Your search keyword '"Mathijssen, RHJ"' showing total 275 results

1. Darolutamide does not interfere with OATP-mediated uptake of docetaxel

Author

Buck, SAJ, Talebi, Z, Drabison, T, Jin, Y, Gibson, AA, Hu, P, de Bruijn, P, de Ridder, CMA, Stuurman, D, Hu, SY, van Weerden, WM, Koolen, SLW, de Wit, R, Sparreboom, A, Mathijssen, RHJ, Eisenmann, ED, Buck, SAJ, Talebi, Z, Drabison, T, Jin, Y, Gibson, AA, Hu, P, de Bruijn, P, de Ridder, CMA, Stuurman, D, Hu, SY, van Weerden, WM, Koolen, SLW, de Wit, R, Sparreboom, A, Mathijssen, RHJ, and Eisenmann, ED

Abstract

The addition of darolutamide, an androgen receptor signalling inhibitor, to therapy with docetaxel has recently been approved as a strategy to treat metastatic prostate cancer. OATP1B3 is an SLC transporter that is highly expressed in prostate cancer and is responsible for the accumulation of substrates, including docetaxel, into tumours. Given that darolutamide inhibits OATP1B3 in vitro, we sought to characterise the impact of darolutamide on docetaxel pharmacokinetics. We investigated the influence of darolutamide on OATP1B3 transport using in vitro and in vivo models. We assessed the impact of darolutamide on the tumour accumulation of docetaxel in a patient-derived xenograft (PDX) model and on an OATP1B biomarker in patients. Darolutamide inhibited OATP1B3 in vitro at concentrations higher than the reported Cmax. Consistent with these findings, in vivo studies revealed that darolutamide does not influence the pharmacokinetics of Oatp1b substrates, including docetaxel. Docetaxel accumulation in PDX tumours was not decreased in the presence of darolutamide. Metastatic prostate cancer patients had similar levels of OATP1B biomarkers, regardless of treatment with darolutamide. Consistent with a low potential to inhibit OATP1B3-mediated transport in vitro, darolutamide does not significantly impede the transport of Oatp1b substrates in vivo or in patients. Our findings support combined treatment with docetaxel and darolutamide, as no OATP1B3 transporter based drug–drug interaction was identified.

Published

2024

2. Tamoxifen Dose De-Escalation:An Effective Strategy for Reducing Adverse Effects?

Author

Buijs, SM, Koolen, SLW, Mathijssen, RHJ, Jager, A, Buijs, SM, Koolen, SLW, Mathijssen, RHJ, and Jager, A

Abstract

Tamoxifen, a cornerstone in the adjuvant treatment of estrogen receptor-positive breast cancer, significantly reduces breast cancer recurrence and breast cancer mortality; however, its standard adjuvant dose of 20 mg daily presents challenges due to a broad spectrum of adverse effects, contributing to high discontinuation rates. Dose reductions of tamoxifen might be an option to reduce treatment-related toxicity, but large randomized controlled trials investigating the tolerability and, more importantly, efficacy of low-dose tamoxifen in the adjuvant setting are lacking. We conducted an extensive literature search to explore evidence on the tolerability and clinical efficacy of reduced doses of tamoxifen. In this review, we discuss two important topics regarding low-dose tamoxifen: (1) the incidence of adverse effects and quality of life among women using low-dose tamoxifen; and (2) the clinical efficacy of low-dose tamoxifen examined in the preventive setting and evaluated through the measurement of several efficacy derivatives. Moreover, practical tools for tamoxifen dose reductions in the adjuvant setting are provided and further research to establish optimal dosing strategies for individual patients are discussed.

Published

2024

3. Recent Clinical Developments of Nanomediated Drug Delivery Systems of Taxanes for the Treatment of Cancer

Author

van Eerden RAG, Mathijssen RHJ, and Koolen SLW

Subjects

nanomedicine, nanoparticle, drug delivery systems, taxane, cancer, Medicine (General), R5-920

Abstract

Ruben AG van Eerden,1 Ron HJ Mathijssen,1 Stijn LW Koolen1,2 1Department of Medical Oncology, Erasmus MC Cancer Institute, Rotterdam, the Netherlands; 2Department of Hospital Pharmacy, Erasmus MC University Medical Center, Rotterdam, the NetherlandsCorrespondence: Ruben AG van EerdenDepartment of Medical Oncology, Erasmus MC Cancer Institute, Erasmus University Medical Center, PO Box 2040, Rotterdam 3000 CA, the NetherlandsTel +31 10 7039640Email r.vaneerden@erasmusmc.nlAbstract: Conventional taxanes are used as cornerstone of the chemotherapeutical treatment for a variety of malignancies. Nevertheless, a large proportion of patients do not benefit from their treatment while they do suffer from severe adverse events related to the solvent or to the active compound. Cremophor EL and polysorbate 80 free formulations, conjugates, oral formulations and different types of drug delivery systems are some examples of the several attempts to improve the treatment with taxanes. In this review article, we discuss recent clinical developments of nanomediated drug delivery systems of taxanes for the treatment of cancer. Targeting mechanisms of drug delivery systems and characteristics of the most commonly used taxane-containing drug delivery systems in the clinical setting will be discussed in this review.Keywords: nanomedicine, nanoparticle, drug delivery systems, taxane, cancer

Published

2020

4. Differential transport of platinum compounds by the human organic cation transporter hOCT2 (hSLC22A2)

Author

Burger, H, Zoumaro-Djayoon, A, Boersma, AWM, Helleman, J, Berns, EMJJ, Mathijssen, RHJ, Loos, WJ, and Wiemer, EAC

Published

2010

5. Influence of OATP1B1 Function on the Disposition of Sorafenib‐β‐D‐Glucuronide

Author

Bins, S, van Doorn, L, Phelps, MA, Gibson, AA, Hu, S, Li, L, Vasilyeva, A, Du, G, Hamberg, P, Eskens, FALM, de Bruijn, P, Sparreboom, A, Mathijssen, RHJ, and Baker, SD

Subjects

Liver, Research, Articles, Sorafenib, Article, Cell Line

Abstract

The oral multikinase inhibitor sorafenib undergoes extensive UGT1A9‐mediated formation of sorafenib‐β‐D‐glucuronide (SG). Using transporter‐deficient mouse models, it was previously established that SG can be extruded into bile by ABCC2 or follow a liver‐to‐blood shuttling loop via ABCC3‐mediated efflux into the systemic circulation, and subsequent uptake in neighboring hepatocytes by OATP1B‐type transporters. Here we evaluated the possibility that this unusual process, called hepatocyte hopping, is also operational in humans and can be modulated through pharmacological inhibition. We found that SG transport by OATP1B1 or murine Oatp1b2 was effectively inhibited by rifampin, and that this agent can significantly increase plasma levels of SG in wildtype mice, but not in Oatp1b2‐deficient animals. In human subjects receiving sorafenib, rifampin acutely increased the systemic exposure to SG. Our study emphasizes the need to consider hepatic handling of xenobiotic glucuronides in the design of drug–drug interaction studies of agents that undergo extensive phase II conjugation.

Published

2017

6. Pharmacometric Modeling of Liver Metastases' Diameter, Volume, and Density and Their Relation to Clinical Outcome in Imatinib-Treated Patients With Gastrointestinal Stromal Tumors

Author

Schindler, E, Krishnan, SM, Mathijssen, RHJ, Ruggiero, A, Schiavon, G, Friberg, LE, and Medical Oncology

Subjects

Adult, Aged, 80 and over, Male, Gastrointestinal Stromal Tumors, Liver Neoplasms, Antineoplastic Agents, Original Articles, Kaplan-Meier Estimate, Middle Aged, Farmaceutiska vetenskaper, Models, Biological, Disease-Free Survival, Tumor Burden, Pharmaceutical Sciences, Treatment Outcome, Imatinib Mesylate, Humans, Original Article, Female, Tomography, X-Ray Computed, Protein Kinase Inhibitors, Aged

Abstract

Three‐dimensional and density‐based tumor metrics have been suggested to better discriminate tumor response to treatment than unidimensional metrics, particularly for tumors exhibiting nonuniform size changes. In the developed pharmacometric modeling framework based on data from 77 imatinib‐treated gastrointestinal patients, the time‐courses of liver metastases' maximum transaxial diameters, software‐calculated actual volumes (Vactual) and calculated ellipsoidal volumes were characterized by logistic growth models, in which imatinib induced a linear dose‐dependent size reduction. An indirect response model best described the reduction in density. Substantial interindividual variability in the drug effect of all response assessments and additional interlesion variability in the drug effect on density were identified. The predictive ability of longitudinal tumor unidimensional and three‐dimensional size and density on overall survival (OS) and progression‐free survival (PFS) were compared using parametric time‐to‐event models. Death hazard increased with increasing Vactual. This framework may guide early clinical interventions based on three‐dimensional tumor responses to enhance benefits for patients with gastrointestinal stromal tumors (GIST).

Published

2017

7. Emphasizing the Value of Phenotyping in Patients Receiving Tamoxifen Reply

Author

Graan, Anne-joy, Binkhorst, Lisette, Loos, Walter, van Schaik, Ron, Verweij, Jaap, Mathijssen, RHJ, Medical Oncology, Pharmacy, and Clinical Chemistry

Published

2012

8. Influence of polyfarmacy and age on the systemic exposure to chemotherapy

Author

de Jonge, Maja, Mathijssen, RHJ, Loos, Walter, Wymenga, A.N.M., and Medical Oncology

Published

2011

9. De behandeling van kanker; wat is de beste dosering?

Author

Mathijssen, RHJ, van Hoogdalem, E.J., Hoogedoonr, K.H., and Medical Oncology

Published

2011

10. Klinische onderzoeksmethodologie in de oncologie

Author

Schellens, JHM, Mathijssen, RHJ, van de Velde, C.J.H., and Medical Oncology

Published

2011

11. What's the correct dosing-strategy.....in particular in the obese patient?

Author

Mathijssen, RHJ, Verweij, Jaap, and Medical Oncology

Published

2008

12. ABCG2 pharmacogenetics: ethnic differences in allele frequency and assessment of influence on irinotecan disposition

Author

de Jong, FA (Floris), Marsh, S, Mathijssen, RHJ, King, C, Verweij, Jaap, Sparreboom, A, McLeod, HL, and Medical Oncology

Subjects

SDG 3 - Good Health and Well-being

Abstract

PURPOSE: The ATP-binding cassette transporter ABCG2 (breast cancer resistance protein) is an efflux protein that plays a role in host detoxification of various xenobiotic substrates, including the irinotecan metabolite 7- ethyl-10-hydroxycamptothecin (SN-38). The ABCG2 421C>A polymorphism has been associated with reduced protein expression and altered function in vitro. The aim of this study was to evaluate the ethnic distribution and potential functional consequence of the ABCG2 421C>A genotype in cancer patients treated with irinotecan. EXPERIMENTAL DESIGN: ABCG2 genotyping was performed using Pyrosequencing on DNA from 88 American Caucasians, 94 African Americans, 938 Africans, and 95 Han Chinese, as well as in 84 European Caucasian patients treated with irinotecan undergoing additional blood sampling for pharmacokinetic studies. RESULTS: Significant differences in allele frequencies were observed between the given world populations (P < 0.001), the variant allele being most common in the Han Chinese population with a frequency as high as 34%. The mean area under the curve of irinotecan and SN-38 were 19,851 and 639 ng x hour/mL, respectively. The frequency of the variant allele (10.7%) was in line with results in American Caucasians. No significant changes in irinotecan pharmacokinetics were observed in relation to the ABCG2 421C>A genotype, although one of two homozygous variant allele carriers showed extensive accumulation of SN-38 and SN-38 glucuronide. CONCLUSIONS: The ABCG2 421C>A polymorphism appears to play a limited role in the disposition of irinotecan in European Caucasians. It is likely that the contribution of this genetic variant is obscured by a functional role of other polymorphic proteins.

