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Norovirus illness is a global problem: emergence and spread of norovirus GII.4 variants, 2001-2007.诺如病毒疾病是一个全球性问题:2001年至2007年诺如病毒GII.4变体的出现和传播。
J Infect Dis. 2009 Sep 1;200(5):802-12. doi: 10.1086/605127.
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Mouse norovirus replication is associated with virus-induced vesicle clusters originating from membranes derived from the secretory pathway.小鼠诺如病毒的复制与源自分泌途径膜的病毒诱导囊泡簇有关。
J Virol. 2009 Oct;83(19):9709-19. doi: 10.1128/JVI.00600-09. Epub 2009 Jul 8.
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A new variant of Norovirus GII.4/2007 and inter-genotype recombinant strains of NVGII causing acute watery diarrhoea among children in Kolkata, India.印度加尔各答儿童中引起急性水样腹泻的诺如病毒GII.4/2007新变种及NVGII基因间重组菌株
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Emergence of the GII4/2006b variant and recombinant noroviruses in China.中国GII4/2006b变异株和重组诺如病毒的出现。
J Med Virol. 2008 Nov;80(11):1997-2004. doi: 10.1002/jmv.21308.

日本 2006 年 5 月至 2009 年 2 月期间,诺如病毒 GII/4 通过基因组重组发生了分歧进化。

Divergent evolution of norovirus GII/4 by genome recombination from May 2006 to February 2009 in Japan.

机构信息

Pathogen Genomics Center, National Institute of Infectious Diseases, Tokyo 208-0011, Japan.

出版信息

J Virol. 2010 Aug;84(16):8085-97. doi: 10.1128/JVI.02125-09. Epub 2010 Jun 9.

DOI:10.1128/JVI.02125-09
PMID:20534859
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2916515/
Abstract

Norovirus GII/4 is a leading cause of acute viral gastroenteritis in humans. We examined here how the GII/4 virus evolves to generate and sustain new epidemics in humans, using 199 near-full-length GII/4 genome sequences and 11 genome segment clones from human stool specimens collected at 19 sites in Japan between May 2006 and February 2009. Phylogenetic studies demonstrated outbreaks of 7 monophyletic GII/4 subtypes, among which a single subtype, termed 2006b, had continually predominated. Phylogenetic-tree, bootscanning-plot, and informative-site analyses revealed that 4 of the 7 GII/4 subtypes were mosaics of recently prevalent GII/4 subtypes and 1 was made up of the GII/4 and GII/12 genotypes. Notably, single putative recombination breakpoints with the highest statistical significance were constantly located around the border of open reading frame 1 (ORF1) and ORF2 (P <or= 0.000001), suggesting outgrowth of specific recombinant viruses in the outbreaks. The GII/4 subtypes had many unique amino acids at the time of their outbreaks, especially in the N-term, 3A-like, and capsid proteins. Unique amino acids in the capsids were preferentially positioned on the outer surface loops of the protruding P2 domain and more abundant in the dominant subtypes. These findings suggest that intersubtype genome recombination at the ORF1/2 boundary region is a common mechanism that realizes independent and concurrent changes on the virion surface and in viral replication proteins for the persistence of norovirus GII/4 in human populations.

摘要

诺如病毒 GII/4 是导致人类急性病毒性胃肠炎的主要病原体。本研究通过对 2006 年 5 月至 2009 年 2 月期间,在日本 19 个地点采集的 199 个近乎全长的 GII/4 基因组序列和 11 个基因组片段克隆进行分析,研究了 GII/4 病毒如何进化以在人类中产生和维持新的流行。系统进化研究表明,有 7 个单系的 GII/4 亚型爆发,其中单一亚型,称为 2006b,一直占主导地位。系统进化树、bootscanning-plot 和信息位分析表明,7 个 GII/4 亚型中有 4 个是最近流行的 GII/4 亚型的嵌合体,其中 1 个是由 GII/4 和 GII/12 基因型组成。值得注意的是,在 ORF1(开放阅读框 1)和 ORF2(开放阅读框 2)边界周围始终存在具有最高统计学意义的单个假定重组断点,这表明在爆发中出现了特定的重组病毒。GII/4 亚型在爆发时具有许多独特的氨基酸,尤其是在 N 端、3A 样和衣壳蛋白中。衣壳蛋白中的独特氨基酸优先位于突出的 P2 结构域的外表面环上,并且在优势亚型中更为丰富。这些发现表明,ORF1/2 边界区域的基因间重组是一种常见机制,可实现病毒表面和病毒复制蛋白的独立和并发变化,从而使诺如病毒 GII/4 在人类中持续存在。