Sierra Eye Associates, Reno, Nevada.
Reno School of Medicine, University of Nevada, Reno.
JAMA Ophthalmol. 2020 Sep 1;138(9):964-972. doi: 10.1001/jamaophthalmol.2020.2699.
Faricimab neutralizes angiopoietin-2 and vascular endothelial growth factor A via both simultaneous and independent binding.
To evaluate extended dosing with faricimab, the first bispecific antibody designed for intraocular use, in patients with neovascular age-related macular degeneration.
DESIGN, SETTING, AND PARTICIPANTS: This phase 2 randomized clinical trial was a 52-week multicenter, active comparator-controlled, parallel-group study. Study participants were enrolled in 25 sites in the US from January and March 2017 with treatment-naive choroidal neovascularization secondary to neovascular age-related macular degeneration and best-corrected visual acuity (BCVA) Early Treatment Diabetic Retinopathy Study letter score of 73 (approximate Snellen equivalent, 20/40) to 24 (approximate Snellen equivalent, 20/320). Analysis began January 2017 and ended March 2018.
Participants were randomized 1:2:2 to receive intravitreal ranibizumab, 0.5 mg, every 4 weeks or faricimab, 6.0 mg, every 12 or 16 weeks. Participants in the faricimab arms initially received 4 monthly injections of faricimab. No rescue injections were allowed. Participants randomized to dosing every 16 weeks were assessed for disease activity at week 24 using prespecified criteria. Those with no active disease continued dosing every 16 weeks through trial end; participants with disease activity continued received dosing every 12 weeks.
Mean change in BCVA from baseline at week 40.
Of 76 participants enrolled (mean [SD] age, 78.5 [8.5] years; age range, 56-94 years; 41 women [58%]; 69 white [97%]), 16 (21.0%) were randomized to ranibizumab every 4 weeks, 29 (38.2%) to faricimab every 12 weeks, and 31 (40.8%) to faricimab every 16 weeks. At week 24, 12 weeks after their last initiation injection, 65% (36 of 55) of all faricimab-treated participants had no disease activity. At week 40, adjusted mean BCVA gains from baseline (Early Treatment Diabetic Retinopathy Study letters) were +11.4 (80% CI, 7.8-15.0), +9.3 (80% CI, 6.4-12.3), and +12.5 (80% CI, 9.9-15.1) for the ranibizumab every 4 weeks, faricimab every 12 weeks, and faricimab every 16 weeks arms, respectively. Participants received a mean (SD) total of 12.9 (0.25), 6.7 (0.91), and 6.2 (0.93) injections, for the ranibizumab every 4 weeks, faricimab every 12 weeks, and faricimab every 16 weeks arms, respectively, through week 52. The secondary BCVA and anatomical imaging end points supported the primary end point and were comparable with ranibizumab every 4 weeks. No new or unexpected safety signals were identified.
At week 52, faricimab dosing every 16 weeks and every 12 weeks resulted in maintenance of initial vision and anatomic improvements comparable with monthly ranibizumab. These results suggest a role for simultaneous neutralization of angiopoietin-2 and vascular endothelial growth factor A in providing sustained efficacy through extended durability, warranting further investigation.
ClinicalTrials.gov Identifier: NCT03038880.
Faricimab 通过同时和独立结合来中和血管生成素-2 和血管内皮生长因子 A。
评估首次用于眼内使用的双特异性抗体 faricimab 的扩展剂量,用于治疗新生血管性年龄相关性黄斑变性。
设计、地点和参与者:这是一项为期 52 周的多中心、活性对照、平行组研究的 2 期随机临床试验。研究参与者于 2017 年 1 月至 3 月从美国的 25 个地点招募,患有新生血管性年龄相关性黄斑变性引起的脉络膜新生血管化,最佳矫正视力(BCVA)早期治疗糖尿病视网膜病变研究字母评分 73(约相当于 Snellen 等效值 20/40)至 24(约相当于 Snellen 等效值 20/320)。分析于 2017 年 1 月开始,于 2018 年 3 月结束。
参与者随机分为 1:2:2 组,分别接受玻璃体腔内雷珠单抗 0.5mg,每 4 周一次,或 faricimab,6.0mg,每 12 周或 16 周一次。faricimab 组的参与者最初接受了 4 次每月的 faricimab 注射。不允许进行救援注射。每 16 周给药组的参与者在第 24 周根据预先指定的标准评估疾病活动情况。没有活动疾病的参与者继续每 16 周给药直至试验结束;有疾病活动的参与者继续每 12 周给药。
第 40 周时与基线相比 BCVA 的平均变化。
76 名入组的参与者(平均[SD]年龄,78.5[8.5]岁;年龄范围,56-94 岁;41 名女性[58%];69 名白人[97%]),16 名(21.0%)被随机分配至雷珠单抗每 4 周组,29 名(38.2%)至 faricimab 每 12 周组,31 名(40.8%)至 faricimab 每 16 周组。在第 24 周,即最后一次起始注射后 12 周,所有接受 faricimab 治疗的参与者中,有 65%(55 名中的 36 名)没有疾病活动。在第 40 周,从基线开始(早期治疗糖尿病视网膜病变研究字母)调整后的平均 BCVA 增益为+11.4(80%CI,7.8-15.0)、+9.3(80%CI,6.4-12.3)和+12.5(80%CI,9.9-15.1),分别为雷珠单抗每 4 周组、faricimab 每 12 周组和 faricimab 每 16 周组。参与者在第 52 周时分别接受了平均(SD)12.9(0.25)、6.7(0.91)和 6.2(0.93)次注射,用于雷珠单抗每 4 周组、faricimab 每 12 周组和 faricimab 每 16 周组。次要的 BCVA 和解剖成像终点支持主要终点,并且与雷珠单抗每 4 周组相当。没有发现新的或意外的安全信号。
在第 52 周时,faricimab 每 16 周和每 12 周给药可维持初始视力和解剖学改善,与每月雷珠单抗相当。这些结果表明,同时中和血管生成素-2 和血管内皮生长因子 A 可通过延长持续时间提供持续的疗效,值得进一步研究。
ClinicalTrials.gov 标识符:NCT03038880。
