A polygenic burden of rare disruptive mutations in schizophrenia

Purcell, Shaun; Moran, Jennifer L.; Fromer, Menachem; Ruderfer, Douglas M.; Solovieff, Nadia; Roussos, Panos; Ó'Dúshláine, Colm; Chambert, Kimberly; Bergen, Sarah E.; Kähler, Anna K.; Duncan, Laramie; Stahl, Eli A.; Genovese, Giulio; Fernández, Esperanza; Collins, Mark O.; Komiyama, Noboru H.; Choudhary, Jyoti S.; Magnusson, Patrik K. E.; Banks, Eric; Shakir, Khalid; Garimella, Kiran; Fennell, Tim; DePristo, Mark A.; Grant, Seth G. N.; Haggarty, Stephen J.; Gabriel, Stacey; Scolnick, Edward M.; Lander, Eric S.; Hultman, Christina M.; Sullivan, Patrick F.; McCarroll, Steven A.; Sklar, Pamela

doi:10.1038/nature12975

Cited by 1,311 publications

(1,526 citation statements)

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“…IRSp53 has been implicated also in other psychiatric disorders, including ADHD (attention deficit/hyperactivity disorder) 207,208 and schizophrenia 209,210 . Overexpression of IRSp53 in cultured neurons increases the density of dendritic spines without affecting spine length or width.…”

Section: Accepted Manuscriptmentioning

confidence: 99%

Dendritic spine actin cytoskeleton in autism spectrum disorder

Joensuu¹,

Lanoue

Hotulainen

2018

Progress in Neuro-Psychopharmacology and Biological Psychiatry

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Section: Accepted Manuscriptmentioning

confidence: 99%

Dendritic spine actin cytoskeleton in autism spectrum disorder

Joensuu¹,

Lanoue

Hotulainen

2018

Progress in Neuro-Psychopharmacology and Biological Psychiatry

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“…Additional detail on sample ascertainment and sequence data generation has been previously published. 8 BAM and VCF files are available in the dbGaP study phs000473.v1 (http://www.ncbi.nlm.nih.gov/ projects/gap/cgi-bin/study.cgi?study_id = phs000473.v1.p1).…”

Section: Sample Ascertainment and Data Generationmentioning

confidence: 99%

“…Recently, large-scale exome-sequencing studies have searched for rare variants that strongly increase risk, 8,9 although the relatively high baseline rate of rare neutral coding variation makes this challenging. 10 To focus on rare variants that are a priori more likely to be highly penetrant for disease, one approach is to study de novo mutations, as these are effectively uncensored by selection pressures.…”

Section: Introductionmentioning

confidence: 99%

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No evidence for rare recessive and compound heterozygous disruptive variants in schizophrenia

et al. 2014

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“…Examination of the cumulative effects of inheriting multiple risk alleles—each of which are significantly or nominally associated with disease risk—has been able to powerfully differentiate groups of cases from controls in independent population‐based studies [Purcell et al, 2014, 2009; Patel et al, 2010; Ayalew et al, 2012; Terwisscha van Scheltinga et al, 2012]. However, despite phenotypic aggregation within families [McGuffin et al, 2003; Lichtenstein et al, 2009], no studies have so far examined polygenic risk incorporating these common genetic factors in a family context in adults, with only one group to date reporting on polygenic risk in adolescent offspring of individuals with BP [Whalley et al, 2012, 2013].…”

Section: Introductionmentioning

confidence: 99%

Assessment of first and second degree relatives of individuals with bipolar disorder shows increased genetic risk scores in both affected relatives and young At‐Risk Individuals

Fullerton

Koller

Edenberg

et al. 2015

American J of Med Genetics Pt B

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Recent studies have revealed the polygenic nature of bipolar disorder (BP), and identified common risk variants associated with illness. However, the role of common polygenic risk in multiplex families has not previously been examined. The present study examined 249 European‐ancestry families from the NIMH Genetics Initiative sample, comparing subjects with narrowly defined BP (excluding bipolar II and recurrent unipolar depression; n = 601) and their adult relatives without BP (n = 695). Unrelated adult controls (n = 266) were from the NIMH TGEN control dataset. We also examined a prospective cohort of young (12–30 years) offspring and siblings of individuals with BPI and BPII disorder (at risk; n = 367) and psychiatrically screened controls (n = 229), ascertained from five sites in the US and Australia and assessed with standardized clinical protocols. Thirty‐two disease‐associated SNPs from the PGC‐BP Working Group report (2011) were genotyped and additive polygenic risk scores (PRS) derived. We show increased PRS in adult cases compared to unrelated controls (P = 3.4 × 10−5, AUC = 0.60). In families with a high‐polygenic load (PRS score ≥32 in two or more subjects), PRS distinguished cases with BPI/SAB from other relatives (P = 0.014, RR = 1.32). Secondly, a higher PRS was observed in at‐risk youth, regardless of affected status, compared to unrelated controls (GEE‐χ2 = 5.15, P = 0.012). This report is the first to explore common polygenic risk in multiplex families, albeit using only a small number of robustly associated risk variants. We show that individuals with BP have a higher load of common disease‐associated variants than unrelated controls and first‐degree relatives, and illustrate the potential utility of PRS assessment in a family context. © 2015 The Authors. American Journal of Medical Genetics Part B: Neuropsychiatric Genetics Published by Wiley Periodicals, Inc.

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A polygenic burden of rare disruptive mutations in schizophrenia

Cited by 1,311 publications

References 50 publications

Dendritic spine actin cytoskeleton in autism spectrum disorder

Dendritic spine actin cytoskeleton in autism spectrum disorder

No evidence for rare recessive and compound heterozygous disruptive variants in schizophrenia

Assessment of first and second degree relatives of individuals with bipolar disorder shows increased genetic risk scores in both affected relatives and young At‐Risk Individuals

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