Journal
ARTHRITIS AND RHEUMATISM
Volume 60, Issue 2, Pages 501-512Publisher
WILEY-LISS
DOI: 10.1002/art.24247
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Funding
- ZonMW [11-400-0082]
- Dutch Arthritis Association [NR 08-1-309]
- AstraZeneca
- IOP Genomics [IGE02032]
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Objective. Wnt signaling pathway proteins are involved in embryonic development of cartilage and bone, and, interestingly, developmental processes appear to be recapitulated in osteoarthritic (OA) cartilage. The present study was undertaken to characterize the expression pattern of Wnt and Fz genes during experimental OA and to determine the function of selected genes in experimental and human OA. Methods. Longitudinal expression analysis was performed in 2 models of OA. Levels of messenger RNA for genes from the Wnt/beta-catenin pathway were determined in synovium and cartilage, and the results were validated using immunohistochemistry. Effects of selected genes were assessed in vitro using recombinant protein, and in vivo by adenoviral overexpression. Results. Wnt-induced signaling protein 1 (WISP-1) expression was strongly increased in the synovium and cartilage of mice with experimental OA. Wnt-16 and Wnt-2B were also markedly up-regulated during the course of disease. Interestingly, increased WISP-1 expression was also found in human OA cartilage and synovium. Stimulation of macrophages anti chondrocytes with recombinant WISP-1 resulted in interleukin-l-independent induction of several matrix metalloproteinases (MMPs) and aggrecanase. Adenoviral overexpression of WISP-1 in murine knee joints induced MMP and aggrecanase expression and resulted in cartilage damage. Conclusion. This study included a comprehensive characterization of Wnt and Frizzled gene expression in experimental and human OA articular joint tissue. The. data demonstrate, for the first time, that WISP-1 expression is a feature of experimental and human OA and that WISP-1 regulates chondrocyte and macro. phage MMP and aggrecanase expression and is capable of inducing articular cartilage damage in models of OA.
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