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Structure of the Tripartite Multidrug Efflux Pump AcrAB-TolC Suggests an Alternative Assembly Mode
Author(s) -
Jinsik Kim,
Hyeongseop Jeong,
Saemee Song,
HyeYeon Kim,
Kangseok Lee,
Jaekyung Hyun,
NamChul Ha
Publication year - 2015
Publication title -
molecules and cells
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.665
H-Index - 79
eISSN - 0219-1032
pISSN - 1016-8478
DOI - 10.14348/molcells.2015.2277
Subject(s) - efflux , escherichia coli , biology , transmembrane protein , fusion protein , bacterial outer membrane , microbiology and biotechnology , transport protein , inner membrane , protein structure , membrane transport protein , biophysics , membrane protein , biochemistry , membrane , recombinant dna , receptor , mitochondrion , gene
Escherichia coli AcrAB-TolC is a multidrug efflux pump that expels a wide range of toxic substrates. The dynamic nature of the binding or low affinity between the components has impeded elucidation of how the three components assemble in the functional state. Here, we created fusion proteins composed of AcrB, a transmembrane linker, and two copies of AcrA. The fusion protein exhibited acridine pumping activity, suggesting that the protein reflects the functional structure in vivo. To discern the assembling mode with TolC, the AcrBA fusion protein was incubated with TolC or a chimeric protein containing the TolC aperture tip region. Three-dimensional structures of the complex proteins were determined through transmission electron microscopy. The overall structure exemplifies the adaptor bridging model, wherein the funnel-like AcrA hexamer forms an intermeshing cogwheel interaction with the α-barrel tip region of TolC, and a direct interaction between AcrB and TolC is not allowed. These observations provide a structural blueprint for understanding multidrug resistance in pathogenic Gram-negative bacteria.

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