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对缺乏μ-阿片受体基因的小鼠的脑和脊髓中的腺苷受体及NBTI敏感的腺苷转运体进行定量放射自显影。

Quantitative autoradiography of adenosine receptors and NBTI-sensitive adenosine transporters in the brains and spinal cords of mice deficient in the mu-opioid receptor gene.

作者信息

Bailey Alexis, Matthes Hans, Kieffer Brigitte, Slowe Susan, Hourani Susanna M O, Kitchen Ian

机构信息

Pharmacology Group, School of Biomedical and Life Sciences, University of Surrey, Guildford, UK.

出版信息

Brain Res. 2002 Jul 5;943(1):68-79. doi: 10.1016/s0006-8993(02)02536-2.

Abstract

There is a large body of evidence indicating important interactions between the adenosine and opioid systems in regulating pain at both the spinal and supraspinal level. Mice lacking the mu-opioid receptor (MOR) gene have been successfully developed and the animals show complete loss of analgesic responses to morphine as well as differences in pain sensitivity. To investigate if there are any compensatory alterations in adenosine systems in mutant animals, we have carried out quantitative autoradiographic mapping of A(1) and A(2A) adenosine receptors and nitrobenzylthioinosine (NBTI) sensitive adenosine transporters in the brains and spinal cords of wild type, heterozygous and homozygous mu-opioid receptor knockout mice. Adjacent coronal sections were cut from the brains and spinal cords of +/+, +/- and -/- mice for the determination of binding of [3H]DPCPX, [3H]CGS21680 or [3H]NBTI to A(1) and A(2A) adenosine receptors and NBTI-sensitive adenosine transporters, respectively. A small but significant reduction in [3H]DPCPX and [3H]NBTI binding was detected in mutant mice brains but not in spinal cords. No significant change in A(2A) binding was detected in mu-opioid receptor knockout brains. The results suggest there may be functional interactions between mu-receptors and A(1) adenosine receptors as well as NBTI-sensitive adenosine transporters in the brain but not in the spinal cord.

摘要

有大量证据表明,腺苷系统和阿片样物质系统在脊髓和脊髓上水平调节疼痛过程中存在重要相互作用。缺乏μ-阿片受体(MOR)基因的小鼠已成功培育出来,这些动物对吗啡的镇痛反应完全丧失,且疼痛敏感性存在差异。为了研究突变动物的腺苷系统是否存在任何代偿性改变,我们对野生型、杂合子和纯合子μ-阿片受体敲除小鼠的脑和脊髓中的A(1)和A(2A)腺苷受体以及对硝基苄硫肌苷(NBTI)敏感的腺苷转运体进行了定量放射自显影定位。从+/+、+/-和-/-小鼠的脑和脊髓中切取相邻的冠状切片,分别用于测定[3H]DPCPX、[3H]CGS21680或[3H]NBTI与A(1)和A(2A)腺苷受体以及对NBTI敏感的腺苷转运体的结合。在突变小鼠的脑中检测到[3H]DPCPX和[3H]NBTI结合有小幅但显著的减少,但在脊髓中未检测到。在μ-阿片受体敲除的脑中未检测到A(2A)结合有显著变化。结果表明,μ-受体与A(1)腺苷受体以及脑中对NBTI敏感的腺苷转运体之间可能存在功能相互作用,但在脊髓中不存在。

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