A genome-wide association study of congenital cardiovascular left-sided lesions shows association with a locus on chromosome 20

Neil A Hanchard; Shanker Swaminathan; Kristine Bucasas; Dieter Furthner; Susan Fernbach; Mahshid S Azamian; Xueqing Wang; Mark Lewin; Jeffrey A Towbin; Lisa C A D'Alessandro; Shaine A Morris; William Dreyer; Susan Denfield; Nancy A Ayres; Wayne J Franklin; Henri Justino; M Regina Lantin-Hermoso; Elena C Ocampo; Alexia B Santos; Dhaval Parekh; Douglas Moodie; Aamir Jeewa; Emily Lawrence; Hugh D Allen; Daniel J Penny; Charles D Fraser; James R Lupski; Mojisola Popoola; Lalita Wadhwa; J David Brook; Frances A Bu'Lock; Shoumo Bhattacharya; Seema R Lalani; Gloria A Zender; Sara M Fitzgerald-Butt; Jessica Bowman; Don Corsmeier; Peter White; Kelsey Lecerf; Gladys Zapata; Patricia Hernandez; Judith A Goodship; Vidu Garg; Bernard D Keavney; Suzanne M Leal; Heather J Cordell; John W Belmont; Kim L McBride

doi:10.1093/hmg/ddw071

A genome-wide association study of congenital cardiovascular left-sided lesions shows association with a locus on chromosome 20

Neil A Hanchard, Shanker Swaminathan, Kristine Bucasas, Dieter Furthner, Susan Fernbach, Mahshid S Azamian, Xueqing Wang, Mark Lewin, Jeffrey A Towbin, Lisa C A D'Alessandro, Shaine A Morris, William Dreyer, Susan Denfield, Nancy A Ayres, Wayne J Franklin, Henri Justino, M Regina Lantin-Hermoso, Elena C Ocampo, Alexia B Santos, Dhaval ParekhDouglas Moodie, Aamir Jeewa, Emily Lawrence, Hugh D Allen, Daniel J Penny, Charles D Fraser, James R Lupski, Mojisola Popoola, Lalita Wadhwa, J David Brook, Frances A Bu'Lock, Shoumo Bhattacharya, Seema R Lalani, Gloria A Zender, Sara M Fitzgerald-Butt, Jessica Bowman, Don Corsmeier, Peter White, Kelsey Lecerf, Gladys Zapata, Patricia Hernandez, Judith A Goodship, Vidu Garg, Bernard D Keavney, Suzanne M Leal, Heather J Cordell, John W Belmont, Kim L McBride

Division of Cardiovascular Sciences (L5)

Research output: Contribution to journal › Article › peer-review

Abstract

Congenital heart defects involving left-sided lesions (LSLs) are relatively common birth defects with substantial morbidity and mortality. Previous studies have suggested a high heritability with a complex genetic architecture, such that only a few LSL loci have been identified. We performed a genome-wide case-control association study to address the role of common variants using a discovery cohort of 778 cases and 2756 controls. We identified a genome-wide significant association mapping to a 200 kb region on chromosome 20q11 [P= 1.72 × 10(-8) for rs3746446; imputed Single Nucleotide Polymorphism (SNP) rs6088703 P= 3.01 × 10(-9), odds ratio (OR)= 1.6 for both]. This result was supported by transmission disequilibrium analyses using a subset of 541 case families (lowest P in region= 4.51 × 10(-5), OR= 1.5). Replication in a cohort of 367 LSL cases and 5159 controls showed nominal association (P= 0.03 for rs3746446) resulting in P= 9.49 × 10(-9) for rs3746446 upon meta-analysis of the combined cohorts. In addition, a group of seven SNPs on chromosome 1q21.3 met threshold for suggestive association (lowest P= 9.35 × 10(-7) for rs12045807). Both regions include genes involved in cardiac development-MYH7B/miR499A on chromosome 20 and CTSK, CTSS and ARNT on chromosome 1. Genome-wide heritability analysis using case-control genotyped SNPs suggested that the mean heritability of LSLs attributable to common variants is moderately high ([Formula: see text] range= 0.26-0.34) and consistent with previous assertions. These results provide evidence for the role of common variation in LSLs, proffer new genes as potential biological candidates, and give further insight to the complex genetic architecture of congenital heart disease.

