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A Modified ToxT Inhibitor Reduces Vibrio cholerae Virulence in Vivo.


ABSTRACT: We have previously designed and synthesized small-molecule inhibitors that reduce Vibrio cholerae virulence in vitro by targeting the transcription factor ToxT. Here we report the synthesis and biological activity of derivatives of our previous bicyclic, fatty acid-like inhibitors. All of the synthesized derivatives show antivirulence activity in vitro. For the most potent compounds, a concentration of 5 ?M completely inhibited ToxT-mediated tcpA expression as measured in the ?-galactosidase assay. One indole compound, 3-(1-butyl-1 H-indol-7-yl)propanoic acid (8), was also effective at inhibiting intestinal colonization in the infant mouse. These modified compounds may serve as good candidates for further anti-cholera drug development.

SUBMITTER: Woodbrey AK 

PROVIDER: S-EPMC6528795 | biostudies-literature | 2018 Sep

REPOSITORIES: biostudies-literature

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A Modified ToxT Inhibitor Reduces Vibrio cholerae Virulence in Vivo.

Woodbrey Anne K AK   Onyango Evans O EO   Kovacikova Gabriela G   Kull F Jon FJ   Gribble Gordon W GW  

Biochemistry 20180912 38


We have previously designed and synthesized small-molecule inhibitors that reduce Vibrio cholerae virulence in vitro by targeting the transcription factor ToxT. Here we report the synthesis and biological activity of derivatives of our previous bicyclic, fatty acid-like inhibitors. All of the synthesized derivatives show antivirulence activity in vitro. For the most potent compounds, a concentration of 5 μM completely inhibited ToxT-mediated tcpA expression as measured in the β-galactosidase ass  ...[more]

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