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本文引用的文献

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Dissociation of the opioid receptor mechanisms that control mechanical and heat pain.控制机械性疼痛和热痛的阿片受体机制的解离。
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Distinct subsets of unmyelinated primary sensory fibers mediate behavioral responses to noxious thermal and mechanical stimuli.无髓初级感觉纤维的不同亚群介导对有害热刺激和机械刺激的行为反应。
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Therapeutic potential of vanilloid receptor TRPV1 agonists and antagonists as analgesics: Recent advances and setbacks.香草酸受体TRPV1激动剂和拮抗剂作为镇痛药的治疗潜力:最新进展与挫折
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Pungent agents from Szechuan peppers excite sensory neurons by inhibiting two-pore potassium channels.花椒中的辛辣成分通过抑制双孔钾通道来刺激感觉神经元。
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Vanilloid receptor 1-positive neurons mediate thermal hyperalgesia and tactile allodynia.香草酸受体1阳性神经元介导热痛觉过敏和触觉异常性疼痛。
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消融 TrpV1 神经元揭示了它们在热痛觉中的选择性作用。

Ablation of TrpV1 neurons reveals their selective role in thermal pain sensation.

机构信息

Molecular Genetics Unit, Laboratory of Sensory Biology, NIDCR, NIH Building 49, Room 1A16, 49 Convent Drive, Bethesda, MD 20892, USA.

出版信息

Mol Cell Neurosci. 2010 Jan;43(1):157-63. doi: 10.1016/j.mcn.2009.10.006. Epub 2009 Oct 21.

DOI:10.1016/j.mcn.2009.10.006
PMID:19853036
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2818468/
Abstract

Here we make use of neural ablation to investigate the properties of the TrpV1-expressing neurons in the trigeminal and dorsal root ganglia of mice. Resiniferotoxin (RTX), a potent TrpV1 agonist, administered either by direct injection in the ganglion or intrathecally killed approximately 70% of TrpV1 cells and resulted in modest thermal analgesia. Interestingly, after carageenan injection in the hind paw, the analgesic effects of RTX were dramatically increased with mice now paradoxically showing far less response to heat applied at sites of inflammation. This additional carageenan and RTX-induced analgesia was transient, lasting less than 2 days, and likely resulted from deafferentation of remaining TrpV1 neurons. Remarkably, although RTX affected sensitivity to heat, mechanical sensitivity (both of normal and inflamed tissue) was completely unaltered by toxin-mediated silencing of the TrpV1 sensory input. Thus, our data demonstrate that TrpV1 neurons are selectively tuned nociceptors that mediate responses to thermal but not mechanical pain and insinuate a labeled line model for somatosensory coding.

摘要

在这里,我们利用神经消融技术来研究小鼠三叉神经节和背根神经节中表达 TRPV1 的神经元的特性。树脂毒素(RTX)是一种有效的 TRPV1 激动剂,无论是直接注射到神经节还是鞘内给药,都会导致约 70%的 TRPV1 细胞死亡,并产生适度的热镇痛作用。有趣的是,在后脚掌注射角叉菜胶后,RTX 的镇痛效果显著增加,而此时小鼠对炎症部位的热刺激反应反而明显减少。这种额外的角叉菜胶和 RTX 诱导的镇痛作用是短暂的,持续时间不到 2 天,可能是由于剩余 TRPV1 神经元的去传入导致的。值得注意的是,尽管 RTX 影响了对热的敏感性,但机械敏感性(正常组织和炎症组织)在 TRPV1 感觉输入被毒素介导沉默后完全没有改变。因此,我们的数据表明 TRPV1 神经元是选择性的伤害感受器,介导对热但不是机械疼痛的反应,并暗示了一种体感编码的标记线模型。