Search

Your search keyword '"Spriet I"' showing total 415 results
Start Over Author "Spriet I"
415 results on '"Spriet I"'

1. Meropenem Target Attainment and Population Pharmacokinetics in Critically Ill Septic Patients with Preserved or Increased Renal Function

Author

Gijsen M, Elkayal O, Annaert P, Van Daele R, Meersseman P, Debaveye Y, Wauters J, Dreesen E, and Spriet I

Subjects
intensive care, pk/pd, exposure, dose optimization, augmented renal clearance, Infectious and parasitic diseases, RC109-216
Abstract

Matthias Gijsen,1,2 Omar Elkayal,1 Pieter Annaert,1,3 Ruth Van Daele,1,2 Philippe Meersseman,4 Yves Debaveye,4 Joost Wauters,4 Erwin Dreesen,1 Isabel Spriet1,2 1Department of Pharmaceutical and Pharmacological Sciences, KU Leuven, Leuven, Belgium; 2Pharmacy Department, University Hospitals Leuven, Leuven, Belgium; 3BioNotus, Niel, Belgium; 4Department of Cellular and Molecular Medicine, KU Leuven, Leuven, BelgiumCorrespondence: Matthias GijsenPharmacy Department, University Hospitals Leuven, Herestraat 49, Leuven, 3000, BelgiumTel +32 16 340087Fax +32 16 343080Email mathias.gijsen@uzleuven.bePurpose: Critically ill patients with preserved or increased renal function have been shown to be at risk of underexposure to meropenem. Although many meropenem population pharmacokinetic (PK) models have been published, there is no large prospective population PK study with rich sampling focusing on patients most at risk of suboptimal pharmacokinetic/pharmacodynamic (PK/PD) target attainment. Therefore, the aim of the present study was to evaluate PK/PD target attainment and to perform a thorough covariate screening using population PK modelling of meropenem in septic patients with preserved or increased renal function.Patients and Methods: A single-centre prospective observational PK study was performed in the intensive care unit (ICU) of the University Hospitals Leuven. Patients with severe sepsis or septic shock and treated with meropenem in the ICU were screened for inclusion. Patients were excluded if they received renal replacement therapy or had an estimated glomerular filtration rate according to the Chronic Kidney Disease Epidemiology collaboration equation < 70 mL/min/1.73m2 on the day of PK sampling. Successful PK/PD target attainment was defined as an unbound meropenem trough concentration above 2 mg/L or 8 mg/L. Population PK modelling was performed with NONMEM7.4.Results: In total, 58 patients were included, contributing 345 plasma samples over 70 dosing intervals. The 2 mg/L and 8 mg/L targets were successfully attained in 46% and 11% of all dosing intervals, respectively. A two-compartment population PK model with linear elimination and interindividual variability on clearance best described meropenem PK. The estimated creatinine clearance according to the Cockcroft-Gault equation was the only covariate retained during population PK analysis.Conclusion: This study provided detailed insight into meropenem PK in critically ill patients with preserved or increased renal function. We observed poor PK/PD target attainment, for which renal function was the only significant covariate.Trial Registration: This study is registered at ClinicalTrials.gov (NCT03560557).Keywords: intensive care, PK/PD, exposure, dose optimization, augmented renal clearance

Published
2022

8. Population Pharmacokinetics of Total and Unbound Isavuconazole in Critically Ill Patients: Implications for Adaptive Dosing Strategies.

Author

Jansen, A.M.E., Mertens, B., Spriet, I., Verweij, P.E., Schouten, J.A., Wauters, J., Debaveye, Y., Heine, R. ter, Bruggemann, R.J.M., Jansen, A.M.E., Mertens, B., Spriet, I., Verweij, P.E., Schouten, J.A., Wauters, J., Debaveye, Y., Heine, R. ter, and Bruggemann, R.J.M.

Abstract

Contains fulltext : 300116.pdf (Publisher’s version ) (Open Access), BACKGROUND AND OBJECTIVES: Isavuconazole is a broad-spectrum antifungal agent for the management of invasive fungal disease. Optimised drug exposure is critical for patient outcomes, specifically in the critically ill population. Solid information on isavuconazole pharmacokinetics including protein binding in patients in the intensive care unit is scarce. We aimed to describe the total and unbound isavuconazole pharmacokinetics and subsequently propose a dosage optimisation strategy. METHODS: A prospective multi-centre study in adult intensive care unit patients receiving isavuconazole was performed. Blood samples were collected on eight timepoints over one dosing interval between days 3-7 of treatment and optionally on one timepoint after discontinuation. Total and unbound isavuconazole pharmacokinetics were analysed by means of population pharmacokinetic modelling using NONMEM. The final model was used to perform simulations to assess exposure described by the area under the concentration-time curve and propose an adaptive dosing approach. RESULTS: Population pharmacokinetics of total and unbound isavuconazole were best described by an allometrically scaled two-compartment model with a saturable protein-binding model and interindividual variability on clearance and the maximum binding capacity. The median (range) isavuconazole unbound fraction was 1.65% (0.83-3.25%). After standard dosing, only 35.8% of simulated patients reached a total isavuconazole area under the concentration-time curve > 60 mg·h/L at day 14. The proposed adaptive dosing strategy resulted in an increase to 62.3% of patients at adequate steady-state exposure. CONCLUSIONS: In critically ill patients, total isavuconazole exposure is reduced and protein binding is highly variable. We proposed an adaptive dosing approach to enhance early treatment optimisation in this high-risk population. CLINICAL TRIAL REGISTRATION: ClinicalTrials.gov identifier: NCT04777058., 01 december 2023

