Pyridylpiperazine-based allosteric inhibitors of RND-type multidrug efflux pumps.
Coline PléHeng-Keat TamAnais Vieira Da CruzNina CompagneJuan-Carlos Jiménez-CastellanosReinke T MüllerElizabeth PradelWuen Ee FoongGiuliano MallociAlexia BalléeMoritz A KirchnerParisa MoshfeghAdrien HerledanAndrea HerrmannBenoit DeprezNicolas WillandAttilio Vittorio VargiuKlaas Martinus PosMarion FlipoRuben Christiaan HartkoornPublished in: Nature communications (2022)
Efflux transporters of the RND family confer resistance to multiple antibiotics in Gram-negative bacteria. Here, we identify and chemically optimize pyridylpiperazine-based compounds that potentiate antibiotic activity in E. coli through inhibition of its primary RND transporter, AcrAB-TolC. Characterisation of resistant E. coli mutants and structural biology analyses indicate that the compounds bind to a unique site on the transmembrane domain of the AcrB L protomer, lined by key catalytic residues involved in proton relay. Molecular dynamics simulations suggest that the inhibitors access this binding pocket from the cytoplasm via a channel exclusively present in the AcrB L protomer. Thus, our work unveils a class of allosteric efflux-pump inhibitors that likely act by preventing the functional catalytic cycle of the RND pump.