Search

Your search keyword '"Tibben, M. M."' showing total 47 results
Start Over Author "Tibben, M. M."
47 results on '"Tibben, M. M."'

12. Liquid chromatography-tandem mass spectrometric assay for the quantification of galunisertib in human plasma and the application in a pre-clinical study

Author

Tibben, M M, Huijberts, S, Li, W, Schinkel, A H, Gebretensae, A, Rosing, H, Beijnen, J H, Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, Afd Pharmacoepi & Clinical Pharmacology, and Pharmacoepidemiology and Clinical Pharmacology

Subjects
Male, Analyte, Bioanalysis, Clinical Biochemistry, Administration, Oral, Pharmaceutical Science, Sensitivity and Specificity, 01 natural sciences, Analytical Chemistry, Matrix (chemical analysis), Mice, Pharmacokinetics, LC–MS/MS, Tandem Mass Spectrometry, Transforming Growth Factor beta, Drug Discovery, Animals, Humans, Galunisertib, Protein precipitation, Protein Kinase Inhibitors, Chromatography, High Pressure Liquid, Spectroscopy, Chromatography, Tandem, human plasma, 010405 organic chemistry, Chemistry, 010401 analytical chemistry, Reproducibility of Results, assay, mouse plasma, quantification, 0104 chemical sciences, Triple quadrupole mass spectrometer, Quinolines, Pyrazoles, Galunisertb, Drug Screening Assays, Antitumor
Abstract

Galunisertib is an anti-cancer drug currently evaluated in phase I and II clinical trials. This study describes the development and validation of a bioanalytical assay to quantify galunisertib in human plasma using HPLC-MS/MS. Stable isotope labelled galunisertib was added as internal standard and the analyte and internal standard were extracted from the matrix by protein precipitation using acetonitrile-methanol (50:50, v/v). Final extracts were injected onto a C18 column, gradient elution was applied for chromatographic separation and detection was performed using a triple quadrupole mass spectrometer operating in the positive ion mode. The assay was linear over the range 0.05-10 ng/mL, with acceptable accuracy (bias ranging from -6.1 to 3.1%) and precision (below 5.7% C.V.) values. The applicability of the assay was demonstrated in a pharmacokinetic experiment in mice.

Published
2019

15. Metabolite profiling of the novel anti-cancer agent, plitidepsin, in urine and faeces in cancer patients after administration of 14C-plitidepsin

Author

van Andel, L, Rosing, H, Tibben, M M, Lucas, L, Lubomirov, R, Avilés, P, Francesch, A, Fudio, S, Gebretensae, A, Hillebrand, M J X, Schellens, J H M, Beijnen, J H, Afd Pharmacoepi & Clinical Pharmacology, and Pharmacoepidemiology and Clinical Pharmacology

Subjects
Total radioactivity, Metabolite profiling, ADME, Plitidepsin, LC-MS/MS, Aplidin
Abstract

PURPOSE: Plitidepsin absorption, distribution, metabolism and excretion characteristics were investigated in a mass balance study, in which six patients received a 3-h intravenous infusion containing 7 mg 14C-plitidepsin with a maximum radioactivity of 100 µCi. METHODS: Blood samples were drawn and excreta were collected until less than 1% of the administered radioactivity was excreted per matrix for two consecutive days. Samples were pooled within-patients and between-patients and samples were screened for metabolites. Afterwards, metabolites were identified and quantified. Analysis was done using Liquid Chromatography linked to an Ion Trap Mass Spectrometer and offline Liquid Scintillation Counting (LC-Ion Trap MS-LSC). RESULTS: On average 4.5 and 62.4% of the administered dose was excreted via urine over the first 24 h and in faeces over 240 h, respectively. Most metabolites were found in faeces. CONCLUSION: Plitidepsin is extensively metabolised and it undergoes dealkylation (demethylation), oxidation, carbonyl reduction, and (internal) hydrolysis. The chemical formula of several metabolites was confirmed using high resolution mass data.

Published
2018

16. Liquid chromatography-tandem mass spectrometric assay for the quantification of galunisertib in human plasma and the application in a pre-clinical study

Author

Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, Tibben, M M, Huijberts, S, Li, W, Schinkel, A H, Gebretensae, A, Rosing, H, Beijnen, J H, Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, Tibben, M M, Huijberts, S, Li, W, Schinkel, A H, Gebretensae, A, Rosing, H, and Beijnen, J H

Published
2019

17. Development and validation of a liquid chromatography-tandem mass spectrometry assay for the quantification of lurbinectedin in human plasma and urine

Author

van Andel, L, Rosing, H, Lubomirov, R, Avilés, P, Fudio, S, Tibben, M M, Nan-Offeringa, L, Schellens, J H M, Beijnen, J H, van Andel, L, Rosing, H, Lubomirov, R, Avilés, P, Fudio, S, Tibben, M M, Nan-Offeringa, L, Schellens, J H M, and Beijnen, J H

Abstract

Lurbinectedin is a novel highly selective inhibitor of RNA polymerase II triggering caspase-dependent apoptosis of cancerous cells. This article describes the development and validation of a liquid chromatography-tandem mass spectrometry (LC-MS/MS) assay to quantify lurbinectedin in human plasma and urine. Plasma samples were pre-treated with 1 M aqueous ammonia after which they were brought onto supported liquid extraction (SLE) columns. Lurbinectedin was eluted from the columns using tert-butyl methyl ether (TBME). Urine was first diluted in plasma and lurbinectedin was extracted from this matrix by liquid-liquid extraction using TBME. Samples were measured by LC-MS/MS in the positive electron ion spray mode. The method was linear over 0.1-100 ng/mL and 1-1000 ng/mL in plasma and urine, respectively, with accuracies and precisions within ±15% (20% for LLOQ) and below 15% (20% for LLOQ), respectively. The method was developed to support a mass balance study in which patients received a dose of 5 mg lurbinectedin.

