Stochastic Prediction of Cyp3a-Mediated Inhibition of Midazolam Clearance by Ketoconazole

Chien, Jenny Y.; Lucksiri, Aroonrut; Ernest, C. Steven; Gorski, J. Christopher; Wrighton, Steven; Hall, Stephen D.

doi:10.1124/dmd.105.008730

Cited by 73 publications

(98 citation statements)

References 49 publications

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“…However, when they are administrated simultaneously, models (1) and (2) need to be connected by (3) (Ito et al 1998) (3) As a result, (A1 I , A2 I , A1 S , A2 S ) need to be jointly solved. In (3), fu I =0.03 (Martinez-Jorda 1990) is the unbound fraction of KETO in plasma, MW I =0.53 is the molecular weight of the inhibitor, and Ki is the inhibition constant.…”

Section: Mdz Pharmacokinetic Model-mentioning

confidence: 99%

“…Assuming a simultaneous oral dose KETO and an IV dose for MDZ, the interaction PK models follow equations (1) and (2) connected by (3). The inhibition constant Ki is assumed to take value of (0.0037, 0.01, 0.18) μM to assess their influence on DDI prediction.…”

Section: Keto/mdz Interaction Predictionmentioning

confidence: 99%

“…The predicted logtransformed drug concentrations for KETO are calculated from the differential equation model (1) and the predicted log-transformed drug concentrations for MDZ are calculated from the differential equation model (2). Based on (known) DDI parameters, (Km I , Km S ,fu I , Ki,MW I ), the DDI outcome, AUCR, is then predicted by models (1) and (2) linked by (3). .…”

Section: Keto/mdz Examplementioning

confidence: 99%

See 2 more Smart Citations

A Bayesian Meta-Analysis on Published Sample Mean and Variance Pharmacokinetic Data with Application to Drug–Drug Interaction Prediction

Kim

Wang

et al. 2008

Journal of Biopharmaceutical Statistics

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SummaryIn drug-drug interaction (DDI) research, a two drug interaction is usually predicted by individual drug pharmacokinetics (PK). Although subject-specific drug concentration data from clinical PK studies on inhibitor or inducer and substrate's PK are not usually published, sample mean plasma drug concentrations and their standard deviations have been routinely reported. Hence there is a great need for meta-analysis and DDI prediction using such summarized PK data. In this paper, an innovative DDI prediction method based on a three-level hierarchical Bayesian meta-analysis model is developed. The three levels model sample means and variances, between-study variances, and prior distributions. Through a ketoconazle-midazolam example and simulations, we demonstrate that our meta-analysis model can not only estimate PK parameters with small bias, but also recover their between-study and between-subject variances well. More importantly, the posterior distributions of PK parameters and their variance components allow us to predict DDI at both population-average and study-specific levels. We are also able to predict the DDI between-subject/study variance. These statistical predictions have never been investigated in DDI research. Our simulation studies show that our meta-analysis approach has small bias in PK parameter estimates and DDI predictions. Sensitivity analysis was conducted to investigate the influences of interaction PK parameters, such as the inhibition constant Ki, on the DDI prediction.

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Section: Mdz Pharmacokinetic Model-mentioning

confidence: 99%

Section: Keto/mdz Interaction Predictionmentioning

confidence: 99%

Section: Keto/mdz Examplementioning

confidence: 99%

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A Bayesian Meta-Analysis on Published Sample Mean and Variance Pharmacokinetic Data with Application to Drug–Drug Interaction Prediction

Kim

Wang

et al. 2008

Journal of Biopharmaceutical Statistics

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“…Michaelis-Menten equations are used for all enzymatic reactions. A competitive Michaelis-Menten inhibition model is used for this simulation as used for midazolam and ketoconazole inhibition by (Chien et al, 2006). In order to increase the predictive performance, a simplified pathway is used for the generation of simulation models from the viewpoint of the trade-off between model complexity and data availability.…”

Section: Automatic Generation Of Drug Metabolic Pharmacokinetic Modelsmentioning

confidence: 99%

Towards an In Silico Approach to Personalized Pharmacokinetics

Konagaya¹

2012

Molecular Interactions

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“…The inhibitor concentration, [I], is often based on plasma concentrations because concentrations at the site of inhibition cannot be measured (47,44). Because of this, various inhibitor concentrations including plasma C max , plasma free C max , portal vein C max (inlet liver concentration) and portal vein free C max have been explored for prediction accuracy (44,(47)(48)(49). In some cases, the use of portal vein C max is fairly accurate in DDI prediction and for other compounds the portal vein free C max or plasma C max is reasonable as well.…”

Section: Use Of Cyp Inhibition Data: Ranking Extrapolation and Ddi Pmentioning

confidence: 99%

In Vitro Evaluation of Reversible and Irreversible Cytochrome P450 Inhibition: Current Status on Methodologies and their Utility for Predicting Drug–Drug Interactions

Fowler

Zhang

2008

AAPS J

157

108

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Abstract. It is widely accepted that today's practice of polypharmacy inevitably increases the incidence of drug-drug interactions (DDIs). Serious DDI is a major liability for any new chemical entity (NCE) entering the pharmaceutical market. As such, pharmaceutical companies employ various strategies to avoid problematic compounds for clinical development. A key cause for DDIs is the inhibition of cytochrome P450 enzymes (CYPs) that are responsible for metabolic clearance of many drugs. Screening for inhibition potency of CYPs by NCEs has therefore become a routine practice during the drug discovery stage. However, in order to make proper use of DDI data, an understanding of the strengths and weaknesses of the various experimental systems in current use is required. An illustrated review of experimental practices is presented with discussion of likely future developments. The combination of high quality in vitro data generation and the application of in vivo CYP inhibition modelling approaches should allow more informed decisions to be made in the search for drug molecules with acceptable DDI characteristics.

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Stochastic Prediction of Cyp3a-Mediated Inhibition of Midazolam Clearance by Ketoconazole

Cited by 73 publications

References 49 publications

A Bayesian Meta-Analysis on Published Sample Mean and Variance Pharmacokinetic Data with Application to Drug–Drug Interaction Prediction

A Bayesian Meta-Analysis on Published Sample Mean and Variance Pharmacokinetic Data with Application to Drug–Drug Interaction Prediction

Towards an In Silico Approach to Personalized Pharmacokinetics

In Vitro Evaluation of Reversible and Irreversible Cytochrome P450 Inhibition: Current Status on Methodologies and their Utility for Predicting Drug–Drug Interactions

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