RETENTION OF ACTIVITY BY SELECTED ANTHRACYCLINES IN A MULTIDRUG RESISTANT HUMAN LARGE CELL LUNG-CARCINOMA LINE WITHOUT P-GLYCOPROTEIN HYPEREXPRESSION

被引：67

作者：

COLEY, HM ^{[1
]}

WORKMAN, P ^{[1
]}

TWENTYMAN, PR ^{[1
]}

机构：

[1] MRC,CLIN ONCOL & RADIOTHERAPEUT UNIT,HILLS RD,CAMBRIDGE CB2 2QH,ENGLAND

来源：

BRITISH JOURNAL OF CANCER | 1991年 / 63卷 / 03期

关键词：

D O I：

10.1038/bjc.1991.84

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

A subline (COR-L23/R) of the human large cell lung cancer line COR-L23, derived by in vivo exposure to doxorubicin, exhibits an unusual multidrug resistant (MDR) phenotype. This subline shows cross-resistance to daunorubicin, vincristine, colchicine and etoposide but does not express P-glycoprotein. Interestingly, COR-L12/R shows little or no resistance to a range of structurally-modified analogues of doxorubicin comprising 9-alkyl and/or sugar modified anthracyclines. We have previously identified these same compounds as effective agents against P-glycoprotein-positive MDR cell lines. In contrast to typical MDR cell lines, COR-L12/R shows only minimal chemosensitisation by verapamil and no collateral sensitivity to verapamil. Compared to the parental cell line, COR-L12/R displays reduced accumulation of doxorubicin and daunorubicin. Accumulation defects were apparent only after 0.5-1 h of incubation of cells with these agents. The rate of daunorubicin efflux was shown to be enhanced by COR-L12/R and this efflux was demonstrated to be energy-dependent. The use of anthracyclines which retain activity in MDR cells thus appears to be a valid approach for the circumvention of MDR, not only in cells which express P-glycoprotein, but also where defective drug accumulation is due to other mechanisms possibly involving an alternative multidrug transporter.

引用

页码：351 / 357

页数：7

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