Published
2018

18. Metabolite profiling of the novel anti-cancer agent, plitidepsin, in urine and faeces in cancer patients after administration of 14C-plitidepsin

Author

Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, van Andel, L, Rosing, H, Tibben, M M, Lucas, L, Lubomirov, R, Avilés, P, Francesch, A, Fudio, S, Gebretensae, A, Hillebrand, M J X, Schellens, J H M, Beijnen, J H, Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, van Andel, L, Rosing, H, Tibben, M M, Lucas, L, Lubomirov, R, Avilés, P, Francesch, A, Fudio, S, Gebretensae, A, Hillebrand, M J X, Schellens, J H M, and Beijnen, J H

Published
2018

19. Development and validation of a liquid chromatography-tandem mass spectrometry assay for the quantification of lurbinectedin in human plasma and urine

Author

Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, van Andel, L, Rosing, H, Lubomirov, R, Avilés, P, Fudio, S, Tibben, M M, Nan-Offeringa, L, Schellens, J H M, Beijnen, J H, Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, van Andel, L, Rosing, H, Lubomirov, R, Avilés, P, Fudio, S, Tibben, M M, Nan-Offeringa, L, Schellens, J H M, and Beijnen, J H

Published
2018

20. Liquid chromatography-tandem mass spectrometry assay for the quantification of niraparib and its metabolite M1 in human plasma and urine

Author

van Andel, L, Zhang, Z, Lu, S, Kansra, V, Agarwal, S, Hughes, L, Tibben, M M, Gebretensae, A, Rosing, H, Schellens, J H M, Beijnen, J H, Pharmacoepidemiology and Clinical Pharmacology, Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, and Afd Pharmacoepi & Clinical Pharmacology

Subjects
Bioanalysis, Electrospray, Indazoles, Formic acid, Metabolite, Clinical Biochemistry, Niraparib, Poly(ADP-ribose) Polymerase Inhibitors, Mass spectrometry, 01 natural sciences, Biochemistry, Analytical Chemistry, MK-4827, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Piperidines, Liquid chromatography–mass spectrometry, Limit of Detection, Tandem Mass Spectrometry, Protein precipitation, Humans, Pharmacokinetics, Chromatography, High Pressure Liquid, Chromatography, Chemistry, HPLC-MS/MS, 010401 analytical chemistry, Selected reaction monitoring, Cell Biology, General Medicine, 0104 chemical sciences, 030220 oncology & carcinogenesis
Abstract

Niraparib (MK-4827) is a novel poly(ADP-Ribose) polymerase (PARP) inhibitor currently investigated in phase III clinical trials to treat cancers. The development of a new drug includes the characterisation of absorption, metabolism and excretion (AME) of the compound. AME studies are a requirement of regulatory agencies and for this purpose bioanalytical assays are essential. This article describes the development and validation of a bioanalytical assay for niraparib and its carboxylic acid metabolite M1 in human plasma and urine using liquid chromatography-tandem mass spectrometry (LC-MS/MS). Sample pre-treatment involved protein precipitation for plasma and dilution of urine samples using acetonitrile-methanol (50:50, v/v). Final extracts were injected onto a SunFire C18 column and gradient elution using 20mM ammonium acetate (mobile phase A) and formic acid:acetonitrile:methanol (0.1:50:50, v/v/v) (mobile phase B) was applied. Detection was performed on an API5500 tandem mass spectrometer operating in the positive electrospray ionisation mode applying multiple reaction monitoring (MRM). The assay was successfully validated in accordance with the Food and Drug Administration and latest European Medicines Agency guidelines on bioanalytical method validation and can therefore be applied in pharmacological clinical studies.

Published
2016

21. Liquid chromatography-tandem mass spectrometry assay for the quantification of niraparib and its metabolite M1 in human plasma and urine

Author

van Andel, L, Zhang, Z, Lu, S, Kansra, V, Agarwal, S, Hughes, L, Tibben, M M, Gebretensae, A, Rosing, H, Schellens, J H M, Beijnen, J H, van Andel, L, Zhang, Z, Lu, S, Kansra, V, Agarwal, S, Hughes, L, Tibben, M M, Gebretensae, A, Rosing, H, Schellens, J H M, and Beijnen, J H

Abstract

Niraparib (MK-4827) is a novel poly(ADP-Ribose) polymerase (PARP) inhibitor currently investigated in phase III clinical trials to treat cancers. The development of a new drug includes the characterisation of absorption, metabolism and excretion (AME) of the compound. AME studies are a requirement of regulatory agencies and for this purpose bioanalytical assays are essential. This article describes the development and validation of a bioanalytical assay for niraparib and its carboxylic acid metabolite M1 in human plasma and urine using liquid chromatography-tandem mass spectrometry (LC-MS/MS). Sample pre-treatment involved protein precipitation for plasma and dilution of urine samples using acetonitrile-methanol (50:50, v/v). Final extracts were injected onto a SunFire C18 column and gradient elution using 20mM ammonium acetate (mobile phase A) and formic acid:acetonitrile:methanol (0.1:50:50, v/v/v) (mobile phase B) was applied. Detection was performed on an API5500 tandem mass spectrometer operating in the positive electrospray ionisation mode applying multiple reaction monitoring (MRM). The assay was successfully validated in accordance with the Food and Drug Administration and latest European Medicines Agency guidelines on bioanalytical method validation and can therefore be applied in pharmacological clinical studies.

