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首页> 外文期刊>Scientific reports. >Dual roles for the ER membrane protein complex in flavivirus infection: viral entry and protein biogenesis
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Dual roles for the ER membrane protein complex in flavivirus infection: viral entry and protein biogenesis

机译:黄病毒感染中ER膜蛋白复合物的双重作用:病毒进入和蛋白质生物发生

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摘要

Hundreds of cellular host factors are required to support dengue virus infection, but their identity and roles are incompletely characterized. Here, we identify human host dependency factors required for efficient dengue virus-2 (DENV2) infection of human cells. We focused on two, TTC35 and TMEM111, which we previously demonstrated to be required for yellow fever virus (YFV) infection and others subsequently showed were also required by other flaviviruses. These proteins are components of the human endoplasmic reticulum membrane protein complex (EMC), which has roles in ER-associated protein biogenesis and lipid metabolism. We report that DENV, YFV and Zika virus (ZIKV) infections were strikingly inhibited, while West Nile virus infection was unchanged, in cells that lack EMC subunit 4. Furthermore, targeted depletion of EMC subunits in live mosquitoes significantly reduced DENV2 propagation in vivo. Using a novel uncoating assay, which measures interactions between host RNA-binding proteins and incoming viral RNA, we show that EMC is required at or prior to virus uncoating. Importantly, we uncovered a second and important role for the EMC. The complex is required for viral protein accumulation in a cell line harboring a ZIKV replicon, indicating that EMC participates in the complex process of viral protein biogenesis.
机译:需要数百种细胞宿主因子来支持登革热病毒感染,但它们的身份和角色是不完全表征的。在这里,我们确定人体细胞有效登革热病毒-2(Denv2)感染所需的人宿主依赖因子。我们专注于两种,TTC35和TMEM111,我们之前证明的黄热病病毒(YFV)感染,随后还需要其他黄病毒也需要。这些蛋白质是人内质网膜蛋白复合物(EMC)的组分,其在ER相关蛋白生物发生和脂质代谢中具有作用。我们举报了Denv,YFV和Zika病毒(ZIKV)感染抑制,而西尼罗病毒感染不变,缺乏EMC亚基4.此外,在生活蚊子中的EMC亚基的目标枯竭显着降低了体内Denv2繁殖。使用新的未涂覆测定,其测量宿主RNA结合蛋白和进入的病毒RNA之间的相互作用,我们表明在病毒未涂覆之前需要EMC。重要的是,我们发现了EMC的第二个和重要作用。含有ZIKV复制子的细胞系中病毒蛋白积累所需的复合物,表明EMC参与病毒蛋白生物发生的复杂过程。

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