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A novel finding for enterovirus virulence from the capsid protein VP1 of EV71 circulating in mainland China

机译:从在中国大陆传播的EV71衣壳蛋白VP1中发现肠道病毒毒力的新发现

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Enterovirus 71 (EV71) is a neurotropic virus that causes various clinical manifestations in young children, ranging from asymptomatic to fatal. Different pathotypes of EV71 notably differ in virulence. Several virulence determinants of EV71 have been predicted. However, these reported virulence determinants could not be used to identify the EV71 strains of subgenotype C4, which mainly circulate in China. In this study, VP1 sequences of 37 EV71 strains from severe cases (SC-EV71) and 192 EV71 strains from mild cases (MC-EV71) in mainland China were analyzed to determine the potential virulence determinants in the capsid protein VP1 of EV71. Although most SC-EV71 strains belonged to subgenotype C4a, no specific genetic lineages in C4a were correlated with EV71 virulence. Interestingly, amino acid substitutions at nine positions (H22Q, P27S, N31S/D, E98K, E145G/Q, D164E, T240A/S, V249I, and A289T) were detected by aligning the VP1 sequences of the SC-EV71 and MC-EV71 strains. Moreover, both the constituent ratios of the conservative or mutated residues in the MC-EV71 and SC-EV71 strains and the changes in the VP1 3D structure resulting from these mutations confirmed that the conservative residues (22H, 249V, and 289A) and the mutated residues (27S, 31S/D, 98K, 145G/Q, 164E, and 240A/S) might be potential virulence determinants in VP1 of EV71. Furthermore, these results led to the hypothesis that VP1 acts as a sandwich switch for viral particle stabilization and cellular receptors attachment, and specific mutations in this protein can convert mild cases into severe cases. These findings highlight new opportunities for diagnostic and therapeutic interventions.
机译:肠病毒71(EV71)是一种引起神经疾病的病毒,可引起幼儿的各种临床表现,从无症状到致命。 EV71的不同病理型在毒力方面明显不同。 EV71的几种毒力决定因素已被预测。但是,这些报道的毒力决定因素不能用于鉴定主要在中国流行的C4亚型EV71菌株。在这项研究中,分析了中国大陆37例重症病例(SC-EV71)和192轻症病例(MC-EV71)EV71株的VP1序列,以确定EV71衣壳蛋白VP1中的潜在毒力决定因素。尽管大多数SC-EV71菌株属于C4a亚型,但C4a中没有特定的遗传谱系与EV71毒力相关。有趣的是,通过比对SC-EV71和MC-EV71的VP1序列,检测了9个位置(H22Q,P27S,N31S / D,E98K,E145G / Q,D164E,T240A / S,V249I和A289T)的氨基酸取代株。此外,MC-EV71和SC-EV71菌株中保守或突变残基的组成比以及由这些突变导致的VP1 3D结构的变化均证实了保守残基(22H,249V和289A)和突变残留(27S,31S / D,98K,145G / Q,164E和240A / S)可能是EV71 VP1中潜在的毒力决定因素。此外,这些结果导致以下假设:VP1充当病毒颗粒稳定和细胞受体附着的三明治开关,并且该蛋白中的特定突变可将轻度病例转化为严重病例。这些发现突出了诊断和治疗干预的新机会。

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