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具有三种中间神经元类型和细胞类型特异性短期可塑性的感觉皮层分层微电路模型。

A layered microcircuit model of somatosensory cortex with three interneuron types and cell-type-specific short-term plasticity.

机构信息

Institute for Advanced Simulation (IAS-6), Jülich Research Centre, Wilhelm-Johnen-Straße, 52428 Jülich, Germany.

Institute of Zoology, University of Cologne, Albertus-Magnus-Platz, 50923 Cologne, Germany.

出版信息

Cereb Cortex. 2024 Sep 3;34(9). doi: 10.1093/cercor/bhae378.

Abstract

Three major types of GABAergic interneurons, parvalbumin-, somatostatin-, and vasoactive intestinal peptide-expressing (PV, SOM, VIP) cells, play critical but distinct roles in the cortical microcircuitry. Their specific electrophysiology and connectivity shape their inhibitory functions. To study the network dynamics and signal processing specific to these cell types in the cerebral cortex, we developed a multi-layer model incorporating biologically realistic interneuron parameters from rodent somatosensory cortex. The model is fitted to in vivo data on cell-type-specific population firing rates. With a protocol of cell-type-specific stimulation, network responses when activating different neuron types are examined. The model reproduces the experimentally observed inhibitory effects of PV and SOM cells and disinhibitory effect of VIP cells on excitatory cells. We further create a version of the model incorporating cell-type-specific short-term synaptic plasticity (STP). While the ongoing activity with and without STP is similar, STP modulates the responses of Exc, SOM, and VIP cells to cell-type-specific stimulation, presumably by changing the dominant inhibitory pathways. With slight adjustments, the model also reproduces sensory responses of specific interneuron types recorded in vivo. Our model provides predictions on network dynamics involving cell-type-specific short-term plasticity and can serve to explore the computational roles of inhibitory interneurons in sensory functions.

摘要

三种主要类型的 GABA 能中间神经元,即表达 Parvalbumin、Somatostatin 和 Vasoactive Intestinal Peptide 的(PV、SOM、VIP)细胞,在皮质微电路中发挥着关键但不同的作用。它们特定的电生理学和连接方式塑造了它们的抑制功能。为了研究这些细胞类型在大脑皮层中的特定网络动态和信号处理,我们开发了一个多层模型,该模型整合了来自啮齿动物体感皮层的具有生物学现实性的中间神经元参数。该模型与细胞类型特异性群体放电率的体内数据拟合。通过细胞类型特异性刺激方案,检查激活不同神经元类型时的网络响应。该模型再现了 PV 和 SOM 细胞对兴奋性细胞的抑制作用和 VIP 细胞的去抑制作用的实验观察结果。我们进一步创建了一个包含细胞类型特异性短期突触可塑性(STP)的模型版本。虽然有和没有 STP 的持续活动相似,但 STP 调节了 Exc、SOM 和 VIP 细胞对细胞类型特异性刺激的反应,可能通过改变主导抑制途径来实现。通过轻微调整,该模型还再现了体内记录的特定中间神经元类型的感觉反应。我们的模型提供了涉及细胞类型特异性短期可塑性的网络动态的预测,并可用于探索抑制性中间神经元在感觉功能中的计算作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/867c/11439972/51b012289421/bhae378f1.jpg

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