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High-dose chemotherapy and autologous bone marrow transplantation for patients with poor prognosis nonseminomatous germ cell tumours.

机译:预后不良的非精原性生殖细胞肿瘤患者需大剂量化疗和自体骨髓移植。

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摘要

Twenty-one patients with poor prognosis nonseminomatous germ cell tumours (six with extreme burden disease at presentation in whom partial remission had been achieved with initial induction therapy, and 15 with recurrent disease after induction therapy) were treated with high-dose chemotherapy and autologous bone marrow transplantation (BMT). The first six received etoposide 3.0 g m-2, ifosfamide 6.0 g m-2 and carboplatin 1.2 g m-2 (Regimen 1), and the subsequent 15 received etoposide 2.4 g m2 (continuous infusion), cyclophosphamide 7.2 g m-2 and carboplatin 0.8 g m-2 (Regimen 2) followed by infusion of previously stored autologous marrow. Regimen 1 was associated with considerable renal toxicity and mucositis, whereas Regimen 2 was relatively well tolerated. Two patients died as a consequence of the treatment: one of candidemia and one of interstitial pulmonary fibrosis. Only one of 17 patients who were autografted in or approaching marker remission subsequently developed disease progression (event-free survival 82%, 95% confidence interval [CI] 55% to 94%), whereas all four patients who had progressive disease at autografting subsequently developed further disease progression and died. Fourteen patients remain well and free of disease 0.5 to 6.5 years (median 3.3) post-BMT (event-free survival 67%, 95% CI 43% to 83%). A strategy of prompt reinduction followed by high-dose chemotherapy and autologous BMT at the first sign of failure of standard therapy may allow cure to be a realistic expectation.
机译:用大剂量化学疗法和自体骨治疗21例预后较差的非精原细胞生殖细胞肿瘤患者(其中6例表现为极度负担疾病,其中初始诱导治疗已部分缓解,15例诱导治疗后复发)。骨髓移植(BMT)。前六个接受依托泊苷3.0 g m-2,异环磷酰胺6.0 g m-2和卡铂1.2 g m-2(方案1),随后15个接受依托泊苷2.4 g m2(连续输注),环磷酰胺7.2 g m-2和卡铂0.8 g m-2(方案2),然后输注先前储存的自体骨髓。方案1与相当大的肾脏毒性和粘膜炎相关,而方案2的耐受性相对较好。该治疗导致两名患者死亡:一名念珠菌血症和一名间质性肺纤维化。自体移植或接近标志物缓解的17名患者中只有1名随后发生疾病进展(无事件生存率82%,95%置信区间[CI] 55%至94%),而所有4名在自体移植后均患有进行性疾病的患者病情进一步恶化并死亡。 BMT后0.5到6.5年(中位数3.3),十四名患者保持健康,无疾病(无事件生存率67%,95%CI 43%至83%)。在标准治疗失败的第一个迹象时,立即减少剂量,然后进行大剂量化疗和自体BMT的策略可能使治愈成为现实。

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