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死后阿米替林再分布的动物模型。

An animal model of postmortem amitriptyline redistribution.

作者信息

Hilberg T, Bugge A, Beylich K M, Ingum J, Bjørneboe A, Mørland J

机构信息

National Institute of Forensic Toxicology, Oslo, Norway.

出版信息

J Forensic Sci. 1993 Jan;38(1):81-90.

PMID:8426162
Abstract

An experimental rat model was developed to study postmortem changes of drug concentration after an acute overdose. Overnight fasted rats were fed 75 mg of amitriptyline (AMI). Two h after dosing, the rats were anaesthetized and blood samples were drawn from the femoral vein (peripheral blood--PB) and the heart (HB). The rats were sacrificed by CO2 and left at room temperature for either 0.1, 0.5, 1, 2, 5, 10, 24, 48, or 96 hours, when samples of heart blood, blood from the inferior vena cava (PB) and tissue samples from different liver lobes, heart, lungs, kidney, thigh muscle, and brain were taken. Samples were analyzed by high performance liquid chromatography. The AMI concentration in HB increased fairly rapidly within the first 2 h postmortem and from then the average ratio was 6.4 +/- 0.8 (mean +/- sem) (n = 31). In PB, the post/antemortem AMI concentration ratio followed an approximately exponential rise; at 2 h postmortem the ratio was 1.6 +/- 0.3 (n = 5), and at 96 h 55.1 +/- 23.8 (n = 4). For the main metabolite nortriptyline (NOR), the concentration changes followed the same pattern, but to a lesser extent. Among the tissues, the liver lobes had high, but variable drug concentrations; lobes lying closest to the stomach had the highest drug concentrations. The drug concentration in the lungs declined significantly. This animal model demonstrates postmortem drug concentration changes similar to those described in humans. Probable mechanisms include drug diffusion from the stomach and GI tract to the surrounding tissues and blood; and postmortem drug release from the lungs and possibly other drug-rich tissues into the blood.

摘要

建立了一种实验大鼠模型,以研究急性过量用药后药物浓度的死后变化。将过夜禁食的大鼠喂食75毫克阿米替林(AMI)。给药后2小时,将大鼠麻醉,从股静脉(外周血 - PB)和心脏(HB)采集血样。通过二氧化碳处死大鼠,并将其置于室温下0.1、0.5、1、2、5、10、24、48或96小时,然后采集心脏血样、下腔静脉血(PB)以及不同肝叶、心脏、肺、肾、大腿肌肉和脑的组织样本。通过高效液相色谱法分析样本。死后最初2小时内,HB中的AMI浓度迅速升高,此后平均比值为6.4±0.8(均值±标准误)(n = 31)。在PB中,死后/生前AMI浓度比值呈近似指数上升;死后2小时时比值为1.6±0.3(n = 5),96小时时为55.1±23.8(n = 4)。对于主要代谢产物去甲替林(NOR),浓度变化遵循相同模式,但程度较小。在各组织中,肝叶的药物浓度较高但变化较大;最靠近胃的肝叶药物浓度最高。肺中的药物浓度显著下降。该动物模型显示出与人类中描述的死后药物浓度变化相似的情况。可能的机制包括药物从胃和胃肠道扩散到周围组织和血液;以及死后药物从肺和可能其他富含药物的组织释放到血液中。

相似文献

1
An animal model of postmortem amitriptyline redistribution.死后阿米替林再分布的动物模型。
J Forensic Sci. 1993 Jan;38(1):81-90.
2
Postmortem drug redistribution--human cases related to results in experimental animals.死后药物再分布——与实验动物结果相关的人类案例
J Forensic Sci. 1999 Jan;44(1):3-9.
3
Redistribution of basic drugs into cardiac blood from surrounding tissues during early-stages postmortem.死后早期阶段基本药物从周围组织再分布至心脏血液中。
J Forensic Sci. 1999 Jan;44(1):10-6.
4
The extent of postmortem drug redistribution in a rat model.大鼠模型中死后药物再分布的程度。
J Forensic Sci. 1999 Sep;44(5):956-62.
5
Postmortem amitriptyline pharmacokinetics in pigs after oral and intravenous routes of administration.猪经口服和静脉给药后阿米替林的死后药代动力学
J Forensic Sci. 1998 Mar;43(2):380-7.
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Postmortem release of amitriptyline from the lungs; a mechanism of postmortem drug redistribution.
Forensic Sci Int. 1994 Jan;64(1):47-55. doi: 10.1016/0379-0738(94)90241-0.
7
Diffusion as a mechanism of postmortem drug redistribution: an experimental study in rats.作为死后药物再分布机制的扩散:大鼠实验研究
Int J Legal Med. 1992;105(2):87-91. doi: 10.1007/BF02340830.
8
Postmortem changes in tissue concentrations of triazolam and diazepam in rats.大鼠死后三唑仑和地西泮组织浓度的变化
Leg Med (Tokyo). 2004 Oct;6(4):224-32. doi: 10.1016/j.legalmed.2004.05.006.
9
Possible markers for postmortem drug redistribution.死后药物再分布的可能标志物。
J Forensic Sci. 1997 Jan;42(1):88-92.
10
Site to site variability of postmortem drug concentrations in liver and lung.
J Forensic Sci. 1996 Nov;41(6):927-32.

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