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γ-氨基丁酸(GABA)和甲碘化荷包牡丹碱对真实和模拟的须状桶中神经元感受野特性的定量影响。

Quantitative effects of GABA and bicuculline methiodide on receptive field properties of neurons in real and simulated whisker barrels.

作者信息

Kyriazi H T, Carvell G E, Brumberg J C, Simons D J

机构信息

Department of Neurobiology, University of Pittsburgh, Pennsylvania 15261, USA.

出版信息

J Neurophysiol. 1996 Feb;75(2):547-60. doi: 10.1152/jn.1996.75.2.547.

Abstract
  1. Carbon fiber multibarrel glass microelectrodes were used to record extracellular single-unit activity during microiontophoretic application of gamma-aminobutyric acid (GABA) or bicuculline methiodide (BMI) onto layer IV barrel neurons in the somatosensory cortex of fentanyl-sedated rats. Excitatory and inhibitory aspects of the neurons' receptive fields were quantified with the use of controlled whisker stimuli. The principally activating whisker and one of its immediately adjacent neighbors were deflected alone or in paired combinations involving a condition-test paradigm. 2. Units were distinguished electrophysiologically on the basis of the time course of their action potential waveforms. Data were obtained from 26 regular-spike units (RSUs; presumed spiny stellate cells) and 7 fast-spike units (FSUs; presumed GABAergic neurons). An average of 15.0 nA of GABA produced a one-third to one-half reduction in RSU responses evoked by the maximally effective stimulus. An average of 8.7 nA of BMI was needed to counteract this reduction. This amount of BMI, in the absence of exogenous GABA, was found to increase average RSU and FSU responses by 98 and 53%, respectively, relative to predrug levels. 3. For RSUs, the BMI-induced twofold increase in responses evoked by moving the principal whisker at the neuron's best deflection angle was accompanied by an almost threefold increase in responses evoked by similarly moving an adjacent whisker. Disproportionately large percentage increases were also seen for responses to nonpreferred directions of principal and adjacent whisker movement. BMI thus effectively increased receptive field size and decreased angular tuning. Similarly, responses to stimulus offsets, which are normally smaller than ON responses, were increased proportionally more. 4. Predrug responses of FSUs were more vigorous than those of RSUs. However, FSUs showed a similar inverse relationship between percentage increase with BMI and initial response magnitude, although the proportional increases were less pronounced. 5. GABA, like BMI, had the greatest proportional effects on those responses that were initially smallest. It produced results opposite those of BMI, effectively decreasing receptive field size and sharpening angular tuning. 6. A previously described computational model of a barrel was tested for its ability to reproduce quantitatively the effects of BMI and GABA. The application of BMI was simulated by decreasing the strength of the inhibitory inputs onto the particular cell under study in the model network. GABA microiontophoresis was simulated by adding a constant hyperpolarizing voltage. The model RSUs and FSUs displayed proportional changes in response magnitude that were quantitatively similar to those of their biological counterparts. 7. Surround inhibition was greatly attenuated by BMI application, both for the real and simulated barrel neurons. Disinhibition was less pronounced for the former, perhaps because, unlike the simulated neurons, they also possess GABAB receptors, which are unaffected by BMI. 8. We conclude that the inhibitory receptive field properties of barrel neurons can be explained by intrabarrel inhibition and that the expansion of receptive field size and loss of angular tuning with BMI is due to an enhanced effectiveness of convergent, multi-whisker thalamocortical input. Examination of the model neurons' behavior suggests that the altered activity in response to GABA or BMI application, respectively, can be explained by the nonlinear effects of shifting somal membrane potential away from or toward the neuron's firing threshold.
摘要
  1. 使用碳纤维多管玻璃微电极,在向芬太尼麻醉大鼠体感皮层IV层桶状神经元微量离子导入γ-氨基丁酸(GABA)或甲碘化荷包牡丹碱(BMI)期间记录细胞外单单位活动。通过使用受控的触须刺激来量化神经元感受野的兴奋和抑制方面。主要激活触须及其紧邻的一个相邻触须单独或按照涉及条件-测试范式的配对组合进行偏转。2. 根据动作电位波形的时间进程在电生理上区分单位。从26个规则放电单位(RSUs;推测为棘状星型细胞)和7个快速放电单位(FSUs;推测为GABA能神经元)获得数据。平均15.0 nA的GABA使最大有效刺激诱发的RSU反应降低三分之一到二分之一。平均需要8.7 nA的BMI来抵消这种降低。发现在没有外源性GABA的情况下,这个量的BMI相对于给药前水平分别使平均RSU和FSU反应增加98%和53%。3. 对于RSUs,在神经元最佳偏转角移动主要触须诱发的反应中,BMI引起的反应增加两倍,同时类似地移动相邻触须诱发的反应增加近三倍。对于主要和相邻触须向非偏好方向移动的反应,也观察到不成比例的大幅增加。因此,BMI有效地增加了感受野大小并降低了角度调谐。同样,对刺激偏移的反应(通常比开启反应小)增加的比例更大。4. FSU的给药前反应比RSU更强烈。然而,FSU在BMI增加百分比和初始反应幅度之间显示出类似的反比关系,尽管比例增加不太明显。5. GABA与BMI一样,对最初最小的那些反应具有最大的比例效应。它产生与BMI相反的结果,有效地减小了感受野大小并锐化了角度调谐。6. 测试了先前描述的桶状模型的计算模型定量再现BMI和GABA效应的能力。通过降低模型网络中正在研究的特定细胞上的抑制性输入强度来模拟BMI的应用。通过添加恒定的超极化电压来模拟GABA微量离子导入。模型RSUs和FSUs在反应幅度上显示出比例变化,在数量上与它们的生物学对应物相似。7. 对于真实的和模拟的桶状神经元,BMI的应用都大大减弱了周围抑制。前者的去抑制不太明显,可能是因为与模拟神经元不同,它们还拥有GABAB受体,而GABAB受体不受BMI影响。8. 我们得出结论,桶状神经元的抑制性感受野特性可以通过桶内抑制来解释,并且BMI导致的感受野大小扩大和角度调谐丧失是由于汇聚的多触须丘脑皮质输入的有效性增强。对模型神经元行为的检查表明,分别对GABA或BMI应用的活动改变可以通过将体细胞膜电位从神经元的放电阈值移开或移向该阈值的非线性效应来解释。

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