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在小鼠中,经抗体工程化多功能纳米颗粒的主动靶向作用,乳腺癌细胞中的 HER2 表达下调。

HER2 expression in breast cancer cells is downregulated upon active targeting by antibody-engineered multifunctional nanoparticles in mice.

机构信息

Dipartimento di Scienze Cliniche Luigi Sacco, Università di Milano, Ospedale L. Sacco, via G.B. Grassi 74, 20157 Milano, Italy.

出版信息

ACS Nano. 2011 Aug 23;5(8):6383-93. doi: 10.1021/nn201570n. Epub 2011 Aug 1.

DOI:10.1021/nn201570n
PMID:21790185
Abstract

Subcellular destiny of targeted nanoparticles in cancer cells within living organisms is still an open matter of debate. By in vivo and ex vivo experiments on tumor-bearing mice treated with antibody-engineered magnetofluorescent nanocrystals, in which we combined fluorescence imaging, magnetic relaxation, and trasmission electron microscopy approaches, we provide evidence that nanoparticles are effectively delivered to the tumor by active targeting. These nanocrystals were demonstrated to enable contrast enhancement of the tumor in magnetic resonance imaging. In addition, we were able to discriminate between the fate of the organic corona and the metallic core upon cell internalization. Accurate immunohistochemical analysis confirmed that hybrid nanoparticle endocytosis is mediated by the complex formation with HER2 receptor, leading to a substantial downregulation of HER2 protein expression on the cell surface. These results provide a direct insight into the pathway of internalization and degradation of targeted hybrid nanoparticles in cancer cells in vivo and suggest a potential application of this immunotheranostic nanoagent in neoadjuvant therapy of cancer.

摘要

靶向纳米颗粒在活体内癌细胞中的亚细胞命运仍然是一个有争议的问题。通过对荷瘤小鼠进行抗体工程化磁荧光纳米晶体的体内和体外实验,我们结合荧光成像、磁共振弛豫和透射电子显微镜方法,提供了纳米颗粒通过主动靶向有效递送到肿瘤的证据。这些纳米晶体被证明能够增强磁共振成像中的肿瘤对比度。此外,我们能够在细胞内化时区分有机冠和金属核的命运。准确的免疫组织化学分析证实,杂交纳米颗粒的内吞作用是通过与 HER2 受体形成复合物介导的,导致细胞表面 HER2 蛋白表达的大量下调。这些结果直接揭示了靶向杂交纳米颗粒在体内癌细胞中的内化和降解途径,并为这种免疫治疗纳米剂在癌症的新辅助治疗中的潜在应用提供了依据。

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