Is Moxifloxacin a Treatment Option for Pancreatic Infections? A Pharmacometric Analysis of Serum and Pancreatic Juice

Wicha, Sebastian G.; Mundkowski, Ralf G.; Klock, Andrea; Hopt, Ulrich T.; Drewelow, Bernd; Kloft, Charlotte; Wellner, Ulrich F.; Keck, Tobias; Wittel, Uwe A.

doi:10.1002/jcph.1445

Cited by 4 publications

(6 citation statements)

References 26 publications

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“…Using a mechanism-based PK modelling approach for microdialysis, it was possible to separate the methodological and clinical variability of MXF PK in the target sites plasma, muscle and skin tissue [11]. Typical MXF PK and variability in plasma identified in the present population of patients with sepsis was similar to those in patients without sepsis [21,22]. Moreover, a minimal PBPK approach [10] was adapted for modelling of microdialysis data and provided additional insight into the distribution pattern of MXF.…”

Section: Discussionmentioning

confidence: 91%

“…The hybrid PBPK approach outlined herein unifies strategies to model the unbound tissue concentrations using microdialysis data. While commonly the target site PK is assigned to scaled central [26], scaled peripheral [22], or separate empirical compartments [27,28], the PBPK approach not only provides mechanistic insight but is also as flexible as empirical approaches due to the estimation of the bloodflow correction factor and the partition coefficient. Nevertheless, application of the hybrid PBPK approach to further microdialysis studies is warranted to systematically elucidate the distribution pattern to target site tissues.…”

Section: Discussionmentioning

confidence: 99%

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A pharmacometric approach to define target site-specific breakpoints for bacterial killing and resistance suppression integrating microdialysis, time–kill curves and heteroresistance data: a case study with moxifloxacin

Iqbal

Broeker

Nowak

et al. 2020

Clinical Microbiology and Infection

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Objectives: Pharmacokineticepharmacodynamic (PK-PD) considerations are at the heart of defining susceptibility breakpoints for antibiotic therapy. However, current approaches follow a fragmented workflow. The aim of this study was to develop an integrative pharmacometric approach to define MICbased breakpoints for killing and suppression of resistance development for plasma and tissue sites, integrating clinical microdialysis data as well as in vitro timeekill curves and heteroresistance information, exemplified by moxifloxacin against Staphylococcus aureus and Escherichia coli. Methods: Plasma and target site samples were collected from ten patients receiving 400 mg moxifloxacin/day. In vitro timeekill studies with three S. aureus and two E. coli strains were performed and resistant subpopulations were quantified. Using these data, a hybrid physiologically based (PB) PK model and a PK-PD model were developed, and utilized to predict site-specific breakpoints. Results: For both bacterial species, the predicted MIC breakpoint for stasis at 400 mg/day was 0.25 mg/L. Less reliable killing was predicted for E. coli in subcutaneous tissues where the breakpoint was 0.125 mg/ L. The breakpoint for resistance suppression was 0.06 mg/L. Notably, amplification of resistant subpopulations was highest at the clinical breakpoint of 0.25 mg/L. High-dose moxifloxacin (800 mg/day) increased all breakpoints by one MIC tier. Conclusions: An efficient pharmacometric approach to define susceptibility breakpoints was developed; this has the potential to streamline the process of breakpoint determination. Thereby, the approach provided additional insight into target site PK-PD and resistance development for moxifloxacin. Application of the approach to further drugs is warranted.

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Section: Discussionmentioning

confidence: 91%

Section: Discussionmentioning

confidence: 99%

A pharmacometric approach to define target site-specific breakpoints for bacterial killing and resistance suppression integrating microdialysis, time–kill curves and heteroresistance data: a case study with moxifloxacin

Iqbal

Broeker

Nowak

et al. 2020

Clinical Microbiology and Infection

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“…Different error models (additive, proportional, or additive‐proportional) were tested to account for residual variability. After identifying a suitable model for plasma BU concentration, saliva measurements were added to the model by testing either a separate saliva compartment or a “scale” parameter assigned to the plasma compartment 27 . Separate error models accounted for residual variability of the BU concentrations in saliva.…”

Section: Methodsmentioning

confidence: 99%

Saliva as a noninvasive sampling matrix for therapeutic drug monitoring of intravenous busulfan in Chinese patients undergoing hematopoietic stem cell transplantation: A prospective population pharmacokinetic and simulation study

