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Excitability of jcBNST Neurons Is Reduced in Alcohol-Dependent Animals during Protracted Alcohol Withdrawal

机译:jcBNsT神经元兴奋持久战酒精戒断过程中减少酒中依赖动物

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摘要

Alcohol dependence and withdrawal has been shown to cause neuroadaptive changes at multiple levels of the nervous system. At the neuron level, adaptations of synaptic connections have been extensively studied in a number of brain areas and accumulating evidence also shows the importance of alcohol dependence-related changes in the intrinsic cellular properties of neurons. At the same time, it is still largely unknown how such neural adaptations impact the firing and integrative properties of neurons. To address these problems, here, we analyze physiological properties of neurons in the bed nucleus of stria terminalis (jcBNST) in animals with a history of alcohol dependence. As a comprehensive approach, first we measure passive and active membrane properties of neurons using conventional current clamp protocols and then analyze their firing responses under the action of simulated synaptic bombardment via dynamic clamp. We find that most physiological properties as measured by DC current injection are barely affected during protracted withdrawal. However, neuronal excitability as measured from firing responses under simulated synaptic inputs with the dynamic clamp is markedly reduced in all 3 types of jcBNST neurons. These results support the importance of studying the effects of alcohol and drugs of abuse on the firing properties of neurons with dynamic clamp protocols designed to bring the neurons into a high conductance state. Since the jcBNST integrates excitatory inputs from the basolateral amygdala (BLA) and cortical inputs from the infralimbic and the insular cortices and in turn is believed to contribute to the inhibitory input to the central nucleus of the amygdala (CeA) the reduced excitability of the jcBNST during protracted withdrawal in alcohol-dependent animals will likely affect ability of the jcBNST to shape the activity and output of the CeA.
机译:酒精依赖和戒断已显示在神经系统的多个层面引起神经适应性改变。在神经元水平上,已经在许多脑区域广泛研究了突触连接的适应性,并且越来越多的证据也表明酒精依赖相关变化对神经元内在细胞特性的重要性。同时,在很大程度上仍不清楚这种神经适应如何影响神经元的放电和整合特性。为了解决这些问题,在这里,我们分析了具有酒精依赖史的动物终末皮层床核(jcBNST)神经元的生理特性。作为一种全面的方法,我们首先使用常规电流钳协议测量神经元的被动和主动膜特性,然后在通过动态钳夹进行的模拟突触轰击作用下分析它们的放电响应。我们发现,长时间停药期间,通过直流电流注入测得的大多数生理特性几乎没有受到影响。但是,在所有3种jcBNST神经元中,用动态钳位从模拟突触输入下的放电反应测量的神经元兴奋性显着降低。这些结果支持使用旨在将神经元带入高电导状态的动态钳位方案研究酒精和滥用药物对神经元放电特性的影响的重要性。由于jcBNST整合了来自基底外侧杏仁核(BLA)的兴奋性输入以及来自下肢和岛状皮质的皮质输入,因此又被认为有助于抑制杏仁核中央核(CeA)的输入,因此jcBNST的兴奋性降低在长期依赖酒精依赖的动物戒断期间,可能会影响jcBNST影响CeA活性和输出的能力。

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