Polygenic Contributions to Performance on the Balloon Analogue Risk Task

Author:

Nurmi Erika1,Laughlin Christopher2,de Wit Harriet3ORCID,Palmer Abraham,MacKillop James4ORCID,Cannon Tyrone5ORCID,Bilder Robert6ORCID,Poldrack Russell7,Congdon Eliza8,Sabb Fred,Seaman Lauren,McElroy Jude,Libowitz Mark,Weafer Jennifer,Gray Joshua,Dean Andy9,Hellemann Gerhard,London Edythe9ORCID

Affiliation:

1. Semel Institute for Neuroscience, University of California, Los Angeles,

2. University of California, Los Angeles

3. Univ of Chicago

4. McMaster University

5. Yale University

6. UCLA Neuropsychiatric Institute

7. Stanford University

8. University of California Los Angeles

9. UCLA

Abstract

Abstract Risky decision-making is a common, heritable endophenotype seen across many psychiatric disorders. Its underlying genetic architecture is incompletely explored. We examined behavior in the Balloon Analogue Risk Task (BART), which tests risky decision-making, in two independent samples of European ancestry. One sample (n=1138) comprised healthy participants and some psychiatric patients (53 schizophrenia, 42 bipolar disorder, 47 ADHD); the other (n=911) excluded for recent treatment of various psychiatric disorders but not ADHD. Participants provided DNA and performed the BART, indexed by mean adjusted pumps. We constructed a polygenic risk score (PRS) for discovery in each dataset and tested it in the other as replication. Subsequently, a genome-wide MEGA-analysis, combining both samples, tested genetic correlation with risk-taking self-report in the UK Biobank sample and psychiatric phenotypes characterized by risk-taking (ADHD, Bipolar Disorder, Alcohol Use Disorder, prior cannabis use) in the Psychiatric Genomics Consortium. The PRS for BART performance in one dataset predicted task performance in the replication sample (r=0.13, p=0.000012, pFDR=0.000052), as did the reciprocal analysis (r=0.09, p=0.0083, pFDR=0.04). Excluding participants with psychiatric diagnoses produced similar results. The MEGA-GWAS identified a single SNP (rs12023073; p=3.24 x 10-8) near IGSF21, a protein involved in inhibitory brain synapses; replication samples are needed to validate this result. A PRS for self-reported cannabis use (p=0.00047, pFDR=0.0053), but not self-reported risk-taking or psychiatric disorder status, predicted behavior on the BART in our MEGA-GWAS sample. The findings reveal polygenic architecture of risky decision-making as measured by the BART and highlight its overlap with cannabis use.

Publisher

Research Square Platform LLC

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