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
441
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
441
|
|
Issue of common shares net of issue costs
|
|
|
-
|
|
|
|
-
|
|
|
|
282
|
|
|
|
312
|
|
|
|
16,554
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
16,866
|
|
Balance as of December 31, 2015
|
|
|
-
|
|
|
$
|
-
|
|
|
|
1,785
|
|
|
$
|
1,943
|
|
|
$
|
173,353
|
|
|
$
|
(1,244
|
)
|
|
|
-
|
|
|
$
|
-
|
|
|
$
|
(166,152
|
)
|
|
$
|
7,900
|
|
Balance as of January 1, 2016
|
|
|
-
|
|
|
$
|
-
|
|
|
|
1,785
|
|
|
$
|
1,943
|
|
|
$
|
173,353
|
|
|
$
|
(1,244
|
)
|
|
|
-
|
|
|
$
|
-
|
|
|
$
|
(166,152
|
)
|
|
$
|
7,900
|
|
Net loss
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
(56,954
|
)
|
|
|
(56,954
|
)
|
Currency translation adjustment
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
(108
|
)
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
(108
|
)
|
Share-based compensation
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
8,547
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
8,547
|
|
Exchange of shares resulting from common control merger
|
|
|
-
|
|
|
|
-
|
|
|
|
21,866
|
|
|
|
(1,680
|
)
|
|
|
1,707
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
27
|
|
Common shares held in treasury at cost
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
25
|
|
|
|
(27
|
)
|
|
|
-
|
|
|
|
(27
|
)
|
Issue of common shares net of issue costs
|
|
|
-
|
|
|
|
-
|
|
|
|
6,097
|
|
|
|
61
|
|
|
|
37,358
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
|
|
37,419
|
|
Balance as of December 31, 2016
|
|
|
-
|
|
|
$
|
-
|
|
|
|
29,748
|
|
|
$
|
324
|
|
|
$
|
220,965
|
|
|
$
|
(1,352
|
)
|
|
|
25
|
|
|
$
|
(27
|
)
|
|
$
|
(223,106
|
)
|
|
$
|
(3,196
|
)
|
*For the year ended December 31, 2016 the Company changed its
functional currency from Euro to U.S. Dollar and adopted the U.S. Dollar as its reporting currency. The change in functional currency
has been applied prospectively and the change in reporting currency has been applied retrospectively. Gains and losses from these
translations are recognized in cumulative translation adjustment included in “Accumulated currency translation adjustment”.
Please refer to the “foreign currency transactions” accounting policy note for further detail.
See accompanying notes to consolidated
financial statements.
INNOCOLL HOLDINGS PLC
CONSOLIDATED
STATEMENTS OF CASH FLOWS
for the years ended December 31, 2016,
2015 and 2014
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Operating activities:
|
|
|
|
|
|
|
|
|
|
|
|
|
Net loss
|
|
$
|
(56,954
|
)
|
|
$
|
(50,856
|
)
|
|
$
|
(23,471
|
)
|
Adjustments to reconcile net loss to net cash used in operating activities:
|
|
|
|
|
|
|
|
|
|
|
|
|
Depreciation
|
|
|
414
|
|
|
|
348
|
|
|
|
535
|
|
Deferred income tax (credit)/expense
|
|
|
(388
|
)
|
|
|
269
|
|
|
|
-
|
|
Loss/(gain) on disposals of property, plant & equipment
|
|
|
8
|
|
|
|
-
|
|
|
|
(100
|
)
|
Share-based compensation
|
|
|
8,547
|
|
|
|
3,982
|
|
|
|
6,926
|
|
Foreign exchange gains
|
|
|
(1,508
|
)
|
|
|
(5,577
|
)
|
|
|
(6,452
|
)
|
Changes in assets and liabilities:
|
|
|
|
|
|
|
|
|
|
|
|
|
(Increase)/decrease in inventories
|
|
|
(595
|
)
|
|
|
(602
|
)
|
|
|
804
|
|
Increase in trade & other receivables
|
|
|
(405
|
)
|
|
|
(426
|
)
|
|
|
(164
|
)
|
Increase in prepaid expenses
|
|
|
(1,864
|
)
|
|
|
(3,381
|
)
|
|
|
(304
|
)
|
(Decrease)/increase in trade payables and accrued expenses
|
|
|
(906
|
)
|
|
|
9,078
|
|
|
|
(1,772
|
)
|
(Decrease)/increase in deferred revenue and defined benefit pension liability
|
|
|
(413
|
)
|
|
|
207
|
|
|
|
(1,052
|
)
|
(Decrease)/increase in warrant liability
|
|
|
(10,644
|
)
|
|
|
4,067
|
|
|
|
8,323
|
|
Increase in interest payable
|
|
|
2,221
|
|
|
|
71
|
|
|
|
-
|
|
Increase/(decrease) in income tax payable
|
|
|
16
|
|
|
|
9
|
|
|
|
(58
|
)
|
Net cash used in operating activities
|
|
|
(62,471
|
)
|
|
|
(42,811
|
)
|
|
|
(16,785
|
)
|
Investing activities:
|
|
|
|
|
|
|
|
|
|
|
|
|
Proceeds from disposals of property, plant and equipment
|
|
|
14
|
|
|
|
2
|
|
|
|
100
|
|
Purchases of property, plant and equipment
|
|
|
(12,445
|
)
|
|
|
(3,262
|
)
|
|
|
(1,208
|
)
|
Restricted cash
|
|
|
(187
|
)
|
|
|
-
|
|
|
|
-
|
|
Net cash used in investing activities
|
|
|
(12,618
|
)
|
|
|
(3,260
|
)
|
|
|
(1,108
|
)
|
Financing activities:
|
|
|
|
|
|
|
|
|
|
|
|
|
Proceeds from interest bearing loans & borrowings
|
|
|
11,240
|
|
|
|
16,331
|
|
|
|
-
|
|
Proceeds from issue of ordinary shares
|
|
|
39,937
|
|
|
|
18,755
|
|
|
|
60,398
|
|
Issuance costs allocated against share premium
|
|
|
(2,913
|
)
|
|
|
(2,027
|
)
|
|
|
(2,688
|
)
|
Proceeds from share options exercised
|
|
|
395
|
|
|
|
-
|
|
|
|
-
|
|
Proceeds from issue of preferred stock and convertible promissory notes
|
|
|
-
|
|
|
|
-
|
|
|
|
11,582
|
|
Net cash inflows from financing activities
|
|
|
48,659
|
|
|
|
33,059
|
|
|
|
69,292
|
|
Effect of foreign exchange rate changes on cash and cash equivalents
|
|
|
9
|
|
|
|
(184
|
)
|
|
|
270
|
|
Net (decrease)/increase in cash and cash equivalents
|
|
|
(26,421
|
)
|
|
|
(13,196
|
)
|
|
|
51,669
|
|
Cash and cash equivalents at the beginning of the year
|
|
|
42,186
|
|
|
|
55,382
|
|
|
|
3,713
|
|
Cash and cash equivalents at the end of the year
|
|
$
|
15,765
|
|
|
$
|
42,186
|
|
|
$
|
55,382
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
Supplemental cash flow information:
|
|
|
|
|
|
|
|
|
|
Interest paid
|
|
$
|
(4
|
)
|
|
$
|
(152
|
)
|
|
$
|
-
|
|
Income taxes paid
|
|
|
(543
|
)
|
|
|
(129
|
)
|
|
|
(260
|
)
|
Notes to the Consolidated Financial Statements
Note 1. Basis of Preparation and Significant
Accounting Policies
On March 16, 2016, Innocoll AG, a German stock corporation
(“Innocoll Germany”), the predecessor to Innocoll Holdings plc, a public limited company formed under Irish law (“Innocoll
Ireland”), merged with Innocoll Ireland by way of a European cross-border merger by acquisition, with Innocoll Germany being
the disappearing entity and Innocoll Ireland being the surviving entity (“the Merger”). By virtue of the Merger, all
of Innocoll Germany’s assets and operations (including all of its subsidiaries) were transferred to Innocoll Ireland for
all periods presented (see note 3 for additional information regarding the Merger). Accordingly, the consolidated financial information
presented herein refers to Innocoll Holdings plc and its direct and indirect subsidiaries, collectively, as the “Company”.
Nature of operations
Innocoll Holdings plc is a global, commercial stage,
specialty pharmaceutical company, with late stage development programs targeting areas of significant unmet medical need.
Basis of preparation
Prior to the Merger, Innocoll Germany prepared its financial
information in accordance with International Financial Reporting Standards (“IFRS”), and Innocoll Ireland was a dormant
Irish private company incorporated on May 28, 2014, that was reregistered as a public limited company on December 1, 2015.
Following the Merger, the Company retroactively transitioned
to accounting principles generally accepted in the United States (“U.S. GAAP”) and applied
U.S. GAAP retrospectively for all prior periods presented. The preparation of the consolidated financial statements in conformity
with U.S. GAAP requires management to make estimates and assumptions that affect the reported amount of assets and liabilities,
disclosure of contingent assets and liabilities and the reported amounts of revenues and expenses. Actual results may differ from
those estimates.
Basis of consolidation
The consolidated financial statements include the accounts
of the Company, its wholly-owned subsidiaries and entities in which they own or control more than fifty percent of the voting
shares, or have the ability to control through similar rights. Intercompany transactions and balances have been eliminated. An
entity is consolidated either if a controlling financial interest is obtained through ownership, directly or indirectly, of a
majority of an entity’s voting interests or a reporting entity is deemed to have a controlling financial interest when it
has both (1) the power to direct the activities that most significantly affect the economic performance of the entity and (2)
the obligation to absorb losses or the right to receive benefits of the entity that could potentially be significant to the entity.
The existence and effect of potential voting rights that are currently exercisable or convertible are considered when assessing
whether the Company controls another entity.
Subsidiaries
Subsidiaries are entities controlled by the Company. The financial
information of subsidiaries is included in the consolidated financial information from the date that control commences until the
date that control ceases. Details of the Company’s subsidiaries are included in note 21.
Foreign currency transactions
Functional and reporting currency
Functional currency - Prior to December
31, 2015, the Company’s functional currency was the Euro. The functional currency was revisited by the Company in late 2015
as a result of a significant increase in the level of U.S. dollar transactions in the third and fourth quarter of 2015. Upon detailed
analysis of all facts and circumstances it was determined based on relevant cash flows and the economic environment to change
the functional currency from the Euro to the U.S. dollar. The change in functional currency was applied prospectively effective
beginning January 1, 2016.
Reporting currency - In addition, beginning January 1, 2016
the Company also changed its reporting currency from Euro to U.S. dollar to provide greater clarity to users of the financial
statements. The change in reporting currency was applied retrospectively effective beginning January 1, 2016. Financial statements
for all periods presented have been recast into U.S. dollar.
All monetary assets and liabilities denominated in foreign
currencies are translated into U.S. dollars using exchange rates in effect as of the date of the balance sheet date. The U.S.
dollar translated amounts of nonmonetary assets and liabilities as of December 31, 2015 became the historical accounting basis
for those assets and liabilities as of December 31, 2015. Revenue and expense transactions are translated at the approximate exchange
rate in effect at the time of the transaction. All resulting exchange differences were recognized within currency translation
adjustment, a separate component of shareholders’ equity.
In applying the change in reporting currency the Company applied
the current rate method for presenting the comparative period presented. Under this method all assets and liabilities of the Company’s
operations were translated from their Euro functional currency into U.S. dollars using the exchange rates in effect on the balance
sheet date and shareholders’ equity were translated at the historical rates. Opening shareholders’ equity
at January 1, 2014 has been translated at the historic rate on that date and any other movements in shareholders’ equity
during the period from January 1, 2014 to December 31, 2015 were translated using the appropriate historical rates at the date
of the respective transaction. All other revenues, expenses and cash flows were translated at the average rates during the
reporting periods presented. The resulting translation adjustments are reported under comprehensive income as a separate component
of shareholders’ equity.
