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用红藻氨酸反复低剂量全身治疗后复发性自发性运动性癫痫发作:颞叶癫痫大鼠模型的评估

Recurrent spontaneous motor seizures after repeated low-dose systemic treatment with kainate: assessment of a rat model of temporal lobe epilepsy.

作者信息

Hellier J L, Patrylo P R, Buckmaster P S, Dudek F E

机构信息

Department of Anatomy and Neurobiology, Colorado State University, Fort Collins 80523, USA.

出版信息

Epilepsy Res. 1998 Jun;31(1):73-84. doi: 10.1016/s0920-1211(98)00017-5.

Abstract

Human temporal lobe epilepsy is associated with complex partial seizures that can produce secondarily generalized seizures and motor convulsions. In some patients with temporal lobe epilepsy, the seizures and convulsions occur following a latent period after an initial injury and may progressively increase in frequency for much of the patient's life. Available animal models of temporal lobe epilepsy are produced by acute treatments that often have high mortality rates and/or are associated with a low proportion of animals developing spontaneous chronic motor seizures. In this study, rats were given multiple low-dose intraperitoneal (i.p.) injections of kainate in order to minimize the mortality rate usually associated with single high-dose injections. We tested the hypothesis that these kainate-treated rats consistently develop a chronic epileptic state (i.e. long-term occurrence of spontaneous, generalized seizures and motor convulsions) following a latent period after the initial treatment. Kainate (5 mg/kg per h, i.p.) was administered to rats every hour for several hours so that class III-V seizures were elicited for > or = 3 h, while control rats were treated similarly with saline. This treatment protocol had a relatively low mortality rate (15%). After acute treatment, rats were observed for the occurrence of motor seizures for 6-8 h/week. Nearly all of the kainate-treated rats (97%) had two or more spontaneous motor seizures months after treatment. With this observation protocol, the average latency for the first spontaneous motor seizure was 77+/-38 (+/-S.D.) days after treatment. Although variability was observed between rats, seizure frequency initially increased with time after treatment, and nearly all of the kainate-treated rats (91%) had spontaneous motor seizures until the time of euthanasia (i.e. 5-22 months after treatment). Therefore, multiple low-dose injections of kainate, which cause recurrent motor seizures for > or = 3 h, lead to the development of a chronic epileptic state that is characterized by (i) a latent period before the onset of chronic motor seizures, and (ii) a high but variable seizure frequency that initially increases with time after the first chronic seizure. This modification of the kainate-treatment protocol is efficient and relatively simple, and the properties of the chronic epileptic state appear similar to severe human temporal lobe epilepsy. Furthermore, the observation that seizure frequency initially increased as a function of time after kainate treatment supports the hypothesis that temporal lobe epilepsy can be a progressive syndrome.

摘要

人类颞叶癫痫与复杂部分性发作相关,后者可继发全身性发作和运动性惊厥。在一些颞叶癫痫患者中,发作和惊厥在初次损伤后的潜伏期后出现,并且在患者的大部分生命中发作频率可能逐渐增加。现有的颞叶癫痫动物模型是通过急性处理产生的,这些处理通常具有高死亡率和/或与发生自发性慢性运动性发作的动物比例较低相关。在本研究中,给大鼠多次腹腔内注射低剂量的红藻氨酸,以尽量降低通常与单次高剂量注射相关的死亡率。我们检验了这样的假设,即这些经红藻氨酸处理的大鼠在初次处理后的潜伏期后会持续发展为慢性癫痫状态(即自发性全身性发作和运动性惊厥的长期发作)。以每小时5mg/kg的剂量给大鼠腹腔内注射红藻氨酸,持续数小时,以使III-V级发作诱发≥3小时,而对照大鼠用生理盐水进行类似处理。该处理方案的死亡率相对较低(15%)。急性处理后,每周观察大鼠6-8小时,记录运动性发作的发生情况。几乎所有经红藻氨酸处理的大鼠(97%)在处理数月后出现两次或更多次自发性运动性发作。按照这个观察方案,首次自发性运动性发作的平均潜伏期为处理后77±38(±标准差)天。尽管不同大鼠之间存在差异,但发作频率在处理后的最初阶段随时间增加,几乎所有经红藻氨酸处理的大鼠(91%)在安乐死时(即处理后5-22个月)都有自发性运动性发作。因此,多次低剂量注射红藻氨酸,诱发复发性运动性发作≥3小时,会导致慢性癫痫状态的发展,其特征为:(i)慢性运动性发作开始前有潜伏期;(ii)发作频率高但有变化,在首次慢性发作后最初随时间增加。这种红藻氨酸处理方案的改进有效且相对简单,慢性癫痫状态的特征似乎与严重的人类颞叶癫痫相似。此外,红藻氨酸处理后发作频率最初随时间增加这一观察结果支持了颞叶癫痫可能是一种进行性综合征的假设。

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