细胞周期蛋白依赖性激酶2(CDK2)选择性叔酰胺抑制剂的发现。
Discovery of Selective Tertiary Amide Inhibitors of Cyclin-Dependent Kinase 2 (CDK2).
作者信息
Zeng Mingshuo, Grandner Jessica M, Bryan Marian C, Verma Vishal, Larouche-Gauthier Robin, Leclerc Jean-Philippe, Zhao Liang, Haghshenas Pouyan, Aubert-Nicol Samuel, Yadav Arun, Ashley Melissa, Chen Jacob Z, Durk Matthew, Samy Karen E, Nespi Marika, Levy Elizabeth, Merrick Karl, Moffat John G, Murray Jeremy, Oh Angela, Orr Christine, Segal Ehud, Sims Jessica, Sneeringer Christopher, Prangley Madeleine, Vartanian Steffan, Magnuson Steven, Parr Brendan T
机构信息
Genentech Inc., South San Francisco, California 94080, United States.
Janssen R&D, 1400 McKean Rd, Spring House, Pennsylvania 19002, United States.
出版信息
ACS Med Chem Lett. 2023 Aug 24;14(9):1179-1187. doi: 10.1021/acsmedchemlett.3c00142. eCollection 2023 Sep 14.
Cyclin-dependent kinases (CDKs) are key regulators of the cell cycle and are frequently altered in cancer cells, thereby leading to uncontrolled proliferation. In this context, CDK2 has emerged as an appealing target for anticancer drug development. Herein, we describe the discovery of a series of selective small molecule inhibitors of CDK2 beginning with historical compounds from our ERK2 program (e.g., compound ). Structure-based drug design led to the potent and selective tool compound , where excellent selectivity against ERK2 and CDK4 was achieved by filling the lipophilic DFG-1 pocket and targeting interactions with CDK2-specific lower hinge binding residues, respectively. Compound demonstrated 112% tumor growth inhibition in mice bearing OVCAR3 tumors with 50 mg/kg (BID) oral dosing.
细胞周期蛋白依赖性激酶(CDKs)是细胞周期的关键调节因子,在癌细胞中经常发生改变,从而导致不受控制的增殖。在这种情况下,CDK2已成为抗癌药物开发的一个有吸引力的靶点。在此,我们描述了一系列CDK2选择性小分子抑制剂的发现,这些抑制剂始于我们ERK2项目中的历史化合物(例如化合物 )。基于结构的药物设计产生了强效且选择性的工具化合物 ,通过填充亲脂性DFG-1口袋和分别靶向与CDK2特异性下铰链结合残基的相互作用,实现了对ERK2和CDK4的优异选择性。化合物 在以50 mg/kg(每日两次)口服给药的携带OVCAR3肿瘤的小鼠中显示出112%的肿瘤生长抑制率。
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