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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Excitatory actions of endogenously released GABA contribute to initiation of ictal epileptiform activity in the developing hippocampus.
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Excitatory actions of endogenously released GABA contribute to initiation of ictal epileptiform activity in the developing hippocampus.

机译:内源性释放的GABA的兴奋作用有助于发育中海马的发作性癫痫样活动。

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摘要

In the developing rat hippocampus, ictal epileptiform activity can be elicited easily in vitro during the first three postnatal weeks. Changes in neuronal ion transport during this time cause the effects of GABA(A) receptor (GABA(A)-R) activation to shift gradually from strongly depolarizing to hyperpolarizing. It is not known whether the depolarizing effects of GABA and the propensity for ictal activity are causally linked. A key question is whether the GABA-mediated depolarization is excitatory, which we defined operationally as being sufficient to trigger action potentials. We assessed the effect of endogenous GABA on ictal activity and neuronal firing rate in hippocampal slices from postnatal day 1 (P1) to P30. In extracellular recordings, there was a strong correlation between the postnatal age at which GABA(A)-R antagonists decreased action potential frequency (P23) and the age at which ictal activity could be induced by elevated potassium (P23). In addition, there was a strong correlation between the fraction of slices in which ictal activity was induced by elevated potassium concentrations and the fractional decrease in action potential firing when GABA(A)-Rs were blocked in the presence of ionotropic glutamate receptor antagonists. Finally, ictal activity induced by elevated potassium was blocked by the GABA(A)-R antagonists bicuculline and SR-95531 (gabazine) and increased in frequency and duration by GABA(A)-R agonists isoguvacine and muscimol. Thus, the propensity of the developing hippocampus for ictal activity is highly correlated with the effect of GABA on action potential probability and reversed by GABA(A) antagonists, indicating that GABA-mediated excitation is causally linked to ictal activity in this developmental window.
机译:在发育中的大鼠海马中,在出生后的前三周可以很容易地在体外诱发发作性癫痫样活动。在此期间神经元离子转运的变化导致GABA(A)受体(GABA(A)-R)激活的作用逐渐从强去极化转变为超极化。尚不清楚GABA的去极化作用与发作的倾向是否因果相关。一个关键问题是GABA介导的去极化是否具有兴奋性,我们在操作中将其定义为足以触发动作电位。我们评估了内源性GABA对从出生后第1天(P1)至P30的海马切片中ictal活性和神经元放电率的影响。在细胞外的记录中,GABA(A)-R拮抗剂降低动作电位频率(P23)的出生后年龄与钾离子升高可诱导发作活性的年龄(P23)之间存在很强的相关性。此外,在钾离子浓度升高的情况下,具有诱动活性的切片比例与在离子型谷氨酸受体拮抗剂的存在下阻断GABA(A)-Rs时动作电位放电的比例降低之间存在很强的相关性。最后,由升高的钾引起的金属活性被GABA(A)-R拮抗剂bicuculline和SR-95531(gabazine)阻断,并且在频率和持续时间方面被GABA(A)-R激动剂异胍卡因和麝香酚增加。因此,发育中的海马对小腿活动的倾向与GABA对动作电位概率的影响高度相关,并被GABA(A)拮抗剂逆转,表明GABA介导的兴奋在此发育窗口中与小腿活动有因果关系。

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