Does sodium oxybate inhibit brain dopamine release in humans? An exploratory neuroimaging study.

IF 1.8 4区 医学 Q3 CLINICAL NEUROLOGY
Stephen J Kish, Gerald O'Leary, Mortimer Mamelak, Tina McCluskey, Jerry J Warsh, Colin Shapiro, Robert Bies, Yifan Yu, Bruce Pollock, Junchao Tong, Isabelle Boileau
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引用次数: 1

Abstract

Objective: To establish in an exploratory neuroimaging study whether γ-hydroxybutyrate (sodium oxybate [SO]), a sedative, anti-narcoleptic drug with abuse potential, transiently inhibits striatal dopamine release in the human.

Methods: Ten healthy participants (30 years; 6M, 4F) and one participant with narcolepsy received a baseline positron emission tomography scan of [C-11]raclopride, a D2/3 dopamine receptor radioligand sensitive to dopamine occupancy, followed approximately one week later by an oral sedative 3g dose of SO and two [C-11]raclopride scans (1 h, 7 h post SO). Plasma SO levels and drowsiness duration were assessed.

Results: No significant changes were detected in [C-11]raclopride binding in striatum overall 1 or 7 h after SO, but a small non-significant increase in [C-11]raclopride binding, implying decreased dopamine occupancy, was noted in limbic striatal subdivision at one hour (+6.5%; p uncorrected = 0.045; +13.2%, narcolepsy participant), returning to baseline at 7 h. A positive correlation was observed between drowsiness duration and percent change in [C-11]raclopride binding in limbic striatum (r = 0.73; p = 0.017).

Conclusions: We did not find evidence in this sample of human subjects of a robust striatal dopamine change, as was reported in non-human primates. Our preliminary data, requiring extension, suggest that a 3g sedative SO dose might cause slight transient inhibition of dopamine release in limbic striatum.

氧酸钠是否能抑制人类大脑多巴胺的释放?探索性神经影像学研究。
目的:通过一项探索性神经影像学研究,探讨γ-羟丁酸(氧化钠[SO])这种具有滥用潜力的镇静、抗发作性睡药物是否能短暂抑制人纹状体多巴胺释放。方法:健康受试者10例(30岁;6M, 4F)和一名发作性睡症患者接受了[C-11]raclopride的基线正电子发射断层扫描,[C-11]raclopride是一种对多巴胺占用敏感的D2/3多巴胺受体放射配体,大约一周后口服镇静3g剂量的SO和两次[C-11]raclopride扫描(SO后1小时,7小时)。评估血浆SO水平和困倦持续时间。结果:在SO后1或7小时,纹状体中[C-11]raclopride结合没有明显变化,但在1小时时,边缘纹状体分支中[C-11]raclopride结合有轻微的非显著性增加,表明多巴胺占用减少(+6.5%;未校正P = 0.045;+13.2%,发作性睡病参与者),7小时后恢复基线。困倦持续时间与边缘纹状体[C-11]raclopride结合百分比变化呈正相关(r = 0.73;p = 0.017)。结论:我们没有在人类受试者样本中发现纹状体多巴胺强劲变化的证据,正如在非人类灵长类动物中报道的那样。我们的初步数据,需要扩展,表明3g镇静SO剂量可能导致边缘纹状体多巴胺释放轻微的短暂抑制。
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来源期刊
CiteScore
4.10
自引率
0.00%
发文量
34
审稿时长
6-12 weeks
期刊介绍: Human Psychopharmacology: Clinical and Experimental provides a forum for the evaluation of clinical and experimental research on both new and established psychotropic medicines. Experimental studies of other centrally active drugs, including herbal products, in clinical, social and psychological contexts, as well as clinical/scientific papers on drugs of abuse and drug dependency will also be considered. While the primary purpose of the Journal is to publish the results of clinical research, the results of animal studies relevant to human psychopharmacology are welcome. The following topics are of special interest to the editors and readers of the Journal: -All aspects of clinical psychopharmacology- Efficacy and safety studies of novel and standard psychotropic drugs- Studies of the adverse effects of psychotropic drugs- Effects of psychotropic drugs on normal physiological processes- Geriatric and paediatric psychopharmacology- Ethical and psychosocial aspects of drug use and misuse- Psychopharmacological aspects of sleep and chronobiology- Neuroimaging and psychoactive drugs- Phytopharmacology and psychoactive substances- Drug treatment of neurological disorders- Mechanisms of action of psychotropic drugs- Ethnopsychopharmacology- Pharmacogenetic aspects of mental illness and drug response- Psychometrics: psychopharmacological methods and experimental design
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