Published

2004

13. Flat-fixed dosing of irinotecan: influence on pharmacokinetic and pharmacodynamic variability

Author

de Jong, FA (Floris), Mathijssen, RHJ, Xie, R, Verweij, Jaap, Sparreboom, A, and Medical Oncology

Subjects

SDG 3 - Good Health and Well-being

Abstract

PURPOSE: In a previous analysis, it was shown that body-surface area (BSA) is not a predictor of irinotecan pharmacokinetic parameters. Here, we prospectively evaluated the effects of administering a flat-fixed irinotecan dose to cancer patients, regardless of BSA. EXPERIMENTAL DESIGN: Twenty-six cancer patients (12 females) received a fixed irinotecan dose of 600 mg, given as a 90-min i.v. infusion. Plasma concentrations of irinotecan and its metabolites SN-38 (7-ethyl-10-hydroxycamptothecin) and SN-38G (SN-38 glucuronide) were measured during the first cycle and analyzed using nonlinear mixed-effect modeling. Data were compared with those obtained in 47 cancer patients (19 females) who received irinotecan at a BSA-normalized dose of 350 mg/m(2). RESULTS: The interindividual variability in irinotecan clearance (25.9% versus 25.1%; P = 0.93), in relative extent of conversion to SN-38 (47.8% versus 42.7%; P = 0.24), and in relative extent of SN-38 glucuronidation (71.2% versus 72.4%; P = 0.95) were not significantly different between the two dose groups. Variance differences in irinotecan-mediated hematological side effects were also similar between the 600 mg and 350 mg/m(2) groups (P > 0.14). CONCLUSIONS: These findings suggest that flat-fixed dosing of irinotecan does not result in increased pharmacokinetic/pharmacodynamic variability and could be safely used to supplant current dosing strategies based on BSA.

Published

2004

14. Mechanism-based models for topotecan-induced neutropenia

Author

Léger, F, Loos, Walter, Bugat, R, Mathijssen, RHJ, Goffinet, M, Verweij, Jaap, Sparreboom, A, Chatelut, E, and Medical Oncology

Published

2004

15. MiR-17-92 and miR-221/222 cluster members target KIT and ETV1 in human gastrointestinal stromal tumours

Author

Gits, Caroline, van Kuijk, Patricia, Jonkers, Moniek, Boersma, Ton, van Ijcken, Wilfred, Wozniak, A, Sciot, R, Rutkowski, P, Schoffski, P, Taguchi, T, Mathijssen, RHJ, Verweij, Jaap, Sleijfer, Stefan, Debiec-Rychter, M, Wiemer, Erik, Gits, Caroline, van Kuijk, Patricia, Jonkers, Moniek, Boersma, Ton, van Ijcken, Wilfred, Wozniak, A, Sciot, R, Rutkowski, P, Schoffski, P, Taguchi, T, Mathijssen, RHJ, Verweij, Jaap, Sleijfer, Stefan, Debiec-Rychter, M, and Wiemer, Erik

Abstract

BACKGROUND: Gastrointestinal stromal tumours (GIST) are characterised by high expression of KIT and ETV1, which cooperate in GIST oncogenesis. Our aim was to identify microRNAs that are deregulated in GIST, have a role in GIST pathogenesis, and could potentially be used as therapeutic tool.METHODS: Differentially expressed microRNAs between primary GIST (n=50) and gastrointestinal leiomyosarcomas (GI-LMS, n=10) were determined using microarrays. Selected microRNA mimics were transfected into GIST-882 and GIST-T1 cell lines to study the effects of microRNA overexpression on GIST cells. Luciferase reporter assays were used to establish regulation of target genes by selected microRNAs.RESULTS: MiR-17-92 and miR-221/222 cluster members were significantly (P<0.01) lower expressed in GIST vs GI-LMS and normal gastrointestinal control tissues. MiR-17/20a/222 overexpression in GIST cell lines severely inhibited cell proliferation, affected cell cycle progression, induced apoptosis and strongly downregulated protein and--to a lesser extent--mRNA levels of their predicted target genes KIT and ETV1. Luciferase reporter assays confirmed direct regulation of KIT and ETV1 by miR-222 and miR-17/20a, respectively.CONCLUSION: MicroRNAs that may have an essential role in GIST pathogenesis were identified, in particular miR-17/20a/222 that target KIT and ETV1. Delivering these microRNAs therapeutically could hold great potential for GIST management, especially in imatinib-resistant disease.

Published

2013

16. Irinotecan: From pharmacokinetics to pharmacogenetics

Author

Mathijssen, RHJ, Verweij, Jaap, and Medical Oncology

Published

2002

17. Clinical pharmacokinetics and metabolism of Irinotecan (CPT-11)

Author

Mathijssen, RHJ, van Alphen, RJ, Verweij, Jaap, Loos, Walter, Nooter, K (Kees), Stoter, Gerrit, Sparreboom, A, and Medical Oncology

Published

2001

18. Pharmacological and clinical aspects of immediate release fentanyl preparations: criteria for selection

Author

Kuip, Evelien, Zandvliet, Maarten, Mathijssen, RHJ, van der Rijt, Karin, Kuip, Evelien, Zandvliet, Maarten, Mathijssen, RHJ, and van der Rijt, Karin

Abstract

In palliative care, pain management is often hampered by episodes of breakthrough pain, characterised by a rapid onset and, on average, duration less than 1 h. Until recently, only immediate release morphine and oxycodon preparations were available for the treatment of these episodes but time until effect is too long for both of these drugs. Recently, immediate release fentanyl products have become available for the treatment of breakthrough pain. These products can be classified as oromucosal and nasal products. Both are absorbed rapidly by the mucosa, although the oromucosally delivered products are partly absorbed by the gastrointestinal tract and therefore reach maximum plasma levels somewhat slower (after 30-90 min) than the nasally delivered products (after similar to 15 min). In clinical placebo controlled studies, all new immediate release fentanyl products were proven to be effective from 15 min after administration in the treatment of breakthrough pain. The first studies comparing immediate release fentanyl with immediate release morphine or oxycodon also found superiority for the new fentanyl products.

Published

2012

19. Effects of methimazole on the elimination of irinotecan

Author

Bol, Jessica, Visser, Theo, Loos, Walter, de Jong, FA (Floris), Wiemer, Erik, van Aken, MO, Planting, AST, Schellens, JH, Verweij, Jaap, Mathijssen, RHJ, Bol, Jessica, Visser, Theo, Loos, Walter, de Jong, FA (Floris), Wiemer, Erik, van Aken, MO, Planting, AST, Schellens, JH, Verweij, Jaap, and Mathijssen, RHJ

Abstract

PURPOSE: To study the possible pharmacokinetic and pharmacodynamic interactions between irinotecan and methimazole.METHODS: A patient treated for colorectal cancer with single agent irinotecan received methimazole co-medication for Graves' disease. Irinotecan pharmacokinetics and side effects were followed during a total of four courses (two courses with and two courses without methimazole).RESULTS: Plasma concentrations of the active irinotecan metabolite SN-38 and its inactive metabolite SN-38-Glucuronide were both higher (a mean increase of 14 and 67%, respectively) with methimazole co-medication, compared to irinotecan monotherapy. As a result, the mean SN-38 glucuronidation rate increased with 47% during concurrent treatment. Other possible confounding factors did not change over time. Specific adverse events due to methimazole co-treatment were not seen.CONCLUSIONS: Additional in vitro experiments suggest that these results can be explained by induction of UGT1A1 by methimazole, leading to higher SN-38G concentrations. The prescribed combination of these drugs may lead to highly toxic intestinal SN-38 levels. We therefore advise physicians to be very careful in combining methimazole with regular irinotecan doses, especially in patients who are prone to irinotecan toxicity.

Published

2011

20. Increasing tumoral 5-fluorouracil concentrations during a 5-day continuous infusion:a microdialysis study

Author

Konings, IRHM, Sleijfer, Stefan, Mathijssen, RHJ, de Bruijn, Peter, Helmantel, Inge, Dam, Linda, Wiemer, Erik, Verweij, Jaap, Loos, Walter, Konings, IRHM, Sleijfer, Stefan, Mathijssen, RHJ, de Bruijn, Peter, Helmantel, Inge, Dam, Linda, Wiemer, Erik, Verweij, Jaap, and Loos, Walter

Abstract

PURPOSE: Response to anticancer therapy is believed to be directly related to the concentration of the anticancer drug in the tumor itself. Assessment of intra-tumor drug pharmacokinetics can be helpful to gain more insight into mechanisms involved in the (in)sensitivity of tumors to anticancer therapy. We explored the pharmacokinetics of 5-fluorouracil in both plasma and tumor tissue during a 5-day continuous infusion of 5-fluorouracil in patients with cancer. Sampling for measurement of 5-fluorouracil in tumor tissue was performed using microdialysis.EXPERIMENTAL DESIGN: In seven patients with an accessible (sub)cutaneous tumor treated with a continuous 5-fluorouracil infusion, plasma and microdialysate samples from tumor and normal adipose tissue were collected over a period of 5 days.RESULTS: For six patients, drug concentrations in both tumor tissue and plasma were available. Concentration-time curves of unbound 5-fluorouracil were lower in tumor tissue compared to the curves in plasma, but exposure ratios of tumor tissue versus plasma increased during the 5-day infusion period. The presence of circadian rhythmicity of 5-fluorouracil pharmacokinetics in the tumor itself was demonstrated as 5-fluorouracil concentrations in tumor extracellular fluid were higher during the night than during daytime.CONCLUSION: Microdialysis was successfully employed in patients with cancer during a continuous 5-day 5-fluorouracil infusion. Plasma and tumor pharmacokinetics of 5-fluorouracil differed substantially with increasing 5-fluorouracil concentrations in tumor over time, possibly resulting from a lowered interstitial fluid pressure by 5-fluorouracil itself. This microdialysis 5-fluorouracil model might be useful to monitor the effect of drug delivery modulating strategies in future studies.

