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小鼠海马区稀疏特定颗粒细胞激活的延长性产后发育。

Protracted postnatal development of sparse, specific dentate granule cell activation in the mouse hippocampus.

机构信息

Division of Neurology and the Pediatric Regional Epilepsy Program, Children's Hospital of Philadelphia, Philadelphia, Pennsylvania 19104, USA.

出版信息

J Neurosci. 2013 Feb 13;33(7):2947-60. doi: 10.1523/JNEUROSCI.1868-12.2013.

Abstract

The dentate gyrus (DG) is a critical entry point regulating function of the hippocampus. Integral to this role are the sparse, selective activation characteristics of the principal cells of the DG, dentate granule cells (DGCs). This sparse activation is important both in cognitive processing and in regulation of pathological activity in disease states. Using a novel, combined dynamic imaging approach capable of resolving sequentially both synaptic potentials and action potential firing in large populations of DGCs, we characterized the postnatal development of firing properties of DG neurons in response to afferent activation in mouse hippocampal-entorhinal cortical slices. During postnatal development, there was a protracted, progressive sparsification of responses, accompanied by increased temporal precision of activation. Both of these phenomena were primarily mediated by changes in local circuit inhibition, and not by alterations in afferent innervation of DGCs because GABA(A) antagonists normalized developmental differences. There was significant θ and γ frequency-dependent synaptic recruitment of DGC activation in adult, but not developing, animals. Finally, we found that the decision to fire or not fire by individual DGCs was robust and repeatable at all stages of development. The protracted postnatal development of sparse, selective firing properties, increased temporal precision and frequency dependence of activation, and the fidelity with which the decision to fire is made are all fundamental circuit determinants of DGC excitation, critical in both normal and pathological function of the DG.

摘要

齿状回(DG)是调节海马功能的关键入口。DG 的主要细胞——颗粒细胞(DGCs)的稀疏、选择性激活特征是其发挥作用的基础。这种稀疏激活对于认知加工以及调节疾病状态下的病理性活动都很重要。我们采用了一种新的、结合的动态成像方法,该方法能够在海马-内嗅皮质脑片的大量 DGC 中依次解析突触电位和动作电位的发射,从而对 DG 神经元在传入激活下的出生后发育中的发射特性进行了特征描述。在出生后的发育过程中,反应逐渐变得稀疏,激活的时间精度也随之提高。这两种现象主要是由局部回路抑制的变化介导的,而不是由 DGC 的传入神经支配的改变引起的,因为 GABA(A)拮抗剂使发育差异正常化。在成年动物中,DGC 的激活存在显著的θ和γ频率依赖性突触募集,但在发育中的动物中则没有。最后,我们发现,单个 DGC 是否发射的决策在发育的所有阶段都是稳健且可重复的。稀疏、选择性发射特性的延长性出生后发育、激活的时间精度和频率依赖性的提高,以及发射决策的准确性,都是 DGC 兴奋的基本电路决定因素,对 DG 的正常和病理功能都至关重要。

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