2004
DOI: 10.1039/b412802h
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Synthesis and stability of small molecule probes for Pseudomonas aeruginosa quorum sensing modulation

Abstract: The human pathogen Pseudomonas aeruginosa uses N-butyryl-L-homoserine lactone (BHL) and N-(3-oxododecanyl)-L-homoserine lactone (OdDHL) as small molecule intercellular signals in a phenomenon known as quorum sensing (QS). QS modulators are effective at attenuating P. aeruginosa virulence; therefore, they are a potential new class of antibacterial agent. The lactone in BHL and OdDHL is hydrolysed under physiological conditions. The hydrolysis proceeds at a rate faster than racemisation of the alpha-chiral centr… Show more

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Cited by 85 publications
(95 citation statements)
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“…AHL B2 is unique, as this D-AHL displays strong agonistic activity and its L-stereoisomer, control AHL 5, is virtually inactive in LasR (but is a moderate to strong antagonist in LuxR and TraR, respectively). This trend is opposite to what has been observed for native AHL ligands, for which the Lstereoisomer is an active agonist and the D-stereoisomer is almost inactive; [17,20] we observed this latter trend in the current study for OOHL (1). The reasons behind this trend reversal for B2 remain unclear, and in view of the complex antagonistic activity trends displayed by the limited set of D enantiomers in library B, suggest that lactone stereochemistry will be an important feature to probe in the future design of AHL-derived QS modulators.…”
Section: Primary Assay Data and Sar For Library Bcontrasting
confidence: 46%
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“…AHL B2 is unique, as this D-AHL displays strong agonistic activity and its L-stereoisomer, control AHL 5, is virtually inactive in LasR (but is a moderate to strong antagonist in LuxR and TraR, respectively). This trend is opposite to what has been observed for native AHL ligands, for which the Lstereoisomer is an active agonist and the D-stereoisomer is almost inactive; [17,20] we observed this latter trend in the current study for OOHL (1). The reasons behind this trend reversal for B2 remain unclear, and in view of the complex antagonistic activity trends displayed by the limited set of D enantiomers in library B, suggest that lactone stereochemistry will be an important feature to probe in the future design of AHL-derived QS modulators.…”
Section: Primary Assay Data and Sar For Library Bcontrasting
confidence: 46%
“…[18] The effect of lactone stereochemistry on R protein activation had only been examined for a limited set of native AHLs, [20] and to our knowledge, had yet to be examined in synthetic AHL antagonists. [17] (We note, however, that many synthetic AHLs have been tested in racemic form, or their reported stereochemistry was not explicit, which adds additional complexity to this analysis. [9][10][11][13][14][15][16]) Lastly, the roles of acyl group aromaticity and spacer length on ligand activity, specifically in our antagonists 8 and 9, were unknown.…”
Section: Design Of Ahl Library Bmentioning
confidence: 99%
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“…38 Briefly, a drop of the AHL previously extracted by LL-extraction method as described as the above section was placed on one of the KBr grid/ plates. Then, the second plate was placed on top and subjected to IR (Brauker Tensor 70 FT-IR Spector-photometer).…”
Section: Determination Of Ahl Functional Groupsmentioning
confidence: 99%
“…Spring and co-workers described the total synthesis of 3-oxo-C 12 -AHL and also reported four 3-oxo-C 12 -AHL analogs 47-48b having various nonhydrolysable cyclic ketone and lactone rings along with changes at the acyl side chain as LasR inhibitors. 94,95 Cyclic ketones, 48a, 48b were found to reduce immunomodulatory responses (for e.g., TNFα factor and nitric oxide production) ( Figure 10). Muh et al screened a library of 200,000 compounds using ultra-high-throughput-cell based screening and identified two LasR inhibitors having a phenyl (49) and tetrazole ring (50) connected to 12 carbon aliphatic chain similar to 3-oxo-C 12 -AHL ( Figure 11).…”
Section: Inhibitors Targeting the Receptormentioning
confidence: 99%