4.1 Article

Genetic liability for substance use associated with medical comorbidities in electronic health records of African- and European-ancestry individuals

Journal

ADDICTION BIOLOGY
Volume 27, Issue 1, Pages -

Publisher

WILEY
DOI: 10.1111/adb.13099

Keywords

electronic health record; genome-wide association study; phenome-wide association study; polygenic risk score; substance use disorders

Funding

  1. TAPITMAT in Translational Medicine and Therapeutics [UL1TR001878]
  2. Million Veteran Program, Office of Research and Development, Veterans Health Administration [I01 BX003341, I01 CX001734]
  3. NIAAA [K01AA028292]

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This study investigated the relationship between SUD PRS and primary phenotypes, finding associations but not diagnostic predictability. PheWAS analysis revealed cross-trait associations in psychiatric disorders and medical conditions.
Polygenic risk scores (PRS) represent an individual's summed genetic risk for a trait and can serve as biomarkers for disease. Less is known about the utility of PRS as a means to quantify genetic risk for substance use disorders (SUDs) than for many other traits. Nonetheless, the growth of large, electronic health record-based biobanks makes it possible to evaluate the association of SUD PRS with other traits. We calculated PRS for smoking initiation, alcohol use disorder (AUD), and opioid use disorder (OUD) using summary statistics from the Million Veteran Program sample. We then tested the association of each PRS with its primary phenotype in the Penn Medicine BioBank (PMBB) using all available genotyped participants of African or European ancestry (AFR and EUR, respectively) (N = 18,612). Finally, we conducted phenome-wide association analyses (PheWAS) separately by ancestry and sex to test for associations across disease categories. Tobacco use disorder was the most common SUD in the PMBB, followed by AUD and OUD, consistent with the population prevalence of these disorders. All PRS were associated with their primary phenotype in both ancestry groups. PheWAS results yielded cross-trait associations across multiple domains, including psychiatric disorders and medical conditions. SUD PRS were associated with their primary phenotypes; however, they are not yet predictive enough to be useful diagnostically. The cross-trait associations of the SUD PRS are indicative of a broader genetic liability. Future work should extend findings to additional population groups and for other substances of abuse.

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