Immatics Announces Multiple Presentations at the 39th Annual
Meeting of the Society for Immunotherapy of Cancer (SITC) on TCR-T
Therapy Candidates Targeting PRAME
Two oral presentations and multiple
posters on clinical and
preclinical-stage candidates to
be presented at SITC, demonstrating
the strength of
Immatics’ TCR-T PRAME franchise to target solid
cancers
- ACTengine® IMA203 demonstrates 54%
cORR, 12.1 months mDOR and 6 months mPFS in heavily pretreated
metastatic melanoma patients and >1-year mPFS in patients with
deep responses; Company plans to start its randomized-controlled
Phase 3 SUPRAME trial in December 2024 to evaluate IMA203 in
second-line or later metastatic melanoma
- Next-generation ACTengine®
IMA203CD8 TCR-T cell therapy targeting PRAME demonstrates enhanced
pharmacology and potency per cell; Phase 1a dose escalation
reinitiated to target higher doses, positioning this TCR-T
candidate for future development in solid cancers with medium-level
PRAME copy numbers, such as ovarian cancer, endometrial cancers and
triple-negative breast cancer
- A first update on Immatics’
Bispecific TCER® IMA402 targeting PRAME and initial clinical data
from the ongoing Phase 1a dose escalation trial is expected to be
reported by year-end
Houston, Texas and Tuebingen, Germany,
November 8, 2024 – Immatics N.V. (NASDAQ: IMTX, “Immatics”
or the “Company”), a clinical-stage biopharmaceutical company
active in the discovery and development of T cell-redirecting
cancer immunotherapies, today announced an expanded clinical
dataset from the ongoing Phase 1b dose expansion clinical trial for
ACTengine® IMA203 in addition to updated Phase 1 dose escalation
clinical data on its next-generation ACTengine® IMA203CD8 TCR-T
cell therapy. For the first time, the Company also reported
preclinical data on other next-generation T cell candidates and
combination strategies as part of its strategy to further exploit
opportunities in additional solid tumor types within its PRAME
franchise.
All dates and times of Immatics’ upcoming oral
and poster presentations at the 39th Annual Meeting of
the Society for Immunotherapy of Cancer (SITC) are available here.
The data slides are accessible in the ‘Events & Presentations’
section of the Investor & Media section of the Company’s
website.
“Immatics remains fully focused on the clinical
development of our most advanced lead product candidate, IMA203, in
second-line or later metastatic melanoma patients. We look forward
to the initiation of SUPRAME, the registration-enabling Phase 3
trial, in December,” said Dr. Cedrik Britten, Chief Medical Officer
at Immatics. “Today, we also provide an update on our first,
next-generation cell therapy, IMA203CD8, which is designed to
achieve enhanced anti-tumor activity. The data announced confirm
IMA203CD8’s enhanced pharmacology and potency per cell in patients.
These attributes highlight the potential of this therapy in
hard-to-treat solid tumors with medium-level PRAME copy numbers,
including ovarian, endometrial and triple-negative breast cancer.
The next step will be to further increase the cell dose to assess
the full clinical potential of IMA203CD8 beyond melanoma. In
addition, we strive to continuously improve the potential
therapeutic benefit for patients with a range of PRAME-positive
cancers through the expansion of our PRAME franchise.”
ACTengine® IMA203 Monotherapy Phase 1b
Trial - Clinical Data and Development Path Summary
On October 10, 2024, Immatics provided a data
update on IMA203 monotherapy in 281 heavily pretreated
metastatic melanoma patients from the ongoing Phase 1b dose
expansion part of the clinical trial in which patients were treated
at the recommended Phase 2 dose (RP2D, 1 to 10 billion total TCR-T
cells).
The data announced today include all infused
patients in the Phase 1b dose expansion part of the trial
(N=412), consisting of the 28 melanoma patients reported
on October 10, 2024, and 13 non-melanoma patients, of which 10
non-melanoma patients were reported on November 8, 2023.
IMA203 monotherapy has maintained a favorable
tolerability profile with no treatment-related Grade 5 events in
the entire safety population (N=703 Phase 1a and Phase
1b patients across all dose levels and all tumor types).
Best Overall Response for IMA203 in Dose
Expansion in All Indications
(N=41#)
Data cut-off Aug 23, 2024;
#First tumor assessment post infusion
pending for 2/28 melanoma patients at data-cut; *Maximum change of
target lesions and RECIST1.1 response at different timepoints.
1Patient A-DL5-23 is off study at data
cut-off; 2Patient received one dose
nivolumab erroneously.
Development Path for IMA203
Based on the Phase 1b data, the Company is on track to commence
SUPRAME, the registration-enabling Phase 3 randomized-controlled
clinical trial in melanoma for IMA203, in December 2024.
