The rapid development of antimicrobial resistance is pushing the search in the discovering of novel antimicrobial molecules to prevent and treat bacterial infections. Self-assembling antimicrobial peptides, as the lipidated peptides, are a novel and promising class of molecules capable of meeting this need. Based on previous work on Temporin L analogs, several new molecules lipidated at the N- or and the C-terminus were synthesised. Our goal is to improve membrane interactions through finely tuning self-assembly to reduce oligomerisation in aqueous solution and enhance self-assembly in bacterial membranes while reducing toxicity against human cells. The results here reported show that the length of the aliphatic moiety is a key factor to control target cell specificity and the oligomeric state of peptides either in aqueous solution or in a membrane-mimicking environment. The results of this study pave the way for the design of novel molecules with enhanced activities.

Novel temporin L antimicrobial peptides: promoting self-assembling by lipidic tags to tackle superbugs / Bellavita, R.; Falanga, A.; Buommino, E.; Merlino, F.; Casciaro, B.; Cappiello, F.; Mangoni, M. L.; Novellino, E.; Catania, M. R.; Paolillo, R.; Grieco, P.; Galdiero, S.. - In: JOURNAL OF ENZYME INHIBITION AND MEDICINAL CHEMISTRY. - ISSN 1475-6366. - 35:1(2020), pp. 1751-1764. [10.1080/14756366.2020.1819258]

Novel temporin L antimicrobial peptides: promoting self-assembling by lipidic tags to tackle superbugs

Bellavita R.
Primo
;
Falanga A.
Secondo
;
Buommino E.;Merlino F.;Novellino E.;Catania M. R.;Paolillo R.;Grieco P.
Penultimo
;
Galdiero S.
Ultimo
2020

Abstract

The rapid development of antimicrobial resistance is pushing the search in the discovering of novel antimicrobial molecules to prevent and treat bacterial infections. Self-assembling antimicrobial peptides, as the lipidated peptides, are a novel and promising class of molecules capable of meeting this need. Based on previous work on Temporin L analogs, several new molecules lipidated at the N- or and the C-terminus were synthesised. Our goal is to improve membrane interactions through finely tuning self-assembly to reduce oligomerisation in aqueous solution and enhance self-assembly in bacterial membranes while reducing toxicity against human cells. The results here reported show that the length of the aliphatic moiety is a key factor to control target cell specificity and the oligomeric state of peptides either in aqueous solution or in a membrane-mimicking environment. The results of this study pave the way for the design of novel molecules with enhanced activities.
2020
Novel temporin L antimicrobial peptides: promoting self-assembling by lipidic tags to tackle superbugs / Bellavita, R.; Falanga, A.; Buommino, E.; Merlino, F.; Casciaro, B.; Cappiello, F.; Mangoni, M. L.; Novellino, E.; Catania, M. R.; Paolillo, R.; Grieco, P.; Galdiero, S.. - In: JOURNAL OF ENZYME INHIBITION AND MEDICINAL CHEMISTRY. - ISSN 1475-6366. - 35:1(2020), pp. 1751-1764. [10.1080/14756366.2020.1819258]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11588/824699
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