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皮质损伤对清醒大鼠青霉素诱发惊厥活动的影响。

The influence of cortical lesions on penicillin induced convulsive activity in the awake rat.

作者信息

Horn E, Esseling K, Kornhuber H H

机构信息

Abteilung für Neurologie, Universitätsklinikum Ulm, F.R.G.

出版信息

Arch Ital Biol. 1990 Jan;128(1):1-18.

PMID:2331205
Abstract
  1. Experiments were performed to investigate the effects of cortical lesions on convulsive behaviour. Rats were lesioned in the left motor or sensory cortex by aspirating cortical tissue 2 to 3 months prior to the elicitation of convulsions. Convulsions were induced in the awake rats by the GABA antagonist Na-penicillin (Na-PCN) which was applied into the superficial layer of the foreleg field of their right motor cortex. Convulsive activity was recorded by means of the EEG. 2. The time courses of convulsive cortical activity were similar in the animals without or with a cortical lesion. Generalized seizures belonged to the tonic-clonic type in both intact and lesioned rats. 3. The early period of convulsive activity was described by the time to the onset (latency) of the first convulsive potential, jerk and seizure, and by the mean repetition rate of jerks during the first ten minutes, and the duration of the first generalized seizure. None of these parameters was significantly affected by a cortical lesion. 4. The median duration of the convulsive activity in intact animals was 162 min. In rats with a lesion in the sensory cortex it raised to more than 540 min while a lesion of the motor cortex increased the median duration to more than 273 min. The differences between intact and lesioned rats were significant (p less than 0.01 and p = 0.05, respectively). 5. The median time to the onset of the last generalized seizure in intact rats corresponded to 92 min with respect to the time of Na-PCN application. In rats with a lesion of the sensory cortex the last seizure was generated 433 min and in animals with a lesion of the motor cortex 167 min after Na-PCN treatment of the motor cortex of one side. This increase of latency of the last seizure was significant for the rats with a lesioned sensory area (p less than 0.02) or motor area (p = 0.05) compared to that of the intact rats. Additionally, the number of generalized seizures was significantly (p less than 0.01) increased by both groups of rats with a lesion of the motor or sensory cortex. 6. It is suggested that a substantial lesion of the cortex decreases predominantly the intrinsic cortical inhibition thus destabilizing brain function. This destabilizing effect becomes pronounced under the condition of superimposed suppression of the GABAergic cortical component. It is concluded that the intrinsic cortical inhibitory mechanism which in the intact brain acts against hyperexcitation and prevents the development of neuronal synchronization, i.e. the formation of seizures, becomes less effective in performing this task once an abnormal brain activation has developed.
摘要
  1. 进行实验以研究皮层损伤对惊厥行为的影响。在诱发惊厥前2至3个月,通过抽吸皮层组织对大鼠左侧运动或感觉皮层进行损伤。通过将GABA拮抗剂青霉素钠(Na-PCN)应用于其右侧运动皮层前肢区域的表层,在清醒大鼠中诱发惊厥。惊厥活动通过脑电图进行记录。2. 有无皮层损伤的动物惊厥皮层活动的时间进程相似。完整大鼠和损伤大鼠的全身性惊厥均属于强直-阵挛型。3. 惊厥活动的早期阶段通过首次惊厥电位、抽搐和惊厥发作的起始时间(潜伏期)、前十分钟内抽搐的平均重复率以及首次全身性惊厥的持续时间来描述。这些参数均未受到皮层损伤的显著影响。4. 完整动物惊厥活动的中位持续时间为162分钟。感觉皮层有损伤的大鼠中,该时间延长至540分钟以上,而运动皮层损伤则使中位持续时间增加至273分钟以上。完整大鼠和损伤大鼠之间的差异具有显著性(分别为p<0.01和p = 0.05)。5. 完整大鼠中最后一次全身性惊厥发作的中位时间相对于青霉素钠应用时间为92分钟。在一侧运动皮层接受青霉素钠治疗后,感觉皮层有损伤的大鼠中最后一次惊厥在433分钟时发生,运动皮层有损伤的动物中为167分钟。与完整大鼠相比,感觉区域或运动区域有损伤的大鼠最后一次惊厥潜伏期的增加具有显著性(感觉皮层损伤组p<0.02,运动皮层损伤组p = 0.05)。此外,运动或感觉皮层有损伤的两组大鼠全身性惊厥的次数均显著增加(p<0.01)。6. 提示皮层的实质性损伤主要降低了皮层内在抑制,从而使脑功能不稳定。在叠加抑制GABA能皮层成分的情况下,这种不稳定作用变得明显。得出结论,在完整大脑中对抗过度兴奋并防止神经元同步化形成(即惊厥形成)的皮层内在抑制机制,一旦出现异常脑激活,在执行该任务时就会变得效率降低。

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