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Development of N-Methyl-(2-arylquinolin-4-yl)oxypropanamidesas Leads to PET Radioligands for Translocator Protein (18 kDa)

机译:N-甲基-(2-芳基喹啉-4-基)氧基丙酰胺的研制导致易位蛋白(18 kDa)的PET放射性配体

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摘要

Translocator protein (18 kDa), known as TSPO, is a recognized biomarker of neuroinflammation. Radioligands with PET accurately quantify TSPO in neuroinflammatory conditions. However, the existence of three human TSPO genotypes that show differential affinity to almost all useful TSPO PET radioligands hampers such studies. There is an unmet need for genotype-insensitive, high-affinity, and moderately lipophilic TSPO ligands that may serve as leads for PET radioligand development. To address this need, we varied the known high-affinity TSPO ligand (l)-N,N-diethyl-2-methyl-3-(2-phenylquinolin-4-yl)propanamide in its aryl scaffold, side chain tether, and pendant substituted amido group while retaining an N-methyl group as a site for labeling with carbon-11. From this effort, oxygen-tethered N-methyl-aryloxypropanamides emerged as new high-affinity TSPO ligands with attenuated lipophilicity, including one example with attractive properties for PET radioligand development, namely N-methyl-N-phenyl-2-{[2-(pyridin-2-yl)quinolin-4-yl]oxy}propanamide (>22a; rat Ki = 0.10 nM; human TSPO genotypes Ki = 1.4 nM; clogD = 4.18).
机译:转运蛋白(18 kDa),称为TSPO,是公认的神经炎症生物标志物。带有PET的放射性配体可准确定量神经炎性疾病中的TSPO。但是,存在三种人类TSPO基因型,它们对几乎所有有用的TSPO PET放射性配体表现出不同的亲和力,从而阻碍了此类研究。对基因型不敏感,高亲和力和中等亲脂性TSPO配体的需求未得到满足,这些配体可作为PET放射性配体发展的先导。为了满足这一需求,我们在其芳基支架,侧链束缚带和碳纳米管中改变了已知的高亲和力TSPO配体(l)-N,N-二乙基-2-甲基-3-(2-苯基喹啉-4-基)丙酰胺侧基取代的酰胺基,同时保留N-甲基作为碳11标记的位点。通过这种努力,氧束缚的N-甲基-芳氧基丙酰胺成为具有亲脂性减弱的新型高亲和力TSPO配体,其中包括一个对PET放射性配体的开发具有吸引力的例子,即N-甲基-N-苯基-2-{[2- (吡啶-2-基)喹啉-4-基]氧基}丙酰胺(> 22a ;大鼠Ki = 0.10 nM;人TSPO基因型Ki = 1.4 nM; clogD = 4.18)。

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