Journal
CURRENT BIOLOGY
Volume 21, Issue 11, Pages 933-941Publisher
CELL PRESS
DOI: 10.1016/j.cub.2011.04.007
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Funding
- National Institutes of Health [P30AR-050953, DK074538, EB006203, AR49785]
- Cleveland Clinic
- Sumitomo Foundation, Japan
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Mechanical forces influence homeostasis in virtually every tissue [1, 2]. Tendon, constantly exposed to variable mechanical force, is an excellent model in which to study the conversion of mechanical stimuli into a biochemical response [3-5]. Here we show in a mouse model of acute tendon injury and in-vitro that physical forces regulate the release of active transforming growth factor (TGF)-beta from the extracellular matrix (ECM). The quantity of active TGF-beta detected in tissue exposed to various levels of tensile loading correlates directly with the extent of physical forces. At physiological levels, mechanical forces maintain, through TGF4t/Smad2/3-mediated signaling, the expression of Scleraxis (Scx), a transcription factor specific for tenocytes and their progenitors. The gradual and temporary loss of tensile loading causes reversible loss of Scx expression, whereas sudden interruption, such as in transection tendon injury, destabilizes the structural organization of the ECM and leads to excessive release of active TGF-beta and massive tenocyte death, which can be prevented by the TGF-beta type I receptor inhibitor SD208. Our findings demonstrate a critical role for mechanical force in adult tendon homeostasis. Furthermore, this mechanism could translate physical force into biochemical signals in a much broader variety of tissues or systems in the body.
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