Your search keyword '"Rene Bouw"' showing total 12 results

1. Design of a patient‐ and investigator‐blind, randomized, placebo‐controlled study to evaluate efficacy, safety, and tolerability of bepranemab, UCB0107, in prodromal to mild Alzheimer’s disease: The TOGETHER Study, AH0003

Author

Matthew E Barton, William Byrnes, Irene Rebollo Mesa, Jos Bloemers, Ralph Paul Maguire, Rene Bouw, Ina Tesseur, Colin Ewen, and Philip Scheltens

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Published

2021

2. Pharmacodynamics of Oral Ganciclovir and Valganciclovir in Solid Organ Transplant Recipients

Author

Atul Humar, Barbara D. Alexander, Nigel Heaton, Emily A. Blumberg, Kenneth Washburn, Edward A. Dominguez, Rene Bouw, Carlos V. Paya, Richard B. Freeman, Hugh Wiltshire, Mark D. Pescovitz, and Klaas P. Zuideveld

Subjects

Male, Ganciclovir, medicine.medical_specialty, viruses, Administration, Oral, Cytomegalovirus, Viremia, Neutropenia, Antiviral Agents, Gastroenterology, Postoperative Complications, Double-Blind Method, stomatognathic system, Internal medicine, medicine, Humans, Valganciclovir, Transplantation, Leukopenia, business.industry, Body Weight, virus diseases, Organ Transplantation, Middle Aged, Viral Load, biochemical phenomena, metabolism, and nutrition, medicine.disease, Body Height, Surgery, surgical procedures, operative, Area Under Curve, Pharmacodynamics, Cytomegalovirus Infections, Female, medicine.symptom, business, Viral load, medicine.drug

Abstract

Background A randomized, double-blind study was conducted to evaluate the pharmacokinetics of ganciclovir following oral administration of ganciclovir or valganciclovir for prophylaxis of cytomegalovirus (CMV) disease in solid organ transplant recipients (n = 240/372). Methods The correlations between individual exposure to ganciclovir during prophylaxis, with CMV viremia incidence during and after treatment, CMV disease up to 12 months posttransplant, and hematological toxicity were assessed. Results Mean daily areas under the curve (AUCs) of ganciclovir from valganciclovir and oral ganciclovir were 46.3 +/- 15.2 and 28.0 +/- 10.9 microg.h/ml (mean +/- SD), respectively. Viremia was suppressed during prophylaxis when exposure to ganciclovir was 40-50 microg.h/ml, AUCs typical of those achieved in valganciclovir-treated patients. The development of viremia 1 month after ending prophylaxis was also reduced with higher ganciclovir AUC (median predicted incidence, 20% and 10% at AUCs of 33 and 50 microg h/ml, respectively). The development of CMV disease within 1 year of transplant was 17.6% and independent of prophylactic exposure to ganciclovir. There was only a weak tendency to increased neutropenia and leukopenia with higher ganciclovir exposure. Conclusions The greater systemic exposure to ganciclovir delivered by valganciclovir was associated with delayed development of viremia. There was only a weak association between AUC and hematological toxicity.

Published

2005

3. Blood-brain barrier transport of morphine in patients with severe brain trauma

Author

Per Ederoth, Rene Bouw, Urban Ungerstedt, C. Johan F. Lundberg, Margareta Hammarlund-Udenaes, Carl-Henrik Nordström, and Karin Tunblad

Subjects

Pharmacology, Microdialysis, medicine.medical_specialty, Neurology, business.industry, Blood–brain barrier, medicine.disease, Confidence interval, Central nervous system disease, Lesion, medicine.anatomical_structure, Endocrinology, Pharmacokinetics, Internal medicine, Anesthesia, medicine, Morphine, Pharmacology (medical), medicine.symptom, business, medicine.drug

Abstract

Results The area under the concentration-time curve (AUC) ratio of unbound morphine in brain tissue to plasma was 0.64 (95% confidence interval 0.40, 0.87) in 'better' brain tissue ( P < 0.05 vs. the subcutaneous fat/plasma ratio), 0.78 (0.49, 1.07) in 'worse' brain tissue and 1.00 (0.86, 1.13) in subcutaneous fat. The terminal half-life and T max were longer in the brain vs. plasma and fat, respectively. The relative recovery for morphine was higher in 'better' than in 'worse' brain tissue. The T max value tended to be shorter in 'worse' brain tissue.

