Quinidine single dose pharmacokinetics and pharmacodynamics are unaltered by omeprazole

Ching, Michael S.; Elliott, Susan L.; Stead, Cheryl K.; Murdoch, Ross; Devenish-Meares, S; Morgan, Denis J.; Smallwood, Richard A.

doi:10.1111/j.1365-2036.1991.tb00521.x

Cited by 14 publications

(13 citation statements)

References 22 publications

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“…The weak response in CYP3A4 mRNA by phenytoin in spite of known induction properties in vivo may be explained by the concentration used in vitro (10 mM), which is below the concentration (40Y80 mM) reported to cause induction in vivo (31). Omeprazole significantly induced CYP3A4 mRNA in the liver slices but is not reported to be an in vivo inducer (32). However, as for CYP1A induction, this can be explained by the supratherapeutic concentrations used in the study.…”

Section: Discussionmentioning

confidence: 67%

Evaluation of Human Liver Slices and Reporter Gene Assays as Systems for Predicting the Cytochrome P450 Induction Potential of Drugs in Vivo in Humans

et al. 2006

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Section: Discussionmentioning

confidence: 67%

Evaluation of Human Liver Slices and Reporter Gene Assays as Systems for Predicting the Cytochrome P450 Induction Potential of Drugs in Vivo in Humans

et al. 2006

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“…(a–f) Predicted compared to observed plasma concentration‐time profiles of quinidine and 3‐hydroxyquinidine alone and after pretreatment with and/or concomitant administration of (a) carbamazepine, (b) fluvoxamine, (c) itraconazole, (d) R‐/S‐omeprazole, (e) rifampicin, and (f) R‐/S‐verapamil (low verapamil dose regimen). Population geometric means are shown as lines (solid: quinidine and 3‐hydroxyquinidinde alone, dashed: quinidine and 3‐hydroxyquinidinde during DDI), geometric standard deviations are shown as shaded areas and observed data are shown as dots (control) and squares (DDI) (±standard deviation, if reported) 26,32–36 . Quinidine doses indicate quinidine sulfate administration.…”

Section: Resultsmentioning

confidence: 99%

“…(a, b) For quinidine acting as a cytochrome P450 (CYP) 3A4 and P-glycoprotein (P-gp) victim, predicted drug−drug interaction (DDI) (a) area under the plasma concentration-time curve calculated between the first and last concentration measurement (AUC last ) and (b) maximum plasma concentration (C max ) ratios of quinidine and 3-hydroxyquinidine are plotted against their respective observed values after pretreatment with and/or concomitant administration of carbamazepine, cimetidine, fluvoxamine, itraconazole, R-/S-omeprazole, rifampicin, and R-/S-verapamil. 26,[32][33][34][35][36]43,44 (c, d) For quinidine acting as a CYP2D6 and P-gp perpetrator, predicted DD(G)I (c) AUC last and (d) C max ratios of dextromethorphan (DEX), dextrorphan-O-glucuronide (DXG), total dextrorphan (DTT), digoxin (DIG), metoprolol (MET), S-metoprolol (SME), and R-metoprolol (RME), mexiletine (MEX) and paroxetine (PAR) are plotted against their respective observed values after pretreatment with and/or concomitant administration of quinidine. 11,[37][38][39][40][41][42]45 The solid line represents the line of identity, whereas 1.25-fold and two-fold prediction limits are shown as dotted and dashed lines, respectively.…”

Section: Quinidinementioning

confidence: 99%

“…(a-f) Predicted compared to observed plasma concentration-time profiles of quinidine and 3-hydroxyquinidine after (a) intravenous and (b-f) oral administration. Population geometric means are shown as lines, geometric standard deviations are shown as shaded areas, and observed data are shown as dots (training dataset) and triangles (test dataset) (±standard deviation, if reported) 8,[25][26][27][28][29]. (g-i) Goodness-of-fit plots comparing predicted and observed (g) plasma concentrations, (h) area under the plasma concentration-time curve calculated between first and last concentration measurement (AUC last ) and (i) maximum plasma concentration (C max ) values.…”

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confidence: 99%

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Physiologically‐based pharmacokinetic modeling of quinidine to establish a CYP3A4, P‐gp, and CYP2D6 drug–drug–gene interaction network

