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从脊髓疼痛处理回路的平均视角转向特定视角。

Moving from an averaged to specific view of spinal cord pain processing circuits.

作者信息

Graham B A, Brichta A M, Callister R J

机构信息

School of Biomedical Sciences, Faculty of Health, Univ. of Newcastle, Callaghan, NSW 2308, Australia.

出版信息

J Neurophysiol. 2007 Sep;98(3):1057-63. doi: 10.1152/jn.00581.2007. Epub 2007 Jun 13.

Abstract

Neurons in the superficial dorsal horn (SDH) of the spinal cord play a critical role in processing potentially painful or noxious signals from skin, muscle, and viscera. Many acute pain therapies are based on the notion that altering the excitability of SDH neurons can block or gate these signals and reduce pain. This same notion also underlies treatments for certain chronic pain states. Basic scientists are now beginning to identify a number of potential molecular targets for spinal cord-based pain therapies with a focus on ion channels and receptors that can alter neuronal excitability. The current challenge in pain research is to identify which are the most promising targets and how their manipulation alters pain processing. In this review, we propose that our understanding of spinal pain processing mechanisms and translation of these discoveries into pain therapies could be improved by 1) better appreciating and understanding neuronal heterogeneity in the SDH; 2) establishing connectivity patterns among SDH neuron types; and 3) testing and extending findings made in vitro to intact (in vivo) animal models. As this information becomes available, it will be possible to determine the precise distribution of potential therapeutic targets on various SDH neuron types within specific circuits known to be functionally important in spinal pain processing.

摘要

脊髓浅表背角(SDH)中的神经元在处理来自皮肤、肌肉和内脏的潜在疼痛或有害信号方面发挥着关键作用。许多急性疼痛疗法基于这样一种观念,即改变SDH神经元的兴奋性可以阻断或控制这些信号并减轻疼痛。这一观念也是某些慢性疼痛状态治疗的基础。基础科学家现在开始确定一些基于脊髓的疼痛疗法的潜在分子靶点,重点是能够改变神经元兴奋性的离子通道和受体。疼痛研究当前面临的挑战是确定哪些是最有前景的靶点,以及对它们的操控如何改变疼痛处理过程。在这篇综述中,我们提出,可以通过以下方式改进我们对脊髓疼痛处理机制的理解以及将这些发现转化为疼痛疗法:1)更好地认识和理解SDH中的神经元异质性;2)建立SDH神经元类型之间的连接模式;3)将体外研究结果测试并扩展到完整的(体内)动物模型。随着这些信息的获得,将有可能确定潜在治疗靶点在已知对脊髓疼痛处理具有功能重要性的特定回路内各种SDH神经元类型上的精确分布。

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