Yu-Wai-Man Patrick, Newman Nancy J, Biousse Valérie, Carelli Valerio, Moster Mark L, Vignal-Clermont Catherine, Klopstock Thomas, Sadun Alfredo A, Sergott Robert C, Hage Rabih, Degli Esposti Simona, La Morgia Chiara, Priglinger Claudia, Karanja Rustum, Taiel Magali, Sahel José-Alain
Cambridge Centre for Brain Repair and MRC Mitochondrial Biology Unit, Department of Clinical Neurosciences, University of Cambridge, Cambridge, United Kingdom.
Cambridge Eye Unit, Addenbrooke's Hospital, Cambridge University Hospitals, Cambridge, United Kingdom.
JAMA Ophthalmol. 2025 Feb 1;143(2):99-108. doi: 10.1001/jamaophthalmol.2024.5375.
Limited studies have assessed the long-term benefit/risk of gene therapy for Leber hereditary optic neuropathy (LHON).
To determine the safety and efficacy of lenadogene nolparvovec in patients with LHON due to the MT-ND4 gene variant for up to 5 years after administration.
DESIGN, SETTING, AND PARTICIPANTS: The RESCUE and REVERSE Long-Term Follow-up Study (RESTORE), conducted from 2018 to 2022, is the 5-year follow-up study of the 2 phase 3 clinical studies RESCUE (Efficacy Study of Lenadogene Nolparvovec for the Treatment of Vision Loss Up to 6 Months From Onset in LHON Due to the MT-ND4 Mutation) and REVERSE (Efficacy Study of Lenadogene Nolparvovec for the Treatment of Vision Loss From 7 Months to 1 Year From Onset in LHON Due to the MT-ND4 Mutation). At the end of each study, ie, 2 years after gene therapy administration, patients were offered enrollment in the RESTORE trial, a multinational, multicenter, prospective study, for an additional 3 years of follow-up. Patients with LHON due to the MT-ND4 gene variant received lenadogene nolparvovec in 1 eye and a sham injection in the other eye.
Lenadogene nolparvovec was administered as a single intravitreal injection in the RESCUE/REVERSE studies.
Measures included best-corrected visual acuity (BCVA), quality of life using the National Eye Institute visual functioning questionnaire 25 (NEI VFQ-25), and adverse events.
Among the 76 patients who received gene therapy in the RESCUE (n = 39) and REVERSE (n = 37) studies, 72 (94.7%) completed these studies; 62 patients (81.6%) participated in the RESTORE trial, and 55 patients (72.4%) completed the 5-year follow-up. Participants were mostly male (49 [79.0%]) with a mean (SD) age of 35.9 (15.3) years at treatment. At baseline, the mean (SD) BCVA was 1.5 (0.5) logMAR (20/600 Snellen) in eyes to be treated with lenadogene nolparvovec and 1.4 (0.5) logMAR (20/500) in sham eyes. At the end of the RESCUE/REVERSE trials, ie, 2 years after treatment, eyes treated with lenadogene nolparvovec and eyes treated with sham reached a mean BCVA value of 1.4 (0.6) logMAR (20/500). The mean (SD) change from baseline to year 2 was -0.05 (0.6) logMAR (+1 line) and 0.01 (0.6) logMAR (-0 line) in gene therapy-treated and sham eyes, respectively (difference, -0.03; 95% CI, -0.16 to 0.09; P = .60). Five years after treatment, the bilateral improvement from nadir was similar to that observed at 2 years, with a mean (SD) change in BCVA of -0.4 (0.5) logMAR (more than +4 lines) for eyes treated with lenadogene nolparvovec and -0.4 (0.4) logMAR (+4 lines) for eyes treated with sham (difference, -0.05; 95% CI, -0.15 to 0.04; P = .27). An improvement of at least -0.3 logMAR (+3 lines) from the nadir in at least 1 eye was observed in 66.1% of participants (41 of 62). Between 2 and 5 years, intraocular inflammation was noted in 4 participants with 8 events in eyes treated with lenadogene nolparvovec and 1 event in an eye treated with sham.
