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首页> 外文期刊>Molecular brain >Dopamine D1 receptor-mediated NMDA receptor insertion depends on Fyn but not Src kinase pathway in prefrontal cortical neurons
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Dopamine D1 receptor-mediated NMDA receptor insertion depends on Fyn but not Src kinase pathway in prefrontal cortical neurons

机译:多巴胺D1受体介导的NMDA受体的插入取决于前额叶皮层神经元中的Fyn,而不取决于Src激酶途径

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Background Interactions between dopamine and glutamate in the prefrontal cortex are essential for cognitive functions such as working memory. Modulation of N-methyl-D-aspartic acid (NMDA) receptor functions by dopamine D1 receptor is believed to play a critical role in these functions. The aim of the work reported here is to explore the signaling pathway underlying D1 receptor-mediated trafficking of NMDA receptors in cultured rat prefrontal cortical neurons. Results Activation of D1 receptor by selective agonist SKF-81297 significantly increased the expression of NR2B subunits. This effect was completely blocked by small interfering RNA knockdown of Fyn, but not Src. Under control conditions, neither Fyn nor Src knockdown exhibited significant effect on basal NR2B expression. D1 stimulation significantly enhanced NR2B insertion into plasma membrane in cultured PFC neurons, a process obstructed by Fyn, but not Src, knockdown. Conclusions Dopamine D1 receptor-mediated increase of NMDA receptors is thus Fyn kinase dependent. Targeting this signaling pathway may be useful in treating drug addiction and schizophrenia.
机译:背景前额叶皮层中多巴胺和谷氨酸之间的相互作用对于认知功能(例如工作记忆)至关重要。据信,多巴胺D1受体对N-甲基-D-天冬氨酸(NMDA)受体功能的调节在这些功能中起关键作用。本文报道的工作目的是探讨在培养的大鼠前额叶皮层神经元中D1受体介导的NMDA受体转运的信号通路。结果选择性激动剂SKF-81297对D1受体的激活显着增加了NR2B亚基的表达。 Fyn的小分子干扰RNA敲低完全阻止了该作用,但Src却没有。在对照条件下,Fyn和Src敲低均未显示出对基础NR2B表达的显着影响。 D1刺激显着增强了NR2B插入培养的PFC神经元的质膜中,这一过程受Fyn(而非Src)敲低的阻碍。结论多巴胺D1受体介导的NMDA受体增加是Fyn激酶依赖性的。靶向该信号传导途径可用于治疗药物成瘾和精神分裂症。

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