Literature DB >> 7943668

Low frequency of the ADH2*2 allele among Atayal natives of Taiwan with alcohol use disorders.

H R Thomasson1, D W Crabb, H J Edenberg, T K Li, H G Hwu, C C Chen, E K Yeh, S J Yin.   

Abstract

Genetic variation at two polymorphic alcohol dehydrogenase loci, ADH2 and ADH3, and at the polymorphic mitochondrial aldehyde dehydrogenase locus, ALDH2, may influence the risk of developing alcoholism by modulating the rate of elimination of ethanol and the rate of formation and elimination of acetaldehyde. Populations differ in allele frequencies at these loci. We determined the genotypes at all three of these loci in Atayal natives of Taiwan. The frequencies of ADH2*2, ADH3*1, and ALDH2*1 alleles (0.91, 0.99, and 0.95, respectively) were significantly higher among the Atayal than among a predominantly Han Chinese population from Taiwan. Among the Atayal, the group with alcohol use disorders (alcohol dependence and alcohol abuse) had a significantly lower frequency of the ADH2*2 allele (0.82) than those without alcohol use disorders (0.91). The ADH2*2 allele encodes the beta 2 subunit; isozymes containing beta 2 subunits oxidize alcohol faster in vitro than the beta 1 beta 1 isozyme encoded by ADH2*1. Thus, the simplest explanation for these data is that individuals with a beta 2 isozymes have a higher rate of ethanol oxidation, which is a deterrent to alcohol abuse and dependence in some individuals. The Atayal with alcohol use disorders also had a lower frequency of ALDH2*2 than the controls; this allele is known to be responsible for the alcohol-flush reaction among Asians, and thereby deters drinking.

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Year:  1994        PMID: 7943668     DOI: 10.1111/j.1530-0277.1994.tb00923.x

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


  31 in total

1.  Interaction between the functional polymorphisms of the alcohol-metabolism genes in protection against alcoholism.

Authors:  C C Chen; R B Lu; Y C Chen; M F Wang; Y C Chang; T K Li; S J Yin
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2.  Linkage disequilibrium at the ADH2 and ADH3 loci and risk of alcoholism.

Authors:  M Osier; A J Pakstis; J R Kidd; J F Lee; S J Yin; H C Ko; H J Edenberg; R B Lu; K K Kidd
Journal:  Am J Hum Genet       Date:  1999-04       Impact factor: 11.025

3.  Alcohol dehydrogenase and alcohol dependence: variation in genotype-associated risk between populations.

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Journal:  Am J Hum Genet       Date:  2002-11       Impact factor: 11.025

4.  Association of alcohol dehydrogenase genes with alcohol-related phenotypes in a Native American community sample.

Authors:  Ian R Gizer; Howard J Edenberg; David A Gilder; Kirk C Wilhelmsen; Cindy L Ehlers
Journal:  Alcohol Clin Exp Res       Date:  2011-06-02       Impact factor: 3.455

5.  A global perspective on genetic variation at the ADH genes reveals unusual patterns of linkage disequilibrium and diversity.

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Journal:  Am J Hum Genet       Date:  2002-06-05       Impact factor: 11.025

6.  The future of association studies: gene-based analysis and replication.

Authors:  Benjamin M Neale; Pak C Sham
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8.  Diplotype trend regression analysis of the ADH gene cluster and the ALDH2 gene: multiple significant associations with alcohol dependence.

Authors:  Xingguang Luo; Henry R Kranzler; Lingjun Zuo; Shuang Wang; Nicholas J Schork; Joel Gelernter
Journal:  Am J Hum Genet       Date:  2006-04-11       Impact factor: 11.025

9.  Personality traits of agreeableness and extraversion are associated with ADH4 variation.

Authors:  Xingguang Luo; Henry R Kranzler; Lingjun Zuo; Shuang Wang; Joel Gelernter
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10.  Associations of ADH and ALDH2 gene variation with self report alcohol reactions, consumption and dependence: an integrated analysis.

Authors:  Stuart Macgregor; Penelope A Lind; Kathleen K Bucholz; Narelle K Hansell; Pamela A F Madden; Melinda M Richter; Grant W Montgomery; Nicholas G Martin; Andrew C Heath; John B Whitfield
Journal:  Hum Mol Genet       Date:  2008-11-07       Impact factor: 6.150

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