Anti-fibroblast antibodies detected by cell-based ELISA in systemic sclerosis enhance the collagenolytic activity and matrix metalloproteinase-1 production in dermal fibroblasts

doi:10.1093/rheumatology/kem241

Rheumatology Advance Access originally published online on November 3, 2007
Rheumatology 2007 46(12):1779-1785; doi:10.1093/rheumatology/kem241

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Anti-fibroblast antibodies detected by cell-based ELISA in systemic sclerosis enhance the collagenolytic activity and matrix metalloproteinase-1 production in dermal fibroblasts

S. Fineschi¹, F. Cozzi², D. Burger¹, J.-M. Dayer¹, P. L. Meroni³ and C. Chizzolini¹

¹Immunology and Allergy, Department of Internal Medicine, University Hospital and School of Medicine, Geneva, Switzerland, ²Rheumatology Unit, University Hospital of Padua and ³Department of Internal Medicine, IRCC Istituto Auxologico Italiano, University of Milan, Milan, Italy.

Correspondence to: C. Chizzolini, Immunology and Allergy, Geneva University Hospital, 1211 Geneva 14, Switzerland. E-mail: chizzolini{at}medecine.unige.ch

Abstract

Objectives. Antibodies binding to the surface of fibroblasts(anti-fibroblast antibodies: AFA) have been described in systemicsclerosis (SSc). We aimed to assess the effect of AFA on extracellularmatrix (ECM) turnover and whether AFA were associated with anti-topoisomerase-Iantibody.

Methods. IgG were purified from AFA-positive and AFA-negativesera selected within 20 SSc and 20 healthy individuals, andtested on normal dermal fibroblasts, at protein and mRNA level,for their capacity to induce collagen deposition or degradation.

Results. Fibroblasts stimulated with AFA-positive but not withAFA-negative and control IgG showed an increased capacity todigest collagen matrix and produce metalloproteinase-1 (MMP-1)while their production of total collagen, type I collagen andtissue inhibitor of metalloproteinase-1 (TIMP-1) was unaffected.The steady-state mRNA levels of MMP-1, COL1A1 and TIMP-1 paralleledthe protein levels. AFA-positive IgG did not induce Smad 2/3phosphorylation, indicating that this transforming growth factor-ßsignalling pathway was not involved. IL-1 and tumour necrosisfactor (TNF) neutralization did not reverse the enhanced productionof MMP-1, suggesting a direct effect of AFA on fibroblasts.Finally, anti-topoisomerase-I antibodies were present in 11of 12 AFA-negative IgG, and an anti-topoisomerase-I monoclonalantibody failed to enhance MMP-1 production, thus indicatinga lack of correlation between AFA and anti-topoisomerase-I antibody.

Conclusions. These results indicate that SSc antibodies bindingto fibroblasts enhance matrix degradation and MMP productionevents that may favour inflammation but do not directly impacton fibrosis development.

KEY WORDS: Anti-fibroblast antibodies, Collagen, Matrix metalloproteinase, Smad2/3, Fibrosis

Submitted 23 April 2007; revised version accepted 8 August 2007.
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