Combination of Botensilimab/Balstilimab with
MiNK Therapeutics’ AgenT-797 Shows Strong Immune Activation and
Potential to Enhance Outcomes in Refractory Gastric Cancer
Agenus Inc. (Nasdaq: AGEN), a leader in immuno-oncology, today
presented data at the American Association for Cancer Research
(AACR) IO Annual Meeting in Los Angeles, California. The oral
presentation highlights translational data from the ongoing Phase 2
study evaluating botensilimab (BOT, multifunctional Fc-enhanced
anti-CTLA-4) and balstilimab (BAL, anti-PD-1) in combination with
MiNK Therapeutics’ agenT-797, an allogeneic invariant natural
killer T (iNKT) cell therapy, in patients with refractory (2L+)
gastric cancer (NCT06251973).
“These latest data demonstrate the remarkable potential of
combining BOT/BAL with a novel iNKT cell therapy to broaden and
intensify immune responses against resistant gastric tumors,” said
Dr. Dhan Chand, Vice President of Research at Agenus. “By driving
strong IFNγ production, deep T-cell infiltration, and memory T-cell
activation—even in PD-1–refractory patients—the addition of
agenT-797 to BOT/BAL could redefine what’s possible in late-line
gastric cancer. We’re particularly encouraged by how these
therapies work in concert with standard-of-care chemotherapy to
transform immunologically 'cold' tumors into 'hot' immune inflamed
tumors, potentially offering a new therapeutic paradigm for
patients facing this challenging disease.”
Highlights
- Broad Immune Activation: The addition of MiNK’s
allogeneic iNKT therapy, agenT-797, to BOT/BAL drove robust immune
activation, including elevated interferon-gamma (IFNγ) levels,
indicating potent systemic engagement and overcoming
immunosuppressive pathways in PD-1–refractory gastric tumors.
- Enhanced T cell Infiltration and Memory T-Cell
Expansion: A marked increase in tumor-infiltrating lymphocytes
(TILs), together with heightened peripheral memory T-cell
activation, underscores the potential for long-lasting anti-tumor
immunity when combining BOT/BAL with agenT-797 (allo-iNKTs).
- Optimized Sequencing with Chemotherapy: Early
administration of agenT-797 alongside BOT/BAL, before standard
chemotherapy significantly amplifies immune responses, potentially
reducing tumor recurrence through optimal T-cell priming,
activation and mobilization.
Presentation Details:
Abstract Title: Biomarker analysis from Phase 2 study of
AgenT-797 (invariant natural killer T-cells), botensilimab (a
Fc-enhanced CTLA-4 Inhibitor) with balstilimab (anti-PD-1) in PD-1
refractory gastroesophageal cancer (GEC)
Presenting Author: Dr. Samuel Cytryn, Memorial Sloan Kettering
Cancer Center, New York, New York
Oral Session: Proffered Papers, Session 2; 1:39-1:45 p.m.
PST
Poster Session: Poster Session, A; 1:45-4:45 p.m. PST
Date: Monday, February 24th
The presentation will be available on the publications page of
the Agenus website at https://agenusbio.com/publications/ following
the start of the conference session.
About Agenus
Agenus is a leading immuno-oncology company targeting cancer
with a comprehensive pipeline of immunological agents. The company
was founded in 1994 with a mission to expand patient populations
benefiting from cancer immunotherapy through combination
approaches, using a broad repertoire of antibody therapeutics,
adoptive cell therapies (through MiNK Therapeutics) and adjuvants
(through SaponiQx). Agenus has robust end-to-end development
capabilities, across commercial and clinical cGMP manufacturing
facilities, research and discovery, and a global clinical
operations footprint. Agenus is headquartered in Lexington, MA. For
more information, visit www.agenusbio.com or @agenus_bio.
Information that may be important to investors will be routinely
posted on our website and social media channels.
About Botensilimab (BOT)
Botensilimab (BOT) is a human Fc enhanced CTLA-4 blocking
antibody designed to boost both innate and adaptive anti-tumor
immune responses. Its novel design leverages mechanisms of action
to extend immunotherapy benefits to “cold” tumors which generally
respond poorly to standard of care or are refractory to
conventional PD-1/CTLA-4 therapies and investigational
therapies.
Approximately 1,100 patients have been treated with botensilimab
and/or balstilimab in phase 1 and phase 2 clinical trials.
Botensilimab alone, or in combination with Agenus’ investigational
PD-1 antibody, balstilimab, has shown clinical responses across
nine metastatic, late-line cancers. For more information about
botensilimab trials, visit www.clinicaltrials.gov with the
identifiers NCT03860272, NCT05608044, NCT05630183, and
NCT05529316.
About Balstilimab (BAL)
Balstilimab is a novel, fully human monoclonal immunoglobulin G4
(IgG4) designed to block PD-1 (programmed cell death protein 1)
from interacting with its ligands PD-L1 and PD-L2. Botensilimab
augments immune responses across a wide range of tumor types by
priming and activating T cells, downregulating intratumoral
regulatory T cells, activating myeloid cells and inducing long-term
memory responses.
About AgenT-797
AgenT-797 is an allogeneic invariant natural killer T (iNKT)
cell therapy that harnesses the dual power of innate and adaptive
immunity. iNKTs function as “master regulators,” combining the
cytotoxic capabilities of NK cells with T-cell–like antigen
recognition and memory. This unique biology enables a robust,
pathogen-agnostic immune response that can be directed against
hard-to-treat tumors.
Manufactured by MiNK Therapeutics in Lexington, MA, agenT-797 is
a scalable, off-the-shelf product designed to provide accessible,
transformative treatment options. In clinical trials, agenT-797 can
bolster peripheral memory T-cell activation, enhance tumor
infiltration, and potentially improve outcomes for patients with
solid cancers (Cytryn et al. AACR IO 2024, Oncogene. 2024) and to
combat inflammation in critically ill patients with severe
respiratory pathology (Nature Communications. 2024).
Forward-Looking Statements
This press release contains forward-looking statements that are
made pursuant to the safe harbor provisions of the federal
securities laws, including statements regarding its botensilimab
and balstilimab programs, expected regulatory timelines and
filings, and any other statements containing the words "may,"
"believes," "expects," "anticipates," "hopes," "intends," "plans,"
"forecasts," "estimates," "will," “establish,” “potential,”
“superiority,” “best in class,” and similar expressions are
intended to identify forward-looking statements. These
forward-looking statements are subject to risks and uncertainties
that could cause actual results to differ materially. These risks
and uncertainties include, among others, the factors described
under the Risk Factors section of our most recent Annual Report on
Form 10-K for 2023, and subsequent Quarterly Reports on Form 10-Q
filed with the Securities and Exchange Commission. Agenus cautions
investors not to place considerable reliance on the forward-looking
statements contained in this release. These statements speak only
as of the date of this press release, and Agenus undertakes no
obligation to update or revise the statements, other than to the
extent required by law. All forward-looking statements are
expressly qualified in their entirety by this cautionary
statement.
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