Tummarello D, Mari D, Graziano F, Isidori P, Cetto G, Pasini F, Santo A, Cellerino R
Department of Medical Oncology, Univeristy of Ancona, Ospedale Torrette, Italy.
Cancer. 1997 Dec 15;80(12):2222-9.
Studies of chemotherapy for patients with small cell lung carcinoma (SCLC) have shown that teniposide (T) may have higher activity than etoposide (E). In this randomized, controlled Phase III study, the authors compared cyclophosphamide, doxorubicin, and vincristine (CAV) with E and CAV with T as induction treatments for patients with SCLC. A second objective of the study was to study patients who had achieved complete response (CR). They were considered for a second randomization to maintenance therapy, in which they would receive either recombinant interferon-alpha (rIFN-alpha) or no treatment.
From June 1990 to December 1995, 140 untreated SCLC patients were enrolled in this study. Patients were stratified by either limited disease (LD) or extensive disease (ED) and randomized to one of two treatment arms. The schedules for both arms included cyclophosphamide 1000 mg/m2 administered intravenously (i.v.), doxorubicin 50 mg/m2 i.v., and vincristine 2 mg i.v. on Day 1. Arm A (CAV-E) involved the addition of E 100 mg/m2 i.v. on Days 2, 3, and 4; Arm B (CAV-T) involved the addition of T 60 mg/m2 i.v. on Days 2, 3, and 4. Courses were repeated every 3 weeks. After 3 courses, patients with LD received chest radiotherapy and 2 additional consolidation courses, whereas patients with ED received 5 consecutive courses only. Patients with CR were considered for the second randomization, which consisted of either maintenance therapy with intramuscular (i.m.) rIFN-alpha-2b, 3 M.U., once a day for 9 months (IFN-alpha arm) or no therapy (control arm).
At 5 years from start-up (3-year median observation time and 90% death rate), the study was closed. Results were as follows: 140 patients (71 in Arm A and 69 in Arm B) were eligible for survival analysis; 131 were evaluable for response and toxicity (66 in Arm A and 65 in Arm B), whereas 9 were not (6 early deaths and 3 with protocol violations). Among evaluable patients, 68 showed LD (35 assigned to Arm A and 33 to Arm B); the responses to treatment were 28.5% (10/35) CR and 51% (18/35) partial response (PR) to CAV-E, and 39% (13/33) CR and 39% PR (13/33) to CAV-T. Sixty-three patients showed ED (31 assigned to Arm A and 32 to Arm B); their responses were 22.5% (7/31) CR and 52% (16/31) PR to CAV-E, and 12.5% (4/32) CR and 50% (16/32) PR to CAV-T. Drug-related toxicity was WHO Grade 3-4 myelosuppression in 20% of 292 CAV-E courses and in 27% of 252 CAV-T courses. There were 6 toxic deaths, 1 in Arm A and 5 in Arm B (chi-square = 2.86); 2 patients in Arm A discontinued therapy due to persistent leukopenia and thrombocytopenia. No other remarkable toxicities were observed. Actuarial median survival (MS) was 13.7 months (range, 1.0-62.5 months) for patients with LD receiving CAV-E (Arm A) and 15.2 months (range, 0.5-68.2 months) for those receiving CAV-T (Arm B) (chi-square = 0.89); in patients with ED it was 10.5 months (range, 0.6-30.4 months) and 8.2 months (range, 0.2-24.8 months), respectively (chi-square = 3.42). Overall, MS was 12 months (range, 0.6-62.5 months) in Arm A and 10 months (range, 0.2-68.2 months) in Arm B (chi-square = 0.059). Thirty-nine patients with CR (27.8%) were candidates for the second randomization. Among them, 26 patients (18.5%) complied with the program and were randomized as follows: 14 were assigned to the IFN-alpha arm and 12 to the control arm. Starting from the second randomization, median time to progression was 12 months (range, 3-51 months) for patients in the IFN-alpha arm versus 7 months (range, 1-59 months) for patients in the control arm (chi-square = 0.12). MS was 15 months (range, 5-52.3 months) versus 9 months (range, 2-60.5 months) (chi-square = 0.13).
