Your search keyword '"Antje Blank"' showing total 79 results

1. Dose‐dependent induction of CYP3A activity by St. John's wort alone and in combination with rifampin

Author

Nicolas Hohmann, Anna S. Friedrichs, Jürgen Burhenne, Antje Blank, Gerd Mikus, and Walter E. Haefeli

Subjects

Therapeutics. Pharmacology, RM1-950, Public aspects of medicine, RA1-1270

Abstract

Abstract The dose dependence of the effect of enzyme inducers and the effect of the combined administration of two inducers that exert their effect via the same induction pathway (pregnane X receptor) have not been well studied. Using oral midazolam microdoses (30 μg), we have investigated CYP3A4 induction by St. John's wort (SJW) in 11 healthy volunteers using low (300 mg/day containing 7.48 mg hyperforin), therapeutic (900 mg/day), and supratherapeutic doses of SJW (1800 mg/day) for 14 days. SJW was then co‐administered with rifampin (600 mg/day) for a further 7 days to evaluate the effect of the combined administration of two inducers. In addition, intravenous midazolam microdoses (10 μg) were administered before SJW, at SJW 1800 mg/day, and during administration of the two inducers to assess the hepatic contribution to total induction (semi‐simultaneous administration). Administration of SJW increased oral midazolam clearance 1.96‐fold (300 mg/day), 3.86‐fold (900 mg/day), and 5.62‐fold (1800 mg/day), and 17.5‐fold after the addition of rifampin. Concurrently, the clearance of intravenous midazolam increased 2.05‐fold (1800 mg/day) and 2.93‐fold (SJW + rifampin). These results show that rifampin significantly enhances the induction of the highest SJW doses both hepatically and overall and suggest that these metabolic effects occur predominantly in the gut. These findings also suggest that in drug interactions involving strong and moderate enzyme inducers, the perpetrator effects of the strong inducer are decisive for the interaction.

Published

2024

2. Multifunctional IgG/IgM antibodies and cellular cytotoxicity are elicited by the full-length MSP1 SumayaVac-1 malaria vaccine

Author

Micha Rosenkranz, Kristin Fürle, Julia Hibbert, Anne Ulmer, Arin Ali, Thomas Giese, Antje Blank, Walter E. Haefeli, Ernst Böhnlein, Michael Lanzer, and Richard Thomson-Luque

Subjects

Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Radical control of malaria likely requires a vaccine that targets both the asymptomatic liver stages and the disease-causing blood stages of the human malaria parasite Plasmodium falciparum. While substantial progress has been made towards liver stage vaccines, the development of a blood stage vaccine is lagging behind. We have recently conducted a first-in-human clinical trial to evaluate the safety and immunogenicity of the recombinant, full-length merozoite surface protein 1 (MSP1FL) formulated with GLA-SE as adjuvant. Here, we show that the vaccine, termed SumayaVac-1, elicited both a humoral and cellular immune response as well as a recall T cell memory. The induced IgG and IgM antibodies were able to stimulate various Fc-mediated effector mechanisms associated with protection against malaria, including phagocytosis, release of reactive oxygen species, production of IFN-γ as well as complement activation and fixation. The multifunctional activity of the humoral immune response remained for at least 6 months after vaccination and was comparable to that of naturally acquired anti-MSP1 antibodies from semi-immune adults from Kenya. We further present evidence of SumayaVac-1 eliciting a recallable cellular cytotoxicity by IFN-γ producing CD8+ T cells. Our study revitalizes MSP1FL as a relevant blood stage vaccine candidate and warrants further evaluation of SumayaVac-1 in a phase II efficacy trial.

Published

2023

3. First‐in‐human, randomized, double‐blind, placebo‐controlled, dose escalation trial of the anti‐herpes simplex virus monoclonal antibody HDIT101 in healthy volunteers

Author

Antje Blank, Nicolas Hohmann, Marlen Dettmer, Anette Manka‐Stuhlik, Gerd Mikus, Felicitas Stoll, Marlies Stützle‐Schnetz, Daniel Thomas, Evelyn Exner, Beate Schmitt‐Bormann, Torsten Schaller, Rico Laage, Oliver Schönborn‐Kellenberger, Michaela Arndt, Walter E. Haefeli, and Jürgen Krauss

Subjects

Therapeutics. Pharmacology, RM1-950, Public aspects of medicine, RA1-1270

Abstract

Abstract HDIT101 is a first‐in‐class humanized monoclonal antibody recognizing a conserved epitope in glycoprotein B, a target present on the surface of herpes simplex virus 1 (HSV‐1) and HSV‐2 particles as well as on virus‐infected cells. This was a first‐in‐human, single‐center, double‐blind, placebo‐controlled trial in 24 healthy volunteers, randomized 3:1 (placebo:active) in each of the six dose levels with escalating doses up to 12,150 mg HDIT101. HDIT101 was administered intravenously, to study safety, pharmacokinetics (PKs), and immunogenicity. HDIT101 was well‐tolerated in all recipients and no serious or severe adverse events, no infusion‐related reactions, and no events suggestive of dose limiting off‐target toxicity occurred. The mean serum exposure (area under the curve from zero to infinity [AUC0‐∞]) of HDIT101 showed a linear increase from 4340 h*μg/ml at a dose of 50 mg to 1,122,247 h*μg/ml at a dose of 12,150 mg. No immunogenic effects following HDIT101 exposure were observed at any of the applied doses. HDIT101 demonstrated the expected PK properties of a monoclonal antibody was well‐tolerated, and could be safely administered even at excessively high doses that may be required for treatment of patients with septical HSV spread.

Published

2022

4. Evaluation of the drug-drug interaction potential of the novel hepatitis B and D virus entry inhibitor bulevirtide at OATP1B in healthy volunteers

Author

Vanessa Zhu, Jürgen Burhenne, Johanna Weiss, Mathias Haag, Ute Hofmann, Matthias Schwab, Stephan Urban, Gerd Mikus, David Czock, Walter E. Haefeli, and Antje Blank

Subjects

bulevirtide, myrcludex B, hepatitis D virus infection, drug-drug interaction (DDI), SLCO1B, OATP1B, Therapeutics. Pharmacology, RM1-950

Abstract

Introduction: Bulevirtide is a first-in-class antiviral drug to treat chronic hepatitis B/D. We investigated the drug-drug interaction potential and pharmacokinetics of high-dose subcutaneous bulevirtide (5 mg twice daily) with organic anion transporting polypeptide 1B1 (OATP1B1) and cytochrome P450 (CYP) 3A4.Methods: This was a single-center, open-label, fixed-sequence drug-drug interaction trial in 19 healthy volunteers. Before and at bulevirtide steady state, participants ingested a single 40 mg dose of pravastatin. A midazolam microdose was applied to quantify CYP3A4 activity.Results: At bulevirtide steady state, pravastatin area under the concentration-time curve (AUC0–∞) increased 1.32-fold (90% CI 1.08-1.61). The 5 mg bulevirtide twice-daily treatment resulted in a mean AUC0-12 of 1210 h*ng/ml (95% CI 1040-1408) and remained essentially unchanged under the influence of pravastatin. CYP3A4 activity did not change to a clinically relevant extent. As expected, total bile acids increased substantially (35-fold) compared to baseline during bulevirtide treatment. All study medication was well tolerated.Discussion: The study demonstrated that high-dose bulevirtide inhibited OATP1B-mediated hepatic uptake of the marker substrate pravastatin but the extent is considered clinically not relevant. Changes in CYP3A4 activity were also not clinically relevant. In conclusion, this study suggests that OATP1B substrate drugs as well as CYP3A4 substrates may safely be used without dose adjustment in patients treated with bulevirtide. However, in patients using high statin doses and where concomitant factors potentially further increase statin exposure, caution may be required when using bulevirtide.

Published

2023

5. Humoral response to SARS-CoV-2 mRNA vaccination in previous non-responder kidney transplant recipients after short-term withdrawal of mycophenolic acid

Author

Louise Benning, Christian Morath, Tessa Kühn, Marie Bartenschlager, Heeyoung Kim, Jörg Beimler, Mirabel Buylaert, Christian Nusshag, Florian Kälble, Marvin Reineke, Maximilian Töllner, Matthias Schaier, Katrin Klein, Antje Blank, Paul Schnitzler, Martin Zeier, Caner Süsal, Ralf Bartenschlager, Thuong Hien Tran, and Claudius Speer

Subjects

SARS-CoV-2, kidney transplantation, variants of concern, delta variant, omicron variant, SARS-CoV-2 vaccination, Medicine (General), R5-920

Abstract

Seroconversion rates after COVID-19 vaccination are significantly lower in kidney transplant recipients compared to healthy cohorts. Adaptive immunization strategies are needed to protect these patients from COVID-19. In this prospective observational cohort study, we enrolled 76 kidney transplant recipients with no seroresponse after at least three COVID-19 vaccinations to receive an additional mRNA-1273 vaccination (full dose, 100 μg). Mycophenolic acid was withdrawn in 43 selected patients 5–7 days prior to vaccination and remained paused for 4 additional weeks after vaccination. SARS-CoV-2-specific antibodies and neutralization of the delta and omicron variants were determined using a live-virus assay 4 weeks after vaccination. In patients with temporary mycophenolic acid withdrawal, donor-specific anti-HLA antibodies and donor-derived cell-free DNA were monitored before withdrawal and at follow-up. SARS-CoV-2 specific antibodies significantly increased in kidney transplant recipients after additional COVID-19 vaccination. The effect was most pronounced in individuals in whom mycophenolic acid was withdrawn during vaccination. Higher SARS-CoV-2 specific antibody titers were associated with better neutralization of SARS-CoV-2 delta and omicron variants. In patients with short-term withdrawal of mycophenolic acid, graft function and donor-derived cell-free DNA remained stable. No acute rejection episode occurred during short-term follow-up. However, resurgence of prior anti-HLA donor-specific antibodies was detected in 7 patients.

