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A triple suicide gene strategy that improves therapeutic effects and incorporates multi-modality molecular imaging for monitoring gene-functions

机译:一种三重自杀基因策略可提高治疗效果并结合了多模态分子成像技术来监测基因功能

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摘要

Gene-directed enzyme prodrug therapy (GDEPT), or suicide gene therapy, has shown promise in clinical trials. In this preclinical study using stable cell lines and xenograft tumor models, we show that a triple-suicide-gene GDEPT approach produce enhanced therapeutic efficacy over previous methods. Importantly all the three genes (thymidine kinase, cytosine deaminase, and uracil phosphoribosyltransferase) function simultaneously as effectors for GDEPT and markers for multimodality molecular imaging (MMI), using positron-emission-tomography (PET), magnetic resonance-spectroscopy (MRS), and optical (fluorescent and bioluminescent) techniques. It was demonstrated that MMI can evaluate the distribution and function/activity of the triple-suicide-gene. The concomitant expression of these genes significantly enhances prodrug cytotoxicity and radiosensitivity in vitro and in vivo.
机译:基因导向的酶前药疗法(GDEPT)或自杀基因疗法在临床试验中显示出了希望。在这项使用稳定细胞系和异种移植肿瘤模型的临床前研究中,我们显示了三自杀基因GDEPT方法比以前的方法产生更高的治疗效果。重要的是,所有三个基因(胸苷激酶,胞嘧啶脱氨酶和尿嘧啶磷酸核糖基转移酶)同时充当GDEPT的效应子和多模态分子成像(MMI)的标记,使用正电子发射断层扫描(PET),磁共振波谱(MRS),以及光学(荧光和生物发光)技术。事实证明,MMI可以评估三自杀基因的分布和功能/活性。这些基因的伴随表达在体外和体内显着增强了前药的细胞毒性和放射敏感性。

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