- Rucaparib NDA Dataset to be presented
in oral presentation today at ESMO
- Rucaparib NDA currently under priority
review with FDA
- Prescription Drug User Fee Act (PDUFA)
date is February 23, 2017
- European Marketing Authorization
Application (MAA) submission planned for Q4 2016
Clovis Oncology (NASDAQ:CLVS) announced today the oral
presentation of the primary efficacy and safety data from its NDA
dataset for rucaparib at the 2016 ESMO Congress in Copenhagen.
Rucaparib is currently under priority review with FDA for the
monotherapy treatment of advanced ovarian cancer in patients with
BRCA-mutated tumors inclusive of both germline and somatic BRCA
mutations who have been treated with two or more chemotherapies,
and the submission has a PDUFA date of February 23, 2017.
Rucaparib is the Company’s oral, small molecule inhibitor of
PARP1, PARP2 and PARP3 currently being developed for the treatment
of ovarian cancer, specifically in patients with tumors with BRCA
mutations and other DNA repair deficiencies beyond BRCA, including
those with high genomic loss of heterozygosity (LOH) also known as
“BRCA-like." The current NDA submission seeks approval in patients
with tumor BRCA mutations, which includes both germline and somatic
mutations.
“These results demonstrate that rucaparib may represent an
important option for women with multiply relapsed BRCA-mutated
ovarian cancer based on its encouraging efficacy and tolerability,”
said Rebecca S. Kristeleit, MD, PhD, The University College London,
Cancer Institute, London, UK. “In my opinion, rucaparib has the
hallmarks of an important new therapeutic option for ovarian cancer
patients.”
“We are pleased to present the primary efficacy and safety
dataset that has been submitted to the FDA as the basis of our NDA
for rucaparib in the treatment of advanced ovarian cancer. If
approved, rucaparib would be the first PARP inhibitor in the U.S.
indicated to treat ovarian cancer patients with germline or somatic
BRCA mutations who have received two prior chemotherapies. Women
with BRCA mutations represent about 25% of patients in the US
living with ovarian cancer,” said Patrick J. Mahaffy, CEO and
President of Clovis Oncology. “Our NDA review is ongoing with FDA,
and in addition we are actively preparing for a European submission
during the fourth quarter of 2016.”
Data from subgroups of two multicenter, single-arm open-label
phase 2 studies, Study 10 (NCT01482715) and ARIEL2 (NCT01891344)
were combined for an integrated efficacy and safety analysis which
further characterized the clinical benefit of rucaparib at the
recommended starting dose of 600 mg BID in women with advanced
ovarian cancer. In the two studies, 377 patients met the criteria
for inclusion in the safety population (diagnosis of ovarian cancer
and having received one or more doses of the recommended dose of
600 mg of rucaparib), and 106 patients met the criteria for
inclusion in the efficacy population (received 2 or more prior
chemotherapies, including 2 or more platinum-based regimens, had a
mutation of BRCA (germline or somatic), and received one or more
doses of the recommended dose of 600 mg of rucaparib.
The major efficacy outcome measure for this analysis was
objective response rate (ORR) and duration of response (DOR) as
assessed by the investigator according to RECIST. All responses
were confirmed.
For the efficacy population (n=106), the median number of prior
chemotherapies was three, with 39% having received two prior
therapies and 61% of patients having received three or more prior
therapies. The median number of prior platinum-based therapies was
two, with 57% having received two prior platinum-based therapies,
and 43% having received three or more prior platinum-based
therapies. Seventy-five percent of patients in the efficacy
population were platinum-sensitive (as defined by recurrence after
progression free interval (PFI) of ≥6 months), 19% were platinum
resistant (recurrence after PFI <6 months) and 7% were platinum
refractory (progression on platinum, PFI <2 months).
Summary of Efficacy Data
The RECIST ORR (objective response rate as assessed by the
investigator, which includes complete and partial responses) in the
efficacy population was 57/106, or 54% (95% CI: 43.8-63.5). This
includes nine (9%) complete responders (CR) and 48 (45%) partial
responders (PR). Thirty-six patients (34%) had stable disease (SD)
as the best response, while nine patients (9%) had progressive
disease (PD) as the best response and four (4%) were not evaluable
(NE). Seventy-five of 106 patients, or 71% (95% CI: 61.1-79.2) had
a RECIST or CA-125 response.
For the 42 patients from Study 10 included in the efficacy
population, the RECIST ORR was 25/42, or 60% (95% CI: 43.3-74.4).
This included four CRs (10%) and 21 PRs (50%). In addition, 12
patients (29%) had SD, two patients (5%) had PD and three (7%) were
NE. For the 64 patients from ARIEL2 included in the efficacy
population, the RECIST ORR was 32/64, or 50% (95% CI: 37.2-62.8).
This included five CRs (8%) and 27 PRs (42%). In addition, 24
patients (38%) had SD, seven (11%) had PD and one (2%) was NE.
Study 10 was limited to platinum sensitive patients; ARIEL2
included platinum sensitive, platinum resistant and platinum
refractory patients.
