Heterogeneity in meta-analyses of genome-wide association investigations.
- Authors
- Ioannidis, John P A; Patsopoulos, Nikolaos A; Evangelou, Evangelos
- Year
- 2007
- Journal
- PloS one
- PMID
- 17786212
- DOI
- 10.1371/journal.pone.0000841
- PMCID
- PMC1950790
BACKGROUND: Meta-analysis is the systematic and quantitative synthesis of effect sizes and the exploration of their diversity across different studies. Meta-analyses are increasingly applied to synthesize data from genome-wide association (GWA) studies and from other teams that try to replicate the genetic variants that emerge from such investigations. Between-study heterogeneity is important to document and may point to interesting leads. METHODOLOGY/PRINCIPAL FINDINGS: To exemplify these issues, we used data from three GWA studies on type 2 diabetes and their replication efforts where meta-analyses of all data using fixed effects methods (not incorporating between-study heterogeneity) have already been published. We considered 11 polymorphisms that at least one of the three teams has suggested as susceptibility loci for type 2 diabetes. The I2 inconsistency metric (measuring the amount of heterogeneity not due to chance) was different from 0 (no detectable heterogeneity) for 6 of the 11 genetic variants; inconsistency was moderate to very large (I2 = 32-77%) for 5 of them. For these 5 polymorphisms, random effects calculations incorporating between-study heterogeneity revealed more conservative p-values for the summary effects compared with the fixed effects calculations. These 5 associations were perused in detail to highlight potential explanations for between-study heterogeneity. These include identification of a marker for a correlated phenotype (e.g. FTO rs8050136 being associated with type 2 diabetes through its effect on obesity); differential linkage disequilibrium across studies of the identified genetic markers with the respective culprit polymorphisms (e.g., possibly the case for CDKAL1 polymorphisms or for rs9300039 and markers in linkage disequilibrium, as shown by additional studies); and potential bias. Results were largely similar, when we treated the discovery and replication data from each GWA investigation as separate studies. SIGNIFICANCE: Between-study heterogeneity is useful to document in the synthesis of data from GWA investigations and can offer valuable insights for further clarification of gene-disease associations.
Meta-analysis of the FTO rs8050136 variant in terms of its association with type 2 diabetes across three GWA investigations.Each investigation is shown by the point estimate of the odds ratio and 95% confidence intervals. Also shown is the diamond of the summary effect by fixed and random effects calculations.
| Name | Type |
|---|---|
| 3 GWA investigations on type 2 diabetes local | cohort |
| African | cohort |
| body mass index | phenotype |
| Caucasians | cohort |
| CDKAL1 local | gene |
| CDKN2B | gene |
| clinical phenotypes | phenotype |
| consortium of investigators local | cohort |
| deCODE | cohort |
| deCODE investigation local | cohort |
| diabetes | phenotype |
| Diabetes Genetics Initiative local | cohort |
| Diabetes Genetics Initiative investigation local | cohort |
| Finland-United States Investigation on NIDDM Genetics (FUSION) local | cohort |
| FTO | gene |
| FUSION | cohort |
| FUSION investigation local | cohort |
| genetic effect heterogeneity local | phenotype |
| genetic variants | cohort |
| genome-wide association studies | cohort |
| genome-wide data local | drug |
| GWA study | cohort |
| heterogeneity local | phenotype |
| HHEX local | gene |
| hypertension | phenotype |
| IGF2BP2 | gene |
| KCNJ11 local | gene |
| KCNJ11 rs5215 local | variant |
| metabolic syndrome | phenotype |
| Molecular phenotype local | phenotype |
| myocardial infarction | phenotype |
| Nonβinsulinβdependent diabetes mellitus local | phenotype |
| obesity | phenotype |
| phenotype | phenotype |
| physical inactivity | phenotype |
| PPARG | gene |
| prospective collaborative GWA investigation local | cohort |
| retrospective meta-analyses local | cohort |
| rs10811661 local | variant |
| rs10946398 local | variant |
| rs1111875 local | variant |
| rs13266634 | variant |
| rs1801282 | variant |
| rs4402960 local | variant |
| rs5015480 local | variant |
| rs564398 local | variant |
| rs7756992 local | variant |
| rs7774594 local | variant |
| rs8050136 | variant |
| rs9300039 local | variant |
| Sladek et al. local | cohort |
| SLC30A8 | gene |
| TCF7L2 | gene |
| TCF7L2 rs7901695 local | variant |
| type 2 diabetes | phenotype |
| TYPE2DIABETES local | phenotype |
| Wellcome Trust case control consortium | cohort |
| Wellcome Trust Case-Control Consortium local | cohort |
| WTCCC | cohort |
