Mechanical Strain Stabilizes Reconstituted Collagen Fibrils against Enzymatic Degradation by Mammalian Collagenase Matrix Metalloproteinase 8 (MMP-8)
- 01Mechanical load protects collagen from enzymatic degradation
- 02Strained collagen fibrils degraded much more slowly than unstrained ones
- 03This protective effect appears to happen at the molecular level
- 04Findings may inform understanding of tissue remodeling and adaptation
Mechanical strain appears to protect collagen fibers from enzymatic breakdown, making them more durable.
Collagen, a triple-helical, self-organizing protein, is the predominant structural protein in mammals. It is found in bone, ligament, tendon, cartilage, intervertebral disc, skin, blood vessel, and cornea. We have recently postulated that fibrillar collagens (and their complementary enzymes) comprise the basis of a smart structural system which appears to support the retention of molecules in fibrils which are under tensile mechanical strain. The theory suggests that the mechanisms which drive the preferential accumulation of collagen in loaded tissue operate at the molecular level and are not solely cell-driven. The concept reduces control of matrix morphology to an interaction between molecules and the most relevant, physical, and persistent signal: mechanical strain. The investigation was carried out in an environmentally-controlled microbioreactor in which reconstituted type I collagen micronetworks were gently strained between micropipettes. The strained micronetworks were exposed to active matrix metalloproteinase 8 (MMP-8) and relative degradation rates for loaded and unloaded fibrils were tracked simultaneously using label-free differential interference contrast (DIC) imaging. It was found that applied tensile mechanical strain significantly increased degradation time of loaded fibrils compared to unloaded, paired controls. In many cases, strained fibrils were detectable long after unstrained fibrils were degraded. In this investigation we demonstrate for the first time that applied mechanical strain preferentially preserves collagen fibrils in the presence of a physiologically-important mammalian enzyme: MMP-8. These results have the potential to contribute to our understanding of many collagen matrix phenomena including development, adaptation, remodeling and disease. Additionally, tissue engineering could benefit from the ability to sculpt desired structures from physiologically compatible and mutable collagen.
- APA
- Brendan P Flynn, Amit P Bhole, Nima Saeidi, Melody Liles, Charles A DiMarzio, & Jeffrey W Ruberti (2010). Mechanical Strain Stabilizes Reconstituted Collagen Fibrils against Enzymatic Degradation by Mammalian Collagenase Matrix Metalloproteinase 8 (MMP-8). https://fasciaresearchdatabase.com/mechanical-strain-stabilizes-reconstituted-collagen-fibrils-against-enzymatic-degradation-by-mammalian-collagenase-matrix-metalloproteinase-8-mmp-8/
- MLA
- Brendan P Flynn, et al. "Mechanical Strain Stabilizes Reconstituted Collagen Fibrils against Enzymatic Degradation by Mammalian Collagenase Matrix Metalloproteinase 8 (MMP-8)." 2010, https://fasciaresearchdatabase.com/mechanical-strain-stabilizes-reconstituted-collagen-fibrils-against-enzymatic-degradation-by-mammalian-collagenase-matrix-metalloproteinase-8-mmp-8/.
- Chicago
- Brendan P Flynn et al. 2010. "Mechanical Strain Stabilizes Reconstituted Collagen Fibrils against Enzymatic Degradation by Mammalian Collagenase Matrix Metalloproteinase 8 (MMP-8).". https://fasciaresearchdatabase.com/mechanical-strain-stabilizes-reconstituted-collagen-fibrils-against-enzymatic-degradation-by-mammalian-collagenase-matrix-metalloproteinase-8-mmp-8/
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