Paracetamol pharmacokinetics and metabolism in young women

Allegaert, Karel; Peeters, Mariska Y. M.; Beleyn, Bjorn; Smits, Anne; Kulo, Aida; Calsteren, Kristel Van; Deprest, Jan; Hoon, Jan de; Knibbe, Catherijne A. J.

doi:10.1186/s12871-015-0144-3

Cited by 17 publications

(19 citation statements)

References 26 publications

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“…In brief, first, a PBPK model was previously developed for both intravenous and oral acetaminophen administration in non-pregnant women. The predictive performance of the model was evaluated by comparing simulations with observed in vivo pharmacokinetic profiles of acetaminophen, acetaminophen-glucuronide, acetaminophen-sulphate, and unchanged acetaminophen after both oral and intravenous acetaminophen administration of standard dosages [20][21][22]. Once the non-pregnant PBPK model captured the observed pharmacokinetics adequately, all drug-specific parameters were fixed and pregnancy-specific changes were incorporated.…”

Section: Development Of Fetal-maternal Physiologically Based Pharmacomentioning

confidence: 99%

“…Once the non-pregnant PBPK model captured the observed pharmacokinetics adequately, all drug-specific parameters were fixed and pregnancy-specific changes were incorporated. Model performance was evaluated by comparing simulations with observed in vivo pharmacokinetic profiles of acetaminophen, acetaminophenglucuronide, acetaminophen-sulphate, and unchanged acetaminophen obtained from third-trimester pregnant women [20]. For more detailed information about parameterization and validation of the previously developed pregnancy PBPK model we refer to Mian et al [17].…”

Section: Development Of Fetal-maternal Physiologically Based Pharmacomentioning

confidence: 99%

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Integration of Placental Transfer in a Fetal–Maternal Physiologically Based Pharmacokinetic Model to Characterize Acetaminophen Exposure and Metabolic Clearance in the Fetus

et al. 2020

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Background and Objective Although acetaminophen is frequently used during pregnancy, little is known about fetal acetaminophen pharmacokinetics. Acetaminophen safety evaluation has typically focused on hepatotoxicity, while other events (fetal ductal closure/constriction) are also relevant. We aimed to develop a fetal-maternal physiologically based pharmacokinetic (PBPK) model (f-m PBPK) to quantitatively predict placental acetaminophen transfer, characterize fetal acetaminophen exposure, and quantify the contributions of specific clearance pathways in the term fetus. Methods An acetaminophen pregnancy PBPK model was extended with a compartment representing the fetal liver, which included maturation of relevant enzymes. Different approaches to describe placental transfer were evaluated (ex vivo cotyledon perfusion experiments, placental transfer prediction based on Caco-2 cell permeability or physicochemical properties [MoBi ® ]). Predicted maternal and fetal acetaminophen profiles were compared with in vivo observations. Results Tested approaches to predict placental transfer showed comparable performance, although the ex vivo approach showed highest prediction accuracy. Acetaminophen exposure in maternal venous blood was similar to fetal venous umbilical cord blood. Prediction of fetal acetaminophen clearance indicated that the median molar dose fraction converted to acetaminophen-sulphate and N-acetyl-p-benzoquinone imine was 0.8% and 0.06%, respectively. The predicted mean acetaminophen concentration in the arterial umbilical cord blood was 3.6 mg/L. Conclusion The median dose fraction of acetaminophen converted to its metabolites in the term fetus was predicted. The various placental transfer approaches supported the development of a generic f-m PBPK model incorporating in vivo placental drug transfer. The predicted arterial umbilical cord acetaminophen concentration was far below the suggested postnatal threshold (24.47 mg/L) for ductal closure.

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Section: Development Of Fetal-maternal Physiologically Based Pharmacomentioning

confidence: 99%

Section: Development Of Fetal-maternal Physiologically Based Pharmacomentioning

confidence: 99%

Integration of Placental Transfer in a Fetal–Maternal Physiologically Based Pharmacokinetic Model to Characterize Acetaminophen Exposure and Metabolic Clearance in the Fetus

et al. 2020

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“…Regarding the plasma concentration-time profiles of oral acetaminophen 1000 mg in non-pregnant and pregnant populations (ESM_2A), maximum concentration (C max ) values were higher in non-pregnant women and decreased with increasing duration of gestational week, while the AUC from time zero to 6 h (AUC 0-6h ) decreased with increasing duration of gestational age. Regarding the plasma concentration-time profiles of NAPQI after administration of oral [31] acetaminophen plasma concentration-time profiles (left) and predicted and observed [31] acetaminophen inactive metabolites urine concentration-time profiles (right) in populations of a non-pregnant women after administration of intravenous acetaminophen 2000 mg and b third trimester pregnant women after administration of an intravenous acetaminophen 2000 mg loading dose followed by 1000 mg every 6 h. For the inactive metabolites, orange, pink, and green indicate acetaminophen glucuronide, acetaminophen sulfate, and unchanged acetaminophen in urine concentrations, respectively. The shaded area denotes the predicted 95% confidence interval.…”