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| Identification of independent risk loci for Graves' disease within the MHC in the Japanese population. | Nakabayashi K et al. | β | 2011 | β |
| Impact of CYP2C19 variant genotypes on clinical efficacy of antiplatelet treatment with clopidogrel: systematic review and meta-analysis. | Bauer T et al. | β | 2011 | β |
| Imputation of sequence variants for identification of genetic risks for Parkinson's disease: a meta-analysis of genome-wide association studies. | International Parkinson Disease Genomics Consortium et al. | β | 2011 | β |
| Large-scale genome-wide association studies in East Asians identify new genetic loci influencing metabolic traits. | Kim YJ et al. | β | 2011 | β |
| Meta-analysis confirms the LCE3C_LCE3B deletion as a risk factor for psoriasis in several ethnic groups and finds interaction with HLA-Cw6. | Riveira-Munoz E et al. | β | 2011 | β |
| Meta-analysis of gene-environment interaction: joint estimation of SNP and SNP Γ environment regression coefficients. | Manning AK et al. | β | 2011 | β |
| Multilocus analyses of seven candidate genes suggest interacting pathways for obesity-related traits in Brazilian populations. | Angeli CB et al. | β | 2011 | β |
| Optimal methods for meta-analysis of genome-wide association studies. | Zhou B et al. | β | 2011 | β |
| Perspectives on genome-wide multi-stage family-based association studies. | Van Steen K | β | 2011 | β |
| Random-effects model aimed at discovering associations in meta-analysis of genome-wide association studies. | Han B et al. | β | 2011 | β |
| Serum selenium, genetic variation in selenoenzymes, and risk of colorectal cancer: primary analysis from the Women's Health Initiative Observational Study and meta-analysis. | Takata Y et al. | β | 2011 | β |
| Strategies for genetic model specification in the screening of genome-wide meta-analysis signals for further replication. | Pereira TV et al. | β | 2011 | β |
| The meta-analysis of genome-wide association studies. | Thompson JR et al. | β | 2011 | β |
| Transethnic meta-analysis of genomewide association studies. | Morris AP | β | 2011 | β |
| Adiponectin concentrations: a genome-wide association study. | Jee SH et al. | β | 2010 | β |
| Allelic heterogeneity in genetic association meta-analysis: an application to DTNBP1 and schizophrenia. | Maher BS et al. | β | 2010 | β |
| An interactive effect of batch size and composition contributes to discordant results in GWAS with the CHIAMO genotyping algorithm. | Chierici M et al. | β | 2010 | β |
| [Association of FTO gene polymorphisms and morbid obesity in the population of Extremadura (Spain)]. | RodrΓguez-LΓ³pez R et al. | β | 2010 | β |
| Characterization of 9p24 risk locus and colorectal adenoma and cancer: gene-environment interaction and meta-analysis. | Kocarnik JD et al. | β | 2010 | β |
| Common variants at 10 genomic loci influence hemoglobin Aβ(C) levels via glycemic and nonglycemic pathways. | Soranzo N et al. | β | 2010 | β |
| Genetic cardiovascular risk prediction: will we get there? | Thanassoulis G et al. | β | 2010 | β |
| Genome-wide association studies--data generation, storage, interpretation, and bioinformatics. | Pare G | β | 2010 | β |
| Genome-wide association studies of hypertension: light at the end of the tunnel. | Hastie CE et al. | β | 2010 | β |
| Genome-wide meta-analyses identify multiple loci associated with smoking behavior. | Tobacco and Genetics Consortium | β | 2010 | β |
| GWAMA: software for genome-wide association meta-analysis. | MΓ€gi R et al. | β | 2010 | β |
| Meta-analysis of genome-wide association scans for genetic susceptibility to endometriosis in Japanese population. | Adachi S et al. | β | 2010 | β |
| No association between oxytocin receptor (OXTR) gene polymorphisms and experimentally elicited social preferences. | Apicella CL et al. | β | 2010 | β |
| Prioritizing GWAS results: A review of statistical methods and recommendations for their application. | Cantor RM et al. | β | 2010 | β |
| Susceptibility variants for rheumatoid arthritis in the TRAF1-C5 and 6q23 loci: a meta-analysis. | Patsopoulos NA et al. | β | 2010 | β |
| The Gene, Environment Association Studies consortium (GENEVA): maximizing the knowledge obtained from GWAS by collaboration across studies of multiple conditions. | Cornelis MC et al. | β | 2010 | β |
| The impact of phenocopy on the genetic analysis of complex traits. | Lescai F et al. | β | 2010 | β |
| Two-stage testing strategies for genome-wide association studies in family-based designs. | Murphy A et al. | β | 2010 | β |
| A framework for interpreting genome-wide association studies of psychiatric disorders. | Psychiatric GWAS Consortium Steering Committee | β | 2009 | β |
| A large-scale genome-wide association study of Asian populations uncovers genetic factors influencing eight quantitative traits. | Cho YS et al. | β | 2009 | β |
