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哺乳动物p97衔接复合体p47以及Ufd1-Npl4与泛素缀合物的直接结合。

Direct binding of ubiquitin conjugates by the mammalian p97 adaptor complexes, p47 and Ufd1-Npl4.

作者信息

Meyer Hemmo H, Wang Yanzhuang, Warren Graham

机构信息

Department of Cell Biology, Yale University School of Medicine, 333 Cedar Street, SHM, C441, PO Box 208002, New Haven, CT 06520-8002, USA.

出版信息

EMBO J. 2002 Nov 1;21(21):5645-52. doi: 10.1093/emboj/cdf579.

Abstract

The multiple functions of the p97/Cdc48p ATPase can be explained largely by adaptors that link its activity to different cellular pathways, but how these adaptors recognize different substrates is unclear. Here we present evidence that the mammalian adaptors, p47 and Ufd1-Npl4, both bind ubiquitin conjugates directly and so link p97 to ubiquitylated substrates. In the case of Ufd1-Npl4, which is involved in endoplasmic reticulum (ER)-associated degradation and nuclear envelope reassembly, binding to ubiquitin is mediated through a putative zinc finger in Npl4. This novel domain (NZF) is conserved in metazoa and is both present and functional in other proteins. In the case of p47, which is involved in the reassembly of the ER, the nuclear envelope and the Golgi apparatus, binding is mediated by a UBA domain. Unlike Ufd1-Npl4, it binds ubiquitin only when complexed with p97, and binds mono- rather than polyubiquitin conjugates. The UBA domain is required for the function of p47 in mitotic Golgi reassembly. Together, these data suggest that ubiquitin recognition is a common feature of p97-mediated reactions.

摘要

p97/Cdc48p ATP酶的多种功能很大程度上可由衔接蛋白来解释,这些衔接蛋白将其活性与不同的细胞通路联系起来,但这些衔接蛋白如何识别不同底物尚不清楚。在此,我们提供证据表明,哺乳动物衔接蛋白p47和Ufd1-Npl4都直接结合泛素缀合物,从而将p97与泛素化底物联系起来。就参与内质网(ER)相关降解和核膜重新组装的Ufd1-Npl4而言,与泛素的结合是通过Npl4中一个假定的锌指介导的。这个新结构域(NZF)在后生动物中保守,并且在其他蛋白质中也存在且具有功能。就参与内质网、核膜和高尔基体重新组装的p47而言,结合是由一个泛素相关结构域(UBA)介导的。与Ufd1-Npl4不同,它仅在与p97复合时才结合泛素,并且结合单泛素而非多泛素缀合物。UBA结构域是p47在有丝分裂高尔基体重新组装中发挥功能所必需的。总之,这些数据表明泛素识别是p97介导反应的一个共同特征。

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