An official website of the United States government
Lower slow wave sleep and rapid eye movement sleep are associated with brain atrophy of Alzheimer's disease-vulnerable regions.
Pubmed ID: 40110600
Pubmed Central ID: PMC12225272
Journal: Journal of clinical sleep medicine : JCSM : official publication of the American Academy of Sleep Medicine
Publication Date: July 1, 2025
MeSH Terms: Humans, Male, Female, Aged, Middle Aged, Magnetic Resonance Imaging, Alzheimer Disease, Brain, Polysomnography, Atrophy, Sleep, REM, Sleep, Slow-Wave
Grants: P30 AG021342, U01 HL096812, U01 HL096917, U01 HL096902, U01 HL096814, U01 HL096899, R24 HL114473, 75N92022D00004, 75N92022D00003, 75N92022D00002, 75N92022D00005, U01 HL053916, U01 HL064360, K76 AG074905, U01 HL053941, U01 HL053937, 75N92022D00001, U01 HL053931, U01 HL063463, R43 AG056250, R44 AG056250, U01 HL053938, U01 HL053934
Authors: Buxton OM, Liu X, Cho G, Mecca AP, Miner B
Cite As: 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 Jul 1;21(7):1165-1173.
Studies:
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 mm<sup>3</sup> [95% confidence interval = -76.62, -11.74] per -1 percentage point of SWS) and cuneus (β = -11.98 [= -20.92, -3.04] mm<sup>3</sup> per -1 percentage point). Having less REM was associated with smaller volumes of the inferior parietal region (β = -75.54 [-129.36, -21.72] mm<sup>3</sup> per 1 percentage point of REM) and precuneus (β = -31.92 [-63.78, -0.06] mm<sup>3</sup> 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. <i>J Clin Sleep Med</i>. 2025;21(7):1165-1173.