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使用[C]甲氧苄啶的定量PET报告基因成像

Quantitative PET Reporter Gene Imaging with [C]Trimethoprim.

作者信息

Sellmyer Mark A, Lee Iljung, Hou Catherine, Lieberman Brian P, Zeng Chenbo, Mankoff David A, Mach Robert H

机构信息

Department of Radiology, University of Pennsylvania, Philadelphia, PA 19104, USA.

Department of Radiology, University of Pennsylvania, Philadelphia, PA 19104, USA.

出版信息

Mol Ther. 2017 Jan 4;25(1):120-126. doi: 10.1016/j.ymthe.2016.10.018.

Abstract

There is a need for improved methods to image genetically engineered cells, including immune cells used for cell-based therapy. Given the genetic manipulation inherent to gene therapy, the use of a reporter protein is a logical solution and positron emission tomography (PET) can provide the desired sensitivity and spatial localization. We developed a broadly applicable PET imaging strategy based on the small bacterial protein E. coli dihydrofolate reductase (Ec dhfr) and its highly specific small molecule inhibitor, trimethoprim (TMP). The difference in TMP affinity for bacterial compared to mammalian DHFR suggests that a TMP radioligand would have a low background in unmodified mammalian tissues and high retention in Ec dhfr engineered cells, providing high contrast imaging. Here, we describe the in vitro properties of [C]TMP and show over 10-fold increased signal in transgenic Ec dhfr cells compared to control. In a mouse xenograft model, [C]TMP rapidly accumulated in Ec dhfr carrying cells within minutes of intravenous administration. Moreover, [C]TMP can identify less than a million xenografted cells in a small volume in tissues other than the abdominal compartment. This limit of detection is a clinically relevant number and bodes well for clinical translation especially given that [C]TMP is an isotopologue of clinically approved antibiotic.

摘要

需要改进对基因工程细胞进行成像的方法,包括用于细胞疗法的免疫细胞。鉴于基因治疗中固有的基因操作,使用报告蛋白是一种合理的解决方案,而正电子发射断层扫描(PET)可以提供所需的灵敏度和空间定位。我们基于小细菌蛋白大肠杆菌二氢叶酸还原酶(Ec dhfr)及其高度特异性的小分子抑制剂甲氧苄啶(TMP)开发了一种广泛适用的PET成像策略。与哺乳动物二氢叶酸还原酶相比,TMP对细菌的亲和力差异表明,TMP放射性配体在未修饰的哺乳动物组织中背景较低,而在Ec dhfr工程细胞中保留率较高,从而提供高对比度成像。在此,我们描述了[C]TMP的体外特性,并表明与对照相比,转基因Ec dhfr细胞中的信号增加了10倍以上。在小鼠异种移植模型中,静脉注射后几分钟内,[C]TMP就在携带Ec dhfr的细胞中迅速积累。此外,[C]TMP可以在腹腔以外的组织中少量识别不到一百万个异种移植细胞。这一检测限是一个与临床相关的数字,对临床转化来说是个好兆头,特别是考虑到[C]TMP是临床批准抗生素的同位素类似物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/75ca/5363299/c2f3d74e5d52/fx1.jpg

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