Truncating mutations in RBM12 are associated with psychosis

Steinberg, Stacy; Guðmundsdóttir, Steinunn; Sveinbjörnsson, Garðar; Suvisaari, Jaana; Paunio, Tiina; Holm, Minna; Frigge, Michael L.; Jónsdóttir, Guðrún A.; Huttenlocher, Johanna; Arnarsdóttir, Sunna; Ingimarsson, Oddur; Haraldsson, Magnús; Tyrfingsson, Þorarinn; Thorgeirsson, Thorgeir E.; Kong, Augustine; Norddahl, Gudmundur L.; Guðbjartsson, Daníel F.; Sigurðsson, Engilbert; Stefánsson, Hreinn; Stefánsson, Kári

doi:10.1038/ng.3894

Cited by 65 publications

(61 citation statements)

References 45 publications

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“…Genomic studies are particularly important for idiopathic psychiatric disorders that have few proven/reproducible biological risk factors despite twinfamily studies conclusively establishing a role for inheritance 3,4 . Hopes that protein-coding variation would provide a key to schizophrenia 5,6 have not eventuated as sizable exome sequencing studies have identified only two genes to date 7,8 . In contrast, exome sequencing studies for autism identified ~100 genes with far fewer cases than for schizophrenia 9 .…”

Section: Introductionmentioning

confidence: 99%

Using three-dimensional regulatory chromatin interactions from adult and fetal cortex to interpret genetic results for psychiatric disorders and cognitive traits

Giusti‐Rodríguez¹,

Yang³

et al. 2018

Preprint

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Genome-wide association studies have identified hundreds of genetic associations for complex psychiatric disorders and cognitive traits. However, interpretation of most of these findings is complicated by the presence of many significant and highly correlated genetic variants located in noncoding regions. Here, we address this issue by creating a high-resolution map of the three-dimensional (3D) genome organization by applying Hi-C to adult and fetal brain cortex with concomitant RNA-seq, open chromatin (ATAC-seq), and ChIP-seq data (H3K27ac, H3K4me3, and CTCF). Extensive analyses established the quality, information content, and salience of these new Hi-C data. We used these data to connect 938 significant genetic loci for schizophrenia, intelligence, ADHD, alcohol dependence, Page 2 Alzheimer's disease, anorexia nervosa, autism spectrum disorder, bipolar disorder, major depression, and educational attainment to 8,595 genes (with 42.1% of these genes implicated more than once). We show that assigning genes to traits based on proximity provides a limited view of the complexity of GWAS findings and that gene set analyses based on functional genomic data provide an expanded view of the biological processes involved in the etiology of schizophrenia and other complex brain traits.URLs 1000 Genomes Selection Browser,

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Section: Introductionmentioning

confidence: 99%

Using three-dimensional regulatory chromatin interactions from adult and fetal cortex to interpret genetic results for psychiatric disorders and cognitive traits

Giusti‐Rodríguez¹,

Yang³

et al. 2018

Preprint

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“…More recent whole exome sequencing (WES)/whole genome sequencing in small/modest sized multiplex families have added to the list of inherited rare protein coding variants. These include variants in previously analyzed candidate genes namely RELN (Zhou et al, 2016), UNC13B (Egawa et al, 2016), GRM5, LRP1B, and PPEF2 (Timms et al, 2013),GRIN3B (Hornig et al, 2017), SHANK2 and SMARCA1 (Homann et al, 2016), ANKK1 (Shirzad et al, 2016), RBM12 (Steinberg et al, 2017), TAAR1 (John et al, 2017), TIMP2 (John et al, 2018)and PTPRA (John et al, 2018).These insightful studies suggest the importance of such variants with large/moderate effects in disease development or in increasing the risk in the respective families with disease clustering.…”

Section: Introductionmentioning

confidence: 85%

Oligogenic rare variant contributions in schizophrenia and their convergence with genes harbouringde novomutations in schizophrenia, autism and intellectual disability: Evidence from multiplex families