In addition, ORR was assessed by subgroups including BRCA
mutation type, number of prior chemotherapies and prior platinum
regimens, PFI and platinum status. Patients with a BRCA1 (n=67) or
BRCA2 (n=39) mutation both showed an ORR of 54% (95% CI: 41.1-66.0,
37.2-69.9, respectively) in line with the overall population. The
ORR for patients with germline BRCA mutations (n=88) and somatic
BRCA mutations (n=13) was 53% (95% CI: 42.5-64.1) and 46% (95% CI:
19.2-74.9), respectively; in addition, five patients with a BRCA
mutation but unknown germline or somatic status had an ORR of 80%
(95% CI: 28.4-99.5). Patients who received two prior chemotherapies
(n=41) achieved an ORR of 68% (95% CI: 51.9-81.9). Patients who
received two prior platinum regimens (n=60) demonstrated an ORR of
65% (95% CI: 51.6-76.9). Response by length of PFI differed for
patients with PFI<6 months (n=27), 6-12 months (n=56) and
greater than 12 months (n=23), reporting 19% (95% CI: 6.3-38.1),
63% (95% CI: 48.6-75.1) and 74% (95% CI: 51.6-89.8), respectively.
Response by platinum status was reported as 0% (95% CI: 0.0-41.0)
for platinum-refractory patients (n=7), 25% (95% CI: 8.7-49.1) for
platinum-resistant patients (n=20), and 66% (95% CI: 54.3-76.1) for
platinum-sensitive patients (n=79).
Duration of response by investigator assessment in the efficacy
population was 9.2 months (95% CI: 6.6-11.7 months), and the
censoring rate among responders was 47%. As of the cutoff dates, 20
patients with a RECIST response had an ongoing response.
Additionally, analyses not contained within the NDA submission
showed median progression-free survival by investigator assessment
in the efficacy population to be 10.0 months. Of 106 patients, 50
patients did not have an event of disease progression or death at
the data cut-off dates. Of these 50 patients, 32 patients were
still on treatment, and 18 patients discontinued treatment for
reasons other than disease progression or death at the data cut-off
dates. Of note, 79% of patients remained progression-free at six
months, and 41% remained progression-free at 12 months.
For the efficacy dataset, the cut off dates were November 30,
2015 and February 29, 2016, for Study 10 and ARIEL2,
respectively.
Summary of Safety Data
Of the 377 ovarian cancer patients treated with a starting dose
of rucaparib 600 mg, 377 (100%) experienced a treatment-emergent
adverse event (AE) of any grade, and 229 (61%) experienced a
treatment-emergent AE grade 3 or higher. A total of 360 patients
(96%) experienced a treatment-related AE of any grade, and 177
(47%) experienced a treatment-related AE that was grade 3 or
higher. AEs leading to dose interruption occurred in 221 patients
(59%). Treatment-related AEs leading to dose reduction occurred in
167 patients (44%), and treatment discontinuation in 30 patients
(8%). The primary reasons for dose reduction were anemia/decreased
hemoglobin (17%), asthenia/fatigue (14%) and nausea (11%). The
primary reasons for treatment discontinuation were asthenia/fatigue
(2%), small intestinal obstruction (2%) and nausea (1%). Nine
patients (2%) had AEs that led to death; eight were due to disease
progression, and one death was due to sepsis, which was assessed by
the investigator to be unrelated to treatment.
The most common treatment-emergent AEs (all grades) reported in
≥20 percent of patients included nausea (77%), asthenia/fatigue
(77%), vomiting (46%), anemia (44%), increased ALT/AST (41%) and
constipation (40%). The most common Grade 3/4 treatment-emergent
AEs reported in ≥10 percent of patients were anemia (25%),
asthenia/fatigue (11%) and ALT/AST elevations (11%).
The increases in aspartate (AST) and alanine (ALT)
aminotransferase levels that were observed were asymptomatic,
reversible and were rarely associated with increases in bilirubin.
The elevations normalized over time with continued rucaparib
treatment.
Mild to moderate creatinine elevations were observed within the
first few weeks of treatment for most patients, for whom 79 (21%)
experienced an AE, of whom two (0.5%) experienced a grade 3/4
event. These elevations in creatinine likely result from inhibition
of the renal transporters MATE1 and MATE2-K, which can lead to an
increase in serum creatinine in the absence of renal injury.
Myelodysplastic syndrome/acute myeloid leukemia was reported in
less than one percent of patients.
The cut-off dates for the safety dataset were March 31, 2016 for
Study 10 and April 29, 2016 for ARIEL2.
Presentation Details
The oral presentation, titled “Clinical activity of the
poly(ADP-ribose) polymerase (PARP) inhibitor rucaparib in patients
(pts) with high grade ovarian carcinoma (HGOC) and a BRCA mutation
(BRCAmut): Analysis of pooled data from Study 10 (parts 1, 2a, and
3) and ARIEL2 (parts 1 and 2)” was presented today by Rebecca S.
