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Effect of Early Glutamate Exposure on EAAT-3 and GAT-1 Protein Expression in Cells of the Dentate Gyrus and CA1 Region of the Adult Rat Hippocampus

机译:早期谷氨酸暴露对成年大鼠海马齿状回和CA1区细胞EAAT-3和GAT-1蛋白表达的影响

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Background and Aims: Glutamate and GABA transporters are cell surface proteins localized on neurons and glial cells that mediate the reuptake of glutamate and GABA from the extracellular space. In different models of the acquisition of epilepsy, important changes in the expression of these transporters have been demonstrated, although to date no such studies have been performed using the monosodium glutamate (MSG)-induced seizure model in neonatal rats. Methods: Following repeated MSG administration, we used immunofluorescence techniques to quantify the number of cells expressing the EAAT-3 and GAT-1 transporters at postnatal days (PD) 14 and 60 in the dentate gyrus (DG) and CA1 region of the hippocampus. Results: EAAT-3 and GAT-1 were expressed around the soma of granular cells and in the soma and dendrites of pyramidal cells in both experimental (MSG) and control (NaCl) rats. In the DG, MSG administration significantly increased the number of granular cells double-labelled for EAAT-3/Neun at PD 60 but not PD 14. No significant changes were observed at either PD 14 or 60 in terms of the number of cells expressing GAT-1 in the DG or CA1. Conclusions: The findings suggest that the selective long-term increase in EAAT-3 expression in granular cells following neonatal MSG treatment reflects an important compensatory or protective response to the excitotoxic and seizure-promoting effects of early glutamate exposure in adult animals.
机译:背景与目的:谷氨酸和GABA转运蛋白是位于神经元和神经胶质细胞上的细胞表面蛋白,介导谷氨酸和GABA从细胞外空间的再摄取。在癫痫发作的不同模型中,已证明这些转运蛋白的表达发生了重要变化,尽管迄今为止,尚未使用谷氨酸一钠(MSG)诱导的新生大鼠癫痫发作模型进行此类研究。方法:在重复施用MSG之后,我们使用免疫荧光技术来量化海马齿状回(DG)和CA1区在出生后第14天和第60天表达EAAT-3和GAT-1转运蛋白的细胞数量。结果:在实验(MSG)和对照(NaCl)大鼠中,EAAT-3和GAT-1在颗粒细胞的体细胞周围以及锥体细胞的体细胞和树突中表达。在DG中,MSG给药显着增加了PD 60而不是PD 14双重标记为EAAT-3 / Neun的粒状细胞的数量,在PD 14或60处未观察到表达GAT的细胞数量的显着变化在DG或CA1中为-1。结论:研究结果表明,新生儿味精治疗后,颗粒细胞中EAAT-3表达的选择性长期增加反映了对成年动物早期谷氨酸暴露的兴奋性毒性和癫痫发作促进作用的重要补偿或保护性反应。

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