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戒断期甲基苯丙胺滥用者的认知功能和黑质纹状体标志物

Cognitive function and nigrostriatal markers in abstinent methamphetamine abusers.

作者信息

Johanson Chris-Ellyn, Frey Kirk A, Lundahl Leslie H, Keenan Pamela, Lockhart Nancy, Roll John, Galloway Gantt P, Koeppe Robert A, Kilbourn Michael R, Robbins Trevor, Schuster Charles R

机构信息

Department of Psychiatry and Behavioral Neurosciences, Wayne State University, Detroit, MI 48207, USA.

出版信息

Psychopharmacology (Berl). 2006 Apr;185(3):327-38. doi: 10.1007/s00213-006-0330-6. Epub 2006 Mar 3.

Abstract

OBJECTIVE

Preclinical investigations have established that methamphetamine (MA) produces long-term changes in dopamine (DA) neurons in the striatum. Human studies have suggested similar effects and correlated motor and cognitive deficits. The present study was designed to further our understanding of changes in brain function in humans that might result from chronic high dose use of MA after at least 3 months of abstinence.

METHOD

Brain function in abstinent users was compared to controls using neuroimaging of monoamine transporters and cognitive assessment. Striatal levels of DA transporter (DAT) and vesicular monoamine transporter type-2 (VMAT2) were determined using [11C]methylphenidate and [11C]dihydrotetrabenazine positron emission tomography, respectively. Cognitive function was evaluated using tests of motor function, memory, learning, attention, and executive function.

RESULTS

Striatal DAT was approximately 15% lower and VMAT2 was 10% lower in MA abusers across striatal subregions. The MA abusers performed within the normal range but performed more poorly compared to controls on three of the 12 tasks.

CONCLUSIONS

Failure to find more substantial changes in transporter levels and neurocognitive function may be attributed to the length of time that MA users were abstinent (ranging from 3 months to more than 10 years, mean 3 years), although there were no correlations with length of abstinence. Persistent VMAT2 reductions support the animal literature indicating a toxic effect of MA on nigrostriatal nerve terminals. However, the magnitude of the MA effects on nigrostriatal projection integrity is sufficiently small that it is questionable whether clinical signs of DA deficiency are likely to develop.

摘要

目的

临床前研究已证实,甲基苯丙胺(MA)会使纹状体中的多巴胺(DA)神经元产生长期变化。人体研究也表明了类似的影响,并将其与运动和认知缺陷联系起来。本研究旨在进一步了解人类在至少3个月 abstinence 后长期高剂量使用MA可能导致的脑功能变化。

方法

通过单胺转运体的神经成像和认知评估,将 abstinent 用户的脑功能与对照组进行比较。分别使用[11C]甲基苯丙胺和[11C]二氢四苯嗪正电子发射断层扫描来测定纹状体中DA转运体(DAT)和2型囊泡单胺转运体(VMAT2)的水平。使用运动功能、记忆、学习、注意力和执行功能测试来评估认知功能。

结果

在纹状体各亚区域,MA滥用者的纹状体DAT约低15%,VMAT2约低10%。MA滥用者的表现处于正常范围内,但在12项任务中的3项任务上,与对照组相比表现较差。

结论

未能在转运体水平和神经认知功能上发现更显著的变化,可能归因于MA使用者 abstinent 的时间长度(从3个月到10多年不等,平均3年),尽管与 abstinent 时间长度没有相关性。VMAT2的持续降低支持了动物研究文献,表明MA对黑质纹状体神经末梢有毒性作用。然而,MA对黑质纹状体投射完整性的影响程度足够小,以至于DA缺乏的临床症状是否可能出现值得怀疑。

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