Published
2023

15. E-book: Reumatologie – Uitgave 2023

Author

Carron, P., primary, De Craemer, A.-S., additional, Van den Bosch, F., additional, Vulsteke, J.-B., additional, Bossuyt, X., additional, De Langhe, E., additional, Willers, N., additional, Berteloot, P., additional, Wittevronghel, I., additional, Jacomen, G., additional, Schelfhout, V., additional, Vanwambeke, K., additional, Desmedt, S., additional, Desmedt, V., additional, Billiet, T., additional, George, C., additional, Meersseman, W., additional, D'Heygere, F., additional, De Bondt, E., additional, Betrains, A., additional, Vanderschueren, S., additional, Hanssens, J., additional, Werbrouck, B., additional, Terryn, W., additional, Deconinck, B., additional, Nollet, A., additional, Cokelaere, K., additional, Timmermans, K., additional, Nachtergaele, M., additional, Vanfraechem, C., additional, Bogaert, A.-M., additional, Hublou, W., additional, Gijsen, M., additional, Declercq, P., additional, Spriet, I., additional, Van der Linden, L., additional, and Quintens, C., additional

Published
2023
Full Text
View/download PDF

16. Incidence of medication-related osteonecrosis of the jaw in patients treated with both bone resorption inhibitors and vascular endothelial growth factor receptor tyrosine kinase inhibitors

Author

van Cann, T., Loyson, T., Verbiest, A., Clement, P. M., Bechter, O., Willems, L., Spriet, I., Coropciuc, R., Politis, C., Vandeweyer, R. O., Schoenaers, J., Debruyne, P. R., Dumez, H., Berteloot, P., Neven, P., Nackaerts, K., Woei-A-Jin, F. J. S. H., Punie, K., Wildiers, H., and Beuselinck, B.

Published
2017
Full Text
View/download PDF

20. Exposure to intravenous posaconazole in critically ill patients with influenza: A pharmacokinetic analysis of the POSA-FLU study

Author

Daele, R. Van, Wauters, J., Dreesen, E., Boelens, J. Jan, Nulens, E., Lormans, P., Vanderbeke, L., Jacobs, Cato, Rijnders, B., Verweij, P.E., Bruggemann, R.J.M., Spriet, I., Daele, R. Van, Wauters, J., Dreesen, E., Boelens, J. Jan, Nulens, E., Lormans, P., Vanderbeke, L., Jacobs, Cato, Rijnders, B., Verweij, P.E., Bruggemann, R.J.M., and Spriet, I.

Abstract

Item does not contain fulltext, BACKGROUND: Data on posaconazole in the critically ill are scarce. In the POSA-FLU study, we examined the prevention of influenza-associated pulmonary aspergillosis with posaconazole in this population. METHODS: In this observational sub-study, we performed a pharmacokinetic analysis, including protein binding and target attainment (TA). Blood samples were collected over a 24 h-dosing interval on both an early (Day 2 or 3) and a later (≥Day 4) treatment day. RESULTS: Target attainment was shown for AUC(0-24) and C(min) prophylaxis but not for C(min) treatment. Moreover, a saturable protein binding with a significant, positive relationship between albumin concentrations and the maximum binding capacity was observed. CONCLUSIONS: Our analysis indicates that posaconazole may be a suitable drug to further investigate for prophylaxis, as TA for prophylaxis was reached. Exposure targets for treatment were insufficiently attained in this population.

Published
2022

22. Liposomal amphotericin B exposure in critically ill patients: a prospective pharmacokinetic study

Author

Daele, R. Van, Wauters, J., Elkayal, O., Dreesen, E., Debaveye, Y., Lagrou, K., Beer, Y. de, Maertens, J., Brüggemann, R.J.M., Spriet, I., Daele, R. Van, Wauters, J., Elkayal, O., Dreesen, E., Debaveye, Y., Lagrou, K., Beer, Y. de, Maertens, J., Brüggemann, R.J.M., and Spriet, I.

Abstract

Item does not contain fulltext, Liposomal amphotericin B (L-AmB) is a broad-spectrum antifungal drug. Little is known about its pharmacokinetics (PK) in critically ill patients. The aim of this study was to document the PK of L-AmB in this population. It was also explored if covariates may be identified that influence its exposure. All adult, critically ill patients (at the intensive care unit or hematology ward) treated with L-AmB between October 2016 and January 2020 were eligible for this study. The administered dose was left at the discretion of the treating clinician. Plasma samples were collected at predose and 1, 2, 4, 8, 12, 16, 20 and 24 h postdose at an early (day 2-3) and/or later (≥ day 6) treatment day. Additionally, daily trough concentrations were collected until day 14. Of 33 included patients, 31 were evaluable; their median [IQR] age and body weight was 59 [54-64] years and 68 [59-77] kg, respectively. L-AmB was administered at doses between 2.7 mg/kg and 12.3 mg/kg, with a median [IQR] trough concentration of 3.1 [2.0-4.7] mg/l. The overall median area under the 24 h concentration-time curve (AUC0-24) and peak plasma concentration (Cmax) were 169.0 [117.0-253.0] mg h/l and 23.2 [16.9-33.7] mg/l, respectively. A considerable intra- and interpatient PK variability for Cmax and AUC0-24 was observed but no explaining variables, except the administered dose, could be identified. The PK of L-AmB in critically ill patients was documented. A considerable variability in exposure was observed between and within patients; however, it was not associated with a multitude of patient-related characteristics.

