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Interactions between bile salts, gut microbiota, and hepatic innate immunity

机译:胆汁盐,肠道微生物肠和肝天生疫苗之间的相互作用

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Summary Bile salts are the water‐soluble end products of hepatic cholesterol catabolism that are released into the duodenum and solubilize lipids due to their amphipathic structure. Bile salts also act as endogenous ligands for dedicated nuclear receptors that exert a plethora of biological processes, mostly related to metabolism. Bile salts are actively reclaimed in the distal part of the small intestine, released into the portal system, and subsequently extracted by the liver. This enterohepatic cycle is critically dependent on dedicated bile salt transporters. In the intestinal lumen, bile salts exert direct antimicrobial activity based on their detergent property and shape the gut microbiota. Bile salt metabolism by gut microbiota serves as a mechanism to counteract this toxicity and generates bile salt species that are distinct from those of the host. Innate immune cells of the liver play an important role in the early recognition and effector response to invading microbes. Bile salts signal primarily via the membrane receptor TGR 5 and the intracellular farnesoid‐x receptor, both present in innate immune cells. In this review, the interactions between bile salts, gut microbiota, and hepatic innate immunity are discussed.
机译:含胆汁盐是肝脏胆固醇分解代谢的水溶性终端产物,其被释放到十二指肠中,并由于其两亲结构而溶解脂质。胆汁盐也充当具有施用过多的生物过程的专用核受体的内源性配体,主要与新陈代谢相关。在小肠的远端部分中积极回收胆汁盐,释放到门户体系中,随后被肝脏提取。这种肠溶循环循环严重依赖于专用的胆汁盐转运蛋白。在肠腔内腔中,胆汁盐基于洗涤剂性能施加直接的抗菌活性并塑造肠道微生物。肠散盐代谢由肠道微生物块用作抵消这种毒性的机制,并产生与宿主中不同的胆汁盐物种。肝脏的先天免疫细胞在早期识别和效应响应对入侵微生物的反应中起重要作用。胆汁盐信号主要通过膜受体TGR 5和细胞内法律-X受体,两者都存在于先天式免疫细胞中。在本文中,讨论了胆汁盐,肠道微生物盐和肝先天免疫之间的相互作用。

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