Your search keyword '"Gerd Mikus"' showing total 208 results

1. Simulation-Based Assessment of the Impact of Non-Adherence on Endoxifen Target Attainment in Different Tamoxifen Dosing Strategies

Author

Anna Mueller-Schoell, Lena Klopp-Schulze, Robin Michelet, Madelé van Dyk, Thomas E. Mürdter, Matthias Schwab, Markus Joerger, Wilhelm Huisinga, Gerd Mikus, and Charlotte Kloft

Subjects

tamoxifen, non-adherence, model-informed precision dosing, pharmacokinetics, pharmacometrics, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Tamoxifen is widely used in breast cancer treatment and minimum steady-state concentrations of its active metabolite endoxifen (CSS,min ENDX) above 5.97 ng/mL have been associated with favourable disease outcome. Yet, about 20% of patients do not reach target CSS,min ENDX applying conventional tamoxifen dosing. Moreover, 4–75% of patients are non-adherent, resulting in worse disease outcomes. Assuming complete adherence, we previously showed model-informed precision dosing (MIPD) to be superior to conventional and CYP2D6-guided dosing in minimising the proportion of patients with subtarget CSS,min ENDX. Given the high non-adherence rate in long-term tamoxifen therapy, this study investigated the impact of non-adherence on CSS,min ENDX target attainment in different dosing strategies. We show that MIPD allows to account for the expected level of non-adherence (here: up to 2 missed doses/week): increasing the MIPD target threshold from 5.97 ng/mL to 9 ng/mL (the lowest reported CSS,min ENDX in CYP2D6 normal metabolisers) as a safeguard resulted in the lowest interindividual variability and proportion of patients with subtarget CSS,min ENDX even in non-adherent patients. This is a significant improvement to conventional and CYP2D6-guided dosing. Adding a fixed increment to the originally selected dose is not recommended, since it inflates interindividual variability.

Published

2021

2. A Physiologically Based Pharmacokinetic Model of Voriconazole Integrating Time-Dependent Inhibition of CYP3A4, Genetic Polymorphisms of CYP2C19 and Predictions of Drug-Drug Interactions

Author

Pertti J. Neuvonen, Uwe Fuhr, Thorsten Lehr, Teijo I. Saari, Chih-hsuan Hsin, Daniel Moj, Klaus T. Olkkola, Max Taubert, Sebastian Frechen, Gerd Mikus, Xia Li, Medicum, Department of Clinical Pharmacology, University of Helsinki, HUS Helsinki and Uusimaa Hospital District, HUS Perioperative, Intensive Care and Pain Medicine, Department of Diagnostics and Therapeutics, and Anestesiologian yksikkö

Subjects

0301 basic medicine, Physiologically based pharmacokinetic modelling, BIOAVAILABILITY, 030106 microbiology, Cmax, Antifungal drug, CYP2C19, METABOLISM, Pharmacology, GUIDELINES, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, Therapeutic index, Pharmacokinetics, STEADY-STATE PHARMACOKINETICS, HUMAN LIVER, Cytochrome P-450 CYP3A, Humans, Medicine, Drug Interactions, Pharmacology (medical), Voriconazole, SPECTRUM, Polymorphism, Genetic, Maintenance dose, business.industry, GENOTYPE, 3. Good health, Cytochrome P-450 CYP2C19, ANTIFUNGAL AGENT, 317 Pharmacy, SAFETY, SHORT-TERM, business, medicine.drug

Abstract

Background Voriconazole, a first-line antifungal drug, exhibits nonlinear pharmacokinetics (PK), together with large interindividual variability but a narrow therapeutic range, and markedly inhibits cytochrome P450 (CYP) 3A4 in vivo. This causes difficulties in selecting appropriate dosing regimens of voriconazole and coadministered CYP3A4 substrates. Objective This study aimed to investigate the metabolism of voriconazole in detail to better understand dose- and time-dependent alterations in the PK of the drug, to provide the model basis for safe and effective use according to CYP2C19 genotype, and to assess the potential of voriconazole to cause drug-drug interactions (DDIs) with CYP3A4 substrates in more detail. Methods In vitro assays were carried out to explore time-dependent inhibition (TDI) of CYP3A4 by voriconazole. These results were combined with 93 published concentration-time datasets of voriconazole from clinical trials in healthy volunteers to develop a whole-body physiologically based PK (PBPK) model in PK-Sim(R). The model was evaluated quantitatively with the predicted/observed ratio of the area under the plasma concentration-time curve (AUC), maximum concentration (C-max), and trough concentrations for multiple dosings (C-trough), the geometric mean fold error, as well as visually with the comparison of predicted with observed concentration-time datasets over the full range of recommended intravenous and oral dosing regimens. Results The result of the half maximal inhibitory concentration (IC50) shift assay indicated that voriconazole causes TDI of CYP3A4. The PBPK model evaluation demonstrated a good performance of the model, with 71% of predicted/observed aggregate AUC ratios and all aggregateC(max)ratios from 28 evaluation datasets being within a 0.5- to 2-fold range. For those studies reporting CYP2C19 genotype, 89% of aggregate AUC ratios and all aggregateC(max)ratios were inside a 0.5- to 2-fold range of 44 test datasets. The results of model-based simulations showed that the standard oral maintenance dose of voriconazole 200 mg twice daily would be sufficient for CYP2C19 intermediate metabolizers (IMs; *1/*2, *1/*3, *2/*17, and *2/*2/*17) to reach the tentative therapeutic range of > 1-2 mg/L to

Published

2023

3. Perpetrator Characteristics of Azole Antifungal Drugs on Three Oral Factor Xa Inhibitors Administered as a Microdosed Cocktail

Author

Jürgen Burhenne, Antje Blank, Gerd Mikus, Walter E. Haefeli, Kathrin I. Foerster, Mazyar Mahmoudi, and Brit Silja Rohr

Subjects

Azoles, Posaconazole, Antifungal Agents, medicine.drug_mechanism_of_action, Factor Xa Inhibitor, Pharmacology, chemistry.chemical_compound, Rivaroxaban, Edoxaban, medicine, Humans, Drug Interactions, Pharmacology (medical), Original Research Article, chemistry.chemical_classification, business.industry, Drug class, Pharmaceutical Preparations, chemistry, Azole, Ketoconazole, Apixaban, business, Factor Xa Inhibitors, medicine.drug

Abstract

Background Factor Xa inhibitors (FXaIs) are increasingly used without having sufficient drug–drug interaction data. Using a microdosed cocktail methodology could support filling the knowledge gap quickly. Methods In a randomised crossover trial, we investigated the drug–drug interactions between six oral azole antifungals and a microdosed FXaI cocktail containing 25 µg rivaroxaban, 25 µg apixaban, and 50 µg edoxaban. Additionally, different enzyme activities were also monitored using a microdosed cocktail approach. The six different azole antifungals were administered in therapeutic doses over a 24 h period, while the microdosed cocktails were administered 1 h after administration of the azole antifungals. Results Ketoconazole and posaconazole were the strongest perpetrators, showing similar increases as apixaban (area under the concentration–time curve ratio [AUCR] 1.64 and 1.62, respectively) and edoxaban (AUCR 2.08 and 2.1, respectively), whereas ketoconazole increased rivaroxaban 2.32-fold but only increased posaconazole 1.37-fold. All other azole antifungals showed less perpetrator effects on the FXaIs. Cytochrome P450 (CYP) 3A inhibition was confirmed using microdosed midazolam, with ketoconazole also the most potent perpetrator (8.42-fold). Conclusion Drug–drug interactions for three victim drugs of the same drug class (FXaIs) with different clearance mechanisms can be studied using a microdosed cocktail approach. Using members of the azole antifungal drug class as perpetrators, multiple interactions can be studied in one trial, and a more detailed insight into the underlying interaction mechanisms is possible. Clinical Trial Registration EudraCT number: 2017-004453-16. Supplementary Information The online version contains supplementary material available at 10.1007/s40262-021-01051-9.

Published

2021

4. Pharmacoenhancement of Low Crizotinib Plasma Concentrations in Patients with Anaplastic Lymphoma Kinase‐Positive Non‐Small Cell Lung Cancer using the CYP3A Inhibitor Cobicistat

Author

Farastuk Bozorgmehr, Antje Blank, Walter E. Haefeli, Michael Thomas, Petros Christopoulos, Jürgen Burhenne, Nicolas Hohmann, and Gerd Mikus

Subjects

Adult, Male, Alectinib, medicine.medical_specialty, Lung Neoplasms, Cost-Benefit Analysis, Gastroenterology, General Biochemistry, Genetics and Molecular Biology, Cmin, Crizotinib, Pharmacokinetics, Carcinoma, Non-Small-Cell Lung, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Cytochrome P-450 CYP3A, Humans, Outpatient clinic, Anaplastic lymphoma kinase, Anaplastic Lymphoma Kinase, General Pharmacology, Toxicology and Pharmaceutics, Lung cancer, Protein Kinase Inhibitors, Dose-Response Relationship, Drug, business.industry, Brief Report, Research, General Neuroscience, Cobicistat, lcsh:Public aspects of medicine, lcsh:RM1-950, Drug Synergism, lcsh:RA1-1270, General Medicine, Middle Aged, medicine.disease, lcsh:Therapeutics. Pharmacology, Mutation, Cytochrome P-450 CYP3A Inhibitors, Feasibility Studies, Female, Brief Reports, business, medicine.drug

Abstract

The inhibitor of anaplastic lymphoma kinase (ALK) crizotinib significantly increases survival in patients with ALK-positive non-small cell lung cancer (NSCLC). When evaluating crizotinib pharmacokinetics (PKs) in patients taking the standard flat oral dose of 250 mg b.i.d., interindividual PK variability is substantial and patient survival is lower in the quartile with the lowest steady-state trough plasma concentrations (Cmin,ss ), suggesting that concentrations should be monitored and doses individualized. We investigated whether the CYP3A inhibitor cobicistat increases Cmin,ss of the CYP3A substrate crizotinib in patients with low exposure. Patients with ALK-positive NSCLC of our outpatient clinic treated with crizotinib were enrolled in a phase I trial (EudraCT 2016-002187-14, DRKS00012360) if crizotinib Cmin,ss was below 310 ng/mL and treated with cobicistat for 14 days. Crizotinib plasma concentration profiles were established before and after a 14-day co-administration of cobicistat to construct the area under the plasma concentration-time curve in the dosing interval from zero to 12 hours (AUC0-12 ). Patients were also monitored for adverse events by physical examination, laboratory tests, and 12-lead echocardiogram. Enrolment was prematurely stopped because of the approval of alectinib, a next-generation ALK-inhibitor with superior efficacy. In the only patient enrolled, cobicistat increased Cmin,ss from 158 ng/mL (before cobicistat) to 308 ng/mL (day 8) and 417 ng/mL (day 14 on cobicistat), concurrently the AUC0-12 increased by 78% from 2,210 ng/mL*h to 3,925 ng/mL*h. Neither safety signals nor serious adverse events occurred. Pharmacoenhancement with cobicistat as an alternative for dose individualisation for patients with NSCLC with low crizotinib exposure appears to be safe and is cost-effective and feasible.

Published

2021

5. Absolute Bioavailability of Microdosed Midazolam After Buccal Administration Is Dependent on Buccal Exposure Time

Author

Jana Grass, Walter E. Haefeli, Gerd Mikus, Jürgen Burhenne, Peter Rose, and Antje Blank

Subjects

Adult, Male, Time Factors, Metabolic Clearance Rate, CYP3A, Midazolam, 030226 pharmacology & pharmacy, Young Adult, 03 medical and health sciences, 0302 clinical medicine, stomatognathic system, Cytochrome P-450 CYP3A, Humans, Hypnotics and Sedatives, Medicine, Pharmacology (medical), Buccal Absorption, Absolute bioavailability, Pharmacology, Cytochrome P450 3A, business.industry, Administration, Buccal, Buccal administration, Confidence interval, Bioavailability, stomatognathic diseases, Area Under Curve, 030220 oncology & carcinogenesis, Anesthesia, Female, business, Half-Life, medicine.drug

Abstract

Midazolam is an established probe drug to assess cytochrome P450 3A activity (phenotyping). Microdosed midazolam is increasingly used for this purpose; a buccal formulation might be of advantage, but buccal absorption might occur. We therefore tested in a single-center, open-label clinical trial with 12 healthy volunteers the absolute bioavailability of 10 μg of midazolam after buccal administration in relation to buccal exposure time. In relation to a drinking solution, there was an increase of midazolam exposure (area under the plasma concentration-time curve from time 0 to infinity) with increasing buccal exposure time with an apparent saturation at 100-second buccal exposure. Absolute bioavailability increased from 27.8% (95% confidence interval, 23.5-32.9) for the drinking solution (0 seconds) to 66.1% (95% confidence interval, 60.0-72.8) after 100-second buccal exposure with no further increase after 150 seconds. A Hill equation described the time dependency of midazolam bioavailability with maximal bioavailability as 64.5% and buccal exposure time resulting in half maximal bioavailability increase as 16 seconds. In conclusion, midazolam bioavailability is highly dependent on buccal exposure time, and even a few seconds of buccal exposure will increase bioavailability due to buccal absorption. This needs to be taken into account for any buccal administration of midazolam.

