On April 8, 2022 Nuvalent, Inc., (Nasdaq: NUVL) a clinical-stage biopharmaceutical company creating precisely targeted therapies for patients with cancer, reported new data to support broad clinical exploration of its parallel lead programs NVL-520 – a ROS1-selective inhibitor – and NVL-655 – an ALK-selective inhibitor (Press release, Nuvalent, APR 8, 2022, View Source [SID1234611782]). NVL-520 and NVL-655 are central nervous system (CNS)-penetrant kinase inhibitors designed to specifically solve for the dual challenges of kinase resistance and selectivity commonly observed with currently available inhibitors.

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The data are available via two posters presented at the American Association for Cancer Research (AACR) (Free AACR Whitepaper) Annual Meeting 2022, which runs from April 8 through April 13. The posters will also be available on the Nuvalent website at www.nuvalent.com/news/.

"We are pleased to share new data today resulting from our continued collaborations with leading investigators in ROS1 and ALK research, which we believe further demonstrate the potential for our highly selective inhibitors to be differentiated within the dynamic treatment landscapes for non-small cell lung cancer (NSCLC) and beyond," said James Porter, Ph.D., Chief Executive Officer of Nuvalent. "These preclinical data support the inclusion of various fusion partners and resistance mutations in our ARROS-1 and ALKOVE-1 clinical trials for ROS1- and ALK-positive NSCLC, respectively, as well as the inclusion of exploratory cohorts for other advanced solid tumors outside of NSCLC."

Monika Davare, Ph.D. is an Associate Professor of Pediatrics, Division of Hematology and Oncology at Oregon Health & Science University School of Medicine and leading expert in ROS1 oncoprotein biology. Professor Davare’s research is directed towards overcoming therapeutic bottlenecks in oncology, including those that arise from the lack of validated translational research models for genomic subsets of cancer.

"Translational models of ROS1-driven cancers have centered on NSCLC, where the clinical impact of fusion partners is not yet well characterized and new treatment-resistant variants continue to emerge. Hypothesizing that broad coverage of fusion partners and resistance mutations is a beneficial feature for next-generation ROS1 inhibitors, we conducted an extensive comparative analysis of NVL-520 versus currently approved as well as investigational ROS1 inhibitors," said Professor Davare. "In contrast to comparator compounds, NVL-520 exhibited consistently high potency (IC50 < 10 nM) across all models tested, and in particular displayed potencies against the recurrently problematic G2032R solvent front mutation that were ≥ 1-order of magnitude higher than all comparative agents tested."

"While models of ROS1-driven cancers outside of NSCLC are sparse, we further present data that NVL-520 induces regression in a human cell-line derived model of glioblastoma driven by a ROS1 fusion," continued Professor Davare. "This suggests potential for clinical utility outside of NSCLC and highlights the importance of developing additional research models to help accelerate the development of new therapies for genomically-driven cancers."

Luc Friboulet, Ph.D. is an investigator at Gustave Roussy focused on investigating molecular mechanisms of tumor adaptation to kinase inhibitors in solid tumors, with particular expertise in understanding resistance to ALK kinase inhibitors.

"ALK oncogenic activations as well as mutations conferring resistance to current ALK inhibitors have been characterized across a range of tumor types, suggesting that broad activity across diverse ALK-driven cancers is a beneficial feature for next-generation ALK inhibitors," said Dr. Friboulet. "In a comparative analysis of NVL-655 versus currently approved as well as investigational ALK inhibitors, NVL-655 exhibited strong activity across a wide range of fusion partners, activating mutations, and disease backgrounds, suggesting potential for broad clinical utility. Importantly, this expansive activity of NVL-655 against ALK does not come at the expense of its ability to avoid inhibition of TRKB, a limitation that has been observed with other investigational ALK inhibitors."

NVL-520 is currently under investigation in the Phase 1 portion of the Phase 1/2 ARROS-1 study (NCT05118789) for advanced ROS1-positive NSCLC and other solid tumors. Nuvalent recently announced the IND clearance for NVL-655 and plans to initiate the Phase 1 portion of the Phase 1/2 ALKOVE-1 study for advanced ALK-positive NSCLC and other solid tumors in the second quarter of 2022. In addition to these parallel lead programs, Nuvalent is advancing a robust discovery pipeline with plans to nominate two new development candidates in 2022 for ALK IXDN compound mutations and HER2 exon 20 insertions.

