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体感诱发电位增强的额部和顶叶成分:病理状态与药物诱导状态的比较

Frontal and parietal components of enhanced somatosensory evoked potentials: a comparison between pathological and pharmacologically induced conditions.

作者信息

Ebner A, Deuschl G

机构信息

Neurologische Klinik und Poliklinik, Universität Freiburg, F.R.G.

出版信息

Electroencephalogr Clin Neurophysiol. 1988 May-Jun;71(3):170-9. doi: 10.1016/0168-5597(88)90002-0.

DOI:10.1016/0168-5597(88)90002-0
PMID:2451599
Abstract

Pathologically enhanced somatosensory evoked potentials (giant SEPs) were recorded in 10 patients with cortical myoclonus of various origins. With non-cephalic reference electrodes a giant frontal negativity corresponding to normal N30 was found over the contra- and ipsilateral hemispheres which was not simply a phase reversal of the well-known enhanced parietal P25. The preceding far-field P14, parietal N20 and frontal P22 were of normal size. A similar result was found when SEPs were studied during the action of etomidate, an ultrashort-acting non-barbiturate hypnotic which produced a marked increase of the parietal P25 and frontal N30 after intravenous administration. These increased components, on the other hand, were abolished when recording was repeated immediately after application of electroconvulsive shock whereas P14, N20, and P22 remained more or less unchanged in both conditions. Our results indicate that there are neuronal elements in the sensorimotor cortex which are more resistant to influences such as narcotic drugs and seizure activity than others, being highly modifiable by these alterations. It is speculated whether these highly modifiable cortical systems are those in which giant SEPs, as well as pharmacologically increased SEP components, arise.

摘要

在10例不同病因的皮质肌阵挛患者中记录到了病理性增强的体感诱发电位(巨大SEP)。使用非头部参考电极时,在对侧和同侧半球发现了一个与正常N30相对应的巨大额叶负波,这并非简单地是众所周知的增强顶叶P25的相位反转。之前的远场P14、顶叶N20和额叶P22大小正常。当在依托咪酯作用期间研究SEP时也发现了类似结果,依托咪酯是一种超短效非巴比妥类催眠药,静脉注射后会使顶叶P25和额叶N30显著增加。另一方面,在应用电惊厥休克后立即重复记录时,这些增加的成分消失了,而P14、N20和P22在两种情况下或多或少保持不变。我们的结果表明,感觉运动皮层中存在一些神经元成分,它们比其他成分对麻醉药物和癫痫活动等影响更具抵抗力,但会因这些改变而高度可塑。推测这些高度可塑的皮质系统是否就是产生巨大SEP以及药理学上增加的SEP成分的系统。

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