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Effect of adenoviral mediated overexpression of fibromodulin on human dermal fibroblasts and scar formation in full-thickness incisional wounds
Authors:Alexander Stoff  Angel A. Rivera  J. Michael Mathis  Steven T. Moore  N. S. Banerjee  Maaike Everts  Antonio Espinosa-de-los-Monteros  Zdenek Novak  Luis O. Vasconez  Thomas R. Broker  Dirk F. Richter  Dale Feldman  Gene P. Siegal  Mariam A. Stoff-Khalili  David T. Curiel
Affiliation:Division of Human Gene Therapy, Gene Therapy Center, University of Alabama at Birmingham, 901 19th Street South, BMR2 502, Birmingham, AL, 35294-2172, USA.
Abstract:Fibromodulin, a member of the small leucine-rich proteoglycan family, has been recently suggested as a biologically significant mediator of fetal scarless repair. To assess the role of fibromodulin in the tissue remodeling, we constructed an adenoviral vector expressing human fibromodulin cDNA. We evaluated the effect of adenovirus-mediated overexpression of fibromodulin in vitro on transforming growth factors and metalloproteinases in fibroblasts and in vivo on full-thickness incisional wounds in a rabbit model. In vitro, we found that Ad-Fibromodulin induced a decrease of expression of TGF-β1 and TGF-β2 precursor proteins, but an increase in expression of TGF-β3 precursor protein and TGF-β type II receptor. In addition, fibromodulin overexpression resulted in decreased MMP-1 and MMP-3 protein secretion but increased MMP-2, TIMP-1, and TIMP-2 secretion, whereas MMP-9 and MMP-13 were not influenced by fibromodulin overexpression. In vivo evaluation by histopathology and tensile strength demonstrated that Ad-Fibromodulin administration could ameliorate wound healing in incisional wounds. In conclusion, although the mechanism of scar formation in adult wounds remains incompletely understood, we found that fibromodulin overexpression improves wound healing in vivo, suggesting that fibromodulin may be a key mediator in reduced scarring.
Contact Information Mariam A. Stoff-KhaliliEmail:
Keywords:Adenovirus  Fibromodulin  Wound healing  Dermal fibroblasts  Scar formation  Transforming growth factor-β    Matrix metalloproteinases  Tissue-derived inhibitors of matrix metalloproteinase
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