IO Biotech (Nasdaq: IOBT), a clinical-stage biopharmaceutical
company developing novel, off-the-shelf, immune modulating
therapeutic cancer vaccines, announced data from the NSCLC cohort
in the company’s Phase 2 basket trial of IO102-IO103, the company’s
lead investigational candidate, given in combination with Merck’s
(known as MSD outside of the United States and Canada) anti-PD-1
therapy KEYTRUDA® (pembrolizumab) (IOB-022/KN-D38). These data, as
well as new pre-clinical data from IO Biotech’s second vaccine
candidate, IO112, will be presented at the Society for
Immunotherapy of Cancer’s 39th Annual Meeting (SITC 2024) in
Houston on November 8-10, 2024.
“These data build on the growing clinical
evidence for IO102-IO103 in hard-to-treat cancers. These Phase 2
NSCLC data evaluating IO102-IO103 in combination with pembrolizumab
demonstrated a positive trend in ORR compared to benchmark data in
the evaluable patient population with no unexpected toxicity,”
stated Jonathan Riess, MD, principal investigator of the trial and
Director, Thoracic Oncology at the UC Davis Comprehensive Cancer
Center. “We need new treatments that can extend the durability of
response for lung cancer patients. No progression in nearly half of
the patients in this study at 12 months is a positive signal.”
The presentation contains clinical and biomarker
data from the fully enrolled cohort of patients (n=37) with
previously untreated metastatic stage NSCLC with PD-L1 high TPS ≥
50. The data from 31 efficacy evaluable patients demonstrated:
- A 55% unconfirmed (16 partial
responses, 1 complete response), 48% confirmed overall response
rate (ORR) in a PD-L1 high population of patients with NSCLC
- An 81% disease control rate
(DCR)
- No disease progression at 12 months
in approximately 50% of patients
- An encouraging 8.1-month median
progression-free survival (PFS)
- Median duration of response (DOR)
not yet reached
- A safety profile consistent with
previously reported data when combining IO102-IO103 with anti-PD-1
monotherapy
- Vaccine-specific T cell responses
to both IO102 (IDO1) and IO103 (PD-L1) were detected in patients on
treatment
“The results of the combination of IO102-IO103
with the anti-PD-1 therapy pembrolizumab in the NSCLC cohort,
combined with the promising data presented at ESMO for the SCCHN
cohort and the previous Phase 1/2 data in melanoma, add to the body
of evidence that our dual-approach of targeting tumor cells and
immune suppressive cells in the tumor microenvironment may drive a
meaningful clinical benefit across a range of hard-to-treat
cancers,” said Qasim Ahmad, MD, Chief Medical Officer of IO
Biotech. “Importantly, we are observing promising activity with no
unexpected toxicity and safety concerns, which addresses a high
unmet medical need and an important gap in current treatment
options for patients.”
To date, the safety profile observed in this
study (IOB-022/KN-D38) is consistent with prior studies of
IO102-IO103 in combination with checkpoint inhibitors, with no
unexpected systemic toxicity compared to anti-PD-1 monotherapy and
low-grade transient injection site reactions reported as the most
common treatment related adverse events. Data from the squamous
cell carcinoma of the head and neck (SCCHN) cohort of this study
were presented at the 2024 European Society for Medical Oncology
congress in September that demonstrated the cohort met its primary
endpoint of ORR with encouraging PFS data.
Pre-clinical data from IO112, IO
Biotech’s second therapeutic cancer vaccine candidate derived from
the company’s T-win® platform, also presented at SITC
2024Arginase 1 (Arg1) plays a central role in immune
suppression, and its overexpression has been reported in several
cancers including renal cell carcinoma, pancreatic cancer, and head
and neck cancer. Importantly, all immune suppressive myeloid cells
in the TME express Arg1, and their key roles in cancer immune
resistance mechanisms have been well described. The data presented
in the poster showcase that IO112 vaccination leads to robust
expansion of Arg1-specific T cells, which in turn directly target
and reprogram immune suppressive TAMs, leading to tumor growth
inhibition.
“Our present data confirm the hypothesis that
the primary and direct target of IO112 treatment are TAMs – and,
what is striking, is how dynamically the vaccine-induced T cells
are impacting TAMs,” said Ayako Wakatsuki Pedersen, PhD, Senior
Vice President of Translational Research at IO Biotech. “Treatment
with IO112 results in TAMs changing their phenotype completely,
from immune suppressive to highly pro-inflammatory, driving the
modulation of the TME, and facilitating the immune attack on tumor
cells. These data give us further confidence in our T-win®
platform, a unique approach to induce a proinflammatory and
anti-tumorigenic TME via T cells that attack the primary drivers of
immune suppression. This strong data adds to the rationale for
IO112 clinical development, and we look forward to submitting an
IND for IO112 in 2025.”
