一项关于伊立替康序贯联合氟吡汀的I期临床试验。
A phase I clinical trial of the sequential combination of irinotecan followed by flavopiridol.
作者信息
Shah Manish A, Kortmansky Jeremy, Motwani Monica, Drobnjak Marija, Gonen Mithat, Yi Sandy, Weyerbacher Amanda, Cordon-Cardo Carlos, Lefkowitz Robert, Brenner Baruch, O'Reilly Eileen, Saltz Leonard, Tong William, Kelsen David P, Schwartz Gary K
机构信息
Department of Medicine, Division of Solid Tumor Oncology, Gastrointestinal Oncology Service, Memorial Sloan Kettering Cancer Center, New York, New York, USA.
出版信息
Clin Cancer Res. 2005 May 15;11(10):3836-45. doi: 10.1158/1078-0432.CCR-04-2651.
PURPOSE
Flavopiridol potently enhances the effect of irinotecan with cures in colorectal cancer xenografts, and is associated with modulation of several molecular targets, including p21, Differentiation-related gene 1 (Drg1), and p53. We initiated a phase I trial of the sequential combination of irinotecan followed by flavopiridol to determine the maximal tolerated dose of this combination therapy.
PATIENTS AND METHODS
Forty-five patients with advanced solid tumors were enrolled. Irinotecan was administered first (100 or 125 mg/m(2)) followed 7 hours later by escalating flavopiridol (10-70 mg/m(2)) given weekly over 1 hour for 4 of 6 weeks. At the maximal tolerated dose, the pharmacokinetic analysis was expanded and pre- and posttreatment tumor biopsies were done.
RESULTS
At irinotecan 100 mg/m(2), dose-limiting diarrhea and myelosuppression were observed with flavopiridol 70 mg/m(2). At irinotecan 125 mg/m(2), we observed dose-limiting hyperbilirubinemia, fatigue, and myelosuppression at flavopiridol 60 mg/m(2). Peak flavopiridol concentrations of >/=2 mumol/L were achieved above flavopiridol 50 mg/m(2). No significant pharmacokinetic interactions with irinotecan were noted. Baseline serum bilirubin significantly predicted cycle 1 dose-limiting toxicity and neutropenia. We observed partial responses in three patients and prolonged stable disease (i.e., >6 months) in 36% of patients including adrenocortical cancer and hepatocellular cancer. Patients with wild-type p53 and either no change or low posttreatment biopsy p21 and a decrease in Drg1 expression showed stable or responsive disease to the combination therapy.
CONCLUSIONS
The recommended phase II dose with irinotecan 100 mg/m(2) is flavopiridol 60 mg/m(2) and with irinotecan 125 mg/m(2) is flavopiridol 50 mg/m(2). Toxicity can be predicted by baseline bilirubin. Clinical activity is encouraging and may correlate to changes in p21 and Drg1 levels in patients with wild type p53 tumors following therapy.
目的
黄酮哌啶醇可有效增强伊立替康对结直肠癌异种移植瘤的治疗效果,并与包括p21、分化相关基因1(Drg1)和p53在内的多个分子靶点的调节有关。我们开展了一项伊立替康序贯联合黄酮哌啶醇的I期试验,以确定这种联合治疗的最大耐受剂量。
患者与方法
纳入45例晚期实体瘤患者。先给予伊立替康(100或125mg/m²),7小时后给予递增剂量的黄酮哌啶醇(10 - 70mg/m²),每周1小时,共6周中的4周。在最大耐受剂量时,扩大药代动力学分析并进行治疗前和治疗后的肿瘤活检。
结果
伊立替康剂量为100mg/m²时,黄酮哌啶醇剂量为70mg/m²时观察到剂量限制性腹泻和骨髓抑制。伊立替康剂量为125mg/m²时,黄酮哌啶醇剂量为60mg/m²时观察到剂量限制性高胆红素血症、疲劳和骨髓抑制。黄酮哌啶醇剂量高于50mg/m²时可达到≥2μmol/L的峰值浓度。未发现与伊立替康有显著的药代动力学相互作用。基线血清胆红素显著预测第1周期的剂量限制性毒性和中性粒细胞减少。我们观察到3例患者部分缓解,36%的患者(包括肾上腺皮质癌和肝细胞癌患者)疾病长期稳定(即>6个月)。野生型p53且治疗后活检p21无变化或降低以及Drg1表达降低的患者对联合治疗表现出稳定或反应性疾病。
结论
伊立替康100mg/m²时推荐的II期剂量为黄酮哌啶醇60mg/m²,伊立替康125mg/m²时为黄酮哌啶醇50mg/m²。毒性可通过基线胆红素预测。临床活性令人鼓舞,可能与野生型p53肿瘤患者治疗后p21和Drg1水平的变化相关。
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