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Glutamate-based anxiolytic ligands in clinical trials

机译:基于谷氨酸的抗焦虑配体的临床试验

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Introduction: With regard to anxiety, the role of the balance between glutamatergic and GABAergic systems was pursued for many years. The majority of drugs used presently as effective anxiolytics enhance the GABAergic system activity, thus increasing inhibition within the central nervous system (CNS). On the other hand, decreasing the activity of glutamatergic neurotransmission may attenuate excitation in the CNS, thus resulting in anxiolysis. Areas covered: The present review focuses on clinical data of well-known and recently discovered glutamatergic and, to a lesser extent, GABAergic agents, which reached at least the Phase II criteria. Expert opinion: A variety of glutamatergic agents active at both N-acetylo-d-asparaginian and metabotropic glutamate (mGlu) receptors have been tested in humans to examine their potential anxiolytic activity. Many compounds acting on the glutamatergic system and approved for the treatment of other disorders than anxiety were shown to exert anxiolytic effects in clinical trials. Those are mainly voltage-dependent ion channel ligands as well as d-cycloserin and memantine. Also, ligands active at mGlu receptors, such as fenobam and LY354740, exhibited activity in controlled clinical trials. However, relatively few trials are found on the agents that are focused on GABAergic neurotransmission. Therefore, it seems that glutamatergic system may become a novel target for modern and effective anxiolytics.
机译:简介:关于焦虑症,人们一直在追求谷氨酸能和GABA能系统之间的平衡。目前用作有效的抗焦虑药的大多数药物增强了GABA能系统的活性,从而增加了中枢神经系统(CNS)的抑制作用。另一方面,降低谷氨酸能神经传递的活性可能会减弱中枢神经系统的兴奋性,从而导致焦虑症。涵盖领域:本综述着重于已知和最近发现的谷氨酸能药物以及较少程度达到至少II期标准的GABA能药物的临床数据。专家意见:已在人体中测试了对N​​-乙酰基-d-天冬酰胺和代谢型谷氨酸(mGlu)受体均具有活性的多种谷氨酸能药物,以检查其潜在的抗焦虑活性。在临床试验中,许多作用于谷氨酸能系统并被批准用于治疗除焦虑症以外的疾病的化合物均表现出抗焦虑作用。这些主要是电压依赖性离子通道配体以及d-环丝氨酸和美金刚。同样,对mGlu受体有活性的配体(如fenobam和LY354740)在受控的临床试验中也具有活性。但是,发现针对GABA能神经传递的药物的试验相对较少。因此,似乎谷氨酸能系统可能成为现代有效的抗焦虑药的新靶标。

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