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Partial mGlu5 Negative Allosteric Modulators Attenuate Cocaine-Mediated Behaviors and Lack Psychotomimetic-Like Effects

机译:局部mGlu5负变构调节剂减弱可卡因介导的行为并缺乏类似拟精神病药物的作用

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摘要

Cocaine abuse remains a public health concern for which pharmacotherapies are largely ineffective. Comorbidities between cocaine abuse, depression, and anxiety support the development of novel treatments targeting multiple symptom clusters. Selective negative allosteric modulators (NAMs) targeting the metabotropic glutamate receptor 5 (mGlu5) subtype are currently in clinical trials for the treatment of multiple neuropsychiatric disorders and have shown promise in preclinical models of substance abuse. However, complete blockade or inverse agonist activity by some full mGlu5 NAM chemotypes demonstrated adverse effects, including psychosis in humans and psychotomimetic-like effects in animals, suggesting a narrow therapeutic window. Development of partial mGlu5 NAMs, characterized by their submaximal but saturable levels of blockade, may represent a novel approach to broaden the therapeutic window. To understand potential therapeutic vs adverse effects in preclinical behavioral assays, we examined the partial mGlu5 NAMs, M-5MPEP and Br-5MPEPy, in comparison with the full mGlu5 NAM MTEP across models of addiction and psychotomimetic-like activity. M-5MPEP, Br-5MPEPy, and MTEP dose-dependently decreased cocaine self-administration and attenuated the discriminative stimulus effects of cocaine. M-5MPEP and Br-5MPEPy also demonstrated antidepressant- and anxiolytic-like activity. Dose-dependent effects of partial and full mGlu5 NAMs in these assays corresponded with increasing in vivo mGlu5 occupancy, demonstrating an orderly occupancy-to-efficacy relationship. PCP-induced hyperlocomotion was potentiated by MTEP, but not by M-5MPEP and Br-5MPEPy. Further, MTEP, but not M-5MPEP, potentiated the discriminative-stimulus effects of PCP. The present data suggest that partial mGlu5 NAM activity is sufficient to produce therapeutic effects similar to full mGlu5 NAMs, but with a broader therapeutic index.
机译:可卡因滥用仍然是一个公共卫生问题,药物治疗在很大程度上没有效果。可卡因滥用,抑郁和焦虑症之间的合并症支持针对多种症状群的新型疗法的发展。目前,针对代谢型谷氨酸受体5(mGlu5)亚型的选择性负变构调节剂(NAM)正在临床试验中,用于治疗多种神经精神疾病,并且在药物滥用的临床前模型中显示出了希望。但是,某些完全的mGlu5 NAM化学型完全阻断或反向激动剂的活性显示出不良反应,包括人的精神病和动物的拟精神病药样作用,这表明治疗范围狭窄。部分mGlu5 NAM的发展以其亚最大但可饱和的阻断水平为特征,可能代表了一种拓宽治疗范围的新颖方法。为了了解临床前行为分析中潜在的治疗效果与不良反应,我们比较了成瘾和拟精神活性模型中的部分mGlu5 NAM,M-5MPEP和Br-5MPEPy,并与完整的mGlu5 NAM MTEP进行了比较。 M-5MPEP,Br-5MPEPy和MTEP剂量依赖性地减少了可卡因的自我给药,并减弱了可卡因的歧视性刺激作用。 M-5MPEP和Br-5MPEPy也表现出抗抑郁和抗焦虑样活性。在这些测定中,部分和全部mGlu5 NAM的剂量依赖性效应与体内mGlu5占有率增加相对应,表明了有序的占有率与功效关系。 PCP诱导的运动过度被MTEP增强,但未被M-5MPEP和Br-5MPEPy增强。此外,MTEP而非M-5MPEP增强了PCP的歧视性刺激作用。目前的数据表明,部分mGlu5 NAM活性足以产生类似于完整mGlu5 NAM的治疗效果,但具有更宽的治疗指数。

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