Literature DB >> 2120402

Proteoglycan alterations following immobilization and remobilization in the articular cartilage of young canine knee (stifle) joint.

A M Säämänen1, M Tammi, J Jurvelin, I Kiviranta, H J Helminen.   

Abstract

The distribution of proteoglycans (PGs) at 11 sites on the knee (stifle joint) cartilage of young female beagle dogs was studied following cast immobilization for 11 weeks in 90 degrees flexion and after a subsequent remobilization for 15 weeks. Immobilization induced a reduction in PG uronic acid at all sites (mean of -38%), but the greatest depletion (-64%) occurred at the anterior and posterior extremes of the femoral condyles, i.e., at locations where the immobilized cartilage lost contact to the opposing cartilage. Following remobilization, the content of uronic acid remained lower than in the age-matched controls (-18% on average), particularly at the minimum contact sites most affected by immobilization (-33%). The chondroitin-6-sulfate to chondroitin-4-sulfate ratio was reduced by immobilization in most locations (average of -14%) and returned to control values after remobilization. There was no consistent change in the percentage of aggregating PGs observed in Sephacryl S-1000 gel filtration after immobilization or remobilization. However, following remobilization, the aggregating PGs showed an enhanced proportion of the slower mobility band in agarose gel electrophoresis, indicative of a larger monomer size. In the contralateral, load-bearing knee joint, both the uronic acid content and PG monomer type distribution were identical to those observed in the experimental joint, suggesting that the state reached after the remobilization period was due to factor(s) influencing both sides. The results suggest that contact forces between articulating surfaces are required to maintain normal PG content and that the control mechanism works locally at each cartilage site. Restriction of joint mobility and loading in young animals is concluded to cause persistent changes in cartilage matrix. Furthermore, the use of the contralateral joint as the sole control in this kind of studies, although experimentally convenient, seems not to be appropriate.

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Year:  1990        PMID: 2120402     DOI: 10.1002/jor.1100080612

Source DB:  PubMed          Journal:  J Orthop Res        ISSN: 0736-0266            Impact factor:   3.494


  17 in total

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Authors:  O T Mäkelä; M J Lammi; H Uusitalo; M M Hyttinen; E Vuorio; H J Helminen; R-M Tulamo
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Review 4.  Activity vs. rest in the treatment of bone, soft tissue and joint injuries.

Authors:  J A Buckwalter
Journal:  Iowa Orthop J       Date:  1995

Review 5.  Animal models for osteoarthritis: processes, problems and prospects.

Authors:  K P Pritzker
Journal:  Ann Rheum Dis       Date:  1994-06       Impact factor: 19.103

6.  Immobilisation causes longlasting matrix changes both in the immobilised and contralateral joint cartilage.

Authors:  M O Jortikka; R I Inkinen; M I Tammi; J J Parkkinen; J Haapala; I Kiviranta; H J Helminen; M J Lammi
Journal:  Ann Rheum Dis       Date:  1997-04       Impact factor: 19.103

7.  Altered Golgi apparatus in hydrostatically loaded articular cartilage chondrocytes.

Authors:  J J Parkkinen; M J Lammi; A Pelttari; H J Helminen; M Tammi; I Virtanen
Journal:  Ann Rheum Dis       Date:  1993-03       Impact factor: 19.103

8.  Adaptation of canine femoral head articular cartilage to long distance running exercise in young beagles.

Authors:  M J Lammi; T P Häkkinen; J J Parkkinen; M M Hyttinen; M Jortikka; H J Helminen; M I Tammi
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9.  Distribution of hyaluronan in articular cartilage as probed by a biotinylated binding region of aggrecan.

Authors:  J J Parkkinen; T P Häkkinen; S Savolainen; C Wang; R Tammi; U M Agren; M J Lammi; J Arokoski; H J Helminen; M I Tammi
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10.  Expression of reduced amounts of structurally altered aggrecan in articular cartilage chondrocytes exposed to high hydrostatic pressure.

Authors:  M J Lammi; R Inkinen; J J Parkkinen; T Häkkinen; M Jortikka; L O Nelimarkka; H T Järveläinen; M I Tammi
Journal:  Biochem J       Date:  1994-12-15       Impact factor: 3.857

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