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Evaluation of the Radiolabeled Boronic Acid-Based FAP Inhibitor MIP-1232 for Atherosclerotic Plaque Imaging

机译:放射性标记的基于硼酸的FAP抑制剂MIP-1232对动脉粥样斑块成像的评估

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Research towards the non-invasive imaging of atherosclerotic plaques is of high clinical priority as early recognition of vulnerable plaques may reduce the incidence of cardiovascular events. The fibroblast activation protein alpha (FAP) was recently proposed as inflammation-induced protease involved in the process of plaque vulnerability. In this study, FAP mRNA and protein levels were investigated by quantitative polymerase chain reaction and immunohistochemistry, respectively, in human endarterectomized carotid plaques. A published boronic-acid based FAP inhibitor, MIP-1232, was synthetized and radiolabeled with iodine-125. The potential of this radiotracer to image plaques was evaluated by in vitro autoradiography with human carotid plaques. Specificity was assessed with a xenograft with high and one with low FAP level, grown in mice. Target expression analyses revealed a moderately higher protein level in atherosclerotic plaques than normal arteries correlating with plaque vulnerability. No difference in expression was determined on mRNA level. The radiotracer was successfully produced and accumulated strongly in the FAP-positive SK-Mel-187 melanoma xenograft in vitro while accumulation was negligible in an NCI-H69 xenograft with low FAP levels. Binding of the tracer to endarterectomized tissue was similar in plaques and normal arteries, hampering its use for atherosclerosis imaging.
机译:由于动脉粥样硬化斑块的早期识别可以减少心血管事件的发生,因此对动脉粥样硬化斑块的非侵入性成像的研究具有很高的临床优先性。最近提出了成纤维细胞活化蛋白α(FAP)作为炎症诱导的蛋白酶,参与斑块易损性过程。在这项研究中,分别通过定量多聚酶链反应和免疫组织化学技术对人动脉内切掉的颈动脉斑块中的FAP mRNA和蛋白水平进行了研究。合成了已发表的基于硼酸的FAP抑制剂MIP-1232,并用碘125放射性标记。通过用人体颈动脉斑块进行体外放射自显影术评估了这种放射性示踪剂对图像斑块的潜力。用在小鼠中生长的高和低FAP水平的异种移植物评估特异性。靶标表达分析显示,与斑块易损性相关的正常动脉中,动脉粥样硬化斑块中的蛋白质水平中等偏高。在mRNA水平上未确定表达差异。放射性示踪剂在FAP阳性SK-Mel-187黑色素瘤异种移植物中成功产生并强烈积累,而在低FAP水平的NCI-H69异种移植物中其积累微不足道。示踪剂在动脉粥样硬化斑块和正常动脉中的结合相似,这阻碍了其在动脉粥样硬化成像中的使用。

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