4.6 Article

Cortical Thickness and Hippocampal Volume in Vascular and Non-vascular Depressed Patients

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FRONTIERS IN PSYCHIATRY
卷 12, 期 -, 页码 -

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FRONTIERS MEDIA SA
DOI: 10.3389/fpsyt.2021.697489

关键词

vascular depression; white matter hyperintensities; cortical thickness; hippocampal volume; mild cognitive impairment

资金

  1. National Institute of Mental Health [K23 MH075006, R21 MH087774]

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Statistical analysis did not find any differences in cortical thickness or hippocampal volume between VD and non-VD patients, suggesting that VD may not be associated with other late-life psychiatric illnesses and that vascular disease may not be a common etiological risk factor for depression and dementia. Further research involving larger datasets, prospective longitudinal studies, and cognitively intact controls is needed to address these questions.
Background: Reduced cortical thickness and hippocampal volume are prevalent markers of late life depression as well as mild cognitive impairment (MCI) but are conspicuously absent in the vascular depression (VD) literature. The present study aimed to determine differences in cortical thickness and hippocampal volume between VD and non-VD patients. Methods: Participants were enrolled in an 8-week open treatment antidepressant trial. Forty-one depressed individuals aged 50 and older underwent brain magnetic resonance imaging at baseline and were classified as VD or non-VD. Cortical thickness values for the left and right entorhinal, parahippocampal, and precuneal cortices, as well as left and right hippocampal volume, were linearly regressed on VD status to determine mean differences between VD and non-VD. Covariates included site, age, sex, and mean thickness or intracranial volume. Results: No statistical differences were found between VD and non-VD patients in cortical thickness of the bilateral precuneal, entorhinal, or parahippocampal cortices, or hippocampal volume (p > 0.001). Conclusions: The absence of statistical differences in gray matter between VD and non-VD patients raises several diagnostic, etiological, and developmental possibilities, namely that VD may not be connected with other late-life psychiatric illnesses such as MCI or dementia and that vascular disease may not be a common etiological risk factor for depression and dementia. Larger datasets, prospective longitudinal studies, and cognitively intact controls are needed to further address these types of questions.

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