AACR Presentation Overview:

* Presenting authors

Title: NVL-520: Preclinical Activity of NVL-520 in ROS1-Driven Cancer Models with Diverse Fusion Partners and Kinase-Domain Mutations
Authors: Anupong Tangpeerachaikul*^, Clare Keddy^, Katelyn Nicholson, Monika A. Davare, and Henry E. Pelish*
^ Equal contributions
Poster Number: 14
Permanent Abstract: 3336
Session Category: Experimental and Molecular Therapeutics
Session Title: Tyrosine Kinase and Phosphatase Inhibitors
Session Date and Time: Tuesday April 12, 2022 from 1:30 – 5:00 p.m. Central Time
Location: New Orleans Convention Center, Exhibit Halls D-H, Poster Section 26

Summary of Presentation:

NVL-520 shows high activity against diverse ROS1 fusion partners tested including CD74, CEP85L, EZR, GOPC(L), GOPC(S), and SLC34A2 and induces regression in a ROS1-driven model of glioblastoma harboring GOPC(L)-ROS1.
NVL-520 shows high activity against diverse ROS1 kinase-domain mutations tested including S1986F, F2004C/V, L2026M, G2032R, D2033N, and G2101A.
NVL-520 shows a differentiated preclinical activity and selectivity profile compared to other inhibitors tested.
Preclinical activity against diverse ROS1 fusion partners and kinase domain mutations suggests broad potential clinical utility of NVL-520.
Title: NVL-655: Preclinical Activity of NVL-655 in ALK-Driven Cancer Models beyond Non-Small Cell Lung Cancer
Authors: Anupong Tangpeerachaikul*, Ludovic Bigot, Luc Friboulet, and Henry E. Pelish*
Poster Number: 15
Permanent Abstract: 3337
Session Category: Experimental and Molecular Therapeutics
Session Title: Tyrosine Kinase and Phosphatase Inhibitors
Session Date and Time: Tuesday April 12, 2022 from 1:30 – 5:00 p.m. Central Time
Location: New Orleans Convention Center, Exhibit Halls D-H, Poster Section 26

Summary of Presentation:

NVL-655 shows strong activity in diverse preclinical models of ALK-driven cancers: cholangiocarcinoma, neuroblastoma, lymphoma, and soft-tissue sarcoma.
Among all inhibitors tested, NVL-655 shows the broadest activity for diverse ALK oncoproteins including fusions, point mutations, and partial N-terminal deletions.
NVL-655 shows larger ALK-vs-TRK selectivity windows than lorlatinib and TPX-0131.
Preclinical activity against diverse ALK oncoproteins (fusions, mutations, and partial deletions) in multiple tumor types suggests broad potential clinical utility of NVL-655.

On April 8, 2022 BrickBio, the leader in RNA facilitated site-specific conjugation for novel protein therapeutics, reported that it will be presenting an invited poster at the annual meeting of the American Association of Cancer Research (AACR) (Free AACR Whitepaper) Conference on April 11th, 2022 during the Antibody-Drug Conjugates Session (Press release, BrickBio, APR 8, 2022, View Source [SID1234611780]). BrickBio will be located at Booth #3334 throughout the conference.

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BrickBio has commercialized its’ novel protein conjugation platform which leverages engineered RNA to introduce site-specific chemistries into any protein while maintaining a homogenous product for best-in-class therapeutics with improved safety, efficacy and dosage. The conjugation platform enables the conjugation of multiple distinct payloads on a single protein and the conjugation of two or more molecules to generate novel therapeutics.

The pipeline candidate depicted in the poster (#3940), Next Generation Site-Specific ADCs targeting Breast and Gastric Cancer was developed using the previously revealed Site-Select Panel and highlights the advantage of the powerful ADC platform towards breast & gastric cancer with improved efficacy, better safety, and overall lower dosage. Identification of the optimal sites are currently being transferred between next-generation antibody scaffolds, such as bispecifics, nanobodies, or other fragments in BrickBio’s undisclosed pipeline.

