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(R)- and (S)-verapamil differentially modulate the multidrug-resistant protein MRP1.
Perrotton, Thomas; Trompier, Doriane; Chang, Xiu-Bao; Di Pietro, Attilio; Baubichon-Cortay, Hélène.
Affiliation
  • Perrotton T; Laboratoire des Protéines de Résistance aux Agents Chimiothérapeutiques, Institut de Biologie et Chimie des Protéines, UMR 5086, IFR 128 BioSciences Lyon-Gerland, CNRS/Université de Lyon, 69367 Lyon Cedex 07, France.
J Biol Chem ; 282(43): 31542-8, 2007 Oct 26.
Article in En | MEDLINE | ID: mdl-17646169
The multidrug-resistant protein MRP1 (involved in the cancer cell multidrug resistance phenotype) has been found to be modulated by racemic verapamil (through stimulation of glutathione transport), inducing apoptosis of human MRP1 cDNA-transfected baby hamster kidney 21 (BHK-21) cells and not of control BHK-21 cells. In this study, we show that the two enantiomers of verapamil have different effects on MRP1 activity. Only the S-isomer (not the R-isomer) potently induced the death of MRP1-transfected BHK-21 cells. The decrease in cellular glutathione content induced by the S-isomer, which was not observed with the R-isomer, was stronger than that induced by the racemic mixture, indicating that the R-isomer antagonized the S-isomer effect. Both enantiomers altered leukotriene C(4) and calcein transport by MRP1. Thus, the R-isomer behaved as an inhibitor, which was confirmed by its ability to revert the multidrug resistance phenotype toward vincristine. Molecular studies on purified MRP1 using fluorescence spectroscopy showed that both enantiomers bound to MRP1 with high affinity, with the binding being prevented by glutathione. Furthermore, conformational changes induced by the two enantiomers (monitored by sodium iodide accessibility of MRP1 tryptophan residues) were quite different, correlating with their distinct effects. (S)-Verapamil induces the death of potentially resistant tumor cells, whereas (R)-verapamil sensitizes MRP1-overexpressing cells to chemotherapeutics. These results might be of great potential interest in the design of new compounds able to modulate MRP1 in chemotherapy.
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Collection: 01-internacional Database: MEDLINE Main subject: Verapamil / Drug Resistance, Multiple / Multidrug Resistance-Associated Proteins Limits: Animals Language: En Journal: J Biol Chem Year: 2007 Document type: Article Affiliation country: France Country of publication: United States
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Collection: 01-internacional Database: MEDLINE Main subject: Verapamil / Drug Resistance, Multiple / Multidrug Resistance-Associated Proteins Limits: Animals Language: En Journal: J Biol Chem Year: 2007 Document type: Article Affiliation country: France Country of publication: United States