How non-rapid eye movement sleep and Alzheimer pathology are linked

Alzheimer's disease(AD)is a multifactorial neurodegenerative disorder characterized by the presence of senile plaques and neurofibrillary tangles.Research attempts to identify characteristic factors that are associated with the presence of the AD pathology on the one hand and that increase the risk of developing AD on the other.Changes in non-rapid eye movement(NREM)sleep may meet both requirements for various reasons.First,NREM-sleep is important for optimal memory function.In addition,studies report that the presence of AD pathology is associated with NREM-sleep changes.Finally,more and more results appear to suggest that sleep problems are not only a symptom of AD but can also increase the risk of AD.Several of these studies suggest that it is primarily a lack of NREM-sleep that is responsible for this increased risk.However,the majority investigated sleep only through subjective reporting,as a result of which NREMsleep could not be analyzed separately.The aim of this literature study is therefore to present the results of the studies that relate the AD pathology and NREM-sleep(registered by electroencephalography).Furthermore,we try to evaluate whether NREM-sleep analysis could be used to support the diagnosis of AD and whether NREM-sleep deficiency could be a causal factor in the development of AD.

Sleep disorders in Alzheimer’s disease:the predictive roles and potential mechanisms

Sleep disorders are common in patients with Alzheimer’s disease,and can even occur in patients with amnestic mild cognitive impairment,which appears before Alzheimer’s disease.Sleep disorders further impair cognitive function and accelerate the accumulation of amyloid-βand tau in patients with Alzheimer’s disease.At present,sleep disorders are considered as a risk factor for,and may be a predictor of,Alzheimer’s disease development.Given that sleep disorders are encountered in other types of dementia and psychiatric conditions,sleep-related biomarkers to predict Alzheimer’s disease need to have high specificity and sensitivity.Here,we summarize the major Alzheimer’s disease-specific sleep changes,including abnormal non-rapid eye movement sleep,sleep fragmentation,and sleep-disordered breathing,and describe their ability to predict the onset of Alzheimer’s disease at its earliest stages.Understanding the mechanisms underlying these sleep changes is also crucial if we are to clarify the role of sleep in Alzheimer’s disease.This paper therefore explores some potential mechanisms that may contribute to sleep disorders,including dysregulation of the orexinergic,glutamatergic,andγ-aminobutyric acid systems and the circadian rhythm,together with amyloid-βaccumulation.This review could provide a theoretical basis for the development of drugs to treat Alzheimer’s disease based on sleep disorders in future work.

Increased Arousal Levels and Decreased Sleep by Brain Music in Rats

More and more studies have been reported on whether music and other types of auditory stimulation would improve the quality of sleep. Many of these studies have found significant results, but others argue that music is not significantly better than the tones or control conditions in improving sleep. For further understanding the relationship between music and sleep or music and arousal, the present study therefore examines the effects of brain music on sleep and arousal by means of biofeedback. The music is from the transformation of rapid eye movement （REM） sleep electroencephalogram （EEG） of rats using an algorithm in the Chengdu Brain Music （CBM） system. When the brain music was played back to rats, EEG data were recorded to assess the efficacy of music to induce or improve sleep, or increase arousal levels by sleep staging, etc. Our results demonstrate that exposure to the brain music increases arousal levels and decreases sleep in rats, and the underlying mechanism of decreased non-rapid eye movement （NREM） and REM sleep may be different.

