Both acute and chronic tendon injuries are disabling sports medicine problems with no effective treatment at present. Sustained oxidative stress has been suggested as the major factor contributing to fibrosis and adhesion after acute tendon injury as well as pathological changes of degenerative tendinopathy. Numerous in vitro and in vivo studies have shown that the inhibition of oxidative stress can promote the tenogenic differentiation of tendon stem/progenitor cells, reduce tissue fibrosis and augment tendon repair. This review aims to systematically review the literature and summarize the clinical and pre-clinical evidence about the potential relationship of oxidative stress and tendon disorders. The literature in PubMed was searched using appropriate keywords. A total of 81 original pre-clinical and clinical articles directly related to the effects of oxidative stress and the activators or inhibitors of oxidative stress on the tendon were reviewed and included in this review article. The potential sources and mechanisms of oxidative stress in these debilitating tendon disorders is summarized. The anti-oxidative therapies that have been examined in the clinical and pre-clinical settings to reduce tendon fibrosis and adhesion or promote healing in tendinopathy are reviewed. The future research direction is also discussed.
Extracellular matrices (ECMs) provide important cues
for cell proliferation
and differentiation in the complex environment, which show a significant
influence on cell functions. Herein, cell-derived ECMs were deposited
on the polydopamine (PDA)-decorated porous Ti-24Nb-4Zr-8Sn (Ti2448)
scaffolds fabricated by the electron beam melting method in order
to improve biological functions. The influence of PDA-ECM coatings
on cell functions was further investigated. The results demonstrated
that the PDA-ECM coating facilitated adhesion, proliferation, and
migration of MC3T3-E1 cells on Ti2448 scaffolds. Moreover, Ti2448-PDA-ECM
scaffolds promoted osteogenesis differentiation of cells indicated
by greater alkaline phosphatase activity and further mineralization,
compared to the plain Ti2448 group. Meanwhile, Ti2448-PDA-ECM scaffolds
enhanced bone growth after implantation for one month in rabbit femoral
bone defects. Our findings suggest that the bioinspired PDA-ECM coating
can be implemented on the porous Ti2448 scaffolds, which significantly
improve the biological functions of orthopedic implants.
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