Published
2017

22. Liquid chromatography-tandem mass spectrometry assay for the quantification of niraparib and its metabolite M1 in human plasma and urine

Author

Pharmacoepidemiology and Clinical Pharmacology, Afd Pharmacoepi & Clinical Pharmacology, van Andel, L, Zhang, Z, Lu, S, Kansra, V, Agarwal, S, Hughes, L, Tibben, M M, Gebretensae, A, Rosing, H, Schellens, J H M, Beijnen, J H, Pharmacoepidemiology and Clinical Pharmacology, Afd Pharmacoepi & Clinical Pharmacology, van Andel, L, Zhang, Z, Lu, S, Kansra, V, Agarwal, S, Hughes, L, Tibben, M M, Gebretensae, A, Rosing, H, Schellens, J H M, and Beijnen, J H

Published
2017

23. Pharmacokinetics and excretion of 14C–Plitidepsin in patients with advanced cancer

Author

Pharmacoepidemiology and Clinical Pharmacology, Afd Pharmacoepi & Clinical Pharmacology, van Andel, L., Fudio, S., Rosing, H., Munt, S., Miguel-Lillo, B., González, I., Tibben, M. M., de Vries, N., de Vries Schultink, Aurelia H M, Schellens, J. H M, Beijnen, J. H., Pharmacoepidemiology and Clinical Pharmacology, Afd Pharmacoepi & Clinical Pharmacology, van Andel, L., Fudio, S., Rosing, H., Munt, S., Miguel-Lillo, B., González, I., Tibben, M. M., de Vries, N., de Vries Schultink, Aurelia H M, Schellens, J. H M, and Beijnen, J. H.

Published
2017

24. Metabolite profiling of the novel anti-cancer agent, plitidepsin, in urine and faeces in cancer patients after administration of 14C-plitidepsin.

Author

Rosing, H., Tibben, M. M., Lucas, L., Gebretensae, A., Hillebrand, M. J. X., van Andel, L., Beijnen, J. H., Schellens, J. H. M., Lubomirov, R., Avilés, P., Francesch, A., and Fudio, S.

Subjects
ANTINEOPLASTIC agents, METABOLITE analysis, URINALYSIS, FECAL analysis, RADIOACTIVITY, DEALKYLATION, CLINICAL trials, COMPARATIVE studies, FECES, LIQUID chromatography, MASS spectrometry, RESEARCH methodology, MEDICAL cooperation, PEPTIDES, RADIOISOTOPES, RESEARCH, TUMORS, EVALUATION research
Abstract

Purpose: Plitidepsin absorption, distribution, metabolism and excretion characteristics were investigated in a mass balance study, in which six patients received a 3-h intravenous infusion containing 7 mg 14C-plitidepsin with a maximum radioactivity of 100 µCi.Methods: Blood samples were drawn and excreta were collected until less than 1% of the administered radioactivity was excreted per matrix for two consecutive days. Samples were pooled within-patients and between-patients and samples were screened for metabolites. Afterwards, metabolites were identified and quantified. Analysis was done using Liquid Chromatography linked to an Ion Trap Mass Spectrometer and offline Liquid Scintillation Counting (LC-Ion Trap MS-LSC).Results: On average 4.5 and 62.4% of the administered dose was excreted via urine over the first 24 h and in faeces over 240 h, respectively. Most metabolites were found in faeces.Conclusion: Plitidepsin is extensively metabolised and it undergoes dealkylation (demethylation), oxidation, carbonyl reduction, and (internal) hydrolysis. The chemical formula of several metabolites was confirmed using high resolution mass data. [ABSTRACT FROM AUTHOR]

Published
2018
Full Text
View/download PDF

26. Phase i and pharmacological trial of lapatinib in combination with gemcitabine in patients with advanced breast cancer

Author

Pharmacoepidemiology and Clinical Pharmacology, Sub Clinical Pharmacology, Van Der Noll, R., Smit, W. M., Wymenga, A. N M, Boss, D. S., Grob, M., Huitema, A. D R, Rosing, H., Tibben, M. M., Keessen, M., Rehorst, H., Beijnen, J. H., Schellens, J. H M, Pharmacoepidemiology and Clinical Pharmacology, Sub Clinical Pharmacology, Van Der Noll, R., Smit, W. M., Wymenga, A. N M, Boss, D. S., Grob, M., Huitema, A. D R, Rosing, H., Tibben, M. M., Keessen, M., Rehorst, H., Beijnen, J. H., and Schellens, J. H M

Published
2015

27. Determination of the absolute oral bioavailability of niraparib by simultaneous administration of a 14C-microtracer and therapeutic dose in cancer patients.

Author

van Andel, L., Rosing, H., Zhang, Z., Hughes, L., Kansra, V., Sanghvi, M., Tibben, M. M., Gebretensae, A., Schellens, J. H. M., and Beijnen, J. H.

Subjects
OVARIAN epithelial cancer, PERITONEAL cancer, BIOAVAILABILITY, SMALL molecules, CANCER treatment, THERAPEUTICS
Abstract

Introduction: Niraparib (Zejula™) is a poly(ADP-ribose) polymerase inhibitor recently approved by the US Food and Drug Administration for the maintenance treatment of patients with recurrent platinum-sensitive epithelial ovarian, fallopian tube, or primary peritoneal cancer who are in a complete or partial response to platinum-based chemotherapy. The pivotal phase III clinical trial has shown improved progression-free survival in patients receiving niraparib compared with those receiving placebo.Purpose: Since niraparib is administered orally, it is of interest to investigate the oral bioavailability (F po) of this novel compound, which is the aim of this study.Methods: Six patients received an oral therapeutic dose of 300 mg niraparib, followed by a 15-min intravenous infusion of 100 µg 14C-niraparib with a radioactivity of approximately 100 nCi. The niraparib therapeutic dose was measured in plasma using a validated liquid chromatography-tandem mass spectrometry method, whereas the total 14C-radioactivity and 14C-niraparib plasma levels were measured by accelerator mass spectrometry and a validated high performance liquid chromatography assay with AMS.Results: The F po of niraparib was determined to be 72.7% in humans. [ABSTRACT FROM AUTHOR]

