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Immobilization of Coacervate Microcapsules in Multilayer Sodium Alginate Beads for Efficient Oral Anticancer Drug Delivery

Authors
Feng, ChaoSong, RuixiSun, GuohuiKong, MingBao, ZixianLi, YangCheng, XiaojieCha, DongsuPark, HyunjinChen, Xiguang
Issue Date
3월-2014
Publisher
AMER CHEMICAL SOC
Citation
BIOMACROMOLECULES, v.15, no.3, pp.985 - 996
Indexed
SCIE
SCOPUS
Journal Title
BIOMACROMOLECULES
Volume
15
Number
3
Start Page
985
End Page
996
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/99102
DOI
10.1021/bm401890x
ISSN
1525-7797
Abstract
We have designed and evaluated coacervate microcapsules-immobilized multilayer sodium alginate beads (CMs-M-ALG-Beads) for oral drug delivery. The CMs-M-ALG-Beads were prepared by immobilization of doxorubicin hydrochloride (DOX) loaded chitosan/carboxymethyl coacervate microcapsules (DOX:CS/CMCS-CMs) in the core and layers of the multilayer sodium alginate beads. The obtained CMs-M-ALG-beads exhibited layer-by-layer structure and rough surface with many nanoscale particles. The swelling characteristic and drug release results indicated that 4-layer CMs-M-ALG-Beads possessed favorable gastric acid tolerance (the swelling rate <5%, the cumulative drug release rate <3.8%). In small intestine, the intact DOX:CS/CMCS-CMs were able to rapidly release from CMs-M-ALG-Beads with the dissolution of ALG matrix. Ex vivo intestinal mucoadhesive and permeation showed that CMs-M-ALG-Beads exhibited continued growth for P-app values of DOX, which was 1.07-1.15 folds and 1.28-1.38 folds higher than DOX:CS:CMCS-CMs in rat jejunum and ileum, respectively, demonstrating that CMs-M-ALG-Beads were able to enhance the absorption of DOX by controlled releasing DOX:CS/CMCS-CMs and prolonging the contact time between the DOX:CS/CMCS-CMs and small intestinal mucosa.
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생명과학대학 (식품공학과)
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