de Win Maartje M L, Reneman Liesbeth, Jager Gerry, Vlieger Erik-Jan P, Olabarriaga Sílvia D, Lavini Cristina, Bisschops Ivo, Majoie Charles B L M, Booij Jan, den Heeten Gerard J, van den Brink Wim
Department of Radiology, Academic Medical Center, University of Amsterdam, Amsterdam, The Netherlands.
Neuropsychopharmacology. 2007 Feb;32(2):458-70. doi: 10.1038/sj.npp.1301225. Epub 2006 Nov 1.
It is debated whether ecstasy use has neurotoxic effects on the human brain and what the effects are of a low dose of ecstasy use. We prospectively studied sustained effects (>2 weeks abstinence) of a low dose of ecstasy on the brain in ecstasy-naive volunteers using a combination of advanced MR techniques and self-report questionnaires on psychopathology as part of the NeXT (Netherlands XTC Toxicity) study. Outcomes of proton magnetic resonance spectroscopy (1H-MRS), diffusion tensor imaging (DTI), perfusion-weighted imaging (PWI), and questionnaires on depression, impulsivity, and sensation seeking were compared in 30 subjects (12M, 21.8+/-3.1 years) in two sessions before and after first ecstasy use (1.8+/-1.3 tablets). Interval between baseline and follow-up was on average 8.1+/-6.5 months and time between last ecstasy use and follow-up was 7.7+/-4.4 weeks. Using 1H-MRS, no significant changes were observed in metabolite concentrations of N-acetylaspartate (NAA), choline (Cho), myo-inositol (mI), and creatine (Cr), nor in ratios of NAA, Cho, and mI relative to Cr. However, ecstasy use was followed by a sustained 0.9% increase in fractional anisotropy (FA) in frontoparietal white matter, a 3.4% decrease in apparent diffusion (ADC) in the thalamus and a sustained decrease in relative regional cerebral blood volume (rrCBV) in the thalamus (-6.2%), dorsolateral frontal cortex (-4.0%), and superior parietal cortex (-3.0%) (all significant at p<0.05, paired t-tests). After correction for multiple comparisons, only the rrCBV decrease in the dorsolateral frontal cortex remained significant. We also observed increased impulsivity (+3.7% on the Barratt Impulsiveness Scale) and decreased depression (-28.0% on the Beck Depression Inventory) in novel ecstasy users, although effect sizes were limited and clinical relevance questionable. As no indications were found for structural neuronal damage with the currently used techniques, our data do not support the concern that incidental ecstasy use leads to extensive axonal damage. However, sustained decreases in rrCBV and ADC values may indicate that even low ecstasy doses can induce prolonged vasoconstriction in some brain areas, although it is not known whether this effect is permanent. Additional studies are needed to replicate these findings.
摇头丸的使用是否会对人类大脑产生神经毒性作用,以及低剂量使用摇头丸会产生何种影响,目前尚无定论。我们前瞻性地研究了低剂量摇头丸对初涉摇头丸的志愿者大脑的持续影响(禁欲超过2周),采用了先进的磁共振技术和关于精神病理学的自我报告问卷相结合的方法,这是荷兰摇头丸毒性(NeXT)研究的一部分。在30名受试者(12名男性,年龄21.8±3.1岁)首次使用摇头丸(1.8±1.3片)前后的两个阶段,比较了质子磁共振波谱(1H-MRS)、扩散张量成像(DTI)、灌注加权成像(PWI)的结果以及关于抑郁、冲动性和寻求刺激的问卷结果。基线与随访之间的间隔平均为8.1±6.5个月,最后一次使用摇头丸与随访之间的时间为7.7±4.4周。使用1H-MRS,未观察到N-乙酰天门冬氨酸(NAA)、胆碱(Cho)、肌醇(mI)和肌酸(Cr)的代谢物浓度有显著变化,NAA、Cho和mI相对于Cr的比率也无显著变化。然而,使用摇头丸后,额顶叶白质的分数各向异性(FA)持续增加0.9%,丘脑的表观扩散系数(ADC)下降3.4%,丘脑、背外侧额叶皮质和顶上叶皮质的相对局部脑血容量(rrCBV)持续下降(分别为-6.2%、-4.0%和-3.0%)(所有p<0.05,配对t检验均显著)。在进行多重比较校正后,仅背外侧额叶皮质的rrCBV下降仍具有显著性。我们还观察到,初次使用摇头丸的使用者冲动性增加(Barratt冲动性量表上增加3.7%),抑郁程度降低(贝克抑郁量表上降低28.0%),尽管效应量有限且临床相关性存疑。由于目前使用的技术未发现结构性神经元损伤迹象,我们的数据不支持偶尔使用摇头丸会导致广泛轴突损伤的担忧。然而,rrCBV和ADC值的持续下降可能表明,即使是低剂量的摇头丸也可能在某些脑区诱发长期血管收缩,尽管尚不清楚这种影响是否是永久性的。需要进一步的研究来重复这些发现。
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