This study did not show a wide difference in activity and toxicity between CAV-E and CAV-T. The number of patients who entered the second randomization was too small to reach the second study endpoint.
针对小细胞肺癌(SCLC)患者的化疗研究表明,替尼泊苷(T)的活性可能高于依托泊苷(E)。在这项随机对照III期研究中,作者比较了环磷酰胺、多柔比星和长春新碱(CAV)联合E与CAV联合T作为SCLC患者诱导治疗的效果。该研究的第二个目标是研究达到完全缓解(CR)的患者。这些患者被考虑进行第二次随机分组以接受维持治疗,即接受重组干扰素-α(rIFN-α)或不接受治疗。
从1990年6月至1995年12月,140例未经治疗的SCLC患者入组本研究。患者按疾病局限期(LD)或广泛期(ED)分层,并随机分为两个治疗组之一。两组的治疗方案均包括第1天静脉注射(i.v.)环磷酰胺1000 mg/m²、多柔比星50 mg/m²和长春新碱2 mg。A组(CAV-E)在第2、3、4天加用静脉注射E 100 mg/m²;B组(CAV-T)在第2、3、4天加用静脉注射T 60 mg/m²。每3周重复一个疗程。3个疗程后,LD患者接受胸部放疗及另外2个巩固疗程,而ED患者仅接受5个连续疗程。达到CR的患者考虑进行第二次随机分组,包括接受肌肉注射(i.m.)rIFN-α-2b 3 MU、每日1次、共9个月的维持治疗(IFN-α组)或不进行治疗(对照组)。
从启动研究开始5年后(中位观察时间3年,死亡率90%),该研究结束。结果如下:140例患者(A组71例,B组69例)符合生存分析条件;131例可评估疗效和毒性(A组66例,B组65例),9例不可评估(6例早期死亡,3例违反方案)。在可评估患者中,68例为LD(A组35例,B组33例);CAV-E治疗的缓解率为28.5%(10/35)CR和51%(18/)PR,CAV-T治疗的缓解率为39%(13/33)CR和39%(13/33)PR。63例为ED(A组31例,B组32例);CAV-E治疗的缓解率为22.5%(7/31)CR和52%(16/31)PR,CAV-T治疗的缓解率为12.5%(4/32)CR和50%(16/32)PR。292个CAV-E疗程中有20%、252个CAV-T疗程中有27%出现与药物相关的WHO 3 - 4级骨髓抑制。有6例毒性死亡,A组1例,B组5例(卡方检验=2.86);A组2例患者因持续性白细胞减少和血小板减少而停止治疗。未观察到其他明显毒性。接受CAV-E(A组)的LD患者的精算中位生存期(MS)为13.7个月(范围1.0 - 62.5个月),接受CAV-T(B组)的患者为15.2个月(范围0.5 - 68.2个月)(卡方检验=0.89);ED患者中分别为10.5个月(范围0.6 - 30.4个月)和8.2个月(范围0.2 - 24.8个月)(卡方检验=3.42)。总体而言,A组的MS为12个月(范围0.6 - 62.5个月),B组为10个月(范围0.2 - 68.2个月)(卡方检验=0.059)。39例达到CR(27.8%)的患者符合第二次随机分组条件。其中,26例患者(18.5%)遵守方案并被随机分组如下:14例分配至IFN-α组,12例分配至对照组。从第二次随机分组开始,IFN-α组患者的中位进展时间为12个月(范围3 - 51个月),对照组患者为7个月(范围1 - 59个月)(卡方检验=0.12)。MS分别为15个月(范围5 - 52.3个月)和9个月(范围2 - 60.5个月)(卡方检验=0.13)。
本研究未显示CAV-E和CAV-T在活性和毒性方面存在显著差异。进入第二次随机分组的患者数量过少,无法达到第二个研究终点。
