重组人粒细胞巨噬细胞集落刺激因子在接受强化骨髓抑制化疗的儿科患者中的随机试验。
Randomized trial of recombinant human granulocyte-macrophage colony-stimulating factor in pediatric patients receiving intensive myelosuppressive chemotherapy.
作者信息
Wexler L H, Weaver-McClure L, Steinberg S M, Jacobson J, Jarosinski P, Avila N, Pizzo P A, Horowitz M E
机构信息
Pediatric and Radiation Oncology Branches, National Cancer Institute, National Institutes of Health, Bethesda, MD, USA.
出版信息
J Clin Oncol. 1996 Mar;14(3):901-10. doi: 10.1200/JCO.1996.14.3.901.
PURPOSE
To evaluate whether recombinant human granulocyte-macrophage colony-stimulating factor (GM-CSF) reduces the hematologic toxicities and supportive care requirements of an intensive combination chemoradiotherapy regimen in pediatric and young adult sarcoma patients.
PATIENTS AND METHODS
Thirty-seven newly diagnosed patients age 1 to 25 years were randomized to receive 18 cycles of chemotherapy alone or with GM-CSF beginning in cycle 3. GM-CSF (5 to 15 micrograms/kg/d subcutaneously) was begun 24 hours after the completion of chemotherapy and continued through day 19 of each cycle or until the absolute granulocyte count (AGC) was > or = 500/microliter on 2 consecutive days.
RESULTS
GM-CSF reduced the median duration of grade 4 granulocytopenia from 9.0 days (range, 2 to 24) to 7.0 days (range, 1 to 21) (P < .0001), but did not significantly affect the grade of granulocyte nadir. No differences were seen in the incidence or types of infectious complications, incidence or duration of hospitalization and antimicrobial therapy, response to chemotherapy, or event-free or overall survival. GM-CSF was associated with more severe and protracted thrombocytopenia (median platelet nadir, 29,500/microliter [range, 3,000 to 288,000] v 59,000/microliter [range, 3,000 to 309,000], P < .0001; median time to recovery > 75,000/microliter, 16.0 days [range, 0 to 61] v 14.0 days [range, 0 to 38], P < .0001).
CONCLUSION
GM-CSF does not produce clinically meaningful reductions in the degree or duration of severe granulocytopenia following intensive multiagent chemotherapy, but is associated with worsened thrombocytopenia. GM-CSF also does not reduce the need for hospitalization or the incidence of febrile neutropenia and infectious complications. We conclude that the costs and increased toxicities associated with the use of this agent are not justified by its minimal clinical benefit for regimens of this level of intensity.
目的
评估重组人粒细胞巨噬细胞集落刺激因子(GM-CSF)是否能降低儿童和青年肉瘤患者强化联合放化疗方案的血液学毒性及支持治疗需求。
患者与方法
37例年龄在1至25岁的新诊断患者被随机分组,分别接受单独化疗18个周期或从第3周期开始联合GM-CSF治疗。GM-CSF(5至15微克/千克/天,皮下注射)在化疗结束后24小时开始使用,并持续至每个周期的第19天,或直至连续两天绝对粒细胞计数(AGC)≥500/微升。
结果
GM-CSF将4级粒细胞减少的中位持续时间从9.0天(范围2至24天)降至7.0天(范围1至21天)(P<.0001),但对粒细胞最低点的分级无显著影响。在感染并发症的发生率或类型、住院和抗菌治疗的发生率或持续时间、化疗反应、无事件生存期或总生存期方面未观察到差异。GM-CSF与更严重和持久的血小板减少相关(血小板最低点中位数,29,500/微升[范围3,000至288,000]对59,000/微升[范围3,000至309,000],P<.0001;恢复至>75,000/微升的中位时间,16.0天[范围0至61天]对14.0天[范围0至38天],P<.0001)。
结论
GM-CSF在强化多药化疗后,并未使严重粒细胞减少的程度或持续时间产生具有临床意义的降低,但与血小板减少加重相关。GM-CSF也未减少住院需求或发热性中性粒细胞减少及感染并发症的发生率。我们得出结论,对于这种强度的方案,该药物使用所带来的成本和增加的毒性因其极小的临床益处而不合理。
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