Wolf M, Havemann K, Holle R, Gropp C, Drings P, Hans K, Schroeder M, Heim M, Dommes M, Mende S
Department of Internal Medicine, Philipps-University of Marburg, Federal Republic of Germany.
J Clin Oncol. 1987 Dec;5(12):1880-9. doi: 10.1200/JCO.1987.5.12.1880.
A total of 144 patients with small-cell lung cancer (SCLC) were randomized to receive cisplatin/etoposide (PE) or ifosfamide/etoposide (IE) combination chemotherapy. PE consisted of cisplatin, 80 mg/m2, intravenously (IV) on day 1, and etoposide, 150 mg/m2, IV on days 3 through 5. IE consisted of ifosfamide, 1,500 mg/m2, IV on days 1 through 5, and etoposide, 120 mg/m2, IV on days 3 through 5. Six cycles were administered in 3-week intervals. Nonresponders were switched immediately to CAV, consisting of cyclophosphamide, 600 mg/m2, IV on days 1 and 2, Adriamycin (Adria Laboratories, Columbus, OH), 50 mg/m2, IV on day 1, and vincristine, 2 mg, IV on day 1. Patients obtaining complete remission (CR) received prophylactic cranial irradiation with 30 Gy. After completion of chemotherapy, patients with limited disease received chest irradiation with 45 Gy. No maintenance therapy was given to patients in CR. Minimum follow-up was 2 years. Of the 141 patients evaluable, the overall response rate was 65% in PE therapy and 68% in IE therapy. The CR rate was 32% v 20% for all patients, 50% v 24% for limited disease, and 22% v 18% for extensive disease, all in favor of PE therapy. Median survival for all patients was 11.6 months v 9.4 months, for limited disease 14.8 months v 11.0 months, and for extensive disease 8.9 months v 7.5 months, all preferring PE therapy. The 2-year survival rate was higher in PE therapy than in IE therapy for all patients (12% v 9%) and for limited disease (23% v 10%), but not for extensive disease (5% v 9%). Median progression-free survival was 7.5 months v 6.0 months for all patients, 12.2 months v 8.8 months for limited disease, and 5.9 months v 4.4 months for extensive disease, all in favor of PE. Relapse in the area of the primary tumor was found less often after PE than after IE therapy (25% v 38%). Response to second-line CAV was seen in 30% of patients with prior PE and 43% with prior IE therapy, but was usually short lasting, and only one patient achieved CR. Toxicity included three lethal complications. Nausea, vomiting, diarrhea, and skin lesions occurred more often after PE than after IE therapy. These results suggest that PE is superior to IE chemotherapy in limited-stage, but not in extensive-stage SCLC, and that CAV is cross-resistant to PE, as well as to IE in the majority of patients.
总共144例小细胞肺癌(SCLC)患者被随机分为两组,分别接受顺铂/依托泊苷(PE)或异环磷酰胺/依托泊苷(IE)联合化疗。PE方案为顺铂80mg/m²,于第1天静脉滴注(IV),依托泊苷150mg/m²,于第3至5天IV。IE方案为异环磷酰胺1500mg/m²,于第1至5天IV,依托泊苷120mg/m²,于第3至5天IV。每3周进行6个周期的治疗。无反应者立即改用CAV方案,该方案包括环磷酰胺600mg/m²,于第1和2天IV,阿霉素(阿德里亚实验室,俄亥俄州哥伦布市)50mg/m²,于第1天IV,长春新碱2mg,于第1天IV。获得完全缓解(CR)的患者接受30Gy的预防性颅脑照射。化疗结束后,局限性疾病患者接受45Gy的胸部照射。CR患者不给予维持治疗。最短随访时间为2年。在141例可评估患者中,PE治疗组的总缓解率为65%,IE治疗组为68%。所有患者的CR率分别为32%对20%,局限性疾病患者为50%对24%,广泛性疾病患者为22%对18%,均显示PE治疗更优。所有患者的中位生存期分别为11.6个月对9.4个月,局限性疾病患者为14.8个月对11.0个月,广泛性疾病患者为8.9个月对7.5个月,均倾向于PE治疗。所有患者(12%对9%)和局限性疾病患者(23%对10%)的2年生存率PE治疗组高于IE治疗组,但广泛性疾病患者并非如此(5%对9%)。所有患者的中位无进展生存期分别为7.5个月对6.0个月,局限性疾病患者为12.2个月对8.8个月,广泛性疾病患者为5.9个月对4.4个月,均有利于PE治疗。与IE治疗相比,PE治疗后原发肿瘤部位复发较少(25%对38%)。接受过PE治疗的患者中30%对二线CAV有反应,接受过IE治疗的患者中43%有反应,但通常持续时间较短,只有1例患者达到CR。毒性反应包括3例致命并发症。PE治疗后恶心、呕吐、腹泻和皮肤病变的发生频率高于IE治疗。这些结果表明,在局限性小细胞肺癌中PE化疗优于IE化疗,但在广泛性小细胞肺癌中并非如此,并且CAV对PE以及大多数患者中的IE具有交叉耐药性。
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