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首页> 外文期刊>Frontiers in Immunology >Targeting Mycobacterium tuberculosis Antigens to Dendritic Cells via the DC-Specific-ICAM3-Grabbing-Nonintegrin Receptor Induces Strong T-Helper 1 Immune Responses
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Targeting Mycobacterium tuberculosis Antigens to Dendritic Cells via the DC-Specific-ICAM3-Grabbing-Nonintegrin Receptor Induces Strong T-Helper 1 Immune Responses

机译:通过DC-Specific-ICAM3-Grabbing-Nonintegrin受体将结核分枝杆菌抗原靶向树突状细胞诱导强T辅助1免疫反应。

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Tuberculosis remains a major global health problem and efforts to develop a more effective vaccine have been unsuccessful so far. Targeting antigens (Ags) to dendritic cells (DCs) in vivo has emerged as a new promising vaccine strategy. In this approach, Ags are delivered directly to DCs via antibodies that bind to endocytic cell-surface receptors. Here, we explored DC-specific-ICAM3-grabbing-nonintegrin (DC-SIGN) targeting as a potential vaccine against tuberculosis. For this, we made use of the hSIGN mouse model that expresses human DC-SIGN under the control of the murine CD11c promoter. We show that in vitro and in vivo delivery of anti-DC-SIGN antibodies conjugated to Ag85B and peptide 25 of Ag85B in combination with anti-CD40, the fungal cell wall component zymosan, and the cholera toxin-derived fusion protein CTA1-DD induces strong Ag-specific CD4~(+)T-cell responses. Improved anti-mycobacterial immunity was accompanied by increased frequencies of Ag-specific IFN-γ~(+)IL-2~(+)TNF-α~(+)polyfunctional CD4~(+)T cells in vaccinated mice compared with controls. Taken together, in this study we provide the proof of concept that the human DC-SIGN receptor can be efficiently exploited for vaccine purposes to promote immunity against mycobacterial infections.
机译:结核病仍然是全球主要的健康问题,迄今为止,开发更有效疫苗的努力一直没有成功。在体内将抗原(Ags)靶向树突状细胞(DC)已成为一种新的有前途的疫苗策略。在这种方法中,Ag通过与胞吞细胞表面受体结合的抗体直接递送至DC。在这里,我们探讨了针对DC的ICAM3抢夺型非整联蛋白(DC-SIGN)靶向作为潜在的抗结核疫苗。为此,我们利用了在鼠CD11c启动子控制下表达人DC-SIGN的hSIGN小鼠模型。我们显示结合抗CD40,真菌细胞壁成分zymosan和霍乱毒素衍生的融合蛋白CTA1-DD诱导的结合于Ag85B和Ag85B的肽25的抗DC-SIGN抗体的体外和体内递送诱导强烈的Ag特异性CD4〜(+)T细胞反应。与对照组相比,接种疫苗的小鼠中,抗分枝杆菌免疫力的提高伴随着Ag特异性IFN-γ〜(+)IL-2〜(+)TNF-α〜(+)多功能CD4〜(+)T细胞的频率增加。两者合计,在这项研究中,我们提供了概念上的证明,即人的DC-SIGN受体可以有效地用于疫苗目的,以增强针对分枝杆菌感染的免疫力。

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