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Genotype diversity and molecular evolution of noroviruses: A 30-year (1982-2011) comprehensive study with children from Northern Brazil

机译:诺如病毒的基因型多样性和分子进化:一项针对巴西北部儿童的为期30年(1982年至2011年)的综合研究

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摘要

A chronologically comprehensive 30-year study was conducted that involved children living in Belém, in the Amazon region of Northern Brazil, who participated in eight different studies from October 1982 to April 2011. The children were followed either in the community or in health units and hospitals in order to identify the norovirus genotypes involved in infections during this time. A total of 2,520 fecal specimens were obtained and subjected to RT-PCR and nucleotide sequencing for regions A, B, C, D and P2 of the viral genome. An overall positivity of 16.9% (n = 426) was observed, and 49% of the positive samples were genotyped (208/426), evidencing the presence of several genotypes as follows: Polymerase gene (GI.P4, GII.Pa, GII.Pc, GII.Pe, GII.Pg, GII.Pj, GII.P3, GII.P4, GII.P6, GII.P7, GII.P8, GII.P12, GII.P13, GII.P14, GII.P21, GII.P22), and VP1 gene (GI.3, GI.7, GII.1, GII.2, GII.3, GII.4, GII.6, GII.7, GII.8, GII.10, GII.12, GII.14, GII.17, GII.23). The GII.P4/GII.4 genotype determined by both open reading frames (ORFs) (partial polymerase and VP1 genes) was found for 83 samples, and analyses of the subdomain P2 region showed 10 different variants: CHDC (1970s), Tokyo (1980s), Bristol_1993, US_95/96, Kaiso_2003, Asia_2003, Hunter_2004, Yerseke_2006a, Den Haag_2006b (subcluster “O”) and New Orleans_2009. Recombination events were confirmed in 47.6% (n = 20) of the 42 samples with divergent genotyping by ORF1 and ORF2 and with probable different breakpoints within the viral genome. The evolutionary analyses estimated a rate of evolution of 1.02 x 10−2 and 9.05 x 10−3 subs./site/year using regions C and D from the VP1 gene, respectively. The present research shows the broad genetic diversity of the norovirus that infected children for 30 years in Belém. These findings contribute to our understanding of noroviruses molecular epidemiology and viral evolution and provide a baseline for vaccine design.
机译:进行了一项按时间顺序进行的为期30年的综合研究,研究对象为居住在巴西北部亚马逊地区贝伦的儿童,他们从1982年10月至2011年4月参加了八项不同的研究。这些儿童在社区或卫生部门得到了随访。为了确定在此期间感染涉及的诺如病毒基因型,需要医院检查。总共获得了2,520个粪便标本,并对病毒基因组的A,B,C,D和P2区域进行了RT-PCR和核苷酸测序。观察到总体阳性率为16.9%(n = 426),并对49%的阳性样品进行了基因分型(208/426),证明存在以下几种基因型:聚合酶基因(GI.P4,GII.Pa,GII .Pc,GII.Pe,GII.Pg,GII.Pj,GII.P3,GII.P4,GII.P6,GII.P7,GII.P8,GII.P12,GII.P13,GII.P14,GII.P21 ,GII.P22)和VP1基因(GI.3,GI.7,GII.1,GII.2,GII.3,GII.4,GII.6,GII.7,GII.8,GII.10, GII.12,GII.14,GII.17,GII.23)。发现了由两个开放阅读框(ORF)(部分聚合酶和VP1基因)确定的GII.P4 / GII.4基因型,共有83个样品,对亚域P2区的分析显示10种不同的变体:CHDC(1970s),Tokyo( 1980年代),布里斯托尔1993年,美国95/96年,凯索2003年,亚洲2003年,亨特2004年,耶尔塞克2006a,海格2006b(“ O”类)和新奥尔良2009年。在42个样本中,有47.6%(n = 20)发生重组事件,其中ORF1和ORF2的基因分型不同,病毒基因组中可能存在不同的断裂点。进化分析估计,使用VP1基因的C和D区域,每个位点/年的进化速率为1.02 x 10 −2 和9.05 x 10 −3 单位/年。分别。本研究显示了在贝伦感染儿童30年的诺如病毒的广泛遗传多样性。这些发现有助于我们对诺如病毒分子流行病学和病毒进化的了解,并为疫苗设计提供了基线。

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