WESTPORT, Conn., Dec. 10, 2021 /PRNewswire/ -- Intensity
Therapeutics, Inc. ("Intensity"), a clinical-stage
biotechnology company focused on the discovery and development of
proprietary, novel immune-based intratumoral cancer therapies
designed to kill tumors and increase immune system recognition of
cancers, today reported safety, pharmacokinetic, biomarker and
efficacy data using INT230-6, with and without pembrolizumab,
in heavily pretreated refractory breast cancer patients as part of
the Company's phase 1/2 study, IT-01. The presentation was made at
the San Antonio Breast Cancer Symposium® (SABCS), being held
virtually and in-person at the Henry B. Gonzales Convention Center in San Antonio, Texas.
The seven heavily pre-treated breast cancer subjects were
enrolled in the study after having progressed on a median of six
(range 2 to 10) prior therapies. The INT230-6 monotherapy subjects
(n=4) were more heavily pre-treated with a median of eight prior
therapies vs. three prior therapies for pembrolizumab combination
subjects (n=3). The disease control rate (DCR), defined as the
percent of breast cancer subjects with a complete response, partial
response, or stable disease at the first radiologic assessment, was
57%. Study authors reported a median overall survival (mOS) of 12
months (CI:7.2, NR), which compares favorably to results seen in
phase 1 studies of subjects with highly refractory or triple
negative breast cancer. Abscopal effects were seen in a
non-injected visceral lesion in 1 of 4 INT230-6 monotherapy
subjects. A number of patients came off study after completion of
INT230-6 dosing without disease progression. One subject continued
receiving INT230-6 injections despite a new lesion.
Peak plasma concentrations of the agent vinblastine were less
than five percent (5%) of that predicted, based on historical IV
kinetics, indicating that 95% of the drug remains in the tumor.
Treatment related adverse events (TRAEs) were favorable with or
without pembrolizumab. Only one subject experienced a grade 3 TRAE
(monotherapy group) and there were no grade 4 or grade 5 TRAEs.
Tissue analysis of matched paired (pre- and 28 days post-dose)
biopsies in injected tumors from subjects receiving their first
INT230-6 treatment cycle (two doses, n=3) had an average reduction
in viable cancer cells of sixty-nine percent (69%).
Immunohistochemistry results showed influx of CD4 and CD8 T-cells
into the tumor microenvironment.
"Preliminary data suggests that INT230-6 demonstrates direct
tumor killing in metastatic breast cancer subjects including those
with triple negative breast cancer (TNBC) and may elicit an
anti-cancer immune response within the injected tumor with or
without pembrolizumab," stated poster presenter and study
investigator, Philippe Bedard, M.D.,
Clinician Investigator, Princess Margaret Cancer Centre in
Toronto Canada. "Additionally,
INT230-6 treatment related adverse events are mostly low grade and
the drug is well-tolerated either as a monotherapy or in
combination with anti-PD-1 therapy, pembrolizumab. These results
provide evidence to continue studying this novel therapeutic drug
approach in breast cancer."
"The data presented at the San Antonio Breast Cancer Symposium
using INT230-6 alone or in combination with pembrolizumab were
generated from refractory breast cancer patients treated in the
dose escalation portion of our phase 1 clinical study, IT-01, and
these results are encouraging. We have also learned a great deal
about our drug in breast cancer from our trial in metastatic
patients and our phase 2 randomized INVINCIBLE study, which is
testing INT230-6 in breast cancer patients in a presurgical
setting," said Lewis H. Bender,
President and Chief Executive Officer of Intensity Therapeutics.
"We are excited about conducting additional clinical studies using
INT230-6 in metastatic breast cancer as part of INT230-6's Fast
Track designation as well as in presurgical patients, as there
remains an unmet medical need for safer more effective treatments
in both settings."
Presentation Title: Safety and efficacy of
INT230-6, a potential first-in-class intratumoral therapy, in
monotherapy and in combination with pembrolizumab: Results from the
IT-01 study [KEYNOTE-A10] in subjects with locally advanced,
unresectable and metastatic breast cancer
Abstract:
541
Poster Number: P-5-16-13
First Author: Philippe Bedard, MD, FRCPC, Princess
Margaret Cancer Centre, Toronto,
ON, Canada.
