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3D-printed porous zinc scaffold combined with bioactive serum exosomes promotes bone defect repair in rabbit radius. | LitMetric

AI Article Synopsis

  • The study addresses challenges in repairing large bone defects due to the lack of effective bone grafts, introducing a new implant made from a degradable porous zinc scaffold combined with bioactive serum exosomes and a thermosensitive hydrogel.
  • Using advanced 3D printing, the zinc scaffold was found to be non-toxic to cells, and the exosomes enhanced its ability to support bone cell activity while inhibiting bone resorption.
  • Experiments on rabbits showed that this composite implant not only reduced toxicity over time but also improved bone repair through increased bone cell activity and angiogenesis, suggesting it could be a promising strategy in bone defect therapy.

Article Abstract

Currently, the repair of large bone defects still faces numerous challenges, with the most crucial being the lack of large bone grafts with good osteogenic properties. In this study, a novel bone repair implant (degradable porous zinc scaffold/BF Exo composite implant) was developed by utilizing laser melting rapid prototyping 3D printing technology to fabricate a porous zinc scaffold, combining it under vacuum conditions with highly bioactive serum exosomes (BF EXO) and Poloxamer 407 thermosensitive hydrogel. The electron microscope revealed the presence of tea saucer-shaped exosomes with a double-layered membrane structure, ranging in diameter from 30-150 nm, with an average size of 86.3 nm and a concentration of 3.28E+09 particles/mL. experiments demonstrated that the zinc scaffold displayed no significant cytotoxicity, and loading exosomes enhanced the zinc scaffold's ability to promote osteogenic cell activity while inhibiting osteoclast activity. experiments on rabbits indicated that the hepatic and renal toxicity of the zinc scaffold decreased over time, and the loading of exosomes alleviated the hepatic and renal toxic effects of the zinc scaffold. Throughout various stages of repairing radial bone defects in rabbits, loading exosomes reinforced the zinc scaffold's capacity to enhance osteogenic cell activity, suppress osteoclast activity, and promote angiogenesis. This effect may be attributed to BF Exo's regulation of p38/STAT1 signaling. This study signifies that the combined treatment of degradable porous zinc scaffolds and BF Exo is an effective and biocompatible strategy for bone defect repair therapy.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11210218PMC
http://dx.doi.org/10.18632/aging.205891DOI Listing

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