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Drug Release from a Chemically-Anchored PEG/Phospholipid Monolayer onto Polymer-Coated Metallic Stents

Authors
Krishna, Ohm DivyamJeon, Ok CheolKim, KwangmeyungByun, YoungroMoon, Hyun Tae
Issue Date
2010-04
Publisher
VSP BV
Citation
JOURNAL OF BIOMATERIALS SCIENCE-POLYMER EDITION, v.21, no.6-7, pp.789 - 802
Abstract
We have prepared a covalently-grafted phsopholipid/PEG mixed monolayer onto drug-loaded polymer-coated stainless-steel stents by in situ polymerization. To introduce a biocompatile surface on the stent surface, AcPC (1-palmitoyl-2-[12-(acryloyloxy) dodecanoyl]-sn-glycero-3-phosphocholine) and AcPEG (12( acryloyloxy) dodecanoyl-poly(ethylene glycol)) were synthesized by modifying phospholipid and PEG with 12-(acryloyloxy)-1-dodecanoic acid and 12-(acryloyloxy)-1-dodecanol, respectively. Also, an acrylated co-polymer was synthesized by the acrylation of poly(octadecyl acrylate-co-hydroxybutyl acrylate, poly(OA-co-HA)) with acryloyl chloride, and poly(OA-co-HA) loaded with a hydrophobic drug, echinomycin, was coated on the stent surface using a spray coating system. In situ polymerization was carried out at the interface between a pre-assembled AcPC/AcPEG mixture and the enchinomycin-loaded acrylated co-polymer-coated stainless steel (Pol-SS). The physicochemical properties of a covalently-grafted phsopholipid/PEG mixed monolayer onto the drug-loaded polymer-coated stainless-steel stents were evaluated using water contact angle, field-emission scanning electron microscopy (FE-SEM) and X-ray photoelectron spectroscopy (XPS). The data confirmed a successful phsopholipid/PEG monolayer grafting on the stents surface. The drug-release profile showed a sustained and controllable release pattern by the top-coated stents, achieved by adjusting the amount of loaded drug. (C) Koninklijke Brill NV, Leiden, 2010
Keywords
IN-SITU PHOTOPOLYMERIZATION; PHOSPHOLIPID MONOLAYER; CYTOMIMETIC BIOMATERIALS; POLY(ETHYLENE GLYCOL); TERMINATED SUBSTRATE; ALKYLATED SURFACE; ELUTING STENTS; RESTENOSIS; ADSORPTION; IN-SITU PHOTOPOLYMERIZATION; PHOSPHOLIPID MONOLAYER; CYTOMIMETIC BIOMATERIALS; POLY(ETHYLENE GLYCOL); TERMINATED SUBSTRATE; ALKYLATED SURFACE; ELUTING STENTS; RESTENOSIS; ADSORPTION; PEG/phospholipid monolayer; biocompatibility; in situ polymerization; drug-eluting stent
ISSN
0920-5063
URI
https://pubs.kist.re.kr/handle/201004/131572
DOI
10.1163/156856209X445294
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KIST Article > 2010
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