一种导致索斯比眼底营养不良的新型TIMP-3突变的临床特征:对疾病机制的启示
Clinical features of a novel TIMP-3 mutation causing Sorsby's fundus dystrophy: implications for disease mechanism.
作者信息
Clarke M, Mitchell K W, Goodship J, McDonnell S, Barker M D, Griffiths I D, McKie N
机构信息
Department of Ophthalmology, Royal Victoria Infirmary, Newcastle upon Tyne NE2 4HH, UK.
出版信息
Br J Ophthalmol. 2001 Dec;85(12):1429-31. doi: 10.1136/bjo.85.12.1429.
AIMS
To describe the phenotype in three family members affected by a novel mutation in the gene coding for the enzyme tissue inhibitor of metalloproteinase-3 (TIMP-3).
METHODS
Three members of the same family were seen with a history of nyctalopia and visual loss due to maculopathy. Clinical features were consistent with Sorsby's fundus dystrophy. Exon 5 of the gene coding for TIMP-3 was amplified by the polymerase chain reaction, single strand conformation polymorphism analysis undertaken and exon 5 amplicons were directly sequenced.
RESULTS
Onset of symptoms was in the third to fourth decade. Five of six eyes had geographic macular atrophy rather than neovascularisation as a cause for central visual loss. Peripheral retinal pigmentary disturbances were present. Scotopic ERGs were abnormal in all three. Mutation analysis showed a G-->T transversion in all three resulting in a premature termination codon, E139X, deleting most of the carboxy terminal domain of TIMP-3.
CONCLUSIONS
The patients described had a form of Sorsby's fundus dystrophy which fell at the severe end of the spectrum of this disease. Postulated disease mechanisms include deposition of dimerised TIMP-3 protein.
目的
描述三名受基质金属蛋白酶-3组织抑制剂(TIMP-3)编码基因突变影响的家庭成员的表型。
方法
观察了同一家族的三名成员,他们有夜盲症病史且因黄斑病变导致视力丧失。临床特征与索斯比眼底营养不良一致。通过聚合酶链反应扩增TIMP-3编码基因的第5外显子,进行单链构象多态性分析并直接对第5外显子扩增子进行测序。
结果
症状在第三至第四个十年开始出现。六只眼中有五只出现地图状黄斑萎缩而非新生血管形成,这是导致中心视力丧失的原因。存在周边视网膜色素紊乱。三名患者的暗视视网膜电图均异常。突变分析显示三名患者均存在G→T颠换,导致提前终止密码子E139X,缺失了TIMP-3的大部分羧基末端结构域。
结论
所描述的患者患有索斯比眼底营养不良的一种形式,属于该疾病谱系中严重的一端。推测的疾病机制包括二聚化TIMP-3蛋白的沉积。
Zotero 插件