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Enhanced oral bioavailability of piroxicam in rats by hyaluronate microspheres

Authors
Piao, Ming GuanKim, Jeong-HoonKim, Jong OhLyoo, Won SeokLee, Mann HyungYong, Chul SoonChoi, Han-Gon
Issue Date
Apr-2007
Publisher
TAYLOR & FRANCIS INC
Keywords
microspheres; piroxicam; sodium hyaluronate; polyethylene glycol; dissolution; bbioavailability
Citation
DRUG DEVELOPMENT AND INDUSTRIAL PHARMACY, v.33, no.4, pp 485 - 491
Pages
7
Indexed
SCIE
SCOPUS
Journal Title
DRUG DEVELOPMENT AND INDUSTRIAL PHARMACY
Volume
33
Number
4
Start Page
485
End Page
491
URI
https://scholarworks.bwise.kr/erica/handle/2021.sw.erica/43807
DOI
10.1080/03639040600865223
ISSN
0363-9045
1520-5762
Abstract
To enhance the dissolution and oral bioavailability of poorly water soluble piroxicam, the piroxicam-loaded hyaluronic microspheres were prepared with various ratios of piroxicam, sodium hyaluronate and polyethylene glycol 4000 (PEG) using a spray dryer, and their physicochemical properties such as shape, size, drug-loading efficiency and dissolution were investigated. The pharmacokinetic study of piroxicam-loaded hyaluronic micropheres in rats was then performed compared to piroxicam powder. The piroxicam-loaded hyaluronic microspheres, spherical in shape, had the geometric mean diameters of about 1.5 mu m and drug loading efficiency of about 90%, irrespective of ratio of piroxicam/sodium hyaluronate/PEG. The hyaluronic microspheres containing PEG gave significantly higher dissolution rates of drug than did piroxicam powder, PEG-based solid dispersion system and hyaluronic microspheres without PEG, suggesting that the hyaluronic microsphere with sodium hyaluronate and PEG was more useful for improving the dissolution rate of poorly water soluble piroxicam. The piroxicam-loaded hyaluronic microcapsule composed of (piroxicam/sodium hyaluronate/PEG; 2: 20: 1) gave about threefold improved dissolution of drug in water for 4 h compared to piroxicam powder. It showed higher plasma concentrations of drug compared to piroxicam powder. It gave significantly higher AUC and faster Tmax of piroxicam than did piroxicam powder. In particular, the AUC of piroxicam from hyaluronic microsphere was about twofold higher than that from piroxicam powder, suggesting that it could enhance the oral bioavailability of piroxicam. Thus, the hyaluronic microsphere developed using spray-drying technique with sodium hyaluronate and PEG was a more effective oral dosage form for poorly water soluble piroxicam.
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