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Design and Engineering Strategies for Synthetic Antimicrobial Peptides

TOSSI, ALESSANDRO
2011
  • book part

Abstract
Thousands of antimicrobial peptides (AMPs) of prokaryotic, fungal, plant, or animal origin have been identified, and their potential as lead compounds for the design of novel therapeutic agents in the treatment of infection, for stimulating the immune system, or in countering septic shock has been widely recognized. Added to this is their possible use in prophylaxis of infectious diseases for animal or plant protection, for disinfection of surgical instruments or industrial surfaces, and for food preservation among other commercially important applications. Since the early eighties, AMPs have been subject to a vast number of studies aimed at understanding what determines their potency and spectrum of activities against bacterial or fungal pathogens, and at maximizing these while limiting cytotoxic activities toward host cells. Much research has also been directed toward understanding specific mechanisms of action underlying the antimicrobial activity and selectivity, to be able to redesign the peptides for optimal performance. A central theme in the mode of action of many AMPs is their dynamic interaction with biological membranes, which involves various properties of these peptides such as, among others, surface hydrophobicity and polarity, charge, structure, and induced conformational variations. These features are often intimately interconnected so that engineering peptides to independently adjust any one property in particular is not an easy task. However, solid-phase peptide synthesis allows the use of a large repertoire of nonproteinogenic amino acids that can be used in the rational design of peptides to finely tune structural and physicochemical properties and precisely probe structure–function relationships.
DOI
10.1007/978-1-4419-7692-5_6
WOS
WOS:000288921200006
Archivio
http://hdl.handle.net/11368/2856329
http://link.springer.com/book/10.1007/978-1-4419-7692-5
Diritti
metadata only access
Soggetti
  • antimicrobial peptide...

Web of Science© citazioni
11
Data di acquisizione
Mar 20, 2024
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