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慢性治疗期间因丙咪嗪和地昔帕明代谢物蓄积导致两名受试者死亡:文献综述及可能机制

Death of two subjects due to imipramine and desipramine metabolite accumulation during chronic therapy: a review of the literature and possible mechanisms.

作者信息

Swanson J R, Jones G R, Krasselt W, Denmark L N, Ratti F

机构信息

Pathology Department, Oregon Health Sciences University, Portland, USA.

出版信息

J Forensic Sci. 1997 Mar;42(2):335-9.

PMID:9068197
Abstract

In two unrelated cases, a 7-year-old boy and a 21-year-old woman died suddenly while receiving chronic imipramine therapy. In the boy, concentrations of imipramine were: Left femoral blood 0.5 mg/L, right femoral blood 1.2 mg/L, aorta blood 1.0 mg/L, liver 68 mg/Kg, and for the active metabolite, desipramine, left femoral blood 6.7 mg/L, right femoral blood 9.9 mg/L, aorta blood 8.7 mg/L, liver 400 mg/Kg. In the woman, the imipramine concentrations were: Femoral blood 0.6 mg/L, liver 37 mg/Kg, and of the active metabolite, desipramine, femoral blood 3.74 mg/L, liver 261 mg/Kg. In both cases, the scene investigation strongly indicated that neither individual had ingested an acute overdose. The very high ratios of desmethyl metabolite to parent drug are consistent with this observation. Impaired metabolism due to a genetically determined "slow metabolizer" phenotype of cytochrome CYP2D6, and/or concurrent therapy with phenothiazines, is suggested as a possible mechanism for the apparent fatal accumulation of these tricyclic antidepressants.

摘要

在两起不相关的病例中,一名7岁男孩和一名21岁女性在接受慢性丙咪嗪治疗时突然死亡。在男孩体内,丙咪嗪的浓度为:左股静脉血0.5毫克/升,右股静脉血1.2毫克/升,主动脉血1.0毫克/升,肝脏68毫克/千克;而活性代谢物地昔帕明的浓度为:左股静脉血6.7毫克/升,右股静脉血9.9毫克/升,主动脉血8.7毫克/升,肝脏400毫克/千克。在女性体内,丙咪嗪的浓度为:股静脉血0.6毫克/升,肝脏37毫克/千克;活性代谢物地昔帕明的浓度为:股静脉血3.74毫克/升,肝脏261毫克/千克。在这两起病例中,现场调查有力地表明两人均未急性过量服药。去甲基代谢物与母体药物的比例极高,这与该观察结果相符。细胞色素CYP2D6基因决定的“慢代谢者”表型导致的代谢受损和/或同时使用吩噻嗪类药物,被认为是这些三环类抗抑郁药明显致命性蓄积的一种可能机制。

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