USH2A mutational spectrum causing syndromic and non-syndromic retinal dystrophies in a large cohort of Mexican patients.

IF 1.8 3区医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY

Molecular Vision Pub Date : 2023-01-01

Vianey Ordoñez-Labastida, Oscar F Chacon-Camacho, Victor R Lopez-Rodriguez, Juan C Zenteno

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引用次数: 0

Abstract

Background: Mutations in the USH2A gene are the leading cause of both non-syndromic autosomal recessive retinitis pigmentosa (RP) and Usher syndrome, a syndromic form of RP characterized by retinal dystrophy and sensorineural hearing loss. To contribute to the expansion of the USH2A-related molecular spectrum, the results of genetic screening in a large cohort of Mexican patients are presented.

Methods: The study population comprised 61 patients with a clinical diagnosis of either non-syndromic RP (n = 30) or Usher syndrome type 2 (USH2; n = 31) who were demonstrated to carry biallelic pathogenic variants in USH2A in a three-year period. Genetic screening was performed either by gene panel sequencing or by exome sequencing. A total of 72 available first- or second-degree relatives were also genotyped for familial segregation of the identified variants.

Results: The USH2A mutational spectrum in RP patients included 39 distinct pathogenic variants, most of them of the missense type. The most common RP-causing variants were p.Cys759Phe (c.2276G>T), p.Glu767Serfs*21 (c.2299delG), and p.Cys319Tyr (c.956G>A), which together accounted for 25% of all RP variants. Novel USH2A mutations included three nonsense, two missense, two frameshift, and one intragenic deletion. The USH2A mutational spectrum in USH2 patients included 26 distinct pathogenic variants, most of them of the nonsense and frameshift types. The most common Usher syndrome-causing variants were p.Glu767Serfs*21 (c.2299delG), p.Arg334Trp (c.1000C>T), and c.12067-2A>G), which together accounted for 42% of all USH2-related variants. Novel Usher syndrome USH2A mutations included six nonsense, four frameshift, and two missense mutations. The c.2299delG mutation was associated with a common haplotype for SNPs located in exons 2-21 of USH2A, indicating a founder mutation effect.

Conclusions: Our work expands the USH2A mutational profile by identifying 20 novel pathogenic variants causing syndromic and non-syndromic retinal dystrophy. The prevalent c.2299delG allele is shown to arise from a founder effect. Our results emphasize the usefulness of molecular screening in underrepresented populations for a better characterization of the molecular spectrum of common monogenic diseases.

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USH2A突变谱在一大批墨西哥患者中引起综合征和非综合征性视网膜营养不良

背景:USH2A基因突变是非综合征性常染色体隐性视网膜色素变性(RP)和Usher综合征的主要原因，Usher综合征是RP的一种综合征形式，以视网膜营养不良和感音神经性听力损失为特征。为了有助于扩大ush2a相关的分子谱，遗传筛选的结果在一个大队列的墨西哥患者提出。方法:研究人群包括61例临床诊断为非综合征性RP (n = 30)或Usher综合征2型(USH2;n = 31)，在三年内被证明携带USH2A双等位致病变异。通过基因面板测序或外显子组测序进行遗传筛查。共有72个可用的一级或二级亲属也被鉴定变异的家族分离进行基因分型。结果:RP患者的USH2A突变谱包括39种不同的致病变异，其中大部分为错义型。最常见的RP变异是p.Cys759Phe (c.2276G>T)、p.Glu767Serfs*21 (c.2299delG)和p.Cys319Tyr (c.956G>A)，占所有RP变异的25%。新的USH2A突变包括3个无义突变、2个错义突变、2个移码突变和1个基因内缺失突变。USH2患者的USH2A突变谱包括26种不同的致病变异，其中大多数为无义型和移码型。最常见的Usher综合征变异为p.g u767serfs *21 (c.2299delG)、p.g arg334trp (c.1000C>T)和c.12067-2A>G)，占所有ush2相关变异的42%。新型Usher综合征USH2A突变包括6个无义突变、4个移码突变和2个错义突变。c.2299delG突变与位于USH2A外显子2-21的SNPs的共同单倍型相关，表明存在始发突变效应。结论:我们的工作通过鉴定20种导致综合征和非综合征性视网膜营养不良的新型致病变异，扩大了USH2A突变谱。普遍存在的c.2299delG等位基因是由奠基人效应产生的。我们的研究结果强调了分子筛选在代表性不足的人群中对更好地表征常见单基因疾病的分子谱的有用性。

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来源期刊

Molecular Vision 生物-生化与分子生物学

CiteScore

4.40

自引率

0.00%

发文量

审稿时长

1 months

期刊介绍： Molecular Vision is a peer-reviewed journal dedicated to the dissemination of research results in molecular biology, cell biology, and the genetics of the visual system (ocular and cortical). Molecular Vision publishes articles presenting original research that has not previously been published and comprehensive articles reviewing the current status of a particular field or topic. Submissions to Molecular Vision are subjected to rigorous peer review. Molecular Vision does NOT publish preprints. For authors, Molecular Vision provides a rapid means of communicating important results. Access to Molecular Vision is free and unrestricted, allowing the widest possible audience for your article. Digital publishing allows you to use color images freely (and without fees). Additionally, you may publish animations, sounds, or other supplementary information that clarifies or supports your article. Each of the authors of an article may also list an electronic mail address (which will be updated upon request) to give interested readers easy access to authors.