Literature DB >> 28525603

Genome-Wide Association Study of Psychosis Proneness in the Finnish Population.

Alfredo Ortega-Alonso1,2, Jesper Ekelund2,3,4, Antti-Pekka Sarin1,2,5, Jouko Miettunen6,7, Juha Veijola7,8,9, Marjo-Riitta Järvelin6,10,11,12, William Hennah1,2.   

Abstract

The current study examined quantitative measures of psychosis proneness in a nonpsychotic population, in order to elucidate their underlying genetic architecture and to observe if there is any commonality to that already detected in the studies of individuals with overt psychotic conditions, such as schizophrenia and bipolar disorder. Heritability, univariate and multivariate genome-wide association (GWAs) tests, including a series of comprehensive gene-based association analyses, were developed in 4269 nonpsychotic persons participating in the Northern Finland Birth Cohort 1966 study with information on the following psychometric measures: Hypomanic Personality, Perceptual Aberration, Physical and Social Anhedonia (also known as Chapman's Schizotypia scales), and Schizoidia scale. Genome-wide genetic data was available for ~9.84 million SNPs. Heritability estimates ranged from 16% to 27%. Phenotypic, genetic and environmental correlations ranged from 0.04-0.43, 0.25-0.73, and 0.12-0.43, respectively. Univariate GWAs tests revealed an intronic SNP (rs12449097) at the TMC7 gene (16p12.3) that significantly associated (P = 3.485 × 10-8) with the hypomanic scale. Bivariate GWAs tests including the hypomanic and physical anhedonia scales suggested a further borderline significant SNP (rs188320715; P-value = 5.261 × 10-8, ~572 kb downstream the ARID1B gene at 6q25.3). Gene-based tests highlighted 20 additional genes of which 5 had previously been associated to schizophrenia and/or bipolar disorder: CSMD1, CCDC141, SLC1A2, CACNA1C, and SNAP25. Altogether the findings explained from 3.7% to 14.1% of the corresponding trait heritability. In conclusion, this study provides preliminary genomic evidence suggesting that qualitatively similar biological factors may underlie different psychosis proneness measures, some of which could further predispose to schizophrenia and bipolar disorder.
© The Author 2017. Published by Oxford University Press on behalf of the Maryland Psychiatric Research Center. All rights reserved. For permissions, please email: journals.permissions@oup.com.

Entities:  

Keywords:  Finnish population; bipolar disorder; genome-wide association study; heritability; psychoses proneness; schizophrenia

Mesh:

Year:  2017        PMID: 28525603      PMCID: PMC5737890          DOI: 10.1093/schbul/sbx006

Source DB:  PubMed          Journal:  Schizophr Bull        ISSN: 0586-7614            Impact factor:   9.306


  65 in total

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3.  Testing the psychosis continuum: differential impact of genetic and nongenetic risk factors and comorbid psychopathology across the entire spectrum of psychosis.

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Journal:  Schizophr Bull       Date:  2011-04-27       Impact factor: 9.306

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Authors: 
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6.  Negative psychotic symptoms and impaired role functioning predict transition outcomes in the at-risk mental state: a latent class cluster analysis study.

Authors:  L R Valmaggia; D Stahl; A R Yung; B Nelson; P Fusar-Poli; P D McGorry; P K McGuire
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Review 8.  A systematic review and meta-analysis of the psychosis continuum: evidence for a psychosis proneness-persistence-impairment model of psychotic disorder.

Authors:  J van Os; R J Linscott; I Myin-Germeys; P Delespaul; L Krabbendam
Journal:  Psychol Med       Date:  2008-07-08       Impact factor: 7.723

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Journal:  Nat Genet       Date:  2013-08-25       Impact factor: 38.330

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Journal:  Neuroscience       Date:  2018-12-21       Impact factor: 3.590

Review 2.  Understanding Anhedonia from a Genomic Perspective.

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Journal:  Curr Top Behav Neurosci       Date:  2022

3.  Variants in regulatory elements of PDE4D associate with major mental illness in the Finnish population.

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6.  CAMDI interacts with the human memory-associated protein KIBRA and regulates AMPAR cell surface expression and cognition.

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7.  Genetic underpinnings of affective temperaments: a pilot GWAS investigation identifies a new genome-wide significant SNP for anxious temperament in ADGRB3 gene.

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10.  Vulnerability to bipolar disorder is linked to sleep and sleepiness.

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