首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Effects of status epilepticus on hippocampal GABAA receptors are age-dependent.
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Effects of status epilepticus on hippocampal GABAA receptors are age-dependent.

机译:癫痫持续状态对海马GABAA受体的影响是年龄依赖性的。

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摘要

Long-term GABA(A) receptor alterations occur in hippocampal dentate granule neurons of rats that develop epilepsy after status epilepticus in adulthood. Hippocampal GABA(A) receptor expression undergoes marked reorganization during the postnatal period, however, and the effects of neonatal status epilepticus on subsequent GABA(A) receptor development are unknown. In the current study, we utilize single cell electrophysiology and antisense mRNA amplification to determine the effect of status-epilepticus induced by lithium-pilocarpine in postnatal day 10 rat pups on GABA(A) receptor subunit expression and function in hippocampal dentate granule neurons. We find that rats subjected to lithium-pilocarpine-induced status epilepticus at postnatal day 10 show long-term GABA(A) receptor changes including a two-fold increase in alpha1 subunit expression (compared with lithium-injected controls) and enhanced type I benzodiazepine augmentation that are opposite of those seen after status epilepticus in adulthood and may serve to enhance dentate gyrus inhibition. Further, unlike adult rats, postnatal day 10 rats subjected to status epilepticus do not become epileptic. These findings suggest age-dependent differences in the effects of status epilepticus on hippocampal GABA(A) receptors that could contribute to the selective resistance of the immature brain to epileptogenesis.
机译:长期GABA(A)受体改变发生在成年癫痫持续状态后癫痫发作的大鼠海马齿状颗粒神经元中。在出生后,海马GABA(A)受体的表达经历了明显的重组,但是,新生儿癫痫持续状态对随后的GABA(A)受体发育的影响尚不清楚。在本研究中,我们利用单细胞电生理学和反义mRNA扩增来确定锂-毛果芸香碱在出生后第10天的幼鼠中对海马齿状颗粒神经元GABA(A)受体亚基表达和功能的影响。我们发现大鼠在出生后第10天接受锂-毛果芸香碱引起的癫痫持续状态显示长期GABA(A)受体变化,包括alpha1亚基表达增加两倍(与注射锂的对照相比)和I型苯并二氮杂增强增强与成年后癫痫持续状态相反,可能有助于增强齿状回的抑制。另外,与成年大鼠不同,遭受癫痫持续状态的出生后第10天的大鼠不会变得癫痫。这些发现表明,癫痫持续状态对海马GABA(A)受体影响的年龄依赖性差异可能会导致未成熟大脑对癫痫发生的选择性抵抗。

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