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首页> 外文期刊>Journal of psychiatric research >The CC genotype in the T102C HTR2A polymorphism predicts relapse in individuals after alcohol treatment
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The CC genotype in the T102C HTR2A polymorphism predicts relapse in individuals after alcohol treatment

机译:T102C HTR2A多态性的CC基因型预测酒精治疗后个体复发

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The serotonin system is hypothesized to contribute to predisposition and course of alcohol dependence. However, the potential association between the T102C polymorphism (rs6313) in the type 2A serotonin receptor (HTR2A) gene and treatment outcomes in alcohol dependence has not been investigated. The aim of the study was to assess the contribution of this genetic polymorphism as a predictor of relapse in relation to other previously identified predictors. A sample of 254 alcohol dependent subjects, were recruited in alcohol treatment centers in Warsaw, Poland and prospectively assessed at baseline and follow-up after 12 months. At baseline, information about demographics, psychopathological symptoms and alcohol problems was obtained. The stop-signal task was performed and blood samples for genetic analysis of HTR2A T102C (rs6313) were collected. Relapse was defined as any drinking during the follow-up period. The statistical analysis showed that the CC genotype was significantly associated with increased relapse. Other significant factors were baseline depressive symptoms, number of drinking days during the 3 months prior to the baseline assessment, severity of alcohol-related problems, and a lifetime history of impulsive suicide attempts. Logistic regression analysis with and without the genetic factor revealed that adding the genetic factor increased the R square value by about 4%, with the CC genotype in the T102C polymorphism being the strongest predictor of relapse (OR = 2.32). The significant influence on relapse of the CC genotype, which is associated with fewer 5-HT2A receptors in the central nervous system, suggests the possibility that this genetic polymorphism could influence response to serotonergic medications. ? 2013 Elsevier Ltd.
机译:假定5-羟色胺系统有助于酒精依赖的易感性和病程。但是,尚未研究2A型血清素受体(HTR2A)基因中T102C多态性(rs6313)与酒精依赖治疗结果之间的潜在关联。该研究的目的是评估与其他先前确定的预测因素相比,这种遗传多态性作为复发预测因素的贡献。在波兰华沙的酒精治疗中心招募了254位酒精依赖受试者的样本,并在基线和12个月后的随访中进行了前瞻性评估。在基线时,获得了有关人口统计学,心理病理症状和酒精问题的信息。进行了停止信号任务,并收集了用于HTR2A T102C(rs6313)遗传分析的血液样本。复发定义为在随访期间饮酒。统计分析表明,CC基因型与复发增加显着相关。其他重要因素包括基线抑郁症状,基线评估前3个月的饮酒天数,与酒精有关的问题的严重程度以及一生的脉冲自杀企图。有和没有遗传因素的Logistic回归分析表明,添加遗传因素可使R平方值增加约4%,T102C多态性的CC基因型是复发的最强预测因子(OR = 2.32)。对CC基因型复发的重大影响与中枢神经系统中较少的5-HT2A受体相关,这表明这种基因多态性可能影响对血清素能药物的反应。 ? 2013爱思唯尔有限公司

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