Scientific Reports (Nov 2024)

The interplay of age, gender and amyloid on brain and cognition in mid-life and older adults

  • Léonie Borne,
  • Renate Thienel,
  • Michelle K. Lupton,
  • Christine Guo,
  • Philip Mosley,
  • Anna Behler,
  • Joseph Giorgio,
  • Robert Adam,
  • Amelia Ceslis,
  • Pierrick Bourgeat,
  • Amir Fazlollahi,
  • Paul Maruff,
  • Christopher C. Rowe,
  • Colin L. Masters,
  • Jurgen Fripp,
  • Gail A. Robinson,
  • Michael Breakspear

DOI
https://doi.org/10.1038/s41598-024-78308-3
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 15

Abstract

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Abstract Deficits in memory are seen as a canonical sign of aging and a prodrome to dementia in older adults. However, our understanding of age-related cognition and brain morphology occurring throughout a broader spectrum of adulthood remains limited. We quantified the relationship between cognitive function and brain morphology (sulcal width, SW) using three cross-sectional observational datasets (PISA, AIBL, ADNI) from mid-life to older adulthood, assessing the influence of age, sex, amyloid (Aβ) and genetic risk for dementia. The data comprised cognitive, genetic and neuroimaging measures of a total of 1570 non-clinical mid-life and older adults (mean age 72, range 49–90 years, 1330 males) and 1365 age- and sex-matched adults with mild cognitive impairment (MCI) or Alzheimer’s disease (AD). Among non-clinical adults, we found robust modes of co-variation between regional SW and multidomain cognitive function that differed between the mid-life and older age range. These cortical and cognitive profiles derived from healthy cohorts predicted out-of-sample AD and MCI. Furthermore, Aβ-deposition and educational attainment levels were associated with cognition but not SW. These findings underscoring the complex interplay between factors influencing cognition and brain structure from mid-life onwards, providing valuable insights for future research into neurodegeneration and the development of future screening algorithms.