Published
2018
Full Text
View/download PDF

28. A mechanism-based pharmacokinetic model for the cytochrome P450 drug-drug interaction between cyclophosphamide and thioTEPA and the autoinduction of cyclophosphamide

Author

Huitema, A. D., Mathôt, R. A., Tibben, M. M., Rodenhuis, S., Beijnen, J. H., and Other departments

Abstract

Cyclophosphamide (CP) is widely used in high-dose chemotherapy regimens in combination with thioTEPA. CP is a prodrug and is activated by cytochrome P450 to 4-hydroxycyclophosphamide (HCP) which yields the final cytotoxic metabolite phosphoramide mustard (PM). The metabolism of CP into HCP exhibits autoinduction but is inhibited by thioTEPA. The aim of this study was to develop a population pharmacokinetic model for the bioactivation route of CP incorporating the phenomena of both autoinduction and the drug-drug interaction between CP and thioTEPA. Plasma samples were collected from 34 patients who received high-dose CP, thioTEPA and carboplatin in short infusions during 4 consecutive days. Elimination of CP was described by a noninducible route and an inducible route leading to HCP. The latter route was mediated by a hypothetical amount of enzyme. Autoinduction leads to a zero-order increase in amount of this enzyme during treatment. Inhibition by thioTEPA was modeled as a reversible, competitive, concentration-dependent inhibition. PM pharmacokinetics were described by first-order formation from HCP and first-order elimination. The final models for CP, HCP, and PM provided an adequate fit of the experimental data. The volume of distribution, noninducible and initial inducible clearances of CP were 31.0 L, 1.58 L/hr and 4.76 L/hr, respectively. The enzyme amount increased with a zero-order rate constant of 0.041 amount * hr-1. After each thioTEPA infusion, however, approximately 80% of the enzyme was inhibited. This inhibition was reversible with a half-life of 6.5 hr. The formation and elimination rate constants of PM were 1.58 and 0.338 hr-1, respectively. The developed model enabled the assessment of the complex pharmacokinetics of CP in combination with thio TEPA. This model provided an adequate description of enzyme induction and inhibition and can be used for treatment optimization in this combination

Published
2001

29. Population pharmacokinetics of thioTEPA and its active metabolite TEPA in patients undergoing high-dose chemotherapy

Author

Huitema, A. D., Mathôt, R. A., Tibben, M. M., Schellens, J. H., Rodenhuis, S., Beijnen, J. H., and Other departments

Abstract

To study the population pharmacokinetics of thioTEPA and its main metabolite TEPA in patients receiving high-dose chemotherapy consisting of thioTEPA (80-120 mg x m(-2) x day(-1)), cyclophosphamide (1000-1500 mg x m(-2) x day(-1)) and carboplatin (265-400 mg x m(-2) x day(-1)) for 4 days. ThioTEPA and TEPA kinetic data were processed with a two-compartment model using the nonlinear mixed effect modelling program NONMEM. Interindividual variability (IIV), interoccasion variability (IOV) and residual variability in the pharmacokinetics were estimated. The influence of patient characteristics on the pharmacokinetics was also determined. A total number of 40 patients receiving 65 courses of chemotherapy was included. Clearance of thioTEPA (CL) was 34 l x h(-1) with an IIV and IOV of 18 and 11%, respectively. The volume of distribution of thioTEPA was 47 l (IIV = 7.5%; IOV = 19%). The fraction of thioTEPA converted to TEPA divided by the volume of distribution of TEPA was 0.030 l-1 (IIV = 39%; IOV = 32%) and the elimination rate constant of TEPA was 0.64 h(-1) (IIV = 27%; IOV = 32%). CL of thioTEPA was correlated with alkaline phosphatase and serum albumin. The volume of distribution of thioTEPA and the elimination rate constant of TEPA were correlated with total protein levels and body weight, respectively. A model for the description of the pharmacokinetics of thioTEPA and TEPA was developed. Factors involved in the interpatient variability of thioTEPA and TEPA pharmacokinetics were identified. Since, IOV of both thioTEPA and TEPA was equal to or smaller than IIV, therapeutic drug monitoring based on data of previous courses may be meaningful using this population model

Published
2001

37. Metabolic Disposition of Lurbinectedin, a Potent Selective Inhibitor of Active Transcription of Protein-Coding Genes, in Nonclinical Species and Patients.

Author

Aviles P, Altares R, van Andel L, Lubomirov R, Fudio S, Rosing H, Márquez Del Pino FM, Tibben MM, Benedit G, Nan-Offeringa L, Luepke Estefan XE, Francesch A, Zeaiter A, Cuevas C, Schellens JHM, and Beijnen JH

Subjects
Animals, Carbolines pharmacology, Carbolines therapeutic use, Feces, Female, Heterocyclic Compounds, 4 or More Rings therapeutic use, Humans, Male, Rats, Lung Neoplasms drug therapy, Lung Neoplasms genetics, Small Cell Lung Carcinoma chemically induced, Small Cell Lung Carcinoma drug therapy, Small Cell Lung Carcinoma pathology
Abstract

