Development and Evaluation of a Virtual Population of Children with Obesity for Physiologically Based Pharmacokinetic Modeling

Gerhart, Jacqueline G.; Carreño, Fernando; Edginton, Andrea N.; Sinha, Jaydeep; Perrin, Eliana M.; Kumar, Karan; Rikhi, Aruna; Hornik, Christoph P.; Harris, Vincent D.; Ganguly, Samit; Cohen‐Wolkowiez, Michael; González, Daniel

doi:10.1007/s40262-021-01072-4

Cited by 19 publications

(81 citation statements)

References 45 publications

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“…V ss can be defined using the equation below:

where V plasma is plasma volume, V tissue is tissue water volume, f u,p is fraction unbound in plasma, and f u,t is fraction unbound in tissue. Increased V plasma and V tissue (given more distribution space) can increase cardiac output during obesity ( Vasan, 2003 ; Colles et al, 2006 ; Gerhart et al, 2021 ), potentially increasing the V ss on an absolute scale. However, the extent of increase in V ss is also dependent on the drug binding to plasma protein (that determines

) as well as to the tissue components (that determines

), which are potentially altered due to altered composition during obesity.…”

Section: Physiological Considerationsmentioning

confidence: 99%

“…However, the extent of increase in V ss is also dependent on the drug binding to plasma protein (that determines

) as well as to the tissue components (that determines

), which are potentially altered due to altered composition during obesity. While studies have shown that plasma composition with respect to serum albumin and hematocrit are largely unaffected by obesity, it changes with respect to α 1-acid glycoprotein (AAG), which increases approximately 2-fold with obesity in adults ( Benedek et al, 1983 , 1984 ; Blouin et al, 1987 ; Gerhart et al, 2021 ). However, this increase in AAG has not yet been identified in pediatric populations with obesity due to limited studies ( Gerhart et al, 2021 ).…”

Section: Physiological Considerationsmentioning

confidence: 99%

“…While studies have shown that plasma composition with respect to serum albumin and hematocrit are largely unaffected by obesity, it changes with respect to α 1-acid glycoprotein (AAG), which increases approximately 2-fold with obesity in adults ( Benedek et al, 1983 , 1984 ; Blouin et al, 1987 ; Gerhart et al, 2021 ). However, this increase in AAG has not yet been identified in pediatric populations with obesity due to limited studies ( Gerhart et al, 2021 ).…”

Section: Physiological Considerationsmentioning

confidence: 99%

“…An increase in body fat with obesity is also accompanied by an increase in lean mass to provide additional structural (e.g., increased skeletal strength) and functional (e.g., increased metabolic need) support due to extra weight gain from adiposity. For example, key clearance organs such as the kidney and liver increase 19% and 18% in mass on average, respectively, with obesity ( Nawaratne et al, 1998 ; Gerhart et al, 2021 ). These organ mass increases were determined by a series of magnetic resonance imaging and dual x-ray absorptiometry studies in adults and ultrasound scans in pediatric populations with and without obesity ( Hwaung et al, 2019 ; Gerhart et al, 2021 ).…”

Section: Physiological Considerationsmentioning

confidence: 99%

“…For example, key clearance organs such as the kidney and liver increase 19% and 18% in mass on average, respectively, with obesity ( Nawaratne et al, 1998 ; Gerhart et al, 2021 ). These organ mass increases were determined by a series of magnetic resonance imaging and dual x-ray absorptiometry studies in adults and ultrasound scans in pediatric populations with and without obesity ( Hwaung et al, 2019 ; Gerhart et al, 2021 ). Unlike body fat, these increases in non-fat organs do not increase proportionately with obesity.…”

Section: Physiological Considerationsmentioning

confidence: 99%

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Characterizing Pharmacokinetics in Children With Obesity—Physiological, Drug, Patient, and Methodological Considerations

et al. 2022

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Childhood obesity is an alarming public health problem. The pediatric obesity rate has quadrupled in the past 30 years, and currently nearly 20% of United States children and 9% of children worldwide are classified as obese. Drug distribution and elimination processes, which determine drug exposure (and thus dosing), can vary significantly between patients with and without obesity. Obesity-related physiological changes, such as increased tissue volume and perfusion, altered blood protein concentrations, and tissue composition can greatly affect a drug’s volume of distribution, which might necessitate adjustment in loading doses. Obesity-related changes in the drug eliminating organs, such as altered enzyme activity in the liver and glomerular filtration rate, can affect the rate of drug elimination, which may warrant an adjustment in the maintenance dosing rate. Although weight-based dosing (i.e., in mg/kg) is commonly practiced in pediatrics, choice of the right body size metric (e.g., total body weight, lean body weight, body surface area, etc.) for dosing children with obesity still remains a question. To address this gap, the interplay between obesity-related physiological changes (e.g., altered organ size, composition, and function), and drug-specific properties (e.g., lipophilicity and elimination pathway) needs to be characterized in a quantitative framework. Additionally, methodological considerations, such as adequate sample size and optimal sampling scheme, should also be considered to ensure accurate and precise top-down covariate selection, particularly when designing opportunistic studies in pediatric drug development. Further factors affecting dosing, including existing dosing recommendations, target therapeutic ranges, dose capping, and formulations constraints, are also important to consider when undergoing dose selection for children with obesity. Opportunities to bridge the dosing knowledge gap in children with obesity include modeling and simulating techniques (i.e., population pharmacokinetic and physiologically-based pharmacokinetic [PBPK] modeling), opportunistic clinical data, and real world data. In this review, key considerations related to physiology, drug parameters, patient factors, and methodology that need to be accounted for while studying the influence of obesity on pharmacokinetics in children are highlighted and discussed. Future studies will need to leverage these modeling opportunities to better describe drug exposure in children with obesity as the childhood obesity epidemic continues.

