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이온토포레시스를 이용한 케토프로펜의 경피전달Iontophoretic Transport of Ketoprofen

Other Titles
Iontophoretic Transport of Ketoprofen
Authors
김정애오승열
Issue Date
Aug-2004
Publisher
한국약제학회
Citation
Journal of Pharmaceutical Investigation, v.34, no.4, pp 275 - 281
Pages
7
Journal Title
Journal of Pharmaceutical Investigation
Volume
34
Number
4
Start Page
275
End Page
281
URI
https://scholarworks.sookmyung.ac.kr/handle/2020.sw.sookmyung/15846
ISSN
2093-5552
2093-6214
Abstract
We have studied the effect of polarity, current density, current duration, crosslinking density, swelling ratio, and permeation enhancers on the transdermal flux of ketoprofen from acrylamide hydrogel. Hydrogel was prepared by free radical crosslinking polymerization of acrylamide. Drug loading was made just before transport experiment by soaking the hydrogel in solution containing drug. In vitro flux study using hairless mouse skin was performed at 36.5℃ using side-byside diffusion cell, and the drug was analysed using HPLC/UV system. The result showed that, compared to passive flux, the total amount of drug transported increased about 18 folds by the application of 0.4 mA/㎠ cathodal current. Anodal delivery with same current density also increased the total amount of drug transported about 13 folds. It seemed that the increase in flux was due to the electrorepulsion and the increase in passive permeability of the skin by the current application. Flux increased as current density, the duration of current application and loading amount (swelling duration) increased. As the crosslinking density of the hydrogel increased, flux clearly decreased. The effect of hydrophilic enhancers (urea, N-methyl pyrrolidone, Tween 20) and some hydrophobic enhancers (propylene glycol monolaurate and isopropyl myristate) was minimal. However, about 3 folds increase in flux was observed when 5% oleic acid was used. Overall, these results provide some useful information on the design of an optimized iontophoretic delivery system of ketoprofen.
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