首页> 外文期刊>Journal of Medicinal Chemistry >Adenosine A(2A) Receptor-Antagonist/Dopamine D-2 Receptor-Agonist Bivalent Ligands as Pharmacological Tools to Detect A(2A)-D-2 Receptor Heteromers
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Adenosine A(2A) Receptor-Antagonist/Dopamine D-2 Receptor-Agonist Bivalent Ligands as Pharmacological Tools to Detect A(2A)-D-2 Receptor Heteromers

机译:腺苷A(2A)受体拮抗剂/多巴胺D-2受体激动剂二价配体作为检测A(2A)-D-2受体异构体的药理工具

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摘要

Adenosine A(2A) (A(2A)R) and dopamine D-2 (D2R) receptors mediate the antagonism between adenosinergic and dopaminergic transmission in striatopallidal GABAergic neurons and are pharmacological targets for the treatment of Parkinson's disease. Here, a family of heterobivalent ligands containing a D,R agonist and an A2AR antagonist linked through a spacer of variable size was designed and synthesized to study A(2A)R-D2R heteromers. Bivalent ligands with shorter linkers bound to D2R or A(2A)R with higher affinity than the corresponding monovalent controls in membranes from brain striatum and from cells coexpressing both receptors. In contrast, no differences in affinity of bivalent versus monovalent ligands were detected in experiments using membranes from cells expressing only one receptor. These findings indicate the existence of A(2A)R-D2R heteromers and of a simultaneous interaction of heterobivalent ligands with both receptors. The cooperative effect derived from the simultaneous interaction suggests the occurrence of A(2A)R-D2R heteromers in cotransfected cells and in brain striatum. The dopamine/adenosine bivalent action could constitute a novel concept in Parkinson's disease pharmacotherapy.
机译:腺苷A(2A)(A(2A)R)和多巴胺D-2(D2R)受体介导纹状体外层GABA能神经元中腺苷能和多巴胺能传递之间的拮抗作用,并且是治疗帕金森氏病的药理学靶标。在这里,设计并合成了一个包含D,R激动剂和一个通过可变大小的间隔子连接的A2AR拮抗剂的异二价配体家族,以研究A(2A)R-D2R异聚体。具有较短接头的二价配体以比大脑纹状体和共表达两种受体的细胞膜中相应的单价对照更高的亲和力与D2R或A(2A)R结合。相反,在使用仅表达一种受体的细胞的膜的实验中,没有发现二价配体与单价配体的亲和力差异。这些发现表明存在A(2A)R-D2R异聚体以及异双价配体与两个受体的同时相互作用。从同时相互作用中获得的协同效应表明在共转染的细胞和脑纹状体中发生了A(2A)R-D2R异聚体。多巴胺/腺苷的二价作用可能构成帕金森氏病药物治疗中的一个新概念。

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