Abstract 1131: ORIC-944, a potent and selective allosteric PRC2 inhibitor, demonstrates robust <i>in vivo</i> activity in prostate cancer models

Daemen, Anneleen; Sun, Jessica; Pankov, Aleksandr; Duong, Frank; Yuen, Natalie; Barkund, Shravani; Kaushik, Shelly; Chang, Jae Hoon; Briere, David; Sudhakar, Niranjan; Calinisan, Andrew; Burns, Aaron C.; Ketcham, John M.; Marx, Matthew A.; Olson, Peter; Christensen, James G.; Junttila, Melissa R.; Friedman, Lori S.

doi:10.1158/1538-7445.am2021-1131

Cited by 3 publications

(1 citation statement)

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“…EZH1, a paralog of EZH2, can also form functional PRC2 complexes as a compensatory mechanism for tumor cells to escape EZH2 inhibition. 490,491 Therefore, co-inhibition of EZH2 and EZH1 [492][493][494] or EED inhibition 492,495 could more completely inhibit the activity of PRC2, especially in the presence of innate or acquired resistance mutations in EZH2 and by addressing the potential compensatory mechanism of EZH1-driven tumor growth. SETD2, an upstream regulator of EZH2, can also be targeted to combat EZH2-high tumors.…”

Section: The Mammalian Bromodomain and Extra-terminal Family Proteins...mentioning

confidence: 99%

Development of pharmacological immunoregulatory anti-cancer therapeutics: current mechanistic studies and clinical opportunities

Yin,

Li,

Zhang

et al. 2024

Sig Transduct Target Ther

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Immunotherapy represented by anti-PD-(L)1 and anti-CTLA-4 inhibitors has revolutionized cancer treatment, but challenges related to resistance and toxicity still remain. Due to the advancement of immuno-oncology, an increasing number of novel immunoregulatory targets and mechanisms are being revealed, with relevant therapies promising to improve clinical immunotherapy in the foreseeable future. Therefore, comprehending the larger picture is important. In this review, we analyze and summarize the current landscape of preclinical and translational mechanistic research, drug development, and clinical trials that brought about next-generation pharmacological immunoregulatory anti-cancer agents and drug candidates beyond classical immune checkpoint inhibitors. Along with further clarification of cancer immunobiology and advances in antibody engineering, agents targeting additional inhibitory immune checkpoints, including LAG-3, TIM-3, TIGIT, CD47, and B7 family members are becoming an important part of cancer immunotherapy research and discovery, as are structurally and functionally optimized novel anti-PD-(L)1 and anti-CTLA-4 agents and agonists of co-stimulatory molecules of T cells. Exemplified by bispecific T cell engagers, newly emerging bi-specific and multi-specific antibodies targeting immunoregulatory molecules can provide considerable clinical benefits. Next-generation agents also include immune epigenetic drugs and cytokine-based therapeutics. Cell therapies, cancer vaccines, and oncolytic viruses are not covered in this review. This comprehensive review might aid in further development and the fastest possible clinical adoption of effective immuno-oncology modalities for the benefit of patients.

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Section: The Mammalian Bromodomain and Extra-terminal Family Proteins...mentioning

confidence: 99%

Development of pharmacological immunoregulatory anti-cancer therapeutics: current mechanistic studies and clinical opportunities

Yin,

Li,

Zhang

et al. 2024

Sig Transduct Target Ther

View full text Add to dashboard Cite

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Stereoselective Amine Synthesis Mediated by a Zirconocene Hydride to Accelerate a Drug Discovery Program

Aloiau,

Bobek,

Caddell Haatveit

et al. 2024

J. Org. Chem.

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Chiral amine synthesis remains a significant challenge in accelerating the design cycle of drug discovery programs. A zirconium hydride, due to its high oxophilicity and lower reactivity, gave highly chemo-and stereoselective reductions of sulfinyl ketimines. The development of this zirconocene-mediated reduction helped to accelerate our drug discovery efforts and is applicable to several motifs commonly used in medicinal chemistry. Computational investigation supported a cyclic half-chair transition state to rationalize the high selectivity in benzyl systems.

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Zirconium Hydride Catalysis Initiated by Tetrabutylammonium Fluoride

Aloiau,

Bobek,

Pearson

et al. 2024

J. Org. Chem.

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In our drug discovery campaigns to target the oncogenic drivers of cancers, the demand for a chemoselective, stereoselective and economical synthesis of chiral benzylamines drove the development of a catalytic zirconium hydride reduction. This methodology uses the inexpensive, bench stable zirconocene dichloride, and a novel tetrabutylammonium fluoride activation tactic to catalytically generate a metal hydride under ambient conditions. The diastereo-and chemoselectivity of this reaction was tested with the preparation of key intermediates from our discovery programs and in the scope of sulfinyl ketimines and carbonyls relevant to medicinal chemistry and natural product synthesis. A preliminary mechanistic investigation conducted into the role of tetrabutylammonium fluoride indicates that formation of a zirconocene fluoride occurs to initiate catalysis. The implications of this convenient activation approach may provide expanded roles for zirconium hydrides in catalytic transformations.

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Abstract 1131: ORIC-944, a potent and selective allosteric PRC2 inhibitor, demonstrates robust in vivo activity in prostate cancer models

Cited by 3 publications

References 0 publications

Development of pharmacological immunoregulatory anti-cancer therapeutics: current mechanistic studies and clinical opportunities

Development of pharmacological immunoregulatory anti-cancer therapeutics: current mechanistic studies and clinical opportunities

Stereoselective Amine Synthesis Mediated by a Zirconocene Hydride to Accelerate a Drug Discovery Program

Zirconium Hydride Catalysis Initiated by Tetrabutylammonium Fluoride

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