Abstract
Background and Objective
The latest vancomycin guideline recommends area under the curve (AUC)-targeted dosing and monitoring for efficacy and safety. However, guidelines for AUC-targeted starting dosing in patients with obesity and/or renal insufficiency are currently lacking. This study quantifies the pharmacokinetics (PK) of vancomycin in this population and provides AUC-targeted dosing recommendations.
Methods
Vancomycin concentrations (n = 1188) from therapeutic drug monitoring of 210 overweight and obese patients with varying degrees of renal (dys)function from the ward (74.8%) and intensive care unit (ICU, 25.2%) were pooled with published rich concentration–time data (n = 207) from 20 (morbidly) obese subjects undergoing bariatric surgery. A population model was developed using NONMEM 7.4. Stochastic simulations were performed to design dosing guidelines targeting an AUC24 between 400–600 mg·h/L.
Results
Vancomycin clearance (CL) was found to increase linearly with total bodyweight and with renal function (CKD-EPI) in a power relation. Additionally, CL proved 15.5% lower in ICU patients. Our model shows that, to reach the target AUC between 400 and 600 mg·h/L in the first 48 h, two loading doses are required for both continuous infusion and intermittent dosing regimens. Maintenance doses were found to require adjustment for total bodyweight, renal function, and ICU admission status. With this guideline, the median AUC24 is well within the target from the start of the treatment onwards.
Conclusions
To achieve safe and effective vancomycin exposure for maintenance doses in overweight and obese patients, renal function, total bodyweight, and ICU admission status should be taken into account.
Trial Registration
The AMIGO trial was registered in the Dutch Trial Registry [NTR6058].
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Avoid common mistakes on your manuscript.
Vancomycin clearance in overweight and obese individuals increases with total bodyweight and renal function, and is slightly reduced in ICU patients compared with non-ICU patients. |
On the basis of our model, we propose a model-derived dosing guideline aiming for an AUC24 between 400 and 600 mg·h/L for patients in all categories of obesity and renal dysfunction. |
To achieve the target of AUC24 400–600 mg·h/L, two vancomycin loading doses within the first 48 h are required for both continuous infusion and intermittent dosing regimens. |
1 Introduction
Obesity is a global epidemic, with a prevalence nearly tripling over the last five decades [1]. The World Health Organization (WHO) reported that approximately 39% of the global adult population are overweight [body mass index (BMI) ≥ 25 kg/m2] and about 13% are obese (BMI ≥ 30 kg/m2) [2]. Increasing numbers of patients with obesity with or without renal insufficiency are admitted to the hospital or develop renal insufficiency during hospital stay. These patients run the risk of getting severe bacterial infections for which antibiotic therapy is required.
Vancomycin is frequently used to treat severe infections caused by Gram-positive bacteria [e.g., methicillin-resistant Staphylococcus aureus (MRSA)]. For patients receiving vancomycin therapy, therapeutic drug monitoring (TDM) based on trough concentration was until recently commonly used as a surrogate target for the ratio of area under the curve over 24 h and minimal inhibitory concentration (AUC24/MIC) [3]. However, the latest consensus guideline of vancomycin, published in 2020, recommends using the direct target of AUC24 of 400–600 mg h/L (assuming a MIC of 1 mg/L) to ensure clinical efficacy and minimize toxicity for various infections [4]. This revision is based on the evidence that the trough concentration is insufficient to predict AUC in at least 25% of cases, resulting in an overestimation of the required dose and a corresponding rise in vancomycin exposure for patients [5]. In addition, evidence also reveals that the AUC-targeted monitoring method is associated with significantly less vancomycin-induced acute kidney injury than a trough concentration-based approach. [6]
The new guideline also strongly recommends AUC-targeted dosing and monitoring in patients with obesity, renal insufficiency, or critical illness, since these conditions may significantly alter vancomycin clearance (CL) and increase the risk of nephrotoxicity if the dosage is not modified [4]. A recent prospective study of obese individuals weighing up to 235 kg and without renal insufficiency from our group quantified the increase of vancomycin CL with bodyweight, confirming reports of other studies showing vancomycin clearance increases with bodyweight [7,8,9,10]. However, this study did not consider overweight and obese individuals with renal dysfunction, who may have lower CL than those without renal dysfunction. To propose starting doses leading to target AUC and reduce the need for TDM-based dosage adjustments, quantification of vancomycin pharmacokinetics (PK) in patients who are overweight or obese with varying levels of renal (dys)function is urgently needed.
