Data showed a 91% ORR with P-BCMA-ALLO1 in
an optimized lymphodepletion arm, including a 100%
ORR in BCMA-naïve patients, and an
86% ORR in those who had received
at least one prior BCMA- and/or GPRC5D-targeting treatment
modality
Differentiated P-BCMA-ALLO1 safety results
with no dose-limiting toxicities, low rates of CRS and ICANS all
Grade 2 or less and no graft vs. host disease or
Parkinsonism
P-BCMA-ALLO1 was recently granted Regenerative
Medicine Advanced Therapy (RMAT) designation from the FDA and is
being evaluated in a Phase 1/1b
clinical trial in patients with relapsed/refractory multiple
myeloma who have previously received three or more
prior lines of therapy
Company to host webcast and conference call
tomorrow at 1 p.m. ET / 10 a.m. PT with multiple myeloma experts to
review the Phase 1 IMS oral presentation data and provide business
updates
SAN
DIEGO, Sept. 27, 2024 /PRNewswire/
-- Poseida Therapeutics, Inc. (Nasdaq: PSTX), a clinical-stage
allogeneic cell therapy and genetic medicines company advancing
differentiated non-viral treatments for patients with cancer and
rare diseases, today announced new interim clinical data from its
ongoing Phase 1 trial of P-BCMA-ALLO1 in patients with
relapsed/refractory multiple myeloma (RRMM). Data1
demonstrated a 91% overall response rate (ORR) and compelling safety results in the 23
heavily pretreated patients in Arm C, an optimized lymphodepletion
arm. The new clinical data were presented today in an oral session
at the 21st International Myeloma Society (IMS) Annual Meeting in
Rio de Janeiro.
P-BCMA-ALLO1 is an investigational non-viral, stem cell memory T
cell (TSCM)-rich allogeneic CAR-T cell therapy in Phase
1/1b clinical development for the
treatment of patients with RRMM. The Company is developing this
investigational off-the-shelf allogeneic CAR-T cell therapy with
Roche as part of a broader collaboration focused on addressing
blood cancers with Poseida's TSCM-rich CAR-T
platform.
"The compelling and differentiated results from the optimized
lymphodepletion arms of the ongoing Phase 1 trial of P-BCMA-ALLO1
showed deep responses and a high response rate in patients with
heavily pre-treated relapsed or refractory multiple myeloma,
regardless of prior exposure to B-cell maturation antigen
(BCMA)-targeting therapy. The high overall response rate of 91% is
remarkable because most study participants in my center had rapidly
proliferative refractory disease, in contrast with those treated in
the pivotal clinical trials of FDA-approved autologous CAR-T
therapies. Such patients treated in the current trial of P-BCMA
ALLO1 would not have qualified for standard of care autologous CAR
T therapy," said Bhagirathbhai R. Dholaria, M.D., Associate
Professor of Medicine, Malignant Hematology & Stem Cell
Transplantation at Vanderbilt
University Medical Center in Nashville, Tenn., and trial investigator. "All
patients in the Phase 1 trial have been treated quickly once
enrolled, with no waiting for manufacturing, with no need for
apheresis or bridging therapy, demonstrating key advantages of
allogeneic CAR-T cell therapy."
"P-BCMA-ALLO1 is one of the most advanced allogeneic CAR-T in
clinical development for multiple myeloma, manufactured using
non-viral technology to produce a TSCM-rich therapy that
has shown a compelling emerging product profile," said Kristin Yarema, Ph.D., president and chief
executive officer of Poseida Therapeutics. "We are encouraged to
see such a high overall response rate in an arm of the Phase 1
trial with optimized lymphodepletion, along with standout safety
results across all arms, given that the study population was
heavily pretreated, high-risk, and in general had many features
that historically have led to a poor prognosis. We are excited to
build on these data as we advance P-BCMA-ALLO1 in the Phase
1b part of the trial, which is
currently enrolling patients."
New Interim Clinical Data from Phase 1 P-BCMA-ALLO1
Trial
The ongoing open-label, multicenter Phase
1/1b dose-escalation and expansion
trial in patients with RRMM is assessing the safety and maximum
tolerated dose of P-BCMA-ALLO1 (primary objective) and its
anti-myeloma activity (secondary objective). As of September 6, 2024, 72 unique patients were
enrolled as an intent-to-treat (ITT) population and were treated
across four study arms (S, A, B and C) that included different
P-BCMA-ALLO1 doses and lymphodepletion regimen combinations. Study
participants were required to have received three or more prior
lines of therapy, including a prior proteasome inhibitor,
immunomodulatory drug and anti-CD38 monoclonal antibody. The trial
enrolled a heavily pretreated patient population with 43% of
patients having received prior BCMA-and/or GPRC5D targeting
therapy. Most prior BCMA therapies included autologous CAR-T and/or
T-cell engagers (TCE). Additionally, 33% of study participants were
racial minorities, demonstrating Poseida's commitment to
underserved patient populations.
