首页> 外文期刊>The Journal of Physiology >Functional interconnectivity between the globus pallidus and the subthalamic nucleus in the mouse brain slice.
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Functional interconnectivity between the globus pallidus and the subthalamic nucleus in the mouse brain slice.

机译:小鼠大脑切片中苍白球与丘脑下核之间的功能互连。

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In accordance with its central role in basal ganglia circuitry, changes in the rate of action potential firing and pattern of activity in the globus pallidus (GP)-subthalamic nucleus (STN) network are apparent in movement disorders. In this study we have developed a mouse brain slice preparation that maintains the functional connectivity between the GP and STN in order to assess its role in shaping and modulating bursting activity promoted by pharmacological manipulations. Fibre-tract tracing studies indicated that a parasagittal slice cut 20 deg to the midline best preserved connectivity between the GP and the STN. IPSCs and EPSCs elicited by electrical stimulation confirmed connectivity from GP to STN in 44/59 slices and from STN to GP in 22/33 slices, respectively. In control slices, 74/76 (97%) of STN cells fired tonically at a rate of 10.3 +/- 1.3 Hz. This rate and pattern of single spiking activity was unaffected by bath application of the GABA(A) antagonist picrotoxin (50 microM, n = 9) or the glutamate receptor antagonist (6-cyano-7-nitroquinoxaline-2, 3-dione (CNQX) 10 microM, n = 8). Bursting activity in STN neurones could be induced pharmacologically by application of NMDA alone (20 microm, 3/18 cells, 17%) but was more robust if NMDA was applied in conjunction with apamin (20-100 nM, 34/77 cells, 44%). Once again, neither picrotoxin (50 microM, n = 5) nor CNQX (10 microM, n = 5) had any effect on the frequency or pattern of the STN neurone activity while paired STN and GP recordings of tonic and bursting activity show no evidence of coherent activity. Thus, in a mouse brain slice preparation where functional GP-STN connectivity is preserved, no regenerative synaptically mediated activity indicative of a dynamic network is evident, either in the resting state or when neuronal bursting in both the GP and STN is generated by application of NMDA/apamin. This difference from the brain in Parkinson's disease may be attributed either to insufficient preservation of cortico-striato-pallidal or cortico-subthalamic circuitry, and/or an essential requirement for adaptive changes resulting from dopamine depletion for the expression of network activity within this tissue complex.
机译:根据其在基底神经节回路中的核心作用,在运动障碍中,苍白球(GP)-丘脑底核(STN)网络中动作电位的发射速率和活动模式的变化很明显。在这项研究中,我们开发了一种小鼠脑切片制剂,该制剂可维持GP和STN之间的功能连接性,从而评估其在塑造和调节药理操作促进的爆发活性中的作用。纤维束追踪研究表明,沿矢状切面切至中线20度可最佳保留GP和STN之间的连通性。电刺激引起的IPSC和EPSC分别证实了44/59切片中从GP到STN和22/33切片中从STN到GP的连通性。在对照切片中,有74/76(97%)个STN细胞以10.3 +/- 1.3 Hz的频率音调发射。加标GABA(A)拮抗剂微毒素(50 microM,n = 9)或谷氨酸受体拮抗剂(6-cyano-7-nitroquinoxaline-2,3-dione(CNQX) )10 microM,n = 8)。单独应用NMDA(20 microm,3/18细胞,17%)可以在药理上诱导STN神经元的爆发活性,但如果将NMDA与apaapamin(20-100 nM,34/77细胞,44)结合使用,则其活性更强%)。再一次,微毒素(50 microM,n = 5)和CNQX(10 microM,n = 5)都对STN神经元活性的频率或模式没有任何影响,而补品和爆裂活性的STN和GP配对记录则没有证据连贯的活动。因此,在保留了功能性GP-STN连接性的小鼠脑切片制剂中,无论是在静止状态还是通过施加GP产生神经元爆发时,都没有明显的突触介导的动态网络指示动态网络的迹象。 NMDA /阿帕明。帕金森氏病与大脑的差异可能归因于皮质-纹状体-苍白球或皮质-丘脑底回路的保存不充分,和/或由于多巴胺耗竭而导致的适应性变化的基本要求,该组织复合物中的网络活性表达。

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