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神经甾体通过对齿状颗粒细胞抑制性回路的双脉冲易化作用对双脉冲抑制产生反常增强。

Neurosteroid paradoxical enhancement of paired-pulse inhibition through paired-pulse facilitation of inhibitory circuits in dentate granule cells.

作者信息

Thomas Michael J, Mameli Manuel, Carta Mario, Valenzuela C Fernando, Li Pui-Kai, Partridge L Donald

机构信息

Department of Neurosciences, University of New Mexico School of Medicine, Albuquerque, NM 87131, USA.

出版信息

Neuropharmacology. 2005 Mar;48(4):584-96. doi: 10.1016/j.neuropharm.2004.11.014.

Abstract

Neurosteroids are produced in the brain independently of peripheral endocrine glands to act locally in the nervous system. They exert potent promnesic effects and play significant roles in mental health-related disorders. In part, neurosteroids act by affecting ligand-gated ion channels and metabotropic receptors through rapid non-genomic processes. We have previously demonstrated that neurosteroids also affect synaptic transmission presynaptically in the CA1 region of the hippocampus. Here we describe the effects of the most abundant neurosteroid in the rodent brain, pregnenolone sulfate (PregS), on signal processing in the dentate subfield of the hippocampus. We show that PregS acts presynaptically at low concentrations (300 nM) to enhance paired-pulse facilitation (PPF) in perforant pathway terminals on dentate granule cells. Similar effects were found with two steroid sulfatase inhibitors demonstrating a potential contribution of endogenous steroids to dentate synaptic plasticity. This enhanced presynaptic facilitation paradoxically increases paired-pulse inhibition (PPI) at short interpulse intervals. Based on these data, a model of dentate gyrus circuit interactions is proposed for the presynaptic action of PregS on the filtering dynamics of the dentate subfield at frequencies similar to those of the endogenous signals from the entorhinal cortex. These modeling studies are consistent with experimental measurements demonstrating positive modulation by PregS at low frequencies and negative modulation at high frequencies. These studies show an important role for the presynaptic action of neurosteroids in modulating input signals to the hippocampus.

摘要

神经甾体在大脑中独立于外周内分泌腺产生,在神经系统中发挥局部作用。它们具有强大的促进记忆作用,在与心理健康相关的疾病中发挥重要作用。神经甾体部分通过快速的非基因组过程影响配体门控离子通道和代谢型受体来发挥作用。我们之前已经证明,神经甾体也会在海马体CA1区对突触传递产生突触前影响。在此,我们描述了啮齿动物大脑中最丰富的神经甾体硫酸孕烯醇酮(PregS)对海马齿状亚区信号处理的影响。我们发现,低浓度(300 nM)的PregS在突触前发挥作用,增强齿状颗粒细胞上穿通通路终末的双脉冲易化(PPF)。两种类固醇硫酸酯酶抑制剂也有类似作用,表明内源性类固醇对齿状突触可塑性有潜在贡献。这种增强的突触前易化在短脉冲间隔时反常地增加了双脉冲抑制(PPI)。基于这些数据,我们提出了一个齿状回回路相互作用模型,用于解释PregS对齿状亚区滤波动力学的突触前作用,其频率与来自内嗅皮质的内源性信号频率相似。这些建模研究与实验测量结果一致,即PregS在低频时起正向调节作用,在高频时起负向调节作用。这些研究表明神经甾体的突触前作用在调节海马体输入信号方面起着重要作用。

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