Lurbinectedin is a novel and potent selective inhibitor of active transcription of protein-coding genes, triggering apoptosis of cancerous cells. It has been approved for the treatment of patients with metastatic small-cell lung cancer with disease progression on or after platinum-based chemotherapy. Studies exploring the disposition and metabolism of lurbinectedin were performed in vitro and in vivo (by intravenous administration of lurbinectedin). Low blood cell partitioning for lurbinectedin in rats, nonhuman primates (NHP), and humans was determined as 23.4%, 29.8%, and 9.8%, respectively. Protein binding was very high (>95%) in total plasma (rat, NHP, and human), albumin, and α -1-acid glycoprotein (both human). In vitro, lurbinectedin underwent intense liver microsome-mediated metabolism-in 10 minutes, 80% of the compound is metabolized in human-with CYP3A4 being the isoform involved in that metabolism. Results also showed NHPs being the nonclinical species which, metabolically, most closely resembles humans. Mass balance studies performed in rats (both genders), NHPs (male only), and patients (both genders) demonstrated that the principal route of excretion of 14 C-lurbinectedin-related radioactivity was through the feces (88.7% ± 10.1% in patients), with only a minor fraction recovered from the urine (5.6% ± 2.0% in patients). In plasma samples, the majority of lurbinectedin-related radioactivity was attributed to unchanged compound (95% ± 3.1% and 70.2% ± 10.9% in NHPs and humans, respectively). Plasma metabolic profiling demonstrated the major (% compared with unchanged compound) circulating metabolites were N -Desmethyl-lurbinectedin (0.4% ± 0.2% and 10.4% ± 2.2% in NHPs and patients, respectively) and 1',3'-Desmethylene-lurbinectedin (0.9% ± 0.7% and 14.3% ± 10.4% in NHP and patients, respectively). SIGNIFICANCE STATEMENT: Lurbinectedin is a novel and potent selective inhibitor of active transcription of protein-coding genes, triggering apoptosis of cancerous cells, and was recently approved for the treatment of patients with metastatic small-cell lung cancer with disease progression on or after platinum-based chemotherapy. The present study provides a complete set of information on the pharmacokinetics, biotransformation, and elimination of 14 C-lurbinectedin and its metabolites, following a single intravenous administration to nonclinical species (rats and nonhuman primates) and patients., (Copyright © 2022 by The American Society for Pharmacology and Experimental Therapeutics.)

Published
2022
Full Text
View/download PDF

38. Liquid chromatography-tandem mass spectrometric assay for the quantification of galunisertib in human plasma and the application in a pre-clinical study.

Author

Tibben MM, Huijberts S, Li W, Schinkel AH, Gebretensae A, Rosing H, and Beijnen JH

Subjects
Administration, Oral, Animals, Chromatography, High Pressure Liquid methods, Drug Screening Assays, Antitumor, Humans, Male, Mice, Protein Kinase Inhibitors administration & dosage, Protein Kinase Inhibitors pharmacokinetics, Pyrazoles administration & dosage, Pyrazoles pharmacokinetics, Quinolines administration & dosage, Quinolines pharmacokinetics, Reproducibility of Results, Sensitivity and Specificity, Transforming Growth Factor beta antagonists & inhibitors, Protein Kinase Inhibitors blood, Pyrazoles blood, Quinolines blood, Tandem Mass Spectrometry methods
Abstract

Galunisertib is an anti-cancer drug currently evaluated in phase I and II clinical trials. This study describes the development and validation of a bioanalytical assay to quantify galunisertib in human plasma using HPLC-MS/MS. Stable isotope labelled galunisertib was added as internal standard and the analyte and internal standard were extracted from the matrix by protein precipitation using acetonitrile-methanol (50:50, v/v). Final extracts were injected onto a C18 column, gradient elution was applied for chromatographic separation and detection was performed using a triple quadrupole mass spectrometer operating in the positive ion mode. The assay was linear over the range 0.05-10 ng/mL, with acceptable accuracy (bias ranging from -6.1 to 3.1%) and precision (below 5.7% C.V.) values. The applicability of the assay was demonstrated in a pharmacokinetic experiment in mice., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published
2019
Full Text
View/download PDF

39. Liquid chromatography-tandem mass spectrometry assay for the quantification of niraparib and its metabolite M1 in human plasma and urine.

Author

van Andel L, Zhang Z, Lu S, Kansra V, Agarwal S, Hughes L, Tibben MM, Gebretensae A, Rosing H, Schellens JHM, and Beijnen JH

Subjects
Humans, Indazoles metabolism, Limit of Detection, Piperidines metabolism, Poly(ADP-ribose) Polymerase Inhibitors metabolism, Chromatography, High Pressure Liquid methods, Indazoles blood, Indazoles urine, Piperidines blood, Piperidines urine, Poly(ADP-ribose) Polymerase Inhibitors blood, Poly(ADP-ribose) Polymerase Inhibitors urine, Tandem Mass Spectrometry methods
Abstract

Niraparib (MK-4827) is a novel poly(ADP-Ribose) polymerase (PARP) inhibitor currently investigated in phase III clinical trials to treat cancers. The development of a new drug includes the characterisation of absorption, metabolism and excretion (AME) of the compound. AME studies are a requirement of regulatory agencies and for this purpose bioanalytical assays are essential. This article describes the development and validation of a bioanalytical assay for niraparib and its carboxylic acid metabolite M1 in human plasma and urine using liquid chromatography-tandem mass spectrometry (LC-MS/MS). Sample pre-treatment involved protein precipitation for plasma and dilution of urine samples using acetonitrile-methanol (50:50, v/v). Final extracts were injected onto a SunFire C18 column and gradient elution using 20mM ammonium acetate (mobile phase A) and formic acid:acetonitrile:methanol (0.1:50:50, v/v/v) (mobile phase B) was applied. Detection was performed on an API5500 tandem mass spectrometer operating in the positive electrospray ionisation mode applying multiple reaction monitoring (MRM). The assay was successfully validated in accordance with the Food and Drug Administration and latest European Medicines Agency guidelines on bioanalytical method validation and can therefore be applied in pharmacological clinical studies., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published
2017
Full Text
View/download PDF

40. Determination of total platinum in plasma and plasma ultrafiltrate, from subjects dosed with the platinum-containing N-(2-hydroxypropyl)methacrylamide copolymer AP5280, by use of graphite-furnace Zeeman atomic-absorption spectrometry.

