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首页> 外文期刊>Journal of neurovirology >The virulence of mouse hepatitis virus strain A59 is not dependent on efficient spike protein cleavage and cell-to-cell fusion.
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The virulence of mouse hepatitis virus strain A59 is not dependent on efficient spike protein cleavage and cell-to-cell fusion.

机译:小鼠肝炎病毒A59株的毒力不依赖有效的刺突蛋白裂解和细胞间融合。

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摘要

The cleavage and fusion properties of recombinant murine hepatitis viruses (MHV) were examined to assess the role of the cleavage signal in determining the extent of S protein cleavage, and the correlation between cleavage and induction of cell-to-cell fusion. Targeted recombination was used to introduce amino acid substitutions into the cleavage signal of the fusion glycoprotein (spike or S protein) of MHV strain A59. The recombinants were then used to address the question of the importance of S protein cleavage and viral-mediated cell-to-cell fusion on pathogenicity. Our data indicate that cleavage of spike is not solely determined by the amino acid sequence at the cleavage site, but may also depend on sequences removed from the cleavage site. In addition, efficient cell-to-cell fusion is not necessary for virulence.
机译:检查了重组鼠肝炎病毒(MHV)的裂解和融合特性,以评估裂解信号在确定S蛋白裂解程度以及裂解与诱导细胞间融合之间的相关性中的作用。使用靶向重组将氨基酸置换引入MHV菌株A59的融合糖蛋白(穗或S蛋白)的切割信号中。然后将重组体用于解决S蛋白裂解和病毒介导的细胞间融合对致病性的重要性的问题。我们的数据表明刺突的切割不仅由切割位点的氨基酸序列决定,而且还可能取决于从切割位点除去的序列。另外,对于毒力而言,有效的细胞间融合不是必需的。

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