Prospective Trial on the Use of Trough Concentration versus Area under the Curve To Determine Therapeutic Vancomycin Dosing

Neely, Michael; Kato, Lauren; Youn, Gilmer; Kraler, Lironn; Bayard, David S.; Guilder, Michael Van; Schumitzky, Alan; Yamada, Walter M.; Jones, Brenda; Minejima, Emi

doi:10.1128/aac.02042-17

Cited by 292 publications

(340 citation statements)

References 26 publications

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“…In agreement with other data, a large percentage of patients had adequate AUC with troughs lower than 15 mg/L. Another study evaluated BestDose with collection of a single vancomycin level . AUC‐guided dosing resulted in shorter durations of therapy, less nephrotoxicity, and lower troughs while maintaining similar efficacy.…”

Section: Discussionsupporting

confidence: 80%

Review and Validation of Bayesian Dose‐Optimizing Software and Equations for Calculation of the Vancomycin Area Under the Curve in Critically Ill Patients

et al. 2018

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Background Vancomycin area under the concentration‐time curve (AUC) has been linked to efficacy and safety. An accurate method of calculating the AUC is needed. Methods Bayesian dose‐optimizing software programs available for clinician use and first‐order pharmacokinetic equations were evaluated for their ability to estimate vancomycin AUC. A previously published rich pharmacokinetic data set of 19 critically ill patients was used for validation of the AUC estimation. The AUC estimated using subsets of the full data set by Bayesian software and equations was compared with the reference AUC. Accuracy (ratio of estimated AUC to the reference AUC) and bias (percentage difference of estimated AUC to reference AUC) were calculated. Results Five Bayesian dose‐optimizing software programs (Adult and Pediatric Kinetics [APK], BestDose, DoseMe, InsightRx, and Precise PK) and two first‐order pharmacokinetic equations were included. Of the Bayesian programs, InsightRx was the most adaptable, visually appealing, easiest to use, and had the most company support. Utilizing only the trough, accuracy (range 0.79–1.03) and bias (range 5.1–21.2%) of the Bayesian dose‐optimizing software were variable. Precise PK and BestDose had the most accurate estimates with the accuracy values of BestDose exhibiting the most variability of all the programs; however, both programs were more difficult to use. Precise PK was the least biased (median 5.1%). Using a single nontrough value produced similar results to that of the trough for most programs. The addition of a second level to the trough improved the accuracy and bias for DoseMe and InsightRx but not Precise PK and BestDose. APK did not reliably estimate the AUC with input of two levels. Using two levels, the pharmacokinetic equations produced similar or better accuracy and bias as compared with Bayesian software. Conclusion Bayesian dose‐optimizing software using one or more vancomycin levels and pharmacokinetic equations utilizing two vancomycin levels produce similar estimates of the AUC.

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Section: Discussionsupporting

confidence: 80%

Review and Validation of Bayesian Dose‐Optimizing Software and Equations for Calculation of the Vancomycin Area Under the Curve in Critically Ill Patients

et al. 2018

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“…The authors report that 97% (36 of 37 patients) reached therapeutic goals for sirolimus after 2 to 3 months of therapy. They noted several important lessons from such a study design, which we have also noted in our own work . First, scheduled samples (eg, trough concentrations) are often not obtained at the correct time under routine clinical circumstances, which is why traditional TDM that relies on exact timing and comparison to therapeutic ranges is less robust than model‐based TDM that can handle such deviations from planned sample times.…”

Section: Clinical Perspectivementioning

confidence: 90%

“…They noted several important lessons from such a study design, which we have also noted in our own work. 49 First, scheduled samples (eg, trough concentrations) are often not obtained at the correct time under routine clinical circumstances, which is why traditional TDM that relies on exact timing and comparison to therapeutic ranges is less robust than model-based TDM that can handle such deviations from planned sample times. Second, there is usually greater within-individual variability in clinical patient populations than in study populations.…”

Section: Clinical Perspectivementioning

confidence: 99%

Pharmacometric Modeling and Simulation Is Essential to Pediatric Clinical Pharmacology

Neely

Bayard

Desai

et al. 2018

The Journal of Clinical Pharma

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Pediatric clinical pharmacology now encompasses a wide range of activities, including drug pharmacokinetic and pharmacodynamic modeling and simulation, also known as pharmacometrics. Pediatric clinical pharmacologists may be physicians but are more likely to be pharmacists or PhD scientists, and pediatric clinical pharmacology today is largely a research specialty rather than a subspecialty for direct patient care. Pharmacometrics, including “top‐down” population modeling and “bottom‐up” physiologically based pharmacokinetic modeling, has become an indispensable tool for pharmaceutical industry scientists, government regulators, academic researchers, and even a handful of patient‐oriented practitioners. This review summarizes the application of pharmacometrics within each of these domains and predicts future trends of further applications across the spectrum of pediatric clinical pharmacology from drug development to patient care.

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“…Although approximately half of adult patients may need trough concentrations >15 mg/L to ensure efficacy, the other half do not, and maintaining trough concentrations in this range puts these patients at undue risk of nephrotoxicity . This concept serves as the basis of continuous infusion vancomycin, and recent clinical data demonstrate reduced vancomycin‐associated nephrotoxicity in patients monitored by AUC relative to those monitored by trough concentrations of 15‐20 mg/L …”

mentioning

confidence: 99%

“…An alternative approach to the logarithmic trapezoidal rule is the use of Bayesian software programs to estimate vancomycin AUC 24h from a single serum concentration . This approach has been shown to estimate AUC 24h from trough‐only sampling with 97% accuracy and has also been applied clinically, resulting in reduced vancomycin‐associated nephrotoxicity . Although this approach typically requires only a single vancomycin concentration, it should be noted that its accuracy depends on the population pharmacokinetic model used as the Bayesian prior and the patient population to which it is applied .…”

mentioning

confidence: 99%

The Importance of Individualized Vancomycin Dosing to Ensure Optimal Exposure Early in Therapy

Zasowski

Lodise

2018

The Journal of Clinical Pharma

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Prospective Trial on the Use of Trough Concentration versus Area under the Curve To Determine Therapeutic Vancomycin Dosing

Cited by 292 publications

References 26 publications

Review and Validation of Bayesian Dose‐Optimizing Software and Equations for Calculation of the Vancomycin Area Under the Curve in Critically Ill Patients

Review and Validation of Bayesian Dose‐Optimizing Software and Equations for Calculation of the Vancomycin Area Under the Curve in Critically Ill Patients

Pharmacometric Modeling and Simulation Is Essential to Pediatric Clinical Pharmacology

The Importance of Individualized Vancomycin Dosing to Ensure Optimal Exposure Early in Therapy

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