Author

Tibben MM, Rademaker-Lakhai JM, Rice JR, Stewart DR, Schellens JH, and Beijnen JH

Subjects
Acrylamides pharmacokinetics, Calibration, Drug Delivery Systems standards, Hemofiltration, Humans, Organoplatinum Compounds pharmacokinetics, Platinum pharmacokinetics, Reproducibility of Results, Sensitivity and Specificity, Spectrophotometry, Atomic, Acrylamides administration & dosage, Organoplatinum Compounds administration & dosage, Platinum blood
Abstract

AP5280 is an N-(2-hydroxypropyl)methacrylamide (HPMA) copolymer to which are linked tetrapeptide side chains containing bioactive platinum complexes at their C-terminal sides. We have developed and validated a rapid and sensitive analytical assay for the determination of total platinum concentrations in plasma, and free platinum of an AP5280 origin in plasma ultrafiltrate (PUF), of subjects dosed with AP5280. The total platinum levels were determined by use of graphite-furnace atomic-absorption spectrometry (GF-AAS) with Zeeman correction after appropriate dilution of the plasma sample with plasma-hydrochloric acid 0.2 mol L(-1) (1:5) as diluent. The limit of quantitation of this assay is 0.25 micromol L(-1) platinum in plasma. Linear calibration curves were obtained over the concentration range 0.25-5.0 micromol L(-1). Accuracy was between 87.7% and 104.2% and precision was 15.3% at the lowest concentration and less than 14% for all other levels tested. Accuracy and precision were thus in accordance with generally accepted criteria for analytical methods. Analysis of samples obtained from patients receiving AP5280 demonstrated the applicability of the described assay. Analysis of free platinum in PUF was performed by use of a previously validated and reported assay from our institute in which the same instrumental method is used.

Published
2002
Full Text
View/download PDF

41. Validation of a therapeutic drug monitoring strategy for thiotepa in a high-dose chemotherapy regimen.

Author

Huitema AD, Mathôt RA, Tibben MM, Rodenhuis S, and Beijnen JH

Subjects
Antineoplastic Combined Chemotherapy Protocols therapeutic use, Area Under Curve, Female, Humans, Thiotepa administration & dosage, Antineoplastic Agents, Alkylating pharmacokinetics, Drug Monitoring methods, Thiotepa pharmacokinetics
Abstract

Thiotepa is an alkylating agent widely used in high-dose chemotherapy. The pharmacokinetics of thiotepa and its main metabolite tepa show a wide interpatient variability, which may be responsible for the interpatient variability in toxicity. The aim of this study was to develop and validate a pharmacokinetically guided dosing strategy with the sum of the thiotepa and tepa area under the concentration-time curve (AUC) as the target parameter. A total of 46 patients received 77 courses of chemotherapy with thiotepa (80-120 mg/m(2) per day) divided into two daily 30-minute infusions in combination with cyclophosphamide and carboplatin. Patients received up to three courses of chemotherapy. The interpatient, course-to-course, day-to-day, and residual variability in the pharmacokinetics of thiotepa and tepa were estimated with a population analysis with the software program NONMEM. The planned strategy consisted of the collection of blood samples on day 1 and either day 3 or day 4 of each 4-day course. The thiotepa dose was planned to be adjusted on day 3 of each course and before the start of a new course on the basis of Bayesian predictions of the pharmacokinetics with data of day 1 and/or the possible previous course. The prediction procedure was validated by dividing the dataset into an index and validation set. The Bayesian predictions of the validation set were compared with true AUC values generated with individual fits of each course. The performance of the complete strategy was tested with a simulation procedure in 1,000 patients. Interpatient variability and course-to-course variability were in the same order (+/-20%); day-to-day variability was less (+/-15%). The sampling strategy resulted in predictions of the AUC without bias with acceptable precision (+/-20%). The simulation showed that variability in exposure was effectively decreased by the dosing strategy. This strategy resulted in a reduction in the variability of the exposure to thiotepa and tepa and can be implemented in a clinical study.

Published
2001
Full Text
View/download PDF

42. A mechanism-based pharmacokinetic model for the cytochrome P450 drug-drug interaction between cyclophosphamide and thioTEPA and the autoinduction of cyclophosphamide.

Author

Huitema AD, Mathôt RA, Tibben MM, Rodenhuis S, and Beijnen JH

Subjects
Adolescent, Adult, Antineoplastic Agents, Alkylating chemistry, Cyclophosphamide chemistry, Drug Interactions physiology, Female, Humans, Male, Middle Aged, Nonlinear Dynamics, Phosphoramide Mustards metabolism, Antineoplastic Agents, Alkylating pharmacokinetics, Cyclophosphamide pharmacokinetics, Cytochrome P-450 Enzyme System metabolism, Models, Chemical, Thiotepa pharmacokinetics
Abstract

Cyclophosphamide (CP) is widely used in high-dose chemotherapy regimens in combination with thioTEPA. CP is a prodrug and is activated by cytochrome P450 to 4-hydroxycyclophosphamide (HCP) which yields the final cytotoxic metabolite phosphoramide mustard (PM). The metabolism of CP into HCP exhibits autoinduction but is inhibited by thioTEPA. The aim of this study was to develop a population pharmacokinetic model for the bioactivation route of CP incorporating the phenomena of both autoinduction and the drug-drug interaction between CP and thioTEPA. Plasma samples were collected from 34 patients who received high-dose CP, thioTEPA and carboplatin in short infusions during 4 consecutive days. Elimination of CP was described by a noninducible route and an inducible route leading to HCP. The latter route was mediated by a hypothetical amount of enzyme. Autoinduction leads to a zero-order increase in amount of this enzyme during treatment. Inhibition by thioTEPA was modeled as a reversible, competitive, concentration-dependent inhibition. PM pharmacokinetics were described by first-order formation from HCP and first-order elimination. The final models for CP, HCP, and PM provided an adequate fit of the experimental data. The volume of distribution, noninducible and initial inducible clearances of CP were 31.0 L, 1.58 L/hr and 4.76 L/hr, respectively. The enzyme amount increased with a zero-order rate constant of 0.041 amount * hr-1. After each thioTEPA infusion, however, approximately 80% of the enzyme was inhibited. This inhibition was reversible with a half-life of 6.5 hr. The formation and elimination rate constants of PM were 1.58 and 0.338 hr-1, respectively. The developed model enabled the assessment of the complex pharmacokinetics of CP in combination with thio TEPA. This model provided an adequate description of enzyme induction and inhibition and can be used for treatment optimization in this combination.

