FOXC1基因新突变致Axenfeld-Rieger综合征伴脑白质病变和皮肤淀粉样变

doi:10.13281/j.cnki.issn.1004-4469.2024.03.005

眼科 ›› 2024, Vol. 33 ›› Issue (3): 187-192.doi: 10.13281/j.cnki.issn.1004-4469.2024.03.005

FOXC1基因新突变致Axenfeld-Rieger综合征伴脑白质病变和皮肤淀粉样变

贾红艳彭楚芝张冉冉焦永红王涛

首都医科大学附属北京同仁医院北京同仁眼科中心眼科学与视觉科学北京市重点实验室，北京100730

收稿日期:2024-05-08 出版日期:2024-05-24 发布日期:2024-05-24
通讯作者: 王涛，Email：stevenwa@126.com

Axenfeld-Rieger syndrome with leukoencephalopathy and cutaneous amyloidosis caused by a novel mutation in the FOXC1 gene in a pedigree

Jia Hongyan, Peng Chuzhi, Zhang Ranran, Jiao Yonghong, Wang Tao

Beijing Tongren Eye Center, Beijing Tongren Hospital, Capital Medical University; Beijing Key Laboraorty Ophthalmology and Visual Sciences, Beijing 100730, China

Received:2024-05-08 Online:2024-05-24 Published:2024-05-24
Contact: Wang Tao, Email: stevenwa@126.com

摘要/Abstract

摘要： 目的分析Axenfeld-Rieger综合征（ARS）一家系的临床及遗传学特征。设计家系调查研究。研究对象 北京同仁医院Axenfeld-Rieger综合征一家系3人。方法对家系成员进行详细眼科检查及全身检查。采集受检者外周静脉血，提取DNA，对先证者进行全外显子组测序（WES），对筛选出的可疑致病基因突变进行Sanger测序验证以及家系共分离验证。主要指标 眼部检查结果、全身体格检查结果、突变基因型、颅脑MRI。结果收集先证者及其父母3个样本。先证者表现为双眼前节发育异常、左眼球震颤、左眼斜视、左眼青光眼、左眼高度近视眼底表现和左眼后巩膜葡萄肿。全身检查提示左耳混合性耳聋、轻度主动脉瓣关闭不全、皮肤淀粉样变。颅脑MRI提示双侧多发脑白质病变。先证者同时还具有内眦距增宽、鼻根宽而扁平等颅面特征。先证者父亲具有与先证者相似的眼前节表现和全身异常。基因检测及生物信息学分析结果提示先证者及其父亲均存在FOXC1基因未报道的新插入变异NM_001453: c.1043_1044insGGCGCTC, p.(Tyr353fs)(chr6:1611723T> TGGCGCTC,hg19)，GWAS、1000g、ESP、GnomeAD、ExAC、HGMD数据库中均未收录该变异，ACMG (美国医学遗传学与基因组学学会)遗传变异分类标准与指南评估该变异位点为致病变异，该变异推测会导致截短蛋白的产生。正常表型家系成员未检测到该变异，符合家系遗传共分离。结论FOXC1基因新的插入突变c.1043_1044insGGCGCTC(p.Tyr353fs)是该家系疾病表型的致病原因。同时，这也是ARS患者首次报道合并脑白质病变和皮肤淀粉样变的表型，拓宽了该疾病的基因型和表型谱。（眼科，2024, 33：187-192）

关键词: , Axenfeld-Rieger综合征；FOXC1基因

Abstract: Objective To analyze the clinical and genetic characteristics of a family with Axenfeld-Rieger syndrome (ARS). Design Pedigree investigation. Participants Three subjects from a family with ARS were admitted to Beijing Tongren Hospital. Methods Detailed ophthalmic examination and general examination were performed for family members. Peripheral venous blood was collected and DNA was extracted. Whole exome sequencing (WES) was performed on the proband, and Sanger sequencing and family co-segregation were used to validate disease-causing mutation. Main Outcome Measures Ocular examination results, physical examination results, genotype, craniocerebral MRI. Results Three samples (proband and their parents) were collected in this study. The proband presented bilateral anterior segments dysplasia. Nystagmus, strabismus, glaucoma, fundus manifestations of high myopiaand posterior staphyloma were presented in the proband’s left eye. A general examination suggested mixed deafness in the left ear, mild aortic insufficiency, and cutaneous amyloidosis. Brain MRI showed multiple bilateral leukoencephalopathy. The proband also had craniofacial features such as telecanthus, a high and broad nasal root. The father of the proband had anterior segment manifestations and systemic abnormalities similar to those of the proband. The results of gene testing and bioinformatics analysis indicated that both the proband and his father had an unreported FOXC1 gene insertion mutation NM_001453: c.1043_1044insGGCGCTC, p. (Tyr353fs) (chr6:1611723T> TGGCGCTC, hg19). The variation was not included in GWAS, 1000g, ESP, GnomeAD, ExAC and HGMD databases. According to ACMG guidelines, the variation was pathogenic. The mutation was predicted to lead to the production of a truncated protein. This mutation co-segregated with disease phenotypes and was not detected in unaffected members. Conclusion A novel insertion mutation of FOXC1 gene c.1043_1044insGGCGCTC (p.Tyr353fs) was the cause of ARS in this family. At the same time, this is also the first report of ARS patients with leukoencephalopathy and cutaneous amyloidosis, extending the genotype and phenotype spectrum of the disease. (Ophthalmol CHN, 2024, 33: 187-192)

Key words: Axenfeld-Rieger syndrome, FOXC1 gene

贾红艳彭楚芝张冉冉焦永红王涛 . FOXC1基因新突变致Axenfeld-Rieger综合征伴脑白质病变和皮肤淀粉样变[J]. 眼科, 2024, 33(3): 187-192.

Jia Hongyan, Peng Chuzhi, Zhang Ranran, Jiao Yonghong, Wang Tao. Axenfeld-Rieger syndrome with leukoencephalopathy and cutaneous amyloidosis caused by a novel mutation in the FOXC1 gene in a pedigree[J]. Ophthalmology in China, 2024, 33(3): 187-192.

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FOXC1基因新突变致Axenfeld-Rieger综合征伴脑白质病变和皮肤淀粉样变

Axenfeld-Rieger syndrome with leukoencephalopathy and cutaneous amyloidosis caused by a novel mutation in the FOXC1 gene in a pedigree

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