Literature

Abstract

Multidrug-resistance (MDR) occurs in many bacterial species and tumour cells. MDR functions by membrane proteins which export drugs from cells, resulting in a low ineffective concentration of the drug. We have shown by molecular modelling that inhibitors of MDR have affinity for substrates of MDR transporters. This affinity may facilitate drug entry into cells and a large inhibitor-drug complex may be a poorer substrate for the MDR mechanism. This complex would effectively 'cloak' the drug rendering it unavailable for efflux.

DOI： 10.1016/j.bmcl.2003.12.015

Inhibitors of multidrug resistance (MDR) have affinity for MDR substrates

Bioorganic & Medicinal Chemistry Letters 2004.0

Evaluation of substrate and inhibitor properties of a novel MDR modulator H17 towards transmembrane efflux pumps

European Journal of Medicinal Chemistry 2009.0

Discovery of substituted 1,4-dihydroquinolines as novel class of ABCB1 modulators

Bioorganic & Medicinal Chemistry 2015.0

Functional characterization of the rat mdr1b encoded P-glycoprotein: not all inducing agents are substrates

Carcinogenesis 1997.0

Discovery of substituted 1,4-dihydroquinolines as novel promising class of P-glycoprotein inhibitors: First structure–activity relationships and bioanalytical studies

Bioorganic & Medicinal Chemistry Letters 2015.0

Inhibition of Bacterial Multidrug Resistance by Celecoxib, a Cyclooxygenase-2 Inhibitor