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Enhanced vaccine-induced CD8+ T cell responses to malaria antigen ME-TRAP by fusion to MHC class ii invariant chain.

机译:通过与MHC II类不变链融合,增强了疫苗诱导的CD8 + T细胞对疟疾抗原ME-TRAP的反应。

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摘要

The orthodox role of the invariant chain (CD74; Ii) is in antigen presentation to CD4+ T cells, but enhanced CD8+ T cells responses have been reported after vaccination with vectored viral vaccines encoding a fusion of Ii to the antigen of interest. In this study we assessed whether fusion of the malarial antigen, ME-TRAP, to Ii could increase the vaccine-induced CD8+ T cell response. Following single or heterologous prime-boost vaccination of mice with a recombinant chimpanzee adenovirus vector, ChAd63, or recombinant modified vaccinia virus Ankara (MVA), higher frequencies of antigen-specific CD4+ and CD8+ T cells were observed, with the largest increases observed following a ChAd63-MVA heterologous prime-boost regimen. Studies in non-human primates confirmed the ability of Ii-fusion to augment the T cell response, where a 4-fold increase was maintained up to 11 weeks after the MVA boost. Of the numerous different approaches explored to increase vectored vaccine induced immunogenicity over the years, fusion to the invariant chain showed a consistent enhancement in CD8+ T cell responses across different animal species and may therefore find application in the development of vaccines against human malaria and other diseases where high levels of cell-mediated immunity are required.
机译:不变链(CD74; II)的正统作用是在抗原呈递给CD4 + T细胞中,但是已经报道了用编码Ii与目的抗原融合体的载体病毒疫苗接种后,CD8 + T细胞应答增强。在这项研究中,我们评估了疟疾抗原ME-TRAP与Ii的融合是否可以增加疫苗诱导的CD8 + T细胞反应。用重组黑猩猩腺病毒载体,ChAd63或重组修饰的痘苗病毒安卡拉(MVA)对小鼠进行单次或异源初免-加强免疫接种后,观察到更高频率的抗原特异性CD4 +和CD8 + T细胞,其中最大的增加是ChAd63-MVA异源初免-加强疗法。对非人类灵长类动物的研究证实了Ii融合能够增强T细胞反应的能力,在MVA增强后的11周内,这种能力一直保持4倍的增长。多年来探索增加载体疫苗诱导的免疫原性的众多不同方法中,与不变链融合显示不同动物物种中CD8 + T细胞反应的持续增强,因此可能在开发针对人类疟疾和其他疾病的疫苗中有所应用需要高水平的细胞介导免疫力的地方。

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