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5-HTTLPR genotype and daily negative mood moderate the effects of sertraline on drinking intensity

机译:5-HTTLPR基因型和每日负面情绪可减轻舍曲林对饮酒强度的影响

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摘要

We previously reported moderating effects of age of onset of alcohol dependence (AD) and a functional polymorphism (5-HTTLPR) in the gene encoding the serotonin transporter protein in a sample of 134 individuals participating in a 12-week, placebo-controlled trial of sertraline. To understand more fully the effects seen in that study, we examined moderation by negative moods reported each evening, with nighttime drinking intensity (i.e. the number of standard drinks consumed at night) as the dependent variable. We found a daily anxiety × age of onset × 5-HTTLPR polymorphism × medication interaction, which reflected a daily anxiety × medication group effect for early-onset individuals homozygous for the high-expression (L′) allele, but not others. Specifically, on days characterized by relatively high levels of anxiety, early-onset L′ homozygotes receiving placebo reduced their drinking intensity significantly. In contrast, early-onset L′ homozygotes treated with sertraline non-significantly increased their drinking intensity. These findings implicate anxiety as a key moderator of the observed pharmacogenetic effects. These findings have important implications because of the high prevalence of AD and the frequency with which SSRIs are prescribed to treat the disorders.
机译:我们先前曾在参与一项为期12周的安慰剂对照试验的134位个体的样本中报告了酒精依赖(AD)发作年龄和功能性多态性(5-HTTLPR)编码5-羟色胺转运蛋白的基因中的调节作用。舍曲林。为了更全面地了解该研究中看到的效果,我们以夜间饮酒强度(即夜间饮用的标准饮料数量)作为因变量,检查了每天晚上报道的负面情绪的缓解程度。我们发现每日焦虑×发病年龄×5-HTTLPR多态性×药物相互作用,这反映了对于高表达(L')等位基因纯合的早期发作个体的每日焦虑×药物组效应,但对其他个体则没有。具体而言,在以相对较高的焦虑水平为特征的日子里,接受安慰剂的早发型L'纯合子会显着降低其饮酒强度。相反,用舍曲林治疗的早发L'纯合子无明显增加其饮酒强度。这些发现暗示焦虑是观察到的药物遗传学作用的关键调节剂。这些发现具有重要意义,因为AD的患病率很高,并且开处方SSRI的频率较高。

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