Protein-altering and regulatory genetic variants near GATA4 implicated in bicuspid aortic valve

Bo Yang,Wei-Wu Zhou,Jiao Jiao,Jonas B. Nielsen,Michael R. Mathis,Mahyar Heydarpour,Guillaume Lettre,Lasse Folkersen,Siddharth K. Prakash,Claudia Schurmann,Lars G. Fritsche,Gregory A. Farnum,Maoxuan Lin,Mohammad Othman,Whitney E. Hornsby,Anisa Driscoll,Alexandra Levasseur,Marc Thomas,Linda Farhat,Marie-Pierre Dubé,Eric M. Isselbacher,Anders Franco-Cereceda,Dongchuan Guo,Erwin P. Bottinger,G. Michael Deeb,Anna M. Booher,Sachin Kheterpal,Y. Eugene Chen,Hyun Min Kang,Jacob O. Kitzman,Heather J. Cordell,Bernard Keavney,Judith A. Goodship,Santhi K. Ganesh,Gonçalo R. Abecasis,Kim A. Eagle,Alan P. Boyle,Ruth J. F. Loos,Per Eriksson,Jean-Claude Tardif,Chad M. Brummett,Dianna M. Milewicz,Simon C. Body,Cristen J. Willer

Protein-altering and regulatory genetic variants near GATA4 implicated in bicuspid aortic valve

2017

Abstract Bicuspid aortic valve (BAV) is a heritable congenital heart defect and an important risk factor for valvulopathy and aortopathy. Here we report a genome-wide association scan of 466 BAV cases and 4,660 age, sex and ethnicity-matched controls with replication in up to 1,326 cases and 8,103 controls. We identify association with a noncoding variant 151 kb from the gene encoding the cardiac-specific transcription factor, GATA4, and near-significance for p.Ser377Gly in GATA4. GATA4 was interrupted by CRISPR-Cas9 in induced pluripotent stem cells from healthy donors. The disruption of GATA4 significantly impaired the transition from endothelial cells into mesenchymal cells, a critical step in heart valve development.

Keywords:

Transcription factor
Induced pluripotent stem cell
Genetics
GATA4
Cancer research
Mesenchymal stem cell
Heart valve
Gene
Risk factor
Endocrinology
Internal medicine
Bicuspid aortic valve
Biology
Bioinformatics

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