Published

2011

21. Effects of mannose-binding lectin polymorphisms on irinotecan-induced febrile neutropenia

Author

Bol, Jessica, de Jong, FA (Floris), van Schaik, Ron, Sparreboom, A, Fessem, Mariane, Geijn, Fleur, van Daele, Paul, Verweij, Jaap, Sleijfer, Stefan, Mathijssen, RHJ, Bol, Jessica, de Jong, FA (Floris), van Schaik, Ron, Sparreboom, A, Fessem, Mariane, Geijn, Fleur, van Daele, Paul, Verweij, Jaap, Sleijfer, Stefan, and Mathijssen, RHJ

Abstract

OBJECTIVE: Mannose-binding lectin (MBL) is important in the innate immune response. MBL2 gene polymorphisms affect MBL expression, and genotypes yielding low MBL levels have been associated with an elevated risk for infections in hematological cancer patients undergoing chemotherapy. However, these reported associations are inconsistent, and data on patients with solid tumors are lacking. Here, we investigated the effects of MBL2 genotypes on irinotecan-induced febrile neutropenia in patients with solid tumors.PATIENTS AND METHODS: Irinotecan-treated patients were genotyped for the MBL2 gene. Two promoter (-550 H/L and -221 X/Y) and three exon polymorphisms (52 A/D, 54 A/B, and 57 A/C) were determined, together with known risk factors for irinotecan-induced toxicity. Neutropenia and febrile neutropenia were recorded during the first course.RESULTS: Of the 133 patients, 28% experienced severe neutropenia and 10% experienced febrile neutropenia. No associations were found between exon polymorphisms and febrile neutropenia. However, patients with the H/H promoter genotype, associated with high MBL levels, experienced significantly more febrile neutropenia than patients with the H/L and L/L genotypes (20% versus 13% versus 5%). Moreover, patients with the HYA haplotype encountered significantly more febrile neutropenia than patients without this high MBL-producing haplotype (16% versus 4%). In the subgroup with wild-type exon polymorphisms (A/A), patients with the high MBL promoter phenotype had the highest incidence of febrile neutropenia, regardless of known risk factors.CONCLUSION: Patients with high MBL2 promoter genotypes and haplotypes seem more at risk for developing febrile neutropenia. If confirmed, these preliminary findings may contribute to more individualized approaches of irinotecan treatment.

Published

2010

22. Irinotecan (CPT-11) metabolism and disposition in cancer patients

Author

Sparreboom, A, de Jonge, Maja, de Bruijn, Peter, Brouwer, E, Nooter, K (Kees), Loos, Walter, van Alphen, RJ, Mathijssen, RHJ, Stoter, Gerrit, Verweij, Jaap, and Medical Oncology

Subjects

SDG 3 - Good Health and Well-being

Published

1998

23. Flat-fixed dosing versus body surface area based dosing of anticancer drugs in adults:does it make a difference?

Author

Mathijssen, RHJ, de Jong, FA (Floris), Loos, Walter, Bol, Jessica, Verweij, Jaap, Sparreboom, A, Mathijssen, RHJ, de Jong, FA (Floris), Loos, Walter, Bol, Jessica, Verweij, Jaap, and Sparreboom, A

Abstract

The current practice of using body-surface area (BSA) in dosing anticancer agents was implemented in clinical oncology half a century ago. By correcting for BSA, it was generally assumed that cancer patients would receive a dose of a particular cytotoxic drug associated with an acceptable degree of toxicities without reducing the agent's therapeutic effect. More recently, doubt has arisen to this hypothesis, and for many drugs, the effects of BSA on the pharmacokinetics of these agents have therefore been studied retrospectively. In (by far) most cases, use of BSA does not reduce the interindividual variation in the pharmacokinetics of adults, and thus, a logical rationale for further use of this tool in dosing adults is lacking. As a result, alternative dosing strategies have been proposed in order to replace BSA-based dosing. Flat-fixed dosing regimens have been suggested, thereby avoiding potential dose calculation mistakes. As flat-fixed dosing does not typically lead to greater pharmacokinetic variability, it does not seem worse than using BSA-based dosing. While it provides a simplification, it can, however, be questioned whether to call this an improvement or not. The implementation of so-called genotyping and phenotyping strategies, and therapeutic drug monitoring, may probably be of more clinical value. In the end, the nonscientifically based BSA-based dosing strategy should be replaced by alternative strategies. Despite the lack of basic fundamentals, BSA-based dosing still seems "untouchable" in clinical oncology. Even when alternatives will be shown to be indisputably better, many hurdles will probably have to be overcome before physicians will be willing to ban BSA-based dosing. Disclosure of potential conflicts of interest is found at the end of this article.

Published

2007

24. Medicinal cannabis does not influence the clinical pharmacokinetics of irinotecan and docetaxel

Author

Engels, Frederike, de Jong, FA (Floris), Sparreboom, A, Mathot, RAA, Loos, Walter, Kitzen, JJEM (Jos), de Bruijn, Peter, Verweij, Jaap, Mathijssen, RHJ, Engels, Frederike, de Jong, FA (Floris), Sparreboom, A, Mathot, RAA, Loos, Walter, Kitzen, JJEM (Jos), de Bruijn, Peter, Verweij, Jaap, and Mathijssen, RHJ

Abstract

OBJECTIVE: To date, data regarding the potential of cannabinoids to modulate cytochrome P450 isozyme 3A (CYP3A) activity are contradictory. Recently, a standardized medicinal cannabis product was introduced in The Netherlands. We anticipated an increased use of medicinal cannabis concurrent with anticancer drugs, and undertook a drug-interaction study to evaluate the effect of concomitant medicinal cannabis on the pharmacokinetics of irinotecan and docetaxel, both subject to CYP3A-mediated biotransformation.PATIENTS AND METHODS: Twenty-four cancer patients were treated with i.v. irinotecan (600 mg, n = 12) or docetaxel (180 mg, n = 12), followed 3 weeks later by the same drugs concomitant with medicinal cannabis (200 ml herbal tea, 1 g/l) for 15 consecutive days, starting 12 days before the second treatment. Blood samples were obtained up to 55 hours after dosing and analyzed for irinotecan and its metabolites (SN-38, SN-38G), respectively, or docetaxel. Pharmacokinetic analyses were performed during both treatments. Results are reported as the mean ratio (95% confidence interval [CI]) of the observed pharmacokinetic parameters with and without concomitant medicinal cannabis.RESULTS: Medicinal cannabis administration did not significantly influence exposure to and clearance of irinotecan (1.04; CI, 0.96-1.11 and 0.97; CI, 0.90-1.05, respectively) or docetaxel (1.11; CI, 0.94-1.28 and 0.95; CI, 0.82-1.08, respectively).CONCLUSION: Coadministration of medicinal cannabis, as herbal tea, in cancer patients treated with irinotecan or docetaxel does not significantly influence the plasma pharmacokinetics of these drugs. The evaluated variety of medicinal cannabis can be administered concomitantly with both anticancer agents without dose adjustments.

Published

2007

25. Prophylaxis of irinotecan-induced diarrhea with neomycin and potential role for UGT1A1*28 genotype screening:a double-blind, randomized, placebo-controlled study

Author

de Jong, FA (Floris), Kehrer, DFS, Mathijssen, RHJ, Creemers, GJ, de Bruijn, Peter, van Schaik, Ron, Planting, AST, van der Gaast, Ate, Eskens, Ferry, Janssen, JTP, Ruit, JB, Verweij, Jaap, Sparreboom, A, de Jonge, Maja, de Jong, FA (Floris), Kehrer, DFS, Mathijssen, RHJ, Creemers, GJ, de Bruijn, Peter, van Schaik, Ron, Planting, AST, van der Gaast, Ate, Eskens, Ferry, Janssen, JTP, Ruit, JB, Verweij, Jaap, Sparreboom, A, and de Jonge, Maja

Abstract

OBJECTIVE: Delayed-type diarrhea is a common side effect of irinotecan and is associated with a bacterial-mediated formation of the active irinotecan metabolite SN-38 from its glucuronide conjugate in the intestine. Based on a pilot study, we hypothesized that concomitant administration of the antibiotic neomycin would diminish exposure of the gut to SN-38 and ameliorate the incidence and severity of diarrhea.PATIENTS AND METHODS: Patients were treated with irinotecan in a multicenter, double-blind, randomized, placebo-controlled trial. Eligible patients received irinotecan (350 mg/m(2) once every 3 weeks) combined with neomycin (660 mg three times daily for three consecutive days, starting 2 days before chemotherapy) or combined with placebo. Blood samples were obtained for additional pharmacokinetic and pharmacogenetic analyses.RESULTS: Sixty-two patients were evaluable for the toxicity analysis. Baseline patient characteristics, systemic SN-38 exposure, and UGT1A1*28 genotype status (i.e., an additional TA repeat in the promoter region of uridine diphosphate-glucuronosyltransferase isoform 1A1) were similar in both arms. Although distribution, severity, and duration of delayed-type diarrhea did not differ significantly between arms, grade 3 diarrhea tended to be less frequent in the neomycin arm. The presence of at least one UGT1A1*28 allele was strongly related to the incidence of grade 2-3 diarrhea. In the neomycin arm, grade 2 nausea was significantly more common.CONCLUSION: Our results do not suggest a major role for neomycin as prophylaxis for irinotecan-induced delayed-type diarrhea. It is suggested that the UGT1A1*28 genotype status could be used as a screening tool for a priori prevention of irinotecan-induced delayed-type diarrhea.

Published

2006

26. Complementary and alternative medicine during cancer treatment:beyond innocence

Author

Tascilar, M (Metin), de Jong, FA (Floris), Verweij, Jaap, Mathijssen, RHJ, Tascilar, M (Metin), de Jong, FA (Floris), Verweij, Jaap, and Mathijssen, RHJ

Abstract

Nowadays, complementary and alternative medicine (CAM) is popular all over the world. Billions of dollars are spent in this booming business. For several reasons, young, female, educated, and higher socioeconomic class cancer patients, in particular, have shown interest in these agents. Unfortunately, besides direct (and sometimes serious) side effects, several CAM ingredients are capable of interfering with the metabolism of concurrently used drugs, which may render the therapeutic outcome of the subscribed drug unpredictable. In the case of anticancer drugs, with their usually narrow therapeutic window, this may have dramatic consequences and can lead to unacceptable toxicities in some cases or decreased therapeutic activity in others. Therefore, cancer patients should be warned for these possible interactions and be advised to discuss CAM use openly with their treating physician. The general concept that natural products are harmless should thus be changed into a more realistic and responsible attitude. A tightened legislation and regulation (including Internet advertising and sales) could play a crucial role in this awareness process. This should finally enable safe exploration of the potential advantageous aspects of CAM, while living with cancer.

