Kirkwood J M
Division of Medical Oncology, University of Pittsburgh, PA 15213.
Semin Oncol. 1991 Oct;18(5 Suppl 7):83-90.
Melanoma does not respond meaningfully to systemic chemotherapy. No significant improvement in overall survival has been observed with any therapy in the setting of advanced disease, nor in the adjuvant setting. The most active single drugs achieve 14% to 22% response rates in larger phase II series, and drug combinations have not in general improved true response rates by 15% or more. Experience with recombinant interferon alpha-2 (rIFN alpha 2) administered by a variety of schedules and routes has demonstrated tumor response rates of 12% to 22% in advanced melanoma. Administered combined with chemotherapy, rIFN alpha 2 has improved response rates in some, but not all trials to date. On the basis of increased responsiveness noted to be inversely related to tumor size, IFN alpha has been explored over the past 7 years as an adjuvant to definitive surgery for melanoma. The North Central Cancer Treatment Group (NCCTG) and Eastern Cooperative Oncology Group (ECOG) have recently completed trials of 3 and 12 months' duration of maximal dosages of rIFN alpha 2 in subjects with high-risk resected deep primary or lymph node metastatic melanoma. These randomized controlled studies completed accrual in 1990. The ECOG trial EST 1684 has tested the effect of rIFN alpha 2b, given intravenously daily for 5 days per week for 4 weeks at 20 x 10(6) IU/m2/d, then subcutaneously three times a week at 10 x 10(6) IU/m2/d for 11 months. A series of three analyses is planned for the ECOG trial, and the first of these interim analyses was reported to the ECOG in June, 1990, revealing an encouraging divergence of survival curves that does not achieve statistical significance at this early time. A randomized controlled study of 3 months' duration of rIFN alpha 2a at 12 x 10(6) IU/m2/d intramuscularly three times a week performed by the NCCTG is also in too early a stage to allow definitive conclusions yet. The toxicity of IFN alpha administered at maximum tolerated doses has been significant in terms of constitutional symptoms and organ dysfunction. There have been two instances of fatal toxicity observed in the ECOG study (286 subjects). Consideration of lower, more tolerable dosage regimens has been derived from the desire to evaluate longer periods of IFN alpha 2 therapy, and long-term maintenance treatment with IFN alpha 2 in adjuvant melanoma therapy. In addition, immunologic studies suggest that dosages of 3 x 10(6) IU/m2/d may be more immunologically active in vivo.(ABSTRACT TRUNCATED AT 400 WORDS)
黑色素瘤对全身化疗没有明显反应。在晚期疾病或辅助治疗中,尚未观察到任何治疗方法能使总生存期有显著改善。在规模较大的II期研究中,最有效的单一药物的缓解率为14%至22%,而且药物联合使用总体上并未使真正的缓解率提高15%或更多。通过多种给药方案和途径使用重组干扰素α-2(rIFNα2)治疗晚期黑色素瘤的经验表明,肿瘤缓解率为12%至22%。与化疗联合使用时,rIFNα2在一些但并非所有的现有试验中提高了缓解率。基于观察到的反应性增加与肿瘤大小呈负相关,在过去7年中,干扰素α被探索作为黑色素瘤根治性手术的辅助治疗。北中部癌症治疗组(NCCTG)和东部肿瘤协作组(ECOG)最近完成了对高危切除的深部原发性或淋巴结转移性黑色素瘤患者使用最大剂量rIFNα2进行3个月和12个月治疗的试验。这些随机对照研究在1990年完成入组。ECOG试验EST 1684测试了rIFNα2b的效果,静脉注射,每周5天,每天20×10⁶IU/m²,共4周,然后皮下注射,每周3次,每次10×10⁶IU/m²,共11个月。ECOG试验计划进行一系列三项分析,其中第一次中期分析于1990年6月报告给ECOG,结果显示生存曲线出现了令人鼓舞的差异,但在这个早期阶段尚未达到统计学意义。NCCTG进行的一项关于每周3次、每次12×10⁶IU/m²肌肉注射rIFNα2a、为期3个月的随机对照研究也尚处于早期阶段,无法得出明确结论。以最大耐受剂量使用干扰素α的毒性在全身症状和器官功能障碍方面较为显著。在ECOG研究(286名受试者)中观察到两例致命毒性。出于评估更长疗程的干扰素α2治疗以及在黑色素瘤辅助治疗中使用干扰素α2进行长期维持治疗的愿望,人们考虑了更低、更易耐受的给药方案。此外,免疫学研究表明,3×10⁶IU/m²/d的剂量在体内可能具有更强的免疫活性。(摘要截选至400字)
