Dastot-Le Moal Florence, Wilson Meredith, Mowat David, Collot Nathalie, Niel Florence, Goossens Michel
INSERM, U654, Université Paris 12, IFR10-IM3, AP-HP, Groupe Hospitalier Henri Mondor-Albert Chenevier, Service de Biochimie et Génétique, Hôpital Henri Mondor, Créteil, France.
Hum Mutat. 2007 Apr;28(4):313-21. doi: 10.1002/humu.20452.
Mowat-Wilson syndrome (MWS) is a recently delineated mental retardation (MR)-multiple congenital anomaly syndrome, characterized by typical facies, severe MR, epilepsy, and variable congenital malformations, including Hirschsprung disease (HSCR), genital anomalies, congenital heart disease (CHD), and agenesis of the corpus callosum (ACC). It is caused by de novo heterozygous mutations or deletions of the ZFHX1B gene located at 2q22. ZFHX1B encodes Smad-interacting protein-1 (SMADIP1 or SIP1), a transcriptional corepressor involved in the transforming growth factor-beta signaling pathway. It is a highly evolutionarily conserved gene, widely expressed in embryological development. Over 100 mutations have been described in patients with clinically typical MWS, who almost always have whole gene deletions or truncating mutations (nonsense or frameshift) of ZFHX1B, suggesting that haploinsufficiency is the basis of MWS pathology. No obvious genotype-phenotype correlation could be identified so far, but atypical phenotypes have been reported with missense or splice mutations in the ZFHX1B gene. In this work we describe 40 novel mutations and we summarize the various mutational reports published since the identification of the causative gene.
莫瓦特-威尔逊综合征(MWS)是一种最近才被明确的智力发育迟缓(MR)-多发性先天性异常综合征,其特征为典型面容、严重智力发育迟缓、癫痫以及多种先天性畸形,包括先天性巨结肠(HSCR)、生殖器异常、先天性心脏病(CHD)和胼胝体发育不全(ACC)。它由位于2q22的ZFHX1B基因的新生杂合突变或缺失引起。ZFHX1B编码Smad相互作用蛋白-1(SMADIP1或SIP1),这是一种参与转化生长因子-β信号通路的转录共抑制因子。它是一个高度进化保守的基因,在胚胎发育中广泛表达。在临床典型的MWS患者中已描述了100多种突变,这些患者几乎总是存在ZFHX1B的全基因缺失或截短突变(无义或移码突变),这表明单倍剂量不足是MWS病理的基础。到目前为止,尚未发现明显的基因型-表型相关性,但已报道ZFHX1B基因的错义或剪接突变会出现非典型表型。在这项工作中,我们描述了40种新突变,并总结了自致病基因被鉴定以来发表的各种突变报告。