Published

2006

27. Effects of St. John's wort on irinotecan metabolism

Author

Mathijssen, RHJ, Verweij, Jaap, de Bruijn, Peter, Loos, Walter, Sparreboom, A, Mathijssen, RHJ, Verweij, Jaap, de Bruijn, Peter, Loos, Walter, and Sparreboom, A

Published

2002

28. Impact of body-size measures on irinotecan clearance:alternative dosing recommendations

Author

Mathijssen, RHJ, Verweij, Jaap, de Jonge, Maja, Nooter, K (Kees), Stoter, Gerrit, Sparreboom, A, Mathijssen, RHJ, Verweij, Jaap, de Jonge, Maja, Nooter, K (Kees), Stoter, Gerrit, and Sparreboom, A

Abstract

PURPOSE: To evaluate relationships between various body-size measures and irinotecan (CPT-11) clearance and metabolism in cancer patients, and to provide future dosing recommendations for this agent.PATIENTS AND METHODS: Pharmacokinetic data were obtained from 82 adult patients (50 men, 32 women; median age, 54 years) receiving CPT-11 as a 90-minute intravenous infusion (dose range, 175 to 350 mg/m(2)). In each patient, plasma samples were collected at timed intervals in the first administration of a 3-week schedule, and CPT-11 and its metabolite, SN-38, were measured by a liquid chromatographic assay.RESULTS: The mean (+/- SD) CPT-11 clearance was 33.6 +/- 10.8 L/h, with an interindividual variability (IIV) of 32.1%. When clearance was adjusted for body-surface area (BSA), the IIV was similar (34.0%). In addition, in a multiple linear regression analysis, none of the studied measures (BSA, lean body mass, [adjusted] ideal body weight, and body mass index) was a significant covariate (P >.13; r(2) <.014) in our population. Similarly, BSA did not significantly contribute to variability in the relative extent of conversion to SN-38 (P =.26).CONCLUSION: BSA is not a predictor of CPT-11 clearance or SN-38 pharmacokinetics and does not contribute to reducing kinetic variability. These findings provide a rationale for the conduct of a comparative phase III study between BSA-based dosing and flat or fixed dosing of CPT-11.

Published

2002

29. Influence of Lean Body Weight on Anticancer Drug Clearance

Author

Mathijssen, RHJ, primary and Sparreboom, A, additional

Published

2008

30. Renal Function as a Predictor of Irinotecan-induced Neutropenia

Author

de Jong, FA, primary, van der Bol, JM, additional, Mathijssen, RHJ, additional, van Gelder, T, additional, Wiemer, EAC, additional, Sparreboom, A, additional, and Verweij, J, additional

Published

2008

31. Interchangeability of immune checkpoint inhibitors: an urgent need for action.

Author

Zietse M, van Leeuwen RWF, Barjesteh van Waalwijk van Doorn-Khosrovani S, de Boer JE, Dupree R, Mathijssen RHJ, and Timmers L

Subjects

Humans, Neoplasms drug therapy, Neoplasms immunology, Programmed Cell Death 1 Receptor antagonists & inhibitors, B7-H1 Antigen antagonists & inhibitors, Drug Costs, Immune Checkpoint Inhibitors therapeutic use, Immune Checkpoint Inhibitors adverse effects

Abstract

Prevailing uncertainties regarding the therapeutic interchangeability of PD-1 and PD-L1 inhibitors affect both clinical decision making and health-care budgeting. This Personal View presents a comprehensive assessment of the fragmented regulatory landscape of PD-1 and PD-L1 inhibitors, highlighting the complex dynamics of market competition, pricing, and the effect on health-care budgets. Our paper explores the current state of clinical trials, uninformative trial designs, and the challenges they pose in evaluating the therapeutic interchangeability of these drugs. To address these challenges, research that will inform us of the extent of interchangeability of PD-1 and PD-L1 inhibitors is needed. We recommend head-to-head randomised controlled trials, standardised study designs for indirect comparisons, trials with monotherapy groups, post-approval trials funded from private or public sources, and adoption of a near-equivalence framework in both conducting and evaluating trials., Competing Interests: Declaration of interests RWFvL reports research grants (all paid to their institution) from Bristol Myers Squibb and Pfizer; received consulting fees from Bristol Myers Squibb, Roche, Pierre Fabre, AstraZeneca, and Pfizer; received speaker fees from AstraZeneca; and declares travel support from Ipsen, all outside the submitted work. SBvWvD-K reports a research grant (paid to their institution) for PRIME-ROSE (grant number 101104269); and received travel support from the European Medicines Agency, Nordic Precision Medicine Forum, Centre for Innovation in Regulatory Science, and Cancer Drug Development Forum, all outside the submitted work. RHJM reports unrestricted research grants (all paid to their institution) from Astellas, Bayer, Boehringer ngelheim, Cristal Therapeutics, Deuter Oncology, Novartis, Nordic Pharma, Pamgene, Pfizer, Roche, Sanofi, and Servier, all outside the submitted work. All other authors declare no competing interests., (Copyright © 2024 Elsevier Ltd. All rights reserved, including those for text and data mining, AI training, and similar technologies.)

Published

2024

32. Levels of circulating tumor DNA correlate with tumor volume in gastro-intestinal stromal tumors: an exploratory long-term follow-up study.

Author

Bleckman RF, Haag CMSC, Rifaela N, Beukema G, Mathijssen RHJ, Steeghs N, Gelderblom H, Desar IME, Cleven A, Ter Elst A, Schuuring E, and Reyners AKL

Subjects

Humans, Female, Male, Follow-Up Studies, Middle Aged, Aged, Gastrointestinal Neoplasms pathology, Gastrointestinal Neoplasms blood, Gastrointestinal Neoplasms genetics, Gastrointestinal Neoplasms drug therapy, Gastrointestinal Neoplasms diagnostic imaging, Gastrointestinal Stromal Tumors pathology, Gastrointestinal Stromal Tumors blood, Gastrointestinal Stromal Tumors genetics, Gastrointestinal Stromal Tumors diagnostic imaging, Gastrointestinal Stromal Tumors drug therapy, Circulating Tumor DNA blood, Circulating Tumor DNA genetics, Tumor Burden, Proto-Oncogene Mas

Abstract

Patients with gastro-intestinal stromal tumors (GISTs) undergoing tyrosine kinase inhibitor therapy are monitored with regular computed tomography (CT) scans, exposing patients to cumulative radiation. This exploratory study aimed to evaluate circulating tumor DNA (ctDNA) testing to monitor treatment response and compare changes in ctDNA levels with RECIST 1.1 and total tumor volume measurements. Between 2014 and 2021, six patients with KIT proto-oncogene, receptor tyrosine kinase (KIT) exon-11-mutated GIST from whom long-term plasma samples were collected prospectively were included in the study. ctDNA levels of relevant plasma samples were determined using the KIT exon 11 digital droplet PCR drop-off assay. Tumor volume measurements were performed using a semi-automated approach. In total, 94 of 130 clinically relevant ctDNA samples were analyzed. Upon successful treatment response, ctDNA became undetectable in all patients. At progressive disease, ctDNA was detectable in five out of six patients. Higher levels of ctDNA correlated with larger tumor volumes. Undetectable ctDNA at the time of progressive disease on imaging was consistent with lower tumor volumes compared to those with detectable ctDNA. In summary, ctDNA levels seem to correlate with total tumor volume at the time of progressive disease. Our exploratory study shows promise for including ctDNA testing in treatment follow-up., (© 2024 The Authors. Molecular Oncology published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.)

Published

2024

33. Selecting the Best Pharmacokinetic Models for a Priori Model-Informed Precision Dosing with Model Ensembling.

Author

Agema BC, Kocher T, Öztürk AB, Giraud EL, van Erp NP, de Winter BCM, Mathijssen RHJ, Koolen SLW, Koch BCP, and Sassen SDT

Subjects

Humans, Female, Male, Middle Aged, Adult, Aged, Anti-Bacterial Agents pharmacokinetics, Anti-Bacterial Agents administration & dosage, Dose-Response Relationship, Drug, Precision Medicine methods, Models, Biological, Vancomycin pharmacokinetics, Vancomycin administration & dosage, Imatinib Mesylate pharmacokinetics, Imatinib Mesylate administration & dosage, Drug Monitoring methods

Abstract

Background and Objective: When utilizing population pharmacokinetic (popPK) models for a priori dosage individualization, selecting the best model is crucial to obtain adequate doses. We developed and evaluated several model-selection and ensembling methods, using external evaluation on the basis of therapeutic drug monitoring (TDM) samples to identify the best (set of) models per patient for a priori dosage individualization., Methods: PK data and models describing both hospitalized patients (n = 134) receiving continuous vancomycin (26 models) and patients (n = 92) receiving imatinib in an outpatient setting (12 models) are included. Target attainment of four model-selection methods was compared with standard dosing: the best model based on external validation, uninformed model ensembling, model ensembling using a weighting scheme on the basis of covariate-stratified external evaluation, and model selection using covariates in decision trees that were subsequently ensembled., Results: Overall, the use of PK models improved the proportion of patients exposed to concentrations within the therapeutic window for both cohorts. Relative improvement of proportion on target for best model, unweighted, weighted, and decision trees were - 7.0%, 2.3%, 11.4%, and 37.0% (vancomycin method-development); 23.2%, 7.9%, 15.6%, and, 77.2% (vancomycin validation); 40.7%, 50.0%, 59.5%, and 59.5% (imatinib method-development); and 19.0%, 28.5%, 38.0%, and 23.8% (imatinib validation), respectively., Conclusions: The best (set of) models per patient for a priori dosage individualization can be identified using a relatively small set of TDM samples as external evaluation. Adequately performing popPK models were identified while also excluding poor-performing models. Dose recommendations resulted in more patients within the therapeutic range for both vancomycin and imatinib. Prospective validation is necessary before clinical implementation., (© 2024. The Author(s).)

