The study met its primary endpoint with a
significant gastrointestinal overall response rate at Day 28 of 62%
and demonstrates the unprecedented efficacy of MaaT013 as
third-line treatment of aGvHD with gastrointestinal involvement
(GI-aGvHD)
- High gastrointestinal overall response rate (GI-ORR) exceeding
the expected response rate of 38%. Complete response (CR), only,
was 38% and very good partial response (VGPR) was 20%.
- Frequent and strong all-organ responses (ORR), prevalently
consisting of complete response (CR) of 36% and very good partial
response (VGPR) of 18%, reflecting systemic effects beyond the
gastrointestinal tract.
- 54% probability of survival at 1 year driven by clinical
response, highlighting MaaT013’s potential to overcome the
short-term mortality of third-line GI-aGvHD.
- Company anticipates MAA submission in Europe in mid-2025,
earlier than initially planned.
Conference call and webcast to be held on
Thursday, January 9, 2025, at 4.00PM CET/ 7.00 AM PST/ 10.00AM EST/
7.00PM GST To register, please click here.
Regulatory News:
MaaT Pharma (EURONEXT: MAAT – the “Company”), a clinical-stage
biotechnology company and a leader in the development of Microbiome
Ecosystem TherapiesTM (MET) dedicated to enhancing survival for
patients with cancer through immune modulation, today announced
topline results from ARES, a pivotal, single-arm, open-label,
multicenter European Phase 3 study evaluating the efficacy and
safety of MaaT013 in acute Graft-versus-Host Disease patients with
gastrointestinal involvement (GI-aGvHD) in third-line treatment,
meaning refractory to steroids and refractory or intolerant to
ruxolitinib. Notably, the study met its primary endpoint, with a
significant gastrointestinal overall response rate (GI-ORR) at 28
Days of 62%, exceeding the expected 38% response rate. Responses
reviewed by an Independent Review Committee (IRC), exceed the
per-protocol prespecified threshold and confirm the unprecedented
clinical efficacy of MaaT013 for the treatment of third-line
GI-aGvHD.
“Gastrointestinal involvement in aGvHD is a devastating
condition, particularly for patients who do not respond to
ruxolitinib. These individuals face an urgent unmet medical need,
with alarmingly low survival rates and a critical lack of effective
treatment options,” stated Professor Mohamad Mohty, Professor of
Hematology and Head of the Hematology and Cellular Therapy
Department at Saint-Antoine Hospital and Sorbonne University. “The
results for MaaT013 in this Phase 3 trial represent a
groundbreaking advancement in third-line treatment for GI-aGvHD. By
directly targeting the gut-immune interface, this innovative
therapy has the potential to redefine disease management, bringing
new hope to patients and clinicians, alike.”
“We would like to thank all patients who participated in this
landmark study. These positive topline results strongly position
MaaT013 as a first-in-class therapeutic for GI-aGvHD, potentially
bringing a new option for patients in need of effective treatments
when both steroids and ruxolitinib have failed. ARES represents the
first-ever positive pivotal clinical study for an
immunosuppressant-sparing, microbiome-based approach, confirming
MaaT Pharma’s leadership in the field, validating the Company’s
therapeutic platform, supporting its programs, and broadens
potential applications in oncology, inflammation, and other
therapeutic areas,” said Gianfranco Pittari, MD PhD, Chief Medical
Officer, MaaT Pharma.
The therapeutic options for patients with GI-aGvHD refractory to
steroids and refractory or intolerant to ruxolitinib remain very
limited despite the poor prognosis for this condition, which has
1-year survival rates of just 15% (Abedin et al., 2021). MaaT013
has the potential to be the first approved third-line treatment
option and thereby transform the survival outcomes and redefine
long-term prospects for approximately 3,000 third-line GI-aGvHD
patients per year in the U.S., Canada and Europe.
