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寻找药物难治性癫痫的新筛查模型:在癫痫啮齿动物中诱发急性癫痫发作是一种合适的方法吗?

The Search for New Screening Models of Pharmacoresistant Epilepsy: Is Induction of Acute Seizures in Epileptic Rodents a Suitable Approach?

作者信息

Löscher Wolfgang

机构信息

Department of Pharmacology, Toxicology and Pharmacy, Center for Systems Neuroscience, University of Veterinary Medicine, Bünteweg 17, 30559, Hannover, Germany.

出版信息

Neurochem Res. 2017 Jul;42(7):1926-1938. doi: 10.1007/s11064-016-2025-7. Epub 2016 Aug 8.

Abstract

Epilepsy, a prevalent neurological disease characterized by spontaneous recurrent seizures (SRS), is often refractory to treatment with anti-seizure drugs (ASDs), so that more effective ASDs are urgently needed. For this purpose, it would be important to develop, validate, and implement new animal models of pharmacoresistant epilepsy into drug discovery. Several chronic animal models with difficult-to-treat SRS do exist; however, most of these models are not suited for drug screening, because drug testing on SRS necessitates laborious video-EEG seizure monitoring. More recently, it was proposed that, instead of monitoring SRS, chemical or electrical induction of acute seizures in epileptic rodents may be used as a surrogate for testing the efficacy of novel ASDs against refractory SRS. Indeed, several ASDs were shown to lose their efficacy on acute seizures, when such seizures were induced by pentylenetetrazole (PTZ) in epileptic rather than nonepileptic rats, whereas this was not observed when using the maximal electroshock seizure test. Subsequent studies confirmed the loss of anti-seizure efficacy of valproate against PTZ-induced seizures in epileptic mice, but several other ASDs were more potent against PTZ in epileptic than nonepileptic mice. This was also observed when using the 6-Hz model of partial seizures in epileptic mice, in which the potency of levetiracetam, in particular, was markedly increased compared to nonepileptic animals. Overall, these observations suggest that performing acute seizure tests in epileptic rodents provides valuable information on the pharmacological profile of ASDs, in particular those with mechanisms inherent to disease-induced brain alterations. However, it appears that further work is needed to define optimal approaches for acute seizure induction and generation of epileptic/drug refractory animals that would permit reliable screening of new ASDs with improved potential to provide seizure control in patients with pharmacoresistant epilepsy.

摘要

癫痫是一种以自发性反复发作为特征的常见神经系统疾病,通常对抗癫痫药物(ASD)治疗具有耐药性,因此迫切需要更有效的ASD。为此,开发、验证并将新的药物难治性癫痫动物模型应用于药物研发至关重要。确实存在几种具有难以治疗的自发性反复发作的慢性动物模型;然而,这些模型大多不适合药物筛选,因为对自发性反复发作进行药物测试需要费力的视频脑电图癫痫监测。最近有人提出,代替监测自发性反复发作,在癫痫啮齿动物中化学或电诱导急性发作可作为测试新型ASD对抗难治性自发性反复发作疗效的替代方法。事实上,当癫痫大鼠而非非癫痫大鼠中由戊四氮(PTZ)诱导急性发作时,几种ASD对急性发作失去了疗效,而在使用最大电休克惊厥试验时未观察到这种情况。随后的研究证实丙戊酸对癫痫小鼠中PTZ诱导的发作失去了抗惊厥疗效,但其他几种ASD在癫痫小鼠中对PTZ的作用比对非癫痫小鼠更强。在癫痫小鼠的部分发作6-Hz模型中也观察到了这种情况,其中特别是左乙拉西坦的效力与非癫痫动物相比明显增加。总体而言,这些观察结果表明在癫痫啮齿动物中进行急性发作试验可提供有关ASD药理学特征的有价值信息,特别是那些具有疾病诱导的脑改变固有机制的ASD。然而,似乎需要进一步开展工作来确定急性发作诱导和癫痫/药物难治性动物生成的最佳方法,这将允许可靠地筛选具有更好潜力以控制药物难治性癫痫患者发作的新型ASD。

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