Abstract

Background and ObjectivesEvidence on the association of cognitive reserve (CR) with the cognitive trajectories is limited. We aimed to examine the influence of CR indicator on domain-specific cognitive trajectories taking brain pathologies into account.MethodsWithin the Rush Memory and Aging Project, 1,697 participants without dementia (mean age 79.6 years) were followed up to 21 years. CR indicator encompassing education, early-life, mid-life, and late-life cognitive activities and late-life social activity was ascertained at baseline and categorized as tertiles (lowest, middle, and highest). Global cognition, episodic memory, semantic memory, working memory, visuospatial ability, and perceptual speed were assessed annually with 19 tests, from which composite scores were derived. During the follow-up, 648 participants died and underwent autopsies to evaluate brain pathologies. Data were analyzed using linear mixed-effect models.ResultsAmong the participants, the score of the CR indicator ranged from −8.00 to 5.74 (mean 0.00 ± 2.23). In multi-adjusted mixed-effect models, compared to the lowest CR, the highest was related to a slower decline in global cognition (β = 0.028, 95% confidence interval [CI] 0.012–0.043), episodic memory (β = 0.028, 95% CI 0.010–0.047), and working memory (β = 0.019, 95% CI 0.005–0.033) during the follow-up. In brain pathologic data analysis, the association of the highest CR with cognitive function changes remained significant among participants with high Alzheimer disease pathology or gross infarcts.DiscussionHigh CR indicator is associated with preserved global cognitive function, episodic memory, and working memory, even in the presence of brain pathologies. Our findings highlight the important role of high CR accumulation in the prevention of cognitive decline.

Highlights

  • Background and ObjectivesEvidence on the association of cognitive reserve (CR) with the cognitive trajectories is limited

  • In multi-adjusted mixed-effect models, compared to the lowest CR, the highest was related to a slower decline in global cognition (β = 0.028, 95% confidence interval [confidence intervals (CIs)] 0.012–0.043), episodic memory (β = 0.028, 95% CI 0.010–0.047), and working memory (β = 0.019, 95% CI 0.005–0.033) during the follow-up

  • High CR indicator is associated with preserved global cognitive function, episodic memory, and working memory, even in the presence of brain pathologies

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Summary

Objectives

We aimed to examine the influence of CR indicator on domain-specific cognitive trajectories taking brain pathologies into account. We aimed to examine the associations of CR indicator with global and domain-specific cognitive function changes over time and to explore whether brain pathologies may play a role in such associations among dementia-free older adults

Methods
Results
Conclusion
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