Published

2024

34. Clinical implications of nintedanib pharmacokinetics in patients with pulmonary fibrosis.

Author

Agema BC, Berrich M, Seuren L, Sassen SDT, Miedema JR, Koch BCP, Wijsenbeek MS, Koolen SLW, Mathijssen RHJ, and Veerman GDM

Subjects

Humans, Male, Female, Aged, Middle Aged, Vital Capacity drug effects, Pulmonary Fibrosis drug therapy, Pulmonary Fibrosis chemically induced, Drug Monitoring methods, Idiopathic Pulmonary Fibrosis drug therapy, Idiopathic Pulmonary Fibrosis physiopathology, Respiratory Function Tests, Dose-Response Relationship, Drug, Protein Kinase Inhibitors pharmacokinetics, Protein Kinase Inhibitors administration & dosage, Protein Kinase Inhibitors adverse effects, Indoles pharmacokinetics, Indoles administration & dosage, Indoles adverse effects

Abstract

Background: Nintedanib is used to treat both idiopathic and progressive pulmonary fibrosis (IPF/PPF). Evidence of both an exposure-response relationship and an exposure-toxicity relationship has been found, suggesting the potential value of therapeutic drug monitoring (TDM). We aimed to define the therapeutic window of nintedanib in a real-world cohort., Methods: Data from two clinical studies were pooled for this analysis. To quantify exposure to nintedanib, a population-pharmacokinetic (PK) model was developed. Associations between PK and decline in forced vital capacity (FVC) and diffusing capacity (DLCO) were performed using linear-mixed-effect models (LMEM). The exposure-toxicity relationship was evaluated using a Cox proportional hazards model., Results: In total, 911 PK samples from 99 patients were used to develop the PK model. The LMEM with random slopes and intercepts included 517 pulmonary function tests (PFT) from 81 patients. The average administered nintedanib dose was associated with the rate of FVC decline (p=0.002). Per 50 mg decrease of daily dosage, the rate of FVC decline increased by 53.5 mL/year. Neither nintedanib exposure nor dose significantly affected DLCO decline and they were also not significantly associated with the occurrence of a dose-limiting toxicity (DLT). This may be explained by a large inter- and intrapatient variability in nintedanib PK., Conclusion: Nintedanib dose was significantly associated with FVC loss. However, no significant relationship between nintedanib exposure and the occurrence of DLTs was found in this real-world population, and no therapeutic window could be established. The findings in this study indicate that nintedanib is an unsuitable candidate for performing TDM., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Masson SAS.. All rights reserved.)

Published

2024

35. Market Entry Agreements for Innovative Pharmaceuticals Subject to Indication Broadening: A Case Study for Pembrolizumab in The Netherlands.

Author

Heine RJSD, Mathijssen RHJ, Verbeek FAJ, Van Gils C, and Uyl-de Groot CA

Subjects

Humans, Netherlands, Drug Costs, Quality of Life, Progression-Free Survival, Antibodies, Monoclonal, Humanized therapeutic use, Antibodies, Monoclonal, Humanized economics, Cost-Benefit Analysis, Quality-Adjusted Life Years, Antineoplastic Agents, Immunological economics, Antineoplastic Agents, Immunological therapeutic use

Abstract

Objectives: Managed entry agreements and especially financial-based agreements are commonly used in European countries for innovative cancer pharmaceuticals. These agreements facilitate access to innovative treatments while mitigating financial risks for payers. This study focuses on the confidential price agreement made by the Dutch government for the reimbursement of pembrolizumab, the implications of broadening indications on cost-effectiveness, and the viability or desirability of said agreement., Methods: We selected 5 indications in which pembrolizumab was deemed effective and developed portioned survival models for each indication. Survival and progression-free survival data from the published trials were utilized to recreate individual patient data, and we extrapolated-using parametric models-to a time horizon of 30 years. Inputs for both quality of life and costs were derived from the available literature and were indexed., Results: The incremental cost-effectiveness ratios ranged between €35 313 and €322 349 per quality-adjusted life-year, depending on the indication. Only 1 indication fell under the €80 000 (or €100 000) cost-effectiveness threshold. When applying the average reported discount on intramural pharmaceuticals in The Netherlands, incremental cost-effectiveness ratios ranged between €20 881 and €252 934 per quality-adjusted life-year gained, and the €80 000 (or €100 000) threshold was met in 3 indications out of 5., Conclusions: Our results show that pembrolizumab could be cost-effective in some indications, depending on the confidential price agreement established. However, the possibility of reimbursing not cost-effective care when the price is anchored in 1 indication remains possible. Indication-based pricing could help align value and price for innovative pharmaceuticals that are subject to indication broadening., Competing Interests: Author Disclosures Author disclosure forms can be accessed below in the Supplemental Material section., (Copyright © 2024. Published by Elsevier Inc.)

Published

2024

36. Systematic Evaluation of Tyrosine Kinase Inhibitors as OATP1B1 Substrates Using a Competitive Counterflow Screen.

Author

Drabison T, Boeckman M, Yang Y, Huang KM, de Bruijn P, Nepal MR, Silvaroli JA, Chowdhury AT, Eisenmann ED, Cheng X, Pabla N, Mathijssen RHJ, Baker SD, Hu S, Sparreboom A, and Talebi Z

Subjects

Humans, Animals, HEK293 Cells, Mice, Pyrimidines pharmacology, Hepatocytes metabolism, Hepatocytes drug effects, Estradiol metabolism, Estradiol analogs & derivatives, Estradiol pharmacology, Liver metabolism, Liver drug effects, Estrone analogs & derivatives, Estrone metabolism, Molecular Docking Simulation, Mice, Knockout, Biological Transport, Male, Tyrosine Kinase Inhibitors, Liver-Specific Organic Anion Transporter 1 metabolism, Liver-Specific Organic Anion Transporter 1 antagonists & inhibitors, Liver-Specific Organic Anion Transporter 1 genetics, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors metabolism, Protein Kinase Inhibitors pharmacokinetics, Sulfonamides pharmacology, Sulfonamides metabolism, Indazoles pharmacology

Abstract

Although the primary elimination pathway for most tyrosine kinase inhibitors (TKI) involves CYP3A4-mediated metabolism, the mechanism by which these agents are brought into hepatocytes remains unclear. In this study, we optimized and validated a competitive counterflow (CCF) assay to examine TKIs as substrates of the hepatic uptake transporter OATP1B1. The CCF method was based on the stimulated efflux of radiolabeled estradiol-17β-glucuronide under steady-state conditions in HEK293 cells engineered to overexpress OATP1B1. Of the 62 approved TKIs examined, 13 agents were identified as putative substrates of OATP1B1, and pazopanib was selected as a representative hit for further validation studies. The transport of pazopanib by OATP1B1 was confirmed by decreased activity of its target VEGFR2 in OATP1B1-overexpressing cells, but not cells lacking OATP1B1, consistent with molecular docking analyses indicating an overlapping binding orientation on OATP1B1 with the known substrate estrone-3-sulfate. In addition, the liver-to-plasma ratio of pazopanib in vivo was decreased in mice with a deficiency of the orthologous transporters, and this was accompanied by diminished pazopanib-induced hepatotoxicity, as determined by changes in the levels of liver transaminases. Our study supports the utility of CCF assays to assess substrate affinity for OATP1B1 within a large set of agents in the class of TKIs and sheds light on the mechanism by which these agents are taken up into hepatocytes in advance of metabolism., Significance: Despite the established exposure-pharmacodynamic relationships for many TKIs, the mechanisms underlying the agents' unpredictable pharmacokinetic profiles remain poorly understood. We report here that the disposition of many TKIs depends on hepatic transport by OATP1B1, a process that has toxicologic ramifications for agents that are associated with hepatotoxicity., (©2024 The Authors; Published by the American Association for Cancer Research.)

Published

2024

37. Nonlinear Mixed-Effects Model of Z-Endoxifen Concentrations in Tamoxifen-Treated Patients from the CEPAM Cohort.

Author

Mc Laughlin AM, Helland T, Klima F, Koolen SLW, van Schaik RHN, Mathijssen RHJ, Neven P, Swen JJ, Guchelaar HJ, Dalenc F, White-Koning M, Michelet R, Mikus G, Schroth W, Mürdter T, Brauch H, Schwab M, Søiland H, Mellgren G, Thomas F, Kloft C, and Hertz DL

Subjects

Humans, Female, Models, Biological, Middle Aged, Cohort Studies, Treatment Outcome, Computer Simulation, Aged, Tamoxifen analogs & derivatives, Tamoxifen pharmacokinetics, Tamoxifen blood, Tamoxifen therapeutic use, Cytochrome P-450 CYP2D6 metabolism, Cytochrome P-450 CYP2D6 genetics, Breast Neoplasms drug therapy, Antineoplastic Agents, Hormonal pharmacokinetics, Antineoplastic Agents, Hormonal therapeutic use, Antineoplastic Agents, Hormonal blood, Nonlinear Dynamics

Abstract

Tamoxifen is widely used in patients with hormone receptor-positive breast cancer. The polymorphic enzyme CYP2D6 is primarily responsible for metabolic activation of tamoxifen, resulting in substantial interindividual variability of plasma concentrations of its most important metabolite, Z-endoxifen. The Z-endoxifen concentration thresholds below which tamoxifen treatment is less efficacious have been proposed but not validated, and prospective trials of individualized tamoxifen treatment to achieve Z-endoxifen concentration thresholds are considered infeasible. Therefore, we aim to validate the association between Z-endoxifen concentration and tamoxifen treatment outcomes, and identify a Z-endoxifen concentration threshold of tamoxifen efficacy, using pharmacometric modeling and simulation. As a first step, the CYP2D6 Endoxifen Percentage Activity Model (CEPAM) cohort was created by pooling data from 28 clinical studies (> 7,000 patients) with measured endoxifen plasma concentrations. After cleaning, data from 6,083 patients were used to develop a nonlinear mixed-effect (NLME) model for tamoxifen and Z-endoxifen pharmacokinetics that includes a conversion factor to allow inclusion of studies that measured total endoxifen but not Z-endoxifen. The final parent-metabolite NLME model confirmed the primary role of CYP2D6, and contributions from body weight, CYP2C9 phenotype, and co-medication with CYP2D6 inhibitors, on Z-endoxifen pharmacokinetics. Future work will use the model to simulate Z-endoxifen concentrations in patients receiving single agent tamoxifen treatment within large prospective clinical trials with long-term survival to identify the Z-endoxifen concentration threshold below which tamoxifen is less efficacious. Identification of this concentration threshold would allow personalized tamoxifen treatment to improve outcomes in patients with hormone receptor-positive breast cancer., (© 2024 The Authors. Clinical Pharmacology & Therapeutics published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published

2024

38. Reasons for non-feasibility of therapeutic drug monitoring of oral targeted therapies in oncology - an analysis of the closed cohorts of a multicentre prospective study.