BrickBio’s pioneering, undisclosed efforts towards Protein Origami Therapeutics and Synthetic Virology are also highlighted, which leverage the same core technology that drive Brick’s novel ADCs. Protein Origami enables the spatial orientation of multiple proteins into a multimeric complex, resulting in synergistic modalities that have yet to be explored due to the inability to generate such structures prior to BrickBio. In addition, Synthetic Virology advancements revolve around the retargeting of capsids via protein conjugation to engineer tropisms, improve safety, increase infectivity, and eliminate immunogenicity. BrickBio is rapidly expanding on its strong base of AAV modification capabilities.

BrickBio is continuing their partnership efforts throughout AACR (Free AACR Whitepaper) 2022 by meeting with potential collaborators for work on novel ADCs, Protein Origami Therapeutics, and Synthetic Virology.

"The BrickBio platform and processes have unleashed the full potential of the unnatural amino acid technology, enabling new therapeutic modalities, all linked by the same conjugation chemistries", said James Italia, VP of Commercial Development at BrickBio, "Specifically, the novel ADC platform highlights the unprecedented precision in our discovery engine, allowing us to pursue novel pipeline candidates which were previously unattainable", Italia concluded.

"BrickBio’s unique and robust platform capabilities have positioned the company to expand its’ internal pipeline of novel, best-in-class ADC candidates, co-develop novel therapeutics with partners, and develop next generation therapeutics," stated Audrey Warner, Head of Business Development of BrickBio, as well as Vice President of Investments of Tiger Gene Ventures. "BrickBio will work with top partners to develop and progress promising candidates through the clinic to ultimately reach more patients," Warner concluded.

On April 8, 2022 Carisma Therapeutics Inc., a clinical stage biopharmaceutical company focused on discovering and developing innovative immunotherapies, reported that study findings accepted for presentation at The American Association for Cancer Research (AACR) (Free AACR Whitepaper) Annual Meeting taking place in New Orleans, LA, Friday, April 8 – Wednesday, April 13 (Press release, Carisma Therapeutics, APR 8, 2022, View Source [SID1234611777]). The accepted data reinforce the potential of Carisma’s differentiated and proprietary cell therapy platform focused on engineered macrophages as a novel treatment pathway for hard-to-treat cancers and other serious illnesses and provides information on the feasibility of a shortened manufacturing process for chimeric antigen receptor (CAR) monocytes.

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Carisma will share key findings from recent studies including, "Chimeric antigen receptor macrophages (CAR-M) sensitize solid tumors to anti-PD1 immunotherapy," presented by Stefano Pierini, PhD, Principal Scientist at Carisma. Findings demonstrate robust synergy between the CAR-Macrophage platform and T cell checkpoint inhibitor therapy. Using pre-clinical solid tumor animal models that are resistant to PD1 blockade, Carisma demonstrated that adding CAR-Macrophages to the treatment regimen significantly enhanced tumor control, overall survival, and tumor microenvironment (TME) activation. Notably, while CAR-Macrophage monotherapy led to TME remodeling, the combination with anti-PD1 led to an increased infiltration of T cells, dendritic cells, and other inflammatory immune cells. Carisma will seek to further evaluate CT-0508, the anti-human epidermal growth factor receptor 2 (HER2) CAR-Macrophage, in a combination study with pembrolizumab in patients with HER2 overexpressing tumors.

"Pre-clinical development of CAR Monocytes (CAR-Mono) for solid tumor immunotherapy," presented by Carisma Principal Scientist, Daniel Blumenthal, PhD, demonstrated that CAR-Monocytes can be produced in a single day, induce robust and targeted anti-tumor activity in vitro and in vivo, differentiate into M1 polarized CAR-Macrophage within tumors, and persist for over six months in animal models. In this study, Carisma established an ultra-rapid, same-day CAR-Monocyte manufacturing process, which holds the potential to significantly reduce the future cost of goods and manufacturing turnaround time associated with the autologous cell therapy.

Also accepted for AACR (Free AACR Whitepaper) presentation is the clinical trial design and foundational details regarding Carisma’s lead candidate, CT-0508, a HER2-targeted CAR-Macrophage, "A phase 1, first in human (FIH) study of autologous anti-HER2 chimeric antigen receptor macrophages (CAR-M) in HER2-overexpressing solid tumors (ST)," presented by Kim A. Reiss, MD, Assistant Professor of Medicine at the Abramson Cancer Center of the University of Pennsylvania (Penn) and the principal investigator for Carisma’s clinical trial of CT-0508. This first-of-its kind Phase 1 clinical trial is actively enrolling patients at five sites, including Penn; the University of North Carolina Lineberger Comprehensive Cancer Center in Chapel Hill; City of Hope in Duarte, California; University of Texas MD Anderson Cancer Center in Houston, Texas; and Sarah Cannon Research Institute at Tennessee Oncology – Nashville.

