Whole Genome Sequencing in Psychiatric Disorders: the WGSPD Consortium

Sanders, Stephan; Neale, Benjamin M.; Huang, Hailiang; Werling, Donna M.; An, Joon-Yong; Dong, Shan; Abecasis, Gonçalo R.; Arguello, P. Alexander; Blangero, John; Boehnke, Michael; Daly, Mark J.; Eggan, Kevin; Geschwind, Daniel H.; Glahn, David C.; Goldstein, David B.; Gur, Raquel E.; Handsaker, Robert E.; McCarroll, Steven A.; Ophoff, Roel A.; Palotie, Aarno; Pato, Carlos N.; Sabatti, Chiara; State, Matthew W.; Willsey, A. Jeremy; Hyman, Steven E.; Addington, Anjené; Lehner, Thomas

doi:10.1101/160499

Cited by 19 publications

(28 citation statements)

References 74 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Burden in annotations experimentally derived from human brain: Annotations from appropriate tissues help predict functional variants 7,28 . We compared case/control burden of noncoding URVs in constrained regions (as defined above CDTS <1% or GERP ≥ 4) within functional annotations experimentally derived from human brain tissue known to effect gene expression.…”

Section: Resultsmentioning

confidence: 99%

“…The analysis of noncoding variants from WGS data is challenging due to the sheer volume of the noncoding genome and limited methods to predict functional changes 28,30,46 . Recently the category-wise association study (CWAS) framework has been developed and applied to WGS studies of autism spectrum disorder using 7608 samples from 1902 families 28,30,46 . The CWAS approach applies multiple annotation methods to define tens of thousands of annotation categories each of which are tested for association and accounted for multiple testing.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Increased burden of ultra-rare structural variants localizing to boundaries of topologically associated domains in schizophrenia

et al. 2020

View full text Add to dashboard Cite

Despite considerable progress in schizophrenia genetics, most findings have been for large rare structural variants and common variants in well-imputed regions with few genes implicated from exome sequencing. Whole genome sequencing (WGS) can potentially provide a more complete enumeration of etiological genetic variation apart from the exome and regions of high linkage disequilibrium. We analyze high-coverage WGS data from 1162 Swedish schizophrenia cases and 936 ancestry-matched population controls. Our main objective is to evaluate the contribution to schizophrenia etiology from a variety of genetic variants accessible to WGS but not by previous technologies. Our results suggest that ultrarare structural variants that affect the boundaries of topologically associated domains (TADs) increase risk for schizophrenia. Alterations in TAD boundaries may lead to dysregulation of gene expression. Future mechanistic studies will be needed to determine the precise functional effects of these variants on biology.

show abstract

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Increased burden of ultra-rare structural variants localizing to boundaries of topologically associated domains in schizophrenia

et al. 2020

View full text Add to dashboard Cite

show abstract

“…As whole-exome and whole-genome sequencing (WES, WGS) have become mainstream, the Whole Genome Sequencing for Psychiatric Disorders consortium is adopting a similar approach as the PGC but for modern resequencing (Sanders et al, 2017). Investigators conducting WES for ASD have formed multiple consortia.…”

Section: Global Consortiamentioning

confidence: 99%

Defining the Genetic, Genomic, Cellular, and Diagnostic Architectures of Psychiatric Disorders

