Korb Christina A, Gerstenberger Eva, Lorenz Katrin, Bell Katharina, Beck Anna, Scheller Yvonne, Beutgen Vanessa M, Wolters Dominik, Grus Franz H
Department of Ophthalmology, University Medical Center, Johannes Gutenberg-University, Langenbeckstrasse 1, 55131 Mainz, Germany.
NHMRC Clinical Trials Centre, University of Sydney, Camperdown, NSW 2050, Australia.
J Clin Med. 2024 Nov 21;13(23):7033. doi: 10.3390/jcm13237033.
Age-related macular degeneration (AMD) is a multifactorial disorder, and there is growing evidence of immunological involvement in its pathogenesis. To address this, we aimed to identify biomarker candidates related to retinal antigens in patients with neovascular AMD treated with ranibizumab and healthy subjects. This study was designed as a prospective, open, parallel-group, interventional, single-center phase IV trial. Fifty subjects with neovascular AMD and twenty healthy volunteers were enrolled. The primary objective was to assess the efficacy of intravitreally (IVT) administered ranibizumab in terms of the change in best-corrected visual acuity in subjects with all subtypes of neovascular AMD and in a subgroup of pretreated AMD subjects. A secondary objective was to assess the efficacy of the same in terms of the change in central retinal thickness (CRT) in the same subjects. Another secondary objective was to identify antibodies against retinal antigens in patients with neovascular AMD treated with ranibizumab and healthy subjects. The last secondary objective was to correlate functional and structural parameters with the identified biomarker candidates to differentiate between initial and deferred responders to IVT administered ranibizumab. Serum was analyzed using customized antigen microarrays containing 58 antigens. After 12 weeks of ranibizumab treatment, treated patients gained 4.02 letters on average. The central retinal thickness (CRT) measured in the complete AMD study population was significantly ( < 0.001) decreased at Week 24 compared to the baseline measurement, and the mean CRT dropped from 393.4 to 296.8 µm. A significant increase in the following autoantibodies was detected between the control group and AMD group at Week 24, as well as in the AMD group between baseline and Week 24: antibodies targeting the proteins serotransferrin, opioid growth factor receptor, 60 kDa chaperonin 2, neurotrophin-4, dermcidin, clusterin and vascular endothelial growth factor. The present trial was able to confirm the efficacy of ranibizumab treatment in neovascular AMD, and treatment-naïve patients benefitted the most. Up- and downregulations of antibodies were observed over the course of treatment with ranibizumab. Some antibodies seemed to have a fair correlation with the classification of initial and deferred responders.
年龄相关性黄斑变性(AMD)是一种多因素疾病,越来越多的证据表明免疫因素参与其发病机制。为了对此进行研究,我们旨在确定接受雷珠单抗治疗的新生血管性AMD患者和健康受试者中与视网膜抗原相关的生物标志物候选物。本研究设计为一项前瞻性、开放性、平行组、干预性、单中心IV期试验。招募了50名新生血管性AMD患者和20名健康志愿者。主要目的是评估玻璃体内(IVT)注射雷珠单抗对所有亚型新生血管性AMD患者以及预处理AMD患者亚组最佳矫正视力变化的疗效。次要目的是评估其对同一受试者视网膜中央厚度(CRT)变化的疗效。另一个次要目的是确定接受雷珠单抗治疗的新生血管性AMD患者和健康受试者中针对视网膜抗原的抗体。最后一个次要目的是将功能和结构参数与已确定的生物标志物候选物相关联,以区分IVT注射雷珠单抗的初始反应者和延迟反应者。使用包含58种抗原的定制抗原微阵列分析血清。雷珠单抗治疗12周后,接受治疗的患者平均视力提高了4.02个字母。在整个AMD研究人群中测量的视网膜中央厚度(CRT)在第24周时与基线测量相比显著降低(<0.001),平均CRT从393.4μm降至296.8μm。在第24周时,对照组和AMD组之间以及AMD组基线和第24周之间检测到以下自身抗体显著增加:针对血清转铁蛋白、阿片样生长因子受体、60 kDa伴侣蛋白2、神经营养因子-4、皮肤杀菌素、簇集素和血管内皮生长因子的抗体。本试验能够证实雷珠单抗治疗新生血管性AMD 的疗效,且未接受过治疗的患者受益最大。在雷珠单抗治疗过程中观察到抗体的上调和下调。一些抗体似乎与初始反应者和延迟反应者的分类有一定相关性。
