Longitudinal changes in neuroimaging markers of small vessel disease: Implications for clinical trials

Files
Lao2025Longitudinal-CCBY.pdf (375.32 KB)
Date
2025-01-09
Authors
Lao, Patrick J.
Edwards, Natalie C.
Flores-Aguilar, Lisi
Rizvi, Batool
Smith, Anna C.
Tudorascu, Dana
Rosas, H. Diana
Yassa, Michael A.
Handen, Benjamin L.
Christian, Bradley T.
Gutierrez, Jose
Wilcock, Donna M.
Head, Elizabeth
Brickman, Adam M.
Language
American English
Embargo Lift Date
Department
Neurology, School of Medicine
Committee Members
Degree
Degree Year
Department
Grantor
Journal Title
Journal ISSN
Volume Title
Found At
Wiley
Abstract

Background: Adults with Down syndrome (DS) overproduce amyloid precursor protein, develop amyloid plaques at an early age, and are diagnosed with Alzheimer’s disease (AD) dementia at a high frequency. There is emerging evidence that cerebrovascular disease is elevated across the AD continuum in older adults with DS, independent of age and vascular risk, around the same time as amyloid and tau, but the regional rates of accumulation within individuals are unknown.

Method: Adults with DS from the multisite Alzheimer’s Biomarker Consortium‐Down Syndrome study (ABC‐DS; n=78; age=50±6; 40% women) have two timepoints of T2 FLAIR MRI (1.2±0.6 years apart) quantified as white matter hyperintensity volume (WMH), which represents ischemic small vessel disease. Participants underwent consensus diagnosis at both timepoints (59% Cognitively‐Stable at both timepoints, 9% Cognitively‐Stable to MCI‐DS, 8% MCI‐DS at both timepoints, 14% MCI‐DS to AD, 10% AD at both timepoints). The annual rate of change in frontal, temporal, parietal, and occipital WMH volume was assessed, adjusting for baseline WMH volume.

Result: The annual rate of change in frontal WMH was not significantly different by diagnosis. The annual rate of change in temporal (0.7 [0.4, 1.1], p<0.001) and in occipital WMH (1.6 [0.7, 2.5], p=0.0008) was faster in the group that remained AD at both timepoints compared to the group that remained Cognitively‐Stable at both timepoints. The annual rate of change in parietal WMH was greater in the group that progressed from MCI‐DS to AD (0.6 [0.1, 1.0], p=0.02) and in the group that remained AD at both timepoints (1.1 [0.6, 1.7], p=0.0002) compared to the group that remained Cognitively‐Stable at both timepoints.

Conclusion: In adults with DS, parietal WMH accumulates fastest in those that progress to or have a diagnosis of AD, while temporal and occipital WMH accumulate fastest in those with a diagnosis of AD. Posteriorly distributed WMH may have specificity for AD progression in adults with DS with implications for anti‐amyloid therapeutics that have cerebrovascular side effects.

Description
Keywords
Down syndrome (DS), Amyloid precursor protein, Amyloid plaques, Alzheimer’s disease (AD), Cerebrovascular disease
item.page.description.tableofcontents
item.page.relation.haspart
Cite As
Lao PJ, Edwards NC, Flores‐Aguilar L, et al. Longitudinal changes in neuroimaging markers of small vessel disease: Implications for clinical trials. Alzheimers Dement. 2025;20(Suppl 2):e092029. Published 2025 Jan 9. doi:10.1002/alz.092029
ISSN
Publisher
Series/Report
Sponsorship
Major
Extent
Identifier
Relation
Journal
Alzheimer's & Dementia
Rights
Attribution 4.0 International Creative Commons licenses
Source
PMC
Alternative Title
Type
Abstract
Number
Volume
Conference Dates
Conference Host
Conference Location
Conference Name
Conference Panel
Conference Secretariat Location
Permanent Link
https://hdl.handle.net/1805/46084
DOI
https://doi.org/10.1002/alz.092029
Version
Final published version
Full Text Available at
This item is under embargo {{howLong}}
Collections
Open Access Policy Articles