Full Authors Block: Philippe
Bedard1, Lillian L Siu1, Jacob Thomas2, Diana Hanna3, Anthony J
Olszanski4, Nilofer
Azad5, Giles
Whalen6, Matthew
Ingham7, Syed
Mahmood8, Lewis H Bender8, Ian B
Walters8 and Anthony
El-Khoueiry2. 1Princess Margaret
Cancer Centre, Toronto, ON,
Canada2USC Norris Comprehensive Cancer Center,
Los Angeles,
CA;3USC Hoag Memorial
Hospital Presbyterian, Newport Beach,
CA;4Fox Chase Cancer Center, Philadelphia, PA;5Johns Hopkins
Sidney Kimmel Comprehensive Cancer Center, Baltimore, MD;6UMass Memorial
Medical Center - University Campus, Worcester, MA;7New York
Presbyterian Hospital/Columbia
University Medical Center, New
York, NY;8Intensity Therapeutics, Inc.,
Westport, CT,
Session: Treatment: Therapeutic Strategies - New Drugs and
Treatment Strategies
Date: Friday, December 10, 2021
Time: 7:00AM – 8:30AM Central
Standard Time
The presentation will be accessible on the "Publications, Papers
and Posters" section of Intensity's website at:
https://intensitytherapeutics.com/news/publications-papers-and-posters
on December 10, 2021.
About INT230-6
INT230-6, Intensity's lead proprietary investigational product
candidate, is designed for direct intratumoral injection. INT230-6
was discovered using Intensity's proprietary DfuseRx℠ technology
platform. The drug is composed of two proven, potent anti-cancer
agents, cisplatin and vinblastine, and an amphiphilic penetration
enhancer molecule that helps disperse the drugs throughout tumors
for diffusion into cancer cells. In addition to local disease
control, direct killing of the tumor by INT230-6 releases
neoantigens specific to the patient's malignancy, leading to
engagement of the immune system and systemic anti-tumor effects.
Importantly, these effects are mediated without the
immunosuppression of concomitant systemic chemotherapy.
INT230-6 is currently being evaluated in several phase 2 cohorts
(NCT03058289) in patients with various advanced solid tumors as
part of Study IT-01. In 2019, the Company signed a clinical
collaboration agreement with Merck Sharpe & Dohme (Merck) to
evaluate the combination of INT230-6 and KEYTRUDA® (pembrolizumab),
Merck's anti-PD-1 (programmed death receptor-1) therapy, in
patients with advanced pancreatic, colon, squamous cell and bile
duct malignancies. In 2020, the Company executed a clinical
collaboration agreement with Bristol-Myers Squibb Company to
evaluate the combination of INT230-6 with Bristol-Myers Squibb's
anti-CTLA-4 antibody, Yervoy® (ipilimumab), in patients with
advanced liver, breast and sarcoma cancers. In 2021, the Company
executed agreements with the Ottawa Hospital Research Institute and
the Ontario Institute of Cancer Research to study INT230-6 in a
randomized controlled neoadjuvant phase 2 study in women with early
stage breast cancer (the INVINCIBLE study) (NCT04781725).
KEYTRUDA® is a registered trademark of Merck Sharp & Dohme
Corp., a subsidiary of Merck & Co., Inc., Kenilworth, NJ, USA.
About Intensity Therapeutics
Intensity Therapeutics, Inc. is a clinical-stage biotechnology
company pioneering a new immune-based approach to treat solid tumor
cancers. Intensity leverages its DfuseRx℠ technology platform to
create new, proprietary drug formulations that, following direct
injection, rapidly disperse throughout a tumor and diffuse
therapeutic agents into cancer cells. Intensity's product
candidates have the potential to induce an adaptive systemic immune
response that not only attacks the injected tumor, but also
non-injected tumors. The Company executed a Cooperative Research
and Development Agreement (CRADA) with the National Cancer
Institute's (NCI) Vaccine Branch in 2014 and has partnerships with
Merck and Bristol-Myers Squibb. For more information, please visit
www.intensitytherapeutics.com.
Forward-Looking Statements
This press release contains forward-looking statements regarding
Intensity Therapeutics' plans, future operations and objectives.
Such statements involve known and unknown risks, uncertainties and
other factors that may cause actual performance or achievements to
be materially different from those currently anticipated. These
forward-looking statements include, among other things, statements
about the initiation and timing of future clinical
trials.
Contact Information
Investor Relations Contact:
Rx Communications
Group
Michael Miller
(917)-633-6086
mmiller@rxir.com
US Media Contact:
KOGS Communication
Edna Kaplan
+1 781 639 1910
kaplan@kogspr.com
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SOURCE Intensity Therapeutics, Inc.