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出生时,GAT-1在限制大鼠CA3锥体神经元中的强直性GABA(A)电流方面发挥作用。

GAT-1 acts to limit a tonic GABA(A) current in rat CA3 pyramidal neurons at birth.

作者信息

Sipilä Sampsa T, Voipio Juha, Kaila Kai

机构信息

Department of Biological and Environmental Sciences, University of Helsinki, FIN-00014 Helsinki, Finland.

出版信息

Eur J Neurosci. 2007 Feb;25(3):717-22. doi: 10.1111/j.1460-9568.2007.05342.x. Epub 2007 Feb 12.

Abstract

Tonic activation of GABA(A) receptors takes place before the development of functional synapses in cortical structures. We studied whether inefficient GABA uptake might explain the presence of a tonic GABA(A)-mediated current (I(GABA-A)) in early postnatal hippocampal pyramidal neurons. The data show, however, that the tonic I(GABA-A) is enhanced by the specific blocker of GABA transporter-1 (GAT-1), NO-711 (1-[2-[[(Diphenylmethyleneimino]oxy]ethyl]-1,2,5,6-tetrahydro-3-pyridinecarboxylic acid hydrochloride), at birth in rat CA3 pyramidal neurons. NO-711 also prolonged the duration of GABA transients during endogenous hippocampal network events (known as giant depolarizing potentials) at postnatal day 0. The endogenous tonic I(GABA-A) was seen and it was enhanced by NO-711 in the presence of tetrodotoxin, which itself had only a minor effect on the holding current under control conditions. This indicates that the source of interstitial GABA is largely independent of action-potential activity. The tonic I(GABA-A) in neonatal CA3 pyramidal neurons was increased by zolpidem, indicating that at least a proportion of the underlying GABA(A) receptors contain gamma2 and alpha1-alpha3 subunits. The present data point to a significant role for GAT-1 in the control of the excitability of immature hippocampal neurons and networks.

摘要

GABA(A)受体的紧张性激活发生在皮质结构中功能性突触形成之前。我们研究了GABA摄取效率低下是否可以解释出生后早期海马锥体神经元中紧张性GABA(A)介导电流(I(GABA-A))的存在。然而,数据显示,在大鼠CA3锥体神经元出生时,GABA转运体-1(GAT-1)的特异性阻滞剂NO-711(1-[2-[[(二苯基亚甲基亚氨基]氧基]乙基]-1,2,5,6-四氢-3-吡啶羧酸盐酸盐)增强了紧张性I(GABA-A)。在出生后第0天,NO-711还延长了内源性海马网络事件(称为巨大去极化电位)期间GABA瞬变的持续时间。在内源性紧张性I(GABA-A)存在的情况下,在河豚毒素存在时可见到它并被NO-711增强,而河豚毒素本身在对照条件下对钳制电流只有轻微影响。这表明间质GABA的来源在很大程度上独立于动作电位活动。新生CA3锥体神经元中的紧张性I(GABA-A)被唑吡坦增加,这表明至少一部分潜在的GABA(A)受体含有γ2和α1-α3亚基。目前的数据表明GAT-1在控制未成熟海马神经元和网络的兴奋性方面具有重要作用。

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