Published

2022

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

Author

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

Subjects

Therapeutics. Pharmacology, RM1-950, Public aspects of medicine, RA1-1270

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

7. Development and Validation of an LC–MS-Based Quantification Assay for New Therapeutic Antibodies: Application to a Novel Therapy against Herpes Simplex Virus

Author

Margaux Fresnais, Rémi Longuespée, Max Sauter, Torsten Schaller, Michaela Arndt, Jürgen Krauss, Antje Blank, Walter E. Haefeli, and Jürgen Burhenne

Subjects

Chemistry, QD1-999

Published

2020

8. Cost-effectiveness of an electronic clinical decision support system for improving quality of antenatal and childbirth care in rural Tanzania: an intervention study

Author

Happiness Pius Saronga, Els Duysburgh, Siriel Massawe, Maxwell Ayindenaba Dalaba, Peter Wangwe, Felix Sukums, Melkizedeck Leshabari, Antje Blank, Rainer Sauerborn, and Svetla Loukanova

Subjects

Clinical decision support system, Pharmacoeconomics, Cost-effectiveness analysis, Antenatal care, Childbirth care, Rural health care, Public aspects of medicine, RA1-1270

Abstract

Abstract Background QUALMAT project aimed at improving quality of maternal and newborn care in selected health care facilities in three African countries. An electronic clinical decision support system was implemented to support providers comply with established standards in antenatal and childbirth care. Given that health care resources are limited and interventions differ in their potential impact on health and costs (efficiency), this study aimed at assessing cost-effectiveness of the system in Tanzania. Methods This was a quantitative pre- and post- intervention study involving 6 health centres in rural Tanzania. Cost information was collected from health provider’s perspective. Outcome information was collected through observation of the process of maternal care. Incremental cost-effectiveness ratios for antenatal and childbirth care were calculated with testing of four models where the system was compared to the conventional paper-based approach to care. One-way sensitivity analysis was conducted to determine whether changes in process quality score and cost would impact on cost-effectiveness ratios. Results Economic cost of implementation was 167,318 USD, equivalent to 27,886 USD per health center and 43 USD per contact. The system improved antenatal process quality by 4.5% and childbirth care process quality by 23.3% however these improvements were not statistically significant. Base-case incremental cost-effectiveness ratios of the system were 2469 USD and 338 USD per 1% change in process quality for antenatal and childbirth care respectively. Cost-effectiveness of the system was sensitive to assumptions made on costs and outcomes. Conclusions Although the system managed to marginally improve individual process quality variables, it did not have significant improvement effect on the overall process quality of care in the short-term. A longer duration of usage of the electronic clinical decision support system and retention of staff are critical to the efficiency of the system and can reduce the invested resources. Realization of gains from the system requires effective implementation and an enabling healthcare system. Trial registration Registered clinical trial at www.clinicaltrials.gov ( NCT01409824 ). Registered May 2009.

Published

2017

9. 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

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

Subjects

COVID-19, Randomised controlled trial, Trial protocol, Hydroxychloroquine, Pantoprazole, Absorption, Medicine (General), R5-920

Abstract

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

10. Impact of an electronic clinical decision support system on workflow in antenatal care: the QUALMAT eCDSS in rural health care facilities in Ghana and Tanzania

Author

Nathan Mensah, Felix Sukums, Timothy Awine, Andreas Meid, John Williams, Patricia Akweongo, Jens Kaltschmidt, Walter E. Haefeli, and Antje Blank

Subjects

electronic clinical decision support system, workflow, antenatal care, health care providers, sequence of events, rural setting, developing countries, sub-Saharan Africa, Public aspects of medicine, RA1-1270

Abstract

Background: The implementation of new technology can interrupt established workflows in health care settings. The Quality of Maternal Care (QUALMAT) project has introduced an (eCDSS) for antenatal care (ANC) and delivery in rural primary health care facilities in Africa. Objective: This study was carried out to investigate the influence of the QUALMAT eCDSS on the workflow of health care workers in rural primary health care facilities in Ghana and Tanzania. Design: A direct observation, time-and-motion study on ANC processes was conducted using a structured data sheet with predefined major task categories. The duration and sequence of tasks performed during ANC visits were observed, and changes after the implementation of the eCDSS were analyzed. Results: In 24 QUALMAT study sites, 214 observations of ANC visits (144 in Ghana, 70 in Tanzania) were carried out at baseline and 148 observations (104 in Ghana, 44 in Tanzania) after the software was implemented in 12 of those sites. The median time spent combined for all centers in both countries to provide ANC at baseline was 6.5 min [interquartile range (IQR) =4.0–10.6]. Although the time spent on ANC increased in Tanzania and Ghana after the eCDSS implementation as compared to baseline, overall there was no significant increase in time used for ANC activities (0.51 min, p=0.06 in Ghana; and 0.54 min, p=0.26 in Tanzania) as compared to the control sites without the eCDSS. The percentage of medical history taking in women who had subsequent examinations increased after eCDSS implementation from 58.2% (39/67) to 95.3% (61/64) p

Published

2015

11. Nesting doctoral students in collaborative North–South partnerships for health systems research

Author

Svetla Loukanova, Helen Prytherch, Antje Blank, Els Duysburgh, Göran Tomson, Lars L. Gustafsson, Ali Sié, John Williams, Melkizedeck Leshabari, Walter E. Haefeli, Rainer Sauerborn, and Sharon Fonn

Subjects

collaborative project, doctoral students, health systems research capacity, North–South Partnership, Public aspects of medicine, RA1-1270

Abstract

Background: The European Union (EU) supports North–South Partnerships and collaborative research projects through its Framework Programmes and Horizon 2020. There is limited research on how such projects can be harnessed to provide a structured platform for doctoral level studies as a way of strengthening health system research capacity in sub-Saharan Africa (SSA). Objective: The aim of this study was to explore the challenges of, and facilitating factors for, ‘nesting’ doctoral students in North–South collaborative research projects. The term nesting refers to the embedding of the processes of recruiting, supervising, and coordinating doctoral students in the overall research plan and processes. Design: This cross-sectional qualitative study was undertaken by the EU-funded QUALMAT Project. A questionnaire was implemented with doctoral students, supervisors, and country principal investigators (PIs), and content analysis was undertaken. Results: Completed questionnaires were received from nine doctoral students, six supervisors, and three country PIs (86% responses rate). The doctoral students from SSA described high expectations about the input they would receive (administrative support, equipment, training, supervision). This contrasted with the expectations of the supervisors for proactivity and self-management on the part of the students. The rationale for candidate selection, and understandings of the purpose of the doctoral students in the project were areas of considerable divergence. There were some challenges associated with the use of the country PIs as co-supervisors. Doctoral student progress was at times impeded by delays in the release of funding instalments from the EU. The paper provides a checklist of essential requirements and a set of recommendations for effective nesting of doctoral students in joint North–South projects. Conclusion: There are considerable challenges to the effective nesting of doctoral students within major collaborative research projects. However, ways can be found to overcome them. The nesting process ultimately helped the institutions involved in this example to take better advantage of the opportunities that collaborative projects offer to foster North–South partnerships as a contribution to the strengthening of local research capacity.

Published

2014

12. Cost-effectiveness of clinical decision support system in improving maternal health care in Ghana.

Author

Maxwell Ayindenaba Dalaba, Patricia Akweongo, Raymond Akawire Aborigo, Happiness Pius Saronga, John Williams, Antje Blank, Jens Kaltschmidt, Rainer Sauerborn, and Svetla Loukanova

Subjects

Medicine, Science

Abstract

ObjectiveThis paper investigated the cost-effectiveness of a computer-assisted Clinical Decision Support System (CDSS) in the identification of maternal complications in Ghana.MethodsA cost-effectiveness analysis was performed in a before- and after-intervention study. Analysis was conducted from the provider's perspective. The intervention area was the Kassena- Nankana district where computer-assisted CDSS was used by midwives in maternal care in six selected health centres. Six selected health centers in the Builsa district served as the non-intervention group, where the normal Ghana Health Service activities were being carried out.ResultsComputer-assisted CDSS increased the detection of pregnancy complications during antenatal care (ANC) in the intervention health centres (before-intervention = 9 /1,000 ANC attendance; after-intervention = 12/1,000 ANC attendance; P-value = 0.010). In the intervention health centres, there was a decrease in the number of complications during labour by 1.1%, though the difference was not statistically significant (before-intervention =107/1,000 labour clients; after-intervention = 96/1,000 labour clients; P-value = 0.305). Also, at the intervention health centres, the average cost per pregnancy complication detected during ANC (cost -effectiveness ratio) decreased from US$17,017.58 (before-intervention) to US$15,207.5 (after-intervention). Incremental cost -effectiveness ratio (ICER) was estimated at US$1,142. Considering only additional costs (cost of computer-assisted CDSS), cost per pregnancy complication detected was US$285.ConclusionsComputer -assisted CDSS has the potential to identify complications during pregnancy and marginal reduction in labour complications. Implementing computer-assisted CDSS is more costly but more effective in the detection of pregnancy complications compared to routine maternal care, hence making the decision to implement CDSS very complex. Policy makers should however be guided by whether the additional benefit is worth the additional cost.

