Huang Guang, Stevens Rhiannon, Hucek Devon G, Purohit Trupta, Li Shuangjiang, Miao Hongzhi, Trost Elise, Hewett Geoff, Clegg Bradley, Park Se Ra, Rajanayake Krishani, Wen Bo, Sun Duxin, Cierpicki Tomasz, Grembecka Jolanta
Department of Pathology, University of Michigan, Ann Arbor, Michigan 48109, United States.
College of Pharmacy, University of Michigan, Ann Arbor, Michigan 48109, United States.
J Med Chem. 2025 Jan 9;68(1):174-195. doi: 10.1021/acs.jmedchem.4c01673. Epub 2024 Dec 16.
The absent, small, or homeotic-like 1 (ASH1L) protein is a histone lysine methyltransferase that plays a crucial role in various cancers, including leukemia. Despite representing an attractive therapeutic target, only one class of ASH1L inhibitors was identified to date. Herein, we report development of advanced ASH1L inhibitors targeting the catalytic SET domain, which were designed to access previously unexplored binding pocket on ASH1L. Extensive medicinal chemistry combined with structure-based design led to identification of (), a highly potent and selective ASH1L inhibitor (IC = 94 nM), representing substantially improved inhibitory activity over previously reported compounds targeting ASH1L. Furthermore, effectively blocked cell proliferation and induced apoptosis and differentiation in leukemia cells harboring translocations. Overall, this work provides a high-quality chemical probe targeting the catalytic SET domain of ASH1L with increased inhibitory activity and cellular efficacy to study biological functions of ASH1L and potentially to develop novel anticancer therapeutics.
缺失、微小或类同源异型1(ASH1L)蛋白是一种组蛋白赖氨酸甲基转移酶,在包括白血病在内的多种癌症中发挥关键作用。尽管它是一个有吸引力的治疗靶点,但迄今为止仅鉴定出一类ASH1L抑制剂。在此,我们报告了靶向催化SET结构域的新型ASH1L抑制剂的研发情况,这些抑制剂旨在进入ASH1L上以前未被探索的结合口袋。广泛的药物化学研究与基于结构的设计相结合,导致鉴定出(),一种高效且选择性的ASH1L抑制剂(IC = 94 nM),与先前报道的靶向ASH1L的化合物相比,其抑制活性有显著提高。此外,()有效阻断了携带易位的白血病细胞的增殖,并诱导了其凋亡和分化。总体而言,这项工作提供了一种高质量的化学探针,靶向ASH1L的催化SET结构域,具有增强的抑制活性和细胞效力,可用于研究ASH1L的生物学功能,并有可能开发新型抗癌疗法。
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