This study uses population PK modeling to quantify the PK of vancomycin in a representative clinical population of overweight and (morbidly) obese patients with varying degrees of renal (dys)function. Using the developed model, AUC-targeted dosing recommendations are designed to obtain effective and safe vancomycin exposures from treatment initiation onward.
2 Patients and Methods
2.1 Patients and Data
Model building was based on the data from two datasets. The first dataset (patient dataset) contained retrospective PK data and patient characteristics extracted from electronic health records of St. Antonius Hospital in the Netherlands. Patients were included in this analysis when they (1) were overweight or obese (BMI ≥ 25 kg/m2), (2) received vancomycin as a continuous infusion or intermittent dosing and had at least one vancomycin plasma concentration measurement within 168 h after the last dose, and (3) had regular serum creatinine measurements across vancomycin treatment. Patients could be admitted to the ward or ICU and were excluded if they received renal replacement therapy during vancomycin treatment. Vancomycin was administered according to protocols for routine clinical practice, including TDM-based initial dosage and dose adjustments. The second dataset (healthy obese dataset) was obtained from the AMIGO trial, a prospective PK study that has been published previously [7]. Data from 20 (morbidly) obese (BMI ≥ 35 kg/m2) subjects undergoing bariatric surgery were included in the analysis. All individuals had normal renal function defined as an estimated glomerular filtration rate (eGFR) ≥ 60 mL/min/1.73 m2. Subjects from this study were all dosed with 12.5 mg/kg vancomycin (maximum 2500 mg) by single intravenous infusion. Rich sampling was performed, yielding a median number of 11 samples per individual within 24 h after infusion.
In both datasets, vancomycin concentrations were measured with a validated and commercially available immune assay (VANC3) using Cobas platforms (Roche Diagnostics GmbH, Mannheim, Germany). The lower limit of quantification was 4 mg/L and the upper limit of quantification was 80 mg/L. The coefficient of variation was ≤ 4.4.
2.2 Ethics
For the first TDM dataset that was obtained during routine clinical care in the hospital, the Institutional Review Board (IRB) approved the protocol and waived the requirement of informed consent. The second dataset was part of the AMIGO trial, which was approved by the local human research and ethics committee (registered in the Dutch Trial Registry [NTR6058]) and all participants provided informed consent. All studies were conducted in accordance with the Declaration of Helsinki and the International Conference on Harmonization Guidelines in Good Clinical Practice.
2.3 Population Pharmacokinetic Analysis
A population PK analysis was performed using NONMEM 7.4 (ICON Development Solutions, Hanover, MD, USA). Pearl-speaks-NONMEM (PSN) 4.9.0 [11], Pirana 2.9.7 (Certara USA, Inc, Princeton, USA) [12], and R 4.0.3 (Xpose4 package 4.7.1) were used to organize, evaluate, and visualize data. ADVAN11 TRANS4 subroutine with the first-order conditional estimation method with interaction was used.
The structural model was selected from one-, two-, and three-compartment candidate models. Inter-individual variability on the parameters was assumed to follow a log-normal distribution and tested for statistical significance on each parameter. Inter-occasion variability (IOV) was investigated. Additive, proportional, and combined error models were tested to describe residual unexplained variability. For model selection, a drop in objective function value (OFV, − 2 log-likelihood) of more than 3.84 was considered statistically significant (p < 0.05, assuming a χ2 distribution).
