New Developments on the Adenosine Mechanisms of the Central Effects of Caffeine and Their Implications for Neuropsychiatric Disorders.

IF 1.7 Q4 Pharmacology, Toxicology and Pharmaceutics
Journal of Caffeine and Adenosine Research Pub Date : 2018-12-01 Epub Date: 2018-12-07 DOI:10.1089/caff.2018.0017
Sergi Ferré, Manuel Díaz-Ríos, John D Salamone, Rui Daniel Prediger
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引用次数: 33

Abstract

Recent studies on interactions between striatal adenosine and dopamine and one of its main targets, the adenosine A2A receptor-dopamine D2 receptor (A2AR-D2R) heteromer, have provided a better understanding of the mechanisms involved in the psychostimulant effects of caffeine and have brought forward new data on the mechanisms of operation of classical orthosteric ligands within G protein-coupled receptor heteromers. The striatal A2AR-D2R heteromer has a tetrameric structure and forms part of a signaling complex that includes a Gs and a Gi protein and the effector adenyl cyclase (subtype AC5). Another target of caffeine, the adenosine A1 receptor-dopamine D1 receptor (A1R-D1R) heteromer, seems to have a very similar structure. Initially suggested to be localized in the striatum, the A1R-D1R heteromer has now been identified in the spinal motoneuron and shown to mediate the spinally generated caffeine-induced locomotion. In this study, we review the recently discovered properties of A2AR-D2R and A1R-D1R heteromers. Our studies demonstrate that these complexes are a necessary condition to sustain the canonical antagonistic interaction between a Gs-coupled receptor (A2AR or D1R) and a Gi-coupled receptor (D2R or A1R) at the adenylyl cyclase level, which constitutes a new concept in the field of G protein-coupled receptor physiology and pharmacology. A2AR antagonists targeting the striatal A2AR-D2R heteromer are already being considered as therapeutic agents in Parkinson's disease. In this study, we review the preclinical evidence that indicates that caffeine and A2AR antagonists could be used to treat the motivational symptoms of depression and attention-deficit/hyperactivity disorder, while A1R antagonists selectively targeting the spinal A1R-D1R heteromer could be used in the recovery of spinal cord injury.

Abstract Image

咖啡因中枢效应的腺苷机制及其对神经精神疾病的影响的新进展。
近年来对纹状体腺苷与多巴胺及其主要靶点之一腺苷A2A受体-多巴胺D2受体(A2AR-D2R)异聚体相互作用的研究,使我们对咖啡因的精神兴奋作用机制有了更好的了解,并对G蛋白偶联受体异聚体中经典正位配体的作用机制提供了新的数据。纹状体A2AR-D2R异聚体具有四聚体结构,是信号复合体的一部分,该复合体包括Gs和Gi蛋白以及效应腺苷环化酶(亚型AC5)。咖啡因的另一个目标,腺苷A1受体-多巴胺D1受体(A1R-D1R)异聚体,似乎有着非常相似的结构。A1R-D1R异聚体最初被认为定位于纹状体,现在已经在脊髓运动神经元中被发现,并被证明介导脊髓产生的咖啡因诱导的运动。本文综述了近年来发现的A2AR-D2R和A1R-D1R异构体的性质。我们的研究表明,这些复合物是维持gs偶联受体(A2AR或D1R)与gi偶联受体(D2R或A1R)在腺苷酸环化酶水平上的典型拮抗相互作用的必要条件,构成了G蛋白偶联受体生理学和药理学领域的新概念。针对纹状体A2AR- d2r异构体的A2AR拮抗剂已经被认为是帕金森病的治疗药物。在本研究中,我们回顾了临床前证据,表明咖啡因和A2AR拮抗剂可用于治疗抑郁症和注意缺陷/多动障碍的动机症状,而选择性靶向脊髓A1R- d1r异构体的A1R拮抗剂可用于脊髓损伤的恢复。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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