ABCA4相关视网膜病变中的新型变异,对意义不确定的变异进行结构性重新评估。

IF 2.1 4区 医学 Q2 OPHTHALMOLOGY
Ophthalmologica Pub Date : 2024-01-01 Epub Date: 2024-07-23 DOI:10.1159/000540361
Kevin Gregory-Evans, Olubayo U Kolawole, Robert S Molday, Cheryl Y Gregory-Evans
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引用次数: 0

摘要

导言:由于基因检测中发现了大量意义不确定的变体(VUS),因此对遗传性视网膜疾病进行确凿的分子遗传学诊断仍是一项重大挑战。在此,我们确定了一组加拿大遗传性视网膜营养不良患者中 ABCA4 基因变异的基因型和表型谱:这项回顾性研究评估了 64 名被诊断为遗传性视网膜营养不良且存在 ABCA4 基因变异的受试者。变异的致病性通过与基因数据库的比较和硅学建模进行评估。利用ABCA4蛋白的低温电子结构模型对归类为VUS的ABCA4变异进行了进一步评估,以预测其对蛋白功能的影响,并对其进化保护进行了评估:结果:在52名患有斯塔加特氏病、锥杆营养不良症、黄斑营养不良症或模式营养不良症的受试者中,检测出了确凿的致病双拷贝ABCA4变体。另外还有 14 个新变异,包括 1 个无义变异、1 个框架移位变异、3 个剪接变异和 9 个错义变异。根据硅学建模、蛋白质建模以及从人类到斑马鱼的进化保护,我们将其中的 5 个变异重新归类为致病变异,另外 3 个变异可能为致病变异。我们还增加了四个已知致病变体(c.2161-2A>G; Leu296Cysfs*4; Arg1640Gln 和 Pro1380Leu)的 ABCA4 表型谱:本研究扩展了 ABCA4 疾病相关变体的基因型和表型谱。通过基于面板的基因检测,我们发现了 14 个新型 ABCA4 变异,其中 8 个被确定为致病或可能致病。这些方法可以在一定程度上避免对新型 ABCA4 变体进行劳动密集型体外和体内评估。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Novel Variants in ABCA4-Related Retinopathies with Structural Re-Assessment of Variants of Uncertain Significance.

Introduction: Conclusive molecular genetic diagnoses in inherited retinal diseases remains a major challenge due to the large number of variants of uncertain significance (VUS) identified in genetic testing. Here, we determined the genotypic and phenotypic spectrum of ABCA4 gene variants in a cohort of Canadian inherited retinal dystrophy subjects.

Methods: This retrospective study evaluated 64 subjects with an inherited retinal dystrophy diagnosis with variants in the ABCA4 gene. Pathogenicity of variants was assessed by comparison to genetic databases and in silico modelling. ABCA4 variants classified as VUS were further evaluated using a cryo-electron structural model of the ABCA4 protein to predict impact on protein function and were also assessed for evolutionary conservation.

Results: Conclusive disease-causing biallelic ABCA4 variants were detected in 52 subjects with either Stargardt's disease, cone-rod dystrophy, macular dystrophy, or pattern dystrophy. A further 14 variants were novel comprising 1 nonsense, 1 frameshift, 3 splicing, and 9 missense variants. Based on in silico modelling, protein modelling and evolutionary conservation from human to zebrafish, we re-classified 5 of these as pathogenic and a further 3 as likely pathogenic. We also added to the ABCA4 phenotypic spectrum seen with four known pathogenic variants (c.2161-2A>G; Leu296Cysfs*4; Arg1640Gln; and Pro1380Leu).

Conclusions: This study expands the genotypic and phenotypic spectrum of ABCA4 disease-associated variants. By panel-based genetic testing, we identified 14 novel ABCA4 variants of which 8 were determined to be disease-causing or likely disease-causing. These methodologies could circumvent somewhat the need for labour intensive in vitro and in vivo assessments of novel ABCA4 variants.

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来源期刊
Ophthalmologica
Ophthalmologica 医学-眼科学
CiteScore
5.10
自引率
3.80%
发文量
39
审稿时长
3 months
期刊介绍: Published since 1899, ''Ophthalmologica'' has become a frequently cited guide to international work in clinical and experimental ophthalmology. It contains a selection of patient-oriented contributions covering the etiology of eye diseases, diagnostic techniques, and advances in medical and surgical treatment. Straightforward, factual reporting provides both interesting and useful reading. In addition to original papers, ''Ophthalmologica'' features regularly timely reviews in an effort to keep the reader well informed and updated. The large international circulation of this journal reflects its importance.
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