Analysis of candidate variants in a Chinese family with monozygotic twins with keratoconus: a case report.

IF 1.2 4区 医学 Q4 GENETICS & HEREDITY Ophthalmic Genetics Pub Date : 2024-11-15 DOI:10.1080/13816810.2024.2427295
Chunyuan Song, Kehua Wang, Ling Li, Luping Hu, Jie Bai, Lin Zhao, Chang Liu, Shaowei Li
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Abstract

Background: Keratoconus (KC) is an asymmetrical bilateral corneal ectasia, of which the pathogenesis is unknown. Moreover, genetic factors play an important role. We reported ophthalmic findings in a Chinese family with monozygotic twins with KC to describe the clinical features and identify genetic variants.

Methods: Comprehensive ophthalmic clinical assessments and examinations, including history, slit-lamp biomicroscopy, best-corrected visual acuity, corneal topography, anterior segment optical coherence tomography, and corneal biomechanics, were carried out on the twins and their parents. Whole-genome sequencing (WGS) was performed to identify variants in this family. SIFT, PolyPhen2, MutationTaster, and CADD were used to predict the effect of amino acid substitutions on the affected protein.

Results: The twins presented typical KC features. However, their mother did not meet the criteria for a KC diagnosis but exhibited KC subclinical manifestations. After screening, 12 potentially pathogenic variants in 10 genes were identified in both twins and emerged as candidate variants for this family. These genes included 1 previously reported KC-associated variant (ZNF469, c.4384 G>A); 8 variants in 6 KC-associated genes (GRHPR, c.337 G>A, c.862_863del; COL6A1, c.920 G>A; FLG, c.8753C>G; HSPG2, c.9503C>T; KRT82, c.1306 G>A; SCN9A, c.5702_5706del, c.641 G>A); and 3 variants in 3 non-KC-associated genes (PDE6G, c.6C>A; HAL, c.1724C>T; AGBL1, c.2381 G>A).

Conclusions: The accumulation of these potentially pathogenic variants in twins may have caused KC in these twins. These results expand the spectrum of KC candidate variants and provide a basis for further studies on KC.

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一个中国单卵双生角膜病家族的候选变异分析:病例报告。
背景:角膜炎(KC)是一种不对称的双侧角膜异位症,其发病机制尚不清楚。此外,遗传因素也起着重要作用。我们报告了一个中国KC单卵双生家庭的眼科检查结果,以描述其临床特征并确定遗传变异:对双胞胎及其父母进行了全面的眼科临床评估和检查,包括病史、裂隙灯生物显微镜检查、最佳矫正视力、角膜地形图、眼前段光学相干断层扫描和角膜生物力学检查。全基因组测序(WGS)用于鉴定该家族的变异。使用 SIFT、PolyPhen2、MutationTaster 和 CADD 预测氨基酸置换对受影响蛋白质的影响:这对双胞胎具有典型的 KC 特征。然而,他们的母亲不符合 KC 诊断标准,但表现出 KC 亚临床表现。经过筛选,在这对双胞胎中发现了 10 个基因中的 12 个潜在致病变体,并成为该家族的候选变体。这些基因包括 1 个以前报道过的 KC 相关变异基因(ZNF469,c.4384 G>A);6 个 KC 相关基因中的 8 个变异基因(GRHPR,c.337 G>A,c.862_863del;COL6A1,c.920 G>A;FLG,c.8753 C>G;HSPG2,c.862_863del)。C>G;HSPG2,c.9503C>T;KRT82,c.1306 G>A;SCN9A,c.5702_5706del,c.641 G>A);以及 3 个非 KC 相关基因中的 3 个变异(PDE6G,c.6C>A;HAL,c.1724C>T;AGBL1,c.2381 G>A):结论:这些潜在的致病变异基因在双胞胎中的累积可能会导致这些双胞胎患上 KC。这些结果扩大了 KC 候选变异的范围,为进一步研究 KC 提供了依据。
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来源期刊
Ophthalmic Genetics
Ophthalmic Genetics 医学-眼科学
CiteScore
2.40
自引率
8.30%
发文量
126
审稿时长
>12 weeks
期刊介绍: Ophthalmic Genetics accepts original papers, review articles and short communications on the clinical and molecular genetic aspects of ocular diseases.
期刊最新文献
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