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离体兔主动脉中5-羟色胺(5-HT2)受体激动剂效能的动力学定义。

Kinetic definition of agonist efficacy at a 5-hydroxytryptamine (5-HT2) receptor in the isolated rabbit aorta.

作者信息

Cory R N, Osman R, Maayani S

出版信息

J Pharmacol Exp Ther. 1986 Jan;236(1):48-54.

PMID:3001293
Abstract

The contractile response of the isolated rabbit aorta elicited by 5-hydroxytryptamine (5-HT) and five partial agonists acting on the 5-HT2 receptor were separated into a phasic and a tonic response by altering the [Ca++] in the buffer. A kinetic analysis of the two responses yields parameters that provide a mechanistic insight into the different nature of these responses. The kinetic parameters of the phasic contraction indicate that the onset of this response depends on the access of the drug to the receptor and that its decay is independent of the nature and the concentration of the agonist. The observed rate constant of the onset of the tonic response, kobs, is saturable with increasing drug concentration, suggesting that the rate determining step is the activation of an effector by the preformed drug-receptor complex. These kinetic characteristics of the 5-HT2-mediated response are similar to those observed previously by us for the alpha-1 adrenergic receptor-mediated response in the rabbit aorta, suggesting that these receptors activate similar mechanisms related to the mobilization of Ca++. Furthermore, it is shown that the maximal values of kobs for the 5-HT2 agonists follow the rank order of maximal amplitudes of the phasic responses and the maximal steady-state levels of the tonic response. It is suggested that the maximal value of kobs may serve as a kinetic measure of drug efficacy.

摘要

通过改变缓冲液中的[Ca++],将5-羟色胺(5-HT)及作用于5-HT2受体的五种部分激动剂引发的离体兔主动脉收缩反应分为相性反应和紧张性反应。对这两种反应进行动力学分析得出的参数,为深入了解这些反应的不同性质提供了机制上的见解。相性收缩的动力学参数表明,该反应的起始取决于药物与受体的结合,其衰减与激动剂的性质和浓度无关。观察到的紧张性反应起始速率常数kobs,会随着药物浓度的增加而达到饱和,这表明速率决定步骤是预先形成的药物-受体复合物对效应器的激活。5-HT2介导反应的这些动力学特征与我们之前在兔主动脉中观察到的α-1肾上腺素能受体介导反应的特征相似,这表明这些受体激活了与Ca++动员相关的类似机制。此外,研究表明,5-HT2激动剂的kobs最大值遵循相性反应最大幅度和紧张性反应最大稳态水平的排序。有人提出,kobs的最大值可能作为药物疗效的动力学指标。

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