Department of Radiation Oncology, Center for Advanced Medicine, Washington University School of Medicine, 4921 Parkview Place, Campus Box #8224, St. Louis, MO, 63110, USA.
Division of Oncology, Department of Medicine, Washington University School of Medicine, St. Louis, USA.
J Neurooncol. 2018 May;138(1):105-111. doi: 10.1007/s11060-018-2775-y. Epub 2018 Jan 27.
Disulfiram has shown promising activity including proteasome inhibitory properties and synergy with temozolomide in preclinical glioblastoma (GBM) models. In a phase I study for newly diagnosed GBM after chemoradiotherapy, we have previously reported our initial dose-escalation results combining disulfiram with adjuvant temozolomide and established the maximum tolerated dose (MTD) as 500 mg per day. Here we report the final results of the phase I study including an additional dose-expansion cohort of disulfiram with concurrent copper. The phase I study consisted of an initial dose-escalation phase of disulfiram 500-1000 mg daily during adjuvant temozolomide, followed by a dose-expansion phase of disulfiram 500 mg daily with copper 2 mg three times daily. Proteasome inhibition was assessed using fluorometric 20S proteasome assay on peripheral blood cell. A total of 18 patients were enrolled: 7 patients received 500 mg disulfiram, 5 patients received 1000 mg disulfiram, and 6 patients received 500 mg disulfiram with copper. Two dose-limiting toxicities occurred with 1000 mg disulfiram. At disulfiram 500 mg with or without copper, only 1 patient (7%) required dose-reduction during the first month of therapy. Addition of copper to disulfiram did not increase toxicity nor proteasome inhibition. The median progression-free survival was 4.5 months (95% CI 0.8-8.2). The median overall survival (OS) was 14.0 months (95% CI 8.3-19.6), and the 2-year OS was 24%. The MTD of disulfiram at 500 mg daily in combination with adjuvant temozolomide was well tolerated by GBM patients, but 1000 mg daily was not. Toxicity and pharmacodynamic effect of disulfiram were similar with or without concurrent copper. The clinical efficacy appeared to be comparable to historical data. Additional clinical trials to combine disulfiram and copper with chemoradiotherapy or to resensitize recurrent GBM to temozolomide are ongoing.
双硫仑在临床前胶质母细胞瘤(GBM)模型中表现出有前景的活性,包括蛋白酶体抑制特性和与替莫唑胺的协同作用。在一项针对放化疗后新诊断的 GBM 的 I 期研究中,我们之前报告了我们联合使用双硫仑和辅助替莫唑胺的初始剂量递增结果,并确定了最大耐受剂量(MTD)为每天 500mg。在这里,我们报告了 I 期研究的最终结果,包括一个额外的双硫仑与铜联合的剂量扩展队列。I 期研究包括一个初始的双硫仑剂量递增阶段,每天 500-1000mg,在辅助替莫唑胺期间,随后是一个双硫仑每天 500mg 与铜 2mg 每日三次的剂量扩展阶段。蛋白酶体抑制作用通过外周血细胞的荧光 20S 蛋白酶体测定来评估。共有 18 名患者入组:7 名患者接受 500mg 双硫仑,5 名患者接受 1000mg 双硫仑,6 名患者接受 500mg 双硫仑与铜。1000mg 双硫仑时出现 2 例剂量限制性毒性。在有或没有铜的情况下,仅 1 名患者(7%)在治疗的第一个月需要减少剂量。双硫仑加铜并未增加毒性或蛋白酶体抑制作用。无进展生存期的中位数为 4.5 个月(95%CI 0.8-8.2)。总生存期(OS)的中位数为 14.0 个月(95%CI 8.3-19.6),2 年 OS 为 24%。每天 500mg 双硫仑联合辅助替莫唑胺的 MTD 被 GBM 患者耐受良好,但每天 1000mg 双硫仑不耐受。双硫仑的毒性和药效学作用与是否同时使用铜相似。临床疗效似乎与历史数据相当。正在进行将双硫仑和铜与放化疗联合使用或使复发性 GBM 对替莫唑胺重新敏感的临床试验。
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