健康和患有CLN5型贝敦氏病的绵羊睡眠稳态的脑电图研究。
An EEG Investigation of Sleep Homeostasis in Healthy and CLN5 Batten Disease Affected Sheep.
作者信息
Perentos Nicholas, Martins Amadeu Q, Cumming Robin J M, Mitchell Nadia L, Palmer David N, Sawiak Stephen J, Morton A Jennifer
机构信息
Department of Physiology Development and Neuroscience, University of Cambridge, Cambridge CB2 3DY, United Kingdom.
Department of Molecular Biosciences, Faculty of Agricultural and Life Sciences, Lincoln University, Lincoln 7647, New Zealand, and.
出版信息
J Neurosci. 2016 Aug 3;36(31):8238-49. doi: 10.1523/JNEUROSCI.4295-15.2016.
UNLABELLED
Sheep have large brains with human-like anatomy, making them a useful species for studying brain function. Sleep homeostasis has not been studied in sheep. Here, we establish correlates of sleep homeostasis in sheep through a sleep deprivation experiment. We then use these correlates to elucidate the nature of sleep deficits in a naturally occurring ovine model of neuronal ceroid lipofuscinosis (NCL, Batten disease) caused by a mutation in CLN5 In humans, mutations in this gene lead to cortical atrophy and blindness, as well as sleep abnormalities. We recorded electroencephalograms (EEGs) from unaffected and early stage CLN5(-/-) (homozygous, affected) sheep over 3 consecutive days, the second day being the sleep deprivation day. In unaffected sheep, sleep deprivation led to increased EEG delta (0.5-4 Hz) power during non-rapid eye movement (NREM) sleep, increased time spent in the NREM sleep state, and increased NREM sleep bout length. CLN5(-/-) sheep showed comparable increases in time spent in NREM sleep and NREM sleep bout duration, verifying the presence of increased sleep pressure in both groups. Importantly, CLN5(-/-) sheep did not show the increase in NREM sleep delta power seen in unaffected sheep. This divergent delta power response is consistent with the known cortical degeneration in CLN5(-/-) sheep. We conclude that, whereas sleep homeostasis is present in CLN5(-/-) sheep, underlying CLN5(-/-) disease processes prevent its full expression, even at early stages. Such deficits may contribute to early abnormalities seen in sheep and patients and warrant further study.
SIGNIFICANCE STATEMENT
Sleep abnormalities pervade most neurological diseases, including the neuronal ceroid lipofuscinoses (NCLs). Here, we show that, in an ovine model of a variant late-infantile NCL, there is abnormal expression of sleep homeostasis. Whereas some sleep pressure correlates respond to sleep deprivation, the strongest electroencephalogram (EEG) correlate of sleep pressure, non-REM delta power, failed to increase. This highlights the relevance of sleep deficits in this disease, in which the drive for sleep exists but the underlying disease prevents its full expression. Sleep abnormalities could contribute to early disease symptoms such as behavioral disorder and cognitive decline. Our study also shows sleep homeostatic EEG correlates in sheep, opening up new opportunities for studying sleep in a large social mammal with complex human-like brain neuroanatomy.
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绵羊的大脑较大,其解剖结构与人类相似,这使其成为研究脑功能的有用物种。尚未对绵羊的睡眠稳态进行研究。在此,我们通过睡眠剥夺实验建立了绵羊睡眠稳态的相关指标。然后,我们利用这些相关指标来阐明由CLN5基因突变引起的神经元蜡样脂褐质沉积症(NCL,巴滕病)自然发生的绵羊模型中的睡眠缺陷本质。在人类中,该基因突变会导致皮质萎缩、失明以及睡眠异常。我们连续三天记录了未受影响和早期CLN5(-/-)(纯合子,患病)绵羊的脑电图(EEG),第二天为睡眠剥夺日。在未受影响的绵羊中,睡眠剥夺导致非快速眼动(NREM)睡眠期间EEGδ波(0.5 - 4赫兹)功率增加、NREM睡眠状态下的时间增加以及NREM睡眠周期长度增加。CLN5(-/-)绵羊在NREM睡眠中花费的时间和NREM睡眠周期持续时间也有类似增加,证实两组均存在睡眠压力增加。重要的是,CLN5(-/-)绵羊未表现出未受影响绵羊中出现的NREM睡眠δ波功率增加。这种不同的δ波功率反应与CLN5(-/-)绵羊中已知的皮质退化一致。我们得出结论,虽然CLN5(-/-)绵羊存在睡眠稳态,但潜在的CLN5(-/-)疾病过程即使在早期也会阻止其充分表达。这些缺陷可能导致绵羊和患者早期出现异常情况,值得进一步研究。
意义声明
睡眠异常普遍存在于大多数神经系统疾病中,包括神经元蜡样脂褐质沉积症(NCLs)。在此,我们表明,在一种变异型晚发性婴儿NCL的绵羊模型中,存在睡眠稳态的异常表达。虽然一些睡眠压力相关指标对睡眠剥夺有反应,但睡眠压力最强的脑电图(EEG)相关指标,即非快速眼动δ波功率,并未增加。这突出了该疾病中睡眠缺陷的相关性,其中睡眠驱动力存在,但潜在疾病阻止其充分表达。睡眠异常可能导致行为障碍和认知衰退等早期疾病症状。我们的研究还显示了绵羊睡眠稳态的EEG相关指标,为在具有复杂人类样脑神经解剖结构的大型群居哺乳动物中研究睡眠开辟了新机会。
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