A Missense Mutation in OPA1 Causes Dominant Optic Atrophy in a Chinese Family

A Missense Mutation in OPA1 Causes Dominant Optic Atrophy in a Chinese Family

Background. To investigate the genetic causes and clinical characteristics of dominant optic atrophy (DOA) in a Chinese family. Methods. A 5-generation pedigree of 35 family members including 12 individuals affected with DOA was recruited from Shenzhen Eye Hospital, China. Four affected family membe...

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Main Authors: Shaoyi Mei, Xiaosheng Huang, Lin Cheng, Shiming Peng, Tianhui Zhu, Liang Chen, Yan Wang, Jun Zhao
Format: Article
Language:English
Published: Hindawi Limited 2019-01-01
Series:Journal of Ophthalmology
Online Access:http://dx.doi.org/10.1155/2019/1424928
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spelling doaj-d9b1bdf388ed41b5851217e928c88f562020-11-25T02:48:25ZengHindawi LimitedJournal of Ophthalmology2090-004X2090-00582019-01-01201910.1155/2019/14249281424928A Missense Mutation in OPA1 Causes Dominant Optic Atrophy in a Chinese FamilyShaoyi Mei0Xiaosheng Huang1Lin Cheng2Shiming Peng3Tianhui Zhu4Liang Chen5Yan Wang6Jun Zhao7Shenzhen Eye Hospital Affiliated to Jinan University, Shenzhen Eye Institute, Shenzhen, Guangdong 518040, ChinaShenzhen Eye Hospital Affiliated to Jinan University, Shenzhen Eye Institute, Shenzhen, Guangdong 518040, ChinaState Key Laboratory of Ophthalmology, Zhongshan Ophthalmic Center, Sun Yat-sen University, Guangzhou 510060, ChinaShenzhen Eye Hospital Affiliated to Jinan University, Shenzhen Eye Institute, Shenzhen, Guangdong 518040, ChinaShenzhen Eye Hospital Affiliated to Jinan University, Shenzhen Eye Institute, Shenzhen, Guangdong 518040, ChinaShenzhen Eye Hospital Affiliated to Jinan University, Shenzhen Eye Institute, Shenzhen, Guangdong 518040, ChinaShenzhen Eye Hospital Affiliated to Jinan University, Shenzhen Eye Institute, Shenzhen, Guangdong 518040, ChinaShenzhen Eye Hospital Affiliated to Jinan University, Shenzhen Eye Institute, Shenzhen, Guangdong 518040, ChinaBackground. To investigate the genetic causes and clinical characteristics of dominant optic atrophy (DOA) in a Chinese family. Methods. A 5-generation pedigree of 35 family members including 12 individuals affected with DOA was recruited from Shenzhen Eye Hospital, China. Four affected family members and one unaffected family member were selected for whole exome sequencing. Sanger sequencing was used to confirm and screen the identified mutation in 18 members of the family. The disease-causing mutation was identified by bioinformatics analysis and confirmed by segregation analysis. The clinical characteristics of the family members were analyzed. Results. A heterozygous missense mutation (c.1313A>G, p.D438G) in optic atrophy 1 (OPA1) was identified in 10 individuals affected with DOA in this family. None of the unaffected family members had the mutation. Patients in this family had vision loss since they were children or adolescence. The visual acuity decreased progressively to hand movement, except for one patient (IV-12) who had relatively good vision of 20/30 and 20/28. The fundus typically manifested as optic disc pallor. The visual fields, optical coherence tomography, and visual evoked potential suggested variable degree of abnormality in patients. Patients who had a history of cigarette smoking and alcohol drinking had more severe clinical manifestations. Conclusions. Our results suggest that the p.D438G mutation in OPA1 causes optic atrophy in this family. The patients who carried the mutation demonstrated heterogeneous clinical manifestations in this family. This is the first report on the c.1313A>G (p.D438G) mutation of OPA1 in a Chinese family affected with DOA.http://dx.doi.org/10.1155/2019/1424928
collection DOAJ
language English
format Article
sources DOAJ
author Shaoyi Mei
Xiaosheng Huang
Lin Cheng
Shiming Peng
Tianhui Zhu
Liang Chen
Yan Wang
Jun Zhao
spellingShingle Shaoyi Mei
Xiaosheng Huang
Lin Cheng
Shiming Peng
Tianhui Zhu
Liang Chen
Yan Wang
Jun Zhao
A Missense Mutation in OPA1 Causes Dominant Optic Atrophy in a Chinese Family
Journal of Ophthalmology
author_facet Shaoyi Mei
Xiaosheng Huang
Lin Cheng
Shiming Peng
Tianhui Zhu
Liang Chen
Yan Wang
Jun Zhao
author_sort Shaoyi Mei
title A Missense Mutation in OPA1 Causes Dominant Optic Atrophy in a Chinese Family
title_short A Missense Mutation in OPA1 Causes Dominant Optic Atrophy in a Chinese Family
title_full A Missense Mutation in OPA1 Causes Dominant Optic Atrophy in a Chinese Family
title_fullStr A Missense Mutation in OPA1 Causes Dominant Optic Atrophy in a Chinese Family
title_full_unstemmed A Missense Mutation in OPA1 Causes Dominant Optic Atrophy in a Chinese Family
title_sort missense mutation in opa1 causes dominant optic atrophy in a chinese family
publisher Hindawi Limited
series Journal of Ophthalmology
issn 2090-004X
2090-0058
publishDate 2019-01-01
description Background. To investigate the genetic causes and clinical characteristics of dominant optic atrophy (DOA) in a Chinese family. Methods. A 5-generation pedigree of 35 family members including 12 individuals affected with DOA was recruited from Shenzhen Eye Hospital, China. Four affected family members and one unaffected family member were selected for whole exome sequencing. Sanger sequencing was used to confirm and screen the identified mutation in 18 members of the family. The disease-causing mutation was identified by bioinformatics analysis and confirmed by segregation analysis. The clinical characteristics of the family members were analyzed. Results. A heterozygous missense mutation (c.1313A>G, p.D438G) in optic atrophy 1 (OPA1) was identified in 10 individuals affected with DOA in this family. None of the unaffected family members had the mutation. Patients in this family had vision loss since they were children or adolescence. The visual acuity decreased progressively to hand movement, except for one patient (IV-12) who had relatively good vision of 20/30 and 20/28. The fundus typically manifested as optic disc pallor. The visual fields, optical coherence tomography, and visual evoked potential suggested variable degree of abnormality in patients. Patients who had a history of cigarette smoking and alcohol drinking had more severe clinical manifestations. Conclusions. Our results suggest that the p.D438G mutation in OPA1 causes optic atrophy in this family. The patients who carried the mutation demonstrated heterogeneous clinical manifestations in this family. This is the first report on the c.1313A>G (p.D438G) mutation of OPA1 in a Chinese family affected with DOA.
url http://dx.doi.org/10.1155/2019/1424928
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