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Rsp5泛素连接酶与Ubp2去泛素化酶相互关联且相互拮抗。

The Rsp5 ubiquitin ligase is coupled to and antagonized by the Ubp2 deubiquitinating enzyme.

作者信息

Kee Younghoon, Lyon Nancy, Huibregtse Jon M

机构信息

Institute for Cellular and Molecular Biology, Section of Molecular Genetics and Microbiology, University of Texas at Austin, Austin, TX 78712, USA.

出版信息

EMBO J. 2005 Jul 6;24(13):2414-24. doi: 10.1038/sj.emboj.7600710. Epub 2005 Jun 2.

Abstract

Saccharomyces cerevisiae Rsp5 is an essential HECT ubiquitin ligase involved in several biological processes. To gain further insight into regulation of this enzyme, we identified proteins that copurified with epitope-tagged Rsp5. Ubp2, a deubiquitinating enzyme, was a prominent copurifying protein. Rup1, a previously uncharacterized UBA domain protein, was required for binding of Rsp5 to Ubp2 both in vitro and in vivo. Overexpression of Ubp2 or Rup1 in the rsp5-1 mutant elicited a strong growth defect, while overexpression of a catalytically inactive Ubp2 mutant or Rup1 deleted of the UBA domain did not, suggesting an antagonistic relationship between Rsp5 and the Ubp2/Rup1 complex. Consistent with this model, rsp5-1 temperature sensitivity was suppressed by either ubp2Delta or rup1Delta mutations. Ubp2 reversed Rsp5-catalyzed substrate ubiquitination in vitro, and Rsp5 and Ubp2 preferentially assembled and disassembled, respectively, K63-linked polyubiquitin chains. Together, these results indicate that Rsp5 activity is modulated by being physically coupled to the Rup1/Ubp2 deubiquitinating enzyme complex, representing a novel mode of regulation for an HECT ubiquitin ligase.

摘要

酿酒酵母Rsp5是一种参与多种生物学过程的必需HECT泛素连接酶。为了进一步深入了解这种酶的调控机制,我们鉴定了与表位标签化的Rsp5共纯化的蛋白质。去泛素化酶Ubp2是一种显著的共纯化蛋白。Rup1是一种先前未被表征的UBA结构域蛋白,在体外和体内,Rsp5与Ubp2的结合都需要它。在rsp5-1突变体中过表达Ubp2或Rup1会引发强烈的生长缺陷,而过表达催化失活的Ubp2突变体或缺失UBA结构域的Rup1则不会,这表明Rsp5与Ubp2/Rup1复合物之间存在拮抗关系。与该模型一致,ubp2Δ或rup1Δ突变可抑制rsp5-1的温度敏感性。Ubp2在体外可逆转Rsp5催化的底物泛素化,并且Rsp5和Ubp2分别优先组装和拆卸K63连接的多聚泛素链。总之,这些结果表明,Rsp5的活性通过与Rup1/Ubp2去泛素化酶复合物物理偶联而受到调节,这代表了一种HECT泛素连接酶的新型调控模式。

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