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1. Prostaglandin D2 metabolites activate asthmatic patient-derived type 2 innate lymphoid cells and eosinophils via the DP2 receptor

Author

Saskia Carstensen, Christina Gress, Veit J. Erpenbeck, Shamsah D. Kazani, Jens M. Hohlfeld, David A. Sandham, and Meike Müller

Subjects
Eosinophil shape change, Type 2 innate lymphocyte cells, Asthma, PGD2, DP2, CRTH2, Diseases of the respiratory system, RC705-779
Abstract

Abstract Background Prostaglandin D2 (PGD2) signaling via prostaglandin D2 receptor 2 (DP2) contributes to atopic and non-atopic asthma. Inhibiting DP2 has shown therapeutic benefit in certain subsets of asthma patients, improving eosinophilic airway inflammation. PGD2 metabolites prolong the inflammatory response in asthmatic patients via DP2 signaling. The role of PGD2 metabolites on eosinophil and ILC2 activity is not fully understood. Methods Eosinophils and ILC2s were isolated from peripheral blood of atopic asthmatic patients. Eosinophil shape change, ILC2 migration and IL-5/IL-13 cytokine secretion were measured after stimulation with seven PGD2 metabolites in presence or absence of the selective DP2 antagonist fevipiprant. Results Selected metabolites induced eosinophil shape change with similar nanomolar potencies except for 9α,11β-PGF2. Maximal values in forward scatter of eosinophils were comparable between metabolites. ILC2s migrated dose-dependently in the presence of selected metabolites except for 9α,11β-PGF2 with EC50 values ranging from 17.4 to 91.7 nM. Compared to PGD2, the absolute cell migration was enhanced in the presence of Δ12-PGD2, 15-deoxy-Δ12,14-PGD2, PGJ2, Δ12-PGJ2 and 15-deoxy-Δ12,14-PGJ2. ILC2 cytokine production was dose dependent as well but with an average sixfold reduced potency compared to cell migration (IL-5 range 108.1 to 526.9 nM, IL-13 range: 125.2 to 788.3 nM). Compared to PGD2, the absolute cytokine secretion was reduced in the presence of most metabolites. Fevipiprant dose-dependently inhibited eosinophil shape change, ILC2 migration and ILC2 cytokine secretion with (sub)-nanomolar potencies. Conclusion Prostaglandin D2 metabolites initiate ILC2 migration and IL-5 and IL-13 cytokine secretion in a DP2 dependent manner. Our data indicate that metabolites may be important for in vivo eosinophil activation and ILC2 migration and to a lesser extent for ILC2 cytokine secretion.

Published
2021
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3. OpenMS 3 enables reproducible analysis of large-scale mass spectrometry data

Author

Pfeuffer, J., Bielow, C., Wein, S., Jeong, K., Netz, E., Walter, A., Alka, O., Nilse, L., Colaianni, P.D., McCloskey, D., Kim, J., Rosenberger, G., Bichmann, L., Walzer, M., Veit, J., Boudaud, B., Bernt, Matthias, Patikas, N., Pilz, M., Startek, M.P., Kutuzova, S., Heumos, L., Charkow, J., Sing, J.C., Feroz, A., Siraj, A., Weisser, H., Dijkstra, T.M.H., Perez-Riverol, Y., Röst, H., Kohlbacher, O., Sachsenberg, T., Pfeuffer, J., Bielow, C., Wein, S., Jeong, K., Netz, E., Walter, A., Alka, O., Nilse, L., Colaianni, P.D., McCloskey, D., Kim, J., Rosenberger, G., Bichmann, L., Walzer, M., Veit, J., Boudaud, B., Bernt, Matthias, Patikas, N., Pilz, M., Startek, M.P., Kutuzova, S., Heumos, L., Charkow, J., Sing, J.C., Feroz, A., Siraj, A., Weisser, H., Dijkstra, T.M.H., Perez-Riverol, Y., Röst, H., Kohlbacher, O., and Sachsenberg, T.

Abstract

Mass spectrometry (MS) has become an indispensable analytical technique in the life sciences. For more than two decades, the OpenMS1 open-source project has been aiding mass spectrometrists with data processing. In version 3, OpenMS extends its capabilities beyond bottom-up proteomics to include high-throughput workflows in top-down proteomics, metabolomics, structural biology and oligonucleotide mass spectrometry. OpenMS makes analyses from emerging fields available to experimentalists, enhances computational workflows, and provides a reworked Python interface to make the computational methods more accessible to bioinformaticians and data scientists (Fig. 1). To help new users explore and quickly become productive with OpenMS, the website and documentation were modernized for this release. For a detailed overview of new tools and changes — based on more than 20,000 Git commits contributed by 150+ developers since the last major release in 2015 — we refer the reader to the Supplementary Note and Supplementary Table 1.

