BriaCell Therapeutics Corp. (Nasdaq: BCTX, BCTXW) (TSX: BCT)
(“BriaCell” or the “Company”), a clinical-stage biotechnology
company that develops novel immunotherapies to transform cancer
care, is pleased to showcase its impressive survival and clinical
benefit data in MBC patients, including those with CNS metastases,
treated with the Bria-IMT™ plus CPI regimen. The data is featured
in BriaCell’s “Spotlight” poster presentation session, at the 2024
San Antonio Breast Cancer Symposium® (SABCS®) held at Henry B.
Gonzalez Convention Center, San Antonio, TX.
“Metastatic breast cancer remains an essentially
incurable disease, with a significant unmet medical need in
patients who are relapsed/refractory to recently approved therapies
such as CPIs and antibody-drug conjugates (ADCs),” stated Dr.
William V. Williams, BriaCell’s President & CEO. “We are very
pleased with the Bria-IMT™ combination regimen’s tolerability
profile, and most importantly its outstanding clinical activity in
heavily pre-treated patients who failed other therapeutic
options.”
“In addition to our striking survival data in
MBC patients, we are excited by potential biomarkers for early
identification of patients who would benefit from treatment with
the Bria-IMT™ combination regimen,” noted Giuseppe Del Priore, MD,
MPH, BriaCell’s Chief Medical Officer. “We expect to replicate
Phase 2’s impressive survival and clinical benefit data in our
ongoing pivotal Phase 3 study.”
“While CNS metastatic disease has historically
had a very poor prognosis, our clinical data to date, shows solid
survival and clinical benefit in patients with CNS metastasis,”
stated Sailaja Kamaraju, MD, Assistant Professor of Medicine at the
Medical College of Wisconsin, Division of Hematology and Oncology.
“We are optimistic that the Bria-IMT™ combination regimen, with its
unique targeted mechanism of action, may be able to produce
meaningful clinical and survival benefits in other cancer patients
with CNS metastases who have lost hope with little to no other
therapeutic options.”
The data presented is from the fully enrolled
BriaCell Phase 2 combination study of Bria-IMT™ plus CPI.
An aggregate of 54 MBC patients were enrolled in
the study – all treated with the Bria-IMT™ combination regimen {11
patients received KEYTRUDA® (pembrolizumab), and 43 patients
received Incyte’s retifanlimab with one patient cross over from the
KEYTRUDA® study to retifanlimab}. Data is available on all 54 of
these heavily pre-treated metastatic breast cancer patients
(average number of prior treatments = 6). Of these 54 patients, 37
were treated with the formulation currently under investigation in
BriaCell’s ongoing pivotal Phase 3 study in metastatic breast
cancer (listed on ClinicalTrials.gov as NCT06072612). Final median
overall survival calculation for the patients in the Phase 2
portion of the study is pending, as most of these patients remain
alive over 1 year following their start on the study. No Bria-IMT™
related discontinuations have been reported to date.
The details about the Spotlight presentation and
other poster sessions are as follows:
Abstract Number: SESS-1071 (Spotlight
Poster)Title: Overall survival results of
Bria-IMT™ allogenic whole cell-based cancer
vaccineTime: Wednesday, December 11, 2024 7:00 AM
– 8:30 AM CSTPresentation ID: PS3-06
Bria-IMT™ regimen’s impressive OS and
tolerability in MBC patients
- Median overall survival (OS) to
date of 13.4 months for Phase 2 patients treated with the Phase 3
formulation (15.6 months for those treated since 2022 with the
Phase 3 formulation) double that of comparable patients in the
literature (Cortes J, et al. Annals of Oncology 2018; Kazmi S, et
al. Breast Cancer Res Treat. 2020; O’Shaughnessy J et al. Breast
Cancer Res Treat. 2022; Tripathy D, et al. JAMA Oncol. 2022; Bardia
A, et al. J Clin Oncol. 2024)
- Final Phase 2 OS calculation is
pending as many patients remain alive well over 1 year after
starting the study
- Median overall survival (OS) for
patients who received the Phase 3 formulation in the Phase 2
portion of the study who also developed an immune response to the
vaccine as measured by delayed-type hypersensitivity (DTH) not yet
reached with >1 year follow-up
- 13.7 months median OS in MBC
patients with central nervous system (CNS)/intracranial tumors
treated with the Bria-IMT™ regimen with or without a CPI
- Objective response rates (ORR) and
clinical benefit rates (CBR) were observed across all MBC patient
subsets, but positive clinical outcomes were more prominent in
HER2+ and HR+/HER2- patient subsets
- Bria-IMT™ regimen was
well-tolerated and produced clinical benefit in heavily pretreated
MBC patients
- Patients who developed a DTH
response had lower neutrophil to lymphocyte ratio (NLR), suggesting
improved clinical benefit in these patients
- Delayed-type hypersensitivity (DTH)
response, and circulating tumor cells (CTC) levels were
significantly different between patients who responded vs those who
did not respond to the Bria-IMT™ combination regimen
In conclusion, clinical findings to date support
the potential safety and efficacy of Bria-IMT™, along with its
potential use in CNS metastases, as well as the possible use of
biomarkers to predict clinical outcomes in BriaCell’s ongoing
pivotal Phase 3 study in MBC.
Abstract Number:
SESS-1431Title: Identification of antigenic
determinants in SV-BR-1 derived cellular breast cancer
vaccinesTime: Wednesday, December 11, 2024 5:30 –
7:00 PM CSTPresentation ID: P2-06-02
Summary: BriaCell successfully
identified immunogenic (i.e. immune system activating) peptides in
patients treated with Bria-IMT™, a cell-based cancer vaccine, and
showed Bria-IMT™’s ability to produce a targeted immune response
against tumor antigens.
