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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Dendritic Cells Control Regulatory T Cell Function Required for Maintenance of Intestinal Tissue Homeostasis
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Dendritic Cells Control Regulatory T Cell Function Required for Maintenance of Intestinal Tissue Homeostasis

机译:树突状细胞控制肠组织稳健所需的调节T细胞功能

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摘要

Dendritic cells (DCs) together with regulatory T cells (Tregs) are essential mediators of immune homeostasis. Disruption of function or frequency of either cell type can lead to fatal autoimmunity. We previously described that mice constitutively lacking DCs (Delta DC) develop autoimmunity characterized by reduced body weight, autoantibodies, and pronounced intestinal inflammation. In this study, we show that lack of DCs leads to an altered gene expression profile in peripheral but not thymic Tregs with increased expression of inhibitory receptors. The suppressive function of Tregs from Delta DC mice was impaired in T cell cocultures. In a model of transfer colitis, Tregs from Delta DC mice were only functional in the presence of DCs in recipient mice. Lack of MHC class II on DCs also resulted in upregulation of inhibitory receptors on Tregs, reduced body weight, and elevated serum IgA levels. Further analysis of the IgA response revealed an expansion of IgA(+) germinal center B cells and plasma cells in mesenteric lymph nodes and more IgA-coated commensal bacteria in feces of Delta DC mice. Thus, we show a critical role for DCs to establish intestinal homeostasis by regulating Treg function for prevention of spontaneous inflammation.
机译:树枝状细胞(DCS)与调节性T细胞(Tregs)是免疫稳态的必需介质。任何细胞类型的功能或频率的破坏都会导致致命的自身免疫。我们以前描述了组成型缺乏DCS(Delta DC)的小鼠的表征体重减轻,自身抗体和明显的肠炎的自身免疫。在这项研究中,我们表明缺乏DCS导致外周中的改变的基因表达谱,而不是具有抑制性受体表达增加的胸腺嘧啶。 Telta DC小鼠的Tregs的抑制函数在T细胞共培养中受到损害。在转移结肠炎的模型中,来自Delta DC小鼠的Tregs仅在受体小鼠的DC存在下起作用。 DCS上的MHC II类II缺乏也导致Tregs,减少体重和血清IgA水平抑制受体上调。进一步分析IGA响应显示IgA(+)发芽中心B细胞和肠系膜淋巴结中的血浆细胞的膨胀和δDC小鼠粪便中的更多IgA涂层的共数细菌。因此,我们对DCS通过调节Treg函数来预防自发性炎症来建立肠道稳态的关键作用。

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