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Cytokine-Regulated Protein Degradation by the Ubiquitination System

机译:泛素化系统对细胞因子调节的蛋白质降解

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摘要

The ubiquitin-mediated protein degradation pathway exerts a wide spectrum of effects and modulates a variety of biological processes including cell cycle progression,transcriptional regulation,signal transduction,antigen presentation,apoptosis (or programmed cell death),oncogenesis,preimplantation,and DNA repair.Recently,the importance of deubiquitination mechanism has been emerged as an essential regulatory step to control these cellular mechanisms for homeostasis.Even though a number of deubiquitinating enzymes have recently been isolated,relatively little is known about their substrates and biological functions.Identified from yeast to human,deubiquitinating (DUB) enzymes are classified into the ubiquitin C-terminal hydrolase (UCH),the ubiquitin-specific processing proteases (UBP or USP),Jab1/Pad1/MPN domain containing metallo-enzymes (JAMM),Otu domain ubiquitin-aldehyde binding proteins (OTU),and Ataxin-3/Josephin domain containing proteins (Ataxin-3/Josephin).Several members of a novel DUB subfamily induced by cytokines in murine lymphocytes have recently been identified.In addition,human DUB enzyme DUB-3,highly homologous to USP17 and induced by cytokines interleukin (IL)-4 and IL-6,has been recently isolated and showed that it has significant homology to the known murine DUB subfamily members.Interestingly,both murine DVB and human USP17 subfamily members are localized and clustered on murine chromosome 7 and on human chromosomes 4 and 8,respectively.This review introduces the reader to provide a great understanding of cytokine-inducible DUB enzymes in both mouse and human,and new insights into DUB subfamily members.
机译:泛素介导的蛋白质降解途径发挥广泛的作用,并调节多种生物学过程,包括细胞周期进程,转录调节,信号转导,抗原呈递,细胞凋亡(或程序性细胞死亡),肿瘤发生,植入前和DNA修复。近年来,去泛素化机制的重要性已成为控制这些稳态机制的必不可少的调节步骤。即使最近已分离出多种去泛素化酶,对其底物和生物学功能的了解也相对较少。人类去泛素化(DUB)酶分为泛素C末端水解酶(UCH),泛素特异性加工蛋白酶(UBP或USP),包含金属酶的Jab1 / Pad1 / MPN域(JAMM),Otu域泛素-醛结合蛋白(OTU)和含有Ataxin-3 / Josephin结构域的蛋白质(Ataxin-3 / Josephin)。最近已经确定了由小鼠淋巴细胞中的细胞因子诱导的新型DUB亚家族。此外,最近已分离出与USP17高度同源并由细胞因子白介素(IL)-4和IL-6诱导的人DUB酶DUB-3。有趣的是,鼠DVB和人类USP17亚家族成员分别定位并聚集在鼠染色体7和人染色体4和8上。和小鼠中人细胞因子诱导的DUB酶的研究,以及对DUB亚家族成员的新见解。

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