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WW 结构域为多蛋白网络的组装提供了一个平台。

WW domains provide a platform for the assembly of multiprotein networks.

作者信息

Ingham Robert J, Colwill Karen, Howard Caley, Dettwiler Sabine, Lim Caesar S H, Yu Joanna, Hersi Kadija, Raaijmakers Judith, Gish Gerald, Mbamalu Geraldine, Taylor Lorne, Yeung Benny, Vassilovski Galina, Amin Manish, Chen Fu, Matskova Liudmila, Winberg Gösta, Ernberg Ingemar, Linding Rune, O'donnell Paul, Starostine Andrei, Keller Walter, Metalnikov Pavel, Stark Chris, Pawson Tony

机构信息

Samuel Lunenfeld Research Institute, Mount Sinai Hospital, Toronto, Ontario, Canada.

出版信息

Mol Cell Biol. 2005 Aug;25(16):7092-106. doi: 10.1128/MCB.25.16.7092-7106.2005.

Abstract

WW domains are protein modules that mediate protein-protein interactions through recognition of proline-rich peptide motifs and phosphorylated serine/threonine-proline sites. To pursue the functional properties of WW domains, we employed mass spectrometry to identify 148 proteins that associate with 10 human WW domains. Many of these proteins represent novel WW domain-binding partners and are components of multiprotein complexes involved in molecular processes, such as transcription, RNA processing, and cytoskeletal regulation. We validated one complex in detail, showing that WW domains of the AIP4 E3 protein-ubiquitin ligase bind directly to a PPXY motif in the p68 subunit of pre-mRNA cleavage and polyadenylation factor Im in a manner that promotes p68 ubiquitylation. The tested WW domains fall into three broad groups on the basis of hierarchical clustering with respect to their associated proteins; each such cluster of bound proteins displayed a distinct set of WW domain-binding motifs. We also found that separate WW domains from the same protein or closely related proteins can have different specificities for protein ligands and also demonstrated that a single polypeptide can bind multiple classes of WW domains through separate proline-rich motifs. These data suggest that WW domains provide a versatile platform to link individual proteins into physiologically important networks.

摘要

WW结构域是一种蛋白质模块,通过识别富含脯氨酸的肽基序和磷酸化的丝氨酸/苏氨酸-脯氨酸位点来介导蛋白质-蛋白质相互作用。为了探究WW结构域的功能特性,我们采用质谱法鉴定了148种与10种人类WW结构域相关的蛋白质。这些蛋白质中有许多代表了新型的WW结构域结合伴侣,并且是参与分子过程(如转录、RNA加工和细胞骨架调节)的多蛋白复合物的组成成分。我们详细验证了一个复合物,结果表明AIP4 E3蛋白-泛素连接酶的WW结构域以促进p68泛素化的方式直接与前体mRNA切割和聚腺苷酸化因子Im的p68亚基中的PPXY基序结合。根据与其相关蛋白质的层次聚类,所测试的WW结构域可分为三大类;每一类结合蛋白质都显示出一组独特的WW结构域结合基序。我们还发现,来自同一蛋白质或密切相关蛋白质的不同WW结构域对蛋白质配体可能具有不同的特异性,并且还证明了单个多肽可以通过不同的富含脯氨酸基序结合多类WW结构域。这些数据表明,WW结构域提供了一个通用平台,可将单个蛋白质连接成生理上重要的网络。

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