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犬肌肉注射奥氮平帕莫酸盐后奥氮平的死后再分布

Postmortem redistribution of olanzapine following intramuscular administration of olanzapine pamoate in dogs.

作者信息

Johnson Jason T, Everly Amy G, Kpakima Felicia E Frazier, Detke Holland C

机构信息

Lilly Research Laboratories, Eli Lilly and Company, Indianapolis, IN 46285, USA.

Lilly Research Laboratories, Eli Lilly and Company, Indianapolis, IN 46285, USA.

出版信息

Forensic Sci Int. 2015 Dec;257:353-358. doi: 10.1016/j.forsciint.2015.09.022. Epub 2015 Oct 22.

Abstract

The potential for postmortem redistribution of olanzapine was investigated in beagle dogs. Olanzapine pamoate monohydrate was administered once every 14 days by intramuscular injection for 3 months to fed male dogs (n=15) at a dose of 20 mg/kg olanzapine (equivalent to 46 mg/kg olanzapine pamoate monohydrate). Blood samples were collected after the fifth (Day 57) and sixth (Day 71) doses to determine olanzapine and N-oxide olanzapine concentrations. On Day 71 at 72 h postdose, dogs were euthanized and placed on their backs without additional manipulation and held for postmortem blood, urine, and tissue collection at room temperature for up to 168 h postdose (96 h after euthanasia). Concentrations of olanzapine and N-oxide olanzapine were determined by liquid chromatography-mass spectroscopy/mass spectroscopy (LC-MS/MS). Postmortem olanzapine concentrations in blood increased up to seven-fold compared to the last quantified antemortem blood concentration. Olanzapine concentrations in vein tissue samples (surrogates for peripheral blood) also increased, whereas other tissue concentrations, such as myocardium, lung, liver, and kidney decreased over the postmortem period. An increase in blood concentration of olanzapine after death was observed in all but one animal, suggesting that postmortem redistribution may occur in dogs following biweekly intramuscular administration of olanzapine pamoate monohydrate. The rise in olanzapine concentrations in blood after death in this study may potentially be attributed to diffusion from multiple tissues to blood and, to a lesser extent, reduction of the N-oxide olanzapine metabolite back to olanzapine. However, the generalizability of these results to humans cannot be confirmed by the present study.

摘要

在比格犬中研究了奥氮平死后再分布的可能性。对15只雄性喂食犬每14天进行一次肌肉注射奥氮平一水合帕莫酸盐,持续3个月,剂量为20mg/kg奥氮平(相当于46mg/kg奥氮平一水合帕莫酸盐)。在第5次(第57天)和第6次(第71天)给药后采集血样,以测定奥氮平和N-氧化奥氮平的浓度。在第71天给药后72小时,对犬实施安乐死,使其仰卧,不进行额外操作,在室温下放置,直至给药后168小时(安乐死后96小时)采集死后血液、尿液和组织样本。通过液相色谱-质谱联用/质谱(LC-MS/MS)测定奥氮平和N-氧化奥氮平的浓度。死后血液中奥氮平浓度比最后一次定量的生前血液浓度增加了高达7倍。静脉组织样本(外周血替代物)中的奥氮平浓度也有所增加,而在死后期间,心肌、肺、肝和肾等其他组织中的浓度则下降。除一只动物外,在所有动物中均观察到死后奥氮平血药浓度升高,这表明在每两周肌肉注射奥氮平一水合帕莫酸盐的犬中可能会发生死后再分布。本研究中死后血液中奥氮平浓度的升高可能潜在地归因于从多个组织扩散至血液,以及在较小程度上N-氧化奥氮平代谢物还原为奥氮平。然而,本研究无法证实这些结果对人类的可推广性。

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