1. Non-Syndromic Cleft Lip with or without Cleft Palate: Genome-Wide Association Study in Europeans Identifies a Suggestive Risk Locus at 16p12.1 and Supports SH3PXD2A as a Clefting Susceptibility Gene.
- Author
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van Rooij, Iris ALM, Ludwig, Kerstin U, Welzenbach, Julia, Ishorst, Nina, Thonissen, Michelle, Galesloot, Tessel E, Ongkosuwito, Edwin, Bergé, Stefaan J, Aldhorae, Khalid, Rojas-Martinez, Augusto, Kiemeney, Lambertus ALM, Vermeesch, Joris Robert, Brunner, Han, Roeleveld, Nel, Devriendt, Koen, Dormaar, Titiaan, Hens, Greet, Knapp, Michael, Carels, Carine, and Mangold, Elisabeth
- Subjects
CLEFT palate ,CLEFT lip ,HUMAN abnormalities ,KNOCKOUT mice ,ZEBRA danio ,GENES ,DATA analysis ,CHROMOSOMES - Abstract
Non-syndromic cleft lip with or without cleft palate (nsCL/P) ranks among the most common human congenital malformations, and has a multifactorial background in which both exogenous and genetic risk factors act in concert. The present report describes a genome-wide association study (GWAS) involving a total of 285 nsCL/P patients and 1212 controls from the Netherlands and Belgium. Twenty of the 40 previously reported nsC/LP susceptibility loci were replicated, which underlined the validity of this sample. SNV-based analysis of the data identified an as yet unreported suggestive locus at chromosome 16p12.1 (p-value of the lead SNV: 4.17 × 10
−7 ). This association was replicated in two of three patient/control replication series (Central European and Yemeni). Gene analysis of the GWAS data prioritized SH3PXD2A at chromosome 10q24.33 as a candidate gene for nsCL/P. To date, support for this gene as a cleft gene has been restricted to data from zebrafish and a knockout mouse model. The present GWAS was the first to implicate SH3PXD2A in non-syndromic cleft formation in humans. In summary, although performed in a relatively small sample, the present GWAS generated novel insights into nsCL/P etiology. [ABSTRACT FROM AUTHOR]- Published
- 2019
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