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首页> 外文期刊>Journal of Fluorine Chemistry >Preparation of the novel fluorine-18-labeled VIP analog for PET imaging studies using two different synthesis methods
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Preparation of the novel fluorine-18-labeled VIP analog for PET imaging studies using two different synthesis methods

机译:使用两种不同的合成方法制备用于PET成像研究的新型氟18标记的VIP类似物

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Vasoactive intestinal peptide (VIP) receptors are expressed on various tumor cells in much higher density than somatostatin receptors,which provides the basis for radiolabeling VIP as tumor diagnostic agent.However,fast proteolytic degradation of VIP in vivo limits its clinical application.With the aim to develop and evaluate new ligands for depicting the VIP receptors with positron emission tomography (PET),the structure modified [R~(8,15,21),L17]-VIP analog was radiolabeled with 18F using two different methods.With the first method,N-4-[18F]fluor- obenzoyl-[R~(8,15,21),L17]-VTP ([18F]FB-[R~(8,15,21),L17]-VIP 7) was produced in a decay-corrected radiochemical yield (RCY) of 33.6 +- 3%,a specific radioactivity of 255 GBq/mu mol (n = 5) within 100 min in four steps.Similarly,N-4-[18F](fluoromethyl)-benzoyl-[R~(8,15,21),L17]-VIP ([18F]FMB-[R~(8,15,21),L17]-VIP 8) was synthesized in a RCY of 34.85 +- 5%,a specific radioactivity of 180 GBq/mu mol (n = 5) within 60 min in only one step.The two products 7 and 8 were both shown good stability in HSA.Moreover,the low bone uptakes of 7 and 8 in vivo of mice showed good defluorination stability.
机译:血管活性肠肽(VIP)受体在各种肿瘤细胞中的表达密度高于生长抑素受体,这为放射性标记VIP作为肿瘤诊断剂提供了基础。但是,VIP在体内的快速蛋白水解作用限制了其临床应用。为了开发和评估新的配体,以正电子发射断层扫描(PET)描绘VIP受体,采用两种不同的方法用18F对结构修饰的[R〜(8,15,21),L17] -VIP类似物进行放射性标记。方法,N-4- [18F]氟邻苯甲酰基-[R〜(8,15,21),L17] -VTP([18F] FB- [R〜(8,15,21),L17] -VIP 7 )经4个步骤在100分钟内以33.6±3%的衰减校正放射化学产率(RCY)产生,比放射性为255 GBq / mu mol(n = 5)。N-4-[18F]合成了(氟甲基)-苯甲酰基-[R〜(8,15,21),L17] -VIP([18F] FMB- [R〜(8,15,21),L17] -VIP 8) 34.85±5%,只需一步即可在60分钟内达到180 GBq / mu mol(n = 5)的比放射性。两种产品7和8均显示出良好的HSA稳定性。此外,小鼠体内7和8的低骨吸收显示出良好的脱氟稳定性。

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