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The interferon stimulated gene 20 protein (ISG20) is an innate defense antiviral factor that discriminates self versus non-self translation

机译:干扰素刺激基因20蛋白(ISG20)是先天防御抗病毒因子可区分自身翻译与非自身翻译

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摘要

ISG20 is a broad spectrum antiviral protein thought to directly degrade viral RNA. However, this mechanism of inhibition remains controversial. Using the Vesicular Stomatitis Virus (VSV) as a model RNA virus, we show here that ISG20 interferes with viral replication by decreasing protein synthesis in the absence of RNA degradation. Importantly, we demonstrate that ISG20 exerts a translational control over a large panel of non-self RNA substrates including those originating from transfected DNA, while sparing endogenous transcripts. This activity correlates with the protein’s ability to localize in cytoplasmic processing bodies. Finally, these functions are conserved in the ISG20 murine ortholog, whose genetic ablation results in mice with increased susceptibility to viral infection. Overall, our results posit ISG20 as an important defense factor able to discriminate the selfon-self origins of the RNA through translation modulation.
机译:ISG20是一种广谱抗病毒蛋白,被认为可以直接降解病毒RNA。但是,这种抑制机制仍存在争议。使用水泡性口炎病毒(VSV)作为模型RNA病毒,我们在这里显示ISG20通过在没有RNA降解的情况下减少蛋白质合成来干扰病毒复制。重要的是,我们证明了ISG20对一大堆非自身RNA底物(包括那些源自转染DNA的非自身RNA底物)施加翻译控制,同时保留了内源性转录本。这种活性与蛋白质定位在细胞质加工体中的能力有关。最后,这些功能在ISG20小鼠直系同源物中得以保留,其基因消融导致小鼠对病毒感染的敏感性增加。总的来说,我们的结果认为ISG20是重要的防御因子,能够通过翻译调节来区分RNA的自身/非自身来源。

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