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运用选择性拮抗剂结合研究鉴定大鼠肺中的三种毒蕈碱受体亚型。

Identification of three muscarinic receptor subtypes in rat lung using binding studies with selective antagonists.

作者信息

Fryer A D, el-Fakahany E E

机构信息

Department of Pharmacology and Toxicology, School of Pharmacy, University of Maryland at Baltimore 21201.

出版信息

Life Sci. 1990;47(7):611-8. doi: 10.1016/0024-3205(90)90572-9.

DOI:10.1016/0024-3205(90)90572-9
PMID:2402185
Abstract

Heterogeneity of the muscarinic receptor population in the rat central and peripheral lung was found in competition binding experiments against [3H]quinuclidinyl benzilate [( 3H]QNB) using the selective antagonists pirenzepine, AF-DX 116 and hexahydrosiladifenidol (HHSiD). Pirenzepine displaced [3H]QNB with low affinity from preparations of central airways indicating the absence of M1 receptors in the trachea and bronchi. Muscarinic receptors in the central airways are comprised of both M2 and M3 receptors since AF-DX 116, an M2-selective antagonist, bound with high affinity to 70% of the available sites while HHSiD, an M3-selective antagonist bound with high affinity to the remaining binding sites. In the peripheral lung, pirenzepine bound with high affinity to 14% of the receptor population, AF-DX 116 bound with high affinity to 79% of the binding sites while HHSiD bound with high affinity to 18% of the binding sites. The presence of M1 receptors in the peripheral airways but not in the central airways was confirmed using [3H]telenzepine, an M1 receptor ligand. [3H]Telenzepine showed specific saturable binding to 8% of [3H]QNB labeled binding sites in homogenates of rat peripheral lung, while there was no detectable specific binding in homogenates of rat trachea or heart. The results presented here demonstrate that there are three muscarinic receptor subtypes in rat lungs, and that the distribution of the different subtypes varies within the lungs. Throughout the airways, the dominant muscarinic receptor subtype is M2. In the trachea and bronchi the remaining receptors are M3, while in the peripheral lungs, the remaining receptors are both M1 and M3.

摘要

利用选择性拮抗剂哌仑西平、AF-DX 116和六氢硅二苯酯(HHSiD),通过与[3H]喹核醇基苯甲酸酯[(3H]QNB)的竞争结合实验,发现大鼠中枢和外周肺中M胆碱能受体群体存在异质性。哌仑西平以低亲和力从中央气道制剂中置换[3H]QNB,表明气管和支气管中不存在M1受体。中央气道中的M胆碱能受体由M2和M3受体组成,因为M2选择性拮抗剂AF-DX 116以高亲和力结合到70%的可用位点,而M3选择性拮抗剂HHSiD以高亲和力结合到其余的结合位点。在外周肺中,哌仑西平以高亲和力结合到14%的受体群体,AF-DX 116以高亲和力结合到79%的结合位点,而HHSiD以高亲和力结合到18%的结合位点。使用M1受体配体[3H]替仑西平证实外周气道中存在M1受体,而中央气道中不存在。[3H]替仑西平在大鼠外周肺匀浆中与8%的[3H]QNB标记结合位点显示出特异性饱和结合,而在大鼠气管或心脏匀浆中未检测到特异性结合。此处呈现的结果表明,大鼠肺中有三种M胆碱能受体亚型,且不同亚型在肺内的分布有所不同。在整个气道中,占主导地位的M胆碱能受体亚型是M2。在气管和支气管中,其余受体是M3,而在外周肺中,其余受体是M1和M3。

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