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脑啡肽分解代谢抑制剂与CCK - B拮抗剂的联合应用:在疼痛管理和阿片类药物成瘾治疗中的潜在用途。

Association of enkephalin catabolism inhibitors and CCK-B antagonists: a potential use in the management of pain and opioid addiction.

作者信息

Roques B P, Noble F

机构信息

Département de Pharmacochimie Moléculaire et Structurale, INSERM U266-CNRS URA D 1500 Université René Descartes, UFR des Sciences Pharmaceutiques et Biologiques 4, Paris, France.

出版信息

Neurochem Res. 1996 Nov;21(11):1397-410. doi: 10.1007/BF02532381.

Abstract

The overlapping distribution of opioid and cholecystokinin (CCK) peptides and their receptors (mu and delta opioid receptors; CCK-A and CCK-B receptors) in the central nervous system have led to a large number of studies aimed at clarifying the functional relationships between these two neuropeptides. Most of the pharmacological studies devoted to the role of CCK and enkephalins have been focused on the control of pain. Recently the existence of regulatory mechanisms between both systems have been proposed, and the physiological antagonism between CCK and endogenous opioid systems has been definitely demonstrated by coadministration of CCK-B selective antagonists with RB 101, a systemically active inhibitor, which fully protects enkephalins from their degradation. Several studies have also been done to investigate the functional relationships between both systems in development of opioid side-effects and in behavioral responses. This article will review the experimental pharmacology of association of enkephalin-degrading enzyme inhibitors and CCK-B antagonists to demonstrate the interest of these molecules in the management of both pain and opioid addiction.

摘要

阿片类肽和胆囊收缩素(CCK)肽及其受体(μ和δ阿片受体;CCK - A和CCK - B受体)在中枢神经系统中的重叠分布引发了大量旨在阐明这两种神经肽之间功能关系的研究。大多数致力于CCK和脑啡肽作用的药理学研究都集中在疼痛控制方面。最近有人提出了这两个系统之间存在调节机制,并且通过将CCK - B选择性拮抗剂与具有全身活性的抑制剂RB 101共同给药,明确证明了CCK与内源性阿片系统之间的生理拮抗作用,RB 101可充分保护脑啡肽不被降解。也有几项研究致力于探究这两个系统在阿片类药物副作用发展和行为反应中的功能关系。本文将综述脑啡肽降解酶抑制剂与CCK - B拮抗剂联合应用的实验药理学,以证明这些分子在疼痛管理和阿片类药物成瘾治疗中的价值。

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