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内源性大麻素的自我调节抑制作用塑造 CA1 锥体神经元的尖峰时间精度。

Self-tuning of inhibition by endocannabinoids shapes spike-time precision in CA1 pyramidal neurons.

机构信息

Inserm, UMR_S 1072, Marseille, France;

出版信息

J Neurophysiol. 2013 Oct;110(8):1930-44. doi: 10.1152/jn.00099.2013. Epub 2013 Jul 31.

Abstract

In the hippocampus, activity-dependent changes of synaptic transmission and spike-timing coordination are thought to mediate information processing for the purpose of memory formation. Here, we investigated the self-tuning of intrinsic excitability and spiking reliability by CA1 hippocampal pyramidal cells via changes of their GABAergic inhibitory inputs and endocannabinoid (eCB) signaling. Firing patterns of CA1 place cells, when replayed in vitro, induced an eCB-dependent transient reduction of spontaneous GABAergic activity, sharing the main features of depolarization-induced suppression of inhibition (DSI), and conditioned a transient improvement of spike-time precision during consecutive burst discharges. When evaluating the consequences of DSI on excitatory postsynaptic potential (EPSP)-spike coupling, we found that transient reductions of uncorrelated (spontaneous) or correlated (feedforward) inhibition improved EPSP-spike coupling probability. The relationship between EPSP-spike-timing reliability and inhibition was, however, more complex: transient reduction of correlated (feedforward) inhibition disrupted or improved spike-timing reliability according to the initial spike-coupling probability. Thus eCB-mediated tuning of pyramidal cell spike-time precision is governed not only by the initial level of global inhibition, but also by the ratio between spontaneous and feedforward GABAergic activities. These results reveal that eCB-mediated self-tuning of spike timing by the discharge of pyramidal cells can constitute an important contribution to place-cell assemblies and memory formation in the hippocampus.

摘要

在海马体中,突触传递和尖峰时间协调的活动依赖性变化被认为介导了信息处理,以实现记忆形成的目的。在这里,我们通过改变 CA1 海马锥体神经元的 GABA 能抑制性输入和内源性大麻素(eCB)信号来研究内在兴奋性和尖峰可靠性的自我调节。当在体外回放 CA1 位置细胞的放电模式时,会诱导 eCB 依赖性的自发 GABA 能活性的瞬时减少,其具有去极化诱导抑制(DSI)的主要特征,并使连续爆发放电期间的尖峰时间精度得到暂时改善。当评估 DSI 对兴奋性突触后电位(EPSP)-尖峰耦合的后果时,我们发现不相关(自发)或相关(前馈)抑制的瞬时减少提高了 EPSP-尖峰耦合概率。然而,EPSP-尖峰时间可靠性与抑制之间的关系更加复杂:相关(前馈)抑制的瞬时减少根据初始尖峰耦合概率破坏或改善了尖峰时间可靠性。因此,eCB 介导的锥体细胞尖峰时间精度的自我调节不仅由全局抑制的初始水平决定,还由自发和前馈 GABA 能活动之间的比率决定。这些结果表明,eCB 介导的锥体细胞放电对尖峰时间的自我调节可以为海马体中的位置细胞集合和记忆形成做出重要贡献。

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