Efficacy signals observed will not achieve
ESSA's target product profile in patients with metastatic
castration-resistant prostate cancer naïve to second-generation
antiandrogens
A futility analysis conducted as part of
a protocol-specified interim review of the safety, PK and efficacy
data showed the single-agent enzalutamide control arm performing
better than historical controls and similar to the combination of
masofaniten and enzalutamide and therefore, unlikely to achieve the
primary endpoint of the study
Additional clinical studies with masofaniten
including the combination study with abiraterone acetate and
apalutamide as well as the remaining investigator sponsored trials
will also be terminated and the IND and CTAs in different
geographies will be withdrawn
Company will initiate a process to explore and
review strategic options focused on maximizing shareholder
value
SOUTH
SAN FRANCISCO, California and VANCOUVER, Canada, Oct. 31,
2024 /CNW/ - ESSA Pharma Inc. ("ESSA", or the
"Company") (NASDAQ: EPIX), a clinical-stage pharmaceutical company
focused on developing novel therapies for the treatment of prostate
cancer, today announced that it has made the decision to terminate
the Phase 2 clinical trial evaluating in a 2:1 randomization
masofaniten combined with enzalutamide versus enzalutamide single
agent in patients with metastatic castration-resistant prostate
cancer ("mCRPC") naïve to second-generation antiandrogens. This
decision, mutually agreed upon by both senior management and the
board of directors, was based on a protocol-specified interim
review of the safety, PK and efficacy data, which showed a much
higher rate of PSA90 response in patients treated with enzalutamide
monotherapy (which is standard of care for this patient population)
than were expected based upon historical data. In addition, there
was no clear efficacy benefit seen with the combination of
masofaniten plus enzalutamide compared to enzalutamide single
agent. A futility analysis determined a low likelihood of meeting
the prespecified primary endpoint of the study. The combination of
masofaniten plus enzalutamide was well-tolerated with no new safety
signals and a safety profile similar to that seen in Phase 1
studies.
"Providing a meaningful clinical benefit to patients in our
clinical trials, along with a robust safety profile, is of utmost
importance to us at ESSA," said David
Parkinson, MD, President and CEO. "We designed this
randomized study to rigorously evaluate the clinical benefit of
adding masofaniten to enzalutamide. We made the difficult decision
to terminate this Phase 2 study following the interim analysis
because we concluded that the emerging efficacy profile of
masofaniten combined with enzalutamide would not likely meet the
primary endpoint of the study, nor our internal requirements for a
prostate cancer therapy candidate. We would like to thank our
partners, investigators, employees, and most importantly, the
patients and their families involved in our clinical trials."
Richard Glickman, LLD, Chairman
of the Board of Directors of ESSA, commented, "Senior management,
together with the board of directors, are actively focused on
preserving capital and will initiate a strategic process to explore
and review a range of strategic options focused on maximizing
shareholder value."
The Phase 2 study (NCT05075577) was designed as an open label,
two-arm randomized (2:1) trial and was planned to enroll a total of
120 patients (80 in the combination arm and 40 in the enzalutamide
single agent arm). The efficacy interim analysis included 52
enrolled patients (48% of the total planned patients) who had at
least one PSA measurement after baseline and 41 patients (34% of
total planned patients) who completed at least three months follow
up. Enrolled patients were from clinical sites located in
the United States, Canada, Australia and France. The primary study endpoint is the
proportion of patients reaching PSA90. Additional PSA-based
secondary endpoints included PSA50 response as well as PSA50 and
PSA90 response rates at 12 weeks as well as time to event
parameters (which were not mature at the time of the interim
analysis).
Primary and PSA-related Secondary Endpoints of the
Study
|
Primary
|
Secondary
|
Secondary
|
Secondary
|
Phase 2 Study
Arm
|
PSA90
response
rate*
|
PSA50
response
rate*
|
PSA50 @ 90
days
response
rate
|
PSA90 @ 90
days
response
rate
|
Enzalutamide
160mg
QD
|
73 %
|
87 %
|
86 %
|
71 %
|
Masofaniten
600mg
BID
+ enzalutamide
160mg QD
|
64 %
|
88 %
|
93 %
|
67 %
|
*The PSA90 response
rate was calculated in patients completing at least 1 month of
treatment
|
As part of the effort to focus its resources, ESSA is also
planning to terminate the other remaining company-sponsored and
investigator-sponsored clinical studies evaluating masofaniten
either as a monotherapy or in combination with other agents.