Published
2001
Full Text
View/download PDF

43. Population pharmacokinetics of thioTEPA and its active metabolite TEPA in patients undergoing high-dose chemotherapy.

Author

Huitema AD, Mathôt RA, Tibben MM, Schellens JH, Rodenhuis S, and Beijnen JH

Subjects
Adolescent, Adult, Algorithms, Analysis of Variance, Antineoplastic Agents, Alkylating blood, Area Under Curve, Bayes Theorem, Female, Humans, Male, Middle Aged, Models, Biological, Neoplasms blood, Population, Thiotepa blood, Triethylenephosphoramide blood, Antineoplastic Agents, Alkylating pharmacokinetics, Thiotepa pharmacokinetics
Abstract

Aims: To study the population pharmacokinetics of thioTEPA and its main metabolite TEPA in patients receiving high-dose chemotherapy consisting of thioTEPA (80-120 mg x m(-2) x day(-1)), cyclophosphamide (1000-1500 mg x m(-2) x day(-1)) and carboplatin (265-400 mg x m(-2) x day(-1)) for 4 days., Methods: ThioTEPA and TEPA kinetic data were processed with a two-compartment model using the nonlinear mixed effect modelling program NONMEM. Interindividual variability (IIV), interoccasion variability (IOV) and residual variability in the pharmacokinetics were estimated. The influence of patient characteristics on the pharmacokinetics was also determined., Results: A total number of 40 patients receiving 65 courses of chemotherapy was included. Clearance of thioTEPA (CL) was 34 l x h(-1) with an IIV and IOV of 18 and 11%, respectively. The volume of distribution of thioTEPA was 47 l (IIV = 7.5%; IOV = 19%). The fraction of thioTEPA converted to TEPA divided by the volume of distribution of TEPA was 0.030 l-1 (IIV = 39%; IOV = 32%) and the elimination rate constant of TEPA was 0.64 h(-1) (IIV = 27%; IOV = 32%). CL of thioTEPA was correlated with alkaline phosphatase and serum albumin. The volume of distribution of thioTEPA and the elimination rate constant of TEPA were correlated with total protein levels and body weight, respectively., Conclusions: A model for the description of the pharmacokinetics of thioTEPA and TEPA was developed. Factors involved in the interpatient variability of thioTEPA and TEPA pharmacokinetics were identified. Since, IOV of both thioTEPA and TEPA was equal to or smaller than IIV, therapeutic drug monitoring based on data of previous courses may be meaningful using this population model.

Published
2001
Full Text
View/download PDF

44. Validation of techniques for the prediction of carboplatin exposure: application of Bayesian methods.

Author

Huitema AD, Mathôt RA, Tibben MM, Schellens JH, Rodenhuis S, and Beijnen JH

Subjects
Adult, Antineoplastic Agents blood, Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Area Under Curve, Carboplatin blood, Cyclophosphamide pharmacokinetics, Female, Glomerular Filtration Rate, Humans, Infusions, Intravenous, Male, Mathematical Computing, Middle Aged, Predictive Value of Tests, Reproducibility of Results, Thiotepa pharmacokinetics, Antineoplastic Agents administration & dosage, Antineoplastic Agents pharmacokinetics, Bayes Theorem, Carboplatin administration & dosage, Carboplatin pharmacokinetics, Models, Statistical
Abstract

Objective: Several methods have been developed for the prediction of carboplatin exposure to facilitate pharmacokinetic guided dosing. The aim of this study was to develop and validate sparse data Bayesian methods for the estimation of carboplatin exposure and to validate other commonly applied techniques, such as the Chatelut formula, the Sorensen limited sampling model, and the Calvert formula, in which glomerular filtration rate was estimated with the Cockcroft-Gault, the Jelliffe, and the recently proposed Wright formulas., Methods: Complete concentration-time curves were available for a total of 43 patients (45 courses) receiving carboplatin (265 or 400 mg/m2/day) in a 1-hour infusion for 4 consecutive days in combination with thiotepa and cyclophosphamide. A population two-compartment model was developed on an index set of 12 courses. The other 33 courses served as validation set. Bayesian estimates were generated with the population parameters by use of either one or two randomly timed samples or two samples at optimal time points determined with the D-optimality theory., Results: The Bayesian methods provided an accurate and precise prediction of the area under the concentration-time curve (bias <4% and precision <18%). The other formulas (Sorensen model, Chatelut, and Calvert with Jelliffe, Cockcroft-Gault, and Wright) resulted in a precision >18%, whereas the Jelliffe formula and the Sorensen model resulted in a bias >12%., Conclusion: The applicability of a Bayesian method for the prediction of the carboplatin exposure by use of one or two samples without the necessity for exact timing of infusion duration and sampling was demonstrated. The Bayesian method may be very instrumental to execute pharmacokinetic guided dosing for carboplatin.

Published
2000
Full Text
View/download PDF

45. Reduction of cyclophosphamide bioactivation by thioTEPA: critical sequence-dependency in high-dose chemotherapy regimens.

