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Antiaversive Effects of Cannabinoids: Is the Periaqueductal Gray Involved?

机译:大麻素的反转效果:是涉及的幽面纱灰色吗?

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Cannabinoids play an important role in activity-dependent changes in synaptic activity and can interfere in several brain functions, including responses to aversive stimuli. The regions responsible for their effects, however, are still unclear. Cannabinoid type 1 (CB1) receptors are widely distributed in the central nervous system and are present in the periaqueductal gray (PAG), a midbrain structure closely involved in responses related to aversive states. Accordingly, exposure to stressful stimuli increases endocannabinoid (eCB) levels in the PAG, and local administration of CB1 agonists or drugs that facilitate eCB-mediated neurotransmission produces antinociceptive and antiaversive effects. To investigate if these drugs would also interfere in animal models that are sensitive to anxiolytic drugs, we verified the responses to intra-PAG injection of CB1 agonists in rats submitted to the elevated plus-maze, the Vogel punished licking test, or contextual aversive conditioning model. The drugs induced anxiolytic-like effects in all tests. The same was observed with the transient receptor potential vanilloid type 1 (TRPV1) antagonist capsazepine and with cannabidiol, a nonpsychotomimetic phytocannabinoid that produces anxiolytic-like effects after systemic administration in humans and laboratory animals. These results, therefore, suggest that the PAG could be an important site for the antiaversive effects of cannabinoids.
机译:大麻素在突触活动的活动依赖性变化中发挥着重要作用,并且可以干扰几个大脑功能,包括对厌恶刺激的反应。然而,负责其效果的地区仍然不清楚。大麻素类型1(CB1)受体广泛分布在中枢神经系统中,并且存在于Periaqueyuctal灰色(PAG)中,中脑结构紧密参与与厌恶国家相关的反应。因此,暴露于施力刺激的暴露增加了PAG中的内胆蛋白(ECB)水平,并且局部施用CB1激动剂或促进ECB介导的神经递血的药物产生抗痛性和抗抗激化作用。调查这些药物如果这些药物也会干扰对抗氧性药物敏感的动物模型,我们验证了对提交的大鼠CB1激动剂的CB1激动剂内注射的反应,Vogel惩罚舔测试或上下文厌恶调理模型。药物在所有测试中引起抗焦虑效果。通过瞬态受体潜在的香草型1(TRPV1)拮抗剂胶囊化合物和大麻,一种非肌肉染色植物植物,一种相同的瞬时受体潜在的肺脂瘤,一种在人类和实验室动物中的系统施用后产生抗焦虑症状的抗精性植物。因此,这些结果表明PAG可能是大麻素对抗抗助性作用的重要部位。

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