The ever-faster rise of antimicrobial resistance (AMR) represents a major global Public Health challenge. New chemical entities with innovative Modes of Action (MoAs) are thus desirable. We recently reported the development of a novel class of broad-spectrum bactericidal agents, the AlkylGuanidino Ureas (AGU). Due to their polycationic structure, they likely target bacterial membranes. In order to better understand their MoA, we synthesized a library of AGU derivatives by structural simplification of selected hit compounds and developed specific assays based on membrane models by means of both analytical and computational techniques. Cell-based assays provided experimental evidence that AGUs disrupt bacterial membranes without showing hemolytic behavior. Hence, we herein report a thorough chemical and biological characterization of a new series of AGUs obtained through molecular simplification, allowing the rational design of potent antibacterial compounds active on antibiotic-resistant strains.
D'Agostino, I., Ardino, C., Poli, G., Sannio, F., Lucidi, M., Poggialini, F., et al. (2022). Antibacterial alkylguanidino ureas: Molecular simplification approach, searching for membrane-based MoA. EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY, 231, 1-23 [10.1016/j.ejmech.2022.114158].
Antibacterial alkylguanidino ureas: Molecular simplification approach, searching for membrane-based MoA
Sannio F.;Poggialini F.;Rango E.;Petricci E.;Docquier J. -D.;Dreassi E.
2022-01-01
Abstract
The ever-faster rise of antimicrobial resistance (AMR) represents a major global Public Health challenge. New chemical entities with innovative Modes of Action (MoAs) are thus desirable. We recently reported the development of a novel class of broad-spectrum bactericidal agents, the AlkylGuanidino Ureas (AGU). Due to their polycationic structure, they likely target bacterial membranes. In order to better understand their MoA, we synthesized a library of AGU derivatives by structural simplification of selected hit compounds and developed specific assays based on membrane models by means of both analytical and computational techniques. Cell-based assays provided experimental evidence that AGUs disrupt bacterial membranes without showing hemolytic behavior. Hence, we herein report a thorough chemical and biological characterization of a new series of AGUs obtained through molecular simplification, allowing the rational design of potent antibacterial compounds active on antibiotic-resistant strains.File | Dimensione | Formato | |
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https://hdl.handle.net/11365/1196857