Detailed structural abnormalities associated with a novel VCAN variant in a family with versican vitreoretinopathy.

IF 1 4区医学 Q4 GENETICS & HEREDITY

Ophthalmic Genetics Pub Date : 2025-08-01 Epub Date: 2025-03-26 DOI:10.1080/13816810.2025.2483421

Anny Zhong, Alexander Sumaroka, Jonathan C Tsui, Erin C O'Neil, Artur V Cideciyan, Emily Datz, Emma C Bedoukian, Tomas S Aleman, Drew Scoles

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引用次数: 0

Abstract

Purpose: To understand the retina micropathology in a family with a novel variant in VCAN.

Methods: Two sisters ages 16 (proband) and 18 years old and their 48-year-old father underwent comprehensive ophthalmic evaluations. Multimodal imaging was performed with spectral domain optical coherence tomography, ultrawide field short-wavelength fundus autofluorescence, and pseudocolor imaging.

Results: Cataracts were present in the sisters along with a penetrant retinal phenotype in all three patients with vitreoretinal ring opacities and traction, peripheral pigmentary clumps, lattice-like features, retinoschisis, foveal ectopia, and nasal displacement of vessels. There were regions with inner retinal thinning with spared outer retina, likely a consequence of vitreoretinal traction, that contrasted with large areas of profound photoreceptor degeneration, but with a rather normal or thickened inner retina. A previously unreported heterozygous variant in intron 7 of VCAN (c.4004-2A>C) segregated with the phenotype in the proband and her father.

Conclusions: Segregation of a versican-associated vitreoretinopathy supports the pathogenicity of the VCAN variant. The patterns of structural abnormalities support classical mechanisms of disease that involve local vitreoretinal traction, as well as possible alternative developmental and/or degenerative changes of the retina, RPE, and/or choroid that result from the primary molecular defect.

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详细的结构异常与一种新的VCAN变异家族与versican玻璃体视网膜病变相关。

目的：了解一个VCAN基因新变异家族的视网膜显微病理学。方法：16岁（先证者）和18岁的两姐妹及其48岁的父亲进行了全面的眼科检查。采用光谱域光学相干层析成像、超宽场短波眼底自体荧光和伪彩色成像进行多模态成像。结果：三名患者的白内障均伴有渗透性视网膜表型，包括玻璃体视网膜环混浊和牵引、周围色素团块、晶格样特征、视网膜裂、中央凹异位和鼻血管移位。有区域内视网膜变薄，外视网膜未受影响，可能是玻璃体视网膜牵引的结果，与大范围的深度光感受器变性形成对比，但与相当正常或增厚的内视网膜形成对比。先前未报道的VCAN内含子7的杂合变异（C .4004- 2a >C）与先证者及其父亲的表型分离。结论：分离的versican相关的玻璃体视网膜病变支持VCAN变异的致病性。结构异常的模式支持疾病的经典机制，包括局部玻璃体视网膜牵拉，以及可能由原发性分子缺陷引起的视网膜、RPE和/或脉络膜的替代发育和/或退行性改变。

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

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.