Literature DB >> 4683882

Metabolism of steroid and amino acid moieties of conjugated bile acids in man. 3. Cholyltaurine (taurocholic acid).

G W Hepner, J A Sturman, A F Hofmann, P J Thomas.   

Abstract

After oral administration of [2,4-(3)H]-cholyl[(35)S]taurine to eight healthy subjects with indwelling nasoduodenal tubes, the specific activity of the cholyl and taurine moieties and the distribution of radioactivity in biliary bile acid and urinary metabolites, as well as total urinary and fecal (35)S and (3)H, were measured at intervals for 4-8 days. Similar measurements were made after [(35)S]taurine was given orally or intravenously or instilled into the distal intestine. The daily fractional turnover rate of the taurine moiety of cholyltaurine was low and similar to that of the cholyl moiety, indicating that deconjugation occurring during enterohepatic cycling was less than half that previously observed for glycine-conjugated bile acids. Some of the cholyl moiety was absorbed but, since reconjugation occurred predominantly with glycine, little reincorporation into the cholyltaurine pool was observed. Some of the taurine moiety was also absorbed intact but entered large taurine pools, and little reincorporation into the cholyltaurine pool was seen. Oral administration of taurine expanded the cholyltaurine pool and induced a decrease in the fractional turnover rate of the cholyl moiety of cholyltaurine, interpreted to indicate a greater reincorporation of the cholyl moiety because of increased reconjugation with taurine. Taurine moiety not absorbed as taurine appeared to be absorbed largely as sulfate which, like taurine, entered large endogenous pools. Little fecal excretion of (35)S occurred. (35)S was excreted in urine as taurine and sulfate, and excretion in the first 24 h (as percentage of administered dose) correlated highly (r = 0.93) with the daily fractional turnover rate of the taurine moiety. When taurine was instilled into the distal intestine, it appeared as such in plasma, but the more distal the site of instillation, the greater the fraction of urinary (35)S present as sulfate. The [(35)S]sulfate appeared to have come from bacterial degradation of [(35)S]taurine because, when [(35)S]taurine was given intravenously, (35)S was excreted in urine chiefly as [(35)S]taurine with little SO(4)=(-)[(35)S] being present.

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Year:  1973        PMID: 4683882      PMCID: PMC302273          DOI: 10.1172/JCI107200

Source DB:  PubMed          Journal:  J Clin Invest        ISSN: 0021-9738            Impact factor:   14.808


  20 in total

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3.  Degradation of steroids by intestinal bacteria. I. Deconjugation of bile salts.

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6.  The enzymatic cleavage of the carbon-nitrogen bond in 3-alpha, 7-alpha, 12-alpha-trihydroxy-5-beta-cholan-24-oylglycine.

Authors:  P P Nair; M Gordon; J Reback
Journal:  J Biol Chem       Date:  1967-01-10       Impact factor: 5.157

7.  Bacterial modification of taurocholate during enterohepatic recirculation in normal man and patients with small intestinal disease.

Authors:  J T Garbutt; R M Wilkins; L Lack; M P Tyor
Journal:  Gastroenterology       Date:  1970-10       Impact factor: 22.682

8.  Identification of mono- and dihydroxy bile acids in human feces by gas-liquid chromatography and mass spectrometry.

Authors:  P Eneroth; B Gordon; R Ryhage; J Sjövall
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9.  Metabolism of steroid and amino acid moieties of conjugated bile acids in man. II. Glycine-conjugated dihydroxy bile acids.

Authors:  G W Hepner; A F Hofmann; P J Thomas
Journal:  J Clin Invest       Date:  1972-07       Impact factor: 14.808

10.  Dietary glycine and taurine on bile acid conjugation in man; bile acids and steroids 75.

Authors:  J SJOVALL
Journal:  Proc Soc Exp Biol Med       Date:  1959-04
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6.  Active and passive bile acid absorption in man. Perfusion studies of the ileum and jejunum.

Authors:  E Krag; S F Phillips
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7.  Effect of oral chenodeoxycholic acid on bile acid kinetics and biliary lipid composition in women with cholelithiasis.

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8.  Alteration of bile acid metabolism in the rat induced by chronic ethanol consumption.

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10.  Description and simulation of a physiological pharmacokinetic model for the metabolism and enterohepatic circulation of bile acids in man. Cholic acid in healthy man.

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