Survivin-targeted T cell therapy continues to
show significant, durable anti-tumor activity and is well-tolerated
in this hard-to-treat cancer patient population
5/19 patients
(26%) achieved a partial regression on target lesions
Strong
translational data link the observed clinical benefits with
DPX-Survivac’s unique mechanism of action; 87% of subjects showing
survivin-specific immune response
Poster to be
presented by Oliver Dorigo, MD, Ph.D. at the ASCO20 Virtual
Scientific Program
IMV Inc. (Nasdaq: IMV; TSX: IMV), a clinical-stage
biopharmaceutical company pioneering a novel class of targeted
cancer immunotherapies and vaccines against infectious diseases,
today reported updated clinical response and translational data
from DeCidE1, its Phase 2 study evaluating the safety and efficacy
of DPX-Survivac with intermittent low-dose cyclophosphamide (CPA)
in patients with recurrent, advanced platinum-sensitive and
-resistant ovarian cancer.
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Results from the ongoing study showed prolonged durable clinical
responses, alongside favorable tolerability, and strong
translational data linking the observed clinical benefit with
DPX-Survivac’ mechanism of action. Oliver Dorigo, M.D., Ph.D.,
Principal Investigator of the DeCidE1 study, is presenting these
results in a poster presentation at the American Society of
Clinical Oncology 2020 (ASCO20) Virtual Scientific Program.
“IMV’s targeted T-cell therapy continues to elicit a rapid and
robust immune response with survivin-specific T cells infiltrating
tumors as soon as 56 days post-treatment. These results validate
DPX-Survivac’s unique mechanism of action and support the
hypothesis that survivin-specific T cells can translate into
clinical benefits when sustained over an extended period of time,”
said Dr. Dorigo associate professor and director of gynecologic
oncology at Stanford University. “These results support
DPX-Survivac as a new and much-needed treatment option, with
potential to improve the quality of life in women with recurrent
late-stage ovarian cancer, a hard-to-treat indication where other
immunotherapies have so far had limited success.”
“With these results, DPX-Survivac continues to exhibit
significant and durable anti-tumor activity, paving the way for
targeted T cell therapies in advanced recurrent ovarian cancer and
other solid tumors. In particular, we are quite pleased to observe
an additional patient with stable disease (SD) convert to partial
response (PR), implying the potential for responses to deepen over
time with ongoing therapy. Additionally, DPX-Survivac continues to
be well tolerated, which is especially meaningful compared to
single-agent chemotherapy and other approaches in development,”
said Joanne Schindler, M.D., D.V.M., Chief Medical Officer at IMV.
“We believe these results highlight DPX-Survivac’s potential to
alter the treatment landscape in advanced ovarian cancer and
support its continued development. We look forward to providing
updates from other studies evaluating DPX-Survivac, in multiple
solid tumors and r/r DLBCL, later this year.”
Updated Results from DeCidE1
As of data cut-off date, May 2, 2020, 19 patients were evaluable
for efficacy with four patients (21%) still receiving treatment.
Notably, 18/19 evaluable patients had stage 3 or 4 disease at time
of diagnosis, the majority of whom had received >3 lines of prior therapy and were platinum
resistant. Key findings on the safety and efficacy of
DPX-Survivac/CPA are outlined below:
- 5/19 patients (26%) achieved a PR with tumor regression >30%
on target lesions
- 15/19 patients (79%) achieved disease control, defined as
Stable Disease (SD) or Partial Response (PR) on target lesions
- Tumor shrinkage of target lesions was observed in 10 patients
(53%)
- Overall, treatment was well-tolerated. The majority of
treatment-related adverse events reported were Grade 1 events and
related to reactions at the injection site.
Durable clinical benefits lasting ≥ 6 months were observed in
seven patients (37%)
- 5/7 patients (71%) have now reached duration of clinical
benefit > 10 months including three patients with PR and two
patients with SD
- The two patients with SD are about to reach the 1-year
mark
Translational analyses on longitudinally collected peripheral
blood mononuclear cell (PBMC) and tumor tissue samples link
observed clinical benefit and survivin-specific T cells, supporting
DPX-Survivac’s unique mechanism of action. Key translational
findings are outlined below:
- Treatment generated a survivin-specific CD8+ T cell response in
PBMC samples of 14/16 (87%) evaluable patients.
- Treatment induced infiltration of survivin-specific T cell
clones into the tumors as early as day 56 following treatment,
which was shown in an analysis of the TCRβ repertoires in five
subjects who achieved stable disease.
These data are presented in a poster session (Abstract Number:
6075) at the ASCO20 Virtual Scientific Program, available on-demand
to ASCO20 participants beginning at 8:00 am ET on Friday, May 29,
2020. A copy of the poster is available under “Scientific Posters”
in the "Events, Webcasts & Presentations" section of IMV’s
website.
