Targeting Myofibroblasts as a Treatment Modality for Dupuytren Disease

Mary E Ziegler; Andres Staben; Melinda Lem; Jason Pham; Leonardo Alaniz; Faris F Halaseh; Sabine Obagi; Amber Leis; Alan D Widgerow

doi:10.1016/j.jhsa.2023.06.007

Targeting Myofibroblasts as a Treatment Modality for Dupuytren Disease

J Hand Surg Am. 2023 Sep;48(9):914-922. doi: 10.1016/j.jhsa.2023.06.007. Epub 2023 Jul 20.

Authors

Mary E Ziegler¹, Andres Staben¹, Melinda Lem¹, Jason Pham¹, Leonardo Alaniz¹, Faris F Halaseh¹, Sabine Obagi¹, Amber Leis¹, Alan D Widgerow²

Affiliations

¹ Center for Tissue Engineering, Department of Plastic Surgery, University of California, Orange, CA.
² Center for Tissue Engineering, Department of Plastic Surgery, University of California, Orange, CA. Electronic address: [email protected].

PMID: 37480917
DOI: 10.1016/j.jhsa.2023.06.007

Abstract

Purpose: Currently, no treatment corrects the contractile nature of Dupuytren myofibroblasts (DMFs) or prevents recurrence following surgery. Antifibrotic and proadipogenic growth factors are released when adipose-derived stem cells (ASCs) are cultured with platelet-rich plasma (PRP), a platelet concentration from whole blood. Reprograming myofibroblasts into adipocytes via growth factors is proposed as a powerful potential tool to target fibrosis. We aimed to assess whether the combination of ASCs and PRP reprograms DMFs into adipocytes in vitro and alters their contractile nature in vivo.

Methods: Normal human dermal fibroblasts (NHDFs) and DMFs from Dupuytren patients were isolated and cocultured with ASCs and PRP either alone or together. Adipocytes were detected by Oil Red O and perilipin staining. DMFs and NHDFs were transplanted into the forepaws of rats (Rowett Nude [rnu/rnu]) and treated with saline, PRP+ASCs, or collagenase Clostridium histolyticum (clinical comparison) 2 months later. After 2 weeks, the tissue was harvested and subjected to Masson trichrome staining, and collagen I and III and alpha-smooth muscle actin detection by immunohistochemistry.

Results: Myofibroblasts transform into adipocytes upon coculture with PRP+ASCs. DMFs show increased alpha-smooth muscle actin expression in vivo compared with NHDFs, which is significantly decreased after PRP+ASCs and collagenase Clostridium histolyticum treatments. DMFs induce collagen I and III expressions in rat paws compared with NHDFs, with a type III to I ratio increase. Treatment with PRP+ASC reduced the ratio, but collagenase Clostridium histolyticum did not.

Conclusions: Treating DMFs with PRP+ASCs provides factors that induce myofibroblast to adipocyte transformation. This treatment reduces the contractile phenotype and fibrosis markers in vivo. Future studies should detail the mechanism of this conversion.

Clinical relevance: The combination of PRP and ASCs to induce the differentiation of DMFs into adipocytes may serve to limit surgery to a percutaneous contracture release and biological injection, rather than a moderate or radical fasciectomy, and reduce the recurrence of Dupuytren contracture.

Keywords: Adipose-derived stem cells; Dupuytren disease; fibrosis; myofibroblasts; platelet-rich plasma.

MeSH terms

Actins
Animals
Collagen Type I
Dupuytren Contracture* / therapy
Humans
Microbial Collagenase
Myofibroblasts
Rats

Substances

Microbial Collagenase
Actins
Collagen Type I