首页> 美国卫生研究院文献>British Journal of Cancer >A study of ethacrynic acid as a potential modifier of melphalan and cisplatin sensitivity in human lung cancer parental and drug-resistant cell lines.
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A study of ethacrynic acid as a potential modifier of melphalan and cisplatin sensitivity in human lung cancer parental and drug-resistant cell lines.

机译:乙ac酸作为人类肺癌亲本和耐药细胞系中美法仑和顺铂敏感性的潜在修饰剂的研究。

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摘要

We have studied alterations in glutathione (GSH) levels and glutathione-S-transferase (GST) activity in a series of in vitro derived multidrug resistant and cisplatin resistant sublines of the human lung cancer lines NCI-H69 (small cell), COR-L23 (large cell) and MOR (adenocarcinoma). We have also investigated the effects of ethacrynic acid, a putative inhibitor of GSTs, on levels of GSH and GST activity and on cellular sensitivity to melphalan and to cisplatin. Neither GSH content nor GST activity were significantly greater in the resistant sublines compared with their respective parental lines. The only effects of treating with ethacrynic acid at doses of 1 microgram ml-1 and 3 micrograms ml-1 for 2 h were a reduction in GSH content in the cisplatin resistant subline H69/CPR at the 3 micrograms ml-1 dose, and an increase to over 140% of control at 1 microgram ml-1 and 3 micrograms ml-1 in the MOR parental line (MOR/P) and at 1 microgram ml-1 in the multidrug resistant subline MOR/R. Exposure of parental line COR-L23/P to 3 micrograms ml-1 and 6 micrograms ml-1 of ethacrynic acid for 24 h, however, increased the GSH content to over 300% and 500% of control respectively. Variable effects of ethacrynic acid on GST activity were seen in these cell lines. Doses of 1 microgram ml-1 and 3 micrograms ml-1 reduced activity to 59% and 48% of control respectively in multidrug resistant subline H69/LX4. On the other hand, activity was increased in the cisplatin resistant subline H69/CPR (to 146% and 218% of control) and in MOR/P (to 117% and 137% of control) by 1 microgram ml-1 and 3 micrograms ml-1 respectively of ethacrynic acid. Addition of ethacrynic acid (3 micrograms ml-1) to treatment of the cell lines with melphalan or with cisplatin did not alter the dose-response curves to these agents.
机译:我们研究了人类肺癌细胞株NCI-H69(小细胞),COR-L23的一系列体外衍生的多药耐药和顺铂耐药亚系中谷胱甘肽(GSH)水平和谷胱甘肽S-转移酶(GST)活性的变化(大细胞)和MOR(腺癌)。我们还研究了推定的GST抑制剂乙炔酸对GSH和GST活性的水平以及对美法仑和顺铂的细胞敏感性的影响。与它们各自的亲本系相比,抗性亚系中的GSH含量和GST活性均没有显着增加。分别以1微克ml-1和3微克ml-1剂量的乙炔酸处理2小时的唯一效果是,以3微克ml-1剂量的顺铂耐药性亚株H69 / CPR的GSH含量降低,并且在MOR亲本系(MOR / P)中以1微克ml-1和3微克ml-1和在多药抗性亚系MOR / R中以1微克ml-1增加至对照的140%以上。将亲本系COR-L23 / P暴露于3微克ml-1和6微克ml-1的乙炔酸24小时,但是,GSH含量分别增加至对照的300%和500%以上。在这些细胞系中观察到了乙炔酸对GST活性的可变影响。在多药耐药性亚株H69 / LX4中,1微克ml-1和3微克ml-1的剂量分别将活性降低至对照组的59%和48%。另一方面,抗顺铂亚系H69 / CPR(分别为对照的146%和218%)和MOR / P(分别为对照的117%和137%)的活性分别增加了1微克ml-1和3微克。 ml-1分别为乙炔酸。将乙炔酸(3微克ml-1)加入用美法仑或顺铂处理细胞系不会改变这些试剂的剂量反应曲线。

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