Published

2004

4. Increased blood-brain barrier permeability of morphine in a patient with severe brain lesions as determined by microdialysis

Author

Margareta Hammarlund-Udenaes, Johan Lundberg, Per Ederoth, Rene Bouw, Carl-Henrik Nordström, and Urban Ungerstedt

Subjects

Microdialysis, business.industry, Central nervous system, Adipose tissue, General Medicine, Human brain, Blood–brain barrier, Anesthesiology and Pain Medicine, medicine.anatomical_structure, Anesthesia, Extracellular fluid, Morphine, Arterial blood, Medicine, business, medicine.drug

Abstract

Intracerebral microdialysis was utilised to obtain information regarding how morphine is transported across the blood-brain barrier (BBB). In a patient with a severe brain injury, we measured simultaneously unbound extracellular fluid (ECF) concentrations of morphine in human brain and in subcutaneous fat tissue, which were compared to morphine levels in arterial blood. This report shows an increase in morphine levels near the trauma site in the brain compared to uninjured brain tissue. The half-life of morphine in uninjured and injured brain tissue of 178 min and 169 min, respectively, were comparable but were longer than in blood (64 min) and adipose tissue (63 min). This indicates that morphine is retained in brain tissue for a longer time than what could be expected from the blood concentration-time profile. These results show the potential of the microdialysis technique in providing new information regarding the pharmacokinetics of drug in the human brain close to the trauma site and in macroscopically intact tissue.

Published

2001

5. Mycophenolic acid exposure after administration of mycophenolate mofetil in the presence and absence of cyclosporin in renal transplant recipients

Author

Richard D. Mamelok, Dirk Kuypers, Josep M. Grinyó, Flavio Vincenti, Henrik Ekberg, Bjoern Nashan, Rene Bouw, and Paul Snell

Subjects

Adult, Graft Rejection, Male, medicine.medical_specialty, Time Factors, Urology, Pharmacology, Mycophenolate, Mycophenolic acid, Nephrotoxicity, Young Adult, Pharmacokinetics, Medicine, Humans, Pharmacology (medical), Drug Interactions, Prospective Studies, Kidney transplantation, Aged, business.industry, Middle Aged, Mycophenolic Acid, medicine.disease, Ciclosporin, Kidney Transplantation, Transplantation, Pharmacodynamics, Cyclosporine, Drug Therapy, Combination, Female, business, medicine.drug

