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Genetic architecture of retinal and macular degenerative diseases: the promise and challenges of next-generation sequencing

机译:视网膜和黄斑变性疾病的遗传结构:下一代测序的前景和挑战

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摘要

Inherited retinal degenerative diseases (RDDs) display wide variation in their mode of inheritance, underlying genetic defects, age of onset, and phenotypic severity. Molecular mechanisms have not been delineated for many retinal diseases, and treatment options are limited. In most instances, genotype-phenotype correlations have not been elucidated because of extensive clinical and genetic heterogeneity. Next-generation sequencing (NGS) methods, including exome, genome, transcriptome and epigenome sequencing, provide novel avenues towards achieving comprehensive understanding of the genetic architecture of RDDs. Whole-exome sequencing (WES) has already revealed several new RDD genes, whereas RNA-Seq and ChIP-Seq analyses are expected to uncover novel aspects of gene regulation and biological networks that are involved in retinal development, aging and disease. In this review, we focus on the genetic characterization of retinal and macular degeneration using NGS technology and discuss the basic framework for further investigations. We also examine the challenges of NGS application in clinical diagnosis and management.
机译:遗传性视网膜变性疾病(RDD)在其遗传模式,潜在的遗传缺陷,发病年龄和表型严重性方面表现出很大的差异。对于许多视网膜疾病尚未阐明分子机制,并且治疗选择受到限制。在大多数情况下,由于广泛的临床和遗传异质性,尚未阐明基因型与表型的相关性。下一代测序(NGS)方法,包括外显子组,基因组,转录组和表观基因组测序,为全面了解RDDs的遗传结构提供了新颖的途径。全基因组测序(WES)已经揭示了几个新的RDD基因,而RNA-Seq和ChIP-Seq分析有望揭示涉及视网膜发育,衰老和疾病的基因调控和生物网络的新方面。在这篇综述中,我们重点研究了使用NGS技术对视网膜和黄斑变性的遗传特征,并讨论了进一步研究的基本框架。我们还将探讨NGS在临床诊断和管理中的应用挑战。

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