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沙土鼠(长爪沙鼠)前腹侧耳蜗核神经元中氯离子介导的抑制作用的发育。

Development of chloride-mediated inhibition in neurons of the anteroventral cochlear nucleus of gerbil (Meriones unguiculatus).

作者信息

Milenković Ivan, Witte Mirko, Turecek Rostislav, Heinrich Marco, Reinert Thomas, Rübsamen Rudolf

机构信息

Institute of Biology II, Faculty of Biosciences, Pharmacy and Psychology, University of Leipzig, Talstr. 33, D-04103 Leipzig, Germany.

出版信息

J Neurophysiol. 2007 Sep;98(3):1634-44. doi: 10.1152/jn.01150.2006. Epub 2007 Jun 27.

Abstract

At the initial stages in neuronal development, GABAergic and glycinergic neurotransmission exert depolarizing responses, assumed to be of importance for maturation, which in turn shift to hyperpolarizing in early postnatal life due to development of the chloride homeostasis system. Spherical bushy cells (SBC) of the mammalian cochlear nucleus integrate excitatory glutamatergic inputs with inhibitory (GABAergic and glycinergic) inputs to compute signals that contribute to sound localization based on interaural time differences. To provide a fundamental understanding of the properties of GABAergic neurotransmission in mammalian cochlear nucleus, we investigated the reversal potential of the GABA-evoked currents (E GABA) by means of gramicidin-perforated-patch recordings in developing SBC. The action of GABA switches from depolarizing to hyperpolarizing by the postnatal day 7 due to the negative shift in E GABA. Furthermore, we studied the expression pattern of the K+-Cl(-)-extruding cotransporter KCC2, previously shown to induce a switch from neonatal Cl(-) efflux to the mature Cl(-) influx in various neuron types, thereby causing a shift from depolarizing to hyperpolarizing GABA action. The KCC2 protein is expressed in SBC already at birth, yet its activity is attained toward the end of the first postnatal week as indicated by pharmacological inhibition. Interruption of the Cl(-) extrusion by [(dihydroindenyl)oxy] alkanoic acid or furosemide gradually shifted E(GABA) in positive direction with increasing maturity, suggesting that KCC2 could be involved in maintaining low [Cl(-)]i after the postnatal day 7 thereby providing the hyperpolarizing Cl(-)-mediated inhibition in SBC.

摘要

在神经元发育的初始阶段,GABA能和甘氨酸能神经传递产生去极化反应,这被认为对成熟很重要,而由于氯稳态系统的发育,在出生后早期这种反应会转变为超极化。哺乳动物耳蜗核的球形布什细胞(SBC)整合兴奋性谷氨酸能输入与抑制性(GABA能和甘氨酸能)输入,以计算基于双耳时间差有助于声音定位的信号。为了从根本上了解哺乳动物耳蜗核中GABA能神经传递的特性,我们通过在发育中的SBC中进行短杆菌肽穿孔膜片钳记录来研究GABA诱发电流的反转电位(E GABA)。由于E GABA的负向移动,GABA的作用在出生后第7天从去极化转变为超极化。此外,我们研究了K+-Cl(-)外向转运体KCC2的表达模式,先前的研究表明,KCC2能在各种神经元类型中诱导从新生儿期的Cl(-)外流转变为成熟的Cl(-)内流,从而导致GABA作用从去极化转变为超极化。KCC2蛋白在出生时就在SBC中表达,但其活性在出生后第一周结束时才达到,这通过药理学抑制得以表明。用[(二氢茚基)氧基]链烷酸或呋塞米阻断Cl(-)外流会随着成熟度增加使E(GABA)逐渐向正向移动,这表明KCC2可能在出生后第7天之后参与维持低[Cl(-)]i,从而在SBC中提供超极化的Cl(-)介导的抑制作用。

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