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Literature DB >> 1982399

Human gastric alcohol dehydrogenase: its inhibition by H2-receptor antagonists, and its effect on the bioavailability of ethanol.

R Hernández-Muñoz¹, J Caballeria, E Baraona, R Uppal, R Greenstein, C S Lieber.

Abstract

Two types of alcohol dehydrogenase isoenzymes (differing in their affinity for ethanol, sensitivity to 4-methylpyrazole, and electrophoretic migration) have been identified in the human stomach. At the high ethanol concentrations prevailing in the gastric lumen during alcohol consumption, the sum of their activities could account for significant oxidation of ethanol. In vitro, these activities were inhibited by cimetidine and ranitidine, but not by famotidine. In vivo, therapeutic doses of cimetidine (but not of famotidine) increased blood ethanol levels when ethanol was given orally, but not when it was given intravenously, indicating a significant contribution of the gastric ADH to the bioavailability and thereby the potential toxicity of ethanol.

Entities: Chemical Disease Gene Species

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Year: 1990 PMID： 1982399 DOI： 10.1111/j.1530-0277.1990.tb01843.x

Source DB: PubMed Journal: Alcohol Clin Exp Res ISSN： 0145-6008 Impact factor: 3.455

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Cited

21 in total

1. Effects of H2-receptor antagonists on gastric alcohol dehydrogenase activity.

Authors: J Caballería; E Baraona; R Deulofeu; R Hernández-Muñoz; J Rodés; C S Lieber
Journal: Dig Dis Sci Date: 1991-12 Impact factor: 3.199

2. Gastroprotection by 4-methylpyrazole against ethanol in humans.

Authors: G Iaquinto; M Del Tacca; L Cuccurullo; M C Parodi; N Giardullo; V D'onofrio; G Natale; D Carignani; F Ferraraccio; S Szabo
Journal: Dig Dis Sci Date: 1998-04 Impact factor: 3.199

Review 3. Pharmacokinetic and pharmacodynamic drug interactions with ethanol (alcohol).

Authors: Lingtak-Neander Chan; Gail D Anderson
Journal: Clin Pharmacokinet Date: 2014-12 Impact factor: 6.447

4. Effect of omeprazole on gastric first-pass metabolism of ethanol.

Authors: R Roine; R Hernández-Muñoz; E Baraona; R Greenstein; C S Lieber
Journal: Dig Dis Sci Date: 1992-06 Impact factor: 3.199

5. First-pass metabolism of alcohol. Absence of diurnal variation and its inhibition by cimetidine after evening meal.

Authors: R Sharma; R T Gentry; R T Lim; C S Lieber
Journal: Dig Dis Sci Date: 1995-10 Impact factor: 3.199

6. Efficacy of famotidine 20 mg twice a day versus 40 mg twice a day in the treatment of erosive or ulcerative reflux esophagitis.

Authors: I C Wesdorp; W Dekker; H P Festen
Journal: Dig Dis Sci Date: 1993-12 Impact factor: 3.199

Human gastric alcohol dehydrogenase: its inhibition by H2-receptor antagonists, and its effect on the bioavailability of ethanol.

1. Effects of H2-receptor antagonists on gastric alcohol dehydrogenase activity.

2. Gastroprotection by 4-methylpyrazole against ethanol in humans.

Review 3. Pharmacokinetic and pharmacodynamic drug interactions with ethanol (alcohol).

4. Effect of omeprazole on gastric first-pass metabolism of ethanol.

5. First-pass metabolism of alcohol. Absence of diurnal variation and its inhibition by cimetidine after evening meal.

6. Efficacy of famotidine 20 mg twice a day versus 40 mg twice a day in the treatment of erosive or ulcerative reflux esophagitis.

7. H2 antagonists and blood alcohol levels.

8. Ranitidine increases the bioavailability of postprandial ethanol by the reduction of first pass metabolism.

9. Lactic acid bacteria prevent alcohol-induced steatohepatitis in rats by acting on the pathways of alcohol metabolism.

10. Glutathione prevents ethanol induced gastric mucosal damage and depletion of sulfhydryl compounds in humans.