Comprehensive ZEB2 gene analysis for Mowat–Wilson syndrome in a North American cohort: A suggested approach to molecular diagnostics

Mowat–Wilson syndrome is a genetic condition characterized by a recognizable facial phenotype in addition to moderate to severe cognitive disability with severe speech impairment and variable multiple congenital anomalies. The anomalies may include Hirschsprung disease, heart defects, structural eye...

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Veröffentlicht in:	American journal of medical genetics. Part A 2009-11, Vol.149A (11), p.2527-2531
Hauptverfasser:	Saunders, Carol J., Zhao, Weiwei, Ardinger, Holly H.
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Sprache:	eng
Schlagworte:	Abnormalities, Multiple - genetics Adolescent Adult Biological and medical sciences Child Cohort Studies Homeodomain Proteins - genetics Humans Medical genetics Medical sciences Middle Aged Mowat–Wilson syndrome Mutation - genetics North America novel mutations partial deletions Pathology, Molecular Repressor Proteins - genetics Syndrome Young Adult ZEB2 Zinc Finger E-box Binding Homeobox 2
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container_title	American journal of medical genetics. Part A
container_volume	149A
creator	Saunders, Carol J. Zhao, Weiwei Ardinger, Holly H.
description	Mowat–Wilson syndrome is a genetic condition characterized by a recognizable facial phenotype in addition to moderate to severe cognitive disability with severe speech impairment and variable multiple congenital anomalies. The anomalies may include Hirschsprung disease, heart defects, structural eye anomalies including microphthalmia, agenesis of the corpus callosum, and urogenital anomalies. Microcephaly, seizure disorder and constipation are common. All typical cases result from haploinsufficiency of the ZEB2 (also known as ZFHX1B or SIP‐1) gene, with over 100 distinct mutations now described. Approximately 80% of patients have a nonsense or frameshift mutation detectable by sequencing, with the rest having gross deletions necessitating a dosage sensitive assay. Here we report on the results of comprehensive molecular testing for 27 patients testing positive for MWS. Twenty‐one patients had a nonsense, frameshift, or splice site mutation identified by sequencing; 14 of which localized to exon 8 and 17 of which are novel. Six patients had deletions in the ZEB2 gene, including two novel partial gene deletions. This report, the first such analysis in North American patients, adds to the growing list of both novel pathogenic mutations associated with MWS, as well as other variants in the ZEB2 gene. In addition, we suggest an economical testing strategy. © 2009 Wiley‐Liss, Inc.
doi_str_mv	10.1002/ajmg.a.33067
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This report, the first such analysis in North American patients, adds to the growing list of both novel pathogenic mutations associated with MWS, as well as other variants in the ZEB2 gene. 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Part A</title><addtitle>Am J Med Genet A</addtitle><description>Mowat–Wilson syndrome is a genetic condition characterized by a recognizable facial phenotype in addition to moderate to severe cognitive disability with severe speech impairment and variable multiple congenital anomalies. The anomalies may include Hirschsprung disease, heart defects, structural eye anomalies including microphthalmia, agenesis of the corpus callosum, and urogenital anomalies. Microcephaly, seizure disorder and constipation are common. All typical cases result from haploinsufficiency of the ZEB2 (also known as ZFHX1B or SIP‐1) gene, with over 100 distinct mutations now described. Approximately 80% of patients have a nonsense or frameshift mutation detectable by sequencing, with the rest having gross deletions necessitating a dosage sensitive assay. Here we report on the results of comprehensive molecular testing for 27 patients testing positive for MWS. Twenty‐one patients had a nonsense, frameshift, or splice site mutation identified by sequencing; 14 of which localized to exon 8 and 17 of which are novel. Six patients had deletions in the ZEB2 gene, including two novel partial gene deletions. This report, the first such analysis in North American patients, adds to the growing list of both novel pathogenic mutations associated with MWS, as well as other variants in the ZEB2 gene. 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subjects	Abnormalities, Multiple - genetics Adolescent Adult Biological and medical sciences Child Cohort Studies Homeodomain Proteins - genetics Humans Medical genetics Medical sciences Middle Aged Mowat–Wilson syndrome Mutation - genetics North America novel mutations partial deletions Pathology, Molecular Repressor Proteins - genetics Syndrome Young Adult ZEB2 Zinc Finger E-box Binding Homeobox 2
title	Comprehensive ZEB2 gene analysis for Mowat–Wilson syndrome in a North American cohort: A suggested approach to molecular diagnostics
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