PLGA nanoparticle-peptide conjugate effectively targets intercellular cell-adhesion molecule-1

PLGA nanoparticle-peptide conjugate effectively targets intercellular cell-adhesion molecule-1

Targeted delivery of therapeutics possesses the potential to localize therapeutic agents to a specific tissue as a mechanism to enhance treatment efficacy and abrogate side effects. Antibodies have been used clinically as therapeutic agents and are currently being explored for targeting drug-loaded...

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Main Authors: Zhang N., Chittasupho C., Duangrat C., Siahaan T.J., Berkland C.
Format: Article
Language:English
Published: 2014
Online Access:http://www.scopus.com/inward/record.url?eid=2-s2.0-38949111716&partnerID=40&md5=fb1fa193c605e55397f6c91e1d839cd4
http://cmuir.cmu.ac.th/handle/6653943832/4487
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Institution: Chiang Mai University
Language: English
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spelling th-cmuir.6653943832-44872014-08-30T02:42:29Z PLGA nanoparticle-peptide conjugate effectively targets intercellular cell-adhesion molecule-1 Zhang N. Chittasupho C. Duangrat C. Siahaan T.J. Berkland C. Targeted delivery of therapeutics possesses the potential to localize therapeutic agents to a specific tissue as a mechanism to enhance treatment efficacy and abrogate side effects. Antibodies have been used clinically as therapeutic agents and are currently being explored for targeting drug-loaded nanoparticles. Peptides such as RGD peptides are also being developed as an inexpensive and stable alternative to antibodies. In this study, cyclo(1,12)PenITDGEATDSGC (cLABL) peptide was used to target nanoparticles to human umbilical cord vascular endothelial cell (HUVEC) monolayers that have upregulated intercellular cell-adhesion molecule-1 (ICAM-1) expression. The cLABL peptide has been previously demonstrated to possess high avidity for ICAM-1 receptors on the cell surface. Poly(DL-lactic-coglycolic acid) nanoparticles conjugated with polyethylene glycol and cLABL demonstrated rapid binding to HUVEC with upregulated ICAM-1, which was induced by treating cells with the proinflammatory cytokine, interferon-γ. Binding of the nanoparticles could be efficiently blocked by preincubating cells with free peptide suggesting that the binding of the nanoparticles is specifically mediated by surface peptide binding to ICAM-1 on HUVEC. The targeted nanoparticles were rapidly endocytosed and trafficked to lysosomes to a greater extent than the untargeted PLGA-PEG nanoparticles. Verification of peptide-mediated nanoparticle targeting to ICAM-1 may ultimately lead to targeting therapeutic agents to inflammatory sites expressing upregulated ICAM-1. © 2008 American Chemical Society. 2014-08-30T02:42:29Z 2014-08-30T02:42:29Z 2008 Article 10431802 10.1021/bc700227z 17997512 BCCHE http://www.scopus.com/inward/record.url?eid=2-s2.0-38949111716&partnerID=40&md5=fb1fa193c605e55397f6c91e1d839cd4 http://cmuir.cmu.ac.th/handle/6653943832/4487 English
institution Chiang Mai University
building Chiang Mai University Library
country Thailand
collection CMU Intellectual Repository
language English
description Targeted delivery of therapeutics possesses the potential to localize therapeutic agents to a specific tissue as a mechanism to enhance treatment efficacy and abrogate side effects. Antibodies have been used clinically as therapeutic agents and are currently being explored for targeting drug-loaded nanoparticles. Peptides such as RGD peptides are also being developed as an inexpensive and stable alternative to antibodies. In this study, cyclo(1,12)PenITDGEATDSGC (cLABL) peptide was used to target nanoparticles to human umbilical cord vascular endothelial cell (HUVEC) monolayers that have upregulated intercellular cell-adhesion molecule-1 (ICAM-1) expression. The cLABL peptide has been previously demonstrated to possess high avidity for ICAM-1 receptors on the cell surface. Poly(DL-lactic-coglycolic acid) nanoparticles conjugated with polyethylene glycol and cLABL demonstrated rapid binding to HUVEC with upregulated ICAM-1, which was induced by treating cells with the proinflammatory cytokine, interferon-γ. Binding of the nanoparticles could be efficiently blocked by preincubating cells with free peptide suggesting that the binding of the nanoparticles is specifically mediated by surface peptide binding to ICAM-1 on HUVEC. The targeted nanoparticles were rapidly endocytosed and trafficked to lysosomes to a greater extent than the untargeted PLGA-PEG nanoparticles. Verification of peptide-mediated nanoparticle targeting to ICAM-1 may ultimately lead to targeting therapeutic agents to inflammatory sites expressing upregulated ICAM-1. © 2008 American Chemical Society.
format Article
author Zhang N.
Chittasupho C.
Duangrat C.
Siahaan T.J.
Berkland C.
spellingShingle Zhang N.
Chittasupho C.
Duangrat C.
Siahaan T.J.
Berkland C.
PLGA nanoparticle-peptide conjugate effectively targets intercellular cell-adhesion molecule-1
author_facet Zhang N.
Chittasupho C.
Duangrat C.
Siahaan T.J.
Berkland C.
author_sort Zhang N.
title PLGA nanoparticle-peptide conjugate effectively targets intercellular cell-adhesion molecule-1
title_short PLGA nanoparticle-peptide conjugate effectively targets intercellular cell-adhesion molecule-1
title_full PLGA nanoparticle-peptide conjugate effectively targets intercellular cell-adhesion molecule-1
title_fullStr PLGA nanoparticle-peptide conjugate effectively targets intercellular cell-adhesion molecule-1
title_full_unstemmed PLGA nanoparticle-peptide conjugate effectively targets intercellular cell-adhesion molecule-1
title_sort plga nanoparticle-peptide conjugate effectively targets intercellular cell-adhesion molecule-1
publishDate 2014
url http://www.scopus.com/inward/record.url?eid=2-s2.0-38949111716&partnerID=40&md5=fb1fa193c605e55397f6c91e1d839cd4
http://cmuir.cmu.ac.th/handle/6653943832/4487
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