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首页> 外文期刊>Acta anaesthesiologica Taiwanica : >Role of neuroinflammation in morphine tolerance: Effect of tumor necrosis factor-@a
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Role of neuroinflammation in morphine tolerance: Effect of tumor necrosis factor-@a

机译:神经炎症在吗啡耐受中的作用:肿瘤坏死因子-a的作用

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摘要

Opioids have been used as potent analgesics in clinics for decades; however, their long-term administration leads to tolerance. Two possible mechanisms for drug tolerance are postulated as within-system and between-systems adaptation. The within-system tolerance is involved in the signal transduction of opioid receptors, including downregulation of opioid receptors, uncoupling of G-protein from opioid receptors, and @b-arrestin recruitment to opioid receptors, which causes receptor desensitization and internalization/endocytosis. The between-systems tolerance comprehends the glutamatergic receptor system and glial activation with the release of proinflammatory cytokines, and thus the analgesic effect of morphine is reduced. Tumor necrosis factor-@a (TNF-@a) is a vital proinflammatory cytokine and exerts either a neurotoxic or neuroprotective effect on different diseases of the central nervous system. TNF-@a has also been demonstrated to correlate with neuronal plasticity via activation of spinal glial cells and enhancement of glutamatergic transmission. Previous studies had revealed an increased expression of TNF-@a in morphine tolerance. This review article focuses on the role of TNF-@a in neuroinflammation and the glutamatergic receptor system in morphine tolerance. It may provide another adjuvant therapy for morphine tolerance, which extends the effectiveness of opioids in clinical pain management.
机译:阿片类药物已在临床上用作有效的镇痛药已有数十年之久。但是,长期服用会导致耐受。假设两种可能的药物耐受机制是系统内和系统间适应。系统内耐受性涉及阿片受体的信号转导,包括阿片受体的下调,G蛋白与阿片受体的解偶联以及阿片受体的b-arrestin募集,这会引起受体脱敏和内在化/内吞。系统间的耐受性包括谷氨酸能受体系统和神经胶质的激活以及促炎性细胞因子的释放,因此吗啡的镇痛作用降低。肿瘤坏死因子-α(TNF-αa)是重要的促炎细胞因子,对中枢神经系统的各种疾病具有神经毒性或神经保护作用。 TNF-αa还被证明通过激活脊髓神经胶质细胞和增强谷氨酸能传递与神经元可塑性相关。先前的研究表明吗啡耐受性中TNF-αa的表达增加。这篇综述文章集中于TNF-α在神经炎症中的作用以及谷氨酸能受体系统在吗啡耐受中的作用。它可能为吗啡耐受提供另一种辅助疗法,从而扩展了阿片类药物在临床疼痛治疗中的有效性。

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