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首页> 外文期刊>Journal of Clinical Oncology >Long-term results of first-line sequential high-dose etoposide, ifosfamide, and cisplatin chemotherapy plus autologous stem cell support for patients with advanced metastatic germ cell cancer: an extended phase I/II study of the German Testicular Can
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Long-term results of first-line sequential high-dose etoposide, ifosfamide, and cisplatin chemotherapy plus autologous stem cell support for patients with advanced metastatic germ cell cancer: an extended phase I/II study of the German Testicular Can

机译:一线序贯大剂量依托泊苷,异环磷酰胺和顺铂化疗加自体干细胞支持治疗晚期转移性生殖细胞癌的长期结果:德国睾丸罐头I / II期扩展研究

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摘要

PURPOSE: Patients with disseminated germ cell cancer and poor prognosis (International Germ Cell Cancer Collaborative Group [IGCCCG] classification) achieve only a 45% to 50% long-term survival by standard chemotherapy. First-line high-dose chemotherapy might be able to improve the result. This analysis reports toxicity and long-term results of a large phase I/II study of sequential high-dose etoposide, ifosfamide, and cisplatin (VIP) in patients with advanced germ cell tumors. PATIENTS AND METHODS: Between July 1993 and November 1999, 221 patients with either Indiana "advanced disease" (n = 39) or IGCCCG "poor prognosis" criteria (n = 182) received one cycle of VIP followed by three to four sequential cycles of high-dose VIP chemotherapy plus stem cell support, every 3 weeks, at six consecutive dose levels. RESULTS: Dose limiting toxicity occurred at level 8 (100 mg/m2 cisplatinum, 1750 mg/m2 etoposide, 12 g/m2 ifosfamide) with grade 4 mucositis (three of eight patients), grade 3 CNS toxicity (one of eight patients), grade 4 renal toxicity (one of eight patients), and prolonged granulocytopenia (one of eight patients). After 4-year median follow-up, progression-free survival and disease-specific survival rates in the poor prognosis subgroup were 69% and 79% at 2 years and 68% and 73% at 5 years, with 76% for gonadal/retroperitoneal versus 67% for mediastinal primaries. Severe toxicity included treatment related death (4%), treatment-related acute myeloid leukemia (1%), long-term impared renal function (3%), chronic renal failure (1%), and persistent grade 2-3 neuropathy (5%). CONCLUSION: Repetitive cycles of high-dose VIP with peripheral stem cell support can be successfully applied in a multicenter setting. Dose level 6 with cisplatin 100 mg/m2, etoposide 1500 mg/m2, and ifosfamide 10 g/m2 is recommended for further investigation in randomized trials. An ongoing randomized trial within the European Organization for Research and Treatment of Cancer evaluates this protocol against four cycles of standard cisplatin, etoposide, and bleomycin.
机译:目的:具有扩散性生殖细胞癌且预后较差的患者(国际生殖细胞癌协作组[IGCCCG]分类)通过标准化学疗法只能获得45%至50%的长期生存率。一线大剂量化疗可能会改善治疗效果。该分析报告了对晚期生殖细胞肿瘤患者进行顺序大剂量依托泊苷,异环磷酰胺和顺铂(VIP)的一项大型I / II期研究的毒性和长期结果。患者与方法:在1993年7月至1999年11月之间,有221例印第安纳州“高级病”(n = 39)或IGCCCG“不良预后”标准(n = 182)的患者接受了一个VIP周期,随后连续3到4个周期大剂量VIP化疗加干细胞支持,每3周一次,连续六个剂量水平。结果:剂量限制毒性发生在8级(100 mg / m2顺铂,1750 mg / m2依托泊苷,12 g / m2异环磷酰胺),4级粘膜炎(8例患者),3级CNS毒性(8例患者), 4级肾毒性(八名患者之一)和长时间粒细胞减少症(八名患者之一)。中位随访4年后,不良预后亚组的无进展生存期和疾病特异性生存率在2年时分别为69%和79%,在5年时分别为68%和73%,其中性腺/腹膜后激素为76%纵隔原发癌占67%。严重毒性包括与治疗有关的死亡(4%),与治疗有关的急性髓性白血病(1%),长期肾功能受损(3%),慢性肾衰竭(1%)和2-3级持续神经病(5) %)。结论:高剂量VIP和外周干细胞支持的重复周期可以成功应用于多中心环境。建议在随机试验中进一步研究6级剂量的顺铂100 mg / m2,依托泊苷1500 mg / m2和异环磷酰胺10 g / m2。欧洲癌症研究与治疗组织内正在进行的一项随机试验针对标准顺铂,依托泊苷和博来霉素的四个周期评估了该方案。

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