吗啡通过腹侧被盖区ampa受体释放谷氨酸:有意识大鼠的微透析研究

H. Alaei, M. Huotari, P. Piepponen, L. Ahtee, O. Hänninen, P. Männistö
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引用次数: 7

摘要

吸毒成瘾已发展成为一种社会疾病。通过在VTA中反复施用成瘾性药物,记录了谷氨酸传递的变化。本研究采用体内微透析法研究吗啡对自由活动大鼠腹侧被盖区谷氨酸释放的影响。用水合氯醛(350 mg/kg, i.p.)麻醉大鼠,置于Kopf立体定向器中。垂直引导套管通过一个毛刺孔植入,用牙水泥固定在颅骨上,并用小螺钉固定。右VTA微透析探头尖端相对于bregma的最终坐标为:正位(AP), 5.8;根据Paxinos图谱,侧位(L)为0.5,背腹位(DV)为9.0。术后1周将微透析探头插入引导管内,灌注人工脑脊液(aCSF)。冲洗60分钟后,透析液样品在20分钟内收集在小瓶和20?m用于谷氨酸高效液相色谱分析。急性腹腔注射和不断增加剂量的吗啡可显著增强谷氨酸释放。对吗啡的这种作用只有轻微的耐受性。每次重复注射吗啡前20分钟给予NMDA受体拮抗剂AP-5(2-氨基-5-磷酸戊酸,0.5 mg/kg i.p.),对刺激的谷氨酸释放无显著影响。相反,在每次给药前20分钟注射AMPA受体拮抗剂CNQX(6-氰-7-硝基喹诺沙林- 2,3 -二酮,0.5 mg/kg i.p)可显著抑制吗啡诱导的VTA谷氨酸释放。在所有的实验中,谷氨酸的释放都随着时间的推移而减少。这些结果首次表明,急性和反复注射吗啡可通过AMPA受体刺激意识大鼠VTA中谷氨酸的释放。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
MORPHINE RELEASES GLUTAMATE THROUGH AMPA RECEPTORS IN THE VENTRAL TEGMENTAL AREA: A MICRODIALYSIS STUDY IN CONSCIOUS RATS
Drug addiction has developed to a social illness. Changes in glutamate transmission have been recorded by the repeated administration of addictive drugs into VTA. In this investigation, In vivo microdialysis was used to study the effects of morphine on glutamate release from the ventral tegmentum area (VTA) in freely moving rats. Rats were anesthetized with chloral hydrate (350 mg/kg, i.p.) and placed in a Kopf stereotaxic apparatus. A vertical guide cannula was implanted through a burr hole and secured with dental cement held on the skull with small screws. The final co-ordinates for the tip of the microdialysis probe in right VTA relative to bregma were: anteroposterior (AP), 5.8; lateral (L), 0.5 and dorsoventral (DV), 9.0 according to atlas of Paxinos. One week after surgery, the microdialysis probe was inserted into the guide cannula and perfused with artificial cerebrospinal fluid (aCSF). After a 60 min wash out period, dialysate samples were collected in 20 min periods in vials and 20?m was used for glutamate HPLC analysis. Intraperitoneal (IP) injection of acute and repeated administration of morphine at increasing doses enhanced significantly glutamate release. Only a minor tolerance developed to this effect of morphine. AP-5 (2-amino-5-phosphonovaleric acid, 0.5 mg/kg i.p.), a NMDA receptor antagonist, given 20 min before each repeated morphine injection, did not have a significant effect on the stimulated glutamate release. Conversely, injection of CNQX (6-cyano-7-nitroquinnoxaline-2, 3-dione, 0.5 mg/kg i.p), an AMPA receptor antagonist, 20 min before each morphine dose was found to markedly inhibit morphine-induced glutamate release in the VTA. In all experiments, release of glutamate reduced by time. These results show for the first time that acute and repeated injection of morphine stimulates glutamate release in the conscious rat VTA via AMPA receptors.
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