Abstract

The pharmacokinetics of mycophenolic acid (MPA) are complex, with large interindividual variability over time. There are also well documented interactions with cyclosporin, and assessment of MPA exposure is therefore necessary when reducing or stopping cyclosporin therapy. Here we report on the pharmacokinetic and pharmacodynamic behaviour of MPA in renal transplant patients on standard dose, reduced dose and no cyclosporin. STUDY DESIGN: The CAESAR study, a prospective 12-month study in primary renal allograft recipients, was designed to determine whether mycophenolate mofetil-based regimens containing either low-dose cyclosporin or low-dose cyclosporin withdrawn by 6 months could minimize nephrotoxicity and improve renal function without an increase in acute rejection compared with a mycophenolate mofetil-based regimen containing standard-dose cyclosporin. PATIENTS AND METHODS: A subset of patients from the CAESAR study contributed to this pharmacokinetic analysis of MPA exposure. Blood samples were taken over one dosing interval on day 7 and at months 3, 7 and 12 post-transplantation. The sampling time points were predose, 20, 40 and 75 minutes and 2, 3, 4, 6, 8 and 12 hours after mycophenolate mofetil dosing. Assessments included plasma concentrations of MPA and mycophenolic acid glucuronide (MPAG) and cyclosporin trough concentrations. The area under the plasma concentration-time curve (AUC) from 0 to 12 hours (AUC(12)) for MPA was the primary pharmacokinetic parameter, and the AUC(12) for MPAG was the secondary parameter. RESULTS: In total, 536 de novo renal allograft recipients were randomized in the CAESAR study. Of these, 114 patients were entered into the pharmacokinetic substudy and 110 patients contributed to the pharmacokinetic analysis. There was a rapid rise in MPA concentrations (median time to peak concentration 0.72-1.25 hours). At day 7 and month 3, the MPA AUC(12) values were similar in the cyclosporin withdrawal and low-dose cyclosporin groups (patients with the same cyclosporin target concentrations to month 6), while at 7 and 12 months, the values in the cyclosporin withdrawal group were higher than in the low-dose group (19.9% and 30.2% higher, respectively). MPA AUC(12) values in the standard-dose cyclosporin group were lower than in the other groups at all time points and increased over time. At all time points, the MPA peak plasma concentration was similar in all groups, and the MPAG concentrations rose more slowly than MPA concentrations. The ratio of the AUC from 6 to 12 hours/AUC(12) suggests that an increasing AUC in the cyclosporin withdrawal group is due to an increase in the enterohepatic recirculation. CONCLUSION: These findings are consistent with the hypothesis that cyclosporin inhibits the biliary secretion and/or hepatic extraction of MPAG, leading to a reduced rate of enterohepatic recirculation of MPA. Several concurrent mechanisms, such as cyclosporin-induced changes in renal tubular MPAG excretion and enhanced elimination of free MPA through competitive albumin binding with MPAG, can also contribute to the altered MPAG pharmacokinetics observed in the presence and absence of cyclosporin. ispartof: Clinical Pharmacokinetics vol:48 issue:5 pages:329-341 ispartof: location:Switzerland status: published

Published

2009

6. Pharmacokinetics, efficacy, and safety of mycophenolate mofetil in combination with standard-dose or reduced-dose tacrolimus in liver transplant recipients

Author

Matthew Bowles, Rene Bouw, Jürgen Klempnauer, Richard D. Mamelok, Paul Marotta, Faouzi Saliba, Angel Bernardos, Diane McKay, Björn Nashan, Peter Neuhaus, Rafael Bárcena, François Durand, David Patch, José Ignacio Herrero, Jane Ives, Gilles Mentha, and Matt Truman

Subjects

Adult, Male, medicine.medical_specialty, medicine.medical_treatment, Urology, Administration, Oral, Liver transplantation, Pharmacology, Mycophenolate, Mycophenolic acid, Tacrolimus, law.invention, Pharmacotherapy, Randomized controlled trial, Pharmacokinetics, law, Immunosuppressive Agents/administration & dosage/blood/*pharmacokinetics, medicine, Liver Transplantation, Humans, Drug Interactions, Infusions, Intravenous, Tacrolimus/administration & dosage/blood/*pharmacokinetics, Transplantation, Hepatology, ddc:617, business.industry, Middle Aged, Mycophenolic Acid, Treatment Outcome, Surgery, Drug Therapy, Combination, Female, Mycophenolic Acid/administration & dosage/*analogs & derivatives/blood/pharmacokinetics, Glucuronide, business, Immunosuppressive Agents, medicine.drug