Published

2015

13. Costs associated with implementation of computer-assisted clinical decision support system for antenatal and delivery care: case study of Kassena-Nankana district of northern Ghana.

Author

Maxwell Ayindenaba Dalaba, Patricia Akweongo, John Williams, Happiness Pius Saronga, Pencho Tonchev, Rainer Sauerborn, Nathan Mensah, Antje Blank, Jens Kaltschmidt, and Svetla Loukanova

Subjects

Medicine, Science

Abstract

OBJECTIVE:This study analyzed cost of implementing computer-assisted Clinical Decision Support System (CDSS) in selected health care centres in Ghana. METHODS:A descriptive cross sectional study was conducted in the Kassena-Nankana district (KND). CDSS was deployed in selected health centres in KND as an intervention to manage patients attending antenatal clinics and the labour ward. The CDSS users were mainly nurses who were trained. Activities and associated costs involved in the implementation of CDSS (pre-intervention and intervention) were collected for the period between 2009-2013 from the provider perspective. The ingredients approach was used for the cost analysis. Costs were grouped into personnel, trainings, overheads (recurrent costs) and equipment costs (capital cost). We calculated cost without annualizing capital cost to represent financial cost and cost with annualizing capital costs to represent economic cost. RESULTS:Twenty-two trained CDSS users (at least 2 users per health centre) participated in the study. Between April 2012 and March 2013, users managed 5,595 antenatal clients and 872 labour clients using the CDSS. We observed a decrease in the proportion of complications during delivery (pre-intervention 10.74% versus post-intervention 9.64%) and a reduction in the number of maternal deaths (pre-intervention 4 deaths versus post-intervention 1 death). The overall financial cost of CDSS implementation was US$23,316, approximately US$1,060 per CDSS user trained. Of the total cost of implementation, 48% (US$11,272) was pre-intervention cost and intervention cost was 52% (US$12,044). Equipment costs accounted for the largest proportion of financial cost: 34% (US$7,917). When economic cost was considered, total cost of implementation was US$17,128-lower than the financial cost by 26.5%. CONCLUSIONS:The study provides useful information in the implementation of CDSS at health facilities to enhance health workers' adherence to practice guidelines and taking accurate decisions to improve maternal health care.

Published

2014

14. Frailty as a Marker for the Plasma Concentrations of Direct Oral Anticoagulants in Older Patients: Results of an Exploratory Study

Author

Annette Eidam, Julian Marji, Petra Benzinger, Kathrin I. Foerster, Jürgen Burhenne, David Czock, Felicitas Stoll, Antje Blank, Gerd Mikus, Walter E. Haefeli, and Jürgen M. Bauer

Subjects

Pharmacology (medical), Geriatrics and Gerontology

Published

2023

15. Treatment of atrial fibrillation with doxapram

Author

Antje Blank, Natasa Jávorszky, Henry Sutanto, Jordi Heijman, Gunther van Loon, Siegfried Lang, Hugo A. Katus, Jamila Kremer, Antonius Büscher, Rawa Arif, Stefan Kallenberger, Susanne Rinné, Amelie Paasche, Walter E. Haefeli, Ibrahim El-Battrawy, Martin Borggrefe, Ursula Tochtermann, Felix Wiedmann, Matthias Karck, Christoph Beyersdorf, Constanze Schmidt, Xiaobo Zhou, Xin Li, Manuel Kraft, Ibrahim Akin, Kathrin I. Foerster, Niels Decher, Cardiologie, RS: Carim - H04 Arrhythmogenesis and cardiogenetics, and RS: Carim - H01 Clinical atrial fibrillation

Subjects

0301 basic medicine, Cell physiology, medicine.medical_specialty, Electrical remodelling, Swine, Physiology, medicine.medical_treatment, Nerve Tissue Proteins, 030204 cardiovascular system & hematology, Cardioversion, MECHANISMS, 03 medical and health sciences, Potassium Channels, Tandem Pore Domain, 0302 clinical medicine, Physiology (medical), Internal medicine, Potassium Channel Blockers, Medicine and Health Sciences, medicine, Animals, Humans, Sinus rhythm, LEAK, Heart Atria, Veterinary Sciences, Potassium channel, TASK-1, SINOATRIAL CONDUCTION, business.industry, ACTION-POTENTIAL DURATION, Atrial fibrillation, Doxapram, medicine.disease, Antiarrhythmic pharmacotherapy, Electrophysiology, Catheter, 030104 developmental biology, K+ CHANNEL, Cardiology, Rhythm control, Cardiology and Cardiovascular Medicine, business, Anti-Arrhythmia Agents, Arrhythmia, medicine.drug

Abstract

Aims TASK-1 (K2P3.1) two-pore domain potassium channels are atrial-specific and significantly upregulated in atrial fibrillation (AF) patients, contributing to AF-related electrical remodelling. Inhibition of TASK-1 in cardiomyocytes of AF patients was shown to counteract AF-related action potential duration shortening. Doxapram was identified as a potent inhibitor of the TASK-1 channel. In the present study, we investigated the antiarrhythmic efficacy of doxapram in a porcine model of AF. Methods and results Doxapram successfully cardioverted pigs with artificially induced episodes of AF. We established a porcine model of persistent AF in domestic pigs via intermittent atrial burst stimulation using implanted pacemakers. All pigs underwent catheter-based electrophysiological investigations prior to and after 14 d of doxapram treatment. Pigs in the treatment group received intravenous administration of doxapram once per day. In doxapram-treated AF pigs, the AF burden was significantly reduced. After 14 d of treatment with doxapram, TASK-1 currents were still similar to values of sinus rhythm animals. Doxapram significantly suppressed AF episodes and normalized cellular electrophysiology by inhibition of the TASK-1 channel. Patch-clamp experiments on human atrial cardiomyocytes, isolated from patients with and without AF could reproduce the TASK-1 inhibitory effect of doxapram. Conclusions Repurposing doxapram might yield a promising new antiarrhythmic drug to treat AF in patients. Translational perspective Pharmacological suppression of atrial TASK 1 potassium currents prolongs atrial refractoriness with no effects on ventricular repolarization, resulting in atrial-specific class III antiarrhythmic effects. In our preclinical pilot study the respiratory stimulant doxapram was successfully administered for cardioversion of acute AF as well as rhythm control of persistent AF in a clinically relevant porcine animal model.

Published

2022

16. Time course of CYP3A activity during and after metamizole (dipyrone) in healthy volunteers

Author

Mareile H. Breithaupt, Evelyn Krohmer, Lenka Taylor, Eva Körner, Torsten Hoppe‐Tichy, Juergen Burhenne, Kathrin I. Foerster, Markus Dachtler, Gerald Huber, Rakesh Venkatesh, Karin Eggenreich, David Czock, Gerd Mikus, Antje Blank, and Walter E. Haefeli

Subjects

Pharmacology, Pharmacology (medical)

Published

2023

17. Effect of Clarithromycin, a Strong CYP3A and P-glycoprotein Inhibitor, on the Pharmacokinetics of Edoxaban in Healthy Volunteers and the Evaluation of the Drug Interaction with Other Oral Factor Xa Inhibitors by a Microdose Cocktail Approach

Author

Alexander Lenard, Simon A. Hermann, Felicitas Stoll, Juergen Burhenne, Kathrin I. Foerster, Gerd Mikus, Andreas D. Meid, Walter E. Haefeli, and Antje Blank

Subjects

Pharmacology, Pharmacology (medical), General Medicine, Cardiology and Cardiovascular Medicine

Abstract

Purpose We assessed the differential effect of clarithromycin, a strong inhibitor of cytochrome P450 (CYP) 3A4 and P-glycoprotein, on the pharmacokinetics of a regular dose of edoxaban and on a microdose cocktail of factor Xa inhibitors (FXaI). Concurrently, CYP3A activity was determined with a midazolam microdose. Methods In an open-label fixed-sequence trial in 12 healthy volunteers, the pharmacokinetics of a microdosed FXaI cocktail (μ-FXaI; 25 μg apixaban, 50 μg edoxaban, and 25 μg rivaroxaban) and of 60 mg edoxaban before and during clarithromycin (2 x 500 mg/d) dosed to steady-state was evaluated. Plasma concentrations of study drugs were quantified using validated ultra-performance liquid chromatography–tandem mass spectrometry methods. Results Therapeutic clarithromycin doses increased the exposure of a therapeutic 60 mg dose of edoxaban with a geometric mean ratio (GMR) of the area under the plasma concentration-time curve (AUC) of 1.53 (90 % CI: 1.37–1.70; p < 0.0001). Clarithromycin also increased the GMR (90% CI) of the exposure of microdosed FXaI apixaban to 1.38 (1.26–1.51), edoxaban to 2.03 (1.84–2.24), and rivaroxaban to 1.44 (1.27–1.63). AUC changes observed for the therapeutic edoxaban dose were significantly smaller than those observed with the microdose (p < 0.001). Conclusion Clarithromycin increases FXaI exposure. However, the magnitude of this drug interaction is not expected to be clinically relevant. The edoxaban microdose overestimates the extent of the drug interaction with the therapeutic dose, whereas AUC ratios for apixaban and rivaroxaban were comparable to the interaction with therapeutic doses as reported in the literature. Trial Registration EudraCT Number: 2018-002490-22

