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Synthesis PharmacologicalCharacterization and Structure–ActivityRelationship Studies of Small Molecular Agonists for the Orphan GPR88Receptor

机译:合成药理学表征和结构活动小分子激动剂对孤儿GPR88的关系研究受体

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摘要

GPR88 is an orphan G-protein-coupled receptor (GPCR) enriched in the striatum. Genetic deletion and gene expression studies have suggested that GPR88 plays an important role in the regulation of striatal functions and is implicated in psychiatric disorders. The signal transduction pathway and receptor functions of GPR88, however, are still largely unknown due to the lack of endogenous and synthetic ligands. In this paper, we report the synthesis of a GPR88 agonist 2-PCCA and its pure diastereomers, which were functionally characterized in both transiently and stably expressing GPR88 HEK293 cells. 2-PCCA inhibited isoproterenol-stimulated cAMP accumulation in a concentration-dependent manner in cells expressing GPR88 but not in the control cells, suggesting that the observed cAMP inhibition is mediated through GPR88 and that GPR88 is coupled to Gαi. 2-PCCA did not induce calcium mobilization in GPR88 cells, indicating no Gαq-mediated response. A structure–activity relationship (SAR) study of 2-PCCA was also conducted to explore the key structural features for GPR88 agonistactivity.
机译:GPR88是富含纹状体的孤儿G蛋白偶联受体(GPCR)。遗传缺失和基因表达研究表明,GPR88在调节纹状体功能中起重要作用,并与精神疾病有关。然而,由于缺乏内源性和合成的配体,GPR88的信号转导途径和受体功能仍然未知。在本文中,我们报告了GPR88激动剂2-PCCA及其纯非对映异构体的合成,它们在瞬时和稳定表达GPR88 HEK293细胞中均具有功能特征。 2-PCCA在表达GPR88的细胞中以异丙基肾上腺素刺激的cAMP积累呈浓度依赖性,但在对照细胞中却没有,这表明观察到的cAMP抑制是通过GPR88介导的,并且GPR88与Gαi偶联。 2-PCCA在GPR88细胞中不诱导钙动员,表明没有Gαq介导的反应。还进行了2-PCCA的构效关系(SAR)研究,以探索GPR88激动剂的关键结构特征活动。

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