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首页> 外文期刊>Cell Reports >A Gorilla Adenovirus-Based Vaccine against Zika Virus Induces Durable Immunity and Confers Protection in Pregnancy
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A Gorilla Adenovirus-Based Vaccine against Zika Virus Induces Durable Immunity and Confers Protection in Pregnancy

机译:基于Gorilla腺病毒的疫苗对Zika病毒诱导耐用的免疫力和赋予怀孕的保护

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The teratogenic potential of Zika virus (ZIKV) has made the development of an effective vaccine a global health priority. Here, we generate two gorilla adenovirus-based ZIKV vaccines that encode for pre-membrane (prM) and envelope (E) proteins (GAd-Zvp) or prM and the ectodomain of E protein (GAd-Eecto). Both vaccines induce humoral and cell-mediated immune responses and prevent lethality after ZIKV challenge in mice. Protection is antibody dependent, CD8sup+/sup T?cell independent, and for GAd-Eecto requires the complement component C1q. Immunization of GAd-Zvp induces antibodies against a key neutralizing epitope on domain III of E protein and confers durable protection as evidenced by memory B and long-lived plasma cell responses and challenge studies 9?months later. In two models of ZIKV infection during pregnancy, GAd-Zvp prevents maternal-to-fetal transmission. The gorilla adenovirus-based vaccine platform encoding full-length prM and E genes is a promising candidate for preventing congenital ZIKV syndrome and possibly infection by other flaviviruses.
机译:Zika病毒(ZIKV)的致畸潜力使得开发有效的疫苗全球卫生优先权。在这里,我们生成两种基于腺病毒的Zikv疫苗,其编码用于预膜(PRM)和包膜(E)蛋白(GAD-ZVP)或PRM和E蛋白(GAD-EECTO)的突出瘤。疫苗诱导患有液体和细胞介导的免疫反应,并在小鼠中撒尿攻击后预防致命性。保护是抗体依赖性的,CD8 + t?细胞无关,并且对于GAD-eecto需要补体组分C1Q。 GAD-ZVP的免疫诱导E蛋白域III结构域III的键中和表位的抗体,并赋予耐用的保护,如记忆B和长寿命的血浆细胞应答和攻击研究9?几个月后。在怀孕期间的两种模型的ZIKV感染,Gad-ZVP防止母体传输。编码全长PRM和E基因的基于Gorilla腺病毒的疫苗平台是预防先天性Zikv综合征并可能被其他黄病毒感染的有希望的候选者。

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