β-Amyloid burden in healthy aging: regional distribution and cognitive consequences

Several lines of evidence suggest that pathologic changes underlying Alzheimer disease (AD) begin years prior to the clinical expression of the disease, underscoring the need for studies of cognitively healthy adults to capture these early changes. The overall goal of the current study was to map th...

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Published inNeurology Vol. 78; no. 6; p. 387
Main Authors Rodrigue, K M, Kennedy, K M, Devous, Sr, M D, Rieck, J R, Hebrank, A C, Diaz-Arrastia, R, Mathews, D, Park, D C
Format Journal Article
LanguageEnglish
Published United States 07.02.2012
Subjects
Adult
Aged
Aged, 80 and over
Aging - metabolism
Alzheimer Disease - diagnostic imaging
Alzheimer Disease - metabolism
Amyloid beta-Peptides - metabolism
Brain - diagnostic imaging
Brain - metabolism
Cognition
Cognition Disorders - diagnostic imaging
Cognition Disorders - metabolism
Female
Humans
Male
Memory
Middle Aged
Neuropsychological Tests
Radionuclide Imaging
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Summary:Several lines of evidence suggest that pathologic changes underlying Alzheimer disease (AD) begin years prior to the clinical expression of the disease, underscoring the need for studies of cognitively healthy adults to capture these early changes. The overall goal of the current study was to map the cortical distribution of β-amyloid (Aβ) in a healthy adult lifespan sample (aged 30-89), and to assess the relationship between elevated amyloid and cognitive performance across multiple domains. A total of 137 well-screened and cognitively normal adults underwent Aβ PET imaging with radiotracer (18)F-florbetapir. Aβ load was estimated from 8 cortical regions. Participants were genotyped for APOE and tested for processing speed, working memory, fluid reasoning, episodic memory, and verbal ability. Aβ deposition is distributed differentially across the cortex and progresses at varying rates with age across cortical brain regions. A subset of cognitively normal adults aged 60 and over show markedly elevated deposition, and also had a higher rate of APOE ε4 (38%) than nonelevated adults (19%). Aβ burden was linked to poorer cognitive performance on measures of processing speed, working memory, and reasoning. Even in a highly selected lifespan sample of adults, Aβ deposition is apparent in some adults and is influenced by APOE status. Greater amyloid burden was related to deleterious effects on cognition, suggesting that subtle cognitive changes accrue as amyloid progresses.
ISSN:1526-632X
DOI:10.1212/WNL.0b013e318245d295