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WIN 55212-2对大鼠脑内大麻素受体的激活会导致其与多种具有不同亲和力的G蛋白α亚基偶联。

Activation of cannabinoid receptors in rat brain by WIN 55212-2 produces coupling to multiple G protein alpha-subunits with different potencies.

作者信息

Prather P L, Martin N A, Breivogel C S, Childers S R

机构信息

Department of Pharmacology and Toxicology, University of Arkansas for Medical Sciences, Little Rock, AR 72205, USA.

出版信息

Mol Pharmacol. 2000 May;57(5):1000-10.

Abstract

Previous studies had shown that the amplification factors for cannabinoid receptors, defined as the number of total G proteins activated per occupied receptor, differs between several rat brain regions. In this study, we sought to determine which specific Gi/Go(alpha) subunits were activated by CB1 receptors in several rat brain regions and if this coupling might explain the regional differences in receptor/G protein amplification factors. Furthermore, we examined whether cannabinoid agonists might activate different subtypes of G(alpha) subunits with varying degrees of efficacy and/or potency. Activation of specific G proteins by cannabinoid receptors was evaluated by the ability of the agonist WIN 55212-2 to stimulate incorporation of [alpha-(32)P]azidoanilido-GTP into G(alpha) subunits in membranes. Photolabeled G proteins were either directly resolved using urea/SDS-polyacrylamide gel electrophoresis or first immunoprecipitated with specific antisera for different G(alpha) subunits before electrophoresis. Individual G(alpha) subunits were separated into distinct bands on a single gel and the amount of agonist-induced increase in radioactivity was quantified by densitometry. Stimulation of CB1 receptors by WIN 55212-2 resulted in the activation of a distinct pattern of at least five different G(ialpha)/G(oalpha) subunits in several brain regions. Furthermore, although the pattern of G proteins activated by WIN 55212-2 appeared to be similar across brain regions, slight differences were observed in both the percentage of increase and the amount of the individual G(alpha) subunits activated. Most importantly, the amount of WIN 55212-2 required to half-maximally activate individual G proteins in the cerebellum varied over a 30-fold range for different G(alpha) subunits. These results suggest that cannabinoid receptors activate multiple G proteins simultaneously in several brain regions and both the efficacy and potency of cannabinoid agonists to activate individual G(alpha) subunits may vary considerably.

摘要

先前的研究表明,大麻素受体的放大因子(定义为每个被占据的受体激活的总G蛋白数量)在大鼠的几个脑区之间存在差异。在本研究中,我们试图确定在大鼠的几个脑区中,CB1受体激活了哪些特定的Gi/Go(α)亚基,以及这种偶联是否可以解释受体/G蛋白放大因子的区域差异。此外,我们还研究了大麻素激动剂是否可能以不同程度的效力和/或效能激活不同亚型的G(α)亚基。通过激动剂WIN 55212-2刺激[α-(32)P]叠氮苯胺基-GTP掺入膜中的G(α)亚基的能力,来评估大麻素受体对特定G蛋白的激活作用。光标记的G蛋白要么直接使用尿素/SDS-聚丙烯酰胺凝胶电泳进行分离,要么在电泳前先用针对不同G(α)亚基的特异性抗血清进行免疫沉淀。单个G(α)亚基在单一凝胶上被分离成不同的条带,激动剂诱导的放射性增加量通过密度测定法进行定量。WIN 55212-2对CB1受体的刺激导致在几个脑区中至少五种不同的G(iα)/G(oα)亚基被激活,呈现出独特的模式。此外,尽管WIN 55212-2激活的G蛋白模式在不同脑区看起来相似,但在激活的单个G(α)亚基的增加百分比和数量上都观察到了细微差异。最重要的是,在小脑中,对于不同的G(α)亚基,半最大激活单个G蛋白所需的WIN 55212-2量在30倍的范围内变化。这些结果表明,大麻素受体在几个脑区中同时激活多种G蛋白,并且大麻素激动剂激活单个G(α)亚基的效力和效能可能有很大差异。

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