Biomea Fusion, Inc. (“Biomea” or “Biomea Fusion” or “the Company”)
(Nasdaq: BMEA), a clinical-stage biopharmaceutical company
dedicated to discovering and developing oral covalent small
molecules to improve the lives of patients with diabetes, obesity,
and genetically defined cancers, today announced its presentations
at the 1st Annual Asian Conference on Innovative Therapies for
Diabetes Management (ATTD-ASIA 2024) taking place in Singapore,
18-20 November 2024.
Biomea will showcase the following three oral presentations and
participate in one industry symposium:
- Trial in Progress COVALENT-111: A Phase 2 Trial of the Oral
Menin Inhibitor Icovamenib (BMF-219) in Patients with Type 2
Diabetes Oral Presentation: November 19 at 12:45 – 12:50 SGT
- Late-Breaker: Assessment of Icovamenib (BMF-219) in Persons
with Poorly Controlled Severe Insulin-Deficient (SIDD) Type 2
Diabetes (T2D): COVALENT-111 Case Studies Oral Presentation:
November 19 at 12:50 – 12:55 SGT
- Unlocking the Potential of Menin Inhibition: Icovamenib and a
Look into the Future of Diabetes ManagementIndustry Symposium:
November 19 at 17:10 – 18:10 SGT
- Trial in Progress COVALENT-112: A Phase 2 Trial of the Oral
Menin Inhibitor Icovamenib (BMF-219) in Type 1 Diabetes Oral
Presentation: November 20 at 11:25 - 11:35 SGT
All presentations will be available for viewing through the
conference virtual platform; they will also be available on
Biomea’s website under:
https://investors.biomeafusion.com/news-events/events.
Data Highlights for Presentations at ATTD-Asia
2024T2D is characterized by a progressive decline in
beta-cell function while type 1 diabetes (T1D) is characterized by
autoimmune destruction of beta cells leading to hyperglycemia.
Preclinical data suggests investigational icovamenib may induce
beta-cell proliferation and improve insulin secretion. In the
multiple ascending dose portion of the Phase II COVALENT-111 trial,
many T2D participants achieved clinically significant improvements
in glycemic control up to 22 weeks after only 4 weeks of daily
icovamenib. At ATTD-Asia the company will report the Phase II
expansion design of COVALENT-111 (NCT05731544) evaluating
icovamenib in adults with T2D and the Phase II design of
COVALENT-112 (NCT06152042) evaluating icovamenib's efficacy and
safety in adults with T1D.
T2D is a heterogenous disease, characterized by varying degrees
of insulin resistance and insulin deficiency. Covalently inhibiting
menin is a new proposed mechanism of action particularly relevant
for diabetes patients with a depleted pool of beta cells. The
severe insulin-deficient diabetes (SIDD) and mild age-related
diabetes (MARD) subgroups, two of five identified by Ahlqvist et
al., encompass approximately 50%-70% of patients with T2D1,
depending on the population, and are distinguished by significant
insulin deficiency.
The company will present a review of insulin-deficient versus
insulin-resistant patients based on T2D participants in the
escalation portion of COVALENT-111, representative of exposure
expected in the expansion portion. Here, after only 4 weeks of
dosing and with a follow up 22 weeks after the last dose, the
insulin-deficient diabetes patients (SIDD and MARD subgroups),
showed a mean 1.23% placebo adjusted decline in HbA1c while the
patients characterized by insulin resistance (severe
insulin-resistant diabetes and mild obesity-related diabetes
subgroups) demonstrated a mean 0.48% placebo adjusted decline.
Subtyping diabetes patients may help identify specific subgroups
for improved targeted treatment approaches in the future.