Covariates that were considered in the analysis were age, sex, bodyweight-related descriptors [including total bodyweight (TBW), lean bodyweight (LBW), adjusted bodyweight (ABW), ideal bodyweight (IBW), and BMI], and renal function estimates (quantified using Cockcroft-Gault calculated with LBW [CG-LBW] or TBW [CG-TBW], modification of diet in renal disease [MDRD], or chronic kidney disease epidemiology collaboration [CKD‐EPI]). MDRD and CKD‐EPI de-indexed for body surface area (BSA) were also tested. The equations for calculating bodyweight descriptors and renal function can be found in Supplementary Table S1. ICU admission status, indicating whether a patient was admitted to ICU, was also explored as a covariate. Potential covariates were implemented into the model separately using a linear function or a power function with an estimated exponent. A covariate relationship was considered statistically significant when OFV dropped more than 10.83 (p < 0.001). The model fits were assessed using goodness-of-fit (GOF) plots stratified for the BMI group [overweight (BMI 25–30 kg/m2) and obese (BMI > 30 kg/m2)], stratified for the estimated renal function group (CKD-EPI < 30, 30–50, 50–90, > 90 mL/min/1.73 m2) and ICU admission status. Plots of individual influence on change in OFV (also known as shark plots) in Xpose 4 were used to ascertain that statistical significance was driven by a sufficient number of individuals and it was checked that the inclusion of a covariate reduced the random inter-individual variability on a parameter [13]. In addition, covariate relationships were visually inspected in plots of eta value versus individual covariate value for time-independent covariates, conditional weighted residuals (CWRES) versus individual covariate value for time-dependent covariates, and individual post hoc parameter estimates versus covariate value overlain with lines representing the obtained covariate relationships, with the stratifications previously mentioned. Finally, relative standard errors of estimates (RSE) were considered to indicate adequate precision if they were below 50%.
2.4 Model Evaluation
In addition to the diagnostic plots used during model development, the robustness of the parameter estimates of the final model was validated by a bootstrap resampling analysis using PsN [12], with 1000 replicates stratified on the two datasets.
The predictive performance of the final model was assessed and visualized by a normalized prediction distribution error (NPDE) analysis using the NPDE package in R [14]. The analysis was based on 1000 simulations of the dataset.
2.5 Model-Based Dose Optimization
On the basis of the obtained covariate relationships in the final model and clinical feasibility, AUC-targeted dosing recommendations for continuous infusion and intermittent dosing regimen were developed, which were assessed in stochastic simulations using the final vancomycin PK model. For representative virtual individuals with assigned values of indexed CKD-EPI (20, 40, 60, 80, and 100 mL/min/1.73 m2), bodyweight (80, 120, 160, and 200 kg), and ICU admission status (non-ICU versus ICU), 1000 simulations with inter-individual variability were performed. The target exposure for efficacy was defined as AUC24/MIC ≥ 400 mg·h/L. An AUC24/MIC threshold of 600 mg·h/L was selected as the safety limit to minimize the probability of nephrotoxicity according to the literature [15,16,17]. Since the MIC was assumed to be 1 mg/L in this study, AUC24/MIC is abbreviated as AUC24 for simplicity. Therefore, optimal dose regimens should achieve the target AUC24 from the first day of dosing onward. To explore the concentrations that are obtained upon these AUC24 400–600 mg·h/L targeted dosing recommendations, concentration–time profiles for the different bodyweight and renal function groups were also explored.
3 Results
3.1 Data
A total of 1188 concentrations were available from 210 overweight and obese hospitalized patients, which were analyzed in conjunction with 207 concentrations from 20 morbidly obese healthy subjects. Of the 1188 concentrations, 11 were peak and 416 were trough concentrations taken upon intermittent infusion, while 761 were random samples taken upon the continuous infusion. A summary of baseline demographics, clinical characteristics, and dosing information from the study groups is presented in Table 1.
3.2 Population Pharmacokinetic Analysis
A three-compartment model outperformed both one- and two-compartment models, exhibiting the best GOF plots. This model, which incorporated inter-individual variability on CL and central volume of distribution (V1), best described the data.
