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The microencapsulated ascorbic acid release in vitro and its effect on iron bioavailability

Authors
Lee, Jun-BeumAhn, JoungjwaLee, JJonghwiKwak, Hae-Soo
Issue Date
Oct-2003
Publisher
PHARMACEUTICAL SOCIETY KOREA
Keywords
microencapsulation; ascorbic acid; iron availability; polyacylglycerol monostearate; medium-chain triacylglycerol
Citation
ARCHIVES OF PHARMACAL RESEARCH, v.26, no.10, pp 874 - 879
Pages
6
Journal Title
ARCHIVES OF PHARMACAL RESEARCH
Volume
26
Number
10
Start Page
874
End Page
879
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/57555
DOI
10.1007/BF02980035
ISSN
0253-6269
1976-3786
Abstract
The present study was carried out to examine the stability of microencapsulated ascorbic acid in simulated-gastric and intestinal situation in vitro and the effect of microencapsulated ascorbic acid on iron bioavailability. Coating materials used were polyglycerol monostearate (PGMS) and medium-chain triacylglycerol (MCT), and core materials were L-ascorbic acid and ferric ammonium sulfate. When ascorbic acid was microencapsulated by MCT, the release of ascorbic acid was 6.3% at pH 5 and 1.32% at pH 2 in simulated-gastric fluids during 60 min. When ascorbic acid was microencapsulated by PGMS, the more ascorbic acid was released in the range of 9.5 to 16.0%. Comparatively, ascorbic acid release increased significantly as 94.7% and 83.8% coated by MCT and PGMS, respectively, for 60 min incubation in simulated-intestinal fluid. In the subsequent study, we tested whether ascorbic acid enhanced the iron bioavailability or not. In results, serum iron content and transferring saturation increased dramatically when subjects consumed milks containing both encapsulated iron and encapsulated ascorbic acid, compared with those when consumed uncapsulated iron or encapsulated iron without ascorbic acid. Therefore, the present data indicated that microencapsulated ascorbic acid with both PGMS and MCT were effective means for fortifying ascorbic acid into milk and for enhancing the iron bioavailability.
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공과대학 (화학공학과)
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