Genetic testing of ocular manifestations of proliferative syndrome to provide pathophysiology-oriented treatment

Q4 Medicine

Russian Journal of Clinical Ophthalmology Pub Date : 2022-01-01 DOI:10.32364/2311-7729-2022-22-1-16-22

M. Weener, N. A. Bakunina, J. Salmasi, G. V. Poryadin, D. Barh, Y. Kuznetsova, L. Balashova

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引用次数: 2

Abstract

Background: uncontrolled cell proliferation of the ocular blood network is one of the leading causes of blindness and low vision worldwide. We summarize relevant published data and our 5-year experience in searching treatment tools for excessive non-productive proliferation. Aim: to describe genetic patterns in patients with ocular blood network proliferation for predicting disease course and selecting adequate treatment. Patients and Methods: 1210 patients with proliferative ocular disorders, retinopathy of prematurity, and diabetes were enrolled. Patients were divided into three groups: (1) monogenic disorders, (2) proliferative vitreoretinopathy and diabetes mellitus, (3) retinopathy of prematurity. Follow-up was 6 to 36 months. Laboratory, genetic, and relevant clinical tests were pursued in all patients. Results: proprietary approach of bioinformatic analysis of whole exome/whole genome sequencing data allows for specifying the proliferative process’s prognosis and severity given clinical and genetic findings. This approach includes the analysis of gene mutations directly or indirectly involved in angiogenesis and key signaling pathways. The analysis of mutation identified in group 2 revealed 509C>T TGFB1 gene polymorphism in two patients and c.3174G>A IGF1R gene polymorphism in three patients. In group 3, the most common VEGFA gene polymorphisms were +13553C>T, -634G>C, +405G>C (rs2010963), and -460C>T (rs833061). Conclusion: specifying the prognosis of the course and severity of proliferative ocular disorders pathogenically-oriented targeted treatment requires specialized genetic testing using an improved data analysis approach. Keywords: proliferative syndrome, diabetes, retinopathy of prematurity, VEGFA, TGFB1, IGF1R, Stickler syndrome, Wagner syndrome, Wolframe syndrome, Marshall syndrome, Norrie disease, Coats disease, retinoschisis. For citation: Weener M.E., Bakunina N.A., Salmasi J.M. et al. Genetic testing of ocular manifestations of proliferative syndrome to provide pathophysiology-oriented treatment. Russian Journal of Clinical Ophthalmology. 2022;22(1):16–22 (in Russ.). DOI: 10.32364/2311-7729- 2022-22-1-16-22.

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眼部增生性综合征的基因检测为病理生理学导向的治疗提供依据

背景:眼血网细胞不受控制的增殖是全世界失明和低视力的主要原因之一。我们总结了相关的已发表的资料和我们5年来寻找过度非生产性增殖治疗工具的经验。目的:描述眼血网增生患者的遗传模式，以预测病程和选择适当的治疗方法。患者和方法:纳入1210例患有增生性眼疾、早产儿视网膜病变和糖尿病的患者。患者分为三组:(1)单基因疾病，(2)增生性玻璃体视网膜病变和糖尿病，(3)早产儿视网膜病变。随访6 ~ 36个月。对所有患者进行实验室、基因和相关临床检查。结果:全外显子组/全基因组测序数据的专有生物信息学分析方法允许指定增殖过程的预后和严重程度，给出临床和遗传发现。该方法包括分析直接或间接参与血管生成和关键信号通路的基因突变。2组突变分析显示2例患者509C>T TGFB1基因多态性，3例患者c.3174G>A IGF1R基因多态性。在第3组中，最常见的VEGFA基因多态性为+13553C>T、-634G>C、+405G>C (rs2010963)和-460C>T (rs833061)。结论:以病因为导向的靶向治疗增生性眼病的病程和严重程度的预后需要使用改进的数据分析方法进行专门的基因检测。关键词:增生性综合征，糖尿病，早产儿视网膜病变，VEGFA, TGFB1, IGF1R, Stickler综合征，Wagner综合征，Wolframe综合征，Marshall综合征，Norrie病，Coats病，视网膜裂出处:Weener m.e.， Bakunina n.a.， Salmasi J.M.等。眼部增生性综合征的基因检测为病理生理学导向的治疗提供依据。俄罗斯临床眼科杂志，2022;22(1):16-22(俄文)。Doi: 10.32364/2311-7729- 2022-22-1-16-22。

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