| An empirical comparison of meta-analyses of published gene-disease associations versus consortium analyses. | Janssens AC et al. | β | 2009 | β |
| A pooling-based genome-wide analysis identifies new potential candidate genes for atopy in the European Community Respiratory Health Survey (ECRHS). | Castro-Giner F et al. | β | 2009 | β |
| Bayesian statistical methods for genetic association studies. | Stephens M et al. | β | 2009 | β |
| Collaborative meta-analysis: associations of 150 candidate genes with osteoporosis and osteoporotic fracture. | Richards JB et al. | β | 2009 | β |
| Data integration in genetics and genomics: methods and challenges. | Hamid JS et al. | β | 2009 | β |
| Discovery properties of genome-wide association signals from cumulatively combined data sets. | Pereira TV et al. | β | 2009 | β |
| FTO gene variation and measures of body mass in an African population. | Hennig BJ et al. | β | 2009 | β |
| Genome-wide association studies, field synopses, and the development of the knowledge base on genetic variation and human diseases. | Khoury MJ et al. | β | 2009 | β |
| Genome-wide association study of alcohol dependence. | Treutlein J et al. | β | 2009 | β |
| Meta-analysis in genome-wide association studies. | Zeggini E et al. | β | 2009 | β |
| Meta-analysis of genetic association studies: methodologies, between-study heterogeneity and winner's curse. | Nakaoka H et al. | β | 2009 | β |
| Prediction of cardiovascular disease outcomes and established cardiovascular risk factors by genome-wide association markers. | Ioannidis JP | β | 2009 | β |
| SOD2 gene polymorphisms in neovascular age-related macular degeneration and polypoidal choroidal vasculopathy. | Kondo N et al. | β | 2009 | β |
| Using genome-wide pathway analysis to unravel the etiology of complex diseases. | Elbers CC et al. | β | 2009 | β |
| Validating, augmenting and refining genome-wide association signals. | Ioannidis JP et al. | β | 2009 | β |
| Biostatistical aspects of genome-wide association studies. | Ziegler A et al. | β | 2008 | β |
| Calibration of credibility of agnostic genome-wide associations. | Ioannidis JP | β | 2008 | β |
| Clinical implications and longitudinal alteration of peripheral blood transcriptional signals indicative of future cardiac allograft rejection. | Mehra MR et al. | β | 2008 | β |
| Common SNPs in HMGCR in micronesians and whites associated with LDL-cholesterol levels affect alternative splicing of exon13. | Burkhardt R et al. | β | 2008 | β |
| Evaluation of the association of IGF2BP2 variants with type 2 diabetes in French Caucasians. | Duesing K et al. | β | 2008 | β |
| Evaluation of the potential excess of statistically significant findings in published genetic association studies: application to Alzheimer's disease. | Kavvoura FK et al. | β | 2008 | β |
| Genetic associations with schizophrenia: meta-analyses of 12 candidate genes. | Shi J et al. | β | 2008 | β |
| Genome-wide association scans identified CTNNBL1 as a novel gene for obesity. | Liu YJ et al. | β | 2008 | β |
| Genome-wide association studies for complex traits: consensus, uncertainty and challenges. | McCarthy MI et al. | β | 2008 | β |
| Hypertension and genome-wide association studies: combining high fidelity phenotyping and hypercontrols. | Padmanabhan S et al. | β | 2008 | β |
| Is replication the gold standard for validating genome-wide association findings? | Liu YJ et al. | β | 2008 | β |
| Meta-analysis of two genome-wide association studies of bipolar disorder reveals important points of agreement. | Baum AE et al. | β | 2008 | β |
| Methods for meta-analysis in genetic association studies: a review of their potential and pitfalls. | Kavvoura FK et al. | β | 2008 | β |
| No significant association of 14 candidate genes with schizophrenia in a large European ancestry sample: implications for psychiatric genetics. | Sanders AR et al. | β | 2008 | β |
| Pathways to injury in chronic pancreatitis: decoding the role of the high-risk SPINK1 N34S haplotype using meta-analysis. | Aoun E et al. | β | 2008 | β |
| Polygenic obesity in humans. | Hinney A et al. | β | 2008 | β |
| Practical aspects of imputation-driven meta-analysis of genome-wide association studies. | de Bakker PI et al. | β | 2008 | β |
| Psychiatric genetics gets a boost. | Maher BS et al. | β | 2008 | β |
| Required sample size and nonreplicability thresholds for heterogeneous genetic associations. | Moonesinghe R et al. | β | 2008 | β |
| The continued need to synthesize the results of genetic associations across multiple studies. | Yesupriya A et al. | β | 2008 | β |
| Genome wide association (GWA) study for early onset extreme obesity supports the role of fat mass and obesity associated gene (FTO) variants. | Hinney A et al. | β | 2007 | β |