Aflibercept Biosimilar MYL-1701P vs Reference Aflibercept in Diabetic Macular Edema: The INSIGHT Randomized Clinical Trial.

IF 7.8 1区医学 Q1 OPHTHALMOLOGY

JAMA ophthalmology Pub Date : 2024-09-12 DOI:10.1001/jamaophthalmol.2024.3458

Susan B Bressler,Abhijit Barve,Prasanna C Ganapathi,Katrin Beckmann,Rajendra S Apte,Dennis M Marcus,Kristine Baumane,Somesh Agarwal,Piotr Oleksy,David A Reichstein,Sunil S Patel,Jan Ernest,Rozsa Dégi,Vishali Gupta,Genichiro Kishino,Motohiro Kamei,Subramanian Loganathan,

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引用次数: 0

Abstract

Importance Biosimilars may be lower-cost alternatives to originator biologic products, potentially offering expanded access or reduced economic burden, but have not been evaluated with aflibercept in diabetic macular edema (DME). Objective To compare efficacy and safety of MYL-1701P, an aflibercept biosimilar, with reference aflibercept (Eylea [Regeneron]) in DME. Design, Setting, and Participants This was a double-masked, randomized clinical trial that included participants at 77 centers across the US, Europe, Japan, and India. Included in the analysis were individuals 18 years and older with type 1 or type 2 diabetes with central DME and best-corrected visual acuity (BCVA) letter score of 73 to 38 in the study eye using an Early Treatment Diabetic Retinopathy Study (ETDRS) chart. Study data were analyzed from October to December 2021. Interventions Formulations of MYL-1701P (0.5-mg vial) or reference aflibercept every 4 weeks for 5 consecutive intravitreal injections, followed by every 8 weeks through week 52. Main Outcomes and Measures The primary outcome was the adjusted difference in least squares mean (SE) change from baseline BCVA letter score at week 8 with an equivalence margin of -3 to +3 letters. Secondary outcomes included change in central subfield thickness (CST), BCVA, number of injections over 52 weeks, incidence of adverse events (AEs), and antidrug antibodies (ADAs). Results A total of 355 participants (mean [SD] age, 62.2 [9.2] years; 216 male [60.8%]) were randomized to MYL-1701P (179 participants [50.4%]) and aflibercept (176 participants [49.6%]). At week 8, mean (SE) change in BCVA was 6.60 (0.55) letters vs 6.56 (0.55) letters in the MYL-1701P vs aflibercept groups. The adjusted mean difference of 0.04 letters (90% CI, -1.16 to 1.24 letters) met the primary outcome. At week 8, mean (SE) change in CST was -112 (7) μm vs -124 (7) μm in the MYL-1701P vs aflibercept groups (adjusted mean difference, 12 μm; 90% CI, -3 to 26 μm). The incidence of treatment-emergent AEs in the MYL-1701P and aflibercept arms were ocular (30.9% [55 of 178] vs 29.5% [52 of 176]), serious ocular (0.6% [1 of 178] vs 1.1% [2 of 176]), nonocular (65.2% [116 of 178] vs 65.3% [115 of 176]), and serious nonocular (16.9% [30 of 178] vs 11.9% [21 of 176]). The mean (SD) total number of injections was 8.4 (2.1) vs 8.7 (1.8) in the MYL-1701P vs aflibercept groups. The incidence of treatment-induced or treatment-boosted ADAs was 2.8% (5 of 177) vs 5.7% (10 of 176) in the MYL-1701P vs aflibercept arms. Conclusions and Relevance MYL-1701P demonstrated clinical equivalence in regard to efficacy, with comparable safety and immunogenicity, to reference aflibercept. These findings support use of MLY-1701P as an alternative to reference aflibercept. Trial Registration ClinicalTrials.gov Identifier: NCT03610646.

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糖尿病黄斑水肿中的阿弗利百普生物类似药 MYL-1701P 与阿弗利百普参考药：INSIGHT 随机临床试验。

重要性生物仿制药可能是原研生物制品的低成本替代品，有可能扩大使用范围或减轻经济负担，但尚未对阿弗利百普治疗糖尿病性黄斑水肿（DME）进行评估。目的比较阿弗利贝西普生物仿制药MYL-1701P与阿弗利贝西普参考药（Eylea [Regeneron]）在DME中的疗效和安全性。分析对象包括18岁及以上、患有中心性DME的1型或2型糖尿病患者，使用早期治疗糖尿病视网膜病变研究（ETDRS）图表对研究眼进行最佳矫正视力（BCVA）字母评分，结果为73至38分。主要结果和测量指标主要结果是第8周时与基线BCVA字母评分的最小二乘法均值（SE）变化的调整差值，等值线为-3到+3个字母。次要结果包括中央子场厚度（CST）变化、BCVA、52周内注射次数、不良事件（AE）发生率和抗药抗体（ADA）。结果共有355名参与者（平均[标码]年龄为62.2[9.2]岁；216名男性[60.8%]）随机接受了MYL-1701P（179名参与者[50.4%]）和aflibercept（176名参与者[49.6%]）治疗。第8周时，MYL-1701P组和aflibercept组BCVA的平均（SE）变化分别为6.60（0.55）个字母和6.56（0.55）个字母。调整后的平均差异为0.04个字母（90% CI，-1.16至1.24个字母），达到了主要结果。第8周时，MYL-1701P组与aflibercept组的CST平均（SE）变化为-112（7）μm，而MYL-1701P组为-124（7）μm（调整后的平均差异为12μm；90% CI为-3至26μm）。MYL-1701P组和aflibercept组的治疗突发AE发生率分别为眼部（30.9% [178例中的55例] vs 29.5% [176例中的52例]）、严重眼部（0.6% [178例中的1例] vs 1.1% [176例中的2例]）、非眼部（65.2% [178例中的116例] vs 65.3% [176例中的115例]）和严重非眼部（16.9% [178例中的30例] vs 11.9% [176例中的21例]）。MYL-1701P组与aflibercept组的平均（标度）总注射次数为8.4（2.1）次 vs 8.7（1.8）次。MYL-1701P组与aflibercept组的治疗诱导或治疗增强型ADA发生率为2.8%（177例中有5例），而MYL-1701P组为5.7%（176例中有10例）。这些研究结果支持使用MLY-1701P替代阿弗利百普：NCT03610646。

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来源期刊

JAMA ophthalmology OPHTHALMOLOGY-

CiteScore

13.20

自引率

3.70%

发文量

340

期刊介绍： JAMA Ophthalmology, with a rich history of continuous publication since 1869, stands as a distinguished international, peer-reviewed journal dedicated to ophthalmology and visual science. In 2019, the journal proudly commemorated 150 years of uninterrupted service to the field. As a member of the esteemed JAMA Network, a consortium renowned for its peer-reviewed general medical and specialty publications, JAMA Ophthalmology upholds the highest standards of excellence in disseminating cutting-edge research and insights. Join us in celebrating our legacy and advancing the frontiers of ophthalmology and visual science.