Ophthalmic Consultants of Boston, Boston, Massachusetts.
California Retina Consultants, Santa Barbara, California.
Ophthalmol Retina. 2020 Jul;4(7):673-688. doi: 10.1016/j.oret.2020.01.019. Epub 2020 Jan 31.
To assess visual function outcomes to 48 weeks in patients with bilateral geographic atrophy (GA) secondary to age-related macular degeneration included in 2 interventional clinical trials: relationship to baseline lesion size, outcomes by baseline lesion characteristic subgroups, and correlation of visual function outcomes with GA area.
The Chroma and Spectri studies (ClinicalTrials.gov identifiers, NCT02247479 and NCT02247531, respectively) were identically designed phase 3, double-masked, multicenter, randomized, sham injection-controlled clinical trials that evaluated intravitreal lampalizumab in GA.
Eligible patients were 50 years of age or older with well-demarcated bilateral GA (lesion size, 1-7 disc areas) without evidence of or previous treatment for choroidal neovascularization in either eye and best-corrected visual acuity (BCVA) letter score of 49 letters or more (≥1 GA lesion within 250 μm of foveal center if BCVA ≥79 letters).
Patients (pooled n = 1881) were randomized 2:1:2:1 to lampalizumab every 4 weeks, sham every 4 weeks, lampalizumab every 6 weeks, or sham every 6 weeks. Sham arms were pooled for analysis.
Functional end points included change in BCVA from baseline to week 48, low-luminance visual acuity, mesopic microperimetry (number of absolute scotomatous points, mean macular sensitivity), binocular and monocular maximum reading speed, and 2 validated patient-reported outcome measures: Functional Reading Independence Index and 25-item National Eye Institute Visual Function Questionnaire.
Enlargement of GA area, approximately 2 mm/year on average across all treatment groups in each study, was accompanied by overall deterioration in all functional end points. No statistically significant differences were found between lampalizumab or sham arms for changes from baseline in functional assessment scores. Of visual function tests, only microperimetry outcomes were correlated moderately with GA lesion area when assessed cross-sectionally at baseline and week 48.
Chroma and Spectri provide a unique data set of functional end points in GA that are relevant for future clinical trials. Patients with bilateral GA experienced a consistent decline in visual function over 48 weeks, but measures of visual function were not correlated strongly with GA lesion area. It is not possible to predict visual function outcomes from GA lesion size.
评估 2 项干预性临床试验中年龄相关性黄斑变性继发双侧地图状萎缩(GA)患者的 48 周视觉功能结果:与基线病变大小的关系、按基线病变特征亚组的结果以及视觉功能结果与 GA 面积的相关性。
Chroma 和 Spectri 研究(ClinicalTrials.gov 标识符分别为 NCT02247479 和 NCT02247531)为完全相同的设计的 3 期、双盲、多中心、随机、假注射对照临床试验,评估了玻璃体内拉帕珠单抗治疗 GA。
符合条件的患者年龄在 50 岁或以上,具有明确界定的双侧 GA(病变大小为 1-7 个视盘面积),双眼均无脉络膜新生血管或先前治疗的证据,最佳矫正视力(BCVA)字母评分在 49 个字母或以上(如果 BCVA≥79 个字母,距中心凹 250μm 范围内有 1 个 GA 病变)。
患者(共 1881 例)按 2:1:2:1 的比例随机分为拉帕珠单抗每 4 周 1 次、假注射每 4 周 1 次、拉帕珠单抗每 6 周 1 次或假注射每 6 周 1 次。假注射组进行汇总分析。
功能终点包括从基线到第 48 周的 BCVA 变化、低亮度视力、中间光微视力(绝对暗点数量、黄斑平均敏感度)、双眼和单眼最大阅读速度以及 2 项经过验证的患者报告的结果测量:功能性阅读独立性指数和 25 项国家眼科研究所视觉功能问卷。
在每个研究中,所有治疗组的 GA 面积平均每年扩大约 2mm,伴随着所有功能终点的总体恶化。在功能评估评分的变化方面,拉帕珠单抗组或假注射组之间未发现统计学上的显著差异。在视功能测试中,只有微视力结果在基线和第 48 周进行横截面评估时与 GA 病变面积中度相关。
Chroma 和 Spectri 提供了 GA 中功能终点的独特数据集,这对于未来的临床试验具有重要意义。双侧 GA 患者在 48 周内视觉功能持续下降,但视觉功能测量与 GA 病变面积相关性不强。无法根据 GA 病变大小预测视觉功能结果。
