Sodium alginate/polycaprolactone co-axial wet-spun microfibers modified with N-carboxymethyl chitosan and the peptide AAPV for Staphylococcus aureus and human neutrophil elastase inhibition in potential chronic wound scenarios

Catarina S Miranda; A Francisca G Silva; Catarina L Seabra; Salette Reis; M Manuela P Silva; Sílvia M M A Pereira-Lima; Susana P G Costa; Natália C Homem; Helena P Felgueiras

doi:10.1016/j.bioadv.2023.213488

Sodium alginate/polycaprolactone co-axial wet-spun microfibers modified with N-carboxymethyl chitosan and the peptide AAPV for Staphylococcus aureus and human neutrophil elastase inhibition in potential chronic wound scenarios

Biomater Adv. 2023 Aug:151:213488. doi: 10.1016/j.bioadv.2023.213488. Epub 2023 Jun 1.

Authors

Catarina S Miranda¹, A Francisca G Silva², Catarina L Seabra³, Salette Reis⁴, M Manuela P Silva⁵, Sílvia M M A Pereira-Lima⁶, Susana P G Costa⁷, Natália C Homem⁸, Helena P Felgueiras⁹

Affiliations

¹ Centre for Textile Science and Technology (2C2T), University of Minho, Campus of Azurém, 4800-058 Guimarães, Portugal. Electronic address: catarina.miranda@2c2t.uminho.pt.
² Centre of Chemistry (CQ), University of Minho, Campus of Gualtar, 4710-057 Braga, Portugal. Electronic address: pg40181@alunos.uminho.pt.
³ Associate Laboratory for Green Chemistry (LAQV), Network of Chemistry and Technology (REQUIMTE), Department of Chemical Sciences, Faculty of Pharmacy, University of Porto, 4050-313 Porto, Portugal. Electronic address: cseabra@ff.up.pt.
⁴ Associate Laboratory for Green Chemistry (LAQV), Network of Chemistry and Technology (REQUIMTE), Department of Chemical Sciences, Faculty of Pharmacy, University of Porto, 4050-313 Porto, Portugal. Electronic address: shreis@ff.up.pt.
⁵ Centre of Chemistry (CQ), University of Minho, Campus of Gualtar, 4710-057 Braga, Portugal. Electronic address: nini@quimica.uminho.pt.
⁶ Centre of Chemistry (CQ), University of Minho, Campus of Gualtar, 4710-057 Braga, Portugal. Electronic address: silviap@quimica.uminho.pt.
⁷ Centre of Chemistry (CQ), University of Minho, Campus of Gualtar, 4710-057 Braga, Portugal. Electronic address: spc@quimica.uminho.pt.
⁸ Digital Transformation CoLab (DTx), Building 1, University of Minho, Campus of Azurém, 4800-058 Guimarães, Portugal. Electronic address: natalia.homem@dtx-colab.pt.
⁹ Centre for Textile Science and Technology (2C2T), University of Minho, Campus of Azurém, 4800-058 Guimarães, Portugal. Electronic address: helena.felgueiras@2c2t.uminho.pt.

PMID: 37285725
DOI: 10.1016/j.bioadv.2023.213488

Abstract

In chronic wound (CW) scenarios, Staphylococcus aureus-induced infections are very prevalent. This leads to abnormal inflammatory processes, in which proteolytic enzymes, such as human neutrophil elastase (HNE), become highly expressed. Alanine-Alanine-Proline-Valine (AAPV) is an antimicrobial tetrapeptide capable of suppressing the HNE activity, restoring its expression to standard rates. Here, we proposed the incorporation of the peptide AAPV within an innovative co-axial drug delivery system, in which the peptide liberation was controlled by N-carboxymethyl chitosan (NCMC) solubilization, a pH-sensitive antimicrobial polymer effective against Staphylococcus aureus. The microfibers' core was composed of polycaprolactone (PCL), a mechanically resilient polymer, and AAPV, while the shell was made of the highly hydrated and absorbent sodium alginate (SA) and NCMC, responsive to neutral-basic pH (characteristic of CW). NCMC was loaded at twice its minimum bactericidal concentration (6.144 mg/mL) against S. aureus, while AAPV was loaded at its maximum inhibitory concentration against HNE (50 μg/mL), and the production of fibers with a core-shell structure, in which all components could be detected (directly or indirectly), was confirmed. Core-shell fibers were characterized as flexible and mechanically resilient, and structurally stable after 28-days of immersion in physiological-like environments. Time-kill kinetics evaluations revealed the effective action of NCMC against S. aureus, while elastase inhibitory activity examinations proved the ability of AAPV to reduce HNE levels. Cell biology testing confirmed the safety of the engineered fiber system for human tissue contact, with fibroblast-like cells and human keratinocytes maintaining their morphology while in contact with the produced fibers. Data confirmed the engineered drug delivery platform as potentially effective for applications in CW care.

Keywords: Antibacterial effects; Controlled drug delivery; Core-shell microfibers; HNE inhibition; Therapeutic peptides; pH-sensitivity.

MeSH terms

Alginates / pharmacology
Chitosan* / chemistry
Chitosan* / pharmacology
Humans
Leukocyte Elastase / metabolism
Leukocyte Elastase / pharmacology
Peptides / pharmacology
Polymers / pharmacology
Staphylococcal Infections*
Staphylococcus aureus / metabolism
Valine / pharmacology
Wound Healing / drug effects
Wound Healing / physiology
Wounds and Injuries / complications
Wounds and Injuries / microbiology
Wounds and Injuries / therapy

Substances

Alginates
Chitosan
Leukocyte Elastase
Peptides
polycaprolactone
Polymers
Valine