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Anxioselective anxiolytics: On a quest for the Holy Grail

机译:选择性抗焦虑药:寻求圣杯

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The discovery of benzodiazepine receptors provided the impetus to discover and develop anxioselective anxiolytics ('Valium without the side effects'). The market potential for an anxioselective based on the γ-aminobutyric acid A (GABA A) receptor resulted in clinical trials of multiple compounds. In contrast to the anxioselective profile displayed in preclinical models, compounds such as bretazenil, TPA023, and MRK 409 produced benzodiazepine-like side effects (sedation, dizziness) in Phase I studies, whereas alpidem and ocinaplon exhibited many of the characteristics of an anxioselective in the clinic. Alpidem was briefly marketed for the treatment of anxiety, but was withdrawn because of liver toxicity. Reversible elevations in liver enzymes halted development of ocinaplon in Phase III. The clinical profiles of these two molecules demonstrate that it is possible to develop GABA A receptor-based anxioselectives. However, despite the formidable molecular toolbox at our disposal, we are no better informed about the GABA A receptors responsible for an anxioselective profile in the clinic. Here, I discuss the evolution of a quest, spanning four decades, for molecules that retain the rapid and robust anti-anxiety actions of benzodiazepines without the side effects that limit their usefulness.
机译:苯并二氮杂receptor受体的发现为发现和开发抗焦虑药(“无副作用的安定”)提供了动力。基于γ-氨基丁酸A(GABA A)受体的抗焦虑药的市场潜力导致了多种化合物的临床试验。与临床前模型中显示的抗焦虑特性相反,化合物bretazenil,TPA023和MRK 409在I期研究中产生了类似苯二氮卓类的副作用(镇静,头晕),而阿立培南和ocinaplon则表现出许多抗焦虑特性。诊所。 Alpidem曾短暂上市用于治疗焦虑症,但由于肝毒性而被撤回。肝酶的可逆升高阻止了三期ocinaplon的发育。这两种分子的临床概况表明,有可能开发基于GABA A受体的焦虑选择性药物。然而,尽管有强大的分子工具箱可供使用,但我们对临床上负责焦虑选择性的GABA A受体的了解却更好。在这里,我讨论了寻找跨越四十年的分子的发展历程,这些分子保留了苯二氮卓类药物的快速而强大的抗焦虑作用,而又没有限制其有用性的副作用。

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