Published
2022

24. Outpatient parenteral antifungal therapy (OPAT) for invasive fungal infections with intermittent dosing of liposomal amphotericin B

Author

Peppel, R.J. van de, Schauwvlieghe, A., Daele, R. van, Spriet, I., van't Wout, J.W., Bruggemann, R.J., Rijnders, B.J.A., Hendriks, B.J.C., Boer, M.G.J. de, Dutch-Belgian Mycosis Study Grp, Internal Medicine, and Medical Microbiology & Infectious Diseases

Subjects
Male, AZOLE RESISTANCE, PHARMACOKINETICS, Antifungal Agents, antifungal stewardship, 0302 clinical medicine, Invasive fungal infection, EUROPEAN ORGANIZATION, Ambulatory Care, Medicine and Health Sciences, 030212 general & internal medicine, liposomal amphotericin B, Netherlands, DISEASES SOCIETY, Aged, 80 and over, 0303 health sciences, education.field_of_study, Incidence (epidemiology), General Medicine, Middle Aged, ASPERGILLUS-FUMIGATUS, triazole resistance, Infectious Diseases, DISEASES, SAFETY, Toxicity, outpatient, Female, Original Article, AcademicSubjects/MED00010, Life Sciences & Biomedicine, Adult, Antifungal, medicine.medical_specialty, Adolescent, medicine.drug_class, Population, SOCIETY, Renal function, Mycology, Young Adult, 03 medical and health sciences, stewardship, Pharmacokinetics, Drug Resistance, Fungal, Amphotericin B, Internal medicine, medicine, MANAGEMENT, Aspergillosis, Humans, Mucormycosis, Veterinary Sciences, education, Aged, Science & Technology, 030306 microbiology, business.industry, PHARMACODYNAMICS, outpatient parenteral antibiotic treatment, EFFICACY, Regimen, lnfectious Diseases and Global Health Radboud Institute for Health Sciences [Radboudumc 4], Pharmacodynamics, RISK-FACTORS, AcademicSubjects/SCI00960, business, parenteral antibiotic treatment, Invasive Fungal Infections, antifungal
Abstract

Contains fulltext : 225336.pdf (Publisher’s version ) (Open Access) Triazole resistant A. fumigatus has been documented in many parts of the world. In the Netherlands, incidence is now above 10% and results in the need for long-term parenteral therapy with liposomal amphotericin B (LAmB). The long terminal half-life of LAmB suggests that intermittent dosing could be effective, making the application of outpatient antifungal therapy (OPAT) possible. Here, we report our experience with the use of OPAT for Invasive Fungal Infections (IFI). All adult patients treated with LAmB with a 2 or 3 times weekly administration via the outpatient departments in four academic tertiary care centers in the Netherlands and Belgium since January 2010 were included in our analysis. Patient characteristics were collected, as well as information about diagnostics, therapy dose and duration, toxicity, treatment history and outcome of the IFI. In total, 18 patients were included. The most frequently used regimen (67%) was 5 mg/kg 3 times weekly. A partial response to the daily treatment prior to discharge was confirmed by CT-scan in 17 (94%) of patients. A favorable outcome was achieved in 13 (72%) patients. Decrease in renal function occurred in 10 (56%) cases but was reversible in all and was treatment limiting in one patient only. The 100-day mortality and 1-year mortality after initiation of OPAT were 0% and 6%, respectively. In a selected population, and after confirmation of initial response to treatment, our data support the use of OPAT with LAmB for treatment of IFI in an intermittent dosing regimen.

Published
2020
Full Text
View/download PDF

26. Highly Variable Paracetamol Pharmacokinetics After Multiple Oral Dosing in Frail Older People: A Population Pharmacokinetic Analysis

Author

van der Heijden, L. T., primary, Mian, P., additional, Hias, J., additional, de Winter, B. C. M., additional, Tournoy, J., additional, Van der Linden, L., additional, Tibboel, D., additional, Walgraeve, K., additional, Flamaing, J., additional, Koch, B. C. P., additional, Allegaert, K., additional, and Spriet, I., additional

Published
2021
Full Text
View/download PDF

27. An electronic decision tree to guide physicians in prescribing parenteral nutrition in hospitalised patients: development, validation and proof of concept

Author

Deleenheer, B., primary, Van den Broucke, E., additional, Meulemans, A., additional, Vanderstappen, J., additional, Nelle, P., additional, Katrien, C., additional, Spriet, I., additional, Van Veer, H., additional, Vangoitsenhoven, R., additional, Sabino, J.P., additional, Declercq, P., additional, Vanuytsel, T., additional, and Quintens, C., additional

Published
2021
Full Text
View/download PDF

28. Pharmacokinetic Variability and Target Attainment of Fluconazole in Critically Ill Patients

Author

Daele, R. Van, Wauters, J., Lagrou, K., Denooz, R., Hayette, M.P., Gijsen, M., Brüggemann, R.J.M., Debaveye, Y., Spriet, I., Daele, R. Van, Wauters, J., Lagrou, K., Denooz, R., Hayette, M.P., Gijsen, M., Brüggemann, R.J.M., Debaveye, Y., and Spriet, I.

Abstract

Contains fulltext : 244672.pdf (Publisher’s version ) (Open Access), Background: Fluconazole is one of the oldest antifungal drugs. Previous studies have raised concerns considering variability in exposure and inadequate target attainment in critically ill patients. The current study aims to define variability and target attainment for fluconazole exposure in a large group of critically ill patients. Methods: In this pharmacokinetic study, daily plasma trough samples and, if possible, 24 h urine samples were collected to determine fluconazole concentration. A minimum target trough concentration of 10-15 mg/L was selected, corresponding to a free area under the concentration-time curve above the minimum inhibitory concentration (fAUC/MIC) of at least 100 for an MIC of 4 mg/L. Covariates that significantly influenced fluconazole exposure were identified. Results: In total, 288 plasma samples from 43 patients, with a median age of 66 years, were included. The median fluconazole trough concentration was 22.9 mg/L. A notable component of the measured concentrations was below the target trough concentrations (13% <10 mg/L and 27% <15 mg/L). The intra- and intersubject variability were 28.3% and 50.5%, respectively. The main covariates determining fluconazole exposure were the administered dose (mg/kg), augmented renal clearance, and renal replacement therapy. Conclusions: Fluconazole trough concentrations are variable in critically ill patients and a considerable number of these concentrations was below the predefined target trough concentrations.

Published
2021

29. Ultra-performance liquid chromatography for quantification of amphotericin B plasma concentrations after use of liposomal amphotericin B

Author

Daele, R. Van, Beer, Y. de, Croes, S., Aarnoutse, R., Wauters, J., Maertens, J., Spriet, I., Brüggemann, R.J.M., Daele, R. Van, Beer, Y. de, Croes, S., Aarnoutse, R., Wauters, J., Maertens, J., Spriet, I., and Brüggemann, R.J.M.

