Alzheimer's & dementia : the journal of the Alzheimer's Association
Published

Biomarkers

Authors

Thomas M Brown, Sarah-Naomi James, Jennifer M Nicholas, Ian B Malone, William Coath, Heidi Murray-Smith, David M Cash, Frederik Barkhof, Jonathan M Schott, Jo Barnes, Carole H Sudre
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Abstract

Alzheimers Dement. 2025 Dec;21 Suppl 2:e104402. doi: 10.1002/alz70856_104402.

ABSTRACT

BACKGROUND: Diffusion weighted imaging (DWI) measures white matter (WM) microstructure (WMMS), with changes in various DWI metrics seen in Alzheimer's disease (AD) progression1. Using data from Insight463-5, a British population-based birth cohort, we previously found poorer WMMS in normal appearing WM (NAWM) age 70 had sex-dependent associations with higher midlife blood pressure and cardiovascular risk, as well as concurrent WM hyperintensity volume (WMHV) and β-Amyloid (Aβ) burden2. Here we explore whether these findings reflect poorer WMMS in areas of NAWM that remained normal appearing ∼2.5 years later, or in areas that later became WMH.

METHOD: Using data from N = 302 Insight46 participants who were scanned for a second time ∼2.5 years later, we used linear regression to re-examine the previously identified significant relationships with NAWM integrity2, as well as sex interactions in men and women that remained robust in the smaller follow-up sample, separately in "stable" (remained NAWM) and "converting" (converted to WMH) regions (Figure 1). WMMS metrics were fractional anisotropy (FA), mean diffusivity (MD) and neurite density index (NDI)2. Analyses were adjusted for sex and age as well as total intracranial volume (TIV) for models with WMHV and Aβ.

RESULT: Summary statistics are shown in Table 1. The associations shown in the total NAWM2 persisted in stable regions (Figure 2). Stronger associations were observed in the converting NAWM, particularly with WMHV at age 70. There was also a significant association between BP at age 53 and FA and MD in males in the converting NAWM, which was only observed in women in the whole region2. The effect of Aβ on MD in men was robust in both regions.

CONCLUSION: Previously demonstrated associations with poorer WMMS (age, midlife cardiovascular risk factors, WMHV and Aβ)2 were not driven solely by NAWM on the verge of becoming WMH. However, stronger effects observed in converting NAWM suggest higher midlife BP, poorer WMMS and WMH development are part of a continuous, related process, particularly in men. The similar effect of Aβ burden in men in the stable and unstable NAWM suggests the effects of Aβ on WMMI are not driven by tissue later converting to WMH.

PMID:41453151 | DOI:10.1002/alz70856_104402