A meta-analysis of protein binding of flucloxacillin in healthy volunteers and hospitalized patients

E. Wallenburg; R. J. M. Brüggemann; J. A. Roberts; N. G. L. Jager; M. Ulldemolins; S. Wilkes; J. Schouten; P. K. L. Chin; R. ter Heine

doi:10.1016/j.cmi.2021.06.039

A meta-analysis of protein binding of flucloxacillin in healthy volunteers and hospitalized patients

E. Wallenburg^*, R. J. M. Brüggemann, J. A. Roberts, N. G. L. Jager, M. Ulldemolins, S. Wilkes, J. Schouten, P. K. L. Chin, R. ter Heine

^*Corresponding author for this work

Pharmacy

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

Objectives: The aim of this study was to develop a mechanistic protein-binding model to predict the unbound flucloxacillin concentrations in different patient populations. Methods: A mechanistic protein-binding model was fitted to the data using non-linear mixed-effects modelling. Data were obtained from four datasets, containing 710 paired total and unbound flucloxacillin concentrations from healthy volunteers, non-critically ill and critically ill patients. A fifth dataset with data from hospitalized patients was used for evaluation of our model. The predictive performance of the mechanistic model was evaluated and compared with the calculation of the unbound concentration with a fixed unbound fraction of 5%. Finally, we performed a fit-for-use evaluation, verifying whether the model-predicted unbound flucloxacillin concentrations would lead to clinically incorrect dose adjustments. Results: The mechanistic protein-binding model predicted the unbound flucloxacillin concentrations more accurately than assuming an unbound fraction of 5%. The mean prediction error varied between –26.2% to 27.8% for the mechanistic model and between –30.8% to 83% for calculation with a fixed factor of 5%. The normalized root mean squared error varied between 36.8% and 69% respectively between 57.1% and 134%. Predicting the unbound concentration with the use of the mechanistic model resulted in 6.1% incorrect dose adjustments versus 19.4% if calculated with a fixed unbound fraction of 5%. Conclusions: Estimating the unbound concentration with a mechanistic protein-binding model outperforms the calculation with the use of a fixed protein binding factor of 5%, but neither demonstrates acceptable performance. When performing dose individualization of flucloxacillin, this should be done based on measured unbound concentrations rather than on estimated unbound concentrations from the measured total concentrations. In the absence of an assay for unbound concentrations, the mechanistic binding model should be preferred over assuming a fixed unbound fraction of 5%.

Original language	English
Pages (from-to)	446.e1-446.e7
Journal	Clinical Microbiology and Infection
Volume	28
Issue number	3
DOIs	https://doi.org/10.1016/j.cmi.2021.06.039
Publication status	Published - Mar 2022

Bibliographical note

Funding Information:
All authors declared no competing interests for this work. This study was supported by the department of Pharmacy at Radboudumc, Nijmegen . No funding was received for this work.

Publisher Copyright:
© 2021 The Author(s)

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title = "A meta-analysis of protein binding of flucloxacillin in healthy volunteers and hospitalized patients",

abstract = "Objectives: The aim of this study was to develop a mechanistic protein-binding model to predict the unbound flucloxacillin concentrations in different patient populations. Methods: A mechanistic protein-binding model was fitted to the data using non-linear mixed-effects modelling. Data were obtained from four datasets, containing 710 paired total and unbound flucloxacillin concentrations from healthy volunteers, non-critically ill and critically ill patients. A fifth dataset with data from hospitalized patients was used for evaluation of our model. The predictive performance of the mechanistic model was evaluated and compared with the calculation of the unbound concentration with a fixed unbound fraction of 5%. Finally, we performed a fit-for-use evaluation, verifying whether the model-predicted unbound flucloxacillin concentrations would lead to clinically incorrect dose adjustments. Results: The mechanistic protein-binding model predicted the unbound flucloxacillin concentrations more accurately than assuming an unbound fraction of 5%. The mean prediction error varied between –26.2% to 27.8% for the mechanistic model and between –30.8% to 83% for calculation with a fixed factor of 5%. The normalized root mean squared error varied between 36.8% and 69% respectively between 57.1% and 134%. Predicting the unbound concentration with the use of the mechanistic model resulted in 6.1% incorrect dose adjustments versus 19.4% if calculated with a fixed unbound fraction of 5%. Conclusions: Estimating the unbound concentration with a mechanistic protein-binding model outperforms the calculation with the use of a fixed protein binding factor of 5%, but neither demonstrates acceptable performance. When performing dose individualization of flucloxacillin, this should be done based on measured unbound concentrations rather than on estimated unbound concentrations from the measured total concentrations. In the absence of an assay for unbound concentrations, the mechanistic binding model should be preferred over assuming a fixed unbound fraction of 5%.",

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note = "Funding Information: All authors declared no competing interests for this work. This study was supported by the department of Pharmacy at Radboudumc, Nijmegen . No funding was received for this work. Publisher Copyright: {\textcopyright} 2021 The Author(s)",

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AU - Wallenburg, E.

AU - Brüggemann, R. J. M.

AU - Roberts, J. A.

AU - Jager, N. G. L.

AU - Ulldemolins, M.

AU - Wilkes, S.

AU - Schouten, J.

AU - Chin, P. K. L.

AU - ter Heine, R.

N1 - Funding Information: All authors declared no competing interests for this work. This study was supported by the department of Pharmacy at Radboudumc, Nijmegen . No funding was received for this work. Publisher Copyright: © 2021 The Author(s)

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Y1 - 2022/3

N2 - Objectives: The aim of this study was to develop a mechanistic protein-binding model to predict the unbound flucloxacillin concentrations in different patient populations. Methods: A mechanistic protein-binding model was fitted to the data using non-linear mixed-effects modelling. Data were obtained from four datasets, containing 710 paired total and unbound flucloxacillin concentrations from healthy volunteers, non-critically ill and critically ill patients. A fifth dataset with data from hospitalized patients was used for evaluation of our model. The predictive performance of the mechanistic model was evaluated and compared with the calculation of the unbound concentration with a fixed unbound fraction of 5%. Finally, we performed a fit-for-use evaluation, verifying whether the model-predicted unbound flucloxacillin concentrations would lead to clinically incorrect dose adjustments. Results: The mechanistic protein-binding model predicted the unbound flucloxacillin concentrations more accurately than assuming an unbound fraction of 5%. The mean prediction error varied between –26.2% to 27.8% for the mechanistic model and between –30.8% to 83% for calculation with a fixed factor of 5%. The normalized root mean squared error varied between 36.8% and 69% respectively between 57.1% and 134%. Predicting the unbound concentration with the use of the mechanistic model resulted in 6.1% incorrect dose adjustments versus 19.4% if calculated with a fixed unbound fraction of 5%. Conclusions: Estimating the unbound concentration with a mechanistic protein-binding model outperforms the calculation with the use of a fixed protein binding factor of 5%, but neither demonstrates acceptable performance. When performing dose individualization of flucloxacillin, this should be done based on measured unbound concentrations rather than on estimated unbound concentrations from the measured total concentrations. In the absence of an assay for unbound concentrations, the mechanistic binding model should be preferred over assuming a fixed unbound fraction of 5%.

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A meta-analysis of protein binding of flucloxacillin in healthy volunteers and hospitalized patients

Abstract

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