In the covariate analysis, indexed CKD-EPI gave the largest reduction in OFV and was identified as the most predictive covariate on CL, with an estimated exponent in a power relationship of 0.658 (p < 0.001). TBW was identified as the second covariate on CL, as it was significantly correlated with vancomycin CL in a linear function (p < 0.001) and found to be superior to the other tested size descriptors. Furthermore, ICU admission status was also significantly correlated with vancomycin CL (p < 0.001), with CL in ICU patients being 15.5% lower than in non-ICU patients. For the volume of distribution of the peripheral compartments and the inter-compartmental clearances, a statistically significant correlation with TBW was found (p < 0.001). However, since for each parameter only three individuals (1.30%) were found to contribute to yielding statistical significance, we decided not to include TBW as a covariate on the peripheral compartments and inter-compartmental clearances. No other covariates were found to have a statistically significant impact on vancomycin PK in our population. The PK parameters of vancomycin for the final model are presented in Table 2.
In the final model, CL was 3.36 L/h in a typical patient with a TBW of 100 kg and indexed CKD-EPI of 75 mL/min/1.73 m2. For a patient admitted to the ICU, this value was 2.84 L/h. The influences of renal function (CKD-EPI), bodyweight (TBW), and ICU admission status on CL are illustrated in Fig. 1.
3.3 Model Evaluation
The GOF plots of the final model, stratified on renal function (CKD-EPI), bodyweight (TBW), and ICU admission status, are shown in Supplementary Fig. S1. The figure shows that observed vancomycin concentrations are described without bias in all subpopulations, with the exception of the group with the worst kidney function (CKD-EPI < 30 mL/min/1.73 m2) in which a small trend towards under-prediction can be seen.
The bootstrap analysis (presented in Table 2) confirmed the robustness of the parameter estimates in the final model. Bootstrapped median values generally deviated less than 10% from the original estimate and all originally estimated values were within the 95% confidence interval (CI) of the bootstrapped values.
Visual inspection and statistical tests of the NPDE results based on 1000 simulation shows the final model have had a good predictive performance for subpopulations with different renal function, bodyweights, and ICU admission status (Supplementary Fig. S2). The model is shown to accurately describe typical trends as well as the variability in the populations.
3.4 Model-Based Dose Optimization
To achieve AUC24 exposure of 400–600 mg·h/L in overweight and obese patients with varying degrees of renal function, dosing guidelines for continuous infusion and intermittent dosing regimens were developed. The regimens for the ward patients are shown in Figs. 2 and 3, while those for the ICU patients are shown in Figs. 4 and 5. These tables present that for both schemes, higher doses are needed with increasing bodyweight and renal function, and in non-ICU patients compared with ICU patients.
To obtain the vancomycin therapeutic exposure immediately at the start of the treatment, two loading dose administrations for both continuous infusion and intermittent dosing regimens were required. For continuous infusion, a loading dose of 1500 mg is given as a 2-h infusion before starting the maintenance infusion on day 1, and another loading dose of 750 mg is given over 2 h on day 2, after which the maintenance infusion is continued. In patients on an intermittent dosing, two loading doses given as a 2-h infusion at 12-h intervals are proposed on the first day of treatment. From the second day onwards, maintenance doses can be given one or two times per day depending on the patient renal function, bodyweight, and ICU admission status. More details of these dosing regimens can be found in Figs. 2, 3, 4 and 5.
The obtained daily AUC24 and concentration profiles in the first week of treatment for the defined representative virtual individuals with various combinations of the bodyweight and renal function are illustrated in Figs. 6 and 7, for the ward patients and ICU patients, respectively. These figures indicate that when our proposed guidelines for either continuous infusion or intermittent dosing are applied, the median AUC24 is within the target of 400–600 mg·h/L, regardless of renal function, bodyweight, and ICU admission status, even though for some ICU subgroups AUC may be slightly above 600 mg·h/L (Fig. 7). However, even though the AUC24 generally reaches the target, the concentrations that are obtained across the entire patient population are highly variable and often lower than previously used target concentrations. More specifically, median (interquartile range) values of (trough) concentration for continuous infusion and intermittent dosing are 23.08 (19.54–27.29) mg/L and 16.89 (12.65–20.50) mg/L, respectively. These figures also show that time to steady-state concentrations in obese patients, particularly in those with renal dysfunction admitted to the ICU, exceeds 5 days.
