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在小鼠中,由携带基因型 V 包膜蛋白的减毒 I 型基因为基础的嵌合日本脑炎病毒株引起的毒力和交叉保护作用。

Virulence and Cross-Protection Conferred by an Attenuated Genotype I-Based Chimeric Japanese Encephalitis Virus Strain Harboring the E Protein of Genotype V in Mice.

机构信息

Shanghai Veterinary Research Institute, Chinese Academy of Agricultural Sciences, Shanghai, China.

Yangtze University, Jingzhou, China.

出版信息

Microbiol Spectr. 2022 Dec 21;10(6):e0199022. doi: 10.1128/spectrum.01990-22. Epub 2022 Oct 27.

Abstract

Japanese encephalitis virus (JEV) genotype V (GV) emerged in China in 2009, then South Korea, and has since spread to other regions in Asia and beyond, raising concern about its pathogenicity and the cross-protection offered by JEV vaccines against different genotypes. In this study, we replaced the structural proteins (C-prM-E) of an attenuated genotype I (GI) SD12-F120 strain with those of a virulent GV XZ0934 strain to construct a recombinant chimeric GI-GV JEV (JEV-GI/V) strain to determine the role of the structural proteins in virulence and cross-protection. The recombinant chimeric virus was highly neurovirulent and neuroinvasive in mice. This demonstrated the determinant role of the structural proteins in the virulence of the GV strain. Intracerebral or intraperitoneal inoculation of mice with JEV-GI/V-E5 harboring a combination of substitutions (N47K, L107F, E138K, H123R, and I176R) in E protein, but not mutants containing single substitution of these residues, resulted in decreased or disappeared mortality, suggesting that these residues synergistically, but not individually, played a role in determining the neurovirulence and neuroinvasiveness of the GV strain. Immunization of mice with attenuated strain JEV-GI/V-E5 provided complete protection and induced high neutralizing antibody titers against parental strain JEV-GI/V, but partial cross-protection and low cross-neutralizing antibodies titers against the heterologous GI and GIII strains in mice, suggesting the reduced cross-protection of JEV vaccines among different genotypes. Overall, these findings suggested the essential role of the structural proteins in determination of the virulence of GV strain, and highlighted the need for a novel vaccine against this newly emerged strain. The GV JEV showed an increase in epidemic areas, which exhibited higher pathogenicity in mice than the prevalent GI and GIII strains. We replaced a recombinant chimeric GI-GV JEV (JEV-GI/V) strain to determine the role of the structural proteins in virulence and cross-protection. It was found that the essential role of the structural proteins is to determinethe virulence of the GV strain. It is also suggested that there is reduced cross-protection of JEV vaccines among different genotypes, which provides basic data for subsequent JEV prevention, control, and new vaccine development.

摘要

日本脑炎病毒(JEV)基因型 V(GV)于 2009 年在中国出现,随后在韩国出现,并已传播到亚洲和其他地区,引起了人们对其致病性和 JEV 疫苗对不同基因型的交叉保护作用的关注。在这项研究中,我们用毒力较强的 GV XZ0934 株的结构蛋白(C-prM-E)替换了减毒株基因型 I(GI)SD12-F120 的结构蛋白,构建了重组嵌合 GI-GV JEV(JEV-GI/V)株,以确定结构蛋白在毒力和交叉保护中的作用。重组嵌合病毒在小鼠中具有高度神经毒力和神经侵袭性。这表明结构蛋白在 GV 株的毒力中起决定作用。用含有 N47K、L107F、E138K、H123R 和 I176R 等氨基酸取代的 JEV-GI/V-E5 (E 蛋白中存在组合取代)的嵌合病毒脑内或腹腔接种小鼠,而不是含有这些残基单一取代的突变体,导致死亡率降低或消失,表明这些残基协同作用,而不是单独作用,决定了 GV 株的神经毒力和神经侵袭性。用减毒株 JEV-GI/V-E5 免疫小鼠可提供完全保护,并诱导针对亲本株 JEV-GI/V 的高中和抗体滴度,但在小鼠中对异源 GI 和 GIII 株仅提供部分交叉保护和低中和抗体滴度,表明不同基因型的 JEV 疫苗的交叉保护作用降低。总的来说,这些发现表明结构蛋白在决定 GV 株的毒力方面起着重要作用,并强调需要针对这种新出现的株系开发新型疫苗。GV JEV 的流行地区有所增加,其在小鼠中的致病性高于流行的 GI 和 GIII 株。我们用重组嵌合 GI-GV JEV(JEV-GI/V)株替换了 JEV-GI/V 株,以确定结构蛋白在毒力和交叉保护中的作用。结果发现,结构蛋白在决定 GV 株的毒力方面起着至关重要的作用。这也表明不同基因型的 JEV 疫苗的交叉保护作用降低,为后续的 JEV 预防、控制和新疫苗的开发提供了基础数据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7bfa/9769820/7aabe964b22a/spectrum.01990-22-f001.jpg

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