Feick

Rüdesheim

Marok

et al. 2023

CPT Pharmacom & Syst Pharma

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The antiarrhythmic agent quinidine is a potent inhibitor of cytochrome P450 (CYP) 2D6 and P‐glycoprotein (P‐gp) and is therefore recommended for use in clinical drug–drug interaction (DDI) studies. However, as quinidine is also a substrate of CYP3A4 and P‐gp, it is susceptible to DDIs involving these proteins. Physiologically‐based pharmacokinetic (PBPK) modeling can help to mechanistically assess the absorption, distribution, metabolism, and excretion processes of a drug and has proven its usefulness in predicting even complex interaction scenarios. The objectives of the presented work were to develop a PBPK model of quinidine and to integrate the model into a comprehensive drug–drug(–gene) interaction (DD(G)I) network with a diverse set of CYP3A4 and P‐gp perpetrators as well as CYP2D6 and P‐gp victims. The quinidine parent‐metabolite model including 3‐hydroxyquinidine was developed using pharmacokinetic profiles from clinical studies after intravenous and oral administration covering a broad dosing range (0.1–600 mg). The model covers efflux transport via P‐gp and metabolic transformation to either 3‐hydroxyquinidine or unspecified metabolites via CYP3A4. The 3‐hydroxyquinidine model includes further metabolism by CYP3A4 as well as an unspecific hepatic clearance. Model performance was assessed graphically and quantitatively with greater than 90% of predicted pharmacokinetic parameters within two‐fold of corresponding observed values. The model was successfully used to simulate various DD(G)I scenarios with greater than 90% of predicted DD(G)I pharmacokinetic parameter ratios within two‐fold prediction success limits. The presented network will be provided to the research community and can be extended to include further perpetrators, victims, and targets, to support investigations of DD(G)Is.

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“…the study inclusion criteria were: a) healthy Caucasian volunteers, b) availability of information about the quinidine pharmacokinetics, ideally presented as a drug plasma concentration change in time, c) PD results presented as Qt/ QTc or ΔQT/ΔQTc (regardless of the correction type), thus comparable with the simulation outputs. Nine papers fulfilling such conditions were identified and used for the study (Belz et al, 1982;Ching et al, 1991;El-Eraky and Thomas, 2003;Fieldman et al, 1977;Kaukonen et al, 1997;laganiere et al, 1996;Min et al, 1996;Olatunde and Price Evans, 1982;Shin et al, 2007). Characteristics of the clinical studies derived from the identified papers are presented in Table 1.…”

Section: Datamentioning

confidence: 99%

In vitro to human in vivo translation – pharmacokinetics and pharmacodynamics of quinidine

Polak

2013

ALTEX

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SummaryThe translational sciences aim to transfer results from basic research to the treatment of animals or patients. One of the approaches that could be utilized to achieve this goal is the in vitro-in vivo extrapolation (IVIVE) concepts of PK and PD mechanistic modeling and simulation to highlight the importance of assessing drug effect and safety in the preliminary phases of the drug development process. the IVIVe application approach necessitates the provision of three data sets: 1) drug related (ADMe processes and activity), 2) system data (describing population and variability of the chosen parameters), and 3) simulated trial design (Rostami-Hodjegan and tucker, 2007). the IVIVe methodology is a robust evaluation tool that assesses inter-individual variability based on the virtual population characteristics in the population study group.to assess the application value of the described approach, quinidine was selected as the model drug in the virtual study described here. the study endpoints covered plasma concentration of the parent compound and its main metabolite, 3-OH quinidine, from the pharmacokinetic side. either Qtc interval or the drug triggered change as compared to the baseline (ΔQT/ ΔQTc) were used as the pharmacodynamic effect descriptors. this pharmacodynamic effect dictates that drug cardiac safety should be regarded as a pivotal focal point of this study. Preclinical studies routinely use in vitro approaches to assess cardiac safety; however, non-rodent species (e.g., dogs, monkeys) are commonly used in the assessment procedure. this study proposes a novel concept based on a combination of mechanistic PBPK/PD modeling and simulation to predict the cardiac effects of drugs and thus help to incorporate the 3Rs concept

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Quinidine single dose pharmacokinetics and pharmacodynamics are unaltered by omeprazole

Cited by 14 publications

References 22 publications

Evaluation of Human Liver Slices and Reporter Gene Assays as Systems for Predicting the Cytochrome P450 Induction Potential of Drugs in Vivo in Humans

Evaluation of Human Liver Slices and Reporter Gene Assays as Systems for Predicting the Cytochrome P450 Induction Potential of Drugs in Vivo in Humans

Physiologically‐based pharmacokinetic modeling of quinidine to establish a CYP3A4, P‐gp, and CYP2D6 drug–drug–gene interaction network

In vitro to human in vivo translation – pharmacokinetics and pharmacodynamics of quinidine

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