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10.1128/mSphereDirect.00375-17

http://scihub22266oqcxt.onion/10.1128/mSphereDirect.00375-17
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C5615136!5615136!28959742
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suck abstract from ncbi


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pmid28959742      mSphere 2017 ; 2 (5): ä
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  • The Biofilm Inhibitor Carolacton Enters Gram-Negative Cells: Studies Using a TolC-Deficient Strain of Escherichia coli #MMPMID28959742
  • Donner J; Reck M; Bunk B; Jarek M; App CB; Meier-Kolthoff JP; Overmann J; Müller R; Kirschning A; Wagner-Döbler I; Kreikemeyer B; Biswas I; Misra R
  • mSphere 2017[Sep]; 2 (5): ä PMID28959742show ga
  • The emergence of pathogens resistant against most or all of the antibiotics currently used in human therapy is a global threat, and therefore the search for antimicrobials with novel targets and modes of action is of utmost importance. The myxobacterial secondary metabolite carolacton had previously been shown to inhibit biofilm formation and growth of streptococci. Here, we investigated if carolacton could act against Gram-negative bacteria, which are difficult targets because of their double-layered cytoplasmic envelope. We found that the model organism Escherichia coli is susceptible to carolacton, similar to the Gram-positive Streptococcus pneumoniae, if its multidrug efflux system AcrAB-TolC is either inactivated genetically, by disruption of the tolC gene, or physiologically by coadministering an efflux pump inhibitor. A carolacton epimer that has a different steric configuration at carbon atom 9 is completely inactive, suggesting that carolacton may interact with the same molecular target in both Gram-positive and Gram-negative bacteria.
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