Elicio Therapeutics, Inc. (Nasdaq: ELTX, “Elicio Therapeutics” or
“Elicio”), a clinical-stage biotechnology company developing a
pipeline of novel immunotherapies for the treatment of cancer,
presented updated preliminary results from the ongoing AMPLIFY-7P
Phase 1 clinical trial (NCT05726864) of ELI-002, an Amphiphile
(“AMP”) cancer vaccine that targets KRAS-mutant tumors at the
Society for Immunotherapy of Cancer (“SITC”) 2024 Annual Meeting.
The poster presentation includes updated translational data
highlighting the relationship between vaccine immunogenicity and
DFS. The AMPLIFY-7P study is evaluating ELI-002 in patients with
mKRAS-driven solid tumors following standard locoregional treatment
and who remain at risk of disease recurrence. The randomized Phase
2 portion of AMPLIFY-7P in patients with pancreatic cancer is
ongoing, with enrollment expected to be completed in Q4 2024.
ELI-002 immunogenicity was based on a longitudinal ex vivo
analysis of peripheral T cells collected from a total of 12
evaluable patients who received either a 1.4 mg dose or the
recommended Phase 2 dose (“RP2D”) of 4.9 mg, with a September 11,
2024 cutoff date. Key observations include:
- mKRAS-specific T cell responses
versus baseline were observed in all evaluable patients; median
response in 4.9 mg (RP2D) group was 12-fold higher than the 1.4 mg
dose group
- T cell specificities covered all
seven KRAS mutants targeted by ELI-002; strongest responses
observed were against the most common variants, including KRAS
G12R, G12D, and G12V
- Induced mKRAS-specific T cells were
fully functional and capable of secreting both granzyme B and
perforin
- Magnitude of T cell response
correlated with duration of DFS, based on a May 23, 2024 cutoff
date; highest three quartiles of T cell responders have not yet
reached mDFS, whereas the lowest quartile achieved a mDFS of 3.1
months (p=0.0027)
- T cell responses against mKRAS
antigens were shown to be durable, extending up to 1.5 years
- Antigen spreading detected in 100%
of RP2D-treated patients (n=6), with T cell responses observed
against 67.5% of tested neoantigens identified from
patient-specific mutanomes—suggesting ELI-002-induced tumor
immunosurveillance to personalized tumor neoantigens beyond
mKRAS
- As of a May 23, 2024 safety data
cutoff, ELI-002 remains safe and well-tolerated, with no
dose-limiting toxicities or cytokine release syndrome observed
Christopher Haqq, M.D., Ph.D., Elicio’s Executive Vice
President, Head of Research and Development and Chief Medical
Officer, commented, “We are encouraged to see a robust expansion of
T cells targeting mutant KRAS antigens as well as a clear
relationship between T cell response and DFS in the Phase 1 portion
of AMPLIFY-7P. Furthermore, we are encouraged by the observed
induced T cell reactivity against personalized neoantigens, which
could improve the breadth and durability of tumor
immunosurveillance. These data recapitulate the previous findings
from the separate AMPLIFY-201 study, published earlier this year in
Nature Medicine. We expect to provide an additional clinical data
update from AMPLIFY-201 in December.”
About Elicio Therapeutics
Elicio Therapeutics, Inc. (Nasdaq: ELTX)
is a clinical-stage biotechnology company advancing novel
immunotherapies to prevent the recurrence of high-prevalence
cancers, including mKRAS-positive pancreatic and colorectal
cancers. Elicio intends to build on recent clinical successes in
the personalized cancer vaccine space to develop effective,
off-the-shelf vaccines. Elicio’s AMP technology aims to enhance the
education, activation, and amplification of cancer-specific T
cells relative to conventional vaccination strategies, with the
goal of promoting durable cancer immunosurveillance in
patients. Elicio’s ELI-002 lead program is an off-the-shelf
vaccine candidate targeting the most common KRAS mutations, which
drive approximately 25% of all solid tumors. ELI-002 is being
studied in an ongoing, randomized clinical trial in patients with
mKRAS-positive pancreatic cancer who completed standard therapy but
remain at high risk of relapse. Elicio’s pipeline includes
additional off-the-shelf therapeutic cancer vaccines, including
ELI-007 and ELI-008, that target BRAF-driven cancers and p53
hotspot mutations, respectively. For more information, please
visit www.elicio.com.
About ELI-002
Our lead product candidate, ELI-002, is a structurally novel
investigational AMP cancer vaccine that targets cancers that are
driven by mutations in the KRAS-gene—a prevalent driver of many
human cancers. ELI-002 is comprised of two powerful components that
are built with our AMP technology consisting of AMP-modified mutant
KRAS peptide antigens and ELI-004, an AMP-modified CpG
oligodeoxynucleotide adjuvant that is available as an off-the-shelf
subcutaneous administration.
