4.7 Article

The association of markers of cerebral small vessel disease and brain atrophy with incidence and course of depressive symptoms-the maastricht study

期刊

JOURNAL OF AFFECTIVE DISORDERS
卷 292, 期 -, 页码 439-447

出版社

ELSEVIER
DOI: 10.1016/j.jad.2021.05.096

关键词

Depression; Depressive symptoms; Cerebral small vessel disease; Brain atrophy; Epidemiology; Cohort studies

资金

  1. European Regional Development Fund via OPZuid
  2. Province of Limburg
  3. Dutch Ministry of Economic Affairs [31O.041]
  4. Stichting De Weijerhorst (Maastricht, The Netherlands)
  5. Pearl String Initiative Diabetes (Amsterdam, the Netherlands)
  6. Cardiovascular Center (CVC, Maastricht, the Netherlands)
  7. CARIM School for Cardiovascular Diseases (Maastricht, the Netherlands)
  8. CAPHRI Care and Public Health Research Institute (Maastricht, the Netherlands)
  9. NUTRIM School for Nutrition and Translational Research in Metabolism (Maastricht, the Netherlands)
  10. Health Foundation Limburg (Maastricht, the Netherlands)
  11. Perimed (Jadrfalla, Sweden)
  12. JanssenCilag B.V. (Tilburg, the Netherlands)
  13. Novo Nordisk Farma B.V. (Alphen aan den Rijn, the Netherlands)
  14. Sanofi Netherlands B.V. (Gouda, the Netherlands)

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Longitudinal investigation revealed that larger white matter hyperintensity volumes were associated with incident and persistent late-life depressive symptoms, while total burden of cerebral small vessel disease was related to persistent depressive symptoms, indicating a potential target for the prevention of chronic late-life depression.
Background: Cerebral small vessel disease (CSVD) and neurodegeneration may be involved in the development and persistence of late-life depressive symptoms, but longitudinal evidence is scarce. We investigated the longitudinal associations of markers of CSVD and brain atrophy with incident depressive symptoms and the course of depressive symptoms, above and below 60 years of age. Methods: White matter hyperintensity volumes (WMH), presence of lacunar infarcts and cerebral microbleeds, and white matter, grey matter, and cerebral spinal fluid volumes were assessed at baseline by 3T MRI in The Maastricht Study (mean age 59.5 +/- 8.5 years, 49.6% women, n=4,347; 16,535 person-years of follow-up). Clinically relevant depressive symptoms (9-item Patient Health Questionnaire >= 10) were assessed at baseline and annually over seven years. We used Cox regression and multinomial logistic regression analyses adjusted for demographic, cardiovascular, and lifestyle risk factors. Results: Above 60 years of age, larger WMH volumes were associated with an increased risk for incident depressive symptoms (HR[95%CI]:1.24[1.04;1.48] per SD) and a persistent course of depressive symptoms (OR:1.44[1.04;2.00] per SD). Total CSVD burden was associated with persistent depressive symptoms irrespective of age (adjusted OR:1.58[1.03;2.43]), while no associations were found for general markers of brain atrophy. Limitationss: Our findings need replication in other large-scale population-based studies. Conclusions: Our findings may suggest a temporal association of larger WMH volume with the incidence and persistence of late-life depression in the general population and may provide a potential target for the prevention of chronic late-life depression.

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