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台湾地区 H3N2 流感病毒的分子流行病学和抗原性分析。

Molecular epidemiology and antigenic analyses of influenza A viruses H3N2 in Taiwan.

机构信息

Center for Research and Diagnostics, Centers for Disease Control, Taipei, Taiwan.

出版信息

Clin Microbiol Infect. 2011 Feb;17(2):214-22. doi: 10.1111/j.1469-0691.2010.03228.x.

Abstract

The severity of an influenza epidemic season may be influenced not only by variability in the surface glycoproteins, but also by differences in the internal proteins of circulating influenza viruses. To better understand viral antigenic evolution, all eight gene segments from 44 human H3N2 epidemic strains isolated during 2004-2008 in Taiwan were analyzed to provide a profile of protein variability. Comparison of the evolutionary profiles of the HA, NA and PB2 genes of influenza A (H3N2) viruses indicated that they were derived from a group of H3N2 isolates first seen in 2004. However, the PA, M and PB1 genes were derived from a different group of H3N2 isolates from 2004. Tree topology revealed the NP and NS genes could each be segregated into two groups similar to those for the polymerase genes. In addition, new genetic variants occurred during the non-epidemic period and become the dominant strain after one or two seasons. Comparison of evolutionary patterns in consecutive years is necessary to correlate viral genetic changes with antigenic changes as multiple lineages co-circulate.

摘要

流感疫情的严重程度不仅可能受到表面糖蛋白的变化影响,还可能受到循环流感病毒内部蛋白的差异影响。为了更好地了解病毒抗原进化,分析了 2004 年至 2008 年在台湾分离的 44 株人源 H3N2 流行株的 8 个基因片段,以提供蛋白质变异性的概况。对流感 A (H3N2) 病毒的 HA、NA 和 PB2 基因的进化情况进行比较,结果表明这些病毒源自于 2004 年首次出现的一组 H3N2 分离株。然而,PA、M 和 PB1 基因则源自于 2004 年另一组不同的 H3N2 分离株。系统发育树拓扑结构显示 NP 和 NS 基因可以各自分为两组,类似于聚合酶基因。此外,在非流行期间会出现新的遗传变异体,并且在一到两个季节后成为主要流行株。需要对连续几年的进化模式进行比较,以便将病毒遗传变化与抗原变化相关联,因为多种谱系同时流行。

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