Published

2020

6. Composite midazolam and 1′-OH midazolam population pharmacokinetic model for constitutive, inhibited and induced CYP3A activity

Author

Andreas D. Meid, Gerd Mikus, and Sabrina T. Wiebe

Subjects

Adult, Male, Metabolic Clearance Rate, CYP3A, Midazolam, Population, Population pharmacokinetics, Pharmacology, Models, Biological, Sensitivity and Specificity, 030226 pharmacology & pharmacy, Drug interactions, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, medicine, Cytochrome P-450 CYP3A, Humans, education, Original Paper, education.field_of_study, Chemistry, Cytochrome P-450 CYP3A Inducers, Middle Aged, Healthy Volunteers, Current analysis, Biological Variation, Population, Drug development, Area Under Curve, 030220 oncology & carcinogenesis, Cytochrome P-450 CYP3A Inhibitors, Female, Drug metabolism, medicine.drug

Abstract

CYP3A plays an important role in drug metabolism and, thus, can be a considerable liability for drug-drug interactions. Population pharmacokinetics may be an efficient tool for detecting such drug-drug interactions. Multiple models have been developed for midazolam, the typical probe substrate for CYP3A activity, but no population pharmacokinetic models have been developed for use with inhibition or induction. The objective of the current analysis was to develop a composite parent-metabolite model for midazolam which could adequately describe CYP3A drug-drug interactions. As an exploratory objective, parameters were assessed for potential cut-points which may allow for determination of drug-drug interactions when a baseline profile is not available. The final interaction model adequately described midazolam and 1′-OH midazolam concentrations for constitutive, inhibited, and induced CYP3A activity. The model showed good internal and external validity, both with full profiles and limited sampling (2, 2.5, 3, and 4 h), and the model predicted parameters were congruent with values found in clinical studies. Assessment of potential cut-points for model predicted parameters to assess drug-drug interaction liability with a single profile suggested that midazolam clearance may reasonably be used to detect inhibition (4.82–16.4 L/h), induction (41.8–88.9 L/h), and no modulation (16.4–41.8 L/h), with sensitivities for potent inhibition and induction of 87.9% and 83.3%, respectively, and a specificity of 98.2% for no modulation. Thus, the current model and cut-points could provide efficient and accurate tools for drug-drug liability detection, both during drug development and in the clinic, following prospective validation in healthy volunteers and patient populations. Electronic supplementary material The online version of this article (10.1007/s10928-020-09704-1) contains supplementary material, which is available to authorized users.

Published

2020

7. Validation of a Drug Transporter Probe Cocktail Using the Prototypical Inhibitors Rifampin, Probenecid, Verapamil, and Cimetidine

Author

Sabrina Wiebe, Ashish Sharma, Martin F. Fromm, Alen Jambrecina, Peter Stopfer, Fabian Müller, Edith Hauel, Kerstin Bader, Mitchell E. Taub, Gerd Mikus, Kathrin Hohl, Sven Schmidt-Gerets, Thomas Giessmann, Thomas Ebner, and Naoki Ishiguro

Subjects

Male, Organic anion transporter 1, Digoxin, Cmax, Pharmacology, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Drug Interactions, Pharmacology (medical), Rosuvastatin, Original Research Article, Cimetidine, biology, Probenecid, Chemistry, Organic anion-transporting polypeptide, Verapamil, Area Under Curve, 030220 oncology & carcinogenesis, biology.protein, Rifampin, medicine.drug

Abstract

Background and Objective A novel cocktail containing four substrates of key drug transporters was previously optimized to eliminate mutual drug–drug interactions between the probes digoxin (P-glycoprotein substrate), furosemide (organic anion transporter 1/3), metformin (organic cation transporter 2, multidrug and toxin extrusion protein 1/2-K), and rosuvastatin (organic anion transporting polypeptide 1B1/3, breast cancer resistance protein). This clinical trial investigated the effects of four commonly employed drug transporter inhibitors on cocktail drug pharmacokinetics. Methods In a randomized open-label crossover trial in 45 healthy male subjects, treatment groups received the cocktail with or without single oral doses of rifampin, verapamil, cimetidine or probenecid. Concentrations of the probe drugs in serial plasma samples and urine fractions were measured by validated liquid chromatography-tandem mass spectrometry assays to assess systemic exposure. Results The results were generally in accordance with known in vitro and/or clinical drug–drug interaction data. Single-dose rifampin increased rosuvastatin area under the plasma concentration–time curve up to the last quantifiable concentration (AUC0–tz) by 248% and maximum plasma concentration (Cmax) by 1025%. Probenecid increased furosemide AUC0–tz by 172% and Cmax by 23%. Cimetidine reduced metformin renal clearance by 26%. The effect of single-dose verapamil on digoxin systemic exposure was less than expected from multiple-dose studies (AUC0–tz unaltered, Cmax + 22%). Conclusions Taking all the interaction results together, the transporter cocktail is considered to be validated as a sensitive and specific tool for evaluating transporter-mediated drug–drug interactions in drug development. Clinical Trial Registration EudraCT number 2017-001549-29. Electronic supplementary material The online version of this article (10.1007/s40262-020-00907-w) contains supplementary material, which is available to authorized users.

Published

2020

8. Application of a microdosed cocktail of 3 oral factor Xa inhibitors to study drug–drug interactions with different perpetrator drugs

Author

Walter E. Haefeli, Gerd Mikus, Marlene Schaumaeker, Jürgen Burhenne, Marie-Louise Lehmann, and Kathrin I. Foerster

Subjects

medicine.drug_mechanism_of_action, Pyridones, Factor Xa Inhibitor, apixaban, Pharmacology, rifampicin, 030226 pharmacology & pharmacy, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Rivaroxaban, MicroDose, Edoxaban, voriconazole, medicine, Humans, Drug Interactions, Pharmacology (medical), 030212 general & internal medicine, Volume of distribution, drug interaction, business.industry, Cobicistat, Anticoagulants, Original Articles, cobicistat, Drug interaction, Pharmaceutical Preparations, chemistry, edoxaban, Original Article, Apixaban, business, Chromatography, Liquid, Factor Xa Inhibitors, medicine.drug

Abstract

Aims Using 3 different perpetrators the impact of voriconazole, cobicistat and rifampicin (single dose), we evaluated the suitability of a microdose cocktail of factor Xa inhibitors (FXaI; rivaroxaban, apixaban and edoxaban; 100 μg in total) to study drug-drug interactions. Methods Three cohorts of 6 healthy volunteers received 2 treatments with microdoses of rivaroxaban, apixaban and edoxaban alone and with coadministration of 1 of the perpetrators. Plasma and urine concentrations of microdosed apixaban, edoxaban and rivaroxaban were quantified using a validated ultra-performance liquid chromatography-tandem mass spectrometry with a lower limit of quantification of 2.5 pg/mL. Results Voriconazole caused only a minor interaction with apixaban and rivaroxaban, none with edoxaban. Cobicistat significantly increased exposure of all 3 FXaI with area under the plasma concentration-time curve ratios of 1.67 (apixaban), 1.74 (edoxaban) and 2.0 (rivaroxaban). A single dose of rifampicin decreased the volume of distribution and elimination half-life of all 3 FXaI. Conclusions The microdosed FXaI cocktail approach is able to generate drug interaction data and can help elucidating the mechanism involved in the clearance of the different victim drugs. This is a safe approach to concurrently study drug-drug interactions with a drug class. (EudraCT 2016-003024-23).

Published

2020

9. Prophylactic Use of Enoxaparin in Adolescents During Bariatric Surgery—a Prospective Clinical Study

Author

Evan P. Nadler, Victoria C. Ziesenitz, Johannes N. van den Anker, Janelle D Vaughns, Gerd Mikus, and Elaine F Williams

Subjects

Adult, Male, Pediatric Obesity, medicine.medical_specialty, Adolescent, Endocrinology, Diabetes and Metabolism, Cmax, Bariatric Surgery, 030209 endocrinology & metabolism, Chemoprevention, Article, Drug Administration Schedule, Young Adult, 03 medical and health sciences, Postoperative Complications, 0302 clinical medicine, Pharmacokinetics, Preoperative Care, medicine, Clinical endpoint, Humans, Prospective Studies, Dosing, Enoxaparin, Child, Nutrition and Dietetics, Dose-Response Relationship, Drug, Surrogate endpoint, business.industry, Anticoagulants, Venous Thromboembolism, medicine.disease, Obesity, Obesity, Morbid, Surgery, Prospective clinical study, Female, 030211 gastroenterology & hepatology, business, Venous thromboembolism

Abstract

INTRODUCTION: Severe obesity predisposes youth to a higher risk of venous thromboembolism (VTE). This study evaluates a BMI-stratified prophylactic dosing regimen of enoxaparin in adolescents with severe obesity undergoing surgery. METHODS: Adolescents aged 12-20 years received prophylactic enoxaparin at 40 mg SC (for a BMI < 50 kg/m(2)) and 60 mg SC (for a BMI ≥ 50 kg/m(2)) every 12 hours until discharge. Blood samples were drawn at pre-dose, 1, 2, 4, 6, and 12 hrs. Plasma Anti-Factor Xa (Anti-FXa) activity was used as a surrogate marker for enoxaparin pharmacokinetics. RESULTS: Ten female and two male obese adolescents (age range 14-19 years) had a mean BMI of 49.9 kg/m(2) (38.4-58 kg/m(2)). Four patients had a BMI of less than 50 kg/m(2) and received 40 mg enoxaparin, resulting in a mean dosage of 0.352 ± 0.070 mg/kg body weight. Eight patients were dosed with 60 mg enoxaparin every 12 hours, resulting in a mean dosage of 0.395 ± 0.028 mg/kg. Peak plasma anti-FXa activity (C(max)) ranged from 0.14 to 0.30 IU/mL, median C(max) was 0.205 IU/mL. Median T(max) was 5.67 hours (range 3.78 to 7.52 hours). Median AUC(i) was 1.00 h*IU/mL (range 0.42 to 1.67 h*IU/mL). 10 out of 12 patients (83%) reached the primary endpoint with anti-FXa activity in the range for VTE prevention (0.1-0.3 IU/mL). CONCLUSIONS: Our dosing scheme of 40 mg vs 60 mg enoxaparin stratified according to BMI proved to be effective in reaching prophylactic anti-FXa activity in 83% of adolescent patients.

Published

2019

10. Simultaneous phenotyping of CYP2E1 and CYP3A using oral chlorzoxazone and midazolam microdoses

Author

Antje Blank, Yosuke Suzuki, Jürgen Burhenne, Walter E. Haefeli, Gerd Mikus, and Nicolas Hohmann

Subjects

Adult, Male, Microdosing, CYP3A, Midazolam, Administration, Oral, Pharmacology, 030226 pharmacology & pharmacy, Young Adult, 03 medical and health sciences, 0302 clinical medicine, MicroDose, Pharmacokinetics, Cytochrome P-450 CYP3A, medicine, Humans, Drug Interactions, Pharmacology (medical), 030212 general & internal medicine, Dose-Response Relationship, Drug, CYP3A4, business.industry, Cytochrome P-450 CYP2E1, Original Articles, Middle Aged, Chlorzoxazone, Phenotype, Area Under Curve, Female, business, medicine.drug

Abstract

Aims Chlorzoxazone is the paradigm marker substrate for CYP2E1 phenotyping in vivo. Because at the commonly used milligram doses (250-750 mg) chlorzoxazone acts as an inhibitor of the CYP3A4/5 marker substrate midazolam, previous attempts failed to combine both drugs in a common phenotyping cocktail. Microdosing chlorzoxazone could circumvent this problem. Method We enrolled 12 healthy volunteers in a trial investigating the dose-exposure relationship of single ascending chlorzoxazone oral doses over a 10,000-fold range (0.05-500 mg) and assessed the effect of 0.1 and 500 mg of chlorzoxazone on oral midazolam pharmacokinetics (0.003 mg). Results Chlorzoxazone area under the concentration-time curve was dose-linear in the dose range between 0.05 and 5 mg. A nonlinear increase occurred with doses ≥50 mg, probably due to saturated presystemic metabolic elimination. While midazolam area under the concentration-time curve increased 2-fold when coadministered with 500 mg of chlorzoxazone, there was no pharmacokinetic interaction between chlorzoxazone and midazolam microdoses. Conclusion The chlorzoxazone microdose did not interact with the CYP3A marker substrate midazolam, enabling the simultaneous administration in a phenotyping cocktail. This microdose assay is now ready to be further validated and tested as a phenotyping procedure assessing the impact of induction and inhibition of CYP2E1 on chlorzoxazone microdose pharmacokinetics.

Published

2019

11. Quantification of microdosed oral yohimbine and its major metabolite in human plasma in the picogram range

Author

Max Sauter, Gerd Mikus, Manuela Vay, and Jürgen Burhenne

Subjects

CYP2D6, Microdosing, Metabolite, Clinical Biochemistry, Administration, Oral, Tandem mass spectrometry, 01 natural sciences, Analytical Chemistry, 03 medical and health sciences, chemistry.chemical_compound, 610 Medical sciences Medicine, 0302 clinical medicine, Pharmacokinetics, Limit of Detection, Oral administration, medicine, Humans, Sample preparation, General Pharmacology, Toxicology and Pharmaceutics, Chromatography, Chemistry, 010401 analytical chemistry, Analytic Sample Preparation Methods, Reproducibility of Results, Yohimbine, General Medicine, 0104 chemical sciences, Medical Laboratory Technology, 030220 oncology & carcinogenesis, Calibration, Blood Chemical Analysis, medicine.drug

Abstract

Aim: Pharmacokinetics after oral microdosing of the anticipated CYP2D6 substrate yohimbine and its metabolite 11-OH-yohimbine is potentially useful for drug–drug interaction trials and profiling of CYP2D6 enzyme activity. Materials & methods: We developed an ultrasensitive ultra performance liquid chromatography coupled to tandem mass spectrometry assay for quantification of yohimbine and its main metabolite 11-OH-yohimbine in plasma with a linear calibration range of 5–2500 pg/ml and validated it according to US FDA’s and EMA’s guidelines. Sample preparation was performed using fast liquid–liquid extraction. The assay was applied for the determination of concentrations of yohimbine and 11-OH-yohimbine in plasma after oral administration of 50 μg yohimbine to two subjects. Conclusion: Ultrasensitive quantification of yohimbine and its metabolite enables the determination of their concentrations in plasma after microdosing which would be applicable to use in CYP2D6 phenotyping.

