Biomechanical Regulatory Factors and Therapeutic Targets in Keloid Fibrosis

Fan Feng(Chongqing University of Technology), Mingying Liu(Xihua University), Lianhong Pan(Chongqing University of Technology), Jiaqin Wu(Chongqing University of Technology), Chunli Wang(Chongqing University of Technology), Yang Li(Chongqing University of Technology), Wanqian Liu(Chongqing University of Technology), Wei Xu(First People's Hospital of Chongqing), Mingxing Lei(Chongqing University of Technology)
Frontiers in Pharmacology
May 9, 2022
Cited by 59Open Access
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Abstract

Keloids are fibroproliferative skin disorder caused by abnormal healing of injured or irritated skin and are characterized by excessive extracellular matrix (ECM) synthesis and deposition, which results in excessive collagen disorders and calcinosis, increasing the remodeling and stiffness of keloid matrix. The pathogenesis of keloid is very complex, and may include changes in cell function, genetics, inflammation, and other factors. In this review, we aim to discuss the role of biomechanical factors in keloid formation. Mechanical stimulation can lead to excessive proliferation of wound fibroblasts, deposition of ECM, secretion of more pro-fibrosis factors, and continuous increase of keloid matrix stiffness. Matrix mechanics resulting from increased matrix stiffness further activates the fibrotic phenotype of keloid fibroblasts, thus forming a loop that continuously invades the surrounding normal tissue. In this process, mechanical force is one of the initial factors of keloid formation, and matrix mechanics leads to further keloid development. Next, we summarized the mechanotransduction pathways involved in the formation of keloids, such as TGF-β/Smad signaling pathway, integrin signaling pathway, YAP/TAZ signaling pathway, and calcium ion pathway. Finally, some potential biomechanics-based therapeutic concepts and strategies are described in detail. Taken together, these findings underscore the importance of biomechanical factors in the formation and progression of keloids and highlight their regulatory value. These findings may help facilitate the development of pharmacological interventions that can ultimately prevent and reduce keloid formation and progression.


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