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腹侧纹状体中的多巴胺D2异源受体复合物及其受体间相互作用:抗精神病药物的新靶点

Dopamine D2 heteroreceptor complexes and their receptor-receptor interactions in ventral striatum: novel targets for antipsychotic drugs.

作者信息

Fuxe Kjell, Borroto-Escuela Dasiel O, Tarakanov Alexander O, Romero-Fernandez Wilber, Ferraro Luca, Tanganelli Sergio, Perez-Alea Mileidys, Di Palma Michael, Agnati Luigi F

机构信息

Department of Neuroscience, Karolinska Institutet, Stockholm, Sweden.

Department of Neuroscience, Karolinska Institutet, Stockholm, Sweden.

出版信息

Prog Brain Res. 2014;211:113-39. doi: 10.1016/B978-0-444-63425-2.00005-2.

Abstract

This review is focused on the D2 heteroreceptor complexes within the ventral striatum with their receptor-receptor interactions and relevance for the treatment of schizophrenia. A "guide-and-clasp" manner for receptor-receptor interactions is proposed where "adhesive guides" may be amino acid triplet homologies, which were determined for different kinds of D2 heteroreceptor complexes. The first putative D2 heteroreceptor complex to be discovered in relation to schizophrenia was the A2A-D2 heteroreceptor complex where antagonistic A2A-D2 receptor-receptor interactions were demonstrated after A2A agonist treatment in the ventral striatum. The A2A agonist CGS 21680 with atypical antipsychotic properties may at least in part act by increasing β-arrestin2 signaling over the D2 protomer in the A2A-D2 heteroreceptor complex in the ventral striatum. The antagonistic NTS1-D2 interactions in the NTS1-D2 heteroreceptor complex in the ventral striatum are proposed as one molecular mechanism for the potential antipsychotic effects of NT. Indications were obtained that the psychotic actions of the 5-HT2AR hallucinogens LSD and DOI can involve enhancement of D2R protomer signaling via a biased agonist action at the 5-HT2A protomer in the D2-5-HT2A heteroreceptor complex in the ventral striatum. Facilitatory allosteric D2likeR-OTR interactions in heteroreceptor complexes in nucleus accumbens may have a role in social and emotional behaviors. By blocking the D2 protomers of these heteroreceptor complexes, antipsychotics can fail to reduce the negative symptoms of schizophrenia. The discovery of different types of D2 heteroreceptor complexes gives an increased understanding of molecular mechanisms involved in causing schizophrenia and new strategies for its treatment and understanding the side effects of antipsychotics.

摘要

本综述聚焦于腹侧纹状体内的D2异源受体复合物,及其受体 - 受体相互作用与精神分裂症治疗的相关性。本文提出了一种受体 - 受体相互作用的“引导 - 扣合”方式,其中“粘附引导物”可能是氨基酸三联体同源性,这是针对不同类型的D2异源受体复合物确定的。与精神分裂症相关的首个被发现的假定D2异源受体复合物是A2A - D2异源受体复合物,在腹侧纹状体中用A2A激动剂处理后,证实了其拮抗的A2A - D2受体 - 受体相互作用。具有非典型抗精神病特性的A2A激动剂CGS 21680可能至少部分通过增强腹侧纹状体中A2A - D2异源受体复合物中D2原聚体上的β - 抑制蛋白2信号传导来发挥作用。腹侧纹状体中NTS1 - D2异源受体复合物中的拮抗NTS1 - D2相互作用被认为是神经降压素潜在抗精神病作用的一种分子机制。有迹象表明,5 - HT2AR致幻剂LSD和DOI的精神病作用可能涉及通过对腹侧纹状体中D2 - 5 - HT2A异源受体复合物中5 - HT2A原聚体的偏向激动剂作用来增强D2R原聚体信号传导。伏隔核异源受体复合物中促进性变构D2样受体 - 催产素受体相互作用可能在社交和情感行为中起作用。通过阻断这些异源受体复合物的D2原聚体,抗精神病药物可能无法减轻精神分裂症的阴性症状。不同类型D2异源受体复合物的发现增进了我们对精神分裂症发病分子机制的理解,并为其治疗以及理解抗精神病药物的副作用提供了新策略。

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