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Tetralogy of Fallot and Hypoplastic Left Heart Syndrome – Complex Clinical Phenotypes Meet Complex Genetic Networks

机译:法洛四联症和发育不良的左心综合征-复杂的临床表型符合复杂的遗传网络

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摘要

In many cases congenital heart disease (CHD) is represented by a complex phenotype and an array of several functional and morphological cardiac disorders. These malformations will be briefly summarized in the first part focusing on two severe CHD phenotypes, hypoplastic left heart syndrome (HLHS) and tetralogy of Fallot (TOF). In most cases of CHD the genetic origin remains largely unknown, though the complexity of the clinical picture strongly argues against a dysregulation which can be attributed to a single candidate gene but rather suggests a multifaceted polygenetic origin with elaborate interactions. Consistent with this idea, genome-wide approaches using whole exome sequencing, comparative sequence analysis of multiplex families to identify de novo mutations and global technologies to identify single nucleotide polymorphisms, copy number variants, dysregulation of the transcriptome and epigenetic variations have been conducted to obtain information about genetic alterations and potential predispositions possibly linked to the occurrence of a CHD phenotype. In the second part of this review we will summarize and discuss the available literature on identified genetic alterations linked to TOF and HLHS.
机译:在许多情况下,先天性心脏病(CHD)表现为复杂的表型以及一系列功能性和形态性心脏病。这些畸形将在第一部分中简要概述,重点关注两种严重的CHD表型,左心发育不全综合征(HLHS)和法洛四联症(TOF)。在大多数冠心病病例中,遗传起源仍然是未知的,尽管临床情况的复杂性强烈反对功能失调,这可能归因于单个候选基因,而是暗示了相互作用复杂的多基因多源起源。与这个想法一致的是,已经进行了使用全外显子组测序的全基因组方法,对多重家族进行比较序列分析以识别从头突变和鉴定单核苷酸多态性,拷贝数变异,转录组失调和表观遗传变异的全球技术。有关可能与冠心病表型发生有关的遗传改变和潜在易感性的信息。在本综述的第二部分中,我们将总结和讨论有关与TOF和HLHS相关的已确定遗传变异的文献。

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