"The preclinical data presented at the AACR (Free AACR Whitepaper) Annual Meeting reinforces the exciting potential of Carisma’s engineered macrophage and monocyte platforms," shared Debora Barton, MD, Chief Medical Officer at Carisma Therapeutics. "Our commitment remains steadfast to providing new solutions to patients and their providers, as we continue our first-of-its-kind clinical trial of CT-0508 and look to expand utilization of this technology."

The following poster presentations will be published on the AACR (Free AACR Whitepaper) Annual Meeting website and available for registered attendees during the dates/times indicated below:

Sunday, April 10 at 1:30 pm ET:
Pre-clinical development of CAR Monocytes (CAR-Mono) for solid tumor immunotherapy
Monday, April 11 at 1:30 pm ET:
Chimeric antigen receptor macrophages (CAR-M) sensitize solid tumors to anti-PD1 immunotherapy
Tuesday, April 12 at 9:00 am ET:
A phase 1, first in human (FIH) study of autologous anti-HER2 chimeric antigen receptor macrophages (CAR-M) in HER2-overexpressing solid tumors (ST)
Editor’s Note: Carisma has licensed certain Penn-owned intellectual property from the University of Pennsylvania, and Penn’s Perelman School of Medicine receives sponsored research and clinical trial funding from the company. Penn may also be entitled to receive additional financial benefits from technologies licensed and optioned to Carisma in the future. In addition, Penn is a co-founder of the company and holds equity interests in Carisma.

On April 8, 2022 Cytovia Therapeutics, Inc., a biopharmaceutical company empowering natural killer (NK) cells to fight cancer through stem cell engineering and multispecific antibodies, reported that the novel data it is presenting at the American Association of Cancer Research’s annual meeting in New Orleans on April 12th, 2022 is now available on both the AACR (Free AACR Whitepaper) and Cytovia websites (Press release, Cytovia Therapeutics, APR 8, 2022, View Source [SID1234611775]).

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"We are very pleased with the decisive progress of Cytovia’s R&D team towards the manufacturing and preclinical validation of its two synergistic platforms," commented Dr. Daniel Teper, CEO and Chairman of Cytovia Therapeutics. "The data presented at AACR (Free AACR Whitepaper) supports the advancement of our lead GPC3-targeting hepatocellular carcinoma (HCC) program towards clinical trials and our differentiated CD38-targeting multiple myeloma program to IND-enabling studies. Cytovia is the first company to combine its own iPSC-derived natural killer (iNK) cells and multispecific, NK cell-engaging antibodies and is building a pipeline that encompasses both hematological malignancies and solid tumors."

"Cytovia’s GPC3-directed NK-engager in combination with iPSC-derived NK cells demonstrated impressive anti-tumor activity in mice that merits clinical development," added Dr. Michael Friedman, a member of Cytovia’s Board of Directors. "For the large number of hepatocellular cancer patients who currently have such limited, poor clinical options, a novel tumor antigen-directed NK engager is needed. It would be a welcome addition to a physician’s armament, with high potential for numerous combinations. The early CYT-338 data, showing superiority over daratumumab in several in vitro assays, is similarly impressive and warrants further preclinical development in my opinion."

Highlights from Posters Presented at the AACR (Free AACR Whitepaper) Annual Meeting

CYT-303

The FLEX-NKTM tetravalent, multifunctional antibody CYT-303 directed against NKp46 and GPC3 demonstrated in vitro and in vivo activity against HCC tumor targets.
iNK cells expressed a favorable combination of multiple activation and few inhibitory receptors that corresponded to more potent cytolytic activity against HCC targets.
The combination of the FLEX-NKTM and iNK platforms demonstrated greater in vitro and in vivo anti-tumor activity in HCC models than iNK cells alone, with a favorable in vitro cytokine release and immune cell subset safety profile.
These preclinical proof of concept studies with CYT-303 alone or in combination with iNK cells in HCC warrant clinical development.
CYT-338

