The role of environmental stress and DNA methylation in the longitudinal course of bipolar disorder
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Published:2020-02-12
Issue:1
Volume:8
Page:
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ISSN:2194-7511
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Container-title:International Journal of Bipolar Disorders
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language:en
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Short-container-title:Int J Bipolar Disord
Author:
Comes Ashley L.ORCID, Czamara Darina, Adorjan Kristina, Anderson-Schmidt Heike, Andlauer Till F. M., Budde Monika, Gade Katrin, Hake Maria, Kalman Janos L., Papiol Sergi, Reich-Erkelenz Daniela, Klöhn-Saghatolislam Farah, Schaupp Sabrina K., Schulte Eva C., Senner Fanny, Juckel Georg, Schmauß Max, Zimmermann Jörg, Reimer Jens, Reininghaus Eva, Anghelescu Ion-George, Konrad Carsten, Thiel Andreas, Figge Christian, von Hagen Martin, Koller Manfred, Dietrich Detlef E., Stierl Sebastian, Scherk Harald, Witt Stephanie H., Sivalingam Sugirthan, Degenhardt Franziska, Forstner Andreas J., Rietschel Marcella, Nöthen Markus M., Wiltfang Jens, Falkai Peter, Schulze Thomas G., Heilbronner Urs
Abstract
Abstract
Background
Stressful life events influence the course of affective disorders, however, the mechanisms by which they bring about phenotypic change are not entirely known.
Methods
We explored the role of DNA methylation in response to recent stressful life events in a cohort of bipolar patients from the longitudinal PsyCourse study (n = 96). Peripheral blood DNA methylomes were profiled at two time points for over 850,000 methylation sites. The association between impact ratings of stressful life events and DNA methylation was assessed, first by interrogating methylation sites in the vicinity of candidate genes previously implicated in the stress response and, second, by conducting an exploratory epigenome-wide association analysis. Third, the association between epigenetic aging and change in stress and symptom measures over time was investigated.
Results
Investigation of methylation signatures over time revealed just over half of the CpG sites tested had an absolute difference in methylation of at least 1% over a 1-year period. Although not a single CpG site withstood correction for multiple testing, methylation at one site (cg15212455) was suggestively associated with stressful life events (p < 1.0 × 10−5). Epigenetic aging over a 1-year period was not associated with changes in stress or symptom measures.
Conclusions
To the best of our knowledge, our study is the first to investigate epigenome-wide methylation across time in bipolar patients and in relation to recent, non-traumatic stressful life events. Limited and inconclusive evidence warrants future longitudinal investigations in larger samples of well-characterized bipolar patients to give a complete picture regarding the role of DNA methylation in the course of bipolar disorder.
Funder
Deutsche Forschungsgemeinschaft Bundesministerium für Bildung und Forschung Dr. Lisa Oehler Foundation National Alliance for Research on Schizophrenia and Depression BONFOR Programme of the University of Bonn, Germany Ilídio Pinho professorship and iBiMED at the University of Aveiro
Publisher
Springer Science and Business Media LLC
Subject
Biological Psychiatry,Psychiatry and Mental health
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