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麻疹病毒通过不同受体进入和传播的效率。

Efficiency of measles virus entry and dissemination through different receptors.

作者信息

Schneider Urs, von Messling Veronika, Devaux Patricia, Cattaneo Roberto

机构信息

Molecular Medicine Program, Mayo Foundation, Rochester, Minnesota 55905, USA.

出版信息

J Virol. 2002 Aug;76(15):7460-7. doi: 10.1128/jvi.76.15.7460-7467.2002.

Abstract

The efficiency with which different measles virus (MV) strains enter cells through the immune cell-specific protein SLAM (CD150) or other receptors, including the ubiquitous protein CD46, may influence their pathogenicity. We compared the cell entry efficiency of recombinant MV differing only in their attachment protein hemagglutinin (H). We constructed these viruses with an additional gene expressing an autofluorescent reporter protein to allow direct detection of every infected cell. A virus with a wild-type H protein entered cells through SLAM two to three times more efficiently than a virus with the H protein of the attenuated strain Edmonston, whereas cell entry efficiency through CD46 was lower. However, these subtle differences were amplified at the cell fusion stage because the wild-type H protein failed to fuse CD46-expressing cells. We also proved formally that a mutation in H protein residue 481 (asparagine to tyrosine) results in improved CD46-specific entry. To define the selective pressure exerted on that codon, we monitored its evolution in different H protein backgrounds and found that several passages in CD46-expressing Vero cells were necessary to shift it in the majority of the MV RNA. To verify the importance of these observations for human infections, we examined MV entry into peripheral blood mononuclear cells and observed that viruses with asparagine 481 H proteins infect these cells more efficiently.

摘要

不同麻疹病毒(MV)毒株通过免疫细胞特异性蛋白信号淋巴细胞激活分子(SLAM,即CD150)或其他受体(包括普遍存在的蛋白CD46)进入细胞的效率,可能会影响其致病性。我们比较了仅附着蛋白血凝素(H)不同的重组MV的细胞进入效率。我们构建这些病毒时带有一个额外的表达自发荧光报告蛋白的基因,以便直接检测每个被感染的细胞。带有野生型H蛋白的病毒通过SLAM进入细胞的效率比带有减毒株埃德蒙斯顿H蛋白的病毒高两到三倍,而通过CD46的细胞进入效率则较低。然而,这些细微差异在细胞融合阶段被放大了,因为野生型H蛋白无法使表达CD46的细胞融合。我们还正式证明,H蛋白第481位残基的突变(天冬酰胺突变为酪氨酸)会导致CD46特异性进入效率提高。为了确定对该密码子施加的选择压力,我们监测了其在不同H蛋白背景下的进化情况,发现在表达CD46的非洲绿猴肾细胞(Vero细胞)中传代数次,对于大多数MV RNA而言,才会使其发生改变。为了验证这些观察结果对人类感染的重要性,我们检测了MV进入外周血单个核细胞的情况,观察到带有第481位天冬酰胺H蛋白的病毒能更有效地感染这些细胞。

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