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特定于中间神经元的细胞提供的树突抑制控制海马反馈抑制回路的发放频率和时间。

Dendritic inhibition provided by interneuron-specific cells controls the firing rate and timing of the hippocampal feedback inhibitory circuitry.

机构信息

Axis of Cellular and Molecular Neuroscience, Institut Universitaire en Santé Mentale de Québec, Department of Biochemistry, Microbiology and Bio-informatics, Université Laval, Québec G1J 2G3, Canada, and Department of Bioengineering, Stanford University, Stanford, California 94305-5444.

出版信息

J Neurosci. 2014 Mar 26;34(13):4534-47. doi: 10.1523/JNEUROSCI.3813-13.2014.

Abstract

In cortical networks, different types of inhibitory interneurons control the activity of glutamatergic principal cells and GABAergic interneurons. Principal neurons represent the major postsynaptic target of most interneurons; however, a population of interneurons that is dedicated to the selective innervation of GABAergic cells exists in the CA1 area of the hippocampus. The physiological properties of these cells and their functional relevance for network computations remain unknown. Here, we used a combination of dual simultaneous patch-clamp recordings and targeted optogenetic stimulation in acute mouse hippocampal slices to examine how one class of interneuron-specific (IS) cells controls the activity of its GABAergic targets. We found that type 3 IS (IS3) cells that coexpress the vasoactive intestinal polypeptide (VIP) and calretinin contact several distinct types of interneurons within the hippocampal CA1 stratum oriens/alveus (O/A), with preferential innervation of oriens-lacunosum moleculare cells (OLMs) through dendritic synapses. In contrast, VIP-positive basket cells provided perisomatic inhibition to CA1 pyramidal neurons with the asynchronous GABA release and were not connected with O/A interneurons. Furthermore, unitary IPSCs recorded at IS3-OLM synapses had a small amplitude and low release probability but summated efficiently during high-frequency firing of IS3 interneurons. Moreover, the synchronous generation of a single spike in several IS cells that converged onto a single OLM controlled the firing rate and timing of OLM interneurons. Therefore, dendritic inhibition originating from IS cells is needed for the flexible activity-dependent recruitment of OLM interneurons for feedback inhibition.

摘要

在皮质网络中,不同类型的抑制性中间神经元控制着谷氨酸能主细胞和 GABA 能中间神经元的活动。主神经元代表大多数中间神经元的主要突触后靶标;然而,海马体 CA1 区存在一类专门用于 GABA 能细胞选择性支配的中间神经元。这些细胞的生理特性及其对网络计算的功能相关性仍然未知。在这里,我们使用双细胞同时膜片钳记录和靶向光遗传刺激的组合,在急性小鼠海马切片中研究了一类特定的中间神经元(IS)细胞如何控制其 GABA 能靶标的活性。我们发现,共表达血管活性肠肽(VIP)和钙视网膜蛋白的 3 型 IS(IS3)细胞与海马 CA1 层的几个不同类型的中间神经元接触,优先通过树突突触支配齿状回分子层细胞(OLM)。相比之下,VIP 阳性篮状细胞通过异步 GABA 释放对 CA1 锥体神经元提供胞体抑制,并且与 O/A 中间神经元没有连接。此外,在 IS3-OLM 突触记录的单位 IPSC 具有较小的幅度和低释放概率,但在 IS3 中间神经元高频放电期间有效总和。此外,几个 IS 细胞中的单个尖峰的同步产生,汇聚到单个 OLM 上,控制 OLM 中间神经元的发放率和时间。因此,起源于 IS 细胞的树突抑制对于灵活的、与活动相关的 OLM 中间神经元的募集用于反馈抑制是必要的。

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