4.5 Article

Biglycan has a major role in maintenance of mature tendon mechanics

Journal

JOURNAL OF ORTHOPAEDIC RESEARCH
Volume 40, Issue 11, Pages 2546-2556

Publisher

WILEY
DOI: 10.1002/jor.25299

Keywords

biglycan; biomechanics; decorin; proteoglycan; tendon

Categories

Funding

  1. National Science Foundation [DGE-1845298]
  2. National Institutes of Health [P30AR069619, R01AR068057]

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It was found in mature mice that knockdown of biglycan led to extensive changes in tendon structure and mechanics, while knockdown of decorin had minimal effects. Specifically, biglycan knockdown resulted in reductions in several mechanical parameters and increased collagen fiber realignment during loading. Furthermore, both decorin and biglycan knockdown led to similar alterations in tendon microstructure.
Decorin and biglycan are two small leucine-rich proteoglycans (SLRPs) that regulate collagen fibrillogenesis and extracellular matrix assembly in tendon. The objective of this study was to determine the individual roles of these molecules in maintaining the structural and mechanical properties of tendon during homeostasis in mature mice. We hypothesized that knockdown of decorin in mature tendons would result in detrimental changes to tendon structure and mechanics while knockdown of biglycan would have a minor effect on these parameters. To achieve this objective, we created tamoxifen-inducible mouse knockdown models targeting decorin or biglycan inactivation. This enables the evaluation of the roles of these SLRPs in mature tendon without the abnormal tendon development caused by conventional knockout models. Contrary to our hypothesis, knockdown of decorin resulted in minor alterations to tendon structure and no changes to mechanics while knockdown of biglycan resulted in broad changes to tendon structure and mechanics. Specifically, knockdown of biglycan resulted in reduced insertion modulus, maximum stress, dynamic modulus, stress relaxation, and increased collagen fiber realignment during loading. Knockdown of decorin and biglycan produced similar changes to tendon microstructure by increasing the collagen fibril diameter relative to wild-type controls. Biglycan knockdown also decreased the cell nuclear aspect ratio, indicating a more spindle-like nuclear shape. Overall, the extensive changes to tendon structure and mechanics after knockdown of biglycan, but not decorin, provides evidence that biglycan plays a major role in the maintenance of tendon structure and mechanics in mature mice during homeostasis.

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