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接种携带基因修饰型寨卡病毒 E 蛋白基因的双血清型重组水疱性口炎病毒疫苗后诱导针对致死性寨卡病毒挑战的保护性免疫应答。

Induction of protective immune responses against a lethal Zika virus challenge post-vaccination with a dual serotype of recombinant vesicular stomatitis virus carrying the genetically modified Zika virus E protein gene.

机构信息

International Vaccine Institute, SNU Research Park, 1 Gwanak-ro, Gwanak-gu, Seoul 08826, Republic of Korea.

Department of Microbiology and Immunology, Schulich School of Medicine and Dentistry, The University of Western Ontario, London, Ontario N6G 2V4, Canada.

出版信息

J Gen Virol. 2021 Apr;102(4). doi: 10.1099/jgv.0.001588.

DOI:10.1099/jgv.0.001588
PMID:33913804
Abstract

The development of a vaccine to prevent Zika virus (ZIKV) infection has been one of the priorities in infectious disease research in recent years. There have been numerous attempts to develop an effective vaccine against ZIKV. It is imperative to choose the safest and the most effective ZIKV vaccine from all candidate vaccines to control this infection globally. We have employed a dual serotype of prime-boost recombinant vesicular stomatitis virus (VSV) vaccine strategy, to develop a ZIKV vaccine candidate, using a type 1 IFN-receptor knock-out () mouse model for challenge studies. Prime vaccination with an attenuated recombinant VSV Indiana serotype (rVSV) carrying a genetically modified ZIKV envelope (E) protein gene followed by boost vaccination with attenuated recombinant VSV New Jersey serotype (rVSV) carrying the same E gene induced robust adaptive immune responses. In particular, rVSV carrying the ZIKV gene with the honeybee melittin signal peptide (msp) at the N terminus and VSV G protein transmembrane domain and cytoplasmic tail (Gtc) at the C terminus of the gene induced strong protective immune responses. This vaccine regimen induced highly potent neutralizing antibodies and T cell responses in the absence of an adjuvant and protected mice from a lethal dose of the ZIKV challenge.

摘要

开发一种预防寨卡病毒(ZIKV)感染的疫苗一直是近年来传染病研究的重点之一。已经有许多尝试开发针对 ZIKV 的有效疫苗。为了控制全球范围内的这种感染,从所有候选疫苗中选择最安全、最有效的 ZIKV 疫苗是至关重要的。我们采用双血清型的初免-加强型重组单纯疱疹病毒(VSV)疫苗策略,使用 1 型干扰素受体敲除()小鼠模型进行挑战研究,开发 ZIKV 疫苗候选物。用携带基因修饰的 ZIKV 包膜(E)蛋白基因的减毒重组 VSV 印第安纳血清型(rVSV)进行初免接种,然后用携带相同 E 基因的减毒重组 VSV 新泽西血清型(rVSV)进行加强接种,诱导了强大的适应性免疫反应。特别是,携带 ZIKV 基因的 rVSV,其 N 端带有蜜蜂蜂毒 melittin 信号肽(msp),C 端带有 VSV G 蛋白跨膜结构域和胞质尾(Gtc),诱导了强烈的保护性免疫反应。这种疫苗方案在没有佐剂的情况下诱导了高效的中和抗体和 T 细胞反应,并保护了小鼠免受 ZIKV 致死剂量的攻击。

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