Identification of a novel mutation in KIF11 with functional analysis in a cohort of 516 familial patients with exudative vitreoretinopathy.

IF 1.8 3区 医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular Vision Pub Date : 2021-09-01 eCollection Date: 2021-01-01
Kezhou Wang, Xiang Zhang, Tian Tian, Peiquan Zhao
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Abstract

Purpose: To identify a novel mutation in KIF11 with clinical and functional analysis among 516 familial patients with exudative vitreoretinopathy (FEVR).

Methods: Next-generation sequencing was performed on 516 patients with FEVR between January 2015 and October 2017. Clinical data were collected from patient charts, including sex, age at presentation, visual acuity if available, axial length, stage, and systemic clinical findings. Protein and mRNA levels were detected with western blotting and real-time quantitative PCR, respectively. Mass spectrometry was used to analyze the interacting protein of KIF11.

Results: In total, 304 of 516 patients were identified with at least one mutation in FEVR causative genes. Mutations in KIF11 were identified in 14.47% of all carriers. The novel mutation p. H718L accounted for the greatest proportion (12/44; 27.30%) among all mutations in KIF11. Fundus presentations in these 12 individuals varied from the avascular zone of the peripheral retina to total retinal detachment. The p. H718L mutation can reduce the proliferation of human retinal endothelial cells (HRECs) compared to the wild type. The mRNA level of vascular endothelial growth factor-α, transforming growth factor-α, metalloproteinase-1, and angiopoietin-like 4 were depressed in the KIF11 (p. H718L) groups under hypoxia stimuli. Mass spectrometry results demonstrated that eukaryotic elongation factor 2 (EEF2) was an interacting protein of KIF11 and that the p. H718L mutation can attenuate the binding activity.

Conclusions: Patients with the most frequent KIF11 mutation p. H718L showed typical FEVR presentations in this cohort. The mutation in KIF11 likely plays a role in the proliferation of HRECs, and the p. H718L mutation can reduce the proliferation.

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516例家族性渗出性玻璃体视网膜病变患者的功能分析鉴定了KIF11的一个新突变。
目的:通过临床和功能分析,在516例家族性渗出性玻璃体视网膜病变(FEVR)患者中发现一种新的KIF11突变。方法:对2015年1月至2017年10月期间516例FEVR患者进行新一代测序。临床资料收集自患者病历,包括性别、就诊年龄、视力(如有)、眼轴长度、分期和全身临床表现。分别用western blotting和real-time定量PCR检测蛋白和mRNA水平。质谱法分析KIF11的相互作用蛋白。结果:516例患者中,304例至少有一种出血热致病基因突变。在14.47%的携带者中发现KIF11突变。新型突变p. H718L所占比例最大(12/44;27.30%)。这12例患者的眼底表现从周围视网膜无血管区到视网膜完全脱离不等。与野生型相比,p. H718L突变可以减少人视网膜内皮细胞(HRECs)的增殖。缺氧刺激下KIF11 (p. H718L)组血管内皮生长因子-α、转化生长因子-α、金属蛋白酶-1、血管生成素样4 mRNA表达水平下降。质谱分析结果表明,真核延伸因子2 (eukaryotic伸长factor 2, EEF2)是KIF11的相互作用蛋白,而p. H718L突变可减弱其结合活性。结论:最常见的KIF11突变p. H718L患者在该队列中表现出典型的发热出血热症状。KIF11的突变可能在HRECs的增殖中起作用,而p. H718L突变可以减少增殖。
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来源期刊
Molecular Vision
Molecular Vision 生物-生化与分子生物学
CiteScore
4.40
自引率
0.00%
发文量
25
审稿时长
1 months
期刊介绍: Molecular Vision is a peer-reviewed journal dedicated to the dissemination of research results in molecular biology, cell biology, and the genetics of the visual system (ocular and cortical). Molecular Vision publishes articles presenting original research that has not previously been published and comprehensive articles reviewing the current status of a particular field or topic. Submissions to Molecular Vision are subjected to rigorous peer review. Molecular Vision does NOT publish preprints. For authors, Molecular Vision provides a rapid means of communicating important results. Access to Molecular Vision is free and unrestricted, allowing the widest possible audience for your article. Digital publishing allows you to use color images freely (and without fees). Additionally, you may publish animations, sounds, or other supplementary information that clarifies or supports your article. Each of the authors of an article may also list an electronic mail address (which will be updated upon request) to give interested readers easy access to authors.
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