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Influence of chitosan and chitosan oligosaccharide on dual antibiotic-loaded bone cement: In vitro evaluations
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Background and purposeThe purpose of this study was to investigate the effect of incorporating chitosan (Ch) and chitosan oligosaccharides (ChO) into the commercially premixed antibiotic-loaded bone cement (ALBC). We compare antibiotic release profiles, antibacterial activity, and mechanical properties among different ALBC formulations. The hypothesis was that increasing the amount of Ch and ChO in the cement mixture would increase the antibiotics released and bacterial control. ALBC mixed with Ch or ChO may create a greater effect due to its superior dissolving property.Materials and methodsThe bone cement samples used in this project were made from Copal®G+V composed of vancomycin and gentamicin. To prepare the Ch and the ChO mixed bone cement samples, different amounts of Ch and ChO were added to the polymethylmethacrylate matrix with three concentrations (1%, 5%, and 10%). Drug elution assay, antimicrobial assay,in vitrocytotoxicity, and mechanical properties were conducted.ResultsBone cement samples made from Copal®G+V alone or combined with Ch or ChO can release vancomycin and gentamicin into the phosphate-buffered saline. Mixing ChO into the bone cements can increase the amount of drug released more than Ch. ChO 10% gave the highest amount of antibiotics released. All samples showed good antibacterial properties with good biocompatibilityin vitro. The microhardness values of the Ch and ChO groups increased significantly compared to the control group. In all groups tested, the microhardness of bone cements was reduced after the drug eluted out. However, this reduction of the Ch and ChO groups was in line with the control.InterpretationVarious attempts have been made to improve the ALBC efficacy. In our study, the best bone cement formulation was bone cement mixed with ChO (10%), which had the highest drug release profiles, was biocompatible, and contained antibacterial properties with acceptable mechanical properties. This phenomenon could result from the superior water solubility of the ChO. When ChO leaves the bone cement specimens, it generates pores that could act as a path that exposes the bone cement matrix to the surrounding medium, increasing antibiotic elution. From all above, ChO is a promising substance that could be added to ALBC in order to increase the drug elution rate. However, morein vitroandin vivoexperiments are needed before being used in the clinic.
Public Library of Science (PLoS)
Title: Influence of chitosan and chitosan oligosaccharide on dual antibiotic-loaded bone cement: In vitro evaluations
Description:
Background and purposeThe purpose of this study was to investigate the effect of incorporating chitosan (Ch) and chitosan oligosaccharides (ChO) into the commercially premixed antibiotic-loaded bone cement (ALBC).
We compare antibiotic release profiles, antibacterial activity, and mechanical properties among different ALBC formulations.
The hypothesis was that increasing the amount of Ch and ChO in the cement mixture would increase the antibiotics released and bacterial control.
ALBC mixed with Ch or ChO may create a greater effect due to its superior dissolving property.
Materials and methodsThe bone cement samples used in this project were made from Copal®G+V composed of vancomycin and gentamicin.
To prepare the Ch and the ChO mixed bone cement samples, different amounts of Ch and ChO were added to the polymethylmethacrylate matrix with three concentrations (1%, 5%, and 10%).
Drug elution assay, antimicrobial assay,in vitrocytotoxicity, and mechanical properties were conducted.
ResultsBone cement samples made from Copal®G+V alone or combined with Ch or ChO can release vancomycin and gentamicin into the phosphate-buffered saline.
Mixing ChO into the bone cements can increase the amount of drug released more than Ch.
ChO 10% gave the highest amount of antibiotics released.
All samples showed good antibacterial properties with good biocompatibilityin vitro.
The microhardness values of the Ch and ChO groups increased significantly compared to the control group.
In all groups tested, the microhardness of bone cements was reduced after the drug eluted out.
However, this reduction of the Ch and ChO groups was in line with the control.
InterpretationVarious attempts have been made to improve the ALBC efficacy.
In our study, the best bone cement formulation was bone cement mixed with ChO (10%), which had the highest drug release profiles, was biocompatible, and contained antibacterial properties with acceptable mechanical properties.
This phenomenon could result from the superior water solubility of the ChO.
When ChO leaves the bone cement specimens, it generates pores that could act as a path that exposes the bone cement matrix to the surrounding medium, increasing antibiotic elution.
From all above, ChO is a promising substance that could be added to ALBC in order to increase the drug elution rate.
However, morein vitroandin vivoexperiments are needed before being used in the clinic.
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