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冠状病毒E1蛋白跨膜结构域中的高尔基体保留信号。

A Golgi retention signal in a membrane-spanning domain of coronavirus E1 protein.

作者信息

Swift A M, Machamer C E

机构信息

Department of Cell Biology and Anatomy, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205.

出版信息

J Cell Biol. 1991 Oct;115(1):19-30. doi: 10.1083/jcb.115.1.19.

DOI:10.1083/jcb.115.1.19
PMID:1655802
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2289920/
Abstract

The E1 glycoprotein from an avian coronavirus is a model protein for studying retention in the Golgi complex. In animal cells expressing the protein from cDNA, the E1 protein is targeted to cis Golgi cisternae (Machamer, C. E., S. A. Mentone, J. K. Rose, and M. G. Farquhar. 1990. Proc. Natl. Acad. Sci. USA. 87:6944-6948). We show that the first of the three membrane-spanning domains of the E1 protein can retain two different plasma membrane proteins in the Golgi region of transfected cells. Both the vesicular stomatitis virus G protein and the alpha-subunit of human chorionic gonadotropin (anchored to the membrane by fusion with the G protein membrane-spanning domain and cytoplasmic tail) were retained in the Golgi region of transfected cells when their single membrane-spanning domains were replaced with the first membrane-spanning domain from E1. Single amino acid substitutions in this sequence released retention of the chimeric G protein, as well as a mutant E1 protein which lacks the second and third membrane-spanning domains. The important feature of the retention sequence appears to be the uncharged polar residues which line one face of a predicted alpha helix. This is the first retention signal to be defined for a resident Golgi protein. The fact that it is present in a membrane-spanning domain suggests a novel mechanism of retention in which the membrane composition of the Golgi complex plays an instrumental role in retaining its resident proteins.

摘要

禽冠状病毒的E1糖蛋白是用于研究在高尔基体中滞留的模型蛋白。在从cDNA表达该蛋白的动物细胞中,E1蛋白靶向顺面高尔基体潴泡(马查默,C.E.,S.A.门托内,J.K.罗斯和M.G.法夸尔。1990年。美国国家科学院院刊。87:6944 - 6948)。我们发现,E1蛋白的三个跨膜结构域中的第一个能够将两种不同的质膜蛋白滞留在转染细胞的高尔基体区域。当水泡性口炎病毒G蛋白和人绒毛膜促性腺激素的α亚基(通过与G蛋白跨膜结构域和胞质尾融合而锚定在膜上)的单个跨膜结构域被E1的第一个跨膜结构域取代时,它们都被滞留在转染细胞的高尔基体区域。该序列中的单个氨基酸取代会解除嵌合G蛋白以及缺乏第二和第三个跨膜结构域的突变E1蛋白的滞留。滞留序列的重要特征似乎是排列在预测的α螺旋一侧的不带电荷的极性残基。这是为驻留高尔基体蛋白定义的第一个滞留信号。它存在于跨膜结构域这一事实提示了一种新的滞留机制,其中高尔基体复合体的膜组成在保留其驻留蛋白方面起着重要作用。