Full Press Release Details
Principal Investigator from City of Hope National
Medical Center Invited to Present Clinical Data from Marker Therapeutics APOLLO Study at 11th Global Summit on Hematologic
Preliminary data from study in patients with
lymphoma enrolled at City of Hope National Medical Center was presented at the 11th Global Summit on Hematologic Malignancies
in Whistler, BC, Canada
Study participants tolerated initial dose level
well and demonstrated durable objective responses after MT-601 treatment
Study participant with Non-Hodgkin's Lymphoma
who relapsed after anti-CD19 CAR T cell therapy remains in complete response nine months after MT-601 treatment
Houston, TX - April 8, 2024 -
Marker Therapeutics, Inc. (Nasdaq: MRKR), a clinical-stage immuno-oncology company focusing on developing next-generation T cell-based
immunotherapies for the treatment of hematological malignancies and solid tumor indications, today reported that Geoffrey Shouse, D.O.,
Ph.D., the Principal Investigator at City of Hope National Medical Center in Duarte, CA, was invited to present his clinical experience
from the APOLLO study at the 11th Global Summit on Hematologic Malignancies in Whistler, BC, Canada (April 2-7, 2024). Dr.
Shouse provided an overview on the clinical observations obtained at City of Hope on Saturday, April 6, 2024.
The Phase 1 APOLLO study is investigating MT-601,
a multi-tumor associated antigen (multiTAA)-specific T cell product, for the treatment of patients with lymphoma who have failed or are
ineligible to receive anti-CD19 chimeric antigen receptor (CAR) T cell therapy. Marker previously reported that the first study participant
tolerated the treatment well and achieved a complete response (CR) eight weeks after the second infusion of MT-601, which was maintained
at the six months follow-up visit (Press Release, September 11, 2023). During the presentation, Dr. Shouse showed that this study participant
remains in CR nine months following initial treatment with MT-601. This APOLLO participant had diffuse large B cell lymphoma (DLBCL) and
failed four prior lines of therapy, including anti-CD19 CAR T cell therapy. The participant relapsed within 90 days of CAR T cell therapy
yet maintained a CR for at least nine months after treatment with MT-601, suggesting that response to MT-601 was more durable compared
to CAR T cells in this study participant.
Dr. Shouse's presentation included data
from two additional study participants that have been treated at City of Hope. One of the study participants had transformed follicular
NHL and failed a total of 12 lines of therapy including mosunetuzumab (bispecific antibody) for follicular NHL, and Yescarta (anti-CD19
CAR T cell therapy) after transformation into DLBCL. At the time of MT-601 administration, only follicular NHL persisted after the last
treatment. Eight weeks after initial infusion with MT-601, this study participant achieved a CR and remains in CR three months following
treatment with MT-601. The third patient treated at City of Hope as part of the APOLLO trial presented with DLBCL with cutaneous involvement
only and was not eligible for CAR T cell therapy. When evaluated at eight weeks post-treatment, the study participant was in partial response
with all lesions decreasing in size including one that has completely resolved.
Dr. Shouse also reported that treatment was well
tolerated among all patients with no significant treatment-related adverse events including no reports of cytokine release syndrome (CRS)
or immune-effector cell associated neurotoxicity syndrome (ICANS), and that all patients will continue to be monitored closely for long-term
treatment effects and durability of response.
"We are encouraged by these clinical results
and the potential impact of MT-601 in patients with lymphoma who have relapsed or are ineligible for CAR T cell therapy," said Geoffrey
Shouse, D.O., Ph.D., the Principal Investigator at City of Hope National Medical Center in Duarte, CA. "Observing objective responses
in three out of three patients with lymphoma treated with MT-601 at our site is a remarkable and gratifying achievement and we are encouraged
by the benefits this therapy has provided to our patients. I am honored to have been invited to showcase these data on MT-601 to leading
experts in the field at the 11th Global Summit on Hematologic Malignancies."
The therapeutic potential of MT-601 is further
reinforced by non-clinical data demonstrating that MT-601 is able to eradicate lymphoma cells resistant to anti-CD19 CAR T cells (Press
Release, May 31, 2023).
