Literature DB >> 1985938

Purification and characterization of a new alcohol dehydrogenase from human stomach.

A Moreno1, X Parés.   

Abstract

Starch gel electrophoresis of homogenates from human stomach mucosa resolves three alcohol dehydrogenase (ADH) forms: the anodic chi-ADH (class III), the cathodic gamma-ADH (class I), and a new form of slow cathodic mobility that has not been previously characterized. In this work, we describe the purification in three chromatographic steps and the physical and kinetic characterization of this new human alcohol dehydrogenase, which we have named sigma-ADH. The enzyme exhibits the general physicochemical features (Mr, zinc content, subunit Mr, cofactor preference) of all mammalian alcohol dehydrogenases. The kinetic studies show a high Km value (41 mM) and a high kcat value (280 min-1) for ethanol at pH 7.5. The Km decreases as the alcohol increases its chain length. The aldehydes are better substrates than the corresponding alcohols, with m-nitrobenzaldehyde being the best substrate examined. sigma-ADH is strongly inhibited by 4-methylpyrazole, but with a Ki (10 microM) still higher than that for a class I isoenzyme. These properties suggest that sigma-ADH is a class II isoenzyme, different from pi-ADH and similar to that previously described by us in rat stomach. At the high ethanol concentrations in stomach after drinking, sigma-ADH is probably the ADH form with the largest contribution to human gastric ethanol metabolism.

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Year:  1991        PMID: 1985938

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  29 in total

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Authors:  C P Day; M F Bassendine
Journal:  Gut       Date:  1992-11       Impact factor: 23.059

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
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Review 3.  Role of variability in explaining ethanol pharmacokinetics: research and forensic applications.

Authors:  Ake Norberg; A Wayne Jones; Robert G Hahn; Johan L Gabrielsson
Journal:  Clin Pharmacokinet       Date:  2003       Impact factor: 6.447

4.  The vertebrate alcohol dehydrogenase system: variable class II type form elucidates separate stages of enzymogenesis.

Authors:  L Hjelmqvist; M Estonius; H Jörnvall
Journal:  Proc Natl Acad Sci U S A       Date:  1995-11-21       Impact factor: 11.205

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

Authors:  A S Brown; J R Fiaterone; C P Day; M K Bennett; P J Kelly; O F James
Journal:  Gut       Date:  1995-09       Impact factor: 23.059

6.  First pass metabolism of ethanol is strikingly influenced by the speed of gastric emptying.

Authors:  C M Oneta; U A Simanowski; M Martinez; A Allali-Hassani; X Parés; N Homann; C Conradt; R Waldherr; W Fiehn; C Coutelle; H K Seitz
Journal:  Gut       Date:  1998-11       Impact factor: 23.059

7.  Contribution of NADH increases to ethanol's inhibition of retinol oxidation by human ADH isoforms.

Authors:  Jennifer R Chase; Mark G Poolman; David A Fell
Journal:  Alcohol Clin Exp Res       Date:  2009-01-16       Impact factor: 3.455

8.  Activity of class I, II, III, and IV alcohol dehydrogenase isoenzymes in human gastric mucosa.

Authors:  Wojciech Jelski; Lech Chrostek; Maciej Szmitkowski; Wiktor Laszewicz
Journal:  Dig Dis Sci       Date:  2002-07       Impact factor: 3.199

Review 9.  Extrahepatic metabolism of drugs in humans.

Authors:  D R Krishna; U Klotz
Journal:  Clin Pharmacokinet       Date:  1994-02       Impact factor: 6.447

10.  A human alcohol dehydrogenase gene (ADH6) encoding an additional class of isozyme.

Authors:  M Yasunami; C S Chen; A Yoshida
Journal:  Proc Natl Acad Sci U S A       Date:  1991-09-01       Impact factor: 11.205

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