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A Pharmacological Rationale to Reduce the Incidence of Opioid Induced Tolerance and Hyperalgesia: A Review

机译:减少阿片类药物引起的耐受性和痛觉过敏发生率的药理学原理:综述

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Chronic pain is an important health and social problem. Misuse and abuse of opioids in chronic non-cancer pain management seem to be a huge problem, in some countries. This could probably affect the normal use of such analgesics in patients in need of them. Basic and clinical researches should find the solution to mitigate the potential damage. Dysregulation of mast cell and microglia activation plays an important role in the pathogenesis and management of chronic pain. Persistent mast cell activation sensitizes nociceptors and initiates central nervous system inflammatory processes, involving microglial cell activation and sensitization of spinal somatosensory neurons. Exposure of mast cells and microglia to opioids is well known to provoke activation of these non-neuronal immune cell populations, thereby contributing to an exacerbation of pro-inflammatory and pro-nociceptive processes and promoting, over the long-term, opioid-induced hyperalgesia and tolerance. This review is intended to provide the reader with an overview of the role for these non-neuronal cells in opioid-induced chronic pain and tolerance as a consequence of prolonged exposure to these drugs. In addition, we will examine a potential strategy with the aim to modulate opioid-induced over-activation of glia and mast cells, based on endogenous defense mechanisms and fatty acid amide signaling molecules.
机译:慢性疼痛是重要的健康和社会问题。在某些国家,在非癌症的慢性疼痛管理中滥用和滥用阿片类药物似乎是一个巨大的问题。这可能会影响需要这种止痛药的患者的正常使用。基础和临床研究应找到减轻潜在损害的解决方案。肥大细胞失调和小胶质细胞活化在慢性疼痛的发病机理和治疗中起着重要作用。持续的肥大细胞活化使伤害感受器敏化并引发中枢神经系统炎症过程,涉及小胶质细胞活化和脊髓体感神经元敏化。众所周知,肥大细胞和小胶质细胞暴露于阿片类药物可激活这些非神经元免疫细胞群,从而加剧炎症和促伤害性过程,并在长期内促进阿片类药物引起的痛觉过敏和宽容。这篇综述旨在为读者提供这些非神经元细胞因长时间接触这些药物而在阿片类药物引起的慢性疼痛和耐受中的作用的概述。此外,我们将基于内源性防御机制和脂肪酸酰胺信号分子,研究旨在调节阿片样物质诱导的神经胶质细胞和肥大细胞过度活化的潜在策略。

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