Published
2024

7. The prostaglandin D2 receptor 2 pathway in asthma: a key player in airway inflammation

Author

Christian Domingo, Oscar Palomares, David A. Sandham, Veit J. Erpenbeck, and Pablo Altman

Subjects
Asthma, Airway inflammation, Prostaglandin D2, Prostaglandin D2 receptor 2, Diseases of the respiratory system, RC705-779
Abstract

Abstract Asthma is characterised by chronic airway inflammation, airway obstruction and hyper-responsiveness. The inflammatory cascade in asthma comprises a complex interplay of genetic factors, the airway epithelium, and dysregulation of the immune response. Prostaglandin D2 (PGD2) is a lipid mediator, predominantly released from mast cells, but also by other immune cells such as TH2 cells and dendritic cells, which plays a significant role in the pathophysiology of asthma. PGD2 mainly exerts its biological functions via two G-protein-coupled receptors, the PGD2 receptor 1 (DP1) and 2 (DP2). The DP2 receptor is mainly expressed by the key cells involved in type 2 immune responses, including TH2 cells, type 2 innate lymphoid cells and eosinophils. The DP2 receptor pathway is a novel and important therapeutic target for asthma, because increased PGD2 production induces significant inflammatory cell chemotaxis and degranulation via its interaction with the DP2 receptor. This interaction has serious consequences in the pulmonary milieu, including the release of pro-inflammatory cytokines and harmful cationic proteases, leading to tissue remodelling, mucus production, structural damage, and compromised lung function. This review will discuss the importance of the DP2 receptor pathway and the current understanding of its role in asthma.

Published
2018
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8. Data on the oral CRTh2 antagonist QAW039 (fevipiprant) in patients with uncontrolled allergic asthma

Author

Veit J. Erpenbeck, Todor A. Popov, David Miller, Steven F. Weinstein, Sheldon Spector, Baldur Magnusson, Wande Osuntokun, Paul Goldsmith, Markus Weiss, and Jutta Beier

Subjects
Computer applications to medicine. Medical informatics, R858-859.7, Science (General), Q1-390
Abstract

This article contains data on clinical endpoints (Peak Flow Expiratory Rate, fractional exhaled nitric oxide and total IgE serum levels) and plasma pharmacokinetic parameters concerning the use of the oral CRTh2 antagonist QAW039 (fevipiprant) in mild to moderate asthma patients. Information on experimental design and methods on how this data was obtained is also described. Further interpretation and discussion of this data can be found in the article “The oral CRTh2 antagonist QAW039 (fevipiprant): a phase II study in uncontrolled allergic asthma” (Erpenbeck et al., in press) [1].

Published
2016
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18. Medication Adherence in Patients With Severe Asthma Prescribed Oral Corticosteroids in the U-BIOPRED Cohort

Author

P. J. Sterk, John H. Riley, Thomas Sandström, Anna Selby, Laurie Pahus, C. Auffray, Ioannis Pandis, Julie Corfield, R. Djukanovic, K. Sun, Massimo Caruso, Jørgen Vestbo, Matthew J. Loza, Andrew J. Simpson, Dominic Burg, I.M. Adcock, S. Bates, Scott Wagers, Ana R. Sousa, J. Corfield, Ariane H. Wagener, René Lutter, Barbro Dahlén, Ratko Djukanovic, G. Praticò, I. Pandis, N. Mores, G. Hedlin, Navin Rao, I. Horváth, Alexander Mazein, B. De Meulder, Richard G. Knowles, John-Olof Thörngren, Wolfgang Seibold, P H Howarth, Victoria M. Goss, Cristina Gómez, Clare S. Murray, Paul Brinkman, Ildiko Horvath, Anthony D. Postle, M. Caruso, Martina Gahlemann, M. Puig Valls, F.K. Chung, P. Montuschi, Dominick E. Shaw, Kai Sun, Aruna T. Bansal, Fahad Alahmadi, Amphun Chaiboonchoe, Graham Roberts, Kian Fan Chung, Yike Guo, H. Ahmed, Thomas Geiser, Klaus Bønnelykke, M. Miralpeix, Simone Hashimoto, Diane Lefaudeux, S.S. Wagers, D. Erzen, B. Thornton, Florian Singer, Louise Fleming, Stephen J. Fowler, Neil Fitch, P. Bakke, Craig E. Wheelock, Nadja Hawwa Vissing, Tim Higenbottam, Jamie Matthews, F. Singer, S.E. Dahlén, Sarah Masefield, Roelinde Middelveld, Jens M. Hohlfeld, Anthony V. D'Amico, Paul Skipp, W.M.C. van Aalderen, Alan J. Knox, Sven-Erik Dahlén, Andrew Bush, A.T. Bansal, Pieter-Paul Hekking, Joost Brandsma, Stewart Bates, L.J. Fleming, Norbert Krug, N. Krug, Magnus Ericsson, J. Riley, P. Powel, Jacek Musiał, Amanda Roberts, Peter J. Sterk, Ian M. Adcock, Pascal Chanez, Cecile T.J. Holweg, F. Baribaud, Stelios Pavlidis, Veit J. Erpenbeck, Z. Weiszhart, C.E. Wheelock, Ralf Sigmund, James P.R. Schofield, Alexander Manta, Andrea Meiser, Susan J. Wilson, Jeanette Bigler, G. Roberts, M. van Geest, Hans Bisgaard, Urs Frey, Michael Boedigheimer, Per Bakke, Chris Compton, Enrica Bucchioni, Paolo Montuschi, David Myles, E.H.D. Bel, Anna James, Elena Formaggio, Anthony Rowe, Dominic E. Shaw, J. Haughney, P. Chanez, A.R. Sousa, S.J. Fowler, K. Fichtner, B. Dahlèn, Publica, Commission of the European Communities, Centre recherche en CardioVasculaire et Nutrition = Center for CardioVascular and Nutrition research (C2VN), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), Pulmonology, AII - Inflammatory diseases, and Paediatric Pulmonology