In this analysis of the RESTORE trial, follow-up of patients with LHON due to the MT-ND4 gene variant unilaterally treated with lenadogene nolparvovec demonstrated a sustained bilateral improvement in BCVA and a good safety profile up to 5 years after treatment. This evidence of persistent benefit over time is promising for the use of gene therapy in these patients.
ClinicalTrials.gov Identifier: NCT03406104.
评估基因疗法对Leber遗传性视神经病变(LHON)的长期益处/风险的研究有限。
确定在给予lenadogene nolparvovec治疗后长达5年的时间里,其对因MT-ND4基因变异导致LHON的患者的安全性和有效性。
设计、地点和参与者:2018年至2022年进行的“拯救与逆转长期随访研究(RESTORE)”,是对两项3期临床研究“拯救(Lenadogene Nolparvovec治疗因MT-ND4突变导致的LHON发病后长达6个月视力丧失的疗效研究)”和“逆转(Lenadogene Nolparvovec治疗因MT-ND4突变导致的LHON发病7个月至1年视力丧失的疗效研究)”的5年随访研究。在每项研究结束时,即基因治疗给药后2年,邀请患者参加RESTORE试验,这是一项跨国、多中心的前瞻性研究,进行额外3年的随访。因MT-ND4基因变异导致LHON的患者一只眼睛接受lenadogene nolparvovec注射,另一只眼睛接受假注射。
在“拯救/逆转”研究中,lenadogene nolparvovec通过单次玻璃体内注射给药。
指标包括最佳矫正视力(BCVA)、使用美国国立眼科研究所视觉功能问卷25(NEI VFQ-25)评估的生活质量以及不良事件。
在“拯救”(n = 39)和“逆转”(n = 37)研究中接受基因治疗的76例患者中,72例(94.7%)完成了这些研究;62例患者(81.6%)参加了RESTORE试验,55例患者(72.4%)完成了5年随访。参与者大多为男性(49例[79.0%]),治疗时的平均(标准差)年龄为35.9(15.3)岁。基线时,拟接受lenadogene nolparvovec治疗的眼睛的平均(标准差)BCVA为1.5(0.5)logMAR(20/600 Snellen视力表),假注射眼睛的平均(标准差)BCVA为1.4(0.5)logMAR(20/500)。在“拯救/逆转”试验结束时,即治疗后2年,接受lenadogene nolparvovec治疗的眼睛和接受假注射的眼睛的平均BCVA值均达到1.4(0.6)logMAR(20/500)。从基线到第2年,基因治疗组和假注射组眼睛的平均(标准差)变化分别为-0.05(0.6)logMAR(提高1行)和0.01(0.6)logMAR(提高0行)(差异为-0.03;95%置信区间为-0.16至0.09;P = 0.60)。治疗5年后,从最低点开始的双眼改善情况与2年时观察到的相似,接受lenadogene nolparvovec治疗的眼睛的BCVA平均(标准差)变化为-0.4(0.5)logMAR(提高超过4行),接受假注射的眼睛的BCVA平均(标准差)变化为-0.4(0.4)logMAR(提高4行)(差异为-0.05;95%置信区间为-0.15至0.04;P = 0.27)。66.1%的参与者(62例中的41例)至少一只眼睛从最低点提高了至少-0.3 logMAR(提高3行)。在2至5年期间,接受lenadogene nolparvovec治疗的眼睛中有4名参与者出现8次眼内炎症事件,接受假注射的眼睛中有1次眼内炎症事件。
在对RESTORE试验的这项分析中,对因MT-ND4基因变异导致LHON且单侧接受lenadogene nolparvovec治疗的患者进行随访,结果显示治疗后长达5年,BCVA持续出现双眼改善,且安全性良好。随着时间推移持续获益的这一证据,为在这些患者中使用基因疗法带来了希望。
ClinicalTrials.gov标识符:NCT03406104。