Published

2019

12. Alteration of drug-metabolizing enzyme activity in palliative care patients: Microdosed assessment of cytochrome P450 3A

Author

Marcus J. P. Geist, Hubert J. Bardenheuer, Gerd Mikus, and Juergen Burhenne

Subjects

Adult, Male, Palliative care, Midazolam, Pharmacology, 030226 pharmacology & pharmacy, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Limited sampling, Cytochrome P-450 CYP3A, Humans, Medicine, Drug Interactions, Prospective Studies, Aged, Aged, 80 and over, Cytochrome P450 3A, chemistry.chemical_classification, Terminal Care, business.industry, Palliative Care, General Medicine, Middle Aged, Drug metabolizing enzymes, Anesthesiology and Pain Medicine, Enzyme, Liver, chemistry, 030220 oncology & carcinogenesis, Female, Liver function, business, medicine.drug

Abstract

Background: Cytochrome P450 3A is the most relevant drug-metabolizing enzyme in humans as it is involved in the elimination of 50% of marketed drugs. Nothing is known about the activity of cytochrome P450 3A in palliative care patients who have complicated symptoms often associated with a terminal illness. Aim: In order to improve drug dosing in end-of-life care and to avoid drug interactions, cytochrome P450 3A activity was determined in patients of a palliative care unit under real-life clinical conditions. Design: As midazolam is an established marker substance for cytochrome P450 3A activity, this single-arm prospective trial was designed to obtain a 4-h pharmacokinetic profile of midazolam after oral administration of a 10-µg dose from each enrolled patient. Plasma concentrations of midazolam and its primary metabolite 1′-hydroxy-midazolam were quantified by mass spectrometry techniques. Cytochrome P450 3A activity was calculated as partial metabolic clearance from a limited sampling area under the curve. All other drugs taken by the participating patients were considered, as well as recent blood test results and patients’ diagnoses. The trial was registered at German Clinical Trials Register ( www.drks.de ): DRKS00011753. Setting/participants: The trial was carried out at a university palliative care unit under real-life clinical conditions. Every patient admitted to the ward was screened for possible participation, independent of the individual performance status. Results: Partial metabolic clearance of midazolam in palliative care patients was 31.7 ± 32.1 L/h. This was a highly significant 40% reduction ( p Conclusion: Dosing of cytochrome P450 3A substrate drugs (e.g. macrolide antibiotics, benzodiazepines, calcium channel blockers) needs to be adjusted in palliative care patients; otherwise, escalation of debilitating symptoms due to drug interactions might occur.

Published

2019

13. Simultaneous quantification of the CYP2D6 substrate yohimbine, its metabolite 11-OH-yohimbine, and the CYP2D6 inhibitor paroxetine in human plasma

Author

Jürgen Burhenne, Gerd Mikus, Gisela Skopp, and Manuela Vay

Subjects

Chromatography, General Chemical Engineering, Metabolite, Electrospray ionization, 010401 analytical chemistry, General Engineering, 02 engineering and technology, 021001 nanoscience & nanotechnology, Tandem mass spectrometry, 01 natural sciences, 0104 chemical sciences, Analytical Chemistry, Yohimbine, chemistry.chemical_compound, Acetic acid, Pharmacokinetics, chemistry, medicine, Sample preparation, 0210 nano-technology, Ammonium acetate, medicine.drug

Abstract

We developed and validated a human plasma LC-MS/MS assay according to FDA guidelines to determine the impact of the CYP2D6 inhibitor paroxetine on the pharmacokinetics of the assumed specific CYP2D6 substrate yohimbine. Yohimbine, its main metabolite 11-OH-yohimbine, and paroxetine were quantified using plasma (100 μL) and liquid–liquid extraction for sample preparation. Analytes were separated with a Phenomenex Luna C18 3 μm LC column using a gradient consisting of ammonium acetate (5 mM), acetic acid, and acetonitrile. Tandem mass spectrometry detection was performed using positive electrospray ionization and selective reaction monitoring utilizing 13C- and deuterium-labeled internal standards in the calibration range from 0.5 to 500 ng mL−1. Accuracy at the lower limit of quantification of 0.5 ng mL−1 was

Published

2019

14. CYP2D6 phenotype explains reported yohimbine concentrations in four severe acute intoxications

Author

Gerd Mikus, Anna Mueller-Schoell, Robin Michelet, Charlotte Kloft, and Ferdinand Weinelt

Subjects

0301 basic medicine, CYP2D6, medicine.drug_class, Short Communication, Health, Toxicology and Mutagenesis, High variability, Drug powder, Pharmacology, Toxicology, Models, Biological, 01 natural sciences, 03 medical and health sciences, Pharmacometrics, Pharmacokinetics, Humans, Medicine, Computer Simulation, business.industry, 010401 analytical chemistry, Yohimbine, General Medicine, Adrenergic alpha-2 Receptor Antagonists, Receptor antagonist, Phenotype, 0104 chemical sciences, 030104 developmental biology, Cytochrome P-450 CYP2D6, Nonlinear Dynamics, Clearance, Sympathomimetic Effects, 500 Naturwissenschaften und Mathematik::540 Chemie::540 Chemie und zugeordnete Wissenschaften, business, Modelling & simulation, medicine.drug

Abstract

The indole alkaloid yohimbine is an alpha-2 receptor antagonist used for its sympathomimetic effects. Several cases of yohimbine intoxication have been reported and the most recent one involved four individuals taking a yohimbine-containing drug powder. All individuals developed severe intoxication symptoms and were admitted to the hospital. Even though all individuals were assumed to have taken the same dose of the drug powder, toxicology analyses revealed yohimbine blood concentrations of 249–5631 ng/mL, amounting to a 22-fold difference. The reason for this high variability remained to be elucidated. We used recently reported knowledge on the metabolism of yohimbine together with state-of-the art nonlinear mixed-effects modelling and simulation and show that a patient’s cytochrome P450 2D6 (CYP2D6) phenotype can explain the large differences observed in the measured concentration after intake of the same yohimbine dose. Our findings can be used both for the identification of safe doses in therapeutic use of yohimbine and for an explanation of individual cases of overdosing.

Published

2021

15. Effect of Pantoprazole on the Absorption of Hydroxychloroquinea A Randomized Drug-Drug Interaction Trial in Healthy Adults

Author

Antje Blank, Simone Hummler, Katja Gümüs, Johanna Weiss, Jürgen Burhenne, David Czock, Felicitas Stoll, Max Sauter, Kathrin I. Foerster, Gerd Mikus, Amin Muhareb, Simon Hermann, and Walter E. Haefeli

Subjects

Adult, business.industry, Drug-drug interaction, Cmax, Pharmaceutical Science, Biological Availability, Hydroxychloroquine, Proton Pump Inhibitors, Absorption (skin), Pharmacology, Bioavailability, Gastric ph, Pharmacokinetics, medicine, Humans, Pharmacology (medical), Drug Interactions, business, Pantoprazole, medicine.drug, Chromatography, Liquid

Abstract

Hydroxychloroquine as a weak basic compound with two amines is strongly enriched in cell compartments with low pH, suggesting that modification of gastric pH by coadministered proton pump inhibitors might reduce its solubility and absorption and thus its efficacy in patients. We addressed this question in a single-center, open-label, randomized, parallel drug-drug interaction trial in healthy adults (EudraCT No. 2020-001470-30). All participants received a single oral dose of 400-mg hydroxychloroquine, and one group additionally received 40 mg of pantoprazole once daily for 9 days dosed to steady state. Whole-blood samples were collected for 72 hours, and hydroxychloroquine was quantified by liquid chromatography-tandem mass spectrometry. Primary endpoints were whole-blood hydroxychloroquine areas under the concentration-time curve from 0 to 72 hours (AUC0-72h ) and peak concentrations (Cmax ). Unpaired 2-sided t-tests of the log transformed pharmacokinetic parameters were performed to compare both groups. Twenty-four participants (12 per group) were included. Hydroxychloroquine AUC0-72h and Cmax did not differ between groups without and with pantoprazole (arithmetic mean; AUC0-72h , 7649 ng/ml • h, and 8429 ng/ml • h, P = .50; Cmax , 448 ng/mL and 451.5 ng/mL, P = .96, respectively). Pantoprazole did not alter hydroxychloroquine absorption, indicating that proton pump inhibitors do not affect its bioavailability.

Published

2021

16. Perspectives on Model-Informed Precision Dosing in the Digital Health Era: Challenges, Opportunities, and Recommendations

Author

Anna Mueller-Schoell, Gerd Mikus, Wilhelm Huisinga, Madelé van Dyk, Corinna Maier, Franziska Kluwe, Charlotte Kloft, Lena Klopp-Schulze, and Robin Michelet

Subjects

Pharmacology, Medical education, Dose-Response Relationship, Drug, business.industry, Digital health, MIPD, Model‐informed precision dosing, Pharmaceutical Preparations, Drug approval, Medicine, Humans, Pharmacology (medical), Dosing, Precision Medicine, business, 500 Naturwissenschaften und Mathematik::540 Chemie::540 Chemie und zugeordnete Wissenschaften

Abstract

Drug approval is based on exposure, response, and variability of studied populations, typically excluding comorbidities/medications and very ill patients, thus not representing real‐world populations. This results in wide variability in therapeutic outcome for individual patients. Model‐informed precision dosing (MIPD) can characterize/quantify this variability, support optimal dose selection, and enable individualized therapy. The aim of this perspective is to raise awareness for MIPD, identify challenges hindering its implementation in clinical practice, provide recommendations, and highlight opportunities.

Published

2021

17. Application of Microdosed Intravenous Omeprazole to Determine Hepatic CYP2C19 Activity

Author

Mazyar Mahmoudi, Gerd Mikus, Kathrin I. Foerster, Johanna Weiss, Jürgen Burhenne, and Walter E. Haefeli

Subjects

Adult, Male, Genotype, Microdosing, Metabolic Clearance Rate, CYP2C19, Pharmacology, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, MicroDose, Oral administration, medicine, Humans, Pharmacology (medical), Drug Interactions, Omeprazole, Voriconazole, Dose-Response Relationship, Drug, business.industry, Drug interaction, Middle Aged, Confidence interval, Cytochrome P-450 CYP2C19, 030220 oncology & carcinogenesis, Area Under Curve, Female, business, medicine.drug, Half-Life

Abstract

Omeprazole is an established probe drug to assess cytochrome P450 (CYP) 2C19 activity (phenotyping). Because it has nonlinear pharmacokinetics (PK) after oral administration (autoinhibition of metabolism), the true impact of coadministered perpetrators on CYP2C19 substrates might be underestimated after regular doses. We tested the dose linearity of an intravenous omeprazole microdose of 100 µg and compared it with a 20-mg dose in 4 healthy poor metabolizers (PMs) and 6 extensive metabolizers (EMs) of CYP2C19 in the presence and absence of a strong inhibitor (voriconazole). Without voriconazole, omeprazole exposure was dose-proportional irrespective of the genotype, but in PMs geometric mean ratios (GMRs) of AUC0-∞ were 6.6-fold higher and molar metabolic ratios of 5-OH omeprazole/omeprazole approximately 10-fold lower. Voriconazole increased omeprazole exposure in EMs approximately 5-fold (AUC0-4 GMR after 100 µg omeprazole, 4.61; 90% confidence interval [CI], 2.69-7.89; AUC0-4 GMR after 20 mg omeprazole, 5.5; 90%CI, 1.07-1.46), whereas no clinically significant impact on PK in PMs was observed (GMR AUC0-4 after 100 µg omeprazole, 1.29; 90%CI, 0.81-2.04; GMR AUC0-4 after 20 mg omeprazole, 1.25; 90%CI, 1.07-1.46). Linear regression and Bland-Altman analyses revealed excellent agreement between AUC0-∞ and AUC0-4 of omeprazole (r2 = 0.987; bias, 0.35%; 95%CI, -3.197% to 3.89%) and also the molar metabolic ratio, 5-OH omeprazole/omeprazole (r2 = 0.987; bias, -3.939; 95%CI, -9.06% to -1.18%), suggesting that an abbreviated sampling protocol can be used for intravenous CYP2C19 phenotyping and drug interaction studies. In conclusion, the PK of intravenous omeprazole microdoses closely reflects the changes observed with regular omeprazole doses; however, to avoid autoinhibition of probe drugs, microdosing appears to be the favorable technique.