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“…V ss can be defined using the equation below:

) as well as to the tissue components (that determines

), which are potentially altered due to altered composition during obesity.…”

Section: Physiological Considerationsmentioning

confidence: 99%

“…However, the extent of increase in V ss is also dependent on the drug binding to plasma protein (that determines

) as well as to the tissue components (that determines

Section: Physiological Considerationsmentioning

confidence: 99%

Section: Physiological Considerationsmentioning

confidence: 99%

Section: Physiological Considerationsmentioning

confidence: 99%

Section: Physiological Considerationsmentioning

confidence: 99%

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Characterizing Pharmacokinetics in Children With Obesity—Physiological, Drug, Patient, and Methodological Considerations

et al. 2022

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Use of Real‐World Data and Physiologically‐Based Pharmacokinetic Modeling to Characterize Enoxaparin Disposition in Children With Obesity

Gerhart

Carreño

Loop

et al. 2022

Clin Pharma and Therapeutics

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Dosing guidance for children with obesity is often unknown despite the fact that nearly 20% of US children are classified as obese. Enoxaparin, a commonly prescribed low-molecular-weight heparin, is dosed based on body weight irrespective of obesity status to achieve maximum concentration within a narrow therapeutic or prophylactic target range. However, whether children with and without obesity experience equivalent enoxaparin exposure remains unclear. To address this clinical question, 2,825 anti-activated factor X (anti-Xa) surrogate concentrations were collected from the electronic health records of 596 children, including those with obesity. Using linear mixed-effects regression models, we observed that 4-hour anti-Xa concentrations were statistically significantly different in children with and without obesity, even for children with the same absolute dose (P = 0.004). To further mechanistically explore obesity-associated differences in anti-Xa concentration, a pediatric physiologically-based pharmacokinetic (PBPK) model was developed in adults, and then scaled to children with and without obesity. This PBPK model incorporated binding of enoxaparin to antithrombin to form anti-Xa and elimination via heparinasemediated metabolism and glomerular filtration. Following scaling, the PBPK model predicted real-world pediatric concentrations well, with an average fold error (standard deviation of the fold error) of 0.82 (0.23) and 0.87 (0.26) in children with and without obesity, respectively. PBPK model simulations revealed that children with obesity have at most 20% higher 4-hour anti-Xa concentrations under recommended, total body weight-based dosing compared to children without obesity owing to reduced weight-normalized clearance. Enoxaparin exposure was better matched across age groups and obesity status using fat-free mass weight-based dosing.

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Another Step Toward Qualification of Pediatric Physiologically Based Pharmacokinetic Models to Facilitate Inclusivity and Diversity in Pediatric Clinical Studies

Small

Johnson

Yeo

2022

Clin Pharma and Therapeutics

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Study HighlightsWHAT IS THE CURRENT KNOWLEDGE ON THE TOPIC? Accurate prediction of pharmacokinetics (PKs) in pediatric subjects of diverse ages, ethnicities, and morbidities is critical. Qualification of pediatric physiologically-based pharmacokinetic (P-PBPK) models is an essential step towards enabling precision dosing of these vulnerable groups. WHAT QUESTION DID THIS STUDY ADDRESS? As a step toward qualification, the prediction accuracy of the pediatric module within the Simcyp simulator was assessed using robust PBPK models published previously for drugs in clinical use or development. WHAT DOES THIS STUDY ADD TO OUR KNOWLEDGE? PK parameters for 22 small-molecule compounds metabolized via CYP, UGT, FMO3, renal, non-renal, and complex routes were adequately predicted in pediatric cohorts, thus providing further confidence in the application of the pediatric module for dose predictions. HOW MIGHT THIS CHANGE CLINICAL PHARMA COLOGY OR TRANSLATIONAL SCIENCE? The analysis presented herein provides context for modelers, regulatory bodies, and other stake holders to support the full integration of P-PBPK modeling into critical Pediatric Investigation Plan and Pediatric Study Plans documents and for making informed decisions in real-world scenarios.

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Development and Evaluation of a Virtual Population of Children with Obesity for Physiologically Based Pharmacokinetic Modeling

Cited by 19 publications

References 45 publications

Characterizing Pharmacokinetics in Children With Obesity—Physiological, Drug, Patient, and Methodological Considerations

Characterizing Pharmacokinetics in Children With Obesity—Physiological, Drug, Patient, and Methodological Considerations

Use of Real‐World Data and Physiologically‐Based Pharmacokinetic Modeling to Characterize Enoxaparin Disposition in Children With Obesity

Another Step Toward Qualification of Pediatric Physiologically Based Pharmacokinetic Models to Facilitate Inclusivity and Diversity in Pediatric Clinical Studies

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