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奥滕泽帕在人胃平滑肌中显示出两类结合位点。

Otenzepad shows two populations of binding sites in human gastric smooth muscle.

作者信息

Bellido I, Fernández J L, Gómez A, Sánchez de la Cuesta F

机构信息

Department of Pharmacology and Clinical Therapeutics, School of Medicine, University of Málaga, Spain.

出版信息

Can J Physiol Pharmacol. 1995 Jan;73(1):124-9. doi: 10.1139/y95-017.

Abstract

Cholinergic agonists and antagonists frequently used for gastrointestinal motility disorders often produce adverse effects. A possible explanation for this is the presence of similar muscarinic receptor subtypes on smooth muscle from different gastrointestinal organs. The aim of this study was to characterize muscarinic receptor subtypes in human gastric smooth muscle with receptor binding methods. N-[3H]Methylscopolamine ([3H]NMS) saturation experiments showed a homogeneous population of noninteracting binding sites (KD = 0.76 +/- 0.07 nM, Bmax = 46.94 +/- 3.69 fmol/mg of tissue protein, nH = 0.99 +/- 0.01). The rank order of inhibition of [3H]NMS binding by nonlabelled compounds was atropine >> otenzepad >> pirenzepine. Atropine and pirenzepine bound to a homogeneous population of binding sites. The inhibition of [3H]NMS binding by otenzepad showed two populations of receptors (nH < 1, p < 0.01), whose apparent Ki1 of 298 +/- 40 nM and apparent Ki2 of 3.463 +/- 0.62 mM were similar to those reported for the M2 and M3 muscarinic receptor subtypes. The M2 subtype was the more abundant of the two, representing 79.12 +/- 5.48% of the total population. We conclude that two muscarinic receptor subpopulations similar to the M2 and M3 subtypes are present in human gastric smooth muscle and that the M2-like receptor is the more abundant of the two.

摘要

常用于胃肠动力障碍的胆碱能激动剂和拮抗剂经常会产生不良反应。对此的一种可能解释是,不同胃肠器官的平滑肌上存在相似的毒蕈碱受体亚型。本研究的目的是用受体结合方法对人胃平滑肌中的毒蕈碱受体亚型进行表征。N-[3H]甲基东莨菪碱([3H]NMS)饱和实验显示存在一组均匀的非相互作用结合位点(KD = 0.76±0.07 nM,Bmax = 46.94±3.69 fmol/mg组织蛋白,nH = 0.99±0.01)。未标记化合物对[3H]NMS结合的抑制作用强度顺序为阿托品>>奥替溴铵>>哌仑西平。阿托品和哌仑西平与一组均匀的结合位点结合。奥替溴铵对[3H]NMS结合的抑制作用显示出两组受体(nH <1,p <0.01),其表观Ki1为298±40 nM,表观Ki2为3.463±0.62 mM,与报道的M2和M3毒蕈碱受体亚型相似。两种亚型中M2亚型更为丰富,占总群体的79.12±5.48%。我们得出结论,人胃平滑肌中存在与M2和M3亚型相似的两个毒蕈碱受体亚群,且M2样受体在两者中更为丰富。

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