ProQR Therapeutics N.V. (Nasdaq:PRQR) today announced that clinical
study PQ-010-002, a proof-of-concept study of nasal potential
difference (NPD), demonstrated that QR-010 restored CFTR function
in a cohort of homozygous ∆F508 cystic fibrosis (CF) patients. The
study met its primary endpoint in this cohort as measured by a
change in total chloride response following 4 weeks of treatment
with QR-010. In the compound heterozygous ∆F508 cohort, no
meaningful difference was found. QR-010 was observed to be safe and
well-tolerated in both cohorts.
ProQR also announced that clinical study PQ-010-001 completed
all four single-dose cohorts. PQ-010-001 is a placebo-controlled
Phase 1b study in subjects with CF homozygous for ∆F508. QR-010 was
observed to be safe and well-tolerated in all four single dose
cohorts. The multiple dose cohorts in this study are ongoing and
topline safety, tolerability and exploratory efficacy data from
this study are expected in mid-2017.
The top-line results of PQ-010-002 will be presented today by
Noreen R. Henig M.D. and John P. Clancy M.D. at the North American
Cystic Fibrosis Conference (NACFC) in Orlando, Florida, USA in
workshop W07: Clinical Advances in Cystic Fibrosis Research from
9:45am – 11:05am ET. Session broadcast information for registered
participants is available at the NACFC website. The company will
also host an investor and analyst event starting at 8:30pm ET with
presentations and webcast starting at 9:00pm ET. The webcast can be
accessed from ProQR’s website via this link.
“Patients with CF feel and do better when the CFTR protein
channel works more normally. Our important first step in helping
patients with CF was to demonstrate that QR-010 could restore CFTR
function in patients with CF due to ∆F508, the most common
mutation. Our proof-of-concept NPD study did exactly that in CF
patients homozygous for ∆F508; it demonstrated that CFTR protein
channels are active in this cohort following administration of
QR-010 as measured by the total chloride response. Having achieved
this major step, we have increased confidence in QR-010’s potential
to make a meaningful clinical impact for patients and will move
forward with an aggressive development plan”, said Noreen R. Henig,
M.D., Chief Development Officer of ProQR.
“NPD is a reliable, direct and specific measurement of CFTR
activity and is therefore used as an important endpoint to assess
CFTR function in clinical trials in CF. As CFTR dysfunction is the
key problem in CF, the restoration of CFTR function as measured by
NPD is an important early signal for potential future clinical
benefit for patients”, said John P. Clancy, M.D., principal
investigator, Professor of Pediatrics and Research Director,
Division of Pulmonary Medicine, Cincinnati Children’s Hospital and
a member of the Cystic Fibrosis Foundation Therapeutic Development
Network’s leadership team. “The change in the total chloride
secretion response observed with QR-010 in this study has never
been demonstrated with a ∆F508 targeting agent before. This outcome
makes us eager to advance this molecule into next clinical
studies.”
“This first clinical data in CF patients with QR-010 is a major
milestone for ProQR, the CF community and the RNA therapeutics
space. Confirming QR-010’s ability to improve CFTR function in
homozygous ∆F508 patients is a strong validation of the preclinical
evidence and reinforces our belief that QR-010 can make a
transformative difference in the lives of CF patients", said Daniel
de Boer, Chief Executive Officer of ProQR. “I want to sincerely
thank all the patients that participated in our studies, and all
our clinical investigators that supported this unique study and
executed it with a level of operational excellence, allowing us to
validate the potential of QR-010 for this patient population with a
significant unmet medical need”.
Study PQ-010-002, a Nasal Potential Difference
proof-of-concept study
PQ-010-002 was an open-label, proof-of-concept study evaluating
the effect of QR-010 on the nasal potential difference (NPD) assay,
an important measurement of CFTR function. The study was conducted
in 5 NPD specialized centers in the US and Europe. The study
enrolled 18 CF patients, 10 homozygous for the ΔF508 mutation and 8
compound heterozygous (one copy of the ΔF508 mutation and one copy
of another cystic fibrosis disease-causing mutation). QR-010 was
applied topically to the nasal mucosa 12 times over a period of 4
weeks. Primary endpoint for each cohort was the change from
baseline in CFTR mediated total chloride transport as measured by
NPD.
In the per-protocol population of subjects homozygous for the
ΔF508 mutation meeting the pre-specified inclusion criteria (n=7),
the average change from baseline in NPD at day 26 was statistically
significant, -4.1 mV (p=0.0389). This finding was supported by a
change in sodium channel activity and other sensitivity analyses of
the NPD measurements, all pointing to strong evidence of
restoration of CFTR activity.
