一种新型的穿透血脑屏障的 NPS 受体拮抗剂,NCGC00185684,可阻断酒精诱导的中枢杏仁核中 ERK 磷酸化,并减少大鼠的操作性酒精自我给药。
A novel brain penetrant NPS receptor antagonist, NCGC00185684, blocks alcohol-induced ERK-phosphorylation in the central amygdala and decreases operant alcohol self-administration in rats.
机构信息
Laboratory of Clinical and Translational Studies, National Institute on Alcohol Abuse and Alcoholism, Bethesda, Maryland 20892, USA.
出版信息
J Neurosci. 2013 Jun 12;33(24):10132-42. doi: 10.1523/JNEUROSCI.4742-12.2013.
Abstract
The Neuropeptide S receptor, a Gs/Gq-coupled GPCR expressed in brain regions involved in mediating drug reward, has recently emerged as a candidate therapeutic target in addictive disorders. Here, we describe the in vitro and in vivo pharmacology of a novel, selective and brain penetrant NPSR antagonist with nanomolar affinity for the NPSR, NCGC00185684. In vitro, NCGC00185684 shows biased antagonist properties, and preferentially blocks ERK-phosphorylation over intracellular cAMP or calcium responses to NPS. In vivo, systemic NCGC00185684 blocks alcohol-induced ERK-phosphorylation in the rat central amygdala, a region involved in regulation of alcohol intake. NCGC00185684 also decreases operant alcohol self-administration, and lowers motivation for alcohol reward as measured using progressive ratio responding. These effects are behaviorally specific, in that they are observed at doses that do not influence locomotor activity or reinstatement responding following extinction. Together, these data provide an initial validation of the NPSR as a therapeutic target in alcoholism.
摘要
神经肽 S 受体是一种 Gs/Gq 偶联的 G 蛋白偶联受体,表达于参与介导药物奖赏的脑区,最近已成为成瘾性疾病的候选治疗靶点。在这里,我们描述了一种新型、选择性且可穿透血脑屏障的 NPSR 拮抗剂的体外和体内药理学特性,该拮抗剂对 NPSR 具有纳摩尔亲和力,编号为 NCGC00185684。在体外,NCGC00185684 表现出偏向性拮抗剂特性,优先阻断 NPS 诱导的 ERK 磷酸化,而不是细胞内 cAMP 或钙反应。在体内,系统给予 NCGC00185684 可阻断大鼠中枢杏仁核中酒精诱导的 ERK 磷酸化,该区域参与调节酒精摄入。NCGC00185684 还可降低操作性酒精自我给药,以及使用递增比率反应测量时降低对酒精奖赏的动机。这些作用具有行为特异性,因为它们是在不影响运动活动或在消退后重新出现反应的剂量下观察到的。总之,这些数据初步验证了 NPSR 作为治疗酒精中毒的靶点。
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