In the ITT population, 100% of patients enrolled as of the data
cutoff were infused with P-BCMA-ALLO1. No patients required
anti-myeloma bridging therapy or prophylaxis with steroids or
tocilizumab, and there was no invasive apheresis or manufacturing
wait time. The median time from enrollment to the start of study
treatment was one day.
The ORR across all four study
arms was 54%; 11% of patients achieved a complete response (CR) or
a stringent complete response (sCR), and 33% achieved a very good
partial response or higher (VGPR+). The median duration of response
(DoR) was 232 days for study Arms A and B – the cohorts with six or
more months of follow-up at the time of data cut-off. Expansion and
persistence of the CAR-T cells in patients after infusion has been
dependent upon the conditioning dose of cyclophosphamide.
P-BCMA-ALLO1 levels measured in the peripheral blood and were much
higher in patients in Arm C (cyclophosphamide 750
mg/m2/day) and Arm B (cyclophosphamide 1000
mg/m2/day) than in patients in Arm S (cyclophosphamide
300 mg/m2/day), and Arm A (cyclophosphamide 500
mg/m2/day). Arm C was identified as the optimized
lymphodepletion arm based on cellular kinetics, safety and
efficacy.
Data from Arm C of the Phase 1 P-BCMA-ALLO1
Trial
Results from 23 study participants in Arm C were
highlighted in the oral session at IMS. Patients received
cyclophosphamide 750 mg/m2/day and fludarabine 30
mg/m2/day and approximately 2x106 cells/kg
P-BCMA-ALLO1. Some patients were treated in an outpatient setting.
Arm C patient details include:
- Nearly half (48%) were age 65 or older
- All were heavily pretreated, with a median of six prior lines
of anti-myeloma therapy and a maximum of 14
- 62% of patients had received prior BCMA-targeting therapy
- 29% had failed both a BCMA CAR-T and a bispecific TCE, and 29%
had failed both a BCMA-targeting therapy and the GPRC5D-targeting
TCE, talquetamab
- Approximately two-thirds of patients (62%) had high-risk
disease by cytogenetics and 38% had extramedullary disease
Efficacy results, which are still evolving, for the 23 patients
in Arm C showed:
- An ORR of 91%, with a 100%
ORR in BCMA-naïve patients, an 86%
ORR in those who had received at
least one prior BCMA-targeting treatment (all had received prior
CAR-T and/or TCE), and an 86% ORR
in those who had received at least one prior BCMA-targeting
treatment and/or talquetamab
- 22% achieved a CR or an sCR
- 48% achieved VGPR+
- Median DoR could not be estimated at the time of data cut-off
because the current median follow-up is less than 3.5 months (for
pooled arms A and B, the median DoR was more than seven months
(estimated range of five-10 months), with a median time to response
of only 16 days)
P-BCMA-ALLO1 was well-tolerated with key safety results from Arm
C, including:
- No dose-limiting toxicities, Grade 3 or higher cytokine release
syndrome (CRS) or immune effector cell neurotoxicity syndrome
(ICANS). The incidence of Grade 1 or 2 CRS was 39% and the
incidence of Grade 1 or 2 ICANS was 13%
- The incidence of infections was 48%, including 30% that were
Grade 1 or 2 and 17% that were Grade 3
- Rapid cytopenia recovery in the vast majority of cases
- No graft-vs-host disease (GvHD), hemophagocytic
lymphohistiocytosis (HLH), Parkinsonism or cranial neuropathies
observed
- The safety results of P-BCMA-ALLO1 in arm C have been
consistent with those observed in the other three arms of the Phase
1 trial, with a total safety database, including 72 unique
patients
The ongoing P-BCMA-ALLO1 Phase 1/1b trial is enrolling patients using the Arm C
lymphodepletion regimen described above, across two dosing cohorts,
with dose optimization ongoing in Arm C.
Company-Hosted IMS Live Webcast and Conference Call
Information
Poseida will host a live webcast and conference
call tomorrow, Saturday, September 28,
2024, at 1 p.m. ET /
10 a.m. PT. The webcast will feature
an expert panel of clinicians who will discuss the new clinical
data and multiple myeloma treatment landscape. The panel will be
moderated by Dr. Rizvi and include Dr. Dholaria and Thomas G. Martin, M.D., Clinical Professor of
Medicine, Adult Leukemia and Bone Marrow Transplantation Program
and Associate Director of the Myeloma Program at the University of California, San Francisco (UCSF), and
Co-Leader of the Cancer Immunology & Immunotherapy Program at
the UCSF Helen Diller Family Comprehensive Cancer Center.
