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N-丙戊酰-L-色氨酸对大鼠脑片高钾、低钙、低镁诱导的 CA1 海马癫痫样爆发活动的抑制作用。

Inhibitory effects of N-valproyl-L-tryptophan on high potassium, low calcium and low magnesium-induced CA1 hippocampal epileptiform bursting activity in rat brain slices.

机构信息

Dipartimento di Biomedicina Sperimentale e Neuroscienze Cliniche, Sezione di Fisiologia umana "G. Pagano", Università degli Studi di Palermo, Corso Tukory 129, 90134 Palermo, Italy.

出版信息

J Neural Transm (Vienna). 2012 Nov;119(11):1249-59. doi: 10.1007/s00702-012-0814-y. Epub 2012 May 10.

Abstract

N-valproyl-L-tryptophan (VPA-Tryp), new antiepileptic drug, was tested on CA1 hippocampal epileptiform bursting activity obtained by increasing potassium and lowering calcium and magnesium concentrations in the fluid perfusing rat brain slices. Each slice was treated with a single concentration (0.2, 0.5, 1 or 2 mM) of Valproate (VPA) or VPA-Tryp. Both burst duration and interburst frequency during and after treatment were off-line compared with baseline values. For both parameters, the latency and the length of statistically significant response periods as well as the magnitude of drug-induced responses were calculated. VPA-Tryp evoked fewer and weaker early excitatory effects than VPA on bursting activity. On the contrary, VPA-Tryp induced powerful and long-lasting inhibitory effects on epileptiform discharge in a significantly higher number of slices than VPA. In fact, greater length and magnitude of VPA-Tryp-induced inhibition on both interburst frequency and burst duration were observed. Furthermore, VPA-Tryp showed antiepileptic activity at lower concentration than VPA and, when testing both drugs at analogue concentrations, VPA-Tryp evoked responses with either shorter latency or greater effect length and magnitude than VPA.

摘要

N-丙戊酰基-L-色氨酸(VPA-Tryp)是一种新型抗癫痫药物,我们在灌流大鼠脑片的液中增加钾浓度和降低钙镁浓度以获得 CA1 海马癫痫样爆发活动,并对此进行了测试。每个脑片用单一浓度(0.2、0.5、1 或 2 mM)的丙戊酸钠(VPA)或 VPA-Tryp 处理。在处理过程中和处理后,比较基线值离线分析爆发持续时间和爆发间期频率。对于这两个参数,计算潜伏期和统计学上显著反应期的长度以及药物诱导反应的幅度。VPA-Tryp 对爆发活动的早期兴奋性影响比 VPA 少且弱。相反,VPA-Tryp 引起的癫痫样放电的抑制作用强且持续时间长,且在显著更多的脑片中观察到这种作用。事实上,VPA-Tryp 引起的爆发间期频率和爆发持续时间的抑制作用在长度和幅度上都更大。此外,VPA-Tryp 在较低浓度下就显示出抗癫痫活性,并且当以类似浓度测试两种药物时,VPA-Tryp 诱导的反应具有较短的潜伏期或更大的效应长度和幅度。

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