Literature DB >> 2841121

Susceptibility of cartilage collagens type II, IX, X, and XI to human synovial collagenase and neutrophil elastase.

S J Gadher1, D R Eyre, V C Duance, S F Wotton, L W Heck, T M Schmid, D E Woolley.   

Abstract

The action of purified rheumatoid synovial collagenase and human neutrophil elastase on the cartilage collagen types II, IX, X and XI was examined. At 25 degrees C, collagenase attacked type II and type X (45-kDa pepsin-solubilized) collagens to produce specific products reflecting one and at least two cleavages respectively. At 35 degrees C, collagenase completely degraded the type II collagen molecule to small peptides whereas a large fragment of the type X molecule was resistant to further degradation. In contrast, collagen type IX (native, intact and pepsin-solubilized type M) and collagen type XI were resistant to collagenase attack at both 25 degrees C and 35 degrees C even in the presence of excess enzyme. Mixtures of type II collagen with equimolar amounts of either type IX or XI did not affect the rate at which the former was degraded by collagenase at 25 degrees C. Purified neutrophil elastase, shown to be functionally active against soluble type III collagen, had no effect on collagen type II at 25 degrees C or 35 degrees C. At 25 degrees C collagen types IX (pepsin-solubilized type M) and XI were also resistant to elastase, but at 35 degrees C both were susceptible to degradation with type IX being reduced to very small peptides. Collagen type X (45-kDa pepsin-solubilized) was susceptible to elastase attack at 25 degrees C and 35 degrees C as judged by the production of specific products that corresponded closely with those produced by collagenase. Although synovial collagenase failed to degrade collagen types IX and XI, all the cartilage collagen species examined were degraded at 35 degrees C by conditioned culture medium from IL1-activated human articular chondrocytes. Thus chondrocytes have the potential to catabolise each cartilage collagen species, but the specificity and number of the chondrocyte-derived collagenase(s) has yet to be resolved.

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Year:  1988        PMID: 2841121     DOI: 10.1111/j.1432-1033.1988.tb14158.x

Source DB:  PubMed          Journal:  Eur J Biochem        ISSN: 0014-2956


  8 in total

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2.  High resistance of the mechanical properties of the chondrocyte pericellular matrix to proteoglycan digestion by chondroitinase, aggrecanase, or hyaluronidase.

Authors:  Rebecca E Wilusz; Farshid Guilak
Journal:  J Mech Behav Biomed Mater       Date:  2013-10-03

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Authors:  J T Thomas; A P Kwan; M E Grant; R P Boot-Handford
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4.  Matrix metalloproteinase-8 inactivates macrophage inflammatory protein-1 alpha to reduce acute lung inflammation and injury in mice.

Authors:  Pablo A Quintero; Martin D Knolle; Luisa F Cala; Yuehong Zhuang; Caroline A Owen
Journal:  J Immunol       Date:  2009-12-30       Impact factor: 5.422

5.  Batch correction of microarray data substantially improves the identification of genes differentially expressed in rheumatoid arthritis and osteoarthritis.

Authors:  Peter Kupfer; Reinhard Guthke; Dirk Pohlers; Rene Huber; Dirk Koczan; Raimund W Kinne
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Review 6.  IL-1 in osteoarthritis: time for a critical review of the literature.

Authors:  Tonia L Vincent
Journal:  F1000Res       Date:  2019-06-21

7.  Enhanced efficiency in isolation and expansion of hAMSCs via dual enzyme digestion and micro-carrier.

Authors:  Bi Foua Claude Alain Gohi; Xue-Ying Liu; Hong-Yan Zeng; Sheng Xu; Kouassi Marius Honore Ake; Xiao-Ju Cao; Kai-Min Zou; Sheila Namulondo
Journal:  Cell Biosci       Date:  2020-01-06       Impact factor: 7.133

8.  Immunoelectron microscopic studies of type X collagen in endochondral ossification.

Authors:  A R Poole; I Pidoux
Journal:  J Cell Biol       Date:  1989-11       Impact factor: 10.539

  8 in total

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