Farnesoid X receptor is an important target for the treatment of disorders of bile acid and fatty acid metabolism in mice with nonalcoholic fatty liver disease combined with cholestasis

法尼甾体X受体 胆汁淤积 内科学 非酒精性脂肪肝 内分泌学 胆汁酸 医学 脂肪肝 脂质代谢 肝损伤 熊去氧胆酸 脂肪酸代谢 胆盐出口泵 新生儿胆汁淤积症 核受体 生物 新陈代谢 生物化学 运输机 疾病 胆道闭锁 移植 转录因子 肝移植 基因
作者
Xinzhu Liu,Jiaxuan Wang,Maogang Li,Jiannan Qiu,Xingying Li,Li Qi,Jia Liu,Ping Liu,Guoxiang Xie,Xiaoning Wang
出处
期刊:Journal of Gastroenterology and Hepatology [Wiley]
卷期号:38 (8): 1438-1446 被引量:6
标识
DOI:10.1111/jgh.16279
摘要

The prevalence of nonalcoholic fatty liver disease (NAFLD) has been rising globally. NAFLD patients combined with cholestasis have more obvious liver fibrosis, impaired bile acid (BA), and fatty acid (FA) metabolism and severer liver injury; however, its therapeutic options are limited, and the underlying metabolic mechanisms are understood. Here, we aimed to investigate the effects of farnesoid X receptor (FXR) on BA and FA metabolism in NAFLD combined with cholestasis and related signaling pathways.A mouse model of NAFLD combined with cholestasis was established by joint intervention with high-fat diet (HFD) and alpha-naphthylisothiocyanate. The effects of FXR on BA and FA metabolism were evaluated by serum biochemical analysis. Liver damage was identified by histopathology. The expression of nuclear hormone receptor, membrane receptor, FA transmembrane transporter, and BA transporter protein in mice were measured by western blot.NAFLD mice combined with cholestasis developed more severe cholestasis and dysregulated BA and FA metabolism. Meanwhile, the expression of FXR protein was decreased in NAFLD mice combined with cholestasis compared to the controls. Fxr-/- mice showed liver injury. HFD aggravated the liver injury with decreased BSEP expression, increased expression of NTCP, LXRα, SREBP-1c, FAS, ACC1, and CD36, and significantly increased BA and FA accumulation.All the results suggested that FXR plays a key role in both FA and BA metabolism in NAFLD combined with cholestasis and thus may be a potential target for the treatment of disorders of BA and FA metabolism in NAFLD combined with cholestasis.
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