首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Glutamate acting at NMDA receptors stimulates embryonic cortical neuronal migration.
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Glutamate acting at NMDA receptors stimulates embryonic cortical neuronal migration.

机译:作用于NMDA受体的谷氨酸刺激胚胎皮质神经元迁移。

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摘要

During cortical development, embryonic neurons migrate from germinal zones near the ventricle into the cortical plate, where they organize into layers. Mechanisms that direct neuronal migration may include molecules that act as chemoattractants. In rats, GABA, which localizes near the target destination for migrating cortical neurons, stimulates embryonic neuronal migration in vitro. In mice, glutamate is highly localized near the target destinations for migrating cortical neurons. Glutamate-induced migration of murine embryonic cortical cells was evaluated in cell dissociates and cortical slice cultures. In dissociates, the chemotropic effects of glutamate were 10-fold greater than the effects of GABA, demonstrating that for murine cortical cells, glutamate is a more potent chemoattractant than GABA. Thus, cortical chemoattractants appear to differ between species. Micromolar glutamate stimulated neuronal chemotaxis that was mimicked by microM NMDA but not by other ionotropic glutamate receptor agonists (AMPA, kainate, quisqualate). Responding cells were primarily derived from immature cortical regions [ventricular zone (vz)/subventricular zone (svz)]. Bromodeoxyuridine (BrdU) pulse labeling of cortical slices cultured in NMDA antagonists (microM MK801 or APV) revealed that antagonist exposure blocked the migration of BrdU-positive cells from the vz/svz into the cortical plate. PCR confirmed the presence of NMDA receptor expression in vz/svz cells, whereas electrophysiology and Ca2+ imaging demonstrated that vz/svz cells exhibited physiological responses to NMDA. These studies indicate that, in mice, glutamate may serve as a chemoattractant for neurons in the developing cortex, signaling cells to migrate into the cortical plate via NMDA receptor activation.
机译:在皮层发育期间,胚胎神经元从心室附近的生发区迁移到皮层板中,在那里它们组织成层。指导神经元迁移的机制可能包括充当趋化因子的分子。在大鼠中,GABA位于皮层神经元迁移的目标位置附近,它在体外刺激胚胎神经元迁移。在小鼠中,谷氨酸高度定位在目标位置附近,以迁移皮层神经元。在细胞解离和皮质切片培养物中评估了谷氨酸诱导的鼠胚胎皮质细胞的迁移。在解离体中,谷氨酸的趋化作用比GABA的作用大10倍,这表明对于鼠皮层细胞而言,谷氨酸的趋化作用比GABA更强。因此,皮质趋化因子似乎在物种之间有所不同。微摩尔谷氨酸刺激的神经元趋化性,可通过microM NMDA模仿,但其他离子型谷氨酸受体激动剂(AMPA,海藻酸盐,喹喹啉)则没有。响应细胞主要来自未成熟的皮质区域[心室区(vz)/脑室下区(svz)]。在NMDA拮抗剂(microM MK801或APV)中培养的皮质切片的溴脱氧尿嘧啶核苷(BrdU)脉冲标记显示,拮抗剂暴露会阻止BrdU阳性细胞从vz / svz迁移到皮质板中。 PCR证实了vz / svz细胞中NMDA受体表达的存在,而电生理学和Ca2 +成像表明vz / svz细胞表现出对NMDA的生理反应。这些研究表明,在小鼠中,谷氨酸可能充当发育中皮层中神经元的趋化因子,从而指示细胞通过NMDA受体激活而迁移到皮层板中。

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