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Development of self-microemulsifying bilayer tablets for pH-independent fast release of candesartan cilexetil

Authors
Sohn, YesungLee, Su YeonLee, Ga HyeonNa, Yeon-JooKim, Seong YeonSeong, IlkyeongLee, Beom-JinKuh, Hyo-JeongLee, Jaehwi
Issue Date
Nov-2012
Publisher
GOVI-VERLAG PHARMAZEUTISCHER VERLAG GMBH
Citation
PHARMAZIE, v.67, no.11, pp 917 - 924
Pages
8
Journal Title
PHARMAZIE
Volume
67
Number
11
Start Page
917
End Page
924
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/20081
DOI
10.1691/ph.2012.2003
ISSN
0031-7144
Abstract
The aim of this study was to design self-microemulsifying tablets for pH-independent fast release of poorly soluble candesartan cilexetil (CDC). To improve the solubility of CDC, a self-microemulsifying drug delivery system (SMEDDS) was prepared composed of Capryol 90, Tween 80 and tetraglycol at a ratio of 5:35:60. Drug containing SMEDDS was adsorbed onto Fujicalin and Neusilin UFL2, respectively, used as solidification carriers and subsequently compressed into tablets (self-microemulsifying tablet, SMET). SMET using Fujicalin (R) exhibited immediate CDC release in pH 1.2 medium while Neusilin (R) UFL2-based SMET showed fast release, especially at pH 6.5. Thus, optimized SMET could be produced with one layer of Fujicalin and the other layer with Neusilin UFL2, demonstrating CDC release of 75% of the initial dose within 15 min in all pH conditions (1.2, 4.5, and 6.5). The average diameter of emulsion droplets formed from SMET was less than 200nm. It was thus expected that Fujicalin (R) and Neusilin (R) UFL2-based bi-layer SMET would overcome low oral bioavailability of CDC due to its limited solubility at physiological pH conditions in the gastrointestinal tract.
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