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Cannabinoids and Vanilloids in Schizophrenia: Neurophysiological Evidence and Directions for Basic Research

机译:精神分裂症中的大麻素和香草类化合物:神经生理学证据和基础研究方向。

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Much of our knowledge of the endocannabinoid system in schizophrenia comes from behavioral measures in rodents, like prepulse inhibition of the acoustic startle and open-field locomotion, which are commonly used along with neurochemical approaches or drug challenge designs. Such methods continue to map fundamental mechanisms of sensorimotor gating, hyperlocomotion, social interaction, and underlying monoaminergic, glutamatergic, and GABAergic disturbances. These strategies will require, however, a greater use of neurophysiological tools to better inform clinical research. In this sense, electrophysiology and viral vector-based circuit dissection, like optogenetics, can further elucidate how exogenous cannabinoids worsen (e.g., tetrahydrocannabinol, THC) or ameliorate (e.g., cannabidiol, CBD) schizophrenia symptoms, like hallucinations, delusions, and cognitive deficits. Also, recent studies point to a complex endocannabinoid-endovanilloid interplay, including the influence of anandamide (endogenous CB_(1)and TRPV_(1)agonist) on cognitive variables, such as aversive memory extinction. In fact, growing interest has been devoted to TRPV_(1)receptors as promising therapeutic targets. Here, these issues are reviewed with an emphasis on the neurophysiological evidence. First, we contextualize imaging and electrographic findings in humans. Then, we present a comprehensive review on rodent electrophysiology. Finally, we discuss how basic research will benefit from further combining psychopharmacological and neurophysiological tools.
机译:我们对精神分裂症中的内源性大麻素系统的大部分了解来自啮齿动物的行为测量,例如声惊吓的预脉冲抑制和开阔地运动,它们通常与神经化学方法或药物挑战性设计一起使用。此类方法继续绘制感觉运动门控,运动过度,社交互动以及潜在的单胺能,谷氨酸能和GABA能干扰的基本机制。然而,这些策略将需要更多地使用神经生理学工具来更好地为临床研究提供信息。从这个意义上讲,电生理学和基于病毒载体的电路解剖,如光遗传学,可以进一步阐明外源性大麻素如何恶化(例如四氢大麻酚,THC)或减轻(例如幻觉,妄想和认知缺陷)精神分裂症症状(例如, 。同样,最近的研究指出了复杂的内源性大麻素-内源性香草素相互作用,包括anandamide(内源性CB_(1)和TRPV_(1)激动剂)对认知变量(例如厌恶性记忆消失)的影响。实际上,人们越来越关注TRPV_(1)受体作为有希望的治疗靶标。在这里,对这些问题进行了回顾,重点是神经生理学证据。首先,我们将人类的成像和电子照相结果与环境联系起来。然后,我们提出了对啮齿动物电生理的全面综述。最后,我们讨论了进一步结合心理药理学和神经生理学工具将如何使基础研究受益。

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