Subjects
Pulmonary and Respiratory Medicine, Male, medicine.medical_specialty, urinary corticosteroids, Prescription Drugs, Settore BIO/14 - FARMACOLOGIA, medicine.drug_class, [SDV]Life Sciences [q-bio], Urinary system, Respiratory System, Administration, Oral, 610 Medicine & health, Critical Care and Intensive Care Medicine, Hospital Anxiety and Depression Scale, Medication Adherence, 03 medical and health sciences, 0302 clinical medicine, Quality of life, Interquartile range, Internal medicine, Surveys and Questionnaires, Administration, Inhalation, Medicine, Humans, 030212 general & internal medicine, adherence, Glucocorticoids, ComputingMilieux_MISCELLANEOUS, U-BIOPRED Study Group, Asthma, Dose-Response Relationship, Drug, business.industry, 1103 Clinical Sciences, Middle Aged, asthma, medicine.disease, 030228 respiratory system, Cohort, Prednisolone, Quality of Life, Corticosteroid, Female, Cardiology and Cardiovascular Medicine, business, medicine.drug
Abstract

Background: Although estimates of suboptimal adherence to oral corticosteroids in asthma range from 30% to 50%, no ideal method for measurement exists; the impact of poor adherence in severe asthma is likely to be particularly high. Research Questions: What is the prevalence of suboptimal adherence detected by self-reporting and direct measures? Is suboptimal adherence associated with disease activity? Study Design and Methods: Data were included from individuals with severe asthma taking part in the U-BIOPRED (Unbiased Biomarkers for the Prediction of Respiratory Disease Outcomes) study and prescribed daily oral corticosteroids. Participants completed the Medication Adherence Report Scale, a five-item questionnaire used to grade adherence on a scale from 1 to 5, and provided a urine sample for analysis of prednisolone and metabolites by liquid chromatography-mass spectrometry. Results: Data from 166 participants were included in this study: mean (SD) age, 54.2 (± 11.9) years; FEV 1, 65.1% (± 20.5%) predicted; female, 58%; 37% completing the Medication Adherence Report Scale reported suboptimal adherence; and 43% with urinary corticosteroid data did not have detectable prednisolone or metabolites in their urine. Good adherence by both methods was detected in 49 of the 142 (35%) of participants in whom both methods were performed; adherence detection did not match between methods in 53%. Self-reported high adherers had better asthma control and quality of life, whereas directly measured high adherers had lower blood eosinophil levels. Interpretation: Low adherence is a common problem in severe asthma, whether measured directly or self-reported. We report poor agreement between the two methods, suggesting some disassociation between self-assessment of medication adherence and regular oral corticosteroid use, which suggests that each approach may provide complementary information in clinical practice.

Published
2021

19. The Roles of Type 2 Cytotoxic T Cells in Inflammation, Tissue Remodeling, and Prostaglandin (PG) D2 Production Are Attenuated by PGD2 Receptor 2 Antagonism

Author

Shamsah Kazani, Ian D. Pavord, Veit J. Erpenbeck, Yuan Ye, Jian Luo, Eric A. Shikatani, Rowie Borst, Wentao Chen, Paul Klenerman, Wei Liu, David Andrew Sandham, Ryan D. Hoyle, and Luzheng Xue

Subjects
integumentary system, Chemistry, medicine.medical_treatment, Immunology, Cell migration, Inflammation, Fevipiprant, Proinflammatory cytokine, Cell biology, 03 medical and health sciences, Paracrine signalling, 0302 clinical medicine, Cytokine, medicine, Immunology and Allergy, Cytotoxic T cell, lipids (amino acids, peptides, and proteins), medicine.symptom, Autocrine signalling, 030215 immunology
Abstract

Human type 2 cytotoxic T (Tc2) cells are enriched in severe eosinophilic asthma and can contribute to airway eosinophilia. PGD2 and its receptor PGD2 receptor 2 (DP2) play important roles in Tc2 cell activation, including migration, cytokine production, and survival. In this study, we revealed novel, to our knowledge, functions of the PGD2/DP2 axis in Tc2 cells to induce tissue-remodeling effects and IgE-independent PGD2 autocrine production. PGD2 upregulated the expression of tissue-remodeling genes in Tc2 cells that enhanced the fibroblast proliferation and protein production required for tissue repair and myofibroblast differentiation. PGD2 stimulated Tc2 cells to produce PGD2 using the routine PGD2 synthesis pathway, which also contributed to TCR-dependent PGD2 production in Tc2 cells. Using fevipiprant, a specific DP2 antagonist, we demonstrated that competitive inhibition of DP2 not only completely blocked the cell migration, adhesion, proinflammatory cytokine production, and survival of Tc2 cells triggered by PGD2 but also attenuated the tissue-remodeling effects and autocrine/paracrine PGD2 production in Tc2 induced by PGD2 and other stimulators. These findings further confirmed the anti-inflammatory effect of fevipiprant and provided a better understanding of the role of Tc2 cells in the pathogenesis of asthma.

