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多巴胺受体超敏反应:发生、机制、表现及临床应用

Dopamine receptor supersensitivity: development, mechanisms, presentation, and clinical applicability.

作者信息

Kostrzewa Richard M, Kostrzewa John P, Brown Russell W, Nowak Przemyslaw, Brus Ryszard

机构信息

Department of Pharmacology, Quillen College of Medicine, East Tennessee State University, Johnson City, TN 37614, USA.

出版信息

Neurotox Res. 2008 Oct;14(2-3):121-8. doi: 10.1007/BF03033804.

Abstract

The process of receptor supersensitivity (RSS) has a long history and is an epiphenomenon of neuronal denervation. Dopamine (DA) RSS (DARSS) similarly occurs after DA denervation, and this process is invoked in neuropsychiatric and neurodegenerative disorders. From studies largely over the past 25 years, much has been learned regarding DARSS. For example, overt D1 DARSS occurs after perinatal destruction of nigrostriatal DA fibers. However, following perinatal destruction of DA innervation, the most-prominent behavioral effects of a D1 agonist are observed after a series of D1 agonist treatments--a process known as priming of D1 DA receptors. Moreover, perinatal lesioning of DA fibers produces prominent serotonin (5-HT) RSS, and in fact 5-HT RSS appears to modulate D1 DA RSS. In rodents, receptor supersensitization by these means appears to be irreversible. In contrast to the observed D1 DARSS, D2 DARSS apparently does not occur after perinatal DA denervation. Also, while repeated D1 agonist treatment of intact rats has no observable effect, repeated D2 agonist treatments, during or after the ontogenetic phase, produces prominent life-long D2 RSS. The process may have an association with substance abuse. Therefore, production of D1 and D2 DARSS occurs by different means and under different circumstances, and in association with perhaps different neuronal phenotypes, and with greater incidence in either intact (D2) or DA-lesioned counterparts (D1). The physiological consequence of RSS are multiple.

摘要

受体超敏反应(RSS)的过程由来已久,是神经元去神经支配的一种附带现象。多巴胺(DA)超敏反应(DARSS)在DA去神经支配后也会类似地发生,并且这个过程在神经精神疾病和神经退行性疾病中会出现。从过去25年的大量研究中,我们对DARSS已经有了很多了解。例如,黑质纹状体DA纤维在围产期被破坏后会出现明显的D1 DARSS。然而,在围产期DA神经支配被破坏后,D1激动剂最显著的行为效应是在一系列D1激动剂治疗后才观察到的——这个过程被称为D1 DA受体的启动。此外,DA纤维的围产期损伤会产生显著的5-羟色胺(5-HT)RSS,事实上5-HT RSS似乎会调节D1 DA RSS。在啮齿动物中,通过这些方式产生的受体超敏似乎是不可逆的。与观察到的D1 DARSS不同,D2 DARSS在围产期DA去神经支配后显然不会出现。而且,虽然对完整大鼠反复给予D1激动剂治疗没有可观察到的效果,但在个体发育阶段期间或之后反复给予D2激动剂治疗,会产生显著的终生D2 RSS。这个过程可能与药物滥用有关。因此,D1和D2 DARSS的产生是通过不同的方式、在不同的情况下发生的,并且可能与不同的神经元表型有关,在完整(D2)或DA损伤(D1)的对应物中发生率更高。RSS的生理后果是多方面的。

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