Congenital heart disease risk loci identified by genomewide association study in European patients

Genetic factors undoubtedly affect the development of congenital heart disease (CHD) but still remain ill defined. We sought to identify genetic risk factors associated with CHD and to accomplish a functional analysis of SNP-carrying genes. We performed a genome-wide association study (GWAS) of 4034...

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Veröffentlicht in:	The Journal of clinical investigation 2021-01, Vol.131 (2)
Hauptverfasser:	Lahm, Harald, Jia, Meiwen, Dreften, Martina, Wirth, Felix, Puluca, Nazan, Gilsbach, Ralf, Keavney, Bernard D, Cleuziou, Julie, Beck, Nicole, Bondareva, Olga, Dzilic, Elda, Burri, Melchior, Konig, Karl C, Ziegelmuller, Johannes A, Abou-Ajram, Claudia, Neb, Irina, Zhang, Zhong, Doppler, Stefanie A, Mastantuono, Elisa, Lichtner, Peter, Eckstein, Gertrud, Horer, Jurgen, Ewert, Peter, Priest, James R, Hein, Lutz, Lange, Rudiger, Meitinger, Thomas, Cordell, Heather J, Muller-Myhsok, Bertram, Krane, Markus
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Sprache:	eng
Schlagworte:	Congenital heart disease Genetic aspects Genetic susceptibility Identification and classification Risk factors
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creator	Lahm, Harald Jia, Meiwen Dreften, Martina Wirth, Felix Puluca, Nazan Gilsbach, Ralf Keavney, Bernard D Cleuziou, Julie Beck, Nicole Bondareva, Olga Dzilic, Elda Burri, Melchior Konig, Karl C Ziegelmuller, Johannes A Abou-Ajram, Claudia Neb, Irina Zhang, Zhong Doppler, Stefanie A Mastantuono, Elisa Lichtner, Peter Eckstein, Gertrud Horer, Jurgen Ewert, Peter Priest, James R Hein, Lutz Lange, Rudiger Meitinger, Thomas Cordell, Heather J Muller-Myhsok, Bertram Krane, Markus
description	Genetic factors undoubtedly affect the development of congenital heart disease (CHD) but still remain ill defined. We sought to identify genetic risk factors associated with CHD and to accomplish a functional analysis of SNP-carrying genes. We performed a genome-wide association study (GWAS) of 4034 White patients with CHD and 8486 healthy controls. One SNP on chromosome 5q22.2 reached genome-wide significance across all CHD phenotypes and was also indicative for septal defects. One region on chromosome 20p12.1 pointing to the MACROD2 locus identified 4 highly significant SNPs in patients with transposition of the great arteries (TGA). Three highly significant risk variants on chromosome 17q21.32 within the GOSR2 locus were detected in patients with anomalies of thoracic arteries and veins (ATAV). Genetic variants associated with ATAV are suggested to influence the expression of WNT3, and the variant rs870142 related to septal defects is proposed to influence the expression of MSX1. We analyzed the expression of all 4 genes during cardiac differentiation of human and murine induced pluripotent stem cells in vitro and by single-cell RNA-Seq analyses of developing murine and human hearts. Our data show that MACROD2, GOSR2, WNT3, and MSX1 play an essential functional role in heart development at the embryonic and newborn stages.
doi_str_mv	10.1172/ICI141837
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We sought to identify genetic risk factors associated with CHD and to accomplish a functional analysis of SNP-carrying genes. We performed a genome-wide association study (GWAS) of 4034 White patients with CHD and 8486 healthy controls. One SNP on chromosome 5q22.2 reached genome-wide significance across all CHD phenotypes and was also indicative for septal defects. One region on chromosome 20p12.1 pointing to the MACROD2 locus identified 4 highly significant SNPs in patients with transposition of the great arteries (TGA). Three highly significant risk variants on chromosome 17q21.32 within the GOSR2 locus were detected in patients with anomalies of thoracic arteries and veins (ATAV). Genetic variants associated with ATAV are suggested to influence the expression of WNT3, and the variant rs870142 related to septal defects is proposed to influence the expression of MSX1. We analyzed the expression of all 4 genes during cardiac differentiation of human and murine induced pluripotent stem cells in vitro and by single-cell RNA-Seq analyses of developing murine and human hearts. 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We analyzed the expression of all 4 genes during cardiac differentiation of human and murine induced pluripotent stem cells in vitro and by single-cell RNA-Seq analyses of developing murine and human hearts. 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subjects	Congenital heart disease Genetic aspects Genetic susceptibility Identification and classification Risk factors
title	Congenital heart disease risk loci identified by genomewide association study in European patients
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