C4 Therapeutics, Inc. (C4T) (Nasdaq: CCCC), a clinical-stage
biopharmaceutical company dedicated to advancing targeted protein
degradation science, today presented clinical data from the ongoing
Phase 1 trial of cemsidomide, an orally bioavailable small molecule
degrader of IKZF1/3, at the ASH Annual Meeting. Presentations
included a poster highlighting results for cemsidomide in
combination with dexamethasone in multiple myeloma, and an oral
presentation delivering initial results for cemsidomide as a
monotherapy for non-Hodgkin’s lymphoma. These presentations
reinforce the potential of cemsidomide to become a backbone therapy
of choice in both multiple myeloma and non-Hodgkin’s lymphoma where
IKZF1/3 degradation is warranted.
C4T designed cemsidomide to be a more potent and selective
degrader of IKZF1/3 with unique pharmacokinetic properties, with
the goal to improve the therapeutic index to treat multiple myeloma
and non-Hodgkin’s lymphoma—both alone and in combination with other
therapeutic agents in these therapeutic areas.
“Cemsidomide continues to deliver clinical data demonstrating
its potential to be used in both multi-refractory patients and as
part of combination therapies across all lines of treatment for a
significant number of patients with multiple myeloma or
non-Hodgkin’s lymphoma,” said Len Reyno, M.D., chief medical
officer of C4 Therapeutics. “We look forward to leveraging today’s
data to inform clinical development strategies in both multiple
myeloma and non-Hodgkin’s lymphoma that has the potential to unlock
the value of cemsidomide for patients in need of innovative
therapies across treatment lines.”
Multiple Myeloma (MM)At the ASH Annual Meeting,
C4T presented safety and anti-myeloma data demonstrating
cemsidomide has the potential to become a best-in-class IKZF1/3
degrader used as a backbone therapy of choice for patients with
multiple myeloma where IKZF1/3 degradation is warranted. These data
support the future development of cemsidomide across treatment
lines in combination with other anti-myeloma agents.
As of the data cutoff date of October 11, 2024, a total of 47
patients received cemsidomide in combination with dexamethasone
across four dose levels (50 µg dosed Monday, Wednesday, Friday
(MWF); 37.5 µg dosed once daily (QD); 62.5 µg QD; 75 µg QD).
Patients were heavily pretreated, receiving a median of six prior
therapies. All patients (100 percent) were triple-class exposed,
defined as exposure to one or more immunomodulatory agents, one or
more proteasome inhibitors, and one anti-CD38 antibody.
Thirty-three patients (70 percent) received prior BCMA directed
therapy. Thirty-one patients (66 percent) received prior CAR-T or
T-cell engager therapy.
Safety: Cemsidomide in combination with dexamethasone was well
tolerated.
- As of the data cutoff date, 47 patients were evaluable for
safety.
- The most common adverse events (AEs) Grade 3 or above were
neutropenia (n=18), anemia (n=10) and infections (n=8). No patients
discontinued therapy due to neutropenia.
- No patients experienced a treatment emergent adverse event that
led to dose reduction.
- The maximum tolerated dose has not yet been identified.
Enrollment is currently ongoing at the 100 µg QD dose level.
Anti-myeloma activity: Cemsidomide in combination with
dexamethasone demonstrated anti-myeloma activity across a broad
range of doses, highlighting a wide therapeutic range.
- As of the data cutoff, 42 patients were evaluable for
anti-myeloma activity.
- Across all dose levels, cemsidomide in combination with
dexamethasone achieved a 26 percent ORR and a 40 percent clinical
benefit rate (CBR).
- At the highest dose level explored to date (75 µg QD),
cemsidomide achieved a 36 percent ORR and a 45 percent CBR.
- At the two highest dose levels evaluated to date (62.5 µg QD
and 75 µg QD), 62 percent of patients remained on therapy as of the
data cutoff date.
Binod Dhakal, M.D., M.S., associate professor of medicine,
Medical College of Wisconsin, Division of Hematology, presented a
poster highlighting the MM results. He commented: “The data
presented at the ASH Annual Meeting demonstrate cemsidomide in
combination with dexamethasone is active and well-tolerated over a
range of doses in a heavily pretreated, relapsed/refractory
multiple myeloma patient population—including a majority of
patients who have received T-cell directed therapies who are
challenging to treat. I look forward to cemsidomide’s continued
development as a potential new treatment option for patients in the
evolving myeloma landscape.”
