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Antigen Targeting to Dendritic Cells Allows the Identification of a CD4 T-Cell Epitope within an Immunodominant Trypanosoma cruzi Antigen

机译:靶向树突状细胞的抗原允许在免疫性锥虫克鲁兹抗原中的CD4 T细胞表位的鉴定。

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摘要

Targeting antigens to dendritic cells (DCs) by using hybrid monoclonal antibodies (mAbs) directed against DC receptors is known to improve activation and support long-lasting T cell responses. in the present work, we used the mAb alpha DEC205 fused to the Trypanosoma cruzi amastigote surface protein 2 (ASP-2) to identify a region of this protein recognized by specific T cells. the hybrid alpha DEC-ASP2 mAb was successfully generated and preserved its ability to bind the DEC205 receptor. Immunization of BALB/c mice with the recombinant mAb in the presence of polyriboinosinic: polyribocytidylic acid (poly (I:C)) specifically enhanced the number of IFN-gamma producing cells and CD4+ T cell proliferation when compared to mice immunized with a mAb without receptor affinity or with the non-targeted ASP-2 protein. the strong immune response induced in mice immunized with the hybrid alpha DEC-ASP2 mAb allowed us to identify an ASP-2-specific CD4+ T cell epitope recognized by the BALB/c MHCII haplotype. We conclude that targeting parasite antigens to DCs is a useful strategy to enhance T cell mediated immune responses facilitating the identification of new T-cell epitopes.
机译:已知通过使用针对DC受体的杂交单克隆抗体(mAb)将抗原靶向树突细胞(DCs),可以改善激活并支持持久的T细胞应答。在目前的工作中,我们使用了与克氏锥虫假单胞菌表面蛋白2(ASP-2)融合的mAb alpha DEC205,以鉴定该蛋白被特定T细胞识别的区域。杂种αDEC-ASP2 mAb成功生成并保留了其与DEC205受体结合的能力。与未用mAb进行免疫的小鼠相比,在多核糖苷酸:多核糖酸(poly(I:C))存在下,用重组mAb对BALB / c小鼠进行免疫可显着增强IFN-γ产生细胞的数量和CD4 + T细胞的增殖。受体亲和力或与非靶向ASP-2蛋白的亲和力。在使用杂种αDEC-ASP2 mAb免疫的小鼠中诱导的强免疫应答使我们能够鉴定出BALB / c MHCII单倍型识别的ASP-2特异性CD4 + T细胞表位。我们得出的结论是,将寄生虫抗原靶向DC是增强T细胞介导的免疫应答,促进新T细胞表位鉴定的有用策略。

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