Any difference which arose between the historical basis for
nonmonetary assets and liabilities set as of January 1, 2016 and the historical basis for nonmonetary assets and liabilities due
to the change in reporting currency was posted to the currency translation adjustment in 2015.
In recasting the amounts presented in the consolidated statements
of (deficit)/equity for the purposes of the previously issued unaudited interim condensed consolidated financial
statements, an incorrect exchange rate was applied. As a result, the Company has revised the balances as of January 1, 2015 with
a net increase in total equity of $4.3 million from the amount previously presented in the unaudited interim condensed
financial statements. The line items impacted were common shares, additional paid-in capital, accumulated currency translation
adjustment and accumulated loss in the consolidated balance sheet and other consolidated comprehensive loss in the consolidated
statement of operations and comprehensive loss. This adjustment has no impact on our net loss for the year in any of the periods
presented and no impact on the previously issued annual financial statements. After evaluating the quantitative and qualitative
aspects of this revision, management concluded that the error was not material to the previously issued unaudited interim
condensed consolidated financial statements.
Transactions and balances
Transactions in currencies other than the functional currency
of the Company entities are recorded at the exchange rates prevailing at the dates of the related transactions. Foreign exchange
gains and losses resulting from the settlement of such transactions, as well as from the translation at year-end exchange rates
of monetary assets and liabilities denominated in foreign currencies, are recognized in the consolidated statements of operations
and comprehensive loss. At each balance sheet date, monetary assets and liabilities that are denominated in foreign currencies
are translated to the respective functional currencies of the Company’s entities at the rates prevailing on the relevant
balance sheet date.
Property, plant and equipment, net
Property, plant and equipment, net are carried at historical
cost less accumulated depreciation. Subsequent costs are included in the asset’s carrying amount or recognized as a separate
asset as appropriate only when it is probable that future economic benefits associated with the item will flow to the Company
and the cost of the item can be measured reliably. All other repair and maintenance costs are charged to the consolidated statements
of operations and comprehensive loss as incurred. The cost of assets retired or otherwise disposed of and the related accumulated
depreciation are recognized in the consolidated statements of operations and comprehensive loss as part of the gain or loss on
disposal in the year of disposal. Gains and losses on disposals of property, plant and equipment are included in operating expense.
Depreciation
Depreciation is calculated using the straight-line method to
allocate the cost of property, plant and equipment over their estimated useful lives, less their estimated residual values, as
follows:
Leasehold improvements
|
|
*
|
|
Plant and machinery
|
|
3 to 10 years
|
|
Furniture and fittings
|
|
5 years
|
|
* Leasehold improvements are amortized over the lesser of the
lease term or the estimated useful life of the related asset.
Depreciation methods, useful lives and residual values are
reassessed at each reporting date. Assets that are subject to amortization or depreciation are reviewed for impairment whenever
events or changes in circumstances indicate that the carrying amount may not be recoverable. An impairment loss is recognized
for the amount by which the asset’s carrying amount exceeds its recoverable amount.
Leased assets
Rentals payable under operating leases are charged to the consolidated
statements of operations and comprehensive loss on a straight-line basis over the relevant lease term.
Capitalized Interest
The interest cost associated with major development and construction
projects is capitalized and included in the cost of the project. Interest expense is capitalized at the applicable weighted-average
borrowing rates of interest and added to the project cost. Interest capitalization ceases once a project is substantially complete
or no longer undergoing construction activities to prepare it for its intended use.
Inventories
Inventories are stated at the lower of cost or market value.
The cost of inventories is based on the weighted average cost method and includes expenditure in acquiring the inventories and
bringing them to their existing location and condition. In the case of work in progress and finished goods, cost includes an appropriate
share of overhead based on normal operating capacity. Market is the current replacement cost, provided that the cost does not
exceed the Net Realizable Value (NRV) or is not less than the NRV reduced by a normal profit margin. NRV is the estimated selling
price in the ordinary course of business less reasonably predictable costs of completion and the estimated costs necessary to
make the sale.
Financial instruments
Non-derivative financial assets
Financial assets are initially recognized on the date they
are originated and when the Company obtains contractual rights to receive cash flows. The Company derecognizes financial assets
when the contractual rights to cash flows expire or it transfers the right to receive cash flows in a transaction which transfers
substantially all the risks and rewards of ownership of the asset.
Trade receivables
Such assets are initially recognized at fair value and subsequently
stated at their net realizable value. The carrying amounts of trade receivables are representative of their fair value due to
their relatively short maturities.
Prepaid expenses
Prepaid expenses consist of amounts paid in advance for which
the company will receive goods or services within the normal operating cycle. Such expense amounted to $5.5 million as of December
31, 2016 and $3.6 million as of December 31, 2015.
Included in this amount are expenses relating to costs for
clinical trials, NDA submission fees, rental deposits and other costs which have been paid in advance by the Company.
Cash and cash equivalents
Cash and cash equivalents are stated at cost, which approximates
fair value. Cash and cash equivalents comprise cash on hand and call deposits (with less than 3 months maturity) and are subject
to an insignificant risk of changes in value.
Warrants
Warrants are classified as a liability, due to certain provisions
pursuant to which the exercise price of the warrants may be reduced in the event that the Company issues or sells any of its ordinary
shares at a price per share less than the exercise price in effect immediately prior to such issue or sale.
The warrants are revalued each reporting period, and the change
in the fair value of the liability is recorded as other income/(expense), on the consolidated statements of operations
and comprehensive loss until the warrant is exercised or
cancelled. The fair value is calculated using a recognized
valuation methodology for the valuation of financial instruments (Monte Carlo simulation model).
Refer to note 16 for additional information on the Company’s
warrants.
Trade payables and other payables
The carrying amounts of trade payable and other payables are
representative of their fair value due to their relatively short maturities.
Equity instruments
Equity instruments issued by the Company are recorded at the
proceeds received, net of direct issue costs.
Temporary Equity
The Company accounted for warrants in accordance with Accounting
Standards Codification (“ASC”) 470, Debt, and allocated proceeds received to the warrants based on relative fair values.
The Company previously issued convertible notes and preferred
shares which provided a liquidation preference and certain redemption rights for the benefit of the holders of such instruments
upon the occurrence of certain events, some of which were not within the Company’s control. On June 16, 2014, the Company’s
shareholders agreed to amend and terminate all preference, redemption and cumulative dividend rights by converting all preferred
shares into ordinary shares of the Company. Prior to the conversion, the convertible Preferred Stock is presented as temporary
equity.
The Company evaluated each series of its convertible preferred
stock and preferred units and determined that each individual series is considered an equity host under ASC 815. In making this
determination, the Company’s analysis followed the whole instrument approach which compares an individual feature against
the entire convertible instrument which includes that feature. The Company’s analysis was based on a consideration of the
economic characteristics and risks of each series of convertible units. More specifically, the Company evaluated all of the stated
and implied substantive terms and features, including: (i) whether the convertible preferred stock and preferred units included
redemption features, (ii) how and when any redemption features could be exercised, (iii) whether the holders of convertible preferred
stock and preferred units were entitled to dividends and how those dividends were calculated, (iv) the voting rights of the convertible
preferred stock and preferred units and (v) the existence and nature of any conversion rights. As a result of the Company’s
conclusion that the convertible instruments represent an equity host, the conversion rights of all series of convertible instruments
were considered to be clearly and closely related to the associated equity host instruments. Accordingly, the conversion rights
of all series of convertible preferred stock were not considered embedded derivatives that required bifurcation.
The Company has also evaluated whether the issuance of the
convertible instruments generates a beneficial conversion feature (“BCF”), which arises when a debt or equity security
is issued with an embedded conversion option that is beneficial to the investor or in the money at inception because the conversion
option has an effective strike price that is less than the market price of the underlying stock at the commitment date. The Company
would recognize the BCF by allocating the intrinsic value of the conversion option, which is the number of ordinary shares available
upon conversion multiplied by the difference between the effective conversion price per share and the fair value of each ordinary
share on the commitment date, to additional paid-in capital, resulting in a discount on the convertible preferred shares. No BCF
has been recognized in the periods presented.
Contingencies
Contingencies are recognized in accordance with ASC 450 - Contingencies,
if the following two conditions are met:
|
·
|
Information
available before the financial statements are issued indicates that it is probable that
an asset had been impaired or a liability had been incurred at the date of the financial
statements;
|
|
·
|
The amount
of loss can be reasonably estimated.
|
With respect to litigation and claims that may result in a
provision to be recognized, the Company exercises judgment in measuring and recognizing provisions or determining exposure to
contingent liabilities that are related to pending litigation or other outstanding claims. These judgment and estimates are subject
to change as new information becomes available.
Employee benefit plans
Pension plans
The Company operates a number of defined contribution retirement
benefit plans, the assets of which are held in separate trustee-administered funds. Payments to defined contribution benefit plans
are charged as an expense to the statement of operations and comprehensive loss as they fall due.
The Company operates a defined benefit pension plan within
its German subsidiary. A defined benefit plan is a pension plan that is not a defined contribution plan. Typically defined benefit
plans define the amount of pension benefit that an employee will receive on retirement, usually dependent on one or more factors
such as age, years of service and compensation. Obligations for contributions to defined benefit pension plans are recognized
as an expense in the income statement as service is received from the relevant employees.
Share-based compensation
The Company issues stock-based awards, including stocking options
and restricted stock units, to employees and non-employee directors.
Stock-based awards issued to employees, including stock options,
are recorded at fair value as of the grant date using the Black-Scholes valuation model and recognized as expense on a straight-line
basis over the employee’s requisite service period, adjusted for estimated forfeitures.
Measurement of share-based payment transactions with non-employees
is based on the fair value of whichever is more reliably measurable: (a) the goods or services received; or (b) the equity
instruments issued. The fair value of the share-based payment transaction is determined at the earlier of performance commitment
date or performance completion date.
The Company from time to time has granted restricted stock
units (“RSUs”) to individual employees and non-employee directors. The employees purchase the stock at an agreed price
which may be below the then fair value of the stock unit. The difference between the purchase price and the fair value is expensed
over the vesting period of the restricted stock unit.
RSUs granted to non-employee directors (“Director RSUs”)
vest between one to three years following the grant date but may not be settled until the director terminates service from the
board. Compensation cost is recognized over the one year service period. Director RSUs may be settled in cash and/or shares of
stock and are accounted for under the liability method of accounting. Fair value is based on the market price of the underlying
stock on the grant date, and compensation expense is adjusted for changes in fair value at each report date through the settlement
date.
The assumptions used in measuring the fair value of the stock
granted, using the Black Scholes model were determined as follows:
|
·
|
Prior to the
shares being publicly traded, the current market value of shares was based on the valuation
of the Company by the managing directors at the share option grant date;
|
|
·
|
Subsequent
to the shares being publically traded, the current market value of shares was based on
the share price at the share option grant date;
|
|
·
|
The estimated
volatility is based on the historical volatility of biotech companies that operate in
the same therapeutic areas as the Company, or that are of a similar size;
|
|
·
|
The expected
duration is calculated as the estimated duration until exercise, taking into account
the specific features of the plans; and
|
|
·
|
The weighted
average risk-free interest rates used are based on government treasury bills at the date
of grant with a term equal to the expected life of the options.
|
Revenue recognition
The Company recognizes revenue from product sales upon
shipment, when there is persuasive evidence that an arrangement exists, title to product and associated risk of loss has
transferred to the customer, the price is fixed or determinable, collectability is reasonably assured and the Company has no
further performance obligations. The shipping terms for the majority of the Company’s revenue arrangements are
“free carrier” (“FCA”). Shipping costs are insignificant.
