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Fos regulates neuronal activity in the nucleus accumbens.

机译:Fos调节伏隔核中的神经元活动。

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摘要

Repeated exposure to drugs of abuse induces a variety of persistent changes in the brain and the dopamine D1 receptor plays a major role in the process. To understand intracellular mechanisms contributing to cocaine-induced neuroadaptations, we previously examined the role of the immediate early gene Fos using a mouse in which Fos is disrupted primarily in D1 receptor-expressing neurons in the brain. We found that both dendritic remodeling of medium spiny neurons and behavioral sensitization induced by repeated exposure to cocaine are attenuated in the mutant mice. Moreover, the expression of genes encoding several transcription factors, neurotransmitter receptors and intracellular signaling molecules following repeated cocaine administration is altered in the mutant mice compared to that in wild-type mice. In the present study, we have investigated the role of Fos in regulating neuronal excitability at a cellular level and found that medium spiny nucleus accumbens neurons in the mutant mice exhibit increased excitability and attenuated inhibitory responses to stimulation of D1 receptors compared to those in wild-type mice. Our findings suggest that Fos functions in D1 receptor-bearing neurons to regulate neuronal activity which may contribute to the persistence of drug-induced changes.
机译:反复接触滥用药物会引起大脑各种持续变化,而多巴胺D1受体在此过程中起主要作用。为了了解可卡因诱导的神经适应的细胞内机制,我们先前使用了其中Fos主要在大脑中表达D1受体的神经元受到破坏的小鼠中研究了早期早期基因Fos的作用。我们发现,在突变小鼠中,中度棘突神经元的树突状重塑和反复暴露于可卡因引起的行为敏化作用均减弱。此外,与野生型小鼠相比,在重复给予可卡因后,编码几种转录因子,神经递质受体和细胞内信号分子的基因的表达发生了变化。在本研究中,我们研究了Fos在细胞水平上调节神经元兴奋性的作用,发现与野生动物相比,突变小鼠中的伏隔核中伏伏伏核神经元表现出增加的兴奋性和对D1受体刺激的抑制反应减弱。型小鼠。我们的发现表明,Fos在带有D1受体的神经元中起着调节神经元活性的作用,这可能有助于药物诱导的变化的持续存在。

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