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出生后早期小鼠小脑颗粒细胞中氯化钾共转运体2的发育定位及其与突触形成的关系

Developmental localization of potassium chloride co-transporter 2 in granule cells of the early postnatal mouse cerebellum with special reference to the synapse formation.

作者信息

Takayama C, Inoue Y

机构信息

Department of Molecular Neuroanatomy, Hokkaido University School of Medicine, Kita-15 Nishi-7, Kita-Ku, Sapporo 060-8638, Japan.

出版信息

Neuroscience. 2006 Dec;143(3):757-67. doi: 10.1016/j.neuroscience.2006.08.044. Epub 2006 Sep 27.

Abstract

In the adult CNS, GABA is the predominant inhibitory neurotransmitter, mediating the hyperpolarization of membrane potential and regulating the glutamatergic activity. In the immature CNS, on the other hand, GABA mediates depolarization and is involved in controlling morphogenesis. This developmental shift in GABA actions from depolarization to hyperpolarization occurs as a result of decreasing the intracellular chloride ion (Cl(-)) concentration (Cl(-)) which is regulated by the potassium (K(+))-Cl(-) co-transporter 2 (KCC2). To clarify the time-course of changes in the GABA actions during development, we examined the developmental localization of the KCC2 in the granule cells of the postnatal mouse cerebellum using specific antibodies against KCC2. The granule cell precursors and migrating granule cells were devoid of immunoreactivity against KCC2 antibodies. At postnatal day 3 (P3), the KCC2-immunolabeling was negative in the internal granular layer, although synaptophysin-positive mossy fiber terminals were detected. At P5, we first detected the KCC2-immunolabeling at the somata of granule cells and their dendrites before granule cells received inhibitory input from Golgi cells. Almost all KCC2-positive dendrites (more than 98%) attached to and formed synapses with mossy fiber terminals. As development proceeded, the number of KCC2-positive granule cells increased, and all granule cells became positive by P21. These results suggested that GABAergic transmission on granule cells might shift from excitation to inhibition after the synapse formation, and the excitatory synapse-formation and related factors might be the triggers for the expression and localization of the KCC2 in the granule cells. Furthermore, it was also suggested that formation of the GABAergic synapses and GABAergic transmission were not necessary for the KCC2-expression in the mouse cerebellar granule cells in vivo.

摘要

在成体中枢神经系统中,γ-氨基丁酸(GABA)是主要的抑制性神经递质,介导膜电位的超极化并调节谷氨酸能活性。另一方面,在未成熟的中枢神经系统中,GABA介导去极化并参与控制形态发生。GABA作用从去极化到超极化的这种发育转变是由于细胞内氯离子(Cl⁻)浓度([Cl⁻]i)降低所致,而这是由钾(K⁺)-氯(Cl⁻)共转运体2(KCC2)调节的。为了阐明发育过程中GABA作用变化的时间进程,我们使用针对KCC2的特异性抗体,研究了出生后小鼠小脑颗粒细胞中KCC2的发育定位。颗粒细胞前体和迁移的颗粒细胞对KCC2抗体无免疫反应性。在出生后第3天(P3),尽管检测到突触素阳性的苔藓纤维终末,但内颗粒层中的KCC2免疫标记为阴性。在P5时,我们首先在颗粒细胞的胞体及其树突上检测到KCC2免疫标记,此时颗粒细胞尚未接受来自高尔基细胞的抑制性输入。几乎所有KCC2阳性树突(超过98%)都与苔藓纤维终末附着并形成突触。随着发育的进行,KCC2阳性颗粒细胞的数量增加,到P21时所有颗粒细胞都变为阳性。这些结果表明,颗粒细胞上的GABA能传递可能在突触形成后从兴奋转变为抑制,并且兴奋性突触形成及相关因素可能是颗粒细胞中KCC2表达和定位的触发因素。此外,还表明在体内小鼠小脑颗粒细胞中,GABA能突触的形成和GABA能传递对于KCC2的表达并非必需。

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