Top-line Data Highlights:
- In the single-arm ARES study, 66 adult patients with GI-aGvHD
refractory to steroids and refractory or intolerant to ruxolitinib
were treated with MaaT013 as third-line treatment across 50
European sites (Austria, Belgium, France, Germany, Italy and
Spain).
- Patients’ characteristics:
- Gender: 47% females, 53% males.
- Median age: 55.5 years (24-76)
- At baseline, aGvHD grading (according to both IRC and
investigators’ assessments):
- Grade II: 9.1%
- Grade III: 57.6%
- Grade IV: 33.3%
- Steroid refractory: 86.4%
- Steroid dependent: 13.6%
- Ruxolitinib refractory: 100%
- Ruxolitinib intolerant: 0
- The study met its primary endpoint of GI-ORR at Day 28 of
treatment with MaaT013 (p <0.0001), as assessed by the
Independent Review Committee (IRC).
- Frequent, strong and durable response rates translating into
prolonged survival
- GI-ORR at Day 28 occurred in 41/66 patients (62%) and
prevalently consisted of complete response (CR) (25/66 patients,
38%) and very good partial response (VGPR) (13/66 patients,
20%).
- ORR in all evaluable organs occurred in 42/66 patients (64%)
patients and was similarly driven by high rates of CR (24/66
patients, 36%) and VGPR (12/66 patients, 18%).
- The 12-month probability of survival was 54% (median survival
not reached). The 12-month probability was significantly higher in
patients who responded at Day 28 than those who did not respond
(67% vs 28% respectively, p <0.0001), demonstrating MaaT013’s
significant survival benefit in refractory GI-aGvHD.
Enrolled patients will continue to be followed for secondary and
exploratory endpoints for the duration of the study. Results are
expected to be presented at future scientific conferences.
MaaT013’s safety has already been confirmed by the ARES Data
Safety Monitoring Board (DSMB) in October 2023 for the first 30
patients, showing it was well tolerated with no increased infection
risk or treatment-related fatal events (Full details here).
Pharmacovigilance and DSMB surveillance for the study remain
ongoing.
With robust data supporting efficacy and safety, MaaT Pharma is
pursuing the regulatory submission of MaaT013, in Europe, as a
treatment for GI-aGvHD in third-line, aiming for a Centralized
Marketing Authorization Application (MAA) submission to the
European Medicines Agency (EMA) in mid-2025, earlier than
previously expected. The centralized procedure enables a single
authorization across the EU (27 members), thus facilitating patient
access and market launch.
In line with its mission to offer new treatment options for high
unmet medical needs, MaaT Pharma will continue to ensure
availability of MaaT013 in Europe, for patients with aGvHD (and
other indications) as part of its Early Access Program (EAP), which
exceeded 100 requests for patients in 2024. The EAP will continue
during the regulatory evaluation phase and up to commercialization,
anticipated for end of 2026. The Early Access Program, has been
expanded to the United States in December 2024, will continue as
the Company advances readiness for the U.S. Phase 3 clinical trial,
which is expected to be launched in 2025, upon securing
financing.
Conference Call and Webcast Information
MaaT Pharma will host a conference call and a webcast tomorrow
on Thursday, January 9th, 2025, at 4.00PM CET/ 7.00AM PST/ 10.00AM
EST/ 7.00PM GST. Hervé Affagard, Chief Executive Officer and
co-founder, Gianfranco Pittari, MD, PhD, Chief Medical Officer,
Eric Soyer, Chief Financial Officer, Sian Crouzet, Chief of Staff,
will further discuss the impact of the ARES Phase 3 results and the
related perspectives for MaaT Pharma. To register, please click
here. Participants can also join the conference by phone by
dialling the following number: +33 1 78 42 94 76 and using the PIN
code 85 99 53.
