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多种相互作用驱动衔接蛋白介导泛素连接酶rsp5在体内和体外对膜蛋白的募集。

Multiple interactions drive adaptor-mediated recruitment of the ubiquitin ligase rsp5 to membrane proteins in vivo and in vitro.

作者信息

Sullivan James A, Lewis Michael J, Nikko Elina, Pelham Hugh R B

机构信息

Medical Research Council Laboratory of Molecular Biology, Cambridge, United Kingdom.

出版信息

Mol Biol Cell. 2007 Jul;18(7):2429-40. doi: 10.1091/mbc.e07-01-0011. Epub 2007 Apr 11.

Abstract

Recognition of membrane proteins by the Nedd4/Rsp5 ubiquitin ligase family is a critical step in their targeting to the multivesicular body pathway. Some substrates contain "PY" motifs (PPxY), which bind to WW domains in the ligase. Others lack PY motifs and instead rely on adaptors that recruit the ligase to them. To investigate the mechanism of adaptor-mediated ubiquitination, we have characterized the interactions between the adaptor Bsd2, the ubiquitin ligase Rsp5, and the membrane proteins Cps1, Tre1, and Smf1 from Saccharomyces cerevisiae. We have reconstituted adaptor-mediated modification of Cps1 and Tre1 in vitro, and we show that two PY motifs in Bsd2 and two WW domains (WW2 and WW3) in Rsp5 are crucial for this. The binding of a weak noncanonical DMAPSY motif in Bsd2 to WW3 is an absolute requirement for Bsd2 adaptor function. We show that sorting of the manganese transporter Smf1, which requires both Bsd2 and Tre1, depends upon two PY motifs in Bsd2 and one motif in Tre1 but only two WW domains in Rsp5. We suggest that sequential assembly of first a Bsd2/Rsp5 complex, then a Tre1/Bsd2/Rsp5 complex followed by a rearrangement of PY-WW interactions is required for the ubiquitination of Smf1.

摘要

Nedd4/Rsp5泛素连接酶家族对膜蛋白的识别是其靶向多囊泡体途径的关键步骤。一些底物含有“PY”基序(PPxY),可与连接酶中的WW结构域结合。其他底物则缺乏PY基序,而是依赖衔接蛋白将连接酶招募至自身。为了研究衔接蛋白介导的泛素化机制,我们对酿酒酵母中衔接蛋白Bsd2、泛素连接酶Rsp5以及膜蛋白Cps1、Tre1和Smf1之间的相互作用进行了表征。我们在体外重建了衔接蛋白介导的Cps1和Tre1修饰,结果表明Bsd2中的两个PY基序以及Rsp5中的两个WW结构域(WW2和WW3)对此至关重要。Bsd2中一个弱的非经典DMAPSY基序与WW3的结合是Bsd2衔接蛋白功能的绝对必要条件。我们发现,锰转运蛋白Smf1的分选需要Bsd2和Tre1,这取决于Bsd2中的两个PY基序和Tre1中的一个基序,但Rsp5中只需两个WW结构域。我们认为,Smf1的泛素化需要先组装Bsd2/Rsp5复合物,然后组装Tre1/Bsd2/Rsp5复合物,随后重新排列PY-WW相互作用。

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