The Company receives a contractually agreed percentage of the
net in-market sales of CollatampG from one of its customers which distributes the product. The Company recognizes revenue for
this arrangement in two parts; the first amount is recognized for the manufacture and sale of product at the point of sale; and
the final amount when the product is sold.
Provisions for certain rebates, sales incentives, product returns
and discounts to customers are accounted for as reductions in sales in the same period the related sales are recorded.
Deferred revenue is calculated when cash is received from a
customer for a product which at the time of receipt has not yet been delivered. The Company had deferred revenue in the amount
of $1.8 million and $2.2 million as of December 31, 2016 and 2015, respectively, relating to upfront payments in the amount of
$0.1 million in respect of Septocoll customers (2015: $0.5 million), $1.2 million in respect of CollaGUARD (2015: $1.3 million)
and the remaining $0.5 million mainly relating to its Regenepro product (2015: $0.4 million). The Company expects to deliver products
to these customers in 2017 in settlement of these advance payments.
Expenses
Research and development expenses
Research and development expenses are charged to the consolidated
statements of operations and comprehensive loss as incurred. Research and development expenses comprise costs incurred in
performing research and development activities, including employee compensation, external clinical research costs, and general
operating costs.
Interest expense and income
Interest expense consists of interest payable on borrowings
and interest income consists of interest receivable on funds invested. Both are calculated using the effective interest rate method.
Other income and expense
Gains or losses from foreign exchange rate
fluctuations on balances demoninated in foreign currencies are reflected in other income/expense, net. This includes foreign
exchange movements recognised on items such as foreign denominated cash and cash equivalents, loans and borrowings, payables,
receivables among other items and transactions. This also includes movements on the re-measurement of the warrant liabilities
at each period end.
Income taxes
Tax expense comprises current and deferred tax.
Current tax is the expected tax payable or receivable on the
taxable result for the year and any adjustments in relation to tax payable or receivable in respect of the previous years.
Deferred tax is recognized in respect of temporary differences
between the carrying amounts of assets and liabilities for financial reporting purposes and the amounts used for taxation purposes.
Deferred tax is not recognized for:
|
·
|
temporary differences
on the initial recognition of assets and liabilities in a transaction that is not a business
combination and that affects neither accounting nor taxable profit; and
|
|
·
|
temporary differences
related to subsidiaries to the extent that it is probable that they will not reverse
in the foreseeable future.
|
Deferred tax is measured at the tax rates at which the temporary
differences are expected to reverse, using tax rates enacted or substantively enacted at the reporting date. Deferred tax assets
and liabilities are offset where the entity has a legally enforceable right to set off current tax assets against current tax
liabilities and the deferred tax assets and liabilities relate to the same taxation authority. The Company maintains valuation
allowances unless it is more likely than not that the deferred tax asset will be realized. With respect to uncertain tax positions,
the Company determines whether the position is more likely than not to be sustained upon examination, based on the technical merits
of the position. Any tax position that meets the more likely than not recognition threshold is measured and recognized in the
consolidated financial statements at the largest amount of benefit that is greater than 50% likely of being realized upon ultimate
settlement. The liability relating to uncertain tax positions is classified as current in the consolidated balance sheets to the
extent the Company anticipates making a payment within one year. Interest and penalties associated with income taxes are classified
in the income tax expense line in the consolidated statements of operations and comprehensive loss.
Deferred tax assets and deferred tax liabilities are off-set
where they are within the same jurisdiction and can be legally off-set with each other.
Government Grants
Grants for the purchase of plant and equipment are recognized
as receivable when there is reasonable assurance that they will be received and the conditions to obtain them have been complied
with. Grants are initially credited to deferred income and released to profit and loss over the same useful life as the plant
and equipment they relate to.
Loss per ordinary share
Basic loss per share is computed by dividing the loss for the
financial period attributable to ordinary shareholders of the Company by the weighted average number of ordinary shares outstanding
during the financial period.
Diluted loss per share is computed by dividing the loss for
the financial period attributable to ordinary shareholders of the Company by the weighted average number of ordinary shares in
issue after adjusting for the effects of all potential dilutive ordinary shares that were outstanding during the financial period.
Critical accounting estimates
In preparing the consolidated financial statements, we use
certain estimates and assumptions that affect reported amounts and disclosures. Estimates are reviewed on an ongoing basis. Estimates
and judgments are based on historical experience and on other factors that are reasonable under current circumstances. Actual
results may differ from these estimates if these assumptions prove to be incorrect or if conditions develop other than as assumed
for the purposes of such estimates.
Recent Accounting Pronouncements
Accounting Standard Update (“ASU”) 2014-09
,
“Revenue from Contracts with Customers.”
In May 2014, the Financial Accounting Standards Board (“FASB”)
issued guidance for revenue recognition for contracts, superseding the previous revenue recognition requirements, along with most
existing industry-specific guidance. The guidance requires an entity to review contracts in five steps:
1) identify the contract;
2) identify performance obligations;
3) determine the transaction price;
4) allocate the transaction price; and
5) recognize revenue.
The ASU will result in enhanced disclosures regarding
the nature, amount, timing, and uncertainty of revenue arising from contracts with customers.
For public business entities, certain not-for-profit
entities, and certain employee benefit plans, the effective date for ASC 606 is annual reporting periods (including interim reporting
periods within those periods) beginning after December 15, 2017. Early application is permitted only as of annual reporting periods
(including interim reporting periods within those periods) beginning after December 15, 2016. The effective date for all other
entities is annual reporting periods beginning after December 15, 2018, and interim reporting periods within annual reporting
periods beginning after December 15, 2019. All other entities may apply the ASU early, as of an annual reporting period beginning
after December 15, 2016, including interim reporting periods within that reporting period. All other entities also may apply ASC
606 early as of an annual reporting period beginning after December 15, 2016, and interim reporting periods within annual reporting
periods beginning one year after the annual reporting period in which the entity first applies ASC 606. The company intends to
adopt the standard for annual periods beginning after December 15, 2018, and interim reporting periods within annual reporting
periods beginning after December 15, 2019.
The Company is currently establishing an implementation
process to complete an initial assessment as to the impact of the standard on its contract portfolio and to commence implementing
the ASU. The Company will select a representative sample of its contracts to review to identify the potential differences that
would result from applying the requirements of the new standard and base its initial assessment on this process. Once completed
the Company will complete a final assessment of the impact of the ASU and determine whether or not it will have a material impact
on the Company’s financial statements and select its method of adoption at that time. The ASU provides detailed disclosure
requirements, which are more detailed than under current U.S. GAAP. This will represent a significant change from current practice
and significantly increase the volume of disclosures required in the financial statements. The Company expects to complete its
impact assessment over the coming months and initiate efforts to redesign impacted processes, policies and controls.
ASU 2014-15, “Presentation of Financial Statements-Going Concern
.”
In
August 2014, the FASB issued guidance for the disclosure of uncertainties about an entity’s ability to continue as a going
concern. Under U.S. GAAP, continuation of a reporting entity as a going concern is presumed as the basis for preparing financial
statements unless and until the entity’s liquidation becomes imminent. Preparation of financial statements under this presumption
is commonly referred to as the going concern basis of accounting. Previously, there was no guidance in U.S. GAAP about management’s
responsibility to evaluate whether there is substantial doubt about an entity’s ability to continue as a going concern or
to provide related footnote disclosures. This was issued to provide guidance in U.S. GAAP about management’s responsibility
to evaluate whether there is substantial doubt about an entity’s ability to continue as a going concern and to provide related
footnote disclosures. In doing so, the amendments should reduce diversity in the timing and content of footnote disclosures. The
amendments in this update are effective for the annual period ending after December 15, 2016, and for annual periods and interim
periods thereafter for all entities both public and nonpublic. The Company has applied this ASU in its current year’s consolidated
financial statements and disclosures.
ASU 2015-11
,
“Simplifying the Measurement of
Inventory.”
In July 2015 FASB issued this ASU in relation to Topic 330 “Inventory.” Under the amendment,
an entity should measure inventory within the scope of the ASU at the lower of cost and net realizable value. Net realizable value
is the estimated selling prices in the ordinary course of business, less reasonably ppredictable costs of completion, disposal,
and transportation. Subsequent measurement is unchanged for inventory measured using last in, first out (“LIFO”) or
the retail inventory method. The amendments in this ASU more closely align the measurement of inventory in U.S. GAAP with the
measurement of inventory in IFRS. The ASU is effective for public business entities for annual periods beginning after December
15, 2016, and interim periods therein. For all other entities the amendments in this Update are effective for annual periods beginning
after December 15, 2016, and interim periods within annual periods beginning after December 15, 2017. Prospective application
is required. The Company is currently assessing the impact of this ASU on its inventory balances and it is not expected to have
a material impact on the Company’s consolidated financial statements. The Company intends to adopt the standard for annual
periods beginning after December 15, 2016, and interim periods within annual periods beginning after December 15, 2017.
ASU 2015-17, “Income Taxes (Topic 740): Balance Sheet
Classification of Deferred Taxes.”
In November 2015, the FASB issued ASU 2015-17. This ASU which requires that
deferred tax liabilities and assets be classified as noncurrent in a balance sheet. The ASU is effective for public companies
for annual periods beginning after December 15, 2016; however, earlier application is permitted. For all other entities, the amendments
in this Update are effective for annual periods beginning after December 15, 2017, and interim periods within annual periods beginning
after December 15, 2018.Additionally, the ASU allows for both retrospective and prospective methods of transition upon adoption.
The Company early adopted this ASU in the fourth quarter of 2016. The ASU was adopted retrospectively and, as a result, the consolidated
balance sheet as of December 31, 2015 was adjusted. The December 31, 2015 current deferred income tax liabilities of $263 thousand
was reclassified as non-current. There was no effect to the Company’s equity or to the consolidated statements of operations
and comprehensive loss as a result of this adoption.
ASU 2016-02, “Leases.” In February 2016, the
FASB issued ASU 2016-02. This ASU requires lessees to put most leases on their balance sheets but recognize expenses in the income
statement in a manner similar to current accounting treatment. This ASU changes the guidance on sale-leaseback transactions,
initial direct costs and lease execution costs, and, for lessors, modifies the classification criteria and the accounting for
sales-type and direct financing leases. This ASU is effective for public entities for annual periods beginning after December
15, 2018, and interim periods therein. For all other entities, the ASU will be effective for annual periods beginning after
December 15, 2019 (i.e., calendar periods beginning on January 1, 2020), and interim periods thereafter. Early adoption will be
permitted for all entities. Entities are required to use a modified retrospective approach for leases that exist or are entered
into after the beginning of the earliest comparative period in the financial statements. There are also some practical expedients
available. The Company is in the process of determining the effect that the adoption of this standard will have on its financial
statements and disclosures. The Company currently expects that most of its operating lease commitments will be subject to the
new standard and recognized as lease liabilities and right-of-use assets upon its adoption of ASU 2016-02. The Company intends
to adopt the standard for annual periods beginning after December 15, 2019 (i.e., calendar periods beginning on January 1, 2020),
and interim periods thereafter.
ASU 2016-09, “Improvements to Employee Share-Based Payment Accounting.
”
In
March 2016, the FASB issued ASU 2016-09. This ASU simplifies several aspects of the accounting for share-based payment transactions,
including the income tax consequences, classification of awards as either equity or liabilities, and classification on the statement
of cash flows. The ASU is effective for public entities for annual periods beginning after December 15, 2016, although early
adoption is permitted. For all other entities, the ASU is effective for annual reporting periods beginning after December
15, 2017, and interim periods within annual reporting periods beginning after December 15, 2018. The Company is currently evaluating
the impact of this ASU on its financial statements and disclosures. The Company intends to adopt the standard for annual periods
beginning after December 15, 2017, and interim periods within annual reporting periods beginning after December 15, 2018.
