Abstract
New N-acyl homoserine lactone analogues, N-acyl-3-amino-5H-furanone derivatives and some 4-halogeno counterparts, were synthesised and tested for their ability to modulate LuxR-dependent bacterial quorum sensing. Both types of analogues proved to be inhibitors, the halogenated compounds being significantly more active. Molecular modelling suggested that the conjugated enamide group induces two preferential conformations leading to specific binding modes. In addition, the presence of the halogen atom could enhance the fitting of the lactone ring through specific interactions with strictly conserved or conservatively replaceable residues in the LuxR protein family, namely Asp79, Trp94 and Ile81.
Publication types
-
Research Support, Non-U.S. Gov't
MeSH terms
-
Acyl-Butyrolactones / chemical synthesis*
-
Acyl-Butyrolactones / chemistry
-
Acyl-Butyrolactones / pharmacology*
-
Aliivibrio fischeri / physiology
-
Furans / chemical synthesis*
-
Furans / chemistry
-
Furans / pharmacology*
-
Inhibitory Concentration 50
-
Models, Molecular
-
Molecular Structure
-
Quorum Sensing / drug effects*
-
Repressor Proteins* / antagonists & inhibitors
-
Repressor Proteins* / chemistry
-
Repressor Proteins* / metabolism
-
Structure-Activity Relationship
-
Trans-Activators* / antagonists & inhibitors
-
Trans-Activators* / chemistry
-
Trans-Activators* / metabolism
Substances
-
Acyl-Butyrolactones
-
Furans
-
Repressor Proteins
-
Trans-Activators
-
LuxR autoinducer binding proteins