CAR T cell therapy is associated with severe adverse
events such as cytokine release syndrome or neurotoxicity, as well as the potential risk of inducing secondary cancers (U.S. Food and
Drug Administration, November 28, 2023). MultiTAA-specific T cell therapies have been well-tolerated in clinical trials to date. Marker
believes that multiTAA-specific T cells represent a safe alternative to CAR T cells due to their non-genetically engineered approach that
selectively expands tumor-specific T cells from a patient's/donor's blood without the risk of mutagenesis.
"Although treatment with CD19-targeting
CAR T cells is rapidly expanding among hematological malignancies, 40-60% of patients relapse within one year of therapy," commented
Juan Vera, M.D., President and Chief Executive Officer of Marker Therapeutics. "The sustained CR for nine months in our first study
participant, who relapsed 90 days following CAR T cell treatment, indicates durable efficacy of MT-601 versus CAR T cell therapy in this
"Though the number of patients treated to
date in our APOLLO study is quite small, observing objective responses in all three study participants treated at City of Hope is encouraging,
and highlights the potential benefit of MT-601 in patients with lymphoma. We are continuing to enroll additional patients to hopefully
reinforce these promising observations and look forward to treating more participants in this Phase 1 study," concluded Dr. Vera.
MT-601 utilizes a novel non-genetically modified
approach that specifically targets six different tumor antigens upregulated in lymphoma cells (Survivin, PRAME, WT-1, NY-ESO-1, SSX-2,
MAGEA-4). Marker is currently investigating MT-601 in the Company-sponsored Phase 1 APOLLO trial (clinicaltrials.gov identifier: NCT05798897)
for the treatment of lymphoma patients who are relapsed/refractory after or ineligible to anti-CD19 CAR T cell therapies.
The APOLLO trial (clinicaltrials.gov Identifier:
NCT05798897) is a Phase 1, multicenter, open-label study designed to evaluate the safety and efficacy of MT-601 in participants with relapsed
or refractory lymphoma who either failed anti-CD19 chimeric antigen receptor (CAR) T cell therapy or are ineligible for anti-CD19 CAR
T cell therapy. The primary objective of this exploratory Phase 1 clinical trial is to evaluate the optimum dose, safety, and preliminary
efficacy of MT-601 in participants with various lymphoma subtypes. Under the APOLLO trial, it is anticipated that nine clinical sites
across the United States will cumulatively enroll up to approximately 30 participants during the dose escalation phase.
About multiTAA-specific T cells
The multi-tumor associated antigen (multiTAA)-specific
T cell platform is a novel, non-genetically modified cell therapy approach that selectively expands tumor-specific T cells from a patient's/donor's
blood capable of recognizing a broad range of tumor antigens. Since multiTAA-specific T cells are not genetically engineered, Marker believes
that its product candidates will be easier and less expensive to manufacture, with reduced toxicities, compared to current engineered
CAR-T and TCR-based approaches, and may provide patients with meaningful clinical benefits. As a result, Marker believes that its portfolio
of T cell therapies has a compelling product profile, as compared to current gene-modified CAR-T and TCR-based therapies.
About Marker Therapeutics, Inc.
Marker Therapeutics, Inc. is a Houston, TX-based
clinical-stage immuno-oncology company specializing in the development of next-generation T cell-based immunotherapies for the treatment
of hematological malignancies and solid tumors. Clinical trials that enrolled more than 200 patients across various hematological and
solid tumor indications showed that the Company's autologous and allogeneic multiTAA-specific T cell products were well tolerated
and demonstrated durable clinical responses. Marker's goal is to introduce novel T cell therapies to the market and improve patient
outcomes. To achieve these objectives, the Company prioritizes the preservation of financial resources and focuses on operational excellence.
Marker's unique T cell platform is strengthened by non-dilutive funding from U.S. state and federal agencies supporting cancer research.
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Statements in this news release concerning the Company's expectations, plans, business outlook or future performance, and any other
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our non-engineered multi-tumor antigen specific T cell therapies; the effectiveness of these programs or the possible range of application
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