Original language	English
Pages (from-to)	2331-2341
Number of pages	11
Journal	Human Molecular Genetics
Volume	25
Issue number	11
DOIs	https://doi.org/10.1093/hmg/ddw071
Publication status	Published - 1 Jun 2016

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10.1093/hmg/ddw071

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Hanchard, N. A., Swaminathan, S., Bucasas, K., Furthner, D., Fernbach, S., Azamian, M. S., Wang, X., Lewin, M., Towbin, J. A., D'Alessandro, L. C. A., Morris, S. A., Dreyer, W., Denfield, S., Ayres, N. A., Franklin, W. J., Justino, H., Lantin-Hermoso, M. R., Ocampo, E. C., Santos, A. B., ... McBride, K. L. (2016). A genome-wide association study of congenital cardiovascular left-sided lesions shows association with a locus on chromosome 20. Human Molecular Genetics, 25(11), 2331-2341. https://doi.org/10.1093/hmg/ddw071

@article{3b9307ad06284bc0bb45a945d5b20f47,

title = "A genome-wide association study of congenital cardiovascular left-sided lesions shows association with a locus on chromosome 20",

abstract = "Congenital heart defects involving left-sided lesions (LSLs) are relatively common birth defects with substantial morbidity and mortality. Previous studies have suggested a high heritability with a complex genetic architecture, such that only a few LSL loci have been identified. We performed a genome-wide case-control association study to address the role of common variants using a discovery cohort of 778 cases and 2756 controls. We identified a genome-wide significant association mapping to a 200 kb region on chromosome 20q11 [P= 1.72 × 10(-8) for rs3746446; imputed Single Nucleotide Polymorphism (SNP) rs6088703 P= 3.01 × 10(-9), odds ratio (OR)= 1.6 for both]. This result was supported by transmission disequilibrium analyses using a subset of 541 case families (lowest P in region= 4.51 × 10(-5), OR= 1.5). Replication in a cohort of 367 LSL cases and 5159 controls showed nominal association (P= 0.03 for rs3746446) resulting in P= 9.49 × 10(-9) for rs3746446 upon meta-analysis of the combined cohorts. In addition, a group of seven SNPs on chromosome 1q21.3 met threshold for suggestive association (lowest P= 9.35 × 10(-7) for rs12045807). Both regions include genes involved in cardiac development-MYH7B/miR499A on chromosome 20 and CTSK, CTSS and ARNT on chromosome 1. Genome-wide heritability analysis using case-control genotyped SNPs suggested that the mean heritability of LSLs attributable to common variants is moderately high ([Formula: see text] range= 0.26-0.34) and consistent with previous assertions. These results provide evidence for the role of common variation in LSLs, proffer new genes as potential biological candidates, and give further insight to the complex genetic architecture of congenital heart disease.",

