Please use this identifier to cite or link to this item: https://ir.swu.ac.th/jspui/handle/123456789/14253
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dc.contributor.authorPhongpradist R.
dc.contributor.authorChittasupho C.
dc.contributor.authorIntasai N.
dc.contributor.authorSiahaan T.J.
dc.contributor.authorBerkland C.J.
dc.contributor.authorCharoenkwan P.
dc.contributor.authorAnuchapreeda S.
dc.contributor.authorAmpasavate C.
dc.date.accessioned2021-04-05T03:33:50Z-
dc.date.available2021-04-05T03:33:50Z-
dc.date.issued2012
dc.identifier.issn19492944
dc.identifier.other2-s2.0-84881137715
dc.identifier.urihttps://ir.swu.ac.th/jspui/handle/123456789/14253-
dc.identifier.urihttps://www.scopus.com/inward/record.uri?eid=2-s2.0-84881137715&doi=10.1115%2f1.4023896&partnerID=40&md5=f41ec658d96b389311aeaa776a8333b3
dc.description.abstractThe lymphocyte function associated antigen-1 (LFA-1) is evaluated for a targeting carrier in leukemia. The cIBR peptide was utilized as the targeting moiety for the drug carrier in direct targeting to LFA-1 expressing cancer cells. This study aims to evaluate the effects of the cIBR peptide conjugation on the specific targeting delivery to the leukemic cell line. Poly (D, L lactide-co-glycolide) (PLGA) nanoparticles were conjugated to the cIBR peptide by three different approaches (coupling, head, and tail) in order to evaluate the nanoparticles' characters, targetability, uptake, drug releasing, and cytotoxicity of each approach. The prepared PLGA nanoparticles were spherical lin shape with a size range of 200-450 nm. The targetability and uptake of three types of cIBR-conjugated nanoparticles (cIBR-NPs) were evidenced and quantified by flow cytometry. The coupling approach presented the highest targetability, uptake, drug releasing, and cytotoxicity followed by the head and tail approaches, respectively. The peptide conjugation method onto the nanoparticles surface was proven to be a key factor for the nanoparticles' physicochemical characteristicss and their efficient delivery. Copyright © 2013 by ASME.
dc.subjectBiodegradable nanoparticle
dc.subjectConjugation method
dc.subjectDrug carrier
dc.subjectLeukemia
dc.subjectPaclitaxel
dc.subjectPLGA nanoparticles
dc.subjectSurface modification techniques
dc.subjectTargeting deliveries
dc.subjectAntigens
dc.subjectCell culture
dc.subjectCopolymers
dc.subjectDiseases
dc.subjectFunction evaluation
dc.subjectLymphocytes
dc.subjectPeptides
dc.subjectNanoparticles
dc.subjectcarboxyl group
dc.subjectcIBR peptide
dc.subjectcIBR peptide polyglactin nanoparticle conjugate
dc.subjectcyclopeptide
dc.subjectdrug carrier
dc.subjectlymphocyte function associated antigen 1
dc.subjectnanoparticle
dc.subjectpaclitaxel
dc.subjectpolyglactin nanoparticle
dc.subjectunclassified drug
dc.subjectarticle
dc.subjectbiodegradability
dc.subjectcell viability
dc.subjectchemical modification
dc.subjectchemical procedures
dc.subjectcontrolled study
dc.subjectcoupling conjugation
dc.subjectdrug binding
dc.subjectdrug conjugation
dc.subjectdrug cytotoxicity
dc.subjectdrug delivery system
dc.subjectdrug dosage form comparison
dc.subjectdrug effect
dc.subjectdrug formulation
dc.subjectdrug release
dc.subjectdrug safety
dc.subjectdrug specificity
dc.subjectdrug stability
dc.subjectdrug targeting
dc.subjectdrug uptake
dc.subjectemulsion
dc.subjectevaporation
dc.subjectflow cytometry
dc.subjecthead conjugation
dc.subjectIC 50
dc.subjectin vitro study
dc.subjectinternalization
dc.subjectleukemia cell
dc.subjectnanoencapsulation
dc.subjectparticle size
dc.subjectphysical chemistry
dc.subjectsolvent displacement
dc.subjectsurface charge
dc.subjectsurface property
dc.subjecttail conjugation
dc.subjectzeta potential
dc.titleBiodegradable nanoparticles surface modification techniques with cIBR peptide targeting to LFA-1 expressing leukemic cells
dc.typeArticle
dc.rights.holderScopus
dc.identifier.bibliograpycitationJournal of Nanotechnology in Engineering and Medicine. Vol 3, No.4 (2012), p.-
dc.identifier.doi10.1115/1.4023896
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