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Early morning executive functioning during sleep deprivation is compromised by a PERIOD3 polymorphism.

机译:PERIOD3多态性损害了睡眠剥夺期间清晨的执行功能。

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STUDY OBJECTIVES: To contrast the effects of total sleep deprivation (TSD) on executive and non-executive function in volunteers homozygous for either the short or long variant of a variable number tandem repeat polymorphism in PERIODS, which is a genetic marker for susceptibility to the negative effect of sleep loss on waking performance. DESIGN: Following two laboratory nights of baseline sleep, both groups underwent an approximately 40-hour constant routine, performing brief tests of executive, memory, attention, and motor function every 2 hours. SETTING: Clinical Research Centre. PARTICIPANTS: Fourteen PER3(4/4) (homozygotes for shorter variant of the gene) and 10 PER3(5/5) (homozygotes for longer variant) healthy, young adults (mean 25.0 +/- 1.0 years). INTERVENTIONS: Total sleep deprivation (approximately 40 hours) following baseline sleep. MEASUREMENTS AND RESULTS: Hormonal assays established that melatonin levels, which reflect circadian phase, reached their midpoint around 04:00 in both genotypes. Cognitive performance deteriorated across the night, and was similar for both genotypes throughout, except 2-4 h after the midpoint of the melatonin rhythm. Only at this time-point and only on tests of executive function (e.g., 3-back, paced visual serial addition task) did PER3(5/5) participants perform reliably worse. Covariance analyses controlling for genotype dependent differences in homeostatic sleep pressure derived from principal component analysis of baseline sleep latency, slow wave sleep and wake after sleep onset largely removed these early morning differences in executive function. CONCLUSIONS: This PER3 polymorphism differentially influences the effects of sleep deprivation on executive and non-executive function in the early morning. These effects appear to be mediated through homeostatic sleep pressure.
机译:研究目的:为了比较全睡眠剥夺(TSD)对PERIODS中可变数目串联重复多态性的短或长变异纯合的志愿者执行和非执行功能的影响,这是遗传易感性睡眠不足对清醒性能的负面影响。设计:经过两个实验室夜间的基准睡眠后,两组患者均进行了大约40小时的固定程序,每2小时对执行力,记忆力,注意力和运动功能进行简短测试。地点:临床研究中心。参与者:健康的年轻成年人(平均25.0 +/- 1.0岁)的14个PER3(4/4)(基因的较短变异为纯合子)和10个PER3(5/5)(较长的变异为纯合子)。干预措施:基线睡眠后总睡眠不足(约40小时)。测量和结果:激素测定表明,反映昼夜节律的褪黑激素水平在两种基因型中均在04:00左右达到中点。整个晚上的认知能力下降,并且除了褪黑激素节律中点后2-4小时外,两种基因型在整个过程中都相似。仅在此时间点,并且仅在执行功能测试(例如,三后卫,有节奏的视觉序列添加任务)上,PER3(5/5)参与者的表现才可靠地变差。从基线睡眠潜伏期,慢波睡眠和入睡后醒来的主成分分析得出的稳态睡眠压力的基因型相关差异控制的协方差分析在很大程度上消除了这些清晨执行功能差异。结论:这种PER3多态性在清晨差异影响睡眠剥夺对执行和非执行功能的影响。这些作用似乎是通过稳态睡眠压力介导的。

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