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首页> 外文期刊>Infection, Genetics and Evolution: Journal of Molecular Epidemiology and Evolutionary Genetics in Infectious Diseases >Genome sequence based molecular epidemiology of unusual US Rotavirus A G9 strains isolated from Omaha, USA between 1997 and 2000
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Genome sequence based molecular epidemiology of unusual US Rotavirus A G9 strains isolated from Omaha, USA between 1997 and 2000

机译:1997年至2000年间从美国奥马哈分离的不寻常的美国轮状病毒A G9株的基于基因组序列的分子流行病学

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After discovery in the early 1980s, Rotavirus A serotype G9 was detected infrequently for almost a decade. Since the mid-1990s, however, serotype G9 has emerged to become a globally common strain linked to the introduction of a single, new genetic variant of G9 VP7 gene. Studies have demonstrated that genetically divergent G9 strains co-circulated at low frequency with the emerging variants. Examples include unique U.S. G9 strains Om46/Hu/USA/1998 and Om67/Hu/USA/1998, isolated in Omaha during the 1997-1998 rotavirus season, that are more closely related phylogenetically to reference strains from the 19805 than to most emerging G9 strains from the U.S. and globally. Here, we sequenced the VP7 full open reading frame for all available G9 strains (n = 12) identified in Omaha during 1996-2000 seasons to investigate their epidemiology and evolution. In addition, the full or partial length open reading frames of the remaining 10 genes for five divergent Om46-like strains and one modern G9 variant were sequenced to evaluate their potential origin. Our findings suggest that Om46-like G9 strains may have been introduced into humans recently, perhaps in 1997-1998 when it was first detected, and the presumed original host of this VP7 gene variant may have been an animal species based on the unexpected detection of porcine rotavirus related NSP2 gene in the genome. The relatively high fitness of Om46-like strains during the 1997-1998 rotavirus season, 1 year after the globally important G9 variant was documented to be already spreading in the study area and other sites of the United States, appears to parallel findings on seasonal replacement of various genetic and antigenic variants of other common human rotavirus antigen specificities.
机译:在1980年代早期发现轮状病毒A血清型G9后,近十年来很少发现它。但是,自1990年代中期以来,血清型G9已成为全球通用的菌株,与引入G9 VP7基因的单个新遗传变异有关。研究表明,遗传分化的G9菌株与新兴变异体在低频下共同流通。例子包括在1997-1998年轮状病毒季节在奥马哈分离出的独特的美国G9菌株Om46 / Hu / USA / 1998和Om67 / Hu / USA / 1998,它们在系统发育上与19805年的参考菌株比在大多数新兴的G9上更密切相关来自美国和全球的菌株。在这里,我们对1996-2000年季节在奥马哈发现的所有可用G9菌株(n = 12)的VP7全开放阅读框进行了测序,以研究其流行病学和演变。此外,对五个不同的Om46样菌株和一个现代G9变体的其余10个基因的全长或部分长度的开放阅读框进行了测序,以评估其潜在起源。我们的发现表明,可能在1997-1998年首次检测到Om46样G9毒株时,已将其引入人体,而这种VP7基因变体的推测原始宿主可能是动物的物种,这是基于意外发现的猪轮状病毒相关基因组中的NSP2基因。在1997-1998年轮状病毒季节(据报道全球重要的G9变体已经在美国的研究区域和其他地方传播了一年)之后的一年,Om46样菌株的适应性相对较高,似乎与季节性更换具有相似的发现其他常见的人类轮状病毒抗原特异性的各种遗传和抗原变异。

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