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CCR6促进稳态下单核吞噬细胞与肠上皮的结合、印记形成及免疫监视。

CCR6 promotes steady-state mononuclear phagocyte association with the intestinal epithelium, imprinting and immune surveillance.

作者信息

McDonald Keely G, Wheeler Leroy W, McDole Jeremiah R, Joerger Shannon, Gustafsson Jenny K, Kulkarni Devesha H, Knoop Kathryn A, Williams Ifor R, Miller Mark J, Newberry Rodney D

机构信息

Department of Internal Medicine, Washington University School of Medicine, St Louis, MO, USA.

Department of Pathology and Immunology, Washington University School of Medicine, St Louis, MO, USA.

出版信息

Immunology. 2017 Dec;152(4):613-627. doi: 10.1111/imm.12801. Epub 2017 Aug 30.

Abstract

The intestinal lamina propria (LP) contains antigen-presenting cells with features of dendritic cells and macrophages, collectively referred to as mononuclear phagocytes (MNPs). Association of MNPs with the epithelium is thought to play an important role in multiple facets of intestinal immunity including imprinting MNPs with the ability to induce IgA production, inducing the expression of gut homing molecules on T cells, facilitating the capture of luminal antigens and microbes, and subsequent immune responses in the mesenteric lymph node (MLN). However, the factors promoting this process in the steady state are largely unknown, and in vivo models to test and confirm the importance of LP-MNP association with the epithelium for these outcomes are unexplored. Evaluation of epithelial expression of chemoattractants in mice where MNP-epithelial associations were impaired suggested CCL20 as a candidate promoting epithelial association. Expression of CCR6, the only known receptor for CCL20, was required for MNPs to associate with the epithelium. LP-MNPs from CCR6 mice did not display defects in acquiring antigen and stimulating T-cell responses in ex vivo assays or in responses to antigen administered systemically. However, LP-MNPs from CCR6-deficient mice were impaired at acquiring luminal and epithelial antigens, inducing IgA production in B cells, inducing immune responses in the MLN, and capturing and trafficking luminal commensal bacteria to the MLN. These findings identify a crucial role for CCR6 in promoting LP-MNPs to associate with the intestinal epithelium in the steady state to perform multiple functions promoting gut immune homeostasis.

摘要

肠固有层(LP)含有具有树突状细胞和巨噬细胞特征的抗原呈递细胞,统称为单核吞噬细胞(MNP)。MNP与上皮细胞的关联被认为在肠道免疫的多个方面发挥重要作用,包括赋予MNP诱导IgA产生的能力、诱导T细胞上肠道归巢分子的表达、促进腔内抗原和微生物的捕获以及随后在肠系膜淋巴结(MLN)中的免疫反应。然而,在稳态下促进这一过程的因素很大程度上尚不清楚,并且用于测试和证实LP-MNP与上皮细胞的关联对这些结果的重要性的体内模型尚未得到探索。对MNP-上皮细胞关联受损的小鼠中趋化因子上皮表达的评估表明CCL20是促进上皮关联的候选因子。CCL20唯一已知的受体CCR6的表达是MNP与上皮细胞关联所必需的。来自CCR6小鼠的LP-MNP在体外试验中获取抗原和刺激T细胞反应或对全身给予的抗原的反应中未显示出缺陷。然而,来自CCR6缺陷小鼠的LP-MNP在获取腔内和上皮抗原、诱导B细胞产生IgA、在MLN中诱导免疫反应以及捕获和运输腔内共生细菌至MLN方面受损。这些发现确定了CCR6在促进LP-MNP在稳态下与肠道上皮细胞关联以执行促进肠道免疫稳态的多种功能中的关键作用。

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