Department of Pharmaceutical Chemistry, University of California, San Francisco, 600 16th Street, San Francisco, California 94143, United States.
School of Pharmaceutical Sciences, Tsinghua University, Beijing 100084, China.
J Am Chem Soc. 2023 May 10;145(18):10015-10021. doi: 10.1021/jacs.2c12240. Epub 2023 Apr 27.
Caspases are a family of cysteine-dependent proteases with important cellular functions in inflammation and apoptosis, while also implicated in human diseases. Classical chemical tools to study caspase functions lack selectivity for specific caspase family members due to highly conserved active sites and catalytic machinery. To overcome this limitation, we targeted a non-catalytic cysteine residue (C264) unique to caspase-6 (C6), an enigmatic and understudied caspase isoform. Starting from disulfide ligands identified in a cysteine trapping screen, we used a structure-informed covalent ligand design to produce potent, irreversible inhibitors () and chemoproteomic probes () of C6 that exhibit unprecedented selectivity over other caspase family members and high proteome selectivity. This approach and the new tools described will enable rigorous interrogation of the role of caspase-6 in developmental biology and in inflammatory and neurodegenerative diseases.
半胱天冬酶是一类半胱氨酸依赖性蛋白酶家族,在炎症和细胞凋亡中具有重要的细胞功能,同时也与人类疾病有关。由于活性位点和催化机制高度保守,用于研究半胱天冬酶功能的经典化学工具缺乏对特定半胱天冬酶家族成员的选择性。为了克服这一限制,我们针对半胱天冬酶-6(C6)特有的一个非催化半胱氨酸残基(C264),半胱天冬酶-6 是一种神秘且研究不足的半胱天冬酶同工型。从半胱氨酸捕获筛选中鉴定出的二硫键配体出发,我们使用结构导向的共价配体设计,产生了强效、不可逆的 C6 抑制剂()和化学蛋白质组学探针(),与其他半胱天冬酶家族成员相比,它们表现出前所未有的选择性和高蛋白质组选择性。这种方法和所描述的新工具将能够严格研究半胱天冬酶-6 在发育生物学以及炎症和神经退行性疾病中的作用。
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