Dharmaraj Sharola, Leroy Bart P, Sohocki Melanie M, Koenekoop Robert K, Perrault Isabelle, Anwar Khalid, Khaliq Shagufta, Devi R Summathi, Birch David G, De Pool Elaine, Izquierdo Natalio, Van Maldergem Lionel, Ismail Mohammad, Payne Annette M, Holder Graham E, Bhattacharya Shomi S, Bird Alan C, Kaplan Josseline, Maumenee Irene H
Johns Hopkins Center for Hereditary Eye Diseases, Wilmer Eye Institute, Johns Hopkins Medical Institutions, Baltimore, MD 21287-9237, USA.
Arch Ophthalmol. 2004 Jul;122(7):1029-37. doi: 10.1001/archopht.122.7.1029.
To describe the phenotype of Leber congenital amaurosis (LCA) in 26 probands with mutations in aryl hydrocarbon receptor interacting protein-like 1 protein (AIPL1) and compare it with phenotypes of other LCA-related genes. To describe the electroretinogram (ERG) in heterozygote carriers.
Patients with AIPL1-related LCA were identified in a cohort of 303 patients with LCA by polymerase chain reaction single-strand confirmational polymorphism mutation screening and/or direct sequencing. Phenotypic characterization included clinical and ERG evaluation. Seven heterozygous carrier parents also underwent ERG testing.
Seventeen homozygotes and 9 compound heterozygotes were identified. The W278X mutation was most frequent (48% of alleles). Visual acuities ranged from light perception to 20/400. Variable retinal appearances, ranging from near normal to varying degrees of chorioretinal atrophy and intraretinal pigment migration, were noted. Atrophic and/or pigmentary macular changes were present in 16 (80%) of 20 probands. Keratoconus and cataracts were identified in 5 (26%) of 19 patients, all of whom were homozygotes. The ERG of a parent heterozygote carrier revealed significantly reduced rod function, while ERGs for 6 other carrier parents were normal.
The phenotype of LCA in patients with AIPL1 mutations is relatively severe, with a maculopathy in most patients and keratoconus and cataract in a large subset. Rod ERG abnormalities may be present in heterozygous carriers of AIPL1 mutations.
Understanding and recognizing the phenotype of LCA may help in defining the course and severity of the disease. Identifying the gene defect is the first step in preparation for therapy since molecular diagnosis in LCA will mandate the choice of treatment.
描述26例芳基烃受体相互作用蛋白样1蛋白(AIPL1)突变的先证者的莱伯先天性黑蒙(LCA)表型,并将其与其他LCA相关基因的表型进行比较。描述杂合子携带者的视网膜电图(ERG)。
通过聚合酶链反应单链构象多态性突变筛查和/或直接测序,在303例LCA患者队列中识别出AIPL1相关LCA患者。表型特征包括临床和ERG评估。7名杂合子携带者父母也接受了ERG检测。
鉴定出17例纯合子和9例复合杂合子。W278X突变最为常见(占等位基因的48%)。视力范围从光感至20/400。观察到视网膜外观各异,从接近正常到不同程度的脉络膜视网膜萎缩和视网膜内色素迁移。20例先证者中有16例(80%)存在萎缩性和/或色素性黄斑改变。19例患者中有5例(26%)发现圆锥角膜和白内障,均为纯合子。1名杂合子携带者父母的ERG显示视杆功能显著降低,而其他6名携带者父母的ERG正常。
AIPL1突变患者的LCA表型相对严重,大多数患者存在黄斑病变,很大一部分患者存在圆锥角膜和白内障。AIPL1突变的杂合子携带者可能存在视杆ERG异常。
了解和认识LCA的表型可能有助于确定疾病的病程和严重程度。识别基因缺陷是治疗准备的第一步,因为LCA的分子诊断将决定治疗方案的选择。
