Lower slow wave sleep and rapid eye movement sleep are associated with brain atrophy of Alzheimer's disease-vulnerable regions.

IF 2.9 3区医学 Q1 CLINICAL NEUROLOGY Journal of Clinical Sleep Medicine Pub Date : 2025-07-01 DOI:10.5664/jcsm.11630

Gawon Cho, Adam P Mecca, Orfeu M Buxton, Xiao Liu, Brienne Miner

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Abstract

Study objectives: Sleep deficiency is associated with Alzheimer's disease (AD) pathogenesis. We examined the association of sleep architecture with anatomical features observed in AD: (1) atrophy of hippocampus, entorhinal, inferior parietal, parahippocampal, precuneus, and cuneus regions ("AD-vulnerable regions") and (2) cerebral microbleeds (CMBs).

Methods: In 270 participants of the Atherosclerosis Risk in the Communities Study, we examined the association of baseline sleep architecture with anatomical features identified on brain magnetic resonance imaging 13-17 years later. Sleep architecture was quantified as the proportion of slow wave sleep (SWS), proportion of rapid eye movement (REM) sleep, and arousals index using polysomnography. Outcomes included (1) volumetric measurements of each AD-vulnerable region and (2) the presence of any CMBs and that of lobar CMBs, which are more specifically associated with AD. We analyzed the association of each sleep predictor with each magnetic resonance imaging outcome, adjusting for covariates.

Results: Median age was 61, 53% were female, 100% were White, and 47% had 16+ years of education. Median times in SWS and REM were 17.4% and 21.5%, respectively. Having less SWS was associated with smaller volumes of the inferior parietal region (β = -44.18 mm³ [95% confidence interval = -76.62, -11.74] per -1 percentage point of SWS) and cuneus (β = -11.98 [= -20.92, -3.04] mm³ per -1 percentage point). Having less REM was associated with smaller volumes of the inferior parietal region (β = -75.54 [-129.36, -21.72] mm³ per 1 percentage point of REM) and precuneus (β = -31.92 [-63.78, -0.06] mm³ per 1 percentage point). After Bonferroni adjustments, lower SWS and REM were associated with significantly smaller inferior parietal region volumes. Arousal index was not associated with the volumes of AD-vulnerable regions. None of the sleep architecture variables were associated with CMBs or lobar CMBs.

Conclusions: Sleep deficiency is associated with the atrophy of the inferior parietal region, which is observed in early AD. Sleep architecture may be a modifiable risk factor for AD.

Citation: Cho G, Mecca AP, Buxton OM, Liu X, Miner B. Lower slow wave sleep and rapid eye movement sleep are associated with brain atrophy of Alzheimer's disease-vulnerable regions. J Clin Sleep Med. 2025;21(7):1165-1173.

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低慢波睡眠和快速眼动睡眠与ad易感区域脑萎缩有关。

研究目的：睡眠不足与阿尔茨海默病（AD）发病机制相关。我们研究了睡眠结构与AD解剖特征之间的关系：(1)海马、内嗅、下顶叶、海马旁、楔叶前和楔叶区域（AD易感区域）的萎缩；(2)脑微出血。方法：在270名社区动脉粥样硬化风险研究的参与者中，我们检查了基线睡眠结构与13 ~ 17年后脑MRI上确定的解剖特征之间的关系。采用多导睡眠图将睡眠结构量化为慢波睡眠（SWS）比例、快速眼动睡眠（REM）比例和唤醒指数。结果包括(1)每个AD易感区域的体积测量和(2)脑微出血（CMBs）和脑大叶CMBs的存在，这与AD更具体地相关。我们分析了每个睡眠预测因子与每个MRI结果的关联，并对协变量进行了调整。结果：中位年龄61岁，53%为女性，100%为白人，47%受教育年限为16年以上。SWS和REM的中位次数分别为17.4%和21.5%。SWS越少，下顶叶面积越小（β=-44.18 mm3 / -1个百分点[PP]， [95%CI=-76.62, -11.74]），楔骨面积越小（β=-11.98 [=-20.92, -3.04] mm3 / -1个百分点[PP]）。快速眼动越少，顶叶下区体积越小（β=-75.54 [-129.36, -21.72] mm3 / 1 PP REM），楔前叶体积越小（β=-31.92 [-63.78,-0.06] mm3 / 1 PP REM）。经FDR调整后，较低的SWS和REM与显著较小的下顶叶区体积相关。唤醒指数与ad易感区域的体积无关。没有一个睡眠结构变量与CMBs或大叶CMBs相关。结论：睡眠不足与下顶叶萎缩有关，这在阿尔茨海默病早期就已观察到。睡眠结构可能是AD的一个可改变的危险因素。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Clinical Sleep Medicine CLINICAL NEUROLOGY-

CiteScore

6.20

自引率

7.00%

发文量

321

审稿时长

1 months

期刊介绍： Journal of Clinical Sleep Medicine focuses on clinical sleep medicine. Its emphasis is publication of papers with direct applicability and/or relevance to the clinical practice of sleep medicine. This includes clinical trials, clinical reviews, clinical commentary and debate, medical economic/practice perspectives, case series and novel/interesting case reports. In addition, the journal will publish proceedings from conferences, workshops and symposia sponsored by the American Academy of Sleep Medicine or other organizations related to improving the practice of sleep medicine.