Hijiya Nobuko, Stewart Clinton F, Zhou Yinmei, Campana Dario, Coustan-Smith Elaine, Rivera Gaston K, Relling Mary V, Pui Ching-Hon, Gajjar Amar
Department of Oncology, St Jude Children's Research Hospital, Memphis, TN, USA.
Cancer. 2008 May 1;112(9):1983-91. doi: 10.1002/cncr.23395.
The authors evaluated the response rate, toxicity, and pharmacokinetics of topotecan given before standard induction therapy for childhood acute lymphoblastic leukemia (ALL) in first relapse.
Patients received topotecan (2.4 mg/m(2) daily as a 30-minute infusion) for 5 days before induction therapy with dexamethasone, vincristine, and asparaginase (native or pegylated Escherichia coli). The pharmacokinetics of topotecan were measured with the first dose of treatment in 23 patients.
Twenty-eight of 31 patients with circulating blast cells were evaluable for response to topotecan. Twenty-five patients (89.3%) had a response (>25% decrease in circulating blast cells). The leukocyte count (P = .0001) and blast cell count (P = .0009) declined significantly during topotecan therapy. The median (range) topotecan lactone area under the concentration-time curve after the first dose was 85.4 L/hour/m(2) (range, 38.7-229.3 L/hour/m(2)). At the end of induction, 23 patients (74.2%) had a complete response, 1 patient (3.2%) had a partial response, 5 patients (16.1%) had no response, and 2 patients had died of infection. Six of the 17 patients who were studied for minimal residual disease (MRD) achieved MRD-negative status at the end of induction. The main toxicities were hematologic, gastrointestinal, and hepatic. The estimated 5-year survival rate, event-free survival rate, and cumulative incidence of second relapse were 24.1% +/- 7.9%, 18.2% +/- 7.4%, and 22.8% +/- 8.7%, respectively, in the 29 patients who had a hematologic first relapse.
A regimen comprising single-agent topotecan given with a standard 3-drug combination was effective in inducing remission in pediatric patients with relapsed ALL and was tolerated well.
作者评估了拓扑替康在儿童急性淋巴细胞白血病(ALL)首次复发时于标准诱导治疗前使用的缓解率、毒性及药代动力学。
患者在接受地塞米松、长春新碱和天冬酰胺酶(天然或聚乙二醇化大肠杆菌)诱导治疗前5天,接受拓扑替康(每日2.4 mg/m²,30分钟静脉输注)。对23例患者在首次治疗剂量时测定拓扑替康的药代动力学。
31例循环母细胞患者中有28例可评估对拓扑替康的反应。25例患者(89.3%)有反应(循环母细胞减少>25%)。在拓扑替康治疗期间白细胞计数(P = 0.0001)和母细胞计数(P = 0.0009)显著下降。首次给药后拓扑替康内酯浓度-时间曲线下面积的中位数(范围)为85.4 L/小时/m²(范围,38.7 - 229.3 L/小时/m²)。诱导结束时,23例患者(74.2%)完全缓解,1例患者(3.2%)部分缓解,5例患者(16.1%)无反应,2例患者死于感染。17例接受微小残留病(MRD)研究的患者中有6例在诱导结束时达到MRD阴性状态。主要毒性为血液学、胃肠道和肝脏毒性。29例血液学首次复发的患者中,估计5年生存率、无事件生存率和第二次复发的累积发生率分别为24.1%±7.9%、18.2%±7.4%和22.8%±8.7%。
包含单药拓扑替康与标准三联药物联合使用的方案在诱导复发的儿童ALL患者缓解方面有效且耐受性良好。