Abstract

The pharmacokinetics of mycophenolate mofetil (MMF) in liver transplant recipients may change because of pharmacokinetic interactions with coadministered immunosuppressants or because changes in the enterohepatic anatomy may affect biotransformation of MMF to mycophenolic acid (MPA) and enterohepatic recirculation of MPA through the hydrolysis of mycophenolate acid glucuronide to MPA in the gut. In the latter case, the choice of formulation (oral versus intravenous) could have important clinical implications. We randomized liver transplant patients (n = 60) to standard (10-15 ng/mL) or reduced (5-8 ng/mL) trough levels of tacrolimus plus intravenous MMF followed by oral MMF (1 g twice daily) with corticosteroids. Pharmacokinetic sampling was performed after the last intravenous MMF dose, after the first oral MMF dose, and at selected times over 52 weeks. The efficacy and safety of the 2 regimens were also assessed. Twenty-eight and 27 patients in the tacrolimus standard-dose and reduced-dose groups, respectively, were evaluated. No significant differences between the tacrolimus standard-dose and reduced-dose groups were seen in dose-normalized MPA values of the time to the maximum plasma concentration (1.25 versus 1.28 hours), the maximum plasma concentration (15.5 +/- 7.93 versus 13.6 +/- 7.03 microg/mL), or the area under the concentration-time curve from 0 to 12 hours (AUC(0-12); 53.0 +/- 20.6 versus 43.8 +/- 15.5 microg h/mL) at week 26 or at any other time point. No relationship was observed between the tacrolimus trough or AUC(0-12) and MPA AUC(0-12). Exposure to MPA after oral and intravenous administration was similar. Safety and efficacy were similar in the two treatment groups. In conclusion, exposure to MPA is not a function of exposure to tacrolimus. The similar safety and efficacy seen with MMF plus standard or reduced doses of tacrolimus suggest that MMF could be combined with reduced doses of tacrolimus.

Published

2009

7. Development of a predictive limited sampling strategy for estimation of mycophenolic acid area under the concentration time curve in patients receiving concomitant sirolimus or cyclosporine

Author

Mark D. Pescovitz, Artur Nawrocki, Rene Bouw, Michal J. Figurski, and Leslie M. Shaw

Subjects

Adult, Male, Mean squared error, Mycophenolic acid, Standard deviation, Young Adult, Animal science, Glucuronides, Pharmacokinetics, Predictive Value of Tests, medicine, Humans, Pharmacology (medical), Chromatography, High Pressure Liquid, Aged, Pharmacology, Sirolimus, Chromatography, Models, Statistical, Dose-Response Relationship, Drug, Chemistry, Reproducibility of Results, Regression analysis, Middle Aged, Mycophenolic Acid, Kidney Transplantation, Dose–response relationship, Liver, Concomitant, Predictive value of tests, Area Under Curve, Cyclosporine, Regression Analysis, Female, Immunosuppressive Agents, medicine.drug

Abstract

Limited sampling strategies for estimation of the area under the concentration time curve (AUC) for mycophenolic acid (MPA) co-administered with sirolimus (SRL) have not been previously evaluated. The authors developed and validated 68 regression models for estimation of MPA AUC for two groups of patients, one with concomitant SRL (n = 24) and the second with concomitant cyclosporine (n=14), using various combinations of time points between 0 and 4 hours after drug administration. To provide as robust a model as possible, a dataset-splitting method similar to a bootstrap was used. In this method, the dataset was randomly split in half 100 times. Each time, one half of the data was used to estimate the equation coefficients, and the other half was used to test and validate the models. Final models were obtained by calculating the median values of the coefficients. Substantial differences were found in the pharmacokinetics of MPA between these groups. The mean MPA AUC as well as the standard deviation was much greater in the SRL group, 56.4 +/- 23.5 mg.h/L, compared with 30.4 +/- 11.0 mg.h/L in the cyclosporine group (P < 0.001). Mean maximum concentration was also greater in the SRL group: 16.4 +/- 7.7 mg/L versus 11.7 +/- 7.1mg/L (P < 0.005). The second absorption peak in the pharmacokinetic profile, presumed to result from enterohepatic recycling of glucuronide MPA, was observed in 70% of the profiles in the SRL group and in 35% of profiles from the cyclosporine group. Substantial differences in the predictive performance of the regression models, based on the same time points, were observed between the two groups. The best model for the SRL group was based on 0 (trough) and 40 minutes and 4 hour time points with R2, root mean squared error, and predictive performance values of 0.82, 10.0, and 78%, respectively. In the cyclosporine group, the best model was 0 and 40 minutes and 2 hours, with R2, RMSE, and predictive performance values of 0.86, 4.1, and 83%, respectively. The model with 2 hours as the last time point is also recommended for the SRL group for practical reasons, with the above parameters of 0.77, 11.3, and 69%, respectively.

