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Abstract
Background: Hypotension, cardiac failure, QT interval prolongation, dysrhythmias, and conduction disturbances are common complications of overdoses with cardiotoxicants. Pharmacokinetic/pharmacodynamic (PK/PD) relationships are useful to assess diagnosis, prognosis, and treatment efficacy in acute poisonings. Objective: To review the utility and limits of PK/PD studies of cardiac toxicity. Methods: Discussion of various models, mainly those obtained in digitalis, cyanide, venlafaxine and citalopram poisonings. Results/conclusions: A sigmoidal Emax model appears adequate to represent the PK/PD relationships in cardiotoxic poisonings. PK/PD correlations investigate the discrepancies between the time course of the effect magnitude and its evolving concentrations. They may help in understanding the mechanisms of occurrence as well as disappearance of a cardiotoxic effect. When data are sparse, population-based PK/PD modeling using computer-intensive algorithms is helpful to estimate population mean values of PK parameters as well as their individual variability. Further PK/PD studies are needed in medical toxicology to allow understanding of the meaning of blood toxicant concentration in acute poisonings and thus improve management.
Acknowledgments
The authors would like to acknowledge Stephen W Borron, from the Division of Emergency Medicine (Surgery), University of Texas Health Science Center at San Antonio, USA for his helpful review of this manuscript.