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新皮质切片中癫痫样电压变化的光学记录。

Optical recording of epileptiform voltage changes in the neocortical slice.

作者信息

Albowitz B, Kuhnt U, Ehrenreich L

机构信息

Max-Planck-Institute for Biophysical Chemistry, Department of Neurobiology, Göttingen, Federal Republic of Germany.

出版信息

Exp Brain Res. 1990;81(2):241-56. doi: 10.1007/BF00228113.

Abstract

Voltage sensitive probes were used to monitor the development, distribution, and spread of epileptiform potentials with a photodiode array in neocortical slices of guinea pigs. Epileptiform activity was induced by bath application of bicuculline-methiodide or 3,4-diaminopyridine and electrical stimulation of white matter or cortical layer I. Stimulation evoked a primary or early potential which was followed by a delayed epileptiform potential with a larger spatial extent. Shape, duration and amplitude of the delayed epileptiform potential varied strongly among slices and across the recording area and could reach largest amplitudes at a distance from the stimulation point. At a specific recording site, however, with repeated stimulation, potentials were generated in a stereotyped way. Intracellularly recorded delayed epileptiform potentials corresponded very closely at least to the early part of the optical response. Epileptiform activity appeared in layer III as soon as the primary potential reached sufficient amplitude there. Apart from this relationship, the distribution and spread of maximal amplitudes of delayed epileptiform potentials were segregated from those of early potentials. Early potentials reached maximal amplitudes close to the stimulation site. In contrast, the largest amplitudes of delayed epileptiform potentials were always found in layer III. A second maximum occasionally occurred in layer V. The horizontal amplitude distribution of epileptiform potentials was asymmetric, i.e. amplitudes increased to one side and decreased to the other. Early potential maxima spread from deeper to upper layers when initiated by white matter stimulation and from upper to deeper layers when initiated by layer I stimulation. In contrast, delayed epileptiform potentials always spread from layer III to lower layers and to the sides. Velocity of spread of early potentials and delayed epileptiform potentials differed systematically along the vertical and horizontal axis. The distribution of maximal amplitudes, shape, and pattern, of spread of epileptiform potentials was the same whether white matter or layer I was stimulated. The independence of delayed epileptiform potential characteristics from the point of stimulation and from early potential characteristics suggests that epileptiform activity is determined by intrinsic properties of the cortex and not by afferent activation.

摘要

使用电压敏感染料探针,通过光电二极管阵列监测豚鼠新皮质切片中癫痫样电位的发生、分布和传播。通过在浴槽中加入荷包牡丹碱甲碘化物或3,4-二氨基吡啶以及对白质或皮质I层进行电刺激来诱发癫痫样活动。刺激引发一个初级或早期电位,随后是一个空间范围更大的延迟癫痫样电位。延迟癫痫样电位的形状、持续时间和幅度在不同切片以及记录区域内差异很大,并且在距刺激点一定距离处可达到最大幅度。然而,在特定记录位点,随着重复刺激,电位以刻板的方式产生。细胞内记录的延迟癫痫样电位至少在光学反应的早期部分与之非常密切对应。一旦初级电位在III层达到足够幅度,癫痫样活动就会在该层出现。除了这种关系外,延迟癫痫样电位最大幅度的分布和传播与早期电位的分布和传播是分开的。早期电位在靠近刺激位点处达到最大幅度。相比之下,延迟癫痫样电位的最大幅度总是出现在III层。偶尔在V层会出现第二个最大值。癫痫样电位的水平幅度分布是不对称的,即幅度向一侧增加而向另一侧减小。当由白质刺激引发时,早期电位最大值从深层向上层传播,而当由I层刺激引发时,从上层向深层传播。相比之下,延迟癫痫样电位总是从III层向下层和向两侧传播。早期电位和延迟癫痫样电位的传播速度在垂直和水平轴上有系统的差异。无论刺激白质还是I层,癫痫样电位最大幅度的分布、形状和传播模式都是相同的。延迟癫痫样电位特征与刺激点和早期电位特征的独立性表明,癫痫样活动是由皮质的内在特性决定的,而不是由传入激活决定的。

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