ASU 2016-15, “Statement of Cash Flows
.”
In August 2016, the FASB issued ASU 2016-15. The amendments in the ASU provide guidance for several new and/or revised disclosures
pertaining to the classification of certain cash receipts and cash payments on the statement of cash flows, including contingent
consideration payments made after a business acquisition. This ASU is effective for public business entities for annual periods
beginning after December 15, 2017, and interim periods therein. For all other entities the amendments in this Update are effective
for annual periods beginning after December 15, 2018, and interim periods within annual periods beginning after December 15, 2019.
Early adoption is permitted. The Company is currently evaluating the impact of this ASU on its financial statements but does not
anticipate a material impact. The Company intends to adopt the standard for annual periods beginning after December 15, 2018,
and interim periods within annual periods beginning after December 15, 2019.
ASU 2016-18
“Statement of Cash Flows
.”
In November 2016, the FASB issued ASU 2016-18. This amendment affects the cash flow statement and requires companies to include
items described as restricted cash and restricted cash equivalents in cash and cash equivalents when reconciling beginning-of-period
and end-of-period total amounts shown on the statement of cash flows. This ASU is effective for public entities for annual periods
beginning after December 15, 2017, and interim periods within those annual periods. For all other entities the amendments in this
Update are effective for annual periods beginning after December 15, 2018, and interim periods within annual periods beginning
after December 15, 2019. Early adoption is permitted, including adoption in an interim period. The Company currently shows movements
in restricted cash as an investing cash flow, however, as a result of this ASU it will be shown in the movement in cash and cash
equivalent. The Company intends to adopt the standard for annual periods beginning after December 15, 2018, and interim periods
within annual periods beginning after December 15, 2019.
ASC 2017-04, “
Intangibles - Goodwill and Other
Topics (Topic 350): Simplifying the Test for Goodwill Impairment.”
In January 2017, the FASB issued ASC 2017-04. The
purpose of this ASU is to reduce the cost and complexity of evaluating goodwill for impairment. It eliminates the need for entities
to calculate the impaired fair value of goodwill by assigning the fair value of a reporting unit to all of its assets and liabilities
as if that reporting unit had been acquired in a business combination. Under this ASU, an entity will perform its goodwill impairment
test by comparing the fair value of a reporting unit with its carrying amount. An impairment charge is recognized for the amount
by which the carrying value exceeds the reporting unit's fair value. The update is effective for public business entities for
annual periods beginning after December 15, 2019, including interim periods within those periods. All other entities, that are
adopting the amendments in this Update should do so for their annual or any interim goodwill impairment tests in annual periods
beginning after December 15, 2021.Early adoption is permitted for interim or annual goodwill impairment tests performed on testing
dates after January 1, 2017. The Company is currently assessing whether or not to early adopt this proposed amendment.
The Company has reviewed all other recently issued, but
not yet adopted, accounting standards in order to determine their effects, if any, on its results of operation, financial position
and cash flows. Based on that review, the Company believes that none of these pronouncements will have a significant effect
on its current or future earnings or operations.
The planned adoption dates for all standards not yet implemented are based on the Company’s current
classification as an Emerging Growth Company. Section 107 of the JOBS Act provides that an emerging growth company can take advantage
of the extended transition period as noted in Section 7(a)(2)(B) of the Securities Act for complying with new or revised accounting
standards. If this classification changes, we will re-valuate our timeline for implementing these standards.
Note 2. Going concern
The accompanying financial statements have been prepared assuming
that the Company will continue as a going concern. The Company generated net losses of $57.0 million in 2016, $50.9 million in
2015 and $23.5 million in 2014. In management’s opinion, the Company’s anticipated expenditures during the next 12
months, from date of approval of the financial statements, to advance its current operations, including plans to conduct
further studies to enable it to submit a revised NDA for Xaracoll and to develop CollaGUARD will be greater than the amount of
its current cash and cash equivalents. This raises substantial doubt about the Company’s ability to continue as a going
concern.
In February 2017, our representatives attended a Type-A meeting
with representatives of the FDA to review potential pathways forward following our receipt of the Refusal to File Letter and to
review a proposed plan for proceeding with additional studies that would allow us to file a revised NDA for XaraColl. During the
meeting, we proposed a plan designed to allow us to submit a revised NDA to the FDA by the latter part of 2017. We proposed conducting
an additional short-term pharmacokinetic study and several short-term non-clinical studies. Under current practice before the FDA,
we received limited feedback during the meeting and we expect to receive shortly from the representatives of the FDA formal written
meeting minutes of our Type-A meeting, which will serve as the official record of the response of the FDA to our proposal during
the meeting. If the FDA concurs with our plan, we will commence the additional studies, and if the results are positive, we would
submit a revised NDA to the FDA soon after the completion of the studies. However, if the FDA suggests that studies beyond those
that we proposed would be necessary, or if the results of the studies that we proposed are not positive, we would not likely be
able to submit our revised NDA for an extended period of time, if at all.
The Company’s need for additional capital will vary depending
on a variety of circumstances, including, for example, if it is required to conduct additional tests not currently contemplated,
the level and timing of regulatory approval, as well as the extent to which it chooses to establish collaboration, co-promotion,
distribution or other similar agreements for its products and product candidates. Moreover, changing circumstances may cause it
to spend cash significantly faster than it currently anticipates, and it may need to spend more cash than currently expected because
of circumstances beyond its control.
The Company’s operating cash and capital requirements, as currently
contemplated, over the next 12 months will depend on many forward-looking factors, including the following:
|
·
|
the timing and
outcome of the FDA’s review of the revised NDA for XaraColl;
|
|
|
|
|
·
|
successful completion
of additional short-term clinical trials and non-clinical studies in anticipation of
filing a revised NDA for XaraColl with the FDA;
|
|
|
|
|
·
|
the extent to
which the FDA may require it to perform additional studies for XaraColl;
|
|
|
|
|
·
|
the timing and
costs to initiate pre-commercialization activities for Xaracoll;
|
|
|
|
|
·
|
the cost and
timing of ensure its manufacturing facilities is ready for commercialization after the
pre-approval inspection;
|
|
|
|
|
·
|
the extent to
which it chooses to establish collaboration, co-promotion, distribution or other similar
agreements for its product candidates; and
|
|
|
|
|
·
|
the costs of
preparing, submitting and prosecuting patent applications and maintaining, enforcing
and defending intellectual property claims.
|
To the extent that the Company’s capital resources are insufficient
to meet our future operating and capital requirements, we will need to finance our cash needs through public or private equity
offerings, debt financings, corporate collaboration and licensing arrangements, other strategic alliances or other financing alternatives.
Note 3. Explanation of Transition to U.S. GAAP
As discussed in note 1, following the Merger, the Company retroactively
transitioned to U.S. GAAP and applied U.S. GAAP retrospectively for
all prior periods presented.
This is the first period that the Company has presented its
consolidated financial statements under U.S. GAAP. The Company’s most current financial statements under IFRS were for the
year ended December 31, 2015, and the Company has presented the historical financial statements of Innocoll Germany, beginning
as of January 1, 2015, according to U.S. GAAP for purposes of comparing prior periods.
Note 4. Description of Merger
On March 16, 2016, the Company became the parent company of
the Innocoll group of companies as a result of the Merger. As a result of the Merger:
|
•
|
All assets and liabilities of Innocoll AG were transferred
by universal succession of title to the Company;
|
|
•
|
Innocoll AG ceased to exist;
|
|
•
|
Each shareholder received, as consideration in the Merger,
13.25 Innocoll Holdings plc ordinary shares for each Innocoll AG ordinary share held
immediately prior to the Merger, rounded down to the nearest whole Innocoll Holdings
plc ordinary share;
|
|
•
|
Aggregated entitlements to fractional Innocoll Holdings
plc ordinary shares were sold by the exchange agent and sale proceeds were distributed
in cash pro rata to registered shareholders whose fractional entitlements were sold;
|
|
•
|
The Innocoll AG American Depositary Share (“ADS”)
facility was terminated and holders of ADSs had their ADSs cancelled with each ADS so
cancelled effectively becoming exchangeable, for one Innocoll Holdings plc ordinary share;
|
|
•
|
Each share of Innocoll AG was cancelled and ceased to
exist; and
|
|
•
|
The Company assumed all rights and obligations of Innocoll
AG (including the employee equity-based plans of Innocoll AG) by operation of law.
|
It was determined that Innocoll AG and the Company meet the
definition of entities under common control, consequently, the provisions of ASC 805-50-30-5 were applied in preparation of the
consolidated financial information as a common control transaction and accounted for at the carrying amount of assets, liabilities
and equity transferred, rather than at fair value.
Note 5. Segment reporting
Due to the nature of the Company’s current activities,
the directors consider there to be one operating segment, the manufacture and sale of collagen-based pharmaceutical products.
The Company principally sells four products; CollatampG globally outside of the United States, Septocoll within Europe and the
Middle East, CollaGUARD within Europe, the Middle East and Asia and RegenePro in the United States. The results of the Company
are reported on a consolidated basis to the chief operating decision maker of the Company, the chief executive officer. There
are no reconciling items between the Company’s reported consolidated statements of operation and comprehensive loss and
balance sheets and the results and financial position, respectively, of the above segment.
The majority of the product revenue, $4.2 million, relates
to sales of CollatampG and Septocoll and is split between two customers; for the year ended December 31, 2016 the split was 90%
and 10% respectively. Revenues from one customer represents approximately $3.8 million of the Company’s consolidated revenues.
The distribution of revenue by customers’ geographical
area was as follows:
|
|
For
the Years Ended December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
France
|
|
$
|
2,046
|
|
|
$
|
2,048
|
|
|
$
|
3,433
|
|
Germany
|
|
|
611
|
|
|
|
38
|
|
|
|
1,366
|
|
Netherlands
|
|
|
429
|
|
|
|
329
|
|
|
|
307
|
|
United Kingdom
|
|
|
580
|
|
|
|
40
|
|
|
|
-
|
|
Europe - other
|
|
|
584
|
|
|
|
236
|
|
|
|
660
|
|
Middle East
|
|
|
65
|
|
|
|
-
|
|
|
|
-
|
|
Asia
|
|
|
16
|
|
|
|
47
|
|
|
|
116
|
|
United States
|
|
|
41
|
|
|
|
132
|
|
|
|
92
|
|
Total revenue
|
|
$
|
4,372
|
|
|
$
|
2,870
|
|
|
$
|
5,974
|
|
The Company attributes revenue from external customers to individual
countries based on product shipment destination.
All non-current assets are located in Germany, Ireland and
the United States. As of December 31, 2016, 2015 and 2014, $16.5 million, $4.1 million and $1.3 million, respectively, of property,
plant and equipment, net is located in Germany. Property, plant and equipment, net within any other individual country was less
than ten percent of the Company’s consolidated property, plant and equipment, net in each of those years.
Note 6. Research and development expenses
|
|
For
the Years Ended December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Employee compensation
|
|
$
|
2,829
|
|
|
$
|
2,440
|
|
|
$
|
1,986
|
|
External clinical research costs
|
|
|
34,774
|
|
|
|
26,394
|
|
|
|
1,890
|
|
General operating costs
|
|
|
1,112
|
|
|
|
987
|
|
|
|
444
|
|
Total research and development expenses
|
|
$
|
38,715
|
|
|
$
|
29,821
|
|
|
$
|
4,320
|
|
Research and development expenses include labor, materials
and direct overheads associated with the various research programs.
