Erdafitinib’s effect on serum phosphate justifies its pharmacodynamically guided dosing in patients with cancer

A population pharmacokinetic (PK)–pharmacodynamic (PD) model was developed using data from 345 patients with cancer. The population PK‐PD model evaluated the effect of erdafitinib total and free plasma concentrations on serum phosphate concentrations after once‐daily oral continuous (0.5–12 mg) and...

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Autores principales: Dosne, Anne‐Gaëlle, Valade, Elodie, Stuyckens, Kim, De Porre, Peter, Avadhani, Anjali, O’Hagan, Anne, Li, Lilian Y., Ouellet, Daniele, Faelens, Ruben, Leirens, Quentin, Poggesi, Italo, Perez Ruixo, Juan Jose
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2021
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9124353/
https://www.ncbi.nlm.nih.gov/pubmed/34755484
http://dx.doi.org/10.1002/psp4.12727
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author Dosne, Anne‐Gaëlle
Valade, Elodie
Stuyckens, Kim
De Porre, Peter
Avadhani, Anjali
O’Hagan, Anne
Li, Lilian Y.
Ouellet, Daniele
Faelens, Ruben
Leirens, Quentin
Poggesi, Italo
Perez Ruixo, Juan Jose
author_facet Dosne, Anne‐Gaëlle
Valade, Elodie
Stuyckens, Kim
De Porre, Peter
Avadhani, Anjali
O’Hagan, Anne
Li, Lilian Y.
Ouellet, Daniele
Faelens, Ruben
Leirens, Quentin
Poggesi, Italo
Perez Ruixo, Juan Jose
author_sort Dosne, Anne‐Gaëlle
collection PubMed
description A population pharmacokinetic (PK)–pharmacodynamic (PD) model was developed using data from 345 patients with cancer. The population PK‐PD model evaluated the effect of erdafitinib total and free plasma concentrations on serum phosphate concentrations after once‐daily oral continuous (0.5–12 mg) and intermittent (10–12 mg for 7 days on/7 days off) dosing, and investigated the potential covariates affecting erdafitinib‐related changes in serum phosphate levels. Phosphate is used as a biomarker for erdafitinib's efficacy and safety: increases in serum phosphate were observed after dosing with erdafitinib, which were associated with fibroblast growth factor receptor target engagement via inhibition of renal fibroblast growth factor 23–mediated signaling. PK‐PD model‐based simulations were performed to assess the approved PD‐guided dosing algorithm of erdafitinib (8 mg once‐daily continuous dosing, with up‐titration to 9 mg based on phosphate levels [<5.5 mg/dl] and tolerability at 14–21 days of treatment). The serum phosphate concentrations increased after the first dose and reached near maximal level after 14 days of continuous treatment. Serum phosphate increased with erdafitinib free drug concentrations: doubling the free concentration resulted in a 1.8‐fold increase in drug‐related phosphate changes. Dose adjustment after at least 14 days of dosing was supported by achievement of >95% maximal serum phosphate concentration. The peak‐to‐trough fluctuation within a dosing interval was limited for serum phosphate concentrations (5.68–5.65 mg/dl on Day 14), supporting phosphate monitoring at any time relative to dosing. Baseline phosphate was higher in women, otherwise, none of the investigated covariate–parameter relationships were considered clinically relevant. Simulations suggest that the starting dose of 8‐mg with up‐titration to 9‐mg on Days 14–21 maximized the number of patients within the target serum phosphate concentrations (5.5–7 mg/dl) while limiting the number of treatment interruptions. The findings from the PK‐PD model provided a detailed understanding of the erdafitinib concentration‐related phosphate changes over time, which supports erdafitinib's dosing algorithm.
