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海马体和听觉皮层中不同形式的短期突触可塑性与慢抑制性突触后电位之间的净相互作用。

Net interaction between different forms of short-term synaptic plasticity and slow-IPSPs in the hippocampus and auditory cortex.

作者信息

Buonomano D V, Merzenich M M

机构信息

Keck Center for Integrative Neuroscience, University of California, San Francisco, California 94143, USA.

出版信息

J Neurophysiol. 1998 Oct;80(4):1765-74. doi: 10.1152/jn.1998.80.4.1765.

Abstract

Paired-pulse plasticity is typically used to study the mechanisms underlying synaptic transmission and modulation. An important question relates to whether, under physiological conditions in which various opposing synaptic properties are acting in parallel, the net effect is facilitatory or depressive, that is, whether cells further or closer to threshold. For example, does the net sum of paired-pulse facilitation (PPF) of excitatory postsynaptic potentials (EPSPs), paired-pulse depression (PPD) of inhibitory postsynaptic potentials (IPSPs), and the hyperpolarizing slow IPSP result in depression or facilitation? Here we examine how different time-dependent properties act in parallel and examine the contribution of gamma-aminobutyric acid-B (GABAB) receptors that mediate two opposing processes, the slow IPSP and PPD of the fast IPSP. Using intracellular recordings from rat CA3 hippocampal neurons and L-II/III auditory cortex neurons, we examined the postsynaptic responses to paired-pulse stimulation (with intervals between 50 and 400 ms) of the Schaffer collaterals and white matter, respectively. Changes in the amplitude, time-to-peak (TTP), and slope of each EPSP were analyzed before and after application of the GABAB antagonist CGP-55845. In both CA3 and L-II/III neurons the peak amplitude of the second EPSP was generally depressed (further from threshold) compared with the first at the longer intervals; however, these EPSPs were generally broader and exhibited a longer TTP that could result in facilitation by enhancing temporal summation. At the short intervals CA3 neurons exhibited facilitation of the peak EPSP amplitude in the absence and presence of CGP-55845. In contrast, on average L-II/III cells did not exhibit facilitation at any interval, in the absence or presence of CGP-55845. CGP-55845 generally "erased" short-term plasticity, equalizing the peak amplitude and TTP of the first and second EPSPs at longer intervals in the hippocampus and auditory cortex. These results show that it is necessary to consider all time-dependent properties to determine whether facilitation or depression will dominate under intact pharmacological conditions. Furthermore our results suggest that GABAB-dependent properties may be the major contributor to short-term plasticity on the time scale of a few hundred milliseconds and are consistent with the hypothesis that the balance of different time-dependent processes can modulate the state of networks in a complex manner and could contribute to the generation of temporally sensitive neural responses.

摘要

配对脉冲可塑性通常用于研究突触传递和调制的潜在机制。一个重要的问题是,在各种相反的突触特性并行起作用的生理条件下,净效应是易化还是抑制,也就是说,细胞是更接近还是更远离阈值。例如,兴奋性突触后电位(EPSP)的配对脉冲易化(PPF)、抑制性突触后电位(IPSP)的配对脉冲抑制(PPD)以及超极化慢IPSP的总和会导致抑制还是易化?在这里,我们研究了不同的时间依赖性特性如何并行起作用,并研究了介导两个相反过程(慢IPSP和快IPSP的PPD)的γ-氨基丁酸B(GABAB)受体的作用。使用大鼠CA3海马神经元和L-II/III听觉皮层神经元的细胞内记录,我们分别研究了对Schaffer侧支和白质的配对脉冲刺激(间隔为50至400毫秒)的突触后反应。在应用GABAB拮抗剂CGP-55845之前和之后,分析了每个EPSP的幅度、峰值时间(TTP)和斜率的变化。在CA3和L-II/III神经元中,在较长间隔时,与第一个EPSP相比,第二个EPSP的峰值幅度通常会降低(更远离阈值);然而,这些EPSP通常更宽,并且表现出更长的TTP,这可能通过增强时间总和而导致易化。在短间隔时,在不存在和存在CGP-55845的情况下,CA3神经元的EPSP峰值幅度均表现出易化。相反,平均而言,在不存在或存在CGP-55845的情况下,L-II/III细胞在任何间隔都未表现出易化。CGP-55845通常会“消除”短期可塑性,使海马体和听觉皮层中较长间隔时第一个和第二个EPSP的峰值幅度和TTP相等。这些结果表明,有必要考虑所有时间依赖性特性,以确定在完整的药理学条件下易化还是抑制将占主导地位。此外,我们的结果表明,GABAB依赖性特性可能是几百毫秒时间尺度上短期可塑性的主要贡献者,并且与以下假设一致:不同时间依赖性过程的平衡可以以复杂的方式调节网络状态,并可能有助于产生时间敏感的神经反应。

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