Tumor-homing photosensitizer-conjugated glycol chitosan nanoparticles for synchronous photodynamic imaging and therapy based on cellular on/off system

Authors
Lee, So JinKoo, HeebeomLee, Dong-EunMin, SolkiLee, SeulkiChen, XiaoyuanChoi, YongseokLeary, James F.Park, KinamJeong, Seo YoungKwon, Ick ChanKim, KwangmeyungChoi, Kuiwon
Issue Date
2011-06
Publisher
ELSEVIER SCI LTD
Citation
BIOMATERIALS, v.32, no.16, pp.4021 - 4029
Abstract
Herein, we developed the photosensitizer, protoporphyrin IX (PpIX), conjugated glycol chitosan (GC) nanoparticles (PpIX-GC-NPs) as tumor-homing drug carriers with cellular on/off system for photodynamic imaging and therapy, simultaneously. In order to prepare PpIX-GC-NPs, hydrophobic PpIXs were chemically conjugated to GC polymer and the amphiphilic PpIX-GC conjugates formed a stable nanoparticle structure in aqueous condition, wherein conjugated PpIX molecules formed hydrophobic inner-cores and they were covered by the hydrophilic GC polymer shell. Based on the nanoparticle structure. PpIX-GC-NPs showed the self-quenching effect that is 'off' state with no fluorescence signal and phototoxicity with light exposure. It is due to the compact crystallized PpIX molecules in the nanoparticles as confirmed by dynamic light scattering and X-ray diffraction methods. However, after cellular uptake, compact nanoparticle structure gradually decreased to generate strong fluorescence signal and singlet oxygen generation when irradiated. Importantly, PpIX-GC-NPs-treated mice presented prolonged blood circulation, enhanced tumor targeting ability, and improved in vivo therapeutic efficiency in tumor-bearing mice, compared to that of free PpIX-treated mice. These results proved that this tumor-homing cellular 'on/off nanoparticle system of PpIX-GC-NPs has a great potential for synchronous photodynamic imaging and therapy in cancer treatment. (C) 2011 Elsevier Ltd. All rights reserved.
Keywords
MICELLES; RELEASE; DELIVERY; MICELLES; RELEASE; DELIVERY; Photosensitizer; Nanoparticle; Photodynamic therapy; Drug delivery; Glycol chitosan; Cellular on-off system
ISSN
0142-9612
URI
https://pubs.kist.re.kr/handle/201004/130298
DOI
10.1016/j.biomaterials.2011.02.009
Appears in Collections:
KIST Article > 2011
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