Please use this identifier to cite or link to this item: https://hdl.handle.net/2440/68386
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Type: Journal article
Title: A galactosamine-mediated drug delivery carrier for targeted liver cancer therapy
Author: Shen, Z.
Wei, W.
Tanaka, H.
Kohama, K.
Ma, G.
Dobashi, T.
Maki, Y.
Wang, H.
Bi, J.
Dai, S.
Citation: Pharmacological Research, 2011; 64(4):410-419
Publisher: Academic Press Ltd
Issue Date: 2011
ISSN: 1043-6618
1096-1186
Statement of
Responsibility: 
Zheyu Shen, Wei Wei, Hideyuki Tanaka, Kazuhiro Kohama, Guanghui Ma, Toshiaki Dobashi, Yasuyuki Maki, Honghui Wang, Jingxiu Bi, Sheng Dai
Abstract: In order to minimize the side effect of cancer chemotherapy, a novel galactosamine-mediated drug delivery carrier, galactosamine-conjugated albumin nanoparticles (GAL-AN), was developed for targeted liver cancer therapy. The albumin nanoparticles (AN) and doxorubicin-loaded AN (DOX-AN) were prepared by the desolvation of albumin in the presence of glutaraldehyde crosslinker. Morphological study indicated the spherical structure of these synthesized particles with an average diameter of around 200 nm. The functional ligand of galactosamine (GAL) was introduced onto the surfaces of AN and DOX-AN via carbodiimide chemistry to obtain GAL-AN and GAL-DOX-AN. Cellular uptake and kinetic studies showed that GAL-AN is able to be selectively incorporated into the HepG2 cells rather than AoSMC cells due to the existence of asialoglycoprotein receptors on HepG2 cell surface. The cytotoxicity, measured by MTT test, indicated that AN and GAL-AN are non-toxic and GAL-DOX-AN is more effective in HepG2 cell killing than that of DOX-AN. As such, our results implied that GAL-AN and GAL-DOX-AN have specific interaction with HepG2 cells via the recognition of GAL and asialoglycoprotein receptor, which renders GAL-AN a promising anticancer drug delivery carrier for liver cancer therapy.
Keywords: Galactosamine
Drug delivery carrier
Targeted therapy
Liver cancer
Rights: Copyright © 2011 Elsevier Ltd. All rights reserved.
DOI: 10.1016/j.phrs.2011.06.015
Published version: http://dx.doi.org/10.1016/j.phrs.2011.06.015
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