Published

2023

18. Evaluation of CYP2C19 activity using microdosed oral omeprazole in humans

Author

Annika Elbe, Kathrin Isabelle Foerster, Antje Blank, Peter Rose, Jürgen Burhenne, Walter Emil Haefeli, and Gerd Mikus

Subjects

Cytochrome P-450 CYP2C19, Pharmacology, Sodium Bicarbonate, Midazolam, Cytochrome P-450 CYP3A, Humans, Yohimbine, Drug Interactions, Pharmacology (medical), General Medicine, Rifampin, Fluconazole, Omeprazole

Abstract

Purpose To investigate the suitability of microdosed oral omeprazole for predicting CYP2C19 activity in vivo in combination with simultaneous assessment of CYP3A and CYP2D6 activity using both microdosed midazolam and yohimbine. Methods An open, fixed-sequence study was carried out in 20 healthy participants. Single microdosed (100 µg) and therapeutic (20 mg) doses of omeprazole were evaluated without comedication and after administration of established CYP2C19 perpetrators fluconazole (inhibition) and rifampicin (induction). To prevent degradation of the uncoated omeprazole microdose, sodium bicarbonate buffer was administered. The pharmacokinetics of omeprazole and its 5-hydroxy-metabolite were assessed as well as the pharmacokinetics of midazolam and yohimbine to estimate CYP3A4 and CYP2D6 activity. Results Calculated pharmacokinetic parameters after administration of 100 µg and 20 mg omeprazole in healthy subjects suggest dose proportionality. Omeprazole clearance was significantly decreased by fluconazole from 388 [95% CI: 266–565] to 47.2 [42.8–52.0] mL/min after 20 mg omeprazole and even further after 100 µg omeprazole (29.4 [24.5–35.1] mL/min). Rifampicin increased CYP2C19-mediated omeprazole metabolism. The omeprazole hydroxylation index was significantly related to omeprazole clearance for both doses. Both fluconazole and rifampicin altered CYP3A4 activity whereas no change of CYP2D6 activity was observed at all. Conclusions Microdosed oral omeprazole is suitable to determine CYP2C19 activity, also during enzyme inhibition and induction. However, the administration of sodium bicarbonate buffer also had a small influence on all victim drugs used. Trial registration EudraCT: 2017–004270-34.

Published

2022

19. Immune Response to COVID-19 mRNA Vaccination in Previous Nonresponder Kidney Transplant Recipients After Short-term Withdrawal of Mycophenolic Acid 1 and 3 Months After an Additional Vaccine Dose

Author

Tessa Kühn, Claudius Speer, Christian Morath, Marie Bartenschlager, Heeyoung Kim, Jörg Beimler, Mirabel Buylaert, Christian Nusshag, Florian Kälble, Marvin Reineke, Maximilian Töllner, Katrin Klein, Antje Blank, Sylvia Parthé, Paul Schnitzler, Martin Zeier, Caner Süsal, Ralf Bartenschlager, Thuong Hien Tran, Matthias Schaier, and Louise Benning

Subjects

Transplantation

Abstract

The impaired immune response to coronavirus disease 2019 (COVID-19) vaccination in kidney transplant recipients (KTRs) leads to an urgent need for adapted immunization strategies.Sixty-nine KTRs without seroconversion after ≥3 COVID-19 vaccinations were enrolled, and humoral response was determined after an additional full-dose mRNA-1273 vaccination by measuring severe acute respiratory syndrome coronavirus 2-specific antibodies and neutralizing antibody activity against the Delta and Omicron variants 1 and 3 mo postvaccination. T-cell response was analyzed 3 mo postvaccination by assessing interferon-γ release. Mycophenolic acid (MPA) was withdrawn in 41 KTRs 1 wk before until 4 wk after vaccination to evaluate effects on immunogenicity. Graft function, changes in donor-specific anti-HLA antibodies, and donor-derived cell-free DNA were monitored in KTRs undergoing MPA withdrawal.Humoral response to vaccination was significantly stronger in KTRs undergoing MPA withdrawal 1 mo postvaccination; however, overall waning humoral immunity was noted in all KTRs 3 mo after vaccination. Higher anti-S1 immunoglobulin G levels correlated with better neutralizing antibody activity against the Delta and Omicron variants, whereas no significant association was detected between T-cell response and neutralizing antibody activity. No rejection occurred during study, and graft function remained stable in KTRs undergoing MPA withdrawal. In 22 KTRs with Omicron variant breakthrough infections, neutralizing antibody activity was better against severe acute respiratory syndrome coronavirus 2 wild-type and the Delta variants than against the Omicron variant.MPA withdrawal to improve vaccine responsiveness should be critically evaluated because withdrawing MPA may be associated with enhanced alloimmune response, and the initial effect of enhanced seroconversion rates in KTRs with MPA withdrawal disappears 3 mo after vaccination.

Published

2023

20. Efficacy and Safety of Bulevirtide Monotherapy Given at 2 mg or 10 mg Dose Level Once Daily for Treatment of Chronic Hepatitis Delta: Week 48 Primary Endpoint Results from a Phase 3 Randomized, Multicenter, Parallel Design Study

Author

Heiner Wedemeyer, Soo Aleman, Maurizia Brunetto, Antje Blank, Pietro Andreone, Pavel Bogomolov, Vladimir Chulanov, Nina Mamonova, Natalia Geyvandova, Viacheslav Morozov, Olga Sagalova, Tatyana Stepanova, Dmitry Manuilov, Vithika Suri, Qi An, John Flaherty, Anu Osinusi, JulianSchulze zur Wiesch, Markus Cornberg, Stefan Zeuzem, and Pietro Lampertico

Published

2023

21. Oral bioavailability of microdoses and therapeutic doses of midazolam as a 2-dimensionally printed orodispersible film in healthy volunteers

Author

Mareile H. Breithaupt, Evelyn Krohmer, Lenka Taylor, Eva Koerner, Torsten Hoppe-Tichy, Juergen Burhenne, Kathrin I. Foerster, Markus Dachtler, Gerald Huber, Rakesh Venkatesh, Karin Eggenreich, David Czock, Gerd Mikus, Antje Blank, and Walter E. Haefeli

Subjects

Pharmacology, Therapeutic Equivalency, Midazolam, Humans, Administration, Oral, Biological Availability, Pharmacology (medical), General Medicine, Child, Healthy Volunteers

Abstract

Purpose The use of two-dimensional (2D) printing technologies of drugs on orodispersible films (ODF) can promote dose individualization and facilitate drug delivery in vulnerable patients, including children. We investigated midazolam pharmacokinetics after the administration of 2D-printed ODF. Methods Midazolam doses of 0.03 and 3 mg were printed on an ODF using a 2D drug printer. We investigated the bioavailability of the two midazolam doses with ODF swallowed immediately (ODF-IS) or delayed after 2 min (ODF-DS) by comparing their pharmacokinetics with intravenous and oral midazolam solution in 12 healthy volunteers. Results The relative bioavailability of ODF-IS 0.03 mg was 102% (90% confidence interval: 89.4–116) compared to oral solution and for 3 mg 101% (86.8–116). Cmax of ODF-IS 0.03 mg was 95.5% (83.2–110) compared to oral solution and 94.3% (78.2–114) after 3 mg. Absolute bioavailability of ODF-IS 0.03 mg was 24.9% (21.2–29.2) and for 3 mg 28.1% (23.4–33.8) (oral solution: 0.03 mg: 24.4% (22.0–27.1); 3 mg: 28.0% (25.0–31.2)). Absolute bioavailability of ODF-DS was significantly larger than for ODF-IS (0.03 mg: 61.4%; 3 mg: 44.1%; both p Conclusion This trial demonstrates the tolerability and unchanged bioavailability of midazolam printed on ODF over a 100-fold dose range, proving the suitability of ODF for dose individualization. Midazolam ODF-IS AUC0–∞ in both doses was bioequivalent to the administration of an oral solution. However, Cmax of the therapeutic dose of ODF-IS missed bioequivalence by a clinically not relevant extent. Prolonged mucosal exposure increased bioavailability. (Trial Registration EudraCT: 2020–003984-24, August 10, 2020).