Note 7. General and administrative expenses
|
|
For
the Years Ended December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Employee compensation
|
|
$
|
6,107
|
|
|
$
|
5,414
|
|
|
$
|
3,624
|
|
Depreciation
|
|
|
414
|
|
|
|
348
|
|
|
|
535
|
|
Share based compensation
|
|
|
8,547
|
|
|
|
3,982
|
|
|
|
6,926
|
|
Other
|
|
|
10,378
|
|
|
|
9,999
|
|
|
|
4,526
|
|
Total general and administrative expenses
|
|
$
|
25,446
|
|
|
$
|
19,743
|
|
|
$
|
15,611
|
|
Note 8. Other income/(expense)
|
|
For
the Years Ended December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Foreign exchange gain
|
|
$
|
1,545
|
|
|
$
|
5,631
|
|
|
$
|
6,290
|
|
Warrant income/(expense)
|
|
|
10,644
|
|
|
|
(4,067
|
)
|
|
|
(8,323
|
)
|
Other expense
|
|
|
(2
|
)
|
|
|
-
|
|
|
|
(10
|
)
|
Total other income/(expense)
|
|
$
|
12,187
|
|
|
$
|
1,564
|
|
|
$
|
(2,043
|
)
|
The foreign exchange gain net was $1.5 million in 2016, $5.6
million in 2015 and $6.3 million in 2014.
The warrant income/(expense), net arises on the change in the
fair value of the liability of the warrants following re-measurement at each period end.
Note 9. Loss per share
The Company calculates basic EPS by dividing the net loss attributable
to ordinary shareholders for the period by the weighted average number of ordinary shares outstanding during the period. The Company
calculates diluted EPS by dividing the net loss attributable to ordinary shareholders for the period by the weighted average number
of ordinary shares and dilutive instruments outstanding during the period. The Company has RSUs and other stock awards which have
been granted to eligible employees. These awards may have a potential dilutive effect if exercised.
The weighted average number of ordinary shares (denominator
- basic) amounted to 26,867,343 in 2016, 22,328,908 in 2015 and 9,744,255 in 2014. The weighted average number of ordinary shares
have been adjusted to reflect the effect of the Merger. The below table presents the basic and diluted EPS:
|
|
For
the Years Ended December 31,
|
|
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Numerator - Thousands of Dollars:
|
|
|
|
|
|
|
|
|
|
|
|
|
Net loss - basic and diluted
|
|
$
|
(56,954
|
)
|
|
$
|
(50,856
|
)
|
|
$
|
(23,471
|
)
|
|
|
|
|
|
|
|
|
|
|
|
|
|
Denominator - number of shares:
|
|
|
|
|
|
|
|
|
|
|
|
|
Weighted-average shares outstanding - basic and diluted
|
|
|
26,867,343
|
|
|
|
22,328,908
|
|
|
|
9,744,255
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
Loss per share:
|
|
|
|
|
|
|
|
|
|
|
|
|
Basic and diluted
|
|
$
|
(2.12
|
)
|
|
$
|
(2.28
|
)
|
|
$
|
(2.41
|
)
|
The basic loss per share was $2.12 in 2016, $2.28 in
2015 and $2.41 in 2014.
For the purpose of calculating diluted loss per share for the
year ended December 31, 2016 and 2015 the potentially exercisable instruments in issue would have the effect of being antidilutive
and, as such, the diluted loss per share is the same as the basic loss per share for those periods.
Note 10. Trade and other receivables, net
|
|
As
of December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
Trade receivables, net
|
|
$
|
320
|
|
|
$
|
560
|
|
VAT receivable
|
|
|
1,030
|
|
|
|
385
|
|
Total trade and other receivables, net
|
|
$
|
1,350
|
|
|
$
|
945
|
|
There was no allowance for doubtful accounts against trade
receivables as of December 31, 2016. The allowance for doubtful accounts against trade receivables was $0.04 million as of December
31, 2015.
Note 11. Inventories
|
|
As
of December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
Raw materials
|
|
$
|
920
|
|
|
$
|
694
|
|
Work in progress
|
|
|
1,266
|
|
|
|
960
|
|
Finished goods
|
|
|
217
|
|
|
|
154
|
|
Total inventories
|
|
$
|
2,403
|
|
|
$
|
1,808
|
|
The market value of inventory does not differ materially from
its carrying value. The Company’s allowance for obsolete and excess inventory was $0.3 million as of December 31, 2016 and
$0.4 million as of December 31, 2015. For the years ended December 31, 2016, 2015 and 2014, raw materials, changes in work and
progress and finished goods included in cost of sales amounted to $7.0 million, $5.3 million and $7.4 million, respectively.
Note 12. Property, plant and equipment, net
|
|
As
of December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
Leasehold improvements
|
|
$
|
10,752
|
|
|
$
|
2,087
|
|
Plant and machinery
|
|
|
16,558
|
|
|
|
13,791
|
|
Furniture and fittings
|
|
|
3,253
|
|
|
|
1,856
|
|
Property, plant and equipment, gross
|
|
|
30,563
|
|
|
|
17,734
|
|
Less: accumulated depreciation
|
|
|
(13,865
|
)
|
|
|
(13,535
|
)
|
Total property, plant and equipment, net
|
|
$
|
16,698
|
|
|
$
|
4,199
|
|
Depreciation expense was $0.4 million in 2016, $0.3 million
in 2015 and $0.5 million in 2014.
Included in property, plant and equipment are assets under
construction, which relate to the manufacturing facility in Germany. Assets under construction are stated at cost. No provision
for depreciation is made on these assets until such time as the relevant assets are completed and put into use. As of December
31, 2016 and 2015, the Company incurred and capitalized assets under construction of $10.3 million and $2.9 million, respectively.
No impairment of plant and machinery were recorded in 2016
and 2015.
The Company disposed of property, plant and equipment with
a cost of $0.1 million in 2016.
Note 13. Taxation
Income tax
The domestic (Ireland) and international components of income
from loss before income taxes were:
|
|
For
the Years Ended December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Domestic
|
|
$
|
(57,750
|
)
|
|
$
|
(52,118
|
)
|
|
$
|
(24,967
|
)
|
International
|
|
|
967
|
|
|
|
1,669
|
|
|
|
1,698
|
|
Total
|
|
$
|
(56,783
|
)
|
|
$
|
(50,449
|
)
|
|
$
|
(23,269
|
)
|
Significant components of income tax expense are as follows:
|
|
For
the Years Ended December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Current:
|
|
|
|
|
|
|
|
|
|
|
|
|
Domestic
|
|
$
|
-
|
|
|
$
|
-
|
|
|
$
|
-
|
|
International
|
|
|
559
|
|
|
|
138
|
|
|
|
202
|
|
Current income tax provision
|
|
|
559
|
|
|
|
138
|
|
|
|
202
|
|
Deferred:
|
|
|
|
|
|
|
|
|
|
|
|
|
Domestic
|
|
|
-
|
|
|
|
-
|
|
|
|
-
|
|
International
|
|
|
(388
|
)
|
|
|
269
|
|
|
|
-
|
|
Deferred income tax (benefit)/provision
|
|
|
(388
|
)
|
|
|
269
|
|
|
|
-
|
|
Total
|
|
$
|
171
|
|
|
$
|
407
|
|
|
$
|
202
|
|
A reconciliation of the expected income tax of the Company
and the actual income tax expense is as follows:
|
|
For
the Years Ended December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Loss before income tax
|
|
$
|
(56,783
|
)
|
|
$
|
(50,449
|
)
|
|
$
|
(23,269
|
)
|
Expected income tax credit, computed by applying the Irish tax rate 12.5%
|
|
|
(7,098
|
)
|
|
|
(6,306
|
)
|
|
|
(2,909
|
)
|
Effect of different tax rates of subsidiaries operating in foreign jurisdictions
|
|
|
182
|
|
|
|
161
|
|
|
|
371
|
|
Unrecognized tax losses carried forward
|
|
|
6,260
|
|
|
|
5,318
|
|
|
|
929
|
|
Non-deductible expenses/non-taxable income
|
|
|
1,220
|
|
|
|
965
|
|
|
|
1,743
|
|
Change in valuation allowance
|
|
|
(388
|
)
|
|
|
269
|
|
|
|
-
|
|
Under provision in prior year
|
|
|
(5
|
)
|
|
|
-
|
|
|
|
68
|
|
Total income taxes
|
|
$
|
171
|
|
|
$
|
407
|
|
|
$
|
202
|
|
One of the main differences between expected tax and effective
tax is explained by unrecognized deferred tax assets on tax losses carried forward amounting as outlined below.
Deferred income tax assets and liabilities
The following temporary differences which might give rise to
deferred taxes relate to:
|
|
As
of December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
Deferred income tax assets:
|
|
|
|
|
|
|
|
|
Tax credits and net operating losses
|
|
|
23,489
|
|
|
|
13,939
|
|
Valuation allowances
|
|
|
(23,364
|
)
|
|
|
(13,678
|
)
|
Total deferred income tax assets
|
|
|
125
|
|
|
|
261
|
|
Deferred income tax liabilities:
|
|
|
|
|
|
|
|
|
Foreign exchange gains/losses
|
|
|
-
|
|
|
|
(524
|
)
|
Total deferred income tax liabilities
|
|
|
-
|
|
|
|
(524
|
)
|
Net deferred income tax asset/(liability)
|
|
|
125
|
|
|
|
(263
|
)
|
The Company has net operating loss carryforwards of $23.5 million
as of December 31, 2016. Of this amount $23.5 million has an indefinite carryforward period.
The net movement in valuation allowances is $9.7 million for
the year ended December 31, 2016 due to uncertainties related to our ability to utilize these assets.
The recognized deferred income tax assets of $0.1 million arises
on losses carried forward from operations in the U.S. The Company has recognized these deferred income tax assets in the period
as management considers that the realization of these deferred income tax balances in the near future is more likely than not.
All of the unrecognized deferred income tax assets arise on
operations in Ireland. Losses arising on operations in Ireland can be carried forward indefinitely, but are limited to the same
trade/trades. The Company has not recognized any deferred income tax assets in the period as management does not consider the
realization of these deferred income tax balances in the near future to be more likely than not due to the significant costs the
Company is likely to incur in the short term in advancing its product pipeline.
As of December 31, 2016, we had no material unrecognized tax
benefits. During the years ended December 31, 2016 and 2015, the amount of recognized interest and penalties was insignificant.
There was no interest or penalties accrued as of December 31, 2016.
Note 14. Trade payables and accrued expenses
|
|
As
of December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
Trade payables
|
|
$
|
6,733
|
|
|
$
|
5,619
|
|
Accrued clinical trial expenses
|
|
|
3,926
|
|
|
|
4,259
|
|
Accrued payroll taxes
|
|
|
805
|
|
|
|
612
|
|
Accrued bonus
|
|
|
517
|
|
|
|
1,401
|
|
Other accrued expenses
|
|
|
1,524
|
|
|
|
2,520
|
|
Total trade payables and accrued expenses
|
|
$
|
13,505
|
|
|
$
|
14,411
|
|
Note 15. Interest-bearing loans and borrowings
Gross liabilities as of December 31, 2016:
Thousands of Dollars
|
|
Interest
Bearing
Loans
|
|
Balance as of December 31, 2015
|
|
$
|
16,400
|
|
Movements during the period
|
|
|
12,548
|
|
Balance as of December 31, 2016
|
|
$
|
28,948
|
|
Reconciliation of gross proceeds to carrying value:
|
|
As
of December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
Gross Proceeds
|
|
$
|
27,571
|
|
|
$
|
16,331
|
|
Accrued interest
|
|
|
2,779
|
|
|
|
69
|
|
Foreign exchange fluctuations
|
|
|
(1,402
|
)
|
|
|
-
|
|
|
|
$
|
28,948
|
|
|
$
|
16,400
|
|
On March 27, 2015, the Company approved the execution of the
Finance Contract between Innocoll Pharmaceuticals Limited and the European Investment Bank (“EIB”) for a loan of up
to $27.6 million.
