首页> 美国卫生研究院文献>Journal of Clinical Microbiology >Genetic Analyses Reveal Differences in the VP7 and VP4 Antigenic Epitopes between Human Rotaviruses Circulating in Belgium and Rotaviruses in Rotarix and RotaTeq
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Genetic Analyses Reveal Differences in the VP7 and VP4 Antigenic Epitopes between Human Rotaviruses Circulating in Belgium and Rotaviruses in Rotarix and RotaTeq

机译:遗传分析揭示在比利时流行的人类轮状病毒与Rotarix和RotaTeq中的轮状病毒之间VP7和VP4抗原表位的差异

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摘要

Two live-attenuated rotavirus group A (RVA) vaccines, Rotarix (G1P[8]) and RotaTeq (G1-G4, P[8]), have been successfully introduced in many countries worldwide, including Belgium. The parental RVA strains used to generate the vaccines were isolated more than 20 years ago in France (G4 parental strain in RotaTeq) and the United States (all other parental strains). At present, little is known about the relationship between currently circulating human RVAs and the vaccine strains. In this study, we determined sequences for the VP7 and VP4 outer capsid proteins of representative G1P[8], G2P[4], G3P[8], G4P[8], G9P[8], and G12P[8] RVAs circulating in Belgium during 2007 to 2009. The analyses showed that multiple amino acid differences existed between the VP7 and VP4 antigenic epitopes of the vaccine viruses and the Belgian isolates, regardless of their G and P genotypes. However, the highest variability was observed among the circulating G1P[8] RVA strains and the G1 and P[8] components of both RVA vaccines. In particular, RVA strains of the P[8] lineage 4 (OP354-like) showed a significant number of amino acid differences with the P[8] VP4 of both vaccines. In addition, the circulating Belgian G3 RVA strains were found to possibly possess an extra N-linked glycosylation site compared to the G3 RVA vaccine strain of RotaTeq. These results indicate that the antigenic epitopes of RVA strains contained in the vaccines differ substantially from those of the currently circulating RVA strains in Belgium. Over time, these differences might result in selection for strains that escape the RVA neutralizing-antibody pressure induced by vaccines.
机译:Rotarix(G1P [8])和RotaTeq(G1-G4,P [8])两种减毒轮状病毒A组(RVA)疫苗已在包括比利时在内的世界许多国家成功引入。二十多年前,在法国(RotaTeq中的G4亲本菌株)和美国(所有其他亲本菌株)分离出了用于产生疫苗的RVA亲本菌株。目前,关于目前流行的人RVA与疫苗株之间的关系知之甚少。在这项研究中,我们确定了代表性G1P [8],G2P [4],G3P [8],G4P [8],G9P [8]和G12P [8] RVA的VP7和VP4外衣壳蛋白的序列比利时在2007年至2009年期间。分析显示,疫苗病毒的VP7和VP4抗原表位与比利时分离株之间存在多个氨基酸差异,无论它们的G和P基因型如何。但是,在循环的G1P [8] RVA菌株以及两种RVA疫苗的G1和P [8]组分之间观察到最高的变异性。特别是,两种疫苗的P [8]谱系4(OP354-like)的RVA株与P [8] VP4表现出显着的氨基酸差异。此外,发现循环的比利时G3 RVA菌株与RotaTeq的G3 RVA疫苗菌株相比,可能具有额外的N-联糖基化位点。这些结果表明,疫苗中包含的RVA株的抗原表位与比利时目前正在流行的RVA株的抗原表位实质上不同。随着时间的流逝,这些差异可能导致选择摆脱疫苗诱导的RVA中和抗体压力的菌株。

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