Reversal of C1300 murine neuroblastoma multidrug resistance by cremophorEL, a solvent for cyclosporin A.

Cancer biotherapy Pub Date : 1993-01-01 DOI:10.1089/cbr.1993.8.67

D S Chervinsky, M L Brecher, R M Baker, M J Hoelcle, C K Tebbi

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引用次数: 13

Abstract

We previously developed a homoharringtonine resistant C-1300 neuroblastoma cell line with cross-resistance to adriamycin and increased levels of p-glycoprotein, and showed that drug resistance could be reversed in this cell line by cyclosporin A. The present study shows that cremophor EL, a parenteral vehicle for cyclosporin A, can also completely reverse this multidrug resistance in a clonogenic assay system. Cremophor EL incubated with resistant cells for up to six days did not reduce levels of p-glycoprotein. Intracellular homoharringtonine analysis using HPLC revealed increased drug accumulation in resistant cells treated with cremophor EL. The increased drug level was not due to blocking of drug efflux commonly seen in other multidrug resistant models. The data suggest that resistance modulation with cyclosporin A should be interpreted with caution when cremophor EL is a solvent. Our work suggests cremophor EL, a relatively nontoxic lipophylic solvent, may have a direct effect on membrane permeability, although other mechanisms cannot be ruled out.

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环孢素a溶剂cremophorEL逆转C1300小鼠神经母细胞瘤多药耐药。

我们之前开发了一种对阿霉素交叉耐药且p-糖蛋白水平升高的C-1300神经母细胞瘤细胞系，并表明环孢素a可以逆转该细胞系的耐药性。本研究表明，环孢素a的肠外载体cremophor EL也可以在克隆测定系统中完全逆转这种多药耐药性。Cremophor EL与耐药细胞孵育长达6天，不降低p糖蛋白水平。用高效液相色谱法分析细胞内的高杉碱分析显示，用cremophor EL处理的耐药细胞中药物积累增加。增加的药物水平不是由于阻断药物外排常见的其他多药耐药模型。数据表明，当cremophor EL是溶剂时，应谨慎解释环孢素A的耐药性调节。我们的研究表明，cremophor EL是一种相对无毒的脂性溶剂，可能对膜通透性有直接影响，尽管不能排除其他机制。

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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Cancer biotherapy

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