The FLEX-NKTM multifunctional engager antibody CYT-338 directed against NKp46 and CD38 demonstrated in vitro activity against multiple myeloma tumor targets.
An analysis of binding sites on CD38 indicates CYT-338 binds an epitope that is distinct from daratumumab.
The binding, cytokine release, cytotoxicity, and fratricide profiles of CYT-338 were superior to daratumumab.
These data support further development of CYT-338 as a therapeutic for targeting CD38 expressing multiple myeloma cells.
For details on in-person poster presentations, please see the following:

Title: Preclinical characterization of FLEX-NKTM tetravalent NKp46 engager directed against GPC3 (CYT-303) alone or in combination with iPSC derived Natural Killer cells (iNKs) against hepatocellular carcinoma (HCC)
Presenter: Antonio Arulanandam
Session Title: Adoptive Cell Therapy
Session Date and Time: Tuesday, Apr 12, 2022, 9:00 AM – 12:30 PM
Location: New Orleans Convention Center, Exhibit Halls D-H, Poster Section 30
Poster Board Number: 8
Permanent Abstract Number: 2752
Abstract Link

Title: Novel multifunctional tetravalent CD38 NKp46 FLEX NKTM engagers actively target and kill multiple myeloma cells
Presenter: Liang Lin
Session Title: Combination Immunotherapies / Therapeutic Antibodies
Session Date and Time: Tuesday, Apr 12, 2022, 1:30 PM – 5:00 PM
Location: New Orleans Convention Center, Exhibit Halls D-H, Poster Section 32
Poster Board Number: 17
Permanent Abstract Number: 3436
Abstract Link

On April 8, 2022 Sumitomo Pharma Oncology, Inc., (SMP Oncology) a clinical-stage company focused on research and development for novel cancer therapeutics, reported it will present new clinical and preclinical data on a range of investigational agents from the company’s pipeline at the American Association for Cancer Research (AACR) (Free AACR Whitepaper) Annual Meeting, held April 8-13, 2022, in New Orleans, LA (Press release, Sumitomo Pharmaceuticals, APR 8, 2022, View Source [SID1234611774]).

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The data that will be presented at the meeting includes Phase 1 clinical data evaluating the potential anti-cancer activity of the cyclin dependent kinase 9 (CDK9) inhibitor oral TP-1287, the WT1 immunotherapeutic cancer vaccine DSP-7888 plus nivolumab (NIV) or pembrolizumab (PEM), and the activin receptor-like kinase-2 (ALK2) inhibitor oral TP-0184.

"The data emphasize our commitment to, and the progress being made in advancing our pipeline to discover novel approaches to address unmet needs in the oncology space," said Patricia S. Andrews, CEO and Global Head of Oncology, SMP Oncology. "These trials represent a significant step forward for patients as we continue toward advancing purposeful research and drug development in oncology."

Below are the details for the presentations:

Abstract Title

Details

Presenter/Authors

CT191 / 16 – Phase 1, first-in-human, dose-escalation study of oral TP-1287, a cyclin dependent kinase 9 (CDK9) inhibitor, in patients (pts) with advanced solid tumors (ASTs)

Abstract

Wednesday April 12, 2022, 9:00AM – 12:30PM

Session PO.CT01.02 – Phase I Clinical Trials 2

Nicholas J. Vogelzang, Ben George, Nissa Ashenbramer, William J. Edenfield, Donald Richards, Mitchell E. Gross, Gil D. Fine, Pablo Martinez. Comprehensive Cancer Centers of Nevada, Las Vegas, NV, LaBahn Pancreatic Cancer Program, Departments of Medicine-Hematology/ Oncology, Medical College of Wisconsin, Milwaukee, WI, Sumitomo Pharma Oncology, Inc., Cambridge, MA, Greenville Health System Cancer Institute, Greenville, SC, Department of Oncology, US Oncology Research, Texas Oncology-Tyler, Tyler, TX, University of Southern California, Keck School of Medicine, Lawrence J. Ellison Institute for Transformative Medicine, Los Angeles, CA

Preliminary safety and efficacy of DSP-7888 plus nivolumab (NIV) or pembrolizumab (PEM) in patients (pts) with advanced solid tumors (ASTs): a phase (Ph) 1b/2 open-label study