Published

2022

22. 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

23. Intact plasma quantification of the large therapeutic lipopeptide bulevirtide

Author

Walter E. Haefeli, Jürgen Burhenne, Felicitas Stoll, Max Sauter, Antje Blank, and Natalie Lutz

Subjects

Bioanalysis, medicine.drug_class, Tandem mass spectrometry, 01 natural sciences, Biochemistry, High-performance liquid chromatography, Antiviral Agents, Analytical Chemistry, 03 medical and health sciences, chemistry.chemical_compound, Plasma, Lipopeptides, 0302 clinical medicine, Limit of Detection, medicine, Protein precipitation, Chemical Precipitation, Humans, Chronic hepatitis B and D, Amino Acid Sequence, Chromatography, UPLC, Bile acid, Chemistry, 010401 analytical chemistry, Lipopeptide, Reproducibility of Results, Hepatitis B, medicine.disease, Hepatitis D, 0104 chemical sciences, 030211 gastroenterology & hepatology, Bulevirtide, Research Paper, Chromatography, Liquid

Abstract

Bulevirtide is a first-in-class entry inhibitor of the hepatitis B and hepatitis delta virus blocking the sodium/bile acid co-transporter NTCP, and was recently approved for the treatment of hepatitis D as a priority medicine (prime) in an accelerated assessment by the European Medicines Agency. It is a very large lipopeptide comprising 47 amino acids in its sequence and a myristoylation at the N-terminus. For support of clinical development, we established highly sensitive plasma quantification assays using 100 μL of plasma, spanning concentrations of 0.1 to 100 ng/mL and 1 to 1000 ng/mL with the option to measure ten-fold diluted samples up to 10,000 ng/mL. Quantification was performed with UPLC-MS/MS measurements after extraction with protein precipitation. Both assays were fully validated according to the pertinent guidelines of the FDA and EMA, including incurred sample reanalyses and cross-validation using clinical study samples. Graphical abstract Supplementary Information The online version contains supplementary material available at 10.1007/s00216-021-03384-7.

Published

2021

24. 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

25. S1179 Bulevirtide Monotherapy at Low and High Dose in Patients With Chronic Hepatitis Delta: 24-Week Interim Data of the Phase 3 MYR301 Study

Author

Stacey Lee, Heiner Wedemeyer, Soo Aleman, Maurizia Brunetto, Antje Blank, Pietro Andreone, Pavel Bogomolov, Vladimir Chulanov, Nina Mamonova, Natalia Geyvandova, Viacheslav Morozov, Olga Sagalova, Tatyana Stepanova, Dmitry Manuilov, Vithika Suri, Qi An, John F. Flaherty, Anu Osinusi, Julian Schulze zur Wiesch, Markus Cornberg, Stefan Zeuzem, and Pietro Lampertico

Subjects

Hepatology, Gastroenterology

Published

2022

26. 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

27. MOR202, a novel anti-CD38 monoclonal antibody, in patients with relapsed or refractory multiple myeloma: a first-in-human, multicentre, phase 1–2a trial

Author

Antje Blank, Hartmut Goldschmidt, Stefan Härtle, Igor Wolfgang Blau, Tiantom Jarutat, Hermann Einsele, Katja Weisel, Manik Chatterjee, Christoph Röllig, Marc S. Raab, Johannes Weirather, Janine Griese, Christian Peschel, Monika Engelhardt, Hermine Agis, Barbara Ferstl, Mark Winderlich, and Natalie Schub

Subjects

Male, medicine.medical_specialty, Population, Antineoplastic Agents, Neutropenia, Antibodies, Monoclonal, Humanized, Gastroenterology, Dexamethasone, 03 medical and health sciences, Antineoplastic Agents, Immunological, 0302 clinical medicine, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Humans, Medicine, Adverse effect, education, Lenalidomide, Multiple myeloma, Aged, education.field_of_study, business.industry, Hematology, Middle Aged, medicine.disease, Pomalidomide, ADP-ribosyl Cyclase 1, Thalidomide, Regimen, Treatment Outcome, 030220 oncology & carcinogenesis, Female, Neoplasm Recurrence, Local, Multiple Myeloma, business, 030215 immunology, medicine.drug

Abstract

Summary Background Treatment of multiple myeloma is not curative, but targeting CD38 improves patient survival. To further explore this therapeutic approach, we investigated the safety and activity of MOR202, a novel monoclonal antibody targeting CD38, in patients with multiple myeloma. Methods This is a multicentre, open-label, phase 1–2a trial done at ten hospitals in Germany and Austria. Enrolled patients were aged 18 years or older with relapsed or refractory multiple myeloma and Karnofsky performance status of 60% or higher. Patients were assigned to the different treatment regimens with MOR202 ranging between 0·01 mg/kg and 16 mg/kg in a 3 + 3 design. Dose-escalation and expansion was done either with MOR202 intravenous infusions alone (MOR202 q2w [twice a week] and q1w [weekly] groups) or in combination with dexamethasone (MOR202 with dexamethasone group), with dexamethasone plus pomalidomide (MOR202 with dexamethasone plus pomalidomide group) or plus lenalidomide (MOR202 with dexamethasone plus lenalidomide group). Primary endpoints were safety, MOR202 maximum tolerated dose (or recommended dose) and regimen, and immunogenicity. The primary analysis was assessed in the safety population, which included patients who received at least one dose of any study drug. This trial is registered with ClinicalTrials.gov , NCT01421186 . Findings Between Aug 24, 2011, and Aug 1, 2017, 91 patients were treated, 35 with MOR202 monotherapy, and 56 with MOR202 combination regimens (18 in the MOR202 with dexamethasone group, 21 in the MOR202 with dexamethasone plus pomalidomide group, and 17 in the MOR202 with dexamethasone plus lenalidomide group). MOR202 intravenous infusions were safely administered within 30 min. Infusion-related reactions occurred in 14 (40%) of 35 patients receiving MOR202 monotherapy without steroids, and in four (7%) of 56 patients receiving MOR202 combination treatment. MOR202 maximum tolerated dose was not reached and the recommended regimens were MOR202 administered as an intravenous infusion for 30 min at doses up to 16 mg/kg with dexamethasone (40 mg), or in combination with dexamethasone plus lenalidomide (25 mg) or pomalidomide (4 mg). 35 (38%) of 91 patients developed lymphopenia, 30 (33%) developed neutropenia, and 27 (30%) developed leukopenia; these were the most common grade 3 or higher treatment-emergent adverse events. Serious adverse events were reported in 51 (56%) of 91 patients. None of the deaths were associated with MOR202. One pomalidomide-associated death occurred in the MOR202 with dexamethasone plus pomalidomide group. No anti-MOR202 antibodies were detected in patients. Interpretation MOR202 is safe and its clinical activity in patients with relapsed or refractory multiple myeloma is promising. Further clinical investigations of combinations with an immunomodulatory drug and dexamethasone are recommended. Funding MorphoSys AG.

Published

2020

28. Safety and efficacy of bulevirtide in combination with tenofovir disoproxil fumarate in patients with hepatitis B virus and hepatitis D virus coinfection (MYR202): a multicentre, randomised, parallel-group, open-label, phase 2 trial

Author

Heiner Wedemeyer, Katrin Schöneweis, Pavel Bogomolov, Antje Blank, Natalia Voronkova, Tatiana Stepanova, Olga Sagalova, Vladimir Chulanov, Marina Osipenko, Viacheslav Morozov, Natalia Geyvandova, Snezhana Sleptsova, Igor G Bakulin, Ilsiyar Khaertynova, Marina Rusanova, Anita Pathil, Uta Merle, Birgit Bremer, Lena Allweiss, Florian A Lempp, Kerstin Port, Mathias Haag, Matthias Schwab, Julian Schulze zur Wiesch, Markus Cornberg, Walter E Haefeli, Maura Dandri, Alexander Alexandrov, and Stephan Urban

Subjects

Adult, Hepatitis B virus, Hepatitis D, Chronic, Coinfection, Adenine, Antiviral Agents, Hepatitis D, Infectious Diseases, Hepatitis B, Chronic, Treatment Outcome, Humans, RNA, Hepatitis Delta Virus, Tenofovir

Abstract

Bulevirtide is a first-in-class peptidic entry inhibitor for hepatitis B virus (HBV) and hepatitis D virus infection. In July, 2020, bulevirtide 2 mg received conditional marketing authorisation by the European Medical Agency for treatment of chronic hepatitis D virus infection. We investigated the antiviral activity of bulevirtide in patients chronically infected with HBV and hepatitis D virus.MYR202 (ClinicalTrials.gov, NCT03546621; EudraCT, 2016-000395-13) was a multicentre, parallel-group, randomised, open-label, phase 2 trial. Adults (aged 18-65 years) with chronic hepatitis D virus infection, including patients with cirrhosis and patients who had contraindications to PegIFNα treatment or for whom treatment did not work, were eligible and were enrolled from four hospitals in Germany and 12 hospitals in Russia. Patients were randomly assigned (1:1:1:1) to receive 2 mg (n=28), 5 mg (n=32), or 10 mg (n=30) subcutaneous bulevirtide once per day with tenofovir disoproxil fumarate (TDF; 245 mg once per day orally) or TDF alone (245 mg once per day orally; n=30) for 24 weeks. Randomisation was done using a digital block scheme with stratification, consisting of 480 randomisation numbers separated into 30 blocks. The primary endpoint was undetectable hepatitis D virus RNA or 2 logBetween Feb 16, 2016, and Dec 8, 2016, 171 patients with chronic hepatitis D virus infection were screened; 51 were ineligible based on the exclusion criteria and 120 patients (59 with cirrhosis) were enrolled. At week 24, 15 (54%, 95% CI 34-73) of 28 patients achieved undetectable hepatitis D virus RNA or a 2 logBulevirtide induced a significant decline in hepatitis D virus RNA over 24 weeks. After cessation of bulevirtide, hepatitis D virus RNA concentrations rebounded. Longer treatment durations and combination therapies should be investigated.Hepatera LLC, MYR GmbH, and the German Centre for Infection Research, TTU Hepatitis.