Author

van der Kleij MBA, Guchelaar NAD, Meertens M, Westerdijk K, Giraud EL, Bleckman RF, Groenland SL, van Eerden RAG, Imholz ALT, Vulink AJE, Otten HM, Fiebrich-Westra HB, Lubberman FJE, Desar IME, Moes DAR, Touw DJ, Koolen SLW, Gelderblom H, Reyners AKL, van Erp NP, Mathijssen RHJ, Huitema ADR, and Steeghs N

Subjects

Humans, Prospective Studies, Feasibility Studies, Administration, Oral, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents administration & dosage, Antineoplastic Agents adverse effects, Molecular Targeted Therapy, Imidazoles pharmacokinetics, Imidazoles administration & dosage, Anilides pharmacokinetics, Anilides administration & dosage, Male, Everolimus pharmacokinetics, Everolimus administration & dosage, Female, Oximes pharmacokinetics, Oximes administration & dosage, Phenylthiohydantoin analogs & derivatives, Phenylthiohydantoin pharmacokinetics, Phenylthiohydantoin administration & dosage, Nitriles pharmacokinetics, Nitriles administration & dosage, Phenylurea Compounds, Pyridones, Pyrimidinones, Piperazines, Benzamides, Drug Monitoring methods, Neoplasms drug therapy, Pyridines pharmacokinetics, Pyridines administration & dosage

Abstract

Background: Therapeutic drug monitoring (TDM) - performing dose adjustments based on measured drug levels and established pharmacokinetic (PK) targets - could optimise treatment with drugs that show large interpatient variability in exposure. We evaluated the feasibility of TDM for multiple oral targeted therapies. Here we report on drugs for which routine TDM is not feasible., Methods: We evaluated drug cohorts from the Dutch Pharmacology Oncology Group - TDM study. Based on PK levels taken at pre-specified time points, PK-guided interventions were performed. Feasibility of TDM was evaluated, and based on the success and practicability of TDM, cohorts could be closed., Results: For 10 out of 24 cohorts TDM was not feasible and inclusion was closed. A high incidence of adverse events resulted in closing the cabozantinib, dabrafenib/trametinib, everolimus, regorafenib and vismodegib cohort. The enzalutamide and erlotinib cohorts were closed because almost all PK levels were above target. Other, non-pharmacological reasons led to closing the palbociclib, olaparib and tamoxifen cohort., Conclusions: Although TDM could help personalising treatment for many drugs, the above-mentioned reasons can influence its feasibility, usefulness and clinical applicability. Therefore, routine TDM is not advised for cabozantinib, dabrafenib/trametinib, enzalutamide, erlotinib, everolimus, regorafenib and vismodegib. Nonetheless, TDM remains valuable for individual clinical decisions., (© 2024. The Author(s).)

Published

2024

39. Therapeutic Drug Monitoring of Oral Oncology Drugs: Finding the Right Nails.

Author

Guchelaar NAD, van der Kleij MBA, Steeghs N, Huitema ADR, Mathijssen RHJ, and Koolen SLW

Subjects

Humans, Administration, Oral, Neoplasms drug therapy, Drug Monitoring methods, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents administration & dosage, Antineoplastic Agents adverse effects

Published

2024

40. Model-Informed Development of a Cost-Saving Dosing Regimen for Sacituzumab Govitecan.

Author

Moes DJAR, Hendrikx JJMA, Guchelaar HJ, Mathijssen RHJ, Bakker JL, Dezentjé VO, de Rouw N, van Erp NP, Smit EF, van den Heuvel MM, Munnink THO, van Kats M, Croes S, Kroep JR, Zwaveling J, and Ter Heine R

Subjects

Humans, Camptothecin analogs & derivatives, Camptothecin pharmacology, Camptothecin therapeutic use, Female, Immunoconjugates pharmacology, Immunoconjugates therapeutic use, Antibodies, Monoclonal, Humanized pharmacology, Antibodies, Monoclonal, Humanized therapeutic use

Abstract

Background: The antibody-drug conjugate sacituzumab govitecan is approved for metastatic triple-negative breast cancer and has shown promising results in various other types of cancer. Its costs may limit patient access to this novel effective treatment modality., Objective: The purpose of this study was to develop an evidence-based rational dosing regimen that results in targeted drug exposure within the therapeutic range while minimizing financial toxicity, to improve treatment access., Patients and Methods: Exposure equivalent dosing strategies were developed based on pharmacokinetic modeling and simulation by using the published pharmacokinetic model developed by the license holder. The alternative dose was based on the principle of using complete vials to prevent spillage and on the established non-linear relationship between body weight and systemic exposure. Equivalent exposure compared to the approved dosing regimen of 10 mg/kg was aimed for. Equivalent exposure was conservatively defined as calculated geometric mean ratios within the 0.9-1.11 boundaries for area under the concentration-time curve (AUC), trough concentration (C trough ) and maximum concentration (C max ) of the alternative dosing regimen compared to the approved dosing regimen. Since different vial sizes are available for the European Union (EU) and United States (US) market, because body weight distributions differ between these populations, we performed our analysis for both scenarios., Results: Dosing regimens of sacituzumab govitecan for the EU (< 50 kg: 400 mg, 50-80 kg: 600 mg, and > 80 kg: 800 mg) and US population (< 40 kg: 360 mg, 40-65 kg: 540 mg, 65-90 kg: 720 mg, and > 90 kg: 900 mg) were developed, based on weight bands. The geometric mean ratios for all pharmacokinetic outcomes were within the predefined equivalence boundaries, while the quantity of drug used was 21.5% and 19.0% lower for the EU and US scenarios, respectively., Conclusions: With the alternative dosing proposal, an approximately 20% reduction in drug expenses for sacituzumab govitecan can be realized while maintaining an equivalent and more evenly distributed exposure throughout the body weight range, without notable increases in pharmacokinetic variability., (© 2024. The Author(s).)

Published

2024

41. Optimizing the Dosing Regimen During Rotation From Subcutaneous to Transdermal Administration of Fentanyl.

Author

Agema BC, Vrielink K, Oomen-de Hoop E, van Tienen F, Geijteman ECT, Van der Rijt CCD, Koch BCP, Koolen SLW, Oosten AW, and Mathijssen RHJ

Subjects

Humans, Male, Female, Middle Aged, Aged, Prospective Studies, Injections, Subcutaneous, Adult, Drug Administration Schedule, Transdermal Patch, Fentanyl administration & dosage, Fentanyl pharmacokinetics, Analgesics, Opioid administration & dosage, Analgesics, Opioid pharmacokinetics, Administration, Cutaneous, Cancer Pain drug therapy

Abstract

Context: Subcutaneous (SC) administration of fentanyl allows for rapid dose titration to treat urgent cancer-related pain. After establishing the optimal fentanyl dose, patients typically rotate towards transdermal (TD) fentanyl patches. Continuing the SC fentanyl up to 12h after application of the patch led to elevated fentanyl concentrations and fentanyl-related toxicities. Based on these findings, and simulations using a pharmacokinetic (PK) model, SC fentanyl administration was discontinued immediately following the application of the patch., Objectives: To validate the fentanyl rotation schedule by assessing the PK equivalence in fentanyl exposure before and after rotation., Methods: PK samples and clinical data were prospectively collected from 12 hours prior to rotation until 12 hours after rotation in patients with cancer-related pain undergoing fentanyl rotation., Results: Between December 2021 and September 2023, 29 evaluable patients were enrolled in the study. The 90% confidence interval (CI) of the geometric mean ratio between the post- over pre-rotation area under the curve (AUC) fell within the prespecified 0.8-1.25 equivalence interval (90% CI 1.05-1.16). Patient-reported intensity of both nausea (P = 0.047) and transpiration (P = 0.034) decreased post-rotation. Pain intensity and other adverse events did not differ significantly pre and post-rotation. One patient needed adjustment of opioid therapy 40 hours after rotation due to fentanyl-related toxicities., Conclusion: The updated rotation scheme, implying a 1:1 dose conversion and discontinuation of SC fentanyl directly after rotation, resulted in equivalent fentanyl exposure pre and post-rotation. Moreover, the dosing regimen showed to be safe and efficacious during rotation. The new dosing regimen when rotating from SC to TD fentanyl can be effectively and safely implemented in routine palliative care., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

42. Discovering novel germline genetic variants linked to severe fluoropyrimidine-related toxicity in- and outside DPYD.

Author

Knikman JE, Zhai Q, Lunenburg CATC, Henricks LM, Böhringer S, van der Lee M, de Man FM, Offer SM, Shrestha S, Creemers GJ, Baars A, Dezentjé VO, Imholz ALT, Jeurissen FJF, Portielje JEA, Jansen RLH, Hamberg P, Droogendijk HJ, Koopman M, Nieboer P, van de Poel MHW, Mandigers CMPW, van Schaik RHN, Gelderblom H, Mathijssen RHJ, Schellens JHM, Cats A, Guchelaar HJ, and Swen JJ

Subjects

Humans, Female, Male, Middle Aged, Genome-Wide Association Study, Germ-Line Mutation, Aged, Polymorphism, Single Nucleotide, Adult, Fluorouracil adverse effects, Pyrimidines adverse effects, Antimetabolites, Antineoplastic adverse effects, Exons, Dihydrouracil Dehydrogenase (NADP) genetics

Abstract

Background: The Alpe-DPD study (NCT02324452) demonstrated that prospective genotyping and dose-individualization using four alleles in DPYD (DPYD*2A/rs3918290, c.1236G > A/rs75017182, c.2846A > T/rs67376798 and c.1679 T > G/rs56038477) can mitigate the risk of severe fluoropyrimidine toxicity. However, this could not prevent all toxicities. The goal of this study was to identify additional genetic variants, both inside and outside DPYD, that may contribute to fluoropyrimidine toxicity., Methods: Biospecimens and data from the Alpe-DPD study were used. Exon sequencing was performed to identify risk variants inside DPYD. In silico and in vitro analyses were used to classify DPYD variants. A genome-wide association study (GWAS) with severe fluoropyrimidine-related toxicity was performed to identify variants outside DPYD. Association with severe toxicity was assessed using matched-pair analyses for the exon sequencing and logistic, Cox, and ordinal regression analyses for GWAS., Results: Twenty-four non-synonymous, frameshift, and splice site DPYD variants were detected in ten of 986 patients. Seven of these variants (c.1670C > T, c.1913 T > C, c.1925 T > C, c.506delC, c.731A > C, c.1740 + 1G > T, c.763 - 2A > G) were predicted to be deleterious. The carriers of either of these variants showed a trend towards a 2.14-fold (95% CI, 0.41-11.3, P = 0.388) increased risk of severe toxicity compared to matched controls (N = 30). After GWAS of 942 patients, no individual single nucleotide polymorphisms achieved genome-wide significance (P ≤ 5 × 10 -8 ), however, five variants were suggestive of association (P < 5 × 10 -6 ) with severe toxicity., Conclusions: Results from DPYD exon sequencing and GWAS analysis did not identify additional genetic variants associated with severe toxicity, which suggests that testing for single markers at a population level currently has limited clinical value. Identifying additional variants on an individual level is still promising to explain fluoropyrimidine-related severe toxicity. In addition, studies with larger samples sizes, in more diverse cohorts are needed to identify potential clinically relevant genetic variants related to severe fluoropyrimidine toxicity., (© 2024. The Author(s).)

