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钆弗塞胺在干细胞中的摄取作为一种新的磁共振成像追踪方法:一项体外和体内研究。

Gadofluorine m uptake in stem cells as a new magnetic resonance imaging tracking method: an in vitro and in vivo study.

作者信息

Giesel Frederik Lars, Stroick Mark, Griebe Martin, Tröster Helmut, von der Lieth Claus W, Requardt Martin, Rius Maria, Essig Marco, Kauczor Hans-Ulrich, Hennerici M G, Fatar Marc

机构信息

German Cancer Research Center, Department of Radiology, Heidelberg, Germany.

出版信息

Invest Radiol. 2006 Dec;41(12):868-73. doi: 10.1097/01.rli.0000246147.44835.4c.

Abstract

OBJECTIVES

Cell tracking using ultrasmall iron particles is well established in magnetic resonance imaging (MRI). However, in experimental models, intrinsic iron signals derived from erythrocytes mask the labeled cells. Therefore, we evaluated Gadofluorine M with other gadolinium chelates for a T1-weighted positive enhancement for cell tracking in vitro. In addition, Gadofluorine M was tested in vivo.

MATERIAL AND METHODS

Gadofluorine M and other gadolinium chelates were used to label stem cells with and without uptake-mediating agents in vitro and in vivo using a 1.5 T MRI. In addition, histology and molecular modeling was investigated.

RESULTS

Gadofluorine M revealed comparable properties to an uptake mediating agent in molecular modeling. Without an uptake-mediating agent Gadofluorine M-labeled cells were detected as a T1-weighted positive contrast in vitro and in vivo. Histology confirmed a 100% success rate for intracellular labeling.

CONCLUSION

This study describes a novel contrast agent with the capability of intracellular accumulation without an uptake mediator providing a T1-positive MRI signal at 1.5 T and may be suitable for cell tracking in animal models with intraparenchymal hemorrhages such as stroke or malignant tumors.

摘要

目的

在磁共振成像(MRI)中,使用超小铁颗粒进行细胞追踪已得到充分证实。然而,在实验模型中,源自红细胞的内源性铁信号会掩盖被标记的细胞。因此,我们评估了钆弗罗胺M与其他钆螯合物在体外细胞追踪中用于T1加权阳性增强的情况。此外,还对钆弗罗胺M进行了体内测试。

材料与方法

使用1.5 T MRI,在体外和体内用钆弗罗胺M和其他钆螯合物标记有或没有摄取介导剂的干细胞。此外,还进行了组织学和分子建模研究。

结果

在分子建模中,钆弗罗胺M显示出与摄取介导剂相当的特性。在没有摄取介导剂的情况下,钆弗罗胺M标记的细胞在体外和体内均被检测为T1加权阳性对比。组织学证实细胞内标记成功率为100%。

结论

本研究描述了一种新型造影剂,它能够在没有摄取介导剂的情况下实现细胞内积累,在1.5 T时提供T1阳性MRI信号,可能适用于在诸如中风或恶性肿瘤等实质内出血的动物模型中进行细胞追踪。

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