与人类先天性心脏缺陷相关的Nkx2 - 5突变在早期胚胎中的短暂表达会导致非洲爪蟾出现心脏缺陷。
Transient early embryonic expression of Nkx2-5 mutations linked to congenital heart defects in human causes heart defects in Xenopus laevis.
作者信息
Bartlett Heather L, Sutherland Lillian, Kolker Sandra J, Welp Chelsea, Tajchman Urszula, Desmarais Vera, Weeks Daniel L
机构信息
Department of Pediatrics, University of Iowa, Iowa City, Iowa 52242-1109, USA.
出版信息
Dev Dyn. 2007 Sep;236(9):2475-84. doi: 10.1002/dvdy.21244.
Abstract
Nkx2-5 is a homeobox containing transcription factor that is conserved and expressed in organisms that form hearts. Fruit flies lacking the gene (tinman) fail to form a dorsal vessel, mice that are homozygous null for Nkx2-5 form small, deformed hearts, and several human cardiac defects have been linked to dominant mutations in the Nkx2-5 gene. The Xenopus homologs (XNkx2-5) of two truncated forms of Nkx2-5 that have been identified in humans with congenital heart defects were used in the studies reported here. mRNAs encoding these mutations were injected into single cell Xenopus embryos, and heart development was monitored. Our results indicate that the introduction of truncated XNkx2-5 variants leads to three principle developmental defects. The atrial septum and the valve of the atrioventricular canal were both abnormal. In addition, video microscopic timing of heart contraction indicated that embryos injected with either mutant form of XNkx2-5 have conduction defects.
摘要
Nkx2-5是一种含有同源盒的转录因子,在形成心脏的生物体中保守且表达。缺乏该基因(tinman)的果蝇无法形成背血管,Nkx2-5基因纯合缺失的小鼠形成小的、畸形的心脏,并且几种人类心脏缺陷与Nkx2-5基因的显性突变有关。本文报道的研究使用了在患有先天性心脏病的人类中鉴定出的两种截短形式的Nkx2-5的非洲爪蟾同源物(XNkx2-5)。将编码这些突变的mRNA注射到单细胞非洲爪蟾胚胎中,并监测心脏发育。我们的结果表明,截短的XNkx2-5变体的引入导致三个主要发育缺陷。房间隔和房室管瓣膜均异常。此外,心脏收缩的视频显微镜计时表明,注射了任何一种XNkx2-5突变形式的胚胎都有传导缺陷。
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