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Genome-Wide Association Meta-Analysis Supports Genes Involved in Valve and Cardiac Development to Associate With Mitral Valve Prolapse

Mengyao Yu, Sergiy Kyryachenko, Stéphanie Debette, Philippe Amouyel, Jean‐Jacques Schott, Thierry Le Tourneau, Christian Dina, Russell A. Norris, Albert Hagège, Xavier Jeunemaı̂tre, Nabila Bouatia‐Naji

2021Circulation Genomic and Precision Medicine18 citationsDOIOpen Access PDF

Abstract

Background: Mitral valve prolapse (MVP) is a common cardiac valve disease, which affects 1 in 40 in the general population. Previous genome-wide association study has identified 6 risk loci for MVP. But these loci explained only partially the genetic risk for MVP. We aim to identify additional risk loci for MVP by adding data set from the UK Biobank. Methods: We also incorporated 434 MVP cases and 4527 controls from the UK Biobank for discovery analyses. Genetic association was conducted using SNPTEST and meta-analyses using METAL. We used Functional Mapping and Annotation of Genome-Wide Association Studies for post-genome-wide association study annotations and Multi-marker Analysis of GenoMic Annotation for gene-based and gene-set analyses. Results: We found Trans-Omics for Precision Medicine imputation to perform better in terms of accuracy in the lower ranges of minor allele frequency below 0.1. Our updated meta-analysis included UK Biobank study for ≈8 million common single-nucleotide polymorphisms (minor allele frequency >0.01) and replicated the association on Chr2 as the top association signal near TNS1 . We identified an additional risk locus on Chr1 ( SYT2 ) and 2 suggestive risk loci on chr8 ( MSRA ) and chr19 ( FBXO46 ), all driven by common variants. Gene-based association using Multi-marker Analysis of GenoMic Annotation revealed 6 risk genes for MVP with pronounced expression levels in cardiovascular tissues, especially the heart and globally part of enriched GO terms related to cardiac development. Conclusions: We report an updated meta-analysis genome-wide association study for MVP using dense imputation coverage and an improved case-control sample. We describe several loci and genes with MVP spanning biological mechanisms highly relevant to MVP, especially during valve and heart development.

Topics & Concepts

Genome-wide association studyMinor allele frequencyBiobankGenetic associationSingle-nucleotide polymorphismLocus (genetics)Imputation (statistics)Meta-analysisGeneticsMitral valve prolapseCandidate genePopulationAlleleBiologyMedicineBioinformaticsComputational biologyGeneGenotypeInternal medicineMitral valveMissing dataComputer scienceMachine learningEnvironmental healthCardiac Valve Diseases and TreatmentsCongenital heart defects researchGenetic Associations and Epidemiology