C4T has identified 75 µg QD as a target dose for various
dexamethasone combination regimens; as dose escalation continues,
higher doses may also be considered. For immune-based combination
strategies, C4T believes doses lower than 75 µg QD will be optimal
based on anti-myeloma activity and immune activation observed in
the previously disclosed monotherapy data set.
C4T has identified the following next steps in cemsidomide MM
development:
- Complete Phase 1 dose escalation trial in MM to establish go
forward doses
- Initiate initial combination trials
- Engage regulatory authorities on registrational path
Non-Hodgkin’s Lymphoma (NHL)At the ASH Annual
Meeting, C4T also presented safety and anti-lymphoma data that
reinforce C4T’s belief that IKZF1/3 degradation remains relevant in
lymphoma. Based on the emerging anti-lymphoma signal demonstrated
in patients with PTCL, C4T believes cemsidomide could be further
developed in areas of high unmet need.
As of the data cutoff date of October 11, 2024, a total of 23
patients received cemsidomide monotherapy across five dose levels
(25 µg MWF; 50 µg MWF QD; 37.5 µg QD; 62.5 µg QD; 100 µg QD).
Patients were heavily pretreated, receiving a median of three prior
therapies. Seventeen patients had refractory progressive PTCL and
six patients had refractory progressive B-cell lymphoma.
Safety: Cemsidomide monotherapy was well tolerated and
additional dose finding is ongoing.
- As of the data cutoff, 23 patients were evaluable for
safety.
- The most common AEs Grade 3 or above were neutropenia (n=11),
infections (n=6), febrile neutropenia (n=4) and anemia (n=4). No
patients discontinued therapy due to neutropenia.
- At this time, the maximum tolerated dose has not been defined.
Two dose-limiting toxicities occurred at the 100 µg QD dose level.
As a result, a 75 µg QD cohort was opened to refine the
understanding of dose and safety in the NHL population; this cohort
is currently enrolling patients. Escalation above 75 µg QD may be
explored pending the outcome of the cohort.
Anti-lymphoma activity: Cemsidomide monotherapy demonstrated
anti-lymphoma activity across a broad range of doses.
- As of the data cutoff, 21 patients were evaluable for efficacy,
16 of which had PTCL.
- Cemsidomide displays a differentiated pharmacokinetic profile
with an approximate two-day half-life and an ability to induce
rapid and potent degradation of IKZF1/3.
- Across all dose levels explored, cemsidomide achieved a 38
percent ORR and 19 percent CMR rate.
- In patients with PTCL, cemsidomide achieved a 44 percent ORR
and 25 percent CMR rate.
Steve Horwitz, M.D., lymphoma specialist and cellular therapist,
Memorial Sloan Kettering Cancer Center, delivered an oral
presentation highlighting the NHL results at the ASH Annual
Meeting. He commented: “I am pleased to share the first clinical
data on monotherapy cemsidomide in non-Hodgkin’s lymphoma, which
demonstrated its well-tolerated safety profile and compelling
anti-lymphoma activity. These initial data are encouraging,
particularly in PTCL where relapsed/refractory patients lack
effective targeted therapies. We believe these Phase 1 monotherapy
data demonstrate that cemsidomide is well suited for further
development in earlier lines of treatment and in combination with
other anti-lymphoma agents.”
C4T has identified the following next steps in cemsidomide NHL
development:
- Complete Phase 1 dose escalation trial and identify go forward
dose
- Initiate expansion cohort for PTCL
- Engage regulatory authorities on registrational path
C4T Webcast for Analysts and InvestorsC4T will
host an investor webcast today December 8, 2024, at 5 pm EST. To
join the webcast, please visit this link or the “Events
& Presentations” page of the Investors section on the company’s
website at www.c4therapeutics.com. A replay of the webcast
will be archived and available following the event.
About CemsidomideCemsidomide is an
investigational, orally bioavailable small-molecule degrader
designed to be a more potent and selective degrader of IKZF1/3,
transcription factors that drive multiple myeloma (MM) and
non-Hodgkin’s lymphomas (NHL), with unique pharmacokinetic
properties. Clinical data has shown that cemsidomide is
well-tolerated. In MM, cemsidomide displays evidence of
anti-myeloma activity and immunomodulatory effects. In NHL,
cemsidomide displays evidence of anti-lymphoma activity. More
information may be accessed
at www.clinicaltrials.gov (identifier: NCT04756726).
