基于细胞的睫状神经营养因子疗法治疗2型黄斑毛细血管扩张症
Cell-Based Ciliary Neurotrophic Factor Therapy for Macular Telangiectasia Type 2.
作者信息
Chew Emily Y, Gillies Mark, Jaffe Glenn J, Gaudric Alain, Egan Cathy, Constable Ian, Clemons Traci, Aaberg Thomas, Manning Debora C, Hohman Thomas C, Bird Alan, Friedlander Martin
机构信息
Division of Epidemiology and Clinical Applications, National Eye Institute, National Institutes of Health, Bethesda, MD.
Save Sight Institute, University of Sydney, NSW.
出版信息
NEJM Evid. 2025 Aug;4(8):EVIDoa2400481. doi: 10.1056/EVIDoa2400481. Epub 2025 Jul 22.
BACKGROUND
Revakinagene taroretcel (NT-501) is an encapsulated cell therapy producing ciliary neurotrophic factor that slowed retinal degeneration in patients with macular telangiectasia type 2 (MacTel) in phase 2 trials.
METHODS
In NTMT-03-A and NTMT-03-B - identically designed phase 3, multicenter, randomized sham-controlled trials - we evaluated efficacy and safety of NT-501 in MacTel. The primary end point was rate of change in ellipsoid zone area (EZA) (photoreceptor) loss over 24 months (mm/24 months). Secondary outcomes included changes in retinal sensitivity, reading speed, and National Eye Institute Visual Function Questionnaire 25 (NEI VFQ-25) scores (range, 0 to 100; higher scores indicate better function). Safety end points included the proportion of participants experiencing one or more treatment-emergent serious adverse event(s) and loss of 15 or more letters in best-corrected visual acuity (BCVA). Delayed dark adaptation and miosis were among the monitored adverse events.
RESULTS
In NTMT-03-A, adjusted rates of change of EZA loss were 0.075 mm/24 months (95% confidence interval [CI], 0.051 to 0.099) and 0.166 mm/24 months (95% CI, 0.141 to 0.191) in the NT-501 (n=58) and sham (n=57) groups, respectively, with a difference of -0.091 mm/24 months (95% CI, -0.125 to -0.056; P<0.001) between groups. In NTMT-03-B, rates of EZA loss were 0.111 mm/24 months (95% CI, 0.084 to 0.139) and 0.160 mm/24 months (95% CI, 0.131 to 0.189) in the NT-501 (n=59) and sham (n=54) groups, respectively, with a difference of -0.049 mm/24 months (95% CI, -0.089 to -0.008; P=0.02). Retinal sensitivity and reading-speed changes between groups were inconsistent in the trials. NEI VFQ-25 scores, BCVA loss, and treatment-emergent serious adverse events did not differ between treatment groups. Miosis was experienced by 17% and 14% of participants receiving NT-501 in NTMT-03-A and NTMT-03-B, respectively, and by none of the participants in sham groups. Delayed dark adaptation was experienced by 17% and 24% of participants receiving NT-501 in NTMT-03-A and NTMT-03-B, respectively, by none in the NTMT-03-A sham group, and by 2% in the NTMT-03-B sham group.
CONCLUSIONS
NT-501 for MacTel resulted in statistically significantly reduced EZA loss compared with sham procedures. (Funded by Neurotech Pharmaceuticals; ClinicalTrials.gov numbers, NCT03316300 and NCT03319849.).
背景
Revakinagene taroretcel(NT - 501)是一种封装细胞疗法,可产生睫状神经营养因子,在2期试验中减缓了2型黄斑毛细血管扩张症(MacTel)患者的视网膜变性。
方法
在NTMT - 03 - A和NTMT - 03 - B这两项设计相同的3期、多中心、随机假手术对照试验中,我们评估了NT - 501治疗MacTel的疗效和安全性。主要终点是24个月内椭圆体区面积(EZA)(光感受器)损失的变化率(mm/24个月)。次要结局包括视网膜敏感度、阅读速度和美国国立眼科研究所视觉功能问卷25(NEI VFQ - 量表(范围为0至100;分数越高表明功能越好)。安全性终点包括经历一种或多种治疗中出现的严重不良事件的参与者比例,以及最佳矫正视力(BCVA)下降15个或更多字母。延迟暗适应和瞳孔缩小是监测的不良事件之一。
结果
在NTMT - 03 - A中,NT - 501组(n = 58)和假手术组(n = 57)的EZA损失调整变化率分别为0.075 mm/24个月(95%置信区间[CI],0.051至0.099)和0.166 mm/24个月(95% CI,0.141至0.191),两组间差异为 - 0.091 mm/24个月(95% CI, - 0.125至 - 0.056;P < 0.001)。在NTMT - 03 - B中,NT - 501组(n = 59)和假手术组(n = 54)的EZA损失率分别为0.111 mm/24个月(95% CI,0.084至0.139)和0.160 mm/24个月(95% CI,0.131至0.189),两组间差异为 - 0.049 mm/24个月(95% CI, - 0.089至 - 0.008;P = 0.02)。试验中两组间视网膜敏感度和阅读速度变化不一致。治疗组之间的NEI VFQ - 25得分、BCVA损失和治疗中出现的严重不良事件无差异。在NTMT - 03 - A和NTMT - 03 - B中,分别有17%和14%接受NT - 501的参与者出现瞳孔缩小,假手术组参与者均未出现。在NTMT - 03 - A中,17%接受NT - 501的参与者出现延迟暗适应;在NTMT - 03 - B中,24%接受NT - 501的参与者出现延迟暗适应,NTMT - 03 - A假手术组参与者均未出现,NTMT - 03 - B假手术组有2%的参与者出现延迟暗适应。
结论
与假手术相比,用于治疗MacTel的NT - 501在统计学上显著降低了EZA损失。(由Neurotech制药公司资助;ClinicalTrials.gov编号,NCT03316300和NCT03319849。)
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