4.6 Article

Molecular Genetic Risk for Psychosis Is Associated With Psychosis Risk Symptoms in a Population-Based UK Cohort: Findings From Generation Scotland

期刊

SCHIZOPHRENIA BULLETIN
卷 46, 期 5, 页码 1045-1052

出版社

OXFORD UNIV PRESS
DOI: 10.1093/schbul/sbaa042

关键词

schizotypal; schizophrenia; genetic; polygenic; risk; Generation Scotland

资金

  1. National Institute of Mental Health [K01MH093731]
  2. Brain & Behavior Research Foundation
  3. Simons Foundation
  4. American Foundation for Suicide Prevention
  5. Tanner Foundation
  6. Chief Scientist Office of the Scottish Government Health Directorates [CZD/16/6]
  7. Scottish Funding Council [HR03006]
  8. Medical Research Council UK
  9. Wellcome Trust [104036/Z/14/Z]
  10. Wellcome Trust [104036/Z/14/Z] Funding Source: researchfish
  11. MRC [MC_UU_00007/10] Funding Source: UKRI

向作者/读者索取更多资源

Objective: Subthreshold psychosis risk symptoms in the general population may be associated with molecular genetic risk for psychosis. This study sought to optimize the association of risk symptoms with genetic risk for psychosis in a large population-based cohort in the UK (N = 9104 individuals 18-65 years of age) by properly accounting for population stratification, factor structure, and sex.Methods: The newly expanded Generation Scotland: Scottish Family Health Study includes 5391 females and 3713 males with age M [SD] = 45.2 [13] with both risk symptom data and genetic data. Subthreshold psychosis symptoms were measured using the Schizotypal Personality Questionnaire-Brief (SPQ-B) and calculation of polygenic risk for schizophrenia was based on 11 425 349 imputed common genetic variants passing quality control. Follow-up examination of other genetic risks included attention-deficit hyperactivity disorder (ADHD), autism, bipolar disorder, major depression, and neuroticism.Results: Empirically derived symptom factor scores reflected interpersonal/negative symptoms and were positively associated with polygenic risk for schizophrenia. This signal was largely sex specific and limited to males. Across both sexes, scores were positively associated with neuroticism and major depressive disorder.Conclusions: A data-driven phenotypic analysis enabled detection of association with genetic risk for schizophrenia in a population-based sample. Multiple polygenic risk signals and important sex differences suggest that genetic data may be useful in improving future phenotypic risk assessment.

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