Two case studies from the escalation portion of COVALENT-111 are
also being presented to highlight the potential of icovamenib in
patients with poorly controlled insulin-deficient T2D. One of the
patients, a 29-year-old man with a four-year history of T2D,
experienced a 2.5% reduction in HbA1c (from 9.5% at baseline to
7.0%) at Week 26, dropping an additional 1.2% at Week 47 (down to
5.8%) leading to the discontinuation of metformin. Both HOMA-B
(+190.0%) and C-peptide (+71.0%) increased significantly during the
26-week study period. The other insulin deficient patient, a
45-year-old man with a 10-year history of T2D, had a 1.1% reduction
in HbA1c from baseline (8.6% to 7.5%) at Week 26 with increases in
HOMA B (+1233.0%) and C-peptide (+59.0%). In both cases icovamenib
was generally well tolerated, there were no adverse events, no dose
discontinuations or modifications reported, and no symptomatic or
clinically significant hypoglycemia was observed.
In addition, the company is hosting an industry symposium
entitled “Unlocking the Potential of Menin Inhibition: Icovamenib
and a Look into the Future of Diabetes Management,” chaired by
Professor Juliana Chan and Dr. Juan Pablo Frías, to discuss
beta-cell biology and introduce the novel therapeutic approach for
diabetes through menin inhibition. Key topics discussed include the
fundamentals of beta-cell biology and its critical role in glucose
homeostasis; the pivotal role of menin in pancreatic beta-cell
function and diabetes pathogenesis, and an overview of the
COVALENT-111 (T2D) and COVALENT-112 (T1D) clinical studies. A focal
point of the symposium will be an in-depth presentation on T2D
subgroups, highlighting their distinct characteristics and
phenotypes to enhance the understanding of T2D heterogeneity and
its implications for personalized treatment strategies.
Upcoming COVALENT-111 Study Read-Out The Phase
IIb expansion portion of COVALENT-111 is designed to further
explore icovamenib’s potential for long-term glycemic control,
dosing patients for up to 12 weeks at various dosing levels with
follow-up at Week 26 and 52. The study aims to identify the optimal
dose for late-stage development and define biomarkers for patients
who respond best to icovamenib alone. Key inclusion criteria are
persons with T2D with a HbA1c greater than 7.0%, a BMI of 25 to 40,
who have had diabetes onset within the last seven years and were
failing their current treatments, which could include up to three
anti-diabetic medications, including GLP-1 based therapies. We
believe the study is designed to help understand the impact of
dosing the broader patient population and determine icovamenib’s
potential impact on insulin-deficient and insulin-resistant
patients. The goal is to select the optimal dose, dose duration,
and patient set to advance to late-stage clinical development.
Inhibiting menin in patients with diabetes is a novel and
investigative treatment modality, and the study will help define a
study population to discuss with the Food and Drug Administration
during a potential end of Phase II meeting in 2025.
"We’re pleased to present our case studies at ATTD-Asia and show
the overall benefit we believe icovamenib may provide, particularly
to insulin-deficient patients with T2D. We expect the upcoming
topline results in December will provide critical insights into how
icovamenib affects both insulin-deficient and insulin-resistant
patients and help us identify the biomarkers for optimal patient
selection. I am very excited about icovamenib’s potential and look
forward to reporting our study results," stated Juan Pablo Frias,
MD, Biomea Fusion’s Chief Medical Officer.
About COVALENT-111COVALENT-111 is a multi-site,
randomized, double-blind, placebo-controlled Phase I/II study. In
the completed Phase I portion of the trial, healthy patients were
enrolled in single ascending dose cohorts to evaluate safety at the
prospective dosing levels for T2D patients. Phase II consists of
multiple ascending dose cohorts and includes adult patients with
T2D uncontrolled by standard of care medicines. Once the escalation
portion of COVALENT-111 was completed, the study advanced into an
expansion portion consisting of multiple cohorts dosing T2D
patients up to 12 weeks with either icovamenib or placebo, followed
by a 40-week off treatment period. To date, approximately 200
patients completed their respective dosing. Additional information
about this Phase I/II clinical trial of icovamenib in T2D can be
found at ClinicalTrials.gov using the identifier NCT05731544.