Published

2021

29. Metabolic Effect of Blocking Sodium-Taurocholate Co-Transporting Polypeptide in Hypercholesterolemic Humans with a Twelve-Week Course of Bulevirtide—An Exploratory Phase I Clinical Trial

Author

Felicitas Stoll, Andrea Seidel-Glätzer, Ina Burghaus, Oliver Göring, Max Sauter, Peter Rose, Volker Daniel, Mathias Haag, Matthias Schwab, Johannes Riffel, Florian André, Lenka Taylor, Johanna Weiss, Jürgen Burhenne, Volker Cleeves, Walter E. Haefeli, and Antje Blank

Subjects

Inorganic Chemistry, Organic Chemistry, LDL cholesterol, bulevirtide, bile acid, NTCP, phase I clinical trial, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Catalysis, Computer Science Applications

Abstract

Bile acids (BA) play an important role in cholesterol metabolism and possess further beneficial metabolic effects as signalling molecules. Blocking the hepatocellular uptake of BA via sodium-taurocholate co-transporting polypeptide (NTCP) with the first-in-class drug bulevirtide, we expected to observe a decrease in plasma LDL cholesterol. In this exploratory phase I clinical trial, volunteers with LDL cholesterol > 130 mg/dL but without overt atherosclerotic disease were included. Thirteen participants received bulevirtide 5 mg/d subcutaneously for 12 weeks. The primary aim was to estimate the change in LDL cholesterol after 12 weeks. Secondary endpoints included changes in total cholesterol, HDL cholesterol, lipoprotein(a), inflammatory biomarkers, and glucose after 12 weeks. In addition, cardiac magnetic resonance imaging (CMR) was performed at four time points. BA were measured as biomarkers of the inhibition of hepatocellular uptake. After 12 weeks, LDL cholesterol decreased not statistically significantly by 19.6 mg/dL [−41.8; 2.85] (Hodges–Lehmann estimator with 95% confidence interval). HDL cholesterol showed a significant increase by 5.5 mg/dL [1.00; 10.50]. Lipoprotein(a) decreased by 1.87 mg/dL [−7.65; 0]. Inflammatory biomarkers, glucose, and cardiac function were unchanged. Pre-dose total BA increased nearly five-fold (from 2026 nmol/L ± 2158 (mean ± SD) at baseline to 9922 nmol/L ± 7357 after 12 weeks of treatment). Bulevirtide was generally well tolerated, with most adverse events being administration site reactions. The exploratory nature of the trial with a limited number of participants allows the estimation of potential effects, which are crucial for future pharmacological research on bile acid metabolism in humans.

Published

2022

30. 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

31. Integrated efficacy analysis of 24-week data from two phase 2 and one phase 3 clinical trials of bulevirtide monotherapy given at 2 mg or 10 mg dose level for treatment of chronic hepatitis delta

Author

Pietro Lampertico, Soo Aleman, Antje Blank, Pavel Bogomolov, Vladimir Chulanov, Nina Mamonova, Morozov Viacheslav, Olga Sagalova, Tatyana Stepanova, Vithika Suri, Dmitry Manuilov, Lei Ye, John F. Flaherty, Anu Osinusi, Markus Cornberg, Maurizia Brunetto, and Heiner Wedemeyer

Subjects

Hepatology

Published

2022

32. 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

33. Development and Validation of an LC-MS-Based Quantification Assay for New Therapeutic Antibodies: Application to a Novel Therapy against Herpes Simplex Virus

Author

Jürgen Krauss, Rémi Longuespée, Antje Blank, Walter E. Haefeli, Margaux Fresnais, Michaela Arndt, Jürgen Burhenne, Torsten Schaller, and Max Sauter

Subjects

biology, business.industry, medicine.drug_class, viruses, General Chemical Engineering, General Chemistry, medicine.disease_cause, Monoclonal antibody, Virology, Clinical study, Chemistry, Herpes simplex virus, Liquid chromatography–mass spectrometry, biology.protein, Medicine, Antibody, business, QD1-999

Abstract

Multiple therapeutic monoclonal antibodies (mAbs) are currently under development or in (pre)clinical study phases to reach regulatory approval. Among these, a new mAb against herpes simplex virus, HDIT101, was recently tested in healthy volunteers during a phase I clinical trial (first-in-human, dose escalation). In the frame of the pharmacokinetic evaluation of this new therapy, a mass spectrometric (MS)-based method was developed for the quantification of HDIT101 in human plasma using liquid chromatography coupled to tandem mass spectrometry. In this work, we describe the development of this bioanalytical assay using the quantification of a HDIT101 surrogate peptide, the assay validation procedure according to the FDA guidelines within the calibration range from 20 to 5000 μg/mL, and its application to plasma samples from the first-in-human clinical trial. This work presents a generic workflow for the development of MS-based quantification assays of new therapeutic antibodies that allows reaching high immunopurification recovery (98% for HDIT101 over the full calibration range with a precision of 6.9% CV). Surrogate peptide and stable isotopically labeled internal standard were stable, and batch-to-batch accuracies and precisions at the four quality standard levels ranged between -2 and 5% bias and 8 and 11% CV, respectively.

Published

2020

34. 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

35. 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

36. Hepatic uptake of conjugated bile acids is mediated by both sodium taurocholate cotransporting polypeptide and organic anion transporting polypeptides and modulated by intestinal sensing of plasma bile acid levels in mice

Author

Ulrich Beuers, Takeshi Katafuchi, Davor Slijepcevic, Reinout L.P. Roscam Abbing, Joanne M. Donkers, Jonathan H. M. van der Meer, Alfred H. Schinkel, Stéphanie van Hoppe, Ronald P.J. Oude Elferink, Manon E. Wildenberg, Stan F.J. van de Graaf, Dagmar Tolenaars, Antje Blank, Dirk R. de Waart, Graduate School, Gastroenterology and Hepatology, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, Tytgat Institute for Liver and Intestinal Research, Other Research, and ACS - Atherosclerosis & ischemic syndromes

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, medicine.drug_class, Down-Regulation, Organic Anion Transporters, Sodium-Dependent, Biology, Cholesterol 7 alpha-hydroxylase, digestive system, Cell Line, Bile Acids and Salts, Lipopeptides, 03 medical and health sciences, Mice, Cholestasis, Ileum, Liver Biology/Pathobiology, Internal medicine, medicine, Protein Isoforms, Animals, Humans, Cholesterol 7-alpha-Hydroxylase, Mice, Knockout, SLC10A1, Symporters, Hepatology, Bile acid, FGF15, FGF19, Biological Transport, Original Articles, medicine.disease, G protein-coupled bile acid receptor, Rats, 3. Good health, Fibroblast Growth Factors, Mice, Inbred C57BL, Organic anion-transporting polypeptide, Enterocytes, 030104 developmental biology, Endocrinology, Liver, biology.protein, Female, Original Article, Signal Transduction

Abstract

The Na+ -taurocholate cotransporting polypeptide (NTCP/SLC10A1) is believed to be pivotal for hepatic uptake of conjugated bile acids. However, plasma bile acid levels are normal in a subset of NTCP knockout mice and in mice treated with myrcludex B, a specific NTCP inhibitor. Here, we elucidated which transport proteins mediate the hepatic uptake of conjugated bile acids and demonstrated intestinal sensing of elevated bile acid levels in plasma in mice. Mice or healthy volunteers were treated with myrcludex B. Hepatic bile acid uptake kinetics were determined in wild-type (WT), organic anion transporting polypeptide (OATP) knockout mice (lacking Slco1a/1b isoforms), and human OATP1B1-transgenic mice. Effects of fibroblast growth factor 19 (FGF19) on hepatic transporter mRNA levels were assessed in rat hepatoma cells and in mice by peptide injection or adeno-associated virus-mediated overexpression. NTCP inhibition using myrcludex B had only moderate effects on bile acid kinetics in WT mice, but completely inhibited active transport of conjugated bile acid species in OATP knockout mice. Cholesterol 7α-hydroxylase Cyp7a1 expression was strongly down-regulated upon prolonged inhibition of hepatic uptake of conjugated bile acids. Fgf15 (mouse counterpart of FGF19) expression was induced in hypercholanemic OATP and NTCP knockout mice, as well as in myrcludex B-treated cholestatic mice, whereas plasma FGF19 was not induced in humans treated with myrcludex B. Fgf15/FGF19 expression was induced in polarized human enterocyte-models and mouse organoids by basolateral incubation with a high concentration (1 mM) of conjugated bile acids. CONCLUSION NTCP and OATPs contribute to hepatic uptake of conjugated bile acids in mice, whereas the predominant uptake in humans is NTCP mediated. Enterocytes sense highly elevated levels of (conjugated) bile acids in the systemic circulation to induce FGF15/19, which modulates hepatic bile acid synthesis and uptake. (Hepatology 2017;66:1631-1643).

