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Bioreducible Micelles Self-Assembled from Poly(ethylene glycol)-Cholesteryl Conjugate As a Drug Delivery Platform
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Title
Bioreducible Micelles Self-Assembled from Poly(ethylene glycol)-Cholesteryl Conjugate As a Drug Delivery Platform
Issued Date
2015-11
Citation
Baek, Chulsu. (2015-11). Bioreducible Micelles Self-Assembled from Poly(ethylene glycol)-Cholesteryl Conjugate As a Drug Delivery Platform. Polymers, 7(11), 2245–2258. doi: 10.3390/polym7111511
Type
Article
Author Keywords
polymeric micellesdrug delivery systembiocompatibledisulfide-thiol exchangestimulus-sensitive polymers
Keywords
BiocompatibilityBiocompatibleCell CultureCELLSControlled Drug DeliveryCovalent BondsCytologyDisulfide-Thiol ExchangeDisulfide-Thiol ExchangesDoxorubicinDrug Delivery SystemDrug ProductsEthylene GlycolINTRACELLULAR DELIVERYMicellesNANOPARTICLESPEGPLA BLOCK-COPOLYMERPolyethylene GlycolsPolymeric MicellePOLYMERIC MICELLESPolymersPolyolsRELEASESolutionsStimulus-Sensitive PolymersSulfur CompoundsSYSTemS
ISSN
2073-4360
Abstract
The ability of polymeric micelles to self-assemble into nanosized particles has created interest in their application as potential anticancer drug delivery systems. A poly(ethylene glycol)-cholesteryl conjugate (Chol-ss-PEG-ss-Chol) connected by cleavable disulfide linkages was synthesized and used as a nanocarrier for in vitro release of doxorubicin (DOX). Owing to its amphiphilic structure, Chol-ss-PEG-ss-Chol was able to self-assemble into micelles with an average diameter 18.6 nm in aqueous solution. The micelles formed large aggregates due to the shedding of the PEG shell through cleavage of disulfide bonds in a reductive environment. The in vitro release studies revealed that Chol-ss-PEG-ss-Chol micelles released 80% and approximately 9% of the encapsulated DOX within 6 h under reductive and non-reductive conditions, respectively. The glutathione (GSH)-mediated intracellular drug delivery was investigated in a KB cell line. The cytotoxicity of DOX-loaded micelles indicated a higher cellular anti-proliferative effect against GSH-pretreated than untreated KB cells. Furthermore, confocal laser scanning microscopy (CLSM) measurement demonstrated that Chol-ss-PEG-ss-Chol micelles exhibited faster drug release in GSH-pretreated KB cells than untreated KB cells. These results suggest the potential usefulness of disulfide-based polymeric micelles as controlled drug delivery carriers. © 2015 by the authors.
URI
http://hdl.handle.net/20.500.11750/2582
DOI
10.3390/polym7111511
Publisher
MDPI AG
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