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铁蛋白作为小鼠癌症模型中细胞追踪磁共振成像造影剂的有效性

The Effectiveness of Ferritin as a Contrast Agent for Cell Tracking MRI in Mouse Cancer Models.

作者信息

Lee Chan Wha, Choi Sun Il, Lee Sang Jin, Oh Young Taek, Park Gunwoo, Park Na Yeon, Yoon Kyoung Ah, Kim Sunshin, Kim Daehong, Kim Yun Hee, Suh Jin Suck

机构信息

Department of Medicine, The Graduate School of Yonsei University, Seoul, Korea.

Research Institute & Hospital, National Cancer Center, Goyang, Korea.

出版信息

Yonsei Med J. 2017 Jan;58(1):51-58. doi: 10.3349/ymj.2017.58.1.51.

Abstract

PURPOSE

We aimed to investigate the effectiveness of ferritin as a contrast agent and a potential reporter gene for tracking tumor cells or macrophages in mouse cancer models.

MATERIALS AND METHODS

Adenoviral human ferritin heavy chain (Ad-hFTH) was administrated to orthotopic glioma models and subcutaneous colon cancer mouse models using U87MG and HCT116 cells, respectively. Brain MR images were acquired before and daily for up to 6 days after the intracranial injection of Ad-hFTH. In the HCT116 tumor model, MR examinations were performed before and at 6, 24, and 48 h after intratumoral injection of Ad-hFTH, as well as before and every two days after intravenous injection of ferritin-labeled macrophages. The contrast effect of ferritin in vitro was measured by MR imaging of cell pellets. MRI examinations using a 7T MR scanner comprised a T1-weighted (T1w) spin-echo sequence, T2-weighted (T2w) relaxation enhancement sequence, and T2*-weighted (T2*w) fast low angle shot sequence.

RESULTS

Cell pellet imaging of Ad-hFTH in vitro showed a strong negatively enhanced contrast in T2w and T2w images, presenting with darker signal intensity in high concentrations of Fe. T2w images of glioma and subcutaneous HCT116 tumor models showed a dark signal intensity around or within the Ad-hFTH tumor, which was distinct with time and apparent in T2w images. After injection of ferritin-labeled macrophages, negative contrast enhancement was identified within the tumor.

CONCLUSION

Ferritin could be a good candidate as an endogenous MR contrast agent and a potential reporter gene that is capable of maintaining cell labeling stability and cellular safety.

摘要

目的

我们旨在研究铁蛋白作为一种造影剂和潜在报告基因,在小鼠癌症模型中追踪肿瘤细胞或巨噬细胞的有效性。

材料与方法

分别使用U87MG和HCT116细胞,将腺病毒人铁蛋白重链(Ad-hFTH)施用于原位胶质瘤模型和皮下结肠癌小鼠模型。在颅内注射Ad-hFTH之前及之后每天采集脑磁共振图像,持续6天。在HCT116肿瘤模型中,在瘤内注射Ad-hFTH之前以及注射后6、24和48小时进行磁共振检查,在静脉注射铁蛋白标记的巨噬细胞之前及之后每两天进行磁共振检查。通过对细胞团块进行磁共振成像来测量铁蛋白在体外的造影效果。使用7T磁共振扫描仪进行的磁共振检查包括T1加权(T1w)自旋回波序列、T2加权(T2w)弛豫增强序列和T2加权(T2w)快速低角度激发序列。

结果

体外Ad-hFTH的细胞团块成像在T2w和T2w图像中显示出强烈的负性增强造影,在高浓度铁时呈现出较暗的信号强度。胶质瘤和皮下HCT116肿瘤模型的T2w图像显示Ad-hFTH肿瘤周围或内部有暗信号强度,其随时间变化明显,在T2w图像中更明显。注射铁蛋白标记的巨噬细胞后,肿瘤内出现负性造影增强。

结论

铁蛋白可能是一种良好的内源性磁共振造影剂候选物和潜在报告基因,能够维持细胞标记稳定性和细胞安全性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cd1a/5122652/81197e847155/ymj-58-51-g001.jpg

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