4.7 Article

Functional screening of congenital heart disease risk loci identifies 5 genes essential for heart development in zebrafish

Journal

CELLULAR AND MOLECULAR LIFE SCIENCES
Volume 80, Issue 1, Pages -

Publisher

SPRINGER BASEL AG
DOI: 10.1007/s00018-022-04669-5

Keywords

Congenital heart malformation; GWAS; Danio rerio; Cardiac development; Notch signaling

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Our previous study identified 53 SNPs associated with CHD in the Han Chinese population. In this study, we conducted functional screening of 27 orthologous genes in zebrafish and identified 5 genes essential for heart development. These novel CHD-related genes have presumptive roles in heart chamber and atrioventricular canal formation. Furthermore, we demonstrated that maml3 is required for Notch signaling in vivo, leading to defective cardiac trabeculation and heart failure in zebrafish embryos.
Congenital heart disease (CHD) is the most common birth defect worldwide and a main cause of perinatal and infant mortality. Our previous genome-wide association study identified 53 SNPs that associated with CHD in the Han Chinese population. Here, we performed functional screening of 27 orthologous genes in zebrafish using injection of antisense morpholino oligos. From this screen, 5 genes were identified as essential for heart development, including iqgap2, ptprt, ptpn22, tbck and maml3. Presumptive roles of the novel CHD-related genes include heart chamber formation (iqgap2 and ptprt) and atrioventricular canal formation (ptpn22 and tbck). While deficiency of maml3 led to defective cardiac trabeculation and consequent heart failure in zebrafish embryos. Furthermore, we found that maml3 mutants showed decreased cardiomyocyte proliferation which caused a reduction in cardiac trabeculae due to inhibition of Notch signaling. Together, our study identifies 5 novel CHD-related genes that are essential for heart development in zebrafish and first demonstrates that maml3 is required for Notch signaling in vivo.

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