Distinct Longitudinal Brain White Matter Microstructure Changes and Associated Polygenic Risk of Common Psychiatric Disorders and Alzheimer’s Disease in the UK Biobank

Max Korbmacher; Dennis van der Meer; Dani Beck; Daniel E. Askeland-Gjerde; Eli Eikefjord; Arvid Lundervold; Ole A. Andreassen; Lars T. Westlye; Ivan I. Maximov

Biological Psychiatry Global Open Science (Jul 2024)

Distinct Longitudinal Brain White Matter Microstructure Changes and Associated Polygenic Risk of Common Psychiatric Disorders and Alzheimer’s Disease in the UK Biobank

Max Korbmacher,
Dennis van der Meer,
Dani Beck,
Daniel E. Askeland-Gjerde,
Eli Eikefjord,
Arvid Lundervold,
Ole A. Andreassen,
Lars T. Westlye,
Ivan I. Maximov

Affiliations

Max Korbmacher: Department of Health and Functioning, Western Norway University of Applied Sciences, Bergen, Norway; NORMENT Centre for Psychosis Research, Division of Mental Health and Addiction, University of Oslo and Oslo University Hospital, Oslo, Norway; Mohn Medical Imaging and Visualization Centre, Bergen, Norway; Address correspondence to Max Korbmacher, M.Sc.
Dennis van der Meer: NORMENT Centre for Psychosis Research, Division of Mental Health and Addiction, University of Oslo and Oslo University Hospital, Oslo, Norway; Faculty of Health, Medicine and Life Sciences, Maastricht University, Maastricht, The Netherlands
Dani Beck: NORMENT Centre for Psychosis Research, Division of Mental Health and Addiction, University of Oslo and Oslo University Hospital, Oslo, Norway; Department of Psychiatric Research, Diakonhjemmet Hospital, Oslo, Norway; Department of Psychology, University of Oslo, Oslo, Norway
Daniel E. Askeland-Gjerde: NORMENT Centre for Psychosis Research, Division of Mental Health and Addiction, University of Oslo and Oslo University Hospital, Oslo, Norway
Eli Eikefjord: Department of Health and Functioning, Western Norway University of Applied Sciences, Bergen, Norway; Mohn Medical Imaging and Visualization Centre, Bergen, Norway
Arvid Lundervold: Mohn Medical Imaging and Visualization Centre, Bergen, Norway; Department of Biomedicine, University of Bergen, Bergen, Norway
Ole A. Andreassen: NORMENT Centre for Psychosis Research, Division of Mental Health and Addiction, University of Oslo and Oslo University Hospital, Oslo, Norway; KG Jebsen Centre for Neurodevelopmental Disorders, University of Oslo, Oslo, Norway
Lars T. Westlye: NORMENT Centre for Psychosis Research, Division of Mental Health and Addiction, University of Oslo and Oslo University Hospital, Oslo, Norway; Department of Psychology, University of Oslo, Oslo, Norway; KG Jebsen Centre for Neurodevelopmental Disorders, University of Oslo, Oslo, Norway
Ivan I. Maximov: Department of Health and Functioning, Western Norway University of Applied Sciences, Bergen, Norway; NORMENT Centre for Psychosis Research, Division of Mental Health and Addiction, University of Oslo and Oslo University Hospital, Oslo, Norway; Ivan I. Maximov, Ph.D.

Journal volume & issue: Vol. 4, no. 4
p. 100323

Abstract

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Background: During the course of adulthood and aging, white matter (WM) structure and organization are characterized by slow degradation processes such as demyelination and shrinkage. An acceleration of such aging processes has been linked to the development of a range of diseases. Thus, an accurate description of healthy brain maturation, particularly in terms of WM features, is fundamental to the understanding of aging. Methods: We used longitudinal diffusion magnetic resonance imaging to provide an overview of WM changes at different spatial and temporal scales in the UK Biobank (UKB) (n = 2678; agescan 1 = 62.38 ± 7.23 years; agescan 2 = 64.81 ± 7.1 years). To examine the genetic overlap between WM structure and common clinical conditions, we tested the associations between WM structure and polygenic risk scores for the most common neurodegenerative disorder, Alzheimer’s disease, and common psychiatric disorders (unipolar and bipolar depression, anxiety, obsessive-compulsive disorder, autism, schizophrenia, attention-deficit/hyperactivity disorder) in longitudinal (n = 2329) and cross-sectional (n = 31,056) UKB validation data. Results: Our findings indicate spatially distributed WM changes across the brain, as well as distributed associations of polygenic risk scores with WM. Importantly, brain longitudinal changes reflected genetic risk for disorder development better than the utilized cross-sectional measures, with regional differences giving more specific insights into gene-brain change associations than global averages. Conclusions: We extend recent findings by providing a detailed overview of WM microstructure degeneration on different spatial levels, helping to understand fundamental brain aging processes. Further longitudinal research is warranted to examine aging-related gene-brain associations.

Published in Biological Psychiatry Global Open Science

ISSN: 2667-1743 (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry: Neurology. Diseases of the nervous system: Psychiatry
Website: https://www.journals.elsevier.com/biological-psychiatry-global-open-science

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