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Vps35p内不同的结构域介导从酵母前液泡/内体区室中回收两种不同的货物蛋白。

Distinct domains within Vps35p mediate the retrieval of two different cargo proteins from the yeast prevacuolar/endosomal compartment.

作者信息

Nothwehr S F, Bruinsma P, Strawn L A

机构信息

Division of Biological Sciences, University of Missouri, Columbia, Missouri 65211, USA.

出版信息

Mol Biol Cell. 1999 Apr;10(4):875-90. doi: 10.1091/mbc.10.4.875.

Abstract

Resident membrane proteins of the trans-Golgi network (TGN) of Saccharomyces cerevisiae are selectively retrieved from a prevacuolar/late endosomal compartment. Proper cycling of the carboxypeptidase Y receptor Vps10p between the TGN and prevacuolar compartment depends on Vps35p, a hydrophilic peripheral membrane protein. In this study we use a temperature-sensitive vps35 allele to show that loss of Vps35p function rapidly leads to mislocalization of A-ALP, a model TGN membrane protein, to the vacuole. Vps35p is required for the prevacuolar compartment-to-TGN transport of both A-ALP and Vps10p. This was demonstrated by phenotypic analysis of vps35 mutant strains expressing A-ALP mutants lacking either the retrieval or static retention signals and by an assay for prevacuolar compartment-to-TGN transport. A novel vps35 allele was identified that was defective for retrieval of A-ALP but functional for retrieval of Vps10p. Moreover, several other vps35 alleles were identified with the opposite characteristics: they were defective for Vps10p retrieval but near normal for A-ALP localization. These data suggest a model in which distinct structural features within Vps35p are required for associating with the cytosolic domains of each cargo protein during the retrieval process.

摘要

酿酒酵母反式高尔基体网络(TGN)的驻留膜蛋白是从液泡前/晚期内体区室中被选择性回收的。羧肽酶Y受体Vps10p在TGN和液泡前区室之间的正常循环依赖于Vps35p,一种亲水性外周膜蛋白。在本研究中,我们使用一个温度敏感型vps35等位基因来表明,Vps35p功能的丧失会迅速导致模型TGN膜蛋白A-ALP错误定位到液泡中。Vps35p是A-ALP和Vps10p从液泡前区室运输到TGN所必需的。这通过对表达缺乏回收或静态保留信号的A-ALP突变体的vps35突变菌株的表型分析以及液泡前区室到TGN运输的测定得以证明。鉴定出了一个新的vps35等位基因,它在A-ALP回收方面有缺陷,但在Vps10p回收方面有功能。此外,还鉴定出了其他几个具有相反特征的vps35等位基因:它们在Vps10p回收方面有缺陷,但在A-ALP定位方面接近正常。这些数据提示了一个模型,即在回收过程中,Vps35p内不同的结构特征对于与每种货物蛋白的胞质结构域结合是必需的。

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