Houghton J A, Cheshire P J, Hallman J D, Lutz L, Luo X, Li Y, Houghton P J
Departments of Molecular Pharmacology and Biostatistics, St. Jude Children's Research Hospital, Memphis, Tennessee 38101, USA.
Clin Cancer Res. 1996 Jan;2(1):107-18.
Irinotecan [7-ethyl-10-(4-[1-piperidino]-1-piperidino)-carbonyloxy-camptothec in] administered i.v. in two courses, each course consisting of administration every day for 5 days [(dx5)2] on days 1-5 and 8-12, has demonstrated significant activity against advanced human tumor xenografts derived from colon adenocarcinomas and several childhood cancers. To build on this therapy, we have evaluated the combination of irinotecan given on this schedule with 5-fluorouracil given on days 1, 7, and 14 with or without leucovorin [(dx5)3 i.v.] against colon tumors, or combined with etoposide administered (dx5)2 i.v. either 2 h before or 2 h after irinotecan for treatment of colon tumors and rhabdomyosarcomas. A combination of 5-fluorouracil at 75% and irinotecan at 50% of their respective maximum tolerated doses when administered as single agents on this schedule gave acceptable toxicity. Against colon adenocarcinoma xenografts, 5-fluorouracil did not enhance the response rate compared with that obtained with the optimum dose of irinotecan given as a single agent. Against GC3/TK- xenografts, which lack thymidine kinase and cannot salvage thymidine to circumvent the inhibition of thymidylate synthase, the addition of leucovorin to the combination increased the complete response rate from 10 to >90%, whereas the response rates for the optimal doses of irinotecan or 5-fluorouracil, as single agents, were 30 and <10%, respectively. Etoposide d x 5 i.v. for two or three courses or (d x 5)3 p.o. did not cause objective regression of any colon tumors. In contrast, three of five rhabdomyosarcoma lines demonstrated a high frequency of partial regressions or complete regressions when treated (d x 5)1 i.v. Repetitive courses [e.g., (d x 5)2 or (d x 5)3] i.v. or p.o. or by 4-h infusion d x3 i.v. were either equally effective or less effective. Irinotecan and etoposide were combined using the (d x 5)2 i.v. schedule for both drugs, in which irinotecan was given 2 h before or 2 h after the administration of etoposide. Each drug could be combined at only 38% of its respective maximum tolerated dose when administered as a single agent, indicating greater than additive toxicity. Toxicity was similar irrespective of the sequence of administration and was manifested by loss of weight (73% of the initial weight, nadir day 7), myelosuppression, and prolonged thrombocytopenia. The responses of colon carcinomas to the combination given in either sequence were similar to that achieved with irinotecan given alone at the same dose as used in the combination. Similarly, when etoposide was given before irinotecan, the responses of rhabdomyosarcomas were similar to those for irinotecan. However, in experiments in which etoposide was administered 2 h after each dose of irinotecan, there was significant antagonism of the antitumor activity of irinotecan.
伊立替康[7 - 乙基 - 10 - (4 - [1 - 哌啶基] - 1 - 哌啶基) - 羰氧基 - 喜树碱]静脉注射分两个疗程给药,每个疗程在第1 - 5天和第8 - 12天每天给药1次,共5天[(dx5)2],已证明对源自结肠腺癌和几种儿童癌症的晚期人类肿瘤异种移植具有显著活性。为了在此治疗基础上进一步拓展,我们评估了按此方案给药的伊立替康与在第1、7和14天给药的5 - 氟尿嘧啶联合使用(加或不加亚叶酸[(dx5)3静脉注射])对结肠肿瘤的疗效,或者与在伊立替康静脉注射前2小时或后2小时给药的依托泊苷[(dx5)2静脉注射]联合用于治疗结肠肿瘤和横纹肌肉瘤。当按此方案以各自最大耐受剂量的75%的5 - 氟尿嘧啶和50%的伊立替康作为单药给药时,毒性可接受。对于结肠腺癌异种移植,与以最佳剂量单药使用伊立替康相比,5 - 氟尿嘧啶并未提高缓解率。对于缺乏胸苷激酶且无法挽救胸苷以规避胸苷酸合成酶抑制作用的GC3/TK - 异种移植,在联合用药中添加亚叶酸可使完全缓解率从10%提高至>90%,而伊立替康或5 - 氟尿嘧啶单药最佳剂量的缓解率分别为30%和<10%。静脉注射5天的依托泊苷进行两个或三个疗程或口服(dx5)3并未使任何结肠肿瘤出现客观消退。相比之下,五条横纹肌肉瘤细胞系中有三条在静脉注射(dx5)1治疗时出现高频率的部分消退或完全消退。静脉注射或口服重复疗程[例如(dx5)2或(dx5)3]或静脉注射4小时(dx3)的疗效相当或更低。伊立替康和依托泊苷按(dx5)2静脉注射方案联合使用,即伊立替康在依托泊苷给药前2小时或后2小时给药。当作为单药给药时,每种药物仅能以其各自最大耐受剂量的38%联合使用,表明毒性大于相加作用。无论给药顺序如何,毒性相似,表现为体重减轻(初始体重的73%,最低点在第7天)、骨髓抑制和血小板减少持续时间延长。结肠腺癌对两种给药顺序的联合用药的反应与以联合用药中相同剂量单药使用伊立替康时的反应相似。同样,当依托泊苷在伊立替康之前给药时,横纹肌肉瘤的反应与伊立替康的反应相似。然而,在每次伊立替康给药后2小时给予依托泊苷的实验中,伊立替康的抗肿瘤活性出现显著拮抗作用。
