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首页> 外文期刊>Scientific reports. >One-step radiosynthesis of the MCTs imaging agent [18F]FACH by aliphatic 18F-labelling of a methylsulfonate precursor containing an unprotected carboxylic acid group
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One-step radiosynthesis of the MCTs imaging agent [18F]FACH by aliphatic 18F-labelling of a methylsulfonate precursor containing an unprotected carboxylic acid group

机译:MCTS成像剂[18F] Fach通过脂族18F标记的甲基磺酸盐前体的一步辐射合成[18F] Fach含有未受保护的羧酸基团的甲基磺酸盐前体

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Monocarboxylate transporters 1 and 4 (MCT1 and MCT4) are involved in tumour development and progression. Their level of expression is particularly upregulated in glycolytic cancer cells and accordingly MCTs are considered as promising drug targets for treatment of a variety of human cancers. The non-invasive imaging of these transporters in cancer patients via positron emission tomography (PET) is regarded to be valuable for the monitoring of therapeutic effects of MCT inhibitors. Recently, we developed the first sup18/supF-radiolabelled MCT1/MCT4 inhibitor [sup18/supF]FACH and reported on a two-step one-pot radiosynthesis procedure. We herein describe now a unique one-step radiosynthesis of this radiotracer which is based on the approach of using a methylsulfonate (mesylate) precursor bearing an unprotected carboxylic acid function. With the new procedure unexpected high radiochemical yields of 43?±?8% at the end of the radiosynthesis could be obtained in a strongly reduced total synthesis time. Moreover, the radiosynthesis was successfully transferred to a TRACERlab FX2 N synthesis module ready for future preclinical applications of [sup18/supF]FACH.
机译:单羧酸转运蛋白1和4(MCT1和MCT4)参与肿瘤发育和进展。它们的表达水平特别是在糖酵解癌细胞中尤其上调,因此MCT被认为是用于治疗各种人类癌症的有希望的药物靶标。通过正电子发射断层扫描(PET)在癌症患者中对这些转运蛋白的非侵入性成像被认为是监测MCT抑制剂治疗效果的价值。最近,我们开发了第一个 18 f-radiolabelled mct1 / mct4抑制剂[ 18℃] fach,并在两步一锅上辐射合成程序报告。我们本文现在描述了这种放射体机构的独特的一步辐射合成,这是基于使用载体含有未受保护的羧酸功能的甲基磺酸盐(甲磺酸盐)前体的方法。随着新的程序意外的高放射化产量为43?±8%,可以在纤维合成的结束时获得强烈降低的总合成时间。此外,可辐射合成剂被成功转移到Tracerlab FX2 N合成模块,可用于[ 18 f] fach的未来临床前应用。

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