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化疗周期延迟7天对低危播散性生殖细胞肿瘤患者完全缓解率和无事件生存率的影响。

The effect of a 7-day delay in chemotherapy cycles on complete response and event-free survival in good-risk disseminated germ cell tumor patients.

作者信息

Motzer R J, Geller N L, Bosl G J

机构信息

Department of Medicine, Memorial Sloan-Kettering Center, New York, NY 10021.

出版信息

Cancer. 1990 Sep 1;66(5):857-61. doi: 10.1002/1097-0142(19900901)66:5<857::aid-cncr2820660508>3.0.co;2-g.

DOI:10.1002/1097-0142(19900901)66:5<857::aid-cncr2820660508>3.0.co;2-g
PMID:1696846
Abstract

The effect of duration of induction treatment on complete response (CR) and event-free survival (EFS) (time to death or relapse) was evaluated in 162 "good-risk" germ cell tumor (GCT) patients treated from November 1982 to July 1986 in a randomized prospective trial with VAB-6 (cyclophosphamide + vinblastine + bleomycin + dactinomycin + cisplatin; 81 patients) versus etoposide + cisplatin (EP; 81 patients). Patients received three cycles of VAB-6 every 28 days or four cycles of EP every 21 days. Treatment cycle with either regimen was routinely postponed for 7 days for leukocytes less than 3000/mm3 or platelets less than 100,000/mm3 and then administered regardless of blood count. The number of treatment days was calculated for each patient from initial treatment day to final induction date plus 28 days for VAB-6 and plus 21 days for EP. The proportion of CR and the EFS for good-risk GCT patients treated with cisplatin-based chemotherapy were not influenced by a less than or equal to 7-day delay resulting from chemotherapy-induced myelosuppression. Short, planned delays in chemotherapy for good-risk GCT patients (less than or equal to 7 days per cycle) appear to be acceptable since they may prevent serious toxicity in this curable patient population. Delays of longer than 7 days are strongly discouraged except in extraordinary life-threatening circumstances.

摘要

在1982年11月至1986年7月期间接受治疗的162例“低危”生殖细胞肿瘤(GCT)患者中,进行了一项随机前瞻性试验,评估诱导治疗持续时间对完全缓解(CR)和无事件生存期(EFS,至死亡或复发时间)的影响。该试验对比了VAB - 6方案(环磷酰胺 + 长春碱 + 博来霉素 + 放线菌素D + 顺铂;81例患者)与依托泊苷 + 顺铂(EP;81例患者)。患者每28天接受三个周期的VAB - 6治疗,或每21天接受四个周期的EP治疗。对于白细胞计数低于3000/mm³或血小板计数低于100,000/mm³的情况,两种方案的治疗周期通常推迟7天,然后无论血细胞计数如何都继续给药。计算每位患者从初始治疗日到最终诱导日期的治疗天数,VAB - 6方案再加28天,EP方案再加21天。基于顺铂的化疗治疗的低危GCT患者,CR比例和EFS不受化疗诱导的骨髓抑制导致的小于或等于7天延迟的影响。对于低危GCT患者,计划的短期化疗延迟(每个周期小于或等于7天)似乎是可以接受的,因为这可能防止在这个可治愈的患者群体中出现严重毒性。强烈不建议延迟超过7天,除非在危及生命的特殊情况下。

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