Keller Patricia J, Adams Elizabeth J, Wu Rentian, Côté Alexandre, Arora Shilpi, Cantone Nico, Meyer Rosana, Mertz Jennifer A, Gehling Victor, Cui Jike, Stuckey Jacob I, Khanna Avinash, Zhao Feng, Chen Zehua, Yu Ziyang, Cummings Richard T, Taimi Mohammed, Lakhani Nehal J, Rasco Drew, Gutierrez Martin, Duska Linda, Devitt Michael, Rippley Ronda, Levell Julian, Truong Jennifer, Wang Jing, Sun Kaiming, Trojer Patrick
Constellation Pharmaceuticals, A MorphoSys Company, Boston, Massachusetts.
START Midwest, Grand Rapids, Michigan.
Cancer Res. 2024 Aug 1;84(15):2501-2517. doi: 10.1158/0008-5472.CAN-24-0398.
Recurrent somatic mutations in the BRG1/BRM-associated factor (BAF) chromatin remodeling complex subunit ARID1A occur frequently in advanced urothelial, endometrial, and ovarian clear cell carcinomas, creating an alternative chromatin state that may be exploited therapeutically. The histone methyltransferase EZH2 has been previously identified as targetable vulnerability in the context of ARID1A mutations. In this study, we describe the discovery of tulmimetostat, an orally available, clinical stage EZH2 inhibitor, and it elucidates the aspects of its application potential in ARID1A mutant tumors. Tulmimetostat administration achieved efficacy in multiple ARID1A mutant bladder, ovarian, and endometrial tumor models and improved cisplatin response in chemotherapy-resistant models. Consistent with its comprehensive and durable level of target coverage, tulmimetostat demonstrated greater efficacy than other PRC2-targeted inhibitors at comparable or lower exposures in a bladder cancer xenograft mouse model. Tulmimetostat mediated extensive changes in gene expression, in addition to a profound reduction in global H3K27me3 levels in tumors. Phase I clinical pharmacokinetic and pharmacodynamic data indicated that tulmimetostat exhibits durable exposure and profound target engagement. Importantly, a tulmimetostat controlled gene expression signature identified in whole blood from a cohort of 32 patients with cancer correlated with tulmimetostat exposure, representing a pharmacodynamic marker for the assessment of target coverage for PRC2-targeted agents in the clinic. Collectively, these data suggest that tulmimetostat has the potential to achieve clinical benefit in solid tumors as a monotherapy but also in combination with chemotherapeutic agents, and may be beneficial in various indications with recurrent ARID1A mutations. Significance: The EZH2 inhibitor tulmimetostat achieves comprehensive target inhibition in ARID1A mutant solid tumor models and cancer patients that can be assessed with a pharmacodynamic gene signature in peripheral blood.
BRG1/BRM相关因子(BAF)染色质重塑复合体亚基ARID1A中的复发性体细胞突变在晚期尿路上皮癌、子宫内膜癌和卵巢透明细胞癌中频繁发生,产生了一种可能具有治疗价值的替代染色质状态。组蛋白甲基转移酶EZH2此前已被确定为ARID1A突变背景下的可靶向弱点。在本研究中,我们描述了可口服的临床阶段EZH2抑制剂图米司他的发现,并阐明了其在ARID1A突变肿瘤中的应用潜力。给予图米司他在多个ARID1A突变的膀胱、卵巢和子宫内膜肿瘤模型中取得了疗效,并改善了化疗耐药模型中对顺铂的反应。与其全面且持久的靶点覆盖水平一致,在膀胱癌异种移植小鼠模型中,图米司他在相当或更低的暴露水平下比其他PRC2靶向抑制剂表现出更高的疗效。图米司他除了使肿瘤中整体H3K27me3水平大幅降低外,还介导了基因表达的广泛变化。I期临床药代动力学和药效学数据表明,图米司他具有持久的暴露和深度的靶点结合。重要的是,在32名癌症患者队列的全血中鉴定出的图米司他控制的基因表达特征与图米司他暴露相关,代表了一种药效学标志物,可用于评估临床中PRC2靶向药物的靶点覆盖情况。总体而言,这些数据表明,图米司他作为单一疗法或与化疗药物联合使用在实体瘤中具有实现临床获益的潜力,并且可能对各种具有复发性ARID1A突变的适应症有益。意义:EZH2抑制剂图米司他在ARID1A突变的实体瘤模型和癌症患者中实现了全面的靶点抑制,可通过外周血中的药效学基因特征进行评估。
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