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2006-2011 年台湾北部地区循环诺如病毒的临床相关性及基因型。

Clinical relevance and genotypes of circulating noroviruses in northern Taiwan, 2006-2011.

机构信息

Graduate Institute of Clinical Medical Sciences, Chang Gung University, Kweishan, Taoyuan, Taiwan.

出版信息

J Med Virol. 2014 Feb;86(2):335-46. doi: 10.1002/jmv.23728. Epub 2013 Sep 5.

Abstract

The incidence of noroviral gastroenteritis has increased dramatically in recent years, and norovirus (NoV) genogroup II.4 (GII.4) is associated with outbreaks worldwide. The NoV genotypes and their clinical relevance in children hospitalized with acute gastroenteritis between 2006 and 2011 in northern Taiwan were evaluated in this study. NoV sequences were amplified from 47 clinical specimens and phylogenetic analysis was performed. Based on noroviral capsid protein (VP1) and RNA dependent RNA polymerase (RdRp) phylogeny, circulating NoV could be divided into GII.2, GII.3, GII.12, and GII.4 and GII.16, GII.12, GII.g, and GII.4; respectively. The GII.4 subtype was predominant and could be divided further into the 2004 (Hunter), 2006b, and 2010 (New Orleans) subtypes. Regarding clinical manifestations, convulsive disorder occurred only in cases caused by NoV GII.4 2006b. Patients affected by NoV GII.4 2006b presented with a higher frequency of diarrhea (P = 0.0204), longer duration of diarrhea (P = 0.0215), more frequent hypoglycemia (P = 0.038), and electrolyte imbalance (P = 0.0487) than acute gastroenteritis caused by NoV GII.4 2010. Structural analysis showed that the amino acid changes in viral VP1 between GII.4 2006b and 2010 subtype were located mainly in the protruding domain 2 (P2 domain). In conclusion, the NoV GII.4 variants 2006b and 2010 were the main causes of acute gastroenteritis in hospitalized children in northern Taiwan during 2006-2011. The clinical presentations and structural changes in VP1 of the two NoV GII.4 variants should be evaluated in the future.

摘要

近年来,诺如病毒胃肠炎的发病率显著上升,诺如病毒(NoV)基因 II.4 组(GII.4)与全球暴发有关。本研究评估了 2006 年至 2011 年台湾北部住院急性胃肠炎患儿中诺如病毒基因型及其临床相关性。从 47 份临床标本中扩增诺如病毒序列,并进行系统进化分析。根据诺如病毒衣壳蛋白(VP1)和 RNA 依赖性 RNA 聚合酶(RdRp)的系统进化,循环诺如病毒可分为 GII.2、GII.3、GII.12 和 GII.4 以及 GII.16、GII.12、GII.g 和 GII.4;分别。GII.4 亚型占优势,可进一步分为 2004 年(猎人)、2006 年 b 型和 2010 年(新奥尔良)亚型。关于临床表现,只有诺如病毒 GII.4 2006b 引起的病例才会出现惊厥。感染诺如病毒 GII.4 2006b 的患者腹泻频率更高(P=0.0204)、腹泻持续时间更长(P=0.0215)、低血糖更频繁(P=0.038)和电解质失衡(P=0.0487)比急性胃肠炎引起的诺如病毒 GII.4 2010 更频繁。结构分析表明,GII.4 2006b 和 2010 亚型病毒 VP1 中的氨基酸变化主要位于突出域 2(P2 域)。总之,2006-2011 年期间,台湾北部住院儿童急性胃肠炎的主要原因是诺如病毒 GII.4 变异体 2006b 和 2010。未来应评估两种 NoV GII.4 变异体在 VP1 中的临床表现和结构变化。

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