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spelling pubmed-91243532022-05-24 Erdafitinib’s effect on serum phosphate justifies its pharmacodynamically guided dosing in patients with cancer Dosne, Anne‐Gaëlle Valade, Elodie Stuyckens, Kim De Porre, Peter Avadhani, Anjali O’Hagan, Anne Li, Lilian Y. Ouellet, Daniele Faelens, Ruben Leirens, Quentin Poggesi, Italo Perez Ruixo, Juan Jose CPT Pharmacometrics Syst Pharmacol Research A population pharmacokinetic (PK)–pharmacodynamic (PD) model was developed using data from 345 patients with cancer. The population PK‐PD model evaluated the effect of erdafitinib total and free plasma concentrations on serum phosphate concentrations after once‐daily oral continuous (0.5–12 mg) and intermittent (10–12 mg for 7 days on/7 days off) dosing, and investigated the potential covariates affecting erdafitinib‐related changes in serum phosphate levels. Phosphate is used as a biomarker for erdafitinib's efficacy and safety: increases in serum phosphate were observed after dosing with erdafitinib, which were associated with fibroblast growth factor receptor target engagement via inhibition of renal fibroblast growth factor 23–mediated signaling. PK‐PD model‐based simulations were performed to assess the approved PD‐guided dosing algorithm of erdafitinib (8 mg once‐daily continuous dosing, with up‐titration to 9 mg based on phosphate levels [<5.5 mg/dl] and tolerability at 14–21 days of treatment). The serum phosphate concentrations increased after the first dose and reached near maximal level after 14 days of continuous treatment. Serum phosphate increased with erdafitinib free drug concentrations: doubling the free concentration resulted in a 1.8‐fold increase in drug‐related phosphate changes. Dose adjustment after at least 14 days of dosing was supported by achievement of >95% maximal serum phosphate concentration. The peak‐to‐trough fluctuation within a dosing interval was limited for serum phosphate concentrations (5.68–5.65 mg/dl on Day 14), supporting phosphate monitoring at any time relative to dosing. Baseline phosphate was higher in women, otherwise, none of the investigated covariate–parameter relationships were considered clinically relevant. Simulations suggest that the starting dose of 8‐mg with up‐titration to 9‐mg on Days 14–21 maximized the number of patients within the target serum phosphate concentrations (5.5–7 mg/dl) while limiting the number of treatment interruptions. The findings from the PK‐PD model provided a detailed understanding of the erdafitinib concentration‐related phosphate changes over time, which supports erdafitinib's dosing algorithm. John Wiley and Sons Inc. 2021-11-22 2022-05 /pmc/articles/PMC9124353/ /pubmed/34755484 http://dx.doi.org/10.1002/psp4.12727 Text en © 2021 Janssen Research and Development. CPT: Pharmacometrics & Systems Pharmacology published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics. https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc-nd/4.0/ (https://creativecommons.org/licenses/by-nc-nd/4.0/) License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Research
Dosne, Anne‐Gaëlle
Valade, Elodie
Stuyckens, Kim
De Porre, Peter
Avadhani, Anjali
O’Hagan, Anne
Li, Lilian Y.
Ouellet, Daniele
Faelens, Ruben
Leirens, Quentin
Poggesi, Italo
Perez Ruixo, Juan Jose
Erdafitinib’s effect on serum phosphate justifies its pharmacodynamically guided dosing in patients with cancer
title Erdafitinib’s effect on serum phosphate justifies its pharmacodynamically guided dosing in patients with cancer
title_full Erdafitinib’s effect on serum phosphate justifies its pharmacodynamically guided dosing in patients with cancer
title_fullStr Erdafitinib’s effect on serum phosphate justifies its pharmacodynamically guided dosing in patients with cancer
title_full_unstemmed Erdafitinib’s effect on serum phosphate justifies its pharmacodynamically guided dosing in patients with cancer
title_short Erdafitinib’s effect on serum phosphate justifies its pharmacodynamically guided dosing in patients with cancer
title_sort erdafitinib’s effect on serum phosphate justifies its pharmacodynamically guided dosing in patients with cancer
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9124353/
https://www.ncbi.nlm.nih.gov/pubmed/34755484
http://dx.doi.org/10.1002/psp4.12727
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