About COVALENT-112COVALENT-112 is a multi-site,
randomized, double-blind, placebo-controlled Phase II study in
adults with stage three T1D. This stage describes the period
following clinical diagnosis of T1D when symptoms are present due
to significant beta cell loss. COVALENT-112 includes an open-label
portion for adults with T1D up to 15 years since diagnosis. The
open-label portion (n=40) examines the efficacy, safety, and
durability of icovamenib at two oral dose levels, 100 mg and 200 mg
over a 12-week treatment period followed by a 40-week off treatment
period. To date, approximately 20 patients completed 8 weeks of
dosing in the open label portion. Additional information about the
Phase II clinical trial of icovamenib in T1D can be found at
ClinicalTrials.gov using the identifier NCT06152042.
About Biomea FusionBiomea Fusion is a
clinical-stage biopharmaceutical company focused on the discovery
and development of oral covalent small molecules to improve the
lives of patients with diabetes, obesity, and genetically defined
cancers. A covalent small molecule is a synthetic compound that
forms a permanent bond to its target protein and offers a number of
potential advantages over conventional non-covalent drugs,
including greater target selectivity, lower drug exposure, and the
ability to drive a deeper, more durable response.
We are utilizing our proprietary FUSION™ System to discover,
design and develop a pipeline of next-generation covalent-binding
small-molecule medicines designed to maximize clinical benefit for
patients. We aim to have an outsized impact on the treatment of
disease for the patients we serve. We aim to cure.
Visit us at biomeafusion.com and follow us
on LinkedIn, X and Facebook.
Forward-Looking StatementsStatements we make in
this press release may include statements which are not historical
facts and are considered forward-looking statements within the
meaning of Section 27A of the Securities Act of 1933, as amended
(the “Securities Act”), and Section 21E of the Securities Exchange
Act of 1934, as amended (the “Exchange Act”). These statements may
be identified by words such as “aims,” “anticipates,” “believes,”
“could,” “estimates,” “expects,” “forecasts,” “goal,” “intends,”
“may,” “plans,” “possible,” “potential,” “seeks,” “will,” and
variations of these words or similar expressions that are intended
to identify forward-looking statements. Any such statements in this
press release that are not statements of historical fact, including
statements regarding the clinical and therapeutic potential of our
product candidates and development programs, and their potential
relative to approved products marketed by third parties; the
potential benefits to future trial design and program development
of subtyping diabetes patients; our research, development and
regulatory plans, the progress of our ongoing and upcoming clinical
trials; the anticipated availability of data from our clinical
trials, anticipated milestones, and the timing of such events may
be deemed to be forward-looking statements. We intend these
forward-looking statements to be covered by the safe harbor
provisions for forward-looking statements contained in Section 27A
of the Securities Act and Section 21E of the Exchange Act and are
making this statement for purposes of complying with those safe
harbor provisions. Any forward-looking statements in this press
release are based on our current expectations, estimates and
projections only as of the date of this release and are subject to
a number of risks and uncertainties that could cause actual results
to differ materially and adversely from those set forth in or
implied by such forward-looking statements, including the risk that
preliminary or interim results of preclinical studies or clinical
trials may not be predictive of future or final results in
connection with future clinical trials and the risk that we may
encounter delays in preclinical or clinical development, patient
enrollment and in the initiation, conduct and completion of our
ongoing and planned clinical trials and other research and
development activities. These risks concerning Biomea Fusion’s
business and operations are described in additional detail in its
periodic filings with the U.S. Securities and Exchange Commission
(SEC), including its most recent periodic report filed with the SEC
and subsequent filings thereafter. Biomea Fusion explicitly
disclaims any obligation to update any forward-looking statements
except to the extent required by law.
Contact: Ramses Erdtmann COO
& President of Biomea Fusionre@biomeafusion.com
References: 1Ahlqvist E, et al. Lancet Diabetes
Endocrinol. 2018;6:361-369
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