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首页> 外文期刊>Trends in Neurosciences >The neural-glial purinergic receptor ensemble in chronic pain states.
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The neural-glial purinergic receptor ensemble in chronic pain states.

机译:慢性疼痛状态下的神经胶质嘌呤受体结合体。

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Chronic pain is characterized by enhanced sensory neurotransmission that underlies increased sensitivity to noxious stimuli and the perception of non-noxious stimuli as painful. Evidence from neurophysiological and pharmacological studies demonstrates that ATP produces pain by directly enhancing neuronal excitability via the activation of specific ligand-gated ion channels, the P2X3 and P2X2/3 receptors. In addition, ATP activates CNS glial cells (e.g. microglia) in response to persistent nociceptive stimulation. This latter effect involves several distinct receptor-mediated signaling pathways linked to the P2X4, P2X7 and P2Y(12) receptors. This review summarizes new data that places these purinergic signaling events in a mechanistic context that illustrates the ability of ATP to initiate and maintain states of heightened sensory neuron excitability associated with persistent pain.
机译:慢性疼痛的特征是感觉神经传递增强,其基础是对有害刺激物的敏感性增加以及对非有害刺激物的疼痛感。神经生理学和药理学研究的证据表明,ATP通过激活特定的配体门控离子通道,P2X3和P2X2 / 3受体直接增强神经元兴奋性而产生疼痛。另外,ATP响应于持续伤害感受刺激而激活CNS神经胶质细胞(例如小胶质细胞)。后一种效应涉及与P2X4,P2X7和P2Y(12)受体相关的几种不同的受体介导的信号通路。这篇综述总结了将这些嘌呤能信号转导事件置于机械背景下的新数据,这些数据说明了ATP启动和维持与持续性疼痛相关的感觉神经元兴奋性增强状态的能力。

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