The First Affiliated Hospital of Fujian Medical University.
Medical Technology and Engineering College of Fujian Medical University, Fuzhou.
J Glaucoma. 2023 Jul 1;32(7):e80-e89. doi: 10.1097/IJG.0000000000002209. Epub 2023 Mar 20.
We report 3 novel variants in fibrillin-1 (FBN1) and latent transforming growth factor-β-binding protein 2 (LTBP2) in 3 families with isolated ectopia lentis (EL), which shed new light on the diagnosis and genetic counseling of EL and secondary glaucoma in clinical settings.
To explore the genetic mechanism in 3 families with isolated EL and secondary angle closure glaucoma.
Three Han Chinese families with EL and glaucoma were recruited. All of the participants underwent complete ocular and general physical examinations and DNA samples were extracted from peripheral venous blood and screened for disease-causing variants using whole exome and Sanger sequencing. In silico analyses were performed to predict the structural and functional changes in gene variants and abnormal proteins.
All 3 probands presented with EL and pupillary-blocking glaucoma. Genetic testing showed that all the patients have zonule-related gene mutations, with the proband (II:1), as well as his mother (I:2) and daughters (III:1 and III:2) from family 1 carrying a heterozygous mutation in FBN1 gene (c.6493G>T:p.(V2165L)); the proband (II:1) from family 2 carrying a heterozygous mutation in FBN1 gene (c.2543C>A:p.(T848N)), and the proband (II:1) from family 3 carrying a pair of compound heterozygous mutations in LTBP2 gene (c.4825T>A:p.(C1609S) / c.529T>C:p.(W177R)). No other genetic variants were found to be associated with the phenotypes of patients and other family members in this study. All variants are predicted to affect the structure and function of proteins as risk factors for EL based on bioinformatics analysis.
Four novel mutations were identified in 3 families with EL, suggesting an intimate link between specific mutations in FBN1 and LTBP2 and isolated EL and angle closure glaucoma. Our results expanded the variant spectrum of zonule-related genes and helped explore the underlying molecular pathology of these disorders.
我们报道了 3 个新的纤维连接蛋白 1(FBN1)和潜伏转化生长因子-β结合蛋白 2(LTBP2)变异体,这些变异体存在于 3 个孤立性晶状体异位(EL)的家族中,这为临床环境中 EL 和继发性青光眼的诊断和遗传咨询提供了新的线索。
探讨 3 个孤立性 EL 和继发性闭角型青光眼家系的遗传机制。
收集 3 个汉族 EL 和青光眼家系。所有参与者均接受了全面的眼部和全身检查,并从外周静脉血中提取 DNA 样本,使用全外显子组和 Sanger 测序筛选致病变异。进行了计算机分析,以预测基因变异和异常蛋白的结构和功能变化。
所有 3 个先证者均表现为 EL 和瞳孔阻滞性青光眼。基因检测显示,所有患者均存在悬韧带相关基因突变,家系 1 的先证者(II:1)及其母亲(I:2)和女儿(III:1 和 III:2)携带纤维连接蛋白 1 基因杂合突变(c.6493G>T:p.(V2165L));家系 2 的先证者(II:1)携带纤维连接蛋白 1 基因杂合突变(c.2543C>A:p.(T848N));家系 3 的先证者(II:1)携带 LTBP2 基因一对复合杂合突变(c.4825T>A:p.(C1609S) / c.529T>C:p.(W177R))。在本研究中,没有发现其他遗传变异与患者和其他家庭成员的表型相关。所有变异均基于生物信息学分析预测会影响蛋白质的结构和功能,成为 EL 的风险因素。
在 3 个 EL 家系中发现了 4 个新的突变,提示 FBN1 和 LTBP2 特定突变与孤立性 EL 和闭角型青光眼之间存在密切联系。我们的研究结果扩展了悬韧带相关基因的变异谱,并有助于探讨这些疾病的潜在分子病理学。
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