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一种21千道尔顿病毒膜蛋白在痘苗病毒从中间区室组装过程中的作用。

The role of a 21-kDa viral membrane protein in the assembly of vaccinia virus from the intermediate compartment.

作者信息

Krijnse-Locker J, Schleich S, Rodriguez D, Goud B, Snijder E J, Griffiths G

机构信息

European Molecular Biology Laboratory, Cell Biology Program, Meyerhofstrasse 1, 69118 Heidelberg, Germany.

出版信息

J Biol Chem. 1996 Jun 21;271(25):14950-8. doi: 10.1074/jbc.271.25.14950.

Abstract

We have recently provided morphological evidence that a key event in the assembly of vaccinia virus is the formation of a novel cisternal domain of the intermediate compartment (IC) between the endoplasmic reticulum and the Golgi complex (Sodeik, B., Doms, R. W., Ericsson, M., Hiller, G., Machamer, C. E., van't Hof, W., van Meer, G., Moss, B., and Griffiths, G. (1993) J. Cell Biol. 121, 521-541). This tightly apposed cisternal domain incompletely surrounds the spherical immature virus that matures into the first of the two distinct infectious forms of vaccinia, the intracellular mature virus (IMV). In this study we describe the characterization of an abundant membrane protein of the IMV, the gene product of A17L, a 21-kDa protein that has recently been shown to be essential for the formation of the viral membranes (Rodriguez, D., Esteban, M., and Rodriguez, J. R. (1995) J. Virol. 69, 4640-4648). Upon translation in vitro, p21 associated with rough microsomal membranes in a co-translational manner. Using NH2- and COOH-terminal specific antibodies, we show that both in vitro as well as in vivo, p21 adopts a topology where the NH2 and COOH termini are cytoplasmically orientated. Immunocytochemical experiments demonstrated that p21 is a component of the inner of the two cisternal membranes of the immature virus as well as of membranes of the IC, identified using antibodies against Rab1. Taken together, these data provide the first molecular evidence in support of our assembly model; they show that an essential membrane protein of the IMV inserts into the rough endoplasmic reticulum, but gets efficiently targeted to the IC and membranes of the viral factory.

摘要

我们最近提供了形态学证据,表明痘苗病毒组装过程中的一个关键事件是在内质网和高尔基体复合体之间形成了一种新型的中间区室(IC)池状结构域(索德克,B.,多姆斯,R. W.,埃里克森,M.,希勒,G.,马查默,C. E.,范特霍夫,W.,范米尔,G.,莫斯,B.,和格里菲思,G.(1993)《细胞生物学杂志》121,521 - 541)。这个紧密相邻的池状结构域不完全包围球形的未成熟病毒,该病毒会成熟为痘苗两种不同感染形式中的第一种,即细胞内成熟病毒(IMV)。在本研究中,我们描述了IMV一种丰富膜蛋白的特性,它是A17L基因的产物,是一种21 kDa的蛋白质,最近已被证明对病毒膜的形成至关重要(罗德里格斯,D.,埃斯特班,M.,和罗德里格斯,J. R.(1995)《病毒学杂志》69,4640 - 4648)。在体外翻译时,p21以共翻译的方式与糙面微粒体膜结合。使用氨基末端和羧基末端特异性抗体,我们表明无论在体外还是体内,p21都呈现一种拓扑结构,其氨基末端和羧基末端都朝向细胞质。免疫细胞化学实验表明,p21是未成熟病毒两个池状膜中内层膜的组成成分,也是使用抗Rab1抗体鉴定的IC膜的组成成分。综上所述,这些数据提供了首个支持我们组装模型的分子证据;它们表明IMV的一种必需膜蛋白插入糙面内质网,但能有效地靶向IC和病毒工厂的膜。

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