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Postfusional regulation of cleft glutamate concentration during LTP at 'silent synapses'.“沉默突触”处长时程增强期间缝隙谷氨酸浓度的融合后调节
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The tetrameric structure of a glutamate receptor channel.谷氨酸受体通道的四聚体结构。
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Determinants of voltage attenuation in neocortical pyramidal neuron dendrites.新皮层锥体神经元树突中电压衰减的决定因素。
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Estimating the time course of the excitatory synaptic conductance in neocortical pyramidal cells using a novel voltage jump method.使用一种新型电压跳跃方法估计新皮层锥体神经元中兴奋性突触电导的时程。
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用于研究突触AMPA受体通道特性的非平稳波动分析的数学建模

Mathematical modelling of non-stationary fluctuation analysis for studying channel properties of synaptic AMPA receptors.

作者信息

Benke T A, Lüthi A, Palmer M J, Wikström M A, Anderson W W, Isaac J T, Collingridge G L

机构信息

MRC Centre for Synaptic Plasticity, Department of Anatomy, University of Bristol, University Walk, Bristol BS8 1TD, UK.

出版信息

J Physiol. 2001 Dec 1;537(Pt 2):407-20. doi: 10.1111/j.1469-7793.2001.00407.x.

DOI:10.1111/j.1469-7793.2001.00407.x
PMID:11731574
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2278972/
Abstract
  1. The molecular properties of synaptic alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionate (AMPA) receptors are an important factor determining excitatory synaptic transmission in the brain. Changes in the number (N) or single-channel conductance (gamma) of functional AMPA receptors may underlie synaptic plasticity, such as long-term potentiation (LTP) and long-term depression (LTD). These parameters have been estimated using non-stationary fluctuation analysis (NSFA). 2. The validity of NSFA for studying the channel properties of synaptic AMPA receptors was assessed using a cable model with dendritic spines and a microscopic kinetic description of AMPA receptors. Electrotonic, geometric and kinetic parameters were altered in order to determine their effects on estimates of the underlying gamma. 3. Estimates of gamma were very sensitive to the access resistance of the recording (R(A)) and the mean open time of AMPA channels. Estimates of gamma were less sensitive to the distance between the electrode and the synaptic site, the electrotonic properties of dendritic structures, recording electrode capacitance and background noise. Estimates of gamma were insensitive to changes in spine morphology, synaptic glutamate concentration and the peak open probability (P(o)) of AMPA receptors. 4. The results obtained using the model agree with biological data, obtained from 91 dendritic recordings from rat CA1 pyramidal cells. A correlation analysis showed that R(A) resulted in a slowing of the decay time constant of excitatory postsynaptic currents (EPSCs) by approximately 150 %, from an estimated value of 3.1 ms. R(A) also greatly attenuated the absolute estimate of gamma by approximately 50-70 %. 5. When other parameters remain constant, the model demonstrates that NSFA of dendritic recordings can readily discriminate between changes in gamma vs. changes in N or P(o). Neither background noise nor asynchronous activation of multiple synapses prevented reliable discrimination between changes in gamma and changes in either N or P(o). 6. The model (available online) can be used to predict how changes in the different properties of AMPA receptors may influence synaptic transmission and plasticity.
摘要
  1. 突触α-氨基-3-羟基-5-甲基-4-异恶唑丙酸(AMPA)受体的分子特性是决定大脑中兴奋性突触传递的一个重要因素。功能性AMPA受体数量(N)或单通道电导(γ)的变化可能是突触可塑性的基础,如长时程增强(LTP)和长时程抑制(LTD)。这些参数已通过非平稳波动分析(NSFA)进行了估算。2. 使用具有树突棘的电缆模型和AMPA受体的微观动力学描述,评估了NSFA用于研究突触AMPA受体通道特性的有效性。改变电紧张、几何和动力学参数,以确定它们对潜在γ估算值的影响。3. γ的估算值对记录的接入电阻(R(A))和AMPA通道的平均开放时间非常敏感。γ的估算值对电极与突触位点之间的距离、树突结构的电紧张特性、记录电极电容和背景噪声不太敏感。γ的估算值对棘突形态、突触谷氨酸浓度和AMPA受体的峰值开放概率(P(o))的变化不敏感。4. 使用该模型获得的结果与从大鼠CA1锥体神经元的91次树突记录中获得的生物学数据一致。相关性分析表明,R(A)导致兴奋性突触后电流(EPSCs)的衰减时间常数减慢约150%,从估计值3.1毫秒开始。R(A)还使γ的绝对估算值大幅衰减约50 - 70%。5. 当其他参数保持恒定时,该模型表明树突记录的NSFA能够轻松区分γ的变化与N或P(o)的变化。背景噪声和多个突触的异步激活均未妨碍可靠地区分γ的变化与N或P(o)的变化。6.该模型(可在线获取)可用于预测AMPA受体不同特性的变化如何影响突触传递和可塑性。