Kristeleit, PhD, The University College London, Cancer Institute,
London, United Kingdom during the Session titled “Gynecological
Cancers”, from 2:00pm-3:30pm CEST (Abstract 856O: 2:45pm-3:00pm
CEST).
The Trials-in-Progress poster presentation, titled “Window study
of the PARP inhibitor rucaparib in patients with primary triple
negative or BRCA1/2 related breast cancer (RIO)” is being presented
Monday by Christy Toms, PhD, The Institute of Cancer Research,
Sutton, United Kingdom during the Poster Session titled “Breast
Cancer, Early Stage” from 1:00pm-2:00pm CEST (Abstract 219TiP,
Poster Board #219).
The presentations will be available online
at http://clovisoncology.com/products-companion-diagnostics/scientific-presentations/
at the time of their scheduled presentation at the Congress.
About Rucaparib
Rucaparib is an oral, small molecule inhibitor of PARP-1, PARP-2
and PARP-3 being developed for advanced ovarian cancer.
Specifically, rucaparib is being developed as monotherapy
treatment of advanced ovarian cancer in patients with deleterious
BRCA-mutated tumors inclusive of both germline and somatic BRCA
mutations (as detected by an FDA-approved test) who have been
treated with two or more chemotherapies. Rucaparib was granted
Breakthrough Therapy designation for this proposed indication by
the U.S. FDA in April 2015; and in late June 2016, Clovis completed
its New Drug Application (NDA) submission to the FDA. The filing
for treatment was accepted and has an action date of February 23,
2017. Rucaparib’s Marketing Authorization Application (MAA) to the
European Medicines Agency for the proposed treatment indication is
planned for Q4 2016.
Foundation Medicine, Clovis’ companion diagnostic partner, has
submitted a Premarket Approval (PMA) application for its
FoundationFocus CDxBRCA to the FDA in June 2016. The test is
designed to identify tumor BRCA mutations. The timing of the
submission is expected to allow for regulatory approval of the
companion diagnostic in a similar timeframe.
Additionally, rucaparib is being developed as maintenance
therapy in the ARIEL3 trial (NCT01968213) for patients with tumors
with BRCA mutations and other DNA repair deficiencies beyond BRCA
(commonly referred to as homologous recombination deficiencies, or
HRD). Data from ARIEL3 are expected in Q4 2017, which is expected
to be followed by the submission of a supplemental NDA for
second-line maintenance therapy.
Clovis is also exploring rucaparib in other solid tumor types
with BRCA mutations or molecular evidence of the HRD signature,
including prostate, breast and gastroesophageal cancers.
Clovis holds worldwide rights for rucaparib.
About Ovarian Cancer
According to the American Cancer Society, more than 22,000 women
will be diagnosed with ovarian cancer in the U.S. during 2016.
There are often no clearly identifiable initial symptoms, and in an
estimated 80 to 85% of ovarian cancer cases, the cancer has spread
to other parts of the body before a person is diagnosed and can be
treated. Ovarian cancer ranks fifth in cancer deaths and causes
more deaths than any other cancer of the female reproductive
system. One in four women with ovarian cancer have a germline or
somatic BRCA mutation, and new treatment options are needed to
treat unique patient populations.
About Clovis Oncology
Clovis Oncology, Inc. is a biopharmaceutical company
focused on acquiring, developing and commercializing innovative
anti-cancer agents in the U.S., Europe and additional
international markets. Clovis Oncology targets
development programs at specific subsets of cancer populations, and
simultaneously develops diagnostic tools that direct a compound in
development to the population that is most likely to benefit from
its use. Clovis Oncology is headquartered
in Boulder, Colorado.
To the extent that statements contained in this press release
are not descriptions of historical facts regarding Clovis
Oncology, they are forward-looking statements reflecting the
current beliefs and expectations of management made pursuant to the
safe harbor provisions of the Private Securities Litigation Reform
Act of 1995. Such forward-looking statements involve
substantial risks and uncertainties that could cause our clinical
development programs, future results, performance or achievements
to differ significantly from those expressed or implied by the
forward-looking statements. Such risks and uncertainties
include, among others, the uncertainties inherent in our clinical
development programs for our drug candidates, the corresponding
development pathways of our companion diagnostics, actions by
the FDA, the EMA or other regulatory authorities regarding
whether to approve drug applications that may be filed, as well as
their decisions regarding drug labeling, and other matters that
could affect the availability or commercial potential of our drug
candidates or companion diagnostics, including competitive
developments. Clovis Oncology does not undertake to
update or revise any forward-looking statements. A further
description of risks and uncertainties can be found in Clovis
Oncology’s filings with the Securities and Exchange
Commission, including its Annual Report on Form 10-K and its
reports on Form 10-Q and Form 8-K.
View source
version on businesswire.com: http://www.businesswire.com/news/home/20161007005279/en/
Clovis OncologyAnna Sussman,
303-907-5358asussman@clovisoncology.comorBreanna Burkart,
303-625-5023bburkart@clovisoncology.com
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