The conference call can be accessed by dialing 800-225-9448 or
203-518-9708 (International) with the conference ID PSTX0928. The
live webcast can be accessed using the link here, or by visiting
the Events and Presentations section of the Poseida website at
investors.poseida.com. After the live webcast, the event will
remain archived on the Poseida website for approximately 90
days.
About P-BCMA-ALLO1
P-BCMA-ALLO1 is an allogeneic CAR-T product candidate licensed to
Roche targeting B-cell maturation antigen (BCMA) for the treatment
of relapsed/refractory multiple myeloma. This allogeneic program
includes a VH-based binder that targets BCMA, and interim clinical
data presented at IMS in September
2024 support the Company's belief that T stem cell
(TSCM)-rich allogeneic CAR-Ts have the potential to
offer effective, safe and reliable treatment addressing unmet needs
in multiple myeloma. The U.S. Food and Drug Administration (FDA)
has granted P-BCMA-ALLO1 Orphan Drug designation for multiple
myeloma and Regenerative Medicine Advanced Therapy (RMAT)
designation for adult patients with relapsed/refractory multiple
myeloma after three or more prior lines of therapies including a
proteasome inhibitor, an immunomodulatory agent and an anti-CD38
antibody.
P-BCMA-ALLO1 is currently being evaluated in a Phase
1/1b trial in patients with multiple
myeloma. Additional information about the Phase 1/1b trial is available at
www.clinicaltrials.gov using identifier: NCT04960579.
About Poseida Therapeutics, Inc.
Poseida Therapeutics
is a clinical-stage biopharmaceutical company advancing
differentiated allogeneic cell therapies and genetic medicines with
the capacity to cure certain cancers and rare diseases. The
Company's pipeline includes investigational allogeneic CAR-T cell
therapies for both solid tumors and hematologic cancers as well as
investigational in vivo genetic medicines that address patient
populations with high unmet medical need. The Company's approach is
based on its proprietary genetic editing platforms, including its
non-viral piggyBac® DNA Delivery System, Cas-CLOVER™
Site-Specific Gene Editing System, Booster Molecule and
nanoparticle gene delivery technologies, as well as in-house GMP
cell therapy manufacturing. The Company has formed strategic
collaborations with Roche and Astellas to unlock the promise of
cell therapies for cancer patients. Learn more
at www.poseida.com and connect
with Poseida on X and LinkedIn.
Forward-Looking Statements
Statements contained
in this press release regarding matters that are not historical
facts are "forward-looking statements" within the meaning of the
Private Securities Litigation Reform Act of 1995. Such
forward-looking statements include statements regarding, among
other things, expected plans with respect to clinical trials; the
potential capabilities and benefits of the Company's technology
platforms and product candidates; the quotes from Drs. Dholaria and
Yarema; and the Company's plans and strategy with respect to
developing its technologies and product candidates. Because such
statements are subject to risks and uncertainties, actual results
may differ materially from those expressed or implied by such
forward-looking statements. These forward-looking statements are
based upon the Company's current expectations and involve
assumptions that may never materialize or may prove to be
incorrect. Actual results could differ materially from those
anticipated in such forward-looking statements as a result of
various risks and uncertainties, which include, without limitation,
the fact that interim data from the Company's clinical trials may
change as more patient data become available and remain subject to
audit and verification procedures that could result in material
differences from the final data; the Company's reliance on third
parties for various aspects of its business; risks and
uncertainties associated with development and regulatory approval
of novel product candidates in the biopharmaceutical industry; the
Company's ability to retain key scientific or management personnel;
the Company's ongoing and planned clinical trials; whether any of
the Company's product candidates will be shown to be effective,
safe and reliable; and the other risks and uncertainties described
in the Risk Factors section of Poseida's Quarterly Report on Form
10-Q filed with the Securities and Exchange Commission (SEC) on
August 5, 2024, and in other filings
Poseida makes with the SEC from time to time. All forward-looking
statements contained in this press release speak only as of the
date on which they were made. The Company undertakes no obligation
to update such statements to reflect events that occur or
circumstances that exist after the date on which they were made,
except as required by law.
1 Based on an efficacy cutoff date of September 6, 2024 and a safety cutoff date of
July 31, 2024
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SOURCE Poseida Therapeutics, Inc.