Drug Disposition in Subjects With Obesity: The Research Work of Darrell R. Abernethy

Greenblatt, David J.; Bruno, Christopher D.; Harmatz, Jerold S.; Zhang, Qingchen; Chow, Christina R.

doi:10.1002/jcph.2093

Cited by 13 publications

(33 citation statements)

References 101 publications

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“…Most body weight scalers demonstrate a nonlinear relationship between clearance and size, a relationship that is evident in both obese and lean individuals [ 1 ]. The rate of clearance increase slows as size increases; consequently dose, when expressed as per kilogram of total body weight, is invariably excessive.…”

Section: Pharmacokinetic Concepts To Determine Dosementioning

confidence: 99%

“…Total body weight dosing in obese children contributes to dose errors because the contribution from the fat mass portion of the body composition is not acknowledged. Although it is recognized that fat mass may influence pharmacokinetic parameters such as volume of distribution (V) or clearance (CL) [ 1 ], that the effect of fat mass is drug-specific [ 1 ], that weight-based dosing is a contributor to dose inaccuracies and that obesity influences disease processes, there are few practical dose recommendations for obese children [ 2 , 3 ]. A smorgasbord of body weight scalers (e.g., total body weight, body surface area, ideal body weight, lean body mass, adjusted body weight, body mass index, fat-free mass, allometry) have been used to determine dose in the obese individual [ 4 ].…”

Section: Introductionmentioning

confidence: 99%

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Considerations for Intravenous Anesthesia Dose in Obese Children: Understanding PKPD

Morse

Cortínez

Anderson

2023

JCM

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The intravenous induction or loading dose in children is commonly prescribed per kilogram. That dose recognizes the linear relationship between volume of distribution and total body weight. Total body weight comprises both fat and fat-free mass. Fat mass influences the volume of distribution and the use of total body weight fails to recognize the impact of fat mass on pharmacokinetics in children. Size metrics alternative to total body mass (e.g., fat-free and normal fat mass, ideal body weight and lean body weight) have been proposed to scale pharmacokinetic parameters (clearance, volume of distribution) for size. Clearance is the key parameter used to calculate infusion rates or maintenance dosing at steady state. Dosing schedules recognize the curvilinear relationship, described using allometric theory, between clearance and size. Fat mass also has an indirect influence on clearance through both metabolic and renal function that is independent of its effects due to increased body mass. Fat-free mass, lean body mass and ideal body mass are not drug specific and fail to recognize the variable impact of fat mass contributing to body composition in children, both lean and obese. Normal fat mass, used in conjunction with allometry, may prove a useful size metric but computation by clinicians for the individual child is not facile. Dosing is further complicated by the need for multicompartment models to describe intravenous drug pharmacokinetics and the concentration effect relationship, both beneficial and adverse, is often poorly understood. Obesity is also associated with other morbidity that may also influence pharmacokinetics. Dose is best determined using pharmacokinetic–pharmacodynamic (PKPD) models that account for these varied factors. These models, along with covariates (age, weight, body composition), can be incorporated into programmable target-controlled infusion pumps. The use of target-controlled infusion pumps, assuming practitioners have a sound understanding of the PKPD within programs, provide the best available guide to intravenous dose in obese children.

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Section: Pharmacokinetic Concepts To Determine Dosementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Considerations for Intravenous Anesthesia Dose in Obese Children: Understanding PKPD

Morse

Cortínez

Anderson

2023

JCM

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“…Failure to account for fat mass contributes to dosing errors. There are few practical dose recommendations for obese children [ 2 , 19 ] even though it is known that fat mass influences the volume of distribution and clearance [ 20 ], that effects from fat mass are drug-specific [ 20 ], and that dosing per kilogram (weight-based linear dosing) is a contributor to dose inaccuracies. Further, obesity can be considered an inflammatory disease that both contributes to disease processes and is sometimes consequent to disease processes.…”

Section: Size Model Foiblesmentioning

confidence: 99%

“…The difference between the linear total body weight prediction and the allometric weight prediction increases with total body weight. Other bodyweight scalers shown in Figure 3 (body surface area, fat-free mass) are also curvilinear in nature, a relationship that exists in both obese and lean individuals [ 20 ]. There is no change at any one weight where a size scaler should be changed from one to another.…”

