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首页> 外文期刊>Pain. >Dose-response study of topical allyl isothiocyanate (mustard oil) as a human surrogate model of pain, hyperalgesia, and neurogenic inflammation
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Dose-response study of topical allyl isothiocyanate (mustard oil) as a human surrogate model of pain, hyperalgesia, and neurogenic inflammation

机译:局部烯丙基异硫氰酸盐(芥菜油)作为疼痛,痛觉过敏和神经源性炎症的人替代模型的剂量 - 反应研究

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Despite being a ubiquitous animal pain model, the natural TRPA1-agonist allyl isothiocyanate (AITC, also known as "mustard oil") has only been sparsely investigated as a potential human surrogate model of pain, sensitization, and neurogenic inflammation. Its dose-response as an algogenic, sensitizing irritant remains to be elucidated in human skin. Three concentrations of AITC (10%, 50%, and 90%) and vehicle (paraffin) were applied for 5 minutes to 333 cm areas on the volar forearms in 14 healthy volunteers, and evoked pain intensity (visual analog scale 0-100 mm) and pain quality were assessed. In addition, a comprehensive battery of quantitative sensory tests was conducted, including assessment of mechanical and thermal sensitivity. Neurogenic inflammation was quantified using full-field laser perfusion imaging. Erythema and hyperpigmentation were assessed before, immediately after, and approximate to 64 hours after AITC exposure. AITC induced significant dose-dependent, moderate-to-severe spontaneous burning pain, mechanical and heat hyperalgesia, and dynamic mechanical allodynia (P < 0.05). No significant differences in induced pain hypersensitivity were observed between the 50% and 90% AITC concentrations. Acute and prolonged inflammation was evoked by all concentrations, and assessments by full-field laser perfusion imaging demonstrated a significant dose-dependent increase with a ceiling effect from 50% to 90%. Topical AITC application produces pain and somatosensory sensitization in a dose-dependent manner with optimal concentrations recommended to be > 10% and <= 50%. The model is translatable to humans and could be useful in pharmacological proof-of-concept studies of TRPA1-antagonists, analgesics, and anti-inflammatory compounds or for exploratory clinical purposes, eg, loss-or gain-of-function in peripheral neuropathies.
机译:尽管是普遍存在的动物疼痛模型,但天然的TRPA1-激动剂烯丙基异硫氰酸酯(AITC,也称为“芥菜油”)才被稀疏地研究了潜在的人类替代痛,敏化和神经源性炎症。其剂量 - 反应作为抗抗抗激刺激性刺激物仍有待阐明的人体皮肤。在14个健康的志愿者中,将三种浓度的Aitc(10%,50%和90%)和载体(石蜡)施加5分钟至333厘米的区域,并诱发疼痛强度(视觉模拟300 mm )和疼痛质量得到评估。此外,进行了定量感官测试的综合电池,包括对机械和热敏的评估。使用全场激光灌注成像量化神经源性炎症。在AITC暴露后,立即,立即进行分发膜和高度沉降,并在AITC暴露后的64小时内进行评估。 AITC诱导显着的剂量依赖性,中度至严重的自发燃烧,机械和热痛觉痛觉,以及动态的机械异常性疼痛(P <0.05)。在50%和90%AITC浓度之间观察到诱导疼痛过敏的显着差异。所有浓度引起急性和延长的炎症,并且全场激光灌注成像的评估表明,显着的剂量依赖性增加,其天花板效果为50%至90%。局部AITC应用以剂量依赖性方式产生疼痛和体感敏感性,推荐的最佳浓度为> 10%和<= 50%。该模型可与人类翻译,可用于TRPA1-拮抗剂,镇痛药和抗炎化合物的药理概念研究或用于外周神经病的探索性临床目的,例如丧失或函数增益。

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