Krämer F, White K, Pauleikhoff D, Gehrig A, Passmore L, Rivera A, Rudolph G, Kellner U, Andrassi M, Lorenz B, Rohrschneider K, Blankenagel A, Jurklies B, Schilling H, Schütt F, Holz F G, Weber B H
Institut für Humangenetik, Universität Würzburg, Germany.
Eur J Hum Genet. 2000 Apr;8(4):286-92. doi: 10.1038/sj.ejhg.5200447.
Recently, the VMD2 gene has been identified as the causative gene in juvenile-onset vitelliform macular dystrophy (Best disease), a central retinopathy primarily characterised by an impaired function of the retinal pigment epithelium. In this study we have further characterised the spectrum of VMD2 mutations in a series of 41 unrelated Best disease patients. Furthermore we expanded our analysis to include 32 unrelated patients with adult vitelliform macular dystrophy (AVMD) and 200 patients with age-related macular degeneration (AMD). Both AVMD and AMD share some phenotypic features with Best disease such as abnormal subretinal accumulation of lipofuscin material, progressive geographic atrophy and choroidal neovascularisation, and may be the consequence of a common pathogenic mechanism. In total, we have identified 23 distinct disease-associated mutations in Best disease and four different mutations in AVMD. Two of the mutations found in the AVMD patients were also seen in Best disease suggesting a considerable overlap in the aetiology of these two disorders. There were no mutations found in the AMD group. In addition, four frequent intragenic polymorphisms did not reveal allelic association of the VMD2 locus with AMD. These data exclude a direct role of VMD2 in the predisposition to AMD.
最近,VMD2基因已被确定为青少年型卵黄样黄斑营养不良(Best病)的致病基因,这是一种主要以视网膜色素上皮功能受损为特征的中心性视网膜病变。在本研究中,我们进一步对41例无亲缘关系的Best病患者的VMD2突变谱进行了特征分析。此外,我们扩大了分析范围,纳入了32例无亲缘关系的成人卵黄样黄斑营养不良(AVMD)患者和200例年龄相关性黄斑变性(AMD)患者。AVMD和AMD都与Best病有一些共同的表型特征,如脂褐素物质在视网膜下异常积聚、进行性地图状萎缩和脉络膜新生血管形成,可能是共同致病机制的结果。我们总共在Best病中鉴定出23种不同的疾病相关突变,在AVMD中鉴定出4种不同的突变。在AVMD患者中发现的两种突变也见于Best病,这表明这两种疾病的病因有相当大的重叠。在AMD组中未发现突变。此外,4种常见的基因内多态性未显示VMD2基因座与AMD存在等位基因关联。这些数据排除了VMD2在AMD易感性中的直接作用。
