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与非典型手足口病相关的人柯萨奇病毒A6变异株的基因特征:重组在病毒出现及致病性中的潜在作用

Genetic characterization of human coxsackievirus A6 variants associated with atypical hand, foot and mouth disease: a potential role of recombination in emergence and pathogenicity.

作者信息

Gaunt Eleanor, Harvala Heli, Österback Riikka, Sreenu Vattipally B, Thomson Emma, Waris Matti, Simmonds Peter

机构信息

Roslin Institute, University of Edinburgh, Easter Bush, Edinburgh EH25 9RG, UK.

Specialist Virology Laboratory, Royal Infirmary of Edinburgh, Edinburgh, UK.

出版信息

J Gen Virol. 2015 May;96(Pt 5):1067-1079. doi: 10.1099/vir.0.000062. Epub 2015 Jan 22.

Abstract

Human coxsackievirus A6 (CVA6) is an enterically transmitted enterovirus. Until recently, CVA6 infections were considered as being of minor clinical significance, and only rarely aetiologically linked with hand, foot and mouth disease (HFMD) associated with other species A enteroviruses (particularly EV71 and CVA16). From 2008 onwards, however, CVA6 infections have been associated with several outbreaks worldwide of atypical HFMD (aHFMD) accompanied by a varicelliform rash. We recently reported CVA6-associated eczema herpeticum occurring predominantly in children and young adults in Edinburgh in January and February 2014. To investigate genetic determinants of novel clinical phenotypes of CVA6, we genetically characterized and analysed CVA6 variants associated with eczema herpeticum in Edinburgh in 2014 and those with aHFMD in CAV isolates collected from 2008. A total of eight recombinant forms (RFs) have circulated worldwide over the past 10 years, with the particularly recent appearance of RF-H associated with eczema herpeticum cases in Edinburgh in 2014. Comparison of phylogenies and divergence of complete genome sequences of CVA6 identified recombination breakpoints in 2A-2C, within VP3, and between 5' untranslated region and VP1. A Bayesian temporal reconstruction of CVA6 evolution since 2004 provided estimates of dates and the actual recombination events that generated more recently appearing recombination groups (RF-E, -F, -G and -H). Associations were observed between recombination groups and clinical presentations of herpangina, aHFMD and eczema herpeticum, but not with VP1 or other structural genes. These observations provided evidence that NS gene regions may potentially contribute to clinical phenotypes and outcomes of CVA6 infection.

摘要

人柯萨奇病毒A6(CVA6)是一种经肠道传播的肠道病毒。直到最近,CVA6感染仍被认为临床意义不大,并且在病因上很少与其他A组肠道病毒(特别是EV71和CVA16)相关的手足口病(HFMD)有关。然而,从2008年起,CVA6感染已与全球范围内几起伴有水痘样皮疹的非典型HFMD(aHFMD)疫情相关。我们最近报告了2014年1月和2月在爱丁堡主要发生于儿童和年轻人中的CVA6相关疱疹样湿疹。为了研究CVA6新临床表型的遗传决定因素,我们对2014年在爱丁堡与疱疹样湿疹相关的CVA6变异株以及2008年收集的CAV分离株中与aHFMD相关的CVA6变异株进行了基因特征分析和分析。在过去10年中,共有8种重组形式(RFs)在全球传播,特别是最近出现的RF-H与2014年爱丁堡的疱疹样湿疹病例相关。对CVA6完整基因组序列的系统发育和差异比较确定了2A-2C、VP3内以及5'非翻译区和VP1之间的重组断点。对2004年以来CVA6进化的贝叶斯时间重建提供了对产生最近出现的重组组(RF-E、-F、-G和-H)的日期和实际重组事件的估计。观察到重组组与疱疹性咽峡炎、aHFMD和疱疹样湿疹的临床表现之间存在关联,但与VP1或其他结构基因无关。这些观察结果提供了证据,表明NS基因区域可能对CVA6感染的临床表型和结果有潜在影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0479/4631059/2db522c217dc/vir-96-05-1067-g001.jpg

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