- Key immunogenic peptides detected
included those with post-translational modifications (PTMs), such
as citrullination and cysteinylation, an important type of
neoantigen that may be shared across many patients with cancer
- Highlighted the advantage of
cell-based cancer vaccines over RNA and peptide-based vaccines
including their ability to present a broad and diverse repertoire
of antigens (i.e. both conventional and unconventional types)
- Cell-based cancer vaccines also
display unknown, patient-specific neoantigens that are hard to
reproduce with RNA or peptide vaccines
- Diverse antigen presentation
produces a robust, polyclonal immune response, engaging both CD8+
and CD4+ T cells against multiple tumor target
In conclusion, scientific data presented
suggests that the unique mechanism of cell-based cancer vaccines
may reduce cancer cells’ immune escape and may potentially lead to
strong and long-lasting clinical outcomes in cancer patients.
Abstract Number:
SESS-2217Title: PD-L1 upregulation in circulating
tumor associated cells predicts for clinical outcomes in a phase
I/II clinical trial using SV-BR-1-GM vaccine with the checkpoint
inhibitor retifanlimab in metastatic breast cancer patients, an
interim analysisTime: Wednesday, December 11, 2024
12:00 – 2:00 PM CSTPresentation ID: P1-01-17
Summary:Interim analysis after
at least one year of Bria-IMT™ plus CPI regimen shows the
following:
- Significantly lowered levels of
circulating tumor cells (CTCs) and cancer associated
macrophage-like cells (CAMLs) in 40% of heavily pre-treated MBC
patients
- Lower CTCs/CAMLs levels were
significantly correlated with better survival outcomes (i.e. better
PFS and trended for better OS)
- Bria-IMT™ appeared to increase
PD-L1 levels in 15 patients which correlated with better clinical
responses to combination treatment with the anti-PD-1 check point
inhibitor retifanlimab
In conclusion, clinical data support the
combination regimen in our ongoing pivotal Phase 3 study and
suggests CTCs and CAMLs and PD-L1 levels may be relevant indicators
of clinical outcome in MBC patients treated with Bria-IMT™ plus
CPI.
Abstract Number:
SESS-1068Abstract Title: ASTRO-VAC CNS: Bria-IMT™
in the management of tumor agnostic metastatic CNS
lesionsTime: Wednesday, December 11, 2024 5:30 –
7:00 PM CSTPresentation ID: P2-10-24
Results: The poster provides
the details of a planned Phase 2 study design expanding the use of
Bria-IMT™ + CPI to tumor agnostic cancer patients (i.e. kidney
cancer, brain cancer, etc.) with central nervous system (CNS)
metastasis.
To view the posters, please visit
https://briacell.com/scientific-publications/.
About BriaCell Therapeutics
Corp.
BriaCell is a clinical-stage biotechnology
company that develops novel immunotherapies to transform cancer
care. More information is available at https://briacell.com/.
Safe Harbor
This press release contains “forward-looking
statements” that are subject to substantial risks and
uncertainties. All statements, other than statements of historical
fact, contained in this press release are forward-looking
statements. Forward-looking statements contained in this press
release may be identified by the use of words such as “anticipate,”
“believe,” “contemplate,” “could,” “estimate,” “expect,” “intend,”
“seek,” “may,” “might,” “plan,” “potential,” “predict,” “project,”
“target,” “aim,” “should,” “will,” “would,” or the negative of
these words or other similar expressions, although not all
forward-looking statements contain these words. Forward-looking
statements, including those about the potential safety and efficacy
of Bria-IMT™, along with its potential use in CNS metastases;
biomarkers assisting with early identification of patients who
would benefit from treatment with the Bria-IMT™ combination
regimen; BriaCell expecting to replicate Phase 2’s survival and
clinical benefit data in its ongoing pivotal Phase 3 study and
the Company’s plans to share the data in the coming months; the
Bria-IMT™ combination regimen’s ability to produce meaningful
clinical and survival benefits in other cancer patients with CNS
metastasis; the Company’s ongoing evaluation of biomarkers to
predict clinical outcomes in its ongoing pivotal Phase 3 study
in MBC; cell-based cancer vaccines potentially reducing cancer
cells’ immune escape and leading to strong and long-lasting
clinical outcomes in cancer patients; and CTCs, CAMLs and PD-L1
levels having the potential to be relevant indicators of clinical
outcomes in MBC patients treated with Bria-IMT™ plus CPI are based
on BriaCell’s current expectations and are subject to inherent
uncertainties, risks, and assumptions that are difficult to
predict. Further, certain forward-looking statements, such as those
are based on assumptions as to future events that may not prove to
be accurate. These and other risks and uncertainties are described
more fully under the heading “Risks and Uncertainties” in the
Company’s most recent Management’s Discussion and Analysis, under
the heading “Risk Factors” in the Company’s most recent Annual
Information Form, and under “Risks and Uncertainties” in the
Company’s other filings with the Canadian securities regulatory
authorities and the U.S. Securities and Exchange Commission, all of
which are available under the Company's profiles on SEDAR+ at
www.sedarplus.ca and on EDGAR at
www.sec.gov. Forward-looking statements contained
in this announcement are made as of this date, and BriaCell
Therapeutics Corp. undertakes no duty to update such information
except as required under applicable law.
Neither the Toronto Stock Exchange nor its
Regulation Services Provider (as that term is defined in the
policies of the Toronto Stock Exchange) accepts responsibility for
the adequacy or accuracy of this release.
Contact Information
Company Contact:William V.
Williams, MDPresident & CEO1-888-485-6340info@briacell.com
Media Relations:Jules
AbrahamCORE IRjulesa@coreir.com
Investor Relations Contact:CORE
IRinvestors@briacell.com
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