The posters can be found on the “Posters &
Publications” page of the IO Biotech website. Details for the
presentations are below:
Title: A phase 2 trial of the
IO102-IO103 cancer vaccine plus pembrolizumab: results from the
first-line (1L) cohort of PD-L1 high metastatic non-small cell lung
cancer (NSCLC) Presenter: Jonathan W. Riess, MD,
MS, UC Davis Comprehensive Cancer CenterAbstract/Poster
number: 756Date: Saturday, November 9,
2024Location: Exhibit Halls AB - George R. Brown
Convention CenterTimes: Poster hall: 9:00 a.m. -
8:30 p.m. CDT; Poster session 12:15 – 1:45 p.m.; Poster reception
7:00-8:30 p.m.
Title: Immune modulating
vaccine against arginase 1 controls tumor growth via modulation of
tumor-associated macrophages Presenters: Evelina
Martinenaite, PhD, Senior Scientist, Translational Research, and
Inés Lecoq, PhD, Scientist, Translational Research, IO
BiotechAbstract/Poster number:
1038Date: Saturday, November 9,
2024Location: Exhibit Halls AB - George R. Brown
Convention CenterTimes: Poster hall: 9:00 a.m. -
8:30 p.m. CDT; Poster session 12:15 – 1:45 p.m.; Poster reception
7:00-8:30 p.m.
About IO102-IO103
IO102-IO103 is an investigational off-the-shelf
therapeutic cancer vaccine designed to kill both tumor cells and
immune-suppressive cells in the tumor microenvironment (TME) by
stimulating activation and expansion of T cells against indoleamine
2,3-dioxygenase (IDO) positive and programmed death-ligand 1
(PD-L1) positive cells. The company is currently conducting a
pivotal Phase 3 trial (IOB-013/KN-D18; NCT05155254) investigating
IO102-IO103 in combination with pembrolizumab versus pembrolizumab
alone in patients with advanced melanoma, a Phase 2 basket trial
(IOB-022/KN-D38; NCT05077709) investigating IO102-IO103 in
combination with pembrolizumab as first line treatment in patients
with solid tumors, and a Phase 2 basket trial (IOB-032/PN-E40;
NCT05280314) investigating IO102-IO103 in combination with
pembrolizumab as neo-adjuvant/adjuvant treatment of patients with
solid tumors.
The clinical trials are sponsored by IO Biotech
and conducted in collaboration with Merck, which is supplying
pembrolizumab. IO Biotech maintains global commercial rights to
IO102-IO103.
KEYTRUDA® is a registered trademark of Merck
Sharp & Dohme LLC, a subsidiary of Merck & Co., Inc.,
Rahway, NJ, USA.
About IO Biotech
IO Biotech is a clinical-stage biopharmaceutical
company developing novel, immune-modulating therapeutic cancer
vaccines based on its T-win® platform. The T-win platform is based
on a novel approach to cancer vaccines designed to activate T cells
to target the immunosuppressive cells in the tumor
microenvironment. IO Biotech is advancing its lead cancer vaccine
candidate, IO102-IO103, in clinical trials, and additional pipeline
candidates through preclinical development. Based on positive Phase
1/2 first line metastatic melanoma data, IO102-IO103, in
combination with pembrolizumab, has been granted a breakthrough
therapy designation for the treatment of advanced melanoma by the
US Food and Drug Administration. IO Biotech is headquartered in
Copenhagen, Denmark and has US headquarters in New York, New
York.
For further information, please visit
www.iobiotech.com. Follow us on our social media channels on
LinkedIn and X (@IOBiotech).
Forward-Looking Statement
This press release contains forward-looking
statements within the meaning of Section 27A of the Securities Act
of 1933, as amended, and Section 21E of the Securities Exchange Act
of 1934, as amended. Forward-looking statements, including
regarding the timing or outcome of primary analysis of the
company’s Phase 3 trial, other current or future clinical trials,
their progress, enrollment or results, or the company’s financial
position or cash runway, are based on IO Biotech’s current
assumptions and expectations of future events and trends, which
affect or may affect its business, strategy, operations or
financial performance, and actual results and other events may
differ materially from those expressed or implied in such
statements due to numerous risks and uncertainties. Forward-looking
statements are inherently subject to risks and uncertainties, some
of which cannot be predicted or quantified. Because forward-looking
statements are inherently subject to risks and uncertainties, you
should not rely on these forward-looking statements as predictions
of future events. These forward-looking statements speak only as of
the date hereof and should not be unduly relied upon. Except to the
extent required by law, IO Biotech undertakes no obligation to
update these statements, whether as a result of any new
information, future developments or otherwise.
Contact:
InvestorsMaryann Cimino, Director of Investor
Relations IO Biotech, Inc.617-710-7305mci@iobiotech.com
MediaJulie
FunestiSalutem917-498-1967julie.funesti@salutemcomms.com
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