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转铁蛋白受体:一种潜在的人类癌症分子成像标志物。

The transferrin receptor: a potential molecular imaging marker for human cancer.

作者信息

Högemann-Savellano Dagmar, Bos Erik, Blondet Cyrille, Sato Fuminori, Abe Tatsuya, Josephson Lee, Weissleder Ralph, Gaudet Justin, Sgroi Dennis, Peters Peter J, Basilion James P

机构信息

Center for Molecular Imaging Research, Massachusetts General Hospital, Charlestown, MA 02129, USA.

出版信息

Neoplasia. 2003 Nov-Dec;5(6):495-506. doi: 10.1016/s1476-5586(03)80034-9.

Abstract

Noninvasive imaging of differences between the molecular properties of cancer and normal tissue has the potential to enhance the detection of tumors. Because overexpression of endogenous transferrin receptor (TfR) has been qualitatively described for various cancers and is presumably due to malignant transformation of cells, TfR may represent a suitable target for application of molecular imaging technologies to increase detection of smaller tumors. In the work reported here, investigation into the biology of this receptor using electron microscopy has demonstrated that iron oxide particles targeted to TfR are internalized and accumulate in lysosomal vesicles within cells. Biochemical analysis of the interaction of imaging probes with cells overexpressing the TfR demonstrated that the extent of accumulation, and therefore probe efficacy, is dependent on the nature of the chemical cross-link between transferrin and the iron oxide particle. These data were utilized to design and synthesize an improved imaging probe. Experiments demonstrate that the novel magnetic resonance imaging (MRI) probe is sensitive enough to detect small differences in endogenous TfR expression in human cancer cell lines. Quantitative measurement of TfR overexpression in a panel of 27 human breast cancer patients demonstrated that 74% of patient cancer tissues overexpressed the TfR and that the sensitivity of the new imaging agent was suitable to detect TfR overexpression in greater than 40% of these cases. Based on a biochemical and cell biological approach, these studies have resulted in the synthesis and development of an improved MRI probe with the best in vitro and in vivo imaging properties reported to date.

摘要

对癌症与正常组织分子特性差异进行无创成像,有潜力提高肿瘤的检测率。由于多种癌症中均有内源性转铁蛋白受体(TfR)过表达的定性描述,且推测这是细胞恶性转化所致,TfR可能是应用分子成像技术增加小肿瘤检测的合适靶点。在本文报道的研究中,利用电子显微镜对该受体生物学特性的研究表明,靶向TfR的氧化铁颗粒会被内化并积聚在细胞内的溶酶体囊泡中。对成像探针与过表达TfR的细胞相互作用的生化分析表明,积聚程度以及探针效能取决于转铁蛋白与氧化铁颗粒之间化学交联的性质。这些数据被用于设计和合成一种改进的成像探针。实验表明,这种新型磁共振成像(MRI)探针足够灵敏,能够检测人类癌细胞系中内源性TfR表达的微小差异。对27名人类乳腺癌患者的一组样本进行TfR过表达的定量测量表明,74%的患者癌组织TfR过表达,且新型成像剂的灵敏度足以在超过40%的此类病例中检测到TfR过表达。基于生化和细胞生物学方法,这些研究已合成并开发出一种改进的MRI探针,其具有迄今报道的最佳体外和体内成像特性。

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