Population pharmacokinetic analysis for risperidone using highly sparse sampling measurements from the CATIE study

Feng, Yi; Pollock, Bruce G.; Coley, Kim C.; Marder, Stephen R.; Miller, Del D.; Kirshner, Margaret A.; Aravagiri, Manickam; Schneider, Lon S.; Bies, Robert R.

doi:10.1111/j.1365-2125.2008.03276.x

Cited by 63 publications

(101 citation statements)

References 28 publications

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“…Furthermore, the distribution of the concentration-to-dose ratios showed an interesting pattern in the sense that patients in the amlodipine group were twice as likely to show C/D levels for RIS and the AM above the median as controls. Although pharmacokinetic parameters showed a high inter-individual variability, which has been detected in other studies as well (Balant-Gorgia et al, 1999;Cabaleiro et al, 2015;Feng et al, 2008), it should be noted that we observed no additional distribution differences regarding plasma concentrations and metabolic ratios of RIS as well as the C/Ds of the active metabolite of RIS (9-OH-RIS) between the groups. To our understanding, the findings presented herein imply a potential inhibiting effect of amlodipine most likely on the CYP3A4/5 mediated metabolism of RIS, leading to significantly higher median values of the concentration-to-dose ratios of RIS, 9-OH-RIS and the AM.…”

Section: Discussionmentioning

confidence: 37%

“…regarding the mean age of the different study groups, it appeared plausible that patients under antihypertensive therapy would be older. Consequently, we avoided stratifying for age despite the well-known effect of age on RIS metabolism (Feng et al, 2008). Although the size of the control group is remarkably bigger, we chose not to reduce our control group taking into account the extent of the skewness of the sample distribution.…”

Section: Limitationsmentioning

confidence: 99%

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Pharmacokinetic considerations in the treatment of hypertension in risperidone-medicated patients – thinking of clinically relevant CYP2D6 interactions

et al. 2016

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Background: Treatment of arterial hypertension in patients with severe mental illnesses often results in polypharmacy, potentially leading to drug-drug interactions. The objective of the study was to analyse the in vivo inhibitory potential of two antihypertensive drugs, amlodipine and metoprolol on CYP2D6 catalysed 9-hydroxylation of risperidone (RIS). Methods: A therapeutic drug monitoring database with plasma concentrations of RIS and 9-hydroxyrisperidone (9-OH-RIS) of 1584 patients was analysed. Three groups were considered; a group of patients receiving RIS without a potentially cytochrome influencing co-medication (control group, R 0 , n=852), a group co-medicated with amlodipine (R A , n=27) and a group, co-medicated with metoprolol (R M , n=41). Plasma concentrations, concentration-to-dose ratios (C/Ds) of RIS, 9-OH-RIS and the active moiety (AM), as well as the metabolic ratios were computed and compared using the Kruskal-Wallis test, the Mann-Whitney U test and the Jonckheere-Terpstra test to determine the means and different patterns of distribution of plasma concentrations as well as the concentration-to-dose ratios. Results: The median daily dosage of RIS did not differ between the groups (p=0.708). No differences were found in median plasma concentrations of RIS, 9-OH-RIS and AM. However, concentration-to-dose ratios for RIS, 9-OH-RIS and AM were significantly higher in the amlodipine group (p=0.025, p=0.048 and p=0.005). In the metoprolol group, the concentration-to-dose ratio for RIS was significantly higher than in the control group (p=0.017), while the C/D for 9-OH-RIS and AM was not. Conclusions and limitations:Our data show a potential pharmacokinetic interaction, most likely via CYP3A4 between amlodipine and RIS, reflected in significantly different C/Ds for RIS, 9-OH-RIS and AM. Although the interaction did not result in significantly higher plasma levels, changes in C/Ds and their distribution with regard to the median concentrations were observed.