author = "Hanchard, \{Neil A\} and Shanker Swaminathan and Kristine Bucasas and Dieter Furthner and Susan Fernbach and Azamian, \{Mahshid S\} and Xueqing Wang and Mark Lewin and Towbin, \{Jeffrey A\} and D'Alessandro, \{Lisa C A\} and Morris, \{Shaine A\} and William Dreyer and Susan Denfield and Ayres, \{Nancy A\} and Franklin, \{Wayne J\} and Henri Justino and Lantin-Hermoso, \{M Regina\} and Ocampo, \{Elena C\} and Santos, \{Alexia B\} and Dhaval Parekh and Douglas Moodie and Aamir Jeewa and Emily Lawrence and Allen, \{Hugh D\} and Penny, \{Daniel J\} and Fraser, \{Charles D\} and Lupski, \{James R\} and Mojisola Popoola and Lalita Wadhwa and Brook, \{J David\} and Bu'Lock, \{Frances A\} and Shoumo Bhattacharya and Lalani, \{Seema R\} and Zender, \{Gloria A\} and Fitzgerald-Butt, \{Sara M\} and Jessica Bowman and Don Corsmeier and Peter White and Kelsey Lecerf and Gladys Zapata and Patricia Hernandez and Goodship, \{Judith A\} and Vidu Garg and Keavney, \{Bernard D\} and Leal, \{Suzanne M\} and Cordell, \{Heather J\} and Belmont, \{John W\} and McBride, \{Kim L\}",

year = "2016",

month = jun,

day = "1",

doi = "10.1093/hmg/ddw071",

language = "English",

volume = "25",

pages = "2331--2341",

journal = "Human Molecular Genetics",

issn = "0964-6906",

publisher = "Oxford University Press",

number = "11",

}

Hanchard, NA, Swaminathan, S, Bucasas, K, Furthner, D, Fernbach, S, Azamian, MS, Wang, X, Lewin, M, Towbin, JA, D'Alessandro, LCA, Morris, SA, Dreyer, W, Denfield, S, Ayres, NA, Franklin, WJ, Justino, H, Lantin-Hermoso, MR, Ocampo, EC, Santos, AB, Parekh, D, Moodie, D, Jeewa, A, Lawrence, E, Allen, HD, Penny, DJ, Fraser, CD, Lupski, JR, Popoola, M, Wadhwa, L, Brook, JD, Bu'Lock, FA, Bhattacharya, S, Lalani, SR, Zender, GA, Fitzgerald-Butt, SM, Bowman, J, Corsmeier, D, White, P, Lecerf, K, Zapata, G, Hernandez, P, Goodship, JA, Garg, V, Keavney, BD, Leal, SM, Cordell, HJ, Belmont, JW & McBride, KL 2016, 'A genome-wide association study of congenital cardiovascular left-sided lesions shows association with a locus on chromosome 20', Human Molecular Genetics, vol. 25, no. 11, pp. 2331-2341. https://doi.org/10.1093/hmg/ddw071

TY - JOUR

T1 - A genome-wide association study of congenital cardiovascular left-sided lesions shows association with a locus on chromosome 20

