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首页> 美国卫生研究院文献>The Journal of Neuroscience >The Striatal Neurotensin Receptor Modulates Striatal and Pallidal Glutamate and GABA Release: Functional Evidence for a Pallidal Glutamate–GABA Interaction via the Pallidal–Subthalamic Nucleus Loop
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The Striatal Neurotensin Receptor Modulates Striatal and Pallidal Glutamate and GABA Release: Functional Evidence for a Pallidal Glutamate–GABA Interaction via the Pallidal–Subthalamic Nucleus Loop

机译:纹状体神经降压素受体调节纹状体和苍白质谷氨酸和GABA的释放:经由苍白质-丘脑底核环的谷氨酸-GABA相互作用的功能证据

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In the present study, we used dual-probe microdialysis to investigate the effects of intrastriatal perfusion with neurotensin (NT) on striatal and pallidal glutamate and GABA release. The role of the pallidal GABAA receptor in the intrastriatal NT-induced increase in pallidal glutamate release was also investigated.Intrastriatal NT (100 and 300 nm) increased striatal glutamate and GABA (100 nm, 155 ± 9 and 141 ± 6%, respectively; 300 nm, 179 ± 8 and 166 ± 11%, respectively) release, as well as pallidal glutamate and GABA (100 nm, 144 ± 8 and 130 ± 5%; 300 nm, 169 ± 9 and 157 ± 8%, respectively) release. These effects were dose-dependently antagonized by the NT receptor antagonist 2-[(1-(7-chloro-4-quinolinyl)-5-(2,6-dimethoxy-phenyl)pyrazol-3-yl)carboxylamino]tricyclo)3.3.1.1.3.7)-decan-2-carboxylic acid (SR48692).Intrasubthalamic injection of the GABAA receptor antagonist (−)-bicuculline (10 pmol/100 nl, 30 sec) rapidly increased pallidal glutamate release, whereas the intrastriatal NT-induced increase in pallidal glutamate release was counteracted by intrapallidal perfusion with (−)-bicuculline, suggesting that an increase in striopallidal GABA-mediated inhibition of the GABAergic pallidal–subthalamic pathway results in an increased glutamatergic drive in the subthalamic–pallidal pathway.These results demonstrate a tonic pallidal GABA-mediated inhibition of excitatory subthalamic–pallidal neurons and strengthen the evidence for a functional role of NT in the regulation of glutamate and GABA transmission in the basal ganglia. The ability of intrastriatal SR48692 to counteract the NT-induced increase in both striatal and pallidal glutamate and GABA release suggests that blockade of the striatal NT receptor may represent a possible new therapeutic strategy in the treatment of those hypokinetic disorders implicated in disorders of the indirect pathway mediating motor inhibition.
机译:在本研究中,我们使用双探针微透析法研究纹状体内神经降压素(NT)灌注对纹状体和苍白质谷氨酸和GABA释放的影响。还研究了苍白质GABAA受体在纹状体内NT诱导的苍白质谷氨酸释放增加中的作用。纹状体内NT(100和300 nm)分别增加纹状体谷氨酸和GABA(100 nm,155±9和141±6%);分别释放300 nm,179±8和166±11%),谷氨酸和GABA(100 nm,144±8和130±5%; 300 nm,169±9和157±8%)释放释放。这些作用被NT受体拮抗剂2-[((1-(7-氯-4-喹啉基)-5-(2,6-二甲氧基-苯基)吡唑-3-基)羧氨基]三环)3.3剂量依赖性拮抗。 .1.1。 3.7 )-癸烷-2-羧酸(SR48692)。丘脑下注射GABAA受体拮抗剂(-)-比瓜氨酸(10 pmol / 100 nl,30秒)迅速增加谷氨酸的释放,而纹状体内NT诱导的苍白质谷氨酸释放的增加被(-)-比库林的苍白质内灌注所抵消,这表明,纹状顶GABA介导的对GABA能性苍白下丘脑途径的抑制作用的增加导致丘脑下谷氨酸能驱动增加-苍白球途径。这些结果证明了强壮的苍白球GABA介导的对兴奋性丘脑-苍白球下神经元的抑制作用,并增强了NT在调节基底神经节中谷氨酸和GABA传递中的功能性作用的证据。纹状体内SR48692抵抗NT引起的纹状体和苍白质谷氨酸和GABA释放增加的能力表明,纹状体NT受体的阻断可能代表了治疗那些与间接途径疾病有关的运动障碍的新治疗策略介导运动抑制。

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