Skin 11β-hydroxysteroid dehydrogenase type 1 enzyme expression regulates burn wound healing and can be targeted to modify scar characteristics

Author:

Tsai Kevin H-Y12,Shi Huaikai2ORCID,Parungao Roxanne J2,Naficy Sina3,Ding Xiaotong4,Ding Xiaofeng5,Hew Jonathan J2,Wang Xiaosuo6,Chrzanowski Wojciech7,Lavery Gareth G8,Li Zhe9,Issler-Fisher Andrea C9,Chen Jun4,Tan Qian5,Maitz Peter K29,Cooper Mark S1,Wang Yiwei24ORCID

Affiliation:

1. The University of Sydney Adrenal Steroid Group, ANZAC Research Institute, Concord Hospital, , Sydney, NSW 2137, Australia

2. The University of Sydney Burns and Reconstructive Surgery Research Group, ANZAC Research Institute, Concord Hospital, , Sydney, NSW 2137, Australia

3. The University of Sydney School of Chemical and Biomolecular Engineering, , Sydney, NSW 2006, Australia

4. Nanjing University of Chinese Medicine Jiangsu Provincial Engineering Research Centre of TCM External Medication Development and Application, , Nanjing, Jiangsu, 210023, China

5. Nanjing University of Chinese Medicine Department of Burns and Plastic Surgery, Nanjing Drum Tower Hospital Clinical College, , Nanjing, Jiangsu, 210008, China

6. The University of Sydney Heart Research Institute, , Sydney, NSW 2006 , Australia

7. The University of Sydney Sydney Nano Institute, Sydney Pharmacy School, Faculty of Medicine and Health, , Sydney, NSW 2006, Australia

8. Nottingham Trent University Department of Biosciences, Centre for Healthy Ageing and Understanding Disease, , NG1 4BU, UK

9. Burns and Reconstructive Surgery Unit, Concord Repatriation General Hospital , Sydney, NSW 2137, Australia

Abstract

AbstractBackgroundExcessive scarring and fibrosis are the most severe and common complications of burn injury. Prolonged exposure to high levels of glucocorticoids detrimentally impacts on skin, leading to skin thinning and impaired wound healing. Skin can generate active glucocorticoids locally through expression and activity of the 11β-hydroxysteroid dehydrogenase type 1 enzyme (11β-HSD1). We hypothesised that burn injury would induce 11β-HSD1 expression and local glucocorticoid metabolism, which would have important impacts on wound healing, fibrosis and scarring. We additionally proposed that pharmacological manipulation of this system could improve aspects of post-burn scarring.MethodsSkin 11β-HSD1 expression in burns patients and mice was examined. The impacts of 11β-HSD1 mediating glucocorticoid metabolism on burn wound healing, scar formation and scar elasticity and quality were additionally examined using a murine 11β-HSD1 genetic knockout model. Slow-release scaffolds containing therapeutic agents, including active and inactive glucocorticoids, were developed and pre-clinically tested in mice with burn injury.ResultsWe demonstrate that 11β-HSD1 expression levels increased substantially in both human and mouse skin after burn injury. 11β-HSD1 knockout mice experienced faster wound healing than wild type mice but the healed wounds manifested significantly more collagen deposition, tensile strength and stiffness, features characteristic of excessive scarring. Application of slow-release prednisone, an inactive glucocorticoid, slowed the initial rate of wound closure but significantly reduced post-burn scarring via reductions in inflammation, myofibroblast generation, collagen production and scar stiffness.ConclusionsSkin 11β-HSD1 expression is a key regulator of wound healing and scarring after burn injury. Application of an inactive glucocorticoid capable of activation by local 11β-HSD1 in skin slows the initial rate of wound closure but significantlyimproves scar characteristics post burn injury.

Funder

National Health and Medical Research Council

National Science Foundation of China

Publisher

Oxford University Press (OUP)

Subject

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

Reference54 articles.

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2. The biology of burn injury;Evers;Exp Dermatol,2010

3. Comparative proteomic analysis of extracellular matrix proteins secreted by hypertrophic scar with normal skin fibroblasts;Ma;Burns & Trauma,2014

4. Patient experience of scar assessment and the use of scar assessment tools during burns rehabilitation: a qualitative study;Price;Burns Trauma,2021

5. Skin biomechanics: a potential therapeutic intervention target to reduce scarring;Hosseini;Burns Trauma,2022

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