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顺铂与抗微管药物紫杉醇和长春新碱联合使用所产生的序列依赖性细胞毒性作用。

Sequence-dependent cytotoxic effects due to combinations of cisplatin and the antimicrotubule agents taxol and vincristine.

作者信息

Rowinsky E K, Citardi M J, Noe D A, Donehower R C

机构信息

Division of Pharmacology and Experimental Therapeutics, Johns Hopkins Oncology Center, Baltimore, Maryland 21205.

出版信息

J Cancer Res Clin Oncol. 1993;119(12):727-33. doi: 10.1007/BF01195344.

Abstract

The antineoplastic activity that taxol has demonstrated in advanced ovarian cancer and other neoplasms in which the platinum analogues are among the most active agents has been the impetus for the development of taxol/platinum combination regimens. Since both classes of agents are known to induce cell-cycle-dependent effects and to delay cell-cycle traverse in specific phases of the cycle, an evaluation of drug sequence dependence was incorporated into initial clinical studies of the drug combination. To complement clinical studies, sequence-dependent interactions were assessed in vitro using L1210 leukemia. Cytotoxicity resulting from the combination of taxol and cisplatin was significantly increased over that achieved with cisplatin alone only when cisplatin was administered after taxol. This sequence was significantly superior to both the reverse sequence and to simultaneous drug treatment. Results achieved with sequence iterations of vincristine and cisplatin were nearly identical. In addition, alkaline-elution studies, using the optimal sequence of cisplatin and either taxol or vincristine, demonstrated that these antimicrotubule agents do not increase the formation of cisplatin-induced DNA interstrand and DNA-protein crosslinking over that produced by cisplatin alone. Although the mechanisms for the sequence-dependent cytotoxic interactions between cisplatin and the antimicrotubule agents have not been determined, it is likely that antagonistic interactions occur with the suboptimal sequences, probably because of cell-cycle-dependent phenomena.

摘要

紫杉醇在晚期卵巢癌和其他肿瘤中所展现出的抗肿瘤活性,而铂类类似物是这些肿瘤中最具活性的药物之一,这推动了紫杉醇/铂联合治疗方案的研发。由于已知这两类药物都会诱导细胞周期依赖性效应,并在细胞周期的特定阶段延迟细胞周期进程,因此在该联合用药的初始临床研究中纳入了对药物给药顺序依赖性的评估。为补充临床研究,使用L1210白血病细胞系在体外评估了顺序依赖性相互作用。仅当顺铂在紫杉醇之后给药时,紫杉醇与顺铂联合使用所产生的细胞毒性才比单独使用顺铂时显著增加。这个给药顺序明显优于相反顺序和同时给药。长春新碱和顺铂按顺序给药所得到的结果几乎相同。此外,采用顺铂与紫杉醇或长春新碱的最佳给药顺序进行的碱性洗脱研究表明,这些抗微管药物并不会比单独使用顺铂时增加更多由顺铂诱导的DNA链间交联和DNA - 蛋白质交联。虽然顺铂与抗微管药物之间顺序依赖性细胞毒性相互作用的机制尚未确定,但很可能是次优给药顺序产生了拮抗作用,这可能是由于细胞周期依赖性现象所致。

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