Pharmacological and molecular characterization of intrinsic and acquired doxorubicin resistance in murine tumor cell lines

We have studied the pharmacological parameters of doxorubicin resistance in three lines of murine cells selected by long-term culture in the presence of this drug or vincristine. A line originating from rat hepatoma spontaneously presented an intrinsic doxorubicin resistance as compared to the other...

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Bibliographic Details
Published in:Journal of cancer research and clinical oncology 1993-07, Vol.119 (9), p.527-532
Main Authors: Schott, B, Londos-Gagliardi, D, Ries, C, Huet, S, Robert, J
Format: Article
Language:English
Subjects:
Animals
ATP Binding Cassette Transporter, Subfamily B, Member 1
Blotting, Western
Carrier Proteins - physiology
Cell Division - drug effects
Doxorubicin - pharmacokinetics
Doxorubicin - pharmacology
Drug Interactions
Drug Resistance
Electrophoresis
Membrane Glycoproteins - physiology
Mice
Neoplasms, Experimental - drug therapy
Neoplasms, Experimental - metabolism
Neoplasms, Experimental - physiopathology
Rats
Tumor Cells, Cultured - drug effects
Verapamil - pharmacology
Vincristine - pharmacokinetics
Vincristine - pharmacology
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Summary:We have studied the pharmacological parameters of doxorubicin resistance in three lines of murine cells selected by long-term culture in the presence of this drug or vincristine. A line originating from rat hepatoma spontaneously presented an intrinsic doxorubicin resistance as compared to the other lines, originating from a rat glioblastoma and from simian-virus-40-transformed mouse hepatocytes. This intrinsic resistance, as well as the doxorubicin resistance exhibited by the vincristine-selected glioblastoma variant, could be entirely attribute to decreased drug accumulation due to drug efflux. In contrast, the doxorubicin-selected variants of the three lines exhibited an intracellular tolerance to this drug. Despite a reduction in drug accumulation when exposed to the same amount of doxorubicin, they accumulated 6-12 times more doxorubicin than wild lines when submitted to equitoxic exposures. Verapamil could restore in these lines the doxorubicin accumulation observed in sensitive lines but could not restore doxorubicin cytotoxicity. Quantitative evaluation of P-glycoprotein expression by Western blotting with the C219 antibody indicated that the wild hepatoma line overexpressed P-glycoprotein by a factor of 5 in comparison with the other wild lines, and that the vincristine-selected glioblastoma variant overexpressed this protein almost as much as the doxorubicin-selected variants. These observations favor the existence of P-glycoprotein-independent mechanisms of doxorubicin resistance, which are added to the classical multidrug-resistant phenotype in doxorubicin-selected highly resistant variant cell lines.
ISSN:0171-5216
1432-1335
DOI:10.1007/BF01686462