Tchekmedyian N S, Egorin M J, Cohen B E, Kaplan R S, Poplin E, Aisner J
Cancer Chemother Pharmacol. 1986;18(1):33-8. doi: 10.1007/BF00253060.
A total of 14 patients, 7 male and 7 female, received in all 21 evaluable courses of cyclophosphamide administered by 5-day continuous infusion. Cyclophosphamide doses were escalated from 300 to 400 mg/m2 per day for 5 days and repeated every 21-28 days. The patient population had a median age of 55 years (range 38-76) and a median Karnofsky performance status of 80 (range 60-100). Only 1 patient had not received prior therapy; 5 patients had received only prior chemotherapy, 1 had received only prior radiotherapy, and 7 had received both. Tumor types were gastric (1), lung (2), colon (4), urethral adenocarcinoma (1), cervical (2), chondrosarcoma (1), melanoma (1), uterine leiomyosarcoma (1), and pancreatic (1). The dose-limiting toxicity was granulocytopenia, with median WBC nadir of 1700/microliter (range 100-4800) in 8 heavily pretreated patients treated at 350 mg/m2 per day for 5 days. One patient without heavy prior treatment received two courses at 400 mg/m2 and had WBC nadirs of 800/microliter and 600/microliter. WBC nadirs occurred between days 9 and 21 (median 14). Drug-induced thrombocytopenia occurred in only one patient (350 mg/m2 per day, nadir 85,000/microliter). Neither hyponatremia nor symptomatic hypo-osmolality was observed. Radiation-induced hemorrhagic cystitis may have been worsened in one patient. Nausea and vomiting were mild. Objective remissions were not observed. The maximum tolerated dose for previously treated patients is 350 mg/m2 per day for 5 days. This dose approximates the doses of cyclophosphamide commonly used with bolus administration. Plasma steady-state concentrations (Css) of cyclophosphamide, measured by gas liquid chromatography, were 2.09-6.79 micrograms/ml. Steady state was achieved in 14.5 +/- 5.9 h (mean +/- SD). After the infusion, cyclophosphamide disappeared from plasma monoexponentially, with a t 1/2 of 5.3 +/- 3.6 h. The area under the curve of plasma cyclophosphamide concentrations versus time (AUC) was 543 +/- 150 micrograms/ml h and reflected a cyclophosphamide total-body clearance (CLTB) of 103 +/- 31.6 ml/min. Plasma alkylating activity, assessed by p-nitrobenzyl-pyridine, remained steady at 1.6-4.3 micrograms/ml nor-nitrogen mustard equivalents. Urinary excretion of cyclophosphamide and alkylating activity accounted for 9.3% +/- 7.6% and 15.1% +/- 2.0% of the administered daily dose, respectively. The t1/2 and AUC of cyclophosphamide associated with the 5-day continuous infusion schedule are similar to those reported after administration of cyclophosphamide 1500 mg/m2 as an i.v. bolus.(ABSTRACT TRUNCATED AT 400 WORDS)
共有14例患者,7例男性和7例女性,共接受了21个可评估疗程的环磷酰胺5天持续静脉输注治疗。环磷酰胺剂量从每天300mg/m²增至400mg/m²,持续5天,每21 - 28天重复一次。患者人群的中位年龄为55岁(范围38 - 76岁),中位卡诺夫斯基体能状态为80(范围60 - 100)。仅1例患者未接受过先前治疗;5例患者仅接受过先前化疗,1例仅接受过先前放疗,7例两者均接受过。肿瘤类型包括胃癌(1例)、肺癌(2例)、结肠癌(4例)、尿道腺癌(1例)、宫颈癌(2例)、软骨肉瘤(1例)、黑色素瘤(1例)、子宫平滑肌肉瘤(1例)和胰腺癌(1例)。剂量限制性毒性为粒细胞减少,8例接受350mg/m²每天共5天治疗的高度预处理患者,白细胞计数最低点的中位数为1,700/微升(范围100 - 4,800)。1例未接受过大量先前治疗的患者接受了两个疗程的400mg/m²治疗,白细胞计数最低点分别为800/微升和600/微升。白细胞计数最低点出现在第9至21天(中位数14天)。药物性血小板减少仅发生在1例患者中(每天350mg/m²,最低点85,000/微升)。未观察到低钠血症或有症状的低渗状态。1例患者的放射性出血性膀胱炎可能有所加重。恶心和呕吐较轻。未观察到客观缓解。先前接受过治疗的患者的最大耐受剂量为每天350mg/m²,共5天。该剂量接近环磷酰胺大剂量推注常用的剂量。通过气相色谱法测得的环磷酰胺血浆稳态浓度(Css)为2.09 - 6.79微克/毫升。在14.5±5.9小时(平均值±标准差)达到稳态。输注后,环磷酰胺从血浆中呈单指数消失,半衰期为5.3±3.6小时。血浆中环磷酰胺浓度随时间变化的曲线下面积(AUC)为543±150微克/毫升·小时,反映环磷酰胺全身清除率(CLTB)为103±31.6毫升/分钟。通过对硝基苄基吡啶评估的血浆烷化活性稳定在1.6 - 4.3微克/毫升非氮芥当量。环磷酰胺及其烷化活性的尿排泄分别占每日给药剂量的9.3%±7.6%和15.1%±2.0%。与5天持续输注方案相关的环磷酰胺的半衰期和AUC与静脉推注1500mg/m²环磷酰胺后报道的相似。(摘要截选至400字)
