小鼠小脑皮质GABA转运蛋白1和3在GABA能突触形成过程中的发育表达

Chitoshi Takayama, Yoshiro Inoue
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引用次数: 48

摘要

γ-氨基丁酸(γ-氨基丁酸,GABA)在脑内GABA能神经元突触外释放,在形态发生、高级功能表达等方面发挥重要作用。在GABA能传递系统中,质膜GABA转运体(GATs)介导成熟脑突触间隙对GABA的摄取,并被认为介导未成熟脑胞浆中GABA的分泌。在本研究中,我们重点研究了小鼠小脑皮层中广泛分布于神经和胶质细胞中的两种gat (GAT-1和GAT-3)。首先,我们检测了GABA在发育中的GABA能神经元的树突和细胞体中的定位,其中GABA在突触外分布,以阐明GABA在突触发生前的分泌。其次,我们研究了GATs定位的发育变化,以揭示gaba摄取系统的发展。未成熟小脑皮层的浦肯野细胞、星状细胞、篮状细胞和高尔基细胞等gaba能神经元的树突和细胞体中均未检测到这两种转运体。出生后第5天(P5)和出生后第7天(P7),在高尔基细胞轴突终末以及星状细胞和篮状细胞的突触前轴突内观察到GAT-1。GAT-3定位于星形胶质细胞突起内,在P10后封闭浦肯野细胞和颗粒层的gaba能突触。这些结果表明gaba -尿在小鼠小脑皮质中不起作用。gat -1的表达早于GAT-3的表达。GAT-1在突触形成过程中开始定位于gaba能轴突末端。当它们封闭突触时,GAT-3开始定位在星形胶质细胞过程中。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Developmental expression of GABA transporter-1 and 3 during formation of the GABAergic synapses in the mouse cerebellar cortex

In the brain, γ-amino butyric acid (GABA), released extrasynaptically and synaptically from GABAergic neurons, plays important roles in morphogenesis, expression of higher functions and so on. In the GABAergic transmission system, plasma membrane GABA transporters (GATs) mediate GABA-uptake from the synaptic cleft in the mature brain and are thought to mediate diacrine of cytosolic GABA in the immature brain. In the present study, we focused on two GATs (GAT-1 and GAT-3) in the mouse cerebellar cortex, which are widely localized in neural and glial cells. Firstly, we examined the localization of GATs in the dendrites and cell bodies of developing GABAergic neurons, where GABA is extrasynaptically distributed, to clarify the GABA-diacrine before synaptogenesis. Secondly, we examined the developmental changes in the localization of GATs to reveal the development of the GABA-uptake system. Neither transporter was detected within the dendrites and cell bodies of GABAergic neurons, including Purkinje, stellate, basket and Golgi cells, in the immature cerebellar cortex. GAT-1 was observed within the Golgi cell axon terminals after postnatal day 5 (P5) and presynaptic axons of stellate and basket cells after P7. GAT-3 was localized within the astrocyte processes, sealing the GABAergic synapses in the Purkinje cell and granular layers after P10. These results indicated that GABA-diacrine did not work in the mouse cerebellar cortex. The onset of GAT-1-expression was prior to that of GAT-3. GAT-1 started to be localized within the GABAergic axon terminals during synapse formation. GAT-3 started to be localized within astrocyte processes when they sealed the synapses.

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