Cartilage oligomeric matrix protein expression in systemic sclerosis reveals heterogeneity of dermal fibroblast responses to transforming growth factor {beta}

doi:10.1136/ard.2007.086850

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Published Online First: 13 April 2008. doi:10.1136/ard.2007.086850
Annals of the Rheumatic Diseases 2009;68:435-441

BASIC AND TRANSLATIONAL RESEARCH

Cartilage oligomeric matrix protein expression in systemic sclerosis reveals heterogeneity of dermal fibroblast responses to transforming growth factor β

G Farina, R Lemaire, P Pancari, J Bayle, R L Widom, R Lafyatis

Rheumatology Section, Department of Medicine, Boston University School of Medicine, Boston, Massachusetts, USA

R Lafyatis, Boston University School of Medicine, Arthritis Center, E5, 715 Albany Street, Boston, Massachusetts, 02118, USA; lafyatis{at}bu.edu

Objective: Cartilage oligomeric matrix protein (COMP) accumulates in systemicsclerosis (SSc) skin and is upregulated by transforming growthfactor (TGF)β. To further characterise the response toTGFβ in SSc, we investigated TGFβ1 and COMP expressionand myofibroblast staining in SSc skin.

Methods: Skin biopsies from patients with diffuse cutaneous SSc (dSSc),limited cutaneous SSc (lSSc) and healthy controls were evaluatedfor COMP mRNA expression using real-time PCR. COMP, ${alpha}$ -smoothmuscle actin (SMA) and TGFβ were assessed in skin sectionsand in cultured fibroblasts by immunohistochemistry. Clinicaldisease status was assessed by the modified Rodnan skin score(mRSS).

Results: Myofibroblasts expressing SMA and COMP were found coexpressedin many cells in dSSc dermis, but each also stained distinctcells in the dermis. Cultured SSc dermal fibroblasts also showedheterogeneity for COMP and SMA expression, with cells expressingSMA, COMP, both or neither. TGFβ treatment increased COMPand SMA-expressing cells. COMP mRNA expression in lesional skinfrom patients with dSSc correlated with the mRSS and TGFβ1staining.

Conclusion: These findings suggest that TGFβ upregulation of COMP and/orSMA expression in subpopulations of fibroblasts contributesto different pathways of fibrosis and that multiple TGFβregulated genes may serve as biomarkers for the degree of SScskin involvement.

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