Published

2008

8. Pharmacokinetics of mycophenolate mofetil in stable pediatric liver transplant recipients receiving mycophenolate mofetil and cyclosporine

Author

Steven J. Lobritto, Rene Bouw, Paul Snell, Mimi Leung, Philip J. Rosenthal, and Richard D. Mamelok

Subjects

Graft Rejection, medicine.medical_specialty, medicine.medical_treatment, Urology, Liver transplantation, Pharmacology, Mycophenolate, Mycophenolic acid, Pharmacokinetics, medicine, Humans, Child, Transplantation, Hepatology, business.industry, Infant, Mean age, Mycophenolic Acid, Liver Transplantation, Area Under Curve, Child, Preschool, Cyclosporine, Surgery, Transplant patient, Drug Therapy, Combination, Adult liver, business, Immunosuppressive Agents, medicine.drug

Abstract

There are few pharmacokinetic data for mycophenolate mofetil (MMF) when used in combination with cyclosporine (CsA) in pediatric liver transplant recipients. The aim of this study was to assess the pharmacokinetics of MMF in stable pediatric liver transplant patients and estimate the dose of MMF required to provide a mycophenolic acid (MPA) exposure similar to that observed in adult liver transplant recipients receiving the recommended dose of MMF (target area under the plasma concentration-time curve from 0 to 12 hours [AUC(0-12)] for MPA of 29 mug.hour/mL in the immediate posttransplantation period and 58 microg x hour/mL after 6 months). A 12-hour pharmacokinetic profile was collected for 8 pediatric patients (mean age 20.9 months) on stable doses of MMF and CsA who had received a liver transplant > or = 6 months prior to entry and who had started on MMF within 2 weeks of transplantation. Mean MMF dosage was 285 mg/m(2) (range, 200-424 mg/m(2)). Of 8 patients, 7 had a MPA AUC(0-12) (range, 11.0-37.2 microg x hour/mL) well below the target. One patient had an AUC(0-12) > or = 58 microg x hour/mL but was considered an outlier and was excluded from analyses. Mean MPA AUC(0-12) and maximum plasma concentration values were 22.7 +/- 10.5 microg x hour/mL and 7.23 +/- 3.27 microg/mL, respectively; values normalized to 600 mg/m(2) (the approved pediatric dose in renal transplantation) were 47.0 +/- 21.8 microg x hour/mL and 14.5 +/- 4.21 microg/mL. In conclusion, assuming that MPA exhibits linear pharmacokinetics, when used in combination with CsA, a MMF dose of 740 mg/m(2) twice daily would be recommended in pediatric liver transplant recipients to achieve MPA exposures similar to those observed in adult liver transplant recipients. This finding should be confirmed by a prospective trial.

Published

2007

9. Concentrations of Gemifloxacin at the Target Site in Healthy Volunteers after a Single Oral Dose

Author

Mathias Stahl, Edith Lackner, Rene Bouw, Hans Georg Eichler, Petra Zeleny, Christian Joukhadar, Markus Müller, Martin Brunner, and Florian Islinger

Subjects

Drug, Adult, Male, Sexually Transmitted Diseases, Bacterial, Gemifloxacin, medicine.drug_class, media_common.quotation_subject, Microdialysis, Antibiotics, Biological Availability, Gemifloxacin Mesylate, Pharmacology, Pharmacokinetics, Oral administration, Medicine, Humans, Pharmacology (medical), Naphthyridines, Adverse effect, Muscle, Skeletal, media_common, Antibacterial agent, business.industry, Anti-Bacterial Agents, Infectious Diseases, Adipose Tissue, Area Under Curve, business, medicine.drug, Fluoroquinolones, Half-Life