The loan terms specify that the amounts drawn will be used
to finance up to 50% of certain research and development and capital expenditures forecast to be made by the Company over a three
year period from 2015 through 2017. The first $16.3 million of the loan commitment may be drawn at any time up to fifteen months
from the date of the Finance Contract. The remaining $11.2 million may be drawn at any time up to eighteen months from the date
of the Finance Contract subject to the delivery of clinical data, certified by the management board of Innocoll Holdings plc,
confirming to the satisfaction of EIB that the primary clinical endpoints for either Cogenzia or XaraColl Phase 3 trials have
been achieved and therefore it can be concluded that the Phase 3 clinical trial has successfully been completed. The loan bears
interest at a fixed rate of 12% per annum, compounded annually. There are no cash payments of interest required during the term
of the loan, interest on the outstanding loan balance accrues daily, and is payable only on the maturity date or prepayment date
of the loan, whichever is earlier. The maturity date of each tranche is three to five years from the draw down date, as may be
determined by the Company in each draw down request. Principal of the loan is payable on the maturity date or the prepayment date,
whichever is earlier. Where a prepayment is made the Company will incur a prepayment indemnity of 1%, 0.75%, 0.5% or 0.25% of
the principal amount to be repaid within one year, two years, three years or four years from date of drawdown, respectively. There
will be no prepayment indemnity for prepayment after the fourth year.
The loan contains an expenditure covenant requiring the Company
to spend at least 75% of our forecast research and development, and capital expenditures during the period from 2015 to 2020 as
set out in a business plan agreed with the EIB. If, upon completion of the Project, it is determined that the total principal
amount of the loan drawn by the Company exceeds 50% of the total cost of the Project, EIB may cancel the undisbursed portion of
the loan and demand prepayment of the loan up to the amount by which the loan, excluding accrued interest, exceeds 50% of the
total cost of the Project.
On December 18, 2015 Innocoll Pharmaceuticals Limited drew
down the first tranche of $16.3 million.
On June 17, 2016, Innocoll Pharmaceuticals Limited drew down
the second and final tranche of $11.3 million.
The security on the Finance Contract includes a guarantee from
the Company on 100% of the outstanding principal, interest, expense, commission, indemnity and other sum owed by Innocoll Pharmaceuticals
Limited, together with a fixed charge over all the shares in Innocoll Pharmaceuticals Limited and a floating charge over all the
assets of Innocoll Pharmaceuticals Limited. As of December 31, 2016 no violations of the covenants occurred.
As of December 31, 2016 the carrying value of the loan equated
the fair value.
As of December, 31, 2016, annual maturities of interest bearing
loans and borrowings during the next five years and thereafter are as follows (in thousands):
For the Years
Ending December 31,
|
|
|
|
2017
|
|
$
|
-
|
|
2018
|
|
|
-
|
|
2019
|
|
|
-
|
|
2020
|
|
|
15,780
|
|
2021
|
|
|
10,520
|
|
Thereafter
|
|
|
-
|
|
Note 16. Warrants
The following table summarizes the change in warrants outstanding
for the years ended December 31, 2016 and 2015
Number
|
|
Exercise
price
|
|
|
Contractual
life
(years)
|
|
|
December
31,
2016
|
|
|
December
31,
2015
|
|
Outstanding at beginning of period
|
|
|
|
|
|
|
|
|
|
|
196,912
|
|
|
|
205,199
|
|
Exercised during the year
|
|
|
|
|
|
|
|
|
|
|
-
|
|
|
|
(8,287
|
)
|
Outstanding at end of period
|
|
€
|
83.25
|
|
|
|
2.45
|
|
|
|
196,912
|
|
|
|
196,912
|
|
Exercisable at end of period
|
|
€
|
83.25
|
|
|
|
2.45
|
|
|
|
196,912
|
|
|
|
196,912
|
|
The Company issued warrants at various times in connection
with the issuance of promissory notes or preferred stock. Although the warrants were issued various times, subsequent to the Company’s
redomestication which occurred in 2013, all of the warrants have the same expiration date and exercise price. All the warrants
have an initial expiration date of June 15, 2019, subject to possible extension for an additional 54 month period subject to a
shareholder resolution. The holders of all warrants can elect for cashless exercise whereby they receive shares to the value of
the difference between the market value at exercise and the exercise price.
All warrants have been classified as a liability due to certain
provisions pursuant to which the exercise price of the warrants may be reduced in the event that the Company issues or sells any
of its ordinary shares at a price per share less than the exercise price in effect immediately prior to such issue or sale.
The carrying value of warrants was as follows:
|
|
As
of December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
Liability
|
|
|
|
|
|
|
|
|
Fair value at beginning of period
|
|
$
|
11,498
|
|
|
$
|
7,881
|
|
Warrants exercised in the period
|
|
|
-
|
|
|
|
(450
|
)
|
Fair value movement on warrants in issue
|
|
|
(10,644
|
)
|
|
|
4,067
|
|
Fair value at end of period
|
|
$
|
854
|
|
|
$
|
11,498
|
|
The following input assumptions were used to fair value the
warrants:
|
|
As
of December 31,
|
|
|
|
2016
|
|
|
2015
|
|
Expected volatility
|
|
|
104.88
|
%
|
|
|
66.09
|
%
|
Risk free rate
|
|
|
-0.53
|
%
|
|
|
-0.05
|
%
|
Exercise price
|
|
€
|
83.25
|
|
|
€
|
88.52
|
|
Contractual life
|
|
|
2.45 years
|
|
|
|
3.46 years
|
|
Stock price on valuation date
|
|
$
|
9.14
|
|
|
$
|
109.97
|
|
Note 17. Financial instruments and fair
value measurements
Financial liabilities measured at fair value in the consolidated
balance sheets are grouped into three levels of fair value hierarchy. This grouping is determined based on the lowest level of
significant inputs used in fair value measurement, as follows:
Level 1 -
quoted prices in active markets
for identical assets or liabilities.
Level 2 -
inputs other than quoted prices
included within Level 1 that are observable for the instrument, either directly (i.e. as prices) or indirectly (i.e., derived
from prices).
Level 3 -
inputs for instrument that are
not based on observable market data (unobservable inputs).
The following table summarizes the bases used to measure the
financial liabilities that are carried at fair value on a recurring basis in the consolidated balance sheets.
|
|
December
31,
2016
|
|
|
Level
1
|
|
|
Level
2
|
|
|
Level
3
|
|
Liabilities:
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
Interest bearing loans & borrowings
|
|
$
|
28,948
|
|
|
$
|
-
|
|
|
$
|
-
|
|
|
$
|
28,948
|
|
Warrants
|
|
|
854
|
|
|
|
-
|
|
|
|
-
|
|
|
|
854
|
|
|
|
$
|
29,802
|
|
|
$
|
-
|
|
|
$
|
-
|
|
|
$
|
29,802
|
|
|
|
December
31,
2015
|
|
|
Level
1
|
|
|
Level
2
|
|
|
Level
3
|
|
Liabilities:
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
Interest bearing loans & borrowings
|
|
$
|
16,400
|
|
|
$
|
-
|
|
|
$
|
-
|
|
|
$
|
16,400
|
|
Warrants
|
|
|
11,498
|
|
|
|
-
|
|
|
|
-
|
|
|
|
11,498
|
|
|
|
$
|
27,898
|
|
|
$
|
-
|
|
|
$
|
-
|
|
|
$
|
27,898
|
|
The following table presents the changes in the fair value
of the Level 3 financial instruments for the years ended December 31, 2016 and 2015.
Thousands of Dollars
|
|
Interest Bearing
Loans
|
|
|
Warrants
|
|
Balance as of December 31, 2014
|
|
$
|
-
|
|
|
$
|
7,881
|
|
Gross proceeds
|
|
|
16,331
|
|
|
|
-
|
|
Accrued interest
|
|
|
69
|
|
|
|
-
|
|
Warrants exercised in the period
|
|
|
-
|
|
|
|
(450
|
)
|
Fair value movement on warrants in issue
|
|
|
-
|
|
|
|
4,067
|
|
Balance as of December 31, 2015
|
|
$
|
16,400
|
|
|
$
|
11,498
|
|
Gross proceeds
|
|
|
11,240
|
|
|
|
-
|
|
Accrued interest
|
|
|
2,710
|
|
|
|
-
|
|
Foreign exchange fluctuations
|
|
|
(1,402
|
)
|
|
|
-
|
|
Fair value movement on warrants in issue
|
|
|
-
|
|
|
|
(10,644
|
)
|
Balance as of December 31, 2016
|
|
$
|
28,948
|
|
|
$
|
854
|
|
There have been no transfers between Level 1, Level 2 and Level
3 during the period.
The interest bearing loans and borrowings relate to a commercial
loan with a fixed interest rate and maturity date. As of December 31, 2016, management considers the carrying amount of the loan
to approximate its fair value.
The fair value of warrants issued by the Company has been estimated
using a Monte Carlo simulation model and, in doing so, the Company’s management utilized a third-party valuation report.
The Monte Carlo simulation is a generally accepted statistical method used to generate a defined number of stock price paths in
order to develop a reasonable estimate of the range of the Company’s future expected stock prices and minimizes standard
error.
The estimated fair value of the liability classified warrants
is determined using Level 3 inputs. Inherent in the Monte Carlo valuation model are assumptions related to expected stock-price
volatility, the risk-free interest rate, exercise price and expected life of the warrants. The Company estimates the volatility
of its common stock based upon a weighted average combining the average implied volatility of its peers, the average most recent
4.45–year weekly volatility of its peer group and the Company’s most recent 1-year weekly historical volatility. A
change in any of the inputs included in the Monte Carlo valuation model could result in a variation in the fair value of the warrants
included in the financial statements.
Other Financial Instruments
The carrying amount of the Company’s cash equivalents,
trade and other receivables, trade payables and accrued expenses approximate fair value due to the short term maturities of these
items.
Note 18. Commitments and contingencies
The Company incurred operating lease rent expenses of $0.6
million in 2016, $0.4 million in 2015 and $0.4 million in 2014 which are included in general and administrative expenses.
Future minimum rental commitments under non-cancelable operating
leases in effect as of December 31, 2016 were (in thousands):
For the Years
Endings December 31,
|
|
|
|
2017
|
|
$
|
677
|
|
2018
|
|
|
682
|
|
2019
|
|
|
322
|
|
2020
|
|
|
243
|
|
2021
|
|
|
242
|
|
Thereafter
|
|
|
1,917
|
|
Legal contingencies
The Company and certain of its officers are subject to two
securities class action lawsuits, which may require significant management and board time and attention and significant legal
expenses and may result in an unfavorable outcome, which could have a material adverse effect on our business, financial condition,
results of operations and cash flows.
The Company and certain of its executive officers have been
named as defendants in a securities class action lawsuit initially filed in the United States District Court for the Eastern District
of Pennsylvania on January 24, 2017, captioned
Anthony Pepicelli v. Innocoll Holdings Public Limited Company,
Anthony P. Zook, Jose Carmona and Lesley Russel, civil action no. 2:17-cv-00341-GEKP. The Company and certain of its executive
officers also have been named as defendants in a securities class action lawsuit initially filed in the United States District
Court for the Eastern District of Pennsylvania on February 16, 2017, captioned Jianmin Huang v. Innocoll Holdings Public Limited
Company, Anthony P. Zook, Jose Carmona and Lesley Russel, civil action no. 2:17-cv-00740-GEKP. Neither complaint has been served,
although the plaintiffs have requested the defendants to waive service of summons pursuant to Federal Rule of Civil Procedure
4. The complaints in both actions allege that the Company and certain of its executive officers violated Section 10(b) of the
Exchange Act and Rule 10b-5 promulgated thereunder by making materially false or misleading statements and omissions relating
to the development of Xaracoll and/or related requests for regulatory approval. The complaints also allege that the defendant
officers violated Section 20(a) of the Exchange Act. While the Company believes that it has substantial legal and factual defenses
to the claims in the class actions and intend to vigorously defend the case, these lawsuits could divert its management’s and
board’s attention from other business matters, the outcome of the pending litigation is difficult to predict and quantify, and
the defense against the underlying claims will likely be costly. The ultimate resolution of this matter could result in payments
of monetary damages or other costs, materially and adversely affect its business, financial condition, results of operations and
cash flows, or adversely affect its reputation, and consequently, could negatively impact the price of its common stock.
