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小泛素样修饰(SUMOylation)调控E6-AP羧基末端同源物(HECT)泛素连接酶Rsp5p。

SUMOylation regulates the homologous to E6-AP carboxyl terminus (HECT) ubiquitin ligase Rsp5p.

机构信息

School of Biological and Chemical Sciences, Queen Mary University of London, Mile End Road, London E1 4NS, United Kingdom.

出版信息

J Biol Chem. 2013 Apr 12;288(15):10308-17. doi: 10.1074/jbc.M112.424234. Epub 2013 Feb 26.

Abstract

The post-translational modifiers ubiquitin and small ubiquitin-related modifier (SUMO) regulate numerous critical signaling pathways and are key to controlling the cellular fate of proteins in eukaryotes. The attachment of ubiquitin and SUMO involves distinct, but related, machinery. However, it is now apparent that many substrates can be modified by both ubiquitin and SUMO and that some regulatory interaction takes place between the respective attachment machinery. Here, we demonstrate that the Saccharomyces cerevisiae ubiquitin ligase Rsp5p, a member of the highly conserved Nedd4 family of ubiquitin ligases, is SUMOylated in vivo. We further show that Rsp5p SUMOylation is mediated by the SUMO ligases Siz1p and Siz2p, members of the conserved family of PIAS SUMO ligases that are, in turn, substrates for Rsp5p-mediated ubiquitylation. Our experiments show that SUMOylated Rsp5p has reduced ubiquitin ligase activity, and similarly, ubiquitylated Siz1p demonstrates reduced SUMO ligase activity leading to respective changes in both ubiquitin-mediated sorting of the manganese transporter Smf1p and polySUMO chain formation. This reciprocal regulation of these highly conserved ligases represents an exciting and previously unidentified system of cross talk between the ubiquitin and SUMO systems.

摘要

翻译后修饰物泛素和小泛素相关修饰物(SUMO)调节众多关键信号通路,是真核生物中控制蛋白质细胞命运的关键。泛素和SUMO的附着涉及不同但相关的机制。然而,现在很明显,许多底物可以同时被泛素和SUMO修饰,并且在各自的附着机制之间发生了一些调节相互作用。在这里,我们证明酿酒酵母泛素连接酶Rsp5p,一种高度保守的泛素连接酶Nedd4家族的成员,在体内被SUMO化。我们进一步表明,Rsp5p的SUMO化由SUMO连接酶Siz1p和Siz2p介导,它们是保守的PIAS SUMO连接酶家族的成员,而PIAS SUMO连接酶家族又是Rsp5p介导的泛素化的底物。我们的实验表明,SUMO化的Rsp5p具有降低的泛素连接酶活性,同样,泛素化的Siz1p表现出降低的SUMO连接酶活性,导致锰转运蛋白Smf1p的泛素介导的分选和多聚SUMO链形成各自发生变化。这些高度保守的连接酶的这种相互调节代表了泛素和SUMO系统之间一个令人兴奋且以前未被识别的串扰系统。

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