Feasibility of a Pragmatic PBPK Modeling Approach: Towards Model-Informed Dosing in Pediatric Clinical Care

Heijden, Joyce E. M. van der; Freriksen, Jolien J. M.; Hoop-Sommen, Marika A. de; Bussel, Lianne P. M. van; Driessen, Sander H. P.; Orlebeke, Anne E. M.; Verscheijden, Laurens F. M.; Greupink, Rick; Wildt, Saskia N. de

doi:10.1007/s40262-022-01181-8

Cited by 12 publications

(6 citation statements)

References 42 publications

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“…Our study sides with recent critiques of the twofold criterion. van der Heijden et al [ 29 ] argued that more stringent ranges for predicted-to-observed ratios should be considered. Another limitation of the twofold ranges was highlighted by Guest et al [ 30 ] and Abduljalil et al [ 13 ] who demonstrated the necessity of incorporating variability of the PK data into the evaluation procedure.…”

Section: Discussionmentioning

confidence: 99%

Towards More Robust Evaluation of the Predictive Performance of Physiologically Based Pharmacokinetic Models: Using Confidence Intervals to Support Use of Model-Informed Dosing in Clinical Care

van Borselen,

Sluijterman,

Greupink

et al. 2024

Clin Pharmacokinet

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Background and Objective With the rise in the use of physiologically based pharmacokinetic (PBPK) modeling over the past decade, the use of PBPK modeling to underpin drug dosing for off-label use in clinical care has become an attractive option. In order to use PBPK models for high-impact decisions, thorough qualification and validation of the model is essential to gain enough confidence in model performance. Currently, there is no agreed method for model acceptance, while clinicians demand a clear measure of model performance before considering implementing PBPK model-informed dosing. We aim to bridge this gap and propose the use of a confidence interval for the predicted-to-observed geometric mean ratio with predefined boundaries. This approach is similar to currently accepted bioequivalence testing procedures and can aid in improved model credibility and acceptance. Methods Two different methods to construct a confidence interval are outlined, depending on whether individual observations or aggregate data are available from the clinical comparator data sets. The two testing procedures are demonstrated for an example evaluation of a midazolam PBPK model. In addition, a simulation study is performed to demonstrate the difference between the twofold criterion and our proposed method. Results Using midazolam adult pharmacokinetic data, we demonstrated that creating a confidence interval yields more robust evaluation of the model than a point estimate, such as the commonly used twofold acceptance criterion. Additionally, we showed that the use of individual predictions can reduce the number of required test subjects. Furthermore, an easy-to-implement software tool was developed and is provided to make our proposed method more accessible. Conclusions With this method, we aim to provide a tool to further increase confidence in PBPK model performance and facilitate its use for directly informing drug dosing in clinical care. Supplementary Information The online version contains supplementary material available at 10.1007/s40262-023-01326-3.

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Section: Discussionmentioning

confidence: 99%

Towards More Robust Evaluation of the Predictive Performance of Physiologically Based Pharmacokinetic Models: Using Confidence Intervals to Support Use of Model-Informed Dosing in Clinical Care

van Borselen,

Sluijterman,

Greupink

et al. 2024

Clin Pharmacokinet

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“…A less time-consuming PBPK modeling approach in which pre-existing compound models are combined with pediatric physiology models can be pragmatic and feasible to predict PK and guide drug dosing in pediatric clinical care. 12,13 Rapid growth of PBPK to support drug development decisions in the last decade resulted in active engagement of major regulators to develop guidelines around the use of this technology. The process is a work in progress.…”

Section: Physiologically-based Pharmacokinetic Modeling For Drug Dosi...mentioning

confidence: 99%

“…We described a pragmatic workflow for pediatric PBPK model verification before, applying it to several drugs. 13 In this approach, a PBPK model is first verified with an adult population to demonstrate adequate predictive performance when predicting PKs in adults before integrating age-related physiological changes to predict PK in pediatrics and subsequently, if relevant, in preterm neonates. Below we describe relevant steps in more detail and we outline how the approach can be applied in three scenarios of decreasing clinical data availability for model verification.…”

Section: Model Verification Workflowmentioning

confidence: 99%

“…Often, these models were developed to simulate PKs in adult populations, and were rarely explored for their potential to guide drug dosing in children. A less time‐consuming PBPK modeling approach in which pre‐existing compound models are combined with pediatric physiology models can be pragmatic and feasible to predict PK and guide drug dosing in pediatric clinical care 12,13 …”

