Evaluating gap junction variants for a role in pediatric cataract: an overview of the genetic landscape and clinical classification of variants in the GJA3 and GJA8 genes

Pub Date : 2022-12-20 DOI:10.1080/17469899.2023.2160320
Johanna L Jones, K. Burdon
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引用次数: 1

Abstract

ABSTRACT Introduction Variants in the two lens-expressed gap junction genes GJA3 and GJA8 are among the most common causes of inherited pediatric cataract. These two genes alone account for up to 18% of the cases, second only to the crystallin gene family. Areas covered All published cataract-associated variants in the GJA3 and GJA8 genes were reviewed for a role in pediatric cataract. Autosomal dominant inheritance was most frequently reported, alongside instances of reduced penetrance and autosomal recessive disease. Variant curation using the ACMG-AMP guidelines identified that many variants do not meet the modern standards for clinical interpretation of pathogenicity. There is broad phenotypic heterogeneity of cataract associated with gap junction gene variants. Pathogenic variants are located throughout both proteins with an enrichment in the N-terminal, first two transmembrane domains, and two extracellular loops. Expert opinion Nearly half the gap junction gene variants observed in cataract patients lack sufficient evidence of pathogenicity to form a useful clinical opinion. For many variants, this may be rectified over time as the variant is observed in additional patients but would be vastly accelerated by the generation of well-characterized and standardized functional data evaluating the specific effect of each variant on protein function.
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评估间隙连接变异在儿童白内障中的作用:GJA3和GJA8基因变异的遗传景观和临床分类概述
两个晶状体表达的间隙连接基因GJA3和GJA8的变异是遗传性儿童白内障的最常见原因之一。仅这两个基因就占了18%的病例,仅次于晶体蛋白基因家族。本文回顾了所有已发表的GJA3和GJA8基因的白内障相关变异在儿童白内障中的作用。常染色体显性遗传是最常见的报道,同时减少外显率和常染色体隐性遗传病的实例。使用ACMG-AMP指南的变异管理发现,许多变异不符合现代临床解释致病性的标准。与间隙连接基因变异相关的白内障存在广泛的表型异质性。致病性变异位于两种蛋白质中,富集在n端,前两个跨膜结构域和两个细胞外环。专家意见在白内障患者中观察到的间隙连接基因变异中,近一半缺乏足够的致病性证据,无法形成有用的临床意见。对于许多变体,这可能会随着时间的推移而纠正,因为变体在其他患者中观察到,但通过生成充分表征和标准化的功能数据来评估每种变体对蛋白质功能的特定影响,这将大大加速。
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