The Company has insurance policies related to the risks associated
with its business, including directors’ and officers’ liability insurance policies. However, there is no assurance that its insurance
coverage will be sufficient or that its insurance carriers will cover all claims in that litigation. If the Company is not successful
in its defense of the claims asserted in the putative action and those claims are not covered by insurance or exceed its insurance
coverage, the Company may have to pay damage awards, indemnify its officers from damage awards that may be entered against them
and pay the costs and expenses incurred in defense of, or in any settlement of, such claims
.
The Company is further subject to legal proceedings taken by
a number of shareholders who objected to the merger of Innocoll Holdings plc with Innocoll AG on March 16, 2016. The number of
shares held by these shareholders is 569 ordinary shares. The Company has offered each shareholder that registered its objection
to acquire its shares for a cash compensation in the amount of €9.30 per share.
Note 19. Equity
|
|
As
of December 31,
|
|
Number
|
|
2016
|
|
|
2015
|
|
Authorized number of shares:
|
|
|
|
|
|
|
|
|
Common shares at €1 nominal value
|
|
|
-
|
|
|
|
1,837,493
|
|
Authorized Capital I
|
|
|
-
|
|
|
|
196,912
|
|
Authorized Capital II
|
|
|
-
|
|
|
|
24,784
|
|
Authorized Capital III
|
|
|
-
|
|
|
|
665,739
|
|
Contingent Capital
|
|
|
-
|
|
|
|
150,920
|
|
Common shares at $0.01 nominal value
|
|
|
1,000,000,000
|
|
|
|
-
|
|
Deferred shares at $0.01 nominal value
|
|
|
25,000,000
|
|
|
|
-
|
|
Deferred shares at €1.00 nominal value
|
|
|
100,000
|
|
|
|
-
|
|
|
|
|
1,025,100,000
|
|
|
|
2,875,848
|
|
Issued, called up and fully paid number of shares:
|
|
|
|
|
|
|
|
|
Common shares at €1 nominal value
|
|
|
-
|
|
|
|
1,785,009
|
|
Common shares at $0.01 nominal value
|
|
|
29,748,239
|
|
|
|
-
|
|
Deferred shares at €1.00 nominal value
|
|
|
25,000
|
|
|
|
-
|
|
|
|
|
29,773,239
|
|
|
|
1,785,009
|
|
Deferred shares
Deferred shares are shares of the Company that are not entitled
to receive any dividend or distribution or receive note of, or attend any shareholder meeting of the Company. The Company may
at any time acquire all or any of the deferred shares in issue otherwise than for valuable consideration. The Company may cancel
any shares so acquired. The holder of deferred shares may at any time request the Company to acquire all or any of the deferred
shares in issue otherwise than for valuable consideration. The Company may cancel any shares so acquired.
Movement on issued ordinary shares during the year
On April 16, 2015 the management board of Innocoll Germany
approved the issuance of 72,370 common shares for a cash contribution of $1.089 (€1.00) per share pursuant to a notarial
deed entered into on June 16, 2014. In connection with an April 2015 public offering, Innocoll Germany issued 150,920 of its common
shares on April 24, 2015 for proceeds net of issuance costs of $16.7 million. On November 20, 2015 the management board of Innocoll
Germany approved the issuance of 8,287 common shares of Innocoll Germany for a cash contribution of $95.28 per share pursuant
to a notarial deed entered into on June 16, 2014. Innocoll Germany also included in issued shares 50,161 of its common shares
held by members of the supervisory board and management board who had previously been granted restricted shares and a portion
of same vested during the year.
In 2016, pursuant to the Merger, stockholders of Innocoll Holdings
plc received 13.25 common shares in Innocoll Holdings plc for each Innocoll AG common share they respectively held immediately
prior to the Merger, rounded down to the nearest whole Innocoll Holdings plc common share (with aggregated entitlements to fractional
Innocoll Holdings plc common shares being sold by the exchange agent and sale proceeds were distributed in cash pro rata to registered
shareholders whose fractional entitlements were sold). As a result of the Merger the number of common shares in issue increased
by 21,866,360 and the increase of $1.7 million in additional paid-in capital was a result of the change in the par value of common
shares from €1 to $0.01 per common share. In connection with a June 2016 public offering, Innocoll Ireland issued 5,725,000
of its common shares on June 22, 2016 for proceeds net of issuance costs of $37.0 million.
Summary of line items contained in equity
|
|
As
of December 31,
|
|
Thousands of Dollars
|
|
2016
|
|
|
2015
|
|
Equity
|
|
|
|
|
|
|
|
|
Common shares
|
|
$
|
324
|
|
|
$
|
1,943
|
|
Additional paid-in capital
|
|
|
220,965
|
|
|
|
173,353
|
|
Accumulated currency translation adjustment
|
|
|
(1,352
|
)
|
|
|
(1,244
|
)
|
Treasury shares
|
|
|
(27
|
)
|
|
|
-
|
|
Accumulated loss
|
|
|
(223,106
|
)
|
|
|
(166,152
|
)
|
|
|
$
|
(3,196
|
)
|
|
$
|
7,900
|
|
Additional paid-in capital
Additional paid-in capital represents the aggregate of the
following components:
|
i.
|
Share premium, which reflects the excess of consideration received,
net of issue costs, over par value of shares issued.
|
|
ii.
|
Capital contribution, which relates to amounts contributed by
shareholders of the Company in previous years.
|
|
Iii
|
Share compensation, which reflects the fair value of stock based
compensation issued in accordance with ASC 718.
|
|
iv
|
Other, which relate to amounts recognized in equity on issuance
of preferred stock and amounts in relation to the 2013 and 2016 re-domicile to Ireland.
|
Accumulated currency
translation adjustment
Accumulated currency translation adjustment comprises
all foreign exchange differences arising from the translation of the financial statements of foreign operations and gains and
losses arising from change in reporting currency.
Treasury shares
Treasury shares comprises the issued share capital of the company
which was repurchased by the company at the time of the Merger. The shares of Innocoll held immediately prior to the Merger converted
to euro deferred shares of par value €1.00 per share on the effective date of the Merger. The euro deferred shares were issued
solely to ensure that Innocoll satisfied Irish law minimum share capital requirements for public limited companies at all times
and carried no voting rights or income rights, having only limited rights on a return of capital equal to the par value of those
shares.
Note 20. Share-based compensation
The company’s stock-based compensation generally includes
stock options and RSUs. Shares issued relating to the Company’s stock based plans are generally issued out of new stock.
Approved in 2016, the company’s Omnibus Incentive Plan
provided for 2.85 million additional shares of common stock available for issuance with respect to awards for participants. As
of December 31, 2016 approximately 0.1 million authorized shares are available for future awards under the company’s stock-based
compensation plans.
Share-based Compensation Expense
Share-based compensation expense was $8.5 million, $4.0 million
and $6.9 million for the years ended December 31, 2016, 2015 and 2014 respectively. There was no tax related benefit recognized.
Stock Options
Stock options are granted to employees and non-employee directors
with exercise prices equal to 100% of the market value on the date of grant. Stock options granted to employees generally vest
one third at the end of year one with the remainder vesting quarterly over the remaining two years. Stock options granted to non-employee
directors generally vest over the year in which they are granted. Stock options typically have a contractual term of ten years.
The Company accounts for share-based compensation awards based on the fair value of the award as of the grant date using the Black
Scholes model. The awards in issue, to eligible employees include Options. These awards are subject to performance base vesting
conditions, the Company recognizes share-based compensation expense on a straight-line basis over the awards’ requisite service
period, adjusted for estimated forfeitures.
The weighted-average assumptions used in the Black-Scholes
option-pricing model are as follows:
|
|
For the Years Ended December 31,
|
|
|
|
2016
|
|
|
2015
|
|
|
2014
|
|
Expected stock option life (years)
|
|
|
9.36
|
|
|
|
8.74
|
|
|
|
4.52
|
|
Expected volatility
|
|
|
66.52
|
%
|
|
|
66.77
|
%
|
|
|
69.68
|
%
|
Risk-free interest rate
|
|
|
1.92
|
%
|
|
|
2.03
|
%
|
|
|
1.66
|
%
|
Exercise price
|
|
$
|
9.46
|
|
|
$
|
10.65
|
|
|
$
|
9.00
|
|
The Company’s stock option activity for the year ended
December 31, 2016 is as follows:
|
|
Number
of
Stock
Options
|
|
|
Weighted-
Average
Exercise
Price
|
|
|
Weighted-
Average
Remaining
Contractual
Term
(Years)
|
|
|
Aggregate
Intrinsic
Value
|
|
Outstanding, January 1, 2016
|
|
|
1,469,796
|
|
|
$
|
10.58
|
|
|
|
|
|
|
|
|
|
Granted
|
|
|
1,546,007
|
|
|
|
8.26
|
|
|
|
|
|
|
|
|
|
Exercised or converted
|
|
|
(25,910
|
)
|
|
|
8.80
|
|
|
|
|
|
|
|
|
|
Forfeited
|
|
|
(186,140
|
)
|
|
|
8.54
|
|
|
|
|
|
|
|
|
|
Expired
|
|
|
-
|
|
|
|
-
|
|
|
|
|
|
|
|
|
|
Outstanding, December 31, 2016
|
|
|
2,803,753
|
|
|
$
|
9.91
|
|
|
|
9.4
|
|
|
|
-
|
|
Vested and exercisable, December 31, 2016
|
|
|
1,019,387
|
|
|
$
|
9.95
|
|
|
|
8.2
|
|
|
|
-
|
|
The weighted average grant date fair value of the stock options
granted during the years ended December 31, 2016, 2015 and 2014 was $6.04, $7.67 and $3.85 per option, respectively. The total
intrinsic value of options exercised during the year ended December 31, 2016 was $0.1 million. There was no intrinsic value of
options exercised during the years ended December 31, 2015 and 2014. Intrinsic value is measured using the fair market value at
the date of exercise (for options exercised) or as of December 31 (for outstanding options), less the applicable exercise price.
As of December 31, 2016, $9.8 million of unrecognized compensation
cost related to stock options is expected to be recognized as expense over a weighted-average period of approximately 2.0 years.
RSU Awards
RSUs are granted to employees and non-employee directors. RSUs
granted to employees generally vest one half after one year with the remainder vesting five months later. RSUs granted to non-employee
directors generally vest in one third increments over a three-year period. The Company accounts for share-based compensation awards
based on the fair value of the award as of the grant date. The awards in issue, to eligible employees include RSU awards and are
subject to performance base vesting conditions, the Company recognizes stock-based compensation expense on a straight-line basis
over the awards requisite service period, adjusted for estimated forfeitures.
A summary of nonvested RSU activity for the year ended December
31,2016 is as follows:
|
|
Number
of RSUs
|
|
|
Weighted-
Average
Grant
Date
Fair
Value
|
|
Outstanding, January 1, 2016
|
|
|
695,412
|
|
|
$
|
0.08
|
|
Granted
|
|
|
1,339,000
|
|
|
|
2.92
|
|
Vested
|
|
|
(347,720
|
)
|
|
|
0.08
|
|
Forfeited
|
|
|
-
|
|
|
|
-
|
|
Outstanding, December 31, 2016
|
|
|
1,686,692
|
|
|
$
|
2.33
|
|
The total grant date fair value of restricted stock units vested
during the years ended December 31, 2016, 2015 and 2014 was $2.5 million, $6.7 million and $1.0 million, respectively.
