Action of Cis-dichlorodiammineplatinum(II) (NSC-119875) at ehe cellular level.

Cancer chemotherapy reports Pub Date : 1975-05-01
B Drewinko, J A Gottlieb
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引用次数: 0

Abstract

Asynchronous human lymphoma cells treated for 1 hour with increasing concentrations of cis-dichlorodiammineplatinum(II) revealed a marked decrease in survival as estimated by the colony-forming technique. When the treatmentwas extended for 8 hours at a concentration of 5micrograms/ml, a killing effect (greater than 3 log decades) was observed which was similar to that obtained when 50micrograms/ml is incubated with the cells for 1 hour. This finding suggests that better antitumor effects with fewer toxic effects may be obtained clinically by prolonged infusion of low doses of cis-dichlorodiammineplatinum (II). Synchronized lymphoma cells showed no significant degree of cell-cycle-stage sensitivity to cis-dichlorodiammineplatinum (II). The drug kills cells with similar efficiency in all stages of the cell cycle. No killing effect was elicited after incubation of the cells with spironolactone, a compound said to protect the kidneys from the toxic effects of heavy metals. However, simultaneous incubation of spironolactone and cis-dichlorodiammineplatinum (II) did not prevent the lethal action of the second drug. If spironolactone is proven to be an inhibitor of cis-dichlorodiammineplatinum (II) nephrotoxicity, it will become a valuable addition to the treatment of human neoplasia with this platinum compound. Lymphoma cells given a "priming" dose of 10 micrograms/ml of cis-dichlorodiammineplatinum (II) failed to repair the induced damage. A second exposure to 10 micrograms/ml of the drug at various subsequent intervals elicited greater killing effect than that produced by 20 micrograms/ml given at one time. A clear synergistic effect was noted when cis-dichlorodiammineplatinum (II) was given simultaneously with camptothecin or BCNU. The molecular mechanism by which this effect is accomplished is not presently apparent.

顺式二氯二胺铂(II)在细胞水平上的作用。
用增加浓度的顺式二氯二胺铂(II)治疗异步人淋巴瘤细胞1小时,通过集落形成技术估计,其存活率明显下降。以5微克/毫升的浓度处理8小时,观察到杀伤效果(大于3 log几十),与50微克/毫升的浓度与细胞孵育1小时的效果相似。这一发现表明,通过长时间输注低剂量顺式二氯二胺铂(II),可以在临床上获得更好的抗肿瘤效果和更少的毒性作用。同步淋巴瘤细胞对顺式二氯二胺铂(II)没有明显的细胞周期阶段敏感性。该药物在细胞周期的所有阶段杀死细胞的效率相似。用螺内酯(一种据说能保护肾脏免受重金属毒害的化合物)对细胞进行孵育后,没有产生杀伤作用。然而,螺内酯和顺式二氯二胺铂(II)同时孵育并不能阻止第二种药物的致死作用。如果螺内酯被证明是顺式二氯二胺铂(II)肾毒性的抑制剂,它将成为用这种铂化合物治疗人类肿瘤的有价值的补充。给予10微克/毫升顺式二氯二胺铂(II)“启动”剂量的淋巴瘤细胞不能修复诱导的损伤。在随后的不同时间间隔内,第二次暴露于10微克/毫升的药物,比一次暴露于20微克/毫升的药物产生更大的杀伤效果。顺式二氯二胺铂(II)与喜树碱或BCNU同时给予时,有明显的协同效应。实现这种效果的分子机制目前还不清楚。
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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