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,
today announced that it will be sharing pipeline updates for all
investigational candidates at the upcoming American Association for
Cancer Research (“AACR”) Annual Meeting, taking place in San Diego,
California from April 5-10, 2024. Among the data presented will be
updated immunogenicity data from the ongoing Phase 1 (AMPLIFY-201)
study of ELI-002, an off-the-shelf investigational therapeutic
cancer vaccine for patients with mutant Kirsten rat sarcoma
(“mKRAS”)-driven pancreatic and colorectal cancers. Preclinical
data on vaccine candidates, ELI-007 and ELI-008, investigational
peptide vaccines targeting BRAF and p53-driven cancers,
respectively, will also be shared.
In the first-in-human, Phase 1 (AMPLIFY-201) study, ELI-002 was
given as adjuvant treatment for patients with high relapse-risk
mKRAS-driven colorectal cancer (“CRC”) and pancreatic ductal
adenocarcinoma (“PDAC”). A majority of patients who received the
booster immunizations maintained or increased mKRAS-specific T cell
responses relative to baseline. ELI-002 demonstrated
several key advantages, including lymph node-targeted vaccine
design, potent immunogenicity with balanced CD4+ and CD8+ T cell
responses, HLA-agnostic activity, and targeting of mKRAS antigens
critical for tumor survival. The mKRAS-specific CD4 and CD8 T cells
generated by ELI-002 exhibited increased cytotoxic function and
development of favorable memory phenotype. Regulatory T cell
responses were not detected. Antigen spreading was observed
following ELI-002 vaccination, with patient-specific tumor
neoantigen-directed T cell responses detected in the majority of
evaluated patients using direct ex vivo immunogenicity assays.
"Earlier data published in Nature Medicine demonstrate that our
off-the-shelf lymph node-targeted cancer vaccine candidate,
ELI-002, induces memory T cell responses. With longer follow-up, we
observed response durability and added antigen-spreading to the
mechanism of ELI-002, where we saw additional personal neoantigen
responses join together with mutated KRAS responses creating a
precision response that may lead to enhanced clinical activity,”
said Christopher Haqq, M.D., Ph.D., Elicio’s Executive Vice
President, Head of Research and Development, and Chief Medical
Officer. “Following positive early findings from the 2-peptide
formulation of ELI-002, we initiated a randomized Phase 2 study of
our 7-peptide formulation, ELI-002 7P, in adjuvant pancreatic
cancer (NCT05726864). We expect to share interim 7-peptide ELI-002
data from the Phase 1A arm in the second quarter of 2024.”
Peter DeMuth, Ph.D., Chief Scientific Officer at Elicio
Therapeutics, added, “These preclinical data demonstrate that
ELI-007 and ELI-008 induce strong tumor antigen-specific T cell
responses targeting BRAF and p53 mutations, respectively. ELI-007
and ELI-008 induced highly potent and functional T cell responses,
often ten to a hundred-fold higher than comparator. These data
build on previous data showing that the AMP strategy can improve
the potency of vaccine immunotherapy by delivering vaccine
components directly to the lymph nodes, the ‘command center’ of the
immune system. These data support the broad applicability of the
technology and represent promising therapeutic product
opportunities targeting mutations shared in a large fraction of
human solid cancers.”
Poster Presentation Summary
Presentation Title: Durable immunogenicity of
ELI-002 2P in AMPLIFY-201: Lymph node targeted mKRAS-specific
amphiphile vaccine in pancreatic and colorectal
cancerSession Title: First-in-Human Phase I
Clinical Trials 1Session Date and Time: Monday,
April 8, 2024, 1:30 PM – 5:00 PM PT
- ELI-002 2P consists
of 2 Amph-modified mKRAS peptide antigens, Amph-G12D and Amph-G12R
(Amph-Peptides 2P), and an Amph-modified immune-stimulatory
oligonucleotide adjuvant (Amph-CpG-7909).
- ELI-002 2P was
administered as an adjuvant treatment for patients with high
relapse-risk mutant KRAS PDAC and CRC.
