Hepatic cytochrome P450 8B1 and cholic acid potentiate intestinal epithelial injury in colitis by suppressing intestinal stem cell renewal
Li Chen, Tingying Jiao, Weiwei Liu, Yuhong Luo, Jue Wang, Xiaozhen Guo, Xiao Tong, Zemin Lin, Chuying Sun, Kanglong Wang, Yifan He, Yuwei Zhang, Hualing Xu, Jiawen Wang, Jianping Zuo, Qiurong Ding, S
Journal:Cell Stem Cell
IF:25.27
DOI:10.1016/j.stem.2022.08.008
PMID:36055192
Published:2022-09-01
research field:植物生物学分子遗传学逆境生理学作物科学
Abstract
Summary Although disrupted bile acid (BA) homeostasis is implicated in inflammatory bowel disease (IBD), the role of hepatic BA metabolism in the pathogenesis of colitis is poorly understood. Here, we found that cholic acid (CA) levels were increased in patients and mice. Cytochrome P450 8B1 (CYP8B1), which synthesizes CA, was induced in livers of colitic mice. CA-treated or liver Cyp8b1 -overexpressing mice developed more severe colitis with compromised repair of the mucosal barrier, whereas Cyp8b1 -knockout mice were resistant to colitis. Mechanistically, CA inhibited peroxisome proliferator-activated receptor alpha (PPARα), resulting in impeded fatty acid oxidation (FAO) and impaired Lgr5 + intestinal stem cell (ISC) renewal. A PPARα agonist restored FAO and improved Lgr5 + ISC function. Activation of the farnesoid X receptor (FXR) suppressed liver CYP8B1 expression and ameliorated colitis in mice. This study reveals a connection between the hepatic CYP8B1-CA axis and colitis via regulating intestinal epithelial regeneration, suggesting that BA-based strategies might be beneficial in IBD treatment.
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