Open Targets Genetics: systematic identification of trait-associated genes using large-scale genetics and functional genomics

Ghoussaini, Maya; Mountjoy, Edward; Carmona, Miguel; Peat, Gareth; Schmidt, Ellen M.; Hercules, Andrew; Fumis, Luca; Miranda, Alfredo; Carvalho-Silva, Denise; Buniello, Annalisa; Burdett, Tony; Hayhurst, James; Baker, Jarrod; Ferrer, Javier; Gonzalez-Uriarte, Asier; Jupp, Simon; Karim, Mohd Anisul; Koscielny, Gautier; Machlitt-Northen, Sandra; Malangone, Claudio; Pendlington, Zoë May; Roncaglia, Paola; Süveges, Dániel; Wright, Deil S.; Vrousgou, Olga; Papa, Eliseo; Parkinson, Helen; MacArthur, Jacqueline A. L.; Todd, John A.; Barrett, Jeffrey C.; Schwartzentruber, Jeremy; Hulcoop, David G.; Ochoa, David; McDonagh, Ellen M.; Dunham, Ian

doi:10.1093/nar/gkaa840

Cited by 340 publications

(380 citation statements)

References 22 publications

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“…Database accessions for the raw gene expression and genotype datasets are listed on the eQTL Catalogue website (https://www.ebi.ac.uk/eqtl/Studies/). Our summary statistics have also been integrated into third party services such as the Open Targets Genetics Portal (102) and FUMA (13). The gene expression matrices will be made available via the EMBL-EBI Expression Atlas (103).…”

Section: Data Availabilitymentioning

confidence: 99%

eQTL Catalogue: a compendium of uniformly processed human gene expression and splicing QTLs

Kerimov

Hayhurst

Manning

et al. 2020

Preprint

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An increasing number of gene expression quantitative trait locus (QTL) studies have made summary statistics publicly available, which can be used to gain insight into human complex traits by downstream analyses such as fine-mapping and colocalisation. However, differences between these datasets in their variants tested, allele codings, and in the transcriptional features quantified are a barrier to their widespread use. Here, we present the eQTL Catalogue, a resource which contains quality controlled, uniformly re-computed QTLs from 19 eQTL publications. In addition to gene expression QTLs, we have also identified QTLs at the level of exon expression, transcript usage, and promoter, splice junction and 3ʹ end usage. Our summary statistics can be downloaded by FTP or accessed via a REST API and are also accessible via the Open Targets Genetics Portal. We demonstrate how the eQTL Catalogue and GWAS Catalog APIs can be used to perform colocalisation analysis between GWAS and QTL results without downloading and reformatting summary statistics. New datasets will continuously be added to the eQTL Catalogue, enabling systematic interpretation of human GWAS associations across a large number of cell types and tissues. The eQTL Catalogue is available at https

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Section: Data Availabilitymentioning

confidence: 99%

eQTL Catalogue: a compendium of uniformly processed human gene expression and splicing QTLs

Kerimov

Hayhurst

Manning

et al. 2020

Preprint

Self Cite

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“…For example, drugs that have targets with underlying evidence for a genetic association with the relevant disease are twice as likely to succeed in clinical trials and be approved ( 5 , 6 ). To this end, a major new feature in the Platform is the incorporation of evidence from the Open Targets Genetics Portal ( https://genetics.opentargets.org/ ), which integrates publicly available human genome-wide association (GWAS) data with functional genomics to associate disease loci with target genes ( 7 ). The evidence from the genetics portal is integrated into our scoring system and informs target prioritisation for a given disease.…”

Section: Introductionmentioning

confidence: 99%

“…Nevertheless, it remains a long-standing challenge to link these loci to targetable causal genes. The Open Targets Genetics Portal addresses this problem by interpreting manually curated associations from the GWAS catalog, as well as independent signals from GWAS with publicly available summary statistics, most importantly the UK Biobank GWAS data ( 7 , 24 , 25 ). The Genetics Portal performs fine-mapping to narrow down the likely set of causal variants at a given trait-associated locus and to identify the potential causal gene for a particular association.…”

Section: Introductionmentioning

confidence: 99%

Open Targets Platform: supporting systematic drug–target identification and prioritisation

Ochoa

Hercules

Carmona

et al. 2020

Nucleic Acids Research

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The Open Targets Platform (https://www.targetvalidation.org/) provides users with a queryable knowledgebase and user interface to aid systematic target identification and prioritisation for drug discovery based upon underlying evidence. It is publicly available and the underlying code is open source. Since our last update two years ago, we have had 10 releases to maintain and continuously improve evidence for target–disease relationships from 20 different data sources. In addition, we have integrated new evidence from key datasets, including prioritised targets identified from genome-wide CRISPR knockout screens in 300 cancer models (Project Score), and GWAS/UK BioBank statistical genetic analysis evidence from the Open Targets Genetics Portal. We have evolved our evidence scoring framework to improve target identification. To aid the prioritisation of targets and inform on the potential impact of modulating a given target, we have added evaluation of post-marketing adverse drug reactions and new curated information on target tractability and safety. We have also developed the user interface and backend technologies to improve performance and usability. In this article, we describe the latest enhancements to the Platform, to address the fundamental challenge that developing effective and safe drugs is difficult and expensive.

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“…These sequence changes are associated with diseases by performing genome-wide association studies (GWAS). The majority of GWAS-associated variants fall in ncRNAs loci, suggesting that they affect complex traits and diseases by altering expression of nearby genes, through regulatory mechanisms [70]. Among the examples that will be mentioned, we will see how the presence of SNPs in the sequence of a ncRNA can inhibit its maturation and therefore its cellular function.…”

Section: Involvement In Human Diseasesmentioning

confidence: 99%

The Implications of ncRNAs in the Development of Human Diseases

López‐Jiménez

Andrés-León

2021

ncRNA

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The mammalian genome comprehends a small minority of genes that encode for proteins (barely 2% of the total genome in humans) and an immense majority of genes that are transcribed into RNA but not encoded for proteins (ncRNAs). These non-coding genes are intimately related to the expression regulation of protein-coding genes. The ncRNAs subtypes differ in their size, so there are long non-coding genes (lncRNAs) and other smaller ones, like microRNAs (miRNAs) and piwi-interacting RNAs (piRNAs). Due to their important role in the maintenance of cellular functioning, any deregulation of the expression profiles of these ncRNAs can dissemble in the development of different types of diseases. Among them, we can highlight some of high incidence in the population, such as cancer, neurodegenerative, or cardiovascular disorders. In addition, thanks to the enormous advances in the field of medical genomics, these same ncRNAs are starting to be used as possible drugs, approved by the FDA, as an effective treatment for diseases.

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Open Targets Genetics: systematic identification of trait-associated genes using large-scale genetics and functional genomics

Cited by 340 publications

References 22 publications

eQTL Catalogue: a compendium of uniformly processed human gene expression and splicing QTLs

eQTL Catalogue: a compendium of uniformly processed human gene expression and splicing QTLs

Open Targets Platform: supporting systematic drug–target identification and prioritisation

The Implications of ncRNAs in the Development of Human Diseases

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