Eye Center, Medical Center, Faculty of Medicine, University of Freiburg, Freiburg, Germany.
Genentech, Inc., South San Francisco, CA, USA.
Graefes Arch Clin Exp Ophthalmol. 2024 Nov;262(11):3437-3451. doi: 10.1007/s00417-024-06531-9. Epub 2024 Jun 7.
Intravitreal anti-vascular endothelial growth factor (VEGF) therapy is the standard of care for diabetic macular edema (DME) and neovascular age-related macular degeneration (nAMD); however, vision gains and anatomical improvements are not sustained over longer periods of treatment, suggesting other relevant targets may be needed to optimize treatments. Additionally, frequent intravitreal injections can prove a burden for patients and caregivers. Angiopoietin-2 (Ang-2) has been explored as an additional therapeutic target, due to the involvement of Ang-2 in DME and nAMD pathogenesis. Recent evidence supports the hypothesis that targeting both VEGF and Ang-2 may improve clinical outcomes in DME and nAMD compared with targeting VEGF alone by enhancing vascular stability, resulting in reduced macular leakage, prevention of neovascularization, and diminished inflammation. Faricimab, a novel bispecific antibody that targets VEGF-A and Ang-2, has been evaluated in clinical trials for DME (YOSEMITE/RHINE) and nAMD (TENAYA/LUCERNE). These trials evaluated faricimab against the anti-VEGFA/B and anti-placental growth factor fusion protein aflibercept, both administered by intravitreal injection. In addition to faricimab efficacy, safety, and pharmacokinetics, durability was evaluated during the trials using a treat-and-extend regimen. At 1 year, faricimab demonstrated non-inferior vision gains versus aflibercept across YOSEMITE/RHINE and TENAYA/LUCERNE. In YOSEMITE/RHINE, faricimab improved anatomic parameters versus aflibercept. Reduction of central subfield thickness (CST), and absence of both DME and intraretinal fluid were greater in faricimab- versus aflibercept-treated eyes. In TENAYA/LUCERNE, CST reductions were greater for faricimab than aflibercept at the end of the head-to-head phase (0-12 weeks), and were comparable with aflibercept at year 1, but with less frequent dosing. CST and vision gains were maintained during year 2 of both YOSEMITE/RHINE and TENAYA/LUCERNE. These findings suggest that dual Ang-2/VEGF-A pathway inhibition may result in greater disease control versus anti-VEGF alone, potentially addressing the unmet needs and reducing treatment burden, and improving real-world outcomes and compliance in retinal vascular diseases. Long-term extension studies (RHONE-X, AVONELLE-X) are ongoing. Current evidence suggests that dual inhibition with faricimab heralds the beginning of multitargeted treatment strategies inhibiting multiple, independent components of retinal pathology, with faricimab providing opportunities to reduce treatment burden and improve outcomes compared with anti-VEGF monotherapy.
玻璃体内抗血管内皮生长因子 (VEGF) 治疗是糖尿病性黄斑水肿 (DME) 和新生血管性年龄相关性黄斑变性 (nAMD) 的标准治疗方法;然而,在较长的治疗期间,视力提高和解剖结构改善并不持久,这表明可能需要其他相关靶点来优化治疗。此外,频繁的玻璃体内注射可能会给患者和护理人员带来负担。血管生成素-2 (Ang-2) 已被探索作为另一个治疗靶点,因为 Ang-2 参与了 DME 和 nAMD 的发病机制。最近的证据支持这样一种假设,即通过增强血管稳定性,与单独靶向 VEGF 相比,靶向 VEGF 和 Ang-2 可能会改善 DME 和 nAMD 的临床结果,从而减少黄斑渗漏、预防新生血管形成和减轻炎症。新型双特异性抗体 faricimab 靶向 VEGF-A 和 Ang-2,已在 DME (YOSEMITE/RHINE) 和 nAMD (TENAYA/LUCERNE) 的临床试验中进行了评估。这些试验评估了 faricimab 与抗 VEGF-A/B 和抗胎盘生长因子融合蛋白 aflibercept 的疗效、安全性和药代动力学,两者均通过玻璃体内注射给药。除了 faricimab 的疗效、安全性和药代动力学外,试验还使用治疗和延长方案评估了耐久性。在 1 年时,faricimab 在 YOSEMITE/RHINE 和 TENAYA/LUCERNE 中与 aflibercept 相比,视力提高无差异。在 YOSEMITE/RHINE 中,faricimab 改善了与 aflibercept 相比的解剖学参数。与 aflibercept 治疗的眼睛相比,faricimab 治疗的眼睛中央视网膜下厚度 (CST) 减少,DME 和视网膜内液均不存在。在 TENAYA/LUCERNE 中,faricimab 在头对头阶段 (0-12 周) 的 CST 减少大于 aflibercept,在第 1 年与 aflibercept 相当,但给药频率较低。在 YOSEMITE/RHINE 和 TENAYA/LUCERNE 的第 2 年,CST 和视力提高均保持稳定。这些发现表明,双重 Ang-2/VEGF-A 通路抑制可能会比单独使用抗 VEGF 产生更大的疾病控制效果,可能会满足未满足的需求并减轻治疗负担,并改善视网膜血管疾病的实际结果和依从性。正在进行长期扩展研究 (RHONE-X、AVONELLE-X)。目前的证据表明,faricimab 的双重抑制预示着多靶点治疗策略的开始,该策略抑制视网膜病理学的多个独立成分,与抗 VEGF 单药治疗相比,faricimab 提供了减少治疗负担和改善结果的机会。
