Wabbels B, Preising M N, Kretschmann U, Demmler A, Lorenz B
Department of Paediatric Ophthalmology, Strabismology and Ophthalmogenetics, University of Regensburg, Klinikum, Franz Josef Strauss Allee 11, 93053 Regensburg, Germany.
Graefes Arch Clin Exp Ophthalmol. 2006 Nov;244(11):1453-66. doi: 10.1007/s00417-006-0286-6. Epub 2006 Apr 13.
Longitudinal course and genotype-phenotype correlation in patients and carriers with heterozygous mutations in hBEST1 (bestrophin).
Thirteen patients and seven possible carriers were characterised by mutation analysis with SSCPA and direct sequencing, clinical examination and fundus autofluorescence (AF). Electrophysiology (EOG and mfERG) and optical coherence tomography (OCT) were additionally performed whenever possible.
We identified seven different heterozygous mutations in ten unrelated families with Best disease. I296del was the most frequent mutation. Five of nine individuals with I295del and two of three with N99K were asymptomatic carriers. One patient with I295del mutation had funduscopically unilateral Best disease. In three children (all with I295del), EOG initially showed a clearly present light peak that deteriorated during 5 years of follow-up in two of them. Increased AF corresponded well to funduscopically visible lesions. During 3-6 years of follow-up, the lesion area did not change significantly, but there were obvious changes in the inner structure of the lesion.
In the present series I295del, the most frequent mutation in our study, and N99K showed reduced penetrance. EOG was normal in young patients even if prime signs were visible. The lesion area did not depend on the mutation and did not correlate with VA. Lower VA was associated with a more irregular AF pattern due to scarring or haemorrhage. Our results indicate a disease causing effect that is cumulative over time.
研究携带hBEST1(视黄醛结合蛋白)杂合突变的患者及携带者的疾病纵向病程及基因型-表型相关性。
通过单链构象多态性分析(SSCPA)和直接测序进行突变分析,同时进行临床检查和眼底自发荧光(AF)检查,对13例患者和7例可能的携带者进行特征分析。尽可能额外进行电生理学检查(眼电图和多焦视网膜电图)和光学相干断层扫描(OCT)。
我们在10个不相关的Best病家族中鉴定出7种不同的杂合突变。I296del是最常见的突变。9例携带I295del突变的个体中有5例以及3例携带N99K突变的个体中有2例为无症状携带者。1例携带I295del突变的患者眼底检查显示为单侧Best病。在3例儿童患者(均为I295del突变)中,眼电图最初显示光峰明显存在,其中2例在5年随访期间光峰恶化。自发荧光增强与眼底可见病变高度吻合。在3至6年的随访期间,病变面积无明显变化,但病变内部结构有明显改变。
在本研究系列中,I295del(我们研究中最常见的突变)和N99K显示出较低的外显率。即使有明显体征,年轻患者的眼电图仍正常。病变面积不取决于突变,且与视力无关。较低的视力与瘢痕或出血导致的自发荧光模式更不规则有关。我们的结果表明疾病致病效应随时间累积。
