Adagene Inc. (“Adagene”) (Nasdaq: ADAG), a company transforming the
discovery and development of novel antibody-based therapies, today
announced data at the SITC 39th Annual Meeting, taking place in
Houston, Nov. 6 – 10, 2024. The two poster presentations provide
new insights on the increased therapeutic index (TI) for ADG126 and
reinforce its clinical safety and efficacy profiles in combination
with pembrolizumab* including in advanced Metastatic
Microsatellite-stable (MSS) Colorectal Cancer (CRC).
“CTLA-4 has an essential role in harnessing the immune system to
improve outcomes for patients with cold and PD-L1 low or negative
tumors, and CTLA-4 inhibition has been shown to prime T cells
contributing to enhanced combination therapy activity,” said Daneng
Li, MD, Associate Professor in the Department of Medical Oncology
& Therapeutics Research at the City of Hope Comprehensive
Cancer Center, and a study investigator. “With its increased
therapeutic index (TI), ADG126 has demonstrated in clinic that a
unique epitope and masking technology can be deployed to deplete
CTLA-4 mediated intratumoral T regulatory cells (Tregs), as
anti-PD-1 alone has a minimum effect.”
In the first poster, Deciphering Improved Clinical Therapeutic
Index (TI) of Muzastotug (ADG126), a Masked Anti-CTLA-4 SAFEbody®
over its Unmasked Form (ADG116) as Monotherapy or in Combination
with anti-PD-1 Therapy (toripalimab), data demonstrate how the
improved TI of ADG126 allows for higher and repeat dosing to
unleash its efficacy to the maximum potential, while maintaining an
improved safety profile. Analyses of the masked ADG126 SAFEbody and
its unmasked version, ADG116, show the improved TI relative to
commercially available anti-CTLA-4 therapies (e.g., ipilimumab) via
enhanced epitope-dependent ADCC and T cell priming. By targeting
the constitutively over-expressed CTLA-4 on T regulatory cells
(Tregs) in the tumor microenvironment (TME) for potent CTLA-4
mediated intratumoral Treg depletion, ADG126 achieves
tumor-specific targeting with minimal on-target off-tumor
toxicities.
Key highlights include:
- The unique epitope of ADG126 and its activated form (ADG116)
drives species cross-reactivity enabling the same antibody to be
used across mice, monkey and human studies, with a unified set of
physiologically relevant parameters for population pharmacokinetic
(PK) modeling. Analyses show a significantly higher and sustained
steady state tumor-specific engagement of CTLA-4 with the masked
ADG126, suggesting increased exposure in the TME and a stronger
ADCC effect.
- New analyses show the seamless translation of preclinical PK
analyses to clinical PK data, including:
- head-to-head comparison of ADG126 to ipilimumab in MC38 mice
(colon cancer model), a single dose of ADG126 showed a three-fold
increased active (e.g., cleaved) drug exposure in homogenized tumor
tissue samples at 10 mg/kg versus a single dose of ipilimumab at 1
mg/kg while maintaining similar plasma active drug exposures.
- A second analysis in the MC38 mice model showed two consecutive
doses of ADG126 at 20 mg/kg increased the tumor cleaved and total
PK versus a single dose, demonstrating continuous intratumoral
cleavage of intact ADG126 and accumulation within the TME. This
reflects the effectiveness of ADG126 repeat dosing to increase drug
exposure within the TME, supporting its mechanism with CTLA-4
mediated intratumoral Treg depletion.
The second poster, Phase 1b/2, Multicenter Dose Escalation and
Expansion Study of Muzastotug (ADG126, a Masked Anti-CTLA-4
SAFEbody®) in Combination with Pembrolizumab in Advanced/Metastatic
MSS CRCs, presents additional follow up data from an ongoing trial
showing the best-in-class therapeutic potential of ADG126 in
combination with anti-PD-1 therapy in patients with the most common
form of colorectal cancer, MSS CRC.
The trial, conducted in patients with advanced MSS CRC without
liver metastases, showed that ADG126 administered at 10 mg/kg Q6W
or Q3W in combination with pembrolizumab (200 mg/Q3W) demonstrated
an encouraging efficacy signal, durable disease control and an
early survival benefit in MSS CRC patients, with dose-dependent
efficacy and objective responses per RECIST criteria observed for
the Q3W schedule.
New findings in the poster at SITC 2024 include:
- In MSS CRC patients, a lower rate of key TRAEs (i.e., diarrhea,
colitis, etc.) with ADG126 at the 10 mg/kg dosing level in
combination with pembrolizumab relative to lower doses of 1-2 mg/kg
of an Fc engineered anti-CTLA-4 antibody in clinical development
when used in combination with anti-PD-1. Clinical PK, particularly
the monitoring of active species of ADG126 in peripheral blood,
supports long-term safety of the combination therapy.
- The rate of Grade 3 and higher TRAEs for ADG126 in combination
with pembrolizumab was also shown to be much lower than
historically reported with currently approved standard of care
combinations. In the combination cohort, there was no Grade 3 or
higher colitis, which is common with other anti-CTLA-4
therapies.