Yang

Zhou

et al. 2023

CPT Pharmacom & Syst Pharma

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Therapeutic drug monitoring (TDM) of busulfan (BU) is currently performed by plasma sampling in patients undergoing hematopoietic stem cell transplantation (HSCT). Saliva samples are considered a noninvasive TDM matrix. Currently, no salivary population pharmacokinetics (PopPKs) model for BU available. This study aimed to develop a PopPK model that can describe the relationship between plasma and saliva kinetics in patients receiving intravenous BU. The performance of the model in predicting the area under the concentration‐time curve at steady state (AUCss) based on saliva samples is evaluated. Sixty‐six patients with HSCT were recruited and administered 0.8 mg/kg BU intravenously. A PopPK model for saliva and plasma was developed using the nonlinear mixed effects model. Bayesian maximum a posteriori (MAP) optimization was used to estimate the model's predictive performance. Plasma and saliva PKs were adequately described with a one‐compartment model and a scaled central compartment. Body surface area correlated positively with both clearance and apparent volume of distribution (Vd), whereas alkaline phosphatase correlated negatively with Vd. Simulations demonstrated that the percentage root mean squared prediction error and lower and upper limits of agreements reduced to 10.02% and −16.96% to 22.86% based on five saliva samples. Saliva can be used as an alternative matrix to plasma in TDM of BU. The AUCss can be predicted from saliva concentration by Bayesian MAP optimization, which can be used to design personalized dosing for BU.

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“…Subsequently, saliva drug concentration-time data were added to the stable plasma model, by testing either a separate saliva compartment or a "scale" parameter assigned to the plasma compartment (Wicha et al, 2019). Separate error models were used to account for residual variability of the saliva drug concentrations.…”

Section: Population Pk Analysismentioning

confidence: 99%

Saliva for Precision Dosing of Antifungal Drugs: Saliva Population PK Model for Voriconazole Based on a Systematic Review.

et al. 2020

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Precision dosing for many antifungal drugs is now recommended. Saliva sampling is considered as a non-invasive alternative to plasma sampling for therapeutic drug monitoring (TDM). However, there are currently no clinically validated saliva models available. The aim of this study is firstly, to conduct a systematic review to evaluate the evidence supporting saliva-based TDM for azoles, echinocandins, amphotericin B, and flucytosine. The second aim is to develop a saliva population pharmacokinetic (PK) model for eligible drugs, based on the evidence. Databases were searched up to July 2019 on PubMed ® and Embase ® , and 14 studies were included in the systematic review for fluconazole, voriconazole, itraconazole, and ketoconazole. No studies were identified for isavuconazole, posaconazole, flucytosine, amphotericin B, caspofungin, micafungin, or anidulafungin. Fluconazole and voriconazole demonstrated a good saliva penetration with an average S/P ratio of 1.21 (± 0.31) for fluconazole and 0.56 (± 0.18) for voriconazole, both with strong correlation (r = 0.89-0.98). Based on the evidence for TDM and available data, population PK analysis was performed on voriconazole using Nonlinear Mixed Effects Modeling (NONMEM 7.4). 137 voriconazole plasma and saliva concentrations from 11 patients (10 adults, 1 child) were obtained from the authors of the included study. Voriconazole pharmacokinetics was best described by one-compartment PK model with first-order absorption, parameterized by clearance of 4.56 L/h (36.9% CV), volume of distribution of 60.7 L, absorption rate constant of 0.858 (fixed), and bioavailability of 0.849. Kinetics of the voriconazole distribution from plasma to saliva was identical to the plasma kinetics, but the extent of distribution was lower, modeled by a scale factor of 0.5 (4% CV). A proportional error model best accounted for the residual variability. The visual and simulation-based model diagnostics confirmed a good predictive performance of the

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Is Moxifloxacin a Treatment Option for Pancreatic Infections? A Pharmacometric Analysis of Serum and Pancreatic Juice

Cited by 4 publications

References 26 publications

A pharmacometric approach to define target site-specific breakpoints for bacterial killing and resistance suppression integrating microdialysis, time–kill curves and heteroresistance data: a case study with moxifloxacin

A pharmacometric approach to define target site-specific breakpoints for bacterial killing and resistance suppression integrating microdialysis, time–kill curves and heteroresistance data: a case study with moxifloxacin

Saliva as a noninvasive sampling matrix for therapeutic drug monitoring of intravenous busulfan in Chinese patients undergoing hematopoietic stem cell transplantation: A prospective population pharmacokinetic and simulation study

Saliva for Precision Dosing of Antifungal Drugs: Saliva Population PK Model for Voriconazole Based on a Systematic Review.

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