J. Lipid Res.
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Journal of Lipid Research, Vol. 41, 2042-2054, December 2000
Copyright © 2000 by Lipid Research, Inc.

Original Article

Cholesterol, bile acid, and lipoprotein metabolism in two strains of hamster, one resistant, the other sensitive (LPN) to sucrose-induced cholelithiasis

Jacqueline Férézoua, Murielle Combettes-Souveraina, Maâmar Souidia, Jeffery L. Smithb, Nathalie Boehlera, Fabien Milliata, Erik Eckhardtc, Géraldine Blancharda, Michel Riottota, Colette Sérougnea, and Claude Luttona
a Physiologie de la Nutrition, Université Paris-Sud, 91 405 Orsay, France
b Lipid Metabolism Laboratory, Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, 4029 Queensland, Australia
c Brigham and Women's Hospital, Gastrointestinal Division, Boston, MA 02115

Correspondence to: Jacqueline Férézou

A comprehensive study of cholesterol, bile acid, and lipoprotein metabolism was undertaken in two strains of hamster that differed markedly in their response to a sucrose-rich/low fat diet. Under basal conditions, hamsters from the LPN strain differed from Janvier hamsters by a lower cholesterolemia, a higher postprandial insulinemia, a more active cholesterogenesis in both liver [3- to 4-fold higher 3-hydroxy 3-methylglutaryl coenzyme A reductase (HMG-CoAR) activity and mRNA] and small intestine, and a lower hepatic acyl-coenzyme A:cholesterol acyltransferase activity. Cholesterol saturation indices in the gallbladder bile were similar for both strains, but the lipid concentration was 2-fold higher in LPN than in Janvier hamsters. LPN hamsters had a lower capacity to transform cholesterol into bile acids, shown by the smaller fraction of endogenous cholesterol converted into bile acids prior to fecal excretion (0.34 vs. 0.77). In LPN hamsters, the activities of cholesterol 7{alpha}-hydroxylase (C7OHase) and sterol 27-hydroxylase (S27OHase), the two rate-limiting enzymes of bile acid synthesis, were disproportionably lower (by 2-fold) to that of HMG-CoAR. When fed a sucrose-rich diet, plasma lipids increased, dietary cholesterol absorption improved, hepatic activities of HMG-CoA reductase, C7Ohase, and S27OHase were reduced, and intestinal S27OHase was inhibited in both strains. Despite a similar increase in the biliary hydrophobicity index due to the bile acid enrichment in chenodeoxycholic acid and derivatives, only LPN hamsters had an increased lithogenic index and developed cholesterol gallstones (75% incidence), whereas Janvier hamsters formed pigment gallstones (79% incidence).

These studies indicate that LPN hamsters have a genetic predisposition to sucrose-induced cholesterol gallstone formation related to differences in cholesterol and bile acid metabolism. Férézou, J., M. Combettes-Souverain, M. Souidi, J. L. Smith, N. Boehler, F. Milliat, E. Eckhardt, G. Blanchard, M. Riottot, C. Sérougne, and C. Lutton. Cholesterol, bile acid, and lipoprotein metabolism in two strains of hamster, one resistant, the other sensitive (LPN) to sucrose-induced cholelithiasis. J. Lipid Res. 2000. 41: 2042;–2054.

Supplementary key words: bile, SR-BI, sterol 27-hydroxylase, cholesterol 7{alpha}-hydroxylase


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