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功能性 ADA 多态性增加人类的睡眠深度并降低警觉注意力。

Functional ADA polymorphism increases sleep depth and reduces vigilant attention in humans.

机构信息

Institute of Pharmacology and Toxicology University of Zurich, Zurich, Switzerland.

出版信息

Cereb Cortex. 2012 Apr;22(4):962-70. doi: 10.1093/cercor/bhr173. Epub 2011 Jul 6.

Abstract

Homeostatically regulated slow-wave oscillations in non-rapid eye movement (REM) sleep may reflect synaptic changes across the sleep-wake continuum and the restorative function of sleep. The nonsynonymous c.22G>A polymorphism (rs73598374) of adenosine deaminase (ADA) reduces the conversion of adenosine to inosine and predicts baseline differences in sleep slow-wave oscillations. We hypothesized that this polymorphism affects cognitive functions, and investigated whether it modulates electroencephalogram (EEG), behavioral, subjective, and biochemical responses to sleep deprivation. Attention, learning, memory, and executive functioning were quantified in healthy adults. Right-handed carriers of the variant allele (G/A genotype, n = 29) performed worse on the d2 attention task than G/G homozygotes (n = 191). To test whether this difference reflects elevated homeostatic sleep pressure, sleep and sleep EEG before and after sleep deprivation were studied in 2 prospectively matched groups of G/A and G/G genotype subjects. Deep sleep and EEG 0.75- to 1.5-Hz oscillations in non-REM sleep were significantly higher in G/A than in G/G genotype. Moreover, attention and vigor were reduced, whereas waking EEG alpha activity (8.5-12 Hz), sleepiness, fatigue, and α-amylase in saliva were enhanced. These convergent data demonstrate that genetic reduction of ADA activity elevates sleep pressure and plays a key role in sleep and waking quality in humans.

摘要

非快速眼动(REM)睡眠中的内稳态调节慢波振荡可能反映了睡眠-觉醒连续体中的突触变化和睡眠的恢复功能。腺苷脱氨酶(ADA)的非同义 c.22G>A 多态性(rs73598374)降低了腺苷向肌苷的转化,并预测了睡眠慢波振荡的基线差异。我们假设这种多态性会影响认知功能,并研究它是否调节脑电图(EEG)、行为、主观和生化对睡眠剥夺的反应。在健康成年人中量化了注意力、学习、记忆和执行功能。携带变异等位基因(G/A 基因型,n = 29)的右利手者在 d2 注意力任务上的表现逊于 G/G 纯合子(n = 191)。为了测试这种差异是否反映了升高的内稳态睡眠压力,在 2 个前瞻性匹配的 G/A 和 G/G 基因型受试者组中研究了睡眠剥夺前后的睡眠和睡眠 EEG。非快速眼动睡眠中的深度睡眠和 EEG 0.75-1.5 Hz 振荡在 G/A 比 G/G 基因型中显著更高。此外,注意力和活力降低,而清醒 EEG α 活动(8.5-12 Hz)、嗜睡、疲劳和唾液中的α-淀粉酶增加。这些收敛数据表明,ADA 活性的遗传降低会增加睡眠压力,并在人类的睡眠和清醒质量中发挥关键作用。

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