Abstract

The spread of antimicrobial resistance requires the development of novel strategies to combat superbugs. Bacteriolytic enzymes (enzybiotics) that selectively eliminate pathogenic bacteria, including resistant strains and biofilms, are attractive alternatives to antibiotics, also as a component of a new generation of antimicrobial wound dressings. AuresinePlus is a novel, engineered enzybiotic effective against Staphylococcus aureus—one of the most common pathogenic bacteria, found in infected wounds with a very high prevalence of antibiotic resistance. We took advantage of its potent lytic activity, selectivity, and safety to prepare a set of biodegradable PLGA/chitosan fibers generated by electrospinning. Our aim was to produce antimicrobial nonwovens to deliver enzybiotics directly to the infected wound and better control its release and activity. Three different methods of enzyme immobilization were tested: physical adsorption on the previously hydrolyzed surface, and covalent bonding formation using N-hydroxysuccinimide/N-(3-Dimethylaminopropyl)-N′-ethylcarbodiimide (NHS/EDC) or glutaraldehyde (GA). The supramolecular structure and functional properties analysis revealed that the selected methods resulted in significant development of nanofibers surface topography resulting in an efficient enzybiotic attachment. Both physically adsorbed and covalently bound enzymes (by NHS/EDC method) exhibited prominent antibacterial activity. Here, we present the extensive comparison between methods for the effective attachment of the enzybiotic to the electrospun nonwovens to generate biomaterials effective against antibiotic-resistant strains. Our intention was to present a comprehensive proof-of-concept study for future antimicrobial wound dressing development.

Highlights

  • Staphylococcus aureus (S. aureus) is one of the most common pathogenic bacteria isolated from infected wounds, and at the same time, one of the most difficult to treat [1,2]

  • There are antibacterial agents combined with wound dressing that are available for treatment, like antibiotics, silver particles, hydrogen peroxide, and iodinebased preparation

  • We observed that all methods caused significant changes in the structure and properties of poly(lactide-co-glycolide)/chitosan fibers and resulted in efficient enzyme immobilization

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Summary

Introduction

Staphylococcus aureus (S. aureus) is one of the most common pathogenic bacteria isolated from infected wounds, and at the same time, one of the most difficult to treat [1,2]. This is due to a very high level of antibiotic resistance among S. aureus strains [3,4], and because of their tendency to generate biofilms and form persistent cells [1,5,6,7]. Antimicrobial wound management is a major challenge that continues to require new solutions against microbes and their biofilms.

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