Abstract

Gemifloxacin, one of the recently developed fluoroquinolones (gemifloxacin mesylate, Factive, and SB-265805), exerts a strong in vitro antibacterial activity against a broad spectrum of pathogens (3, 18). The adverse reaction profile is similar to that of older members of this class (3, 24). Previous studies have shown that gemifloxacin displays a favorable plasma pharmacokinetic (PK) profile allowing a once-daily dosing regimen (1, 2). Gemifloxacin was approved by the U.S. Food and Drug Administration in April 2003 for infections of the upper respiratory tract (24), but initially the manufacturer did not seek to receive approval for the therapy of soft tissue infections (STIs). Regulatory authorities such as the Food and Drug Administration and the European Agency for the Evaluation of Medicinal Products advocate that the concentration of an antibiotic at the target site needs to be determined before the approval of drugs is extended to new indications (9, 10). This determination allows for the assessment of the bacterial growth inhibition and killing potential of an antimicrobial agent at the relevant site of drug action. It is generally accepted that for most infections, this site is represented by the interstitial space fluid (ISF) of the tissue (23), and the in vivo microdialysis technique is capable of sampling interstitial fluid at the target site (8, 20). In the present study, we used microdialysis to investigate the potential of gemifloxacin to penetrate skeletal muscle and subcutaneous adipose tissue in healthy volunteers. Thus, we clarified whether gemifloxacin might be an appropriate therapeutic option for the treatment of STIs. For this purpose, the PK of gemifloxacin was measured in the ISF of soft tissues and compared to the PK of this drug in plasma.

Published

2004

10. Zilucoplan in patients with acute hypoxic respiratory failure due to COVID-19 (ZILU-COV): A structured summary of a study protocol for a randomised controlled trial

Author

Jozefien Declercq, Cedric Bosteels, Karel Van Damme, Elisabeth De Leeuw, Bastiaan Maes, Ans Vandecauter, Stefanie Vermeersch, Anja Delporte, Bénédicte Demeyere, Marnik Vuylsteke, Marianna Lalla, Trevor Smart, Laurent Detalle, René Bouw, Johannes Streffer, Thibo Degeeter, Marie Vergotte, Tanguy Guisez, Eva Van Braeckel, Catherine Van Der Straeten, and Bart N. Lambrecht

Subjects

COVID-19, Randomised controlled trial, protocol, zilucoplan, complement system, complement C5 inhibition, Medicine (General), R5-920

