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Bioactive/Natural Polymeric Scaffolds Loaded with Ciprofloxacin for Treatment of Osteomyelitis
Authors:Amany A Mostafa  Mayyada M H El-Sayed  Azza A Mahmoud  Amira M Gamal-Eldeen
Institution:1.Ceramics Department,National Research Centre (NRC),Cairo,Egypt;2.Nanomedicine and Tissue Engineering Laboratory,Medical Research Centre of Excellence, NRC,Cairo,Egypt;3.Chemical Engineering Department,National Research Centre (NRC),Cairo,Egypt;4.Chemistry Department,American University in Cairo,New Cairo,Egypt;5.Pharmaceutical Technology Department,National Research Centre,Cairo,Egypt;6.Pharmaceutics and Pharmaceutical Technology Department, Faculty of Pharmaceutical Sciences and Pharmaceutical Industries,Future University in Egypt,Cairo,Egypt;7.Cancer Biology and Genetics Laboratory, Centre of Excellence for Advanced Sciences,NRC,Cairo,Egypt;8.Biochemistry Department,NRC,Cairo,Egypt
Abstract:Local delivery of antibiotic into injured bone is a demand. In this work, different scaffolds of chitosan (C) with or without bioactive glass (G) were prepared using the freeze-drying technique in 2:1, 1:1, and 1:2 weight ratios. Chitosan scaffolds and selected formulas of chitosan to bioglass were loaded with ciprofloxacin in 5%, 10%, and 20% w/w. Scaffold morphology showed an interconnected porous structure, where the glass particles were homogeneously dispersed in the chitosan matrix. The kinetic study confirmed that the scaffold containing 1:2 weight ratio of chitosan to glass (CG12) showed optimal bioactivity with good compromise between Ca and P uptake capacities and Si release rate. Chitosan/bioactive glass scaffolds showed larger t 50 values indicating less burst drug release followed by a sustained drug release profile compared to that of chitosan scaffolds. The cell growth, migration, adhesion, and invasion were enhanced onto CG12 scaffold surfaces. Samples of CG12 scaffolds with or without 5% drug induced vascular endothelial growth factor (VEGF), while those containing 10% drug diminished VEGF level. Only CG12 induced the cell differentiation (alkaline phosphatase activity). In conclusion, CG12 containing 5% drug can be considered a biocompatible carrier which would help in the localized osteomyelitis treatment.
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