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Gershon W. Hepner, Alan F. Hofmann, Paul J. Thomas
J Clin Invest. 1972;
51(7):1898
doi:10.1172/JCI106992
Abstract |
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henodeoxycholyl-2,4-3H-glycine-1-14C and deoxycholyl-2,4-3H-glycine-1-14C were synthesized and administered orally to 10 healthy subjects. Distribution of radioactivity among bile acids and specific activity of steroid and amino acid moieties were determined in bile samples. 3H and 14C were measured in feces. 14C in breath was calculated from interval 14CO2 specific activity determinations.The daily fractional turnover of the glycine moiety of chenodeoxycholyl and deoxycholylglycines was more than three times that of the steroid moiety. Pool size of chenodeoxycholylglycine was about twice that of deoxycholylglycine, but similar fractional turnover rates of steroid and amino acid moieties suggested that intestinal absorption of the two conjugated bile acids was equally efficient (about 95%). The amount of unlabeled deoxycholic acid (newly formed by bacterial 7α-dehydroxylation) absorbed from the intestine approximated 30% of the cholic acid that was lost. 3H radioactivity remained predominantly in administered bile acid implying that, normally, secondary bile acids derived from chenodeoxycholic acid are not appreciably absorbed from the intestine and that deoxycholic acid is not hydroxylated by the liver.Approximately 25% of administered 14C was recovered in the breath in the first 24 hr and less than 8% in the feces in 8 days; 14CO2 excretion correlated highly with fractional turnover of the glycine moiety. 3H appeared predominantly in feces, and the rate of excretion correlated highly with the fractional turnover of the steroid moiety of bile acids. From the results in this paper plus previous measurements on the metabolism of cholylglycine, we calculated that about 6 mmoles/day of glycine is used for bile acid conjugation in health.
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(18)
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Comprehensive Physiology
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Comprehensive Physiology
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2011 |
Bile acids: Trying to understand their chemistry and biology with the hope of helping patients
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2009 |
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Review article: epidemiology of gall-bladder disease - role of intestinal transit
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Aliment Pharmacol Ther
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2000 |
Bile acid conjugation in early stage cholestatic liver disease before and during treatment with ursodeoxycholic acid
Mario Fracchia, Kenneth D.R. Setchell, Andrea Crosignani, Mauro Podda, Nancy O'Connell, Roberto Ferraris, Alan F. Hofmann, Giovanni Galatola
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Clinica Chimica Acta
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1996 |
Tauroursodeoxycholate increases rat liver ursodeoxycholate levels and limits lithocholate formation better than ursodeoxycholate
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Gastroenterology
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1995 |
N-ethyl-tauroursodeoxycholic acid, a novel deconjugation-resistant bile salt analogue: Effects of acute feeding in the rat
Mario Angelico, Andrea Mangiameli, Alessandra Nistri, Leonardo Baiocchi, Mara Sofia, Mario Maina, Mario Di Martino, Adriano Blasi
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Hepatology
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1995 |
Deoxycholic acid is not reconverted to cholic acid in humans — a study by isotope ratio mass spectrometry
Sven Fischer, Ulrich Beuers, Frieder Berr, Gustav Paumgartner
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Clinica Chimica Acta
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1991 |
Prevention of ursodeoxycholate hepatotoxicity in the rabbit by conjugation withN-methyl amino acids
Adrian Schmassmann, Alan F. Hofmann, M. Antonietta Angellotti, Huong-Thu Ton-Nu, Claudio D. Schteingart, Carlo Clerici, Steven S. Rossi, Marcus A. Rothschild, Bertram I. Cohen, Richard J. Stenger, Erwin H. Mosbach
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Hepatology
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1990 |
Taurine: an essential nutrient for cats
J. G. Morris, Q. R. Rogers, L. M. Pacioretty
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J Small Animal Practice
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1990 |
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