Lank Center for Genitourinary Oncology, Department of Medicine, Dana-Farber Cancer Institute and Harvard Medical School, Boston, MA 02215, USA.
BJU Int. 2012 Dec;110(11):1729-35. doi: 10.1111/j.1464-410X.2012.11456.x. Epub 2012 Aug 29.
Study Type--Therapy (cohort) Level of Evidence 2a. What's known on the subject? and What does the study add? Despite expanding treatment options for castration-resistant prostate cancer (CRPC), therapies with long response duration remain intangible due to prostate cancer cells' natural ability to develop iterative resistance. Androgen receptor (AR) signaling has been shown to play a critical role in CRPC and its expression is regulated by the PI3K-Akt pathway. Thus inhibition of AR signalling and PI3K-Akt-mTOR (a downstream mediator of the PI3K-Akt pathway) pathway is a logical combination in CRPC and we report a phase II trial of RAD001 and bicalutamide. Our study is the first clinical trial report of an AR inhibitor of PI3K-Akt-mTOR. The AR pathway and the PI3K-Akt-mTOR pathway are two of the most relevant growth pathway for CRPC. Despite low efficacy results from our trial there will be significant interest in the field for these data (dose, schedule, response, toxicity, trial design) as newer generations of both AR inhibitors and PI3K-Akt-mTOR inhibitors are in development and likely will be tested in combination in CRPC.
• To determine best overall response and duration of response of RAD001, a selective inhibitor of mammalian target of rapamycin, in combination with bicalutamide in castration-resistant prostate cancer (CRPC). • To characterize the toxicity profile of RAD001 in combination with bicalutamide in patients with CRPC.
• A phase II study was conducted to explore the efficacy and tolerability of RAD001 (10 mg daily) in combination with bicalutamide (50 mg daily) in men with progressive CRPC. • The primary endpoint was a composite of prostate-specific antigen (PSA) level and measurable disease response by standard criteria. • This single-stage trial with a sample size of 38 eligible patients provided 90% power to differentiate a response rate of ≥ 40% from a response rate of ≤ 20%, as expected for bicalutamide alone (α= 0.10, power = 0.90).
• In total, 36 men were enrolled, with a median (range) age of 68 (60-72) years and median (range) baseline PSA level of 22.2 (8.4-121.3) ng/mL, and 89% had metastatic disease. • There were 31 (86%) patients had previously used bicalutamide for a median duration of 7.4 months. • There were two patients with a confirmed PSA level decline ≥ 50%. • The median (interquartile range) time to progression was 8.7 (7.9-15.9) weeks. • The most common toxicity was grade 1/2 mucositis, which was observed in 20 (56%) patients.
• The combination of RAD001 and bicalutamide in men with CRPC was well tolerated but had low activity and failed to achieve the primary endpoint of improved response compared to the results previously achieved for bicalutamide alone in this population.
研究类型——治疗(队列)证据水平 2a. 目前已知的信息是什么?本研究有何新发现? 尽管针对去势抵抗性前列腺癌(CRPC)的治疗方案不断增多,但由于前列腺癌细胞具有天然的迭代耐药性,因此仍难以实现具有长期缓解作用的疗法。雄激素受体(AR)信号已被证明在 CRPC 中发挥关键作用,其表达受 PI3K-Akt 通路调控。因此,抑制 AR 信号和 PI3K-Akt-mTOR(PI3K-Akt 通路的下游介质)通路是 CRPC 的合理联合治疗方法,我们报告了 RAD001 和比卡鲁胺的 II 期临床试验。我们的研究是首例 AR 抑制剂联合 PI3K-Akt-mTOR 治疗 CRPC 的临床试验报告。AR 通路和 PI3K-Akt-mTOR 通路是与 CRPC 最相关的两种生长通路。尽管我们的试验结果疗效较低,但该研究结果仍将引起该领域的极大关注(剂量、方案、反应、毒性、试验设计),因为新一代 AR 抑制剂和 PI3K-Akt-mTOR 抑制剂正在研发中,并且可能会在 CRPC 中联合测试。
• 确定 RAD001(一种哺乳动物雷帕霉素靶蛋白的选择性抑制剂)联合比卡鲁胺治疗去势抵抗性前列腺癌(CRPC)患者的最佳总缓解率和缓解持续时间。• 描述 RAD001 联合比卡鲁胺治疗 CRPC 患者的毒性特征。
• 进行了一项 II 期研究,以探讨 RAD001(每日 10mg)联合比卡鲁胺(每日 50mg)在进展性 CRPC 男性中的疗效和耐受性。• 主要终点是前列腺特异性抗原(PSA)水平和按标准标准衡量的可测量疾病反应的综合指标。• 这项单阶段试验的样本量为 38 名合格患者,提供了 90%的效力来区分预期比卡鲁胺单独治疗时(α=0.10,效力=0.90)的缓解率≥40%与缓解率≤20%。
• 共纳入 36 名男性,中位(范围)年龄为 68(60-72)岁,中位(范围)基线 PSA 水平为 22.2(8.4-121.3)ng/ml,89%有转移疾病。• 有 31 名(86%)患者曾接受比卡鲁胺治疗,中位治疗时间为 7.4 个月。• 有 2 名患者 PSA 水平下降≥50%。• 中位(四分位距)无进展生存期为 8.7(7.9-15.9)周。• 最常见的毒性是 1/2 级粘膜炎,见于 20 名(56%)患者。
• RAD001 联合比卡鲁胺在 CRPC 男性中具有良好的耐受性,但活性较低,与该人群中比卡鲁胺单独治疗的结果相比,未能达到改善反应的主要终点。
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