Leveraging longitudinal diffusion MRI data to quantify differences in white matter microstructural decline in normal and abnormal aging

Author:

Archer Derek B.,Schilling KurtORCID,Shashikumar Niranjana,Jasodanand Varuna,Moore Elizabeth E.,Pechman Kimberly R.,Bilgel MuratORCID,Beason-Held Lori L.ORCID,An Yang,Shafer AndreaORCID,Ferrucci Luigi,Risacher Shannon L.,Gifford Katherine A.,Landman Bennett A.,Jefferson Angela L.,Saykin Andrew J.ORCID,Resnick Susan M.,Hohman Timothy J.ORCID,

Abstract

AbstractINTRODUCTIONIt is unclear how rates of white matter microstructural decline differ between normal aging and abnormal aging.METHODSDiffusion MRI data from several well-established longitudinal cohorts of aging [Alzheimer’s Neuroimaging Initiative (ADNI), Baltimore Longitudinal Study of Aging (BLSA), Vanderbilt Memory & Aging Project (VMAP)] was free-water corrected and harmonized. This dataset included 1,723 participants (age at baseline: 72.8±8.87 years, 49.5% male) and 4,605 imaging sessions (follow-up time: 2.97±2.09 years, follow-up range: 1–13 years, mean number of visits: 4.42±1.98). Differences in white matter microstructural decline in normal and abnormal agers was assessed.RESULTSWhile we found global decline in white matter in normal/abnormal aging, we found that several white matter tracts (e.g., cingulum bundle) were vulnerable to abnormal aging.CONCLUSIONSThere is a prevalent role of white matter microstructural decline in aging, and future large-scale studies in this area may further refine our understanding of the underlying neurodegenerative processes.HIGHLIGHTSLongitudinal data was free-water corrected and harmonizedGlobal effects of white matter decline were seen in normal and abnormal agingThe free-water metric was most vulnerable to abnormal agingCingulum free-water was the most vulnerable to abnormal aging

Publisher

Cold Spring Harbor Laboratory

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