一项针对整合素 α(v)β(3)的单克隆抗体 etaracizumab(etaracizumab)联合或不联合达卡巴嗪治疗 IV 期转移性黑色素瘤患者的随机 2 期研究。
A randomized phase 2 study of etaracizumab, a monoclonal antibody against integrin alpha(v)beta(3), + or - dacarbazine in patients with stage IV metastatic melanoma.
机构信息
Newcastle Melanoma Unit, Newcastle, Australia.
出版信息
Cancer. 2010 Mar 15;116(6):1526-34. doi: 10.1002/cncr.24821.
BACKGROUND
The alpha (v) beta (3) (alpha(v)beta(3)) integrin is involved in intracellular signaling regulating cell proliferation, migration, and differentiation and is important for tumor-induced angiogenesis.
METHODS
This phase 2, randomized, open-label, 2-arm study was designed to capture safety data and evaluate the antitumor efficacy of etaracizumab (Abegrin), an IgG1 humanized monoclonal antibody against the alpha(v)beta(3) integrin, in patients with previously untreated metastatic melanoma. The objective was to evaluate whether etaracizumab + or - dacarbazine had sufficient clinical activity to warrant further study in a phase 3 clinical trial.
RESULTS
One hundred twelve patients were randomized to receive etaracizumab alone (N = 57) or etaracizumab + dacarbazine (N = 55). Safety of etaracizumab + or - dacarbazine was acceptable with infusion-related, gastrointestinal, and metabolic reactions being the most common adverse events (AEs). The majority of AEs were grade 1 or 2 in severity in both study arms; most events were not considered serious, except for cardiovascular (myocardial infarction, atrial fibrillation) and thromboembolic events, which occurred in 3 and 5 patients, respectively. None of the patients in the etaracizumab-alone study arm and 12.7% of patients in the etaracizumab + dacarbazine study arm achieved an objective response. The median duration of objective response in the etaracizumab + dacarbazine study arm was 4.2 months. Stable disease rate, time to progression (TTP), and progression-free survival (PFS) appeared to be similar between the 2 treatment arms. Stable disease occurred in 45.6% of patients in the etaracizumab-alone study arm and 40.0% of patients in the etaracizumab + dacarbazine study arm. Median TTP and median PFS were both 1.8 months in the etaracizumab-alone study arm and 2.5 and 2.6 months in the etaracizumab + dacarbazine study arm, respectively. Median overall survival was 12.6 months in the etaracizumab-alone study arm and 9.4 months in the etaracizumab + dacarbazine study arm.
CONCLUSIONS
The survival results in both treatment arms of this study were considered unlikely to result in clinically meaningful improvement over dacarbazine alone.
背景
α(v)β(3)(α(v)β(3))整联蛋白参与细胞内信号转导,调节细胞增殖、迁移和分化,对肿瘤诱导的血管生成很重要。
方法
这项 2 期、随机、开放标签、2 臂研究旨在获取安全性数据,并评估 Abegrin(etaracizumab)在未经治疗的转移性黑色素瘤患者中的抗肿瘤疗效。Abegrin 是一种针对α(v)β(3)整联蛋白的 IgG1 人源化单克隆抗体。研究的目的是评估etaracizumab+/-达卡巴嗪是否具有足够的临床活性,以在 3 期临床试验中进一步研究。
结果
112 名患者被随机分配接受etaracizumab 单药治疗(N=57)或etaracizumab+达卡巴嗪治疗(N=55)。etaracizumab+或-dacarbazine 的安全性可接受,输注相关、胃肠道和代谢反应是最常见的不良事件(AE)。在这两个研究臂中,大多数 AE 的严重程度为 1 级或 2 级;大多数事件不被认为是严重的,除了心血管(心肌梗死、心房颤动)和血栓栓塞事件,分别发生在 3 名和 5 名患者中。etaracizumab 单药治疗组无患者和etaracizumab+达卡巴嗪治疗组 12.7%的患者达到客观缓解。etaracizumab+达卡巴嗪治疗组的客观缓解持续时间中位数为 4.2 个月。在这两个治疗臂之间,客观缓解率、无进展生存期(PFS)和疾病进展时间(TTP)似乎相似。在 etaracizumab 单药治疗组中,45.6%的患者出现疾病稳定,在 etaracizumab+达卡巴嗪治疗组中,40.0%的患者出现疾病稳定。在 etaracizumab 单药治疗组中,中位 TTP 和中位 PFS 分别为 1.8 个月,在 etaracizumab+达卡巴嗪治疗组中,分别为 2.5 和 2.6 个月。在 etaracizumab 单药治疗组中,中位总生存期为 12.6 个月,在 etaracizumab+达卡巴嗪治疗组中为 9.4 个月。
结论
本研究两个治疗组的生存结果被认为不太可能导致临床意义上的改善,优于达卡巴嗪单药治疗。
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