Building population pharmacokineticpharmacodynamic models. I. Models for covariate effects

Mandema, Jaap W.; Verotta, Davide; Sheiner, Lewis B.

doi:10.1007/bf01061469

Cited by 453 publications

(299 citation statements)

References 7 publications

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“…The benefits of this approach lie in the predictive performance of the model for both interpolating PK responses that were not explicitly studied as well as predicting PK responses that arise from situations that exceed the scope of the original study (although care should be taken in this latter scenario). The interested reader is referred to Mandema [45], Wade [46] and Whalby [47,48] for reviews and considerations when building covariate models in population analysis.…”

Section: Methods Used To Assess the Impact Of Obesity On Pk Parametersmentioning

confidence: 99%

“…Nevertheless, this method is widely used and is a valuable tool both in its own right and when used in conjunction with a fully population method (e.g. perhaps within a generalized additive modelling framework or using the Wald's approximation method) [44,45]. However, it is unfortunately common that results of such studies are published without reporting the coefficient estimates of the regression relationship, in these cases typically describing only the degree of association between covariate and parameter values as R 2 .…”

Section: Methods Used To Assess the Impact Of Obesity On Pk Parametersmentioning

confidence: 99%

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What is the best size descriptor to use for pharmacokinetic studies in the obese?

Green

Duffull

2004

Brit J Clinical Pharma

312

244

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The prevalence of obesity in the western world is dramatically rising, with many of these individuals requiring therapeutic intervention for a variety of disease states. Despite the growing prevalence of obesity there is a paucity of information describing how doses should be adjusted, or indeed whether they need to be adjusted, in the clinical setting. This review is aimed at identifying which descriptors of body size provide the most information about the relationship between dose and concentration in the obese. The size descriptors, weight, lean body weight, ideal body weight, body surface area, body mass index, fat-free mass, percent ideal body weight, adjusted body weight and predicted normal body weight were considered as potential size descriptors. We conducted an extensive review of the literature to identify studies that have assessed the quantitative relationship between the parameters clearance (CL) and volume of distribution ( V ) and these descriptors of body size. Surprisingly few studies have addressed the relationship between obesity and CL or V in a quantitative manner. Despite the lack of studies there were consistent findings: (i) most studies found total body weight to be the best descriptor of V . A further analysis of the studies that have addressed V found that total body weight or another descriptor that incorporated fat mass was the preferred descriptor for drugs that have high lipophilicity; (ii) in contrast, CL was best described by lean body mass and no apparent relationship between lipophilicity or clearance mechanism and preference for body size descriptor was found. In conclusion, no single descriptor described the influence of body size on both CL and V equally well. For drugs that are dosed chronically, and therefore CL is of primary concern, dosing for obese patients should not be based on their total weight. If a weight-based dose individualization is required then we would suggest that chronic drug dosing in the obese subject should be based on lean body weight, at least until a more robust size descriptor becomes available.

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Section: Methods Used To Assess the Impact Of Obesity On Pk Parametersmentioning

confidence: 99%

Section: Methods Used To Assess the Impact Of Obesity On Pk Parametersmentioning

confidence: 99%

What is the best size descriptor to use for pharmacokinetic studies in the obese?

Green

Duffull

2004

Brit J Clinical Pharma

312

244

View full text Add to dashboard Cite

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“…Once a model providing an adequate description of the data without the incorporation of covariates was selected, patient characteristics were explored for significance using the generalised additive model (GAM) approach [23] implemented in the software Xpose version 3 [24]. The covariates initially selected during the GAM analysis were further tested for significance in NONMEM using the forward inclusion and backward elimination approach.…”

Section: Covariate Model Selectionmentioning

confidence: 99%

Semi-mechanistic population pharmacokinetic/pharmacodynamic model for neutropenia following therapy with the Plk-1 inhibitor BI 2536 and its application in clinical development

