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SUMO化与去SUMO化:癌症中的潜在治疗靶点

SUMOylation and DeSUMOylation: Prospective therapeutic targets in cancer.

作者信息

Wu Wenyan, Huang Chao

机构信息

Kunming University of Science and Technology, Medical School, Kunming 650500, China.

Kunming University of Science and Technology, Medical School, Kunming 650500, China.

出版信息

Life Sci. 2023 Nov 1;332:122085. doi: 10.1016/j.lfs.2023.122085. Epub 2023 Sep 16.

Abstract

The SUMO family is a type of ubiquitin-like protein modification molecule. Its protein modification mechanism is similar to that of ubiquitination: both involve modifier-activating enzyme E1, conjugating enzyme E2 and substrate-specific ligase E3. However, polyubiquitination can lead to the degradation of substrate proteins, while poly-SUMOylation only leads to the degradation of substrate proteins through the proteasome pathway after being recognized by ubiquitin as a signal factor. There are currently five reported subtypes in the SUMO family, namely SUMO1-5. As a reversible dynamic modification, intracellular sentrin/SUMO-specific proteases (SENPs) mainly regulate the reverse reaction pathway of SUMOylation. The SUMOylation modification system affects the localization, activation and turnover of proteins in cells and participates in regulating most nuclear and extranuclear molecular reactions. Abnormal expression of proteins related to the SUMOylation pathway is commonly observed in tumors, indicating that this pathway is closely related to tumor occurrence, metastasis and invasion. This review mainly discusses the composition of members in the protein family related to SUMOylation pathways, mutual connections between SUMOylation and other post-translational modifications on proteins as well as therapeutic drugs developed based on these pathways.

摘要

SUMO家族是一类类泛素蛋白修饰分子。其蛋白质修饰机制与泛素化相似:二者均涉及修饰激活酶E1、结合酶E2和底物特异性连接酶E3。然而,多聚泛素化可导致底物蛋白降解,而多聚SUMO化只有在被泛素识别为信号因子后,才会通过蛋白酶体途径导致底物蛋白降解。目前SUMO家族已报道有五个亚型,即SUMO1 - 5。作为一种可逆的动态修饰,细胞内的sentrin/SUMO特异性蛋白酶(SENPs)主要调节SUMO化的逆反应途径。SUMO化修饰系统影响细胞内蛋白质的定位、激活和周转,并参与调控大多数核内和核外分子反应。在肿瘤中常观察到与SUMO化途径相关的蛋白质表达异常,这表明该途径与肿瘤的发生、转移和侵袭密切相关。本文综述主要探讨了与SUMO化途径相关的蛋白质家族成员组成、SUMO化与蛋白质上其他翻译后修饰之间的相互联系以及基于这些途径开发的治疗药物。

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