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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Pathway-Specific Drive of Cerebellar Golgi Cells Reveals Integrative Rules of Cortical Inhibition
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Pathway-Specific Drive of Cerebellar Golgi Cells Reveals Integrative Rules of Cortical Inhibition

机译:小脑GOLGI细胞的途径特异性驱动揭示了皮质抑制的综合规则

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Cerebellar granule cells (GrCs) constitute over half of all neurons in the vertebrate brain and are proposed to decorrelate convergent mossy fiber (MF) inputs in service of learning. Interneurons within the GrC layer, Golgi cells (GoCs), are the primary inhibitors of this vast population and therefore play a major role in influencing the computations performed within the layer. Despite this central function for GoCs, few studies have directly examined how GoCs integrate inputs from specific afferents, which vary in density to regulate GrC population activity. We used a variety of methods in mice of either sex to study feedforward inhibition recruited by identified MFs, focusing on features that would influence integration by GrCs. Comprehensive 3D reconstruction and quantification of GoC axonal boutons revealed tightly clustered boutons that focus feedforward inhibition in the neighborhood of GoC somata. Acute whole-cell patch-clamp recordings from GrCs in brain slices showed that, despite high GoC bouton density, fast phasic inhibition was very sparse relative to slow spillover mediated inhibition. Dynamic-clamp simulating inhibition combined with optogenetic MF activation at moderate rates supported a predominant role of slow spillover mediated inhibition in reducing GrC activity. Whole-cell recordings from GoCs revealed a role for the density of active MFs in preferentially driving them. Thus, our data provide empirical confirmation of predicted rules by which MFs activate GoCs to regulate GrC activity levels.
机译:小脑颗粒细胞(GRC)构成脊椎动物中所有神经元的一半,并建议在学习服务中取消封闭会聚的苔藓纤维(MF)输入。 GOLGI细胞(GOCS)内的巨大抑制剂是这种庞大的人口的初级抑制剂,因此在影响层内执行的计算来发挥重要作用。尽管GOCS的核心功能,但很少有研究直接检查了GOCS如何从密度的密度变化,以调节GRC种群活动的特定传入。我们在任何性别中使用了各种方法,以研究通过识别的MFS募集的前馈抑制,专注于将影响GRC集成的功能。 GoC轴突围绕GoC轴突展示的全面的3D重建和量化揭示了GOC Somata附近的前馈抑制的紧密聚集的前置。来自脑切片中GRC的急性全细胞贴片夹具显示,尽管GOC Bouton密度高,相对于缓慢溢出介导的抑制,快速相位抑制非常稀疏。动态钳位模拟抑制与中等速率以磷酸盐MF激活相结合,支持缓冲介导的抑制在减少GRC活性中的抑制作用。来自GOC的全部细胞记录揭示了活性MFS密度优先驱动它们的作用。因此,我们的数据提供了预测规则的经验确认,通过该规则,MFS激活GOCs来调节GRC活动水平。

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