About the DeCidE1 Study
“DeCidE1” is a Phase 2 multicenter, open-label study evaluating
the safety and effectiveness of DPX-Survivac, with intermittent
low-dose cyclophosphamide (CPA) used as an immunomodulator to
increase the level of survivin-specific T cells. This Phase 2 arm
enrolled 19 evaluable patients with recurrent, advanced
platinum-sensitive and –resistant ovarian cancer. Except for one
patient, all patients had stage 3 or 4 disease at time of
diagnosis. 12 patients had received 3 or more lines of prior
therapy.
Patients received 2 subcutaneous injections of DPX-Survivac
three weeks apart and every eight weeks thereafter, and
intermittent low dose CPA one week on and one week off for up to 1
year. Paired tumor biopsies were performed prior to treatment and
on treatment.
Primary endpoints of this study are overall response rate,
disease control rate and safety. Secondary endpoints include cell
mediated immunity, immune cell infiltration in paired biopsy
samples, duration of response, time to progression, overall
survival and biomarker analyses.
About DPX-Survivac
DPX-Survivac is the lead candidate in IMV’s new class of
targeted immunotherapies designed to elicit antigen-specific
functional, robust and sustained de novo T cell response. IMV
believes this mechanism of action is key to generating durable
solid tumor regressions. DPX-Survivac consists of five unique
HLA-restricted survivin peptides formulated in IMV’s proprietary
DPX drug delivery platform and known to induce a cytotoxic CD8+ T
cell response against survivin expressing cancer cells.
Survivin, recognized by the National Cancer Institute (NCI) as a
promising tumor-associated antigen, is broadly over-expressed in
most cancer types and plays an essential role in antagonizing cell
death, supporting tumor-associated angiogenesis and promoting
resistance to chemotherapies. IMV has identified over 20 cancer
indications in which survivin can be targeted by DPX-Survivac.
DPX-Survivac has received Fast Track designation from the U.S.
Food and Drug Administration (FDA) as maintenance therapy in
advanced ovarian cancer, as well as orphan drug designation status
from the U.S. FDA and the European Medicines Agency (EMA) in the
ovarian cancer indication.
About IMV
IMV Inc. is a clinical stage biopharmaceutical company dedicated
to making immunotherapy more effective, more broadly applicable,
and more widely available to people facing cancer and other serious
diseases. IMV is pioneering a new class of cancer-targeted
immunotherapies and vaccines based on the Company’s proprietary
drug delivery platform. This patented technology leverages a novel
mechanism of action that enables the programming of immune cells in
vivo, which are aimed at generating powerful new synthetic
therapeutic capabilities. IMV’s lead candidate, DPX-Survivac, is a
T cell-activating immunotherapy that combines the utility of the
platform with a target: survivin. IMV is currently assessing
DPX-Survivac as a monotherapy in advanced ovarian cancer, as well
as a combination therapy in multiple clinical studies with Merck.
IMV is also developing a DPX-based vaccine to fight against
COVID-19. Visit www.imv-inc.com and connect with us on Twitter and
LinkedIn.
Cautionary Language Regarding Forward-Looking Statements
This press release contains forward-looking information under
applicable securities law. All information that addresses
activities or developments that we expect to occur in the future is
forward-looking information. Forward-looking statements are based
on the estimates and opinions of management on the date the
statements are made. In the press release, such forward-looking
statements include, but are not limited to, statements regarding
the FDA potentially granting accelerated regulatory approval of
DPX-Survivac and the timing of expected results from other
DPX-Survivac’s studies with other tumor types. However, they should
not be regarded as a representation that any of the plans will be
achieved. Actual results may differ materially from those set forth
in this press release due to risks affecting the Corporation,
including access to capital, the successful design and completion
of clinical trials and the receipt and timely receipt of all
regulatory approvals. IMV Inc. assumes no responsibility to update
forward-looking statements in this press release except as required
by law. These forward-looking statements involve known and unknown
risks and uncertainties and those risks and uncertainties include,
but are not limited to, our ability to access capital, the
successful and timely completion of clinical trials and studies,
the receipt of all regulatory approvals and other risks detailed
from time to time in our ongoing quarterly filings and annual
information form Investors are cautioned not to rely on these
forward-looking statements and are encouraged to read IMV’s
continuous disclosure documents, including its current annual
information form, as well as its audited annual consolidated
financial statements which are available on SEDAR at www.sedar.com
and on EDGAR at www.sec.gov/edgar
View source
version on businesswire.com: https://www.businesswire.com/news/home/20200529005281/en/
Investor Relations Marc Jasmin, Senior Director, Investor
Relations, IMV O: (902) 492-1819 ext : 1042 M: (514) 617-9481
E: mjasmin@imv-inc.com
Josh Rappaport, Director, Stern IR O: (212) 362-1200 E:
josh.rappaport@sternir.com
Media Delphine Davan, Director of Communications, IMV O:
(514) 968-1046 E: ddavan@imv-inc.com
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