Epigenetic markers in inflammation-related genes associated with mood disorder: a cross-sectional and longitudinal study in high-risk offspring of bipolar parents

Anne Duffy; Sarah M. Goodday; Charles Keown-Stoneman; Martina Scotti; Malosree Maitra; Corina Nagy; Julie Horrocks; Gustavo Turecki

doi:10.1186/s40345-019-0152-1

International Journal of Bipolar Disorders (Aug 2019)

Epigenetic markers in inflammation-related genes associated with mood disorder: a cross-sectional and longitudinal study in high-risk offspring of bipolar parents

Anne Duffy,
Sarah M. Goodday,
Charles Keown-Stoneman,
Martina Scotti,
Malosree Maitra,
Corina Nagy,
Julie Horrocks,
Gustavo Turecki

Affiliations

Anne Duffy: Division of Student Mental Health, Department of Psychiatry, Queen’s University
Sarah M. Goodday: Department of Psychiatry, University of Oxford
Charles Keown-Stoneman: Dalla Lana School of Public Health, University of Toronto
Martina Scotti: McGill Group for Suicide Studies, Department of Psychiatry, Douglas Institute, McGill University
Malosree Maitra: McGill Group for Suicide Studies, Department of Psychiatry, Douglas Institute, McGill University
Corina Nagy: McGill Group for Suicide Studies, Department of Psychiatry, Douglas Institute, McGill University
Julie Horrocks: Department of Mathematics and Statistics, Guelph University
Gustavo Turecki: McGill Group for Suicide Studies, Department of Psychiatry, Douglas Institute, McGill University

DOI: https://doi.org/10.1186/s40345-019-0152-1
Journal volume & issue: Vol. 7, no. 1
pp. 1 – 8

Abstract

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Abstract Bipolar disorder is highly heritable and typically onsets in late adolescence or early adulthood. Evidence suggests that immune activation may be a mediating pathway between genetic predisposition and onset of mood disorders. Building on a prior study of mRNA and protein levels in high-risk offspring published in this Journal, we conducted a preliminary examination of methylation profiles in candidate immune genes from a subsample of well-characterized emergent adult (mean 20 years) offspring of bipolar parents from the Canadian Flourish high-risk cohort. Models were adjusted for variable age at DNA collection, sex and antidepressant and mood stabilizer use. On cross-sectional analysis, there was evidence of higher methylation rates for BDNF-1 in high-risk offspring affected (n = 27) and unaffected (n = 23) for mood disorder compared to controls (n = 24) and higher methylation rates in affected high-risk offspring for NR3C1 compared to controls. Longitudinal analyses (25 to 34 months) provided evidence of steeper decline in methylation rates in controls (n = 24) for NR3C1 compared to affected (n = 15) and unaffected (n = 11) high-risk offspring and for BDNF-2 compared to affected high-risk. There was insufficient evidence that changes in any of the candidate gene methylation rates were associated with illness recurrence in high-risk offspring. While preliminary, findings suggest that longitudinal investigation of epigenetic markers in well-characterized high-risk individuals over the peak period of risk may be informative to understand the emergence of bipolar disorder.

Published in International Journal of Bipolar Disorders

ISSN: 2194-7511 (Online)
Publisher: SpringerOpen
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry; Science: Physiology: Neurophysiology and neuropsychology
Website: http://www.journalbipolardisorders.com/

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Abstract

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