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参与先天性心脏病发生发展的转录因子和信号分子的基因改变——一篇叙述性综述

Genetic Alterations of Transcription Factors and Signaling Molecules Involved in the Development of Congenital Heart Defects-A Narrative Review.

作者信息

Bolunduț Alexandru Cristian, Lazea Cecilia, Mihu Carmen Mihaela

机构信息

1st Department of Pediatrics, "Iuliu Hațieganu" University of Medicine and Pharmacy, 400370 Cluj-Napoca, Romania.

1st Pediatrics Clinic, Emergency Pediatric Hospital, 400370 Cluj-Napoca, Romania.

出版信息

Children (Basel). 2023 Apr 29;10(5):812. doi: 10.3390/children10050812.

DOI:10.3390/children10050812
PMID:37238360
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10216998/
Abstract

Congenital heart defects (CHD) are the most common congenital abnormality, with an overall global birth prevalence of 9.41 per 1000 live births. The etiology of CHDs is complex and still poorly understood. Environmental factors account for about 10% of all cases, while the rest are likely explained by a genetic component that is still under intense research. Transcription factors and signaling molecules are promising candidates for studies regarding the genetic burden of CHDs. The present narrative review provides an overview of the current knowledge regarding some of the genetic mechanisms involved in the embryological development of the cardiovascular system. In addition, we reviewed the association between the genetic variation in transcription factors and signaling molecules involved in heart development, including TBX5, GATA4, NKX2-5 and CRELD1, and congenital heart defects, providing insight into the complex pathogenesis of this heterogeneous group of diseases. Further research is needed in order to uncover their downstream targets and the complex network of interactions with non-genetic risk factors for a better molecular-phenotype correlation.

摘要

先天性心脏病(CHD)是最常见的先天性异常,全球总体出生患病率为每1000例活产中有9.41例。CHD的病因复杂,目前仍知之甚少。环境因素约占所有病例的10%,其余病例可能由仍在深入研究的遗传因素解释。转录因子和信号分子是研究CHD遗传负担的有前景的候选对象。本叙述性综述概述了目前关于心血管系统胚胎发育中一些遗传机制的知识。此外,我们回顾了心脏发育中涉及的转录因子和信号分子(包括TBX5、GATA4、NKX2 - 5和CRELD1)的基因变异与先天性心脏病之间的关联,深入了解了这一异质性疾病组的复杂发病机制。为了揭示它们的下游靶点以及与非遗传风险因素的复杂相互作用网络,以实现更好的分子 - 表型相关性,还需要进一步的研究。

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