Published

2017

37. 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

38. 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

39. 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

40. 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

41. Immunization with full-length

Author

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

Subjects

Protein vaccines, parasitic diseases, Article, 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

2019

42. 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

43. Treatment of chronic hepatitis D with the entry inhibitor myrcludex B: First results of a phase Ib/IIa study

Author

Florian A. Lempp, Ksenia Y. Kokina, Antje Blank, Matthias Schwab, Maria Macievich, Thorsten Lehr, Natalia Voronkova, A. Alexandrov, Walter E. Haefeli, Maria Petrachenkova, Stephan Urban, Heiner Wedemeyer, Pavel O. Bogomolov, and Mathias Haag

Subjects

0301 basic medicine, Hepatitis B virus, HBsAg, medicine.disease_cause, Lipopeptides, 03 medical and health sciences, 0302 clinical medicine, Pegylated interferon, medicine, Humans, SLC10A1, Hepatology, biology, business.industry, Hepatitis B, medicine.disease, Hepatitis D, Virology, 030104 developmental biology, HBeAg, biology.protein, 030211 gastroenterology & hepatology, Hepatitis D virus, Hepatitis Delta Virus, business, medicine.drug

Abstract

Background & Aims The therapeutic option for patients with chronic hepatitis delta virus infection (CHD) is limited to interferon alpha with rare curative outcome. Myrcludex B is a first-in-class entry inhibitor inactivating the hepatitis B virus (HBV) and hepatitis D virus (HDV) receptor sodium taurocholate co-transporting polypeptide. We report the interim results of a pilot trial on chronically infected HDV patients treated with myrcludex B, or pegylated interferon alpha (PegIFNα-2a) or their combination. Methods Twenty-four patients with CHD infection were equally randomized (1:1:1) to receive myrcludex B, or PegIFNα-2a or their combination. Patients were evaluated for virological and biochemical response and tolerability of the study drugs at weeks 12 and 24. Results Myrcludex B was well tolerated and no serious adverse event occurred. Although hepatitis B surface antigen levels remained unchanged, HDV RNA significantly declined at week 24 in all cohorts. HDV RNA became negative in two patients each in the Myrcludex B and PegIFNα-2a cohorts, and in five patients of the Myrcludex B+PegIFNα-2a cohort. ALT decreased significantly in the Myrcludex B cohort (six of eight patients), and HBV DNA was significantly reduced at week 24 in the Myrcludex B+PegIFNα-2a cohort. Virus kinetic modeling suggested a strong synergistic effect of myrcludex B and PegIFNα-2a on both HDV and HBV. Conclusions Myrcludex B showed a strong effect on HDV RNA serum levels and induced ALT normalization under monotherapy. Synergistic antiviral effects on HDV RNA and HBV DNA in the Myr-IFN cohort indicated a benefit of the combination of entry inhibition with PegIFNα-2a to treat CHD patients. Lay summary Myrcludex B is a new drug to treat hepatitis B and D infection. After 24weeks of treatment with myrcludex B and/or pegylated interferon α-2a, HDV R NA, a relevant marker for hepatitis D infection, decreased in all patients with chronic hepatitis B and D. Two of eight patients which received either myrcludex B or pegylated interferon α-2a, became negative for HDV RNA, and five of seven patients who received both drugs at the same time became negative. The drug was well tolerated.

Published

2016

44. Arzneimitteltherapie in der Schwangerschaft

Author

Antje Blank, A. Pathil-Warth, A. Eidam, A. Lampert, and G. Mikus

Subjects

Gynecology, 03 medical and health sciences, medicine.medical_specialty, 0302 clinical medicine, business.industry, Gastroenterology, medicine, 030211 gastroenterology & hepatology, 030212 general & internal medicine, business

Abstract

Arzneimittel fur schwangere Frauen konnen durch Therapie von Erkrankungen grosen Nutzen, aber auch Gefahren durch Toxizitat auf Entwicklungsprozesse mit sich bringen. Eine Nutzen-Risiko-Analyse muss die Aspekte der mutterlichen und kindlichen Seite betrachten und abwagen. Die Datenlage ist dabei oft nicht ausreichend und weitere klinische Studien waren notwendig, um das Gefahrdungspotenzial mancher Substanzen besser definieren zu konnen. Die Mehrzahl der Frauen nimmt im Verlauf einer Schwangerschaft Arzneimittel und damit potenzielle Noxen ein. Es ist deshalb wichtig, Einflussfaktoren auf die Variabilitat zu berucksichtigen und v. a. die Exposition von schadigenden Substanzen im ersten Trimenon zu vermeiden. Notwendige Verschreibungen auserhalb der Zulassung mussen den Patientinnen erklart und dokumentiert werden. Das pranataltoxikologische Risiko medikamentoser Therapieansatze fur ausgewahlte gastroenterologische Symptome und Krankheitsbilder wird in Grundzugen beschrieben.

Published

2016

45. Herpevizumab, a potent humanized antibody to treat anogenital herpes simplex virus (HSV-1/2) infection – Summary of preclinical data and perspectives of an ongoing clinical trial

Author

N Seyfizadeh, M Arndt, Walter E. Haefeli, T Schaller, Antje Blank, E Exner, N Hohmann, P Schnitzler, and J Krauss

Subjects

Clinical trial, business.industry, Medicine, business, Humanized antibody, Herpes simplex virus HSV-1, Preclinical data, Virology

Published

2018

46. Impact of patient education on plasma concentrations and effectiveness of posaconazole oral suspension under clinical conditions

Author

Antje Blank, Alexandra Carls, Gerd Mikus, Marcus J. P. Geist, Gerlinde Egerer, Nicolas Hohmann, and Werner J. Heinz

Subjects

Adult, Male, Posaconazole, medicine.medical_specialty, Antifungal Agents, Posaconazole Oral Suspension, Administration, Oral, Antineoplastic Agents, Toxicology, Lower risk, 030226 pharmacology & pharmacy, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Patient Education as Topic, Suspensions, Internal medicine, Medicine, Humans, Prospective Studies, Aged, Retrospective Studies, Pharmacology, business.industry, Induction chemotherapy, General Medicine, Induction Chemotherapy, Antibiotic Prophylaxis, Middle Aged, Triazoles, Bioavailability, Leukemia, Myeloid, Acute, Treatment Outcome, Plasma concentration, Female, business, 030217 neurology & neurosurgery, Fluconazole, Invasive Fungal Infections, Patient education, medicine.drug, Program Evaluation

Abstract

Posaconazole prophylaxis is recommended for patients with acute myeloid leukaemia during induction chemotherapy. Although a tablet formulation with better oral bioavailability is available, some patients have to rely on the oral suspension in clinical routine. Therefore, effectiveness of posaconazole oral suspension under real-life clinical conditions and impact of patient education about the correct intake on its plasma concentrations were assessed in this study. Altogether 96 patients receiving 160 cycles of induction chemotherapy were retrospectively (40 patients) and prospectively (56 patients) analysed. Patients were assigned into two groups for each chemotherapy cycle according to the application of antifungal prophylaxis (A: posaconazole oral suspension, 200 mg three times a day ≥7 days; B: intake

Published

2018

47. Quality of antenatal and childbirth care in rural health facilities in Burkina Faso, Ghana and Tanzania: an intervention study

Author

John W Williams, Els Duysburgh, A. Williams, Svetla Loukanova, Antje Blank, Siriel Massawe, Rose Mpembeni, Maurice Yé, Marleen Temmerman, and Walter E. Haefeli

Subjects

Program evaluation, medicine.medical_specialty, Pediatrics, 030219 obstetrics & reproductive medicine, biology, business.industry, Rural health, Public Health, Environmental and Occupational Health, Psychological intervention, biology.organism_classification, Clinical decision support system, 03 medical and health sciences, 0302 clinical medicine, Infectious Diseases, Tanzania, Health facility, Intervention (counseling), Family medicine, Childbirth, Medicine, Parasitology, 030212 general & internal medicine, business

Abstract

Objective To assess the impact of an intervention consisting of a computer-assisted clinical decision support system and performance-based incentives aiming at improving quality of antenatal and childbirth care. Methods Intervention study in rural primary healthcare (PHC) facilities in Burkina Faso Ghana and Tanzania. In each country six intervention and six non-intervention PHC facilities located in one intervention and one non-intervention rural districts were selected. Quality was assessed in each facility by health facility surveys direct observation of antenatal and childbirth care exit interviews and reviews of patient records and maternal and child health registers. Findings of pre- and post-intervention and of intervention and non-intervention health facility quality assessments were analyzed and assessed for significant (P < 0.05) quality of care differences. Results Post-intervention quality scores do not show a clear difference to pre-intervention scores and scores at non-intervention facilities. Only a few variables had a statistically significant better post-intervention quality score and when this is the case this is mostly observed in only one study-arm being pre-/post-intervention or intervention/non-intervention. Post-intervention care shows similar deficiencies in quality of antenatal and childbirth care and in detection prevention and management of obstetric complications as at baseline and non-intervention study facilities. Conclusion Our intervention study did not show a significant improvement in quality of care during the study period. However the use of new technology seems acceptable and feasible in rural PHC facilities in resource-constrained settings creating the opportunity to use this technology to improve quality of care.

