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首页> 外文期刊>Journal of clinical virology: The official publication of the Pan American Society for Clinical Virology >Molecular and antigenic evolution of human influenza A/H3N2 viruses in Quebec, Canada, 2009-2011
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Molecular and antigenic evolution of human influenza A/H3N2 viruses in Quebec, Canada, 2009-2011

机译:2009-2011年加拿大魁北克人类A / H3N2流感病毒的分子和抗原进化

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摘要

Background: A/H3N2 variability leads to poor vaccine effectiveness when the vaccine strain is not well matched to the circulating virus. Objectives: We aim to describe the molecular and antigenic evolution of A/H3N2 viruses recovered during the last 3 influenza seasons in Quebec, Canada. Study design: Clinical samples from 33 patients with culture-confirmed A/H3N2 infections were collected over 3 consecutive seasons (March 2009-2011). The isolates' HA gene was amplified and sequenced; phylogenetic analyses of the HA1 region were conducted. To characterize A/H3N2 antigenic properties, standard hemagglutination inhibition (HI) and microneutralization (MN) assays were performed. Results: In 2009, we observed an antigenic drift from A/Brisbane/10/2007 (vaccine strain used in 2008-2009 and 2009-2010) to A/Perth/16/2009 (vaccine strain used in 2010-2011). Antigenic analysis of clinical influenza strains recovered in Quebec during 2009-2010 also illustrated antigenic drift from the previously prevalent A/Brisbane/10/2007-like (March 2009) to A/Perth/16/2009-like (December 2009) strains. In 2010-2011, the emergence of >4 substitutions in 4 different H3 antigenic sites suggested a genetic drift. However, HI and MN results confirmed the emergence of a drift in only 1 strain (8-fold difference in titers), while 19 others remained antigenically similar to A/Perth/16/2009 but exhibited titer differences (2-4-fold) just inferior to the standard definition of a drift. Conclusion: Antigenic and molecular characterization of H3N2 viruses over three seasons revealed that not only is the number of HA mutations important, but the nature and location of key mutations may play a significant role in antigenic drift.
机译:背景:当疫苗株与正在传播的病毒不完全匹配时,A / H3N2变异性会导致疫苗效果不佳。目的:我们旨在描述在加拿大魁北克省最近三个流感季节中回收的A / H3N2病毒的分子和抗原进化。研究设计:在连续3个季节(2009年3月至2011年3月)收集了33例经培养证实的A / H3N2感染的患者的临床样本。分离株的HA基因被扩增并测序;进行了HA1区的系统发育分析。为了表征A / H3N2抗原特性,进行了标准的血凝抑制(HI)和微中和(MN)分析。结果:2009年,我们观察到抗原从A / Brisbane / 10/2007(用于2008-2009和2009-2010的疫苗株)到A / Perth / 16/2009(用于2010-2011的疫苗株)的抗原漂移。对在2009-2010年期间在魁北克回收的临床流感病毒株进行的抗原分析也表明,抗原从以前流行的A / Brisbane / 10 / 2007-like(2009年3月)到A / Perth / 16 / 2009-like(2009年12月)。在2010-2011年间,在4个不同的H3抗原位点中出现了> 4个替换,表明存在遗传漂移。但是,HI和MN结果证实只有1个菌株出现了漂移(滴度相差8倍),而其他19个在抗原上仍与A / Perth / 16/2009相似,但表现出滴度相差(2-4倍)仅次于漂移的标准定义。结论:在三个季节中,H3N2病毒的抗原和分子表征表明,不仅HA突变的数量很重要,而且关键突变的性质和位置在抗原漂移中也可能起重要作用。

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