Published
2021

28. Prostaglandin D2 metabolites activate asthmatic patient-derived type 2 innate lymphoid cells and eosinophils via the DP2 receptor

Author

Jens M. Hohlfeld, Christina Gress, Saskia Carstensen, Shamsah Kazani, David Andrew Sandham, Veit J. Erpenbeck, and Meike Müller

Subjects
Adult, Male, CRTH2, Adolescent, Prostaglandin Antagonists, Pyridines, medicine.medical_treatment, Receptors, Prostaglandin, Fevipiprant, Eosinophil shape change, Pharmacology, Diseases of the respiratory system, Young Adult, chemistry.chemical_compound, Type 2 innate lymphocyte cells, Cell Movement, 13,14-Dihydro-15-keto-PGD2, Eosinophil activation, medicine, PGD2 metabolites, Humans, PGD2, DP2, Lymphocytes, Receptors, Immunologic, Cell Shape, Cells, Cultured, Aged, Prostaglandin D2 receptor, Interleukin-13, RC705-779, Indoleacetic Acids, Prostaglandin D2, Research, Innate lymphoid cell, Middle Aged, Eosinophil, Asthma, Eosinophils, Cytokine, medicine.anatomical_structure, chemistry, lipids (amino acids, peptides, and proteins), Female, Cytokine secretion, Interleukin-5, Signal Transduction
Abstract

BackgroundProstaglandin D2(PGD2) signaling via prostaglandin D2receptor 2 (DP2) contributes to atopic and non-atopic asthma. Inhibiting DP2has shown therapeutic benefit in certain subsets of asthma patients, improving eosinophilic airway inflammation. PGD2metabolites prolong the inflammatory response in asthmatic patients via DP2signaling. The role of PGD2metabolites on eosinophil and ILC2 activity is not fully understood.MethodsEosinophils and ILC2s were isolated from peripheral blood of atopic asthmatic patients. Eosinophil shape change, ILC2 migration and IL-5/IL-13 cytokine secretion were measured after stimulation with seven PGD2metabolites in presence or absence of the selective DP2antagonist fevipiprant.ResultsSelected metabolites induced eosinophil shape change with similar nanomolar potencies except for 9α,11β-PGF2. Maximal values in forward scatter of eosinophils were comparable between metabolites. ILC2s migrated dose-dependently in the presence of selected metabolites except for 9α,11β-PGF2with EC50values ranging from 17.4 to 91.7 nM. Compared to PGD2, the absolute cell migration was enhanced in the presence of Δ12-PGD2, 15-deoxy-Δ12,14-PGD2, PGJ2, Δ12-PGJ2and 15-deoxy-Δ12,14-PGJ2. ILC2 cytokine production was dose dependent as well but with an average sixfold reduced potency compared to cell migration (IL-5 range 108.1 to 526.9 nM, IL-13 range: 125.2 to 788.3 nM). Compared to PGD2, the absolute cytokine secretion was reduced in the presence of most metabolites. Fevipiprant dose-dependently inhibited eosinophil shape change, ILC2 migration and ILC2 cytokine secretion with (sub)-nanomolar potencies.ConclusionProstaglandin D2metabolites initiate ILC2 migration and IL-5 and IL-13 cytokine secretion in a DP2dependent manner. Our data indicate that metabolites may be important for in vivo eosinophil activation and ILC2 migration and to a lesser extent for ILC2 cytokine secretion.

Published
2021

30. Cell counting in human endobronchial biopsies--disagreement of 2D versus 3D morphometry.

Author

Vlad A Bratu, Veit J Erpenbeck, Antonia Fehrenbach, Tanja Rausch, Susanne Rittinghausen, Norbert Krug, Jens M Hohlfeld, and Heinz Fehrenbach

Subjects
Medicine, Science
Abstract

QUESTION: Inflammatory cell numbers are important endpoints in clinical studies relying on endobronchial biopsies. Assumption-based bidimensional (2D) counting methods are widely used, although theoretically design-based stereologic three-dimensional (3D) methods alone offer an unbiased quantitative tool. We assessed the method agreement between 2D and 3D counting designs in practice when applied to identical samples in parallel. MATERIALS AND METHODS: Biopsies from segmental bronchi were collected from healthy non-smokers (n = 7) and smokers (n = 7), embedded and sectioned exhaustively. Systematic uniform random samples were immunohistochemically stained for macrophages (CD68) and T-lymphocytes (CD3), respectively. In identical fields of view, cell numbers per volume unit (NV) were assessed using the physical disector (3D), and profiles per area unit (NA) were counted (2D). For CD68+ cells, profiles with and without nucleus were separately recorded. In order to enable a direct comparison of the two methods, the zero-dimensional CD68+/CD3+-ratio was calculated for each approach. Method agreement was tested by Bland-Altmann analysis. RESULTS: In both groups, mean CD68+/CD3+ ratios for NV and NA were significantly different (non-smokers: 0.39 and 0.68, p

Published
2014
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32. The Roles of Type 2 Cytotoxic T Cells in Inflammation, Tissue Remodeling, and Prostaglandin (PG) D2 Production Are Attenuated by PGD2 Receptor 2 Antagonism

Author

Chen, Wentao, primary, Luo, Jian, additional, Ye, Yuan, additional, Hoyle, Ryan, additional, Liu, Wei, additional, Borst, Rowie, additional, Kazani, Shamsah, additional, Shikatani, Eric A., additional, Erpenbeck, Veit J., additional, Pavord, Ian D., additional, Klenerman, Paul, additional, Sandham, David A., additional, and Xue, Luzheng, additional

Published
2021
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33. Additional file 1 of Prostaglandin D2 metabolites activate asthmatic patient-derived type 2 innate lymphoid cells and eosinophils via the DP2 receptor

Author

Carstensen, Saskia, Gress, Christina, Erpenbeck, Veit J., Kazani, Shamsah D., Hohlfeld, Jens M., Sandham, David A., and Müller, Meike