Published

2015

48. Quantitative bile acid profiling by liquid chromatography quadrupole time-of-flight mass spectrometry: monitoring hepatitis B therapy by a novel Na+-taurocholate cotransporting polypeptide inhibitor

Author

Stephan Urban, Thomas E. Mürdter, Georg Heinkele, Ute Hofmann, Matthias Schwab, A. Alexandrov, Walter E. Haefeli, Mathias Haag, Antje Blank, and Patrick Leuthold

Subjects

Adult, Male, Spectrometry, Mass, Electrospray Ionization, Analyte, medicine.drug_class, Ion suppression in liquid chromatography–mass spectrometry, Mass spectrometry, Sensitivity and Specificity, Biochemistry, Analytical Chemistry, Bile Acids and Salts, chemistry.chemical_compound, medicine, Glycochenodeoxycholic acid, Humans, History, Ancient, Chromatography, Bile acid, Reproducibility of Results, Tauroursodeoxycholic acid, Hepatitis B, medicine.disease, Blood proteins, Hepatitis D, Treatment Outcome, chemistry, Female, Drug Monitoring, Biomarkers

Abstract

A novel analytical approach for the targeted profiling of bile acids (BAs) in human serum/plasma based on liquid chromatography quadrupole time-of-flight mass spectrometry (LC-QTOF-MS) is presented. Reversed-phase chromatography enabled the baseline separation of 15 human BA species which could be readily detected by accurate mass analysis in negative ion mode. Blood proteins were removed by methanol precipitation in the presence of deuterium-labeled internal standards which allowed BA quantification in 50 μl plasma/serum. The assay was validated according to FDA guidance achieving quantification limits from 7.8 to 156 nM. Calibration curves prepared in charcoal-stripped serum/plasma showed excellent regression coefficients (R 2 > 0.997) and covered quantities from 7.8 to 10,000 nM depending on the analyzed species. Intra- and inter-day accuracy and precision were below 15 % for all analytes. Apparent extraction recoveries were above 97 %, and ion suppression rates were between 4 and 53 %. Mean BA level in serum/plasma from healthy volunteers ranged from 11 ± 4 nM (tauroursodeoxycholic acid) to 1321 ± 1442 nM (glycochenodeoxycholic acid). As a proof of concept, the assay was applied to plasma samples derived from a clinical phase I study of myrcludex B, a novel first-in-class virus entry inhibitor for the treatment of chronic hepatitis B and D. The results demonstrate that myrcludex-induced inhibition of the hepatic BA transporter Na+-taurocholate cotransporting polypeptide (NTCP) significantly affects plasma BA level. These observations provide novel insights into drug-induced metabolic responses and will be indispensable for the assessment of side effects and dose-finding processes during future clinical trials.

Published

2015

49. Cost-effectiveness of an electronic clinical decision support system for improving quality of antenatal and childbirth care in rural Tanzania: an intervention study

Author

Rainer Sauerborn, Els Duysburgh, Svetla Loukanova, Siriel Massawe, Antje Blank, Felix Sukums, Maxwell Ayindenaba Dalaba, Melkizedeck T. Leshabari, Happiness P. Saronga, and Peter Wangwe

Subjects

Rural Population, Time Factors, Cost effectiveness, Cost-Benefit Analysis, Childbirth care, Antenatal care, Clinical decision support system, Medical health information technology, Tanzania, Health administration, 03 medical and health sciences, 610 Medical sciences Medicine, 0302 clinical medicine, Ambulatory care, Nursing, Pregnancy, Health care, Humans, Medicine, Maternal Health Services, 030212 general & internal medicine, Unlicensed assistive personnel, health care economics and organizations, HRHIS, business.industry, lcsh:Public aspects of medicine, Cost-effectiveness analysis, 030503 health policy & services, Health Policy, Nursing research, Infant, Newborn, lcsh:RA1-1270, Decision Support Systems, Clinical, Delivery, Obstetric, Quality Improvement, Rural health care, Pharmacoeconomics, Perinatal Care, Female, 0305 other medical science, business, Research Article

Abstract

Background: QUALMAT project aimed at improving quality of maternal and newborn care in selected health care facilities in three African countries. An electronic clinical decision support system was implemented to support providers comply with established standards in antenatal and childbirth care. Given that health care resources are limited and interventions differ in their potential impact on health and costs (efficiency), this study aimed at assessing cost-effectiveness of the system in Tanzania.Methods: This was a quantitative pre- and post- intervention study involving 6 health centres in rural Tanzania. Cost information was collected from health provider's perspective. Outcome information was collected through observation of the process of maternal care. Incremental cost-effectiveness ratios for antenatal and childbirth care were calculated with testing of four models where the system was compared to the conventional paper-based approach to care. One-way sensitivity analysis was conducted to determine whether changes in process quality score and cost would impact on cost-effectiveness ratios.Results: Economic cost of implementation was 167,318 USD, equivalent to 27,886 USD per health center and 43 USD per contact. The system improved antenatal process quality by 4.5% and childbirth care process quality by 23.3% however these improvements were not statistically significant. Base-case incremental cost-effectiveness ratios of the system were 2469 USD and 338 USD per 1% change in process quality for antenatal and childbirth care respectively. Cost-effectiveness of the system was sensitive to assumptions made on costs and outcomes.Conclusions: Although the system managed to marginally improve individual process quality variables, it did not have significant improvement effect on the overall process quality of care in the short-term. A longer duration of usage of the electronic clinical decision support system and retention of staff are critical to the efficiency of the system and can reduce the invested resources. Realization of gains from the system requires effective implementation and an enabling healthcare system.Trial registration: Registered clinical trial at www.clinicaltrials.gov ( NCT01409824). Registered May 2009.

Published

2017

50. Individual immune cell and cytokine profiles determine platelet-rich plasma composition

Author

Marcel Niemann, Melanie Ort, Luis Lauterbach, Mathias Streitz, Andreas Wilhelm, Gerald Grütz, Florian N. Fleckenstein, Frank Graef, Antje Blankenstein, Simon Reinke, Ulrich Stöckle, Carsten Perka, Georg N. Duda, Sven Geißler, Tobias Winkler, and Tazio Maleitzke

Subjects

Osteoarthritis, Inflammation, Orthobiologics, Regenerative therapies, Immune system, Diseases of the musculoskeletal system, RC925-935

Abstract

Abstract Objective Platelet-rich plasma (PRP) therapy is increasingly popular to treat musculoskeletal diseases, including tendinopathies and osteoarthritis (OA). To date, it remains unclear to which extent PRP compositions are determined by the immune cell and cytokine profile of individuals or by the preparation method. To investigate this, we compared leukocyte and cytokine distributions of different PRP products to donor blood samples and assessed the effect of pro-inflammatory cytokines on chondrocytes. Design For each of three PRP preparations (ACP®, Angel™, and nSTRIDE® APS), products were derived using whole blood samples from twelve healthy donors. The cellular composition of PRP products was analyzed by flow cytometry using DURAClone antibody panels (DURAClone IM Phenotyping Basic and DURAClone IM T Cell Subsets). The MESO QuickPlex SQ 120 system was used to assess cytokine profiles (V-PLEX Proinflammatory Panel 1 Human Kit, Meso Scale Discovery). Primary human chondrocyte 2D and 3D in vitro cultures were exposed to recombinant IFN-γ and TNF-α. Proliferation and chondrogenic differentiation were quantitatively assessed. Results All three PRP products showed elevated portions of leukocytes compared to baseline levels in donor blood. Furthermore, the pro-inflammatory cytokines IFN-γ and TNF-α were significantly increased in nSTRIDE® APS samples compared to donor blood and other PRP products. The characteristics of all other cytokines and immune cells from the donor blood, including pro-inflammatory T cell subsets, were maintained in all PRP products. Chondrocyte proliferation was impaired by IFN-γ and enhanced by TNF-α treatment. Differentiation and cartilage formation were compromised upon treatment with both cytokines, resulting in altered messenger ribonucleic acid (mRNA) expression of collagen type 1A1 (COL1A1), COL2A1, and aggrecan (ACAN) as well as reduced proteoglycan content. Conclusions Individuals with elevated levels of cells with pro-inflammatory properties maintain these in the final PRP products. The concentration of pro-inflammatory cytokines strongly varies between PRP products. These observations may help to unravel the previously described heterogeneous response to PRP in OA therapy, especially as IFN-γ and TNF-α impacted primary chondrocyte proliferation and their characteristic gene expression profile. Both the individual’s immune profile and the concentration method appear to impact the final PRP product. Trial registration This study was prospectively registered in the Deutsches Register Klinischer Studien (DRKS) on 4 November 2021 (registration number DRKS00026175).

Published

2023