Polydopamine mediated assembly of hydroxyapatite nanoparticles and bone morphogenetic protein‐2 on magnesium alloys for enhanced corrosion resistance and bone regeneration

Magnesium alloys have the great potential to be used as orthopedic implants due to their biodegradability and mechanical resemblance to human cortical bone. However, the rapid degradation in physiological environment with the evolution of hydrogen gas release hinders their clinical applications. In...

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Veröffentlicht in:Journal of biomedical materials research. Part A 2017-10, Vol.105 (10), p.2750-2761
Hauptverfasser: Jiang, Yanan, Wang, Bi, Jia, Zhanrong, Lu, Xiong, Fang, Liming, Wang, Kefeng, Ren, Fuzeng
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Sprache:eng
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Zusammenfassung:Magnesium alloys have the great potential to be used as orthopedic implants due to their biodegradability and mechanical resemblance to human cortical bone. However, the rapid degradation in physiological environment with the evolution of hydrogen gas release hinders their clinical applications. In this study, we developed a novel functional and biocompatible coating strategy through polydopamine mediated assembly of hydroxyapatite nanoparticles and growth factor, bone morphogenetic protein‐2 (BMP‐2), onto the surface of AZ31 Mg alloys. Such functional coating has strong bonding with the substrate and can increase surface hydrophilicity of magnesium alloys. In vitro electrochemical corrosion and hydrogen evolution tests demonstrate that the coating can significantly enhance the corrosion resistance and therefore slow down the degradation of AZ31 Mg alloys. In vitro cell culture reveals that immobilization of HA nanoparticles and BMP‐2 can obviously promote cell adhesion and proliferation. Furthermore, in vivo implantation tests indicate that with the synergistic effects of HA nanoparticles and BMP‐2, the coating does not cause obvious inflammatory response and can significantly reduce the biodegradation rate of the magnesium alloys and induce the new bone formation adjacent to the implants. © 2017 Wiley Periodicals, Inc. J Biomed Mater Res Part A: 105A: 2750–2761, 2017.
ISSN:1549-3296
1552-4965
DOI:10.1002/jbm.a.36138