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The interplay of genes and adolescent development in substance use disorders: Leveraging findings from GWAS meta-analyses to test developmental hypotheses about nicotine consumption

机译:在物质使用障碍的基因和青少年发展的相互影响:从GWas荟萃分析结果利用测试尼古丁消费发育假说

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摘要

The present study evaluated gene by development interaction in cigarettes smoked per day (CPD) in a longitudinal community-representative sample (N=3231) of Caucasian twins measured at ages 14, 17, 20, and 24. Biometric heritability analyses show strong heritabilities and shared environmental influences, as well as cross-age genetic and shared-environmental correlations. SNPs previously associated with CPD according to meta-analysis were summed to create a SNP score. At best, the SNP score accounted for 1% of the variance in CPD. The results suggest developmental moderation with a larger significant SNP score effect on CPD at age 20 and 24, and smaller non-significant effect at age 14 and 17. These results are consistent with the notion that nicotine-specific genetic substance use risk is less important at younger ages, and becomes more important as individuals age into adulthood. In a complementary analysis, the same nicotine-relevant SNP score was unrelated to the frequency of alcohol use at ages 14, 17, 20, or 24. These results indicate that the SNP score is specific to nicotine in this small sample and that increased exposure to nicotine at ages 20 and 24 does not influence the extent of concurrent or later alcohol use. Increased sample sizes and replication or meta-analysis are necessary to confirm these results. The methods and results illustrate the importance and difficulty of considering developmental processes in understanding the interplay of genes and environment.
机译:本研究通过在14,17,20岁及24岁测量的白种人双胞胎中的纵向群落代表样品(N = 3231)中的纵向群落代表样品(N = 3231)中的卷烟中的卷烟中的卷烟中的纵向群体(CPD)进行了评估。生物识别遗传性分析表现出强烈的遗传性和共同的环境影响,以及次龄遗传和共享环境相关性。概括了先前与CPD相关联的SNP,以创建SNP分数。最多,SNP得分占CPD方差的1%。结果表明,在20和24岁及24岁的CPD中具有更大的显着SNP评分效果的发育适度,并且在14岁和17岁时的非显着效果较小。这些结果与尼古丁特异性遗传物质使用风险不太重要的观点一致在年轻的年龄,随着个人年龄变成成年期更重要。在互补分析中,与年龄17,17,20或24岁的醇类使用频率不相关。这些结果表明SNP评分在该小样本中对尼古丁特异,并且增加了暴露在20岁和24岁的尼古丁不影响同时或以后的酒精使用的程度。需要增加的样本尺寸和复制或元分析以确认这些结果。方法和结果说明了考虑了解理解基因和环境相互作用方面的发展过程的重要性和难度。

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