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利用由单一共识登革热包膜序列组成的亚单位疫苗来阐述针对登革热病毒的四价抗体反应。

Elaboration of tetravalent antibody responses against dengue viruses using a subunit vaccine comprised of a single consensus dengue envelope sequence.

机构信息

Viral Disease and Vaccine Translational Research Unit, CAS Key Laboratory of Molecular Virology and Immunology, Institut Pasteur of Shanghai, Chinese Academy of Sciences, Shanghai 200025, China.

Viral Disease and Vaccine Translational Research Unit, CAS Key Laboratory of Molecular Virology and Immunology, Institut Pasteur of Shanghai, Chinese Academy of Sciences, Shanghai 200025, China; University of Chinese Academy of Sciences, Beijing 100049, China.

出版信息

Vaccine. 2017 Nov 1;35(46):6308-6320. doi: 10.1016/j.vaccine.2017.09.063. Epub 2017 Oct 4.

DOI:10.1016/j.vaccine.2017.09.063
PMID:28987441
Abstract

Dengue viruses (DENVs) are re-emerging pathogens transmitted by mosquitoes mainly in tropical and subtropical regions. Each year, they are estimated to infect 390 million people globally. The major challenge confronting dengue vaccine development is the need to induce balanced, long lasting tetravalent immune responses against four co-circulating virus serotypes (DENV-I, -II, -III, -IV), because primary infection by any one of which may predispose infected individuals to more severe diseases during a heterotypic secondary infection. Another difficulty is to select representative strains in vaccine design to provide cross-protection against most circulating virus strains. In this study, aimed at developing a tetravalent subunit vaccine with a representative single protein, we designed two vaccines (named cE80(D4) and cE80(max)) based on the consensus sequences of the ectodomain of envelope protein of 3127 DENV strains, and then expressed them in the baculovirus expression system. Both vaccines were capable of eliciting specific antibodies against all four DENV serotypes, and the predominant IgG subtype elicited by the two vaccines was IgG1. Moreover, these vaccines activated both type I and type II antigen-specific helper T cells that secreted IFN-γ and IL-4, respectively. This proof-of-concept study has set foundation for further optimization of a single protein-based tetravalent DENV vaccine.

摘要

登革热病毒(DENV)是主要在热带和亚热带地区通过蚊子传播的重新出现的病原体。据估计,每年有 3.9 亿人感染登革热病毒。登革热疫苗开发面临的主要挑战是需要诱导针对四种循环病毒血清型(DENV-I、-II、-III、-IV)的平衡、持久的四价免疫应答,因为任何一种血清型的初次感染都可能使感染个体在异型二次感染时更容易患上更严重的疾病。另一个困难是选择疫苗设计中的代表性毒株,以提供针对大多数循环病毒株的交叉保护。在这项旨在开发具有代表性的单价蛋白的四价亚单位疫苗的研究中,我们基于 3127 株登革热病毒包膜蛋白外域的共有序列设计了两种疫苗(命名为 cE80(D4)和 cE80(max)),然后在杆状病毒表达系统中表达。两种疫苗都能够针对所有四种登革热病毒血清型诱导特异性抗体,两种疫苗诱导的主要 IgG 亚型为 IgG1。此外,这些疫苗激活了分别分泌 IFN-γ和 IL-4 的 I 型和 II 型抗原特异性辅助 T 细胞。这项概念验证研究为进一步优化单价蛋白基四价登革热疫苗奠定了基础。

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