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Review

. 2020 Apr 4;15(3):91-94.

doi: 10.1002/cld.861. eCollection 2020 Mar.

VSports注册入口 - Bile Acid Biology, Pathophysiology, and Therapeutics

John Y L Chiang¹, Jessica M Ferrell¹

Affiliations

PMID: 32257118
PMCID: PMC7128030
DOI: 10.1002/cld.861

Review

Bile Acid Biology, Pathophysiology, and Therapeutics

"VSports app下载" John Y L Chiang et al. Clin Liver Dis (Hoboken). 2020.

. 2020 Apr 4;15(3):91-94.

doi: 10.1002/cld.861. eCollection 2020 Mar.

Authors (VSports注册入口)

John Y L Chiang¹, Jessica M Ferrell¹

"VSports app下载" Affiliation

¹ Department of Integrative Medical Sciences Northeast Ohio Medical University Rootstown OH.

PMID: 32257118
PMCID: PMC7128030
DOI: 10.1002/cld.861

Abstract

http://aasldpubs. onlinelibrary. wiley. com/hub/journal/10. 1002/(ISSN)2046-2484/video/15-3-reading-chiang a video presentation of this article http://aasldpubs. onlinelibrary. wiley. com/hub/journal/10. 1002/(ISSN)2046-2484/video/15-3-interview-chiang an interview with the author. VSports手机版.

© 2020 by the American Association for the Study of Liver Diseases V体育安卓版. .

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Figures

Figure 1
Bile acid synthesis. Bile acids are synthesized from cholesterol in the liver. A total of 17 enzymes located in the cytosol, endoplasmic reticulum, mitochondria, and peroxisomes of hepatocytes are involved in bile acid synthesis. The classic pathway is initiated by the rate‐limiting enzyme, CYP7A1, to synthesize the two primary bile acids in humans, CA and CDCA. CYP8B1 is required for CA synthesis, and mitochondrial CYP27A1 catalyzes a steroid side‐chain oxidation. The alternative pathway is initiated by CYP27A1, followed by CYP7B1. A common precursor of CA and CDCA, C4, is used as a serum marker for bile acid synthesis rate. After synthesis, bile acids are conjugated to the amino acids taurine or glycine for biliary secretion. In the distal ileum and colon, gut bacterial BSH deconjugates the conjugated bile acids, and bacterial 7α‐dehydroxylase removes the 7α‐hydroxyl group to convert CA and CDCA to the secondary bile acids DCA and LCA, respectively. The classic pathway is the major pathway for daily synthesis of about 80% of the bile acids in humans, whereas the alternative pathway synthesizes about 20%. Most bile acids (~95%) are reabsorbed in the ileum and transported via portal blood to the liver to inhibit bile acid synthesis. A small amount of bile acids (~5%) lost in feces is replenished by de novo synthesis.

Figure 2
FXR regulation of bile acid synthesis and enterohepatic circulation of bile acids. In hepatocytes, FXR induces SHP, which inhibits transcription of CYP7A1 and bile acid synthesis. FXR induces BSEP, which actively excretes bile acids into bile. Bile acids also facilitate biliary cholesterol secretion via ATP binding cassette family G5 and G8 transporters (ABCG5, ABCG8). MDR3 (ABCB4) transports phospholipids into bile, whereas MRP2 transports bilirubin, glutathione, and unconjugated bile acids. In the ileum, bile acids are reabsorbed into enterocytes via ASBT. Intestinal FXR induces sinusoidal OSTα/OSTβ heterodimer to efflux bile acids into the portal blood circulation to the liver, where NTCP takes up bile acids into hepatocytes. Intestinal FXR induces FGF19, which circulates to the liver and binds to hepatic FGFR4, inhibiting bile acid synthesis. Bile acids also activate FXR to induce OSTα/OSTβ and MRP4 to efflux bile acids as an adaptive response to cholestasis. FXR induces TGR5 expression in enteroendocrine cells to stimulate secretion of glucagon‐like peptide 1 (GLP‐1), which stimulates insulin secretion from the pancreas and improves insulin sensitivity, and also promotes adipose tissue browning and energy metabolism.

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"VSports在线直播" References

1. Chiang JYL, Ferrell JM. Bile acids as metabolic regulators and nutrient sensors. Annu Rev Nutr. Available at: 10.1146/annurev-nutr-082018-124344. - DOI - PMC - PubMed
1. Chiang JY. Bile acids: regulation of synthesis. J Lipid Res 2009;50:1955‐1966. - PMC (VSports最新版本) - PubMed
1. Hardy T, Oakley F, Anstee QM, et al. Nonalcoholic fatty liver disease: pathogenesis and disease spectrum. Annu Rev Pathol 2016;11:451‐496. - V体育官网 - PubMed
1. Haeusler RA, Astiarraga B, Camastra S, et al. Human insulin resistance is associated with increased plasma levels of 12alpha‐hydroxylated bile acids. Diabetes 2013;62:4184‐4191. - PMC - PubMed
1. Bozadjieva N, Heppner KM, Seeley RJ. Targeting FXR and FGF19 to treat metabolic diseases‐lessons learned from bariatric surgery. Diabetes 2018;67:1720‐1728. - "V体育官网" PMC - PubMed

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