4.7 Article

Late-life depression accentuates cognitive weaknesses in older adults with small vessel disease

Journal

NEUROPSYCHOPHARMACOLOGY
Volume 47, Issue 2, Pages 580-587

Publisher

SPRINGERNATURE
DOI: 10.1038/s41386-021-00973-z

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Funding

  1. National Institute of Mental Health (NIMH) [R01 MH097735, T32 MH019132-30]

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The neuroimaging features of small vessel disease (SVD) are highly prevalent in older adults and are associated with significant variability in clinical symptoms. A novel metric, peak width of skeletonized mean diffusivity (PSMD), was found to predict cognitive performance disparities in late-life depression (LLD). PSMD outperformed conventional markers in predicting cognitive deficits associated with vascular pathology in LLD participants.
Neuroimaging features of small vessel disease (SVD) are highly prevalent in older adulthood and associated with significant variability in clinical symptoms, yet the factors predicting these symptom disparities are poorly understood. We employed a novel metric of SVD, peak width of skeletonized mean diffusivity (PSMD), to elucidate the relationship of late-life depression (LLD) to the cognitive presentation of vascular pathology. A total of 109 older adults without a diagnosis of a neurocognitive disorder were enrolled in the study; 44 with major depressive disorder and 65 age-matched controls. Subjects completed neuropsychological testing and magnetic resonance imaging including FLAIR and diffusion tensor imaging sequences, from which white matter hyperintensity volume and diffusion metrics (fractional anisotropy, mean diffusivity, PSMD) were quantified. In hierarchical models, the relationship between vascular burden and cognitive performance varied as a function of diagnostic status, such that the negative association between PSMD and processing speed was significantly stronger in participants with LLD compared to controls. Greater PSMD also predicted poorer performance on delayed memory and executive function tasks specifically among those with LLD, while there were no associations between PSMD and task performance among controls. PSMD outperformed conventional SVD and diffusion markers in predicting cognitive performance and dysexecutive behaviors in participants with LLD. These data suggest that LLD may confer a vulnerability to the cognitive manifestations of white matter abnormalities in older adulthood. PSMD, a novel biomarker of diffuse microstructural changes in SVD, may be a more sensitive marker of subtle cognitive deficits stemming from vascular pathology in LLD.

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