Department of Medicine, Division of Hematology-Oncology, University of California Los Angeles, CA90095, USA.
Clin Cancer Res. 2012 Jan 15;18(2):336-41. doi: 10.1158/1078-0432.CCR-11-2323. Epub 2011 Dec 5.
During the past 3 decades, the field of clinical research for the treatment of advanced melanoma lacked significant advances. Available drugs had low antitumor activity and no proven benefit in overall survival. Recently, new drugs developed based on an in-depth understanding of the biology of this disease have shown significant benefit, with ipilimumab and vemurafenib having recently shown a positive impact in overall survival in patients with metastatic melanoma leading to approval in this indication by the U.S. Food and Drug Administration. This rapid introduction of new active agents is likely to challenge current notions on how to develop future agents for the treatment of melanoma. The strong evidence of benefit for initial agents that modulate immune regulatory checkpoints or target driver oncogenes has spurred great interest in developing other similarly acting agents. However, this will pose problems in the choice of endpoints for the future definitive clinical trials, and the hurdles for achieving these endpoints will be higher given the similar activity for comparator agents or the availability of competing agents for salvage therapy. This new reality will likely require tailoring registrational clinical trial endpoints to the patient benefits shown in early clinical testing. In this perspective article, we illustrate the challenges in the choice of endpoints for registrational trials in metastatic melanoma and that, with an improved understanding of the agent being developed, the design of the registrational programs can be informed by earlier mechanistic studies to define the assumptions for definitive clinical testing.
在过去的 30 年中,晚期黑色素瘤的临床治疗领域缺乏显著进展。现有的药物抗肿瘤活性低,总生存期无明显获益。最近,基于对该疾病生物学的深入了解而开发的新药显示出显著的获益,依匹单抗和威罗非尼最近在转移性黑色素瘤患者的总生存期方面显示出积极影响,因此被美国食品和药物管理局批准用于该适应证。这种新的有效药物的快速引入可能会挑战目前关于如何开发治疗黑色素瘤的未来药物的观念。最初的调节免疫调节检查点或靶向驱动致癌基因的药物的强有力的获益证据,激发了开发其他具有类似作用的药物的极大兴趣。然而,鉴于比较药物或挽救治疗的竞争药物的相似活性,这将给未来的决定性临床试验选择终点带来问题,并且达到这些终点的障碍将会更高。这种新的现实情况可能需要根据早期临床试验中显示的患者获益来调整注册临床试验的终点。在本文中,我们说明了在转移性黑色素瘤的注册临床试验中选择终点的挑战,并且随着对开发药物的认识的提高,注册计划的设计可以通过早期的机制研究来了解,从而为明确的临床试验提供假设。