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首页> 外文期刊>Trends in Neurosciences >D1 and D2 dopamine-receptor modulation of striatal glutamatergic signaling in striatal medium spiny neurons.
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D1 and D2 dopamine-receptor modulation of striatal glutamatergic signaling in striatal medium spiny neurons.

机译:纹状体中等棘神经元中纹状体谷氨酸能信号传导的D1和D2多巴胺受体调节。

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摘要

Dopamine shapes a wide variety of psychomotor functions. This is mainly accomplished by modulating cortical and thalamic glutamatergic signals impinging upon principal medium spiny neurons (MSNs) of the striatum. Several lines of evidence suggest that dopamine D1 receptor signaling enhances dendritic excitability and glutamatergic signaling in striatonigral MSNs, whereas D2 receptor signaling exerts the opposite effect in striatopallidal MSNs. The functional antagonism between these two major striatal dopamine receptors extends to the regulation of synaptic plasticity. Recent studies, using transgenic mice in which cells express D1 and D2 receptors, have uncovered unappreciated differences between MSNs that shape glutamatergic signaling and the influence of DA on synaptic plasticity. These studies have also shown that long-term alterations in dopamine signaling produce profound and cell-type-specific reshaping of corticostriatal connectivity and function.
机译:多巴胺可塑造多种精神运动功能。这主要是通过调节皮层和丘脑的谷氨酸能信号来实现的,该信号撞击在纹状体的主要中棘神经元上。几条证据表明,多巴胺D1受体信号传导增强了纹状体MSN中的树突兴奋性和谷氨酸能信号传导,而D2受体信号传导对纹状体最高MSN具有相反的作用。这两个主要的纹状体多巴胺受体之间的功能拮抗作用扩展到突触可塑性的调节。使用细胞表达D1和D2受体的转基因小鼠的最新研究发现,形成谷氨酸能信号传导的MSN和DA对突触可塑性的影响之间未发现明显差异。这些研究还表明,多巴胺信号转导的长期改变会产生深刻的和特定于细胞类型的皮质骨连接性和功能重塑。

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