BACKGROUND:Subjective response to alcohol has been examined as a marker of alcoholism risk. The A118G single-nucleotide polymorphism (SNP) of the mu-opioid receptor (OPRM1) gene has been previously associated with subjective response to alcohol in heavy drinkers. This study seeks to extend the literature by examining the effect of OPRM1 genotype on responses to alcohol in a sample of alcohol-dependent individuals. A secondary aim of this study is to examine alcoholism severity as a predictor of subjective responses to alcohol. METHODS:Nontreatment seeking problem drinkers (n = 295) were assessed in the laboratory for clinical dimensions of alcohol dependence. Following prospective genotyping, 43 alcohol-dependent individuals across the 2 genotype conditions (AA, n = 23 and AG/GG, n = 20) were randomized to 2 intravenous infusion sessions: 1 of alcohol (target breath alcohol concentration = 0.06 g/dl) and 1 of saline. Measures of subjective responses to alcohol were administered in both infusion sessions. RESULTS:Alcohol-dependent G-allele carriers reported greater alcohol-induced stimulation, vigor, and positive mood, as compared to A-allele homozygotes. There was no genotype effect on alcohol-induced sedation or craving. There was a statistical trend-level severity × alcohol interaction such that individuals at higher levels of severity reported greater alcohol-induced tension reduction. CONCLUSIONS:These results support the hypothesis that OPRM1 genotype moderates the hedonic effects of alcohol, but not the sedative and unpleasant effects of alcohol, in a sample of alcohol-dependent patients. Results are discussed in light of a clinical neuroscience framework to alcoholism.

译文

背景:对酒精的主观反应已被视为酒精中毒风险的标志。阿片类阿片受体(OPRM1)基因的A118G单核苷酸多态性(SNP)以前与酗酒者对酒精的主观反应有关。这项研究试图通过检查OPRM1基因型对酒精依赖型个体对酒精反应的影响来扩展文献。这项研究的第二个目的是检查酒精中毒的严重程度,以此作为对酒精的主观反应的预测指标。
方法:在实验室评估未寻求治疗的问题饮酒者(n = 295)的酒精依赖临床表现。在进行前瞻性基因分型后,将在2个基因型条件下(AA,n = 23和AG / GG,n = 20)的43个酒精依赖个体随机分配到2个静脉输注阶段:1个酒精(目标呼吸酒精浓度= 0.06 g / dl) )和1的盐水。在两个输液阶段都对酒精的主观反应进行了测量。
结果:与A等位基因纯合子相比,依赖酒精的G等位基因携带者报告了更大的酒精诱导的刺激,活力和积极情绪。对酒精引起的镇静或渴望没有基因型影响。统计趋势级别的严重程度×酒精相互作用,因此,严重程度较高的个人报告说,酒精引起的紧张情绪降低更大。
结论:这些结果支持这样的假设:在一个依赖酒精的患者样本中,OPRM1基因型可减轻酒精的享乐作用,但不会减轻酒精的镇静作用和令人不快的作用。根据酒精中毒的临床神经科学框架讨论了结果。

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