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对构建的小鼠肝炎病毒E基因变异体的分析证实了E蛋白在冠状病毒组装中起关键作用。

Analysis of constructed E gene mutants of mouse hepatitis virus confirms a pivotal role for E protein in coronavirus assembly.

作者信息

Fischer F, Stegen C F, Masters P S, Samsonoff W A

机构信息

Departments of Biomedical Sciences, State University of New York at Albany, Albany, New York 12201, USA.

出版信息

J Virol. 1998 Oct;72(10):7885-94. doi: 10.1128/JVI.72.10.7885-7894.1998.

Abstract

Expression studies have shown that the coronavirus small envelope protein E and the much more abundant membrane glycoprotein M are both necessary and sufficient for the assembly of virus-like particles in cells. As a step toward understanding the function of the mouse hepatitis virus (MHV) E protein, we carried out clustered charged-to-alanine mutagenesis on the E gene and incorporated the resulting mutations into the MHV genome by targeted recombination. Of the four possible clustered charged-to-alanine E gene mutants, one was apparently lethal and one had a wild-type phenotype. The two other mutants were partially temperature sensitive, forming small plaques at the nonpermissive temperature. Revertant analyses of these two mutants demonstrated that the created mutations were responsible for the temperature-sensitive phenotype of each and provided support for possible interactions among E protein monomers. Both temperature-sensitive mutants were also found to be markedly thermolabile when grown at the permissive temperature, suggesting that there was a flaw in their assembly. Most significantly, when virions of one of the mutants were examined by electron microscopy, they were found to have strikingly aberrant morphology in comparison to the wild type: most mutant virions had pinched and elongated shapes that were rarely seen among wild-type virions. These results demonstrate an important, probably essential, role for the E protein in coronavirus morphogenesis.

摘要

表达研究表明,冠状病毒小包膜蛋白E和含量多得多的膜糖蛋白M对于细胞中病毒样颗粒的组装都是必需且充分的。作为了解小鼠肝炎病毒(MHV)E蛋白功能的第一步,我们对E基因进行了成簇的电荷到丙氨酸诱变,并通过靶向重组将产生的突变整合到MHV基因组中。在四种可能的成簇电荷到丙氨酸E基因突变体中,一种显然是致死性的,一种具有野生型表型。另外两个突变体部分温度敏感,在非允许温度下形成小噬斑。对这两个突变体的回复分析表明,产生的突变导致了每个突变体的温度敏感表型,并为E蛋白单体之间可能的相互作用提供了支持。还发现这两个温度敏感突变体在允许温度下生长时也明显热不稳定,表明它们的组装存在缺陷。最显著的是,当通过电子显微镜检查其中一个突变体的病毒粒子时,发现它们与野生型相比具有明显异常的形态:大多数突变体病毒粒子具有收缩和拉长的形状,这在野生型病毒粒子中很少见。这些结果证明了E蛋白在冠状病毒形态发生中起重要的、可能是必不可少的作用。

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