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不同类型海马生长抑素中间神经元的突触和树突结构。

Synaptic and dendritic architecture of different types of hippocampal somatostatin interneurons.

机构信息

Laboratory of Cerebral Cortex Research, HUN-REN Institute of Experimental Medicine, Budapest, Hungary.

János Szentágothai Doctoral School of Neurosciences, Semmelweis University, Budapest, Hungary.

出版信息

PLoS Biol. 2024 Mar 12;22(3):e3002539. doi: 10.1371/journal.pbio.3002539. eCollection 2024 Mar.

Abstract

GABAergic inhibitory neurons fundamentally shape the activity and plasticity of cortical circuits. A major subset of these neurons contains somatostatin (SOM); these cells play crucial roles in neuroplasticity, learning, and memory in many brain areas including the hippocampus, and are implicated in several neuropsychiatric diseases and neurodegenerative disorders. Two main types of SOM-containing cells in area CA1 of the hippocampus are oriens-lacunosum-moleculare (OLM) cells and hippocampo-septal (HS) cells. These cell types show many similarities in their soma-dendritic architecture, but they have different axonal targets, display different activity patterns in vivo, and are thought to have distinct network functions. However, a complete understanding of the functional roles of these interneurons requires a precise description of their intrinsic computational properties and their synaptic interactions. In the current study we generated, analyzed, and make available several key data sets that enable a quantitative comparison of various anatomical and physiological properties of OLM and HS cells in mouse. The data set includes detailed scanning electron microscopy (SEM)-based 3D reconstructions of OLM and HS cells along with their excitatory and inhibitory synaptic inputs. Combining this core data set with other anatomical data, patch-clamp electrophysiology, and compartmental modeling, we examined the precise morphological structure, inputs, outputs, and basic physiological properties of these cells. Our results highlight key differences between OLM and HS cells, particularly regarding the density and distribution of their synaptic inputs and mitochondria. For example, we estimated that an OLM cell receives about 8,400, whereas an HS cell about 15,600 synaptic inputs, about 16% of which are GABAergic. Our data and models provide insight into the possible basis of the different functionality of OLM and HS cell types and supply essential information for more detailed functional models of these neurons and the hippocampal network.

摘要

GABA 能抑制性神经元从根本上塑造了皮质回路的活动和可塑性。这些神经元的一个主要亚群包含生长抑素(SOM);这些细胞在包括海马体在内的许多大脑区域的神经可塑性、学习和记忆中发挥着关键作用,并与几种神经精神疾病和神经退行性疾病有关。海马体 CA1 区含有 SOM 的两种主要细胞类型是始层-腔隙-分子层(OLM)细胞和海马-隔核(HS)细胞。这些细胞类型在它们的体树突结构上有许多相似之处,但它们的轴突靶标不同,在体内表现出不同的活动模式,并且被认为具有不同的网络功能。然而,要全面了解这些中间神经元的功能作用,需要精确描述它们的内在计算特性及其突触相互作用。在当前的研究中,我们生成、分析并提供了几个关键数据集,这些数据集使我们能够对小鼠中 OLM 和 HS 细胞的各种解剖和生理特性进行定量比较。该数据集包括 OLM 和 HS 细胞的详细基于扫描电子显微镜(SEM)的 3D 重建,以及它们的兴奋性和抑制性突触输入。将这个核心数据集与其他解剖学数据、膜片钳电生理学和分区模型相结合,我们研究了这些细胞的精确形态结构、输入、输出和基本生理特性。我们的研究结果突出了 OLM 和 HS 细胞之间的关键差异,特别是在它们的突触输入和线粒体的密度和分布方面。例如,我们估计一个 OLM 细胞接收约 8400 个突触输入,而一个 HS 细胞接收约 15600 个突触输入,其中约 16%是 GABA 能的。我们的数据和模型提供了对 OLM 和 HS 细胞类型不同功能的可能基础的深入了解,并为这些神经元和海马体网络的更详细功能模型提供了必要信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e19d/10959371/db5b0d5f9f5e/pbio.3002539.g001.jpg

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