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在体外用实验方法测定发现,多巴胺D2高亲和力受体在苯丙胺致敏的动物中有所升高。

Dopamine D2High receptors measured ex vivo are elevated in amphetamine-sensitized animals.

作者信息

Seeman Philip

机构信息

Clera Inc., 260 Heath Street West, Toronto, Ontario, Canada.

出版信息

Synapse. 2009 Mar;63(3):186-92. doi: 10.1002/syn.20595.

Abstract

Although dopamine supersensitivity is a fundamental aspect of diseases such as schizophrenia and Parkinson's disease, the molecular basis of dopamine supersensitivity is not known. Because behavioral dopamine supersensitivity is associated with a marked elevation of striatal dopamine D2(High) receptors in vitro, it is important to develop methods to measure D2(High) receptors in vivo. The present ex vivo study found that the dopamine agonist NPA ([-]-N-propyl-norapomorphine) inhibited the binding of the agonist (3)HPHNO to rat striatal D2 receptors significantly more than the D2 antagonist [(3)H]raclopride, when NPA was coinjected i.v. with each radioligand. These results suggest that the greater sensitivity of (3)HPHNO to inhibition by the coinjected NPA reflects in vivo competition at D2(High) receptors. Using rats that had been sensitized to amphetamine, this ex vivo method found that the specific binding of (3)HPHNO that was displaced by 10 microg/kg of NPA was 2.4-fold higher than that for control rats. These data agree with in vitro data showing a marked increase in D2(High) sites after amphetamine sensitization. Therefore, it is recommended that this method of co-injecting the D2 radioligand and the dopamine agonist displacer be used in human positron tomography to detect D2(High) receptors in health and disease.

摘要

尽管多巴胺超敏反应是精神分裂症和帕金森病等疾病的一个基本特征,但多巴胺超敏反应的分子基础尚不清楚。由于行为性多巴胺超敏反应与体外纹状体多巴胺D2(高亲和力)受体的显著升高有关,因此开发体内测量D2(高亲和力)受体的方法很重要。目前的离体研究发现,当静脉内同时注射NPA([-]-N-丙基去甲阿扑吗啡)与每种放射性配体时,多巴胺激动剂NPA对激动剂(3)HPHNO与大鼠纹状体D2受体结合的抑制作用明显大于D2拮抗剂[(3)H]雷氯必利。这些结果表明,(3)HPHNO对同时注射的NPA抑制作用的更高敏感性反映了D2(高亲和力)受体的体内竞争。使用对苯丙胺致敏的大鼠,这种离体方法发现,被10μg/kg NPA置换的(3)HPHNO的特异性结合比对照大鼠高2.4倍。这些数据与体外数据一致,体外数据显示苯丙胺致敏后D2(高亲和力)位点显著增加。因此,建议在人体正电子断层扫描中使用这种同时注射D2放射性配体和多巴胺激动剂置换剂的方法来检测健康和疾病状态下的D2(高亲和力)受体。

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