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Development of an itraconazole-loaded gelatin microcapsule with enhanced oral bioavailability: physicochemical characterization and in-vivo evaluation

Authors
Li, Dong XunPark, Young-JoonOh, Dong HoonJoe, Kwan HyungLee, Jung HoonYeo, Woo HyunYong, Chul SoonChoi, Han-Gon
Issue Date
Apr-2010
Publisher
WILEY
Keywords
gelatin microcapsule without ethanol; itraconazole; rats; spray drying
Citation
JOURNAL OF PHARMACY AND PHARMACOLOGY, v.62, no.4, pp 448 - 455
Pages
8
Indexed
SCI
SCIE
SCOPUS
Journal Title
JOURNAL OF PHARMACY AND PHARMACOLOGY
Volume
62
Number
4
Start Page
448
End Page
455
URI
https://scholarworks.bwise.kr/erica/handle/2021.sw.erica/39903
DOI
10.1211/jpp.62.04.0006
ISSN
0022-3573
2042-7158
Abstract
Objectives The aim of this study was to develop a novel itraconazole-loaded gelatin microcapsule without ethanol with enhanced oral bioavailability. Methods Various gelatin microcapsules were prepared using a spray-drying technique. Their physicochemical properties, dissolution, characteristics and pharmacokinetics in rats were evaluated and compared with those of a commercial product. Key findings The gelatin microcapsule at a weight ratio for itraconazole/gelatin/citric acid of 1 : 3 : 0.3 was spherical in shape with a smooth surface and inner hole, and gave a maximum drug solubility of about 700 mu g/ml. The gelatin microcapsule dramatically increased the initial dissolution rate of itraconazole compared with a commercial product in simulated gastric fluids (pH 1.2). Moreover, at the same dose as the commercial product, it gave significantly higher initial plasma concentrations, C-max and AUC of itraconazole in rats than did the commercial product, indicating that providing the drug in the gelatin microcapsule caused enhanced absorption in rats. At half dose, it gave similar AUC, C-max and T-max values to the commercial product, suggesting that it was bioequivalent to the commercial product in rats. Conclusions The itraconazole-loaded gelatin microcapsule without ethanol developed using a spray-drying technique at half the dose of the commercial product can deliver itraconazole in a pattern that allows fast absorption in the initial phase, making it bioequivalent to the commercial product.
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