As of December 31, 2016 $4.9 million of unrecognized compensation
cost related to RSUs is expected to be recognized as expense over a weighted-average period of approximately 1.1 years.
Note 21. Company entities
Name of subsidiary
|
|
Place
of
incorporation
and
operation
|
|
Proportion
of
ownership
interest
|
|
|
Principal activity
|
Innocoll Inc.
|
|
US
|
|
|
100
|
%
|
|
Administration
|
Syntacoll GmbH
|
|
Germany
|
|
|
100
|
%
|
|
Manufacturing
|
Innocoll Pharmaceuticals Limited
|
|
Ireland
|
|
|
100
|
%
|
|
Selling & distribution
|
The registered office of Innocoll Holdings plc and its main
place of business is Unit 9, Block D, Monksland Business Park, Monksland, Athlone, Co. Roscommon, Ireland.
Note 22. Quarterly financial information (unaudited)
|
|
Three Months Ended
|
|
|
|
March 31,
|
|
|
June 30,
|
|
|
September 30,
|
|
|
December 31,
|
|
|
March 31,
|
|
|
June 30,
|
|
|
September 30,
|
|
|
December 31
|
|
Thousands of Dollars (except
per share data)
|
|
2015
|
|
|
2015
|
|
|
2015
|
|
|
2015
|
|
|
2016
|
|
|
2016
|
|
|
2016
|
|
|
2016
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
Revenue
|
|
$
|
694
|
|
|
$
|
629
|
|
|
$
|
660
|
|
|
$
|
885
|
|
|
$
|
1,560
|
|
|
$
|
1,305
|
|
|
$
|
918
|
|
|
$
|
590
|
|
Gross loss
|
|
|
(844
|
)
|
|
|
(662
|
)
|
|
|
(587
|
)
|
|
|
(370
|
)
|
|
|
(151
|
)
|
|
|
(573
|
)
|
|
|
(916
|
)
|
|
|
(973
|
)
|
Loss for the period -
all attributable to equity holders of the company
|
|
|
(6,347
|
)
|
|
|
(27,604
|
)
|
|
|
(9,143
|
)
|
|
|
(7,763
|
)
|
|
|
(23,054
|
)
|
|
|
(12,849
|
)
|
|
|
(17,204
|
)
|
|
|
(3,847
|
)
|
Basic and diluted loss per share
|
|
$
|
(0.32
|
)
|
|
$
|
(1.24
|
)
|
|
$
|
(0.39
|
)
|
|
$
|
(0.33
|
)
|
|
$
|
(0.97
|
)
|
|
$
|
(0.53
|
)
|
|
$
|
(0.58
|
)
|
|
$
|
(0.13
|
)
|
Average quarterly currency translation rate was utilized for
2015 quarters above.
Note 23. Subsequent events
There have been no significant post balance sheet events,
other than those disclosed in the financial statements.
Exhibit Index
Exhibit
No.
|
|
Description
|
2.1
|
|
Merger Proposal, dated December 20, 2015, between Innocoll AG and Innocoll Holdings plc. (Incorporated by reference to
Exhibit 2.1 of our Report of Foreign Private Issuer on Form 6-K filed with the Commission on December 21, 2015 (File No. 001-36565)).
|
3.1
|
|
Innocoll Holdings plc Constitution. (Incorporated by reference to Exhibit 3.1 of our Report of Foreign Private Issuer
on Form 6-K filed with the Commission on June 20, 2016 (File No. 001-37720)).
|
4.1
|
|
Specimen Ordinary Share Certificate. (Incorporated by reference to Exhibit 4.1 of our Report of Foreign Private Issuer
on Form 6-K filed with the Commission on August 2, 2016 (File No. 001-37720)).
|
10.1#
|
|
License and Supply Agreement, dated August 14, 2013, between Innocoll Pharmaceuticals Ltd. and Takeda GmbH, an affiliate
of Takeda Pharmaceutical Company Limited, as amended on March 19, 2014. (Incorporated by reference to Exhibit 10.1 of
our Registration Statement on Form F-1, as amended, initially filed with the Commission on June 19, 2014 (File No. 333-196910)).
|
10.2#
|
|
Licensing, Manufacturing and Supply Agreement, dated October 12, 2011, between Innocoll Pharmaceuticals Ltd. and Pioneer
Pharma Co. Ltd., as amended on August 6, 2012. (Incorporated by reference to Exhibit 10.2 of our Registration Statement
on Form F-1, as amended, initially filed with the Commission on June 19, 2014 (File No. 333-196910)).
|
10.3#
|
|
Exclusive Distribution Agreement, dated April 3, 2013, between Innocoll Pharmaceuticals Ltd. and Biomet 3i, LLC. (Incorporated
by reference to Exhibit 10.3 of our Registration Statement on Form F-1, as amended, initially filed with the Commission on
June 19, 2014 (File No. 333-196910)).
|
10.4#
|
|
Manufacture and Supply Agreement, dated August 17, 2007, among Innocoll Pharmaceuticals Ltd., Syntacoll AG and EUSA Pharma
(Europe) Limited (later acquired by Jazz Pharmaceuticals), as amended and restated on April 27, 2010. (Incorporated
by reference to Exhibit 10.4 of our Registration Statement on Form F-1, as amended, initially filed with the Commission on
June 19, 2014 (File No. 333-196910)).
|
10.5#
|
|
Manufacturing and Supply Agreement, dated June 1, 2004, between Innocoll Technologies Ltd., and Biomet Orthopedics Switzerland
GmbH, as amended on January 1, 2006; December 15, 2009; September 1, 2010; April 1, 2011; March 15, 2012; March 1, 2013 and
July 26, 2013. (Incorporated by reference to Exhibit 10.5 of our Registration Statement on Form F-1, as amended, initially
filed with the Commission on June 19, 2014 (File No. 333-196910)).
|
10.6#
|
|
Licensing, Manufacturing and Supply Agreement, dated December 5, 2011, between Innocoll Pharmaceuticals Ltd. and Saudi
Centre for Pharmaceuticals. (Incorporated by reference to Exhibit 10.6 of our Registration Statement on Form F-1,
as amended, initially filed with the Commission on June 19, 2014 (File No. 333-196910)).
|
10.7+
|
|
Innocoll Holdings plc Amended and Restated 2015 Stock Option Plan (formerly adopted by Innocoll
AG). (Incorporated by reference to Exhibit 10.2 of our Registration Statement on Form S-8 filed with the Commission on
June 3, 2016 (File No. 333-211801)).
|
10.8+
|
|
Amended and Restated Option Agreement. (Incorporated by reference to Exhibit 10.3 of our Registration
Statement on Form S-8 filed with the Commission on June 3, 2016 (File No. 333-211801)).
|
10.9+
|
|
Form of Innocoll GmbH Option Agreement, as amended and restated. (Incorporated by reference to Exhibit 10.8 of our
Amendment No. 1 to our Registration Statement on Form F-1 filed with the Commission on July 15, 2014 (File No. 333-196910)).
|
10.10+
|
|
Form of Innocoll AG Restricted Share Award Agreement. (Incorporated by reference to Exhibit 10.9 of our Amendment
No. 1 to our Registration Statement on Form F-1 filed with the Commission on July 15, 2014 (File No. 333-196910)).
|
10.11+
|
|
Innocoll Holdings plc 2016 Omnibus Incentive Compensation Plan. (Incorporated by reference to Exhibit 10.1 of our Registration
Statement on Form S-8 filed with the Commission on June 3, 2016 (File No. 333-211801)).
|
10.12+
|
|
Employment Agreement by and between Anthony Zook and Innocoll AG, dated as of December 2014 (Incorporated by reference
to Exhibit 4.19 of our Annual Report on Form 20-F filed with the Commission on March 19, 2015 (File No. 001-36565)).
|
10.13+
|
|
Restricted Share Award Agreement by and between Anthony Zook and Innocoll AG, dated December 7, 2014 (Incorporated by reference to Exhibit 4.20 of our Annual
Report on Form 20-F filed with the Commission on March 19, 2015 (File No. 001-36565)).
|
10.14+
|
|
Employment Agreement by and between Rich Fante and Innocoll, Inc., dated as of August 20, 2015 (Incorporated by reference to Exhibit 4.14 of our Annual Report on Form 20-F filed with the Commission on March 17, 2016
(File No. 001-37720)).
|
Exhibit
No.
|
|
Description
|
10.15+
|
|
Employment Agreement by and between Jose Carmona and Innocoll, Inc., dated as of September 1, 2015.
(Incorporated
by reference to Exhibit 4.15 of our Annual Report on Form 20-F filed with the Commission on March 17, 2016 (File No. 001-37720)).
|
10.16+
|
|
Employment Agreement by and between Charles F. Katzer and Innocoll Pharmaceuticals Ltd., dated as of December 14, 2015. (Incorporated
by reference to Exhibit 4.16 of our Annual Report on Form 20-F filed with the Commission on March 17, 2016 (File No. 001-37720)).
|
10.17#
|
|
Lease Agreement between Karl Sipmeier and Syntacoll GmbH, dated December 17, 2009 (English translation). (Incorporated
by reference to Exhibit 10.17 of our Registration Statement on Form F-1, as amended, initially filed with the Commission on
June 19, 2014 (File No. 333-196910)).
|
10.18
|
|
Lease Agreement between Athlone Institute of Technology and Innocoll Technologies Ltd., dated November 24, 2008. (Incorporated
by reference to Exhibit 10.18 of our Registration Statement on Form F-1, as amended, initially filed with the Commission on
June 19, 2014 (File No. 333-196910)).
|
10.19
|
|
Lease Agreement between Thomas Angerer and Syntacoll GmbH, effective as of February 1, 2016. (Incorporated by reference
to Exhibit 4.19 of our Annual Report on Form 20-F filed with the Commission on March 17, 2016 (File No. 001-37720)).
|
10.20
|
|
Lease Agreement between Campus Investors H Building, L.P. and Innocoll AG, dated October 31, 2015. (Incorporated
by reference to Exhibit 4.20 of our Annual Report on Form 20-F filed with the Commission on March 17, 2016 (File No. 001-37720)).
|
10.21
|
|
Finance Contract between the European Investment Bank and Innocoll Pharmaceuticals Ltd. and Innocoll AG, dated March 27,
2015. (Incorporated by reference to Exhibit 10.23 our Registration Statement on Form F-1, as amended, initially
filed with Commission on April 10, 2015 (File No. 333-23362)).
|
|
|
|
21.1*
|
|
List of Subsidiaries.
|
|
|
|
23.1*
|
|
Consent of Independent Registered Public Accounting Firm.
|
|
|
|
31.1*
|
|
Certification of Principal Executive Officer Pursuant to SEC Rule 13a-14(a)/15d-14(a).*
|
|
|
|
31.2*
|
|
Certification of Principal Financial Officer Pursuant to SEC Rule 13a-14(a)/15d-14(a).*
|
|
|
|
32.1*
|
|
Certification of Principal Executive Officer and Principal Financial Officer Pursuant to 18 U.S.C. Section 1350.*
|
* Filed
herewith.
+ Indicates
a management contract or compensatory plan.
# Portions
of this exhibit (indicated by asterisks) have been omitted pursuant to a request for confidential treatment pursuant to Rule 406
under the Securities Act of 1933.
Innocoll AG (NASDAQ:INNL)
Historical Stock Chart
From Aug 2024 to Sep 2024
Innocoll AG (NASDAQ:INNL)
Historical Stock Chart
From Sep 2023 to Sep 2024