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单核细胞衍生的树突状细胞上甘露糖受体的交联激活了抗炎性免疫抑制程序。

Cross-linking of the mannose receptor on monocyte-derived dendritic cells activates an anti-inflammatory immunosuppressive program.

作者信息

Chieppa Marcello, Bianchi Giancarlo, Doni Andrea, Del Prete Annalisa, Sironi Marina, Laskarin Gordana, Monti Paolo, Piemonti Lorenzo, Biondi Andrea, Mantovani Alberto, Introna Martino, Allavena Paola

机构信息

Department of Immunology, Istituto Mario Negri, Milan, Italy.

出版信息

J Immunol. 2003 Nov 1;171(9):4552-60. doi: 10.4049/jimmunol.171.9.4552.

Abstract

Immature monocyte-derived dendritic cells (DC) strongly express the endocytic mannose receptor (MR). Addition of a specific anti-MR mAb (clone PAM-1) for 24 h to cultures of immature DC induced phenotypical and functional maturation of the cells, assessed as up-regulation of costimulatory molecules and CD83, and chemotactic response to CCL19. A different isotype-matched anti-MR mAb (clone 19.2) had no significant effect. Engagement of MR with mAb PAM-1 induced the production of the anti-inflammatory cytokines IL-10, IL-1R antagonist, and of the nonsignaling IL-1R type II. In contrast IL-1beta, TNF, and IL-12 were not produced. PAM-1-treated DC were unable to polarize Th1 effector cells and did not secrete the chemokines CXCL10 and CCL19; in turn, they produced large amounts of CCL22 and CCL17, thus favoring the amplification of Th2 circuits. T cells cocultured with PAM-1-matured DC initially proliferated but later became anergic and behaved as suppressor/regulatory cells. Natural ligands binding to MR had differential effects. MUC III (a partially purified mucin), biglycan (a purified complex proteoglycan), and mannosylated lipoarabinomannan from Mycobacterium tuberculosis affected cytokine production with high IL-10, IL-1R antagonist, IL-1R type II, and inhibition of IL-12. In contrast, mannan, dextran, and thyroglobulin had no significant effect. In conclusion, the appropriate engagement of the MR by mAb PAM-1 and selected natural ligands elicit a secretory program in mono-derived DC characterized by a distinct profile of cytokines/chemokines with the ability to dampen inflammation and to inhibit the generation of Th1-polarized immune responses.

摘要

未成熟的单核细胞衍生树突状细胞(DC)强烈表达内吞性甘露糖受体(MR)。向未成熟DC培养物中添加特异性抗MR单克隆抗体(克隆PAM-1)24小时可诱导细胞发生表型和功能成熟,表现为共刺激分子和CD83上调以及对CCL19的趋化反应。另一种同型匹配的抗MR单克隆抗体(克隆19.2)则无显著影响。用单克隆抗体PAM-1使MR结合可诱导抗炎细胞因子IL-10、IL-1R拮抗剂和无信号传导功能的II型IL-1R的产生。相比之下,IL-1β、TNF和IL-12则未产生。经PAM-1处理的DC无法使Th1效应细胞极化,也不分泌趋化因子CXCL10和CCL19;相反,它们产生大量CCL22和CCL17,从而有利于Th2回路的扩增。与经PAM-1成熟的DC共培养的T细胞最初会增殖,但随后会变成无反应状态并表现为抑制/调节性细胞。与MR结合的天然配体具有不同的作用。MUC III(一种部分纯化的粘蛋白)、双糖链蛋白聚糖(一种纯化的复合蛋白聚糖)和来自结核分枝杆菌的甘露糖基化脂阿拉伯甘露聚糖影响细胞因子的产生,可导致IL-10、IL-1R拮抗剂、II型IL-1R水平升高并抑制IL-12。相比之下,甘露聚糖、右旋糖酐和甲状腺球蛋白则无显著影响。总之,单克隆抗体PAM-1和选定的天然配体与MR的适当结合可在单核细胞衍生的DC中引发一个分泌程序,其特征是具有独特的细胞因子/趋化因子谱,能够减轻炎症并抑制Th1极化免疫反应的产生。

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