Popliteal cysts and their relation to the gastrocnemio-semimembranosus bursa a clinical and anatomical study /

Rauschning, Wolfgang.

January 1979

Thesis (doctoral)--Uppsala University, 1979. / Includes bibliographical references (p. 20-22).

Mechanisms of human articular cartilage degradation in arthritic disease

Warnock, Mark George

January 1995

No description available.

610

Osteoarthritis; Synovial fluid

The regeneration of articular tissues

Lawrence, C. E.

January 1987

Changes in the structural organization of cartilage and synovial tissue, or in the macromolecules produced by their cells, alter the properties of the tissues. Elucidation of the changes under controlled experimental conditions could make a significant contribution to the understanding of the pathogenesis of arthritis. To this end a model system has been developed to study proteoglycan and collagen regeneration in porcine articular cartilage and synovial tissue: partially depleted of matrix by exogenous enzyme(s), the tissues were maintained in organ culture, the medium consisting of Dulbecco's modification of Eagle's medium and 15% rabbit serum, and the responses of the chondrocytes and synoviocytes studied biochemically and histologically. Cleavage of proteoglycan core protein in cartilage explants by trypsin, equivalent to the disruption occurring in joint inflammation, induced glycosaminoglycan synthesis. The chondrocytes, particularly of the mid and hypertrophic zones, acquiring a basophilic territorial matrix and eventually an interterritorial matrix, which replaced the ex vivo material. Further damage to collagen by bacterial collagenase induced collagen synthesis, and enhanced glycosaminoglycan synthesis, but hyaluronic acid disruption proved partially inhibitory to recovery, the interterritorial matrix being less basophilic than comparable trypsinized explants. ³⁵SO₄ uptake by depleted explants showed a similar but sustained rate of glycosaminoglycan synthesis compared with untreated explants. The effects of corticosteroids, currently used for the temporary palliation of joint inflammation, on the regeneration processes were studied. The hydrolytic potential of the cultures and the frequency of medium changes had a profound effect on biologically active cortisol levels when cortisol succinate was present. Lower than physiological levels of cortisol (≤2.76 x 10^-7M) promoted glycosaminoglycan synthesis in all disrupted explants except those with cleaved hyaluronic acid chains. During the later stages of culture, in the presence of cortisol, (≤2.76 x 10-7M), the interterritorial glycosaminoglycan concentration increased. Whether collagen fibres were disrupted or not, collagen synthesis was evident, although with pharmacological concentrations of steroid (≤2.76 x 10^-6 M) all synthetic processes were increasingly inhibited. Exogenous trypsin induced extensive resorption of collagen fibres in minced synovial tissue, probably by activation of synovial collagenase. The destruction was partially reduced with trypsin inhibitor or cortisol. In areas of degradation macrophage-like cells accumulated but with early removal of trypsin, despite loss of collagen, fibroblast-like cells accumulated at the base of the explants with synthesized pericellular collagen evident. Collagen release into the medium was measured by an improved hydroxyproline assay designed to reduce interference from serum proteins. Although physiological doses of cortisol (≤2.76 x 10-7 M) enhanced collagen synthesis by, and the development of, the fibroblastic cells, extensive tissue repair was not observed, merely the formation of a cell population in the Millipore membrane. This model of tissue regeneration, remodelling and repair leads to the conclusion that within the arthritic joint the chondrocyte has the potential to rapidly attempt to repair damaged matrix, the extent of synthesis being proportional to the extent and type of matrix disruption. The chondrocyte responds by synthesizing glycosaminoglycans, that aggregate within the matrix, and collagen, with cortisol, at below physiological concentrations, enhancing this regeneration. Synovial tissue did not recover from disruption although the synoviocytes, on reversion to fibroblast-like cells, accumulated new collagen.

612

Synovial/cartilage tissues

Studies of the genetic and immunological basis of rheumatoid arthritis

Milicic, Anita

January 2002

No description available.

616.7230796

Synovial joints

Molecular and cellular basis of synovial joint formation

Feng, Chen, Amy, 冯琛

January 2014

abstract / Biochemistry / Doctoral / Doctor of Philosophy

Joints

Synovial fluid

The enzymatic and mechanical analysis of human synovial fluid

Duffy, John M.

January 1991

No description available.

572

Arthritis and synovial joints

Structure and function of synovial joints, with particular reference to the mechanism of their lubrication

Piper, Michael Stafford

January 1972

The structure and physiology of synovial joints has been studied for years. Recent advances in technology and investigative tools have enabled workers to greatly elucidate the nature of these remarkably functional joints. This thesis presents a review of the literature dealing with the morphology and physiology of diarthrodial joints. The embryological development and the gross structure of these joints is presented as is a discussion of the light and electron microscopic features of articular cartilage and synovial membrane. In addition, some of the features of synovial fluid are presented. The results of recent investigation into the biochemistry and metabolism of articular cartilage are discussed. As the main function of synovial joints is to provide painless, controlled motion, much interest has recently focused on the mechanism of lubrication in these joints. A review of the literature concerning the nature of joint lubrication is presented, and a theory of lubrication enhancement by electrical repulsive forces is proposed. This theory was developed from the results of a technique of synovianalysis conducted on a series of 61 samples of synovial fluid. The samples were collected from a series of hospital patients. One group of patients suffered from rheumatoid arthritis, while a second group was comprised of patients suffering from conditions not associated with rheumatoid arthritis. The samples were subjected to analysis using cation sensitive glass electrodes, and the concentrations of ionized sodium and potassium were measured. In addition, sodium and potassium concentrations were measured in the synovial fluid samples using a spectrophotometer. As a result of these investigations, it was found that the synovial fluid samples from patients with rheumatoid arthritis contained a significantly lower concentration of ionized sodium. It is concluded that the lower concentration of sodium ions in synovial fluid of rheumatoid arthritis may result in a diminution of electrical repulsive forces acting within synovial joints, and explain, in part, the cartilage attrition seen in this disease. / Science, Faculty of / Botany, Department of / Zoology, Department of / Graduate

Joints

Synovial fluid

The mechanical failure of articular cartilage

Kerin, Alexander James

January 1998

No description available.

610.28

In vitro investigation into the role of synovium-derived proteinases in cartilage aggrecan breakdown

Vankemmelbeke, Mireille Nancy

January 2000

No description available.

612

Bovine; Aggrecanase; Synovial; Arthritis

Rheological properties and free radical stability of cross-linked hyaluronan (Hylan)

Al-Assaf, Saphwan

January 1997

No description available.

541

Biocompatable materials; Synovial fluid