Published

2020

18. Midazolam microdosing applied in early clinical development for drug-drug interaction assessment

Author

Armin Schultz, Richard Vinisko, Werner Kadus, Gerd Mikus, Alen Jambrecina, Laura Schlieker, Andreas Huennemeyer, Sabrina Wiebe, Markus Goettel, and Lena Herich

Subjects

Pharmacology, Microdosing, CYP3A, business.industry, Midazolam, Drug-drug interaction, Cmax, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, MicroDose, Pharmaceutical Preparations, Area Under Curve, Linear regression, medicine, Cytochrome P-450 CYP3A, Humans, Pharmacology (medical), Drug Interactions, 030212 general & internal medicine, Analysis of variance, business, medicine.drug

Abstract

Aims We aimed to incorporate a pharmacologically inactive midazolam microdose into early clinical studies for the assessment of CYP3A drug-drug interaction liability. Methods Three early clinical studies were conducted with substances (Compounds A, B and C) which gave positive CYP3A perpetrator signals in vitro. A 75 μg dose of midazolam was administered alone (baseline CYP3A activity) followed by administration with the highest dose groups tested for each compound on Day 1/3 and Day 14 or Day 17. Midazolam exposure (AUC0-∞ , Cmax ) during administration with the test substances was compared to baseline data via an analysis of variance on log-transformed data. Partial AUC2-4 ratios were also compared to AUC0-∞ ratios using linear regression on log-transformed data. Results Test compound Cmax values exceeded relevant thresholds for drug-drug interaction liability. Midazolam concentrations were quantifiable over the full profiles for all subjects in all studies. Point estimates of the midazolam AUC0-∞ gMean ratios ranged from 108.3 to 127.1% for Compound A, from 93.3 to 114.5% for Compound B, and from 92.0 to 96.7% for the two highest dose groups of Compound C. Cmax gMean ratios were in the same range. Thus, no relevant drug-drug interactions were evident, based on the results of midazolam microdosing. AUC2-4 ratios from these studies were comparable to the AUC0-∞ ratios. Conclusion Midazolam microdosing incorporated into early clinical studies is a feasible tool for reducing dedicated drug-drug interaction studies, meaning reduced subject burden. Limited sampling could further reduce subject burden, costs and needed resources.

Published

2020

19. No alteration of Cyp3A4 activity after major hepatectomy in the early postoperative period - A prospective before-after study

Author

Ulrika Asenbaum, Klaus Kaczirek, Christoph Schwarz, Juergen Burhenne, J. Jedamzik, Gerd Mikus, Fabian Fitschek, and Jakob Mühlbacher

Subjects

Adult, Male, medicine.medical_specialty, CYP3A, medicine.medical_treatment, Midazolam, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, In vivo, Internal medicine, medicine, Cytochrome P-450 CYP3A, Hepatectomy, Humans, Postoperative Period, Prospective Studies, Aged, Before after study, CYP3A4, business.industry, General Medicine, Middle Aged, Controlled Before-After Studies, 030220 oncology & carcinogenesis, 030211 gastroenterology & hepatology, Surgery, Female, business, Major hepatectomy, medicine.drug

Abstract

Background The impact of major liver resection (LR) on the detoxifying function of the remaining liver tissue as represented by CYP3A activity has yet to be assessed. Therefore, this study evaluates the changes in CYP3A activity between preoperative values and after liver resection. Material and methods To determine CYP3A activity, midazolam (MDZ) was used as a marker substance, 3 μg were applied intravenously one day before surgery and on the 3rd day after surgery. Subsequently blood was withdrawn at 0, 0.25, 0.5, 1.0, 1.5, 2.0, 2.5, 3, 4 and 6 h post application of the study drug. Plasma MDZ and 1-OH-MDZ concentration was assessed using a LC-MS/MS method. Volumetric analysis of the resected liver was done by syngo.CT liver analysis software (Siemens Healthineers) using preoperative multidetector computed tomography. Results N = 13 (8 male/5 female) patients were included in this study and received preoperative evaluation, 11 patients were studied also after liver resection. The mean age was 62 (±15.3) years with a mean BMI of 23.6 ± 4.8 kg/m2. No patient suffered from acute liver dysfunction postoperatively. None of the pharmacokinetic parameters assessed were significantly altered by liver resection. CYP3A activity over time was not significantly reduced by major liver resection. Conclusion This study gives first time data on the impact of major liver resection on CYP3A activity. It was shown that MDZ clearance representing in vivo CYP3A activity is not altered by major liver resection. This suggests no dose adjustment of commonly applied drugs which are CYP3A substrates needs to be carried out.

Published

2020

20. Oral Yohimbine as a New Probe Drug to Predict CYP2D6 Activity: Results of a Fixed-Sequence Phase I Trial

Author

Gisela Skopp, Mladen V. Tzvetkov, Gerd Mikus, Manuela Vay, Peter Rose, Antje Blank, and Marleen Julia Meyer

Subjects

CYP2D6, Genotype, CYP3A, Pharmacology, 030226 pharmacology & pharmacy, digestive system, 03 medical and health sciences, 0302 clinical medicine, MicroDose, Pharmacokinetics, Oral administration, medicine, Humans, Pharmacology (medical), Original Research Article, skin and connective tissue diseases, business.industry, Yohimbine, Paroxetine, Cytochrome P-450 CYP2D6, 030220 oncology & carcinogenesis, Midazolam, business, medicine.drug

Abstract

Objective Yohimbine pharmacokinetics were determined after oral administration of a single oral dose of yohimbine 5 mg and a microdose of yohimbine 50 µg in relation to different cytochrome P450 (CYP) 2D6 genotypes. The CYP2D6 inhibitor paroxetine was used to investigate the influence on yohimbine pharmacokinetics. Microdosed midazolam was applied to evaluate a possible impact of yohimbine on CYP3A activity and the possibility of combining microdosed yohimbine and midazolam to simultaneously determine CYP2D6 and CYP3A activity. Methods In a fixed-sequence clinical trial, 16 healthy volunteers with a known CYP2D6 genotype [extensive (10), intermediate (2) and poor (4) metaboliser] received an oral dose of yohimbine 50 µg, yohimbine 5 mg at baseline and during paroxetine as a CYP2D6 inhibitor. Midazolam (30 µg) was co-administered to determine CYP3A activity at each occasion. Plasma concentrations of yohimbine, its main metabolite 11-OH-yohimbine, midazolam and paroxetine were quantified using validated liquid chromatography-tandem mass spectrometry assays. Results Pharmacokinetics of yohimbine were highly variable and a CYP2D6 genotype dependent clearance was observed. After yohimbine 5 mg, the clearance ranged from 25.3 to 15,864 mL/min and after yohimbine 50 µg, the clearance ranged from 39.6 to 38,822 mL/min. A more than fivefold reduction in clearance was caused by paroxetine in CYP2D6 extensive metabolisers, while the clearance in poor metabolisers was not affected. Yohimbine did not alter CYP3A activity as measured by microdosed midazolam. Conclusions The pharmacokinetics of yohimbine were highly correlated with CYP2D6, which was further supported by the clearance inhibition caused by the CYP2D6 inhibitor paroxetine. With these data, yohimbine is proposed to be a suitable probe drug to predict CYP2D6 activity. In addition, the microdose can be used in combination with microdosed midazolam to simultaneously evaluate CYP2D6 and CYP3A activity without any interaction between the probe drugs and because the microdoses exert no pharmacological effects. Clinical Trial Registration EudraCT2017-001801-34. Electronic supplementary material The online version of this article (10.1007/s40262-020-00862-6) contains supplementary material, which is available to authorized users.

Published

2020

21. Proposal of a Safe and Effective Study Design for CYP3A-Mediated Drug-Drug Interactions

Author

Gerd Mikus and Brit Silja Rohr

Subjects

Drug, Adult, Azoles, Male, medicine.medical_specialty, Antifungal Agents, Itraconazole, media_common.quotation_subject, 030226 pharmacology & pharmacy, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Internal medicine, medicine, Cytochrome P-450 CYP3A, Humans, Pharmacology (medical), Drug Interactions, Adverse effect, Volunteer, media_common, Pharmacology, Voriconazole, chemistry.chemical_classification, Clinical Trials as Topic, business.industry, Middle Aged, Healthy Volunteers, Ketoconazole, chemistry, 030220 oncology & carcinogenesis, Midazolam, Azole, Cytochrome P-450 CYP3A Inhibitors, Female, business, medicine.drug

Abstract

Numerous drug-drug interaction (DDI) trials have to be conducted in healthy volunteers based on current regulatory guidelines. Because the worst-case scenario of strong cytochrome P450 (CYP) inhibitors has to be tested, the results and their validity have to be balanced with the risk to volunteer safety. The use of ketoconazole in clinical DDI studies has been discouraged by regulatory agencies due to an alleged risk of liver injury. In order to reduce the risk to healthy volunteers, we carried out a study with single-day exposure to each of 6 perpetrator azole fungistatic drugs. They were evaluated regarding their CYP3A inhibition using microdosed midazolam and a limited sampling strategy. Ratios of areas under the concentration-time curves ranged from 1.93 with isavuconazole to 8.42 with ketoconazole. The highest number of adverse events occurred with voriconazole, followed by ketoconazole; 2 dropouts occurred due to adverse events following itraconazole administration. Literature data on adverse events of azole fungistatic drugs in DDI trials are rare and inconclusive. Only in recent years with the newer drugs are they more precise and reliable. It can be concluded that the duration of preexposure of perpetrator drugs can be reduced to 1 hour before administration of the victim drug. This still can be sufficient to achieve the scientific objectives of the trial with the lowest possible risk.

Published

2020

22. Immunization with full-length Plasmodium falciparum merozoite surface protein 1 is safe and elicits functional cytophilic antibodies in a randomized first-in-human trial

Author

Gerd Mikus, Ernst Böhnlein, Michael Lanzer, Anja Jäschke, Walter E. Haefeli, Kirsten Heiss, Kristin Fürle, Antje Blank, Hermann Bujard, Johannes Hüsing, Darrick Carter, Monika Lehmann, and Thomas Giese

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, medicine.medical_treatment, Immunology, Placebo, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, parasitic diseases, medicine, Pharmacology (medical), 030212 general & internal medicine, Pharmacology, biology, business.industry, Immunogenicity, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Clinical trial, Titer, 030104 developmental biology, Infectious Diseases, Immunization, biology.protein, Antibody, lcsh:RC581-607, business, Adjuvant, Malaria

Abstract

A vaccine remains a priority in the global fight against malaria. Here, we report on a single-center, randomized, double-blind, placebo and adjuvant-controlled, dose escalation phase 1a safety and immunogenicity clinical trial of full-length Plasmodium falciparum merozoite surface protein 1 (MSP1) in combination with GLA-SE adjuvant. Thirty-two healthy volunteers were vaccinated at least three times with MSP1 plus adjuvant, adjuvant alone, or placebo (24:4:4) to evaluate the safety and immunogenicity. MSP1 was safe, well tolerated and immunogenic, with all vaccinees sero-converting independent of the dose. The MSP1-specific IgG and IgM titers persisted above levels found in malaria semi-immune humans for at least 6 months after the last immunization. The antibodies were variant- and strain-transcending and stimulated respiratory activity in granulocytes. Furthermore, full-length MSP1 induced memory T-cells. Our findings encourage challenge studies as the next step to evaluate the efficacy of full-length MSP1 as a vaccine candidate against falciparum malaria (EudraCT 2016-002463-33).

Published

2020

23. New Insights Into the Pharmacokinetics of Vancomycin After Oral and Intravenous Administration: An Investigation in Beagle Dogs

Author

Philipp Uhl, Gerd Mikus, Max Sauter, Jürgen Burhenne, Andreas D. Meid, and Walter E. Haefeli

Subjects

Drug, media_common.quotation_subject, Pharmaceutical Science, Administration, Oral, Biological Availability, 02 engineering and technology, Absorption (skin), Pharmacology, 030226 pharmacology & pharmacy, Beagle, Intestinal absorption, 03 medical and health sciences, 0302 clinical medicine, Dogs, Pharmacokinetics, Oral administration, Vancomycin, Medicine, Animals, media_common, business.industry, 021001 nanoscience & nanotechnology, Bioavailability, Solubility, Administration, Intravenous, 0210 nano-technology, business, medicine.drug

Abstract

Intestinal absorption of orally administered peptides is often negligible because one or more key requirements for successful absorption (water solubility, peptic resistance, mucosal permeation) are not met. Due to its high water solubility and stability in the gastro-intestinal tract, vancomycin is an ideal model peptide for evaluating the factors influencing the critical step of mucosal permeation. Therefore, to support formulation development for the systemic oral delivery of peptide therapeutics, we investigated the pharmacokinetics of vancomycin in beagle dogs after intravenous and oral administration comparing enteric encapsulated drug to the drug in solution, which revealed mean absolute bioavailabilities of 0.27% and 1.66%, respectively. Additionally, in depth pharmacokinetic analyses of intravenously administered vancomycin revealed a deep compartment slowly releasing the compound over many hours into the blood.

