Journal article

The multidrug resistance protein is photoaffinity labeled by a quinoline-based drug at multiple sites

R Daoud, J Desneves, LW Deady, L Tilley, RJ Scheper, P Gros, E Georges

Biochemistry | AMER CHEMICAL SOC | Published : 2000

DOI: 10.1021/bi9922188

Abstract

Tumor cells overcome cytotoxic drug pressure by the overexpression of either or both transmembrane proteins, the P-glycoprotein (P-gp) and the multidrug resistance protein (MRP). The MRP has been shown to mediate the transport of cytotoxic natural products, in addition to glutathione-, glucuronidate-, and sulfate-conjugated cell metabolites. However, the mechanism of MRP drug binding and transport is at present not clear. In this study, we have used a photoreactive quinoline-based drug, N- (hydrocinchonidin-8'-yl)-4-azido-2-hydroxybenzamide (IACI), to show the photoaffinity labeling of the 190 kDa protein in membranes from the drug resistant SCLC H69/AR cells. The photoaffinity labeling of t..

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University of Melbourne Researchers

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Keywords

Mrp
32 Biomedical and Clinical Sciences
Science & Technology
31 Biological Sciences
Human Tumor-Cells
P-Glycoprotein
Cancer
Receptor Antagonist
Conjugate Export Pump
Biochemistry & Molecular Biology
3101 Biochemistry and Cell Biology
Gene Leads
Generic Health Relevance
Leukotriene C-4
Life Sciences & Biomedicine
Biotechnology
Plasma-Membrane
Increased Sensitivity
Pharmacological Characterization