Liu Xing-Yuan, Wang Juan, Yang Yi-Qing, Zhang Yang-Yang, Chen Xiao-Zhong, Zhang Wei, Wang Xiao-Zhou, Zheng Jing-Hao, Chen Yi-Han
Department of Pediatrics, Tongji Hospital, Tongji University School of Medicine, Shanghai, China.
Pediatr Cardiol. 2011 Feb;32(2):193-201. doi: 10.1007/s00246-010-9859-6. Epub 2010 Dec 25.
Atrial septal defect (ASD) is a common cardiovascular malformation and an important contributor to substantial morbidity and mortality. Increasing evidence demonstrates that mutated NKX2-5, a gene encoding a homeobox transcription factor crucial to cardiogenesis, is a significant genetic determinant for congenital ASD. Nevertheless, the genetic basis for ASD in a majority of ASD patients remains largely unknown. In the current study, the entire coding region of NKX2-5 was sequenced initially for 58 unrelated probands with familial ASD. The relatives of the probands harboring identified mutations and 200 unrelated control individuals were subsequently genotyped. Three novel heterozygous NKX2-5 mutations (p.P43GfsX59, p.C46 W, and p.S179F) were identified respectively in three families with autosomal dominantly inherited ASD. These mutations, absent in 200 control individuals, cosegregated with ASD in the families that had complete penetrance. The findings expand the spectrum of mutations in NKX2-5 linked to ASD and contribute to genetic counseling, clinical interventions, and prenatal prevention of ASD for individuals with genetic susceptibility.
房间隔缺损(ASD)是一种常见的心血管畸形,是导致严重发病和死亡的重要因素。越来越多的证据表明,编码对心脏发生至关重要的同源盒转录因子的基因NKX2-5发生突变,是先天性ASD的一个重要遗传决定因素。然而,大多数ASD患者ASD的遗传基础在很大程度上仍然未知。在本研究中,首先对58名患有家族性ASD的无关先证者的NKX2-5整个编码区进行了测序。随后对携带已鉴定突变的先证者亲属和200名无关对照个体进行了基因分型。在三个常染色体显性遗传ASD家族中分别鉴定出三个新的杂合NKX2-5突变(p.P43GfsX59、p.C46W和p.S179F)。这些突变在200名对照个体中不存在,在具有完全外显率的家族中与ASD共分离。这些发现扩展了与ASD相关的NKX2-5突变谱,有助于为具有遗传易感性的个体进行ASD的遗传咨询、临床干预和产前预防。
