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心脏病的发育模式:来自tinman的见解

Developmental paradigms in heart disease: insights from tinman.

作者信息

Prall Owen W J, Elliott David A, Harvey Richard P

机构信息

Victor Chang Cardiac Research Institute, St. Vincent's Hospital, Darlinghurst, NSW, Australia.

出版信息

Ann Med. 2002;34(3):148-56.

Abstract

Congenital heart disease is a significant cause of morbidity and mortality in humans, and gene mutations that underlie some of these anomalies are now being described. The NKX2.5 gene, which encodes a homeobox transcription factor, was initially discovered in mice through its similarity to the tinman gene of the fruitfly Drosophila. Tinman is required for formation of the dorsal pulsatile vessel or 'heart' of the fly. Tinman and NKX2.5 share structural and functional features, and in mice the gene is required for normal cardiac looping and differentiation of chamber myocardium. Humans with heterozygous mutations in the NKX2.5 gene generally have a disorder involving progressive atrio-ventricular conduction block and atrial septal defect, although sometimes other abnormalities including tetralogy of Fallot. The TBX5 gene, which encodes another cardiac transcription factor that collaborates with NKX2.5, is also an important cardiac disease gene, with heterozygous mutations responsible for Holt-Oram (hand/heart) syndrome. These contributions to human pathology underscore the relevance of studying biological phenomena in lower organisms, and examination of other genes acting in this and associated pathways will expand our knowledge of congenital abnormalities and disease predisposition, and improve genetic counseling.

摘要

先天性心脏病是人类发病和死亡的重要原因,目前正在描述一些此类异常情况背后的基因突变。NKX2.5基因编码一种同源盒转录因子,最初是在小鼠中通过与果蝇tinman基因的相似性发现的。tinman是果蝇背侧搏动血管或“心脏”形成所必需的。Tinman和NKX2.5具有结构和功能特征,在小鼠中,该基因是正常心脏环化和心室心肌分化所必需的。NKX2.5基因杂合突变的人类通常患有涉及进行性房室传导阻滞和房间隔缺损的疾病,尽管有时还包括其他异常,如法洛四联症。TBX5基因编码另一种与NKX2.5协同作用的心脏转录因子,也是一种重要的心脏病基因,其杂合突变导致霍尔特-奥拉姆(手/心脏)综合征。这些对人类病理学的贡献强调了研究低等生物中生物学现象的相关性,对该途径及相关途径中其他作用基因的研究将扩展我们对先天性异常和疾病易感性的认识,并改善遗传咨询。

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