首页> 外文期刊>Bone marrow transplantation >Topotecan, thiotepa, and carboplatin for neuroblastoma: failure to prevent relapse in the central nervous system.
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Topotecan, thiotepa, and carboplatin for neuroblastoma: failure to prevent relapse in the central nervous system.

机译:托泊替康,硫替替帕和卡铂用于神经母细胞瘤:未能阻止中枢神经系统复发。

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摘要

We report on a three-drug myeloablative regimen designed to consolidate remission and to prevent central nervous system (CNS) relapse of high-risk neuroblastoma (NB). Sixty-six NB patients received topotecan 2 mg/m2/day, x 4 days; thiotepa 300 mg/m2/day, x 3 days; and carboplatin approximately 500 mg/m2/day, x 3 days. Post-SCT treatments included radiotherapy, immunotherapy, 13-cis-retinoic acid, +/-oral etoposide. Significant nonhematologic toxicities were mucositis and skin-related in all patients, convulsions in three patients, and cardiac failure and venocclusive disease of liver in one patient each. Grade 2 hepatotoxicity led to truncating cytoreduction in two patients; both later relapsed in brain. Among 46 patients transplanted in first complete/very good partial remission (CR/VGPR), event-free survival is 54% (s.e.+/-8%) at 36 months post-SCT; notable events were three non-NB-related deaths (adenovirus on day +9, bowel necrosis at 5 months, multiorgan failure at seven months) and four relapses in brain. Of 12 patients transplanted with evidence of NB, two became long-term event-free survivors and two relapsed in the brain. Of eight patients transplanted in second or greater CR/VGPR, one became a long-term event-free survivor and seven relapsed though not in the CNS. This regimen has manageable toxicity but does not prevent CNS relapse.
机译:我们报告了一种三药清髓疗法,旨在巩固缓解并预防高危神经母细胞瘤(NB)的中枢神经系统(CNS)复发。 66名NB患者接受拓扑替康2 mg / m2 /天,×4天;噻替帕300 mg / m2 /天,x 3天;和卡铂约500毫克/平方米/天x 3天。 SCT后的治疗包括放射疗法,免疫疗法,13-顺-视黄酸,+ /-口服依托泊苷。所有患者的重大非血液学毒性为粘膜炎和皮肤相关性,三例为惊厥,每例一名患者为心脏衰竭和肝静脉阻塞性疾病。 2级肝毒性导致两名患者的截短性细胞减少。后来都复发了。在46例首次完全/非常好部分缓解(CR / VGPR)移植的患者中,SCT后36个月的无事件生存率为54%(s.e。+ /-8%);值得注意的事件是3例与NB无关的死亡(第9天出现腺病毒,5个月时肠坏死,7个月时多器官衰竭)和4例脑复发。在移植了NB证据的12位患者中,有2位成为长期无事件生存者,另外2位在大脑中复发。在接受第二次或更多次CR / VGPR移植的8例患者中,1例成为长期无事件生存者,7例复发,尽管未在CNS中复发。该方案具有可控制的毒性,但不能防止中枢神经系统复发。

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