4.8 Article

Amphetamine modulates brain signal variability and working memory in younger and older adults

出版社

NATL ACAD SCIENCES
DOI: 10.1073/pnas.1504090112

关键词

brain signal variability; dopamine; aging; working memory; fMRI

资金

  1. Intramural Innovation Fund of the Max Planck Society
  2. Federal Ministry for Education and Research
  3. Max Planck UCL Centre for Computational Psychiatry and Ageing Research
  4. Gottfried Wilhelm Leibniz Award of the German Research Foundation
  5. Swedish Research Council
  6. Swedish Brain Power, an Alexander von Humboldt Research Award

向作者/读者索取更多资源

Better-performing younger adults typically express greater brain signal variability relative to older, poorer performers. Mechanisms for age and performance-graded differences in brain dynamics have, however, not yet been uncovered. Given the age-related decline of the dopamine (DA) system in normal cognitive aging, DA neuromodulation is one plausible mechanism. Hence, agents that boost systemic DA [such as d-amphetamine (AMPH)] may help to restore deficient signal variability levels. Furthermore, despite the standard practice of counterbalancing drug session order (AMPH first vs. placebo first), it remains understudied how AMPH may interact with practice effects, possibly influencing whether DA up-regulation is functional. We examined the effects of AMPH on functional-MRI-based blood oxygen level-dependent (BOLD) signal variability (SDBOLD) in younger and older adults during a working memory task (letter n-back). Older adults expressed lower brain signal variability at placebo, but met or exceeded young adult SDBOLD levels in the presence of AMPH. Drug session order greatly moderated change-change relations between AMPH-driven SDBOLD and reaction time means (RTmean) and SDs (RTSD). Older adults who received AMPH in the first session tended to improve in RTmean and RTSD when SDBOLD was boosted on AMPH, whereas younger and older adults who received AMPH in the second session showed either a performance improvement when SDBOLD decreased (for RTmean) or no effect at all (for RTSD). The present findings support the hypothesis that age differences in brain signal variability reflect aging-induced changes in dopaminergic neuromodulation. The observed interactions among AMPH, age, and session order highlight the state-and practice-dependent neurochemical basis of human brain dynamics.

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