Loh S Y, Mistry P, Kelland L R, Abel G, Harrap K R
Drug Development Section, Institute of Cancer Research, Belmont, Sutton, Surrey, UK.
Br J Cancer. 1992 Dec;66(6):1109-15. doi: 10.1038/bjc.1992.419.
Acquired resistance to cisplatin (cis-diamminedichloroplatinum (II)) has been generated in vitro in the 41M human ovarian carcinoma cell line, established from a previously untreated patient. Three cisplatin-resistant variants were selected at approximately 2, 4 and 6-fold resistance (in terms of 50% inhibitory concentrations), in order to study the underlying mechanisms of acquired cisplatin resistance. Compared to the parent line, platinum accumulation following exposure to equimolar concentrations of cisplatin was on average (across the entire concentration range) 2.9, 3.6 and 4.8-fold lower in the 41McisR2, 41McisR4 and 41McisR6 cell lines, respectively. Thus the difference in uptake corresponded closely with their resistance factor in the three resistant variants. Moreover, a significant reduction in platinum accumulation was observed as early as 5 min after exposure to cisplatin in the 41M vs 41McisR6 cell lines. Platinum accumulation was similar in all cell lines following exposure to equitoxic concentrations (2 h IC50) of cisplatin. Enhanced efflux of drug was not observed between the 41M and 41McisR6 cells. In addition, there was no difference in intracellular glutathione (GSH) levels. Our previous studies have shown no indication of metallothionein involvement and the decrease in cisplatin uptake in the 41McisR6 cells was reflected by a similar reduction in DNA interstrand cross-links (ISC) formation. These results suggest that the mechanism of acquired resistance to cisplatin in the 41McisR6 cell line may be predominantly due to reduced drug uptake. The 41McisR6 cells were not found to be cross-resistant to ouabain, a postulated specific inhibitor of sodium-potassium adenosine triphosphatase (Na+, K(+)-ATPase), suggesting that decreased cisplatin accumulation in these cells is probably not regulated by alterations in their Na+, K(+)-ATPase levels, and Na+ potential across the plasma membrane. Cellular accumulation of a novel class of platinum (IV) ammine/cyclohexylamine dicarboxylates, which exhibit enhanced cytotoxicity over cisplatin and completely circumvent resistance to cisplatin in the 41McisR line, was also examined. The data suggests that increased accumulation of these compounds, as a result of their enhanced lipophilicity, could account for the dramatic increase in their potency over cisplatin.
在源自一名未经治疗患者的41M人卵巢癌细胞系中,已在体外诱导出对顺铂(顺二氨二氯铂(II))的获得性耐药。选择了三种对顺铂耐药的变体,其耐药倍数分别约为2倍、4倍和6倍(以50%抑制浓度计),以研究获得性顺铂耐药的潜在机制。与亲本细胞系相比,在41McisR2、41McisR4和41McisR6细胞系中,暴露于等摩尔浓度顺铂后铂的积累平均(在整个浓度范围内)分别低2.9倍、3.6倍和4.8倍。因此,摄取差异与这三种耐药变体中的耐药因子密切相关。此外,在41M细胞系与41McisR6细胞系中,早在暴露于顺铂5分钟后就观察到铂积累显著减少。暴露于等毒性浓度(2小时IC50)的顺铂后,所有细胞系中的铂积累相似。在41M细胞与41McisR6细胞之间未观察到药物外排增强。此外,细胞内谷胱甘肽(GSH)水平没有差异。我们之前的研究未显示金属硫蛋白参与的迹象,41McisR6细胞中顺铂摄取的减少反映在DNA链间交联(ISC)形成的类似减少上。这些结果表明,41McisR6细胞系中获得性顺铂耐药的机制可能主要是由于药物摄取减少。未发现41McisR6细胞对哇巴因(一种假定的钠钾腺苷三磷酸酶(Na +,K(+)-ATPase)特异性抑制剂)有交叉耐药性,这表明这些细胞中顺铂积累的减少可能不受其Na +,K(+)-ATPase水平和质膜上Na +电位变化的调节。还研究了一类新型铂(IV)氨/环己胺二羧酸盐的细胞积累情况,这类化合物比顺铂具有更强的细胞毒性,并且在41McisR细胞系中完全规避了对顺铂的耐药性。数据表明,由于这些化合物亲脂性增强,其积累增加可能解释了它们相对于顺铂效力的显著提高。
