作者
Suzanne Yzer, Gerald A Fishman, Julie Racine, Sana Al-Zuhaibi, Hadi Chakor, Allison Dorfman, Janet Szlyk, Pierre Lachapelle, L Ingeborgh Van Den Born, Rando Allikmets, Irma Lopez, Frans PM Cremers, Robert K Koenekoop
发表日期
2006/9/1
期刊
Investigative ophthalmology & visual science
卷号
47
期号
9
页码范围
3736-3744
出版商
The Association for Research in Vision and Ophthalmology
简介
purpose. To test human CRB1 heterozygotes for possible clinical or functional retinal changes and to evaluate whether a patient with Leber congenital amaurosis (LCA) with CRB1 mutations not consistent with previously described CRB1 phenotypes carried a modifier allele in another LCA gene.
methods. Seven unrelated heterozygous carriers of CRB1 mutations underwent phenotyping by full eye examinations (indirect ophthalmoscopy and slit lamp biomicroscopy) and functional testing (standard full-field electroretinography [ERG] and multifocal ERG). For genotyping of the LCA patients and their parents, denaturing high-performance liquid chromatography (dHPLC) analyses were performed, followed by sequence analysis of CRB1, followed by sequence analysis of the AIPL1 and CRX genes to identify a putative modifier effect in a patient with an atypical CRB1 phenotype.
results. Reduced full-field ERG b-wave amplitudes were observed with scotopic–2 dB flash (140 μV; P< 0.05), normal full-field cone ERGs, and significant regional retinal dysfunction on mfERG in five of seven carriers of CRB1 mutations. A known AIPL1 mutation (p. R302L) was identified as a potential modifier allele in a patient with LCA carrying two CRB1 mutations and with a prominent maculopathy.
conclusions. In human heterozygotes of CRB1 mutations (parents of offspring with LCA), distinctive regional retinal dysfunctions were found by multifocal ERG measurements that were consistent with the focal histologic abnormalities reported for the two CRB1 knockout mice models. This phenotypic finding may identify CRB1 carriers and point to the causal gene defect in …
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