Liquidity and Outstanding Share Capital
- As of September 30, 2024, the
Company had available cash reserves and short-term investments of
$126.8 million and net working
capital of $124.3 million (unaudited
figures). The Company has no long-term debt facilities.
- As of September 30, 2024, the
Company had 44,388,551 common shares issued and outstanding, and
there were 2,920,000 common shares issuable upon the exercise of
prefunded warrants at an exercise price of $0.0001.
About the Phase 2 Study
The Phase 2 dose expansion portion of this Phase 1/2 study is a
two-arm, randomized, open-label study (NCT05075577) that evaluated
the safety, tolerability and preliminary efficacy of masofaniten,
and was expected to enroll approximately 120 patients. Criteria for
entry into the Phase 2 dose expansion were similar to those in the
Phase 1 dose escalation. Patients continued to receive androgen
deprivation therapy and were randomized 2:1 to receive either the
combination of masofaniten (600mg twice-daily ("BID")) and
enzalutamide (160mg once daily ("QD")) or enzalutamide (160mg QD)
as a single agent. Patients were eligible to remain on study
treatment as long as they tolerated treatment without disease
progression based on RECIST v1.1 and/or Prostate Cancer Clinical
Trials Working Group 3 (PCWG3) criteria.
About Masofaniten
Masofaniten (formerly known as EPI-7386) is a first-in-class
investigational oral, small molecule inhibitor of the androgen
receptor ("AR"). Masofaniten's unique mechanism of action disrupts
the AR signaling pathway, the primary pathway that drives prostate
cancer growth. The U.S. Food and Drug Administration has granted
Fast Track designation to masofaniten for the treatment of adult
male patients with mCRPC resistant to standard-of-care treatment.
ESSA retains all rights to masofaniten worldwide.
About ESSA Pharma Inc.
ESSA is a clinical-stage pharmaceutical company focused on
developing novel and proprietary therapies for the treatment of
patients with prostate cancer. For more information, please
visit www.essapharma.com, and follow us
on X and LinkedIn.
Forward-Looking Statement Disclaimer
This release contains certain information which, as presented,
constitutes "forward-looking statements" within the meaning of the
Private Securities Litigation Reform Act of 1995 and
"forward-looking information" within the meaning of applicable
Canadian securities laws (collectively, "forward-looking
statements"). Forward-looking statements include, but are not
limited to, statements that relate to future events and often
addresses expected future business and financial performance,
containing words such as "anticipate", "believe", "plan",
"estimate", "expect", and "intend", statements that an action or
event "may", "might", "could", "should", or "will" be taken or
occur, or other similar expressions and includes, but is not
limited to, statements regarding the termination of the Company's
clinical studies of masofaniten, the Company's financial
resources, the evaluation of the Company's strategic alternatives,
the primary and PSA-related endpoints of the Phase 2 study and
other statements surrounding the Company's evaluation of
masofaniten.
Forward-looking statements are subject to various known and
unknown risks and uncertainties, many of which are beyond the
ability of ESSA to control or predict, and which may cause ESSA's
actual results, performance or achievements to be materially
different from those expressed or implied thereby. Such statements
reflect ESSA's current views with respect to future events, are
subject to risks and uncertainties and are necessarily based upon a
number of estimates and assumptions that, while considered
reasonable by ESSA as of the date of such statements, are
inherently subject to significant medical, scientific, business,
economic, competitive, political and social uncertainties and
contingencies. In making forward looking statements, ESSA may make
various material assumptions, including but not limited to (i) the
accuracy of ESSA's financial projections; (ii) obtaining positive
results of clinical trials; (iii) obtaining necessary regulatory
approvals; and (iv) general business, market and economic
conditions.
Forward-looking statements are developed based on assumptions
about such risks, uncertainties and other factors set out herein
and in ESSA's Annual Report on Form 10-K dated December 12, 2023, under the heading "Risk
Factors", a copy of which is available on ESSA's profile on EDGAR
at www.sec.gov and on SEDAR+ at www.sedarplus.ca, and as
otherwise disclosed from time to time on ESSA's EDGAR and SEDAR+
profiles. Forward-looking statements are made based on management's
beliefs, estimates and opinions on the date that statements are
made and ESSA undertakes no obligation to update forward-looking
statements if these beliefs, estimates and opinions or other
circumstances should change, except as may be required by
applicable United States and
Canadian securities laws. Readers are cautioned against attributing
undue certainty to forward-looking statements.
Contacts
ESSA Pharma, Inc.
Peter Virsik, Chief Operating
Officer
778.331.0962
pvirsik@essapharma.com
Investors and Media:
Argot Partners
212.600.1902
essa@argotpartners.com
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