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人肠道病毒的全面全长序列分析:多样性和重组。

Comprehensive full-length sequence analyses of human parechoviruses: diversity and recombination.

机构信息

Laboratory of Clinical Virology, Department of Medical Microbiology, Academic Medical Center, Amsterdam, The Netherlands.

出版信息

J Gen Virol. 2010 Jan;91(Pt 1):145-54. doi: 10.1099/vir.0.014670-0. Epub 2009 Sep 16.

DOI:10.1099/vir.0.014670-0
PMID:19759239
Abstract

Human parechoviruses (HPeVs) are highly prevalent pathogens among very young children. Although originally classified into two serologically distinct types, HPeV1 and -2, recent analyses of variants collected worldwide have revealed the existence of 12 further types classified genetically by sequence comparisons of complete genome sequences or the capsid (VP1) gene. To investigate the nature of HPeV evolution, its population dynamics and recombination breakpoints, this study generated 18 full-length genomic sequences of the most commonly circulating genotypes, HPeV1 and -3, collected over a time span of 14 years from The Netherlands. By inclusion of previously published full-length sequences, 35 sequences were analysed in total. Analysis of contemporary strains of HPeV1 and those most similar to the prototype strain (Harris) showed that HPeV1 variants fall into two genetically distinct clusters that are much more divergent from each other than those observed within other HPeV types. Future classification criteria for HPeVs may require modification to accommodate the occurrence of variants with intermediate degrees of diversity within types. Recombination was frequently observed among HPeV1, -4, -5 and -6, but was much more restricted among HPeV3 strains. Favoured sites for recombination were found to flank the capsid region, and further sites were found within the non-structural region, P2. In contrast to other HPeV types, the majority of the HPeV3 sequences remained monophyletic across the genome, a possible reflection of its lower diversity and potentially more recent emergence than other HPeV types, or biological and/or epidemiological constraints that limit opportunities for co-infections with potential recombination partners.

摘要

人肠道病毒(HPeV)是婴幼儿中高度流行的病原体。尽管最初被分为两种血清学上明显不同的类型,HPeV1 和 -2,但最近对全球收集的变异体的分析显示,存在 12 种进一步的类型,根据完整基因组序列或衣壳(VP1)基因的序列比较进行遗传分类。为了研究 HPeV 的进化性质、其群体动态和重组断点,本研究在 14 年的时间跨度内从荷兰收集了最常见循环基因型 HPeV1 和 -3 的 18 个全长基因组序列。通过包含以前发表的全长序列,总共分析了 35 个序列。对当代 HPeV1 株和与原型株(哈里斯)最相似的株进行分析表明,HPeV1 变异体分为两个遗传上明显不同的簇,彼此之间的差异比其他 HPeV 类型之间的差异大得多。未来 HPeV 的分类标准可能需要修改,以适应类型内具有中间多样性的变异体的出现。HPeV1、-4、-5 和 -6 之间经常观察到重组,但 HPeV3 株之间的重组受到更多限制。重组的首选部位位于衣壳区周围,进一步的部位位于非结构区 P2 内。与其他 HPeV 类型相比,大多数 HPeV3 序列在整个基因组中保持单系,这可能反映了其较低的多样性和潜在的比其他 HPeV 类型更新的出现,或者限制与潜在重组伙伴共同感染机会的生物学和/或流行病学限制。

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