In subjects compound heterozygous for the ΔF508 mutation, the
average change from baseline in NPD was not significantly different
at day 26. A responder analysis of individual subjects assessing
the impact of the second mutation is currently ongoing.
Study PQ-010-001, a Phase 1b safety and tolerability
study in CF ΔF508 homozygous patients
PQ-010-001 is a Phase 1b randomized, double-blind,
placebo-controlled, dose-escalation 28-day study currently
enrolling patients in more than 20 centers in North America and
Europe. This study evaluates the safety, tolerability and
pharmacokinetics of single and multiple ascending doses of inhaled
QR-010 in a total of 64 CF patients homozygous for the ΔF508
mutation. Exploratory efficacy endpoints in the multiple dose
cohorts include sweat chloride, weight gain, CFQ-R Respiratory
Symptom Score and lung function, measured by FEV1. The single dose
portion of the study consisting of 4 cohorts has been completed. No
dose-limited toxicity was observed up to the highest dose tested.
The dose escalating multiple-dose study (12 doses administered over
4 weeks) is currently enrolling cohort 6 and topline results are
expected to be available in mid-2017.
About QR-010
QR-010 is a first-in-class RNA-based oligonucleotide designed to
address the underlying cause of the disease by targeting the mRNA
in CF patients that have the DF508 mutation. The DF508 mutation is
a deletion of three of the coding base pairs, or nucleotides, in
the CFTR gene, which results in the production of a misfolded CFTR
protein that does not function normally. QR-010 is designed to bind
to the defective CFTR mRNA and to restore CFTR function. QR-010 is
designed to be self-administered via an optimized
eFlow® Nebulizer (PARI Pharma GmbH). eFlow® is a small,
handheld aerosol delivery device which nebulizes QR-010 into a mist
inhaled directly into the lungs. QR-010 has been granted orphan
drug designation in the United States and the European Union and
fast-track status by the FDA. The QR-010 project has received
funding from the European Union’s Horizon 2020 research and
innovation programme under grant agreement No 633545.
About cystic fibrosis
CF is the most common fatal inherited disease in the Western
world and affects an estimated 70,000 to 100,000 patients
worldwide. In people with CF, a defective CFTR gene causes a thick,
buildup of mucus in the lungs, pancreas and other organs. In the
lungs, the mucus clogs the airways and traps bacteria leading to
infections, extensive lung damage and eventually, respiratory
failure. There is no cure for CF. Disease manifestations lead to a
shortened life expectancy with a median age of death of 27 years.
Although over 1,900 CF-causing gene mutations have been identified,
approximately 70% of all CF patients are affected by the DF508
mutation. Among all CF patients, approximately 50% are homozygous
for the DF508 mutation.
About ProQR
ProQR Therapeutics is dedicated to changing lives through the
creation of transformative RNA medicines for the treatment of
severe orphan diseases such as cystic fibrosis and Leber’s
congenital amaurosis. Based on our unique proprietary RNA repair
platform technologies we are growing our pipeline with patients and
loved ones in mind. *Since 2012*
FORWARD-LOOKING STATEMENTS
This press release contains “forward-looking statements” within
the meaning of the safe harbor provisions of the U.S. Private
Securities Litigation Reform Act of 1995. All statements other than
statements of historical fact are forward-looking statements, which
are often indicated by terms such as “anticipate,” “believe,”
“could,” “estimate,” “expect,” “goal,” “intend,” “look forward to,”
“may,” “plan,” “potential,” “predict,” “project,” “should,” “will,”
“would” and similar expressions. Forward-looking statements are
based on management’s beliefs and assumptions and on information
available to management only as of the date of this press release.
These forward-looking statements include, but are not limited to,
statements regarding QR-010, its therapeutic potential and its
clinical development and timing of clinical trials including the
statements related to PQ-010-001 and PQ-010-002. Our actual results
could differ materially from those anticipated in these
forward-looking statements for many reasons, including, without
limitation, risks associated with our clinical development
activities, including the risk that positive results observed in
our prior and ongoing studies may not be replicated in later trials
or guarantee approval of any product candidate by regulatory
authorities, manufacturing processes and facilities, regulatory
oversight, product commercialization, intellectual property claims,
and the risks, uncertainties and other factors in our filings made
with the Securities and Exchange Commission, including certain
sections of our annual report filed on Form 20-F for the year ended
December 31, 2015, and any subsequent SEC filings. Given these
risks, uncertainties and other factors, you should not place undue
reliance on these forward-looking statements, and we assume no
obligation to update these forward-looking statements, even if new
information becomes available in the future, except as required by
law.
ProQR Therapeutics N.V.:Smital ShahChief
Financial OfficerT: +1 415 231 6431ir@proqr.com
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