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Immunization of Zika virus envelope protein domain III induces specific and neutralizing immune responses against Zika virus

机译:Zika病毒包膜蛋白结构域III的免疫诱导针对Zika病毒的特异性和中和免疫应答

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In this study, we described the generation and immunogenicity of the Zika Virus (ZIKV) envelope protein (E) domain III (DIII) as a protein subunit vaccine candidate. ZIKV EDIII (zEDIII) was rapidly produced in E. coli in inclusion bodies. ZIKV EDIII was solubilized, refolded and purified to >95% homogeneity with a one-step Ni2+ affinity chromatography process. Further analysis revealed that zEDIII was refolded properly and demonstrated specific binding to an anti-zEDIII monoclonal antibody that recognizes a zEDIII conformational epitope. Subcutaneous immunization of mice with 25 and 50 mu g of zEDIII was performed over a period of 11 weeks. zEDIII evoked ZIKV-specific and neutralizing antibody response with titers that exceed the threshold that correlates with protective immunity against ZIKV. The antigen-specific IgG isotypes were predominantly IgG1 and splenocyte cultures from immunized mice secreted IFN-gamma, IL-4 and IL-6. Notably, zEDIII-elicited antibodies did not enhance the infection of dengue virus in Fc gamma receptor (Fc gamma R)-expressing cells. This study provided a proof of principle for the further development of recombinant protein-based subunit vaccines against ZIKV. (C) 2017 Elsevier Ltd. All rights reserved.
机译:在该研究中,我们描述了Zika病毒(Zikv)包络蛋白(E)结构域III(DIII)作为蛋白质亚基疫苗候选者的产生和免疫原性。 ZIKV EDIII(Zediii)在包涵体中迅速生产。用一步Ni2 +亲和层析方法溶解,将Zikv Ediii溶解,重新折叠和纯化> 95%均匀性。进一步的分析表明,ZedIII正确折叠并证明了与识别ZediII构象表位的抗ZediII单克隆抗体的特异性结合。在11周的时间内进行25和50μgZediII的皮下免疫小鼠。 Zediii诱发Zikv特异性和中和抗体反应,其滴度超过与ZIKV的保护性免疫相关的阈值。抗原特异性IgG同学主要是来自免疫小鼠的IgG1和脾细胞培养物分泌的IFN-γ,IL-4和IL-6。值得注意的是,Zediii引发的抗体在FCγ受体(Fcγr)-Expring细胞中没有增强登革热病毒的感染。本研究提供了一种原理证明,用于进一步发展对ZIKV的重组蛋白的亚基疫苗。 (c)2017 Elsevier Ltd.保留所有权利。

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