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豚鼠脑中[3H]右美沙芬的放射自显影定位:罗哌嗪的变构增强作用

Autoradiographic localization of [3H]dextromethorphan in guinea pig brain: allosteric enhancement by ropizine.

作者信息

Canoll P D, Smith P R, Gottesman S, Musacchio J M

机构信息

Department of Pharmacology, NYU Medical Center, NY 10016.

出版信息

J Neurosci Res. 1989 Oct;24(2):311-28. doi: 10.1002/jnr.490240224.

Abstract

Dextromethorphan (DM) is an antitussive with anticonvulsant activity that binds to high- and low-affinity sites in guinea pig brain homogenates. We examined the autoradiographic localization of [3H]DM using the anticonvulsant ropizine, an allosteric modifier that decreases the dissociation rate of [3H]DM. Competition studies demonstrated that the binding to brain sections was identical to that of brain homogenates [Craviso and Musacchio: Mol Pharmacol 23:629-640, 1983b]. Computer-assisted quantitative analysis of the autoradiographic images demonstrated that [3H]DM binds to discrete structures throughout the brain, but with higher density in the midbrain, pons, and medulla oblongata. The most intense labeling was observed in the rhabdoid, dorsal raphe, median raphe, caudal linear raphe nuclei, and cranial motor nerve nuclei. The central gray showed moderate to high-density labeling throughout its entire rostro-caudal extent, with very high binding in the dorsal tegmental nucleus and the locus coeruleus. Moderate and high binding was also seen in several hypothalamic structures. Distinct bands of moderate binding were seen in the pyramidal cell layer of the piriform cortex, the retrosplenial cortex, the granular cell layer of the dentate gyrus, the pyramidal cell layer of the hippocampus, and the Purkinje cell layer of the cerebellum. The striking similarity between the binding distribution of [3H]DM and sigma ligands, plus competition studies in brain homogenate, support the hypothesis that DM and sigma ligands share a common high-affinity binding site [Musacchio et al: Mol Pharmacol 35:1-5, 1989]. The distribution of [3H]DM binding provides possible anatomical substrates for both the antitussive and anticonvulsant actions of DM.

摘要

右美沙芬(DM)是一种具有抗惊厥活性的镇咳药,它能与豚鼠脑匀浆中的高亲和力和低亲和力位点结合。我们使用抗惊厥药罗匹嗪(一种变构调节剂,可降低[3H]DM的解离速率)研究了[3H]DM的放射自显影定位。竞争研究表明,[3H]DM与脑切片的结合与脑匀浆的结合相同[Craviso和Musacchio:《分子药理学》23:629 - 640,1983b]。对放射自显影图像的计算机辅助定量分析表明,[3H]DM与整个大脑中的离散结构结合,但在中脑、脑桥和延髓中的密度更高。在横纹肌样、背侧中缝、中缝正中、尾侧线性中缝核和颅运动神经核中观察到最强的标记。中央灰质在其整个头尾范围内显示出中度至高密度标记,在背侧被盖核和蓝斑中有非常高的结合。在几个下丘脑结构中也观察到中度和高度结合。在梨状皮质的锥体细胞层、压后皮质、齿状回的颗粒细胞层、海马的锥体细胞层和小脑的浦肯野细胞层中可见明显的中度结合带。[3H]DM的结合分布与西格玛配体之间的惊人相似性,以及在脑匀浆中的竞争研究,支持了DM和西格玛配体共享一个共同的高亲和力结合位点的假说[Musacchio等人:《分子药理学》35:1 - 5,1989]。[3H]DM结合的分布为DM的镇咳和抗惊厥作用提供了可能的解剖学基础。

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Dextromethorphan binding sites in the guinea pig brain.豚鼠脑中右美沙芬结合位点
Cell Mol Neurobiol. 1988 Jun;8(2):149-56. doi: 10.1007/BF00711241.

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