B.J. Pearlman scite author profile

A B S T R A C T Chenodeoxycholic acid (CDC), through its metabolite, lithocholic acid (LC), is hepatotoxic in certain species. The cause of elevations of serum transaminase in 25% of humans ingesting CDC, however, is unknown, but also may be due to LC. Because efficient hepatic sulfation of LC may protect against hepatic injury, the aim of this study was to determine if sulfation of LC might modify CDCinduced elevations of transaminase. Pretreatment sulfation fraction (SF) was estimated in 63 randomly selected patients with gallstones in a double-blind randomized trial of CDC, 750 mg/d, 375 mg/d, or placebo; in 27 of these, SF was repeated at 1 or 2 yr. In four other patients, the SF was measured at 2 yr only. Serum glutamic oxaloacetic transaminase and serum glutamic pyruvic transaminase were determined monthly for 3 mo and then every 3 or 4 mo; an elevation of transaminase was defined as >150% of the normal upper limit in asymptomatic patients. 10 ,Ci of 3H-glyco-LC (sp act 84 mCi/mol) was ingested 10-12 h before fasting duodenal biliary drainage. Bile acids in bile were separated by thin-layer chromatography. The SF was estimated as a percentage of total radioactivity (scintillation counting) in sulfated glyco-LC. The standard deviation for replicate SF determinations (n = 311) was 2.1% The pretreatment SF (mean 60.7±+1.7 SEM) correlated inversely with age (r = 0.336, P <0.005) and directly with the obesity index (r = 0.495, P > 0.001), but was independent of This work was presented in part at

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Gallstones: The Present and Future of Medical Dissolution

Pearlman

Schoenfield

1978

Medical Clinics of North America

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B.J. Pearlman

Cholesterol gallstone formation and prevention by chenodeoxycholic and ursodeoxycholic acids

Sulfation of Lithocholate as a Possible Modifier of Chenodeoxycholic Acid-induced Elevations of Serum Transaminase in Patients with Gallstones

Gallstones: The Present and Future of Medical Dissolution

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