Department of Ophthalmology, Hospital de São João, Porto, Portugal.
Graefes Arch Clin Exp Ophthalmol. 2011 Feb;249(2):201-8. doi: 10.1007/s00417-010-1482-y. Epub 2010 Aug 20.
Enhanced S-cone syndrome (ESCS) is an autosomal recessive retinal disorder characterized by an increased number of S-cones over L/M cones and rods. Mutations in the NR2E3 gene, encoding a photoreceptor-specific nuclear receptor, are identified in patients with ESCS. The purpose of this study is to report the ophthalmic features of a 25-year-old Portuguese male with a typical ESCS phenotype and a novel homozygous NR2E3 mutation.
The patient underwent a detailed ophthalmic examination including fundus photography, fluorescein angiography (FAF), fundus autofluorescence imaging (FAI), and spectral domain optical coherence tomography (SD-OCT). Full-field electroretinography (ERG), S-cone ERG, and multifocal ERG were performed. Mutation screening of the NR2E3 gene was performed with polymerase chain reaction amplification and direct sequencing.
The patient had poor visual acuity but good color vision. Funduscopy showed degenerative changes from the vascular arcades to the midperipheral retina. The SD-OCT revealed macular schisis and cystoid changes that had no fluorescein leakage. The posterior pole showed diffusely increased autofluorescence compared with eccentric areas in both eyes. International-standard full-field ERG showed the typical pathognomonic changes associated with ESCS and the short-wavelength flash ERG was simplified, delayed, and similar to the standard photopic flash ERG. Multifocal ERG showed widespread delay and reduction. Genetic analysis revealed a novel homozygous mutation (p.C83Y), which resides in the second zinc finger of the DNA-binding domain.
This homozygous mutation is likely to affect binding to target DNA sites, resulting in a non-functional behavior of NR2E3 protein. It is associated with a typical form of ESCS with a nondetectable rod response and reduced/delayed mfERG responses at all eccentricities.
增强型 S- cones 综合征(ESCS)是一种常染色体隐性视网膜疾病,其特征是 S- cones 的数量多于 L/M cones 和 rods。在 ESCS 患者中,已鉴定出编码感光细胞特异性核受体的 NR2E3 基因突变。本研究旨在报告一名 25 岁葡萄牙男性的眼部特征,该男性具有典型的 ESCS 表型和新的纯合 NR2E3 突变。
患者接受了详细的眼科检查,包括眼底照相、荧光素血管造影(FAF)、眼底自发荧光成像(FAI)和谱域光相干断层扫描(SD-OCT)。进行全视野视网膜电图(ERG)、S- cone ERG 和多焦 ERG。使用聚合酶链反应扩增和直接测序对 NR2E3 基因进行突变筛选。
患者视力较差,但色觉良好。眼底检查显示从血管弓到周边视网膜的退行性改变。SD-OCT 显示黄斑裂孔和囊样改变,无荧光素渗漏。后极与偏心区相比,双眼均呈现弥漫性自发荧光增加。国际标准全视野 ERG 显示与 ESCS 相关的典型特征性改变,短波闪烁 ERG 简化、延迟且与标准明视闪光 ERG 相似。多焦 ERG 显示广泛的延迟和减少。基因分析显示一种新的纯合突变(p.C83Y),位于 DNA 结合域的第二个锌指内。
这种纯合突变可能影响与靶 DNA 位点的结合,导致 NR2E3 蛋白的非功能性行为。它与典型的 ESCS 形式相关,表现为 rod 反应不可检测,并且所有偏心度的 mfERG 反应减少/延迟。