Abstract

Item does not contain fulltext, OBJECTIVES: Liposomal amphotericin B is widely used to treat life-threatening invasive fungal infections and has replaced conventional amphotericin B deoxycholate due to its more favourable toxicity profile. Despite the fact that liposomal amphotericin B has been licensed for several decades, there is still a paucity of clinical pharmacokinetic data. An assay for the quantification of amphotericin B is necessary to allow the study of its pharmacokinetics. METHODS: A UPLC-photodiode array (PDA) analytical method was developed and validated (linearity, accuracy, precision, dilution integrity, carry-over, selectivity and stability) in accordance with EMA requirements. RESULTS: The analytical method was validated over a concentration range of 0.5-50.0 mg/L. Accuracy ranged from 97.6% to 112.1% and within-day repeatability and between-day reproducibility from 1.0% to 6.6% and from 0.4% to 4.6%, respectively, dependent on the concentration. Originally, the goal was to develop an analytical method to separate the liposomal and free amphotericin B fractions, but this was not achieved. Difficulties and bottlenecks encountered are presented. CONCLUSIONS: A UPLC-PDA analytical method was developed to quantify total amphotericin B in plasma after the use of liposomal amphotericin B.

Published
2021

30. Pharmacokinetics and target attainment of intravenous posaconazole in critically ill patients during extracorporeal membrane oxygenation

Author

Daele, R. Van, Bruggemann, R.J.M., Dreesen, Erwin, Depuydt, P., Rijnders, Bart J.A., Cotton, Frederic, Wauters, Joost, Spriet, I., Daele, R. Van, Bruggemann, R.J.M., Dreesen, Erwin, Depuydt, P., Rijnders, Bart J.A., Cotton, Frederic, Wauters, Joost, and Spriet, I.

Abstract

Contains fulltext : 233979.pdf (Publisher’s version ) (Closed access)

Published
2021

31. Concomitant use of isavuconazole and CYP3A4/5 inducers: Where pharmacogenetics meets pharmacokinetics

Author

Daele, R. Van, Debaveye, Y., Vos, R., Bleyenbergh, P. Van, Brüggemann, R.J.M., Dreesen, E., Elkayal, O., Guchelaar, H.J., Vermeersch, P., Lagrou, K., Spriet, I., Daele, R. Van, Debaveye, Y., Vos, R., Bleyenbergh, P. Van, Brüggemann, R.J.M., Dreesen, E., Elkayal, O., Guchelaar, H.J., Vermeersch, P., Lagrou, K., and Spriet, I.

Abstract

Item does not contain fulltext, BACKGROUND: Isavuconazole is a triazole antifungal drug, approved for the treatment of invasive aspergillosis and mucormycosis. Isavuconazole is metabolised by CYP3A4 and CYP3A5, and it has been shown that the CYP3A inducer rifampin reduces isavuconazole exposure. By extrapolation, the concomitant use of isavuconazole with moderate and strong CYP450 inducers is contraindicated, although it is known that some CYP450 inducers are less potent in comparison with rifampin. OBJECTIVES: We aim to document exposure to isavuconazole in patients concomitantly treated with a CYP450 inducer that is less potent compared to rifampin. Moreover, although it is well known that CYP3A enzymes are important for the metabolism of isavuconazole, this induction effect has never been studied in combination with the patient's CYP3A genotype. PATIENTS: We report three patients treated with both isavuconazole and a CYP3A inducer that is less potent compared to rifampin (rifabutin or phenobarbital), in whom we determined isavuconazole concentrations. RESULTS: These cases suggest that the CYP3A4/5 genotype is an important determinant for isavuconazole exposure and that it might also influence the CYP450 induction interaction. CONCLUSIONS: CYP3A inducers that are less potent compared to rifampin, may be combined with isavuconazole in patients with loss of CYP3A5 activity (CYP3A5*3/*3). Therapeutic drug monitoring is recommended during this combination. However, low-isavuconazole exposure was observed in the extensive metaboliser with CYP3A4*1/*1 and CYP3A5*1/*3 alleles.

Published
2021

32. Concomitant Treatment with Voriconazole and Flucloxacillin: A Combination to Avoid

Author

Daele, R. Van, Wauters, J., Cock, P. De, Buyle, F., Leys, J., Brantegem, P. Van, Gijsen, M., Annaert, P., Debaveye, Y., Lagrou, K., Peetermans, W.E., Brüggemann, R.J.M., Spriet, I., Daele, R. Van, Wauters, J., Cock, P. De, Buyle, F., Leys, J., Brantegem, P. Van, Gijsen, M., Annaert, P., Debaveye, Y., Lagrou, K., Peetermans, W.E., Brüggemann, R.J.M., and Spriet, I.

Abstract

Contains fulltext : 238513.pdf (Publisher’s version ) (Open Access), BACKGROUND: Voriconazole is an antifungal drug used as one of the first-line treatments for invasive aspergillosis. This drug is extensively metabolized, predominantly via cytochrome P450 enzymes. An interaction between flucloxacillin and voriconazole, leading to subtherapeutic voriconazole concentrations, has previously been reported. We aimed to demonstrate that flucloxacillin independently influences voriconazole exposure. METHODS: Patients from three Belgian hospitals, treated with a combination of voriconazole and flucloxacillin, were included in this retrospective study. Voriconazole concentrations were collected both in a timeframe with and without flucloxacillin co-treatment. Multivariate analyses were performed to study the independent effect of flucloxacillin treatment on voriconazole exposure and the possible influence of the flucloxacillin dose. RESULTS: Thirty-three patients were included in this study and 145 trough concentrations (51 with, and 94 without concomitant flucloxacillin treatment) were analyzed. The median (IQR) voriconazole trough concentration sampled during flucloxacillin co-treatment was 0.5 (0-1.8) mg/L, whereas samples without flucloxacillin co-treatment had a median (IQR) voriconazole trough concentration of 3.5 (1.7-5.1) mg/L (p = 0.002), while receiving similar voriconazole doses. Subtherapeutic concentrations (<1 mg/L) were observed in 69% and 7% of the samples with flucloxacillin co-treatment versus samples without flucloxacillin co-treatment, respectively. CONCLUSION: This study shows that flucloxacillin co-treatment independently decreases voriconazole exposure. Caution is needed when these two drugs are administered simultaneously.

