Intestine and Innate Immunity

Bioscience and microflora Pub Date : 2009-07-01 DOI:10.12938/BIFIDUS.28.69

S. Uematsu, S. Akira

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Abstract

While the intestinal immune system coexists[DPM1] with commensal bacterial flora through immunological tolerance, invading microorganisms are recognized and properly eliminated. However, it remains unknown what kinds of cells in the intestine initiate immune responses and how they activate host immunity. Recently, we identified a subset of CD11c hi CD11b hi lamina propria (LP) dendritic cells (DCs) as TLR5-expressing cells, which have the ability to activate adaptive immune responses. The LPDCs induced antigen-specific Th17 cells as well as Th1 cells in a TLR5-dependent manner. In addition, they acted on naive B cells to induce their development to immunoglobulin A (IgA) + plasma cells in response to flagellin, and such IgA + plasma cell generation took place in a gut-associated lymphoid tissue (GALT)-independent fashion. Our findings demonstrate unique properties of LPDCs and the importance of TLR5 for adaptive immunity in the intestine. We also generated and examined mutant mice of ATG16L1. ATG16L1 is a component of autophagy machinery and has been reported to be a candidate gene responsible for susceptibility to Crohn's disease. We discuss a novel role for autophagy in the regulation of the inflammatory immune responses in the intestine.

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肠道与先天免疫

肠道免疫系统通过免疫耐受与共生菌群共存[DPM1]，入侵微生物被识别并适当清除。然而，目前尚不清楚肠道中哪种细胞启动免疫反应以及它们如何激活宿主免疫。最近，我们发现CD11c hi CD11b hi固有层(LP)树突状细胞(dc)的一个亚群作为tlr5表达细胞，具有激活适应性免疫反应的能力。LPDCs以tlr5依赖的方式诱导抗原特异性Th17细胞和Th1细胞。此外，它们作用于幼稚B细胞，诱导其发育为免疫球蛋白A (IgA) +浆细胞，以响应鞭毛蛋白，这种IgA +浆细胞的生成以肠道相关淋巴组织(GALT)不依赖的方式发生。我们的研究结果证明了LPDCs的独特特性以及TLR5对肠道适应性免疫的重要性。我们还生成并检测了ATG16L1突变小鼠。ATG16L1是自噬机制的一个组成部分，据报道是导致克罗恩病易感性的候选基因。我们讨论了自噬在肠道炎症免疫反应调节中的新作用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Bioscience and microflora

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