首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >Compartmentalized beta subunit distribution determines characteristics and ethanol sensitivity of somatic, dendritic, and terminal large-conductance calcium-activated potassium channels in the rat central nervous system.
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Compartmentalized beta subunit distribution determines characteristics and ethanol sensitivity of somatic, dendritic, and terminal large-conductance calcium-activated potassium channels in the rat central nervous system.

机译:分区的β亚基分布决定了大鼠中枢神经系统中体细胞,树突状细胞和终末大传导钙激活钾通道的特征和乙醇敏感性。

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摘要

Neurons are highly differentiated and polarized cells, whose various functions depend upon the compartmentalization of ion channels. The rat hypothalamic-neurohypophysial system (HNS), in which cell bodies and dendrites reside in the hypothalamus, physically separated from their nerve terminals in the neurohypophysis, provides a particularly powerful preparation in which to study the distribution and regional properties of ion channel proteins. Using electrophysiological and immunohistochemical techniques, we characterized the large-conductance calcium-activated potassium (BK) channel in each of the three primary compartments (soma, dendrite, and terminal) of HNS neurons. We found that dendritic BK channels, in common with somatic channels but in contrast to nerve terminal channels, are insensitive to iberiotoxin. Furthermore, analysis of dendritic BK channel gating kinetics indicates that they, like somatic channels, have fast activation kinetics, in contrast to the slow gating of terminal channels. Dendritic and somatic channels are also more sensitive to calcium and have a greater conductance than terminal channels. Finally, although terminal BK channels are highly potentiated by ethanol, somatic and dendritic channels are insensitive to the drug. The biophysical and pharmacological properties of somatic and dendritic versus nerve terminal channels are consistent with the characteristics of exogenously expressed alphabeta1 versus alphabeta4 channels, respectively. Therefore, one possible explanation for our findings is a selective distribution of auxiliary beta1 subunits to the somatic and dendritic compartments and beta4 to the terminal compartment. This hypothesis is supported immunohistochemically by the appearance of distinct punctate beta1 or beta4 channel clusters in the membrane of somatic and dendritic or nerve terminal compartments, respectively.
机译:神经元是高度分化和极化的细胞,其各种功能取决于离子通道的分隔。大鼠下丘脑神经下垂系统(HNS),其中的细胞体和树突位于下丘脑中,与神经下垂体中的神经末梢物理分离,为研究离子通道蛋白的分布和区域特性提供了特别有力的准备。使用电生理和免疫组化技术,我们表征了HNS神经元的三个主要区室(体,树突和末端)中的每一个的大电导钙激活钾(BK)通道。我们发现树突状的BK通道,与体细胞通道相同,但与神经末梢通道相反,对纤毛毒素不敏感。此外,对树突状BK通道门控动力学的分析表明,与体细胞通道一样,与末端通道的慢门控相反,它们具有快速的激活动力学。与末端通道相比,树突通道和体细胞通道对钙更敏感并且具有更大的电导率。最后,尽管末端BK通道被乙醇高度增强,但体细胞和树突状通道对药物不敏感。体细胞和树突状相对于神经末梢通道的生物物理和药理特性分别与外源表达的alpha1a通道与alpha7a4通道的特征一致。因此,对我们的发现的一种可能的解释是,辅助β1亚基选择性分布于体细胞和树突区室,β4分布于终末区室。免疫组织化学法通过在体细胞和树突状或神经末梢隔室的膜中分别出现不同的点状β1或β4通道簇来支持这一假设。

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