Published
2021

33. Posaconazole for prevention of invasive pulmonary aspergillosis in critically ill influenza patients (POSA-FLU): a randomised, open-label, proof-of-concept trial

Author

Vanderbeke, L., Vanderbeke, L., Janssen, N.A.F., Bergmans, D.C.J.J., Bourgeois, M., Buil, J.B., Debaveye, Y., Depuydt, P., Feys, S., Hermans, G., Hoiting, O., van der Hoven, B., Jacobs, C., Lagrou, K., Lemiale, V., Lormans, P., Maertens, J., Meersseman, P., Megarbane, B., Nseir, S., van Oers, J.A.H., Reynders, M., Rijnders, B.J.A., Schouten, J.A., Spriet, I., Thevissen, K., Thille, A.W., Van Daele, R., van de Veerdonk, F.L., Verweij, P.E., Wilmer, A., Bruggemann, R.J.M., Wauters, J., Dutch Belgian Mycosis Study Grp, Vanderbeke, L., Vanderbeke, L., Janssen, N.A.F., Bergmans, D.C.J.J., Bourgeois, M., Buil, J.B., Debaveye, Y., Depuydt, P., Feys, S., Hermans, G., Hoiting, O., van der Hoven, B., Jacobs, C., Lagrou, K., Lemiale, V., Lormans, P., Maertens, J., Meersseman, P., Megarbane, B., Nseir, S., van Oers, J.A.H., Reynders, M., Rijnders, B.J.A., Schouten, J.A., Spriet, I., Thevissen, K., Thille, A.W., Van Daele, R., van de Veerdonk, F.L., Verweij, P.E., Wilmer, A., Bruggemann, R.J.M., Wauters, J., and Dutch Belgian Mycosis Study Grp

Abstract

Purpose Influenza-associated pulmonary aspergillosis (IAPA) is a frequent complication in critically ill influenza patients, associated with significant mortality. We investigated whether antifungal prophylaxis reduces the incidence of IAPA. Methods We compared 7 days of intravenous posaconazole (POS) prophylaxis with no prophylaxis (standard-of-care only, SOC) in a randomised, open-label, proof-of-concept trial in patients admitted to an intensive care unit (ICU) with respiratory failure due to influenza (ClinicalTrials.gov, NCT03378479). Adult patients with PCR-confirmed influenza were block randomised (1:1) within 10 days of symptoms onset and 48 h of ICU admission. The primary endpoint was the incidence of IAPA during ICU stay in patients who did not have IAPA within 48 h of ICU admission (modified intention-to-treat (MITT) population). Results Eighty-eight critically ill influenza patients were randomly allocated to POS or SOC. IAPA occurred in 21 cases (24%), the majority of which (71%, 15/21) were diagnosed within 48 h of ICU admission, excluding them from the MITT population. The incidence of IAPA was not significantly reduced in the POS arm (5.4%, 2/37) compared with SOC (11.1%, 4/36; between-group difference 5.7%; 95% CI - 10.8 to 21.7; p = 0.32). ICU mortality of early IAPA was high (53%), despite rapid antifungal treatment. Conclusion The higher than expected incidence of early IAPA precludes any definite conclusion on POS prophylaxis. High mortality of early IAPA, despite timely antifungal therapy, indicates that alternative management strategies are required. After 48 h, still 11% of patients developed IAPA. As these could benefit from prophylaxis, differentiated strategies are likely needed to manage IAPA in the ICU.

Published
2021

34. Global guideline for the diagnosis and management of rare yeast infections: an initiative of the ECMM in cooperation with ISHAM and ASM

Author

Chen, S. C. -A., Perfect, J., Colombo, A. L., Cornely, O. A., Groll, A. H., Seidel, D., Albus, K., de Almeida, J. N., Garcia-Effron, G., Gilroy, N., Lass-Florl, C., Ostrosky-Zeichner, L., Pagano, L., Papp, T., Rautemaa-Richardson, R., Salmanton-Garcia, J., Spec, A., Steinmann, J., Arikan-Akdagli, S., Arenz, D. E., Sprute, R., Duran-Graeff, L., Freiberger, T., Girmenia, C., Harris, M., Kanj, S. S., Roudbary, M., Lortholary, O., Meletiadis, J., Segal, E., Tuon, F. F., Wiederhold, N., Bicanic, T., Chander, J., Chen, Y. -C., Hsueh, P. -R., Ip, M., Munoz, P., Spriet, I., Temfack, E., Thompson, L., Tortorano, A. M., Velegraki, A., Govender, N. P., Pagano L. (ORCID:0000-0001-8287-928X), Chen, S. C. -A., Perfect, J., Colombo, A. L., Cornely, O. A., Groll, A. H., Seidel, D., Albus, K., de Almeida, J. N., Garcia-Effron, G., Gilroy, N., Lass-Florl, C., Ostrosky-Zeichner, L., Pagano, L., Papp, T., Rautemaa-Richardson, R., Salmanton-Garcia, J., Spec, A., Steinmann, J., Arikan-Akdagli, S., Arenz, D. E., Sprute, R., Duran-Graeff, L., Freiberger, T., Girmenia, C., Harris, M., Kanj, S. S., Roudbary, M., Lortholary, O., Meletiadis, J., Segal, E., Tuon, F. F., Wiederhold, N., Bicanic, T., Chander, J., Chen, Y. -C., Hsueh, P. -R., Ip, M., Munoz, P., Spriet, I., Temfack, E., Thompson, L., Tortorano, A. M., Velegraki, A., Govender, N. P., and Pagano L. (ORCID:0000-0001-8287-928X)

