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Original Article

In vitro evaluation of gentamicin- and vancomycin-containing minitablets as a replacement for fortified eye drops

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Pages 1259-1270 | Received 04 Nov 2009, Accepted 19 Feb 2010, Published online: 14 Jun 2010
 

Abstract

Objective: Ocular bioadhesive minitablets containing gentamicin and vancomycin were developed using different powder mixtures of pregelatinized starch and Carbopol (physical or cospray-dried mixtures). Methods: Drug content, antimicrobial activity, and radical formation of the powders used for tablet preparation were evaluated immediately and 30 days after gamma sterilization. Tablet properties and in vitro drug release from the sterilized minitablets were determined. Storage stability of vancomycin and gentamicin in sterilized bioadhesive mixtures was examined by LC–UV/MS and a microbiological assay, respectively. A bioadhesive powder mixture containing only vancomycin was irradiated by X electron-magnetic radiation to evaluate vancomycin stability following sterilization through irradiation. Results: The antimicrobial activity of gentamicin against Staphylococcus epidermidis was not altered in comparison to nonsterilized formulations. Only after an overkill dose of 50 kGy, the concentration of vancomycin decreases to an extent that was pharmaceutically significant. No significant difference in radiation stability between drug substance and product (i.e., powder mixture) was observed. A shift in stability profile was not observed at 6 weeks after irradiation. All other degradation products were present only in small quantities not exceeding 1.0%. The in vitro drug release from the minitablets prepared with physical powder mixtures of pregelatinized starch and Carbopol® 974P NF (96 : 4) was faster compared to the cospray-dried mixtures of starch with Carbopol® 974P NF (ratio: 95:5 and 85:15). The electron paramagnetic resonance signals of the radicals formed during sterilization were still visible after storage for 30 days. The slug mucosal irritation test indicated mild irritation properties of the bioadhesive powder mixtures although no tissue damage was observed.

Acknowledgments

S. Bozdag is grateful to the University of Antwerp and to Ghent University (Belgium) for the scholarship provided. The authors thank Dr. Pierre Dardenne, IBA Mediris S.A. (Fleurus, Belgium), for gamma sterilization of the minitablets, Cerestar (Vilvoorde, Belgium) for drum dried waxy maize starch, Prof. Luc Van Hoorebeke (Department of Subatomic and Radiation Physics, Ghent University, Belgium) for radiation of the gentamicin and vancomycin stability samples, and S. Bodé for the help provided during LC–UV/MS analysis.

Declaration of interest

The authors report no conflicts of interest. The authors alone are responsible for the content and writing of this paper.

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