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一种用于抗疟药物形成高铁血红蛋白的改进药效学模型。

An improved pharmacodynamic model for formation of methemoglobin by antimalarial drugs.

作者信息

Fasanmade A A, Jusko W J

机构信息

Department of Pharmaceutics, School of Pharmacy, State University of New York at Buffalo 14260, USA.

出版信息

Drug Metab Dispos. 1995 May;23(5):573-6.

PMID:7587933
Abstract

The widely used 8-aminoquinoline antimalarial group of compounds and the derivatives such as WR242511 that are being developed for possible prophylactic anticyanide applications have complex interactions with erythrocytes. Methemoglobin (MetHb) levels following the use of this drug predicted by earlier authors grossly deviated from the observed steady state levels under multiple-dose conditions. We propose a pharmacokinetic-pharmacodynamic model to characterize literature data for blood levels of MetHb generated after administration of WR242511. The model is based on an indirect mechanism involving WR242511 putative metabolite concentration, Cm on the formation of MetHb (rate constant, kr) and on depletion of reducing equivalents leading to accumulation of MetHb. Eventual depletion of MetHb is modeled as related to the disposition of both the drug metabolite and MetHb. The rate of change of MetHb concentration in the blood under the influence of a dose of WR242511 in dogs was governed by this relationship: d[MetHb]/d(t) = kr.Cm.[Hb]-kh.[MetHb], where kr is 2.9 x 10(-5) ml.ng-1.hr-1 and kh is 0.0418 hr-1. This model was validated with multiple-dose data. The model is simple and compatible with the physiological behavior of MetHb in vivo under single-dose and multiple-dose conditions of WR242511 administration.

摘要

广泛使用的8-氨基喹啉类抗疟化合物以及正在研发用于可能的预防性抗氰化物应用的衍生物(如WR242511)与红细胞有复杂的相互作用。早期作者预测使用该药物后的高铁血红蛋白(MetHb)水平与多剂量条件下观察到的稳态水平有很大偏差。我们提出了一个药代动力学-药效学模型来表征WR242511给药后产生的MetHb血药浓度的文献数据。该模型基于一种间接机制,涉及WR242511假定代谢物浓度Cm对MetHb形成(速率常数kr)以及导致MetHb积累的还原当量消耗的影响。最终MetHb的消耗被建模为与药物代谢物和MetHb的处置相关。在犬类中,一剂WR242511影响下血液中MetHb浓度的变化率由以下关系决定:d[MetHb]/d(t) = kr.Cm.[Hb]-kh.[MetHb],其中kr为2.9 x 10(-5) ml.ng-1.hr-1,kh为0.0418 hr-1。该模型用多剂量数据进行了验证。该模型简单,并且与WR242511单剂量和多剂量给药条件下体内MetHb的生理行为相符。

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