激动剂亲和估计的解释:分布受体状态的问题。

J W Black, N P Shankley
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引用次数: 26

摘要

在药物激动作用的受体-换能器模型中,摈弃了受体分子大量过剩换能器分子的传统假设,允许受体在未结合、结合和复杂状态下分布。在这种情况下,当使用不可逆受体拮抗方法时,激动剂的亲和力容易被高估。已经开发了图形测试来检测分布,并将这些测试应用于5-HT和苯氧苄胺在主动脉组织上相互作用的实验数据。该方法未检测到显著的受体分布。然而,在模型中假设三元配合物浓度与药理作用之间存在线性关系。如果用饱和关系代替这种关系,受体分布的影响就会被掩盖。讨论了对药理学家和药物化学家的影响。
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Interpretation of agonist affinity estimations: the question of distributed receptor states.

In the receptor-transducer model of pharmacological agonism, rejection of the traditional assumption that receptor molecules are in vast excess of transducer molecules permits the receptors to become distributed among unbound, bound and complexed states. Under these conditions, agonist affinities are liable to be overestimated when the method of irreversible receptor antagonism is used. Graphical tests have been developed to detect distribution, and these were applied to experimental data from the interaction between 5-HT and phenoxybenzamine on aortic tissue. Significant receptor distribution was not detected by the method. However, in the model it was assumed that there was a linear relation between the concentration of ternary complex and pharmacological effect. If this relation was replaced with a saturable one the effect of receptor distribution would be masked. The implications for pharmacologists and medicinal chemists are discussed.

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Proceedings of the Royal Society of London Series B-Containing Papers of Abiological Character
Proceedings of the Royal Society of London Series B-Containing Papers of Abiological Character 生命科学, 发育生物学与生殖生物学, 发育生物学
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