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在年轻成年人样本中,睡眠质量和昼夜节律偏好与 5HTTLPR、PER3 和 CLOCK 3111 的关联。

Sleep quality and diurnal preference in a sample of young adults: associations with 5HTTLPR, PER3, and CLOCK 3111.

机构信息

Department of Psychology, Goldsmiths, University of London, UK.

出版信息

Am J Med Genet B Neuropsychiatr Genet. 2011 Sep;156B(6):681-90. doi: 10.1002/ajmg.b.31210. Epub 2011 Jun 28.

Abstract

Research investigating associations between specific genes and individual differences with regards to the quality and timing of sleep has primarily focussed on serotonin-related and clock genes. However, there are only a few studies of this type and most of those to date have not considered the possibility of gene-environment interaction. Here, we describe associations between sleep quality and diurnal preference and three functional polymorphisms: 5HTTLPR, PERIOD3, and CLOCK 3111. Furthermore, we assessed whether associations between genotypes and sleep phenotypes were moderated by negative life events-a test of gene-environment interaction. DNA from buccal swabs was collected from 947 individuals [mean age = 20.3 years (SD = 1.77), age range = 18-27 years; 61.8% female] and genotyped for the three polymorphisms. Participants completed the Pittsburgh Sleep Quality Index and the Morningness-Eveningness Questionnaire. There was a significant main effect of 5HTTLPR on sleep quality, indicating that "long-long" homozygotes experienced significantly poorer sleep quality (mean = 6.35, SD = 3.36) than carriers of at least one "short" allele (mean = 5.67, SD = 2.96; β = -0.34, P = 0.005). There were no main effects of 5HTTLPR on diurnal preference; no main effects of PERIOD3 or CLOCK on sleep quality or diurnal preference; and no significant interactions with negative life events. The main effect of the "long" 5HTTLPR allele contradicts previous research, suggesting that perhaps the effects of this gene are heterogeneous in different populations. Failure to replicate previous research in relation to PERIOD3 and CLOCK concurs with previous research suggesting that the effects of these genes are small and may be related to population composition.

摘要

研究主要集中在与睡眠质量和时间有关的特定基因和个体差异上,涉及 5-羟色胺相关基因和时钟基因。然而,这类研究很少,迄今为止的大多数研究都没有考虑基因-环境相互作用的可能性。在这里,我们描述了睡眠质量和昼夜倾向与三个功能多态性之间的关联:5HTTLPR、PERIOD3 和 CLOCK 3111。此外,我们评估了基因型和睡眠表型之间的关联是否受到负性生活事件的调节,这是对基因-环境相互作用的检验。从 947 名个体(平均年龄=20.3 岁(SD=1.77),年龄范围=18-27 岁;61.8%女性)的口腔拭子中采集 DNA,并对三种多态性进行基因分型。参与者完成了匹兹堡睡眠质量指数和晨晚倾向问卷。5HTTLPR 对睡眠质量有显著的主效应,表明“长-长”纯合子的睡眠质量明显较差(平均值=6.35,SD=3.36),而至少携带一个“短”等位基因的携带者(平均值=5.67,SD=2.96;β=-0.34,P=0.005)。5HTTLPR 对昼夜倾向没有主效应;PERIOD3 或 CLOCK 对睡眠质量或昼夜倾向没有主效应;与负性生活事件没有显著的相互作用。“长”5HTTLPR 等位基因的主要效应与以前的研究相反,这表明该基因的效应在不同人群中可能是异质的。PERIOD3 和 CLOCK 与以前的研究结果一致,即以前的研究未能复制与这些基因相关的研究结果,这表明这些基因的效应很小,可能与人群组成有关。

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