A Review of the Evidence for and against a Role for Mast Cells in Cutaneous Scarring and Fibrosis

Traci A. Wilgus, Sara Ud-din, Ardeshir Bayat

Research output: Contribution to journalArticlepeer-review

Abstract

Scars are generated in mature skin as a result of the normal repair process, but the replacement of normal tissue with scar tissue can lead to biomechanical and functional deficiencies in the skin as well as psychological and social issues for patients that negatively affect quality of life. Abnormal scars, such as hypertrophic scars and keloids, and cutaneous fibrosis that develops in diseases such as systemic sclerosis and graft-versus-host disease can be even more challenging for patients. There is a large body of literature suggesting that inflammation promotes the deposition of scar tissue by fibroblasts. Mast cells represent one inflammatory cell type in particular that has been implicated in skin scarring and fibrosis. Most published studies in this area support a pro-fibrotic role for mast cells in the skin, as many mast cell-derived mediators stimulate fibroblast activity and studies generally indicate higher numbers of mast cells and/or mast cell activation in scars and fibrotic skin. However, some studies in mast cell-deficient mice have suggested that these cells may not play a critical role in cutaneous scarring/fibrosis. Here, we will review the data for and against mast cells as key regulators of skin fibrosis and discuss scientific gaps in the field.
Original languageEnglish
Article number9673
JournalInternational Journal of Molecular Sciences
Volume21
Issue number24
Early online date18 Dec 2020
DOIs
Publication statusPublished - 18 Dec 2020

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