Section: Pbpk Models For Acetaminophenmentioning

confidence: 99%

“…Following oral administration of acetaminophen 1000 mg, the predicted C ss,avg (median [interquartile range, IQR]) was 6.7 Goodness-of-fit plot (predicted concentration versus observed concentration) for acetaminophen and its metabolites (acetaminophen unchanged, acetaminophen glucuronide, acetaminophen sulfate). For non-pregnant women, observed acetaminophen data were taken from Allegaert et al [31], Mitchell et al [34], and Beaulac-Baillargeon and Rocheleau [33]; for pregnant women, observed acetaminophen, acetaminophen glucuronide, and acetaminophen sulfate data were taken from Allegaert et al [31] and Beaulac-Baillargeon and Rocheleau [33]. The solid line denotes the line of identity.…”

Section: Acetaminophen Average Concentration At Steady State and Acetmentioning

confidence: 99%

“…Observed PK parameters for acetaminophen for both non-pregnant and pregnant women following oral administration of 650 mg are taken from Beaulac-Baillargeon and Rocheleau [33] and those following intravenous administration of 2000 mg from Allegaert et al [31]. Data are expressed as mean AUC ∞ area under the plasma concentration-time curve from time zero to infinity, CL clearance, C max maximum concentration, F bioavailability, PK pharmacokinetic, mg/L in non-pregnant women and in the first, second, and third trimester of pregnancy, respectively (Fig.…”

Section: Acetaminophen Average Concentration At Steady State and Acetmentioning

confidence: 99%

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Physiologically Based Pharmacokinetic Modeling to Characterize Acetaminophen Pharmacokinetics and N-Acetyl-p-Benzoquinone Imine (NAPQI) Formation in Non-Pregnant and Pregnant Women

et al. 2019

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Background and Objective Little is known about acetaminophen (paracetamol) pharmacokinetics during pregnancy. The aim of this study was to develop a physiologically based pharmacokinetic (PBPK) model to predict acetaminophen pharmacokinetics throughout pregnancy. Methods PBPK models for acetaminophen and its metabolites were developed in non-pregnant and pregnant women. Physiological and enzymatic changes in pregnant women expected to impact acetaminophen pharmacokinetics were considered. Models were evaluated using goodness-of-fit plots and by comparing predicted pharmacokinetic profiles with in vivo pharmacokinetic data. Predictions were performed to illustrate the average concentration at steady state (C ss,avg) values, used as an indicator for efficacy, of acetaminophen achieved following administration of 1000 mg every 6 h. Furthermore, as a measurement of potential hepatotoxicity, the molar dose fraction of acetaminophen converted to N-acetyl-p-benzoquinone imine (NAPQI) was estimated. Results PBPK models successfully predicted the pharmacokinetics of acetaminophen and its metabolites in non-pregnant and pregnant women. Predictions resulted in the lowest C ss,avg in the third trimester (median [interquartile range]: 4.5 [3.8-5.1] mg/L), while C ss,avg was 6.7 [5.9-7.4], 5.6 [4.7-6.3], and 4.9 [4.1-5.5] mg/L in non-pregnant, first trimester, and second trimester populations, respectively. Assuming a constant raised cytochrome P450 2E1 activity throughout pregnancy, the molar dose fraction of acetaminophen converted to NAPQI was highest during the first trimester (median [interquartile range]: 11.0% [9.1-13.4%]), followed by the second (9.0% [7.5-11.0%]) and third trimester (8.2% [6.8-10.1%]), compared with non-pregnant women (7.7% [6.4-9.4%]). Conclusion Acetaminophen exposure is lower in pregnant than in non-pregnant women, and is related to pregnancy duration. Despite these findings, higher dose adjustments cannot be advised yet as it is unknown whether pregnancy affects the toxicodynamics of NAPQI. Information on glutathione abundance during pregnancy and NAPQI in vivo data are required to further refine the presented model.

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Predisposing Factors for Adverse Drug Reactions

Jose,

de Abajo

2024

Principles and Practice of Pharmacovigilance and Drug Safety

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Paracetamol pharmacokinetics and metabolism in young women

Cited by 17 publications

References 26 publications

Integration of Placental Transfer in a Fetal–Maternal Physiologically Based Pharmacokinetic Model to Characterize Acetaminophen Exposure and Metabolic Clearance in the Fetus

Integration of Placental Transfer in a Fetal–Maternal Physiologically Based Pharmacokinetic Model to Characterize Acetaminophen Exposure and Metabolic Clearance in the Fetus

Physiologically Based Pharmacokinetic Modeling to Characterize Acetaminophen Pharmacokinetics and N-Acetyl-p-Benzoquinone Imine (NAPQI) Formation in Non-Pregnant and Pregnant Women

Predisposing Factors for Adverse Drug Reactions

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