Receptorome screening: a powerful, facile approach to better understand and engineer drugs.

Drug news & perspectives Pub Date : 2009-10-01
Vincent Setola
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引用次数: 0

Abstract

Receptorome screening is the process of characterizing one or more compounds for pharmacological activity (e.g., inhibition of radioligand binding, positive or negative efficacy) at a large panel of 'targets' (e.g., biologically relevant recombinant G protein-coupled receptors, ion channels and small-molecule transporters). Recently, receptorome profiles have led to mechanistic insights into the actions -both intentional and adverse- of several drugs. In the present review, I discuss in detail how receptorome screening increased our understanding of three drugs (salvinorin A, amisulpride and fenfluramine) and a class of medications (atypical antipsychotics). The cases presented suggest that receptorome screening of current medications, as well as investigational drugs and future compounds destined for use in humans, might enable us to predict salutary effects, as well as side effects, at the preclinical stage, which would have important economic and public health implications.

受体组筛选:一种强大、便捷的方法,可以更好地理解和设计药物。
受体组筛选是表征一种或多种化合物在大量“靶标”(例如,生物相关的重组G蛋白偶联受体、离子通道和小分子转运体)上的药理活性(例如,抑制放射性配体结合、阳性或阴性功效)的过程。最近,受体组的概况导致了对几种药物的作用(包括有意的和不利的)的机制见解。在本综述中,我详细讨论了受体组筛选如何增加我们对三种药物(salvinorin A, amisulpride和fenfluramine)和一类药物(非典型抗精神病药物)的理解。上述案例表明,对现有药物以及研究药物和未来用于人类的化合物进行受体组筛选,可能使我们能够在临床前阶段预测有益效果和副作用,这将具有重要的经济和公共卫生意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Drug news & perspectives
Drug news & perspectives 医学-药学
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