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使用亚砷酸弹头对丙酮酸激酶M2进行选择性共价靶向

Selective Covalent Targeting of Pyruvate Kinase M2 Using Arsenous Warheads.

作者信息

Wang Jingyao, Zhou Shaoqing, Cheng Yan, Cheng Lin, Qin Ying, Zhang Zhenfeng, Bi Aiwei, Xiang Huaijiang, He Xinheng, Tian Xiaoxu, Liu Wenbin, Zhang Jian, Peng Chao, Zhu Zhengjiang, Huang Min, Li Ying, Zhuang Guanglei, Tan Li

机构信息

Interdisciplinary Research Center on Biology and Chemistry, Shanghai Institute of Organic Chemistry, Chinese Academy of Sciences, Shanghai 201210, China.

University of Chinese Academy of Sciences, Beijing 100049, China.

出版信息

J Med Chem. 2023 Feb 23;66(4):2608-2621. doi: 10.1021/acs.jmedchem.2c01563. Epub 2023 Feb 1.

Abstract

There is growing interest in covalent targeted inhibitors in drug discovery against previously "undruggable" sites and targets. These molecules typically feature an electrophilic warhead that reacts with nucleophilic groups of protein residues, most notably the thiol group of cysteines. One main challenge in the field is to develop versatile utilizable warheads. Here, we characterize the unique features of novel arsenous warheads for reaction with thiol species in a reversible manner and further demonstrate that organoarsenic probes can be chemically tuned toward specific molecular targets by developing selective and potent inhibitors of pyruvate kinase M2 (PKM2). We show that compound is a covalent and allosteric inhibitor of PKM2 and its orally bioavailable prodrug exerts efficacious inhibition of PKM2-dependent tumor growth and . Our results introduce and its derivatives as useful pharmacological tools and provide a general road map for targeting the protein cysteinome using arsenous warheads.

摘要

在药物研发中,针对先前“不可成药”的位点和靶点的共价靶向抑制剂正引起越来越多的关注。这些分子通常具有一个亲电弹头,它能与蛋白质残基的亲核基团发生反应,最显著的是半胱氨酸的巯基。该领域的一个主要挑战是开发通用的可利用弹头。在此,我们描述了新型亚砷酸弹头以可逆方式与硫醇类物质反应的独特特征,并进一步证明通过开发丙酮酸激酶M2(PKM2)的选择性强效抑制剂,有机砷探针可针对特定分子靶点进行化学调控。我们表明化合物是PKM2的共价变构抑制剂,其口服生物利用度高的前药对PKM2依赖的肿瘤生长和有有效的抑制作用。我们的结果引入了及其衍生物作为有用的药理学工具,并为使用亚砷酸弹头靶向蛋白质半胱氨酸组提供了一个通用路线图。

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