4 Discussion
In this study, we quantified vancomycin PK in a large and representative clinical population, covering patients with varying degrees of overweight or obesity and renal function who were admitted to the hospital ward or ICU. Using the obtained insights, we proposed dosing guidelines for both continuous infusion and intermittent dosing regimens taking renal function, bodyweight, and ICU admission status into account. The proposed model-derived regimen is expected to yield better initial dosing and may reduce requirements for dose adjustment.
Following our developed dosing guideline, daily AUC24/MIC exposure is maintained between 400 and 600 mg h/L in patients with varying degrees of obesity and renal function who are admitted to the hospital ward or ICU. The AUC24/MIC target of 400–600 mg h/L was chosen to ensure clinical efficacy while enhancing patient safety, which is in line with the advice given by the recently released vancomycin consensus guideline [4, 18]. The vancomycin MIC is assumed to be 1 mg/L because the vancomycin MIC for serious infections (e.g., MRSA) is 1 mg/L at most institutions [19]. In cases of increased MIC values, the proposed doses should be increased proportionally, even though, in case the MIC is above 2 mg/L, an alternative agent would probably be preferable.
Achieving targeted AUC24 exposures within the initial 24–48 h of the vancomycin treatment course is recommended for early and appropriate therapy [19]. To achieve this, loading doses are necessary. Traditional vancomycin loading doses are administered in mg per kg as a 2-h infusion before the maintenance dose begins. However, on the basis of our model, we developed a dosing guideline for overweight and obese individuals with varying renal functions that involve two loading doses. For continuous infusion, a loading dose of 1500 mg is given as a 2-h infusion before starting the maintenance infusion on day 1, and another loading dose of 750 mg is given as a 2-h infusion on day 2, after which the maintenance infusion is continued. For intermittent dosing regimen, two loading doses are administered every 12 h on the first day to quickly achieve an effective and safe exposure. Even though this is a deviation from current clinical practice, these loading doses are necessary to achieve effective exposure early in the treatment.
Even though the AUC24 reaches the target range for most individuals with the proposed regimen, concentrations tend to fall below the commonly expected target ranges with continuous infusion and intermittent dosing. This suggests that dose adjustment based on concentration at the early stages of treatment may result in concentration and AUC24 values outside the target window at later time points. Therefore, we recommended using AUC24 values, rather than solely relying on trough concentration values, to interpret TDM samples to guide dosing adjustments. AUC24 values can be accurately and reliably obtained by a Bayesian dose-optimization software program that embeds an appropriate reference population PK model. For overweight and obese patients, especially those with renal dysfunction admitted to ICU, particular attention should be paid as the time to steady-state might be prolonged to over a week, but with the appropriate software and models this will be taken into account properly [20].
Readily available and convenient biomarkers for renal function remain limited in overweight and obese patients, as most of the equations calculating renal function estimates are not confirmed in this population [21]. In fact, the equation of CG, which is commonly used, has been reported to have a low accuracy and high bias in estimating glomerular filtration rate in patients with obesity and should therefore be avoided [22, 23]. In our study, among the renal function estimates available in clinical practice, we found indexed CKD-EPI to be superior to CG and other renal function estimates, in correlation with vancomycin CL, which is in line with the vancomycin PK study of Kim et al. [24]. Moreover, our study confirmed that in overweight and obese populations, TBW is better correlated with CL than other bodyweight descriptors [8]. However, this is not always the case, as for cefazolin and ciprofloxacin, CL remains unchanged with different degrees of obesity [25, 26].
In addition to renal function and bodyweight, ICU admission status was identified as a significant independent covariate on CL, indicating differences between subjects from ICU and non-ICU. The age of ICU and non-ICU patients is comparable (median [range] values for ICU versus non-ICU: 70 [33–88] versus 71 [35–92] years). In addition, the eGFR range is similar between patients in the two settings (ICU 75 [20–155] versus non-ICU 74 [6–137] mL/min/1.73 m2). The potential reason for different CL in these two settings could be that rapidly varying disease states of ICU patients can lead to reduced kidney function and limited drug elimination [27], with serum creatinine being an inappropriate and/or late marker to indicate this [28]. Interestingly, Smit et al. also identified ICU status as an independent predictor for CL in a comparable gentamicin PK study, reporting a 24.9% reduced CL in ICU patients [29]. These results contradict a seeming consensus from several studies indicating an augmented renal clearance (eGFR > 130 mL/min/1.73 m2) in critically ill patients [30,31,32]. This difference could be because compared with the other studies, our study included patients with more severe concomitant disease, but without trauma or burns. Future research investigating the underlying cause of the decreased CL in obese individuals with critical illnesses should be considered.
