Literature DB >> 21524893

Effect of bases with different solubility on the release behavior of risperidone loaded PLGA microspheres.

Zhenhua Hu1, Yajun Liu, Weien Yuan, Fei Wu, Jing Su, Tuo Jin.   

Abstract

Poly (D, L-lactide-co-glycolide) (PLGA) microspheres are attractive delivery vehicles due to their excellent sustained release capabilities. One major problem with PLGA microspheres is that the hydrophobic properties of PLGA generally cause a lag period in the process of drug release, leading to fluctuation of drug concentration in the blood and various resulting adverse reactions. Herein, Mg(OH)₂, an inorganic base, and arginine, an organic base, were separately co-encapsulated into risperidone-loaded PLGA microspheres at varying concentration using the solvent evaporation method to improve release profiles from the microspheres. High encapsulation efficiencies were obtained in all formulations. The surface of base-free microspheres was smooth, whereas a few pores formed in base co-encapsulated microspheres. After 7-days degradation, many inter-connecting pores were formed in the interior of the microspheres containing 10 mg Mg(OH)₂. The final pH in the microspheres with Mg(OH)₂ was higher than in those with arginine after 28-days degradation. The initial release of risperidone from microspheres containing Mg(OH)₂ was higher than from those containing arginine, and the latter release exhibited a more uniform pattern. Microspheres with 5mg and 10mg arginine exhibited zero-order release kinetics. However, both bases eliminated the lag phase of release. These results indicate that the incorporation of bases has potential in addressing the problem of the lag period in drug release from PLGA microspheres, and improving release behavior toward an ideal model.
Copyright © 2011 Elsevier B.V. All rights reserved.

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Year:  2011        PMID: 21524893     DOI: 10.1016/j.colsurfb.2011.03.043

Source DB:  PubMed          Journal:  Colloids Surf B Biointerfaces        ISSN: 0927-7765            Impact factor:   5.268


  10 in total

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5.  The effect of topical administration of simvastatin on entochondrostosis and intramembranous ossification: An animal experiment.

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7.  How bulk fluid renewal can affect in vitro drug release from PLGA implants: Importance of the experimental set-up.

Authors:  C Bassand; L Benabed; J Freitag; J Verin; F Siepmann; J Siepmann
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8.  Exenatide Microspheres for Monthly Controlled-Release Aided by Magnesium Hydroxide.

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9.  Risperidone Controlled Release Microspheres Based on Poly(Lactic Acid)-Poly(Propylene Adipate) Novel Polymer Blends Appropriate for Long Acting Injectable Formulations.

Authors:  Stavroula Nanaki; Panagiotis Barmpalexis; Alexandros Iatrou; Evi Christodoulou; Margaritis Kostoglou; Dimitrios N Bikiaris
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10.  Risperidone-Loaded PLGA-Lipid Particles with Improved Release Kinetics: Manufacturing and Detailed Characterization by Electron Microscopy and Nano-CT.

Authors:  Christopher Janich; Andrea Friedmann; Juliana Martins de Souza E Silva; Cristine Santos de Oliveira; Ligia E de Souza; Dan Rujescu; Christian Hildebrandt; Moritz Beck-Broichsitter; Christian E H Schmelzer; Karsten Mäder
Journal:  Pharmaceutics       Date:  2019-12-09       Impact factor: 6.321

  10 in total

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