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FYVE结构域将Pib1p泛素连接酶靶向至内体和液泡膜。

FYVE domain targets Pib1p ubiquitin ligase to endosome and vacuolar membranes.

作者信息

Shin M E, Ogburn K D, Varban O A, Gilbert P M, Burd C G

机构信息

Department of Cell and Developmental Biology, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania 19104-6058, USA.

出版信息

J Biol Chem. 2001 Nov 2;276(44):41388-93. doi: 10.1074/jbc.M105665200. Epub 2001 Aug 28.

DOI:10.1074/jbc.M105665200
PMID:11526110
Abstract

Signaling by phosphatidylinositol 3-kinases (PI3Ks) is often mediated by proteins which bind PI3K products directly and are localized to intracellular membranes rich in PI3K products. The FYVE finger domain binds with high specificity to PtdIns3P and proteins containing this domain have been shown to be important components of diverse PI3K signaling pathways. The genome of the yeast Saccharomyces cerevisiae encodes five proteins containing FYVE domains, including Pib1p, whose function is unknown. In addition to a FYVE finger motif, the primary structure of Pib1p contains a region rich in cysteine and histidine residues that we demonstrate binds 2 mol eq of zinc, consistent with this region containing a RING structural domain. The Pib1p RING domain exhibited E2-dependent ubiquitin ligase activity in vitro, indicating that Pib1p is an E3 RING-type ubiquitin ligase. Fluorescence microscopy was used to demonstrate that a GFP-Pib1p fusion protein localized to endosomal and vacuolar membranes and deletional analysis of Pib1p domains indicated that localization of GFP-Pib1p is mediated solely by the FYVE domain. These results suggest that Pib1p mediates ubiquitination of a subset of cellular proteins localized to endosome and vacuolar membranes, and they expand the repertoire of PI3K-regulated pathways identified in eukaryotic cells.

摘要

磷脂酰肌醇3激酶(PI3K)的信号传导通常由直接结合PI3K产物并定位于富含PI3K产物的细胞内膜的蛋白质介导。FYVE指结构域与磷脂酰肌醇-3-磷酸(PtdIns3P)具有高度特异性结合,含有该结构域的蛋白质已被证明是多种PI3K信号通路的重要组成部分。酿酒酵母基因组编码五种含有FYVE结构域的蛋白质,包括功能未知的Pib1p。除了FYVE指基序外,Pib1p的一级结构还包含一个富含半胱氨酸和组氨酸残基的区域,我们证明该区域结合2摩尔当量的锌,这与该区域含有一个RING结构域一致。Pib1p的RING结构域在体外表现出E2依赖性泛素连接酶活性,表明Pib1p是一种E3 RING型泛素连接酶。荧光显微镜用于证明GFP-Pib1p融合蛋白定位于内体和液泡膜,对Pib1p结构域的缺失分析表明GFP-Pib1p的定位仅由FYVE结构域介导。这些结果表明,Pib1p介导定位于内体和液泡膜的一部分细胞蛋白的泛素化,并且它们扩展了在真核细胞中鉴定出的PI3K调节途径的种类。

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