In this study, we included patients undergoing bariatric surgery receiving a single dose of vancomycin and patients treated with vancomycin for infections, resulting in a group covering a broad spectrum of bodyweight. However, patients with a bodyweight higher than 143 kg all had a good renal function. As a result, our dosing guidelines in this group are based on less evidence compared with the group below 143 kg. Moreover, as our dataset included only 15 patients (6.52%) with extremely poor renal function (CKD-EPI < 30 mL/min/1.73 m2), caution is warranted when employing the proposed dosing recommendation for this subgroup. In addition, the lack of covariates and the large inter-individual variability in volume may be due to the fact that we did not have enough peak samples to fully characterize volume and its covariates. However, for the AUC-targeted dose, CL is the primary parameter of interest, whereas volume is mainly related to the time to reach steady state. Because we had many (trough) samples both early after initiation of treatment and after several weeks of treatment, we are convinced that our model can be used for AUC-targeted dosing, which was the overall goal of our study, even though it may not accurately predict the peak concentration reached immediately after a 2-h infusion dose.
5 Conclusion
When dosing vancomycin in overweight and obese patients, renal function, bodyweight, and ICU admission status should be taken into account to get safe and effective vancomycin exposure. We propose a practical vancomycin dosing guideline for both continuous infusion and intermittent dosing regimens that can be used for this purpose.
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Acknowledgements
The authors would like to thank Alex Kollaart for the code review.
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Funding
The work of Tan Zhang was supported by the China Scholarship Council (201906010328). The AMIGO trial was funded by institutional research from The Netherlands Organization for Health Research and Development (ZonMW, 836041004).
Conflict of interest
No disclosures are applicable for this work. Disclosures outside of this work: RJMB has served as consultants to Astellas Pharma, Inc., F2G, Amplyx, Gilead Sciences, Merck Sharp & Dohme Corp., and Pfizer, Inc., and has received unrestricted and research grants from Astellas Pharma, Inc., Gilead Sciences, Merck Sharp & Dohme Corp., and Pfizer, Inc. All contracts were through Radboudumc, and all payments were invoiced by Radboudumc. None of the other authors have any conflicts to declare.
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Data are available from the corresponding author upon request.
Ethics approval
For the study that was conducted during routine clinical care in the hospital, the Institutional Review Board (IRB) approved the protocol and waived the requirement of informed consent. The AMIGO trial was approved by the local human research and ethics committee (registered in the Dutch Trial Registry, NTR6058). All studies were conducted in accordance with the Declaration of Helsinki and the International Conference on Harmonization Guidelines in Good Clinical Practice.
Consent to participate
Written, informed consent was obtained from all participants in the AMIGO trial.
Consent for publication
Not applicable.
Code availability
The final model code will be made available in the DDMoRe model repository (http://repository.ddmore.eu/).
Author contributions
Conception and design of the research: TZ, EHJK, CS, and CAJK; data collection: CS and EPAD; data analysis: TZ; interpretation of findings: TZ, EHJK, CS, EPAD, RJMB, and CAJK; drafting the manuscript: TZ; critical revision of manuscript: EHJK, CS, EPAD, RJMB, and CAJK. All authors provided final manuscript approval.
Supplementary Information
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Zhang, T., Krekels, E.H.J., Smit, C. et al. How to Dose Vancomycin in Overweight and Obese Patients with Varying Renal (Dys)function in the Novel Era of AUC 400–600 mg·h/L-Targeted Dosing. Clin Pharmacokinet 63, 79–91 (2024). https://doi.org/10.1007/s40262-023-01324-5
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DOI: https://doi.org/10.1007/s40262-023-01324-5