Subjects
integumentary system, lipids (amino acids, peptides, and proteins)
Abstract

Additional file 1: Table S1. Detailed information on flow cytometric antibodies used for cell sorting of ILC2s. Table S2. Calculated agonist EC70 values for PGD2 and seven selected PGD2 metabolites. Table S3. Characteristics of study subjects. All subjects had a history of allergic asthma since at least 12 months. BMI had to be between 19 to 32 kg/ m2. Figure S1. Eosinophil shape change induced by PGD2, DK-PGD2, ∆12-PGD2, 15-deoxy-∆12,14-PGD2, PGJ2, 9a,11b-PGF2, ∆12-PGJ2 and 15-deoxy-∆12,14-PGJ2. Granulocytes were isolated from whole blood of asthmatic patients and were incubated with increasing concentrations of metabolites, n=3, 9α,11β-PGF2: n=2. The mean fluorescence values of the forward scatter were determined by flow cytometry and the percentage of shape change above basal was calculated. Values are given as mean ± SD. Figure S2. Concentration of IL-5 cytokine secretion of ILC2s in the presence of ascending concentrations of PGD2 and selected metabolites, n=3. Values are given for three different subjects (circle, square and triangle). Figure S3. Concentration of IL-13 cytokine secretion of ILC2s in the presence of ascending concentrations of PGD2 and selected metabolites, n=3. Values are given for three different subjects (circle, square and triangle).

Published
2021
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36. The Roles of Type 2 Cytotoxic T Cells in Inflammation, Tissue Remodeling, and Prostaglandin (PG) D

Author

Wentao, Chen, Jian, Luo, Yuan, Ye, Ryan, Hoyle, Wei, Liu, Rowie, Borst, Shamsah, Kazani, Eric A, Shikatani, Veit J, Erpenbeck, Ian D, Pavord, Paul, Klenerman, David A, Sandham, and Luzheng, Xue

Subjects
Inflammation, Indoleacetic Acids, Prostaglandin D2, Pyridines, Receptors, Prostaglandin, Humans, Mucosal Immunology, Receptors, Immunologic, Cells, Cultured, Coculture Techniques, T-Lymphocytes, Cytotoxic
Abstract

Key Points Multiple proinflammatory effects of Tc2 cells are inhibited by DP2 antagonism. Tissue-remodeling functions of Tc2 cells are attenuated by DP2 antagonism. Autocrine/paracrine PGD2 production in Tc2 cells is reduced by DP2 antagonism., Human type 2 cytotoxic T (Tc2) cells are enriched in severe eosinophilic asthma and can contribute to airway eosinophilia. PGD2 and its receptor PGD2 receptor 2 (DP2) play important roles in Tc2 cell activation, including migration, cytokine production, and survival. In this study, we revealed novel, to our knowledge, functions of the PGD2/DP2 axis in Tc2 cells to induce tissue-remodeling effects and IgE-independent PGD2 autocrine production. PGD2 upregulated the expression of tissue-remodeling genes in Tc2 cells that enhanced the fibroblast proliferation and protein production required for tissue repair and myofibroblast differentiation. PGD2 stimulated Tc2 cells to produce PGD2 using the routine PGD2 synthesis pathway, which also contributed to TCR-dependent PGD2 production in Tc2 cells. Using fevipiprant, a specific DP2 antagonist, we demonstrated that competitive inhibition of DP2 not only completely blocked the cell migration, adhesion, proinflammatory cytokine production, and survival of Tc2 cells triggered by PGD2 but also attenuated the tissue-remodeling effects and autocrine/paracrine PGD2 production in Tc2 induced by PGD2 and other stimulators. These findings further confirmed the anti-inflammatory effect of fevipiprant and provided a better understanding of the role of Tc2 cells in the pathogenesis of asthma.

Published
2020

37. A Study of the Effect of Cyclosporine on Fevipiprant Pharmacokinetics and its Absolute Bioavailability Using an Intravenous Microdose Approach

Author

Kenichi Umehara, Veit J. Erpenbeck, Markus Zollinger, H. Markus Weiss, Meredith Cain, Walid Elbast, and Janardhana Vemula

Subjects
Drug, Adult, Male, ATP Binding Cassette Transporter, Subfamily B, Adolescent, Pyridines, media_common.quotation_subject, Cmax, Pharmaceutical Science, Administration, Oral, Biological Availability, Fevipiprant, Absorption (skin), Pharmacology, 030226 pharmacology & pharmacy, 03 medical and health sciences, Solute Carrier Organic Anion Transporter Family Member 1B3, Young Adult, 0302 clinical medicine, Pharmacokinetics, MicroDose, Humans, Drug Interactions, media_common, Cross-Over Studies, Indoleacetic Acids, Chemistry, Drug interaction, Middle Aged, Healthy Volunteers, Competitive antagonist, 030220 oncology & carcinogenesis, Area Under Curve, Cyclosporine, Administration, Intravenous, Female
Abstract