Abstract

Uncommon, or rare, yeast infections are on the rise given increasing numbers of patients who are immunocompromised or seriously ill. The major pathogens include those of the genera Geotrichum, Saprochaete, Magnusiomyces, and Trichosporon (ie, basidiomycetes) and Kodamaea, Malassezia, Pseudozyma (ie, now Moesziomyces or Dirkmeia), Rhodotorula, Saccharomyces, and Sporobolomyces (ie, ascomycetes). A considered approach to the complex, multidisciplinary management of infections that are caused by these pathogens is essential to optimising patient outcomes; however, management guidelines are either region-specific or require updating. In alignment with the One World–One Guideline initiative to incorporate regional differences, experts from diverse geographical regions analysed publications describing the epidemiology and management of the previously mentioned rare yeasts. This guideline summarises the consensus recommendations with regards to the diagnostic and therapeutic options for patients with these rare yeast infections, with the intent of providing practical assistance in clinical decision making. Because there is less clinical experience of patients with rare yeast infections and studies on these patients were not randomised, nor were groups compared, most recommendations are not robust in their validation but represent insights by use of expert opinions and in-vitro susceptibility results. In this Review, we report the key features of the epidemiology, diagnosis, antifungal susceptibility, and treatment outcomes of patients with Geotrichum, Saprochaete, Magnusiomyces, and Trichosporon spp infections.

Published
2021

39. Review of influenza-associated pulmonary aspergillosis in ICU patients and proposal for a case definition: an expert opinion

Author

Verweij, P.E., Rijnders, BJA, Brüggemann, RJM, Azoulay, E., Bassetti, M., Blot, S., Calandra, T., Clancy, C.J., Cornely, O.A., Chiller, T., Depuydt, P., Giacobbe, D.R., Janssen, NAF, Kullberg, B.J., Lagrou, K., Lass-Flörl, C., Lewis, R.E., Liu, P.W., Lortholary, O., Maertens, J., Martin-Loeches, I., Nguyen, M.H., Patterson, T.F., Rogers, T.R., Schouten, J.A., Spriet, I., Vanderbeke, L., Wauters, J., and van de Veerdonk, F.L.

Subjects
Antifungal Agents/therapeutic use, Aspergillus/isolation & purification, Betacoronavirus, Bronchoalveolar Lavage Fluid/chemistry, Bronchoalveolar Lavage Fluid/microbiology, Coronavirus Infections/complications, Humans, Influenza, Human/complications, Intensive Care Units, Mannans/analysis, Pandemics, Pneumonia, Viral/complications, Pulmonary Aspergillosis/diagnosis, Pulmonary Aspergillosis/etiology, Pulmonary Aspergillosis/prevention & control, COVID-19, ICU, Influenza, Invasive aspergillosis, Viral pneumonia
Abstract

Invasive pulmonary aspergillosis is increasingly reported in patients with influenza admitted to the intensive care unit (ICU). Classification of patients with influenza-associated pulmonary aspergillosis (IAPA) using the current definitions for invasive fungal diseases has proven difficult, and our aim was to develop case definitions for IAPA that can facilitate clinical studies. A group of 29 international experts reviewed current insights into the epidemiology, diagnosis and management of IAPA and proposed a case definition of IAPA through a process of informal consensus. Since IAPA may develop in a wide range of hosts, an entry criterion was proposed and not host factors. The entry criterion was defined as a patient requiring ICU admission for respiratory distress with a positive influenza test temporally related to ICU admission. In addition, proven IAPA required histological evidence of invasive septate hyphae and mycological evidence for Aspergillus. Probable IAPA required the detection of galactomannan or positive Aspergillus culture in bronchoalveolar lavage (BAL) or serum with pulmonary infiltrates or a positive culture in upper respiratory samples with bronchoscopic evidence for tracheobronchitis or cavitating pulmonary infiltrates of recent onset. The IAPA case definitions may be useful to classify patients with COVID-19-associated pulmonary aspergillosis (CAPA), while awaiting further studies that provide more insight into the interaction between Aspergillus and the SARS-CoV-2-infected lung. A consensus case definition of IAPA is proposed, which will facilitate research into the epidemiology, diagnosis and management of this emerging acute and severe Aspergillus disease, and may be of use to study CAPA.

Published
2020

40. Itraconazole for COVID-19: Preclinical Studies and a Proof-of-Concept Pilot Clinical Study

Author

Ewout Landeloos, Tatjana Geukens, Joost Wauters, Geert Meyfroidt, Linden LVd, Iwein Gyselinck, Matthias M. Engelen, Rita Vos, Lana Langendries, Spriet I, Peter Verhamme, Laure-Anne Teuwen, Birgit Weynand, Kaptein Sjf, Laurens Liesenborghs, Leen Delang, Thomas Vanassche, Sofie Jacobs, Eric Van Wijngaerden, Johan Neyts, Wim Janssens, Horst St, Helga Ceunen, Dirk Jochmans, Pieter Vermeersch, Barbara Debaveye, Geert Verbeke, Erwin Dreesen, Ann Belmans, Joana Rocha-Pereira, Paul De Munter, Geldhof, Timothy Devos, Robbert Boudewijns, and Bert Vandenberk

Subjects
medicine.medical_specialty, business.industry, Itraconazole, Antifungal drug, Interim analysis, Clinical trial, Internal medicine, Good clinical practice, medicine, Dosing, business, Viral load, Declaration of Helsinki, medicine.drug
Abstract

