The spectrum of ZEB2 mutations causing the Mowat-Wilson syndrome in Japanese populations.

[hirschsprung disease]

Mowat-Wilson syndrome (MWS ) is a multiple congenital anomaly syndrome characterized by moderate or severe intellectual disability , a characteristic facial appearance , microcephaly , epilepsy , agenesis or hypoplasia of the corpus callosum , congenital heart defects , Hirschsprung disease , and urogenital /renal anomalies . It is caused by de novo heterozygous loss of function mutations including nonsense mutations , frameshift mutations , and deletions in ZEB 2 at 2 q 22 . ZEB 2 encodes the zinc finger E -box binding homeobox 2 protein consisting of 1 ,214 amino acids . Herein , we report 13 nonsense and 27 frameshift mutations from 40 newly identified MWS patients in Japan . Although the clinical findings of all the Japanese MWS patients with nonsense and frameshift mutations were quite similar to the previous review reports of MWS caused by nonsense mutations , frameshift mutations and deletions of ZEB 2 , the frequencies of microcephaly , Hirschsprung disease , and urogenital /renal anomalies were small . Patients harbored mutations spanning the region between the amino acids 55 and 1 ,204 in wild-type ZEB 2 . There was no obvious genotype-phenotype correlation among the patients . A transfection study demonstrated that the cellular level of the longest form of the mutant ZEB 2 protein harboring the p .D 1204 Rfs *29 mutation was remarkably low . The results showed that the 3 '-end frameshift mutation of ZEB 2 causes MWS due to ZEB 2 instability .