Literature DB >> 7677443

In vivo model of cartilage degradation--effects of a matrix metalloproteinase inhibitor.

E H Karran1, T J Young, R E Markwell, G P Harper.   

Abstract

OBJECTIVES: To develop a model of cartilage degradation that (i) enables the testing of synthetic, small molecular weight matrix metalloproteinase (MMP) inhibitors as agents to prevent cartilage erosion, (ii) permits the direct assay of the principal constituents of the extracellular matrix (collagen and proteoglycan) in both the non-calcified articular cartilage and the calcified cartilage compartments, and (iii) is mediated by a chronic, granulomatous tissue that closely apposes intact articular cartilage, and in this respect resembles the pannus-cartilage junction of rheumatoid arthritis.
METHODS: Femoral head cartilage was obtained from donor rats, wrapped in cotton and implanted subcutaneously into recipient animals. After a two stage papain digestion procedure, the proteoglycan and collagen contents were measured by assaying for glycosaminoglycans and hydroxyproline, respectively, in both the non-calcified cartilage that comprises the articular surface layer and the calcified cartilage compartment. The incorporation in vitro of [35S]-sulphate into glycosaminoglycans was assayed as a measure of proteoglycan biosynthesis. An osmotic minipump was cannulated to the implanted femoral head cartilage and synthetic MMP inhibitors (MI-1 and MI-2) were infused continuously over a 14 day period.
RESULTS: The implanted, cotton wrapped femoral head cartilages provoked a granulomatous response that resulted in the removal of collagen and proteoglycan from the cartilage matrix. The removal of proteoglycan and collagen was exclusively from the non-calcified articular cartilage, whereas the proteoglycan and collagen content of the calcified compartment increased during the experiments. MI-1 reproducibly reduced the degradation of proteoglycan and collagen in implanted femoral head cartilage.
CONCLUSIONS: We have described an in vivo model of cartilage degradation that permits the measurement of proteoglycan and collagen in both non-calcified articular cartilage and calcified cartilage compartments. The model can be used to test the effects of agents of unknown systemic bioavailability and pharmacokinetic profile by infusing them directly to the site of cartilage degradation. The removal of cartilage extracellular matrix by granulomatous tissue was inhibited by an MMP inhibitor, thus proving the involvement of this family of proteinases in cartilage catabolism in this model.

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Year:  1995        PMID: 7677443      PMCID: PMC1009964          DOI: 10.1136/ard.54.8.662

Source DB:  PubMed          Journal:  Ann Rheum Dis        ISSN: 0003-4967            Impact factor:   19.103


  28 in total

1.  A rapid and reproducible assay for collagenase using [1-14C]acetylated collagen.

Authors:  T E Cawston; A J Barrett
Journal:  Anal Biochem       Date:  1979-11-01       Impact factor: 3.365

2.  Improved quantitation and discrimination of sulphated glycosaminoglycans by use of dimethylmethylene blue.

Authors:  R W Farndale; D J Buttle; A J Barrett
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Journal:  Arthritis Rheum       Date:  1984-08

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Authors:  F B De Brito; A R Moore; M J Holmes; D A Willoughby
Journal:  Br J Exp Pathol       Date:  1987-10

5.  Effect of synthetic metalloprotease inhibitors on cartilage autolysis in vitro.

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Journal:  J Pharmacol Exp Ther       Date:  1987-02       Impact factor: 4.030

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Journal:  J Pathol       Date:  1984-01       Impact factor: 7.996

7.  The production in culture of metalloproteinases and an inhibitor by joint tissues from normal rabbits, and from rabbits with a model arthritis. II. Articular cartilage.

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Journal:  Rheumatol Int       Date:  1981       Impact factor: 2.631

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Authors:  D L Scott; D P Symmons; B L Coulton; A J Popert
Journal:  Lancet       Date:  1987-05-16       Impact factor: 79.321

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Authors:  M C Burleigh; A J Barrett; G S Lazarus
Journal:  Biochem J       Date:  1974-02       Impact factor: 3.857

10.  Studies into the influence of carrageenan-induced inflammation on articular cartilage degradation using implantation into air pouches.

Authors:  A D Sedgwick; A R Moore; A Y Al-Duaij; J C Edwards; D A Willoughby
Journal:  Br J Exp Pathol       Date:  1985-08
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  5 in total

Review 1.  Matrix metalloproteinases. Novel targets for directed cancer therapy.

Authors:  A E Yu; R E Hewitt; E W Connor; W G Stetler-Stevenson
Journal:  Drugs Aging       Date:  1997-09       Impact factor: 3.923

2.  Suppression of adjuvant arthritis of rats by a novel matrix metalloproteinase-inhibitor.

Authors:  T Hamada; N Arima; M Shindo; K Sugama; Y Sasaguri
Journal:  Br J Pharmacol       Date:  2000-12       Impact factor: 8.739

3.  Proteoglycan degrading activity in granulomatous inflammation: comparison between the C57b1/6 and C57bg/bg mouse.

Authors:  D Prigent; M M Trancart; M P Seed; D A Willoughby
Journal:  Inflamm Res       Date:  1996-10       Impact factor: 4.575

4.  Relaxin's induction of metalloproteinases is associated with the loss of collagen and glycosaminoglycans in synovial joint fibrocartilaginous explants.

Authors:  Tabassum Naqvi; Trang T Duong; Gihan Hashem; Momotoshi Shiga; Qin Zhang; Sunil Kapila
Journal:  Arthritis Res Ther       Date:  2004-10-29       Impact factor: 5.156

5.  Biotribology of Synovial Cartilage: A New Method for Visualization of Lubricating Film and Simultaneous Measurement of the Friction Coefficient.

Authors:  Pavel Čípek; Martin Vrbka; David Rebenda; David Nečas; Ivan Křupka
Journal:  Materials (Basel)       Date:  2020-04-30       Impact factor: 3.623

  5 in total

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