Preparation and characterisation of phenytoin-loaded alginate and alginate-chitosan microparticles

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Abstract

We aimed to prepare and investigate microparticles with the varying contents of calcium gelling ion, loaded with phenytoin, a standard antiepileptic agent, in its acidic form. Two different methods of alginate-based microparticles preparation were used: with and without treatment with chitosan. Furthermore, two standard procedures, the one-stage and the two-stage, were applied. Microparticle size of 12 one-stage formulations ranged from 466 to 636 μm. Both types of formulations, chitosan-treated and nontreated, appeared to be highly loaded with the model drug (91-96%). The chitosan-coated alginate-based microparticles prepared by the one-stage procedure exhibited kinetics of phenytoin liberation comparable to a similar sustained release system that had been tested at pH 6.8, as published earlier. As the gel erosion of alginate-based microparticles should be potentiated by the higher pH (used in the present study at pH 7.4), the most favorable of 12 formulations, with the liberation half-time of about 2 hr, seemed to be eligible for further modifications. Counterintuitively, the applied two-stage procedure did not appear to beneficially affect the dissolution behavior of phenytoin when tested in two formulations, which makes further modifications necessary. Copyright © Informa Healthcare USA, Inc.

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Cekić, N. D., Savić, S. D., Milić, J., Savić, M. M., Jović, Ž., & Malešević, M. (2007). Preparation and characterisation of phenytoin-loaded alginate and alginate-chitosan microparticles. Drug Delivery, 14(8), 483–490. https://doi.org/10.1080/10717540701604769

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