不同年龄阶段重度阻塞性睡眠呼吸暂停低通气综合征患者睡眠脑电波特征研究

背景 阻塞性睡眠呼吸暂停低通气综合征(OSAHS)是一种常见的睡眠障碍,既往研究表明,年长患者更容易出现睡眠结构的变化和认知功能下降,其原因尚未完全明确,且目前关于睡眠脑电波(EEG)和睡眠结构与不同年龄阶段OSAHS患者关系的研究较少.目的 探究不同年龄阶段重度OSAHS的EEG特征,旨在进一步为大脑可塑性变化提供重要信息,指导临床治疗.方法 选取2017年6月-2018年3月在北京大学深圳医院睡眠呼吸障碍疾病诊疗中心确诊的67例重度OSAHS患者,依据我国最新的年龄划分标准将其分为年轻组(18~40岁,n=34)和年长组(41~65岁,n=33).比较两组患者呼吸暂停低通气指数(AHI)、夜间最低血氧饱和度(LSpO2)、睡眠有效率,非快速眼动睡眠(NREM)各分期(N1、N2、N3期)、快速眼动睡眠(REM)期睡眠时间占总睡眠时间百分比,NREM期各波〔δ 波(0.5~4.0 Hz)、θ 波(4.1~8.0 Hz)、α 波(8.1~12.0 Hz)和 β 波(12.1~30.0 Hz)〕脑电能量密度;并分析两组患者NREM期各波脑电能量密度、REM期睡眠时间、睡眠有效率与AHI的相关性.结果 年长组患者N1期、N2期睡眠时间占总睡眠时间百分比大于年轻组,年长组患者N3期、REM期睡眠时间占总睡眠时间百分比小于年轻组(P<0.05).年长组患者N1期、N2期、N3期 δ 波脑电能量密度均低于年轻组(P<0.05).年长组患者N3期 θ 波脑电能量密度低于年轻组(P<0.05).年长组患者N2期、N3期 α 波脑电能量密度低于年轻组(P<0.05).年长组患者N1期、N2期、N3期 β 波脑电能量密度均高于年轻组(P<0.05).年轻组患者NREM期 δ 波、θ 波、α 波脑电能量密度及REM期睡眠时间、睡眠有效率与AHI呈负相关(r值分别为-0.338、-0.315、-0.383、-0.483、-0.501,P值均<0.05);年轻组患者NREM期 β 波脑电能量密度与AHI无直线相关关系(P>0.05).年长组患者NREM期各波脑电能量密度、REM期睡眠时间和睡眠有效率与AHI无直线相关关系(P>0.05).结论 重度OSAHS的年轻患者与年长患者的EEG存在明显差异,年长患者N1期、N2期睡眠时间较长,而N3、REM期睡眠时间较短;与年轻患者相比,年长患者NREM期的 δ 波、N3期的 θ 波和 α 波均减少,而NREM期的 β 波却明显增加.这些EEG的改变导致了重度OSAHS的年长患者深睡眠时间减少,而浅睡眠时间增加,外界的刺激及间歇性低氧更容易导致觉醒,直接导致睡眠片段化增加.

无抽搐电休克治疗对男性抑郁症病人多导睡眠图的影响

目的:探讨无抽搐电休克(MECT)治疗对抑郁症病人睡眠脑电活动的影响。方法:应用多导睡眠图(PSG)对12例男性首发抑郁症病人在MECT治疗前后进行整夜PSG记录,观察MECT治疗前后PSG的变化。结果:与正常对照组比较,病人组睡眠总时间减少、睡眠潜伏期延迟、觉醒增加、快动眼睡眠(REM)时间增多、REM潜伏期缩短、S1和S2增加以及慢波睡眠减少。病人组经过MECT治疗后PSG显示睡眠总时间增加[治疗前:(342±s51)min,治疗后:(437±25)min,t值11.840,P<0.01],睡眠潜伏期缩短[治疗前:(68±12)min,治疗后:(56±7)min,t值4.249,P<0.01],觉醒时间减少[治疗前:(163±43)min,治疗后:(30±7)min,t值10.409,P<0.01],REM睡眠时间减少[治疗前:(164±19)min,治疗后:(120±5)min,t值9.333,P<0.01],S1减少[治疗前:(46±15)min,治疗后:(39±11)min,t值5.071,P<0.01],慢波睡眠增加[治疗前:(34±19)min,治疗后:(99±7)min,t值-13.146,P<0.01]。REM潜伏期和S2未见明显变化(P>0.05)。结论:MECT有改善睡眠的作用。这可能是MECT起到治疗抑郁症的重要机制之一。

Relationships between Rapid Eye Movement Sleep Behavior Disorder and Neurodegenerative Diseases： Clinical Assessments, Biomarkers, and Treatment

Objective： Rapid eye movement sleep behavior disorder （RBD） is characterized by dream enactment and loss of muscle atonia during rapid eye movement sleep. RBD is closely related to α-synucleinopathies including Parkinson＇s disease, dementia with Lewy bodies, and multiple system atrophy. Many studies have investigated the markers of imaging and neurophysiological, genetic, cognitive, autonomic function of RBD and their predictive value for neurodegenerative diseases. This report reviewed the progress of these studies and discussed their limitations and future research directions. Data Sources： Using the combined keywords： ＂RBD＂, ＂neurodegenerative disease＂, ＂Parkinson disease＂, and ＂magnetic resonance imaging＂, the PubMed/MEDLINE literature search was conducted up to January 1, 2018. Study Selection： A total of 150 published articles were initially identified citations. Of the 150 articles, 92 articles were selected after further detailed review. This study referred to all the important English literature in full. Results： Single-nucleotide polymorphisms in SCARB2 （rs6812193） and MAPT （rs12185268） were significantly associated with RBD. The olfactory loss, autonomic dysfunction, marked electroencephalogram slowing during both wakefulness and rapid eye movement sleep, and cognitive impairments were potential predictive markers for RBD conversion to neurodegenerative diseases. Traditional structural imaging studies reported relatively inconsistent results, whereas reduced functional connectivity between the left putamen and substantia nigra and dopamine transporter uptake demonstrated by functional imaging techniques were relatively consistent findings. Conclusions： More longitudinal studies should be conducted to evaluate the predictive value of biomarkers of RBD. Moreover, because the glucose and dopamine metabolisms are not specific for assessing cognitive cognition, the molecular metabolism directly related to cognition should be investigated. There is a need for more treatnaent trials to determine the effectiveness of interventions of RBD on preventing the conversion to neurodegenerative diseases.