Fluorescent light energy modulates healing in skin grafted mouse model

Author:

Ding Jie1,Mellergaard Maiken23,Zhu Zhensen1,Kwan Peter1,Edge Deirdre3,Ma Zengshuan1,Hebert Lise4,Alrobaiea Saad1,Iwasaki Takashi1,Nielsen Michael Canova Engelbrecht5,Tredget Edward E.6

Affiliation:

1. Wound Healing Research Group, Department of Surgery, Faculty of Medicine and Dentistry, University of Alberta, 161 HMRC , Edmonton , Canada

2. Department of Veterinary and Animal Sciences, Faculty of Health and Medical Sciences , University of Copenhagen , Denmark

3. Department of Research and Development, Klox Technologies Europe Ltd , Dublin , Ireland

4. Department of Research and Development, Klox Technologies Inc. , Laval , Canada

5. Department of Research and Development, Klox R&D Center, Guangdong Klox Biomedical Group Co., Ltd , Room 603, 6/F, Building 8, No. 6, Nanjiang Second Road, Zhujiang Street, Nansha District , Guangzhou , China

6. Divisions of Plastic and Reconstructive Surgery and Critical Care, 2D2.28 Walter C MacKenzie Health Sciences Centre & Wound Healing Research Group , 161 HMRC, Department of Surgery, University of Alberta , Edmonton , Alberta , Canada

Abstract

Abstract Skin grafting is often the only treatment for skin trauma when large areas of tissue are affected. This surgical intervention damages the deeper dermal layers of the skin with implications for wound healing and a risk of scar development. Photobiomodulation (PBM) therapy modulates biological processes in different tissues, with a positive effect on many cell types and pathways essential for wound healing. This study investigated the effect of fluorescent light energy (FLE) therapy, a novel type of PBM, on healing after skin grafting in a dermal fibrotic mouse model. Split-thickness human skin grafts were transplanted onto full-thickness excisional wounds on nude mice. Treated wounds were monitored, and excised xenografts were examined to assess healing and pathophysiological processes essential for developing chronic wounds or scarring. Results demonstrated that FLE treatment initially accelerated re-epithelialization and rete ridge formation, while later reduced neovascularization, collagen deposition, myofibroblast and mast cell accumulation, and connective tissue growth factor expression. While there was no visible difference in gross morphology, we found that FLE treatment promoted a balanced collagen remodeling. Collectively, these findings suggest that FLE has a conceivable effect at balancing healing after skin grafting, which reduces the risk of infections, chronic wound development, and fibrotic scarring.

Publisher

Walter de Gruyter GmbH

Subject

General Medicine

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