John

Kukshal

Bhatia

et al. 2019

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Clinical and genetic heterogeneity has been documented extensively in schizophrenia, a common behavioural disorder with heritability estimates of about 80%. Common and rare de novo variant based studies have provided notable evidence for the likely involvement of a range of pathways including glutamatergic, synaptic signalling and neurodevelopment. To complement these studies, we sequenced exomes of 11 multimember affected schizophrenia families from India. Variant prioritisation performed based on their rarity (MAF <0.01), shared presence among the affected individuals in the respective families and predicted deleterious nature, yielded a total of 785 inherited rare protein sequence altering variants in 743 genes among the 11 families. These showed an enrichment of genes involved in the extracellular matrix and cytoskeleton components, synaptic and neuron related ontologies and neurodevelopmental pathways, consistent with major etiological hypotheses. We also noted an overrepresentation of genes from previously reported gene sets with de novo protein sequence altering variants in schizophrenia, autism, intellectual disability; FMRP target and loss of function intolerant genes. Furthermore, a minimum of five genes known to manifest behavioural/neurological and nervous system abnormalities in rodent models had deleterious variants in them shared among all affected individuals in each of the families. Majority of such variants segregated within and not across families providing strong suggestive evidence for the genetically heterogeneous nature of disease.More importantly, study findings unequivocally support the classical paradigm of cumulative contribution of multiple genes, notably with an apparent threshold effect for disease manifestation and offer a likely explanation for the unclear mode of inheritance in familial schizophrenia.Polyphen2_HDIV, Polyphen2_HVAR, LRT, MutationTaster, MutationAssessor, FATHMM, PROVEAN, MetaSVM, M-CAP and fathmm-MKL_coding and CADD scaled score =>15; or CADD scaled score>=10 and <15 but predicted to be damaging by at least two different software listed above) for further analysis. All these tools were part of Kggseq (Li et al., 2012). All these variants are henceforth referred to as "deleterious shared variants".

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“…SCZ cases have been repeatedly shown to carry a greater burden of large/rare CNV (>100 kb and <1%), particularly deletions affecting brainexpressed genes. Multiple rare recurrent CNV with substantial effects on risk for SCZ (genotypic relative risks [4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20] have been identified (e.g., 16p11.2 and 22q11.21) (5)(6)(7)(8)(9)(10). Most of these known CNV risk loci are megabase-sized and affect the dosages of many genes, but if specific genes contributing to risk could be identified it would aid our understanding of the neurobiology of the disorder.…”

Section: Introductionmentioning

confidence: 99%

“…Most of these known CNV risk loci are megabase-sized and affect the dosages of many genes, but if specific genes contributing to risk could be identified it would aid our understanding of the neurobiology of the disorder. Thus far, only a few specific genes from genetic studies of CNV and SNV have been implicated in SCZ: NRXN1 (11), TOP3B (12), RBM12 (13) and SETD1A (14), all of which provided novel insights into SCZ pathophysiology. Therefore, gene-focused CNV evaluation in large samples with high resolution capture is needed.…”

Section: Introductionmentioning

confidence: 99%

Characterization of single gene copy number variants in schizophrenia

Szatkiewicz

Fromer

Nonneman

et al. 2019

Preprint

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Genetic studies of schizophrenia (SCZ) have now implicated numerous genomic loci that contribute to risk including several copy number variants (CNV) of large effect and hundreds of associated loci of small effect. However, in only a few cases has a specific gene been clearly identified. Rare CNV that affect only a single gene offer a potential avenue to discovering specific SCZ risk genes. Here, we use CNV generated from exome-sequencing of 4,913 SCZ cases and 6,188 controls in a homogenous Swedish cohort to assess the contribution of singlegene deletions and duplications to SCZ risk. As previously seen, we found an excess of rare deletions (p = 0.0004) and duplications (p = 0.0006) in SCZ cases compared to controls. When limiting to only single-gene CNV we identified nominally significant excess of deletions (p = 0.04) and duplications (p = 0.03). In an effort to increase the number of single-gene CNV, we reduced strict filtering criteria but required support from two independent CNV calling methods to create an expanded set that showed a significant burden of deletions in 11 out of 22 gene sets previously implicated in SCZ and in the combined set of genes across those sets (p = 0.008).Finally, for the significantly enriched set of voltage-gated calcium channels, we performed an extensive validation of all deletions generated from exome-sequencing as well as any deletion with evidence from previously analyzed genotyping arrays. In total, 4 exonic, single-gene deletions validated in cases and none in controls (p = 0.039), of which all were identified by exome-sequencing. Broadly, these results point to the potential contribution of single-gene CNV to SCZ and the added value of a deeper dive into CNV calls from exome-sequencing.

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Truncating mutations in RBM12 are associated with psychosis

Cited by 65 publications

References 45 publications

Using three-dimensional regulatory chromatin interactions from adult and fetal cortex to interpret genetic results for psychiatric disorders and cognitive traits

Using three-dimensional regulatory chromatin interactions from adult and fetal cortex to interpret genetic results for psychiatric disorders and cognitive traits

Oligogenic rare variant contributions in schizophrenia and their convergence with genes harbouringde novomutations in schizophrenia, autism and intellectual disability: Evidence from multiplex families

Characterization of single gene copy number variants in schizophrenia

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