Night‐to‐night variability in sleep and amyloid beta burden in normal aging

Author:

Jouvencel Aurore1,Baillet Marion2,Meyer Marie13,Dilharreguy Bixente1,Lamare Frederic13,Pérès Karine4,Helmer Catherine4,Dartigues Jean‐François4,Amieva Hélène4,Mayo Willy1,Catheline Gwenaëlle1

Affiliation:

1. INCIA, EPHE, Université PSL Univ Bordeaux CNRS Bordeaux France

2. GIGA‐CRC‐In Vivo Imaging Research Unit University of Liège Liège Belgium

3. Nuclear Medicine Department University Hospital of Bordeaux Bordeaux France

4. INSERM Bordeaux Population Health Research Center University of Bordeaux UMR U1219 Bordeaux France

Abstract

AbstractINTRODUCTIONAlzheimer's disease is associated with sleep disturbances and accumulation of cerebral amyloid beta. The objective was to examine whether actigraphy‐detected sleep parameters might be biomarkers for early amyloid burden.METHODSParticipants underwent a week of actigraphy and an amyloid positron emission tomography (PET) scan. Sleep duration and continuity disruption (sleep fragmentation and nocturnal awakenings) were extracted and compared between amyloid‐positive and amyloid‐negative participants. Then multiple linear regressions were used between mean or night‐to‐night intra‐individual variability (standard deviation) of sleep parameters and brain amyloid burden in a voxel‐wise analysis.RESULTSEighty‐six subjects were included (80.3 ± 5.4 years; 48.8% of women). Amyloid‐positive participants had a higher variability of sleep fragmentation compared to amyloid‐negative participants. This parameter was associated with a higher amyloid burden in the frontal and parietal regions, and in the precuneus, in the whole sample.DISCUSSIONThis study highlights the relevance of using variability in sleep continuity as a potential biomarker of early amyloid pathogenesis.

Publisher

Wiley

Subject

Psychiatry and Mental health,Neurology (clinical)

Reference50 articles.

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