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confidence: 99%

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Physiologically‐Based Pharmacokinetic Modeling for Drug Dosing in Pediatric Patients: A Tutorial for a Pragmatic Approach in Clinical Care

Heijden

Freriksen

Hoop-Sommen

et al. 2023

Clin Pharma and Therapeutics

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It is well accepted that off‐label drug dosing recommendations for pediatric patients should be based on the best available evidence. However, the available traditional evidence is often low. To bridge this gap, physiologically‐based pharmacokinetic (PBPK) modeling is a scientifically well‐founded tool that can be used to enable model‐informed dosing (MID) recommendations in children in clinical practice. In this tutorial, we provide a pragmatic, PBPK‐based pediatric modeling workflow. For this approach to be successfully implemented in pediatric clinical practice, a thorough understanding of the model assumptions and limitations is required. More importantly, careful evaluation of a MID approach within the context of overall benefits and the potential risks is crucial. The tutorial is aimed to help modelers, researchers and clinicians, to effectively employ PBPK simulations to support pediatric drug dosing.

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“…However, in the field of paediatric pharmacokinetics, the use of pharmacokinetic modelling, particularly physiological-based pharmacokinetics (PBPK), has revolutionised the ability to extrapolate drug pharmacokinetics across age groups, allowing for pragmatic determination of paediatric plasma concentrations to support drug licensing and clinical dosing. This approach relies on the established principles of mechanistic PBPK modelling to describe tissue volumes, tissue perfusion, renal/liver function, blood biochemistry and drug metabolism enzyme/and drug transporter protein expression [ 15 ], in addition to the inclusion of development changes [ 16 , 17 , 18 , 19 , 20 , 21 , 22 ].…”

Section: Introductionmentioning

confidence: 99%

Virtual Clinical Trials Guided Design of an Age-Appropriate Formulation and Dosing Strategy of Nifedipine for Paediatric Use

et al. 2023

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The rapid onset of action of nifedipine causes a precipitous reduction in blood pressure leading to adverse effects associated with reflex sympathetic nervous system (SNS) activation, including tachycardia and worsening myocardial and cerebrovascular ischemia. As a result, short acting nifedipine preparations are not recommended. However, importantly, there are no modified release preparations of nifedipine authorised for paediatric use, and hence a paucity of clinical studies reporting pharmacokinetics data in paediatrics. Pharmacokinetic parameters may differ significantly between children and adults due to anatomical and physiological differences, often resulting in sub therapeutic and/or toxic plasma concentrations of medication. However, in the field of paediatric pharmacokinetics, the use of pharmacokinetic modelling, particularly physiological-based pharmacokinetics (PBPK), has revolutionised the ability to extrapolate drug pharmacokinetics across age groups, allowing for pragmatic determination of paediatric plasma concentrations to support drug licensing and clinical dosing. In order to pragmatically assess the translation of resultant dissolution profiles to the paediatric populations, virtual clinical trials simulations were conducted. In the context of formulation development, the use of PBPK modelling allowed the determination of optimised formulations that achieved plasma concentrations within the target therapeutic window throughout the dosing strategy. A 5 mg sustained release mini-tablet was successfully developed with the duration of release extending over 24 h and an informed optimised dosing strategy of 450 µg/kg twice daily. The resulting formulation provides flexible dosing opportunities, improves patient adherence by reducing frequent administration burden and enhances patient safety profiles by maintaining efficacious levels of consistent drug plasma levels over a sustained period of time.

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Feasibility of a Pragmatic PBPK Modeling Approach: Towards Model-Informed Dosing in Pediatric Clinical Care

Cited by 12 publications

References 42 publications

Towards More Robust Evaluation of the Predictive Performance of Physiologically Based Pharmacokinetic Models: Using Confidence Intervals to Support Use of Model-Informed Dosing in Clinical Care

Towards More Robust Evaluation of the Predictive Performance of Physiologically Based Pharmacokinetic Models: Using Confidence Intervals to Support Use of Model-Informed Dosing in Clinical Care

Physiologically‐Based Pharmacokinetic Modeling for Drug Dosing in Pediatric Patients: A Tutorial for a Pragmatic Approach in Clinical Care

Virtual Clinical Trials Guided Design of an Age-Appropriate Formulation and Dosing Strategy of Nifedipine for Paediatric Use

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