Increased Attributable Risk Related to a Functional μ-Opioid Receptor Gene Polymorphism in Association with Alcohol Dependence in Central Sweden

被引:0
|
作者
Gavin Bart
Mary Jeanne Kreek
Jurg Ott
K Steven LaForge
Dmitri Proudnikov
Lotta Pollak
Markus Heilig
机构
[1] The Rockefeller University,The Laboratory of the Biology of Addictive Diseases
[2] Karolinska Institute,The Laboratory of Statistical Genetics
[3] The Rockefeller University,Laboratory of Clinical Science
[4] NIAAA,undefined
[5] NIH,undefined
来源
Neuropsychopharmacology | 2005年 / 30卷
关键词
alcohol dependence; single-nucleotide polymorphism; opioid system; endogenous; association study; opioid receptor;
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中图分类号
学科分类号
摘要
The μ-opioid receptor (MOR), through its effects on reward and stress-responsivity, modulates alcohol intake in both animal and human laboratory studies. We have previously demonstrated that the frequently occurring A118G single-nucleotide polymorphism (SNP) in exon 1 of the MORgene (OPRM1), which encodes an amino-acid substitution, is functional and receptors encoded by the variant 118G allele bind the endogenous opioid peptide β-endorphin with three-fold greater affinity than prototype receptors. Other groups subsequently reported that this variant alters stress-responsivity in normal volunteers and also increases the therapeutic response to naltrexone (a μ-preferring opioid antagonist) in the treatment of alcohol dependence. We compared frequencies of genotypes containing an 118G allele in 389 alcohol-dependent individuals and 170 population-based controls without drug or alcohol abuse or dependence. The A118G SNP was present in the Hardy–Weinberg equilibrium with an overall frequency of the 118G allele of 10.9%. There was a significant overall association between genotypes with an 118G allele and alcohol dependence (p=0.0074). The attributable risk for alcohol dependence in subjects with an 118G allele was 11.1%. There was no difference in A118G genotype between type 1 and type 2 alcoholics. In central Sweden, the functional variant 118G allele in exon 1 of OPRM1 is associated with an increased attributable risk for alcohol dependence.
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页码:417 / 422
页数:5
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