An exploration of the genetic epidemiology of non-suicidal self-harm and suicide attempt

Abigail Emma Russell; Gibran Hemani; Hannah J Jones; Tamsin Ford; David Gunnell; Jon Heron; Carol Joinson; Paul Moran; Caroline Relton; Matthew Suderman; Sarah Watkins; Becky Mars

doi:10.1186/s12888-021-03216-z

An exploration of the genetic epidemiology of non-suicidal self-harm and suicide attempt

BMC Psychiatry. 2021 Apr 23;21(1):207. doi: 10.1186/s12888-021-03216-z.

Authors

Abigail Emma Russell¹, Gibran Hemani^{2

3}, Hannah J Jones⁴, Tamsin Ford⁵, David Gunnell^{4

6}, Jon Heron⁴, Carol Joinson⁴, Paul Moran^{4

6}, Caroline Relton^{2

3}, Matthew Suderman^{2

3}, Sarah Watkins⁴, Becky Mars^{4

6}

Affiliations

¹ Children and Young People's Mental Health Research Collaboration (ChYMe), University of Exeter College of Medicine and Health, Exeter, UK. a.e.russell@exeter.ac.uk.
² MRC Integrative Epidemiology Unit, University of Bristol Medical School, Bristol, UK.
³ Population Health Sciences, University of Bristol Medical School, Bristol, UK.
⁴ Centre for Academic Mental Health, Population Health Sciences, University of Bristol Medical School, Bristol, UK.
⁵ University of Cambridge Department of Psychiatry, Cambridge, UK.
⁶ NIHR Biomedical Research Centre at the University Hospitals Bristol NHS Foundation Trust and the University of Bristol, Bristol, UK.

Abstract

Background: Empirical evidence supporting the distinction between suicide attempt (SA) and non-suicidal self-harm (NSSH) is lacking. Although NSSH is a risk factor for SA, we do not currently know whether these behaviours lie on a continuum of severity, or whether they are discrete outcomes with different aetiologies. We conducted this exploratory genetic epidemiology study to investigate this issue further.

Methods: We explored the extent of genetic overlap between NSSH and SA in a large, richly-phenotyped cohort (the Avon Longitudinal Study of Parents and Children; N = 4959), utilising individual-level genetic and phenotypic data to conduct analyses of genome-wide complex traits and polygenic risk scores (PRS).

Results: The single nucleotide polymorphism heritability of NSSH was estimated to be 13% (SE 0.07) and that of SA to be 0% (SE 0.07). Of the traits investigated, NSSH was most strongly correlated with higher IQ (rG = 0.31, SE = 0.22), there was little evidence of high genetic correlation between NSSH and SA (rG = - 0.1, SE = 0.54), likely due to the low heritability estimate for SA. The PRS for depression differentiated between those with NSSH and SA in multinomial regression. The optimal PRS prediction model for SA (Nagelkerke R² 0.022, p < 0.001) included ADHD, depression, income, anorexia and neuroticism and explained more variance than the optimal prediction model for NSSH (Nagelkerke R² 0.010, p < 0.001) which included ADHD, alcohol consumption, autism spectrum conditions, depression, IQ, neuroticism and suicide attempt.

Conclusions: Our findings suggest that SA does not have a large genetic component, and that although NSSH and SA are not discrete outcomes there appears to be little genetic overlap between the two. The relatively small sample size and resulting low heritability estimate for SA was a limitation of the study. Combined with low heritability estimates, this implies that family or population structures in SA GWASs may contribute to signals detected.

Keywords: Genetic epidemiology; Polygenic risk scores; Suicide, self-harm, non-suicidal self-injury.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Child
Humans
Longitudinal Studies
Molecular Epidemiology
Risk Factors
Self-Injurious Behavior* / epidemiology
Self-Injurious Behavior* / genetics
Suicidal Ideation
Suicide, Attempted*

Abstract

Publication types

MeSH terms

Grants and funding