SUPRAME will evaluate IMA203 targeting PRAME in
360 HLA-A*02:01-positive patients with second-line or later (2L+)
unresectable or metastatic melanoma who have received prior
treatment with a checkpoint inhibitor. Patients will be randomized
1:1 for IMA203 or investigator’s choice of selected approved
treatments in the 2L+ setting, including nivolumab/relatlimab,
nivolumab, ipilimumab, pembrolizumab, lifileucel (US only) or
chemotherapy. The primary endpoint for full approval will be median
PFS and secondary endpoints will include objective response rate,
safety, duration of response, no overall survival detriment and
patient-reported outcomes.
Patient enrollment for SUPRAME is forecast to be
completed in 2026, and a pre-specified interim analysis is planned
for early 2026. Immatics aims to submit a Biologics License
Application (BLA) in early 2027 for full approval.
ACTengine® IMA203CD8 (GEN2) Monotherapy
Phase 1 Dose Escalation Trial - Patient Population & Clinical
Data Summary
Patient population: Heavily
pretreated patients with solid tumors
As of data cut-off on September 30, 2024, 444 heavily
pretreated HLA-A*02:01 and PRAME-positive patients with solid
tumors were infused with IMA203CD8 monotherapy across four
escalating dose levels, of which 415 patients were
evaluable for efficacy. The median total infused dose was
1.48x109 TCR-T cells, and the patient population is
composed of patients with a median of three lines of prior systemic
treatments.
Safety: Treatment with
IMA203CD8 demonstrates a manageable tolerability profile across
dose levels
IMA203CD8 monotherapy has maintained a manageable tolerability
profile in the 44 patients treated. The most frequent adverse
events at or above Grade 3 were expected cytopenia associated with
lymphodepletion. Some patients also experienced mild to moderate
CRS (Grade 1: 36% Grade 2: 48% Grade 3: 11% Grade 4: 2%).
As previously reported, two patients experienced
dose-limiting toxicities at dose level 4b, which prompted a dosing
adjustment to dose level 4a. After further assessing the
tolerability profile of IMA203CD8 in additional patients treated at
dose level 4a, the eligibility criteria and the IL-2 dose regimen
were modified, and dose escalation beyond dose level 4a was
reinitiated. One Grade 5 adverse event classified as possibly
related to treatment with IMA203CD8 was also observed as reported
previously in March 2024. The maximum tolerated dose has not yet
been determined.
Anti-tumor activity and
durability: Deep and durable objective responses
observed
- As of data cut-off on September 30,
2024, 10 of 17 responses were ongoing, of which three confirmed
responses were ongoing at 14+, 15+ and 24+ months.
- Of note, these patients had been
treated at substantially lower doses compared to IMA203 (GEN1),
i.e. in a range of 0.2-0.48x109 TCR-T
cells/m2 BSA (dose level 3) to 0.801-1.2x109
TCR-T cells/m2 BSA (dose level 4c) T cells infused.
- Deep responses with ≥50% tumor size
reduction were observed in 11 out of 17 responders. This group
included two patients with complete response of target lesions, of
which one patient showed a complete metabolic response according to
PET-CT scan6.
- 41% (14/34) confirmed objective
response rate (cORR) and 41% (17/41) objective response rate
(ORR).
- Median duration of response (mDOR)
of 9.2 months at a median follow-up (mFU) of 13.1 months.
- Tumor shrinkage7 of 84%
(32/38) and disease control rate8 at week 6 of 85%
(34/40).
Translational data:
Opportunity of IMA203CD8 in medium-level PRAME expressing
indications
Translational data indicate that PRAME expression level is
associated with clinical activity in IMA203 and IMA203CD8 treated
patients. Both IMA203 and IMA203CD8 achieved deep responses despite
IMA203CD8 patients receiving lower product doses. Based on the
enhanced pharmacology of IMA203CD8, the evaluation of higher doses
of IMA203CD8 in the ongoing dose escalation trial opens the
possibility of addressing hard-to-treat solid tumor indications
with a medium-level of PRAME copy numbers, such as ovarian cancer,
endometrial cancers and triple-negative breast cancer.
Preclinical Data on New Approaches for
TCR-T Based Cell Therapies
As part of Immatics’ long-term strategy to
expand its PRAME franchise, the Company has conducted preclinical
studies for the potential future clinical development of
next-generation TCR-T-based cell therapies targeting PRAME to
further enhance the efficacy and durability of IMA203. These
efforts include the evaluation of TCR-T cells armored with
membrane-bound IL-15 (mbIL15) targeting tumor types with low PRAME
copy numbers, such as squamous non-small-cell lung cancer and
squamous head and neck cancers. In addition, the Company is
developing an allogeneic cell therapy approach to further increase
commercial attractiveness and to reach patients quickly with its
next-generation off-the-shelf cell therapy, ACTallo®. The
preclinical data will be presented during poster sessions at
SITC.
