Oligogenic Architecture of Rare Noncoding Variants Distinguishes 4 Congenital Heart Disease Phenotypes

Mengyao Yu; Matthew Aguirre; Meiwen Jia; Ketrin Gjoni; Aldo Cordova-Palomera; Chad Munger; Dulguun Amgalan; X Rosa Ma; Alexandre Pereira; Catherine Tcheandjieu; Christine Seidman; Jonathan Seidman; Martin Tristani-Firouzi; Wendy Chung; Elizabeth Goldmuntz; Deepak Srivastava; Ruth J F Loos; Nathalie Chami; Heather Cordell; Martina Dreßen; Bertram Mueller-Myhsok; Harald Lahm; Markus Krane; Katherine S Pollard; Jesse M Engreitz; Sarah A Gagliano Taliun; Bruce D Gelb; James R Priest

doi:10.1161/CIRCGEN.122.003968

Oligogenic Architecture of Rare Noncoding Variants Distinguishes 4 Congenital Heart Disease Phenotypes

Circ Genom Precis Med. 2023 Jun;16(3):258-266. doi: 10.1161/CIRCGEN.122.003968. Epub 2023 Apr 7.

Authors

Mengyao Yu^{1

2}, Matthew Aguirre^{1

3}, Meiwen Jia⁴, Ketrin Gjoni⁵, Aldo Cordova-Palomera¹, Chad Munger⁶, Dulguun Amgalan⁶, X Rosa Ma⁶, Alexandre Pereira⁷, Catherine Tcheandjieu^{1

5}, Christine Seidman⁷, Jonathan Seidman⁷, Martin Tristani-Firouzi⁸, Wendy Chung⁹, Elizabeth Goldmuntz¹⁰, Deepak Srivastava⁵, Ruth J F Loos¹¹, Nathalie Chami¹¹, Heather Cordell¹², Martina Dreßen¹³, Bertram Mueller-Myhsok⁴, Harald Lahm¹³, Markus Krane^{13

14}, Katherine S Pollard^{5

15}, Jesse M Engreitz^{6

16}, Sarah A Gagliano Taliun^{17

18}, Bruce D Gelb¹⁹, James R Priest¹

Affiliations

¹ Department of Pediatrics (M.Y., M.A., A.C.-P., C.T., J.R.P.), Stanford University School of Medicine.
² Fudan University, Shanghai, Chinia (M.Y.).
³ Department of Biomedical Data Science, Stanford University, CA (M.A.).
⁴ Department of Translational Research in Psychiatry, Max Planck Institute of Psychiatry Munich, Germany (M.J., B.M.-M.).
⁵ Gladstone Institutes; University of California San Francisco (K.G., C.T., D.S., K.S.P.).
⁶ Department of Genetics (C.M., D.A., X.R.M., J.M.E.), Stanford University School of Medicine.
⁷ Department of Genetics, Harvard University, Cambridge, MA (A.P., C.S., J.S.).
⁸ Department of Pediatrics, University of Utah, Salt Lake City (M.T.-F.).
⁹ Department of Pediatrics, Columbia University, NY (W.C.).
¹⁰ Department of Pediatrics, University of Pennsylvania, Philadelphia (E.G.).
¹¹ Icahn School of Medicine at Mount Sinai, NY (R.J.F.L., N.C.).
¹² Population Health Sciences Institute, Faculty of Medical Sciences, Newcastle University, International Centre for Life, Central Parkway, Newcastle upon Tyne, United Kingdom (H.C.).
¹³ Department of Cardiovascular Surgery, Division of Experimental Surgery, Institute Insure (Institute for Translational Cardiac Surgery), German Heart Center Munich & Technical University of Munich, School of Medicine & Health, Germany (M.D., H.L., M.K.).
¹⁴ Department of Cardiac Surgery, Yale School of Medicine, New Haven, CT (M.K.).
¹⁵ Chan Zuckerberg Biohub, San Francisco (K.S.P.).
¹⁶ Basic Sciences and Engineering (BASE) Initiative, Betty Irene Moore Children's Heart Center, Lucile Packard Children's Hospital, Stanford, CA (J.M.E.).
¹⁷ Department of Medicine & Department of Neurosciences, Faculty of Medicine, University ersité de Montréal (S.A.G.T.).
¹⁸ Montreal Heart Institute, Montreal, Quebec, Canada (S.A.G.T.).
¹⁹ The Mindich Child Health & Development Institute at the Hess Center for Science & Medicine at Mount Sinai, NY (B.D.G.).

PMID: 37026454
PMCID: PMC10330096 (available on 2024-06-01)
DOI: 10.1161/CIRCGEN.122.003968

Abstract

Background: Congenital heart disease (CHD) is highly heritable, but the power to identify inherited risk has been limited to analyses of common variants in small cohorts.

Methods: We performed reimputation of 4 CHD cohorts (n=55 342) to the TOPMed reference panel (freeze 5), permitting meta-analysis of 14 784 017 variants including 6 035 962 rare variants of high imputation quality as validated by whole genome sequencing.

Results: Meta-analysis identified 16 novel loci, including 12 rare variants, which displayed moderate or large effect sizes (median odds ratio, 3.02) for 4 separate CHD categories. Analyses of chromatin structure link 13 of the genome-wide significant loci to key genes in cardiac development; rs373447426 (minor allele frequency, 0.003 [odds ratio, 3.37 for Conotruncal heart disease]; P=1.49×10^-8) is predicted to disrupt chromatin structure for 2 nearby genes BDH1 and DLG1 involved in Conotruncal development. A lead variant rs189203952 (minor allele frequency, 0.01 [odds ratio, 2.4 for left ventricular outflow tract obstruction]; P=1.46×10^-⁸) is predicted to disrupt the binding sites of 4 transcription factors known to participate in cardiac development in the promoter of SPAG9. A tissue-specific model of chromatin conformation suggests that common variant rs78256848 (minor allele frequency, 0.11 [odds ratio, 1.4 for Conotruncal heart disease]; P=2.6×10^-⁸) physically interacts with NCAM1 (P_FDR=1.86×10^-²⁷), a neural adhesion molecule acting in cardiac development. Importantly, while each individual malformation displayed substantial heritability (observed h2 ranging from 0.26 for complex malformations to 0.37 for left ventricular outflow tract obstructive disease) the risk for different CHD malformations appeared to be separate, without genetic correlation measured by linkage disequilibrium score regression or regional colocalization.

Conclusions: We describe a set of rare noncoding variants conferring significant risk for individual heart malformations which are linked to genes governing cardiac development. These results illustrate that the oligogenic basis of CHD and significant heritability may be linked to rare variants outside protein-coding regions conferring substantial risk for individual categories of cardiac malformation.

Keywords: alleles; chromatin; live birth; phenotype; prevalence.

Publication types

Meta-Analysis
Research Support, N.I.H., Extramural

MeSH terms

Adaptor Proteins, Signal Transducing / genetics
Chromatin
Gene Frequency
Heart Defects, Congenital* / diagnosis
Heart Defects, Congenital* / genetics
Humans
Phenotype
Whole Genome Sequencing

Substances

Chromatin
SPAG9 protein, human
Adaptor Proteins, Signal Transducing

Abstract

Publication types

MeSH terms

Substances

Grants and funding