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内毒素休克中的多种阿片受体:体内δ受体参与及μ-δ相互作用的证据

Multiple opioid receptors in endotoxic shock: evidence for delta involvement and mu-delta interactions in vivo.

作者信息

D'Amato R, Holaday J W

出版信息

Proc Natl Acad Sci U S A. 1984 May;81(9):2898-901. doi: 10.1073/pnas.81.9.2898.

Abstract

The use of selective delta and mu opioid antagonists has provided evidence that delta opioid receptors within the brain mediate the endogenous opioid component of endotoxic shock hypotension. The selectivity of these delta and mu antagonists was demonstrated by their differing effects upon morphine analgesia and endotoxic hypotension. The mu antagonist beta-funaltrexamine, at doses that antagonized morphine analgesia, failed to alter shock, whereas the delta antagonist M 154,129: [N,N-bisallyl-Tyr-Gly-Gly-psi-(CH2S)-Phe-Leu-OH] (ICI) reversed shock at doses that failed to block morphine analgesia. Therefore, selective delta antagonists may have therapeutic value in reversing circulatory shock without altering the analgesic actions of endogenous or exogenous opioids. Additional data revealed that prior occupancy of mu binding sites by irreversible opioid antagonists may allosterically attenuate the actions of antagonists with selectivity for delta binding sites. For endogenous opioid systems, this observation provides an opportunity to link in vivo physiological responses with receptor-level biochemical interactions.

摘要

选择性δ和μ阿片受体拮抗剂的使用已证明,脑内的δ阿片受体介导内毒素性休克低血压的内源性阿片成分。这些δ和μ拮抗剂的选择性通过它们对吗啡镇痛和内毒素性低血压的不同作用得以证明。μ拮抗剂β-芬太尼环已胺,在拮抗吗啡镇痛的剂量下,未能改变休克,而δ拮抗剂M 154,129:[N,N-双烯丙基-Tyr-Gly-Gly-ψ-(CH2S)-Phe-Leu-OH](ICI)在未能阻断吗啡镇痛的剂量下却能逆转休克。因此,选择性δ拮抗剂在不改变内源性或外源性阿片类药物镇痛作用的情况下,可能对逆转循环性休克具有治疗价值。更多数据显示,不可逆阿片拮抗剂预先占据μ结合位点可能会变构减弱对δ结合位点具有选择性的拮抗剂的作用。对于内源性阿片系统而言,这一观察结果为将体内生理反应与受体水平的生化相互作用联系起来提供了契机。

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