鞘内给予瑞芬太尼诱导镇痛后大鼠急性痛觉及传出功能的保留。

Preservation of acute pain and efferent functions following intrathecal resiniferatoxin-induced analgesia in rats.

机构信息

Department of Pharmacology, Southern Illinois University School of Medicine, Springfield, Illinois 62702, USA.

出版信息

J Pain. 2011 Sep;12(9):991-1003. doi: 10.1016/j.jpain.2011.03.005. Epub 2011 Jun 16.

DOI:10.1016/j.jpain.2011.03.005

PMID:21680254

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3645374/

Abstract

UNLABELLED

Resiniferatoxin (RTX) is a potent agonist of TRPV1, which possesses unique properties that can be utilized to treat certain modalities of pain. In the present study, systemic intraperitoneal (i.p.) administration of RTX resulted in a significant decrease in acute thermal pain sensitivity, whereas localized intrathecal (i.t.) administration had no effect on acute thermal pain sensitivity. Both i.p. and i.t. administration of RTX prevented TRPV1-induced nocifensive behavior and inflammatory thermal hypersensitivity. There were no alterations in mechanical sensitivity either by i.p. or i.t. administration of RTX. In spinal dorsal horn (L4-L6), TRPV1 and substance P immunoreactivity were abolished following i.p. and i.t. administration of RTX. In dorsal root ganglia (DRG), TRPV1 immunoreactivity was diminished following i.p. administration, but was unaffected following i.t. administration of RTX. Following i.p. administration, basal and evoked calcitonin gene-related peptide release were reduced both in the spinal cord and peripheral tissues. However, following i.t. administration, basal and evoked calcitonin gene-related peptide release were reduced in spinal cord (L4-L6), but were unaffected in peripheral tissues. Both i.p. and i.t. RTX administration lowered the body temperature acutely, but this effect reversed with time. Targeting TRPV1-expressing nerve terminals at the spinal cord can selectively abolish inflammatory thermal hypersensitivity without affecting acute thermal sensitivity and can preserve the efferent functions of DRG neurons at the peripheral nerve terminals. I.t. administration of RTX can be considered as a strategy for treating certain chronic and debilitating pain conditions.

PERSPECTIVE

Localized administration of RTX in spinal cord could be a useful strategy to treat chronic debilitating pain arising from certain conditions such as cancer and at the same time could maintain normal physiological peripheral efferent functions mediated by TRPV1.

摘要

未加标签

树脂毒素（RTX）是 TRPV1 的有效激动剂，具有独特的特性，可用于治疗某些类型的疼痛。在本研究中，RTX 的全身腹腔内（i.p.）给药导致急性热痛觉敏感性显著降低，而局部鞘内（i.t.）给药对急性热痛觉敏感性没有影响。RTX 的 i.p. 和 i.t. 给药均预防 TRPV1 诱导的伤害性行为和炎症性热过敏。无论是通过 i.p. 还是 i.t. 给予 RTX，机械敏感性均无改变。在脊髓背角（L4-L6）中，RTX 的 i.p. 和 i.t. 给药消除了 TRPV1 和 P 物质的免疫反应性。在背根神经节（DRG）中，RTX 的 i.p. 给药减少了 TRPV1 免疫反应性，但 i.t. 给药则没有影响。在 i.p. 给药后，脊髓和外周组织中的降钙素基因相关肽的基础和诱发释放均减少。但是，在 i.t. 给药后，脊髓（L4-L6）中的基础和诱发降钙素基因相关肽释放减少，但外周组织中不受影响。RTX 的 i.p. 和 i.t. 给药均可使体温急剧下降，但这种作用会随着时间的推移而逆转。在脊髓靶向表达 TRPV1 的神经末梢可以选择性地消除炎症性热过敏，而不影响急性热敏感性，并可以维持外周神经末梢中 DRG 神经元的传出功能。RTX 的 i.t. 给药可被视为治疗某些慢性和使人衰弱的疼痛状况的策略。

观点

脊髓内局部给予 RTX 可能是治疗某些疾病（如癌症）引起的慢性使人衰弱的疼痛的有用策略，同时可以维持 TRPV1 介导的正常生理外周传出功能。

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