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Glutamate receptor antagonists with the potential for migraine treatment

偏头痛 临床试验 医学 谷氨酸的 偏头痛治疗 皮质扩散性抑郁症 神经科学 药理学 谷氨酸受体 伤害 生物信息学 受体 麻醉 心理学 内科学 生物
作者
Anna Ferrari,Cecilia Rustichelli,Carlo Baraldi
出处
期刊:Expert Opinion on Investigational Drugs [Taylor & Francis]
卷期号:26 (12): 1321-1330 被引量:12
标识
DOI:10.1080/13543784.2017.1395411
摘要

Preclinical, clinical, and other (e.g., genetic) evidence support the concept that migraine susceptibility may at least partially result from a glutamatergic system disorder. Therefore, the receptors of the glutamatergic system are considered relatively new targets for investigational drugs to treat migraine. Investigational and established glutamate receptor antagonists (GluRAs) have been shown to possess antinociceptive properties in preclinical models of trigeminovascular nociception and have been evaluated in clinical trials. This review focuses on preclinical and clinical studies of GluRAs for the treatment of migraine. Areas covered: A PubMed database search (from 1987 to December 2016) and a review of published studies on GluRAs in migraine were conducted. Expert opinion: All published clinical trials of investigational GluRAs have been unsuccessful in establishing benefit for acute migraine treatment. Clinical trial results contrast with the preclinical data, suggesting that glutamate (Glu) does not play a decisive role after the attack has already been triggered. These antagonists may instead be useful for migraine prophylaxis. Improving patient care requires further investigating and critically analyzing the role of Glu in migraine, designing experimental models to study more receptors and their corresponding antagonists, and identifying biomarkers to facilitate trials designed to target specific subgroups of migraine patients.
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