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首页> 美国卫生研究院文献>other >Prolonged withdrawal from cocaine self-administration affects prefrontal cortex- and basolateral amygdala-nucleus accumbens core circuits but not accumbens GABAergic local interneurons
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Prolonged withdrawal from cocaine self-administration affects prefrontal cortex- and basolateral amygdala-nucleus accumbens core circuits but not accumbens GABAergic local interneurons

机译:长期退出可卡因自我管理会影响伏隔前核心皮层和基底外侧杏仁核-伏隔核核心回路但伏隔不会影响GABA能性局部中间神经元

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Withdrawal from extended-access cocaine self-administration leads to progressive intensification (‘incubation’) of cocaine craving. After prolonged withdrawal (1–2 months), when craving is high, expression of incubation depends on strengthening of excitatory inputs to medium spiny neurons (MSN) of the nucleus accumbens (NAc). These excitatory inputs interact with the intra-NAc GABAergic ‘microcircuit’, composed of MSN axon collaterals and GABAergic interneurons. Here, we investigated whether the increased glutamatergic neurotransmission observed after prolonged withdrawal is accompanied by altered GABAergic neurotransmission, focusing on NAc core. Rats self-administered cocaine or saline (6 h/day) and then underwent >40 days of withdrawal. First, we investigated parvalbumin positive (PV+) interneurons, GABAergic fast-spiking interneurons that regulate MSN activity. Immunohistochemical studies revealed no significant change in PV signal intensity or the number of PV+ cells in cocaine rats versus saline controls. We then screened PV and other interneuron markers using immunoblotting. We detected no changes in levels of PV, calretinin, calbindin, or neuronal nitric oxide synthase. Since expression of these markers is activity-dependent, our results suggest no marked changes in interneuron activity. Finally, we utilized local field potential recording, which can detect GABA-mediated alterations at the circuit level, to investigate potential changes in two circuits implicated in cocaine craving: prelimbic prefrontal cortex to NAc core and basolateral amygdala to NAc core. We detected differential adaptations in these circuits, some of which may involve GABA. Overall, our results suggest that alterations in GABA transmission may accompany incubation of cocaine craving, but they are circuit-specific and less pronounced than alterations in glutamate transmission.
机译:可卡因自我管理的退出使人们对可卡因的渴望逐渐增强(“孵化”)。在长期戒断(1-2个月)后,当渴望很高时,孵育的表达取决于对伏伏核(NAc)的中棘神经元(MSN)的兴奋性输入的增强。这些兴奋性输入与由MSN轴突侧支和GABA能中神经元组成的NAc内GABA能“微电路”相互作用。在这里,我们调查了长期停药后观察到的增加的谷氨酸能神经传递是否伴有改变的GABA能神经传递,重点是NAc核心。大鼠自行服用可卡因或生理盐水(每天6小时),然后停药> 40天。首先,我们研究了小白蛋白阳性(PV +)中枢神经元,即调节MSN活性的GABA能快速加标中枢神经元。免疫组织化学研究显示,与盐水对照组相比,可卡因大鼠的PV信号强度或PV +细胞数量没有显着变化。然后,我们使用免疫印迹筛选了PV和其他中间神经元标记。我们没有检测到PV,钙调蛋白,钙结合蛋白或神经元一氧化氮合酶水平的变化。由于这些标志物的表达是活性依赖性的,因此我们的结果表明中间神经元活性没有明显变化。最后,我们利用局部场电势记录来检测电路中GABA介导的改变,以调查涉及可卡因渴望的两个电路的电势变化:前缘前额叶皮层至NAc核心和基底外侧杏仁核至NAc核心。我们在这些电路中检测到差分自适应,其中一些可能涉及GABA。总体而言,我们的结果表明,可卡因渴望的孵化可能伴随着GABA传递的改变,但它们具有电路特异性,且不如谷氨酸传递改变那么明显。

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