Volume 44, Issue 9 pp. 2055-2064
Research Article

Raised serum vascular endothelial growth factor levels are associated with destructive change in inflammatory arthritis

Sundeept Ballara

Sundeept Ballara

Imperial College School of Medicine, London, UK

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Peter C. Taylor

Peter C. Taylor

Imperial College School of Medicine, London, UK

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Petra Reusch

Petra Reusch

Institute of Molecular Medicine, Tumor Biology Center, Freiburg, Germany

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Dieter Marmé

Dieter Marmé

Institute of Molecular Medicine, Tumor Biology Center, Freiburg, Germany

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Marc Feldmann

Marc Feldmann

Imperial College School of Medicine, London, UK

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Ravinder N. Maini

Ravinder N. Maini

Imperial College School of Medicine, London, UK

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Ewa M. Paleolog

Corresponding Author

Ewa M. Paleolog

Imperial College School of Medicine, London, UK

Kennedy Institute of Rheumatology Division, Imperial College School of Medicine, Arthritis Research Campaign Building, 1 Aspenlea Road, London W6 8LH, UKSearch for more papers by this author

Abstract

Objective

To determine whether elevated levels of the angiogenic cytokine vascular endothelial growth factor (VEGF), detected on presentation to an early arthritis clinic, are associated with the development of chronic and erosive arthritis.

Methods

Concentrations of VEGF and its soluble receptor, soluble fms-like tyrosine kinase 1 (sFlt-1), were measured by enzyme-linked immunosorbent assay in serum samples from patients with early (<2 years from onset) arthritic symptoms in the peripheral joints, namely early rheumatoid arthritis (RA), self-limiting arthritis (viral, reactive, and idiopathic inflammatory arthritis), or psoriatic arthritis. In addition, measurements were made in random samples from patients with longstanding (>3 years from symptom onset) RA treated with disease-modifying antirheumatic drugs, from patients with osteoarthritis (OA), and from patients with polyarthralgia without arthritis, as well as from nonarthritic controls.

Results

Serum VEGF levels at presentation were elevated in patients with inflammatory arthritis (RA, psoriatic, and self-limiting arthritis) as well as in patients with OA, in comparison with nonarthritic controls. Moreover, serum VEGF concentrations were significantly higher in patients with early RA than in patients with self-limiting arthritis. Serum VEGF levels at presentation in patients with early RA correlated significantly with the development of radiographic damage after 1 year. Improvement in the clinical symptoms of RA was associated with a reduction in serum VEGF levels. Serum sFlt-1 levels were raised in patients with early and longstanding RA and in those with self-limiting arthritis, and correlated positively with the serum VEGF concentrations in patients with inflammatory arthritis.

Conclusion

These findings implicate the proangiogenic cytokine VEGF in the persistence of inflammatory arthritis, and support the hypothesis that expansion of the synovial vasculature is important for the development of joint destruction in RA.

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