Bile Acid–Mediated Activation of Brown Fat Protects From Alcohol-Induced Steatosis and Liver Injury in Mice

BACKGROUND & AIMS: Alcohol-associated liver disease (AALD) is one of the most common causes of liver injury and failure. Limited knowledge of the mechanisms underlying AALD impedes the development of efficacious therapies. Bile acid (BA) signaling was shown to participate in the progression of A...

Descripción completa

Detalles Bibliográficos
Autores principales: Fan, Mingjie, Wang, Yangmeng, Jin, Lihua, Fang, Zhipeng, Peng, Jiangling, Tu, Jui, Liu, Yanjun, Zhang, Eryun, Xu, Senlin, Liu, Xiaoqian, Huo, Yuqing, Sun, Zhaoli, Chao, Xiaojuan, Ding, Wen-Xing, Yan, Qingfeng, Huang, Wendong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8802063/
https://www.ncbi.nlm.nih.gov/pubmed/34896286
http://dx.doi.org/10.1016/j.jcmgh.2021.12.001
_version_ 1784642594321465344
author Fan, Mingjie
Wang, Yangmeng
Jin, Lihua
Fang, Zhipeng
Peng, Jiangling
Tu, Jui
Liu, Yanjun
Zhang, Eryun
Xu, Senlin
Liu, Xiaoqian
Huo, Yuqing
Sun, Zhaoli
Chao, Xiaojuan
Ding, Wen-Xing
Yan, Qingfeng
Huang, Wendong
author_facet Fan, Mingjie
Wang, Yangmeng
Jin, Lihua
Fang, Zhipeng
Peng, Jiangling
Tu, Jui
Liu, Yanjun
Zhang, Eryun
Xu, Senlin
Liu, Xiaoqian
Huo, Yuqing
Sun, Zhaoli
Chao, Xiaojuan
Ding, Wen-Xing
Yan, Qingfeng
Huang, Wendong
author_sort Fan, Mingjie
collection PubMed
description BACKGROUND & AIMS: Alcohol-associated liver disease (AALD) is one of the most common causes of liver injury and failure. Limited knowledge of the mechanisms underlying AALD impedes the development of efficacious therapies. Bile acid (BA) signaling was shown to participate in the progression of AALD. However, the mechanisms remain poorly understood. METHODS: C57BL/6J wild-type (WT), Takeda G-protein–coupled bile acid receptor 5 (TGR5) knockout (KO) and brown adipose tissue (BAT)-specific TGR5 knockdown mice were subjected to ethanol feeding–induced AALD. Liver samples from alcoholic hepatitis patients were used to examine the BA circulation signaling. Human Embryonic Kidney Cells 293 were used for the TGR5 reporter assay. 23(S)-methyl-lithocholic acid was used as a molecular tool to confirm the regulatory functions of BAT in the AALD mouse model. RESULTS: Ethanol feeding increased the expression of the thermogenesis genes downstream of TGR5 in BAT of WT, but not TGR5 KO, mice. TGR5 deficiency significantly blocked BAT activity and energy expenditure in mice after ethanol feeding. Alcohol increased serum BA levels in mice and human beings through altering BA transportation, and the altered BAs activated TGR5 signaling to regulate metabolism. Compared with ethanol-fed WT mice, ethanol-fed TGR5 KO mice showed less free fatty acid (FFA) β-oxidation in BAT, leading to higher levels of FFA in the circulation, increased liver uptake of FFAs, and exacerbated AALD. BAT-specific TGR5 knockdown mice showed similar results with TGR5 KO mice in AALD. Agonist treatment significantly activated TGR5 signaling in BAT, increased thermogenesis, reduced serum FFA level, and ameliorated hepatic steatosis and injury in AALD mice, while these effects were lost in TGR5 KO mice. CONCLUSIONS: BA signaling plays a protective role in AALD by enhancing BAT thermogenesis. Targeting TGR5 in BAT may be a promising approach for the treatment of AALD.
format Online
Article
Text
id pubmed-8802063
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-88020632022-02-09 Bile Acid–Mediated Activation of Brown Fat Protects From Alcohol-Induced Steatosis and Liver Injury in Mice Fan, Mingjie Wang, Yangmeng Jin, Lihua Fang, Zhipeng Peng, Jiangling Tu, Jui Liu, Yanjun Zhang, Eryun Xu, Senlin Liu, Xiaoqian Huo, Yuqing Sun, Zhaoli Chao, Xiaojuan Ding, Wen-Xing Yan, Qingfeng Huang, Wendong Cell Mol Gastroenterol Hepatol Original Research BACKGROUND & AIMS: Alcohol-associated liver disease (AALD) is one of the most common causes of liver injury and failure. Limited knowledge of the mechanisms underlying AALD impedes the development of efficacious therapies. Bile acid (BA) signaling was shown to participate in the progression of AALD. However, the mechanisms remain poorly understood. METHODS: C57BL/6J wild-type (WT), Takeda G-protein–coupled bile acid receptor 5 (TGR5) knockout (KO) and brown adipose tissue (BAT)-specific TGR5 knockdown mice were subjected to ethanol feeding–induced AALD. Liver samples from alcoholic hepatitis patients were used to examine the BA circulation signaling. Human Embryonic Kidney Cells 293 were used for the TGR5 reporter assay. 