Review article: insights into the bile acid‐gut microbiota axis in intestinal failure‐associated liver disease—redefining the treatment approach

肝肠循环 肠道菌群 医学 胆汁酸 肝病 内科学 失调 肠功能衰竭 发病机制 胃肠病学 免疫学 肠外营养
作者
Yaoxuan Wang,Lei Zheng,Zhiyuan Zhou,Danhua Yao,Yuhua Huang,Bin Liu,Yantao Duan,Yousheng Li
出处
期刊:Alimentary Pharmacology & Therapeutics [Wiley]
卷期号:55 (1): 49-63 被引量:8
标识
DOI:10.1111/apt.16676
摘要

Summary Background Intestinal failure‐associated liver disease (IFALD) increases mortality of patients with intestinal failure (IF), but lacks effective prevention or treatment approaches. Bile acids, gut microbiota and the host have close and complex interactions, which play a central role in modulating host immune and metabolic homeostasis. Increasing evidence suggests that derangement of the bile acid‐gut microbiota (BA‐GM) axis contributes to the development of IFALD. Aims To review the BA‐GM axis in the pathogenesis and clinical applications of IFALD, and to explore future directions for effective disease management. Methods We conducted a literature search on bile acid and gut microbiota in IF and liver diseases. Results The BA‐GM axis demonstrates a unique IF signature manifesting as an increase in primary‐to‐secondary bile acids ratio, disturbed enterohepatic circulation, blunted bile acid signalling pathways, gut microbial dysbiosis, and altered microbial metabolic outputs. Bile acids and gut microbiota shape the compositional and functional alterations of each other in IF; collaboratively, they promote immune dysfunction and metabolic aberration in the liver. Diagnostic markers and treatments targeting the BA‐GM axis showed promising potential in the management of IFALD. Conclusions Bile acids and gut microbiota play a central role in the development of IFALD and make attractive biomarkers as well as therapeutic targets. A multitarget, individualised therapy aiming at different parts of the BA‐GM axis may provide optimal clinical benefits and requires future investigation.
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