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The endocannabinoid system: Novel targets for treating cancer induced bone pain

机译:Endocannabinoid系统:治疗癌症诱导骨疼痛的新靶标

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Treating Cancer-induced bone pain (CIBP) continues to be a major clinical challenge and underlying mechanisms of CIBP remain unclear. Recently, emerging body of evidence suggested the endocannabinoid system (ECS) may play essential roles in CIBP. Here, we summarized the current understanding of the antinociceptive mechanisms of endocannabinoids in CIBP and discussed the beneficial effects of endocannabinoid for CIBP treatment. Targeting nonselective cannabinoid 1 receptors or selective cannabinoid 2 receptors, and modulation of peripheral AEA and 2-AG, as well as the inhibition the function of fatty acid amide hydrolase (FAAH) and monoacylglycerol lipase (MAGL) have produced analgesic effects in animal models of CIBP. Management of ECS therefore appears to be a promising way for the treatment of CIBP in terms of efficacy and safety. Further clinical studies are encouraged to confirm the possible translation to humans of the very promising results already obtained in the preclinical studies.
机译:治疗癌症诱导的骨疼痛(CIBP)仍然是一个主要的临床挑战,CIBP的潜在机制仍然不清楚。最近,新兴的证据表明Endocannabinoid系统(ECS)可能在CIBP中起重要作用。在这里,我们总结了目前对CIBP中Endocannabinoids的抗血巧机制的理解,并讨论了Endannabinoid对CIBP治疗的有益作用。靶向非选择性大麻素1受体或选择性大麻素2受体,以及外周AEA和2-AG的调节,以及抑制脂肪酸酰胺水解酶(FAAH)和单酰基甘油脂肪酶(MAGL)的抑制作用在动物模型中产生镇痛作用CIBP。因此,ECS的管理似乎是在疗效和安全方面治疗CIBP的有希望的方式。鼓励进一步的临床研究确认在临床前研究中已经获得的非常有前景结果的人类的可能翻译。

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