Background: Drug repurposing is an attractive strategy to rapidly develop affordable therapy against COVID-19. The antifungal drug itraconazole exerts in vitro activity against SARS-CoV-2 comparable to that of hydroxychloroquine. Preclinical and clinical studies are required to investigate if itraconazole is effective for the treatment and/or prevention of COVID-19. Methods: Due to the initial absence of preclinical models the effect of itraconazole was explored in a clinical, proof-of-concept, open-label, single-center study, in which hospitalized patients with COVID-19 were randomly assigned to receive standard of care with or without itraconazole. The primary outcome was the cumulative score of the clinical status until day 15 based on the 7-point ordinal scale of the World Health Organization. Other outcomes included time to sustained clinical improvement, duration of supplemental oxygen and evolution of nasopharyngeal viral load. In parallel, itraconazole was evaluated in a newly established hamster model of acute SARS-CoV-2 infection and transmission, as soon as the model was validated. Findings: In the hamster acute infection model, itraconazole did not reduce viral load in lungs, stools or ileum, despite adequate plasma and lung drug concentrations. In the transmission model, itraconazole failed to prevent viral transmission. The clinical trial was prematurely discontinued after evaluation of the preclinical studies and interim analysis that showed no trends for a more favorable outcome with itraconazole: mean cumulative score of the clinical status 49 vs 47, ratio of geometric means 1.01 (95% CI 0.85 to 1.19), median time to clinical improvement 10 vs 9 days, hazard ratio 0.94 (95% CI 0.56 to 1.60) for itraconazole vs standard of care. Interpretation: Despite in vitro activity, itraconazole was not effective in a preclinical COVID-19 hamster model. A proof-of-concept clinical study was ended prematurely because of futility. Trial Registration: (EudraCT 2020-001243-15) Funding: Covid-19-Fund KU Leuven, Research Foundation - Flanders (FWO), Horizon 2020, Bill and Melinda Gates Foundation Declaration of Interests: Initial dug screening and discovery of the antiviral effect of itraconazole was done in collaboration with Johnson & Johnson and described in a separate manuscript. Scientists from Johnson & Johnson also performed drug measurements on hamster samples and provided guidance on the dosing regimens for the preclinical studies. The company had no role in the design, execution, analysis, publication or funding of the clinical trial. Author Conflict of Interests: None to declare. Ethics Approval Statement: The institutional Ethical Committee approved all animal experiments (license P065-2020). The study was conducted in accordance with the International Conference on Harmonization Guidelines for Good Clinical Practice and the Declaration of Helsinki. The protocol was approved by the institutional Ethics Committee and by the Belgian Federal Agency for Medicines and Health Products (EudraCT 2020-001243-15). The trial was part of the DAWn clinical studies.

Published
2020
Full Text
View/download PDF

41. European confederation of medical mycology expert consult-An ECMM excellence center initiative

Author

Koehler, P., Denis, B., Denning, D.W., Gangneux, J.P., Hoenigl, M., Kontoyiannis, D.P., Krause, R., Lagrou, K., Lass-Florl, C., Maertens, J., Marekovic, I., Meis, J.F.G.M., Molina, J.M., Plesko, S., Prattes, J., Rath, P.M., Rautemaa-Richardson, R., Richardson, M., Segal, E., Seidel, D., Spriet, I., Steinmann, J., Verweij, P.E., Cornely, O.A., Koehler, P., Denis, B., Denning, D.W., Gangneux, J.P., Hoenigl, M., Kontoyiannis, D.P., Krause, R., Lagrou, K., Lass-Florl, C., Maertens, J., Marekovic, I., Meis, J.F.G.M., Molina, J.M., Plesko, S., Prattes, J., Rath, P.M., Rautemaa-Richardson, R., Richardson, M., Segal, E., Seidel, D., Spriet, I., Steinmann, J., Verweij, P.E., and Cornely, O.A.

Abstract

Contains fulltext : 220076.pdf (Publisher’s version ) (Open Access), OBJECTIVES: Difficult-to-treat invasive fungal infections require infectious diseases expert consultation to improve treatment outcome and increase survival rates. METHODS: The European Confederation of Medical Mycology (ECMM) intends to provide expert help free of charge by a newly founded ECMM Expert Consultation Service for medical centres around the globe seeking advice when there is no fungal infection consultant available. The expert consult will provide recommendations and broad expertise on difficult-to-treat invasive fungal infections (eg azole-resistant Aspergillus species, Candida auris, mucormycosis) to improve diagnostic and therapeutic management and outcome. RESULTS: The initiative plans global outreach through video conferencing between ECMM Excellence Centers and treating physicians. FungiScope((R)) registries will be used to structure case information and to evaluate the impact of the collegial advice system at regular intervals. Advice will follow recent guidelines, and EQUAL Scores will be used to measure guideline adherence. CONCLUSIONS: Infectious diseases expert consultation should be an integral component of care for patients with difficult-to-treat invasive fungal infections. The ECMM Expert Consult will attend to this matter on a global scale.

Published
2020

42. Outpatient parenteral antifungal therapy (OPAT) for invasive fungal infections with intermittent dosing of liposomal amphotericin B

Author

van de Peppel, R.J., Schauwvlieghe, A., van Daele, R., Spriet, I., van’t Wout, J.W., Brüggemann, R.J.M., Rijnders, B.J.A. (Bart), Hendriks, B.J.C., de Boer, M.G.J., van de Peppel, R.J., Schauwvlieghe, A., van Daele, R., Spriet, I., van’t Wout, J.W., Brüggemann, R.J.M., Rijnders, B.J.A. (Bart), Hendriks, B.J.C., and de Boer, M.G.J.

Abstract

Triazole resistant A. fumigatus has been documented in many parts of the world. In the Netherlands, incidence is now above 10% and results in the need for long-term parenteral therapy with liposomal amphotericin B (LAmB). The long terminal half-life of LAmB suggests that intermittent dosing could be effective, making the application of outpatient antifungal therapy (OPAT) possible. Here, we report our experience with the use of OPAT for Invasive Fungal Infections (IFI). All adult patients treated with LAmB with a 2 or 3 times weekly administration via the outpatient departments in four academic tertiary care centers in the Netherlands and Belgium since January 2010 were included in our analysis. Patient characteristics were collected, as well as information about diagnostics, therapy dose and duration, toxicity, treatment history and outcome of the IFI. In total, 18 patients were included. The most frequently used regimen (67%) was 5 mg/kg 3 times weekly. A partial response to the daily treatment prior to discharge was confirmed by CT-scan in 17 (94%) of patients. A favorable outcome was achieved in 13 (72%) patients. Decrease in renal function occurred in 10 (56%) cases but was reversible in all and was treatment limiting in one patient only. The 100-day mortality and 1-year mortality after initiation of OPAT were 0% and 6%, respectively. In a selected population, and after confirmation of initial response to treatment, our data support the use of OPAT with LAmB for treatment of IFI in an intermittent dosing regimen.

