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Literature DB >> 28442273

The role of bile acids in nonalcoholic fatty liver disease and nonalcoholic steatohepatitis.

Monica D Chow¹, Yi-Horng Lee², Grace L Guo³.

Abstract

Nonalcoholic fatty liver disease is growing in prevalence worldwide. It is marked by the presence of macrosteatosis on liver histology but is often clinically asymptomatic. However, it can progress into nonalcoholic steatohepatitis which is a more severe form of liver disease characterized by inflammation and fibrosis. Further progression leads to cirrhosis, which predisposes patients to hepatocellular carcinoma or liver failure. The mechanism by which simple steatosis progresses to steatohepatitis is not entirely clear. However, multiple pathways have been proposed. A common link amongst many of these pathways is disruption of the homeostasis of bile acids. Other than aiding in the absorption of lipids and lipid-soluble vitamins, bile acids act as ligands. For example, they bind to farnesoid X receptor, which is critically involved in many of the pathways responsible for maintaining bile acid, glucose, and lipid homeostasis. Alterations to these pathways can lead to dysregulation of energy balance and increased inflammation and fibrosis. Repeated insults over time may be the key to development of steatohepatitis. For this reason, current drug therapies target aspects of these pathways to try to reduce and halt inflammation and fibrosis. This review will focus on the role of bile acids in these various pathways and how changes in these pathways may result in steatohepatitis. While there is no approved pharmaceutical treatment for either hepatic steatosis or steatohepatitis, this review will also touch upon the multitude of potential therapies.

Entities: Chemical Disease Gene Species

Keywords: Bile acids; Enterohepatic circulation; Farnesoid X receptor (FXR); Gut-liver crosstalk; Nonalcoholic fatty liver disease (NAFLD); Nonalcoholic steatohepatitis (NASH)

Mesh：

Substances：

Year: 2017 PMID： 28442273 PMCID： PMC5812256 DOI： 10.1016/j.mam.2017.04.004

Source DB: PubMed Journal: Mol Aspects Med ISSN： 0098-2997

141 in total

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Journal: J Lipid Res Date: 2016-08-17 Impact factor: 5.922

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Journal: Gastroenterology Date: 2013-05-30 Impact factor: 22.682

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Authors: Eric Kwong; Yunzhou Li; Phillip B Hylemon; Huiping Zhou
Journal: Acta Pharm Sin B Date: 2015-02-09 Impact factor: 11.413

25 in total

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Review 2. Gut Microbiota in Liver Disease: What Do We Know and What Do We Not Know?

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Journal: Physiology (Bethesda) Date: 2020-07-01

3. Cytochrome P450 1A1 (CYP1A1) protects against nonalcoholic fatty liver disease caused by Western diet containing benzo[a]pyrene in mice.

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Journal: Food Chem Toxicol Date: 2018-01-31 Impact factor: 6.023

Review 4. Applying Non-Invasive Fibrosis Measurements in NAFLD/NASH: Progress to Date.

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Journal: Pharmaceut Med Date: 2019-12

5. Ursodeoxycholic acid accelerates bile acid enterohepatic circulation.

Authors: Yunjing Zhang; Runqiu Jiang; Xiaojiao Zheng; Sha Lei; Fengjie Huang; Guoxiang Xie; Sandi Kwee; Herbert Yu; Christine Farrar; Beicheng Sun; Aihua Zhao; Wei Jia
Journal: Br J Pharmacol Date: 2019-07-06 Impact factor: 8.739

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Authors: Xiaohan Xu; Kyle L Poulsen; Lijuan Wu; Shan Liu; Tatsunori Miyata; Qiaoling Song; Qingda Wei; Chenyang Zhao; Chunhua Lin; Jinbo Yang
Journal: Signal Transduct Target Ther Date: 2022-08-13

7. Host Metabolic Response in Early Lyme Disease.

Authors: Bryna L Fitzgerald; Claudia R Molins; M Nurul Islam; Barbara Graham; Petronella R Hove; Gary P Wormser; Linden Hu; Laura V Ashton; John T Belisle
Journal: J Proteome Res Date: 2020-01-09 Impact factor: 4.466

8. SIRT6 controls hepatic lipogenesis by suppressing LXR, ChREBP, and SREBP1.

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Journal: Int J Mol Sci Date: 2018-06-28 Impact factor: 5.923

Review 10. Gut microbiota alterations are distinct for primary colorectal cancer and hepatocellular carcinoma.

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Journal: Protein Cell Date: 2020-08-14 Impact factor: 14.870