吡唑吖啶用于难治性癌症儿童和青年成人的I期试验及药代动力学研究。

Phase I trial and pharmacokinetic study of pyrazoloacridine in children and young adults with refractory cancers.

作者信息

Berg S L, Blaney S M, Adamson P C, O'Brien M, Poplack D G, Arndt C, Blatt J, Balis F M

机构信息

Texas Children's Cancer Center, Texas Children's Hospital and Baylor College of Medicine, Houston 77030, USA.

出版信息

J Clin Oncol. 1998 Jan;16(1):181-6. doi: 10.1200/JCO.1998.16.1.181.

DOI:10.1200/JCO.1998.16.1.181

PMID:9440741

Abstract

PURPOSE

To define the maximum-tolerated dose (MTD), quantitative and qualitative toxicities, recommended phase II dose, and pharmacokinetics of pyrazoloacridine (PZA) administered as a 1- or 24-hour infusion in children and young adults with refractory cancers.

PATIENTS AND METHODS

Twenty-two patients received PZA as a 1-hour infusion at doses of 380 mg/m2 (n = 3), 495 mg/m2 (n = 6), 640 mg/m2 (n = 6), and 835 mg/m2 (n = 7). An additional four patients received PZA as a 24-hour infusion at the MTD (640 mg/m2) for the 1-hour infusion schedule. Plasma samples were obtained for pharmacokinetic analysis in 17 patients. PZA concentration in plasma was measured by reverse-phase high-performance liquid chromatography (HPLC). A two-compartment pharmacokinetic model was fit to the PZA plasma concentration data.

RESULTS

On the 1-hour infusion schedule, dose-limiting myelosuppression (neutropenia more than thrombocytopenia) was observed in two of seven patients at the 835-mg/m2 dose level. Myelosuppression did not appear to be ameliorated by prolonging the infusion to 24 hours. Nonhematologic toxicities were minor. Significant neurotoxicity, which was dose-limiting in adults treated with a 1-hour infusion of PZA, was observed in one patient treated at 640 mg/m2, but was not dose-limiting. There was marked interpatient variability in plasma PZA concentrations at all dose levels. The pharmacokinetic profile of PZA was characterized by an initial rapid decline (alpha half-life [t(1/2)alpha], 0.5 hours) followed by a prolonged elimination phase (t(1/2)beta, 30 hours). The volume of distribution at steady-state (Vd(ss)) was 700 L/m2 and the clearance was 300 mL/min/m2. There was no evidence of dose-dependent clearance. The area under the PZA concentration-time curve (AUC) correlated poorly with dose and was more predictive of the degree of myelosuppression than was PZA dose.

CONCLUSION

PZA administered as 1- or 24-hour infusion is well tolerated by children and young adults. The dose-limiting toxicity (DLT) is myelosuppression. Neurotoxicity is not prominent in this age group. There was marked interpatient variation in plasma concentrations of PZA. The recommended dose for phase II studies is 640 mg/m2.

摘要

目的

确定以1小时或24小时输注方式给予难治性癌症儿童和年轻成人的吡唑并吖啶（PZA）的最大耐受剂量（MTD）、定量和定性毒性、推荐的II期剂量以及药代动力学。

患者与方法

22例患者接受PZA 1小时输注，剂量分别为380mg/m²（n = 3）、495mg/m²（n = 6）、640mg/m²（n = 6）和835mg/m²（n = 7）。另外4例患者接受PZA 24小时输注，剂量为1小时输注方案的MTD（640mg/m²）。采集17例患者的血浆样本进行药代动力学分析。采用反相高效液相色谱法（HPLC）测定血浆中PZA浓度。用二室药代动力学模型拟合PZA血浆浓度数据。

结果

在1小时输注方案中，835mg/m²剂量水平的7例患者中有2例出现剂量限制性骨髓抑制（中性粒细胞减少多于血小板减少）。将输注时间延长至24小时似乎并未改善骨髓抑制。非血液学毒性较轻。在1例接受640mg/m²治疗的患者中观察到明显的神经毒性，这在接受1小时输注PZA治疗的成人中是剂量限制性的，但并非剂量限制性。在所有剂量水平下，患者血浆PZA浓度存在显著的个体间差异。PZA的药代动力学特征为初始快速下降（α半衰期[t(1/2)α]，0.5小时），随后是较长的消除期（t(1/2)β，30小时）。稳态分布容积（Vd(ss)）为700L/m²，清除率为300mL/min/m²。没有证据表明存在剂量依赖性清除。PZA浓度-时间曲线下面积（AUC）与剂量的相关性较差，且比PZA剂量更能预测骨髓抑制程度。