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Markers of joint tissue turnover in joint fluids from hips with osteonecrosis of the femoral head

✍ Scribed by Seiya Jingushi; L. Stefan Lohmander; Masayuki Shinmei; Lori A. Hoerrner; Michael W. Lark; Yoichi Sugioka; Yukihide Iwamoto


Publisher
Elsevier Science
Year
2000
Tongue
English
Weight
678 KB
Volume
18
Category
Article
ISSN
0736-0266

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✦ Synopsis


Abstract

Osteonecrosis of the femoral head often results in secondary osteoarthritis of the hip joint; however, the pathologic processes underlying the destruction of articular cartilage are not fully understood. Molecular markers in the hip joint fluids were measured to examine the changes in turnover of cartilage and other joint tissues. Marker data were related to clinical, radiological, and histopathological changes in the articular cartilage of the hip. Forty‐five patients (median age: 43 years) were studied. The median time between the onset of symptoms and sampling of hip synovial fluid was 6 months. Aggrecan fragments, C‐propeptide of type‐II collagen, matrix metalloproteinase‐3, and tissue inhibitor of metalloproteinases‐1 levels in joint fluid were determined by immunoassay. Osteonecrosis of the femoral head was graded by radiology as minimal collapse of the femoral head (stage 2: 26 patients), severe collapse (stage 3: 15 patients), or severe collapse with osteoarthritis (stage 4: four patients). Histologica changes of the articular cartilage, consistent with early‐stage osteoarthritis, were evident at stage 3 and were more advanced at stage 4. The average concentrations of proteoglycan fragments and C‐propeptide of type‐II collagen were 207 (SD 182) μg/ml and 19.6 (SD 19.3) ng/ml, respectively. The average concentrations of matrix metalloproteinase‐3 and tissue inhibitor of metalloproteinases‐ 1 were 177 (SD 291) nM and 23.0 (SD 9.9) n__M__, respectively. Measurable levels for all markers assayed were noted in the earliest stage of the disease, only a few months after the onset of symptoms and well before the appearance of radiological changes. Levels of matrix metalloproteinase‐3 and molar ratios of matrix metalloproteinase‐3/tissue inhibitor of metalloproteinases‐1 were higher in early stage disease than in later stage disease.


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