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Small molecule probes of the receptor binding site in the Vibrio cholerae CAI-1 quorum sensing circuit.


ABSTRACT: Based on modification of separate structural features of the Vibrio cholerae quorum sensing signal, (S)-3-hydroxytridecan-4-one (CAI-1), three focused compound libraries have been synthesized and evaluated for biological activity. Modifications to the acyl tail and ?-hydroxy ketone typically provided agonists with activities correlated to tail length and conservative changes to the hydroxy ketone. Among the molecules identified within this collection of agonists is Am-CAI-1 (B11), which is among the most potent agonists reported to date with an EC(50) of 0.21 ?M. Modifications to the ethyl side chain delivered molecules with both agonist and antagonist activity, including m-OH-Ph-CAI-1 (C13) which is the most potent antagonist reported to date with an IC(50) of 36 ?M. The molecules described in this manuscript are anticipated to serve as valuable tools in the study of quorum sensing in Vibrio cholerae and provide new leads in the development of an antivirulence therapy against this human pathogen.

SUBMITTER: Bolitho ME 

PROVIDER: S-EPMC3673537 | biostudies-other | 2011 Nov

REPOSITORIES: biostudies-other

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Small molecule probes of the receptor binding site in the Vibrio cholerae CAI-1 quorum sensing circuit.

Bolitho Megan E ME   Perez Lark J LJ   Koch Matthew J MJ   Ng Wai-Leung WL   Bassler Bonnie L BL   Semmelhack Martin F MF  

Bioorganic & medicinal chemistry 20110917 22


Based on modification of separate structural features of the Vibrio cholerae quorum sensing signal, (S)-3-hydroxytridecan-4-one (CAI-1), three focused compound libraries have been synthesized and evaluated for biological activity. Modifications to the acyl tail and α-hydroxy ketone typically provided agonists with activities correlated to tail length and conservative changes to the hydroxy ketone. Among the molecules identified within this collection of agonists is Am-CAI-1 (B11), which is among  ...[more]

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