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多聚小泛素样修饰物缀合物对Slx5-Slx8泛素连接酶的激活作用。

Activation of the Slx5-Slx8 ubiquitin ligase by poly-small ubiquitin-like modifier conjugates.

作者信息

Mullen Janet R, Brill Steven J

机构信息

Department of Molecular Biology and Biochemistry, Rutgers University, Piscataway, NJ 08854, USA.

出版信息

J Biol Chem. 2008 Jul 18;283(29):19912-21. doi: 10.1074/jbc.M802690200. Epub 2008 May 22.

Abstract

Protein sumoylation is a regulated process that is important for the health of human and yeast cells. In budding yeast, a subset of sumoylated proteins is targeted for ubiquitination by a conserved heterodimeric ubiquitin (Ub) ligase, Slx5-Slx8, which is needed to suppress the accumulation of high molecular weight small ubiquitin-like modifier (SUMO) conjugates. Structure-function analysis indicates that the Slx5-Slx8 complex contains multiple SUMO-binding domains that are collectively required for in vivo function. To determine the specificity of Slx5-Slx8, we assayed its Ub ligase activity using sumoylated Siz2 as an in vitro substrate. In contrast to unsumoylated or multisumoylated Siz2, substrates containing poly-SUMO conjugates were efficiently ubiquitinated by Slx5-Slx8. Although Siz2 itself was ubiquitinated, the bulk of the Ub was conjugated to SUMO residues. Slx5-Slx8 primarily mono-ubiquitinated the N-terminal SUMO moiety of the chain. These data indicate that the Slx5-Slx8 Ub ligase is stimulated by poly-SUMO conjugates and that it can ubiquitinate a poly-SUMO chain.

摘要

蛋白质SUMO化是一个受调控的过程,对人类和酵母细胞的健康至关重要。在芽殖酵母中,一部分SUMO化蛋白会被一种保守的异二聚体泛素(Ub)连接酶Slx5-Slx8靶向进行泛素化,该连接酶是抑制高分子量小泛素样修饰物(SUMO)缀合物积累所必需的。结构-功能分析表明,Slx5-Slx8复合物包含多个SUMO结合结构域,这些结构域共同对体内功能是必需的。为了确定Slx5-Slx8的特异性,我们使用SUMO化的Siz2作为体外底物检测其Ub连接酶活性。与未SUMO化或多SUMO化的Siz2不同,含有多聚SUMO缀合物的底物被Slx5-Slx8有效地泛素化。尽管Siz2本身被泛素化,但大部分Ub与SUMO残基缀合。Slx5-Slx8主要对链的N端SUMO部分进行单泛素化。这些数据表明,Slx5-Slx8 Ub连接酶受到多聚SUMO缀合物的刺激,并且它可以使多聚SUMO链泛素化。

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