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A mutant herpes simplex virus type 1 thymidine kinase reporter gene shows improved sensitivity for imaging reporter gene expression with positron emission tomography

机译:突变的单纯疱疹病毒1型胸苷激酶报告基因突变体显示正电子发射断层显像成像基因表达的敏感性提高

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摘要

We are developing assays for noninvasive, quantitative imaging of reporter genes with positron emission tomography (PET), for application both in animal models and in human gene therapy. We report here a method to improve the detection of lower levels of PET reporter gene expression by utilizing a mutant herpes simplex virus type 1 thymidine kinase (HSV1-sr39tk) as a PET reporter gene. The HSV1-sr39tk mutant was identified from a library of site-directed mutants. Accumulation (net uptake) of the radioactively labeled substrates [8-3H]penciclovir ([8-3H]PCV), and 8-[18F]fluoropenciclovir (FPCV) in C6 rat glioma cells expressing HSV1-sr39tk is increased by a factor of ≈2.0 when compared with C6 cells expressing wild-type HSV1-tk. The increased imaging sensitivity of HSV1-sr39tk when FPCV is used is also demonstrated in vivo both with tumor cells stably transfected with either HSV1-tk or HSV1-sr39tk, and after hepatic delivery of HSV1-tk or HSV1-sr39tk by using adenoviral vectors. The use of HSV1-sr39tk as a PET reporter gene and FPCV as a PET reporter probe results in significantly enhanced sensitivity for imaging reporter gene expression in vivo.
机译:我们正在开发利用正电子发射断层扫描(PET)对报告基因进行无创定量成像的检测方法,以用于动物模型和人类基因治疗。我们在这里报告了一种方法,可通过利用突变型单纯疱疹病毒1型胸苷激酶(HSV1-sr39tk)作为PET报告基因来提高检测PET报告基因较低水平的方法。 HSV1-sr39tk突变体是从定点突变体文库中鉴定的。放射性标记底物[8- 3 H] penciclovir([8- 3 H] PCV)和8-[ 18 <与表达野生型HSV1-tk的C6细胞相比,表达HSV1-sr39tk的C6大鼠神经胶质瘤细胞中的F]氟penciclovir(FPCV)增加约2.0倍。当使用FPCV稳定转染的肿瘤细胞在体内以及使用腺病毒载体肝递送HSV1-tk或HSV1-sr39tk后,在体内使用FPCV时,HSV1-sr39tk的成像灵敏度也得到了提高。 HSV1-sr39tk作为PET报告基因,FPCV作为PET报告探针的使用,可以显着增强体内成像报告基因表达的敏感性。

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