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新皮层中的同步伽马频率抑制取决于兴奋性-抑制性相互作用,而非电突触。

Synchronized gamma-frequency inhibition in neocortex depends on excitatory-inhibitory interactions but not electrical synapses.

作者信息

Neske Garrett T, Connors Barry W

机构信息

Department of Neuroscience, Brown University, Providence, Rhode Island.

Department of Neuroscience, Brown University, Providence, Rhode Island

出版信息

J Neurophysiol. 2016 Aug 1;116(2):351-68. doi: 10.1152/jn.00071.2016. Epub 2016 Apr 27.

Abstract

Synaptic inhibition plays a crucial role in the precise timing of spiking activity in the cerebral cortex. Synchronized, rhythmic inhibitory activity in the gamma (30-80 Hz) range is thought to be especially important for the active, information-processing neocortex, but the circuit mechanisms that give rise to synchronized inhibition are uncertain. In particular, the relative contributions of reciprocal inhibitory connections, excitatory-inhibitory interactions, and electrical synapses to precise spike synchrony among inhibitory interneurons are not well understood. Here we describe experiments on mouse barrel cortex in vitro as it spontaneously generates slow (<1 Hz) oscillations (Up and Down states). During Up states, inhibitory postsynaptic currents (IPSCs) are generated at gamma frequencies and are more synchronized than excitatory postsynaptic currents (EPSCs) among neighboring pyramidal cells. Furthermore, spikes in homotypic pairs of interneurons are more synchronized than in pairs of pyramidal cells. Comparing connexin36 knockout and wild-type animals, we found that electrical synapses make a minimal contribution to synchronized inhibition during Up states. Estimations of the delays between EPSCs and IPSCs in single pyramidal cells showed that excitation often preceded inhibition by a few milliseconds. Finally, tonic optogenetic activation of different interneuron subtypes in the absence of excitation led to only weak synchrony of IPSCs in pairs of pyramidal neurons. Our results suggest that phasic excitatory inputs are indispensable for synchronized spiking in inhibitory interneurons during Up states and that electrical synapses play a minimal role.

摘要

突触抑制在大脑皮层尖峰活动的精确计时中起着至关重要的作用。γ(30 - 80赫兹)范围内同步的、节律性抑制活动被认为对活跃的、进行信息处理的新皮层尤为重要,但产生同步抑制的电路机制尚不确定。特别是,相互抑制性连接、兴奋性 - 抑制性相互作用以及电突触对抑制性中间神经元之间精确的尖峰同步的相对贡献还没有得到很好的理解。在这里,我们描述了对体外培养的小鼠桶状皮层进行的实验,它会自发产生缓慢(<1赫兹)的振荡(上行和下行状态)。在下行状态期间,抑制性突触后电流(IPSCs)以γ频率产生,并且在相邻锥体细胞之间比兴奋性突触后电流(EPSCs)更同步。此外,同型中间神经元对之间的尖峰比锥体细胞对之间的尖峰更同步。比较连接蛋白36基因敲除小鼠和野生型小鼠,我们发现电突触在下行状态期间对同步抑制的贡献最小。对单个锥体细胞中EPSCs和IPSCs之间延迟的估计表明,兴奋通常比抑制提前几毫秒。最后,在没有兴奋的情况下对不同中间神经元亚型进行强直光遗传学激活仅导致锥体细胞对中IPSCs的微弱同步。我们的结果表明,在下行状态期间,相位性兴奋性输入对于抑制性中间神经元的同步尖峰是不可或缺的,并且电突触起的作用最小。

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