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Circulating specific antibodies enhance systemic cross-priming by delivery of complexed antigen to dendritic cells in vivo

机译:循环特定抗体增强系统性cross-priming抗原复合体的交付树突细胞在体内

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摘要

Increasing evidence suggests that antibodies can have stimulatory effects on T-cell immunity. However, the contribution of circulating antigen-specific antibodies on MHC class I cross-priming in vivo has not been conclusively established. Here, we defined the role of circulating antibodies in cross-presentation of antigen to CD8 + T cells. Mice with hapten-specific circulating antibodies, but na?ve for the T-cell antigen, were infused with haptenated antigen and CD8 + T-cell induction was measured. Mice with circulating hapten-specific antibodies showed significantly enhanced cross-presentation of the injected antigen compared with mice that lacked these antibodies. The enhanced cross-presentation in mice with circulating antigen-specific antibodies was associated with improved antigen capture by APCs. Importantly, CD11c + APCs were responsible for the enhanced and sustained cross-presentation, although CD11c - APCs had initially captured a significant amount of the injected antigen. Thus, in vivo formation of antigen-antibody immune complexes improves MHC class I cross-presentation, and CD8 + T-cell activation, demonstrating that humoral immunity can aid the initiation of systemic cellular immunity. These findings have important implications for the understanding of the action of therapeutic antibodies against tumor-associated antigens intensively used in the clinic nowadays.
机译:越来越多的证据表明,抗体有刺激对t细胞免疫的影响。然而,循环的贡献我在MHC抗原抗体类cross-priming体内还没有结论建立。在cross-presentation循环抗体CD8 + T细胞抗原。hapten-specific循环抗体,但na吗?t细胞抗原,被注入了haptenated抗原和CD8 + t细胞诱导测量。抗体显示显著增强cross-presentation注射抗原与小鼠相比缺乏这些抗体。增强cross-presentation在老鼠身上循环抗原抗体是与改善相关抗原捕获装甲运兵车。重要的是,CD11c +装甲运兵车负责增强和持续cross-presentation,尽管CD11c——装甲运兵车最初捕获大量的注射抗原。体内抗原抗体免疫的形成复合物改善MHC I类cross-presentation, CD8 + t细胞激活,证明体液免疫可以帮助启动系统的细胞免疫。发现有重要的意义了解治疗的作用针对肿瘤相关抗原的抗体现在集中应用于临床。

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