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甲型、乙型、丙型和丁型流感病毒NS1蛋白的功能表征及直接比较 以及 。(原文最后“and.”表述不完整,可能影响准确理解)

Functional Characterization and Direct Comparison of Influenza A, B, C, and D NS1 Proteins and .

作者信息

Nogales Aitor, Aydillo Teresa, Ávila-Pérez Gines, Escalera Alba, Chiem Kevin, Cadagan Richard, DeDiego Marta L, Li Feng, García-Sastre Adolfo, Martínez-Sobrido Luis

机构信息

Department of Microbiology and Immunology, School of Medicine and Dentistry, University of Rochester, Rochester, NY, United States.

Centro de Investigación en Sanidad Animal, Madrid, Spain.

出版信息

Front Microbiol. 2019 Dec 17;10:2862. doi: 10.3389/fmicb.2019.02862. eCollection 2019.

Abstract

Influenza viruses are important pathogens that affect multiple animal species, including humans. There are four types of influenza viruses: A, B, C, and D (IAV, IBV, ICV, and IDV, respectively). IAV and IBV are currently circulating in humans and are responsible of seasonal epidemics (IAV and IBV) and occasional pandemics (IAV). ICV is known to cause mild infections in humans and pigs, while the recently identified IDV primarily affect cattle and pigs. Influenza non-structural protein 1 (NS1) is a multifunctional protein encoded by the NS segment in all influenza types. The main function of NS1 is to counteract the host antiviral defense, including the production of interferon (IFN) and IFN-stimulated genes (ISGs), and therefore is considered an important viral pathogenic factor. Despite of homologous functions, the NS1 protein from the diverse influenza types share little amino acid sequence identity, suggesting possible differences in their mechanism(s) of action, interaction(s) with host factors, and contribution to viral replication and/or pathogenesis. In addition, although the NS1 protein of IAV, IBV and, to some extent ICV, have been previously studied, it is unclear if IDV NS1 has similar properties. Using an approach that allow us to express NS1 independently of the nuclear export protein from the viral NS segment, we have generated recombinant IAV expressing IAV, IBV, ICV, and IDV NS1 proteins. Although recombinant viruses expressing heterotypic (IBV, ICV, and IDV) NS1 proteins were able to replicate similarly in canine MDCK cells, their viral fitness was impaired in human A549 cells and they were highly attenuated . Our data suggest that despite the similarities to effectively counteract innate immune responses , the NS1 proteins of IBV, ICV, or IDV do not fully complement the functions of IAV NS1, resulting in deficient viral replication and pathogenesis .

摘要

流感病毒是影响包括人类在内的多种动物物种的重要病原体。流感病毒有四种类型:A、B、C和D(分别为IAV、IBV、ICV和IDV)。IAV和IBV目前在人类中传播,分别导致季节性流行(IAV和IBV)以及偶尔的大流行(IAV)。已知ICV会在人类和猪中引起轻度感染,而最近发现的IDV主要感染牛和猪。流感非结构蛋白1(NS1)是所有流感病毒类型中由NS片段编码的多功能蛋白。NS1的主要功能是对抗宿主的抗病毒防御,包括干扰素(IFN)和干扰素刺激基因(ISG)的产生,因此被认为是一种重要的病毒致病因子。尽管功能同源,但不同流感病毒类型的NS1蛋白氨基酸序列同源性很低,这表明它们在作用机制、与宿主因子的相互作用以及对病毒复制和/或发病机制的贡献方面可能存在差异。此外,尽管IAV、IBV以及在一定程度上ICV的NS1蛋白此前已被研究,但尚不清楚IDV NS1是否具有类似特性。通过一种使我们能够独立于病毒NS片段的核输出蛋白来表达NS1的方法,我们构建了表达IAV、IBV、ICV和IDV NS1蛋白的重组IAV。尽管表达异型(IBV、ICV和IDV)NS1蛋白的重组病毒能够在犬MDCK细胞中类似地复制,但其病毒适应性在人A549细胞中受损,并且它们高度减毒。我们的数据表明,尽管在有效对抗先天免疫反应方面存在相似性,但IBV、ICV或IDV的NS1蛋白不能完全补充IAV NS1的功能,导致病毒复制和发病机制不足。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2de4/6927920/d9cf7fd74b9f/fmicb-10-02862-g001.jpg

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