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Synthesis and Evaluation of Methylated ArylazepineCompounds for PET Imaging of 5-HT2c Receptors

机译:甲基化阿氮平的合成与评价用于5-HT2c受体PET成像的化合物

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摘要

The serotonin 5-HT2c receptor is implicated in a number of diseases including obesity, depression, anxiety, and schizophrenia. In order to ascribe the role of 5-HT2c in these diseases, a method for measuring 5-HT2c density and function in vivo, such as with positron emission tomography (PET), must be developed. Many high-affinity and relatively selective ligands exist for 5-HT2c but cannot be accessed with current radiosynthetic methods for use as PET radiotracers. We propose that N-methylation of an arylazepine moiety, a frequent structural feature in 5-HT2c ligands, may be a suitable method for producing new radiotracers for 5-HT2c. The impact of N-methylation has not been previously reported. For the agonists that we selected herein, N-methylation was found to increase affinity up to 8-fold without impairing selectivity. Compound 5, an N-methylated azetidine-derived arylazepine, was found to be brain penetrant and reached a brain/blood ratio of 2.05:1. However, our initial test compound was rapidly metabolized within 20 min of administration and exhibited high nonspecific binding. N-Methylation, with 16 ± 3% isolated radiochemical yield (decay corrected), is robust and may facilitate screening other 5-HT2c ligands as radiotracers for PET.
机译:5-羟色胺5-HT2c受体与多种疾病有关,包括肥胖,抑郁,焦虑和精神分裂症。为了归因于5-HT2c在这些疾病中的作用,必须开发一种用于测量体内5-HT2c密度和功能的方法,例如正电子发射断层扫描(PET)。对于5-HT 2c存在许多高亲和力和相对选择性的配体,但是不能用当前的放射性合成方法用作PET放射性示踪剂来获得。我们建议,氮杂氮杂庚烷部分的N-甲基化是5-HT2c配体的常见结构特征,可能是生产5-HT2c新放射性示踪剂的合适方法。以前尚未报道过N-甲基化的影响。对于我们在本文中选择的激动剂,发现N-甲基化将亲和力增加至高达8倍,而不会损害选择性。发现化合物5,一种N-甲基化氮杂环丁烷衍生的阿来氮平,具有脑渗透性,脑/血比例为2.05:1。然而,我们最初的测试化合物在给药后20分钟内迅速代谢,并表现出很高的非特异性结合。 N-甲基化具有16±3%的分离放射化学收率(已校正衰变),具有很强的稳定性,可有助于筛选其他5-HT2c配体作为PET的放射性示踪剂。

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