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Section: Discussionmentioning

confidence: 37%

Section: Limitationsmentioning

confidence: 99%

Pharmacokinetic considerations in the treatment of hypertension in risperidone-medicated patients – thinking of clinically relevant CYP2D6 interactions

et al. 2016

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“…Pharmacokinetic analyses from the Clinical Antipsychotic Trials of Intervention Effectiveness (CATIE) study, by Feng et al [52] found that poor risperidone clearance was clearly associated with the PM status of CYP2D6 [53]. In this study, risperidone and 9-OH risperidone concentration data distinguished CYP2D6 polymorphism-related subpopulations.…”

Section: Studies From Several Research Groups Elucidate the Pharmacogmentioning

confidence: 98%

Pharmacogenetics of antipsychotic treatment response and side effects

Mackenzie

Souza²,

Likhodi³

et al. 2010

Therapy

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Antipsychotic drugs are particularly interesting in pharmacogenetic studies as they are associated with a large interindividual variability in terms of response and side effects and, therefore, frequently need to be discontinued, requiring switches to other antipsychotics. Any information that allows the prediction of outcome to a given antipsychotic in a particular patient will, therefore, be of great help for the clinician to minimize time and find the right drug for the right patient, thus optimizing response and minimizing side effects. This will also have a substantial impact on compliance and doctor-patient relationships. Moreover, antipsychotic drug treatments are often required for life-long treatment and are also frequently prescribed to the more 'vulnerable' populations: children, adolescents and the elderly. This article focuses on some important studies performed with candidate gene variants associated with antipsychotic response. In addition, important findings in pharmacogenetic studies of antipsychotic-induced side effects will be briefly summarized, such as antipsychotic treatment induced tardive dyskinesia and weight gain.

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“…Joint pharmacokinetic (PK) modeling accounts for the uncertainties in the data and allows feedback from the metabolite data to the parent drug data to influence the estimation. Thus, more and more studies now use this approach (2)(3)(4). Also, joint modeling allows to correctly evaluate and predict the impact of drug-drug interactions, and in the case of reversible metabolic systems, it is the only way to properly assess covariate effects.…”

Section: Introductionmentioning

confidence: 99%

“…To solve the issue of structural identifiability, it is important to identify the parameters or "apparent" parameters that can be estimated (3), and for the sake of parameter interpretation or covariate analysis, it might be needed to make some assumptions on the parameters (e.g., fixing one parameter to a given value) (4). Also, instability during the estimation is likely to result in solutions at local minima which may lead to biased parameter estimates and potentially wrong conclusions.…”

Section: Introductionmentioning

confidence: 99%

Development of a Complex Parent-Metabolite Joint Population Pharmacokinetic Model

Bertrand

Laffont

Chenel

et al. 2011

AAPS J

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Abstract. This study aimed to develop a joint population pharmacokinetic model for an antipsychotic agent in development (S33138) and its active metabolite (S35424) produced by reversible metabolism. Because such a model leads to identifiability problems and numerical difficulties, the model building was performed using the FOCE-I and the Stochastic Approximation Expectation Maximization (SAEM) estimation algorithms in NONMEM and MONOLIX, respectively. Four different structural models were compared based on Bayesian information criteria. Models were first written as ordinary differential equations systems and then in closed form (CF) to facilitate further analyses. The impact of polymorphisms on genes coding for the CYP2C19 and CYP2D6 enzymes, respectively involved in the parent drug and the metabolite elimination were investigated using permutation Wald test. The parent drug and metabolite plasma concentrations of 101 patients were analyzed on two occasions after 4 and 8 weeks of treatment at 1, 3, 6, and 24 h following daily oral administration. All configurations led to a two compartment model with back-transformation of the metabolite into the parent drug and a first-pass effect. The elimination clearance of the metabolite through other processes than back-transformation was decreased by 35% [9-53%] in CYP2D6 poor metabolizer. Permutation tests were performed to ensure the robustness of the analysis, using SAEM and CF. In conclusion, we developed a complex joint pharmacokinetic model adequately predicting the impact of CYP2D6 polymorphisms on the parent drug and its metabolite concentrations through the back-transformation mechanism.

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Population pharmacokinetic analysis for risperidone using highly sparse sampling measurements from the CATIE study

Cited by 63 publications

References 28 publications

Pharmacokinetic considerations in the treatment of hypertension in risperidone-medicated patients – thinking of clinically relevant CYP2D6 interactions

Pharmacokinetic considerations in the treatment of hypertension in risperidone-medicated patients – thinking of clinically relevant CYP2D6 interactions

Pharmacogenetics of antipsychotic treatment response and side effects

Development of a Complex Parent-Metabolite Joint Population Pharmacokinetic Model

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