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对吗啡依赖小鼠中大麻素受体结合及大麻素激动剂刺激的[35S]GTPγS结合的放射自显影分析。

Autoradiographic analysis of cannabinoid receptor binding and cannabinoid agonist-stimulated [35S]GTP gamma S binding in morphine-dependent mice.

作者信息

Romero J, Fernández-Ruiz J J, Vela G, Ruiz-Gayo M, Fuentes J A, Ramos J A

机构信息

Instituto Complutense de Drogodependencias, Department of Biochemistry, Faculty of Medicine, Complutense University, Madrid, Spain.

出版信息

Drug Alcohol Depend. 1998 May 1;50(3):241-9. doi: 10.1016/s0376-8716(98)00036-2.

Abstract

The present study was designed to test the possible existence of changes in brain cannabinoid receptors in morphine-dependent mice. To this end, we compared cannabinoid receptor binding and WIN 55,212-2-stimulated [35S]guanylyl-5'-O-(gamma-thio)-triphosphate ([35S]GTP gamma S) binding in several brain regions of mice chronically exposed to morphine or saline. The existence of opiate dependence in morphine-injected mice was assessed by analyzing the well-known jumping behavior induced by the blockade of opioid receptors with naloxone, whereas these animals were unresponsive to the blockade of cannabinoid receptors with SR141716. The different structures analyzed exhibited similar cannabinoid receptor binding levels in morphine-dependent and control mice, with the only exception of the globus pallidus, which exhibited a very small, but statistically significant, increase. In addition, the activation of cannabinoid receptors with WIN 55,212-2 increased [35S]GTP gamma S binding in most of the structures examined. The increase was of similar magnitude in morphine-dependent and control mice, except in the substantia nigra, where morphine-dependent mice exhibited lesser [35S]GTP gamma S binding levels in basal conditions, although a significantly higher WIN 55,212-2-stimulated binding. Other structures, such as the central gray substance, where there was a poor agonist-induced stimulation in control mice, exhibited, however, higher levels of WIN 55,212-2-stimulated [35S]GTP gamma S binding in morphine-dependent mice, whereas these animals tended to exhibit a higher [35S]GTP gamma S binding levels in basal conditions, although a lesser and not statistically significant WIN 55,22-2-stimulated binding, in the deep layers of the cerebral cortex. Thus, the data support the potential existence of a specific effect of morphine in the coupling of cannabinoid receptors to GTP-binding proteins, rather than on receptor binding, although this was observed only in the substantia nigra and central gray substance.

摘要

本研究旨在检测吗啡依赖小鼠脑内大麻素受体是否可能发生变化。为此,我们比较了长期暴露于吗啡或生理盐水的小鼠多个脑区中大麻素受体结合以及WIN 55,212-2刺激的[35S]鸟苷-5'-O-(γ-硫代)-三磷酸([35S]GTPγS)结合情况。通过分析用纳洛酮阻断阿片受体所诱导的众所周知的跳跃行为来评估注射吗啡小鼠中阿片依赖的存在,而这些动物对用SR141716阻断大麻素受体无反应。所分析的不同结构在吗啡依赖小鼠和对照小鼠中表现出相似的大麻素受体结合水平,唯一的例外是苍白球,其表现出非常小但具有统计学意义的增加。此外,用WIN 55,212-2激活大麻素受体可增加大多数所检测结构中的[35S]GTPγS结合。在吗啡依赖小鼠和对照小鼠中增加幅度相似,除了黑质,在基础条件下吗啡依赖小鼠的[35S]GTPγS结合水平较低,尽管WIN 55,212-2刺激后的结合显著更高。然而,其他结构,如中脑导水管周围灰质,在对照小鼠中激动剂诱导的刺激较弱,但在吗啡依赖小鼠中表现出较高水平的WIN 55,212-2刺激的[35S]GTPγS结合,而这些动物在基础条件下往往表现出较高的[35S]GTPγS结合水平,尽管在大脑皮层深层WIN 55,212-2刺激后的结合较少且无统计学意义。因此,数据支持吗啡在大麻素受体与GTP结合蛋白偶联方面存在特定作用的可能性,而非对受体结合的作用,尽管这仅在黑质和中脑导水管周围灰质中观察到。

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