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The IFITM Proteins Mediate Cellular Resistance to Influenza A H1N1 Virus, West Nile Virus, and Dengue Virus

机译:IFITM蛋白介导细胞对甲型H1N1流感病毒,西尼罗河病毒和登革热病毒的抗性

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Influenza viruses exploit host cell machinery to replicate, resulting in epidemics of respiratory illness. In turn, the host expresses antiviral restriction factors to defend against infection. To find host cell modifiers of influenza A H1N1 viral infection, we used a functional genomic screen and identified over 120 influenza A virus-dependency factors with roles in endosomal acidification, vesicular trafficking, mitochondrial metabolism, and RNA splicing. We discovered that the interferon-inducible transmembrane proteins IFITM1, 2, and 3 restrict an early step in influenza A viral replication. The IFITM proteins confer basal resistance to influenza A virus but are also inducible by interferons type I and II and are critical for interferon's virustatic actions. Further characterization revealed that the IFITM proteins inhibit the early replication of flaviviruses, including dengue virus and West Nile virus. Collectively this work identifies a family of antiviral restriction factors that mediate cellular innate immunity to at least three major human pathogens.
机译:流感病毒利用宿主细胞机制进行复制,从而导致呼吸道疾病的流行。反过来,宿主表达抗病毒限制因子以防御感染。为了找到甲型H1N1流感病毒感染的宿主细胞修饰剂,我们使用了功能基因组筛选,并鉴定了120多种甲型流感病毒依赖性因子,这些因子在内体酸化,水泡运输,线粒体代谢和RNA剪接中起作用。我们发现干扰素诱导的跨膜蛋白IFITM1、2和3限制了甲型流感病毒复制的早期步骤。 IFITM蛋白赋予甲型流感病毒基本的抵抗力,但也可被I型和II型干扰素诱导,对于干扰素的病毒作用至关重要。进一步的特征表明,IFITM蛋白抑制了包括登革热病毒和西尼罗河病毒在内的黄病毒的早期复制。总的来说,这项工作确定了介导细胞对至少三种主要人类病原体的固有免疫力的抗病毒限制因子家族。

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