About IKZF1/3IKZF1 (Ikaros) and IKZF3 (Aiolos)
are transcription factors that directly regulate the activity of
IRF4, a transcription factor that regulates downstream immune cell
differentiation. Aberrant IRF4 is associated with both lymphoma and
multiple myeloma proliferative T, B and plasma cell populations.
Down regulation of IRF4 promotes the death of both myeloma and
lymphoma cells.
About Multiple MyelomaMultiple myeloma (MM) is
a rare blood cancer affecting plasma cells. Approximately 36,000
people in the United States are diagnosed with MM each year.
Despite advances in treatment, multiple myeloma remains incurable.
Treatment combinations include IKZF1/3 degraders, which are
established backbone therapies, across lines of therapy.
About non-Hodgkin’s LymphomaNon-Hodgkin’s
lymphoma (NHL) is one of the most common cancers in the United
States. NHL forms in cells of the immune system called lymphocytes.
In the United States, approximately 80,000 people are diagnosed
with NHL each year. IKZF1/3 degraders are used across NHL
subtypes.
About C4 TherapeuticsC4 Therapeutics (C4T)
(Nasdaq: CCCC) is a clinical-stage biopharmaceutical company
dedicated to delivering on the promise of targeted protein
degradation science to create a new generation of medicines that
transforms patients’ lives. C4T is progressing targeted oncology
programs through clinical studies and leveraging its
TORPEDO® platform to efficiently design and optimize
small-molecule medicines to address difficult-to-treat diseases.
C4T’s degrader medicines are designed to harness the body’s natural
protein recycling system to rapidly degrade disease-causing
proteins, offering the potential to overcome drug resistance, drug
undruggable targets and improve patient outcomes. For more
information, please visit www.c4therapeutics.com.
Forward Looking StatementsThis press release
contains “forward-looking statements” of C4 Therapeutics, Inc.
within the meaning of the Private Securities Litigation Reform Act
of 1995. These forward-looking statements may include, but may not
be limited to, express or implied statements regarding our ability
to develop potential therapies for patients; the design and
potential efficacy of our therapeutic approaches; the predictive
capability of our TORPEDO® platform in the development of novel,
selective, orally bioavailable BiDAC™ and MonoDAC™ degraders; the
potential timing, design and advancement of our preclinical studies
and clinical trials, including the potential timing for and receipt
of regulatory authorization related to clinical trials and other
clinical development activities including clinical trial
commencement or cohort initiation; our ability and the potential to
successfully manufacture and supply our product candidates for
clinical trials; our ability to replicate results achieved in our
preclinical studies or clinical trials in any future studies or
trials; our ability to replicate interim or early-stage results
from our clinical trials in the results obtained when those
clinical trials are completed or when those therapies complete
later-stage clinical trials; regulatory developments in the United
States and foreign countries; the potential timing for updates on
our clinical and research programs; and our ability to fund our
future operations. Any forward-looking statements in this press
release are based on management’s current expectations and beliefs
of future events 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. These risks and uncertainties include,
but are not limited to: uncertainties related to the initiation,
timing, advancement and conduct of preclinical and clinical studies
and other development requirements for our product candidates; the
risk that any one or more of our product candidates will cost more
to develop or may not be successfully developed and commercialized;
and the risk that the results of preclinical studies and/or
clinical trials will or will not be predictive of results in
connection with future studies or trials. For a discussion of these
and other risks and uncertainties, and other important factors, any
of which could cause our actual results to differ from those
contained in the forward-looking statements, see the section
entitled “Risk Factors” in C4 Therapeutics’ most recent Annual
Report on Form 10-K and/or Quarterly Report on Form 10-Q, as filed
with the Securities and Exchange Commission. All information in
this press release is as of the date of the release and C4
Therapeutics undertakes no duty to update this information unless
required by law.
Contacts:Investors: Courtney SolbergSenior
Manager, Investor RelationsCSolberg@c4therapeutics.com
Media: Loraine Spreen Senior Director, Corporate
Communications & Patient
Advocacy LSpreen@c4therapeutics.com
C4 Therapeutics (NASDAQ:CCCC)
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