Haemodynamic effects of the bacterial quorum sensing signal molecule, N‐(3‐oxododecanoyl)‐L‐homoserine lactone, in conscious, normal and endotoxaemic rats

N‐acylhomoserine lactones (AHLs) are small, diffusible signalling molecules, employed by Gram‐negative bacteria to coordinate gene expression with cell population density. Recent in vitro findings indicate that AHLs may function as virulence determinants per se, through modification of cytokine prod...

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Published inBritish journal of pharmacology Vol. 133; no. 7; pp. 1047 - 1054
Main Authors Gardiner, S M, Chhabra, S R, Harty, C, Williams, P, Pritchard, D I, Bycroft, B W, Bennett, T
Format Journal Article
LanguageEnglish
Published Oxford, UK Blackwell Publishing Ltd 01.08.2001
Nature Publishing
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Summary:N‐acylhomoserine lactones (AHLs) are small, diffusible signalling molecules, employed by Gram‐negative bacteria to coordinate gene expression with cell population density. Recent in vitro findings indicate that AHLs may function as virulence determinants per se, through modification of cytokine production by eukaryotic cells, and by stimulating the relaxation of blood vessels. In the present study, we assessed the influence of AHLs on cardiovascular function in conscious rats, and draw attention to the ability of the N‐(3‐oxododecanoyl)‐L‐homoserine lactone (3‐oxo‐C12‐HSL), a signal molecule produced by P. aeruginosa, to cause marked bradycardia. This bradycardic effect was blocked by atropine and atenolol, and did not occur in vitro. Furthermore, modification of the acyl side chain length resulted in the loss of activity, whereas removal of the homoserine lactone ring, did not. The bradycardic effect of 3‐oxo‐C12‐HSL was also observed in endotoxaemic animals, albeit attenuated. In normal rats, 3‐oxo‐C12‐HSL caused initial mesenteric and hindquarters vasoconstriction, but only slight, and delayed signs of vasodilatation in the renal and mesenteric vascular beds. Furthermore, administration of 3‐oxo‐C12‐HSL (pre‐treatment or 2 h post‐treatment) together with LPS, did not modify the established regional haemodynamic effects of the LPS, 6 h after the onset of its infusion. Our observations do not provide any clear evidence for an ability of 3‐oxo‐C12‐HSL to modify the haemodynamic responses to LPS infusion. However, they are not inconsistent with the hypothesis that some of the cardiovascular sequelae of bacterial infection may be modulated by an influence of bacterial quorum sensing signalling molecules on the host. British Journal of Pharmacology (2001) 133, 1047–1054; doi:10.1038/sj.bjp.0704174
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ISSN:0007-1188
1476-5381
DOI:10.1038/sj.bjp.0704174