Genome-wide association meta-analysis identifies novel ancestry-specific primary open-angle glaucoma loci and shared biology with vascular mechanisms and cell proliferation

Faro, Valeria Lo; Bhattacharya, Arjun; Zhou, Wei; Zhou, Dan; Wang, Ying; Läll, Kristi; Kanai, Masahiro; Lopera-Maya, Esteban A.; Straub, Péter; Pawar, Priyanka; Tao, Ran; Zhong, Xue; Namba, Shinichi; Nolte, Ilja M.; Okada, Yukinori; Ingold, Nathan; MacGregor, Stuart; Snieder, Harold; Surakka, Ida; Willer, Cristen J.; Martin, Alicia R.; Brantley, Milam A.; Gamazon, Eric R.; Jansonius, Nomdo M.; Joos, Karen M.; Cox, Nancy J.; Hirbo, Jibril

doi:10.1101/2021.12.16.21267891

Cited by 8 publications

(10 citation statements)

References 224 publications

(224 reference statements)

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“…Motivated by successful validation of SLALOM performance, we investigated whether fine-mapping confidence and resolution were improved in the GBMI meta-analyses over individual biobanks. To this end, we used our fine-mapping results 16,17 of nine disease endpoints (asthma 64 , COPD 64 , gout, heart failure 73 , IPF 62 , primary open angle glaucoma 74 , thyroid cancer, stroke 75 , and venous thromboembolism 76 ) in BBJ 58 , FinnGen 20 , and UKBB 19 Europeans that also contributed to the GBMI meta-analyses for the same traits.…”

Section: Resultsmentioning

confidence: 99%

“…To directly compare with fine-mapping results from the GBMI meta-analyses, we used our fine-mapping results of nine disease endpoints (asthma 64 , COPD 64 , gout, heart failure 73 , IPF 62 , primary open angle glaucoma 74 , thyroid cancer, stroke 75 , and venous thromboembolism 76 ) in BBJ 58 , FinnGen 20 , and UKBB 19 Europeans that were also part of the GBMI meta-analyses for the same traits. For comparison, we computed the maximum PIP for each variant and the minimum size of 95% CS across BBJ, FinnGen, and UKBB.…”

Section: Methods Detailsmentioning

confidence: 99%

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Meta-analysis fine-mapping is often miscalibrated at single-variant resolution

Kanai

Elzur

Zhou

et al. 2022

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Meta-analysis is pervasively used to combine multiple genome-wide association studies (GWAS) into a more powerful whole. To resolve causal variants, meta-analysis studies typically apply summary statistics-based fine-mapping methods as they are applied to single-cohort studies. However, it is unclear whether heterogeneous characteristics of each cohort (e.g., ancestry, sample size, phenotyping, genotyping, or imputation) affect fine-mapping calibration and recall. Here, we first demonstrate that meta-analysis fine-mapping is substantially miscalibrated in simulations when different genotyping arrays or imputation panels are included. To mitigate these issues, we propose a summary statistics-based QC method, SLALOM, that identifies suspicious loci for meta-analysis fine-mapping by detecting outliers in association statistics based on ancestry-matched local LD structure. Having validated SLALOM performance in simulations and the GWAS Catalog, we applied it to 14 disease endpoints from the Global Biobank Meta-analysis Initiative and found that 68% of loci showed suspicious patterns that call into question fine-mapping accuracy. These predicted suspicious loci were significantly depleted for having likely causal variants, such as nonsynonymous variants, as a lead variant (2.8x; Fisher's exact P = 6.2 × 10−4). Compared to fine-mapping results in individual biobanks, we found limited evidence of fine-mapping improvement in the GBMI meta-analyses. Although a full solution requires complete synchronization across cohorts, our approach identifies likely spurious results in meta-analysis fine-mapping. We urge extreme caution when interpreting fine-mapping results from meta-analysis.

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Section: Resultsmentioning

confidence: 99%

Section: Methods Detailsmentioning

confidence: 99%

Meta-analysis fine-mapping is often miscalibrated at single-variant resolution

Kanai

Elzur

Zhou

et al. 2022

Preprint

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“…This suggests that the PRS evaluation may be biased upwards from the prior GWAS for POAG. Also, the phenotypes of POAG across different biobanks are likely more heterogeneous in GBMI than targeted case-control studies 18,32 . The meta-analysis of GBMI with International Glaucoma Genetics Consortium (IGGC) did not lead to substantially improved prediction performance 32 .…”

Section: Resultsmentioning

confidence: 99%

“…Also, the phenotypes of POAG across different biobanks are likely more heterogeneous in GBMI than targeted case-control studies 18,32 . The meta-analysis of GBMI with International Glaucoma Genetics Consortium (IGGC) did not lead to substantially improved prediction performance 32 . Another concern might be the disproportional case/control ratio of POAG in GBMI, of ∼27,000 cases and ∼1.4M controls, thus POAG-related phenotypes with shared genetics in the controls or possible uncontrolled ancestry differences between cases and controls might confound the GBMI GWAS.…”

Section: Resultsmentioning

confidence: 99%

“…To boost statistical power, we can meta-analyze GBMI GWAS with other non-overlapping cohorts as shown in other GBMI working groups [33][34][35] . However, we should note that more heterogeneity might be introduced from different resources such as population structure and phenotype definitions, which we cannot control with summary statistics data and that could exacerbate the heterogeneous performance of PRS across target populations.…”

Section: Prs Accuracy Is Heterogeneous Across Ancestries and Biobanksmentioning

confidence: 99%

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Global biobank analyses provide lessons for developing polygenic risk scores across diverse cohorts

Wang

Namba

Lopera-Maya

et al. 2021

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SummaryWith the increasing availability of biobank-scale datasets that incorporate both genomic data and electronic health records, many associations between genetic variants and phenotypes of interest have been discovered. Polygenic risk scores (PRS), which are being widely explored in precision medicine, use the results of association studies to predict the genetic component of disease risk by accumulating risk alleles weighted by their effect sizes. However, limited studies have thoroughly investigated best practices for PRS in global populations across different diseases. In this study, we utilize data from the Global-Biobank Meta-analysis Initiative (GBMI), which consists of individuals from diverse ancestries and across continents, to explore methodological considerations and PRS prediction performance in 9 different biobanks for 14 disease endpoints. Specifically, we constructed PRS using heuristic (pruning and thresholding, P+T) and Bayesian (PRS-CS) methods. We found that the genetic architecture, such as SNP-based heritability and polygenicity, varied greatly among endpoints. For both PRS construction methods, using a European ancestry LD reference panel resulted in comparable or higher prediction accuracy compared to several other non-European based panels; this is largely attributable to European descent populations still comprising the majority of GBMI participants. PRS-CS overall outperformed the classic P+T method, especially for endpoints with higher SNP-based heritability. For example, substantial improvements are observed in East-Asian ancestry (EAS) using PRS-CS compared to P+T for heart failure (HF) and chronic obstructive pulmonary disease (COPD). Notably, prediction accuracy is heterogeneous across endpoints, biobanks, and ancestries, especially for asthma which has known variation in disease prevalence across global populations. Overall, we provide lessons for PRS construction, evaluation, and interpretation using the GBMI and highlight the importance of best practices for PRS in the biobank-scale genomics era.

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