Published

2024

43. Early Identification of Patients at Risk of Cabazitaxel-induced Severe Neutropenia.

Author

Agema BC, Buck SAJ, Viskil M, Isebia KT, de Neijs MJ, Sassen SDT, Koch BCP, Joerger M, de Wit R, Koolen SLW, and Mathijssen RHJ

Subjects

Humans, Male, Middle Aged, Aged, Female, Antineoplastic Agents adverse effects, Neutrophils drug effects, Adult, Prostatic Neoplasms drug therapy, Leukocyte Count, Neutropenia chemically induced, Neutropenia blood, Taxoids adverse effects, Taxoids therapeutic use, Taxoids pharmacokinetics

Abstract

Background: Cabazitaxel frequently causes severe neutropenia. A higher cabazitaxel systemic exposure is related to a lower nadir absolute neutrophil count (ANC)., Objective: To describe the effect of cabazitaxel systemic exposure on ANC by a population pharmacokinetic/pharmacodynamic (POP-PK/PD) model, and to identify patients at risk of severe neutropenia early in their treatment course using a PK threshold., Design, Setting, and Participants: Data from five clinical studies were pooled to develop a POP-PK/PD model using NONMEM, linking both patient characteristics and cabazitaxel systemic exposure directly to ANC., Outcome Measurements and Statistical Analysis: A PK threshold, predictive of severe neutropenia (grade ≥3), was determined using a receiver operating characteristic curve., Results and Limitations: Ninety-six patients were included with a total of 1726 PK samples and 1081 ANCs. The POP-PK/PD model described both cabazitaxel PK and ANC accurately. A cabazitaxel plasma concentration of >4.96 ng/ml at 6 h after the start of infusion was found to be predictive of severe neutropenia, with a sensitivity of 76% and a specificity of 65%., Conclusions: Early cabazitaxel plasma levels are predictive of severe neutropenia. Implementation of the proposed PK threshold results in early identification of almost 76% of all severe neutropenias. If prospectively validated, patients at risk could benefit from prophylactic administration of granulocyte colony stimulating factors, preventing severe neutropenia in an early phase of treatment. Implementation of this threshold permits a less restricted use of the 25 mg/m 2 dose, potentially increasing the therapeutic benefit., Patient Summary: Treatment with cabazitaxel chemotherapy often causes neutropenia, leading to susceptibility to infections, which might be life threatening. We found that a systemic cabazitaxel concentration above 4.96 ng/ml 6 h after the start of infusion is predictive of the occurrence of severe neutropenia. Measurement of systemic cabazitaxel levels provides clinicians with the opportunity to prophylactically stimulate neutrophil growth., (Copyright © 2023 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published

2024

44. Systemic Treatment Strategies and Outcomes of Patients With Synchronous Peritoneal Metastases of Gastric Origin: A Nationwide Population-Based Study.

Author

Guchelaar NAD, Noordman BJ, Welten MW, van Santen MT, de Neijs MJ, Koolen SLW, Verhoeven RHA, Oomen-de Hoop E, van der Sluis PC, Lagarde SM, van Laarhoven HWM, de Hingh IHJT, Creemers GJ, Mostert B, Wijnhoven BPL, and Mathijssen RHJ

Subjects

Humans, Female, Male, Middle Aged, Aged, Netherlands epidemiology, Treatment Outcome, Adenocarcinoma secondary, Adenocarcinoma therapy, Adenocarcinoma mortality, Adenocarcinoma drug therapy, Adult, Registries, Peritoneal Neoplasms secondary, Peritoneal Neoplasms therapy, Peritoneal Neoplasms mortality, Stomach Neoplasms pathology, Stomach Neoplasms mortality, Stomach Neoplasms therapy, Stomach Neoplasms drug therapy, Stomach Neoplasms epidemiology, Antineoplastic Combined Chemotherapy Protocols therapeutic use

Abstract

Background: Palliative systemic treatment is currently standard of care for metastatic gastric cancer. However, patients with peritoneal metastases of gastric origin are often underrepresented in clinical studies due to unmeasurable radiologic disease. This study describes the systemic treatment strategies and outcomes in patients with peritoneal metastases in a nationwide real-world setting., Methods: Patients with gastric adenocarcinoma and synchronous peritoneal metastases (with or without other metastases) diagnosed in the Netherlands between 2015 and 2020 were identified from the nationwide Netherlands Cancer Registry. Median overall survival (OS) and time-to-treatment failure were determined and multivariable Cox regression analyses were used to compare treatment groups, corrected for relevant tumor and patient characteristics., Results: In total, 1,972 patients were included, of whom 842 (43%) were treated with palliative systemic therapy. The majority received capecitabine + oxaliplatin (CAPOX; 44%), followed by fluorouracil/leucovorin/oxaliplatin (FOLFOX; 19%), and epirubicin + capecitabine + oxaliplatin (EOX; 8%). Of the 99 (45%) patients who received second-line systemic treatment, ramucirumab + paclitaxel were administered most frequently (63%). After adjustment for sex, age, comorbidities, performance status, tumor location, Lauren classification, and the presence of metastases outside of the peritoneum, patients treated with a triplet containing docetaxel and those treated with a regimen containing trastuzumab had a significantly longer OS compared with patients treated with a doublet containing a fluoropyrimidine derivate + oxaliplatin (hazard ratio [HR], 0.69; 95% CI, 0.52-0.91, and HR, 0.68; 95% CI, 0.51-0.91, respectively). Monotherapy was associated with a shorter OS (HR, 2.08, 95% CI, 1.53-2.83)., Conclusions: There is substantial heterogeneity in systemic treatment choices in patients with gastric cancer and peritoneal metastases in the Netherlands. In this study, patients treated with triplets containing docetaxel and with trastuzumab-containing regimens survived longer than patients who received doublet therapy. Despite this, median OS for all treatment groups remained below one year.

Published

2024

45. Is uracil enough for effective pre-emptive DPD testing?

Author

Heersche N, Matic M, Mathijssen RHJ, Coenen MJH, and van Schaik RHN

Subjects

Humans, Dihydrouracil Dehydrogenase (NADP) metabolism, Dihydrouracil Dehydrogenase (NADP) analysis, Dihydrouracil Dehydrogenase (NADP) genetics, Male, Uracil analogs & derivatives, Dihydropyrimidine Dehydrogenase Deficiency diagnosis

Published

2024

46. Darolutamide does not interfere with OATP-mediated uptake of docetaxel.

Author

Buck SAJ, Talebi Z, Drabison T, Jin Y, Gibson AA, Hu P, de Bruijn P, de Ridder CMA, Stuurman D, Hu S, van Weerden WM, Koolen SLW, de Wit R, Sparreboom A, Mathijssen RHJ, and Eisenmann ED

Subjects

Humans, Male, Animals, Mice, Drug Interactions, Cell Line, Tumor, HEK293 Cells, Docetaxel pharmacology, Docetaxel pharmacokinetics, Solute Carrier Organic Anion Transporter Family Member 1B3 metabolism, Prostatic Neoplasms drug therapy, Prostatic Neoplasms metabolism, Prostatic Neoplasms pathology, Xenograft Model Antitumor Assays, Pyrazoles pharmacology, Pyrazoles pharmacokinetics

Abstract

The addition of darolutamide, an androgen receptor signalling inhibitor, to therapy with docetaxel has recently been approved as a strategy to treat metastatic prostate cancer. OATP1B3 is an SLC transporter that is highly expressed in prostate cancer and is responsible for the accumulation of substrates, including docetaxel, into tumours. Given that darolutamide inhibits OATP1B3 in vitro, we sought to characterise the impact of darolutamide on docetaxel pharmacokinetics. We investigated the influence of darolutamide on OATP1B3 transport using in vitro and in vivo models. We assessed the impact of darolutamide on the tumour accumulation of docetaxel in a patient-derived xenograft (PDX) model and on an OATP1B biomarker in patients. Darolutamide inhibited OATP1B3 in vitro at concentrations higher than the reported C max . Consistent with these findings, in vivo studies revealed that darolutamide does not influence the pharmacokinetics of Oatp1b substrates, including docetaxel. Docetaxel accumulation in PDX tumours was not decreased in the presence of darolutamide. Metastatic prostate cancer patients had similar levels of OATP1B biomarkers, regardless of treatment with darolutamide. Consistent with a low potential to inhibit OATP1B3-mediated transport in vitro, darolutamide does not significantly impede the transport of Oatp1b substrates in vivo or in patients. Our findings support combined treatment with docetaxel and darolutamide, as no OATP1B3 transporter based drug-drug interaction was identified., (© 2024 The Authors. International Journal of Cancer published by John Wiley & Sons Ltd on behalf of UICC.)

Published

2024

47. Evaluating the Clinical Impact and Feasibility of Therapeutic Drug Monitoring of Pazopanib in a Real-World Soft-Tissue Sarcoma Cohort.

Author

Meertens M, Giraud EL, van der Kleij MBA, Westerdijk K, Guchelaar NAD, Bleckman RF, Rieborn A, Imholz ALT, Otten HM, Vulink A, Los M, Hamberg P, van der Graaf WTA, Gelderblom H, Moes DJAR, Broekman KE, Touw DJ, Koolen SLW, Mathijssen RHJ, Huitema ADR, van Erp NP, Desar IME, and Steeghs N

Subjects

Humans, Male, Female, Middle Aged, Aged, Adult, Cohort Studies, Angiogenesis Inhibitors pharmacokinetics, Angiogenesis Inhibitors administration & dosage, Angiogenesis Inhibitors therapeutic use, Progression-Free Survival, Aged, 80 and over, Retrospective Studies, Indazoles pharmacokinetics, Sulfonamides pharmacokinetics, Sulfonamides administration & dosage, Sulfonamides therapeutic use, Sarcoma drug therapy, Pyrimidines pharmacokinetics, Pyrimidines administration & dosage, Pyrimidines therapeutic use, Drug Monitoring methods, Feasibility Studies

Abstract

Introduction and Objective: Pazopanib is registered for metastatic renal cell carcinoma and soft-tissue sarcoma (STS). Its variable pharmacokinetic (PK) characteristics and narrow therapeutic range provide a strong rationale for therapeutic drug monitoring (TDM). Prior studies have defined target levels of drug exposure (≥ 20.5 mg/L) linked to prolonged progression-free survival (PFS), but the added value of using TDM remains unclear. This study investigates the effect of TDM of pazopanib in patients with STS on survival outcomes and dose-limiting toxicities (DLTs) and evaluates the feasibility of TDM-guided dosing., Methods: A TDM-guided cohort was compared to a non-TDM-guided cohort for PFS, overall survival (OS) and DLTs. PK samples were available from all patients, though not acted upon in the non-TDM-guided cohort. We evaluated the feasibility of TDM by comparing the proportion of underdosed patients in our TDM cohort with data from previous publications., Results: A total of 122 STS patients were included in the TDM-guided cohort (n = 95) and non-TDM-guided cohort (n = 27). The average exposure in the overall population was 30.5 mg/L and was similar in both groups. Median PFS and OS did not differ between the TDM-guided cohort and non-TDM-guided cohort (respectively 5.5 vs 4.4 months, p = 0.3, and 12.6 vs 10.1 months, p = 0.8). Slightly more patients in the non-TDM-guided cohort experienced DLTs (54%) compared to the TDM-guided cohort (44%). The proportion of underdosed patients (13.3%) was halved compared to historical data (26.7%)., Conclusion: TDM reduced the proportion of patients with subtherapeutic exposure levels by ~ 50%. Nonetheless, the added value of TDM for achieving target trough levels of ≥ 20.5 mg/L for pazopanib on survival outcomes could not be confirmed in STS patients., (© 2024. The Author(s).)

