Luyin Lin scite author profile

The drug-loaded polyvinyl alcohol (PVA)/chitosan (CS) composite nanofibers intended to be used as matrix for transdermal drug delivery were fabricated by electrospinning, and then crosslinked through glulataraldehyde (GA). The morphology, chemical structure, thermal behavior, mechanical properties, hydrophilicity and drug release properties of drug-loaded PVA/CS composite nanofibers before and after crosslinking were characterized. The results showed that the morphology of PVA/CS composite nanofibers was not been destroyed in both crosslinking and in vitro drug release process. The Young's modulus, tensile strength, thermal properties and hydrophobicity of crosslinked PVA/CS composite nanofibers significantly increased in comparison with those of PVA/CS (without crosslinking) due to the formation of crosslinking network structure. In vitro release studies showed that crosslinked PVA/ CS composite nanofibers had lower drug release rate and smaller amount of drug burst release than that of PVA/CS. According to release exponent "n", the release of ampicillin sodium from crosslinked PVA/CS composite nanofibers fit to the Fickian diffusion mechanism. Those results demonstrate the potential utilization of crosslinked PVA/CS composite nanofibers as a transdermal drug delivery system. K E Y W O R D Schitosan (CS), crosslinking, drug delivery, electrospinning, polyvinyl alcohol (PVA) How to cite this article: Cui Z, Zheng Z, Lin L, et al. Electrospinning and crosslinking of polyvinyl alcohol/ chitosan composite nanofiber for transdermal drug delivery.

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Fabrication and characterization of chitosan/OGP coated porous poly(ε-caprolactone) scaffold for bone tissue engineering

Cui

Lin

et al. 2017

Journal of Biomaterials Science, Polymer Edition

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As one of the stimulators on bone formation, osteogenic growth peptide (OGP) improves both proliferation and differentiation of the bone cells in vitro and in vivo. The aim of this work was the preparation of three dimensional porous poly(ε-caprolactone) (PCL) scaffold with high porosity, well interpore connectivity, and then its surface was modified by using chitosan (CS)/OGP coating for application in bone regeneration. In present study, the properties of porous PCL and CS/OGP coated PCL scaffold, including the microstructure, water absorption, porosity, hydrophilicity, mechanical properties, and biocompatibility in vitro were investigated. Results showed that the PCL and CS/OGP-PCL scaffold with an interconnected network structure have a porosity of more than 91.5, 80.8%, respectively. The CS/OGP-PCL scaffold exhibited better hydrophilicity and mechanical properties than that of uncoated PCL scaffold. Moreover, the results of cell culture test showed that CS/OGP coating could stimulate the proliferation and growth of osteoblast cells on CS/OGP-PCL scaffold. These finding suggested that the surface modification could be a effective method on enhancing cell adhesion to synthetic polymer-based scaffolds in tissue engineering application and the developed porous CS/OGP-PCL scaffold should be considered as alternative biomaterials for bone regeneration.

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Luyin Lin

Electrospinning and crosslinking of polyvinyl alcohol/chitosan composite nanofiber for transdermal drug delivery

Fabrication and characterization of chitosan/OGP coated porous poly(ε-caprolactone) scaffold for bone tissue engineering

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