Primo: integration of multiple GWAS and omics QTL summary statistics for elucidation of molecular mechanisms of trait-associated SNPs and detection of pleiotropy in complex traits

Gleason, Kevin J.; Yang, Fan; Pierce, Brandon L.; He, Xin; Chen, Lin S.

doi:10.1101/579581

Cited by 20 publications

(28 citation statements)

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“…To quantify the cross-tissue cis-association probability, Pr(α c = 0 in all K tissue types) in (1), we first obtained the gene-level cis-association statistics for M cis-genes by F -tests. We applied a recently developed integrative association analysis approach, Primo [15,21], to the association statistics to obtain the probabilities of Pr(α c = 0 in all K tissue types) for gene i = 1, . .…”

Section: Methods Overviewmentioning

confidence: 99%

“…For each (GWAS SNP, cis-gene) pair, we conducted regression (6) described in the Methods, regressing cis-gene expression on the GWAS SNP genotype and adjusting for GTEx-reported eQTLs, to obtain the cis-association statistics in each tissue type. We applied Primo [15] to the M g ×K matrix of cis-association statistics {F G } where M g is the number of (GWAS SNP, cis-gene) pairs, and estimated the probability of each GWAS SNP being also an eQTL in at least 2 tissue types, conditioning on other cis-eQTLs. There were 40 (GWAS SNP, cis-gene) pairs showing evidence of cis-association in at least 2 tissue types (with cross-2-tissue cis-association posterior probability > 80%).…”

Section: Simulations To Evaluate Ccmed In Detecting Robust Cis-mediatmentioning

confidence: 99%

“…For each of the 40 (GWAS SNP, cis-gene) pairs, we further conducted conditional correlation analysis with each of its trans-genes in each tissue type using the regression model (7) described in Methods to obtain a matrix of conditional correlation statistics, {Z G i.. }, conditioning on cis-eQTL and GWAS SNP genotypes. We applied Primo [15] to {Z G i.. } to estimate the probability of non-zero conditional cis-trans gene-expression correlation for each possible pair of tissues s . Using equation (2), we obtained a lower bound estimate of the probability of cis-mediated trans-association in at least two brain tissue types for each trio, and identified 1492 (GWAS SNP, cis-gene, trans-gene) trios with P GWAS med,ij > 80% (FDR = 7.9%) with 1418 unique trans-genes.…”

Section: Simulations To Evaluate Ccmed In Detecting Robust Cis-mediatmentioning

confidence: 99%

“…To estimate Pr(α c = 0 in all K tissues), we apply a recently developed integrative association analysis approach, Primo [15,21]. Primo takes as input the M × K matrix of cis-association summary statistics {F ik }, considers all 2 K possible crosstissue association patterns and estimates the density function for each pattern, and returns the probabilities of P 1i = Pr(α c = 0 in all K tissue types) for gene i = 1, .…”

Section: Ccmed Gene For Detecting Cross-tissue Gene-level Cis-mediatementioning

confidence: 99%

“…In addition to mapping robust gene-level trans-associations in the genome, another major focus of this work is to study the trans-genes of GWAS SNPs and further understand how genetic variation affects complex traits -a long-standing question in genetics research. Increasing evidence has suggested that many susceptibility loci may affect complex traits/diseases via the modulation of their cisgene expression levels [14,15,16,17]. Those cis-gene expression levels may further affect other distal genes in functional pathways, some of which also con-tribute to phenotypic variation.…”

Section: Introductionmentioning

confidence: 99%

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CCmed: cross-condition mediation analysis for identifying robust trans-eQTLs and assessing their effects on human traits

Yang

Gleason

Wang

et al. 2019

Preprint

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Trans-eQTLs collectively explain a substantial proportion of expression variation, yet are challenging to detect and replicate since their effects are individually weak. Many trans-effects are mediated by cis-gene expression and some of those effects are shared across tissue types/conditions. To detect robust cis-mediated trans-associations at the gene-level and for specific single nucleotide polymorphisms (SNPs), we proposed two Cross-Condition Mediation methods -CCmed gene and CCmed GWAS , respectively. We analyzed data from 13 brain tissue types from the Genotype-Tissue Expression (GTEx) project, and identified trios with cis-eQTLs of a cis-gene having associations with a trans-gene, many of which show evidence of replication in other datasets. By applying CCmed GWAS , we identified trans-genes associated with known schizophrenia susceptibility loci. We further conducted validation analyses assessing the schizophrenia-risk-associations of the identified trans-genes, by harnessing GWAS summary statistics from the Psychiatric Genomics Consortium and multitissue eQTL statistics from GTEx. Availability of data and materialThe R package CCmed is available at https://github.com/kjgleason/CCmed. The R package MrRobin is available at https://github.com/kjgleason/MrRobin.Author's contributions LSC and FY conceived the project and developed the methods. LSC, FY and KJG wrote the manuscript. LSC and KJG analyzed the data. JW, JD, XH and BLP provided valuable suggestions to the development of the methods and analysis. KJG and FY developed the R software package.

