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晚期神经母细胞瘤的双重大剂量化疗及自体骨髓移植:LMCE2研究

Double megatherapy and autologous bone marrow transplantation for advanced neuroblastoma: the LMCE2 study.

作者信息

Philip T, Ladenstein R, Zucker J M, Pinkerton R, Bouffet E, Louis D, Siegert W, Bernard J L, Frappaz D, Coze C

机构信息

Centre Léon Bérard, Pediatric and Bone Marrow Transplant Department, Lyon, France.

出版信息

Br J Cancer. 1993 Jan;67(1):119-27. doi: 10.1038/bjc.1993.21.

Abstract

In the LMCE1 study using a single course of megatherapy most of the relapses occurred during the first 2 years after autologous bone marrow transplantation. A second pilot study (LMCE2) was therefore set up using a double harvest/double graft approach with two different megatherapy regimens. Objectives were to test the role of increased dose intensity on response status, relapse pattern and overall survival. Thirty-three patients (20 boys, 13 girls) with a median age of 53 months at first megatherapy (range, 17-202 months) entered this study. They were cases either with refractory disease in partial response after second line treatment for stage 4 neuroblastoma (n = 25) or after relapse from stage 4 (n = 5) or stage 3 disease (n = 3). All patients received Etoposid and/or Cisplatinum (or Carboplatin) containing treatments before megatherapy. The first megatherapy regimen was a combination of Tenoposid, Carmustine and Cisplatinum (or Carboplatin), the second applied Vincristin, Melphalan and Total Body Irradiation. The first harvest was scheduled 4 weeks after the last chemotherapy, the second 60 to 90 days after megatherapy. All marrows were purged in vitro by an immunomagnetic technique. Median follow up time since first megatherapy is 56 months. Response rates for evaluable patients were 65% (complete response rate: 16%) for megatherapy 1 and 60% (complete response rate: 25%) for megatherapy 2. Considering that only patients with delayed response or relapse were eligible for this pilot study the overall survival was encouraging with 36% at 2 years and still 32% at 5 years. The costs for these survival rates were high in terms of morbidity (four early and four late toxic deaths; toxic death rate: 24%). Double harvesting may have the disadvantage of delayed engraftments related in part to a disturbance of marrow microenvironment by megatherapy 1. This double megatherapy approach achieved a prolonged relapse free interval (median 11 months, range 2-31 months) in patients reaching megatherapy 2 and justifies further evaluation of concepts with consecutive dose-escalation.

摘要

在使用单一疗程大剂量疗法的LMCE1研究中,大多数复发发生在自体骨髓移植后的头两年。因此,开展了第二项试点研究(LMCE2),采用双采集/双移植方法及两种不同的大剂量疗法方案。目的是测试增加剂量强度对缓解状态、复发模式和总生存期的作用。33例患者(20例男孩,13例女孩)首次接受大剂量疗法时的中位年龄为53个月(范围为17 - 202个月)进入本研究。他们均为4期神经母细胞瘤二线治疗后部分缓解但疾病难治的病例(n = 25),或4期(n = 5)或3期疾病复发后的病例(n = 3)。所有患者在接受大剂量疗法前均接受过含依托泊苷和/或顺铂(或卡铂)的治疗。第一种大剂量疗法方案为替尼泊苷、卡莫司汀和顺铂(或卡铂)联合应用,第二种应用长春新碱、美法仑和全身照射。第一次采集安排在最后一次化疗后4周,第二次在大剂量疗法后60至90天。所有骨髓均采用免疫磁技术在体外进行净化处理。自首次大剂量疗法以来的中位随访时间为56个月。可评估患者中,第一种大剂量疗法的缓解率为65%(完全缓解率:16%),第二种大剂量疗法的缓解率为60%(完全缓解率:25%)。考虑到只有反应延迟或复发的患者才有资格参加这项试点研究,其总生存期令人鼓舞,2年时为36%,5年时仍为32%。就发病率而言(4例早期和4例晚期毒性死亡;毒性死亡率:24%),这些生存率的代价高昂。双采集可能有植入延迟的缺点,部分原因是第一种大剂量疗法对骨髓微环境的干扰。这种双大剂量疗法方案使达到第二种大剂量疗法的患者无复发生存期延长(中位11个月,范围2 - 31个月),证明对连续剂量递增概念进行进一步评估是合理的。

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