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Resource Genome-wide CRISPR/Cas9 Screen Identifies Host Factors Essential for Influenza Virus Replication

机译:资源全基因组CRISPR / Cas9筛选确定了流感病毒复制必不可少的宿主因子

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Summary The emergence of influenza A viruses (IAVs) from zoonotic reservoirs poses a great threat to human health. As seasonal vaccines are ineffective against zoonotic strains, and newly transmitted viruses can quickly acquire drug resistance, there remains a need for host-directed therapeutics against IAVs. Here, we performed a genome-scale CRISPR/Cas9 knockout screen in human lung epithelial cells with a human isolate of an avian H5N1 strain. Several genes involved in sialic acid biosynthesis and related glycosylation pathways were highly enriched post-H5N1 selection, including SLC35A1 , a sialic acid transporter essential for IAV receptor expression and thus viral entry. Importantly, we have identified capicua (CIC) as a negative regulator of cell-intrinsic immunity, as loss of CIC resulted in heightened antiviral responses and restricted replication of multiple viruses. Therefore, our study demonstrates that the CRISPR/Cas9 system can be utilized for the discovery of host factors critical for the replication of intracellular pathogens.
机译:小结从人畜共患病的水库中出现的甲型流感病毒(IAV)对人类健康构成了巨大威胁。由于季节性疫苗对人畜共患病毒株无效,并且新传播的病毒可以快速获得耐药性,因此仍然需要针对宿主的针对IAV的疗法。在这里,我们用人H5N1禽流感病毒分离株在人肺上皮细胞中进行了基因组规模的CRISPR / Cas9基因敲除筛选。在H5N1选择后,涉及唾液酸生物合成和相关糖基化途径的几个基因高度富集,包括SLC35A1,这是IAV受体表达和病毒进入所必需的唾液酸转运蛋白。重要的是,我们已经确定capicua(CIC)是细胞内在免疫力的负调节剂,因为CIC的丧失导致增强的抗病毒反应和多种病毒的复制受到限制。因此,我们的研究表明,CRISPR / Cas9系统可用于发现对细胞内病原体复制至关重要的宿主因子。

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