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用于光学生物成像的血清稳定量子点-蛋白质杂化纳米胶囊

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

作者信息

Lee Jeong Yu, Heon Nam Dong, Oh Mi Hwa, Kim Youngsun, Choi Hyung Seok, Jeon Duk Young, Park Chan Beum, Nam Yoon Sung

机构信息

Department of Materials Science and Engineering, Korea Advanced Institute of Science and Technology, Daejeon 305-701, Republic of Korea.

出版信息

Nanotechnology. 2014 May 2;25(17):175702. doi: 10.1088/0957-4484/25/17/175702. Epub 2014 Apr 10.

DOI:10.1088/0957-4484/25/17/175702
PMID:24722191
Abstract

We introduce shell cross-linked protein/quantum dot (QD) hybrid nanocapsules as a serum-stable 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 tumor-targeting 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 QD-loaded 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 cadmium-based 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.

摘要

我们引入了壳交联蛋白/量子点(QD)杂化纳米胶囊,作为一种血清稳定的全身递送纳米载体,用于肿瘤靶向体内生物成像应用。合成了高发光、无重金属的Cu0.3InS2/ZnS(CIS/ZnS)核壳量子点,并在二氯甲烷中与胺反应性六臂聚乙二醇(PEG)混合。在含有人类血清白蛋白(HSA)的水溶液中乳化,得到包含CIS/ZnS量子点的壳交联纳米胶囊,在含血清培养基中表现出高发光性和优异的分散稳定性。引入叶酸作为肿瘤靶向配体。通过将纳米胶囊尾静脉注射到裸鼠体内后测量几个主要器官和肿瘤组织的荧光强度,证明了肿瘤靶向体内生物成像的可行性。还在几种类型的细胞中检测了负载量子点的HSA-PEG纳米胶囊的细胞毒性。我们的结果表明,量子点的细胞摄取对细胞毒性至关重要。此外,与负载镉基量子点的纳米胶囊相比,在CIS/ZnS量子点中观察到的细胞死亡水平显著更低。这项研究表明,使用壳交联HSA-PEG杂化纳米胶囊对无重金属量子点进行全身肿瘤靶向是一种有前途的体内肿瘤诊断途径,可降低非特异性毒性。

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