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Modeling Nociception in Zebrafish: A Way Forward for Unbiased Analgesic Discovery

机译:斑马鱼中的伤害感受建模:无偏见镇痛药发现的前进之路

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摘要

Acute and chronic pain conditions are often debilitating, inflicting severe physiological, emotional and economic costs and affect a large percentage of the global population. However, the development of therapeutic analgesic agents based primarily on targeted drug development has been largely ineffective. An alternative approach to analgesic development would be to develop low cost, high throughput, untargeted animal based behavioral screens that model complex nociceptive behaviors in which to screen for analgesic compounds. Here we describe the development of a behavioral based assay in zebrafish larvae that is effective in identifying small molecule compounds with analgesic properties. In a place aversion assay, which likely utilizes supraspinal neuronal circuitry, individually arrayed zebrafish larvae show temperature-dependent aversion to increasing and decreasing temperatures deviating from rearing temperature. Modeling thermal hyperalgesia, the addition of the noxious inflammatory compound and TRPA1 agonist allyl isothiocyanate sensitized heat aversion and reversed cool aversion leading larvae to avoid rearing temperature in favor of otherwise acutely aversive cooler temperatures. We show that small molecules with known analgesic properties are able to inhibit acute and/or sensitized temperature aversion.
机译:急性和慢性疼痛状况常常使人衰弱,造成严重的生理,情感和经济损失,并影响全球很大一部分人口。然而,主要基于靶向药物开发的治疗性镇痛药的开发在很大程度上是无效的。镇痛剂开发的另一种方法是开发低成本,高通量,基于目标的无目标动物行为筛查方法,该方法可对复杂的伤害性行为进行建模,以筛选镇痛剂化合物。在这里,我们描述了在斑马鱼幼虫中基于行为的检测方法的发展,该方法可有效识别具有镇痛作用的小分子化合物。在可能利用脊椎上神经元回路的地方厌恶分析中,单独排列的斑马鱼幼虫表现出对温度的厌恶,厌恶升高和降低的温度与饲养温度不同。模拟热痛觉过敏,添加有毒的炎症化合物和TRPA1激动剂异硫氰酸烯丙酯敏化了热厌恶感,并通过反向冷厌恶感导致幼虫避免了饲养温度,而采用了另外的强烈厌恶的较凉温度。我们表明,具有已知镇痛作用的小分子能够抑制急性和/或敏化的温度厌恶。

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