Progression of Late-Onset Stargardt Disease

被引:52
作者
Lambertus, Stanley [1 ]
Lindner, Moritz [2 ]
Bax, Nathalie M. [1 ]
Mauschitz, Matthias M. [2 ]
Nadal, Jennifer [3 ]
Schmid, Matthias [3 ]
Schmitz-Valckenberg, Steffen [2 ]
den Hollander, Anneke I. [1 ,4 ]
Weber, Bernhard H. F. [5 ]
Holz, Frank G. [2 ]
van der Wilt, Gert Jan [6 ]
Fleckenstein, Monika [2 ]
Hoyng, Carel B. [1 ]
机构
[1] Radboud Univ Nijmegen, Donders Inst Brain Cognit & Behav, Dept Ophthalmol, Med Ctr, Nijmegen, Netherlands
[2] Univ Bonn, Dept Ophthalmol, Bonn, Germany
[3] Univ Bonn, Inst Med Biometry Informat & Epidemiol, Bonn, Germany
[4] Radboud Univ Nijmegen, Donders Inst Brain Cognit & Behav, Dept Human Genet, Med Ctr, Nijmegen, Netherlands
[5] Univ Regensburg, Inst Human Genet, Regensburg, Germany
[6] Radboud Univ Nijmegen, Donders Inst Brain Cognit & Behav, Med Ctr, Dept Hlth Evidence, Nijmegen, Netherlands
关键词
late-onset Stargardt; fundus autofluorescence; retinal pigment epithelium atrophy; biomarker; disease progression; VISUAL-ACUITY LOSS; MACULAR DEGENERATION; GEOGRAPHIC ATROPHY; FUNDUS AUTOFLUORESCENCE; FLAVIMACULATUS; QUANTIFICATION; PHENOTYPE; GENE;
D O I
10.1167/iovs.16-19833
中图分类号
R77 [眼科学];
学科分类号
100212 ;
摘要
PURPOSE. Identification of sensitive biomarkers is essential to determine potential effects of emerging therapeutic trials for Stargardt disease. This study aimed to describe the natural history of late-onset Stargardt, and demonstrates the accuracy of retinal pigment epithelium (RPE) atrophy progression as an outcome measure. METHODS. We performed a retrospective cohort study collecting multicenter data from 47 patients (91 eyes) with late-onset Stargardt, defined by clinical phenotype, at least one ABCA4 mutation, and age at disease onset >= 45 years. We analyzed RPE atrophy progression on fundus autofluorescence and near-infrared reflectance imaging using semiautomated software and a linear mixed model. We performed sample size calculations to assess the power in a simulated 2-year interventional study and assessed visual endpoints using time-to-event analysis. RESULTS. Over time, progression of RPE atrophy was observed (mean: 0.22 mm/year, 95% confidence interval [CI]: 0.19-0.27). By including only patients with bilateral RPE atrophy in a future trial, 32 patients are needed to reach a power of 83.9% (95% CI: 83.1-84.6), assuming a fixed therapeutic effect size of 30%. We found a median interval between disease onset and visual acuity decline to 20/32, 20/80, and 20/200 of 2.74 (95% CI: 0.54-4.41), 10.15 (95% CI: 6.13-11.38), and 11.38 (95% CI: 6.13-13.34) years, respectively. CONCLUSIONS. We show that RPE atrophy represents a robust biomarker to monitor disease progression in future therapeutic trials. In contrast, the variability in terms of the course of visual acuity was high.
引用
收藏
页码:5186 / 5191
页数:6
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