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易感性差异预防:γ-氨基丁酸能、多巴胺能和多基因座效应。

Differential susceptibility to prevention: GABAergic, dopaminergic, and multilocus effects.

机构信息

Center for Family Research, Institute for Behavioral Research, University of Georgia, Athens, GA 30602-4527, USA.

出版信息

J Child Psychol Psychiatry. 2013 Aug;54(8):863-71. doi: 10.1111/jcpp.12042. Epub 2013 Jan 7.

DOI:10.1111/jcpp.12042
PMID:23294086
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3771493/
Abstract

BACKGROUND

Randomized prevention trials provide a unique opportunity to test hypotheses about the interaction of genetic predispositions with contextual processes to create variations in phenotypes over time.

METHODS

Using two longitudinal, randomized prevention trials, molecular genetic and alcohol use outcome data were gathered from more than 900 youths to determine whether prevention program participation would, across 2 years, moderate genetic risk for increased alcohol use conferred by the dopaminergic and GABAergic systems.

RESULTS

We found that (a) variance in dopaminergic (DRD2, DRD4, ANKK1) and GABAergic (GABRG1, GABRA2) genes forecast increases in alcohol use across 2 years, and (b) youths at genetic risk who were assigned to the control condition displayed greater increases in alcohol use across 2 years than did youths at genetic risk who were assigned to the prevention condition or youths without genetic risk who were assigned to either condition.

CONCLUSIONS

This study is unique in combining data from two large prevention trials to test hypotheses regarding genetic main effects and gene × prevention interactions. Focusing on gene systems purported to confer risk for alcohol use and abuse, the study demonstrated that participation in efficacious prevention programs can moderate genetic risk. The results also support the differential susceptibility hypothesis that some youths, for genetic reasons, are more susceptible than others to both positive and negative contextual influences.

摘要

背景

随机预防试验为检验遗传倾向与情境过程相互作用的假设提供了独特的机会,以创造随时间变化的表型差异。

方法

使用两个纵向随机预防试验,从 900 多名青少年中收集分子遗传和酒精使用结果数据,以确定预防计划的参与是否会在 2 年内缓和多巴胺能和 GABA 能系统遗传风险增加的酒精使用。

结果

我们发现,(a)多巴胺能(DRD2、DRD4、ANKK1)和 GABA 能(GABRG1、GABRA2)基因的变异预测了 2 年内酒精使用的增加,(b)分配到对照组的具有遗传风险的青少年在 2 年内的酒精使用增加幅度大于分配到预防组的具有遗传风险的青少年或分配到任何一组的无遗传风险的青少年。

结论

本研究结合了两个大型预防试验的数据,独特地检验了关于遗传主效应和基因×预防相互作用的假设。该研究关注被认为赋予酒精使用和滥用风险的基因系统,表明参与有效的预防计划可以减轻遗传风险。研究结果还支持了差异易感性假说,即由于遗传原因,一些青少年比其他青少年更容易受到积极和消极的环境影响。

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