ELI-002 2P (2-peptide formulation) has been studied in the Phase
1 (AMPLIFY-201) trial in patients with high relapse risk
mKRAS-driven solid tumors, following surgery and chemotherapy
(NCT04853017). ELI-002 7P (7-peptide formulation) is currently
being studied in a Phase 1/2 (AMPLIFY-7P) trial in patients with
mKRAS-driven pancreatic cancer (NCT05726864). The ELI-002 7P
formulation is designed to provide immune response coverage against
seven of the most common KRAS mutations present in 25% of all solid
tumors, thereby increasing the potential patient population for
ELI-002.
About the Amphiphile Platform
Our proprietary AMP platform delivers investigational
immunotherapeutics directly to the “brain center” of the immune
system – the lymph nodes. We believe this site-specific delivery of
disease-specific antigens, adjuvants and other immunomodulators may
efficiently educate, activate and amplify critical immune cells,
potentially resulting in induction and persistence of potent
adaptive immunity required to treat many diseases. In preclinical
models, we have observed lymph node-specific engagement driving
therapeutic immune responses of increased magnitude, function and
durability. We believe our AMP lymph node-targeted approach will
produce superior clinical benefits compared to immunotherapies that
do not engage the lymph nodes based on preclinical studies.
Our AMP platform, originally developed at the Massachusetts
Institute of Technology, has broad potential in the cancer space to
advance a number of development initiatives through internal
activities, in-licensing arrangements or development collaborations
and partnerships.
The AMP platform has been shown to deliver immunotherapeutics
directly to the lymph nodes by latching on to the protein albumin,
found in the local injection site, as it travels to lymphatic
tissue. In preclinical models, we have observed lymph node-specific
engagement driving immune responses of increased magnitude,
function and durability.
Cautionary Note on Forward-Looking
Statements
Certain statements contained in this communication regarding
matters that are not historical facts, are forward-looking
statements within the meaning of Section 21E of the Securities
Exchange Act of 1934, as amended, and the Private Securities
Litigation Reform Act of 1995, known as the PSLRA. These include
statements regarding Elicio’s planned clinical programs, including
planned clinical trials, the potential of Elicio’s product
candidates, including the observed induced T cell reactivity
against personalized neoantigens, which could improve the breadth
and durability of tumor immunosurveillance; the expected
participation and presentation at upcoming conferences and medical
meetings, and other statements regarding management’s intentions,
plans, beliefs, expectations or forecasts for the future, and,
therefore, you are cautioned not to place undue reliance on them.
No forward-looking statement can be guaranteed, and actual results
may differ materially from those projected. Elicio undertakes no
obligation to publicly update any forward-looking statement,
whether as a result of new information, future events or otherwise,
except to the extent required by law. We use words such as
“anticipates,” “believes,” “plans,” “expects,” “projects,”
“future,” “intends,” “may,” “will,” “should,” “could,” “estimates,”
“predicts,” “potential,” “continue,” “guidance,” and similar
expressions to identify these forward-looking statements that are
intended to be covered by the safe-harbor provisions of the PSLRA.
Such forward-looking statements are based on our expectations and
involve risks and uncertainties; consequently, actual results may
differ materially from those expressed or implied in the statements
due to a number of factors, including, but not limited to, Elicio’s
financial condition, including its anticipated cash runway and
ability to obtain the funding necessary to advance the development
of ELI-002 and any other future product candidates, and Elicio’s
ability to continue as a going concern; Elicio’s plans to develop
and commercialize its product candidates, including ELI-002; the
timing of initiation of Elicio’s planned clinical trials, including
Elicio’s expected completion of enrollment for the AMPLIFY-7P Phase
2 randomized clinical trial in the fourth quarter of 2024; the
timing of the availability of data from Elicio’s clinical trials,
including updated data from the AMPLIFY-201 trial expected in
December 2024 and Phase 2 interim event-driven DFS analysis from
the AMPLIFY-7P trial expected in the first half of 2025; the timing
of any planned investigational new drug application or new drug
application; Elicio’s plans to research, develop and commercialize
its current and future product candidates; and Elicio’s estimates
regarding future revenue, expenses, capital requirements and need
for additional financing.
New factors emerge from time to time, and it is not possible for
us to predict all such factors, nor can we assess the impact of
each such factor on the business or the extent to which any factor,
or combination of factors, may cause actual results to differ
materially from those contained in any forward-looking statements.
These risks are more fully discussed in the Annual Report on Form
10-K filed with the SEC on March 29, 2024, as amended on April 29,
2024, under the heading “Risk Factors”, and any subsequent reports
and other documents filed from time to time with the SEC.
Forward-looking statements included in this release are based on
information available to Elicio as of the date of this release.
Elicio does not undertake any obligation to update such
forward-looking statements to reflect events or circumstances after
the date of this release, except to the extent required by law.
Investor Relations Contact
Carlo Tanzi, Ph.D.ctanzi@kendallir.com
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