TY - JOUR
T1 - De novo variants in congenital diaphragmatic hernia identify MYRF as a new syndrome and reveal genetic overlaps with other developmental disorders
AU - Qi, Hongjian
AU - Yu, Lan
AU - Zhou, Xueya
AU - Wynn, Julia
AU - Zhao, Haoquan
AU - Guo, Yicheng
AU - Zhu, Na
AU - Kitaygorodsky, Alexander
AU - Hernan, Rebecca
AU - Aspelund, Gudrun
AU - Lim, Foong Yen
AU - Crombleholme, Timothy
AU - Cusick, Robert
AU - Azarow, Kenneth
AU - Danko, Melissa E.
AU - Chung, Dai
AU - Warner, Brad W.
AU - Mychaliska, George B.
AU - Potoka, Douglas
AU - Wagner, Amy J.
AU - ElFiky, Mahmoud
AU - Wilson, Jay M.
AU - Nickerson, Debbie
AU - Bamshad, Michael
AU - High, Frances A.
AU - Longoni, Mauro
AU - Donahoe, Patricia K.
AU - Chung, Wendy K.
AU - Shen, Yufeng
N1 - Publisher Copyright:
© 2018 Qi et al. http://creativecommons.org/licenses/by/4.0/.
PY - 2018/12
Y1 - 2018/12
N2 - Congenital diaphragmatic hernia (CDH) is a severe birth defect that is often accompanied by other congenital anomalies. Previous exome sequencing studies for CDH have supported a role of de novo damaging variants but did not identify any recurrently mutated genes. To investigate further the genetics of CDH, we analyzed de novo coding variants in 362 proband-parent trios including 271 new trios reported in this study. We identified four unrelated individuals with damaging de novo variants in MYRF (P = 5.3x10 -8 ), including one likely gene-disrupting (LGD) and three deleterious missense (D-mis) variants. Eight additional individuals with de novo LGD or missense variants were identified from our other genetic studies or from the literature. Common phenotypes of MYRF de novo variant carriers include CDH, congenital heart disease and genitourinary abnormalities, suggesting that it represents a novel syndrome. MYRF is a membrane associated transcriptional factor highly expressed in developing diaphragm and is depleted of LGD variants in the general population. All de novo missense variants aggregated in two functional protein domains. Analyzing the transcriptome of patient-derived diaphragm fibroblast cells suggest that disease associated variants abolish the transcription factor activity. Furthermore, we showed that the remaining genes with damaging variants in CDH significantly overlap with genes implicated in other developmental disorders. Gene expression patterns and patient phenotypes support pleiotropic effects of damaging variants in these genes on CDH and other developmental disorders. Finally, functional enrichment analysis implicates the disruption of regulation of gene expression, kinase activities, intra-cellular signaling, and cytoskeleton organization as pathogenic mechanisms in CDH.
AB - Congenital diaphragmatic hernia (CDH) is a severe birth defect that is often accompanied by other congenital anomalies. Previous exome sequencing studies for CDH have supported a role of de novo damaging variants but did not identify any recurrently mutated genes. To investigate further the genetics of CDH, we analyzed de novo coding variants in 362 proband-parent trios including 271 new trios reported in this study. We identified four unrelated individuals with damaging de novo variants in MYRF (P = 5.3x10 -8 ), including one likely gene-disrupting (LGD) and three deleterious missense (D-mis) variants. Eight additional individuals with de novo LGD or missense variants were identified from our other genetic studies or from the literature. Common phenotypes of MYRF de novo variant carriers include CDH, congenital heart disease and genitourinary abnormalities, suggesting that it represents a novel syndrome. MYRF is a membrane associated transcriptional factor highly expressed in developing diaphragm and is depleted of LGD variants in the general population. All de novo missense variants aggregated in two functional protein domains. Analyzing the transcriptome of patient-derived diaphragm fibroblast cells suggest that disease associated variants abolish the transcription factor activity. Furthermore, we showed that the remaining genes with damaging variants in CDH significantly overlap with genes implicated in other developmental disorders. Gene expression patterns and patient phenotypes support pleiotropic effects of damaging variants in these genes on CDH and other developmental disorders. Finally, functional enrichment analysis implicates the disruption of regulation of gene expression, kinase activities, intra-cellular signaling, and cytoskeleton organization as pathogenic mechanisms in CDH.
UR - http://www.scopus.com/inward/record.url?scp=85058925741&partnerID=8YFLogxK
U2 - 10.1371/journal.pgen.1007822
DO - 10.1371/journal.pgen.1007822
M3 - Article
C2 - 30532227
AN - SCOPUS:85058925741
SN - 1553-7390
VL - 14
JO - PLoS genetics
JF - PLoS genetics
IS - 12
M1 - e1007822
ER -