A physiologically based pharmacokinetic and pharmacodynamic (PBPK/PD) model of the histone deacetylase (HDAC) inhibitor vorinostat for pediatric and adult patients and its application for dose specification

Moj, Daniel; Britz, Hannah; Burhenne, Jürgen; Stewart, Clinton F.; Egerer, Gerlinde; Haefeli, Walter E.; Lehr, Thorsten

doi:10.1007/s00280-017-3447-x

Cited by 22 publications

(7 citation statements)

References 72 publications

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“…The P‐PBPK dose prediction articles included in the study, the name of the drug, the platform, and the study's funding are described in Table 1. Verified PBPK models of drugs are presented in support of pediatric dose prediction (Figure 4): 13 articles reported results from P‐PBPK models, which are presented in support of dose selection, 30–42 five articles were on the optimization of dosage in the design of future pediatric clinical studies, 3,29,43–45 and six articles reported findings from studies on determining dose regimens 46–51 . Fourteen publications were on some special pediatric populations and uncommon diseases with an assessment of renal impairment, 52–56 children with obesity, 57–60 and pediatric patients with severe coronavirus disease 2019 (COVID‐19) disease 61–65 .…”

Section: Resultsmentioning

confidence: 99%

Predicting the correct dose in children: Role of computational Pediatric Physiological‐based pharmacokinetics modeling tools

Zhang

Dun

Chen

et al. 2022

CPT Pharmacom & Syst Pharma

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The pharmacokinetics (PKs) and safety of medications in particular groups can be predicted using the physiologically-based pharmacokinetic (PBPK) model. Using the PBPK model may enable safe pediatric clinical trials and speed up the process of new drug research and development, especially for children, a population in which it is relatively difficult to conduct clinical trials. This review summarizes the role of pediatric PBPK (P-PBPK) modeling software in dose prediction over the past 6 years and briefly introduces the process of general P-PBPK modeling.We summarized the theories and applications of this software and discussed the application trends and future perspectives in the area. The modeling software's extensive use will undoubtedly make it easier to predict dose prediction for young patients.

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Section: Resultsmentioning

confidence: 99%

Predicting the correct dose in children: Role of computational Pediatric Physiological‐based pharmacokinetics modeling tools

Zhang

Dun

Chen

et al. 2022

CPT Pharmacom & Syst Pharma

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“…Secondly, phenoconversion for some conditions (e.g., inflammation) may only develop after prolonged or repeated exposure, which requires in-vitro models, such as 3D liver spheroids, in which the long-term consequences of these factors for drug metabolism can be adequately studied [ 68 , 69 ]. In-silico models, such as physiologically based pharmacokinetic (PBPK) models, have also been suggested as an excellent approach to study phenoconversion [ 70 , 71 , 72 , 73 , 74 , 75 ]. These models are particularly suitable to investigate the effects of complex interactions between multiple drugs and disease states.…”

Section: Discussionmentioning

confidence: 99%

Phenoconversion of Cytochrome P450 Metabolism: A Systematic Review

Klomp

Manson

Guchelaar

et al. 2020

JCM

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Phenoconversion is the mismatch between the individual’s genotype-based prediction of drug metabolism and the true capacity to metabolize drugs due to nongenetic factors. While the concept of phenoconversion has been described in narrative reviews, no systematic review is available. A systematic review was conducted to investigate factors contributing to phenoconversion and the impact on cytochrome P450 metabolism. Twenty-seven studies met the inclusion criteria and were incorporated in this review, of which 14 demonstrate phenoconversion for a specific genotype group. Phenoconversion into a lower metabolizer phenotype was reported for concomitant use of CYP450-inhibiting drugs, increasing age, cancer, and inflammation. Phenoconversion into a higher metabolizer phenotype was reported for concomitant use of CYP450 inducers and smoking. Moreover, alcohol, pregnancy, and vitamin D exposure are factors where study data suggested phenoconversion. The studies reported genotype–phenotype discrepancies, but the impact of phenoconversion on the effectiveness and toxicity in the clinical setting remains unclear. In conclusion, phenoconversion is caused by both extrinsic factors and patient- and disease-related factors. The mechanism(s) behind and the extent to which CYP450 metabolism is affected remain unexplored. If studied more comprehensively, accounting for phenoconversion may help to improve our ability to predict the individual CYP450 metabolism and personalize drug treatment.

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“…These models have been used frequently to simulate drug pharmacokinetics [ 13 – 15 ] and especially in elucidating complex DDI with various co-medications, all of which may be impossible to study through dedicated clinical trials [ 16 – 18 ]. PBPK models are often linked with PD models in order to predict changes in drug effect due to extrinsic or intrinsic factors that affect the drug PK, for which a recent example being the work of Moj et al [ 19 ]. Blei [ 20 ] developed a PBPK model for amlodipine, but the model did not include CYP3A4-mediated clearance, which is essential in order to model mechanistic DDI with perpetrator drugs.…”

Section: Introductionmentioning

confidence: 99%

Guiding dose adjustment of amlodipine after co-administration with ritonavir containing regimens using a physiologically-based pharmacokinetic/pharmacodynamic model

Mukherjee

Zha

Menon

et al. 2018

J Pharmacokinet Pharmacodyn

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Amlodipine, a commonly prescribed anti-hypertensive drug, shows increased systemic exposure with cytochrome P450 (CYP) 3A inhibitors. Ritonavir (RTV) is a potent mechanism-based and reversible CYP3A inhibitor and moderate inducer that is used as a pharmacokinetic enhancer in several antiviral treatment regimens. Drug–drug interaction (DDI) between RTV and amlodipine is due to mixed inhibition and induction of CYP3A4, which is challenging to predict without a mechanistic model that accounts for the complexity of both mechanisms occurring simultaneously. A novel physiologically-based pharmacokinetic (PBPK) model was developed for amlodipine, and the model was verified using published clinical PK and DDI data. The verified amlodipine PBPK model was linked to a pharmacodynamics model that describes changes in systolic blood pressure (SBP) during and after co-administration with RTV. The magnitude and time course of RTV effects on amlodipine plasma exposures and SBP were evaluated, to provide guidance on dose adjustment of amlodipine during and after co-administration with RTV-containing regimens. Model simulations suggested that the increase in amlodipine’s plasma exposure by RTV diminishes by approximately 80% within 5 days after the last dose of RTV. PBPK simulations suggested that resuming a full dose of amlodipine [5 mg once daily (QD)] immediately after RTV’s last dose would decrease daily average SBP by a maximum of 3.3 mmHg, while continuing with the reduced dose (2.5 mg QD) for 5 days after the last dose of RTV would increase daily average SBP by a maximum of 5.8 mmHg. Based on these results, either approach of resuming amlodipine’s full dose could be appropriate when combined with appropriate clinical monitoring.Electronic supplementary materialThe online version of this article (10.1007/s10928-018-9574-0) contains supplementary material, which is available to authorized users.

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A physiologically based pharmacokinetic and pharmacodynamic (PBPK/PD) model of the histone deacetylase (HDAC) inhibitor vorinostat for pediatric and adult patients and its application for dose specification

Cited by 22 publications

References 72 publications

Predicting the correct dose in children: Role of computational Pediatric Physiological‐based pharmacokinetics modeling tools

Predicting the correct dose in children: Role of computational Pediatric Physiological‐based pharmacokinetics modeling tools

Phenoconversion of Cytochrome P450 Metabolism: A Systematic Review

Guiding dose adjustment of amlodipine after co-administration with ritonavir containing regimens using a physiologically-based pharmacokinetic/pharmacodynamic model

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