Monoclonal antibody-conjugated superparamagnetic iron oxide nanoparticles for imaging of epidermal growth factor receptor-targeted cells and gliomas.

IF 2.2 4区 医学 Q3 BIOCHEMICAL RESEARCH METHODS Molecular Imaging Pub Date : 2015-01-01 DOI:10.2310/7290.2015.00002
Ketao Mu, Shun Zhang, Tao Ai, Jingjing Jiang, Yihao Yao, Lingyu Jiang, Qing Zhou, Hongbing Xiang, Yanhong Zhu, Xiangliang Yang, Wenzhen Zhu
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引用次数: 32

Abstract

The objective of this study was to successfully synthesize epidermal growth factor receptor monoclonal antibody-conjugated superparamagnetic iron oxide nanoparticles (EGFRmAb-SPIONs) and explore their biocompatibility and potential applications as a targeted magnetic resonance imaging (MRI) contrast agent for the EGFR-specific detection of brain glioma in vivo. After conjugation of EGFRmAb with SPIONs, the magnetic characteristics of EGFRmAb-SPIONs were investigated. Thereafter, the targeting abilities of EGFRmAb-SPIONs with MRI were qualitatively and quantitatively assessed in EGFR-positive C6 glioma cells in vitro and in a Wistar rat model bearing C6 glioma in vivo. Furthermore, the preliminary biocompatibility and toxicity of EGFRmAb-SPIONs were evaluated in normal rats through hematology assays and histopathologic analyses. Statistical analysis was performed using one-way analysis of variance and Student t-test, with a significance level of p < .05. From the results of EGFRmAb-SPION characterizations, the average particle size was 10.21 nm and the hydrodynamic diameter was 161.5 ± 2.12 nm. The saturation magnetization was 55 emu/g·Fe, and T2 relaxivity was 92.73 s-1mM-1 in distilled water. The preferential accumulation of the EGFRmAb-SPIONs within glioma and subsequent MRI contrast enhancement were demonstrated both in vitro in C6 cells and in vivo in rats bearing C6 glioma. After intravenous administration of EGFRmAb-SPIONs, T2-weighted MRI of the rat model with brain glioma exhibited an apparent hypointense region within glioma from 2 to 48 hours. The maximal image contrast was reached at 24 hours, where the signal intensity decreased and the R2 value increased by 30% compared to baseline. However, T2-weighted imaging of the rat model administered with SPIONs showed no visible signal changes within the tumor over the same time period. Moreover, no evident toxicities in vitro and in vivo with EGFRmAb-SPIONs were clearly identified based on the laboratory examinations. EGFRmAb-SPIONs could potentially be employed as a targeted contrast agent in the molecule-specific diagnosis of brain glioma in MRI.

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单克隆抗体偶联超顺磁性氧化铁纳米颗粒用于表皮生长因子受体靶向细胞和胶质瘤的成像。
本研究的目的是成功合成表皮生长因子受体单克隆抗体偶联超顺磁性氧化铁纳米颗粒(EGFRmAb-SPIONs),并探索其作为egfr特异性脑胶质瘤体内靶向磁共振成像(MRI)造影剂的生物相容性和潜在应用前景。将EGFRmAb与SPIONs偶联后,研究了EGFRmAb-SPIONs的磁性特性。随后,在体外egfr阳性的C6胶质瘤细胞和体内携带C6胶质瘤的Wistar大鼠模型中,通过MRI对EGFRmAb-SPIONs的靶向能力进行定性和定量评估。此外,通过血液学和组织病理学分析,对EGFRmAb-SPIONs在正常大鼠体内的初步生物相容性和毒性进行了评价。统计学分析采用单因素方差分析和学生t检验,显著性水平p < 0.05。EGFRmAb-SPION表征结果显示,平均粒径为10.21 nm,水动力粒径为161.5±2.12 nm。饱和磁化强度为55 emu/g·Fe, T2在蒸馏水中的弛豫度为92.73 s-1mM-1。体外C6细胞和体内C6胶质瘤大鼠均证实了EGFRmAb-SPIONs在胶质瘤内的优先积累和随后的MRI对比增强。静脉注射EGFRmAb-SPIONs后,脑胶质瘤大鼠模型的t2加权MRI在2 ~ 48小时内显示胶质瘤内明显的低信号区。在24小时达到最大图像对比度,此时信号强度下降,R2值较基线增加30%。然而,给予SPIONs的大鼠模型的t2加权成像显示,在同一时间段内肿瘤内没有可见的信号变化。此外,根据实验室检查,EGFRmAb-SPIONs在体外和体内没有明显的毒性。EGFRmAb-SPIONs有可能作为MRI中脑胶质瘤分子特异性诊断的靶向造影剂。
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来源期刊
Molecular Imaging
Molecular Imaging Biochemistry, Genetics and Molecular Biology-Biotechnology
自引率
3.60%
发文量
21
期刊介绍: Molecular Imaging is a peer-reviewed, open access journal highlighting the breadth of molecular imaging research from basic science to preclinical studies to human applications. This serves both the scientific and clinical communities by disseminating novel results and concepts relevant to the biological study of normal and disease processes in both basic and translational studies ranging from mice to humans.
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