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孤儿 G 蛋白偶联受体 GPR88 调节纹状体多巴胺系统的功能:精神疾病的潜在治疗靶点?

The orphan GPCR, GPR88, modulates function of the striatal dopamine system: a possible therapeutic target for psychiatric disorders?

机构信息

Discovery Neuroscience, Wyeth Research, CN 8000, Princeton, NJ 08543, USA.

出版信息

Mol Cell Neurosci. 2009 Dec;42(4):438-47. doi: 10.1016/j.mcn.2009.09.007. Epub 2009 Sep 29.

Abstract

In rodents, the orphan G protein-coupled receptor, Gpr88, is highly expressed in brain regions implicated in the pathophysiology of and is modulated by treatments for schizophrenia. We compared striatal function of Gpr88 knockout mice (Gpr88KOs) to wild-type mice using molecular, neurochemical and behavioral tests. Gpr88KOs lacked expression of Gpr88 in striatum, nucleus accumbens and layer IV of cortex. Gpr88KOs had normal striatal dopamine D2 receptor density and affinity and DARPP-32 expression but Gpr88KOs had higher basal striatal phosphorylated DARPP-32 Thr-34. In vivo microdialysis detected lower basal dopamine in Gpr88KOs while amphetamine-induced dopamine release was normal. Behaviorally, Gpr88KOs demonstrated disrupted prepulse inhibition of startle (PPI) and increased sensitivity to apomorphine-induced climbing and stereotypy (AICS) and amphetamine-stimulated locomotor activity. Antipsychotic administration to Gpr88KOs normalized the PPI deficit and blocked AICS. The modulatory role of Gpr88 in striatal dopamine function suggests it may be a new target for treatments for psychiatric disorders.

摘要

在啮齿动物中,孤儿 G 蛋白偶联受体 Gpr88 在大脑区域中高度表达,这些区域与精神分裂症的病理生理学有关,并受精神分裂症治疗的调节。我们使用分子、神经化学和行为测试比较了 Gpr88 敲除小鼠(Gpr88KOs)和野生型小鼠的纹状体功能。Gpr88KOs 在纹状体、伏隔核和皮层 IV 层中缺乏 Gpr88 的表达。Gpr88KOs 具有正常的纹状体多巴胺 D2 受体密度和亲和力以及 DARPP-32 表达,但 Gpr88KOs 具有更高的基础纹状体磷酸化 DARPP-32 Thr-34。体内微透析检测到 Gpr88KOs 中的基础多巴胺水平较低,而安非他命诱导的多巴胺释放正常。行为上,Gpr88KOs 表现出惊吓前脉冲抑制(PPI)受损,对阿扑吗啡诱导的攀爬和刻板行为(AICS)和安非他命刺激的运动活动敏感增加。抗精神病药物治疗可使 Gpr88KOs 的 PPI 缺陷正常化并阻断 AICS。Gpr88 在纹状体多巴胺功能中的调节作用表明,它可能是治疗精神疾病的新靶点。

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