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首页> 外文期刊>Brain research >Early developmental alterations of low-Mg2+ -induced epileptiform activity in the intact corticohippocampal formation of the newborn mouse in vitro.
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Early developmental alterations of low-Mg2+ -induced epileptiform activity in the intact corticohippocampal formation of the newborn mouse in vitro.

机译:低Mg2 +诱发的癫痫样活动在早期新生小鼠的完整皮质海马体形成中的早期发育变化。

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The generation, propagation and pharmacological properties of low-Mg2+ -induced epileptiform activity were examined in the intact corticohippocampal formation (CHF) of the newborn (P0-4) mouse in vitro. Multi-site field potential recordings in dentate gyrus (DG), CA3, CA1, entorhinal cortex (EC) and temporal cortex (TC) revealed in 0.2 mM Mg2+ -containing ACSF a stable pattern of spontaneous epileptiform activity consisting of recurrent ictal-like events (ILEs) and interictal events (IEs). Although this activity could be consistently observed as early as P0, ILEs were smaller in amplitude, less frequent and showed a slower onset in P0-2 as compared to P3-4 animals. In all age groups, epileptiform events were largest in CA3 and smallest in EC and TC. A specific pacemaker region could not be identified since ILEs appeared simultaneously at all recording sites. Reducing the extracellular Mg2+ concentration to 0.1 mM or nominally zero caused an increase in ILE frequency. Pharmacological studies in the P3-4 age group with 0.2 mM Mg2+ revealed a complete blockade of the ILEs by an NMDA receptor antagonist and a pronounced suppression of epileptiform activity by an AMPA/kainate antagonist. Application of a GABA-A receptor antagonist induced repetitive bursts of interictal discharges, which persisted for at least 1.5 h after washout of the antagonist. Our data demonstrate that the intact CHF in vitro preparation of the newborn mouse offers a most valuable model to study epileptiform activity in the immature limbic system.
机译:在体外(P0-4)小鼠的完整皮质海马体形成(CHF)中检查了低Mg2 +诱导的癫痫样活性的产生,繁殖和药理特性。齿状回(DG),CA3,CA1,内嗅皮层(EC)和颞皮层(TC)中的多位场电势记录显示,在含0.2 mM Mg2 +的ACSF中,稳定的自发性癫痫样活动模式由反复发作的发作样事件组成(ILE)和发作间事件(IE)。尽管可以早在P0观察到这种活性,但与P3-4动物相比,ILE的振幅较小,频率较低且在P0-2中起病较慢。在所有年龄组中,癫痫样事件在CA3中最大,在EC和TC中最小。由于ILE同时出现在所有记录位置,因此无法确定特定的起搏器区域。将细胞外Mg2 +浓度降低至0.1 mM或名义上为零会导致ILE频率增加。在P3-4年龄组中使用0.2 mM Mg2 +的药理研究表明,NMDA受体拮抗剂可完全阻断ILE,而AMPA /海藻酸酯拮抗剂可显着抑制癫痫样活性。 GABA-A受体拮抗剂的应用引起了反复发作的室间隔放电,该持续时间至少在拮抗剂冲洗后持续1.5 h。我们的数据表明,新生小鼠的完整CHF体外制备为研究未成熟边缘系统中的癫痫样活动提供了最有价值的模型。

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