Population Pharmacokinetics and Pharmacodynamics of Chloroquine in a <i>Plasmodium vivax</i> Volunteer Infection Study

Abd-Rahman, Azrin N; Marquart, Louise; Gobeau, Nathalie; Kümmel, Anne; Simpson, Julie A.; Chalon, Stephan; Möhrle, Jörg J.; McCarthy, James S.

doi:10.1002/cpt.1893

Cited by 8 publications

(11 citation statements)

References 43 publications

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“…To more accurately incorporate clinical drug concentrations, we implemented models based on quantitative PK studies on these drugs. 9,10,11,12 Simulations with a model developed for lopinavir + ritonavir therapy, 10 shown in Fig 2A, predict higher lopinavir concentrations with combination therapy (400 mg/100 mg twice daily) than with lopinavir therapy alone (400 mg twice daily). This occurs due to PK interactions whereby ritonavir inhibits lopinavir clearance.…”

Section: Resultsmentioning

confidence: 99%

“…The AZ PK model 11 was a three‐compartment model with first‐order absorption, lag time, and first‐order elimination, and this model calculated free drug concentrations directly. Finally, a PK model for CQ plasma concentrations was recently published using data from 24 healthy subjects 12 . This model consists of two‐compartments, with first‐order absorption and elimination.…”

Section: Methodsmentioning

confidence: 99%

“…The former can be studied with pharmacometrics approaches, whereas the latter can be addressed with quantitative systems pharmacology (QSP) models that explicitly incorporate drug mechanisms of action. Both PK and QSP simulations are likely to become particularly important for proposed COVID-19 treatments because: (1) adverse cardiac events, including QT prolongation, have been associated with several of these drugs, 6,7,8 (2) drug disposition has previously been characterized for most of the drugs being considered for treatment; 9,10,11,12 (3) modeling of pharmacological effects on cardiac electrophysiology, including adverse events, is a mature area of research; 13,14,15 and (4) QSP models can simulate the effects of drugs applied in different context, thereby allowing for the effects of factors such as comorbidities to be considered.…”

Section: Accepted Articlementioning

confidence: 99%

“…To link drug concentrations in the QSP simulations with free plasma drug concentrations that are likely to be observed in patients, we used PK models to simulate drug disposition of either azithromycin, 11 choloroquine 12 or lopinavir + ritonavir. 10 These models, implemented as published, allowed us to simulate temporal changes in either total or free plasma concentrations with different dosing regimens.…”

Section: Modeling Of Pharmacokineticsmentioning

confidence: 99%

“…Finally, a PK model for chloroquine plasma concentrations was recently published using data from 24 healthy subjects. 12 This model consists of twocompartments, with first-order absorption and elimination. Because chloroquine has been shown to accumulate in target tissues, including the heart, we also used results from a physiologically-based PK model 9 developed in Simcyp (Version 18, Certara, UK).…”

Section: Accepted Articlementioning

confidence: 99%

See 4 more Smart Citations

Investigational Treatments for COVID‐19 may Increase Ventricular Arrhythmia Risk Through Drug Interactions

Varshneya

Irurzun-Arana

Campana

et al. 2021

CPT Pharmacom & Syst Pharma

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Many drugs that have been proposed for treatment of COVID‐19 are reported to cause cardiac adverse events, including ventricular arrhythmias. In order to properly weigh risks against potential benefits, particularly when decisions must be made quickly, mathematical modeling of both drug disposition and drug action can be useful for predicting patient response and making informed decisions. Here we explored the potential effects on cardiac electrophysiology of 4 drugs proposed to treat COVID‐19: lopinavir, ritonavir, chloroquine, and azithromycin, as well as combination therapy involving these drugs. Our study combined simulations of pharmacokinetics (PK) with quantitative systems pharmacology (QSP) modeling of ventricular myocytes to predict potential cardiac adverse events caused by these treatments. Simulation results predicted that drug combinations can lead to greater cellular action potential prolongation, analogous to QT prolongation, compared with drugs given in isolation. The combination effect can result from both pharmacokinetic and pharmacodynamic drug interactions. Importantly, simulations of different patient groups predicted that females with pre‐existing heart disease are especially susceptible to drug‐induced arrhythmias, compared with diseased males or healthy individuals of either sex. Statistical analysis of population simulations revealed the molecular factors that certain females with heart failure especially susceptible to arrhythmias. Overall, the results illustrate how PK and QSP modeling may be combined to more precisely predict cardiac risks of COVID‐19 therapies.

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Accepted Articlementioning

confidence: 99%

Section: Modeling Of Pharmacokineticsmentioning

confidence: 99%

Section: Accepted Articlementioning

confidence: 99%

See 3 more Smart Citations

Investigational Treatments for COVID‐19 may Increase Ventricular Arrhythmia Risk Through Drug Interactions

Varshneya

Irurzun-Arana

Campana

et al. 2021

CPT Pharmacom & Syst Pharma

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Pharmacokinetics of chloroquine in patients with malaria by P. vivax from the Western Brazilian Amazon basin

Melo

Costa

Filho

et al. 2022

Biomedicine & Pharmacotherapy

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Characterisation of Plasmodium vivax lactate dehydrogenase dynamics in P. vivax infections

Cao,

Kho,

Grigg

et al. 2024

Commun Biol

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Plasmodium vivax lactate dehydrogenase (PvLDH) is an essential enzyme in the glycolytic pathway of P. vivax. It is widely used as a diagnostic biomarker and a measure of total-body parasite biomass in vivax malaria. However, the dynamics of PvLDH remains poorly understood. Here, we developed mathematical models that capture parasite and matrix PvLDH dynamics in ex vivo culture and the human host. We estimated key biological parameters characterising in vivo PvLDH dynamics based on longitudinal data of parasitemia and PvLDH concentration collected from P. vivax-infected humans, with the estimates informed by the ex vivo data as prior knowledge in a Bayesian hierarchical framework. We found that the in vivo accumulation rate of intraerythrocytic PvLDH peaks at 10–20 h post-invasion (late ring stage) with a median estimate of intraerythrocytic PvLDH mass at the end of the life cycle to be 9.4 × 10−3ng. We also found that the median estimate of in vivo PvLDH half-life was approximately 21.9 h. Our findings provide a foundation with which to advance our quantitative understanding of P. vivax biology and will facilitate the improvement of PvLDH-based diagnostic tools.

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Population Pharmacokinetics and Pharmacodynamics of Chloroquine in a Plasmodium vivax Volunteer Infection Study

Cited by 8 publications

References 43 publications

Investigational Treatments for COVID‐19 may Increase Ventricular Arrhythmia Risk Through Drug Interactions

Investigational Treatments for COVID‐19 may Increase Ventricular Arrhythmia Risk Through Drug Interactions

Pharmacokinetics of chloroquine in patients with malaria by P. vivax from the Western Brazilian Amazon basin

Characterisation of Plasmodium vivax lactate dehydrogenase dynamics in P. vivax infections

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