口蹄疫病毒的前导蛋白酶:一种蛋白水解毒力因子的结构-功能关系
The leader proteinase of foot-and-mouth disease virus: structure-function relationships in a proteolytic virulence factor.
作者信息
Steinberger Jutta, Skern Tim
出版信息
Biol Chem. 2014 Oct;395(10):1179-85. doi: 10.1515/hsz-2014-0156.
Abstract
The leader proteinase (Lpro) of the foot-and-mouth disease virus inhibits the host innate immune response by at least three different mechanisms. The most well-characterised of these is the prevention of the synthesis of cytokines such as interferons immediately after infection, brought about by specific proteolytic cleavage of the eukaryotic initiation factor 4G. This prevents the recruitment of capped cellular mRNA; however, the viral RNA can be translated under these conditions. The two other mechanisms are the induction of NF-κB cleavage and the deubiquitination of immune signalling molecules. This review focuses on the structure-function relationships in Lpro responsible for these widely divergent activities.
摘要
口蹄疫病毒的前导蛋白酶(Lpro)至少通过三种不同机制抑制宿主的先天免疫反应。其中最广为人知的机制是在感染后立即通过对真核起始因子4G进行特异性蛋白水解切割,来阻止细胞因子如干扰素的合成。这会阻止加帽细胞mRNA的募集;然而,病毒RNA在这些条件下仍可被翻译。另外两种机制是诱导NF-κB切割和免疫信号分子的去泛素化。本综述聚焦于Lpro中负责这些差异极大的活性的结构-功能关系。
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