Frontiers in Psychiatry (Feb 2024)

Genetic risk for hospitalization of African American patients with severe mental illness reveals HLA loci

  • Adriana Lori,
  • Adriana Lori,
  • Brad D. Pearce,
  • Seyma Katrinli,
  • Sierra Carter,
  • Charles F. Gillespie,
  • Bekh Bradley,
  • Aliza P. Wingo,
  • Aliza P. Wingo,
  • Tanja Jovanovic,
  • Vasiliki Michopoulos,
  • Erica Duncan,
  • Erica Duncan,
  • Rebecca C. Hinrichs,
  • Alicia Smith,
  • Alicia Smith,
  • Kerry J. Ressler,
  • Kerry J. Ressler

DOI
https://doi.org/10.3389/fpsyt.2024.1140376
Journal volume & issue
Vol. 15

Abstract

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BackgroundMood disorders such as major depressive and bipolar disorders, along with posttraumatic stress disorder (PTSD), schizophrenia (SCZ), and other psychotic disorders, constitute serious mental illnesses (SMI) and often lead to inpatient psychiatric care for adults. Risk factors associated with increased hospitalization rate in SMI (H-SMI) are largely unknown but likely involve a combination of genetic, environmental, and socio-behavioral factors. We performed a genome-wide association study in an African American cohort to identify possible genes associated with hospitalization due to SMI (H-SMI).MethodsPatients hospitalized for psychiatric disorders (H-SMI; n=690) were compared with demographically matched controls (n=4467). Quality control and imputation of genome-wide data were performed following the Psychiatric Genetic Consortium (PGC)-PTSD guidelines. Imputation of the Human Leukocyte Antigen (HLA) locus was performed using the HIBAG package.ResultsGenome-wide association analysis revealed a genome-wide significant association at 6p22.1 locus in the ubiquitin D (UBD/FAT10) gene (rs362514, p=9.43x10-9) and around the HLA locus. Heritability of H-SMI (14.6%) was comparable to other psychiatric disorders (4% to 45%). We observed a nominally significant association with 2 HLA alleles: HLA-A*23:01 (OR=1.04, p=2.3x10-3) and HLA-C*06:02 (OR=1.04, p=1.5x10-3). Two other genes (VSP13D and TSPAN9), possibly associated with immune response, were found to be associated with H-SMI using gene-based analyses.ConclusionWe observed a strong association between H-SMI and a locus that has been consistently and strongly associated with SCZ in multiple studies (6p21.32-p22.1), possibly indicating an involvement of the immune system and the immune response in the development of severe transdiagnostic SMI.

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