About ACTengine® IMA203, IMA203CD8 and
Target PRAME
ACTengine® IMA203 is Immatics’ most advanced TCR-based
autologous cell therapy that is directed against an
HLA-A*02-presented (human leukocyte antigen) peptide derived from
preferentially expressed antigen in melanoma (PRAME), a protein
frequently expressed in a large variety of solid cancers. PRAME is
homogeneously and specifically expressed in tumor tissue and
Immatics’ PRAME peptide is present at a high copy number per tumor
cell. The peptide has been identified and characterized by
Immatics’ proprietary mass spectrometry-based target discovery
platform, XPRESIDENT®. Through its proprietary TCR
discovery and engineering platform XCEPTOR®, Immatics
has generated a highly specific T cell receptor (TCR) against this
target for ACTengine® IMA203.
ACTengine® IMA203 TCR-T is currently
being evaluated as a monotherapy in a Phase 1 clinical trial in
patients with solid tumors expressing PRAME, such as cutaneous
melanoma. An IMA203 registration-enabling randomized controlled
Phase 3 trial, “SUPRAME,” is planned to commence in December
2024.
ACTengine® IMA203 TCR-T is also currently being
evaluated in Phase 1 IMA203CD8 (GEN2) monotherapy, where IMA203
engineered T cells are co-transduced with a CD8αβ co-receptor.
- END -
About Immatics
Immatics combines the discovery of true targets for cancer
immunotherapies with the development of the right T cell receptors
with the goal of enabling a robust and specific T cell response
against these targets. This deep know-how is the foundation for our
pipeline of Adoptive Cell Therapies and TCR Bispecifics as well as
our partnerships with global leaders in the pharmaceutical
industry. We are committed to delivering the power of T cells and
to unlocking new avenues for patients in their fight against
cancer.
Immatics intends to use its website
www.immatics.com as a means of disclosing material non-public
information. For regular updates you can also follow us on X,
Instagram and LinkedIn.
Forward-Looking Statements
Certain statements in this press release may be considered
forward-looking statements. Forward-looking statements generally
relate to future events or the Company’s future financial or
operating performance. For example, statements concerning timing of
data read-outs for product candidates, the timing, outcome and
design of clinical trials, the nature of clinical trials (including
whether such clinical trials will be registration-enabling), the
timing of IND or CTA filing for pre-clinical stage product
candidates, the timing of BLA filings for clinical stage product
candidates, estimated market opportunities of product candidates,
the Company’s focus on partnerships to advance its strategy, and
other metrics are forward-looking statements. In some cases, you
can identify forward-looking statements by terminology such as
“may”, “should”, “expect”, “plan”, “target”, “intend”, “will”,
“estimate”, “anticipate”, “believe”, “predict”, “potential” or
“continue”, or the negatives of these terms or variations of them
or similar terminology. Such forward-looking statements are subject
to risks, uncertainties, and other factors which could cause actual
results to differ materially from those expressed or implied by
such forward-looking statements. These forward-looking statements
are based upon estimates and assumptions that, while considered
reasonable by Immatics and its management, are inherently
uncertain. New risks and uncertainties may emerge from time to
time, and it is not possible to predict all risks and
uncertainties. Factors that may cause actual results to differ
materially from current expectations include, but are not limited
to, various factors beyond management's control including general
economic conditions and other risks, uncertainties and factors set
forth in the Company’s Annual Report on Form 20-F and other filings
with the Securities and Exchange Commission (SEC). Nothing in this
press release should be regarded as a representation by any person
that the forward-looking statements set forth herein will be
achieved or that any of the contemplated results of such
forward-looking statements will be achieved. You should not place
undue reliance on forward-looking statements, which speak only as
of the date they are made. The Company undertakes no duty to update
these forward-looking statements. All the scientific and clinical
data presented within this press release are – by definition prior
to completion of the clinical trial and a clinical study report –
preliminary in nature and subject to further quality checks
including customary source data verification.
For more information, please contact:
|
Media |
|
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Trophic Communications |
|
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Phone: +49 171 3512733 |
|
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immatics@trophic.eu |
|
|
Immatics N.V. |
|
|
Jordan Silverstein |
|
|
Head of Strategy |
|
|
Phone: +1 346 319-3325 |
|
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InvestorRelations@immatics.com |
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1 Includes one patient who started lymphodepletion
but did not receive IMA203 TCR-T cells.
2 All infused patients, first tumor assessment post
infusion pending for 2/28 melanoma patients at data-cut.
3 All patients who started lymphodepletion as of the
data cut-off on August 23, 2024.
4 All patients who started lymphodepletion.
5 All infused patients with at least one tumor
assessment postbaseline.
6 Metabolic CR on investigator-initiated PET month 14
post infusion.
7 Three patients excluded from tumor shrinkage analysis
and figures due to lack of post-treatment assessment.
8 One patient had an early tumor assessment, outside the
first assessment visit window and is not included in DCR
calculation.
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