Sullivan

Geschwind

2019

Cell

Self Cite

346

303

View full text Add to dashboard Cite

Studies of the genetics of psychiatric disorders have become one of the most exciting and fastmoving areas in human genetics. A decade ago, there were few reproducible findings, and now there are hundreds. In this review, we focus on the findings that have illuminated the genetic architecture of psychiatric disorders and the challenges of using these findings to inform our understanding of pathophysiology. The evidence is now overwhelming that psychiatric disorders are ''polygenic''-that many genetic loci contribute to risk. With the exception of a subset of those with ASD, few individuals with a psychiatric disorder have a single, deterministic genetic cause; rather, developing a psychiatric disorder is influenced by hundreds of different genetic variants, consistent with a polygenic model. As progressively larger studies have uncovered more about their genetic architecture, the need to elucidate additional architectures has become clear. Even if we were to have complete knowledge of the genetic architecture of a psychiatric disorder, full understanding requires deep knowledge of the functional genomic architecture-the implicated loci impact regulatory processes that influence gene expression and the functional coordination of genes that control biological processes. Following from this is cellular architecture: of all brain regions, cell types, and developmental stages, where and when are the functional architectures operative? Given that the genetic architectures of different psychiatric disorders often strongly overlap, we are challenged to re-evaluate and refine the diagnostic architectures of psychiatric disorders using fundamental genetic and neurobiological data.

show abstract

“…Over the past two decades, the genetics of autism spectrum disorder (ASD) have advanced spectacularly. From the early hard-won successes cloning genes for monogenic forms of intellectual and social disability (European Chromosome 16 Tuberous Sclerosis Consortium, 1993;van Slegtenhorst et al, 1997;Verkerk et al, 1991) to current large-scale studies utilizing wholegenome sequencing (Brandler et al, 2018;Sanders et al, 2017;Turner et al, 2017;Werling et al, 2018;Yuen et al, 2015), the field has evolved to a point where discovery in so-called idiopathic or ''non-syndromic'' forms of the syndrome (nsASD) is now highly reliable and reproducible, yielding dozens of well-established risk genes (De Rubeis et al, 2014;Dong et al, 2014;Iossifov et al, 2012Iossifov et al, , 2014Neale et al, 2012;O'Roak et al, 2011O'Roak et al, , 2012bSanders et al, 2012Sanders et al, , 2015. Importantly, in contrast to later-onset psychiatric disorders, such as schizophrenia, bipolar disorder, and major depression, where genomic studies aimed at identifying individual genes have mainly highlighted a highly polygenic risk architecture involving the simultaneous contribution of multiple alleles of very small effect (Bipolar Disorder and Schizophrenia Working Group, 2018;Lee et al, 2013;Schizophrenia Working Group of the Psychiatric Genomics Consortium, 2014;Wray et al, 2018), progress in nsASD has been notable for the discovery of rare, de novo, germline, coding, heterozygous mutations carrying large effects in the individual.…”

mentioning

confidence: 99%

Lost in Translation: Traversing the Complex Path from Genomics to Therapeutics in Autism Spectrum Disorder

Šestan

State

2018

Neuron

Self Cite

104

View full text Add to dashboard Cite

Recent progress in the genomics of non-syndromic autism spectrum disorder (nsASD) highlights rare, largeeffect, germline, heterozygous de novo coding mutations. This distinguishes nsASD from later-onset psychiatric disorders where gene discovery efforts have predominantly yielded common alleles of small effect. These differences point to distinctive opportunities for clarifying the neurobiology of nsASD and developing novel treatments. We argue that the path ahead also presents key challenges, including distinguishing human pathophysiology from the potentially pleiotropic neurobiology mediated by established risk genes. We present our view of some of the conceptual limitations of traditional studies of model organisms, suggest a strategy focused on investigating the convergence of multiple nsASD genes, and propose that the detailed characterization of the molecular and cellular landscapes of developing human brain is essential to illuminate disease mechanisms. Finally, we address how recent advances are leading to novel strategies for therapeutics that target various points along the path from genes to behavior.

show abstract

Whole Genome Sequencing in Psychiatric Disorders: the WGSPD Consortium

Cited by 19 publications

References 74 publications

Increased burden of ultra-rare structural variants localizing to boundaries of topologically associated domains in schizophrenia

Increased burden of ultra-rare structural variants localizing to boundaries of topologically associated domains in schizophrenia

Defining the Genetic, Genomic, Cellular, and Diagnostic Architectures of Psychiatric Disorders

Lost in Translation: Traversing the Complex Path from Genomics to Therapeutics in Autism Spectrum Disorder

Contact Info

Product

Resources

About