WWAMI Medical Education Program, Sleep and Performance Research Center, Washington State University, Spokane, WA 99202, USA.
J Clin Sleep Med. 2011 Oct 15;7(5 Suppl):S16-8. doi: 10.5664/JCSM.1346.
Electroencephalographic (EEG) δ waves during non-rapid eye movement sleep (NREMS) after sleep deprivation are enhanced. That observation eventually led to the use of EEG δ power as a parameter to model process S in the two-process model of sleep. It works remarkably well as a model parameter because it often co-varies with sleep duration and intensity. Nevertheless there is a large volume of literature indicating that EEG δ power is regulated independently of sleep duration. For example, high amplitude EEG δ waves occur in wakefulness after systemic atropine administration or after hyperventilation in children. Human neonates have periods of sleep with an almost flat EEG. Similarly, elderly people have reduced EEG δ power, yet retain substantial NREMS. Rats provided with a cafeteria diet have excess duration of NREMS but simultaneously decreased EEG δ power for days. Mice challenged with influenza virus have excessive EEG δ power and NREMS. In contrast, if mice lacking TNF receptors are infected, they still sleep more but have reduced EEG δ power. Sleep regulatory substances, e.g., IL1, TNF, and GHRH, directly injected unilaterally onto the cortex induce state-dependent ipsilateral enhancement of EEG δ power without changing duration of organism sleep. IL1 given systemically enhances duration of NREMS but reduces EEG δ power in mice. Benzodiazepines enhance NREMS but inhibit EEG δ power. If duration of NREMS is an indicator of prior sleepiness then simultaneous EEG δ power may or may not be a useful index of sleepiness. Finally, most sleep regulatory substances are cerebral vasodilators and blood flow affects EEG δ power. In conclusion, it seems unlikely that a single EEG measure will be reliable as a marker of sleepiness for all conditions.
剥夺睡眠后非快速眼动睡眠(NREMS)期间的脑电图(EEG)δ 波增强。这一观察结果最终导致使用 EEG δ 功率作为模型睡眠双过程模型中过程 S 的参数。它作为模型参数的效果非常好,因为它通常与睡眠持续时间和强度共同变化。尽管有大量文献表明 EEG δ 功率是独立于睡眠持续时间调节的。例如,全身阿托品给药后或儿童过度通气后,觉醒时会出现高振幅 EEG δ 波。人类新生儿有一段时间的睡眠,脑电图几乎呈平坦状。同样,老年人的 EEG δ 功率降低,但仍保留大量的 NREMS。给予自助餐厅饮食的大鼠有 NREMS 持续时间延长,但 EEG δ 功率持续数日下降。感染流感病毒的小鼠会出现过多的 EEG δ 波和 NREMS。相比之下,如果缺乏 TNF 受体的小鼠被感染,它们仍然会睡得更多,但 EEG δ 功率降低。睡眠调节物质,如 IL1、TNF 和 GHRH,直接单侧注射到皮质上会引起 EEG δ 波的状态依赖性同侧增强,而不改变机体的睡眠持续时间。全身性给予 IL1 会增强 NREMS,但会降低小鼠的 EEG δ 波功率。苯二氮䓬类药物增强 NREMS,但抑制 EEG δ 波功率。如果 NREMS 的持续时间是先前困倦的指标,那么同时的 EEG δ 波功率可能是也可能不是困倦的有用指标。最后,大多数睡眠调节物质都是脑血管扩张剂,而血流量会影响 EEG δ 波功率。总之,似乎不太可能有一种单一的 EEG 测量作为所有情况下困倦的可靠标志物。