Familial Exudative Vitreoretinopathy‐Like Retinal Findings in Adams‐Oliver Syndrome Type 2

先证者 桑格测序 遗传学 医学 移码突变 外显子组测序 表型 无义突变 突变 胡说 遗传异质性 生物 错义突变 基因
作者
You Wang,Aohan Hou,Wenjia Yan,Jinglin Lu,Qiong Wang,Limei Chen,Xiaoyan Ding
出处
期刊:Clinical and Experimental Ophthalmology [Wiley]
卷期号:53 (9): 1181-1190
标识
DOI:10.1111/ceo.14594
摘要

ABSTRACT Background This study investigated the clinical characteristics and the genotype–phenotype correlation of DOCK6 ‐associated autosomal recessive Adams‐Oliver Syndrome in a large cohort of familial exudative vitreoretinopathy patients. Methods Comprehensive ocular examinations were conducted on probands and their family members. Whole‐exome sequencing (WES) was performed on the probands, with Sanger sequencing validation for family members. In vitro experiments validated copy number variation (CNV) and splice‐site mutations. Results A total of 642 families with FEVR phenotypes were included, leading to the identification of seven probands with biallelic pathogenic DOCK6 mutations, corresponding to a prevalence of 1.09%. Thirteen mutation sites were identified, including seven frameshift mutations, four splice mutations, one CNV, and one nonsense mutation, indicating the pathogenic mechanism of DOCK6 in FEVR is more likely due to functional loss. Among the 14 eyes of the seven probands, five eyes (35.71%) and four eyes (28.57%) exhibited total retinal detachment and retinal folds, respectively. Conclusions Biallelic DOCK6 mutations represent a genetic cause of FEVR. These pathogenic mutations typically result in loss of function, leading to severe ocular and systemic manifestations. These findings highlight the importance of considering DOCK6 mutations in patients presenting with atypical or severe FEVR phenotypes.
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