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丁丙诺啡:“部分激动剂”的阿片类药物。

Buprenorphine: The Opioid that Cried 'Partial Agonist'.

出版信息

J Opioid Manag. 2024 Jul-Aug;20(4):B9. doi: 10.5055/bupe.24.rpj.1040.

Abstract

Although buprenorphine use has increased dramatically over the past decade, its unique pharmacologic and pharmacokinetic profile often leads to misconceptions about its overall utility and has created a drastic underrepresentation in patients with chronic non-can- cer pain. A common misnomer associated with buprenorphine is because of 'partial agonist' activity, it exhibits a plateauing of typical opioid-related side effects (including respiratory depression, constipation, euphoria, and hypogonadal axis suppression), but additionally it must exhibit a plateauing effect of overall analgesic potential. However, novel downstream molecular and cellular mechanisms offer new insights that help support the clinical potential that buprenorphine's analgesic actions may not have a ceiling, like its side effect profile. This interactive symposium will provide an enhanced review of the evolving research that helps unravel the complexity around buprenorphine's varying pharmacologic effects including actions on various opioid receptors, promiscuity to elicit varying actions on mu-opioid receptors coupled with different isoforms of G~ subunits, role in the intracellular recruitment of beta-arrestin, binding to different splice variants of mu-opioid receptors, and greater spinal versus supraspinal activity. The final half of this symposium will be designed to substantiate evidence with various human clinical trial data to further support buprenorphine's place on the analgesic ladder.

摘要

虽然丁丙诺啡的使用在过去十年中大幅增加,但它独特的药理学和药代动力学特征常常导致人们对其整体效用产生误解,并导致慢性非癌症疼痛患者的严重代表性不足。与丁丙诺啡相关的一个常见误解是,由于其“部分激动剂”活性,它表现出典型阿片类药物相关副作用(包括呼吸抑制、便秘、欣快感和性腺轴抑制)的平台效应,但它还必须表现出整体镇痛潜力的平台效应。然而,新的下游分子和细胞机制提供了新的见解,有助于支持丁丙诺啡的镇痛作用可能没有上限的临床潜力,就像它的副作用特征一样。本次互动研讨会将对不断发展的研究进行深入回顾,有助于揭示丁丙诺啡不同药理学效应的复杂性,包括对各种阿片受体的作用、与不同 G 亚基同工型偶联的 mu 阿片受体的变构作用、在细胞内募集β-arrestin 的作用、与 mu 阿片受体不同剪接变体的结合以及脊髓与脊髓上活性的差异。研讨会的最后一半将旨在用各种人体临床试验数据来证实证据,以进一步支持丁丙诺啡在镇痛阶梯上的地位。

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