Article ID Journal Published Year Pages File Type
155764 Chemical Engineering Science 2012 11 Pages PDF
Abstract

The analysis of the release kinetics from a delivery system containing amorphous and/or nano-crystalline drug requires the evaluation of many parameters among which the water solubility of the amorphous/nano-crystalline drug is one of the most important. This, in turn, needs the determination of the drug melting enthalpy/temperature dependence on the curvature radius of the crystalline phase (thought, for the sake of simplicity, of spherical shape). Accordingly, this paper is aimed to develop a general theoretical approach devoted to model the melting enthalpy/temperature variation with nano-crystals radius, the solubility dependence on nano-crystals radius and the release process from an ensemble of polymeric particles (crosslinked polyvinylpyrrolidone) containing a poorly water soluble drug (nimesulide) in its amorphous and nano-crystalline status. Drug loading was achieved by means of drug and polymer co-grinding. This study allowed the determination of the nanocrystals fraction and size distribution in the co-ground systems, the drug solubility increase of nano-crystals and the estimation of amorphous drug solubility. This approach yielded to the conclusion that, in the case of nimesulide, a significant increase of solubility occurs for the amorphous form and for nanocrystals characterised by radii lower than 4 nm.

► Drug solubility, melting enthalpy-temperature, crystal radius: theoretical relation. ► Determination of nanocrystal mass fraction and size distribution from DSC data. ► Drug release from coground polymer–drug system: modelling. ► Determination of amorphous drug solubility.

Related Topics
Physical Sciences and Engineering Chemical Engineering Chemical Engineering (General)
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