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Use of Cyclic Backbone NGR-Based SPECT to Increase Efficacy of Postmyocardial Infarction Angiogenesis Imaging

机译:基于循环骨干NGR的SPECT的使用以增加心肌梗塞后血管新生显像的功效

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摘要

As CD13 is selectively expressed in angiogenesis, it can serve as a target for molecular imaging tracers to noninvasively visualize angiogenic processes in vivo. The CD13-targeting moiety NGR was synthesized and cyclized by native chemical ligation (NCL) instead of disulfide bridging, leading to a cyclic peptide backbone: cyclo(Cys-Asn-Gly-Arg-Gly) (coNGR). Beside this new monomeric coNGR, a tetrameric NGR peptide co(NGR)4 was designed and synthesized. After radiolabeling, their in vitro and in vivo characteristics were determined. Both coNGR-based imaging agents displayed considerably higher standardized uptake values (SUVs) at infarcted areas compared to the previously reported disulfide-cyclized cNGR imaging agent. Uptake patterns of 111In-coNGR and 111In-co(NGR)4 coincided with CD13 immunohistochemistry on excised hearts. Blood stability tests indicated better stability for both novel imaging agents after 50 min blood incubation compared to the disulfide-cyclized cNGR imaging agent. In mice, both coNGR peptides cleared rapidly from the blood mainly via the kidneys. In addition, co(NGR)4 showed a significantly higher specific uptake in infarcted myocardium compared to coNGR and thus is a promising sensitive imaging agent for detection of angiogenesis in infarcted myocardium.
机译:由于CD13在血管生成中选择性表达,因此它可以用作分子成像示踪剂的靶标,以无创地观察体内的血管生成过程。合成CD13靶向部分NGR,并通过天然化学连接(NCL)而不是二硫键桥接进行环化,形成环肽骨架:环(Cys-Asn-Gly-Arg-Gly)(coNGR)。除了这种新的单体coNGR,还设计并合成了四聚NGR肽co(NGR)4。放射性标记后,确定其体外和体内特征。与先前报道的二硫化物环化的cNGR成像剂相比,两种基于coNGR的成像剂在梗死区域均显示出更高的标准化摄取值(SUV)。在切除的心脏上, 111 In-coNGR和 111 In-co(NGR)4的摄取模式与CD13免疫组化相吻合。血液稳定性测试表明,与二硫化物环化的cNGR显像剂相比,两种新型显像剂在经过50分钟的血液孵育后具有更好的稳定性。在小鼠中,两种coNGR肽都主要通过肾脏从血液中迅速清除。另外,与coNGR相比,co(NGR)4在梗塞心肌中显示出明显更高的特异性摄取,因此是用于检测梗塞心肌中血管生成的有希望的敏感成像剂。

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