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Acute effects of D-1 and D-2 dopamine receptor agonist and antagonist drugs on basal ganglia Met5- and Leu5-enkephalin and neurotensin content in the rat

机译:D-1和D-2多巴胺受体激动剂和拮抗剂药物对大鼠基底神经节Met5-和Leu5-脑啡肽和神经降压素含量的急性影响

摘要

The effects of acute systemic injection of the D-1 agonist SKF 38393 (2.5¿20 mg/kg) or the D-1 antagonist SCH 23390 (0.25¿2.0 mg/kg), and of the D-2 agonist quinpirole (0.12¿1.0 mg/kg) or the D-2 antagonist sulpiride (25¿100 mg/kg) on the neuropeptide content of rat basal ganglia were investigated. In striatum, the [Met5]- and [Leu5]-enkephalin content was unaffected by administration of SKF 38393 or SCH 23390. Quinpirole had no effect on [Met5]- and [Leu5]-enkephalin levels but sulpiride produced an increase in both [Met5]- and (Leu5]-enkephalin content. In the nucleus accumbens, SKF 38393 decreased and SCH 23390 increased [Met5]- and [Leu5]-enkephalin levels. Quinpirole decreased [Met5]- and- [Leu5]-enkephalin levels, while sulpiride decreased [Leu5]-enkephalin levels alone. The content of [Leu5]- but not [Met5]-enkephalin levels in the substantia nigra was increased by administration of SKF 38393, and decreased by SCH 23390. Quinpirole and sulpiride were without effect on the [Met5]- or [Leu5]-enkephalin content of substantia nigra. Neurotensin levels in striatum were increased by administration of SKF 38393 and decreased by SCH 23390. Similarly, quinpirole decreased the neurotensin content while sulpiride caused an increase. In the nucleus accumbens, the neurotensin content was not affected by administration of SKF 38393 but increased by SCH 23390. Neither quinpirole nor sulpiride altered neurotensin levels in the nucleus accumbens. Neurotensin levels in substantia nigra were unaffected by the administration of SKF 38393 and SCH 23390, or by quinpirole and sulpiride. These results indicate that acute administration of D-1 and D-2 agonist and antagonist drugs can alter the levels of [Met5]- and [Leu5]-enkephalin and neurotensin in basal ganglia. However, there are marked differences between brain regions in the regulation of peptide levels by acute D-1 and D-2 receptor occupation
机译:急性全身注射D-1激动剂SKF 38393(2.5?20 mg / kg)或D-1拮抗剂SCH 23390(0.25?2.0 mg / kg)和D-2激动剂喹吡罗(0.12?研究了对大鼠基底神经节神经肽含量的1.0 mg / kg或D-2拮抗剂舒必利(25?100 mg / kg)。在纹状体中,[Met5]-和[Leu5]-脑啡肽的含量不受SKF 38393或SCH 23390的影响。喹吡洛尔对[Met5]-和[Leu5]-脑啡肽水平没有影响,但舒必利使[ Met5]-和(Leu5]-脑啡肽含量。伏伏核中,SKF 38393降低,SCH 23390升高[Met5]-和[Leu5]-脑啡肽水平;喹吡罗降低[Met5]-和-[Leu5]-脑啡肽水平,舒必利单独降低[Leu5]-脑啡肽水平,黑素中[Leu5]-而不是[Met5]-脑啡肽水平通过施用SKF 38393而增加,而通过SCH 23390降低,喹吡罗尔和舒必利无效对黑质的[Met5]-或[Leu5]-脑啡肽含量有影响,施用SKF 38393可增加纹状体中神经降压素水平,而SCH 23390则可降低纹状体中神经降压素水平;同样地,喹吡罗降低神经降压素含量,而舒必利则升高。伏隔中神经降压素含量不受SKF 38393的影响,但受SCH 23390的影响有所增加。喹吡罗和舒必利均未改变伏隔核中的神经降压素水平。黑色素中的神经降压素水平不受SKF 38393和SCH 23390或喹吡罗和舒必利的影响。这些结果表明,D-1和D-2激动剂和拮抗剂的急性给药可以改变基底神经节中[Met5]-和[Leu5]-脑啡肽和神经降压素的水平。然而,大脑区域之间在急性D-1和D-2受体占领对肽水平的调节方面存在明显差异

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