AU - Hanchard, Neil A

AU - Swaminathan, Shanker

AU - Bucasas, Kristine

AU - Furthner, Dieter

AU - Fernbach, Susan

AU - Azamian, Mahshid S

AU - Wang, Xueqing

AU - Lewin, Mark

AU - Towbin, Jeffrey A

AU - D'Alessandro, Lisa C A

AU - Morris, Shaine A

AU - Dreyer, William

AU - Denfield, Susan

AU - Ayres, Nancy A

AU - Franklin, Wayne J

AU - Justino, Henri

AU - Lantin-Hermoso, M Regina

AU - Ocampo, Elena C

AU - Santos, Alexia B

AU - Parekh, Dhaval

AU - Moodie, Douglas

AU - Jeewa, Aamir

AU - Lawrence, Emily

AU - Allen, Hugh D

AU - Penny, Daniel J

AU - Fraser, Charles D

AU - Lupski, James R

AU - Popoola, Mojisola

AU - Wadhwa, Lalita

AU - Brook, J David

AU - Bu'Lock, Frances A

AU - Bhattacharya, Shoumo

AU - Lalani, Seema R

AU - Zender, Gloria A

AU - Fitzgerald-Butt, Sara M

AU - Bowman, Jessica

AU - Corsmeier, Don

AU - White, Peter

AU - Lecerf, Kelsey

AU - Zapata, Gladys

AU - Hernandez, Patricia

AU - Goodship, Judith A

AU - Garg, Vidu

AU - Keavney, Bernard D

AU - Leal, Suzanne M

AU - Cordell, Heather J

AU - Belmont, John W

AU - McBride, Kim L

PY - 2016/6/1

Y1 - 2016/6/1

N2 - Congenital heart defects involving left-sided lesions (LSLs) are relatively common birth defects with substantial morbidity and mortality. Previous studies have suggested a high heritability with a complex genetic architecture, such that only a few LSL loci have been identified. We performed a genome-wide case-control association study to address the role of common variants using a discovery cohort of 778 cases and 2756 controls. We identified a genome-wide significant association mapping to a 200 kb region on chromosome 20q11 [P= 1.72 × 10(-8) for rs3746446; imputed Single Nucleotide Polymorphism (SNP) rs6088703 P= 3.01 × 10(-9), odds ratio (OR)= 1.6 for both]. This result was supported by transmission disequilibrium analyses using a subset of 541 case families (lowest P in region= 4.51 × 10(-5), OR= 1.5). Replication in a cohort of 367 LSL cases and 5159 controls showed nominal association (P= 0.03 for rs3746446) resulting in P= 9.49 × 10(-9) for rs3746446 upon meta-analysis of the combined cohorts. In addition, a group of seven SNPs on chromosome 1q21.3 met threshold for suggestive association (lowest P= 9.35 × 10(-7) for rs12045807). Both regions include genes involved in cardiac development-MYH7B/miR499A on chromosome 20 and CTSK, CTSS and ARNT on chromosome 1. Genome-wide heritability analysis using case-control genotyped SNPs suggested that the mean heritability of LSLs attributable to common variants is moderately high ([Formula: see text] range= 0.26-0.34) and consistent with previous assertions. These results provide evidence for the role of common variation in LSLs, proffer new genes as potential biological candidates, and give further insight to the complex genetic architecture of congenital heart disease.

AB - Congenital heart defects involving left-sided lesions (LSLs) are relatively common birth defects with substantial morbidity and mortality. Previous studies have suggested a high heritability with a complex genetic architecture, such that only a few LSL loci have been identified. We performed a genome-wide case-control association study to address the role of common variants using a discovery cohort of 778 cases and 2756 controls. We identified a genome-wide significant association mapping to a 200 kb region on chromosome 20q11 [P= 1.72 × 10(-8) for rs3746446; imputed Single Nucleotide Polymorphism (SNP) rs6088703 P= 3.01 × 10(-9), odds ratio (OR)= 1.6 for both]. This result was supported by transmission disequilibrium analyses using a subset of 541 case families (lowest P in region= 4.51 × 10(-5), OR= 1.5). Replication in a cohort of 367 LSL cases and 5159 controls showed nominal association (P= 0.03 for rs3746446) resulting in P= 9.49 × 10(-9) for rs3746446 upon meta-analysis of the combined cohorts. In addition, a group of seven SNPs on chromosome 1q21.3 met threshold for suggestive association (lowest P= 9.35 × 10(-7) for rs12045807). Both regions include genes involved in cardiac development-MYH7B/miR499A on chromosome 20 and CTSK, CTSS and ARNT on chromosome 1. Genome-wide heritability analysis using case-control genotyped SNPs suggested that the mean heritability of LSLs attributable to common variants is moderately high ([Formula: see text] range= 0.26-0.34) and consistent with previous assertions. These results provide evidence for the role of common variation in LSLs, proffer new genes as potential biological candidates, and give further insight to the complex genetic architecture of congenital heart disease.

U2 - 10.1093/hmg/ddw071

DO - 10.1093/hmg/ddw071

M3 - Article

C2 - 26965164

SN - 0964-6906

VL - 25

SP - 2331

EP - 2341

JO - Human Molecular Genetics

JF - Human Molecular Genetics

IS - 11

ER -

A genome-wide association study of congenital cardiovascular left-sided lesions shows association with a locus on chromosome 20

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