首页> 美国卫生研究院文献>The Journal of Neuroscience >The 5-HT3 Subtype of Serotonin Receptor Contributes to Nociceptive Processing via a Novel Subset of Myelinated and Unmyelinated Nociceptors
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The 5-HT3 Subtype of Serotonin Receptor Contributes to Nociceptive Processing via a Novel Subset of Myelinated and Unmyelinated Nociceptors

机译:5-羟色胺受体的5-HT3亚型通过有髓和无髓伤害感受器的新子集有助于伤害感受过程。

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摘要

Serotonin is a major component of the inflammatory chemical milieu and contributes to the pain of tissue injury via an action on multiple receptor subtypes. Here we studied mice after genetic or pharmacological disruption of the 5-HT3 receptor, an excitatory serotonin-gated ion channel. We demonstrate that tissue injury-induced persistent, but not acute, nociception is significantly reduced after functional elimination of this receptor subtype. Specifically, in the setting of tissue injury, the 5-HT3receptor mediates activation of nociceptors but does not contribute to injury-associated edema. This result is explained by the localization of 5-HT3 receptor transcripts to a previously uncharacterized subset of myelinated and unmyelinated afferents, few of which express the proinflammatory neuropeptide substance P. Finally, we provide evidence that central serotonergic circuits modulate nociceptive transmission via a facilitatory action at spinal 5-HT3 receptors. We conclude that activation of both peripheral and central 5-HT3 receptors is pronociceptive and that the contribution of peripheral 5-HT3 receptors involves a novel complement of primary afferent nociceptors.
机译:5-羟色胺是炎症化学环境的主要成分,并通过对多种受体亚型的作用而导致组织损伤。在这里,我们研究了5-HT3受体(一种兴奋性血清素门控离子通道)的遗传或药理作用后的小鼠。我们证明,在功能消除该受体亚型后,组织损伤诱导的持续性但不是急性伤害性显着降低。具体而言,在组织损伤的情况下,5-HT3受体介导伤害感受器的激活,但不会导致与损伤相关的水肿。通过将5-HT3受体转录物定位到先前未鉴定的髓鞘和未髓鞘的传入子集中来解释这一结果,其中很少表达促炎性神经肽物质P。在脊髓5-HT3受体上。我们得出的结论是,外围和中枢5-HT3受体的激活都是感受感受性的,外围5-HT3受体的贡献涉及初级传入伤害感受器的新补体。

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