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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Stimulated D(1) dopamine receptors couple to multiple Galpha proteins in different brain regions.
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Stimulated D(1) dopamine receptors couple to multiple Galpha proteins in different brain regions.

机译:刺激的D(1)多巴胺受体耦合到不同大脑区域中的多个Galpha蛋白。

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Previous studies have revealed that activation of rat striatal D(1) dopamine receptors stimulates both adenylyl cyclase and phospholipase C via G(s) and G(q), respectively. The differential distribution of these systems in brain supports the existence of distinct receptor systems. The present communication extends the study by examining other brain regions: hippocampus, amygdala, and frontal cortex. In membrane preparations of these brain regions, selective stimulation of D(1) dopamine receptors increases the hydrolysis of phosphatidylinositol/phosphatidylinositol 4,5-biphosphate. In these brain regions, D(1) dopamine receptors couple differentially to multiple Galpha protein subunits. Antisera against Galpha(q) blocks dopamine-stimulated PIP(2) hydrolysis in hippocampal and in striatal membranes. The binding of [(35)S]GTPgammaS or [alpha-(32)P]GTP to Galpha(i) was enhanced in all brain regions. Dopamine also increased the binding of [(35)S]GTPgammaS or [alpha-(32)P]GTP to Galpha(q) in these brain regions: hippocampus = amygdala > frontal cortex. However, dopamine-stimulated binding of [(35)S]GTPgammaS to Galphas only in the frontal cortex and striatum. This differential coupling profile in the brain regions was not related to a differential regional distribution of the Galpha proteins. Dopamine induced increases in GTPgammaS binding to Galpha(s) and Galpha(q) was blocked by the D(1) antagonist SCH23390 but not by D(2) receptor antagonist l-sulpiride, suggesting that D(1) dopamine receptors couple to both Galpha(s) and Galpha(q) proteins. Co-immunoprecipitation of Galpha proteins with receptor-binding sites indicate that in the frontal cortex, D(1) dopamine-binding sites are associated with both Galpha(s) and Galpha(q) and, in hippocampus or amygdala, D(1) dopamine receptors couple solely to Galpha(q). The results indicate that in addition to the D(1)/G(s)/adenylyl cyclase system, brain D(1)-like dopamine receptor sites activate phospholipase C through Galpha(q) protein.
机译:先前的研究表明,大鼠纹状体D(1)多巴胺受体的激活分别通过G(s)和G(q)刺激腺苷酸环化酶和磷脂酶C。这些系统在脑中的差异分布支持不同受体系统的存在。本交流通过检查其他大脑区域(海马,杏仁核和额叶皮层)扩展了研究范围。在这些大脑区域的膜准备中,D(1)多巴胺受体的选择性刺激会增加磷脂酰肌醇/磷脂酰肌醇4,5-二磷酸酯的水解。在这些大脑区域,D(1)多巴胺受体差异地耦合到多个Galpha蛋白亚基。针对Galpha(q)的抗血清可阻断多巴胺刺激的海马和纹状体膜中的PIP(2)水解。 [(35)S] GTPgammaS或[alpha-(32)P] GTP与Galpha(i)的结合在所有脑区域中都得到增强。多巴胺还增加了以下区域的[(35)S] GTPgammaS或[α-(32)P] GTP与Galpha(q)的结合:海马=杏仁核>额叶皮层。但是,多巴胺仅在额叶皮层和纹状体中刺激[(35)S] GTPgammaS与Galphas的结合。脑区中的这种差异性耦合分布与Galpha蛋白的差异性区域分布无关。多巴胺诱导的GTPgammaS与Galpha(s)和Galpha(q)的结合增加被D(1)拮抗剂SCH23390阻止,但未被D(2)受体拮抗剂l-舒必利阻断,这表明D(1)多巴胺受体与两者结合Galpha和Galpha(q)蛋白。 Galpha蛋白与受体结合位点的共免疫沉淀表明,在额叶皮层中,D(1)多巴胺结合位点与Galpha(s)和Galpha(q)相关,在海马或杏仁核中,D(1)多巴胺受体仅与Galpha(q)偶联。结果表明,除了D(1)/ G(s)/腺苷酸环化酶系统,脑D(1)-样多巴胺受体位点通过Galpha(q)蛋白激活磷脂酶C。

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