Abstract

Monday, April 11, 2022, 1:30PM – 5:00PM

Session PO.CT01.01 – Phase I Clinical Trials 1

Wael A. Harb, Makoto Origuchi, Patrick W. Cobb, Trisha Wise-Draper, Natsuko Suginobe, Megumi Nakamura, Masashi Goto, Aaron Chen, Jian Li, James L. Wade III. Syneos Health, Morrisville, NC, Horizon Oncology Center, Lafayette, IN, Sumitomo Pharma Oncology, Inc., Cambridge, MA, St. Vincent Frontier Cancer Center, Billings, MT, Department of Internal Medicine, Division of Hematology/Oncology, University of Cincinnati, Cincinnati, OH, Sumitomo Pharma Co., Ltd., Osaka, Japan, Cancer Care Specialists of Illinois, Decatur, IL

CT134 / 1 – Phase 1, first-in-human, dose-escalation, safety, pharmacokinetic (PK), and pharmacodynamic study of oral TP-0184, an activin receptor-like kinase-2 (ALK2) inhibitor, in patients (pts) with advanced solid tumors (ASTs)

Abstract

Tuesday April 11, 2022, 1:30PM – 5:00PM

Session PO.CT01.01 – Phase I Clinical Trials 1

Joaquina Baranda, Michael S. Gordon, Aparna R. Parikh, Huyuan Yang, Gregory K. Pennock, Philip Komarnitsky, Muhammad S. Beg. Division of Medical Oncology, Department of Medicine, University of Kansas Cancer Center, Westwood, KS, HonorHealth Research Institute, Scottsdale, AZ, Massachusetts General Hospital Cancer Center and Department of Medicine, Harvard Medical School, Boston, MA, Sumitomo Pharma Oncology, Inc., Cambridge, MA, The University of Texas Southwestern Medical Center, Dallas, TX

Additionally, at AACR (Free AACR Whitepaper) SMP Oncology will present preclinical data on TP-1287 in sarcomas in a poster.

Below are the details for the poster:

Poster Title

Details

Presenter/Authors

CDK9 as a potential therapeutic target in sarcomas

Poster:

Wednesday April 12, 2022, 9:00AM – 12:30PM

Session PO.MCB06.01 – Cell Cycle Control and Cell Cycle Regulators as Therapeutic Targets

Yuta Matsumura, Hiroki Umehara, Jun Oishi, Adam Siddiqui, Jason M. Foulks, Setsuko Yamamoto, Steven L. Warner. Sumitomo Pharma Oncology, Inc., Lehi, UT, Sumitomo Pharma Co., Ltd., Osaka, Japan

About TP-1287
TP-1287 is an investigational oral CDK9 inhibitor that has shown favorable oral bioavailability in preclinical models. TP-1287 is enzymatically cleaved, yielding the active moiety, a potent inhibitor of CDK9.1 Inhibiting CDK9 is thought to downregulate the transcription of target genes, including MCL-1, reducing leukemic blast viability in MCL-1–dependent hematologic malignancies, and c-MYC, an important oncogene across multiple tumor types.2, 3, 4 TP-1287 is in a Phase 1 first-in-human study of oral TP-1287 in patients with advanced solid tumors (NCT03604783).

About DSP-7888
Ombipepimut-S Emulsion (DSP-7888) is an investigational immunotherapeutic cancer vaccine containing 2 peptides that induce WT1-specific cytotoxic T lymphocytes (WT1-CTLs) and helper T cells to attack WT1-expressing cancerous cells found in various types of hematologic malignancies and solid tumors.5, 6 Researchers have identified that adding helper T-cell–inducing peptides improved WT1-specific CTL induction, which may contribute to tumor cytotoxicity.5 Ombipepimut-S Emulsion is in a Phase 1/2 study with immune checkpoint inhibitors in adult patients with advanced solid tumors (NCT03311334).

About TP-0184
TP-0184 is an investigational inhibitor of activin receptor-like kinase 2 (ALK2) and ALK5 (also known as TGFβR1). This bimodal inhibitor is believed to downregulate multiple TGF-β superfamily signaling pathways, enabling hematopoietic regulation in myelodysplastic syndrome (MDS) through hepcidin decreases, bioavailable iron increases, and hemoglobin restoration, as well as antitumor activity in several cancers.7, 8, 9 TP-0184 is in two clinical trials; A Phase 1/2 study to treat anemia in adults with IPSS-R low or intermediate risk MDS (NCT04623996); A first-in-human study of oral TP-0184 in patients with advanced solid tumors (NCT03429218).