Published

2020

24. Drug–Drug Interactions with Direct Oral Anticoagulants

Author

Gerd Mikus, Walter E. Haefeli, Kathrin I. Foerster, and Simon Hermann

Subjects

Pharmacology, Polypharmacy, Drug, medicine.medical_specialty, medicine.diagnostic_test, medicine.drug_class, business.industry, media_common.quotation_subject, Anticoagulant, Review Article, 030204 cardiovascular system & hematology, 030226 pharmacology & pharmacy, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, Pharmacotherapy, Therapeutic drug monitoring, Stroke prevention, Concomitant, medicine, Pharmacology (medical), Intensive care medicine, business, Major bleeding, media_common

Abstract

A large body of evidence suggests that not only direct anticoagulant effects but also major bleeding events and stroke prevention depend on plasma concentrations of direct oral anticoagulants (DOACs). Concomitant drugs that cause drug-drug interactions (DDIs) alter DOAC exposure by increasing or decreasing DOAC bioavailability and/or clearance; hence, they might affect the efficacy and safety of DOAC therapy. Patients with renal impairment already receive smaller DOAC maintenance doses because avoidance of elevated DOAC exposure might prevent serious bleeding events. For other causes of increased exposure such as DDIs, management is often less well-defined. Considering that DOAC patients are often older and have multiple co-morbidities, polypharmacy is highly prevalent. However, the effect of multiple drugs on DOAC exposure, and especially the impact of DDIs when concurring with drug-disease interactions as observed in renal impairment, has not been thoroughly elucidated. In order to provide effective and safe anticoagulation with DOACs, understanding the mechanisms and magnitude of DDIs appears relevant. Instead of avoiding drug combinations with DOACs, more DDI trials should be conducted and new strategies such as dose adjustments based on therapeutic drug monitoring should be investigated. However, dose adjustments based on concentration measurements cannot currently be recommended because evidence-based data are missing.

Published

2020

25. Does the circulating ketoconazole metabolite N-deacetyl ketoconazole contribute to the drug-drug interaction potential of the parent compound?

Author

Johanna Weiss, Jürgen Burhenne, Thorsten Lehr, Gerd Mikus, Walter E. Haefeli, Kathrin I. Foerster, and Maria Theresia Weber

Subjects

CYP2D6, Metabolite, Pharmaceutical Science, Pharmacology, chemistry.chemical_compound, Pharmacokinetics, In vivo, CYP, Drug transporters, medicine, ATP Binding Cassette Transporter, Subfamily G, Member 2, Drug Interactions, N-deacetyl ketoconazole, CYP3A4, biology, Chemistry, Neoplasm Proteins, Organic anion-transporting polypeptide, Ketoconazole, Pharmaceutical Preparations, UPLC-MS/MS, biology.protein, Drug metabolism, Drug-drug interaction, medicine.drug

Abstract

Ketoconazole is a strong inhibitor of cytochrome P450 3A4 (CYP3A4) and of P-glycoprotein (P-gp) and is often used as an index inhibitor especially for CYP3A4-mediated drug metabolism. A preliminary physiologically based pharmacokinetic (PBPK) model for drug-drug interactions indicated possible involvement of a metabolite to the perpetrator potential of ketoconazole. Still unknown for humans, in rodents, N-deacetyl ketoconazole (DAK) has been identified as the major ketoconazole metabolite. We therefore investigated in vitro, whether DAK also inhibits the human CYPs and drug transporters targeted by ketoconazole and quantified DAK in human plasma from healthy volunteers after receiving a single oral dose of 400 mg ketoconazole. Our data demonstrated that DAK also inhibits CYP3A4 (2.4-fold less potent than ketoconazole), CYP2D6 (13-fold more potent than ketoconazole), CYP2C19 (equally potent), P-gp (3.4-fold less potent than ketoconazole), breast cancer resistance protein (more potent than ketoconazole) and organic anion transporting polypeptide 1B1 and 1B3 (7.8-fold and 2.6-fold less potent than ketoconazole). After a single oral dose of 400 mg ketoconazole, maximum concentrations of DAK in human plasma were only 3.1 ‰ of the parent compound. However, assuming that DAK also highly accumulates in the human liver as demonstrated for rodents, inhibition of the proteins investigated could also be conceivable in vivo. In conclusion, DAK inhibits several CYPs and drug transporters, which might contribute to the perpetrator potential of ketoconazole.

Published

2022

26. Rivaroxaban and macitentan can be coadministered without dose adjustment but the combination of rivaroxaban and St John's wort should be avoided

Author

Lars Werntz, Kathrin I. Foerster, Gerd Mikus, Andrea Huppertz, Jürgen Burhenne, Walter E. Haefeli, David Czock, and Andreas D. Meid

Subjects

Pharmacology, Rivaroxaban, business.industry, CYP3A, Cmax, Phases of clinical research, 030204 cardiovascular system & hematology, 030226 pharmacology & pharmacy, 03 medical and health sciences, Saint john's wort, chemistry.chemical_compound, 0302 clinical medicine, Pharmacokinetics, chemistry, Medicine, Midazolam, Pharmacology (medical), business, medicine.drug, Macitentan

Abstract

Aims We assessed the potential mutual interaction of oral macitentan (cytochrome P450 (CYP) 3A4 substrate) at steady-state with single-dose oral rivaroxaban (CYP3A4 and P-glycoprotein substrate) and evaluated the effect of the CYP3A and P-glycoprotein inducer St John's wort (SJW) on the pharmacokinetics of these drugs in healthy volunteers. Methods Twelve healthy volunteers completed this open-label, monocentre, two-period, one-sequence phase I clinical trial. The pharmacokinetics of macitentan (10 mg) was assessed on study days 3 (single dose), 15 (steady-state), 16 (impact of rivaroxaban) and 29 (after induction by oral SJW), and of rivaroxaban on days 2 (single dose), 16 (impact of macitentan at steady-state) and 29 (after induction by SJW). Concurrently, we quantified changes of CYP3A activity using oral microdoses of midazolam (30 μg). Results Rivaroxaban and macitentan did not significantly change the pharmacokinetics of each other. After induction with SJW, CYP3A activity increased by 272% and geometric mean ratios of macitentan AUC decreased by 48% and of Cmax by 45%. Concurrently, also geometric mean ratios of rivaroxaban AUC and Cmax decreased by 25%. Conclusions There is no evidence for a relevant pharmacokinetic interaction between macitentan and rivaroxaban suggesting that these two drugs can be combined without dose adjustment. SJW strongly increased CYP3A activity and substantially reduced rivaroxaban and macitentan exposure while estimated net endothelin antagonism only decreased by 20%, which is considered clinically irrelevant. The combination of SJW with rivaroxaban should be avoided.

Published

2018

27. Higher chlorzoxazone clearance in obese children compared with nonobese peers

Author

Gerd Mikus, Tonny Studsgaard Petersen, Helle Holst, Hanne Rolighed Christensen, Camilla Schmeltz, Juergen Burhenne, Elizaveta Chabanova, Jens-Christian Holm, Christina Gade, Kim Dalhoff, and T. Riis

Subjects

0301 basic medicine, Pharmacology, medicine.medical_specialty, business.industry, Urine, medicine.disease, 030226 pharmacology & pharmacy, Obesity, Gastroenterology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Dose adjustment, Internal medicine, Diabetes mellitus, Chlorzoxazone, Liver fat, medicine, Pharmacology (medical), business, Body mass index, Drug metabolism, medicine.drug

Abstract

AIMS To test the in vivo activity of Cytochrome P450 (CYP) 2E1 in obese children vs. nonobese children, aged 11-18 years. Secondly, whether the activity of CYP2E1 in these patients is associated with NALFD, diabetes or hyperlipidaemia. METHODS Seventy children were divided into groups by body mass index (BMI) standard deviation score (SDS). All children received 250 mg oral chlorzoxazone (CLZ) as probe for CYP2E1 activity. Thirteen blood samples and 20-h urine samples were collected per participant. RESULTS Obese children had an increased oral clearance and distribution of CLZ, indicating increased CYP2E1 activity, similar to obese adults. The mean AUC0-∞ value of CLZ was decreased by 46% in obese children compared to nonobese children. The F was was increased twofold in obese children compared to nonobese children, P

Published

2018

28. Methadone against cancer: Lost in translation

Author

Gerd Mikus and Dirk Theile

Subjects

Cancer Research, Programmed cell death, medicine.drug_class, Analgesic, Antineoplastic Agents, Apoptosis, Bioinformatics, OGFr, 03 medical and health sciences, 0302 clinical medicine, Opioid receptor, Neoplasms, medicine, Animals, Humans, Receptor, business.industry, Cancer, medicine.disease, Oncology, 030220 oncology & carcinogenesis, Cancer pain, business, Methadone, 030217 neurology & neurosurgery, medicine.drug

Abstract

Recently, the opioid analgesic d,l-methadone has gained much attention as a potential antineoplastic compound, considerably triggered through lay press and media. In consequence, physicians and pharmacists are currently confronted with numerous patients willing to use d,l-methadone against their malignancies. Well-performed in vitro and in vivo models have in fact shown pro-apoptotic effects of d,l-methadone or other opioids, but also proliferation-stimulating properties. Moreover, the mechanisms of proposed opioid-stimulated apoptosis are incompletely described or contradicting. Finally, the receptors mostly responsible for induction of apoptosis by d,l-methadone remain unclear as contributions of both µ-opioid receptors, Fas cell death receptors, toll-like receptors, N-Methyl-d-aspartate receptors and opioid growth factor receptors were suggested. Such ambiguity prevents rational application of d,l-methadone or patient stratification to enhance beneficial antineoplastic effects. From a clinical point of view, d,l-methadone and other opioids might in fact prolong survival, but such effects likely originate from their analgesic and neuro-psychotropic properties and, thus, improvements of quality of life. Crucial obstacles to the administration of d,l-methadone are incomplete knowledge about its systemic disposition, highly variable pharmacokinetics, profound drug-drug- or drug-disease interaction and QT-prolongation potential. This article summarizes and rates the pharmacological basis of d,l-methadone as an antineoplastic agent and puts its administration in clinical oncology into perspective. Despite enthralling experimental findings about d,l-methadone-mediated apoptosis in cancerous cells or tissues, clinicians should realize the current lack of evidence for the use of d,l-methadone as an antineoplastic agent. Its administration against cancer pain is, however, tenable, albeit restricted to certain clinical situations.

Published

2018

29. No clinically relevant interaction of voriconazole with microdosed apixaban, edoxaban and rivaroxaban

Author

Kathrin I. Foerster, Gerd Mikus, Walter E. Haefeli, Marie-Louise Lehmann, and Marlene Schaumaeker

Subjects

Voriconazole, Oncology, medicine.medical_specialty, Rivaroxaban, business.industry, Applied Mathematics, General Mathematics, chemistry.chemical_compound, chemistry, Edoxaban, Internal medicine, medicine, Apixaban, business, medicine.drug

Published

2018

30. The Interaction between Sildenafil and Phenobarbital in Infants with Congenital Heart Defects

Author

Walter E. Haefeli, Johannes N. van den Anker, Gilbert Koch, Juergen Burhenne, Victoria C. Ziesenitz, Sabine Grommes, Gerd Mikus, and Matthias Gorenflo

Subjects

chemistry.chemical_compound, chemistry, business.industry, Sildenafil, Applied Mathematics, General Mathematics, Anesthesia, medicine, Phenobarbital, business, medicine.drug

Published

2018

31. Higher chlorzoxazone clearance in obese children compared with none-obese peers, an open-label explorative pharmacokinetic study of CYP2E1 activity

Author

Tonny Studsgaard Petersen, Hanne Rolighed Christensen, Jens C Holm, Jürgen Burhenne, Helle Holst, Elizaveta Chabanova, Camilla Schmeltz, Christina Gade, Gerd Mikus, and Kim Dalhoff

Subjects

Pharmacokinetics, business.industry, Applied Mathematics, General Mathematics, Chlorzoxazone, Medicine, Pharmacology, Open label, CYP2E1, business, medicine.drug

Published

2018

32. Correction to: Pharmacokinetics of Fentanyl and Its Derivatives in Children: A Comprehensive Review

Author

Janelle D. Vaughns, Victoria C. Ziesenitz, Gerd Mikus, Gilbert Koch, and Johannes N. van den Anker

Subjects

Pharmacology, business.industry, Remifentanil, 030226 pharmacology & pharmacy, Fentanyl, Sufentanil, 03 medical and health sciences, 0302 clinical medicine, Pharmacotherapy, Pharmacokinetics, 030202 anesthesiology, Anesthesia, medicine, Pharmacology (medical), Nasal administration, Dosing, Alfentanil, business, medicine.drug

Abstract

Fentanyl and its derivatives sufentanil, alfentanil, and remifentanil are potent opioids. A comprehensive review of the use of fentanyl and its derivatives in the pediatric population was performed using the National Library of Medicine PubMed. Studies were included if they contained original pharmacokinetic parameters or models using established routes of administration in patients younger than 18 years of age. Of 372 retrieved articles, 44 eligible pharmacokinetic studies contained data of 821 patients younger than 18 years of age, including more than 46 preterm infants, 64 full-term neonates, 115 infants/toddlers, 188 children, and 28 adolescents. Underlying diagnoses included congenital heart and pulmonary disease and abdominal disorders. Routes of drug administration were intravenous, epidural, oral-transmucosal, intranasal, and transdermal. Despite extensive use in daily clinical practice, few studies have been performed. Preterm and term infants have lower clearance and protein binding. Pharmacokinetics was not altered by chronic renal or hepatic disease. Analyses of the pooled individual patients’ data revealed that clearance maturation relating to body weight could be best described by the Hill function for sufentanil (R 2 = 0.71, B max 876 mL/min, K 50 16.3 kg) and alfentanil (R 2 = 0.70, B max (fixed) 420 mL/min, K 50 28 kg). The allometric exponent for estimation of clearance of sufentanil was 0.99 and 0.75 for alfentanil clearance. Maturation of remifentanil clearance was described by linear regression to bodyweight (R 2 = 0.69). The allometric exponent for estimation of remifentanil clearance was 0.76. For fentanyl, linear regression showed only a weak correlation between clearance and bodyweight in preterm and term neonates (R 2 = 0.22) owing to a lack of data in older age groups. A large heterogeneity regarding study design, clinical setting, drug administration, laboratory assays, and pharmacokinetic estimation was observed between studies introducing bias into the analyses performed in this review. A limitation of this review is that pharmacokinetic data, based on different modes of administration, dosing schemes, and parameter estimation methods, were combined.

