Trio-based whole-exome sequencing reveals mutations in early-onset high myopia.

IF 2 Q2 OPHTHALMOLOGY BMJ Open Ophthalmology Pub Date : 2024-05-24 DOI:10.1136/bmjophth-2024-001720
Lu Ye, Yi-Ming Guo, Yi-Xin Cai, Junhan Wei, Juan Huang, Jiejing Bi, Ding Chen, Fen-Fen Li, Xiu-Feng Huang
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Abstract

Purpose: Myopia, especially high myopia (HM), represents a widespread visual impairment with a globally escalating prevalence. This study aimed to elucidate the genetic foundations associated with early-onset HM (eoHM) while delineating the genetic landscape specific to Shaanxi province, China.

Methods: A comprehensive analysis of whole-exome sequencing was conducted involving 26 familial trios displaying eoHM. An exacting filtration protocol identified potential candidate mutations within acknowledged myopia-related genes and susceptibility loci. Subsequently, computational methodologies were employed for functional annotations and pathogenicity assessments.

Results: Our investigation identified 7 genes and 10 variants associated with HM across 7 families, including a novel mutation in the ARR3 gene (c.139C>T, p.Arg47*) and two mutations in the P3H2 gene (c.1865T>C, p.Phe622Ser and c.212T>C, p.Leu71Pro). Pathogenic mutations were found in syndromic myopia genes, notably encompassing VPS13B, TRPM1, RPGR, NYX and RP2. Additionally, a thorough comparison of previously reported causative genes of syndromic myopia and myopia risk genes with the negative sequencing results pinpointed various types of mutations within risk genes.

Conclusions: This investigation into eoHM within Shaanxi province adds to the current understanding of myopic genetic factors. Our results warrant further functional validation and ocular examinations, yet they provide foundational insights for future genetic research and therapeutic innovations in HM.

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基于三重全外显子组测序揭示了早发性高度近视的突变。
目的:近视,尤其是高度近视(HM),是一种广泛存在的视力障碍,其发病率在全球范围内呈上升趋势。本研究旨在阐明与早发性HM(eoHM)相关的遗传基础,同时勾勒出中国陕西省特有的遗传图谱:方法:对26例家族性三联症患者进行了全外显子组测序综合分析。方法:对 26 例家族性三倍体 eoHM 进行了全外显子组测序的综合分析,并通过严格的筛选方案确定了公认的近视相关基因和易感基因位点中的潜在候选突变。随后,采用计算方法进行功能注释和致病性评估:我们的调查在 7 个家族中发现了与 HM 相关的 7 个基因和 10 个变体,包括 ARR3 基因中的一个新型突变(c.139C>T,p.Arg47*)和 P3H2 基因中的两个突变(c.1865T>C,p.Phe622Ser 和 c.212T>C,p.Leu71Pro)。在综合近视基因中发现了致病突变,主要包括 VPS13B、TRPM1、RPGR、NYX 和 RP2。此外,将以前报告的综合近视致病基因和近视风险基因与阴性测序结果进行了全面比较,发现风险基因中存在各种类型的突变:这项对陕西省易近视人群的调查加深了人们对近视遗传因素的认识。我们的研究结果还需要进一步的功能验证和眼部检查,但它们为未来的遗传研究和 HM 的治疗创新提供了基础性的见解。
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
BMJ Open Ophthalmology
BMJ Open Ophthalmology OPHTHALMOLOGY-
CiteScore
3.40
自引率
4.20%
发文量
104
审稿时长
20 weeks
期刊最新文献
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