马凡综合征和晶状体异位患者的角膜生物力学与FBN1突变有关。
Corneal Biomechanics Are Associated With FBN1 Mutations in Patients With Marfan Syndrome and Ectopia Lentis.
作者信息
Huo Qiu-Yi, Zhang Rui-Zheng, Jia Wan-Nan, Wang Ya-Lei, Shen Xin, Chen Xin-Yao, Chen Tian-Hui, Liu Yan, Song Ling-Hao, Wang Xinyue, Lv Yong, Chen Ze-Xu, Jiang Yong-Xiang
机构信息
Eye Institute and Department of Ophthalmology, Eye & ENT Hospital, Fudan University, Shanghai, China.
NHC Key Laboratory of Myopia (Fudan University), Key Laboratory of Myopia, Chinese Academy of Medical Sciences, Shanghai, China.
出版信息
Invest Ophthalmol Vis Sci. 2025 Mar 3;66(3):23. doi: 10.1167/iovs.66.3.23.
BACKGROUND
We investigated the corneal biomechanical properties and their genotype-phenotype correlation correlations in patients with Marfan syndrome (MFS) and ectopia lentis (EL).
METHODS
Patients with MFS with EL underwent panel-based next-generation sequencing in this retrospective cohort study. The FBN1 genotypes were categorized into the dominant-negative (DN) group and the haploinsufficiency (HI) group. The DN variants were further subclassified based on the affected residues and their locations. Corneal biomechanical parameters were measured using dynamic Scheimpflug-based biomechanical analysis (CorVis ST). The correlations between corneal biomechanical properties and FBN1 genotype or nongenetic factors were analyzed. The differences between patients with MFS and normal control were also evaluated after matching confounding factors.
RESULTS
One hundred one consecutive MFS probands participated in this study, with a median age of 6 years. Patients with HI and DN variants affecting critical residues, namely the DN (-Cys + CaB) variants, exhibited significantly higher deformation amplitude ratios (P = 0.029) and lower stress-strain index values (P = 0.007) compared with those in the DN (others) group, indicating lower corneal stiffness in the former group. DN variants in the FUN-EGF3 region were associated with lower deformation amplitude ratios (P = 0.011) and higher stress-strain index values (P = 0.002), whereas those in the DN-CD region exhibited the opposite pattern. Compromised corneal stiffness was significantly associated with HI and DN (-Cys + CaB) variants (b = -0.184; P = 0.01) and variants located outside the FUN-EGF3 region (b = 0.256; P = 0.001), after adjusting for confounding factors. Compared with matched controls, patients with MFS demonstrated significantly higher deformation amplitude ratios (P = 0.023), further confirming decreased corneal stiffness in this population.
CONCLUSIONS
The FBN1 genotype impacts the corneal biomechanical properties of patients with MFS and EL. Corneal biomechanics provide a novel platform to study the genotype-phenotype correlation of MFS.
背景
我们研究了马凡综合征(MFS)和晶状体异位(EL)患者的角膜生物力学特性及其基因型 - 表型相关性。
方法
在这项回顾性队列研究中,对患有MFS合并EL的患者进行基于面板的下一代测序。FBN1基因型被分为显性负性(DN)组和单倍体不足(HI)组。DN变异体根据受影响的残基及其位置进一步细分。使用基于动态Scheimpflug的生物力学分析(CorVis ST)测量角膜生物力学参数。分析角膜生物力学特性与FBN1基因型或非遗传因素之间的相关性。在匹配混杂因素后,还评估了MFS患者与正常对照之间的差异。
结果
101名连续的MFS先证者参与了本研究,中位年龄为6岁。与DN(其他)组相比,HI和影响关键残基的DN变异体,即DN(-Cys + CaB)变异体,表现出显著更高的变形幅度比(P = 0.029)和更低的应力 - 应变指数值(P = 0.007),表明前一组的角膜硬度较低。FUN - EGF3区域的DN变异体与较低的变形幅度比(P = 0.011)和较高的应力 - 应变指数值(P = 0.002)相关,而DN - CD区域的变异体则表现出相反的模式。在调整混杂因素后,受损的角膜硬度与HI和DN(-Cys + CaB)变异体(b = -0.184;P = 0.01)以及位于FUN - EGF3区域之外的变异体(b = 0.256;P = 0.001)显著相关。与匹配的对照相比,MFS患者表现出显著更高的变形幅度比(P = 0.023),进一步证实了该人群角膜硬度降低。
结论
FBN1基因型影响MFS和EL患者的角膜生物力学特性。角膜生物力学为研究MFS的基因型 - 表型相关性提供了一个新平台。
Zotero 插件