以谷氨酸为靶点的焦虑治疗进展

Asher B. Simon, Jack M. Gorman
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引用次数: 44

摘要

我们目前对焦虑症的精神药理学治疗显示出许多缺点,包括令人烦恼的副作用和缺乏主要效果。尽管在过去的几十年里已经开发了许多新药,但大多数都是基于这些疾病发病机理的过时理论(即单胺假说),因此阻碍了我们创造更具体和有效的干预措施的能力。然而,最近,神经生物学文献显示了集中在焦虑障碍中的谷氨酸能系统的发现,以及针对这些受体的药理学工具的发展,导致了对人类和动物都具有抗焦虑作用的新型治疗方法的发展。此外,由于该系统有望成为焦虑症发病机制的最终共同途径,我们可能能够采用谷氨酸特异性神经成像技术(例如,n -乙酰-天冬氨酸,GLX)来指导治疗决策,并为治疗效果提供可靠的客观生物标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Advances in the Treatment of Anxiety: Targeting Glutamate

Our current psychopharmacological treatments for anxiety disorders evince a number of shortcomings, including troublesome side effects and lack of primary effects. Whereas many new drugs have been developed in the past few decades, most are based on outmoded theories of the pathogenesis of these disorders (i.e., monoamine hypotheses), thus frustrating our ability to create more specific and effective interventions. Recently, however, the neurobiological literature has shown a convergence of findings focusing on the glutamatergic system in anxiety disorders, and the growth of pharmacological tools targeting these receptors has led to the development of novel treatments having anxiolytic effects in humans and animals alike. Additionally, as this system is showing promise as a final common pathway in the pathogenesis of anxiety disorders, we may be able to employ glutamate-specific neuroimaging techniques (e.g., N-acetyl-aspartate, GLX) to both guide treatment decisions and present reliable objective biomarkers for treatment efficacy.

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