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克隆化阿片受体的分子生物学与药理学

Molecular biology and pharmacology of cloned opioid receptors.

作者信息

Knapp R J, Malatynska E, Collins N, Fang L, Wang J Y, Hruby V J, Roeske W R, Yamamura H I

机构信息

Department of Pharmacology, University of Arizona, Tucson 85724, USA.

出版信息

FASEB J. 1995 Apr;9(7):516-25. doi: 10.1096/fasebj.9.7.7737460.

Abstract

The cloning and expression of DNA for the three major opioid receptor types (mu, delta, and kappa) present new research opportunities for the characterization of opioid drugs and their interactions with these receptors. Genomic and cDNA clones for opioid receptors exist for several animal species including mouse, rat, guinea pig, and human. These include clones for all three human opioid receptor types. The receptor proteins consist of about 400 amino acids and have the characteristic seven transmembrane domain structure of G-protein-coupled receptors. There is about 60% amino acid identity between opioid receptor types and about 90% identity between a receptor type cloned from different animal species. All opioid receptor types mediate the inhibition of adenylyl cyclase in response to agonist binding. Radioligand binding and functional studies using the cloned receptors tend to support current conclusions on opioid drug receptor selectivity and activity. Investigations of opioid receptor chimeras and single amino acid mutants are providing information on the ligand recognition sites of these receptors and essential support for the development of computational opioid receptor models. A molecular model of the human delta opioid receptor is included in this review.

摘要

三种主要阿片受体类型(μ、δ和κ)的DNA克隆与表达为阿片类药物的特性及其与这些受体的相互作用研究带来了新机遇。包括小鼠、大鼠、豚鼠和人类在内的多种动物物种都存在阿片受体的基因组和cDNA克隆。其中包括所有三种人类阿片受体类型的克隆。受体蛋白由约400个氨基酸组成,具有G蛋白偶联受体特有的七跨膜结构域。阿片受体类型之间的氨基酸同一性约为60%,从不同动物物种克隆的同一受体类型之间的同一性约为90%。所有阿片受体类型在激动剂结合后都会介导腺苷酸环化酶的抑制。使用克隆受体进行的放射性配体结合和功能研究倾向于支持目前关于阿片类药物受体选择性和活性的结论。对阿片受体嵌合体和单氨基酸突变体的研究正在提供有关这些受体配体识别位点的信息,并为计算阿片受体模型的开发提供重要支持。本综述中包含了人类δ阿片受体的分子模型。

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