The development of cartilage pathology in osteoarthritis involves excessive damage to the collagen fibrillar network, which appears to be mediated primarily by the chondrocyte-generated cytokines interleukin-1 and tumour necrosis factor α and the collagenases matrix metalloproteinase-1 (MMP-1) and MMP-13. The damage to matrix caused by these and other MMPs can result in the production of sufficient degradation products that can themselves elicit further degradation, leading to chondrocyte differentiation and eventually matrix mineralization and cell death. Knowledge of these MMPs, cellular receptors and cytokine pathways, and the ability to selectively antagonize them by selective blockade of function, may provide valuable therapeutic opportunities in the treatment of osteoarthritis and other joint diseases involving cartilage resorption, such as rheumatoid arthritis. The ability to detect the products of these degradative events released into body fluids of patients may enable us to monitor disease activity, predict disease progression and determine more rapidly the efficacy of new therapeutic agents.
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September 2003
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Conference Article|
September 01 2003
Proteolysis of the collagen fibril in osteoarthritis
A Robin Poole;
A Robin Poole
1
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
1To whom correspondence should be addressed (e-mail [email protected]).
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Fred Nelson;
Fred Nelson
2
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
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Leif Dahlberg;
Leif Dahlberg
3
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
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Elena Tchetina;
Elena Tchetina
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
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Masahiko Kobayashi;
Masahiko Kobayashi
4
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
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Tadashi Yasuda;
Tadashi Yasuda
5
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
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Sheila Laverty;
Sheila Laverty
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
†Faculty of Veterinary Sciences, University of Montreal, Ste-Hyacinthe, Quebec, Canada
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Ginette Squires;
Ginette Squires
6
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
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Toshihisa Kojima;
Toshihisa Kojima
7
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
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William Wu;
William Wu
8
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
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R. Clark Billinghurst
R. Clark Billinghurst
9
*Joint Diseases Laboratory, Shriners Hospitals for Children and Departments of Surgery and Medicine, McGill University, 1529 Cedar Avenue, Montreal, Quebec H3G 1A6, Canada
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Publisher: Portland Press Ltd
Online ISSN: 1744-1439
Print ISSN: 0067-8694
© 2003 The Biochemical Society
2003
Biochem Soc Symp (2003) 70: 115–123.
Citation
Jeremy Saklatvala, Hideaki Nagase, Guy Salvesen, A Robin Poole, Fred Nelson, Leif Dahlberg, Elena Tchetina, Masahiko Kobayashi, Tadashi Yasuda, Sheila Laverty, Ginette Squires, Toshihisa Kojima, William Wu, R. Clark Billinghurst; Proteolysis of the collagen fibril in osteoarthritis. Biochem Soc Symp 1 September 2003; 70 115–123. doi: https://doi.org/10.1042/bss0700115
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