# Genetic Liabilities to Neuropsychiatric Conditions in Suicide Deaths With No Prior Suicidality

**Authors:** Hilary Coon, Andrey A. Shabalin, Eric T. Monson, Emily DiBlasi, Seonggyun Han, Lisa M. Baird, Erin A. Kaufman, Douglas Tharp, Michael J. Staley, Zhe Yu, Qingqin S. Li, Sarah M. Colbert, Amanda V. Bakian, Anna R. Docherty, Andrew M. McIntosh, Heather C. Whalley, Dierdre Amaro, David K. Crockett, Niamh Mullins, Brooks R. Keeshin

PMC · DOI: 10.1001/jamanetworkopen.2025.38204 · JAMA Network Open · 2025-10-20

## TL;DR

This study finds that suicide deaths without prior attempts have lower genetic risks for neuropsychiatric conditions compared to those with prior attempts, suggesting different risk factors.

## Contribution

The study identifies distinct polygenic liabilities in suicide deaths without prior suicidality, challenging the assumption of a single core risk for suicide mortality.

## Key findings

- Suicide deaths without prior suicidality had significantly lower polygenic scores for major depressive disorder, anxiety, and neuroticism compared to those with prior suicidality.
- Genetic liabilities in suicide deaths without prior suicidality were not significantly different from controls for depressed affect, neuroticism, or Alzheimer disease.
- The findings suggest a departure from the traditional view that neuropsychiatric traits alone drive suicide mortality risk.

## Abstract

Although suicide attempt is the most robust estimator of suicide death, few individuals who attempt it go on to die by suicide (<10%), and approximately 50% of suicide deaths occur in the absence of evidence of prior attempts. The risks are particularly poorly understood in this group.

To study underlying polygenic liabilities among suicide deaths without evidence of prior nonfatal suicidality (SD-N) compared with suicide deaths with prior suicidality (SD-S), testing prior results showing significantly lower clinical risks of neuropsychiatric traits in SD-N vs SD-S.

In this cohort study, polygenic scores (PGS) were computed using summary statistics from 12 published source studies, then compared across SD-N and SD-S groups taken from the Utah Suicide Mortality Research Study (cases accrued between December 1998 and October 2022). PGS from the suicide death cohorts were also compared to unselected population controls. Evidence of prior suicidality was determined from diagnoses and clinical notes.

Cohort differences in PGS reflecting neuropsychiatric conditions were tested using analysis of covariance, adjusting for sex, age, and genetic ancestry, followed by additional analyses within sex and within subgroups defined by age at death (50 years or younger vs older than 50 years). PGS spanned 12 neuropsychiatric conditions. Data were analyzed between July 2024 and July 2025.

The SD-N cohort (n = 1337) had significantly more male suicide deaths (1105 [82.65%] vs 974 [67.95%]), with an older mean (SD) age at death (47.5 [18.9] vs 41.4 [15.6] years) than the SD-S cohort (n = 1432). The control cohort (n = 19 499) had significantly fewer males (8597 [44.09%]) than both suicide death subsets. Genetic ancestry was similar across the SD-N and SD-S groups (96.77% and 96.81% European ancestry), and control (97.38% European ancestry) groups. Socioeconomic status was not significantly different across suicide cohorts adjusted for age and sex (occupation ranking SD-N mean [SD], 57.16 [24.54]; SD-S mean [SD], 54.72 [25.29]; t = 1.30; P = .70; maximum education SD-N mean [SD], 2.70 [1.12]; SD-S mean [SD], 2.67 [1.13]; Fisher exact test P = .38). Comparing SD-N to SD-S revealed significantly lower (false discovery rate P < .05) PGS in the SD-N group for major depressive disorder (adjusted mean difference, 0.085 [95% CI, 0.018-0.152]; P = .01), depressed affect (adjusted mean difference, 0.081 [95% CI, 0.012-0.149]; P = .02), anxiety (adjusted mean difference, 0.091 [95% CI, 0.021-0.161]; P = .01), neuroticism (adjusted mean difference, 0.102 [95% CI, 0.033-0.171]; P = .004), and Alzheimer disease (adjusted mean difference, 0.090 [95% CI, 0.021-0.1658]; P = .01), and lower (false discovery rate P < .10) PGS in SD-N for posttraumatic stress disorder (adjusted mean difference, 0.070 [95% CI, 0.001-0.139]; P = .04). Of note, SD-N PGS were not significantly different from controls for depressed affect (adjusted mean difference, 0.037 [95% CI, −0.019 to 0.093]), neuroticism (adjusted mean difference, −0.001 [95% CI, −0.057 to 0.055]), or Alzheimer disease (adjusted mean difference, −0.027 [95% CI, −0.083 to 0.029]).

In this cohort study, SD-N showed significantly different genetic liabilities to neuropsychiatric conditions from SD-S. Results have implications for future suicide research and prevention for persons at risk of mortality.

This cohort study compares polygenic liabilities associated with neuropsychiatric conditions between suicide deaths with vs without evidence of prior nonfatal suicidality.

Do underlying genetic liabilities associated with neuropsychiatric conditions in suicide deaths without evidence of prior suicidality differ from liabilities in suicide deaths with prior suicidality?

This cohort study involving 2769 suicide deaths found that persons in the cohort without prior suicidality showed significantly lower polygenic liabilities associated with neuropsychiatric conditions, mirroring previous clinical results.

Differences in underlying genetic liabilities in suicide deaths without prior suicidality suggest a departure from the traditional assumption that neuropsychiatric traits form a sole central core of suicide mortality risk and impel new directions for future research and prevention efforts.

## Linked entities

- **Diseases:** major depressive disorder (MONDO:0002009), anxiety (MONDO:0005618), Alzheimer disease (MONDO:0004975), posttraumatic stress disorder (MONDO:0005146)

## Full-text entities

- **Diseases:** depressed affect (MESH:D003866), Alzheimer disease (MESH:D000544), Neuropsychiatric Conditions (MESH:D001523), S. (MESH:D018455), SD (MESH:D012735), anxiety (MESH:D001007), death (MESH:D003643), neuropsychiatric traits (MESH:C000631768), posttraumatic stress disorder (MESH:D013313)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Full text

_Full body text omitted from this summary view._ Fetch the complete paper as Markdown: https://tomesphere.com/paper/PMC12538367/full.md

## Figures

4 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12538367/full.md

## References

40 references — full list in the complete paper: https://tomesphere.com/paper/PMC12538367/full.md

---
Source: https://tomesphere.com/paper/PMC12538367