- 25 patients received
ELI-002 2P at 1.4 mg of Amph-Peptides 2P and Amph-CpG-7909 at 5
escalating dose levels: 0.1, 0.5, 2.5, 5, and 10 mg.
- Peripheral blood and
circulating tumor DNA (“ctDNA”) or serum tumor antigen were
collected longitudinally to assess T cell immunogenicity and
reductions in clinical tumor biomarkers.
- A majority of
patients who received ELI-002 booster immunizations maintained or
increased mKRAS-specific T cell responses relative to baseline.
Durable responses were associated with increased memory T cell
phenotype compared to baseline.
- ELI-002 induced
increased mKRAS-specific CD4 and CD8 T cells with cytotoxic
function, associated with increased memory phenotype in a majority
of patients.
- CD4+ T regulatory
cells were not induced after ELI-002 2P immunization.
- Antigen spreading
was observed with T cell responses to patient-specific tumor
mutations (not mKRAS) after ELI-002 2P vaccination in a majority of
patients tested.
- Data demonstrated
several advantages of ELI-002 including lymph node-targeted vaccine
design, potent immunogenicity with durable and balanced CD4+ and
CD8+ T cell responses, increased T cell cytotoxic function, and
antigen spreading to induce T cells targeting additional tumor
mutations beyond mKRAS.
Presentation Title: AMP-peptide vaccination
against mutant BRAF epitopes promotes lymph node delivery to
generate potent, functional T cell immunitySession
Title: Vaccines, Antigens, and Antigen Presentation
1Session Date and Time: Tuesday, April 9, 2024,
9:00 AM – 12:30 PM PT
- Our preclinical program, ELI-007, is an investigational
multivalent lymph node–targeted AMP peptide vaccine comprised of
the V600E and V600K mutant antigens, developed to target BRAF gene
mutations.
- AMP-immunization generated robust in vivo immune responses
yielding strong T cell activation against mBRAF epitopes.
- Lymph node-targeted AMP-vaccination resulted in a 19-fold
increase in immune response after only 3 doses and a 42-fold
increase after 5 doses when compared to conventional comparator
vaccines.
- Induced T cells were polyfunctional exhibiting the production
of multiple effector cytokines (IFNγ, TNFα, IL2, GM-CSF) as well as
cytotoxic molecules (Granzyme B) important in the lysis of tumor
cells.
- Substantial populations of mBRAF-specific T cells were found
patrolling peripheral organs like the lung, which is one of the
predominant sites for metastatic spread in melanoma and colorectal
carcinoma.
Presentation Title: AMP-peptide vaccination
against multiple p53 mutant epitopes promotes lymph node delivery
to generate potent, functional T cell immunitySession
Title: Vaccines, Antigens, and Antigen Presentation
1Session Date and Time: Tuesday, April 9,
2024, 9:00 AM – 12:30 PM PT
- Our preclinical program, ELI-008, is an investigational
multivalent lymph node–targeted AMP peptide vaccine developed to
target p53 hotspot mutations.
- AMP-immunization generated robust immune responses yielding
strong T cell activation against common p53 hot spot mutations
(R248W, R248Q, R175H, R273H, R273C, R282W, G245S, Y220C, C135Y,
R158H, H214R).
- Potent T cell
responses were observed after only two doses with AMP-p53 R248W,
which were further improved after a third bi-weekly dose. For
multiple p53 mutations, ELI-008 demonstrated a several-hundred-fold
increase over conventional comparator vaccines.
- Induced T cells were polyfunctional
exhibiting production of multiple effector cytokines (IFNγ, TNFα,
IL2, GM-CSF) and showed high cytotoxic potential by secreting large
quantities of Granzyme B and effectively killing target cells in
vivo.
- Substantial populations of
p53-specific T cells were found patrolling peripheral organs like
the lung, which is one of the predominant sites for the metastatic
spread of many cancers.
