Coding de novo mutations identified by WGS reveal novel orofacial cleft genes

Authors :: David J. Cutler
Yah Huei Wu-Chou
Eleanor Feingold
Nandita Mukhopadhyay
Elizabeth J. Leslie
George L. Wehby
Ingo Ruczinski
Jeffrey C. Murray
Samantha Ho
Philip Kuo-Ting Chen
Kimberly K. Diaz Perez
Claudia P. Restrepo Muñeton
Robert J. Lipinski
Madison R. Bishop
Frederic W.-B. Deleyiannis
Luz Consuelo Valencia-Ramirez
Pankaj Chopra
Mary L. Marazita
Harrison Brand
Terri H. Beaty
Seth M. Weinberg
Lina Moreno-Uribe
Jacqueline B. Hetmanski
Miranda Sun
Margaret A. Taub
Michael P. Epstein
Jacqueline T. Hecht
Publication Year :: 2020
Publisher :: Cold Spring Harbor Laboratory, 2020.
Abstract: While de novo mutations (DNMs) are known to increase risk of congenital defects, DNMs have not been fully explored regarding orofacial clefts (OFCs), one of the most common human birth defects. Therefore, whole-genome sequencing of 756 case-parent trios of European, Colombian, and Taiwanese ancestry was performed to determine the contributions of coding DNMs to OFC risk. Overall, we identified a significant excess of loss-of-function DNMs in genes highly expressed in craniofacial tissues, as well as genes associated with known autosomal dominant OFC syndromes. This analysis also revealed roles for zinc-finger homeobox domain and SOX2-interacting genes in OFC etiology.