Whole Exome Sequencing as an Effective Molecular Diagnosis Tool for Craniofacial Fibrous Dysplasia with Ocular Complications.

IF 1.7 4区 医学 Q3 OPHTHALMOLOGY Current Eye Research Pub Date : 2024-09-01 Epub Date: 2024-05-06 DOI:10.1080/02713683.2024.2349634
Bingyan Shen, Yenan Fang, Qin Dai, Qiqi Xie, Wencan Wu, Min Wang
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Abstract

Purpose: To summarize the clinical manifestations of craniofacial fibrous dysplasia (CFD) patients with ocular complications, and find effective methods to diagnose early.

Methods: Nine CFD patients with ocular complications, and their parents were recruited in this study. All patients underwent ocular and systemic examinations. Bone lesions from all patients and peripheral blood from patients and their parents were collected for whole exome sequencing (WES). According to the screening for low-frequency deleterious variants, and bioinformatics variants prediction software, possible disease-causing variants were found in multiple CFD patients. The variants were validated by Sanger sequencing. Trio analysis was performed to verify the genetic patterns of CFD.

Results: All patients were diagnosed with CFD, according to the clinical manifestations, classic radiographic appearance, and pathological biopsy. The main symptoms of the 9 CFD patients, included visual decline (9/9), craniofacial deformity (3/9) and strabismus (2/9), with few extraocular manifestations. The family backgrounds of all the CFD patients indicated that only the patient was affected, and their immediate family members were normal. GNAS variants were identified in all bone lesions from CFD patients, including two variant types: c.601C > T:p.R201C(6/9) and c.602G > A:p.R201H (3/9) in exon 8. The detection rate reached 100% by WES, but only 77.8% by Sanger sequencing. Interestingly, we found GNAS variants could not be detected in peripheral blood samples from CFD patients or their parents, and other potentially disease-causing gene variants related to CFD were not found.

Conclusions: For CFD patients with bone lesions involving the optic canal or sphenoid sinus regions, ocular symptoms should also be considered. Furthermore, we confirmed that CFD is not inherited, somatic variants in the GNAS gene are the main pathogenic gene causing CFD. Compared to the traditional methods in molecular genetic diagnosis of CFD, WES is more feasible and effective but limited in the type of samples.

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全外显子组测序是颅面纤维发育不良伴眼部并发症的有效分子诊断工具
目的:总结颅面纤维发育不良(CFD)患者眼部并发症的临床表现,并寻找早期诊断的有效方法:方法:本研究招募了9名患有眼部并发症的颅面纤维发育不良患者及其家长。所有患者均接受了眼部和全身检查。收集所有患者的骨病变和患者及其父母的外周血进行全外显子组测序(WES)。根据低频有害变异筛选和生物信息学变异预测软件,在多名 CFD 患者中发现了可能的致病变异。这些变异通过桑格测序进行了验证。三组分析验证了 CFD 的遗传模式:结果:根据临床表现、典型影像学表现和病理活检结果,所有患者均被确诊为 CFD。9名CFD患者的主要症状包括视力下降(9/9)、颅面畸形(3/9)和斜视(2/9),很少有眼外表现。从所有 CFD 患者的家族背景来看,只有患者本人受到影响,其直系亲属均正常。在所有CFD患者的骨病变中都发现了GNAS变异,包括两种变异类型:第8外显子中的c.601C > T:p.R201C (6/9)和c.602G > A:p.R201H (3/9)。WES 的检出率达到 100%,但 Sanger 测序的检出率仅为 77.8%。有趣的是,我们发现在CFD患者或其父母的外周血样本中检测不到GNAS变异,也没有发现与CFD相关的其他潜在致病基因变异:结论:对于骨病变累及视管或蝶窦区域的 CFD 患者,还应考虑眼部症状。此外,我们还证实 CFD 不具有遗传性,GNAS 基因的体细胞变异是导致 CFD 的主要致病基因。与传统的 CFD 分子遗传学诊断方法相比,WES 更为可行和有效,但受样本类型的限制。
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
Current Eye Research
Current Eye Research 医学-眼科学
CiteScore
4.60
自引率
0.00%
发文量
163
审稿时长
12 months
期刊介绍: The principal aim of Current Eye Research is to provide rapid publication of full papers, short communications and mini-reviews, all high quality. Current Eye Research publishes articles encompassing all the areas of eye research. Subject areas include the following: clinical research, anatomy, physiology, biophysics, biochemistry, pharmacology, developmental biology, microbiology and immunology.
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