首页> 外文期刊>The European Journal of Neuroscience >Induction of neonatal sodium channel II and III alpha-isoform mRNAs in neurons and microglia after status epilepticus in the rat hippocampus.
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Induction of neonatal sodium channel II and III alpha-isoform mRNAs in neurons and microglia after status epilepticus in the rat hippocampus.

机译:癫痫持续状态在大鼠海马体中诱导神经元和小胶质细胞新生钠通道II和IIIα-亚型mRNA的表达。

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摘要

Sodium channels (NaChs) regulate neuronal excitability in both physiological and pathological conditions, including epilepsy and are therefore an important target for antiepileptic drugs. In the present study, we examined the distribution of mRNAs encoding neonatal NaChs II and III alpha-isoforms in control rat hippocampus and after electrically-induced status epilepticus (SE), using nonradioactive in situ hybridization (ISH). Only weak expression of neonatal NaCh II and III mRNAs was observed in control hippocampus. By contrast, increased expression of neonatal NaCh II and III mRNAs was observed 4 h after the induction of SE in neurons of CA1-CA3 and the dentate granule cell layer. These changes were detected only in rats in which SE was successfully induced and persisted, although less intense, for up to 3 months, when rats display spontaneous seizures. Strong expression of neonatal NaCh alpha-isoforms was observed 1 week after SE in microglial cells, as confirmed by double labelling, combining ISH with immunocytochemistry for microglia markers. The increased expression of neonatal isoforms of the NaCh in both neurons and microglial cells may represent a critical mechanism for modulation of neuronal excitability, glial function and pharmacological response to antiepileptic drugs in the course of epileptogenesis.
机译:钠通道(NaChs)在生理和病理条件(包括癫痫)中调节神经元兴奋性,因此是抗癫痫药的重要靶标。在本研究中,我们使用非放射性原位杂交(ISH)研究了在对照大鼠海马中和电诱发的癫痫持续状态(SE)后编码新生NaChs II和IIIα-亚型的mRNA的分布。在对照海马中仅观察到新生儿NaCh II和III mRNA的弱表达。相反,在CA1-CA3神经元和齿状颗粒细胞层中SE诱导后4小时,观察到新生NaCh II和III mRNA的表达增加。仅在成功诱发SE并持续SE的大鼠中检测到这些变化,尽管SE强度较低,但在大鼠表现出自发性癫痫发作后长达3个月。 SE后1周,在小胶质细胞中观察到新生NaChα-亚型的强表达,这是通过双重标记证实的,将ISH与免疫细胞化学结合用于小胶质细胞标记。在神经元和小胶质细胞中,NaCh的新生儿同工型的表达增加可能代表了在癫痫发生过程中调节神经元兴奋性,神经胶质功能和对抗癫痫药药理反应的关键机制。

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