---
About MaaT Pharma
MaaT Pharma is a leading, late-stage clinical company focused on
developing innovative gut microbiome-driven therapies to modulate
the immune system and enhance cancer patient survival. Supported by
a talented team committed to making a difference for patients
worldwide, the Company was founded in 2014 and is based in Lyon,
France. As a pioneer, MaaT Pharma is leading the way in bringing
the first microbiome-driven immunomodulator in oncology. Using its
proprietary pooling and co-cultivation technologies, MaaT Pharma
develops high diversity, standardized drug candidates, aiming at
extending life of cancer patients. MaaT Pharma has been listed on
Euronext Paris (ticker: MAAT) since 2021.
About MaaT013
MaaT Pharma’s Microbiome Ecosystem Therapies (MET) are designed
to leverage a full microbiome ecosystem to restore balance and
maximize clinical benefits for patients with severe,
treatment-induced dysbiosis in acute diseases. MaaT013 is a
full-ecosystem, off-the-shelf, standardized, pooled-donor, enema
Microbiome Ecosystem TherapyTM for acute, hospital use. It is
characterized by a consistently high diversity and richness of
microbial species and the presence of ButycoreTM (a group of
bacterial species known to produce anti-inflammatory metabolites).
MaaT013 aims to restore the symbiotic relationship between the
patient’s functional gut microbiome and their immune system to
correct the responsiveness and tolerance of immune functions and
thus reduce steroid-resistant, gastrointestinal (GI)-aGvHD. MaaT013
has been granted Orphan Drug Designation by the US Food and Drug
Administration (FDA) and the European Medicines Agency (EMA).
About acute Graft-versus-Host Disease
Acute Graft-versus-Host Disease occurs in patients within 100
days of undergoing a stem cell or bone marrow transplant, where the
transplanted cells initiate an immune response and attack the
transplant recipient’s organs, causing inflammation of the skin,
liver and/or gastro-intestinal tract and leading to significant
morbidity and mortality. GI involvement is associated with severe
complications such as profound diarrhea, abdominal pain, intestinal
bleeding, and death. These complications are often
life-threatening, with increased mortality risk, due to the
challenges of managing severe GI inflammation and the associated
risks of infection, malnutrition, and organ failure. The standard
first line therapy for treating aGvHD is the use of systemic
steroids. If patients do not respond to steroids, they are
considered Steroid Resistant (SR) and other agents can be
administered. Currently the only agent approved for treating SR
aGvHD after failure of steroid treatment is ruxolitinib, which is
currently approved for this indication in USA and has received
approval from the European Medical Agency’s Committee for Human
Medicinal Products (CHMP) on March 25, 2022.
Forward-looking Statements
All statements other than statements of historical fact included
in this press release about future events are subject to (i) change
without notice and (ii) factors beyond the Company’s control. These
statements may include, without limitation, any statements preceded
by, followed by, or including words such as “target,” “believe,”
“expect,” “aim”, “intend,” “may,” “anticipate,” “estimate,” “plan,”
“project,” “will,” “can have,” “likely,” “should,” “would,” “could”
and other words and terms of similar meaning or the negative
thereof. Forward-looking statements are subject to inherent risks
and uncertainties beyond the Company’s control that could cause the
Company’s actual results or performance to be materially different
from the expected results or performance expressed or implied by
such forward-looking statements.
View source
version on businesswire.com: https://www.businesswire.com/news/home/20250108967308/en/
MaaT Pharma – Investor Relations Guilhaume DEBROAS, Ph.D.
Head of Investor Relations +33 6 16 48 92 50 invest@maat-pharma.com
Rx Communications Group – U.S. Investor Relations
Michael Miller Managing Director +1-917-633-6086 mmiller@rxir.com
MaaT Pharma – Media Relations Pauline RICHAUD Senior PR
& Corporate Communications Manager +33 6 14 06 45 92
media@maat-pharma.com Catalytic Agency – U.S. Media
Relations Heather Shea Media relations for MaaT Pharma +1
617-286-2013 heather.shea@catalyticagency.com
Maat Pharma (EU:MAAT)
Historical Stock Chart
Von Dez 2024 bis Jan 2025
Maat Pharma (EU:MAAT)
Historical Stock Chart
Von Jan 2024 bis Jan 2025
