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多巴胺D2样受体的反复刺激:黑质纹状体和中伏隔核多巴胺神经元对喹吡罗的反应性降低。

Repeated stimulation of dopamine D2-like receptors: reduced responsiveness of nigrostriatal and mesoaccumbens dopamine neurons to quinpirole.

作者信息

Pitts D K, Wang L, Kelland M D, Freeman A S, Chiodo L A

机构信息

Department of Pharmaceutical Sciences, College of Pharmacy and Allied Health Professions, Wayne State University, Detroit, Michigan, USA.

出版信息

J Pharmacol Exp Ther. 1995 Oct;275(1):412-21.

PMID:7562579
Abstract

Extracellular recording techniques were used to study antidromically activated nigrostriatal (NSDA) and mesoaccumbens (MADA) dopamine neurons in chloral hydrate-anesthetized rats. Repeated 14-day i.p. treatment with the dopamine D2-like receptor agonists, quinpirole (2 mg/kg/day) or EMD 23448 (2.6 mg/kg/day), resulted in a significant decrease in the average potency and efficacy of i.v. quinpirole (cumulative doses administered on day 15) to inhibit the spontaneous activity of NSDA neurons relative to vehicle controls. Repeated 14-day quinpirole treatment caused a significantly greater decrease in the sensitivity of MADA neurons to i.v. quinpirole challenges than NSDA neurons. When the effects on NSDA neurons were examined after a shorter treatment period, the decrease in the average potency and efficacy of i.v. quinpirole appeared to occur after only 2 days of i.p. quinpirole treatment (2 mg/kg/day). Iontophoretic studies, however, indicated that the average dopamine sensitivity of somatodendritic dopamine autoreceptors on MADA neurons, but not NSDA neurons, was significantly lower relative to controls after 14-day quinpirole treatment (2 mg/kg/day). These results suggest that this quinpirole treatment regimen can differentially affect the average sensitivity of somatodendritic dopamine autoreceptors on MADA and NSDA neurons. The somatodendritic autoreceptors on MADA neurons appear to be more sensitive to the effects of repeated 14-day quinpirole treatment than those on NSDA neurons.

摘要

采用细胞外记录技术,研究水合氯醛麻醉大鼠中经逆向激活的黑质纹状体(NSDA)和中脑伏隔核(MADA)多巴胺能神经元。用多巴胺D2样受体激动剂喹吡罗(2毫克/千克/天)或EMD 23448(2.6毫克/千克/天)对大鼠进行为期14天的腹腔注射重复治疗,相对于溶剂对照组,静脉注射喹吡罗(第15天给予累积剂量)抑制NSDA神经元自发活动的平均效力和效能显著降低。与NSDA神经元相比,为期14天的喹吡罗重复治疗使MADA神经元对静脉注射喹吡罗刺激的敏感性降低更为显著。在较短治疗期后检查对NSDA神经元的影响时,腹腔注射喹吡罗(2毫克/千克/天)仅2天后,静脉注射喹吡罗的平均效力和效能就出现了下降。然而,离子电渗法研究表明,在接受为期14天的喹吡罗治疗(2毫克/千克/天)后,相对于对照组,MADA神经元而非NSDA神经元上树突体多巴胺自身受体的平均多巴胺敏感性显著降低。这些结果表明,这种喹吡罗治疗方案可对MADA和NSDA神经元上树突体多巴胺自身受体的平均敏感性产生不同影响。MADA神经元上的树突体自身受体似乎比NSDA神经元上的树突体自身受体对为期14天的喹吡罗重复治疗的影响更敏感。

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