通过PROTAC策略同时抑制SIRT2去乙酰化酶和去脂肪酰化酶活性
Simultaneous Inhibition of SIRT2 Deacetylase and Defatty-Acylase Activities via a PROTAC Strategy.
作者信息
Hong Jun Young, Jing Hui, Price Ian Robert, Cao Ji, Bai Jessica Jingyi, Lin Hening
机构信息
Department of Chemistry and Chemical Biology, Cornell University, Ithaca, New York 14853, United States.
Howard Hughes Medical Institute, Department of Chemistry and Chemical Biology, Cornell University, Ithaca, New York 14853, United States.
出版信息
ACS Med Chem Lett. 2020 Sep 21;11(11):2305-2311. doi: 10.1021/acsmedchemlett.0c00423. eCollection 2020 Nov 12.
Abstract
As a member of the sirtuin family of enzymes, SIRT2 promotes tumor growth and regulates various biological pathways through lysine deacetylation and defatty-acylation. In the past few years, many SIRT2-selective small molecule inhibitors have been developed, but none have demonstrated simultaneous inhibition of both SIRT2 activities in cells. To further scrutinize the physiological importance and significance of SIRT2 deacetylase and defatty-acylase activities, small molecules that can selectively inhibit both activities of SIRT2 in living cells are needed. Here, we have applied the Proteolysis Targeting Chimera (PROTAC) strategy and synthesized a new SIRT2 inhibitor (TM-P4-Thal) to degrade SIRT2 selectively, which led to simultaneous inhibition of its deacetylase and defatty-acylase activities in living cells. Additionally, this compound exemplifies the advantage of the PROTAC strategy that allows complete eradication of an enzyme and its activity in biological settings.
摘要
作为酶的沉默调节蛋白家族的一员,SIRT2通过赖氨酸去乙酰化和去脂肪酰化促进肿瘤生长并调节各种生物途径。在过去几年中,已经开发了许多SIRT2选择性小分子抑制剂,但没有一种能在细胞中同时抑制SIRT2的两种活性。为了进一步研究SIRT2去乙酰化酶和去脂肪酰化酶活性的生理重要性和意义,需要能够在活细胞中选择性抑制SIRT2两种活性的小分子。在这里,我们应用了蛋白酶靶向嵌合体(PROTAC)策略,合成了一种新的SIRT2抑制剂(TM-P4-Thal)以选择性降解SIRT2,这导致其在活细胞中的去乙酰化酶和去脂肪酰化酶活性同时受到抑制。此外,该化合物体现了PROTAC策略的优势,即能够在生物环境中完全消除一种酶及其活性。
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