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炎症在小肠中引发单核细胞分化的即时而非进行性变化。

Inflammation triggers immediate rather than progressive changes in monocyte differentiation in the small intestine.

机构信息

Institute of Molecular Medicine, RWTH Aachen University, D-52074, Aachen, Germany.

Institute of Immunology, Hannover Medical School, D-30625, Hannover, Germany.

出版信息

Nat Commun. 2019 Jul 19;10(1):3229. doi: 10.1038/s41467-019-11148-2.

Abstract

Bone marrow-derived circulating monocytes contribute to the replenishment and maintenance of the intestinal macrophage population. Intestinal monocytes undergo context-dependent phenotypic and functional adaptations to either maintain local immune balance or support intestinal inflammation. Here we use monocyte adoptive transfer to dissect the dynamics of monocyte-to-macrophage differentiation in normal and inflamed small intestine. We find that during homeostasis CCR2 and β7-integrin mediate constitutive homing of monocytes to the gut. By contrast, intestinal inflammation increases monocyte recruitment via CCR2, but not β7-integrin. In the non-inflamed intestine, monocytes gradually differentiate to express genes typically associated with tolerogenic macrophage functions. Conversely, immediately upon entry into the inflamed intestine, monocytes adapt a different expression pattern in a partly Trem-1-dependent manner. Our observations suggest that inflammation fundamentally changes the kinetics and modalities of monocyte differentiation in tissues.

摘要

骨髓来源的循环单核细胞有助于补充和维持肠道巨噬细胞群体。肠道单核细胞会根据具体情况发生表型和功能上的适应性改变,以维持局部免疫平衡或支持肠道炎症。在这里,我们使用单核细胞过继转移来解析正常和炎症状态下小肠中单核细胞向巨噬细胞分化的动态变化。我们发现,在稳态下,CCR2 和 β7 整联蛋白介导单核细胞向肠道的固有归巢。相比之下,肠道炎症通过 CCR2 而不是 β7 整联蛋白增加单核细胞的募集。在非炎症肠道中,单核细胞逐渐分化表达通常与耐受型巨噬细胞功能相关的基因。相反,单核细胞一旦进入炎症肠道,就会以部分 Trem-1 依赖的方式适应不同的表达模式。我们的观察结果表明,炎症从根本上改变了组织中单核细胞分化的动力学和方式。

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