Congenital anterior segment ocular disorders: Genotype-phenotype correlations and emerging novel mechanisms

IF 18.6 1区 医学 Q1 OPHTHALMOLOGY
Linda M. Reis , Sarah E. Seese , Deborah Costakos , Elena V. Semina
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引用次数: 0

Abstract

Development of the anterior segment of the eye requires reciprocal sequential interactions between the arising tissues, facilitated by numerous genetic factors. Disruption of any of these processes results in congenital anomalies in the affected tissue(s) leading to anterior segment disorders (ASD) including aniridia, Axenfeld-Rieger anomaly, congenital corneal opacities (Peters anomaly, cornea plana, congenital primary aphakia), and primary congenital glaucoma. Current understanding of the genetic factors involved in ASD remains incomplete, with approximately 50% overall receiving a genetic diagnosis. While some genes are strongly associated with a specific clinical diagnosis, the majority of known factors are linked with highly variable phenotypic presentations, with pathogenic variants in FOXC1, CYP1B1, and PITX2 associated with the broadest spectrum of ASD conditions. This review discusses typical clinical presentations including associated systemic features of various forms of ASD; the latest functional data and genotype-phenotype correlations related to 25 ASD factors including newly identified genes; promising novel candidates; and current and emerging treatments for these complex conditions. Recent developments of interest in the genetics of ASD include identification of phenotypic expansions for several factors, discovery of multiple modes of inheritance for some genes, and novel mechanisms including a growing number of non-coding variants and alleles affecting specific domains/residues and requiring further studies.

先天性前节眼病:基因型与表型的相关性和新出现的机制。
眼球前段的发育需要在多种遗传因素的作用下,各组织之间依次进行相互影响。其中任何一个过程的中断都会导致受影响组织出现先天性异常,从而引发前段疾病(ASD),包括无眼球症、阿克森菲尔德-里格异常、先天性角膜翳(彼得斯异常、平面角膜、先天性原发性无眼球症)和原发性先天性青光眼。目前对 ASD 遗传因素的了解仍不全面,大约 50%的患者会得到遗传诊断。虽然有些基因与特定的临床诊断密切相关,但大多数已知的因素都与千差万别的表型表现有关,其中 FOXC1、CYP1B1 和 PITX2 的致病变异会导致最广泛的 ASD 病症。本综述讨论了典型的临床表现,包括各种形式的 ASD 的相关系统特征;与 25 种 ASD 因子(包括新发现的基因)相关的最新功能数据和基因型与表型的相关性;有希望的新候选基因;以及针对这些复杂病症的现有和新兴治疗方法。ASD 遗传学的最新进展包括:确定了几种因素的表型扩展、发现了一些基因的多种遗传模式以及新的机制,包括越来越多的非编码变异和影响特定结构域/残基并需要进一步研究的等位基因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
34.10
自引率
5.10%
发文量
78
期刊介绍: Progress in Retinal and Eye Research is a Reviews-only journal. By invitation, leading experts write on basic and clinical aspects of the eye in a style appealing to molecular biologists, neuroscientists and physiologists, as well as to vision researchers and ophthalmologists. The journal covers all aspects of eye research, including topics pertaining to the retina and pigment epithelial layer, cornea, tears, lacrimal glands, aqueous humour, iris, ciliary body, trabeculum, lens, vitreous humour and diseases such as dry-eye, inflammation, keratoconus, corneal dystrophy, glaucoma and cataract.
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