Published

2017

33. Real-world complexity of atrial fibrillation treatment with oral anticoagulants: design and interpretation of pharmacoepidemiological studies

Author

Andreas D. Meid, Gerd Mikus, Walter E. Haefeli, and Sarah Mächler

Subjects

Pharmacology, medicine.medical_specialty, business.industry, Interpretation (philosophy), Atrial fibrillation, 030204 cardiovascular system & hematology, Pharmacoepidemiology, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Cardiology, Pharmacology (medical), 030212 general & internal medicine, Myocardial infarction, business, Letter to the Editor

Published

2017

34. Pharmacokinetics of Fentanyl and Its Derivatives in Children: A Comprehensive Review

Author

Johannes N. van den Anker, Gerd Mikus, Victoria C. Ziesenitz, Janelle D. Vaughns, Gilbert Koch, and Pediatric Surgery

Subjects

Adolescent, Sufentanil, Remifentanil, Models, Biological, 030226 pharmacology & pharmacy, Article, Fentanyl, 03 medical and health sciences, 0302 clinical medicine, Pharmacotherapy, Pharmacokinetics, 030202 anesthesiology, medicine, Humans, Pharmacology (medical), Dosing, Alfentanil, Child, Pharmacology, business.industry, Body Weight, Infant, Newborn, Infant, 3. Good health, Analgesics, Opioid, Child, Preschool, Anesthesia, Linear Models, Nasal administration, business, medicine.drug

Abstract

Fentanyl and its derivatives sufentanil, alfentanil, and remifentanil are potent opioids. A comprehensive review of the use of fentanyl and its derivatives in the pediatric population was performed using the National Library of Medicine PubMed. Studies were included if they contained original pharmacokinetic parameters or models using established routes of administration in patients younger than 18 years of age. Of 372 retrieved articles, 44 eligible pharmacokinetic studies contained data of 821 patients younger than 18 years of age, including more than 46 preterm infants, 64 full-term neonates, 115 infants/toddlers, 188 children, and 28 adolescents. Underlying diagnoses included congenital heart and pulmonary disease and abdominal disorders. Routes of drug administration were intravenous, epidural, oral-transmucosal, intranasal, and transdermal. Despite extensive use in daily clinical practice, few studies have been performed. Preterm and term infants have lower clearance and protein binding. Pharmacokinetics was not altered by chronic renal or hepatic disease. Analyses of the pooled individual patients’ data revealed that clearance maturation relating to body weight could be best described by the Hill function for sufentanil (R 2 = 0.71, B max 876 mL/min, K 50 16.3 kg) and alfentanil (R 2 = 0.70, B max (fixed) 420 mL/min, K 50 28 kg). The allometric exponent for estimation of clearance of sufentanil was 0.99 and 0.75 for alfentanil clearance. Maturation of remifentanil clearance was described by linear regression to bodyweight (R 2 = 0.69). The allometric exponent for estimation of remifentanil clearance was 0.76. For fentanyl, linear regression showed only a weak correlation between clearance and bodyweight in preterm and term neonates (R 2 = 0.22) owing to a lack of data in older age groups. A large heterogeneity regarding study design, clinical setting, drug administration, laboratory assays, and pharmacokinetic estimation was observed between studies introducing bias into the analyses performed in this review. A limitation of this review is that pharmacokinetic data, based on different modes of administration, dosing schemes, and parameter estimation methods, were combined.

Published

2017

35. The NTCP-inhibitor Myrcludex B: Effects on Bile Acid Disposition and Tenofovir Pharmacokinetics

Author

Thomas Bruckner, A. Alexandrov, Antje Blank, Nicolas Hohmann, Stephan Urban, Juergen Burhenne, Johanna Weiss, Katrin Meier, Gerd Mikus, Hans H. Maurer, Walter E. Haefeli, Michael Schwab, Annette Eidam, Mathias Haag, Meyer, and Sfj van de Graaf

Subjects

Adult, Male, 0301 basic medicine, Organic anion transporter 1, medicine.drug_class, CYP3A, Injections, Subcutaneous, Administration, Oral, Organic Anion Transporters, Sodium-Dependent, Pharmacology, Antiviral Agents, Risk Assessment, Bile Acids and Salts, Lipopeptides, Young Adult, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Pharmacokinetics, Cholestasis, medicine, Cytochrome P-450 CYP3A, Humans, Drug Interactions, Pharmacology (medical), Prospective Studies, Tenofovir, SLC10A1, Symporters, biology, Bile acid, Chemistry, Middle Aged, Hepatitis B, medicine.disease, Taurocholic acid, Up-Regulation, 030104 developmental biology, biology.protein, Reverse Transcriptase Inhibitors, Female, 030211 gastroenterology & hepatology, Biomarkers

Abstract

Myrcludex B acts as a hepatitis B and D virus entry inhibitor blocking the sodium taurocholate cotransporting polypeptide (SLC10A1). We investigated the effects of myrcludex B on plasma bile acid disposition, tenofovir pharmacokinetics, and perpetrator characteristics on cytochrome P450 (CYP) 3A. Twelve healthy volunteers received 300 mg tenofovir disoproxil fumarate orally and 10 mg subcutaneous myrcludex B. Myrcludex B increased total plasma bile acid exposure 19.2-fold without signs of cholestasis. The rise in conjugated bile acids was up to 124-fold (taurocholic acid). Coadministration of tenofovir with myrcludex B revealed no relevant changes in tenofovir pharmacokinetics. CYP3A activity slightly but significantly decreased by 29% during combination therapy. Myrcludex B caused an asymptomatic but distinct rise in plasma bile acid concentrations and had no relevant impact on tenofovir pharmacokinetics. Changes in CYP3A activity might be due to alterations in bile acid signaling. Long-term effects of elevated bile acids will require critical evaluation.

Published

2017

36. Management von chronischem Schmerz mit retardiertem Tilidin

Author

Jürgen Burhenne, C. Wolfert, G. Stammler, Gerd Mikus, Antje Blank, A. M. Meid, M. Merbach, and O. Emrich

Subjects

Gynecology, medicine.medical_specialty, business.industry, Chronic pain, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, Anesthesiology and Pain Medicine, Medicine, 030212 general & internal medicine, Neurology (clinical), Extended release, business, Tilidine, 030217 neurology & neurosurgery, medicine.drug

Abstract

Das synthetisch hergestellte Opioid Tilidin wird zur Behandlung chronischer Schmerzen eingesetzt. Jedoch ist der Metabolismus des Prodrugs zum analgetisch aktiven Metaboliten Nortilidin im klinischen Setting bisher nicht untersucht. Daher wurden Effektivitat der Schmerztherapie, Metabolismus von Tilidin sowie die Lebensqualitat bei chronischen Schmerzpatienten untersucht. In diese multizentrische Beobachtungsstudie wurden 48 Patienten eingeschlossen. Diese nahmen eine seit mindestens 7 Tagen konstante Dosis eines retardierten Tilidinpraparats ein. Die Komedikation wurde erfasst und eine Blutentnahme zur Bestimmung von Leber- und Nierenfunktion wurde durchgefuhrt. Im restlichen Plasma wurden die Konzentrationen von Tilidin, Nortilidin und Bisnortilidin mithilfe einer validierten LC/MS/MS-Methode bestimmt. Jeder Patient fullte standardisierte Fragebogen zur Erfassung der Lebensqualitat aus. Die mittlere Tagesdosis betrug 180 mg Tilidin. Die dosisnormalisierten Plasmakonzentrationen des aktiven Metaboliten Nortilidin lagen zwischen 1,6 ng/ml und 76,5 ng/ml (29,2 ± 25,1 ng/ml). Das Verhaltnis Tilidin zu Nortilidin betrug im Mittel 0,28 (Median = 0,13, Standardabweichung = 0,67). Die Anzahl der eingenommenen Medikamente variierte zwischen 1 und 14. Etwa 66 % der Patienten hatten eine suffiziente analgetische Therapie, unter Tilidin wurden kaum opioidinduzierte Obstipationen berichtet. Nur wenige Patienten hatten eine eingeschrankte Leber- oder Nierenfunktion, die Nortilidinkonzentrationen wurden dadurch nicht beeinflusst. Bei einer Schmerztherapie mit Tilidin werden variable Konzentrationen des aktiven Metaboliten Nortilidin beobachtet, die aber wenn uberhaupt nur unwesentlich durch Komedikation oder Einschrankungen von Leber- oder Nierenfunktion verandert werden. Nebenwirkungen traten kaum in Erscheinung, auch nicht die opioidinduzierte Obstipation.

Published

2017

37. Autoinhibitory properties of the parent but not of the N-oxide metabolite contribute to infusion rate-dependent voriconazole pharmacokinetics

Author

Antje Blank, Nicolas Hohmann, Walter E. Haefeli, Johanna Weiss, Jürgen Burhenne, Rebecca Kreuter, and Gerd Mikus

Subjects

0301 basic medicine, Pharmacology, Voriconazole, CYP3A4, CYP3A, Metabolite, 030106 microbiology, Urine, 030226 pharmacology & pharmacy, Crossover study, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Pharmacokinetics, medicine, Midazolam, Pharmacology (medical), medicine.drug

Abstract

Aims The pharmacokinetics of voriconazole show a nonlinear dose-exposure relationship caused by inhibition of its own CYP3A-dependent metabolism. Because the magnitude of autoinhibition also depends on voriconazole concentrations, infusion rate might modulate voriconazole exposure. The impact of four different infusion rates on voriconazole pharmacokinetics was investigated. Methods Twelve healthy participants received 100 mg voriconazole intravenous over 4 h, 400 mg over 6 h, 4 h, and 2 h in a crossover design. Oral midazolam (3 μg) was given at the end of infusion. Blood and urine samples were collected up to 48 h. Voriconazole and its N-oxide metabolite were quantified using high-performance liquid chromatography coupled to tandem mass spectrometry. Midazolam estimated metabolic clearance (eCLmet) was calculated using a limited sampling strategy. Voriconazole-N-oxide inhibition of cytochrome P450 (CYP) isoforms 2C19 and 3A4 were assessed with the P450-Glo luminescence assay. Results Area under the concentration-time curve for 400 mg intravenous voriconazole was 16% (90% confidence interval: 12-20%) lower when administered over 6 h compared to 2 h infusion. Dose-corrected area under the concentration-time curve for 100 mg over 4 h was 34% lower compared to 400 mg over 4 h. Midazolam eCLmet was 516 ml min-1 (420-640) following 100 mg 4 h-1 voriconazole, 152 ml min-1 (139-166) for 400 mg 6 h-1 , 192 ml min-1 (167-220) for 400 mg 4 h-1 , and 202 ml min-1 (189-217) for 400 mg 2 h-1 . Concentration giving 50% CYP inhibition of voriconazole N-oxide was 146 ± 23 μmol l-1 for CYP3A4, and 40.2 ± 4.2 μmol l-1 for CYP2C19. Conclusions Voriconazole pharmacokinetics is modulated by infusion rate, an autoinhibitory contribution voriconazole metabolism by CYP3A and 2C19 and to a lesser extent its main N-oxide metabolite for CYP2C19. To avoid reduced exposure, the infusion rate should be 2 h.

Published

2017

38. Semisimultaneous Midazolam Administration to Evaluate the Time Course of CYP3A Activation by a Single Oral Dose of Efavirenz

Author

Gerd Mikus, Johanna Weiss, Julia Bödigheimer, Jürgen Burhenne, Tilman Heinrich, Walter E. Haefeli, Anne‐Kathrin Matthee, and Claudia Röder

Subjects

0301 basic medicine, Pharmacology, Efavirenz, Reverse-transcriptase inhibitor, business.industry, CYP3A, 030106 microbiology, 030226 pharmacology & pharmacy, Single oral dose, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, In vivo, Anesthesia, Time course, Medicine, Midazolam, heterocyclic compounds, Pharmacology (medical), business, medicine.drug

Abstract

This study aimed to assess whether a single oral dose of the nonnucleoside reverse transcriptase inhibitor efavirenz can alter CYP3A in vivo. In 12 healthy participants individual CYP3A activity was quantified using a semisimultaneous methodology (midazolam orally and 6 hours later intravenously) both alone and during a period of 22 days after a single oral dose of 400 mg efavirenz. Twelve hours after efavirenz administration, midazolam apparent oral clearance was significantly increased by 70%, and midazolam systemic clearance after intravenous administration was significantly increased by 27%. Similar effects were still present on day 6, after which midazolam clearances slowly returned to baseline on day 22. At least on day 1, the midazolam clearance increase is consistent with the in vitro observed CYP3A activation. The onset of an efavirenz treatment will almost immediately result in enhanced elimination of CYP3A substrates.

