首页> 外文期刊>The Journal of Physiology >The dynamics of synchronized neurotransmitter release determined from compound spontaneous IPSCs in rat dentate granule neurones in vitro.
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The dynamics of synchronized neurotransmitter release determined from compound spontaneous IPSCs in rat dentate granule neurones in vitro.

机译:从大鼠齿状颗粒神经元中的复合自发IPSCs确定同步神经递质释放的动力学。

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1. The properties of GABAA receptor-mediated spontaneous IPSCs generated in hippocampal dentate granule neurones were analysed using whole-cell voltage-clamp techniques in order to explore the functional consequences of the low number (6-12) and close proximity of synaptic contacts made by single GABAergic interneurones. 2. Spontaneous IPSCs (sIPSCs) occurred with a frequency of 14.0 +/- 9.1 Hz (n = 31) and revealed a multi-modal positively skewed amplitude distribution (39.0 +/- 19.8 pA, median values). 3. The variance of 10-90% rise times and decay kinetics between IPSCs decreased with increasing peak amplitude. Larger amplitude events had significantly faster rise times, consistent with their site of generation being proximal to the soma. The decay kinetics of sIPSCs did not significantly change with amplitude. 4. Large amplitude sIPSCs occurred singularly or in discrete bursts, repeated regularly at low frequency. The rising phase of such sIPSCs were multi-phasic, composed of clear step-like inflections that were not a product of noise. The variability between the rising phase of individual sIPSCs was quantified by calculating their standard deviation, which produced fast rising (0.22 +/- 0.05 ms time to peak, n = 16) functions with half-widths of 0.38 +/- 0.10 ms, which declined to plateaux. 5. Computer simulations demonstrated that IPSCs with properties similar to those recorded experimentally could be generated by the linear summation of groups of temporally dispersed component events. Standard deviation functions of the rising phase of simulated IPSCs accurately described distributions of the temporal dispersion of unitary components. 6. The GABA uptake inhibitor (R)-N[4,4-bis(3-methyl-2-thienyl)but-3-enl-yl] nipecotic acid (tiagabine) (10 microM, n = 12) significantly prolonged the decay of mIPSCs (6.5 +/- 0.8 to 8.7 +/- 1.0 ms, median values) and sIPSCs (6.2 +/- 0.4 to 7.3 +/- 1.2 ms, median values), but failed to alter the frequency of occurrence, 10-90% rise times or peak amplitude of events. The application of flurazepam (30 microM, n = 7; 50 microM, n = 4) prolonged the decay of sIPSCs regardless of their amplitude. 7. These data indicate that sIPSCs are formed by the summation of unitary components that occur asynchronously and that GABA released from multiple sites has independent post-synaptic actions.
机译:1.使用全细胞电压钳技术分析了海马齿状颗粒神经元中GABAA受体介导的自发IPSC的特性,以探讨低数目(6-12)和紧密接触突触所产生的功能后果通过单个GABA能性神经元产生。 2.发生自发IPSC(sIPSC),频率为14.0 +/- 9.1 Hz(n = 31),并且显示出多模式正偏振幅分布(39.0 +/- 19.8 pA,中值)。 3. IPSC之间的10-90%上升时间方差和衰减动力学随峰幅度的增加而减小。较大的振幅事件具有明显更快的上升时间,这与它们的产生部位靠近躯体一致。 sIPSCs的衰减动力学没有随振幅而显着变化。 4.大振幅sIPSC单独或以离散脉冲串出现,并在低频下定期重复。这种sIPSC的上升阶段是多相的,由明显的阶梯状拐点构成,而不是噪声的产物。通过计算各个sIPSC的标准偏差来量化各个sIPSC上升阶段之间的差异,从而产生具有半宽度0.38 +/- 0.10 ms的快速上升(达到峰值的时间为0.22 +/- 0.05毫秒,n = 16)函数。拒绝高原。 5.计算机模拟表明,可以通过对时间分散的组分事件的组进行线性求和来生成具有与实验记录的特性相似的IPSC。模拟IPSC上升阶段的标准偏差函数准确地描述了单一成分的时间色散分布。 6. GABA吸收抑制剂(R)-N [4,4-双(3-甲基-2-噻吩基)丁-3-烯丙基]乳酸(替加滨)(10 microM,n = 12)显着延长了其吸收时间。 mIPSCs(6.5 +/- 0.8至8.7 +/- 1.0 ms,中值)的衰减和sIPSCs(6.2 +/- 0.4至7.3 +/- 1.2 ms,中值),但未能改变发生的频率10 -90%的上升时间或事件的峰值幅度。氟西epa(30 microM,n = 7; 50 microM,n = 4)的应用延长了sIPSCs的衰减,无论其幅度如何。 7.这些数据表明,sIPSC是由异步发生的单一成分的总和形成的,并且从多个位点释放的GABA具有独立的突触后作用。

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