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Target specific and long-acting delivery of protein, peptide, and nucleotide therapeutics using hyaluronic acid derivatives SCIE SCOPUS

Title
Target specific and long-acting delivery of protein, peptide, and nucleotide therapeutics using hyaluronic acid derivatives
Authors
Oh, EJPark, KKim, KSKim, JYang, JAKong, JHLee, MYHoffman, ASHahn, SK
Date Issued
2010-01-04
Publisher
ELSEVIER SCIENCE BV
Abstract
Hyaluronic acid (HA) is a biodegradable, biocompatible, non-toxic, non-immunogenic and non-inflammatory linear polysaccharide, which has been used for various medical applications such as arthritis treatment, ocular surgery, tissue augmentation, and so on. In this review, the effect of chemical modification of HA on its distribution throughout the body was reported for target specific and long-acting delivery applications of protein, peptide, and nucleotide therapeutics. According to the real-time bio-imaging of HA derivatives using quantum dots (QDot). HA-QDot conjugates with 35 mol% HA modification maintaining enough binding sites for HA receptors were mainly accumulated in the liver, while those with 68 mol% HA modification losing much of HA characteristics were evenly distributed to the tissues in the body. The results are well matched with the fact that HA receptors are abundantly present in the liver with a high specificity to HA molecules. Accordingly, slightly modified HA derivatives were used for target specific intracellular delivery of nucleotide therapeutics and highly modified HA derivatives were used for long-acting conjugation of peptide and protein therapeutics. HA has been also used as a novel depot system in the forms of physically and chemically crosslinked hydrogels for various protein drug delivery. This review will give you a peer overview on novel HA derivatives and the latest advances in HA-based drug delivery systems of various biopharmaceuticals for further clinical development. (C) 2009 Elsevier B.V. All rights reserved.
Keywords
Hyaluronic acid; Bio-imaging; Conjugation; Hydrogel; Drug delivery; SUSTAINED-RELEASE FORMULATION; IN-VIVO; QUANTUM-DOT; GENE DELIVERY; DRUG-DELIVERY; INTRACELLULAR DELIVERY; SODIUM HYALURONATE; EXTRACELLULAR GLYCOSAMINOGLYCANS; ANTITUMOR BIOCONJUGATE; LYMPHATIC ENDOTHELIUM
URI
https://oasis.postech.ac.kr/handle/2014.oak/26410
DOI
10.1016/J.JCONREL.2009.09.010
ISSN
0168-3659
Article Type
Article
Citation
JOURNAL OF CONTROLLED RELEASE, vol. 141, no. 1, page. 2 - 12, 2010-01-04
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한세광HAHN, SEI KWANG
Dept of Materials Science & Enginrg
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