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Issue title: Selected papers of the Euromech Colloquium No. 420, Mechanobiology of Cells and Tissues
Article type: Research Article
Authors: Martin, J.A. | Mehr, D. | Pardubsky, P.D. | Buckwalter, J.A.
Affiliations: Iowa City Veterans Administration Medical Center and University of Iowa Department of Orthopaedics, Iowa City, IA 52242, USA
Note: [] Address for correspondence: Joseph A. Buckwalter, 01008 Pappajohn Pavilion, Department of Orthopaedics, University of Iowa College of Medicine, Iowa City, IA 52242, USA. Tel.: +1 319 356 2595; Fax: +1 319 356 8999; E‐mail: joseph‐buckwalter@uiowa.edu.
Abstract: Although most tendon regions are subjected primarily to high tensile loads, selected regions, primarily those that directly contact bones that change the direction of the tendon, must withstand high compressive loads as well. Compressed tendon regions differ from regions subjected to primarily tensile loads: they have a fibrocartilaginous structure with spherical cells surrounded by a matrix containing aggrecan and collagen types I and II, in contrast regions not exposed to compression have a fibrous structure with spindle shaped fibroblasts surrounded by a matrix of dense, longitudinally oriented type I collagen fibrils. The spherical shape of cells in fibrocartilagenous regions indicates these cells are more loosely attached to the matrix than their spindle‐shaped counterparts in fibrous regions, a feature that may help to minimize cell deformation during tendon compression. We hypothesized that expression of tenascin‐C, an anti‐adhesive protein, is part of the adaptation of tendon cells to compression that helps establish and maintain fibrocartilaginous regions. To test this hypothesis we compared tenascin‐C content and expression in compressed (distal) versus uncompressed (proximal) segments of bovine flexor tendons. Immunohistochemistry and immunoblot analyses showed that tenascin‐C content was increased in the distal tendon where it co‐distributed with type II collagen and aggrecan. Tendon cells from the distal segments expressed more tenascin‐C than did cells from the proximal segments for up to four days in cell culture, indicating that increased tenascin‐C expression is a relatively stable feature of the distal cells. These observations support the hypothesis that tenascin‐C expression is a cellular adaptation to compression that helps establish and maintain fibrocartilagenous regions of tendons.
Journal: Biorheology, vol. 40, no. 1-3, pp. 321-329, 2003
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