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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Regulation of intracellular Cl- levels by Na(+)-dependent Cl- cotransport distinguishes depolarizing from hyperpolarizing GABAA receptor-mediated responses in spinal neurons.
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Regulation of intracellular Cl- levels by Na(+)-dependent Cl- cotransport distinguishes depolarizing from hyperpolarizing GABAA receptor-mediated responses in spinal neurons.

机译:Na(+)依赖的Cl-共转运对细胞内Cl-水平的调节将脊髓神经元中的去极化与超极化GABAA受体介导的应答区分开。

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Rohon-Beard (RB) spinal neurons of Xenopus larvae are depolarized by GABA. To study the mechanisms underlying this distinctive response, intracellular and patch-clamp recordings were made from RB neurons in situ. The intracellularly recorded GABA reversal potential (EREV) was near -30 mV in normal saline and was approximately 25 mV more negative in Na(+)-free saline. Whole-cell recordings from RB neurons and from neighboring dorsolateral interneurons (DLi) revealed that GABA responses of both cells were mediated by GABAA receptors. Currents elicited by GABA were mimicked by muscimol and reversibly blocked by bicuculline, and EREV shifted with changes in Cl- concentration ([Cl]) in agreement with Cl- selectivity. In perforated patch recordings, EREV for RB cells was significantly more positive than for DLi cells (-38 vs -63 mV), indicating that intact RB cells maintain higher levels of intracellular Cl-. Replacement of external Na+ or exposure to the Cl- transport inhibitor bumetanide (100 microM) shifted RB cell EREV to move negative values, consistent with Na+(-)dependent Cl cotransport contributing to higher internal [Cl]. In contrast, these treatments did not change DLi cell EREV. The results indicate that a Na+(-)dependent Cl- transport mechanism underlies GABAA receptor-mediated depolarizing Cl- conductances in RB neurons. Thus, both inhibitory and excitatory GABA responses appear to be present during the same developmental period in vivo. GABA may stimulate Ca2+ influx in RB neurons because the intracellular GABA EREV is above the threshold for low voltage-activated Ca2+ channels.
机译:非洲爪蟾幼虫的Rohon-Beard(RB)脊髓神经元通过GABA消极化。为了研究这种独特反应的机制,从RB神经元原位制作了细胞内和膜片钳记录。在生理盐水中,细胞内记录的GABA逆转电位(EREV)接近-30 mV,而在无Na(+)的生理盐水中,其负离子大约多25 mV。 RB神经元和邻近背外侧中间神经元(DLi)的全细胞记录表明,两种细胞的GABA反应均由GABAA受体介导。由GABA引发的电流被麝香酚模仿,并被双小分子可逆地阻断,EREV随Cl浓度([Cl])的变化而变化,与Cl选择性一致。在打孔录音中,RB细胞的EREV比DLi细胞的EREV明显更强(-38 vs -63 mV),表明完整的RB细胞保持较高的细胞内Cl-水平。更换外部Na +或暴露于Cl-转运抑制剂布美他尼(100 microM)会使RB细胞EREV移动至负值,这与Na +(-)依赖的Cl共转运一致,从而有助于提高内部[Cl]。相反,这些处理并没有改变DLi细胞EREV。结果表明,Na +(-)依赖性Cl-转运机制是RB神经元中GABAA受体介导的去极化Cl-电导的基础。因此,在体内相同的发育时期似乎同时存在抑制性和兴奋性GABA反应。 GABA可能会刺激RB神经元中的Ca2 +流入,因为细胞内GABA EREV高于低电压激活的Ca2 +通道的阈值。

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