Kelly William Kevin, Zhu Andrew X, Scher Howard, Curley Tracey, Fallon Mary, Slovin Susan, Schwartz Lawrence, Larson Steve, Tong William, Hartley-Asp Beryl, Pellizzoni Cinzia, Rocchetti Maurizio
Genitourinary Oncology Service, Division of Solid Tumor, Department of Medicine, Memorial Sloan Kettering Cancer Center, New York, New York 10021, USA.
Clin Cancer Res. 2003 Jun;9(6):2098-107.
The purpose is to determine a safe weekly dose of i.v. estramustine phosphate (EMP) to combine with weekly paclitaxel and monthly carboplatin in patients with advanced prostate cancer.
Patients with advanced prostate cancer (castrate and noncastrate) were administered escalating doses of weekly 1-h infusion of i.v. EMP (500-1000-1500 mg/m(2)) in combination with weekly paclitaxel (100 mg/m(2) over 1 h) and i.v. carboplatin (area under the curve 6 mg/ml-min every 4 weeks). Four weeks of therapy were considered one cycle. In the first three cohorts, EMP was given i.v. 3 h before paclitaxel. Cohorts 4 and 5 reversed the administration order: EMP (doses 1000-1500 mg/m(2)) was given immediately after the end of paclitaxel infusion. Plasma levels of EMP and its metabolites, estramustine and estromustine, were monitored at time 0, at 120 min, and approximately at 20, 21, and 168 h from the start of EMP infusion. Paclitaxel concentrations were determined at basal (0), 30, 60, 90, and 120 min and 18 h after the start of paclitaxel infusion, and a concentration-time curve was estimated. Pharmacokinetic evaluation was performed in cycles 1 and 2 during the first week of therapy.
Nineteen patients were entered on the initial three dose levels (cohorts 1-3). Dose-limiting transient hepatic toxicity was encountered in cohort 3 (EMP = 1500 mg/m(2)). An additional 13 patients were treated with paclitaxel (100 mg/m(2)) first, followed by i.v. EMP at 1000 mg/m(2) (cohort 4), and 1500 mg/m(2) (cohort 5). No dose-limiting toxicities were seen, and cohort 5 was determined safe for Phase II studies. Thromboembolic events were observed in 9% of patients (no prophylactic coumadin was used). Plasma concentrations of EMP and metabolites increased proportionally with dose. In all cohorts, there was a slight decrease in EMP and estramustine plasma concentrations between cycles 1 and 2. Although not significant, higher levels of estromustine at cycle 2 were observed in comparison to cycle 1. Decreased clearance of paclitaxel leading to higher than expected paclitaxel plasma concentrations was observed during the first cycle of therapy. Paclitaxel plasma concentrations were lower during cycle 2. In 17 patients with androgen-independent disease, 59% had >/=50% posttherapy decline in PSA and 22% showed measurable disease regression.
The regimen of weekly i.v. EMP in combination with paclitaxel and carboplatin can be safely administered with hepatic toxicity being transient and reversible. Pharmacokinetic results suggest that EMP competitively inhibits the biotransformation of paclitaxel after the first administration. This effect is counterbalanced, after repeated administrations, by a possible induction of the metabolic system caused by EMP. Phase II testing is ongoing to evaluate the efficacy of this combination.
确定晚期前列腺癌患者静脉注射磷酸雌莫司汀(EMP)的安全周剂量,以便与每周一次的紫杉醇和每月一次的卡铂联合使用。
晚期前列腺癌患者(去势和非去势)接受递增剂量的静脉注射EMP(500 - 1000 - 1500 mg/m²),每周输注1小时,同时联合每周一次的紫杉醇(100 mg/m²,输注1小时)和静脉注射卡铂(曲线下面积6 mg/ml·min,每4周一次)。四周的治疗被视为一个周期。在前三个队列中,EMP在紫杉醇静脉注射前3小时给药。队列4和5颠倒了给药顺序:EMP(剂量1000 - 1500 mg/m²)在紫杉醇输注结束后立即给药。在EMP输注开始后的0、120分钟以及大约20、21和168小时监测EMP及其代谢产物雌莫司汀和雌二醇氮芥的血浆水平。在紫杉醇输注开始后的基础值(0)、30、60、90和120分钟以及18小时测定紫杉醇浓度,并估算浓度 - 时间曲线。在治疗的第一周的第1和第2周期进行药代动力学评估。
19名患者进入最初的三个剂量水平(队列1 - 3)。队列3(EMP = 1500 mg/m²)出现剂量限制性短暂肝毒性。另外13名患者先接受紫杉醇(100 mg/m²)治疗,随后静脉注射1000 mg/m²的EMP(队列4)和1500 mg/m²的EMP(队列5)。未观察到剂量限制性毒性,队列5被确定对II期研究安全。9%的患者观察到血栓栓塞事件(未使用预防性香豆素)。EMP及其代谢产物的血浆浓度随剂量成比例增加。在所有队列中,第1和第2周期之间EMP和雌莫司汀的血浆浓度略有下降。尽管不显著,但与第1周期相比,第2周期观察到更高水平的雌二醇氮芥。在治疗的第一个周期中观察到紫杉醇清除率降低,导致紫杉醇血浆浓度高于预期。第2周期的紫杉醇血浆浓度较低。在17名雄激素非依赖性疾病患者中,59%的患者治疗后PSA下降≥50%,22%的患者显示可测量的疾病消退。
每周静脉注射EMP联合紫杉醇和卡铂的方案可以安全给药,肝毒性是短暂且可逆的。药代动力学结果表明,首次给药后EMP竞争性抑制紫杉醇的生物转化。在重复给药后,这种作用被EMP可能诱导的代谢系统所抵消。正在进行II期试验以评估这种联合用药的疗效。
