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对大鼠内侧颞叶癫痫海马内红藻氨酸模型的各种改良,均未能消除该模型中自发癫痫发作类型和频率在大鼠与小鼠之间存在的显著差异。

Various modifications of the intrahippocampal kainate model of mesial temporal lobe epilepsy in rats fail to resolve the marked rat-to-mouse differences in type and frequency of spontaneous seizures in this model.

作者信息

Klee Rebecca, Brandt Claudia, Töllner Kathrin, Löscher Wolfgang

机构信息

Department of Pharmacology, Toxicology, and Pharmacy, University of Veterinary Medicine Hannover, Germany, and Center for Systems Neuroscience, Hannover, Germany.

Department of Pharmacology, Toxicology, and Pharmacy, University of Veterinary Medicine Hannover, Germany, and Center for Systems Neuroscience, Hannover, Germany.

出版信息

Epilepsy Behav. 2017 Mar;68:129-140. doi: 10.1016/j.yebeh.2016.11.035. Epub 2017 Feb 4.

Abstract

Temporal lobe epilepsy (TLE) is the most common type of acquired epilepsy in adults. TLE can develop after diverse brain insults, including traumatic brain injury, infections, stroke, or prolonged status epilepticus (SE). Post-SE rodent models of TLE are widely used to understand mechanisms of epileptogenesis and develop treatments for epilepsy prevention. In this respect, the intrahippocampal kainate model of TLE in mice is of interest, because highly frequent spontaneous electrographic seizures develop in the kainate focus, allowing evaluation of both anti-seizure and anti-epileptogenic effects of novel drugs with only short EEG recording periods, which is not possible in any other model of TLE, including the intrahippocampal kainate model in rats. In the present study, we investigated whether the marked mouse-to-rat difference in occurrence and frequency of spontaneous seizures is due to a species difference or to technical variables, such as anesthesia during kainate injection, kainate dose, or location of kainate injection and EEG electrode in the hippocampus. When, as in the mouse model, anesthesia was used during kainate injection, only few rats developed epilepsy, although severity or duration of SE was not affected by isoflurane. In contrast, most rats developed epilepsy when kainate was injected without anesthesia. However, frequent electrographic seizures as observed in mice did not occur in rats, irrespective of location of kainate injection (CA1, CA3) or EEG recording electrode (CA1, CA3, dentate gyrus) or dose of kainate injected. These data indicate marked phenotypic differences between mice and rats in this model. Further studies should explore the mechanisms underlying this species difference.

摘要

颞叶癫痫(TLE)是成人中最常见的获得性癫痫类型。TLE可在多种脑损伤后发生,包括创伤性脑损伤、感染、中风或长时间癫痫持续状态(SE)。TLE的SE后啮齿动物模型被广泛用于了解癫痫发生机制并开发预防癫痫的治疗方法。在这方面,小鼠海马内注射红藻氨酸盐的TLE模型很受关注,因为在红藻氨酸盐病灶中会出现高度频繁的自发性脑电图发作,这使得仅通过短时间的脑电图记录就能评估新药的抗癫痫发作和抗癫痫发生作用,而这在任何其他TLE模型中都无法实现,包括大鼠海马内注射红藻氨酸盐的模型。在本研究中,我们调查了自发性癫痫发作的发生率和频率在小鼠和大鼠之间存在显著差异是由于物种差异还是技术变量,如红藻氨酸盐注射期间的麻醉、红藻氨酸盐剂量或红藻氨酸盐注射及脑电图电极在海马中的位置。与小鼠模型一样,当在红藻氨酸盐注射期间使用麻醉时,只有少数大鼠发生癫痫,尽管SE的严重程度或持续时间不受异氟烷影响。相比之下,当在无麻醉情况下注射红藻氨酸盐时,大多数大鼠发生癫痫。然而,无论红藻氨酸盐注射位置(CA1、CA3)、脑电图记录电极位置(CA1、CA3、齿状回)或注射的红藻氨酸盐剂量如何,大鼠都不会出现小鼠中观察到的频繁脑电图发作。这些数据表明该模型中小鼠和大鼠之间存在显著的表型差异。进一步的研究应探索这种物种差异背后的机制。

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