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地图样萎缩中的黄斑敏感性终点:色度和光谱临床试验的探索性分析。

Macular Sensitivity Endpoints in Geographic Atrophy: Exploratory Analysis of Chroma and Spectri Clinical Trials.

作者信息

Chang Dolly S, Callaway Natalia F, Steffen Verena, Csaky Karl, Guymer Robyn H, Birch David G, Patel Praveen J, Ip Michael, Gao Simon S, Briggs Jayla, Honigberg Lee, Lai Phillip, Ferrara Daniela, Sepah Yasir J

机构信息

Genentech, Inc., South San Francisco, California.

Byers Eye Institute, Stanford University School of Medicine, Palo Alto, California.

出版信息

Ophthalmol Sci. 2023 Jun 12;4(1):100351. doi: 10.1016/j.xops.2023.100351. eCollection 2024 Jan-Feb.

Abstract

PURPOSE

To assess different microperimetry (MP) macular sensitivity outcome measures capturing functional deterioration in eyes with geographic atrophy (GA) secondary to age-related macular degeneration (AMD).

DESIGN

Patients were included from 2 identically designed, phase III, double-masked, randomized controlled clinical trials, Chroma (NCT02247479) and Spectri (NCT02247531).

PARTICIPANTS

Patients enrolled were aged ≥ 50 years with bilateral GA and no evidence of previous or active neovascular AMD.

METHODS

Patients were randomized 2:1:2:1 to receive through 96 weeks intravitreal lampalizumab 10 mg every 4 weeks (LQ4W), every 6 weeks (LQ6W), or corresponding sham procedures. For this study, mesopic macular sensitivity of the central 20° was assessed using MP-1 microperimeter at selected sites.

MAIN OUTCOME MEASURES

Two exploratory endpoints were developed, namely perilesional sensitivity (average of points adjacent to absolute scotomatous points) and responding sensitivity (average of all nonscotomatous points; > 0 dB at baseline) by using customized masks for each patient. These were compared with conventional MP endpoints (mean macular sensitivity and number of absolute scotomatous points).

RESULTS

Of 1881 Chroma and Spectri participants, 277 agreed to participate in the present study. Of these, 197 (LQ4W, n = 63; LQ6W, n = 68; pooled sham, n = 66) had reliable MP results. Enlargement of GA lesion area by approximately 2 mm/year across treatment groups was accompanied by deterioration in all MP parameters. There was no difference in worsening of macular sensitivity or absolute scotomatous points among treatment groups. Perilesional and responding sensitivities showed greater decline over time than mean macular sensitivity. Change in GA lesion area at week 48 showed better correlation with perilesional sensitivity (r = -0.17) and responding sensitivity (r = -0.20) than mean macular sensitivity (r = -0.03), while the correlation was highest with the number of absolute scotomatous points (r = 0.37).

CONCLUSIONS

Perilesional or responding macular sensitivity measured by MP should be considered more sensitive endpoints than mean macular sensitivity for monitoring functional decline over time in GA. Although perilesional, responding, and mean macular sensitivity had weak correlation with GA lesion area, the number of absolute scotomatous points may provide additional information on the anatomic/functional correlation.

FINANCIAL DISCLOSURES

Proprietary or commercial disclosure may be found after the references.

摘要

目的

评估不同的微视野检查(MP)黄斑敏感度结果指标,以捕捉年龄相关性黄斑变性(AMD)继发地图样萎缩(GA)患者眼睛的功能恶化情况。

设计

患者来自两项设计相同的III期双盲随机对照临床试验,即色度(Chroma,NCT02247479)试验和光谱(Spectri,NCT02247531)试验。

参与者

纳入的患者年龄≥50岁,患有双侧GA,且无既往或活动性新生血管性AMD的证据。

方法

患者按2:1:2:1随机分组,接受为期96周的玻璃体内注射兰帕利单抗,每4周注射10 mg(LQ4W)、每6周注射10 mg(LQ6W)或相应的假手术。在本研究中,使用MP-1微视野计在选定部位评估中心20°的中视黄斑敏感度。

主要结果指标

制定了两个探索性终点,即使用针对每位患者定制的视标,测量病变周围敏感度(绝对暗点相邻点的平均值)和反应敏感度(所有非暗点的平均值;基线时>0 dB)。将这些指标与传统的MP终点(平均黄斑敏感度和绝对暗点数量)进行比较。

结果

在1881名色度试验和光谱试验参与者中,277人同意参与本研究。其中,197人(LQ4W组,n = 63;LQ6W组,n = 68;合并假手术组,n = 66)获得了可靠的MP结果。各治疗组GA病变面积每年大约扩大2 mm,同时所有MP参数均出现恶化。各治疗组黄斑敏感度恶化或绝对暗点数量方面无差异。病变周围敏感度和反应敏感度随时间的下降幅度大于平均黄斑敏感度。第48周时GA病变面积的变化与病变周围敏感度(r = -0.17)和反应敏感度(r = -0.20)的相关性,高于与平均黄斑敏感度(r = -0.03)的相关性,而与绝对暗点数量的相关性最高(r = 0.37)。

结论

对于监测GA患者随时间的功能下降情况,MP测量的病变周围或反应性黄斑敏感度应被视为比平均黄斑敏感度更敏感的终点指标。尽管病变周围、反应性和平均黄斑敏感度与GA病变面积的相关性较弱,但绝对暗点数量可能提供有关解剖/功能相关性的额外信息。

财务披露

专有或商业披露信息可在参考文献之后找到。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ab60/10587617/3282f044d040/gr1.jpg

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