Rosenfeld Philip J, Berger Brian, Reichel Elias, Danis Ronald P, Gress Angie, Ye Li, Magee Mindy, Parham Laura R, McLaughlin Megan M
Bascom Palmer Eye Institute, University of Miami Miller School of Medicine, Miami, Florida.
Retina Research Center, Austin, Texas.
Ophthalmol Retina. 2018 Oct;2(10):1028-1040. doi: 10.1016/j.oret.2018.03.001. Epub 2018 Apr 17.
To investigate the efficacy of intravenous GSK933776, a humanized monoclonal antibody directed against the N-terminal amino acids of amyloid β, for the treatment of geographic atrophy (GA) in age-related macular degeneration (AMD).
Prospective, randomized, placebo-controlled, double-masked, multicenter phase 2 clinical trial.
Patients with GA secondary to AMD, a visual acuity score of at least 35 letters, and GA with a total area of 1.9 to 17 mm were enrolled.
Participants were monitored monthly for 4 months during an observation period to determine the rate of GA enlargement in the study eye. After the observation period, randomization was performed into 1 of 4 treatment arms (GSK933776 at 3, 6, and 15 mg/kg/month and placebo). At each monthly visit over 18 months, participants underwent visual acuity testing under normal luminance and low-luminance conditions. Ocular imaging included color fundus photography, fundus autofluorescence, fluorescein angiography, and spectral-domain OCT.
Enlargement in the area of GA measured from color fundus photographs with reference to fundus autofluorescence images.
A total of 191 participants were randomized into the study, with 139 (73%) fulfilling the efficacy population criteria. Over 18 months, GSK933776 did not reduce the rate of GA enlargement relative to placebo. Overall, there were no consistent meaningful differences relative to placebo in any of the visual function measures. There was a correlation between the low-luminance visual acuity (LLVA) deficit at baseline and the rate of GA enlargement. Genetic variations in complement factor I (CFI) gene did not correlate with GA progression. No ocular serious adverse events considered related to the GSK933776 treatment were identified, and a similar number of nonocular serious adverse events were reported across all treatment groups.
Intravenous amyloid β inhibition with GSK933776 did not slow the rate of GA enlargement compared with placebo, and no clinically meaningful differences relative to placebo were observed in visual function testing over 18 months. The LLVA deficit was associated with faster GA enlargement; however, no correlation was shown between genetic variations in the CFI gene and the rate of GA enlargement.
研究静脉注射GSK933776(一种针对淀粉样β蛋白N端氨基酸的人源化单克隆抗体)治疗年龄相关性黄斑变性(AMD)中地图样萎缩(GA)的疗效。
前瞻性、随机、安慰剂对照、双盲、多中心2期临床试验。
纳入继发于AMD的GA患者,视力评分至少为35个字母,且GA总面积为1.9至17平方毫米。
在观察期内,参与者每月接受监测,为期4个月,以确定研究眼GA扩大的速率。观察期结束后,随机分为4个治疗组之一(GSK933776,剂量分别为3、6和15毫克/千克/月,以及安慰剂)。在18个月的每月随访中,参与者在正常亮度和低亮度条件下接受视力测试。眼部成像包括彩色眼底照相、眼底自发荧光、荧光素血管造影和光谱域光学相干断层扫描(OCT)。
根据彩色眼底照片并参照眼底自发荧光图像测量GA面积的扩大情况。
共有191名参与者被随机纳入研究,其中139名(73%)符合疗效人群标准。在18个月内,与安慰剂相比,GSK933776并未降低GA扩大的速率。总体而言,在任何视觉功能测量指标上,与安慰剂相比均无一致的有意义差异。基线时的低亮度视力(LLVA)缺陷与GA扩大速率之间存在相关性。补体因子I(CFI)基因的遗传变异与GA进展无关。未发现任何被认为与GSK933776治疗相关的眼部严重不良事件,且所有治疗组报告的非眼部严重不良事件数量相似。
与安慰剂相比,静脉注射GSK933776抑制淀粉样β蛋白并未减缓GA扩大的速率,且在18个月的视觉功能测试中,与安慰剂相比未观察到具有临床意义的差异。LLVA缺陷与GA更快扩大相关;然而,CFI基因的遗传变异与GA扩大速率之间未显示出相关性。
