Abstract

Bile acids are physiological agents required for the absorption, transport and disposal of lipid-soluble vitamins, steroids and xenobiotics. Bile acids are synthesized from cholesterol by two pathways. The major pathway starting with the rate-limiting enzyme, cholesterol 7a-hydroxylase, has been the focus of research. The gene CYP7A is regulated by a complex mechanism. A repressor and an activator region in the promoter have been mapped to contain elements responsive to bile acid, phorbol esters and retinoic acid. Yeast one-hybrid system will be used to isolate DNA-binding proteins isolated. Bile acid feedback is a physiological mechanism which not only inhibits CYP7A but also has a diverse effect on the expression of other lier genes. Imbalance in bile acid metabolism causes malabsorption of nutrients, proliferation of hepatocytes, cholestasis, liver cirrhosis and colon cancer in humans. Polymerase chain reaction based-differential display of mRNAs in hepatocytes will be used to identify genes differentially affected by bile acid. Bile acid synthesis pathway initiated with mitochondrial sterol 27- hydroxylase, and 27-hydorxycholeserol 7a-hydorxylase (oxysterol 7a- hydroxylase) has been uncovered recently. When cholesterol 7a- hydroxylase activity is expressed at a low level in neonatal animals, in liver disease, and in transgenic mice deficient the CYp7a gene, 27- hydroxycholestrerol synthesized in the extrahepatic tissues may be converted to bile acids in the liver as a compensatory mechanism. This pathway also regulate the levels of oxysterols which are potent repressors of cholesterol synthesis and transport. The CYP27 gene mutations have been identified in cerebrotendinous xanthomatosis but regulation of the CYP27 gene is unknown. The hypothesis that both sterol 27-hydorxylase and oxysterol-7a-hydroxylase may play important roles in regulation of bile acid and oxysterol syntheses will tested. Regulatory regions in the CYP27 upstream sequence will be mapped by transient transection assay of CYP27/luciferase reporter genes, DNase I foot printing and gel mobility shift assays. Oxysterol 7a-hydroxylase will be purified and cDNA will be cloned to study its role in the regulation of oxysterols and bile acid syntheses. The long term objective of this research project is to understand molecular mechanisms of regulation of bile acid synthesis and mechanisms of human diseases in bile acid metabolism and cholesterol homeostasis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK044442-06
Application #
2905464
Study Section
Metabolism Study Section (MET)
Program Officer
Serrano, Jose
Project Start
1997-09-30
Project End
2002-09-29
Budget Start
1999-09-30
Budget End
2000-09-29
Support Year
6
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Northeast Ohio Medical University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
City
Rootstown
State
OH
Country
United States
Zip Code
44272

  Publications

Donepudi, Ajay C; Ferrell, Jessica M; Boehme, Shannon et al. (2018) Deficiency of cholesterol 7?-hydroxylase in bile acid synthesis exacerbates alcohol-induced liver injury in mice. Hepatol Commun 2:99-112
Pathak, Preeti; Xie, Cen; Nichols, Robert G et al. (2018) Intestine farnesoid X receptor agonist and the gut microbiota activate G-protein bile acid receptor-1 signaling to improve metabolism. Hepatology 68:1574-1588
Chiang, John Y L; Ferrell, Jessica M (2018) Bile Acid Metabolism in Liver Pathobiology. Gene Expr 18:71-87
Chiang, John Y L (2017) Linking Sex Differences in Non-Alcoholic Fatty Liver Disease to Bile Acid Signaling, Gut Microbiota, and High Fat Diet. Am J Pathol 187:1658-1659
Chiang, John Y L (2017) Linking long noncoding RNA to control bile acid signaling and cholestatic liver fibrosis. Hepatology 66:1032-1035
Chiang, John Y L; Pathak, Preeti; Liu, Hailiang et al. (2017) Intestinal Farnesoid X Receptor and Takeda G Protein Couple Receptor 5 Signaling in Metabolic Regulation. Dig Dis 35:241-245
Chiang, John Y L (2017) Bile acid metabolism and signaling in liver disease and therapy. Liver Res 1:3-9
Pathak, Preeti; Liu, Hailiang; Boehme, Shannon et al. (2017) Farnesoid X receptor induces Takeda G-protein receptor 5 cross-talk to regulate bile acid synthesis and hepatic metabolism. J Biol Chem 292:11055-11069
Donepudi, Ajay C; Boehme, Shannon; Li, Feng et al. (2017) G-protein-coupled bile acid receptor plays a key role in bile acid metabolism and fasting-induced hepatic steatosis in mice. Hepatology 65:813-827
Chiang, John Y L (2017) Targeting bile acids and lipotoxicity for NASH treatment. Hepatol Commun 1:1002-1004

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