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Epidural optogenetics for controlled analgesia

机译:硬膜外光遗传学用于控制性镇痛

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摘要

Optogenetic tools enable cell selective and temporally precise control of neuronal activity; yet, difficulties in delivering sufficient light to the spinal cord of freely behaving animals have hampered the use of spinal optogenetic approaches to produce analgesia. We describe an epidural optic fiber designed for chronic spinal optogenetics that enables the precise delivery of light at multiple wavelengths to the spinal cord dorsal horn and sensory afferents. The epidural delivery of light enabled the optogenetic modulation of nociceptive processes at the spinal level. The acute and repeated activation of channelrhodopsin-2 expressing nociceptive afferents produced robust nocifensive behavior and mechanical sensitization in freely behaving mice, respectively. The optogenetic inhibition of GABAergic interneurons in the spinal cord dorsal horn through the activation of archaerhodopsin also produced a transient, but selective induction of mechanical hypersensitivity. Finally, we demonstrate the capacity of optogenetics to produce analgesia in freely behaving mice through the inhibition of nociceptive afferents via archaerhodopsin. Epidural optogenetics provides a robust and powerful solution for activation of both excitatory and inhibitory opsins in sensory processing pathways. Our results demonstrate the potential of spinal optogenetics to modulate sensory behavior and produce analgesia in freely behaving animals.
机译:光遗传学工具可以对神经元活动进行细胞选择性和时间精确控制。但是,难以向行为自由的动物的脊髓提供足够的光,这阻碍了使用脊髓光遗传学方法来产生镇痛作用。我们描述了一种专为慢性脊柱光遗传学设计的硬膜外光纤,它能够将多种波长的光精确传递到脊髓背角和感觉传入神经。硬膜外递送光使得能够在脊髓水平上对伤害感受过程进行光遗传学调节。表达channelrhodopsin-2的伤害性传入传入的急性和反复激活分别在行为自由的小鼠中产生了强大的伤害性行为和机械敏化作用。通过激活古细菌视紫红质对脊髓背角中的GABA能中间神经元的光遗传抑制也产生了短暂但选择性的机械超敏反应。最后,我们证明了光遗传学通过古细菌视紫红质通过抑制伤害感受传入来在行为自由的小鼠中产生镇痛的能力。硬膜外光遗传学为激活感官加工途径中的兴奋性和抑制性视蛋白提供了强大而强大的解决方案。我们的结果证明了脊髓光遗传学在调节行为自由的动物中调节感觉行为并产生镇痛作用的潜力。

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