Abstract

Experiments are described with two overall aims. The first is to define the relationship between bile acid (BA) structure, hepatic transport of BA, BA bio-transformation and enterohepatic cycling. The second is to define the influence of BA structure on biliary secretion, i.e. bile volume and secretion of biliary lipids and biliary CA++. To do this, novel BA will be synthesized (C23-nor and C22-bis-nor; amino-alkyl-sulfonate conjugates; and """"""""epimeric"""""""" BA, i.e. BA with 7BetaOH and 12BetaOH groups), such as ursocholic acid. The following physicochemical properties of these BA will be characterized: a) critical micellar concentration (CMC) using surface tension; b) CMC in systems to which a phosphatidyl choline analogue (PCA) has been added; c) solubilizing capacity of novel BA for PCA; d) CMC and solubilizing capacity of selected novel BA for phosphatidyl choline (PC); e) solubilizing capacity of BA-PCA and BA-PC systems for cholesterol. Osmotic activity of these systems will be measured, and the interaction of CA++ with conjugated BA will be defined. Physiological experiments will be carried out using the isolated perfused liver or appropriate animal models to define hepatic transport, biotransformation, and enterohepatic cycling of these novel BA. The enterohepatic circulation of C23 nor and C22 bisnor BA will be defined in experimental animals to show that BA which are not amidated during hepatic transport display prolonged retention in the enterohepatic circulation. Physiological experiments will determine the effects of these novel BA on induced bile flow, biliary lipid secretion, and CA++ secretion in the isolated perfused liver and biliary fistula animal. If successful, these experiments should provide """"""""principles"""""""" of hepatic BA transformation and induced biliary lipid secretion which are applicable to man. They should provide further insight into the mechanism of biliary lipid secretion, and they should aid in the identification of BA structures of potential therapeutic value in man. The long term aim of these studies is the prevention of calculous biliary disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK021506-09
Application #
3227010
Study Section
(GCN)
Project Start
1978-04-01
Project End
1988-03-31
Budget Start
1986-04-01
Budget End
1987-03-31
Support Year
9
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of California San Diego
Department
Type
Schools of Medicine
DUNS #
077758407
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Hofmann, Alan F; Zakko, Salam F; Lira, Marco et al. (2005) Novel biotransformation and physiological properties of norursodeoxycholic acid in humans. Hepatology 42:1391-8
Jover, A; Meijide, F; Soto, Victor H et al. (2004) Successful prediction of the hydrogen bond network of the 3-oxo-12alpha-hydroxy-5beta-cholan-24-oic acid crystal from resolution of the crystal structure of deoxycholic acid and its three 3,12-dihydroxy epimers. Steroids 69:379-88
Meng, Ling-Jie; Wang, Pijun; Wolkoff, Allan W et al. (2002) Transport of the sulfated, amidated bile acid, sulfolithocholyltaurine, into rat hepatocytes is mediated by Oatp1 and Oatp2. Hepatology 35:1031-40
Cantz, T; Nies, A T; Brom, M et al. (2000) MRP2, a human conjugate export pump, is present and transports fluo 3 into apical vacuoles of Hep G2 cells. Am J Physiol Gastrointest Liver Physiol 278:G522-31
Hofmann, A F (1999) The continuing importance of bile acids in liver and intestinal disease. Arch Intern Med 159:2647-58
Gruy-Kapral, C; Little, K H; Fordtran, J S et al. (1999) Conjugated bile acid replacement therapy for short-bowel syndrome. Gastroenterology 116:15-21
Bolder, U; Trang, N V; Hagey, L R et al. (1999) Sulindac is excreted into bile by a canalicular bile salt pump and undergoes a cholehepatic circulation in rats. Gastroenterology 117:962-71
Gerloff, T; Stieger, B; Hagenbuch, B et al. (1998) The sister of P-glycoprotein represents the canalicular bile salt export pump of mammalian liver. J Biol Chem 273:10046-50
Schroeder, A; Eckhardt, U; Stieger, B et al. (1998) Substrate specificity of the rat liver Na(+)-bile salt cotransporter in Xenopus laevis oocytes and in CHO cells. Am J Physiol 274:G370-5
Ricci, P; Hofmann, A F; Hagey, L R et al. (1998) Adjuvant cholylsarcosine during ursodeoxycholic acid treatment of primary biliary cirrhosis. Dig Dis Sci 43:1292-5

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