尼古丁可保护机体免受β-芬太尼环唑对μ-阿片受体的拮抗作用：尼古丁诱导脑内内源性阿片类物质释放的证据。

Nicotine protects against mu-opioid receptor antagonism by beta-funaltrexamine: evidence for nicotine-induced release of endogenous opioids in brain.

作者信息

Davenport K E, Houdi A A, Van Loon G R

机构信息

Department of Medicine, University of Kentucky, Lexington.

出版信息

Neurosci Lett. 1990 May 18;113(1):40-6. doi: 10.1016/0304-3940(90)90491-q.

DOI:10.1016/0304-3940(90)90491-q

PMID:2164174

Abstract

We have hypothesized that some effects of nicotine are mediated through endogenous opioids. This study was designed to demonstrate in rats that nicotine releases endogenous opioids in brain. In the control group, subcutaneous morphine (8 mg/kg) produced analgesia or antinociception as measured by prolongation of tail flick latency. Intracerebroventricular administration 24 h earlier of beta-funaltrexamine (beta-FNA, 2.5 micrograms), an antagonist which irreversibly alkylates opioid receptors, markedly reduced (66%) morphine analgesia. Subcutaneous administration of nicotine (0.1 mg/kg) prior to beta-FNA attenuated (31%) the inhibitory effect of beta-FNA on morphine analgesia. These data support our hypothesis that endogenous opioids released by nicotine bind to mu-opioid receptors in brain and protect them against inactivation by beta-FNA.

摘要

我们已经提出假设，即尼古丁的某些作用是通过内源性阿片类物质介导的。本研究旨在在大鼠中证明尼古丁会在大脑中释放内源性阿片类物质。在对照组中，皮下注射吗啡（8毫克/千克）会产生镇痛或抗伤害感受作用，这可通过甩尾潜伏期的延长来衡量。在24小时前脑室内注射β-氟纳曲酮（β-FNA，2.5微克），一种不可逆地使阿片受体烷基化的拮抗剂，可显著降低（66%）吗啡的镇痛作用。在注射β-FNA之前皮下注射尼古丁（0.1毫克/千克）可减弱（31%）β-FNA对吗啡镇痛作用的抑制效果。这些数据支持了我们的假设，即尼古丁释放的内源性阿片类物质会与大脑中的μ-阿片受体结合，并保护它们不被β-FNA灭活。

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尼古丁可保护机体免受β-芬太尼环唑对μ-阿片受体的拮抗作用：尼古丁诱导脑内内源性阿片类物质释放的证据。

Nicotine protects against mu-opioid receptor antagonism by beta-funaltrexamine: evidence for nicotine-induced release of endogenous opioids in brain.

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