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增加多巴胺对 D2 样受体与 D1 样受体的亲和力。对解释 PET 研究结果的容积传递的相关性。

Increased affinity of dopamine for D(2) -like versus D(1) -like receptors. Relevance for volume transmission in interpreting PET findings.

机构信息

Department of Neuroscience, Karolinska Institutet, SE-17177, Stockholm, Sweden.

出版信息

Synapse. 2012 Mar;66(3):196-203. doi: 10.1002/syn.21501. Epub 2011 Nov 18.

DOI:10.1002/syn.21501
PMID:22034017
Abstract

Evidence indicates that dopamine (DA) mainly acts as a volume transmission (VT) transmitter through its release into the extracellular fluid where the D(1) -like and D(2) -like receptors are predominantly extrasynaptic. It was therefore of interest to compare the affinities of the two major families of DA receptors. [(3)H] raclopride /DA and [(3)H] SCH23390/DA competition assays compared the affinity of DA at D(2) -like and D(1) -like receptors in rat dorsal striatal membrane preparations as well as in membrane preparations from CHO cell lines stably transfected with human D(2L) and D(1) receptors. The IC(50) values of DA at D(2) -like receptors in dorsal striatal membranes and CHO cell membranes were markedly and significantly reduced compared with the IC(50) values of DA at D(1) -like receptors. These IC(50) values reflect differences in both the high and low affinity states. The K(iH) value for DA at [(3)H] raclopride-labeled D(2) -like receptors in dorsal striatum was 12 nM, and this can help explain PET findings that amphetamine-induced increases in DA release can produce an up to 50% decrease of [(11)C] raclopride binding in the dorsal striatum in vivo. These combined results give indications for the existence of striatal D(2) -like receptor-mediated DA VT at the local circuit level in vivo. The demonstration of a K(iH) value of 183 nM for DA at D(1) antagonist-labeled D(1) -like receptors instead gives a likely explanation for the failure of a reduction of D(1) -like receptor binding after amphetamine-induced DA release in PET studies using the D(1) -like antagonist radioligands [(11)C] SCH23390 and [(11)C] NNC. It seems difficult to evaluate the role of the extrasynaptic D(1) receptors in VT in vivo with the PET radioligands available for this receptor.

摘要

证据表明,多巴胺(DA)主要通过将其释放到细胞外液中而起作用,在细胞外液中,D1 样和 D2 样受体主要是 extrasynaptic。因此,比较两种主要的 DA 受体家族的亲和力很有趣。[(3)H]raclopride/DA 和 [(3)H]SCH23390/DA 竞争测定法比较了 DA 在大鼠背侧纹状体膜制剂以及稳定转染人 D2L 和 D1 受体的 CHO 细胞系膜制剂中 D2 样和 D1 样受体上的亲和力。与 D1 样受体相比,DA 在背侧纹状体膜和 CHO 细胞膜上的 D2 样受体的 IC50 值显著降低。这些 IC50 值反映了高亲和力和低亲和力状态的差异。DA 在 [(3)H]raclopride 标记的 D2 样受体上的 K(iH) 值为 12 nM,这有助于解释 PET 研究结果,即安非他命诱导的 DA 释放增加可导致体内背侧纹状体中 [(11)C]raclopride 结合减少高达 50%。这些综合结果表明,在体内局部回路水平上存在纹状体 D2 样受体介导的 DA VT。DA 在 D1 拮抗剂标记的 D1 样受体上的 K(iH) 值为 183 nM,这为使用 D1 样拮抗剂放射性配体 [(11)C]SCH23390 和 [(11)C]NNC 在 PET 研究中安非他命诱导的 DA 释放后 D1 样受体结合减少失败提供了一个可能的解释。使用现有的用于该受体的 PET 放射性配体评估 extrasynaptic D1 受体在体内 VT 中的作用似乎很困难。

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