首页> 外文期刊>European Journal of Immunology >Downregulation of microRNA-107 in intestinal CD11c+ myeloid cells in response to microbiota and proinflammatory cytokines increases IL-23p19 expression
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Downregulation of microRNA-107 in intestinal CD11c+ myeloid cells in response to microbiota and proinflammatory cytokines increases IL-23p19 expression

机译:Downregulation肠道的微rna - 107CD11c +髓细胞应对微生物群和促炎细胞因子增加IL-23p19表达式

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摘要

Commensal flora plays an important role in the development of the mucosal immune system and in maintaining intestinal homeostasis. However, the mechanisms involved in regulation of host-microbiota interaction are still not completely understood. In this study, we examined how microbiota and intestinal inflammatory conditions regulate host microRNA expression and observed lower microRNA-107 (miR-107) expression in the inflamed intestines of colitic mice, compared with that in normal control mice. miR-107 was predominantly reduced in epithelial cells and CD11c+ myeloid cells including dendritic cells and macrophages in the inflamed intestines. We demonstrate that IL-6, IFN-γ, and TNF-α downregulated, whereas TGF-β promoted, miR-107 expression. In addition, miR-107 expression was higher in the intestines of germ-free mice than in mice housed under specific pathogen-free conditions, and the presence of microbiota downregulated miR-107 expression in DCs and macrophages in a MyD88- and NF-κB-dependent manner. We determined that the ectopic expression of miR-107 specifically repressed the expression of IL-23p19, a key molecule in innate immune responses to commensal bacteria. We concluded that regulation of miR-107 by intestinal microbiota and proinflammatory cytokine serve as an important pathway for maintaining intestinal homeostasis.
机译:共生的菌群中起着重要的作用粘膜免疫系统的发展维持肠道内稳态。参与的监管机制host-microbiota交互还没有完全理解。微生物群和肠道炎症如何调节宿主微rna表达和条件观察到较低的微rna - 107 (mir - 107)表达式colitic肠道发炎的老鼠,相比之下,在正常控制老鼠。mir - 107在上皮主要是减少了细胞和CD11c +髓细胞包括树突状细胞和巨噬细胞的发炎肠道。肿瘤坏死因子-α表达下调,而TGF -β提拔,mir - 107的表达。表达更高的肠子无菌鼠比老鼠住在特定无菌条件下,的存在微生物群表达下调mir - 107的表达MyD88和DCs和巨噬细胞NF -κB-dependent方式。异位表达mir - 107压抑的表达IL-23p19,一个密钥同桌的先天免疫反应的分子细菌。肠道菌群与促炎细胞因子作为的一个重要途径维持肠道内稳态。

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