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辣椒平对辣椒素的选择性拮抗作用:辣椒素诱导的抗伤害感受中脊髓受体位点的证据。

Selective antagonism of capsaicin by capsazepine: evidence for a spinal receptor site in capsaicin-induced antinociception.

作者信息

Dickenson A H, Dray A

机构信息

Department of Pharmacology, University College, London.

出版信息

Br J Pharmacol. 1991 Dec;104(4):1045-9. doi: 10.1111/j.1476-5381.1991.tb12547.x.

Abstract
  1. Capsazepine has recently been described as a competitive capsaicin antagonist. We have used this compound to test the hypotheses that the in vitro and in vivo effects of capsaicin are due to interactions with a specific receptor. 2. In an in vitro preparation of the neonatal rat spinal cord with functionally connected tail, the activation of nociceptive afferent fibres by the application of capsaicin, bradykinin or noxious heat (48 degrees C) to the tail could be measured by recording a depolarizing response from a spinal ventral root. Application of capsaicin or substance P to the spinal cord also evoked a depolarizing response which was recorded in a ventral root. 3. When capsazepine (50 nM-20 microM) was administered to the tail or spinal cord it did not evoke any measurable response. However on the tail, capsazepine reversibly antagonized (IC50 = 254 +/- 28 nM) the responses to capsaicin but not to heat or bradykinin administered to the same site. Similarly capsazepine administration to the spinal cord antagonized the responses evoked by capsaicin (IC50 = 230 +/- 20 nM) applied to the cord but not responses evoked by substance P on the cord or by noxious heat and capsaicin on the tail. 4. In halothane anaesthetized rats, C-fibre responses evoked by transcutaneous electrical stimulation of the receptive field were recorded from single wide dynamic range neurones located in the spinal dorsal horn. C-fibre evoked discharges were consistently reduced by the systemic administration of capsaicin (20 mumol kg-1, s.c.) and this action of capsaicin was antagonized by capsazepine (100 mumol kg-1) administered by the same route. In addition the systemic effect of capsaicin was antagonized by a spinal intrathecal administration of capsazepine (5-50 nmol). 5. Intradermal injections of capsaicin, localized to the peripheral receptive field, usually one toe of the ipsilateral hind-paw, produced a transient increase in C-fibre-evoked activity followed by a prolonged period of localized insensitivity to transcutaneous C-fibre stimulation. These effects of capsaicin were significantly reduced by the concommitant administration of capsazepine to the same site. 6. These data demonstrate that capsazepine is a selective antagonist of capsaicin on nociceptive neurones in vitro and in vivo and suggest that the effects of capsaicin were mediated by activation of a specific receptor. Since the antinociceptive effect produced by systemically administered capsaicin was antagonised by spinal intrathecal capsazepine this further supports the hypothesis that capsaicin exerts its antinociceptive effect by acting on specific receptors localized to sensory nerve fibres in the spinal cord.
摘要
  1. 辣椒平最近被描述为一种竞争性辣椒素拮抗剂。我们已使用该化合物来检验以下假设:辣椒素的体外和体内效应是由于与特定受体相互作用所致。2. 在新生大鼠具有功能连接尾巴的脊髓体外制备物中,通过记录脊髓腹根的去极化反应,可测量向尾巴施加辣椒素、缓激肽或有害热(48℃)对伤害性传入纤维的激活。向脊髓施加辣椒素或P物质也会诱发在腹根中记录到的去极化反应。3. 当向尾巴或脊髓给予辣椒平(50 nM - 20 μM)时,它不会诱发任何可测量的反应。然而,在尾巴上,辣椒平可逆性拮抗(IC50 = 254 ± 28 nM)对辣椒素的反应,但对在同一部位施加的热或缓激肽的反应无拮抗作用。同样,向脊髓给予辣椒平可拮抗施加于脊髓的辣椒素所诱发的反应(IC50 = 230 ± 20 nM),但对脊髓上P物质诱发的反应或尾巴上有害热和辣椒素诱发的反应无拮抗作用。4. 在氟烷麻醉的大鼠中,从位于脊髓背角的单个广动力范围神经元记录经皮电刺激感受野所诱发的C纤维反应。全身给予辣椒素(20 μmol kg-1,皮下注射)可使C纤维诱发的放电持续减少,而辣椒平(100 μmol kg-1)经相同途径给药可拮抗辣椒素的这一作用。此外,脊髓鞘内注射辣椒平(5 - 50 nmol)可拮抗辣椒素的全身效应。5. 皮内注射局限于外周感受野(通常是同侧后爪的一个脚趾)的辣椒素,会使C纤维诱发的活动短暂增加,随后是对经皮C纤维刺激的局部长时间不敏感。同时向同一部位给予辣椒平可显著降低辣椒素的这些效应。6. 这些数据表明,辣椒平在体外和体内是辣椒素对伤害性神经元的选择性拮抗剂,并提示辣椒素的效应是由特定受体的激活介导的。由于脊髓鞘内注射辣椒平可拮抗全身给予辣椒素产生的抗伤害感受作用,这进一步支持了以下假设:辣椒素通过作用于脊髓感觉神经纤维上的特定受体发挥其抗伤害感受作用。

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