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首页> 外文期刊>Clinical & translational immunology. >The tetravalent formulation of domain III-capsid proteins recalls memory B- and T-cell responses induced in monkeys by an experimental dengue virus infection
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The tetravalent formulation of domain III-capsid proteins recalls memory B- and T-cell responses induced in monkeys by an experimental dengue virus infection

机译:结构域III衣壳蛋白的四价制剂可回忆起实验性登革热病毒感染猴子诱导的记忆B细胞和T细胞反应

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Tetra DIIIC is a vaccine candidate against dengue virus (DENV) composed by four chimeric proteins that fuse the domain III of the envelope protein of each virus to the corresponding capsid protein. Containing B- and T-cell epitopes, these proteins form aggregates after the incubation with an immunostimulatory oligodeoxynucleotide, and their tetravalent formulation induces neutralizing antibodies and cellular immune response in mice and monkeys. Also, Tetra DIIIC protects mice after challenge with each DENV, and the monovalent formulation obtained from DENV-2 protects monkeys upon homologous viral challenge. However, in the last years, new evidences have arisen regarding domain III of DENV envelope protein as irrelevant target for neutralizing antibodies in humans. Nevertheless, vaccination with domain III induces a neutralizing antibody response that confers protection against re-infection. In addition, it has been demonstrated that the induction of a cellular immune response is essential to protect during the infection. This response can also avoid severe manifestations of dengue disease, associated to the antibody-dependent enhancement of the infection. In this study, we observed that Tetra DIIIC was able to boost the antiviral and neutralizing antibody responses previously generated in monkeys during an experimental DENV infection, demonstrating that domain III is targeted by B cells during the viral infection. Additionally, Tetra DIIIC successfully boosted the cellular immune response generated by the viruses, probably against T-cells epitopes in the capsid proteins. These results highlight the functionality of Tetra DIIIC as a vaccine candidate against DENV.
机译:Tetra DIIIC是针对登革热病毒(DENV)的候选疫苗,该疫苗由四种嵌合蛋白组成,这些融合蛋白将每种病毒的包膜蛋白的结构域III与相应的衣壳蛋白融合。这些蛋白质包含B细胞和T细胞表位,在与免疫刺激性寡脱氧核苷酸孵育后形成聚集体,它们的四价制剂在小鼠和猴子中诱导中和抗体和细胞免疫应答。同样,在用每个DENV攻击后,Tetra DIIIC可以保护小鼠,而从DENV-2获得的单价制剂在同源病毒攻击后可以保护猴子。但是,近年来,关于DENV包膜蛋白的结构域III作为中和人抗体的不相关靶标的新证据出现了。然而,用结构域III进行疫苗接种会诱导中和抗体反应,从而赋予保护以防止再次感染。另外,已经证明诱导细胞免疫应答对于感染期间的保护是必不可少的。该反应还可避免与抗体依赖的感染增强相关的登革热疾病的严重表现。在这项研究中,我们观察到Tetra DIIIC能够增强先前在实验性DENV感染过程中在猴子中产生的抗病毒和中和抗体反应,表明在病毒感染期间B细胞靶向了结构域III。此外,Tetra DIIIC成功地增强了病毒产生的细胞免疫应答,可能针对衣壳蛋白中的T细胞表位。这些结果突出了Tetra DIIIC作为针对DENV的候选疫苗的功能。

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