Expression of collagen and aggrecan genes in normal and osteoarthritic murine knee joints

Objective The STR/ort mouse strain develops osteoarthritis (OA) of the medial tibial cartilage whilst CBA mice do not develop this disease. We investigated whether changes occur in the expression of genes encoding major extracellular matrix proteins in the connective tissue of the murine knee joint...

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Veröffentlicht in:Osteoarthritis and cartilage 2002-01, Vol.10 (1), p.51-61
Hauptverfasser: Chambers, M.G, Kuffner, T, Cowan, S.K, Cheah, K.S.E, Mason, R.M
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Sprache:eng
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Zusammenfassung:Objective The STR/ort mouse strain develops osteoarthritis (OA) of the medial tibial cartilage whilst CBA mice do not develop this disease. We investigated whether changes occur in the expression of genes encoding major extracellular matrix proteins in the connective tissue of the murine knee joint in OA. Design Expression of the genes encoding collagens II (Col2α1), X (Col10α1), α2(XI) (Col11α2) and aggrecan (Agc) was detected in skeletally mature and immature male mice of the CBA and STR/ort strains by in situ hybridization. ResultsCol2α1 was expressed by chondrocytes of the tibial and patella–femoral cartilage and by the meniscal cartilage in all young mice (4–9 weeks) but only in the patella–femoral cartilage in older mice of both strains (36–45 weeks). In contrast Col2α1 was expressed by growth plate chondrocytes of both species at all ages. Similarly, Col2α1 transcripts were detected in cruciate ligament cells in both strains at all ages. Col10α1 transcripts were detected in cruciate ligament cells in both strains at all ages. Col10α1 expression was evident in the hypertrophic chondrocytes in the growth plate of young CBA and STR mice, but was not active in these cells in mature animals. However,Col10α1 was transcribed in articular chondrocytes of the tibia, meniscal and patella–femoral cartilages of all ages, in normal and osteoarthritic mice. Transcripts were also present in ligament of some mature animals.Col11α2 followed a similar pattern of expression in CBA cartilages to Col2α1, being active in adult growth plate but generally inactive in adult articular cartilages. Young CBA and STR/ort mice expressedCol11α2 in articular cartilage and very strongly throughout the growth plate. Agc expression was detected in all articular cartilages at all ages in both strains. Interestingly, transcripts for all four genes were absent in tibial articular chondrocytes located close to osteoarthritic lesions in STR/ort mice, indicating that these cells are unable to synthesize matrix proteins. Adult STR/ort mice also showed evidence of tissue remodeling around the periphery of the knee joint. Cells in remodeling areas actively transcribed Col2α1, Col10α1,Col11α2 and Agc. Conclusion It is unlikely that OA develops in STR/ort mice because of failure to express major proteins in joint tissue. However, once lesions develop in articular cartilage neighbouring chondrocytes fail to express genes encoding several matrix proteins.
ISSN:1063-4584
1522-9653
DOI:10.1053/joca.2001.0481