Porcine‐derived collagen peptides promote re‐epithelialisation through activation of integrin signalling

Author:

Mistry Krishan12ORCID,Richardson Grant13ORCID,Vleminckx Sara4ORCID,Smith Robert13ORCID,Gevaert Elien4ORCID,Lovat Penny E.13ORCID

Affiliation:

1. Translational and Clinical Research Institute, Newcastle University Newcastle upon Tyne Tyne and Wear UK

2. Department of Materials, University of Manchester Manchester Greater Manchester United Kingdom of Great Britain and Northern Ireland

3. AMLo Biosciences Newcastle upon Tyne Tyne and Wear UK

4. Rousselot Ghent Belgium

Abstract

AbstractChronic non‐healing cutaneous wounds represent a major burden to patients and healthcare providers worldwide, emphasising the continued unmet need for credible and efficacious therapeutic approaches for wound healing. We have recently shown the potential for collagen peptides to promote proliferation and migration during cutaneous wound healing. In the present study, we demonstrate that the application of porcine‐derived collagen peptides significantly increases keratinocyte and dermal fibroblast expression of integrin α2β1 and activation of an extracellular signal‐related kinase (ERK)‐focal adhesion kinase (FAK) signalling cascade during wound closure in vitro. SiRNA‐mediated knockdown of integrin β1 impaired porcine‐derived collagen peptide‐induced wound closure and activation of ERK‐FAK signalling in keratinocytes but did not impair ERK or FAK signalling in dermal fibroblasts, implying the activation of differing downstream signalling pathways. Studies in ex vivo human 3D skin equivalents subjected to punch biopsy‐induced wounding confirmed the ability of porcine‐derived collagen peptides to promote wound closure by enhancing re‐epithelialisation. Collectively, these data highlight the translational and clinical potential for porcine‐derived collagen peptides as a viable therapeutic approach to promote re‐epithelialisation of superficial cutaneous wounds.

Publisher

Wiley

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