Published

2017

39. Use of Fentanyl in Adolescents with Clinically Severe Obesity Undergoing Bariatric Surgery: A Pilot Study

Author

Alvina Mushtaq, Victoria C. Ziesenitz, Ricarda Bachmann, Johannes N. van den Anker, Janelle D. Vaughns, Gisela Skopp, Elaine F Williams, Johanna Weiss, Gerd Mikus, and Pediatric Surgery

Subjects

medicine.medical_specialty, Adolescent, Narcotic, medicine.medical_treatment, Bariatric Surgery, Pilot Projects, 030226 pharmacology & pharmacy, Fentanyl, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Pharmacokinetics, SDG 3 - Good Health and Well-being, 030202 anesthesiology, medicine, Humans, Pharmacology (medical), Dosing, Prospective Studies, Young adult, Prospective cohort study, Volume of distribution, business.industry, medicine.disease, Obesity, Surgery, Obesity, Morbid, Anesthesia, Pediatrics, Perinatology and Child Health, Administration, Intravenous, Female, business, Anesthetics, Intravenous, medicine.drug

Abstract

The number of obese pediatric patients requiring anesthesia is rapidly increasing. Although fentanyl is a commonly used narcotic during surgery, there are no pharmacokinetic (PK) data available for optimal dosing of fentanyl in adolescents with clinically severe obesity. An institutional review board-approved exploratory pilot study was conducted in six adolescents aged 14–19 years undergoing bariatric surgery. Mean total body weight (TBW) and mean BMI were 137.4 ± 14.3 kg and 49.6 ± 6.4 kg/m2 (99.5th BMI percentile), respectively. Fentanyl was administered intravenously for intraoperative analgesia based on ideal body weight per standard of care. PK blood samples were drawn over a 24-h post-dose period. Fentanyl PK parameters were calculated by non-compartmental analysis. Mean fentanyl AUC0–∞ was 1.5 ± 0.5 h·ng/mL. Systemic clearance of fentanyl was 1522 ± 310 mL/min and 11.2 ± 2.6 mL/min·kg TBW. Volume of distribution was 635 ± 282 L and 4.7 ± 2.1 L/kg TBW. While absolute clearance was increased, absolute volume of distribution was comparable to previously established adult values. These results suggest that fentanyl clearance is enhanced in adolescents with clinically severe obesity while volume of distribution is comparable to previously published studies. NCT01955993 (clinicaltrials.gov).

Published

2017

40. Who is a ‘healthy subject’?—consensus results on pivotal eligibility criteria for clinical trials

Author

Karin Goehler, Thomas Sudhop, Martin Coenen, Klaus Peter Kammerer, Klaus Francke, Georg Wensing, Hildegard Sourgens, Jens Rengelshausen, Frank Donath, Mario Iovino, Kerstin Breithaupt-Groegler, Reinhard Schinzel, Gerd Mikus, Christoph Coch, and Katharina Erb-Zohar

Subjects

medicine.medical_specialty, Consensus, Health Status, education, Pharmacology toxicology, Alternative medicine, Inclusion/exclusion criteria, Blood Pressure, Review, 030226 pharmacology & pharmacy, German, 03 medical and health sciences, Electrocardiography, 0302 clinical medicine, Phase I, Safety parameters, Medicine, Stopping rules, Humans, Pharmacology (medical), 030212 general & internal medicine, health care economics and organizations, Pharmaceutical industry, Pharmacology, Clinical Trials, Phase I as Topic, business.industry, Healthy subjects, Ethics committee, General Medicine, Investigational medicinal product, language.human_language, Healthy Volunteers, Clinical trial, Family medicine, language, business, Healthy subject

Abstract

Introduction/Methods A discussion forum was hosted by the German not-for-profit Association for Applied Human Pharmacology (AGAH e.V.) to critically review key eligibility criteria and stopping rules for clinical trials with healthy subjects, enrolling stakeholders from the pharmaceutical industry, contract research organisations, academia, ethics committees and competent authority. Results Pivotal eligibility criteria were defined for trials with new investigational medicinal products (IMPs) or with clinically established IMPs. In general, a pulse rate ranging between 50 and 90 beats/min is recommended for first-in-human (FIH) trials, while wider ranges seem acceptable for trials with clinically established IMPs, provided there are no indications of thyroid dysfunction. Hepatic laboratory parameters not to exceed the upper limit of normal (ULN) comprise ALT (alanine aminotransferase) and AST (aspartate aminotransferase) in FIH trials, whereas slight elevations (10% above ULN) seem acceptable in trials with clinically established IMPs without known hepatotoxicity. A normal renal function is required for any clinical trial in healthy subjects. A risk-adapted approach for stopping rules was adopted. Stopping rules for an individual subject are one adverse event of severe intensity or one serious adverse event. In case of a severe adverse event, some stakeholders demand a causal relationship with the IMP (i.e. an adverse reaction). Stopping rules for a cohort are one serious adverse reaction or ≥50% of subjects experiencing any adverse reaction of moderate or severe intensity. Consequences The application of this consensus resulted in a reduction in protocol deficiencies issued by the competent authority.

Published

2017

41. Impact of pantoprazole on absorption and disposition of hydroxychloroquine, a drug used in Corona Virus Disease-19 (Covid-19): A structured summary of a study protocol for a randomised controlled trial

Author

Katja Häußler, Walter E. Haefeli, Felicitas Stoll, Antje Blank, Amin Muhareb, Gerd Mikus, Simon Hermann, David Czock, Simone Hummler, Kathrin I. Foerster, Johanna Weiss, and Jürgen Burhenne

Subjects

medicine.medical_specialty, Letter, Trial protocol, Midazolam, Cmax, Medicine (miscellaneous), law.invention, Absorption, Randomized controlled trial, law, Internal medicine, Clinical endpoint, Medicine, Pharmacology (medical), Pantoprazole, Randomised controlled trial, lcsh:R5-920, business.industry, Area under the curve, Yohimbine, COVID-19, Hydroxychloroquine, Clinical trial, Microdosing, business, lcsh:Medicine (General), medicine.drug, Drug-drug interaction

Abstract

Objectives Primary objective: Evaluation of the effect of the proton pump inhibitor (PPI) pantoprazole on the absorption of hydroxychloroquine (HCQ). Secondary objectives: • Evaluation of the relationship between HCQ concentrations in whole blood, plasma and intracellular concentrations in target cells - peripheral blood mononuclear cells (PBMCs). • Evaluation of HCQ as a potential perpetrator in drug-drug interactions at the level of cytochrome P450 (CYP) 3A4 and CYP2D6 (major drug metabolizing enzymes). Trial design Single centre, open-label, parallel group, two-arm, phase I drug-drug interaction trial. Participants Healthy volunteers (18-60 years old) are treated in the Clinical Pharmacological Trial Center of Heidelberg University Hospital, Germany. Intervention and comparator • Participants are randomized in a group to either receive a nine-day course of pantoprazole, or to a control group without pantoprazole. All participants receive a single dose of HCQ 400 mg. • Additionally, CYP3A4 and CYP2D6 phenotyping with microdosed probe drugs is performed using midazolam and yohimbine as enzyme activity markers, respectively. Main outcomes Primary endpoint: Area under the curve (AUC)0-72 h and maximum concentration (Cmax) of a single oral dose of 400 mg HCQ with and without pantoprazole (changes in these two values describe relevant aspects of exposure to HCQ with and without administration of pantoprazole). Secondary endpoints: • AUC2-4 h, AUC0-6 h and Cmax of midazolam and yohimbine. • Correlation of HCQ concentrations in whole blood with concentrations in plasma and peripheral blood mononuclear cells (PBMC). Randomisation Participants are assigned to treatment groups by using a randomisation list (1:1, block size = 4) and consecutive enrolment. Blinding (masking) The trial is an open-label trial, participants and investigators are not blinded. Numbers to be randomised (sample size) A total number of 24 participants (12 per group) are planned to be randomised. Trial Status Protocol version 2.1 dated 24/04/2020, first patient first visit. April 30th, 2020, recruitment ongoing, anticipated end of study June 30th, 2020. Trial registration EudraCT Number: 2020-001470-30, registered on 31 March 2020 German Clinical trials register number / International Clinical Trials Registry Platform: DRKS00021573, registered on 27 April 2020 Full protocol The full trial 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 trial protocol. The trial protocol has been reported in accordance with the Standard Protocol Items: Recommendations for Clinical Interventional Trials (SPIRIT) guidelines (Additional file 2).

Published

2020

42. Midazolam Pharmacokinetics in Obese and Non-obese Children and Adolescents

Author

Gerd Mikus, Hanne Rolighed Christensen, Jens-Christian Holm, Kim Dalhoff, Jürgen Burhenne, Jesper Sonne, Christina Gade, Helle Holst, Mia Østergaard Johansen, Eva Sverrisdóttir, and Trine Meldgaard Lund

Subjects

Pediatric Obesity, Adolescent, Midazolam, 030226 pharmacology & pharmacy, Models, Biological, Body Mass Index, 03 medical and health sciences, 0302 clinical medicine, MicroDose, Pharmacokinetics, medicine, Distribution (pharmacology), Humans, Pharmacology (medical), 030212 general & internal medicine, Dosing, Child, Pharmacology, Volume of distribution, business.industry, Body Weight, Buccal administration, Anesthesia, business, Body mass index, medicine.drug

Abstract

Midazolam is a first-line drug for the treatment of status epilepticus, both by buccal and intravenous administration. In children and adolescents with obesity, midazolam pharmacokinetics may be altered, and the current dosing guidelines may therefore be insufficient. The objective of this study was to investigate the pharmacokinetics of midazolam, after intravenous administration, in obese and non-obese adolescents aged 11–18 years. All trial participants received a 1-µg midazolam microdose as an intravenous bolus. 13 blood samples were collected per participant at pre-specified timepoints. Plasma concentration–time data were fitted to pharmacokinetic models using non-linear mixed-effects modeling. Covariates such as weight, age, and body mass index standard deviation score were tested to explain the inter-individual variability associated with the pharmacokinetic parameters. Sixty-seven adolescents were included in the analysis. The pharmacokinetics of midazolam was best described with a two-compartment model. The rate of distribution was faster, and the peripheral volume of distribution was larger in adolescents with a high body mass index standard deviation score compared with adolescents with a lower standard deviation score. Simulations revealed that long-term infusions based on total body weight could lead to high plasma concentrations in adolescents with obesity. Furthermore, simulated plasma concentrations after a fixed buccal dose indicated that adolescents with obesity may be at risk of sub-therapeutic midazolam plasma concentrations. The body mass index standard deviation score was shown to have a significant influence on the peripheral volume of distribution and the inter-compartmental clearance of midazolam. The current dosing guidelines for status epilepticus, where the midazolam dose is adjusted to total body weight or age, may lead to supra- and sub-therapeutic plasma concentrations, respectively, in adolescents with obesity. EudraCT: 2014-004554-34.

Published

2019

43. Novel insights into the complex pharmacokinetics of voriconazole: a review of its metabolism

Author

Robin Michelet, Charlotte Kloft, Josefine Schulz, Gerd Mikus, and Franziska Kluwe

Subjects

Voriconazole, Metabolizing enzymes, biology, business.industry, Nonlinear pharmacokinetics, Cytochrome P450, Metabolism, Bioinformatics, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, Therapeutic index, Pharmacokinetics, 030220 oncology & carcinogenesis, biology.protein, Medicine, Animals, Cytochrome P-450 CYP3A Inhibitors, Humans, Pharmacology (medical), Dosing, General Pharmacology, Toxicology and Pharmaceutics, business, medicine.drug

Abstract

Voriconazole, a second-generation triazole frequently used for the prophylaxis and treatment of invasive fungal infections, undergoes complex metabolism mainly involving various (polymorphic) cytochrome P450 enzymes in humans. Although high inter- and intraindividual variability in voriconazole pharmacokinetics have been observed and the therapeutic range for this compound is relatively narrow, the metabolism of voriconazole has not been fully elucidated yet. The available literature data investigating the multiple different pathways and metabolites are extremely unbalanced and thus the absolute or relative contribution of the different pathways and enzymes involved in the metabolism of voriconazole remains uncertain. Furthermore, other factors such as nonlinear pharmacokinetics caused by auto-inhibition or -induction and polymorphisms of the metabolizing enzymes hinder safe and effective voriconazole dosing in clinical practice and have not yet been studied sufficiently. This review aimed at amalgamating the available literature on the pharmacokinetics of voriconazole in vitro and in vivo, with a special focus on metabolism in adults and children, in order to congregate an overall landscape of the current body of knowledge and identify knowledge gaps, opening the way towards further research in order to foster the understanding, towards better therapeutic dosing decisions.

