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氟吡汀在新生缺氧缺血性脑病动物模型中的抗惊厥作用。

Anticonvulsant effect of flupirtine in an animal model of neonatal hypoxic-ischemic encephalopathy.

机构信息

Department of Pediatrics, Division of Neurology, School of Medicine, Translational Epilepsy Research Program, University of Colorado, Anschutz Medical Campus, Aurora, CO 80045, USA.

Department of Pediatrics, Division of Neurology, School of Medicine, Translational Epilepsy Research Program, University of Colorado, Anschutz Medical Campus, Aurora, CO 80045, USA.

出版信息

Neuropharmacology. 2017 Sep 1;123:126-135. doi: 10.1016/j.neuropharm.2017.06.002. Epub 2017 Jun 3.

Abstract

Research studies suggest that neonatal seizures, which are most commonly associated with hypoxic-ischemic injury, may contribute to brain injury and adverse neurologic outcome. Unfortunately, neonatal seizures are often resistant to treatment with current anticonvulsants. In the present study, we evaluated the efficacy of flupirtine, administered at clinically relevant time-points, for the treatment of neonatal seizures in an animal model of hypoxic-ischemic injury that closely replicates features of the human syndrome. We also compared the efficacy of flupirtine to that of phenobarbital, the current first-line drug for neonatal seizures. Flupirtine is a KCNQ potassium channel opener. KCNQ channels play an important role in controlling brain excitability during early development. In this study, hypoxic-ischemic injury was induced in neonatal rats, and synchronized video-EEG records were acquired at various time-points during the experiment to identify seizures. The results revealed that flupirtine, administered either 5 min after the first electroclinical seizure, or following completion of 2 h of hypoxia, i.e., during the immediate reperfusion period, reduced the number of rats with electroclinical seizures, and also the frequency and total duration of electroclinical seizures. Further, daily dosing of flupirtine decreased the seizure burden over 3 days following HI-induction, and modified the natural evolution of acute seizures. Moreover, compared to a therapeutic dose of phenobarbital, which was modestly effective against electroclinical seizures, flupirtine showed greater efficacy. Our results indicate that flupirtine is an extremely effective treatment for neonatal seizures in rats and provide evidence for a trial of this medication in newborn humans.

摘要

研究表明,新生儿癫痫发作最常与缺氧缺血性损伤有关,可能导致脑损伤和不良神经结局。不幸的是,目前的抗癫痫药物通常对新生儿癫痫发作的治疗效果不佳。在本研究中,我们评估了氟比汀在缺氧缺血性损伤动物模型中的治疗效果,该模型非常接近人类综合征的特征,并在临床相关时间点给药。我们还比较了氟比汀与苯巴比妥的疗效,苯巴比妥是目前新生儿癫痫发作的一线药物。氟比汀是一种 KCNQ 钾通道开放剂。KCNQ 通道在早期发育过程中控制大脑兴奋性方面发挥着重要作用。在这项研究中,我们在新生大鼠中诱导缺氧缺血性损伤,并在实验的各个时间点采集同步视频-脑电图记录以识别癫痫发作。结果表明,氟比汀在首次临床电发作后 5 分钟内给药,或在缺氧 2 小时后给药,即在再灌注期立即给药,可减少发生临床电发作的大鼠数量,并降低临床电发作的频率和总持续时间。此外,氟比汀的每日给药可减少 HI 诱导后 3 天内的发作负担,并改变急性发作的自然演变。此外,与治疗剂量的苯巴比妥相比,氟比汀对临床电发作更有效。我们的研究结果表明,氟比汀是治疗大鼠新生儿癫痫发作的一种非常有效的药物,并为在新生儿中试用这种药物提供了证据。

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