Authors
Seonjoo Lee
Molly E. Zimmerman
Atul Narkhede
Sara E. Nasrabady
Giuseppe Tosto
Irene B. Meier
Tammie L.S. Benzinger
Daniel S. Marcus
Anne M. Fagan
Nick C. Fox
Nigel J. Cairns
David M. Holtzman
Virginia Buckles
Bernardino Ghetti
Eric McDade
Ralph Martins, Edith Cowan UniversityFollow
Andrew J. Saykin
Colin L. Masters
John M. Ringman
Stefan Fӧrster
Peter R. Schofield
Reisa A. Sperling
Keith A. Johnson
Jasmeer P. Chhatwal
Stephen Salloway
Stephen Correia
Clifford R. Jack, Jr
Michael Weiner
Randall J. Bateman
John C. Morris
Richard Mayeux
Adam M. Brickman
Document Type
Journal Article
Publication Title
PLoS ONE
Publisher
PLOS
School
School of Medical and Health Sciences
RAS ID
27876
Abstract
Introduction: White matter hyperintensity (WMH) volume on MRI is increased among presymptomatic individuals with autosomal dominant mutations for Alzheimer’s disease (AD). One potential explanation is that WMH, conventionally considered a marker of cerebrovascular disease, are a reflection of cerebral amyloid angiopathy (CAA) and that increased WMH in this population is a manifestation of this vascular form of primary AD pathology. We examined whether the presence of cerebral microbleeds, a marker of CAA, mediates the relationship between WMH and estimated symptom onset in individuals with and without autosomal dominant mutations for AD.
Participants and methods: Participants (n = 175, mean age = 41.1 years) included 112 with an AD mutation and 63 first-degree non-carrier controls. We calculated the estimated years from expected symptom onset (EYO) and analyzed baseline MRI data for WMH volume and presence of cerebral microbleeds. Mixed effects regression and tests of mediation were used to examine microbleed and WMH differences between carriers and non-carriers and to test the whether the association between WMH and mutation status is dependent on the presence of microbleeds.
Results: Mutation carriers were more likely to have microbleeds than non-carriers (p<0.05) and individuals with microbleeds had higher WMH volume than those without (p<0.05). Total WMH volume was increased in mutation carriers compared with non-carriers, up to 20 years prior to EYO, after controlling for microbleed status, as we demonstrated previously. Formal testing of mediation demonstrated that 21% of the association between mutation status and WMH was mediated by presence of microbleeds (p = 0.03) but a significant direct effect of WMH remained (p = 0.02) after controlling for presence of microbleeds.
Discussion: Although there is some co-dependency between WMH and microbleeds, the observed increases in WMH among mutation carriers does not appear to be fully mediated by this marker of CAA. The findings highlight the possibility that WMH represent a core feature of AD independent of vascular forms of beta amyloid.
DOI
10.1371/journal.pone.0195838
Creative Commons License
This work is licensed under a Creative Commons Attribution 4.0 License.
Comments
Lee, S., Zimmerman, M. E., Narkhede, A., Nasrabady, S. E., Tosto, G., Meier, I. B., ... & Cairns, N. J. (2018). White matter hyperintensities and the mediating role of cerebral amyloid angiopathy in dominantly-inherited Alzheimer’s disease. PloS one, 13(5), e0195838. Available here