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
mKRAS-gene—a prevalent driver of many human cancers. ELI-002 is
comprised of two powerful components that are built with our AMP
platform consisting of AMP-modified mutant KRAS peptide antigens
and an AMP-modified CpG adjuvant that is available as an
off-the-shelf subcutaneous administration.
ELI-002 2P (2 peptide formulation) is currently being studied in
an ongoing 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 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 and potentially reducing the chance of bypass resistance
mechanisms.
About ELI-007 and ELI-008 Our preclinical
programs, ELI-007 and ELI-008, are being evaluated in studies
funded by the Gastro-Intestinal (“GI”) Research Foundation with the
aim of developing multivalent cancer vaccines targeting several
mutations.
ELI-007 is an investigational multivalent lymph node–targeted
AMP peptide vaccine comprised of the V600E and V600K mutant
antigens, which make up >95% of all BRAF-driven cancers in
humans, representing up to 1.5 million cancer incidences worldwide
each year. The BRAF gene is part of an intracellular signaling
pathway that drives cell growth and division. BRAF mutations can
lead to uncontrolled cell growth and ultimately cancer.
ELI-008 is an investigational multivalent lymph node–targeted
AMP peptide vaccine developed to target p53 hotspot mutations. p53
is a tumor-suppressing protein that controls the cell cycle, DNA
replication and cell division. Mutations in the p53 protein lead to
uncontrolled tumor progression and growth. Similar to KRAS, p53
mutations are present in a broad spectrum of cancer types,
accounting for >30% of solid tumors.
In preclinical models, ELI-007 and ELI-008 have shown strong T
cell activation and demonstrated strong induction of
tumor-antigen-specific T cell responses.
About Elicio Therapeutics Elicio
Therapeutics, Inc. (Nasdaq: ELTX) is a clinical-stage biotechnology
company advancing a pipeline of novel lymph node-targeted
immunotherapies for the treatment of some of the most aggressive
cancers. By combining expertise in immunology and immunotherapy,
Elicio is harnessing the natural power of the immune system with
Amphiphile (“AMP”) Technology which allows for therapeutic payloads
to be delivered directly to the lymph nodes, enhancing the immune
system’s cancer-fighting capabilities. By targeting cancer
immunotherapies to the core of the immune response, AMP aims to
optimize the lymph nodes’ natural ability to educate, activate and
amplify cancer-specific T cells, which are essential for
recognizing and eliminating tumor cells. Engineered to synchronize
immunity in these highly potent sites, AMP is built to enhance the
magnitude, potency, quality, and durability of the immune response
to drive antitumor activity. The Company’s R&D pipeline
includes off-the-shelf therapeutic cancer vaccines ELI-002,
(targeting mKRAS-driven cancers) as well as ELI-007 and ELI-008
(targeting BRAF-driven cancers and p53 hotspot mutations,
respectively). For more information, please visit
www.elicio.com.
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 (“PSLRA”). These include
statements regarding Elicio’s planned clinical programs, including
planned clinical trials, the potential of Elicio’s product
candidates, including the potential for the AMP strategy to improve
the potency of vaccine immunotherapy, the broad applicability of
Elicio’s technology and the potential therapeutic product
opportunities; the expected participation and presentation at
upcoming conferences, 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 plans to develop and commercialize its
product candidates, including ELI-002; the timing of the
availability of data from Elicio’s clinical trials, including
initial data from the AMPLIFY-7P Phase 1 study of ELI-002 7P
expected in the second quarter of 2024; Elicio’s plans to research,
develop and commercialize its current and future product
candidates; Elicio’s ability to successfully collaborate with
existing collaborators or enter into new collaborations, and to
fulfill its obligations under any such collaboration agreements;
and Elicio’s ability to advance ELI-002 outside of PDAC monotherapy
and Elicio’s pipeline programs.
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 that was filed with the SEC on March
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.
Media ContactKristin PolitiLifeSci
Communicationskpoliti@lifescicomms.com646-876-4783
Investor Relations ContactHeather
DiVecchiaElicio TherapeuticsIR@elicio.com857-209-0153
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