Published
2020
Full Text
View/download PDF

43. Review of influenza-associated pulmonary aspergillosis in ICU patients and proposal for a case definition: an expert opinion

Author

Verweij, P.E. (Paul), Rijnders, B.J.A. (Bart), Brüggemann, M. (Monika), Azoulay, E. (Elie), Bassetti, M. (Matteo), Blot, S. (Stijn), Calandra, T. (Thierry), Clancy, C.J. (Cornelius J.), Cornely, O.A. (Oliver A.), Chiller, T. (Tom), Depuydt, P. (Pieter), Giacobbe, D.R. (Daniele Roberto), Janssen, N.A.F. (Nico A. F.), Kullberg, B.J. (Bart Jan), Lagrou, K. (Katrien), Lass-Flörl, C. (Cornelia), Lewis, R.E. (Russell E.), Liu, P.W.-L. (Peter Wei-Lun), Lortholary, O. (Olivier), Maertens, J. (Johan), Martin-Loeches, I., Nguyen, M.H. (M. Hong), Patterson, T.F. (Thomas F.), Rogers, T.R. (Thomas R.), Schouten, J.A. (Jeroen A.), Spriet, I. (Isabel), Vanderbeke, L. (Lore), Wauters, J. (Joost), Veerdonk, F. (Frank) van de, Verweij, P.E. (Paul), Rijnders, B.J.A. (Bart), Brüggemann, M. (Monika), Azoulay, E. (Elie), Bassetti, M. (Matteo), Blot, S. (Stijn), Calandra, T. (Thierry), Clancy, C.J. (Cornelius J.), Cornely, O.A. (Oliver A.), Chiller, T. (Tom), Depuydt, P. (Pieter), Giacobbe, D.R. (Daniele Roberto), Janssen, N.A.F. (Nico A. F.), Kullberg, B.J. (Bart Jan), Lagrou, K. (Katrien), Lass-Flörl, C. (Cornelia), Lewis, R.E. (Russell E.), Liu, P.W.-L. (Peter Wei-Lun), Lortholary, O. (Olivier), Maertens, J. (Johan), Martin-Loeches, I., Nguyen, M.H. (M. Hong), Patterson, T.F. (Thomas F.), Rogers, T.R. (Thomas R.), Schouten, J.A. (Jeroen A.), Spriet, I. (Isabel), Vanderbeke, L. (Lore), Wauters, J. (Joost), and Veerdonk, F. (Frank) van de

Abstract

Purpose: Invasive pulmonary aspergillosis is increasingly reported in patients with influenza admitted to the intensive care unit (ICU). Classification of patients with influenza-associated pulmonary aspergillosis (IAPA) using the current definitions for invasive fungal diseases has proven difficult, and our aim was to develop case definitions for IAPA that can facilitate clinical studies. Methods: A group of 29 international experts reviewed current insights into the epidemiology, diagnosis and management of IAPA and proposed a case definition of IAPA through a process of informal consensus. Results: Since IAPA may develop in a wide range of hosts, an entry criterion was proposed and not host factors. The entry criterion was defined as a patient requiring ICU admission for respiratory distress with a positive influenza test temporally related to ICU admission. In addition, proven IAPA required histological evidence of invasive septate hyphae and mycological evidence for Aspergillus. Probable IAPA required the detection of galactomannan or positive Aspergillus culture in bronchoalveolar lavage (BAL) or serum with pulmonary infiltrates or a positive culture in upper respiratory samples with bronchoscopic evidence for tracheobronchitis or cavitating pulmonary infiltrates of recent onset. The IAPA case definitions may be useful to classify patients with COVID-19-associated pulmonary aspergillosis (CAPA), while awaiting further studies that provide more insight into the interaction between Aspergillus and the SARS-CoV-2-infected lung. Conclusion: A consensus case definition of IAPA is proposed, which will facilitate research into the epidemiology, diagnosis and management of this emerging acute and severe Aspergillus disease, and may be of use to study CAPA.

Published
2020
Full Text
View/download PDF

45. Review of influenza-associated pulmonary aspergillosis in ICU patients and proposal for a case definition: an expert opinion

Author

Verweij, P, Rijnders, Bart, Brüggemann, RJM, Azoulay, E, Bassetti, M, Blot, S, Calandra, T, Clancy, CJ, Cornely, OA, Chiller, T, Depuydt, P, Giacobbe, DR, Janssen, N, Kullberg, BJ, Lagrou, K, Lass-Flörl, C, Lewis, RE, Liu, P, Lortholary, O, Maertens, JA, Martin-Loeches, I, Nguyen, MP, Patterson, TF, Rogers, T T, Schouten, J, Spriet, I, Vanderbeke, L, Wauters, J, van de Veerdonk, FL, Verweij, P, Rijnders, Bart, Brüggemann, RJM, Azoulay, E, Bassetti, M, Blot, S, Calandra, T, Clancy, CJ, Cornely, OA, Chiller, T, Depuydt, P, Giacobbe, DR, Janssen, N, Kullberg, BJ, Lagrou, K, Lass-Flörl, C, Lewis, RE, Liu, P, Lortholary, O, Maertens, JA, Martin-Loeches, I, Nguyen, MP, Patterson, TF, Rogers, T T, Schouten, J, Spriet, I, Vanderbeke, L, Wauters, J, and van de Veerdonk, FL

Published
2020

Catalog

Books, media, physical & digital resources
See catalog results