Published

2024

48. Clinical Utility of Circulating Tumor DNA in Patients With Advanced KRAS G12C -Mutated NSCLC Treated With Sotorasib.

Author

Ernst SM, van Marion R, Atmodimedjo PN, de Jonge E, Mathijssen RHJ, Paats MS, de Bruijn P, Koolen SL, von der Thüsen JH, Aerts JGJV, van Schaik RHN, Dubbink HJ, and Dingemans AC

Subjects

Adult, Aged, Aged, 80 and over, Female, Humans, Male, Middle Aged, Biomarkers, Tumor genetics, Biomarkers, Tumor blood, Mutation, Piperazines therapeutic use, Prospective Studies, Pyridines therapeutic use, Pyrimidines therapeutic use, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung genetics, Carcinoma, Non-Small-Cell Lung pathology, Carcinoma, Non-Small-Cell Lung blood, Circulating Tumor DNA genetics, Circulating Tumor DNA blood, Lung Neoplasms drug therapy, Lung Neoplasms genetics, Lung Neoplasms pathology, Lung Neoplasms blood, Proto-Oncogene Proteins p21(ras) genetics

Abstract

Introduction: For patients with KRAS G12C -mutated NSCLC who are treated with sotorasib, there is a lack of biomarkers to guide treatment decisions. We therefore investigated the clinical utility of pretreatment and on-treatment circulating tumor DNA (ctDNA) and treatment-emergent alterations on disease progression., Methods: Patients with KRAS G12C -mutated NSCLC treated with sotorasib were prospectively enrolled in our biomarker study (NCT05221372). Plasma samples were collected before sotorasib treatment, at first-response evaluation and at disease progression. The TruSight Oncology 500 panel was used for ctDNA and variant allele frequency analysis. Tumor response and progression-free survival were assessed per Response Evaluation Criteria in Solid Tumors version 1.1., Results: Pretreatment KRAS G12C ctDNA was detected in 50 of 66 patients (76%). Patients with detectable KRAS G12C had inferior progression-free survival (hazard ratio [HR] 2.13 [95% confidence interval [CI]: 1.06-4.30], p = 0.031) and overall survival (HR 2.61 [95% CI: 1.16-5.91], p = 0.017). At first-response evaluation (n = 40), 29 patients (73%) had a molecular response. Molecular nonresponders had inferior overall survival (HR 3.58 [95% CI: 1.65-7.74], p = 0.00059). The disease control rate was significantly higher in those with a molecular response (97% versus 64%, p = 0.015). KRAS amplifications were identified as recurrent treatment-emergent alterations., Conclusions: Our data suggest detectable pretreatment KRAS G12C ctDNA as a marker for poor prognosis and on-treatment ctDNA clearance as a marker for treatment response. We identified KRAS amplifications as a potential recurring resistance mechanism to sotorasib. Identifying patients with superior prognosis could aid in optimizing time of treatment initiation, and identifying patients at risk of early progression could allow for earlier treatment decisions., Competing Interests: Disclosure Dr. Mathijssen reports receiving institutional fees for investigator-initiated trials from Astellas, Bayer, Boehringer-Ingelheim, Cristal Therapeutics, Deuter Oncology, Nordic Pharma, Novartis, Pamgene, Pfizer, Roche, Sanofi, and Servier, outside the current work. Dr. Paats reports receiving institutional fees from AstraZeneca, Bayer, Eli Lilly, Janssen, Novartis, Pfizer, Roche, and Takeda, outside the current work. Dr. Koolen reports receiving speaker fees from Promise Proteomics, outside the current work. Dr. von der Thüsen reports receiving advisory board and speaker fees from Eli Lilly, Bristol-Myers Squibb, Merck Sharp & Dohme, AstraZeneca, Bayer, Janssen, and Pfizer, outside the current work. Dr. Aerts reports receiving advisory board and speaker fees from Eli Lilly, Bristol-Myers Squibb, Merck Sharp & Dohme, AstraZeneca, Bayer, and Amphera and is a stock owner of Amphera, outside the current work. Dr. Dubbink reports receiving translational research funding and support from AstraZeneca, Merck Sharp & Dohme, and Illumina; advisory board fees from AbbVie, AstraZeneca, Bayer, Janssen, Lilly, Merck Sharp & Dohme, and Pfizer; honorarium from AstraZeneca, Lilly, Novartis, and Pfizer; and consultant fees from Bayer. Dr. Dingemans reports receiving institutional fees from Roche, Eli Lilly, Boehringer Ingelheim, AstraZeneca, Janssen, Chiezi, Amgen, Pfizer, Bayer, Takeda, Pharmamar, Sanofi, and Daiichi, outside the current work. All other authors report no disclosures., (Copyright © 2024 International Association for the Study of Lung Cancer. Published by Elsevier Inc. All rights reserved.)

Published

2024

49. The OCT2/MATE1 Interaction Between Trifluridine, Metformin and Cimetidine: A Crossover Pharmacokinetic Study.

Author

Guchelaar NAD, Buck SAJ, van Doorn L, Hussaarts KGAM, Sandberg Y, van der Padt-Pruijsten A, van Alphen RJ, Poppe-Manenschijn L, Vleut I, de Bruijn P, van Leeuwen RWF, Mostert B, Eskens FALM, Oomen-de Hoop E, Koolen SLW, and Mathijssen RHJ

Subjects

Adult, Aged, Female, Humans, Male, Middle Aged, Colorectal Neoplasms drug therapy, Colorectal Neoplasms metabolism, Drug Combinations, Organic Cation Transporter 2 metabolism, Prospective Studies, Pyrrolidines pharmacokinetics, Pyrrolidines administration & dosage, Stomach Neoplasms drug therapy, Stomach Neoplasms metabolism, Thymine, Cimetidine pharmacokinetics, Cimetidine pharmacology, Cimetidine administration & dosage, Cross-Over Studies, Drug Interactions, Metformin pharmacokinetics, Metformin administration & dosage, Metformin pharmacology, Organic Cation Transport Proteins metabolism, Organic Cation Transport Proteins antagonists & inhibitors, Trifluridine pharmacokinetics, Trifluridine administration & dosage

Abstract

Background and Objectives: Trifluridine/tipiracil, registered for the treatment of patients with metastatic gastric and colorectal cancer, is a substrate and inhibitor for the organic cation transporter 2 (OCT2) and the multidrug and toxin extrusion protein 1 (MATE1), which raises the potential for drug-drug interactions with other OCT2/MATE1 modulators. Therefore, we prospectively examined the effect of an OCT2/MATE1 inhibitor (cimetidine) and substrate (metformin) on the pharmacokinetics of trifluridine., Methods: In this three-phase crossover study, patients with metastatic colorectal or gastric cancer were sequentially treated with trifluridine/tipiracil alone (phase A), trifluridine/tipiracil concomitant with metformin (phase B) and trifluridine/tipiracil concomitant with cimetidine (phase C). The primary endpoint was the relative difference in exposure of trifluridine assessed by the area under the curve from timepoint zero to infinity. A > 30% change in exposure was considered clinically relevant. A p-value of < 0.025 was considered significant because of a Bonferroni correction., Results: Eighteen patients were included in the analysis. Metformin did not significantly alter the exposure to trifluridine (- 12.6%; 97.5% confidence interval - 25.0, 1.8; p = 0.045). Cimetidine did alter the exposure to trifluridine significantly (+ 18.0%; 97.5% confidence interval 4.5, 33.3; p = 0.004), but this increase did not meet our threshold for clinical relevance. Metformin trough concentrations were not influenced by trifluridine/tipiracil., Conclusions: Our result suggests that the OCT2/MATE1 modulators cimetidine and metformin can be co-administered with trifluridine/tipiracil without clinically relevant effects on drug exposure., Clinical Trial Registration: NL8067 (registered 04-10-2019)., (© 2024. The Author(s).)

Published

2024

50. Intraperitoneal pharmacokinetics of systemic oxaliplatin, 5-fluorouracil and bevacizumab in patients with colorectal peritoneal metastases.

Author

Rietveld PCS, Guchelaar NAD, van Eerden RAG, de Boer NL, de Bruijn P, Sassen SDT, Madsen EVE, Koch BCP, Verhoef C, Burger JWA, Mathijssen RHJ, and Koolen SLW

Subjects

Humans, Male, Middle Aged, Female, Aged, Adult, Ascitic Fluid metabolism, Area Under Curve, Injections, Intraperitoneal, Bevacizumab pharmacokinetics, Bevacizumab administration & dosage, Colorectal Neoplasms drug therapy, Colorectal Neoplasms pathology, Peritoneal Neoplasms drug therapy, Peritoneal Neoplasms secondary, Fluorouracil pharmacokinetics, Fluorouracil administration & dosage, Oxaliplatin pharmacokinetics, Oxaliplatin administration & dosage, Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Antineoplastic Combined Chemotherapy Protocols administration & dosage

Abstract

Background: Peritoneal metastases (PM) commonly occur in colorectal cancer patients. Systemic chemotherapy yields poor outcomes for these patients. It is hypothesised that traditional systemic chemotherapy is not very effective for this patient population. This study investigates to what extent systemic anti-cancer therapy crosses the peritoneal barrier., Methods: In a Phase I study, eighteen patients received systemic oxaliplatin, 5-FU, and bevacizumab. Plasma and peritoneal fluid samples were collected to measure drug concentrations. A non-compartmental analysis determined the Area Under the Curve (AUC) for oxaliplatin and 5-FU in both matrices. Intraperitoneal (IP) and intravenous (IV) exposure ratios were calculated, along with the bevacizumab concentration IP/IV ratio. The relationship between tumour load and IP/IV ratios and the correlation between the IP/IV ratios of different treatments were assessed statistically., Results: A total of 438 5-FU samples and 578 oxaliplatin samples were analysed in plasma and peritoneal fluid. Bevacizumab was quantified with 17 measurements in plasma and 15 measurements IP. Median IP/IV ratios were 0.143, 0.352 and 0.085 for 5-FU, oxaliplatin and bevacizumab, respectively. Oxaliplatin exhibited a longer IP half-life than 5-FU. A correlation was found between oxaliplatin and bevacizumab IP/IV ratios (R=0.69, p=0.01). No statistical correlations were found between the other investigated drugs., Conclusions: Our findings indicate that only a small percentage of systemically administered anti-cancer treatment reaches the IP cavity, questioning their efficacy against PM. This strengthens the hypothesis for repeated intraperitoneal chemotherapy to reach adequate anti-cancer drug levels., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Masson SAS.. All rights reserved.)

Published

2024