Serum-stable quantum dot-protein hybrid nanocapsules for optical bio-imaging

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We introduce shell cross-linked protein/quantum dot (QD) hybrid nanocapsules as a serumstable systemic delivery nanocarrier for tumor-targeted in vivo bio-imaging applications. Highly luminescent, heavy-metal-free Cu0.3InS2/ZnS (CIS/ZnS) core-shell QDs are synthesized and mixed with amine-reactive six-armed poly(ethylene glycol) (PEG) in dichloromethane. Emulsification in an aqueous solution containing human serum albumin (HSA) results in shell cross-linked nanocapsules incorporating CIS/ZnS QDs, exhibiting high luminescence and excellent dispersion stability in a serum-containing medium. Folic acid is introduced as a tumortargeting ligand. The feasibility of tumor-targeted in vivo bio-imaging is demonstrated by measuring the fluorescence intensity of several major organs and tumor tissue after an intravenous tail vein injection of the nanocapsules into nude mice. The cytotoxicity of the QDloaded HSA-PEG nanocapsules is also examined in several types of cells. Our results show that the cellular uptake of the QDs is critical for cytotoxicity. Moreover, a significantly lower level of cell death is observed in the CIS/ZnS QDs compared to nanocapsules loaded with cadmiumbased QDs. This study suggests that the systemic tumor targeting of heavy-metal-free QDs using shell cross-linked HSA-PEG hybrid nanocapsules is a promising route for in vivo tumor diagnosis with reduced non-specific toxicity.
Publisher
IOP PUBLISHING LTD
Issue Date
2014-05
Language
English
Article Type
Article
Citation

NANOTECHNOLOGY, v.25, no.17

ISSN
0957-4484
DOI
10.1088/0957-4484/25/17/175702
URI
http://hdl.handle.net/10203/189048
Appears in Collection
MS-Journal Papers(저널논문)
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