Prediction of exposure-driven myelotoxicity of continuous infusion 5-fluorouracil by a semi-physiological pharmacokinetic–pharmacodynamic model in gastrointestinal cancer patients

Purpose To describe 5-fluorouracil (5FU) pharmacokinetics, myelotoxicity and respective covariates using a simultaneous nonlinear mixed effect modelling approach. Methods Thirty patients with gastrointestinal cancer received 5FU 650 or 1000 mg/m 2 /day as 5-day continuous venous infusion (14 of whom...

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Bibliographic Details
Published in:Cancer chemotherapy and pharmacology 2020-04, Vol.85 (4), p.711-722
Main Authors: Arshad, Usman, Ploylearmsaeng, Su-arpa, Karlsson, Mats O., Doroshyenko, Oxana, Langer, Dorothee, Schömig, Edgar, Kunze, Sabine, Güner, Semih A., Skripnichenko, Roman, Ullah, Sami, Jaehde, Ulrich, Fuhr, Uwe, Jetter, Alexander, Taubert, Max
Format: Article
Language:English
Subjects:
5-Fluorouracil
Blood
Cancer
Cancer Research
Cancer therapies
Chemotherapy
Cisplatin
Cytotoxicity
Drug dosages
Esophageal cancer
Exposure
Gastrointestinal cancer
Medicine
Medicine & Public Health
Myelosuppression
Oncology
Original
Original Article
Patients
Pharmacodynamics
Pharmacogenetics
Pharmacokinetics
Pharmacology
Pharmacology/Toxicology
Physiology
Radiation therapy
Time lag
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Summary:Purpose To describe 5-fluorouracil (5FU) pharmacokinetics, myelotoxicity and respective covariates using a simultaneous nonlinear mixed effect modelling approach. Methods Thirty patients with gastrointestinal cancer received 5FU 650 or 1000 mg/m 2 /day as 5-day continuous venous infusion (14 of whom also received cisplatin 20 mg/m 2 /day). 5FU and 5-fluoro-5,6-dihydrouracil (5FUH2) plasma concentrations were described by a pharmacokinetic model using NONMEM. Absolute leukocyte counts were described by a semi-mechanistic myelosuppression model. Covariate relationships were evaluated to explain the possible sources of variability in 5FU pharmacokinetics and pharmacodynamics. Results Total clearance of 5FU correlated with body surface area (BSA). Population estimate for total clearance was 249 L/h. Clearances of 5FU and 5FUH2 fractionally changed by 77%/m 2 difference from the median BSA. 5FU central and peripheral volumes of distribution were 5.56 L and 28.5 L, respectively. Estimated 5FUH2 clearance and volume of distribution were 121 L/h and 96.7 L, respectively. Baseline leukocyte count of 6.86 × 10 9 /L, as well as mean leukocyte transit time of 281 h accounting for time delay between proliferating and circulating cells, was estimated. The relationship between 5FU plasma concentrations and absolute leukocyte count was found to be linear. A higher degree of myelosuppression was attributed to combination therapy (slope = 2.82 L/mg) with cisplatin as compared to 5FU monotherapy (slope = 1.17 L/mg). Conclusions BSA should be taken into account for predicting 5FU exposure. Myelosuppression was influenced by 5FU exposure and concomitant administration of cisplatin.
ISSN:0344-5704
1432-0843
1432-0843
DOI:10.1007/s00280-019-04028-5