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H3N2 流感 A 病毒在原代猪呼吸道上皮细胞中的感染表型受唾液酸结合控制。

Infectivity phenotypes of H3N2 influenza A viruses in primary swine respiratory epithelial cells are controlled by sialic acid binding.

机构信息

Department of Pathobiological Sciences, School of Veterinary Medicine, University of Wisconsin-Madison, Madison, WI 53706, USA.

出版信息

Influenza Other Respir Viruses. 2012 Nov;6(6):424-33. doi: 10.1111/j.1750-2659.2012.00333.x. Epub 2012 Feb 21.

DOI:10.1111/j.1750-2659.2012.00333.x
PMID:22353399
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3360128/
Abstract

BACKGROUND

In the late 1990s, triple reassortant H3N2 influenza A viruses emerged and spread widely in the US swine population. We have shown previously that an isolate representative of this virus-lineage, A/Swine/Minnesota/593/99 (Sw/MN), exhibits phenotypic differences compared to a wholly human-lineage H3N2 virus isolated during the same time period, A/Swine/Ontario/00130/97 (Sw/ONT). Specifically, Sw/MN was more infectious for pigs and infected a significantly higher proportion of cultured primary swine respiratory epithelial cells (SRECs). In addition, reverse genetics-generated Sw/MN × Sw/ONT reassortant and point mutant viruses demonstrated that the infectivity phenotypes in SRECs were strongly dependent on three amino acids within the hemagglutinin (HA) gene.

OBJECTIVES

To determine the mechanism by which Sw/MN attains higher infectivity than Sw/ONT in SRECs.

METHODS

A/Swine/Minnesota/593/99, Sw/ONT, and mutant (reverse genetics-generated HA reassortant and point mutant) viruses were compared at various HA-mediated stages of infection: initial sialic acid binding, virus entry, and the pH of virus-endosome fusion.

RESULTS/CONCLUSIONS: Sialic acid binding was the sole stage where virus differences directly paralleled infectivity phenotypes in SRECs, indicating that binding is the primary mechanism responsible for differences in the infectivity levels of Sw/MN and Sw/ONT.

摘要

背景

20 世纪 90 年代末,三重重配的 H3N2 甲型流感病毒在美国猪群中出现并广泛传播。我们之前已经表明,该病毒谱系的代表分离株 A/Swine/Minnesota/593/99(Sw/MN)与同一时期分离的完全人谱系 H3N2 病毒 A/Swine/Ontario/00130/97(Sw/ONT)相比表现出表型差异。具体而言,Sw/MN 对猪更具传染性,并且感染了培养的原发性猪呼吸道上皮细胞(SRECs)的比例明显更高。此外,通过反向遗传学生成的 Sw/MN×Sw/ONT 重配和点突变病毒表明,SRECs 中的感染性表型强烈依赖于血凝素(HA)基因内的三个氨基酸。

目的

确定 Sw/MN 在 SRECs 中比 Sw/ONT 具有更高感染性的机制。

方法

比较 A/Swine/Minnesota/593/99、Sw/ONT 和突变(反向遗传学生成的 HA 重配和点突变)病毒在各种 HA 介导的感染阶段的情况:初始唾液酸结合、病毒进入和病毒-内体融合的 pH 值。

结果/结论:唾液酸结合是唯一直接与 SRECs 中感染性表型平行的病毒差异阶段,表明结合是导致 Sw/MN 和 Sw/ONT 感染性水平差异的主要机制。

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