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抗精神病药物与活体中脑边缘神经元结合的可视化揭示了D2受体、亲酸和亲脂成分。

Visualization of antipsychotic drug binding to living mesolimbic neurons reveals D2 receptor, acidotropic, and lipophilic components.

作者信息

Rayport S, Sulzer D

机构信息

Department of Psychiatry, Columbia University, New York, New York, USA.

出版信息

J Neurochem. 1995 Aug;65(2):691-703. doi: 10.1046/j.1471-4159.1995.65020691.x.

DOI:10.1046/j.1471-4159.1995.65020691.x
PMID:7616225
Abstract

To examine the binding of antipsychotic drugs to living neurons, we applied fluoroprobe derivatives of the D2 antagonist spiperone to mesolimbic system neurons in postnatal culture. We found that rhodamine-N-(p-aminophenethyl)spiperone (rhodamine-NAPS) stereospecifically labeled the plasma membranes of 38 +/- 6% of ventral tegmental area neurons, 22 +/- 7% of which were dopaminergic, and 50 +/- 6% of medium-sized putatively GABAergic nucleus accumbens neurons, with a time constant of approximately 8 min. In contrast, the BODIPY derivative of NAPS rapidly labeled intracellular sites in all neurons in a punctate pattern, consistent with acidotropic uptake. Native antipsychotics also show acidotropic uptake, which we visualized by their displacement of the fluorescent weak base vital dye acridine orange from acidic intracellular compartments. We found that acidotropic uptake correlated best with the partition coefficients of the drugs. With a time constant of 23 min, rhodamine-NAPS labeled all neurons in a pattern suggestive of lipophilic solvation. Thus, initially rhodamine-NAPS makes possible visualization of D2 receptors on living neurons; however, acidotropic uptake and lipophilic solvation obscure receptor labeling and may account for time-dependent factors in the action of antipsychotic drugs, as well as affect their use as radioreceptor ligands.

摘要

为了研究抗精神病药物与活神经元的结合情况,我们将D2拮抗剂螺哌隆的荧光探针衍生物应用于出生后培养的中脑边缘系统神经元。我们发现,罗丹明-N-(对氨基苯乙基)螺哌隆(罗丹明-NAPS)能立体特异性地标记38±6%的腹侧被盖区神经元的质膜,其中22±7%为多巴胺能神经元,以及50±6%的中等大小的假定为γ-氨基丁酸能的伏隔核神经元,时间常数约为8分钟。相比之下,NAPS的BODIPY衍生物能以点状模式快速标记所有神经元的细胞内位点,这与亲酸性摄取一致。天然抗精神病药物也表现出亲酸性摄取,我们通过它们将荧光弱碱活性染料吖啶橙从酸性细胞内区室中置换出来的现象来观察这一点。我们发现亲酸性摄取与药物的分配系数相关性最好。罗丹明-NAPS以一种提示亲脂性溶剂化的模式标记所有神经元,时间常数为23分钟。因此,最初罗丹明-NAPS使可视化活神经元上的D2受体成为可能;然而,亲酸性摄取和亲脂性溶剂化会使受体标记变得模糊,并可能解释抗精神病药物作用中的时间依赖性因素,以及影响它们作为放射性受体配体的用途。

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