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TRIM7 抑制肠道病毒复制并促进具有更高致病性的病毒变异体的出现。

TRIM7 inhibits enterovirus replication and promotes emergence of a viral variant with increased pathogenicity.

机构信息

Department of Microbiology, UT Southwestern Medical Center, Dallas, TX 75390, USA.

Green Center for Molecular, Computational, and Systems Biology, UT Southwestern Medical Center, Dallas, TX 75390, USA.

出版信息

Cell. 2021 Jun 24;184(13):3410-3425.e17. doi: 10.1016/j.cell.2021.04.047. Epub 2021 May 31.

DOI:10.1016/j.cell.2021.04.047
PMID:34062120
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8276836/
Abstract

To control viral infection, vertebrates rely on both inducible interferon responses and less well-characterized cell-intrinsic responses composed of "at the ready" antiviral effector proteins. Here, we show that E3 ubiquitin ligase TRIM7 is a cell-intrinsic antiviral effector that restricts multiple human enteroviruses by targeting viral 2BC, a membrane remodeling protein, for ubiquitination and proteasome-dependent degradation. Selective pressure exerted by TRIM7 results in emergence of a TRIM7-resistant coxsackievirus with a single point mutation in the viral 2C ATPase/helicase. In cultured cells, the mutation helps the virus evade TRIM7 but impairs optimal viral replication, and this correlates with a hyperactive and structurally plastic 2C ATPase. Unexpectedly, the TRIM7-resistant virus has a replication advantage in mice and causes lethal pancreatitis. These findings reveal a unique mechanism for targeting enterovirus replication and provide molecular insight into the benefits and trade-offs of viral evolution imposed by a host restriction factor.

摘要

为了控制病毒感染,脊椎动物依赖于诱导型干扰素反应和特征不太明显的细胞固有反应,这些反应由“随时待命”的抗病毒效应蛋白组成。在这里,我们表明 E3 泛素连接酶 TRIM7 是一种细胞内抗病毒效应因子,通过靶向病毒 2BC(一种膜重塑蛋白)进行泛素化和蛋白酶体依赖性降解,限制多种人类肠道病毒。TRIM7 施加的选择压力导致出现一种 TRIM7 抗性柯萨奇病毒,其病毒 2C ATPase/解旋酶中存在单点突变。在培养细胞中,该突变有助于病毒逃避 TRIM7,但会损害最佳病毒复制,这与 2C ATPase 的过度活跃和结构可塑性相关。出乎意料的是,TRIM7 抗性病毒在小鼠中具有复制优势,并导致致命性胰腺炎。这些发现揭示了靶向肠道病毒复制的独特机制,并为宿主限制因子施加的病毒进化的益处和权衡提供了分子见解。

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