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首页> 外文期刊>Virology Journal >Recombinant tandem multi-linear neutralizing epitopes of human enterovirus 71 elicited protective immunity in mice
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Recombinant tandem multi-linear neutralizing epitopes of human enterovirus 71 elicited protective immunity in mice

机译:人类肠道病毒71的重组串联多线性中和表位引发小鼠保护性免疫

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Background Human Enterovirus 71 (EV71) has emerged as the leading cause of viral encephalitis in children, especially in the Asia-Pacific regions. EV71 vaccine development is of high priority at present, and neutralization antibodies have been documented to play critical roles during in vitro and in vivo protection against EV71 infection. Results In this study, a novel strategy to produce EV71 vaccine candidate based on recombinant multiple tandem linear neutralizing epitopes (mTLNE) was proposed. The three well identified EV71 linear neutralizing epitopes in capsid proteins, VP1-SP55, VP1-SP70 and VP2-SP28, were sequentially linked by a Gly-Ser linker ((G4S)3), and expressed in E.coli in fusion with the Trx and His tag at either terminal. The recombinant protein mTLNE was soluble and could be purified by standard affinity chromatography. Following three dosage of immunization in adult mice, EV71-specific IgG and neutralization antibodies were readily induced by recombinant mTLNE. IgG subtyping demonstrated that lgG1 antibodies dominated the mTLNE-induced humoral immune response. Especially, cytokine profiling in spleen cells from the mTLNE-immunized mice revealed high production of IL-4 and IL-6. Finally, in vivo challenge experiments showed that passive transfer with anti-mTLNE sera conferred full protection against lethal EV71 challenge in neonatal mice. Conclusion Our results demonstrated that this rational designed recombinant mTLNE might have the potential to be further developed as an EV71 vaccine in the future.
机译:背景技术人类肠道病毒71(EV71)已成为儿童病毒性脑炎的主要原因,尤其是在亚太地区。目前,EV71疫苗的开发非常重要,而且据报道中和抗体在针对EV71感染的体外和体内保护中起着至关重要的作用。结果在这项研究中,提出了一种基于重组多重串联线性中和表位(mTLNE)生产EV71候选疫苗的新策略。衣壳蛋白中的三个可很好识别的EV71线性中和表位VP1-SP55,VP1-SP70和VP2-SP28通过Gly-Ser接头((G 4 S) 3 ),并在E.coli中与Trx和His标签在任一末端融合在一起表达。重组蛋白mTLNE是可溶的,可以通过标准亲和层析纯化。在成年小鼠中进行三剂免疫后,重组mTLNE可以轻松诱导EV71特异性IgG和中和抗体。 IgG亚型证明,IgG1抗体主导了mTLNE诱导的体液免疫反应。尤其是,来自mTLNE免疫小鼠的脾细胞中的细胞因子谱显示出高产量的IL-4和IL-6。最后,体内攻击实验表明,抗mTLNE血清的被动转移赋予新生小鼠抗致命EV71攻击的全面保护。结论我们的结果表明,这种合理设计的重组mTLNE可能会在将来作为EV71疫苗进一步开发。

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