Bayesian Test for Colocalisation between Pairs of Genetic Association Studies Using Summary Statistics

Giambartolomei, Claudia; Vukcevic, Damjan; Schadt, Eric E.; Franke, Lude; Hingorani, Aroon D.; Wallace, Chris; Plagnol, Vincent

doi:10.1371/journal.pgen.1004383

Cited by 2,432 publications

(2,966 citation statements)

References 49 publications

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“…Two distinct approaches have emerged, with overlapping goals: the first is to identify genes with an eQTL driven by an MS risk variant in a locus and the second is to identify specific regulatory elements driving disease risk, and through these, the genes were affected, which must by definition be pathogenic. In attempts to overlap GWAS and eQTL data, the key issue is not just to identify eQTLs in a GWAS locus, but to identify those that appear to be driven by the same underlying genetic variant driving disease risk 59. This has proven a difficult challenge, as a result of linkage disequilibrium60.…”

Section: Identifying Causal Variants and Pathogenic Genesmentioning

confidence: 99%

“…Practically, because eQTL are very common, and many variants show association to disease in a locus, it is likely that at least some variants associated with disease will also have eQTL evidence for a nearby gene 61. Several methods have been proposed to address this colocalisation issue,59, 62 each of which aims to compare GWAS and eQTL data to identify pleiotropic effects between them. Recently, we developed a joint likelihood approach to this problem and used it to compare MS risk associations from the IMSGC ImmunoChip study to eQTL in CD4 + T cells, CD14 + monocytes and lymphoblastoid cell lines 63.…”

Section: Identifying Causal Variants and Pathogenic Genesmentioning

confidence: 99%

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Genome‐wide association studies of multiple sclerosis

Cotsapas¹,

Mitrovič

2018

Clin & Trans Imm

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Large‐scale genetic studies of multiple sclerosis have identified over 230 risk effects across the human genome, making it a prototypical common disease with complex genetic architecture. Here, after a brief historical background on the discovery and definition of the disease, we summarise the last fifteen years of genetic discoveries and map out the challenges that remain to translate these findings into an aetiological framework and actionable clinical understanding.

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Section: Identifying Causal Variants and Pathogenic Genesmentioning

confidence: 99%

Section: Identifying Causal Variants and Pathogenic Genesmentioning

confidence: 99%

Genome‐wide association studies of multiple sclerosis

Cotsapas¹,

Mitrovič

2018

Clin & Trans Imm

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“…Moreover, the cis -eQTL signal for IRF1 co-localized with the trans -eQTL signals for both trans -eGenes (Fig. 6d; posterior probability >0.99) 43 . Together, these results suggest that cis -regulatory loci affecting IRF1 are regulators of interferon-responsive inflammatory processes involving genes including PSME1 and PARP10 , with implications for complex traits specific to muscle tissue.…”

Section: Expression Qtls and Complex Disease Associationsmentioning

confidence: 83%

“…In order to assess the probability that molecular traits as estimated by cis - and trans -eQTLs and physiological traits as estimated by GWAS share the same causal variant, we applied the coloc R package 43 . For each GWAS, we approximated the number of independent loci by extracting variants with at least genome-wide significance ( P <5 ×10 −8 ) and farther than 1 Mb away from all other variants of higher statistical significance.…”

Section: Methodsmentioning

confidence: 99%

“…However, the mechanism of any cis -effects of these trans -eVariants remains uncertain from the GTEx data; a post hoc analysis demonstrated that PEER correction removed broad regulatory signals from the 9q22 locus, and particularly from cis - and trans -eQTL signals for FOXE1 (Supplementary Information 17). In PEER-corrected data, cis - and trans -eQTL signals co-localized for another cis -eGene in 9q22, TRMO , for both trans -eGenes 43 (posterior probability >0.99). Mendelian randomization analysis of the PEER-corrected data supported the idea that TRMO regulates TMEM253 ( P ≤1.3×10 −9 ) and ARFGEF3 ( P ≤2.1×10 −11 ) based on trans -eVariant rs1867277.…”

Section: Expression Qtls and Complex Disease Associationsmentioning

confidence: 98%

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Genetic effects on gene expression across human tissues

groups

Fund

Nhgri³

et al. 2017

Nature

3,555

2,412

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Characterization of the molecular function of the human genome and its variation across individuals is essential for identifying the cellular mechanisms that underlie human genetic traits and diseases. The Genotype-Tissue Expression (GTEx) project aims to characterize variation in gene expression levels across individuals and diverse tissues of the human body, many of which are not easily accessible. Here we describe genetic effects on gene expression levels across 44 human tissues. We find that local genetic variation affects gene expression levels for the majority of genes, and we further identify inter-chromosomal genetic effects for 93 genes and 112 loci. On the basis of the identified genetic effects, we characterize patterns of tissue specificity, compare local and distal effects, and evaluate the functional properties of the genetic effects. We also demonstrate that multi-tissue, multi-individual data can be used to identify genes and pathways affected by human disease-associated variation, enabling a mechanistic interpretation of gene regulation and the genetic basis of disease.

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Association of Lipid-Lowering Drugs With Risk of Psoriasis

2023

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ImportanceLipid pathways have been implicated in the pathogenesis of psoriasis, and some lipid-lowering drugs, such as statins, are hypothesized to have disease-modifying properties. However, large population-level studies are scarce, and causal interpretation of results from traditional observational designs is limited by confounding.ObjectiveTo investigate the causal association between genetically proxied lipid-lowering drugs and psoriasis risk.Design, Setting, and ParticipantsThis 2-sample mendelian randomization study was performed from August to October 2022 and included population-level genome-wide association studies of psoriasis in the UK Biobank and FinnGen studies and low-density lipoprotein (LDL) by the Global Lipids Genetics Consortium. The inverse variance–weighted method was used with pleiotropy robust methods and colocalization as sensitivity analyses.ExposuresGenetically proxied inhibition of 3-hydroxy-3-methylglutaryl CoA reductase (HMGCR, targeted by statins), Niemann-Pick C1–like 1 (NPC1L1, targeted by ezetimibe), and proprotein convertase subtilisin/kexin type 9 (PCSK9, targeted by, eg, alirocumab), using LDL as the biomarker.Main Outcomes and MeasuresRisk of psoriasis.ResultsData from 12 116 patients with psoriasis and approximately 1.3 million individuals with LDL measurement were analyzed. Genetically proxied PCSK9 inhibition was associated with reduced risk of psoriasis (odds ratio, 0.69 per standard deviation reduction in LDL; 95% CI, 0.55-0.88; P = .003), which was replicated in FinnGen (odds ratio, 0.71; 95% CI, 0.57-0.88; P = .002). Sensitivity analyses did not provide statistical evidence of bias from pleiotropy or genetic confounding. No robust association was found for HMGCR or NPC1L1 inhibition.Conclusions and RelevanceThis mendelian randomization study suggests that PCSK9 is implicated in psoriasis pathogenesis, and its inhibition is associated with reduced psoriasis risk. These findings potentially pave the way for future studies that may allow personalized selection of lipid-lowering drugs for those at risk of psoriasis.

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Bayesian Test for Colocalisation between Pairs of Genetic Association Studies Using Summary Statistics

Cited by 2,432 publications

References 49 publications

Genome‐wide association studies of multiple sclerosis

Genome‐wide association studies of multiple sclerosis

Genetic effects on gene expression across human tissues

Association of Lipid-Lowering Drugs With Risk of Psoriasis

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