小细胞肺癌中两种依托泊苷给药方案的随机试验：药代动力学对疗效和毒性的影响。

A randomized trial of two etoposide schedules in small-cell lung cancer: the influence of pharmacokinetics on efficacy and toxicity.

作者信息

Clark P I, Slevin M L, Joel S P, Osborne R J, Talbot D I, Johnson P W, Reznek R, Masud T, Gregory W, Wrigley P F

机构信息

Medical Oncology Department, St Bartholomew's Hospital, London, United Kingdom.

出版信息

J Clin Oncol. 1994 Jul;12(7):1427-35. doi: 10.1200/JCO.1994.12.7.1427.

DOI:10.1200/JCO.1994.12.7.1427

PMID:8021734

Abstract

PURPOSE

Etoposide is a schedule-dependent drug, as demonstrated by the superiority of 5 consecutive daily infusions over a continuous 24-hour infusion in patients with small-cell lung cancer. A randomized trial has therefore been conducted to compare an extended 8-day regimen with the 5-day schedule.

PATIENTS AND METHODS

Ninety-four patients with small-cell lung cancer (35 limited disease, 59 extensive disease) were randomized to receive single-agent etoposide 500 mg/m2, either as 5 daily 2-hour infusions of 100 mg/m2 or as 8 daily 75-minute infusions of 62.5 mg/m2, both repeated every 3 weeks for six cycles. Single-agent carboplatin was administered at relapse in both arms of the study. Patients were stratified at randomization according to extent of disease and Karnofsky performance status (KPS).

RESULTS

The overall response rate was 81% in the 5-day arm and 87% in the 8-day arm, with median survival durations of 7.1 and 9.4 months, respectively (no significant differences). The time over which plasma etoposide exceeded low plasma concentrations was significantly longer in patients who responded compared with patients who did not respond. This was most significant for time at concentrations greater than 1, 1.5, and 2 micrograms/mL. Hematologic toxicity was significantly worse in the 5-day arm of the study (cycle no. 1 nadir neutrophil count, 0.8 x 10(9)/L v 1.7 x 10(9)/L). Stepwise regression analysis found duration of exposure to plasma etoposide greater than 3 micrograms/mL to be predictive of nadir neutrophil count and duration of exposure to plasma etoposide greater than 2 micrograms/mL to be predictive of nadir WBC count.

CONCLUSION

The 5-day and 8-day regimens had equivalent activity in small-cell lung cancer. A pharmacokinetic association between concentrations of etoposide and response and toxicity was found. Antitumor activity was associated with the maintenance of lower levels of etoposide than found to be associated with hematologic toxicity. This supports the hypothesis that the schedule of etoposide administration may affect efficacy and toxicity, and that prolonged exposure to low concentrations of etoposide may improve the therapeutic ratio for this drug.

摘要

目的

依托泊苷是一种给药方案依赖性药物，小细胞肺癌患者连续24小时输注与连续5天每日输注相比，后者疗效更优，即证明了这一点。因此开展了一项随机试验，比较延长至8天的方案与5天方案。

患者与方法

94例小细胞肺癌患者（35例局限性疾病，59例广泛性疾病）被随机分组，接受单药依托泊苷500mg/m²，采用两种方式给药，一种是每日100mg/m²、每次输注2小时、连续5天输注；另一种是每日62.5mg/m²、每次输注75分钟、连续8天输注，均每3周重复一次，共六个周期。研究的两组在复发时均给予单药卡铂。患者在随机分组时根据疾病范围和卡氏评分（KPS）进行分层。

结果

5天方案组的总缓解率为81%，8天方案组为87%，中位生存期分别为7.1个月和9.4个月（无显著差异）。缓解患者血浆依托泊苷超过低血浆浓度的时间明显长于未缓解患者。在浓度大于1、1.5和2μg/mL时，这种差异最为显著。研究的5天方案组血液学毒性明显更严重（第1周期最低点中性粒细胞计数，0.8×10⁹/L对1.7×10⁹/L）。逐步回归分析发现，血浆依托泊苷暴露时间大于3μg/mL可预测最低点中性粒细胞计数，血浆依托泊苷暴露时间大于2μg/mL可预测最低点白细胞计数。