- A case study of one responder who received two prior lines of
therapy before receiving ADG126 in combination with pembrolizumab
showed an 80% decrease in target lesions (50 mm at baseline). This
confirmed partial response (PR) correlated with a 100% decrease in
carcinoembryonic antigen (CEA) levels versus baseline.
Individualized PK data also demonstrated the correlation of tumor
shrinkage and plasma exposure. After five cycles, the patient
experienced TRAEs, after which dosing was modified and treatment
resumed, showing durable clinical benefit for over 12 months. This
response is one of four PRs reported from the ongoing 10 mg/kg Q3W
combination cohort of MSS CRC patients without liver metastases
(n=24).
- Repeat doses of ADG126 10 mg/kg in combination with
pembrolizumab shows encouraging dose-dependent clinical efficacy
and well-tolerated safety in accordance with plasma cleaved ADG126
concentrations. These data support that ADG126 may be a potential
best-in-class anti-CTLA-4 and may be considered as a backbone
therapy.
Follow up continues for MSS CRC patients treated with ADG126 10
mg/kg doses in combination with pembrolizumab. In addition, Adagene
is evaluating a single dose of ADG126 at 20 mg/kg followed by a 10
mg/kg Q3W maintenance dose in combination with pembrolizumab in a
cohort of 12 enrolled patients with data expected in 2025.
Poster Presentation DetailsBoth posters can be
viewed during SITC on Saturday, November 9 at the George R. Brown
Convention Center (Level 1, Exhibit Halls AB). They will also be
available on the Publications page of the company’s
website here.
About AdageneAdagene Inc. (Nasdaq:
ADAG) is a platform-driven, clinical-stage biotechnology company
committed to transforming the discovery and development of novel
antibody-based cancer immunotherapies. Adagene combines
computational biology and artificial intelligence to design novel
antibodies that address globally unmet patient needs. The company
has forged strategic collaborations with reputable global partners
that leverage its SAFEbody® precision masking technology in
multiple approaches at the vanguard of science.
Powered by its proprietary Dynamic Precision
Library (DPL) platform, composed of NEObody™, SAFEbody, and
POWERbody™ technologies, Adagene’s highly differentiated pipeline
features novel immunotherapy programs. The company’s SAFEbody
technology is designed to address safety and tolerability
challenges associated with many antibody therapeutics by using
precision masking technology to shield the binding domain of the
biologic therapy. Through activation in the tumor microenvironment,
this allows for tumor-specific targeting of antibodies in tumor
microenvironment, while minimizing on-target off-tumor toxicity in
healthy tissues.
Adagene’s lead clinical program, ADG126 (muzastotug), is a
masked, anti-CTLA-4 SAFEbody that targets a unique epitope of
CTLA-4 in regulatory T cells (Tregs) in the tumor microenvironment.
ADG126 is currently in phase 1b/2 clinical studies in combination
with anti-PD-1 therapy, particularly focused on Metastatic
Microsatellite-stable (MSS) Colorectal Cancer (CRC). Validated by
ongoing clinical research, the SAFEbody platform can be applied to
a wide variety of antibody-based therapeutic modalities, including
Fc empowered antibodies, antibody-drug conjugates, and
bi/multispecific T-cell engagers.
For more information, please
visit: https://investor.adagene.com.Follow Adagene on WeChat, LinkedIn and Twitter.
SAFEbody® is a registered trademark in the United
States, China, Australia, Japan, Singapore, and
the European Union.
* KEYTRUDA® is a registered trademark of Merck Sharp & Dohme
LLC, a subsidiary of Merck & Co., Inc., Rahway, NJ, USA.
Safe Harbor StatementThis press release
contains forward-looking statements, including statements regarding
certain clinical results of ADG126, the potential implications of
clinical data for patients, and Adagene’s advancement of, and
anticipated preclinical activities, clinical development,
regulatory milestones, and commercialization of its product
candidates. Actual results may differ materially from those
indicated in the forward-looking statements as a result of various
important factors, including but not limited to Adagene’s ability
to demonstrate the safety and efficacy of its drug candidates; the
clinical results for its drug candidates, which may not support
further development or regulatory approval; the content and timing
of decisions made by the relevant regulatory authorities regarding
regulatory approval of Adagene’s drug candidates; Adagene’s ability
to achieve commercial success for its drug candidates, if approved;
Adagene’s ability to obtain and maintain protection of intellectual
property for its technology and drugs; Adagene’s reliance on third
parties to conduct drug development, manufacturing and other
services; Adagene’s limited operating history and Adagene’s ability
to obtain additional funding for operations and to complete the
development and commercialization of its drug candidates; Adagene’s
ability to enter into additional collaboration agreements beyond
its existing strategic partnerships or collaborations, and the
impact of the COVID-19 pandemic on Adagene’s clinical development,
commercial and other operations, as well as those risks more fully
discussed in the “Risk Factors” section in Adagene’s filings with
the U.S. Securities and Exchange Commission. All
forward-looking statements are based on information currently
available to Adagene, and Adagene undertakes no
obligation to publicly update or revise any forward-looking
statements, whether as a result of new information, future events
or otherwise, except as may be required by law.
Investor & Media Contact:Ami
KnoeflerAdagene650-739-9952ir@adagene.com
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