Abstract

Abstract Objectives Zilucoplan (complement C5 inhibitor) has profound effects on inhibiting acute lung injury post COVID-19, and can promote lung repair mechanisms that lead to improvement in lung oxygenation parameters. The purpose of this study is to investigate the efficacy and safety of Zilucoplan in improving oxygenation and short- and long-term outcome of COVID-19 patients with acute hypoxic respiratory failure. Trial design This is a phase 2 academic, prospective, 2:1 randomized, open-label, multi-center interventional study. Participants Adult patients (≥18y old) will be recruited at specialized COVID-19 units and ICUs at 9 Belgian hospitals. The main eligibility criteria are as follows: 1) Inclusion criteria: a. Recent (≥6 days and ≤16 days) SARS-CoV-2 infection. b. Chest CT scan showing bilateral infiltrates within the last 2 days prior to randomisation. c. Acute hypoxia (defined as PaO2/FiO2 below 350 mmHg or SpO2 below 93% on minimal 2 L/min supplemental oxygen). d. Signs of cytokine release syndrome characterized by either high serum ferritin, or high D-dimers, or high LDH or deep lymphopenia or a combination of those. 2) Exclusion criteria: e. Mechanical ventilation for more than 24 hours prior to randomisation. f. Active bacterial or fungal infection. g. History of meningococcal disease (due to the known high predisposition to invasive, often recurrent meningococcal infections of individuals deficient in components of the alternative and terminal complement pathways). Intervention and comparator Patients in the experimental arm will receive daily 32,4 mg Zilucoplan subcutaneously and a daily IV infusion of 2g of the antibiotic ceftriaxone for 14 days (or until hospital discharge, whichever comes first) in addition to standard of care. These patients will receive additional prophylactic antibiotics until 14 days after the last Zilucoplan dose: hospitalized patients will receive a daily IV infusion of 2g of ceftriaxone, discharged patients will switch to daily 500 mg of oral ciprofloxacin. The control group will receive standard of care and a daily IV infusion of 2g of ceftriaxone for 1 week (or until hospital discharge, whichever comes first), to control for the effects of antibiotics on the clinical course of COVID-19. Main outcomes The primary endpoint is the improvement of oxygenation as measured by mean and/or median change from pre-treatment (day 1) to post-treatment (day 6 and 15 or at discharge, whichever comes first) in PaO2/FiO2 ratio, P(A-a)O2 gradient and a/A PO2 ratio. (PAO2= Partial alveolar pressure of oxygen, PaO2=partial arterial pressure of oxygen, FiO2=Fraction of inspired oxygen). Randomisation Patients will be randomized in a 2:1 ratio (Zilucoplan: control). Randomization will be done using an Interactive Web Response System (REDCap). Blinding (masking) In this open-label trial neither participants, caregivers, nor those assessing the outcomes will be blinded to group assignment. Numbers to be randomised (sample size) A total of 81 patients will be enrolled: 54 patients will be randomized to the experimental arm and 27 patients to the control arm. Trial Status ZILU-COV protocol Version 4.0 (June 10 2020). Participant recruitment started on June 23 2020 and is ongoing. Given the uncertainty of the pandemic, it is difficult to predict the anticipated end date. Trial registration The trial was registered on Clinical Trials.gov on May 11th, 2020 (ClinicalTrials.gov Identifier: NCT04382755 ) and on EudraCT (Identifier: 2020-002130-33 ). Full protocol The full protocol is attached as an additional file, accessible from the Trials website (Additional file 1). In the interest in expediting dissemination of this material, the familiar formatting has been eliminated; this Letter serves as a summary of the key elements of the full protocol.

Published

2020

11. Room C, 10/17/2000 9: 00 AM - 11: 00 AM (PS) Morphine Pharmacokinetics in Human Brain Varies with the Degree of Tissue Injury in Patients with Severe Brain Trauma

Author

Karin Tunblad, Rene Bouw, Carl-Henrik Nordström, Johan Lundberg, and Per Ederoth

Subjects

medicine.medical_specialty, business.industry, Human brain, Degree (temperature), Surgery, Anesthesiology and Pain Medicine, medicine.anatomical_structure, Pharmacokinetics, Anesthesia, medicine, Morphine, In patient, business, Brain trauma, medicine.drug

Published

2000

12. A Relational Approach to Leadership for Multi-Actor Governance

Author

Marc Craps, Inge Vermeesch, Art Dewulf, Koen Sips, Katrien Termeer, and René Bouwen

Subjects

relational approach, inter-organizational collaboration, multi-actor governance, complexity leadership theory, landfill mining, Political institutions and public administration (General), JF20-2112

Abstract

Multi-actor governance, in which a broad mix of actors collaborates to deal with complex societal problems, requires a leadership approach that can take into account the dynamic interdependencies between the involved actors. A relational approach to leadership, focusing on processes and practices, is more adequate for that purpose than approaches focusing on individuals and positions. Complexity leadership theory offers such a relational approach to leadership within organizations. In this article, we use complexity leadership theory to capture the emergent leadership processes between organizations. We focus on the characteristics of the informal relations between representatives of different organizations that enable dealing with the often-conflicting goals and values in multi-actor governance. The case of a landfill mining initiative for sustainable materials governance is used as an illustration to clarify the main concepts and arguments.

Published

2019