Genome‐wide DNA methylation analysis of aggressive behaviour: a longitudinal population‐based study

Author:

Pishva Ehsan12,van den Hove Daniel L. A.13,Laroche Valentin1,Lvovs Aneth45,Roy Arunima3,Ortega Gabriela3,Burrage Joe2,Veidebaum Toomas6,Kanarik Margus5,Mill Jonathan2,Lesch Klaus‐Peter13,Harro Jaanus5

Affiliation:

1. Department of Psychiatry and Neuropsychology, School for Mental Health and Neuroscience (MHeNs) Maastricht University Maastricht The Netherlands

2. College of Medicine and Health University of Exeter Medical School Exeter UK

3. Division of Molecular Psychiatry, Center of Mental Health University of Würzburg Würzburg Germany

4. School of Natural Sciences and Health Tallinn University Tallinn Estonia

5. Chair of Neuropsychopharmacology, Institute of Chemistry University of Tartu Tartu Estonia

6. National Institute for Health Development Tallinn Estonia

Abstract

BackgroundHuman aggression is influenced by an interplay between genetic predisposition and experience across the life span. This interaction is thought to occur through epigenetic mechanisms, inducing differential gene expression, thereby moderating neuronal cell and circuit function, and thus shaping aggressive behaviour.MethodsGenome‐wide DNA methylation (DNAm) levels were measured in peripheral blood obtained from 95 individuals participating in the Estonian Children Personality Behaviours and Health Study (ECPBHS) at 15 and 25 years of age. We examined the association between aggressive behaviour, as measured by Life History of Aggression (LHA) total score and DNAm levels both assessed at age 25. We further examined the pleiotropic effect of genetic variants regulating LHA‐associated differentially methylated positions (DMPs) and multiple traits related to aggressive behaviours. Lastly, we tested whether the DNA methylomic loci identified in association with LHA at age 25 were also present at age 15.ResultsWe found one differentially methylated position (DMP) (cg17815886; p = 1.12 × 10−8) and five differentially methylated regions (DMRs) associated with LHA after multiple testing adjustments. The DMP annotated to the PDLIM5 gene, and DMRs resided in the vicinity of four protein‐encoding genes (TRIM10, GTF2H4, SLC45A4, B3GALT4) and a long intergenic non‐coding RNA (LINC02068). We observed evidence for the colocalization of genetic variants associated with top DMPs and general cognitive function, educational attainment and cholesterol levels. Notably, a subset of the DMPs associated with LHA at age 25 also displayed altered DNAm patterns at age 15 with high accuracy in predicting aggression.ConclusionsOur findings highlight the potential role of DNAm in the development of aggressive behaviours. We observed pleiotropic genetic variants associated with identified DMPs, and various traits previously established to be relevant in shaping aggression in humans. The concordance of DNAm signatures in adolescents and young adults may have predictive value for inappropriate and maladaptive aggression later in life.

Funder

Horizon 2020 Framework Programme

Publisher

Wiley

Subject

Psychiatry and Mental health,Developmental and Educational Psychology,Pediatrics, Perinatology and Child Health

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