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兔体内3,4-亚甲基二氧甲基苯丙胺(摇头丸,MDMA)的死后再分布。第一部分:体内静脉输注后的实验方法

Post-mortem redistribution of 3,4-methylenedioxymethamphetamine (MDMA, "ecstasy") in the rabbit. Part I: experimental approach after in vivo intravenous infusion.

作者信息

De Letter Els A, Clauwaert Karine M, Belpaire Frans M, Lambert Willy E, Van Bocxlaer Jan F, Piette Michel H A

机构信息

Ghent University, Department of Forensic Medicine, J. Kluyskensstraat 29, 9000 Ghent, Belgium.

出版信息

Int J Legal Med. 2002 Aug;116(4):216-24. doi: 10.1007/s00414-002-0292-0. Epub 2002 May 28.

Abstract

Post-mortem redistribution is known to influence blood and tissue levels of various drugs. An animal model was used in an attempt to elucidate this problem for the amphetamine analogue, 3,4-methylenedioxymethamphetamine (MDMA). Rabbits received 1 mg/kg MDMA intravenously (iv) and were killed 2 h later in order to simulate the state of complete distribution in the body. MDMA and 3,4-methylenedioxyamphetamine (MDA) concentrations were determined in blood, urine, bile, vitreous humour, and various tissues (eye globe walls, brain, cardiac muscle, lungs, liver, kidneys, iliopsoas muscle and adipose tissue) using a high pressure liquid chromatographic (HPLC) procedure with fluorescence detection. In the first group (control group, sampling immediately post mortem) considerable MDMA concentrations were found in the brain and both lungs. In addition, our data indicate the elimination of MDMA by hepatic biotransformation and excretion via the bile. When the animals were preserved either 24 or 72 h post mortem (second group), an increase of MDMA and MDA levels in the liver and the eye globe walls was noticed. In the lungs, on the other hand, they tended to decline as a function of increasing post-mortem interval. MDMA levels in cardiac and iliopsoas muscle were fairly comparable and remained stable up to 72 h after death. In the third group, ligation of the large vessels around the heart took place immediately post mortem, but significant differences in blood and tissue MDMA concentrations between rabbits of group 2 and 3 could not be demonstrated. We therefore conclude that post-mortem redistribution of MDMA at the cellular level (viz. by pure diffusion gradient from higher to lower concentrations) is more important than its redistribution via the vascular pathway. Finally, MDA levels were relatively low in all samples, thus indicating that this is not a major metabolite in the rabbit, at least within the first 2 h after administration.

摘要

已知死后再分布会影响各种药物的血液和组织水平。为阐明苯丙胺类似物3,4-亚甲基二氧甲基苯丙胺(摇头丸)的这一问题,使用了动物模型。兔子静脉注射1mg/kg摇头丸,2小时后处死,以模拟药物在体内完全分布的状态。采用带荧光检测的高压液相色谱法(HPLC)测定血液、尿液、胆汁、玻璃体液及各种组织(眼球壁、脑、心肌、肺、肝、肾、髂腰肌和脂肪组织)中摇头丸和3,4-亚甲基二氧苯丙胺(MDA)的浓度。在第一组(对照组,死后立即取样)中,在脑和双肺中发现了相当高的摇头丸浓度。此外,我们的数据表明,摇头丸可通过肝脏生物转化并经胆汁排泄而消除。当动物在死后保存(第二组)24或72小时时,肝脏和眼球壁中摇头丸和MDA水平升高。另一方面,在肺中,它们往往随着死后间隔时间的延长而下降。心脏和髂腰肌中的摇头丸水平相当,在死亡后72小时内保持稳定。在第三组中,死后立即结扎心脏周围的大血管,但未显示出第二组和第三组兔子在血液和组织中摇头丸浓度的显著差异。因此我们得出结论,摇头丸在细胞水平的死后再分布(即通过从高浓度到低浓度的纯扩散梯度)比其通过血管途径的再分布更为重要。最后,所有样本中的MDA水平相对较低,因此表明至少在给药后的前2小时内,MDA不是兔子体内的主要代谢产物。

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