Sex and APOE4-specific links between cardiometabolic risk factors and white matter alterations in individuals with a family history of Alzheimer’s disease

  1. Stefanie A. Tremblay
  2. R. Nathan Spreng
  3. Alfie Wearn
  4. Zaki Alasmar
  5. Amir Pirhadi
  6. Christine L. Tardif
  7. Mallar M. Chakravarty
  8. Sylvia Villeneuve
  9. Ilana R. Leppert
  10. Felix Carbonell
  11. Yasser Iturria Medina
  12. Christopher J. Steele
  13. Claudine J. Gauthier
  14. PREVENT-AD Research Group
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Abstract

INTRODUCTION

White matter (WM) alterations are among the earliest changes in Alzheimer’s disease (AD), yet limited work has comprehensively characterized the effects of AD risk factors on WM.

METHODS

In older adults with a family history of AD, we investigated the sex-specific and APOE genotype-related relationships between WM microstructure and risk factors. Multiple MRI-derived metrics were integrated using a multivariate approach based on the Mahalanobis distance (D2). The links between WM D2 and cognition were also explored.

RESULTS

WM D2 in several regions was associated with high systolic blood pressure, BMI, and glycated hemoglobin, and low cholesterol, in both males and females. APOE4+ displayed a distinct risk pattern, with LDL-cholesterol having a detrimental effect only in carriers, and this pattern was linked to immediate memory performance. Myelination was the main mechanism underlying WM alterations.

DISCUSSION

Our findings reveal that combined exposure to multiple cardiometabolic risk factors negatively impacts microstructural health, which may subsequently affect cognition. Notably, APOE4 carriers exhibited a different risk pattern, especially in the role of LDL, suggesting distinct underlying mechanisms in this group.

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  1. Version published to 10.1101/2024.08.21.608995v1 on bioRxiv