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Section: Methods Overviewmentioning

confidence: 99%

Section: Simulations To Evaluate Ccmed In Detecting Robust Cis-mediatmentioning

confidence: 99%

Section: Simulations To Evaluate Ccmed In Detecting Robust Cis-mediatmentioning

confidence: 99%

Section: Ccmed Gene For Detecting Cross-tissue Gene-level Cis-mediatementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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CCmed: cross-condition mediation analysis for identifying robust trans-eQTLs and assessing their effects on human traits

Yang

Gleason

Wang

et al. 2019

Preprint

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A robust two‐sample transcriptome‐wide Mendelian randomization method integrating GWAS with multi‐tissue eQTL summary statistics

Gleason

Yang

Chen

2021

Genetic Epidemiology

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By treating genetic variants as instrumental variables (IVs), two-sample Mendelian randomization (MR) methods detect genetically regulated risk exposures for complex diseases using only summary statistics. When considering gene expression as exposure in transcriptome-wide MR (TWMR) analyses, the eQTLs (expression-quantitative-trait-loci) may have pleiotropic effects or be correlated with variants that have effects on disease not via expression, and the presence of those invalid IVs would lead to biased inference. Moreover, the number of eQTLs as IVs for a gene is generally limited, making the detection of invalid IVs challenging. We propose a method, "MR-MtRobin," for accurate TWMR inference in the presence of invalid IVs.By leveraging multi-tissue eQTL data in a mixed model, the proposed method makes identifiable the IV-specific random effects due to pleiotropy from estimation errors of eQTL summary statistics, and can provide accurate inference on the dependence (fixed effects) between eQTL and GWAS (genomewide association study) effects in the presence of invalid IVs. Moreover, our method can improve power and precision in inference by selecting cross-tissue eQTLs as IVs that have improved consistency of effects across eQTL and GWAS data. We applied MR-MtRobin to detect genes associated with schizophrenia risk by integrating summary-level data from the Psychiatric Genomics Consortium and the Genotype-Tissue Expression project (V8).

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Quantifying the role of transcript levels in mediating DNA methylation effects on complex traits and diseases

et al. 2022

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High-dimensional omics datasets provide valuable resources to determine the causal role of molecular traits in mediating the path from genotype to phenotype. Making use of molecular quantitative trait loci (QTL) and genome-wide association study (GWAS) summary statistics, we propose a multivariable Mendelian randomization (MVMR) framework to quantify the proportion of the impact of the DNA methylome (DNAm) on complex traits that is propagated through the assayed transcriptome. Evaluating 50 complex traits, we find that on average at least 28.3% (95% CI: [26.9%–29.8%]) of DNAm-to-trait effects are mediated through (typically multiple) transcripts in the cis-region. Several regulatory mechanisms are hypothesized, including methylation of the promoter probe cg10385390 (chr1:8’022’505) increasing the risk for inflammatory bowel disease by reducing PARK7 expression. The proposed integrative framework can be extended to other omics layers to identify causal molecular chains, providing a powerful tool to map and interpret GWAS signals.

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Primo: integration of multiple GWAS and omics QTL summary statistics for elucidation of molecular mechanisms of trait-associated SNPs and detection of pleiotropy in complex traits

Cited by 20 publications

References 54 publications

CCmed: cross-condition mediation analysis for identifying robust trans-eQTLs and assessing their effects on human traits

CCmed: cross-condition mediation analysis for identifying robust trans-eQTLs and assessing their effects on human traits

A robust two‐sample transcriptome‐wide Mendelian randomization method integrating GWAS with multi‐tissue eQTL summary statistics

Quantifying the role of transcript levels in mediating DNA methylation effects on complex traits and diseases

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