Skin biomechanics: a potential therapeutic intervention target to reduce scarring

Author:

Hosseini Motaharesadat12,Brown Jason34,Khosrotehrani Kiarash5,Bayat Ardeshir6789,Shafiee Abbas345ORCID

Affiliation:

1. Centre for Biomedical Technologies , School of Mechanical, Medical and Process Engineering (MMPE), Faculty of Engineering, , Brisbane, QLD 4059 , Australia

2. Queensland University of Technology , School of Mechanical, Medical and Process Engineering (MMPE), Faculty of Engineering, , Brisbane, QLD 4059 , Australia

3. Herston Biofabrication Institute, Metro North Hospital and Health Service , Brisbane, QLD 4029 , Australia

4. Royal Brisbane and Women's Hospital, Metro North Hospital and Health Service , Brisbane, QLD 4029 , Australia

5. The University of Queensland Diamantina Institute, Translational Research Institute, The University of Queensland , Brisbane, QLD 4102 , Australia

6. Centre for Dermatology Research , NIHR Manchester Biomedical Research Centre, Stopford Building, , Oxford Road, Manchester, M13 9PT , England, UK

7. University of Manchester , NIHR Manchester Biomedical Research Centre, Stopford Building, , Oxford Road, Manchester, M13 9PT , England, UK

8. MRC-SA Wound Healing Unit , Hair & Skin Research Laboratory, Division of Dermatology, , Cape Town 7935 , South Africa

9. University of Cape Town , Hair & Skin Research Laboratory, Division of Dermatology, , Cape Town 7935 , South Africa

Abstract

Abstract Pathological scarring imposes a major clinical and social burden worldwide. Human cutaneous wounds are responsive to mechanical forces and convert mechanical cues to biochemical signals that eventually promote scarring. To understand the mechanotransduction pathways in cutaneous scarring and develop new mechanotherapy approaches to achieve optimal scarring, the current study highlights the mechanical behavior of unwounded and scarred skin as well as intra- and extracellular mechanisms behind keloid and hypertrophic scars. Additionally, the therapeutic interventions that promote optimal scar healing by mechanical means at the molecular, cellular or tissue level are extensively reviewed. The current literature highlights the significant role of fibroblasts in wound contraction and scar formation via differentiation into myofibroblasts. Thus, understanding myofibroblasts and their responses to mechanical loading allows the development of new scar therapeutics. A review of the current clinical and preclinical studies suggests that existing treatment strategies only reduce scarring on a small scale after wound closure and result in poor functional and aesthetic outcomes. Therefore, the perspective of mechanotherapies needs to consider the application of both mechanical forces and biochemical cues to achieve optimal scarring. Moreover, early intervention is critical in wound management; thus, mechanoregulation should be conducted during the healing process to avoid scar maturation. Future studies should either consider combining mechanical loading (pressure) therapies with tension offloading approaches for scar management or developing more effective early therapies based on contraction-blocking biomaterials for the prevention of pathological scarring.

Funder

Metro North Hospital and Health Service

Publisher

Oxford University Press (OUP)

Subject

Critical Care and Intensive Care Medicine,Dermatology,Biomedical Engineering,Emergency Medicine,Immunology and Allergy,Surgery

Reference134 articles.

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