Author

Huitema AD, Kerbusch T, Tibben MM, Rodenhuis S, and Beijnen JH

Subjects
Biotransformation, Cyclophosphamide administration & dosage, Cyclophosphamide analogs & derivatives, Cyclophosphamide blood, Drug Administration Schedule, Hematopoietic Stem Cell Transplantation, Humans, Kinetics, Microsomes metabolism, Neoplasms blood, Thiotepa administration & dosage, Time Factors, Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Cyclophosphamide pharmacokinetics, Neoplasms drug therapy, Thiotepa pharmacokinetics
Abstract

Purpose: Cyclophosphamide and thioTEPA are frequently used simultaneously in high-dose chemotherapy regimens. During a pharmacokinetic study of 31 courses in 20 patients of cyclophosphamide and its activated metabolite 4-hydroxycyclophosphamide given in the combination cyclophosphamide thioTEPA carboplatin, a sharp decrease in 4-hydroxycyclophosphamide concentration was observed immediately after the start of the thioTEPA infusion. A drug-drug interaction was suspected. This putative interaction was investigated in this study., Methods: Possible sequence dependency, due to inhibition of the formation of 4-hydroxycyclophosphamide by thioTEPA, was investigated by altering the sequence of infusion in three patients (four courses) receiving high-dose chemotherapy with cyclophosphamide (1,000 or 1,500 mg/m2 per day), thioTEPA (80 or 120 mg/m2 per day) and carboplatin (265 or 400 mg/m2 per day) in short infusions for four consecutive days. The pharmacokinetics of cyclophosphamide and 4-hydroxycyclophosphamide were established. Possible inhibition of the metabolism of cyclophosphamide and thioTEPA was investigated in human microsomes., Results: A striking sequence dependency of the pharmacokinetics of 4-hydroxycyclophosphamide was observed. Administration of thioTEPA 1 h prior to cyclophosphamide resulted in decreased Cmax (-62%) and AUC (-26%) values of 4-hydroxycyclophosphamide compared to those of thioTEPA administered 1 h after cyclophosphamide. In human microsomes an inhibition of the conversion of cyclophosphamide to 4-hydroxycyclophosphamide by thioTEPA was observed at clinically relevant concentrations with an IC50 of 23 microM. No inhibition of the formation of TEPA by cyclophosphamide was observed., Conclusions: ThioTEPA strongly inhibits the bioactivation of cyclophosphamide and this may decrease both efficacy and toxicity. Our results seriously question the practice of the simultaneous continuous infusion of cyclophosphamide and thioTEPA and suggest that the sequencing and scheduling of these two agents in high-dose chemotherapy regimens may be of critical importance.

Published
2000
Full Text
View/download PDF

46. Degradation of azaglycinamido residues in model tripeptides derived from goserelin.

Author

Hoitink MA, Beijnen JH, Bult A, Damen JM, van der Houwen OA, Kruijtzer JA, Tibben MM, Wiese G, and Underberg WJ

Subjects
Antineoplastic Agents, Hormonal chemistry, Buffers, Chromatography, High Pressure Liquid methods, Hydrazines chemistry, Hydrogen-Ion Concentration, Kinetics, Mass Spectrometry, Nuclear Magnetic Resonance, Biomolecular, Protein Denaturation, Thermodynamics, Goserelin chemistry, Oligopeptides chemistry, Peptide Fragments chemistry
Abstract

Three model tripeptides, N-acetyl-Tyr-Pro-azaGly-NH(2) (NYPaG), Tyr-Pro-azaGly-NH(2) (YPaG), and Tyr-Pro-Gly-NH(2)(YPG), were subjected to a systematic degradation study to get information about the degradation of the azaglycinamido residue. The degradation products were characterized with LC-MS. Main degradation products of NYPaG possess partially or totally eliminated azaglycinamido residues, while YPaG and YPG are exhibit cyclo(Tyr-Pro) formation, a diketopiperazine. The influence of the pH on the degradation rate constant k(obs) was investigated for NYPaG and YPaG in the pH range 0.4-11. An U-shaped profile with an inflexion around pH 9 was found for NYPaG while the degradation rate of YPaG was independent of the pH. NYPaG apparently was subject to proton-, solvent-, and hydroxyl-catalyzed degradation reactions whereas YPaG only underwent solvent-catalyzed reactions. Some influence of acetate and phosphate ions on k(obs) was found for YPaG. Arrhenius plots of NYPaG and YPaG were found to be linear., (Copyright 2000 Wiley-Liss, Inc. and the American Pharmaceutical Association J Pharm Sci 89: 108-114, 2000)

Published
2000
Full Text
View/download PDF

47. Sampling technique from central venous catheters proves critical for pharmacokinetic studies.

Author

Huitema AD, Holtkamp M, Tibben MM, Rodenhuis S, and Beijnen JH

Subjects
Cyclophosphamide pharmacokinetics, Evaluation Studies as Topic, Humans, Catheterization, Central Venous, Pharmacokinetics, Sampling Studies
Abstract

Double-lumen central venous access (CVA) catheters are occasionally used in pharmacokinetic studies for drug administration and blood sampling. The samples are often collected by the nursing staff and thus the investigator may not be aware of the specific sampling technique used. We present an example of the dramatic effect that an incorrect sampling technique from double-lumen CVA catheters can have on pharmacokinetic outcomes. Using a double-lumen Hickman catheter (PolyCath Central Venous Catheter; Strato Medical Corporation/Infusaid Inc., Manchester, GA, U.S.A.), sampling during the infusion can be performed when the infusion is connected to the lumen with the end most downstream and blood is collected from the proximal opening. With a normal double-lumen catheter, sampling can only be performed by briefly interrupting the infusion or after the infusion.

Published
1999
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results