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Radiosynthesis and evaluation of [11C]EMPA as a potential PET tracer for orexin 2 receptors

机译:放射性合成和评估[11C] EMPA作为orexin 2受体的潜在PET示踪剂

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EMPA is a selective antagonist of orexin 2 (OX2) receptors. Previous literature with [3H]-EMPA suggest that it may be used as an imaging agent for OX2 receptors; however, brain penetration is known to be modest. To evaluate the potential of EMPA as a PET radiotracer in non-human primate (as a step to imaging in man), we radiolabeled EMPA with carbon-11. Radiosynthesis of [11C]N-ethyl-2-(N-(6-methoxypyridin-3- yl)-2-methylphenylsulfonamido)-N-(pyridin-3-ylmethyl)acetamide ([ 11C]EMPA), and evaluation as a potential PET tracer for OX 2 receptors is described. Synthesis of an appropriate non-radioactive O-desmethyl precursor was achieved from EMPA with sodium iodide and chlorotrimethylsilane. Selective O-methylation using [11C]CH 3I in the presence of cesium carbonate in DMSO at room temp afforded [11C]EMPA in 1.5-2.5% yield (non-decay corrected relative to trapped [11C]CH3I at EOS) with ≥95% chemical and radiochemical purities. The total synthesis time was 34-36 min from EOB. Studies in rodent suggested that uptake in tissue was dominated by nonspecific binding. However, [11C]EMPA also showed poor uptake in both rats and baboon as measured with PET imaging.
机译:EMPA是orexin 2(OX2)受体的选择性拮抗剂。以前[3H] -EMPA的文献表明,它可以用作OX2受体的显像剂。然而,众所周知,大脑的渗透是适度的。为了评估EMPA在非人类灵长类动物中作为PET放射性示踪剂的潜力(作为在人体中成像的步骤),我们用碳11放射性标记了EMPA。 [11C] N-乙基-2-(N-(6-甲氧基吡啶-3-基)-2-甲基苯基磺酰胺基)-N-(吡啶-3-基甲基)乙酰胺([11C] EMPA)的放射合成,并作为评价描述了潜在的OX 2受体PET示踪剂。由EMPA与碘化钠和氯代三甲基硅烷一起合成合适的非放射性O-去甲基前体。在碳酸铯存在下于室温下在碳酸铯中使用[11C] CH 3I进行选择性O-甲基化,以1.5-2.5%的产率提供[11C] EMPA(相对于EOS捕集的[11C] CH3I进行非衰减校正),≥95 %化学和放射化学纯度。距EOB的总合成时间为34-36分钟。在啮齿动物中的研究表明,组织中的吸收以非特异性结合为主导。然而,[11C] EMPA也显示出大鼠和狒狒的摄取差,这是通过PET成像测量的。

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