23(S)-methyl-lithocholic acid was used as a molecular tool to confirm the regulatory functions of BAT in the AALD mouse model. RESULTS: Ethanol feeding increased the expression of the thermogenesis genes downstream of TGR5 in BAT of WT, but not TGR5 KO, mice. TGR5 deficiency significantly blocked BAT activity and energy expenditure in mice after ethanol feeding. Alcohol increased serum BA levels in mice and human beings through altering BA transportation, and the altered BAs activated TGR5 signaling to regulate metabolism. Compared with ethanol-fed WT mice, ethanol-fed TGR5 KO mice showed less free fatty acid (FFA) β-oxidation in BAT, leading to higher levels of FFA in the circulation, increased liver uptake of FFAs, and exacerbated AALD. BAT-specific TGR5 knockdown mice showed similar results with TGR5 KO mice in AALD. Agonist treatment significantly activated TGR5 signaling in BAT, increased thermogenesis, reduced serum FFA level, and ameliorated hepatic steatosis and injury in AALD mice, while these effects were lost in TGR5 KO mice. CONCLUSIONS: BA signaling plays a protective role in AALD by enhancing BAT thermogenesis. Targeting TGR5 in BAT may be a promising approach for the treatment of AALD. Elsevier 2021-12-09 /pmc/articles/PMC8802063/ /pubmed/34896286 http://dx.doi.org/10.1016/j.jcmgh.2021.12.001 Text en © 2021 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Research
Fan, Mingjie
Wang, Yangmeng
Jin, Lihua
Fang, Zhipeng
Peng, Jiangling
Tu, Jui
Liu, Yanjun
Zhang, Eryun
Xu, Senlin
Liu, Xiaoqian
Huo, Yuqing
Sun, Zhaoli
Chao, Xiaojuan
Ding, Wen-Xing
Yan, Qingfeng
Huang, Wendong
Bile Acid–Mediated Activation of Brown Fat Protects From Alcohol-Induced Steatosis and Liver Injury in Mice
title Bile Acid–Mediated Activation of Brown Fat Protects From Alcohol-Induced Steatosis and Liver Injury in Mice
title_full Bile Acid–Mediated Activation of Brown Fat Protects From Alcohol-Induced Steatosis and Liver Injury in Mice
title_fullStr Bile Acid–Mediated Activation of Brown Fat Protects From Alcohol-Induced Steatosis and Liver Injury in Mice
title_full_unstemmed Bile Acid–Mediated Activation of Brown Fat Protects From Alcohol-Induced Steatosis and Liver Injury in Mice
title_short Bile Acid–Mediated Activation of Brown Fat Protects From Alcohol-Induced Steatosis and Liver Injury in Mice
title_sort bile acid–mediated activation of brown fat protects from alcohol-induced steatosis and liver injury in mice
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8802063/
https://www.ncbi.nlm.nih.gov/pubmed/34896286
http://dx.doi.org/10.1016/j.jcmgh.2021.12.001
work_keys_str_mv AT fanmingjie bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT wangyangmeng bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT jinlihua bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT fangzhipeng bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT pengjiangling bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT tujui bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT liuyanjun bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT zhangeryun bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT xusenlin bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT liuxiaoqian bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT huoyuqing bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT sunzhaoli bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT chaoxiaojuan bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT dingwenxing bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT yanqingfeng bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice
AT huangwendong bileacidmediatedactivationofbrownfatprotectsfromalcoholinducedsteatosisandliverinjuryinmice

Ejemplares similares