Published

2019

44. Decreased Cytochrome P450 3A activity in palliative patients with haematological diseases: Potential impact on supportive drug therapies

Author

Hubert J. Bardenheuer, Gerd Mikus, Nelly Siller, Marcus J. P. Geist, Juergen Burhenne, and Gerlinde Egerer

Subjects

Adult, Drug, medicine.medical_specialty, Metabolic Clearance Rate, Midazolam, media_common.quotation_subject, Administration, Oral, Toxicology, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Oral administration, Hematologic Agents, Internal medicine, medicine, Cytochrome P-450 CYP3A, Humans, Drug Interactions, Prospective Studies, Dosing, Aged, media_common, Pharmacology, business.industry, Palliative Care, Area under the curve, General Medicine, Middle Aged, Drug interaction, Hematologic Diseases, Healthy Volunteers, Biological Variation, Population, Area Under Curve, Case-Control Studies, Liver function, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

Cytochrome P450 3A (CYP3A) is the most relevant drug-metabolizing enzyme in human beings involved in the elimination of about 50% of the marketed drugs. Comprehensive in vivo data of CYP3A activity in palliative patients with haematological diseases are missing. Therefore, CYP3A activity was determined under real-life clinical conditions in patients to gain knowledge about dose adjustments for supportive therapies and symptom management in haematology. The single-arm, prospective trial obtained a 4-hours pharmacokinetic profile of midazolam after oral administration of a microdose as marker substance from each enrolled patient. Plasma concentrations of midazolam and its primary metabolite 1'-hydroxy-midazolam were quantified by mass spectrometry techniques. CYP3A activity was calculated as partial metabolic clearance from an established limited sampling area under the curve. All other drugs taken by the participating patients were considered as well as recent laboratory test results and the patients' diagnoses. Partial metabolic clearance of midazolam in patients with haematological diseases was highly variable (36.9 ± 52.7 L/h). In comparison with the CYP3A activity of healthy individuals, this was a highly significant 30% reduction of activity (P < 0.0001). Dosing of major CYP3A substrate drugs needs to be reduced in palliative patients with haematological diseases, otherwise escalation of debilitating symptoms due to drug interactions might occur.

Published

2019

45. Microdosed Cocktail of Three Oral Factor Xa Inhibitors to Evaluate Drug-Drug Interactions with Potential Perpetrator Drugs

Author

Walter E. Haefeli, Marie-Louise Lehmann, Gerd Mikus, Jürgen Burhenne, Marlene Schaumaeker, and Kathrin I. Foerster

Subjects

Drug, Adult, Male, medicine.drug_mechanism_of_action, Adolescent, Pyridines, Pyridones, media_common.quotation_subject, Factor Xa Inhibitor, Administration, Oral, 030204 cardiovascular system & hematology, Pharmacology, 030226 pharmacology & pharmacy, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Pharmacokinetics, Rivaroxaban, Edoxaban, Tandem Mass Spectrometry, Atrial Fibrillation, medicine, Humans, Pharmacology (medical), Drug Interactions, media_common, Cross-Over Studies, business.industry, Drug interaction, Middle Aged, Thiazoles, Ketoconazole, chemistry, Case-Control Studies, Cytochrome P-450 CYP3A Inhibitors, Pyrazoles, Apixaban, Female, business, medicine.drug, Chromatography, Liquid, Factor Xa Inhibitors

Abstract

The aim of this study was to prove the suitability of simultaneously administered microdoses of the factor Xa inhibitors (FXaIs) rivaroxaban, apixaban and edoxaban (100 µg in total). To evaluate drug–drug interactions, the impact of ketoconazole, a known strong inhibitor of cytochrome P450 3A4 and P-glycoprotein, was studied. In a crossover clinical trial, 18 healthy volunteers were randomized to the two treatments using microdoses of rivaroxaban, apixaban and edoxaban alone and when coadministered with ketoconazole. Plasma and urine concentrations of microdosed apixaban, edoxaban and rivaroxaban were quantified using a validated ultra-performance liquid chromatography–tandem mass spectrometry assay with a lower limit of quantification of 2.5 pg/ml. The microdosed FXaI cocktail showed similar pharmacokinetic parameters compared with published data, using normal therapeutic doses of each FXaI. Ketoconazole significantly increased exposure, with geometric mean AUC ratios of 1.90 (apixaban), 2.35 (edoxaban) and 2.27 (rivaroxaban). The microdosed FXaI cocktail approach was able to precisely predict the drug interaction with ketoconazole. This is the first study that has been conducted to evaluate drug–drug interactions with a drug class, and the low administered doses also allow evaluation in vulnerable target populations. EudraCT 2016-003024-23.

Published

2019

46. Ketoconazole and Liver Injury: A Five-Year Update

Author

Gerd Mikus and David J. Greenblatt

Subjects

Liver injury, medicine.medical_specialty, Antifungal Agents, business.industry, MEDLINE, Pharmaceutical Science, medicine.disease, Healthy Volunteers, Text mining, Ketoconazole, Internal medicine, Healthy volunteers, medicine, Humans, Pharmacology (medical), Drug Interactions, Chemical and Drug Induced Liver Injury, business, medicine.drug, Tablets

Published

2019

47. First-in-human application of the novel hepatitis B and hepatitis D virus entry inhibitor myrcludex B

Author

Antje Blank, Walter E. Haefeli, Gerd Mikus, Nicolas Hohmann, Christoph Markert, Thorsten Lehr, A. Alexandrov, Alexandra Carls, Stephan Urban, Mathias Haag, and Matthias Schwab

Subjects

0301 basic medicine, Hepatitis B virus, HBsAg, Hepatology, business.industry, Phases of clinical research, Pharmacology, Hepatitis B, medicine.disease, medicine.disease_cause, Bioavailability, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Tolerability, Pharmacokinetics, medicine, 030211 gastroenterology & hepatology, Hepatitis D virus, business

Abstract

Background & Aims Myrcludex B is a first-in-class compound, which blocks entry of hepatitis B and D virus into hepatocytes in vitro and in animal models. Based on the required preclinical data we aimed to translate this compound into the first application in humans. Methods Single ascending doses of myrcludex B, a 47 amino acid peptide, were administered up to 20mg intravenously and 10mg subcutaneously in a prospective open first-in-human, phase I clinical trial to 36 healthy volunteers. Safety, tolerability and plasma concentrations of myrcludex B were assessed and a pharmacokinetic model was derived. Results Myrcludex B was well tolerated and no serious or relevant AEs representing off-target effects, and no immunogenic effects were observed up to the highest applied dose of 20mg (intravenously). Myrcludex B showed dose-dependent pharmacokinetics, best described by a 2-compartment target-mediated drug disposition model. Bioavailability of the subcutaneous application was large (85%). Interindividual variability was moderate. The pharmacokinetic model suggested that subcutaneous doses of 10mg and above reach a target saturation of over 80% for at least 15h. Conclusions Myrcludex B showed excellent tolerability up to high doses. Pharmacologic properties followed a 2-compartment target-mediated drug disposition model. These findings are vital for planning of further multiple dose efficacy trials in patients. Lay summary After showing antiviral activity in cell culture and animal models, myrcludex B, a new drug intended for the treatment of hepatitis B and D, has been administered the first time in humans. Healthy volunteers received the drug intravenously and subcutaneously up to high doses (20mg). The drug was well tolerated and the characteristics of the drug determining its way in the human body could be described. These results will allow testing myrcludex B in hepatitis B and D patients.

Published

2016

48. No Increased Risk of Ketoconazole Toxicity in Drug-Drug Interaction Studies

Author

Noémi Outeiro, Gerd Mikus, and Nicolas Hohmann

Subjects

Pharmacology, Antifungal Agents, business.industry, Drug interaction, 030226 pharmacology & pharmacy, 03 medical and health sciences, Ketoconazole, 0302 clinical medicine, Pharmacotherapy, Oral administration, 030220 oncology & carcinogenesis, Toxicity, Animals, Cytochrome P-450 CYP3A Inhibitors, Humans, Medicine, Drug Interactions, Pharmacology (medical), Liver function, Adverse effect, business, Drug metabolism, medicine.drug

Abstract

In July 2013 the U.S. Food and Drug Administration (FDA) released a safety announcement regarding the use of ketoconazole and its adverse drug reactions. The FDA report advised against the use ketoconazole tablets as a first-line treatment for any fungal infections because of the risk of potentially serious drug-drug interactions and liver and adrenal gland complications. The European Medicines Agency (EMA) also proposed to limit the use of oral ketoconazole in fungal infections because of the same risk of harmful effects and interactions. In addition, the FDA also advised against the use of oral ketoconazole in drug interaction studies, in which it has been extensively used as an index inhibitor of drug metabolism. The aim of this investigation was to evaluate the risks of ketoconazole-induced hepatotoxicity described by the FDA and EMA in published drug interaction studies with ketoconazole and compare these data with the toxicity reported for ketoconazole when used as antifungal treatment. In the drug interaction studies (2355 participants; healthy volunteers and patients; median treatment duration, 6 days), only 40 participants were reported to have increased liver transaminase activity (1.7%), and no deaths were reported or associated with ketoconazole. In studies investigating ketoconazole treatment, patients were treated for 276 days (median), and 5.6% of patients had elevated liver enzyme activity. Because of the short treatment period in drug interaction studies the risk of drug-induced hepatic injury is considered very low. As such, we recommend that ketoconazole remain a safe CYP3A index inhibitor for use in drug interaction studies with healthy volunteers.

Published

2016

49. Ultrasensitive quantification of the CYP2E1 probe chlorzoxazone and its main metabolite 6-hydroxychlorzoxazone in human plasma using ultra performance liquid chromatography coupled to tandem mass spectrometry after chlorzoxazone microdosing

Author

Yosuke Suzuki, Jürgen Burhenne, Nicolas Hohmann, Gerd Mikus, Lukas Witt, and Walter E. Haefeli

Subjects

Microdosing, Electrospray ionization, Clinical Biochemistry, Administration, Oral, Tandem mass spectrometry, 030226 pharmacology & pharmacy, 01 natural sciences, Biochemistry, High-performance liquid chromatography, Analytical Chemistry, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Limit of Detection, Tandem Mass Spectrometry, medicine, Humans, Chromatography, High Pressure Liquid, Detection limit, Chromatography, Chemistry, 010401 analytical chemistry, Selected reaction monitoring, Reproducibility of Results, Cytochrome P-450 CYP2E1, Cell Biology, General Medicine, 0104 chemical sciences, Chlorzoxazone, medicine.drug

Abstract

Chlorzoxazone is a probe drug to assess cytochrome P450 (CYP) 2E1 activity (phenotyping). If the pharmacokinetics of the probe drug is linear, pharmacologically ineffective doses are sufficient for the purpose of phenotyping and adverse effects can thus be avoided. For this reason, we developed and validated an assay for the ultrasensitive quantification of chlorzoxazone and 6-hydroxychlorzoxazone in human plasma. Plasma (0.5mL) and liquid/liquid partitioning were used for sample preparation. Extraction recoveries ranged between 76 and 93% for both analytes. Extracts were separated within 3min on a Waters BEH C18 Shield 1.7μm UPLC column with a fast gradient consisting of aqueous formic acid and acetonitrile. Quantification was achieved using internal standards labeled with deuterium or (13)C and tandem mass spectrometry in the multiple reaction monitoring mode using negative electrospray ionization, which yielded lower limits of quantification of 2.5pgmL(-1), while maintaining a precision always below 15%. The calibrated concentration ranges were linear for both analytes (2.5-1000pgmL(-1)) with correlation coefficients of >0.99. Within-batch and batch-to-batch precision in the calibrated ranges for both analytes were

Published

2016

50. Treatment with rilpivirine does not alter plasma concentrations of the CYP3A substrates tadalafil and midazolam in humans

Author

Gerd Mikus, Sven Schnaidt, Alexandra Carls, Lukas Witt, Nicolas Hohmann, Walter E. Haefeli, Jürgen Burhenne, and Raphael Reinhard

Subjects

Adult, Male, Microbiology (medical), Adolescent, Combination therapy, Anti-HIV Agents, Sildenafil, Midazolam, Phases of clinical research, Pharmacology, 030226 pharmacology & pharmacy, Tadalafil, Plasma, Young Adult, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Pharmacokinetics, Cytochrome P-450 CYP3A, Humans, Medicine, Drug Interactions, Pharmacology (medical), business.industry, Rilpivirine, Middle Aged, Phosphodiesterase 5 Inhibitors, medicine.disease, Healthy Volunteers, Infectious Diseases, Erectile dysfunction, chemistry, 030220 oncology & carcinogenesis, cGMP-specific phosphodiesterase type 5, Female, business, medicine.drug

Abstract

OBJECTIVES Antiretroviral combination therapy of patients infected with HIV has greatly increased their life expectancy. Hence, the treatment of HIV-related long-term complications and age-related comorbidities has become more important. Reported incidence rates of erectile dysfunction (ED) and pulmonary arterial hypertension (PAH) are increasing in HIV-positive patients, potentially requiring treatment with phosphodiesterase 5 inhibitors such as sildenafil or tadalafil. In vitro, the NNRTI rilpivirine is both a pregnane X receptor agonist and cytochrome P450 (CYP) 3A inhibitor. Clinical data concerning the potential effects of rilpivirine coadministration on the pharmacokinetics of the CYP3A substrate tadalafil are lacking. METHODS We enrolled 20 healthy volunteers in an open-label, two-part, one-arm Phase I clinical trial to investigate acute and chronic effects of multiple doses of 25 mg of oral rilpivirine on single-dose and steady-state pharmacokinetics of multiple oral 20 mg doses of tadalafil. CYP3A activity was measured simultaneously with the oral midazolam microdose test. RESULTS We did not observe a change of tadalafil single-dose and steady-state exposure or of CYP3A activity measured at initiation, during maintenance and upon discontinuation of rilpivirine treatment after single-dose and chronic administration of rilpivirine. CONCLUSIONS Tadalafil can be combined with rilpivirine without dose adjustment or drug monitoring in HIV patients with ED or PAH. Rilpivirine at daily therapeutic doses of 25 mg does not induce or inhibit CYP3A-dependent drug metabolism.

Published

2016