Soto

Staab

Tillmann

et al. 2010

Cancer Chemother Pharmacol

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Purpose (1) To describe the neutropenic response of BI 2536 a polo-like kinase 1 inhibitor in patients with cancer using a semi-mechanistic model. (2) To explore by simulations (a) the neutropenic effects for the maximum tolerated dose (MTD) and the dose at which dose-limiting toxicity occurred, (b) the possibility to reduce the cycle duration without increasing neutropenia substantially, and (c) the impact of the initial absolute neutrophil count (ANC) on the degree of neutropenia for different doses. Experimental design BI 2536 was administered as intravenous infusion over 60 min in the dose range from 25 to 250 mg. Three different administration schedules were explored: (a) day 1, (b) days 1, 2, and 3 or (c) days 1 and 8 within a 3 week treatment cycle. BI 2536 plasma concentrations and ANC obtained during the first treatment cycle from 104 patients were analysed using the population approach with NONMEM VI. Results Neutropenia was described by a semi-mechanistic model resembling proliferation at the stem cell compartment, maturation, degradation, and homeostatic regulation. BI 2536 acts decreasing proliferation rate.Simulations showed that (1) all MTD doses showed an acceptable risk of neutropenia, (2) when BI 2536 is given as 200 mg single administration, cycle duration can be reduced from 3 to 2 weeks, and (3) baseline ANC might be considered to individualise the dose of BI 2536. Conclusions A semi-mechanistic population model was applied to describe the neutropenic effects of BI 2536. The model was used for simulations to support further clinical development.

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“…A stepwise generalized additive model based on the P i estimates from the basic population model as dependent variables was used to select the most important covariates and select the functional relationship between the covariate and the parameter [14]. The covariates assessed were age, weight, sex and baseline IGF-1 concentration.…”

Section: Pharmacodynamic Modelling and Simulationmentioning

confidence: 99%

Population PK and PK/PD modelling of microencapsulated octreotide acetate in healthy subjects

Zhou

Chen

Marino

et al. 2000

Brit J Clinical Pharma

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AimsTo develop a population model that can describe the pharmacokinetic pro®le of microencapsulated octreotide acetate in healthy cholecystectomized subjects. To investigate the correlation between serum IGF-1 and octreotide concentration. Methods A population pharmacokinetic analysis was performed on octreotide data obtained following a single dose of 30 mg microencapsulated octreotide acetate intramuscularly. The relationship between serum IGF-1 concentration and octreotide concentration was effectively described by a population pharmacokinetic/pharmacodynamic model. Results The pharmacokinetic pro®le of octreotide was characterized by an initial peak of octreotide followed by a sustained-release of drug. Plateau concentration were sustained up to day 70, and gradually declined to below the detection limit by day 112. A one-compartment linear model was constructed which consisted of two absorption processes, characterized by K IR and K SR , rate constants for immediate-release and sustained-release, respectively, with ®rst-order elimination (K e ; 1.05 h x1 ). The surface, unencapsulated drug was immediately absorbed into the central compartment with ®rst-order absorption (K IR ; 0.0312 h x1 ), while the microencapsulated drug was ®rst released in a zero-order fashion into a depot before being absorbed into the central compartment with ®rst-order absorption (K SR ; 0.00469 h x1 ) during a period of t (1680 h). Body weight and gender were important covariates for the apparent volume of distribution. The type of formulation was an important covariate for K IR but had no effect on K SR . An inhibitory E max population pharmacokinetic/pharmacodynamic model could adequately describe the relationship between IGF-1 (expressed as percent baseline) and octreotide concentration. Baseline IGF-1 concentration was found to be a signi®cant covariate for the baseline effect (E 0 ). A relationship between GH concentration and octreotide concentration was not established. Conclusions The pharmacokinetic pro®le of microencapsulated octreotide acetate was effectively described by the derived population model. The relationship between IGF-1 and drug concentration could be used to guide optimization of therapeutic octreotide dosage regimens.

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Building population pharmacokineticpharmacodynamic models. I. Models for covariate effects

Cited by 453 publications

References 7 publications

What is the best size descriptor to use for pharmacokinetic studies in the obese?

What is the best size descriptor to use for pharmacokinetic studies in the obese?

Semi-mechanistic population pharmacokinetic/pharmacodynamic model for neutropenia following therapy with the Plk-1 inhibitor BI 2536 and its application in clinical development

Population PK and PK/PD modelling of microencapsulated octreotide acetate in healthy subjects

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