Localizing components of shared transethnic genetic architecture of complex traits from GWAS summary data

Shi, Huwenbo; Burch, Kathryn S.; Johnson, Ruth; Freund, Malika K.; Kichaev, Gleb; Mancuso, Nicholas; Manuel, Astrid M.; Dong, Natalie; Paşaniuc, Bogdan

doi:10.1101/858431

Cited by 28 publications

(52 citation statements)

References 88 publications

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“…Prior studies have shown that complex traits and diseases are genetically correlated at different levels between EAS and European (EUR) populations 21–23 , but the genetic overlap within EAS populations has not been characterized yet. Leveraging existing GWAS summary statistics from BBJ and UKBB, we investigated the comparative genetic architecture of quantitative traits within EAS (TWB vs. BBJ), and between EAS and EUR populations (TWB vs. UKBB and BBJ vs. UKBB).…”

Section: Mainmentioning

confidence: 99%

Analysis across Taiwan Biobank, Biobank Japan and UK Biobank identifies hundreds of novel loci for 36 quantitative traits

Chen

et al. 2021

Preprint

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Genome-wide association studies (GWAS) have identified tens of thousands of genetic loci associated with human complex traits and diseases. However, the majority of GWAS were conducted in individuals of European ancestry. Failure to capture global genetic diversity has limited biological discovery and impeded equitable delivery of genomic knowledge to diverse populations. Here we report findings from 102,900 individuals across 36 human quantitative traits in the Taiwan Biobank (TWB), a major biobank effort that broadens the population diversity of genetic studies in East Asia (EAS). We identified 979 novel genetic loci, pinpointed novel causal variants through fine-mapping, compared the genetic architecture across TWB, Biobank Japan (BBJ) and UK Biobank (UKBB), and demonstrated the utility of cross-phenotype, cross-population polygenic risk scores (PRS) in disease risk prediction. We release all GWAS summary statistics, fine-mapping results, and single nucleotide polymorphism (SNP) weights and TWB-based PRS reference distributions for polygenic prediction (link to appear upon publication) to facilitate within-EAS and cross-population genetic research.

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Section: Mainmentioning

confidence: 99%

Analysis across Taiwan Biobank, Biobank Japan and UK Biobank identifies hundreds of novel loci for 36 quantitative traits

Chen

et al. 2021

Preprint

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“…Tier 2 anc-eQTLs also had nonoverlapping 95% credible sets for each gene but were commonly segregating (MAF ≥ 0.01) in both high and low ancestry groups. This class of anc-eQTLs was identified using PESCA 17 , which accounted for population-specific LD patterns. We identified 109 genes (1.1%) with eQTLs having a posterior probability (PP) > 80% of being specific to AFRhigh and 33 genes (0.4%) matching the same criteria for IAMhigh.…”

Section: Identification Of Ancestry-specific Eqtlsmentioning

confidence: 99%

“…For genes with non-overlapping lead eQTL signals (Figure 3a, left branch), eQTLs from the high group were categorized into Tier 1 anc-eQTLs if they were common variants (MAF >= 0.01) in the high group but rare or absent in the low group. If the eQTLs were common variants in both the high and low groups, their specificity was further assessed using PESCA 17 for differential effect size while accounting for LD between eQTLs. LD pruning on eQTLs with r2 > 0.95 was performed prior to PESCA analysis.…”

Section: Identification Of Egenes Cis-eqtls and Ancestry-specific Cis-eqtlsmentioning

confidence: 99%

Gene expression in African Americans and Latinos reveals ancestry-specific patterns of genetic architecture

Mak

Kachuri

et al. 2021

Preprint

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We explored the role of genetic ancestry in shaping the genetic architecture of whole blood gene expression using whole genome and RNA sequencing data from 2,733 African American and Hispanic/Latino children. We find that heritability of gene expression significantly increases with greater proportion of genome-wide African ancestry and decreases with higher levels of Indigenous American ancestry. Fine-mapping of expression quantitative trait loci (eQTLs) in individuals with predominantly African or Indigenous American ancestry revealed ancestry-specific eQTLs in over 30% of heritable genes. We leveraged our data to train genetically derived transcriptome prediction models, which identified significantly more associated genes when applied to 28 traits from a multi-ancestry population. Our findings underscore the importance of increasing representation from ancestrally diverse populations in genomic studies to enable new discoveries and ensure their equitable translation.

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“…Initial studies have indicated that the genetic architectures of many complex traits and diseases are concordant between populations -both at the single-variant level and at the genome-wide level. In particular, many genetic associations identified in European populations have been replicated in non-European GWAS, and recent studies have estimated the trans-ethnic genetic correlation between European and non-European populations to be moderate or high for many traits [16][17][18][19] . These findings suggest that the transferability of PRS may be improved by integrating GWAS summary statistics from diverse populations.…”

Section: Introductionmentioning

confidence: 99%

Improving Polygenic Prediction in Ancestrally Diverse Populations

Ruan

Feng

Chen

et al. 2021

Preprint

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Polygenic risk scores (PRS) have attenuated cross-population predictive performance. As existing genome-wide association studies (GWAS) were predominantly conducted in individuals of European descent, the limited transferability of PRS reduces its clinical value in non-European populations and may exacerbate healthcare disparities. Recent efforts to level ancestry imbalance in genomic research have expanded the scale of non-European GWAS, although they remain under-powered. Here we present a novel PRS construction method, PRS-CSx, which improves cross-population polygenic prediction by integrating GWAS summary statistics from multiple populations. PRS-CSx couples genetic effects across populations via a shared continuous shrinkage prior, enabling more accurate effect size estimation by sharing information between summary statistics and leveraging linkage disequilibrium (LD) diversity across discovery samples, while inheriting computational efficiency and robustness from PRS-CS. We show that PRS-CSx outperforms alternative methods across traits with a wide range of genetic architectures and cross-population genetic correlations in simulations, and substantially improves the prediction of quantitative traits and schizophrenia risk in non-European populations.

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Localizing components of shared transethnic genetic architecture of complex traits from GWAS summary data

Cited by 28 publications

References 88 publications

Analysis across Taiwan Biobank, Biobank Japan and UK Biobank identifies hundreds of novel loci for 36 quantitative traits

Analysis across Taiwan Biobank, Biobank Japan and UK Biobank identifies hundreds of novel loci for 36 quantitative traits

Gene expression in African Americans and Latinos reveals ancestry-specific patterns of genetic architecture

Improving Polygenic Prediction in Ancestrally Diverse Populations

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