首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >A simple method for estimation of agonist activity at receptor subtypes: comparison of native and cloned M3 muscarinic receptors in guinea pig ileum and transfected cells.
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A simple method for estimation of agonist activity at receptor subtypes: comparison of native and cloned M3 muscarinic receptors in guinea pig ileum and transfected cells.

机译:一种简单的评估受体亚型激动剂活性的方法:比较豚鼠回肠和转染细胞中天然和克隆的M3毒蕈碱受体。

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摘要

We describe a simple method for calculating the pharmacological activity of an agonist (A) relative to a standard agonist (S) using only the concentration-response curves of the two agonists. In most situations, we show that the product of the ratios of maximal responses (Emax - A/Emax - S) and potencies (EC50 - S/EC50 - A) is equivalent to the product of the affinity and intrinsic efficacy of A expressed relative to that of S. We refer to this term as the IRA value of A. In a cooperative system where the concentration-response curve of the standard agonist is steep and that of the test agonist is flatter with a lower maximal response, the simple calculation of IRA described above underestimates agonist activity; however, we also describe a means of correcting the IRA in this situation. We have validated our analysis with modeling techniques and have shown experimentally that the IRA values of muscarinic agonists for stimulating contractions in the guinea pig ileum (M3 response) are in excellent agreement with those measured in the phosphoinositide assay on Chinese hamster ovary cells expressing the M3 muscarinic receptor.
机译:我们描述了一种仅使用两种激动剂的浓度-响应曲线计算相对于标准激动剂(S)的激动剂(A)的药理活性的简单方法。在大多数情况下,我们显示最大响应(Emax-A / Emax-S)与效能(EC50-S / EC50-A)之比的乘积等于A表示的亲和力和内在功效的乘积我们将这个术语称为A的IRA值。在一个协作系统中,标准激动剂的浓度-响应曲线陡峭,测试激动剂的浓度-响应曲线较平坦,最大响应较低,因此简单计算上述IRA的研究低估了激动剂的活性;但是,我们还描述了一种在这种情况下纠正IRA的方法。我们已经通过建模技术验证了我们的分析结果,并通过实验表明毒蕈碱激动剂的IRA值可刺激豚鼠回肠收缩(M3反应),与磷酸肌醇测定法在表达M3的中国仓鼠卵巢细胞中测得的IRA值非常一致毒蕈碱受体。

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