4.5 Article

Early trauma and familial risk in the development of the extended psychosis phenotype in adolescence

Journal

ACTA PSYCHIATRICA SCANDINAVICA
Volume 126, Issue 4, Pages 266-273

Publisher

WILEY
DOI: 10.1111/j.1600-0447.2012.01857.x

Keywords

adolescence; psychosis; development; trauma; parental psychopathology

Categories

Funding

  1. Eli Lilly
  2. BMS
  3. Lundbeck
  4. Organon
  5. Janssen-Cilag
  6. GSK
  7. AstraZeneca
  8. Pfizer
  9. Servier
  10. Astra Zeneca

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Wigman JTW, van Winkel R, Ormel J, Verhulst FC, van Os J, Vollebergh WAM. Early trauma and familial risk in the development of the extended psychosis phenotype in adolescence. Objective: Both genetic and environmental factors are thought to play a role in the development of psychotic outcomes; however, their respective contributions over time, including possible developmental interactions, remain largely unknown. Method: The contribution of parental general and psychotic psychopathology as proxies of genetic risk to the development of subthreshold psychosis and its hypothesized interaction with childhood trauma were studied in a general population sample of 2230 adolescents, followed from age 1016 years. Outcome measures were: i) level of psychotic experiences at age 16 years and ii) persistence of such experiences over the total follow-up period. Results: General parental psychopathology was associated with CAPE score (OR = 1.08; P < 0.043 for highest quintile) and suggestively predicted psychosis persistence (OR, 1.16; P < 0.072). Psychotic parental psychopathology was suggestively associated with CAPE score (OR, 2.25; P < 0.063 for highest quintile), predicted membership of the Persistent group (OR, 3.72; P < 0.039) and suggestively predicted membership of the Decreasing group (OR 2.04; P < 0.051). Childhood trauma was associated with CAPE score and with all developmental trajectories of subclinical psychosis. No evidence was found for an interaction between trauma and parental psychopathology. Conclusion: The development and persistence of subthreshold psychotic symptoms may be conditional on non-interacting proxy genetic and environmental influences.

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