This drug-drug interaction (DDI) study determined the effect of cyclosporine, an inhibitor of OATP1B3 and P-gp, on the pharmacokinetics (PK) of fevipiprant, an oral, highly selective, competitive antagonist of the prostaglandin D2 receptor 2 and a substrate of the two transporters. The concomitant administration of an intravenous (IV) microdose of stable isotope-labeled fevipiprant provided the absolute bioavailability of fevipiprant, as well as mechanistic insights in its PK and sensitivity to drug interactions. Liquid chromatography-mass spectrometry/mass spectrometry was used to measure plasma and urine concentrations. Geometric mean ratios (90% CI) for oral fevipiprant with or without cyclosporine were: for Cmax, 3.02 (2.38, 3.82); for AUClast, 2.50 (2.17, 2.88); and for AUCinf, 2.35 (1.99, 2.77). The geometric mean ratios (90% CI) for fevipiprant IV microdose with or without cyclosporine were: for Cmax, 1.04 (0.86, 1.25); for AUClast, 2.04 (1.83, 2.28) and for AUCinf, 1.95 (1.76, 2.16). The absolute bioavailability for fevipiprant was approximately 0.3-0.4 in the absence and 0.5 in the presence of cyclosporine. The IV microdose allowed differentiation between systemic and pre-systemic effects of cyclosporine on fevipiprant, demonstrating a small (approximately 1.2-fold) pre-systemic effect of cyclosporine and a larger (approximately 2-fold) effect on systemic elimination of fevipiprant. Uptake by OATP1B3 appears to be the rate-limiting step in the hepatic elimination of fevipiprant while P-gp does not have a relevant effect on oral absorption. SIGNIFICANCE STATEMENT The drug interaction investigated here with cyclosporine, an inhibitor of several drug transporters, provides a refined quantitative understanding of the role of active transport processes in liver and intestine for the absorption and elimination of fevipiprant, as well as the basis to assess the need for dose adjustment in the presence of transporter inhibitors. The applied IV microdose approach presents a strategy to maximize learnings from a trial, limit the number and duration of clinical trials, and enhance mechanistic DDI understanding.

Published
2020

38. Secukinumab Use in Patients with Moderate to Severe Psoriasis, Psoriatic Arthritis and Ankylosing Spondylitis in Real-World Setting in Europe: Baseline Data from SERENA Study

Author

Kiltz, U. Sfikakis, P.P. Gaffney, K. Sator, P.-G. von Kiedrowski, R. Bounas, A. Gullick, N. Conrad, C. Rigopoulos, D. Lespessailles, E. Romanelli, M. Ghislain, P.-D. Brandt-Jürgens, J. Rashkov, R. Aassi, M. Orsenigo, R. Perella, C. Pournara, E. Gathmann, S. Jagiello, P. Veit, J. Augustin, M.

Abstract

Introduction: Secukinumab, a fully human monoclonal antibody that directly inhibits interleukin-17A, has demonstrated robust efficacy in the treatment of moderate to severe psoriasis (PsO), psoriatic arthritis (PsA) and ankylosing spondylitis (AS), with a rapid onset of action, sustained long-term clinical responses and a consistently favourable safety profile across phase 3 trials. Here, we report the clinical data at enrolment from SERENA, designed to investigate the real-world use of secukinumab across all three indications. Methods: SERENA is an ongoing, longitudinal, observational study conducted at 438 sites across Europe in patients with moderate to severe plaque PsO, active PsA or active AS. Patients should have received at least 16 weeks of secukinumab treatment before enrolment in the study. Results: Overall 2800 patients were included in the safety set; patients with PsA (N = 541) were older than patients with PsO (N = 1799) and patients with AS (N = 460); patients with PsO had a higher mean body weight than patients with PsA and patients with AS; and patients with PsO and patients with AS were predominantly male. Time since diagnosis was longer in patients with PsO compared with patients with PsA and patients with AS, and about 40% of patients were either current or former smokers. The proportion of obese patients (body mass index ≥ 30 kg/m2) was similar across indications. Patients were treated with secukinumab for a mean duration of 1 year prior to enrolment (range 0.89–1.04). The percentages of patients with prior biologics exposure were 31.5% PsO, 59.7% PsA and 55% AS. The percentages of patients prescribed secukinumab monotherapy were 75% (n = 1349) in PsO, 48.2% (n = 261) in PsA and 48.9% (n = 225) in AS groups. Conclusion: Baseline demographics of the study population are consistent with existing literature. This large observational study across all secukinumab indications will provide valuable information on the long-term effectiveness and safety of secukinumab in the real-world setting. © 2020, The Author(s).

Published
2020

40. Omalizumab normalizes the gene expression signature of lesional skin in patients with chronic spontaneous urticaria: A randomized, double‐blind, placebo‐controlled study

Author

Martin Letzkus, Michael T. Beste, Martin Metz, Veit J. Erpenbeck, Petra Staubach, Janine Gericke, Nicole Hartmann, Andrea Bauer, Randolf Brehler, Sergio Kaiser, Marcus Maurer, and Rebecca I. Torene

Subjects
Adult, Male, 0301 basic medicine, medicine.medical_specialty, Adolescent, Biopsy, Immunology, Placebo-controlled study, Omalizumab, Placebo, Gastroenterology, Lesion, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Statistical significance, Internal medicine, Anti-Allergic Agents, medicine, Humans, Immunology and Allergy, Chronic Urticaria, Aged, Skin, medicine.diagnostic_test, business.industry, Middle Aged, Fold change, Treatment Outcome, 030104 developmental biology, 030228 respiratory system, Monoclonal, Female, medicine.symptom, Transcriptome, business, medicine.drug
Abstract

