Abstract

The purpose of this grant is to define the pathogenesis of calcium-containing gallstones in order to develop a rationale for their prevention and medical treatment. Since calcium salts are a major constituent of all pigment stones, precipitation of calcium with various anions (bilirubinate, carbonate, phosphate, 'palmitate') is a clear requisite event in the initiation and growth of pigment gallstones. In addition, since all cholesterol stones have been found to have pigment stone centers, we postulate, as a first major hypothesis, that calcium precipitation is a critical event in the initiation of cholesterol gallstones, so that the latter should be considered a 2-part problem: (1) Precipitation of calcium salts to form a nidus, and (2) precipitation of cholesterol from its supersaturated state on this nidus. According to this view, calcium plays a crucial role in the fomation of both pigment and cholesterol gallstones, and retards or inhibits cholesterol stone dissolution by cheno- or ursodeoxycholic acids. Further elucidation of gallstone formation therefore requires definition and quantification of free Ca++ in bile, the reactive species for precipitation with 'calcium-sensitive' anions. The second major hypothesis is that bile acid anions are the major buffers for Ca++ in bile, and that free [Ca++] is largely governed by calcium complexation with bile salts. The third major hypothesis is that pH plays a key role in determining which of the calcium-sensitive anions will precipitate. The fourth hypothesis to be tested is that the biliary calcium originates primarily at the hepatic canaliculus, and that its secretion is coupled to that of bile acids. The fifth, and most important hypothesis is that gallstones are potentially preventable by prevention of calcium precipitation in bile. Any measure which will reduce free [Ca++] in bile, either by reducing calcium secretion, or by increasing Ca++ complexation, will reduce calcium lithogenicity. The proposed experiments will test these and other specific hypotheses, and will provide the first systematic studies of: (1) Free [Ca++] in bile and bile salt solutions; (2) Ca++-bile salt interactions; (3) The CO2 system in bile and bile salt solutions; and (4) Calcium carbonate and calcium bilirubinate solubilities in bile. The results should lead to new approaches to the medical management and prevention of gallstone disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis, Diabetes, Digestive and Kidney Diseases (NIADDK)
Type
Research Project (R01)
Project #
5R01AM032130-03
Application #
3152430
Study Section
Surgery and Bioengineering Study Section (SB)
Project Start
1983-03-01
Project End
1988-02-29
Budget Start
1985-03-01
Budget End
1986-02-28
Support Year
3
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
Virginia Commonwealth University
Department
Type
Schools of Medicine
DUNS #
City
Richmond
State
VA
Country
United States
Zip Code
23298

  Publications

Shiffman, M L; Carithers Jr, R L; Posner, M P et al. (1991) Recovery of bile secretion following orthotopic liver transplantation. J Hepatol 12:351-61
Dawes, L G; Moore, E W; Rege, R V et al. (1991) Canine bile contains anticrystallization factors that inhibit precipitation of calcium carbonate. Hepatology 14:701-6
D'Agostino, H B; vanSonnenberg, E; Schteingart, C D et al. (1991) Thin-layer chromatography to monitor cholesterol gallstone dissolution by methyl tert-butyl ether. AJR Am J Roentgenol 157:33-6
Rege, R V; Dawes, L G; Moore, E W (1990) Biliary calcium secretion in the dog occurs primarily by passive convection and diffusion and is linked to bile flow. J Lab Clin Med 115:593-602
Rege, R V; Webster, C C; Ostrow, J D (1988) Interactions of unconjugated bilirubin with bile salts. J Lipid Res 29:1289-96
Ostrow, J D; Celic, L; Mukerjee, P (1988) Molecular and micellar associations in the pH-dependent stable and metastable dissolution of unconjugated bilirubin by bile salts. J Lipid Res 29:335-48
Moore, E W; Verine, H J (1987) Pancreatic calcification and stone formation: a thermodynamic model of calcium in pancreatic juice. Am J Physiol 252:G707-18
Rossi, S S; Converse, J L; Hofmann, A F (1987) High pressure liquid chromatographic analysis of conjugated bile acids in human bile: simultaneous resolution of sulfated and unsulfated lithocholyl amidates and the common conjugated bile acids. J Lipid Res 28:589-95
Palmer, K R; Gurantz, D; Hofmann, A F et al. (1987) Hypercholeresis induced by norchenodeoxycholate in biliary fistula rodent. Am J Physiol 252:G219-28
Rege, R V; Webster, C C; Ostrow, J D (1987) Enzymatic oxidation of unconjugated bilirubin to assess its interactions with taurocholate. J Lipid Res 28:673-83

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