The role of drug sequence in therapeutic selectivity of the combination of 5-fluorouracil and cis-platin.

S Palmeri, F Trave, O Russello, Y M Rustum
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引用次数: 12

Abstract

The therapeutic efficacy of 5-fluorouracil (FUra) and cis-dichlorodiamine-platinum (cis-DDP) in mice bearing transplantable leukemia and solid tumors was evaluated using different sequences of combination of these agents. The optimal sequence was cis-DDP administered 24 h after FUra. The administration of FUra at its maximally tolerated dose (MTD) followed 24 h later by low doses of cis-DDP yielded less toxicity and higher response rate against L1210 and colon 26 than the administration of these two agents in the opposite sequence or concurrently at the MTD. The sequence of administration of these two agents was not therapeutically important when the antitumor activity was evaluated against mice bearing lymphoma P388. These results indicate that the importance of sequencing of FUra and cis-DDP varies among different tumors. The biochemical basis for the therapeutic importance of sequencing in treatments with cis-DDP and FUra was investigated in mice bearing leukemia L1210 cells. While cis-DDP has no significant effects on the activity of thymidylate synthase (dTMP-S), the target enzyme for FUra action, recovery of dTMP-S inhibition following pretreatment with FUra was significantly delayed when cis-DDP was administered 12-24 h after the initial dose of FUra.

药物序列对5-氟尿嘧啶与顺铂联合治疗选择性的影响。
以5-氟尿嘧啶(FUra)和顺式二氯二胺-铂(cis-DDP)两种药物不同组合序列对移植性白血病和实体瘤小鼠的治疗效果进行了评价。最佳顺序为FUra后24 h给药顺式ddp。以最大耐受剂量(MTD)给药FUra, 24小时后再给低剂量cis-DDP,与以相反顺序或同时给药这两种药物相比,对L1210和结肠26的毒性更小,反应率更高。当对P388淋巴瘤小鼠进行抗肿瘤活性评估时,这两种药物的给药顺序在治疗上并不重要。这些结果表明,FUra和cis-DDP测序的重要性在不同的肿瘤中有所不同。在携带白血病L1210细胞的小鼠中,研究了测序在顺式ddp和FUra治疗中具有治疗意义的生化基础。虽然顺式ddp对胸苷酸合成酶(dmp - s) (FUra作用的靶酶)的活性没有显著影响,但在FUra初始剂量后12-24小时给药,顺式ddp对FUra预处理后dmp - s抑制的恢复明显延迟。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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