Role of drug transporters and drug accumulation in the temporal acquisition of drug resistance

Stacey L Hembruff,Monique L Laberge,David J Villeneuve,Baoqing Guo,Melanie Cecchetto,Amadeo M Parissenti,Zachary Veitch

doi:10.1186/1471-2407-8-318

Stacey L Hembruff, Monique L Laberge + Show 5 more

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https://doi.org/10.1186/1471-2407-8-318

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Abstract

BackgroundAnthracyclines and taxanes are commonly used in the treatment of breast cancer. However, tumor resistance to these drugs often develops, possibly due to overexpression of drug transporters. It remains unclear whether drug resistance in vitro occurs at clinically relevant doses of chemotherapy drugs and whether both the onset and magnitude of drug resistance can be temporally and causally correlated with the enhanced expression and activity of specific drug transporters. To address these issues, MCF-7 cells were selected for survival in increasing concentrations of doxorubicin (MCF-7DOX-2), epirubicin (MCF-7EPI), paclitaxel (MCF-7TAX-2), or docetaxel (MCF-7TXT). During selection cells were assessed for drug sensitivity, drug uptake, and the expression of various drug transporters.ResultsIn all cases, resistance was only achieved when selection reached a specific threshold dose, which was well within the clinical range. A reduction in drug uptake was temporally correlated with the acquisition of drug resistance for all cell lines, but further increases in drug resistance at doses above threshold were unrelated to changes in cellular drug uptake. Elevated expression of one or more drug transporters was seen at or above the threshold dose, but the identity, number, and temporal pattern of drug transporter induction varied with the drug used as selection agent. The pan drug transporter inhibitor cyclosporin A was able to partially or completely restore drug accumulation in the drug-resistant cell lines, but had only partial to no effect on drug sensitivity. The inability of cyclosporin A to restore drug sensitivity suggests the presence of additional mechanisms of drug resistance.ConclusionThis study indicates that drug resistance is achieved in breast tumour cells only upon exposure to concentrations of drug at or above a specific selection dose. While changes in drug accumulation and the expression of drug transporters does occur at the threshold dose, the magnitude of resistance cannot be attributed solely to changes in drug accumulation or the activity of drug transporters. The identities of these additional drug-transporter-independent mechanisms are discussed, including their likely clinical relevance.

Highlights

Introduction to resistance to anticancer agentsOncogene 2003, 22:7262-7264.5
This strongly suggests that the cell lines are isogenic and that the drug-resistant derivative cell lines do not stem from rare variants or contaminating cells within the population
A number of genes were upregulated or downregulated in the drug-resistant cell lines relative to MCF-7CC cells, but these were few in number and likely relate to changes in gene expression associated with the acquisition of drug resistance

Summary

Introduction

Introduction to resistance to anticancer agentsOncogene 2003, 22:7262-7264.5. Sparreboom A, Danesi R, Ando Y, Chan J, Figg WD: Pharmacogenomics of ABC transporters and its role in cancer chemotherapy. Six drug transporters have been shown to play a role in multidrug resistance in tumour cells in vitro These include ABCB1 (P-glycoprotein), ABCC1 (MRP1), ABCC2 (MRP2), ABCC4 (MRP4), ABCG2 (BCRP), and the lung resistance protein (LRP). Three are overexpressed in the large majority of tumour cell lines that have been successfully selected for resistance to anthracyclines and taxanes These include ABCB1, ABCC1, and ABCG2, and all play a role in reducing the ability of tumour cells to accumulate specific chemotherapy drugs [5,6]. These transporters are unique in their sequences, there is some overlap in the drugs that can be transported by each protein. While there is little direct evidence that the proteins can directly transport chemotherapy drugs, it has been shown that overexpression of LRP alters the subcellular distribution of doxorubicin, such that the drug localizes to cytoplasmic organelles rather than to DNA within the nucleus [28]

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