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天然 IgM 对早期新抗原识别和适应性免疫的启动至关重要。

Immune Surveillance by Natural IgM Is Required for Early Neoantigen Recognition and Initiation of Adaptive Immunity.

机构信息

1 Department of Pediatrics, National Jewish Health, Denver, Colorado; and.

2 Department of Immunology and Microbiology, University of Colorado, Aurora, Colorado.

出版信息

Am J Respir Cell Mol Biol. 2018 Nov;59(5):580-591. doi: 10.1165/rcmb.2018-0159OC.

Abstract

Early recognition of neoantigen-expressing cells is complex, involving multiple immune cell types. In this study, in vivo, we examined how antigen-presenting cell subtypes coordinate and induce an immunological response against neoantigen-expressing cells, particularly in the absence of a pathogen-associated molecular pattern, which is normally required to license antigen-presenting cells to present foreign or self-antigens as immunogens. Using two reductionist models of neoantigen-expressing cells and two cancer models, we demonstrated that natural IgM is essential for the recognition and initiation of adaptive immunity against neoantigen-expressing cells. Natural IgM antibodies form a cellular immune complex with the neoantigen-expressing cells. This immune complex licenses surveying monocytes to present neoantigens as immunogens to CD4 T cells. CD4 T helper cells, in turn, use CD40L to license cross-presenting CD40 Batf3 dendritic cells to elicit a cytotoxic T cell response against neoantigen-expressing cells. Any break along this immunological chain reaction results in the escape of neoantigen-expressing cells. This study demonstrates the surprising, essential role of natural IgM as the initiator of a sequential signaling cascade involving multiple immune cell subtypes. This sequence is required to coordinate an adaptive immune response against neoantigen-expressing cells.

摘要

早期识别表达新抗原的细胞很复杂,涉及多种免疫细胞类型。在这项研究中,我们在体内研究了抗原呈递细胞亚型如何协调并诱导针对表达新抗原的细胞的免疫反应,特别是在没有病原体相关分子模式的情况下,该模式通常需要赋予抗原呈递细胞呈递外来或自身抗原作为免疫原的能力。使用两种表达新抗原的细胞的简化模型和两种癌症模型,我们证明了天然 IgM 对于识别和启动针对表达新抗原的细胞的适应性免疫反应至关重要。天然 IgM 抗体与表达新抗原的细胞形成细胞免疫复合物。这种免疫复合物赋予了探测单核细胞将新抗原呈递为 CD4 T 细胞免疫原的能力。反过来,CD4 T 辅助细胞利用 CD40L 赋予交叉呈递 CD40 Batf3 树突状细胞以引发针对表达新抗原的细胞的细胞毒性 T 细胞反应的能力。沿着这条免疫连锁反应的任何中断都会导致表达新抗原的细胞逃逸。这项研究表明,天然 IgM 作为涉及多种免疫细胞类型的连续信号级联反应的启动子的惊人的、必要的作用。这个序列是协调针对表达新抗原的细胞的适应性免疫反应所必需的。

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