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Cited 16 time in webofscience Cited 20 time in scopus
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Amino-Functionalized Mesoporous Silica Particles for Ocular Delivery of Brimonidine

Authors
Kim, SN[Kim, Se-Na]Ko, SA[Ko, Song Ah]Park, CG[Park, Chun Gwon]Lee, SH[Lee, Seung Ho]Huh, BK[Huh, Beom Kang]Park, YH[Park, Yoh Han]Kim, YK[Kim, Young Kook]Ha, A[Ha, Ahnul]Park, KH[Park, Ki Ho]Choy, YB[Choy, Young Bin]
Issue Date
Aug-2018
Publisher
AMER CHEMICAL SOC
Keywords
brimonidine; drug delivery; glaucoma; mesoporous silica; mucosal adhesion
Citation
MOLECULAR PHARMACEUTICS, v.15, no.8, pp.3143 - 3152
Indexed
SCIE
SCOPUS
Journal Title
MOLECULAR PHARMACEUTICS
Volume
15
Number
8
Start Page
3143
End Page
3152
URI
https://scholarworks.bwise.kr/skku/handle/2021.sw.skku/19126
DOI
10.1021/acs.molpharmaceut.8b00215
ISSN
1543-8384
Abstract
To treat glaucoma, conventional eye drops are often prescribed. However, the eye drops have limited effectiveness as a result of low drug bioavailability due to their rapid clearance from the preocular space. To resolve this, we proposed amino-functionalized mesoporous silica (AMS) particles as delivery carriers of the glaucoma drug, brimonidine. Because of the presence of mesopores, brimonidine (BMD) could be encapsulated in the AMS with a loading amount of 41.73 mu g/mg (i.e., drug loading capacity of about 4.17%) to give the BMD-AMS, which could release the drug in a sustained manner over 8 h. BMD-AMS was also shown to be mucoadhesive due to the presence of both hydroxyl and amino groups in the surface, allowing for formation of hydrogen bonds and an ionic complex with the mucin, respectively. Therefore, when topically administered to rabbit eyes in vivo, BMD-AMS could reside in the preocular space for up to 12 h because of its adherence to the mucous layer. To assess in vivo efficacy, we examined the variance in intraocular pressure (IOP) and brimonidine concentration in the aqueous humor (AH) after applying BMD-AMS to the eye, which was compared with that induced by Alphagan P, the marketed brimonidine eye drops. For BMD-AMS, the duration in the decrease in IOP and the area under the drug concentration in the AH-time curve (AUC) were 12 h and 2.68 mu g.h/mL, respectively, which were about twice as large as those obtained with Alphagan P; this finding indicated enhanced ocular bioavailability of brimonidine with BMD-AMS.
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