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A method for quantitative cell tracking using SPECT for the evaluation of myocardial stem cell therapy.

机译:一种使用SPECT评估心肌干细胞疗法的定量细胞追踪方法。

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PURPOSE: A promising SPECT-based method for evaluating stem cells therapy uses (111)In-labelled cells, transfected with a reporter gene. Cells are first transplanted to the infarct, and subsequently interrogated for transgenic expression using a systemic injection of an (131)I-labelled reporter probe. The method is impeded by the physical effects of scatter, (131)I/(111)In cross-talk, and attenuation. We hypothesize that correcting for physical effects improves detection of transgenic expression in transplanted cells when (111)In localization is available. METHODS: Canine bone marrow mesenchymal cells (BMMCs), radiolabelled and transfected, were injected into infarcted myocardium. Next, a reporter probe was injected systemically, and 22 SPECT scans were acquired over 20 h. Finally, (99m)Tc-sestamibi was injected and imaged. The animal was killed, the heart sectioned, and counted for (131)I and (111)In in a well-counter ('gold standard'). Canine SPECTs were reconstructed in two ways: with corrections for physical effects and without corrections. The first (111)In reconstruction and the (99m)Tc reconstruction were used to define volumes-of-interest over the transplanted BMMC (VBMMC) and normal myocardium (VNM), respectively. RESULTS: (131)I reconstructions without corrections for physical effects had negligible differential uptake. With corrections, VBMMC was consistently higher than VNM, demonstrating transgene expression. (131)I had the following VBMMC:VNM activity ratio: without correction for physical effects=0.869; with corrections=1.23; and well-counter=1.21. VNM showed the following (131)I:(111)In activity ratio: without corrections=3.07; with corrections=1.38; and well-counter=1.58. CONCLUSIONS: In dual-isotope SPECT, corrections for physical effects were required to detect transgene expression in cells transplanted into an infarction when localization information was available.
机译:目的:一种有前途的基于SPECT的干细胞疗法评估方法,该方法使用(111)In标记细胞,并用报道基因转染。首先将细胞移植到梗塞处,然后使用系统注射(131)I标记的报告探针探询转基因表达。该方法受到散射,(131)I /(111)串扰和衰减的物理效应的阻碍。我们假设对物理效应的校正可改善在(111)In本地化时可移植细胞中转基因表达的检测。方法:将经放射性标记和转染的犬骨髓间充质细胞(BMMC)注射到梗死的心肌中。接下来,系统性地注射了一个报告探针,并在20小时内获得了22次SPECT扫描。最后,注入(99m)Tc-司他米比并成像。杀死动物,将心脏切开,并在一个小计数器(“金标准”)中计数(131)I和(111)In。犬SPECTs的重建方法有两种:对物理效应进行校正和不进行校正。首次(111)In重建和(99m)Tc重建分别用于定义移植的BMMC(VBMMC)和正常心肌(VNM)的目标体积。结果:(131)I重建没有物理效应的校正具有微不足道的差异吸收。经过更正,VBMMC始终高于VNM,表明转基因表达。 (131)我具有以下VBMMC:VNM活性比:未经校正的物理效应= 0.869;更正= 1.23;算数= 1.21 VNM显示出以下(131)I:(111)活性比:未经校正= 3.07;更正= 1.38;并且counter-counter = 1.58。结论:在双同位素SPECT中,当可获得定位信息时,需要对物理效应进行校正以检测移植到梗塞细胞中的转基因表达。

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