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正电子发射断层扫描(PET)配体11C-雷氯必利在纹状体的结合会受到改变突触多巴胺水平的药物的影响。

Striatal binding of the PET ligand 11C-raclopride is altered by drugs that modify synaptic dopamine levels.

作者信息

Dewey S L, Smith G S, Logan J, Brodie J D, Fowler J S, Wolf A P

机构信息

Chemistry Department, Brookhaven National Laboratory, Upton, New York 11973.

出版信息

Synapse. 1993 Apr;13(4):350-6. doi: 10.1002/syn.890130407.

Abstract

Bilateral decreases in striatal 11C-raclopride binding were observed in adult female baboons with high resolution PET following administration of drugs that act centrally on dopaminergic neurons. At baseline and following administration of d-amphetamine (a dopamine-releasing drug), GBR-12909 (a potent dopamine reuptake inhibitor), or tetrabenazine (a biogenic amine depleting drug) PET scans of 11C-raclopride binding were obtained in a CTI 931 positron tomograph. In all studies, the ratio of the distribution volumes for the striatum to the cerebellum for 11C-raclopride binding decreased significantly by an average of 16.2% for d-amphetamine, 22.1% for GBR-12909, and 28.3% for tetrabenazine while there were no significant changes observed in the cerebellum or in the rate of systemic metabolism of the radiotracer. These decreases exceed the test/retest variability of striatal 11C-raclopride binding measured in the same animals under identical experimental conditions (Dewey et al., 1992b). Together these studies demonstrate that PET measurements of striatal 11C-raclopride binding can be used to indirectly and non-invasively monitor changes in synaptic dopamine concentrations that result from a variety of neurophysiologic mechanisms.

摘要

在成年雌性狒狒中,使用对多巴胺能神经元起中枢作用的药物后,通过高分辨率正电子发射断层扫描(PET)观察到纹状体中11C-雷氯必利结合的双侧减少。在基线以及给予d-苯丙胺(一种多巴胺释放药物)、GBR-12909(一种有效的多巴胺再摄取抑制剂)或丁苯那嗪(一种生物胺耗竭药物)后,在CTI 931正电子断层扫描仪中获得了11C-雷氯必利结合的PET扫描图像。在所有研究中,11C-雷氯必利结合的纹状体与小脑分布体积之比显著降低,d-苯丙胺平均降低16.2%,GBR-12909降低22.1%,丁苯那嗪降低28.3%,而小脑或放射性示踪剂的全身代谢率未观察到显著变化。这些降低超过了在相同实验条件下对同一动物测量的纹状体11C-雷氯必利结合的重测变异性(杜威等人,1992b)。这些研究共同表明,PET测量纹状体11C-雷氯必利结合可用于间接和非侵入性地监测由多种神经生理机制导致的突触多巴胺浓度变化。

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