The myofibroblast in wound healing and fibrocontractive diseases

G Gabbiani

inflammation α-smooth muscle actin stress fibres TGF-β1 fibronectin tension

Key takeaways

01Fibroblasts can transform into contractile myofibroblasts
02These cells help pull wound edges together
03They also produce matrix components like collagen
04Their persistence can contribute to fibrotic diseases

Myofibroblasts help close wounds but can contribute to fibrosis and scarring if they don't disappear after healing is complete.

Abstract

The demonstration that fibroblastic cells acquire contractile features during the healing of an open wound, thus modulating into myofibroblasts, has open a new perspective in the understanding of mechanisms leading to wound closure and fibrocontractive diseases. Myofibroblasts synthesize extracellular matrix components such as collagen types I and III and during normal wound healing disappear by apoptosis when epithelialization occurs. The transition from fibroblasts to myofibroblasts is influenced by mechanical stress, TGF-beta and cellular fibronectin (ED-A splice variant). These factors also play important roles in the development of fibrocontractive changes, such as those observed in liver cirrhosis, renal fibrosis, and stroma reaction to epithelial tumours.

Cite this study

APA: G Gabbiani (2003). The myofibroblast in wound healing and fibrocontractive diseases. https://fasciaresearchdatabase.com/the-myofibroblast-in-wound-healing-and-fibrocontractive-diseases/
MLA: G Gabbiani. "The myofibroblast in wound healing and fibrocontractive diseases." 2003, https://fasciaresearchdatabase.com/the-myofibroblast-in-wound-healing-and-fibrocontractive-diseases/.
Chicago: G Gabbiani. 2003. "The myofibroblast in wound healing and fibrocontractive diseases.". https://fasciaresearchdatabase.com/the-myofibroblast-in-wound-healing-and-fibrocontractive-diseases/