Altering the communication networks of multispecies microbial systems using a diverse toolbox of AI-2 analogues.

نویسندگان

  • Sonja Gamby
  • Varnika Roy
  • Min Guo
  • Jacqueline A I Smith
  • Jingxin Wang
  • Jessica E Stewart
  • Xiao Wang
  • William E Bentley
  • Herman O Sintim
چکیده

There have been intensive efforts to find small molecule antagonists for bacterial quorum sensing (QS) mediated by the "universal" QS autoinducer, AI-2. Previous work has shown that linear and branched acyl analogues of AI-2 can selectively modulate AI-2 signaling in bacteria. Additionally, LsrK-dependent phosphorylated analogues have been implicated as the active inhibitory form against AI-2 signaling. We used these observations to synthesize an expanded and diverse array of AI-2 analogues, which included aromatic as well as cyclic C-1-alkyl analogues. Species-specific analogues that disrupted AI-2 signaling in Escherichia coli and Salmonella typhimurium were identified. Similarly, analogues that disrupted QS behaviors in Pseudomonas aeruginosa were found. Moreover, we observed a strong correlation between LsrK-dependent phosphorylation of these acyl analogues and their ability to suppress QS. Significantly, we demonstrate that these analogues can selectively antagonize QS in single bacterial strains in a physiologically relevant polymicrobial culture.

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عنوان ژورنال:
  • ACS chemical biology

دوره 7 6  شماره 

صفحات  -

تاریخ انتشار 2012