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Cited 9 time in webofscience Cited 10 time in scopus
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Brimonidine-montmorillonite hybrid formulation for topical drug delivery to the eye

Authors
Park, CG[Park, Chun Gwon]Choi, G[Choi, Goeun]Kim, MH[Kim, Myung Hun]Kim, SN[Kim, Se-Na]Lee, H[Lee, Hanna]Lee, NK[Lee, Na Kyeong]Choy, YB[Choy, Young Bin]Choy, JH[Choy, Jin-Ho]
Issue Date
Sep-2020
Publisher
ROYAL SOC CHEMISTRY
Citation
JOURNAL OF MATERIALS CHEMISTRY B, v.8, no.35, pp.7914 - 7920
Indexed
SCIE
SCOPUS
Journal Title
JOURNAL OF MATERIALS CHEMISTRY B
Volume
8
Number
35
Start Page
7914
End Page
7920
URI
https://scholarworks.bwise.kr/skku/handle/2021.sw.skku/3130
DOI
10.1039/d0tb01213k
ISSN
2050-750X
Abstract
Brimonidine (BMD) is often prescribed as an eye drop to reduce the intraocular pressure (IOP) for glaucoma treatment. However, eye drops are limited by rapid clearance from the preocular surface, and hence a low ocular drug bioavailability. Therefore, in this study, we propose montmorillonite (MMT), as a delivery carrier, hybridized with BMD (BMD-MMT) for topical drug delivery to the eye. The BMD-MMT hybrid was prepared by intercalating the BMD molecules in the interlayer space of the MMT lattice via ion-exchange reaction; it was then formulated with polyvinyl alcohol (PVA) to produce a dry tablet (i.e., BMD-MMT@PVA). The BMD-MMT@PVA hybrid drug released BMD in a sustained manner for more than 5 h under in vitro conditions. When the hybrid drug was administered to rabbit eyes in vivo, 43% and 18.5% BMD-MMT still remained on the preocular surface for 10 and 60 min after administration, respectively. Thus, the BMD-MMT@PVA hybrid drug exhibited a prolonged decrease in IOP, that is, for 12 h, which was approximately two times longer than that observed with the commercially available BMD eye drop, Alphagan (R) P.
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