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      The ATP-binding cassette transporter Cbc (choline/betaine/carnitine) recruits multiple substrate-binding proteins with strong specificity for distinct quaternary ammonium compounds

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          Summary

          We identified a choline, betaine and carnitine transporter, designated Cbc, from Pseudomonas syringae and Pseudomonas aeruginosa that is unusual among members of the ATP-binding cassette (ABC) transporter family in its use of multiple periplasmic substrate-binding proteins (SBPs) that are highly specific for their substrates. The SBP encoded by the cbcXWV operon, CbcX, binds choline with a high affinity ( K m, 2.6 μM) and, although it also binds betaine ( K m, 24.2 μM), CbcXWV-mediated betaine uptake did not occur in the presence of choline. The CbcX orthologue ChoX from Sinorhizobium meliloti was similar to CbcX in these binding properties. The core transporter CbcWV also interacts with the carnitine-specific SBP CaiX ( K m, 24 μM) and the betaine-specific SBP BetX ( K m, 0.6 μM). Unlike most ABC transporter loci, caiX, betX and cbcXWV are separated in the genome. CaiX-mediated carnitine uptake was reduced by CbcX and BetX only when they were bound by their individual ligands, providing the first in vivo evidence for a higher affinity for ligand-bound than ligand-free SBPs by an ABC transporter. These studies demonstrate not only that the Cbc transporter serves as a useful model for exploring ABC transporter component interactions, but also that the orphan SBP genes common to bacterial genomes can encode functional SBPs.

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          Author and article information

          Journal
          8712028
          5753
          Mol Microbiol
          Mol. Microbiol.
          Molecular microbiology
          0950-382X
          1365-2958
          6 May 2017
          17 November 2009
          January 2010
          10 July 2017
          : 75
          : 1
          : 29-45
          Affiliations
          [1 ]Department of Plant Pathology, Iowa State University, Ames, IA 50011, USA
          [2 ]Department of Microbiology and Immunology, Dartmouth Medical School, Hanover, NH 03755, USA
          [3 ]Department of Microbiology and Molecular Genetics, University of Vermont College of Medicine, Burlington, VT 05405, USA
          Author notes
          [* ]For correspondence: gbeattie@ 123456iastate.edu ; Tel. (+1) 515 294 5571; Fax (+1) 515 294 6019
          Article
          PMC5503199 PMC5503199 5503199 nihpa872723
          10.1111/j.1365-2958.2009.06962.x
          5503199
          19919675
          56bd06d1-794d-4141-8401-2e1d776f0af8
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