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首页> 外文期刊>Epilepsia: Journal of the International League against Epilepsy >Drug repurposing for Dravet syndrome in scn1Lab(-/-) mutant zebrafish
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Drug repurposing for Dravet syndrome in scn1Lab(-/-) mutant zebrafish

机译:SCN1LAB( - / - )突变体斑马鱼中DRAVET综合征的药物修复

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Dravet syndrome (DS) is a severe genetic epileptic encephalopathy with onset during the first year of life. Zebrafish models recapitulating human diseases are often used as drug discovery platforms, but also for drug repurposing testing. It was recently shown that pharmacological modulation of three serotonergic (5-HT) receptors (5-HT1D, 5-HT2C, 5-HT2A) exerts antiseizure effects in a zebrafish scn1Lab(-/-) mutant model of DS. Using the zebrafish DS model, our aim was to examine the possibility of repurposing efavirenz (EFA), lisuride (LIS), and rizatriptan (RIZA), marketed medicines with a 5-HT on- or off-target profile, as antiepileptic drugs for DS. To examine whether these compounds have a broader antiseizure profile, they were tested in pentylenetetrazol and ethyl ketopentenoate (EKP) zebrafish models. Pharmacological effects were assessed by locomotor behavior, local field potential brain recordings, and bioluminescence. EFA was active in all models, whereas LIS was selectively active in the zebrafish DS model. Mainly, a poor response was observed to RIZA. Taken together, our preclinical results show that LIS could be a potential candidate for DS treatment. EFA was also active in the EKP model, characterized by a high level of treatment resistance, and hence these data are potentially important for future treatment of drug-resistant epilepsy.
机译:Dravet综合征(DS)是一个严重的遗传癫痫脑病,在生命的第一年期间发病。斑马鱼模型综合人类疾病通常用作药物发现平台,也可以用于药物探测平台。最近表明,三种serotonergic(5-HT)受体(5-HT1D,5-HT2C,5-HT2A)的药理调节在DS的斑马鱼SCN1LAB( - / - )突变模型中施加抗肿瘤作用。使用Zebrafish DS模型,我们的目的是检查重新培养Efaviraz(EFA),Lisuride(LIS)和Rizatriptan(Riza)的可能性,用5-HT或离心目标概况作为抗癫痫药物DS。为了检查这些化合物是否具有更宽的抗血糖型材,它们在五苯甲酸四氢唑和乙基酮烯酸乙醇(EKP)斑马鱼模型中进行测试。通过运动行为,局部场势脑记录和生物发光评估药理效应。 EFA在所有型号中都活跃,而Lis在斑马鱼DS模型中选择性地活跃。主要是,对riza观察到较差的反应。在一起,我们的临床前结果表明,LIS可能是DS治疗的潜在候选者。 EFA在EKP模型中也是活跃的,其特征在于高水平的处理阻力,因此这些数据对于未来治疗耐药性癫痫的治疗可能是重要的。

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