Department of Radiation Oncology, University Hospital Zürich, Zürich, Switzerland.
Oncology. 2012;83(1):1-9. doi: 10.1159/000339152. Epub 2012 Jun 8.
Patients with glioblastoma (GBM) inevitably develop recurrent or progressive disease after initial multimodal treatment and have a median survival of 6-9 months from time of progression. To date, there is no accepted standard treatment for GBM relapse or progression. Patupilone (EPO906) is a novel natural microtubule-stabilizing cytotoxic agent that crosses the blood-brain barrier and has been found to have preclinical activity in glioma models.
This is a single-institution, early-phase I/II trial of GBM patients with tumor progression who qualified for second surgery with the goal of evaluating efficacy and safety of the single-agent patupilone (10 mg/m(2), every 3 weeks). Patients received patupilone 1 week prior to second surgery and every 3 weeks thereafter until tumor progression or toxicity. Primary end points were progression-free survival (PFS) and overall survival (OS) at 6 months as well as patupilone concentration in tumor tissue. Secondary end points were toxicity, patupilone concentration in plasma and translational analyses for predictive biomarkers.
Nine patients with a mean age of 54.6 ± 8.6 years were recruited between June 2008 and April 2010. Median survival and 1-year OS after second surgery were 11 months (95% CI, 5-17 months) and 45% (95% CI, 14-76), respectively. Median PFS was 1.5 months (95% CI, 1.3-1.7 months) and PFS6 was 22% (95% CI, 0-46), with 2 patients remaining recurrence-free at 9.75 and 22 months. At the time of surgery, the concentration of patupilone in tumor tissue was 30 times higher than in the plasma. Tumor response was not predictable by the tested biomarkers. Treatment was generally well tolerated with no hematological, but cumulative, though reversible sensory neuropathy grade ≤3 was seen in 2 patients (22%) at 8 months and grade 4 diarrhea in the 2nd patient (11%). Non-patupilone-related peri-operative complications occurred in 2 patients resulting in discontinuation of patupilone therapy. There were no neurocognitive changes 3 months after surgery compared to baseline.
In recurrent GBM, patupilone can be given safely pre- and postoperatively. The drug accumulates in the tumor tissue. The treatment results in long-term PFS in some patients. Patupilone represents a valuable novel compound which deserves further evaluation in combination with radiation therapy in patients with GBM.
胶质母细胞瘤(GBM)患者在初始多模式治疗后不可避免地会出现复发或进展,从进展开始中位生存期为 6-9 个月。迄今为止,GBM 复发或进展尚无公认的标准治疗方法。紫杉醇(EPO906)是一种新型天然微管稳定细胞毒性药物,可穿透血脑屏障,并已在神经胶质瘤模型中发现具有临床前活性。
这是一项针对肿瘤进展后符合二次手术条件的 GBM 患者的单机构、早期 I/II 期试验,目的是评估单药紫杉醇(10mg/m2,每 3 周)的疗效和安全性。患者在二次手术前 1 周接受紫杉醇治疗,此后每 3 周接受一次治疗,直至肿瘤进展或出现毒性。主要终点为 6 个月时的无进展生存期(PFS)和总生存期(OS),以及肿瘤组织中的紫杉醇浓度。次要终点为毒性、血浆中的紫杉醇浓度和预测性生物标志物的转化分析。
2008 年 6 月至 2010 年 4 月期间共招募了 9 名平均年龄为 54.6±8.6 岁的患者。二次手术后中位生存期和 1 年 OS 分别为 11 个月(95%CI,5-17 个月)和 45%(95%CI,14-76)。中位 PFS 为 1.5 个月(95%CI,1.3-1.7 个月),PFS6 为 22%(95%CI,0-46),有 2 名患者在 9.75 和 22 个月时仍无复发。手术时,肿瘤组织中紫杉醇的浓度是血浆中的 30 倍。测试的生物标志物不能预测肿瘤的反应。治疗总体耐受良好,无血液学毒性,但 2 名患者(22%)在 8 个月时出现累积但可逆转的感觉神经病变 3 级,第 2 名患者(11%)出现 4 级腹泻。2 名患者发生与紫杉醇无关的围手术期并发症,导致紫杉醇治疗中断。与基线相比,术后 3 个月无神经认知变化。
在复发性 GBM 中,紫杉醇可在术前和术后安全使用。药物在肿瘤组织中积累。该治疗在一些患者中产生了长期的 PFS。紫杉醇是一种有价值的新型化合物,值得在接受放疗的 GBM 患者中进一步评估。
