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DDC 基因中的 rs3779084 与饮酒之间的关系受定期吸烟者饮酒动机的影响。

The relationship between rs3779084 in the dopa decarboxylase (DDC) gene and alcohol consumption is mediated by drinking motives in regular smokers.

机构信息

Department of Psychiatry, Washington University School of Medicine, St. Louis, Missouri, USA.

出版信息

Alcohol Clin Exp Res. 2012 Jan;36(1):162-70. doi: 10.1111/j.1530-0277.2011.01596.x. Epub 2011 Jul 28.

Abstract

BACKGROUND

Motivational models of alcohol use propose that the motivation to consume alcohol is the final common pathway to its use. Both alcohol consumption and drinking motives are influenced by latent genetic factors that partially overlap. This study investigated whether drinking motives mediate the associations between alcohol consumption and 2 single-nucleotide polymorphisms (SNPs) from genes involved in serotonin (TPH2; rs1386496) and dopamine synthesis (DDC; rs3779084). Based on earlier work showing that enhancement and coping motives were heritable in regular smokers but not in nonregular smokers, we hypothesized these motives would mediate the relationships between alcohol consumption and these SNPs in regular smokers.

METHODS

Drinking motives data were available from 830 young adult female twins (n = 344 regular smokers and n = 486 never/nonregular smokers). We used confirmatory factor analyses to model enhancement, coping, and alcohol consumption factors and to conduct mediation analyses in the regular smoker and never/nonregular smoker groups.

RESULTS

Our hypothesis was partially supported. The relationship between alcohol consumption and rs1386496 was not mediated by drinking motives in either group. However, in the regular smokers, the relationship between alcohol consumption and rs3779084 was mediated by enhancement and coping motives. Carriers of the rs3779084 minor allele who were regular smokers reported more motivation to consume alcohol. Given this pattern of results was absent in the never/nonregular smokers, our results are consistent with a gene × smoking status interaction.

CONCLUSIONS

In regular smokers, variability at the locus marked by rs3779084 in the DDC gene appears to index biologically based individual differences in the motivation to consume alcohol to attain or improve a positive affective state or to relieve a negative one. These results could be because of increased sensitivity to the reinforcing effects of alcohol among minor allele carriers who smoke, which might be due to structural or functional differences in mesorticolimic dopamine "reward" circuitry.

摘要

背景

酒精使用的动机模型提出,饮酒的动机是其使用的最终共同途径。酒精消费和饮酒动机都受到潜在遗传因素的影响,这些因素部分重叠。本研究调查了饮酒动机是否在酒精消费和涉及血清素(TPH2;rs1386496)和多巴胺合成(DDC;rs3779084)的基因的 2 个单核苷酸多态性(SNP)之间的关联中起中介作用。基于早期的研究表明,增强和应对动机在规律吸烟者中是可遗传的,但在非规律吸烟者中则不是,我们假设这些动机将在规律吸烟者中调节酒精消费和这些 SNP 之间的关系。

方法

有 830 名年轻成年女性双胞胎(n=344 名规律吸烟者和 n=486 名非/非规律吸烟者)的饮酒动机数据。我们使用验证性因素分析来对增强、应对和酒精消费因素进行建模,并在规律吸烟者和非/非规律吸烟者群体中进行中介分析。

结果

我们的假设得到了部分支持。在两个群体中,酒精消费与 rs1386496 的关系都没有通过饮酒动机来调节。然而,在规律吸烟者中,酒精消费与 rs3779084 的关系受到增强和应对动机的调节。携带 rs3779084 次要等位基因的规律吸烟者报告了更多的饮酒动机。鉴于这种结果模式在非/非规律吸烟者中不存在,我们的结果与基因-吸烟状态的相互作用一致。

结论

在规律吸烟者中,DDC 基因中由 rs3779084 标记的位置的变异性似乎表明了个体在获取或改善积极情绪状态或缓解消极情绪状态时对酒精的消费动机存在生物学基础上的差异。这些结果可能是由于携带次要等位基因的吸烟者对酒精的强化作用更为敏感,这可能是由于中脑边缘多巴胺“奖励”回路的结构或功能差异所致。

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