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Eugenol and carvacrol induce temporally desensitizing patterns of oral irritation and enhance innocuous warmth and noxious heat sensation on the tongue

机译:丁香酚和香芹酚会引起口腔刺激的暂时性脱敏模式并增强无害的保暖性和对舌头的有害热感

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摘要

Eugenol and carvacrol, from the spices clove and oregano, respectively, are agonists of TRPV3 which is implicated in transduction of warmth and possibly heat pain. We presently investigated the temporal dynamics of lingual irritation elicited by these agents, and their effects on innocuous warmth and heat pain, using a half-tongue method in human subjects. The irritant sensation elicited by both eugenol and carvacrol decreased across repeated applications at a 1-min interstimulus interval (self-desensitization) which persisted for at least 10 min. Both agents also cross-desensitized capsaicin-evoked irritation. Eugenol and carvacrol significantly increased the magnitude of perceived innocuous warmth (44°C) for >10 min, and briefly (<5 min) enhanced heat pain elicited by a 49°C stimulus. Similar albeit weaker effects were observed when thermal stimuli were applied after the tongue had been desensitized by repeated application of eugenol or carvacrol, indicating that the effect is not due solely to summation of chemoirritant and thermal sensations. Neither chemical affected sensations of innocuous cool or cold pain. A separate group of subjects were asked to subdivide eugenol and carvacrol irritancy into subqualities, the most frequently-reported being numbing and warmth, with brief burning, stinging/pricking and tingle, confirming an earlier study. Eugenol, but not carvacrol, reduced detection of low-threshold mechanical stimuli. Eugenol and carvacrol enhancement of innocuous warmth may involve sensitization of thermal gating of TRPV3 expressed in peripheral warm fibers. The brief heat hyperalgesia following eugenol may involve a TRPV3-mediated enhancement of thermal gating of TRPV1 expressed in lingual polymodal nociceptors.
机译:丁香和牛至中的丁香酚和香芹酚分别是TRPV3的激动剂,可能与温暖和热痛的发生有关。我们目前在人类受试者中使用半舌法研究了由这些药物引起的舌头刺激的时间动态及其对无害的温暖和热痛的影响。丁香酚和香芹酚均引起的刺激性感觉在重复使用间隔为1分钟(自我脱敏)持续至少10分钟的情况下不断下降。两种药物还使辣椒素引起的脱敏交叉反应。丁香酚和香芹酚在大于10分钟的时间内显着增加了感知的无害温度(44°C)的幅度,并且短暂地(<5分钟)增强了由49°C刺激引起的热痛。在通过反复使用丁子香酚或香芹酚使舌头脱敏后再施加热刺激时,观察到类似的效果较弱,这表明该效果并非仅由于化学刺激性和热感的总和。化学品不会影响无害的凉爽或冷痛的感觉。要求另一组受试者将丁子香酚和香芹酚的刺激性细分为次要质量,最常报告的是麻木和温暖,伴有短暂的灼痛,刺痛/刺痛和刺痛感,这证实了较早的研究。丁香酚,而不是香芹酚,减少了低阈值机械刺激的检测。丁香酚和香芹酚提高无害保暖性可能涉及敏化外围保暖纤维中表达的TRPV3的热门控。丁香酚后的短暂性热痛觉过敏可能涉及TRPV3介导的多语种伤害感受器表达的TRPV1热门控的增强。

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