Introduction and objectives. Chronic spontaneous urticaria (CSU), including severe and treatment-refractory CSU, shows a strong response to omalizumab, a humanized recombinant monoclonal anti-IgE antibody. The effect of omalizumab on gene expression was assessed in skin biopsies from CSU patients enrolled in a double-blind placebo-controlled study (ClinicalTrials.gov Identifier: NCT01599637). Methods. CSU patients (18-75 years) were randomized to either 300 mg omalizumab (n=20) or placebo (n=10) administered s.c. every 4 weeks for 12 weeks. Lesional and non-lesional skin biopsies were collected from the same body area of consenting subjects and assessed at baseline and on Day 85. Skin biopsies from the same area of 10 untreated healthy volunteers (HV) were also processed as reference. Gene expression data were generated using Affymetrix HG-U133plus2.0 microarrays. Statistical analyses were performed using R packages. In brief, after normalization, low-intensity transcripts (i.e. probesets with intensities less than 100 in ≥50% of the samples) were filtered out. To identify transcriptional changes, linear models were constructed taking into account the type of biopsy (lesional or non-lesional), the study visit and the treatment for each patient. Thresholds for statistical significance and minimal fold change (FC) were defined as P-value ≤0.05 (no multiple testing correction) and absolute FC ≥1.5, respectively. Results. At baseline, 63 transcripts were differentially expressed between lesional and non-lesional skin. Two thirds of this lesional signature was also differentially expressed between lesional and HV skin. Upon treatment with omalizumab, over 75% of this lesional signature changed to reflect non-lesional skin expression levels (different to placebo, P-value 16). Conclusions. Omalizumab, in treatment responders, reverted transcriptional signatures associated with the CSU lesion phenotype to reflect non-lesional/HV expression levels. This result is consistent with observed omalizumab-mediated clinical improvement observed in patients with CSU.

Published
2018

41. A robust screen-free brain-computer interface for robotic object selection

Author

Kolkhorst, H., Veit, J., Burgard, W., Tangermann, M.W., Kolkhorst, H., Veit, J., Burgard, W., and Tangermann, M.W.

Abstract

Contains fulltext : 222466.pdf (publisher's version ) (Open Access), Brain signals represent a communication modality that can allow users of assistive robots to specify high-level goals, such as the object to fetch and deliver. In this paper, we consider a screen-free Brain-Computer Interface (BCI), where the robot highlights candidate objects in the environment using a laser pointer, and the user goal is decoded from the evoked responses in the electroencephalogram (EEG). Having the robot present stimuli in the environment allows for more direct commands than traditional BCIs that require the use of graphical user interfaces. Yet bypassing a screen entails less control over stimulus appearances. In realistic environments, this leads to heterogeneous brain responses for dissimilar objects-posing a challenge for reliable EEG classification. We model object instances as subclasses to train specialized classifiers in the Riemannian tangent space, each of which is regularized by incorporating data from other objects. In multiple experiments with a total of 19 healthy participants, we show that our approach not only increases classification performance but is also robust to both heterogeneous and homogeneous objects. While especially useful in the case of a screen-free BCI, our approach can naturally be applied to other experimental paradigms with potential subclass structure.

Published
2020

43. The prostaglandin D2 receptor 2 pathway in asthma: a key player in airway inflammation

Author

Pablo Altman, David Andrew Sandham, Oscar Palomares, Veit J. Erpenbeck, and Christian Domingo

Subjects
0301 basic medicine, Pathophysiology of asthma, Receptors, Prostaglandin, Prostaglandin, Review, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Immune system, Animals, Humans, Medicine, Anti-Asthmatic Agents, Receptors, Immunologic, Receptor, Lung, Inflammation, lcsh:RC705-779, business.industry, Prostaglandin D2, Innate lymphoid cell, Degranulation, lcsh:Diseases of the respiratory system, Asthma, respiratory tract diseases, 030104 developmental biology, 030228 respiratory system, chemistry, Prostaglandin D2 receptor 2, Immunology, Respiratory epithelium, Inflammation Mediators, business, Signal Transduction, Airway inflammation
Abstract

Asthma is characterised by chronic airway inflammation, airway obstruction and hyper-responsiveness. The inflammatory cascade in asthma comprises a complex interplay of genetic factors, the airway epithelium, and dysregulation of the immune response. Prostaglandin D2 (PGD2) is a lipid mediator, predominantly released from mast cells, but also by other immune cells such as TH2 cells and dendritic cells, which plays a significant role in the pathophysiology of asthma. PGD2 mainly exerts its biological functions via two G-protein-coupled receptors, the PGD2 receptor 1 (DP1) and 2 (DP2). The DP2 receptor is mainly expressed by the key cells involved in type 2 immune responses, including TH2 cells, type 2 innate lymphoid cells and eosinophils. The DP2 receptor pathway is a novel and important therapeutic target for asthma, because increased PGD2 production induces significant inflammatory cell chemotaxis and degranulation via its interaction with the DP2 receptor. This interaction has serious consequences in the pulmonary milieu, including the release of pro-inflammatory cytokines and harmful cationic proteases, leading to tissue remodelling, mucus production, structural damage, and compromised lung function. This review will discuss the importance of the DP2 receptor pathway and the current understanding of its role in asthma.

Published
2018

44. Expression of xenobiotic metabolizing enzymes in different lung compartments of smokers and nonsmokers

Author

Thum, Thomas, Erpenbeck, Veit J., Moeller, Julia, Hohlfeld, Jens M., Krug, Norbert, and Borlak, Jurgen

Subjects
Enzymes -- Genetic aspects, Smokers -- Genetic aspects, Gene expression -- Genetic aspects, Smoking -- Genetic aspects
Abstract

BACKGROUND: Cytochrome P450 monooxygenases (CYP) play an important role in the defense against inhaled toxicants, and expression of CYP enzymes may differ among various lung cells and tissue compartments. METHODS: [...]