Section: Dosing Concepts In the Childmentioning

confidence: 99%

Perioperative Acetaminophen Dosing in Obese Children

Anderson

Cortínez

2023

Children

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Acetaminophen is a commonly used perioperative analgesic drug in children. The use of a preoperative loading dose achieves a target concentration of 10 mg/L associated with a target analgesic effect that is 2.6 pain units (visual analogue scale 1–10). Postoperative maintenance dosing is used to keep this effect at a steady-state concentration. The loading dose in children is commonly prescribed per kilogram. That dose is consistent with the linear relationship between the volume of distribution and total body weight. Total body weight is made up of both fat and fat-free mass. The fat mass has little influence on the volume of distribution of acetaminophen but fat mass should be considered for maintenance dosing that is determined by clearance. The relationship between the pharmacokinetic parameter, clearance, and size is not linear. A number of size metrics (e.g., fat-free and normal fat mass, ideal body weight and lean body weight) have been proposed to scale clearance and all consequent dosing schedules recognize curvilinear relationships between clearance and size. This relationship can be described using allometric theory. Fat mass also has an indirect influence on clearance that is independent of its effects due to increased body mass. Normal fat mass, used in conjunction with allometry, has proven a useful size metric for acetaminophen; it is calculated using fat-free mass and a fraction (Ffat) of the additional mass contributing to total body weight. However, the Ffat for acetaminophen is large (Ffat = 0.82), pharmacokinetic and pharmacodynamic parameter variability high, and the concentration–response slope gentle at the target concentration. Consequently, total body weight with allometry is acceptable for the calculation of maintenance dose. The dose of acetaminophen is tempered by concerns about adverse effects, notably hepatotoxicity associated with use after 2–3 days at doses greater than 90 mg/kg/day.

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“…The HPLC retention index has been used to explain drug uptake into specific tissues and partially explain the variability in volume of distribution. 18 LogP, the logarithm of the partition coefficient, is another widely used quantitative measure of lipophilicity, it can be measured experimentally or by way of computational methods based on molecular descriptors, which offer a fast and cost-effective way to estimate lipophilicity. 15 Like HPLC, logP measures have been found to explain a portion of the variability in the volume of distribution measures.…”

Section: What Is the Role Of The Therapeutic Window Of A Drug For Inf...mentioning

confidence: 99%

Is There a Need for a Dedicated Pharmacokinetic Trial for a Drug in Obese Populations? A Drug Prioritization Decision Tree Framework

Langevin,

Gobburu,

Gopalakrishnan

2023

The Journal of Clinical Pharma

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Obesity is a growing global health concern associated with high comorbidity rates, leading to an increasing number of patients who are obese requiring medication. However, clinical trials often exclude or under‐represent individuals who are obese, creating the need for a methodology to adjust labeling to ensure safe and effective dosing for all patients. To address this, we developed a 2‐part decision tree framework to prioritize drugs for dedicated pharmacokinetic studies in obese subjects. Leveraging current drug knowledge and modeling techniques, the decision tree system predicts expected exposure changes and recommends labeling strategies, allowing stakeholders to prioritize resources toward the drugs most in need. In a case study evaluating 30 drugs from literature across different therapeutic areas, our first decision tree predicted the expected direction of exposure change accurately in 73% of cases. We conclude that this decision tree system offers a valuable tool to advance research in obesity pharmacology and personalize drug development for patients who are obese, ensuring safe and effective medication.

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Drug Disposition in Subjects With Obesity: The Research Work of Darrell R. Abernethy

Cited by 13 publications

References 101 publications

Considerations for Intravenous Anesthesia Dose in Obese Children: Understanding PKPD

Considerations for Intravenous Anesthesia Dose in Obese Children: Understanding PKPD

Perioperative Acetaminophen Dosing in Obese Children

Is There a Need for a Dedicated Pharmacokinetic Trial for a Drug in Obese Populations? A Drug Prioritization Decision Tree Framework

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