Published
2006

45. Surfactant protein D decreases pollen-induced IgE-dependent mast cell degranulation

Author

Malherbe, Delphine C., Erpenbeck, Veit J., Abraham, Soman N., Crouch, Erika C., Hohlfeld, Jens M., and Wright, Jo Rae

Subjects
Mast cells -- Analysis, Mast cells -- Research, Surface active agents -- Analysis, Immunoglobulins -- Analysis, Asthma, Allergic reaction, Allergy, Biological sciences
Abstract

Mast cells play a key role in allergy and asthma. They reside at the host-environment interface and are among the first cells to make contact with inhaled microorganisms and particulate antigens. Pulmonary surfactant proteins A and D (SP-A and SP-D) function in lung host defense by enhancing microbe phagocytosis and mediating other immune cell functions, but little is known about their effects on mast cells. We hypothesized that SP-A and/or SP-D modulate IgE-dependent mast cell functions. Pollen starch granules (PSG) extracted from Dactylis glomerata and coated with trinitrophenol (TNP) were used as a model of an inhaled organic particulate allergen. Our data revealed that SP-D inhibited by 50% the release of [beta]-hexosaminidase by peritoneal mast cells sensitized with IgE anti-TNP and stimulated with TNP-PSG. In contrast, SP-A had no effect. Furthermore, SP-D aggregated PSG in a dose-dependent manner, and this aggregation was mediated by SP-D's carbohydrate recognition domain. A single arm SP-D mutant (RrSP-Dser 15,20) neither aggregated PSG nor inhibited degranulation, suggesting that multimefization of SP-D is required for maximal PSG aggregation and inhibition of PSG-induced mast cell degranulation. This study is the first to demonstrate that SP-D modulates IgE-mediated mast cell functions, which are important in asthma and allergic inflammation. collectins; allergen; lung; innate immunity; immunoglobulin E

Published
2005

47. Surfactant protein D increases phagocytosis and aggregation of pollen-allergen starch granules

Author

Erpenbeck, Veit J., Malherbe, Delphine C., Sommer, Stefanie, Schmiedl, Andreas, Steinhilber, Wolfram, Ghio, Andrew J., Krug, Norbert, Wright, Jo Rae, and Hohlfeld, Jens M.

Subjects
Allergic reaction -- Research, Allergic reaction -- Physiological aspects, Allergy -- Research, Allergy -- Physiological aspects, Phagocytosis -- Research, Phagocytosis -- Physiological aspects, Biological sciences
Abstract

Recent studies have shown that surfactant components, in particular the collectins surfactant protein (SP)-A and -D, modulate the phagocytosis of various pathogens by alveolar macrophages. This interaction might be important not only for the elimination of pathogens but also for the elimination of inhaled allergens and might explain anti-inflammatory effects of SP-A and SP-D in allergic airway inflammation. We investigated the effect of surfactant components on the phagocytosis of allergen-containing pollen starch granules (PSG) by alveolar macrophages. PSG were isolated from Dactylis glomerata or Phleum pratense, two common grass pollen allergens, and incubated with either rat or human alveolar macrophages in the presence of recombinant human SP-A, SP-A purified from patients suffering from alveolar proteinosis, a recombinant fragment of human SP-D, dodecameric recombinant rat SP-D, or the commercially available surfactant preparations Curosurf and Alveofact. Dodecameric rat recombinant SP-D enhanced binding and phagocytosis of the PSG by alveolar macrophages, whereas the recombinant fragment of human SP-D, SP-A, or the surfactant lipid preparations had no effect. In addition, recombinant rat SP-D bound to the surface of the PSG and induced aggregation. Binding, aggregation, and enhancement of phagocytosis by recombinant rat SP-D was completely blocked by EDTA and inhibited by D-maltose and to a lesser extent by D-galactose, indicating the involvement of the carbohydrate recognition domain of SP-D in these functions. The modulation of allergen phagocytosis by SP-D might play an important role in allergen clearance from the lung and thereby modulate the allergic inflammation of asthma. innate immunity; antigen processing; allergy; lung

Published
2005

49. Consensus on current management of endometriosis

Author

Johnson, Neil P., Hummelshoj, Lone, Abrao, M.S., Adamson, G.D., Allaire, C., Amelung, V., Andersson, E., Becker, C., Birna Árdal, K.B., Bush, D., de Bie, B., Chwalisz, K., Critchley, H., DʼHooghe, T., Dunselman, G., Evers, J.L.H., Farquhar, C., Faustmann, T., Forman, A., Fourquet, J., Fraser, I., Giudice, L., Gordts, S., Guidone, H., Guo, S.W., Healy, D., Hedon, B., Hulkkonen, J., Hull, L., Hummelshoj, L., Johnson, N.P., Just, M., Kiesel, L., Lam, A., Lynam, C., Mettler, L., Miller, C., North, H., Pai, R., Petta, C., Prentice, L., Reilly, S., Reis, F., Rolla, E., Rombauts, L., Schweppe, K.W., Seckin, T., Sharpe-Timms, K., Shepperson Mills, D., Singh, S., Soriano, D., Stafford-Bell, M., Stratton, P., Taylor, R., Tsaltas, J., Veit, J., and Vercellini, P.

Published
2013
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