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1. The Natural Fungal Metabolite Beauvericin Exerts Anticancer Activity in vivo: A Pre-Clinical Pilot Study

Author

Heilos, Daniela, primary, Rodriguez-Carrasco, Yelko, additional, Englinger, Bernhard, additional, Timelthaler, Gerald, additional, Schoonhoven, Sushilla van, additional, Sulyok, Michael, additional, Boecker, Simon, additional, Sussmuth, Roderich D., additional, Heffeter, Petra, additional, Lemmens-Gruber, Rosa, additional, Dornetshuber-Fleiss, Rita, additional, and Berger, Walter, additional

Published
2022
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2. Surgical versus Medical Management of Progressive Familial Intrahepatic Cholestasis—Case Compilation and Review of the Literature

Author

Maria Noelle Hüpper, Judith Pichler, Wolf-Dietrich Huber, Andreas Heilos, Rebecca Schaup, Martin Metzelder, and Sophie Langer

Subjects
progressive familial intrahepatic cholestasis, surgery, children, odevixibat, maralixibiat, biliary diversion, Pediatrics, RJ1-570
Abstract

(1) Background: Progressive familial intrahepatic cholestasis (PFIC) is a rare cause of liver failure. Surgical biliary diversion (SBD) and ileal bile salt inhibitors (IBAT) can delay or prevent liver transplantation (LTX). A comparison of the two methodologies in the literature is lacking. The combination has not been investigated. (2) Methods: We performed a literature survey on medical and surgical treatments for PFIC and reviewed the charts of our patients with PFIC of a tertiary hospital. The end points of our analysis were a decrease in serum bile acid (sBA) levels, reduction of pruritus and delay or avoidance of (LTX). (3) Results: We included 17 case series on SBD with more than 5 patients and a total of 536 patients. External or internal SBD, either conventional or minimally invasive, can reduce pruritus and sBA, but not all PFIC types are suitable for SBD. Six publications described the use of two types of IBAT in PFIC with a total of 118 patients. Treatment response was dependent on genetic type and subtype. Patients with PFIC 2 (nt-BSEP) showed the best response to treatment. Four out of eleven PFIC patients underwent SBD at our centre, with two currently receiving IBAT. (4) Conclusions: Limited data on IBAT in selected patients with PFIC show safety and effectiveness, although surgical methods should still be considered as a successful bridging procedure. Further studies to evaluate a possible combination of IBAT and SBD in PFIC are warranted and treatment decision should be discussed in an interdisciplinary board.

Published
2023
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3. Kinesin family member 12‐related hepatopathy: A generally indolent disorder with elevated gamma‐glutamyl‐transferase activity.

Author

Vogel, Georg‐Friedrich, Podpeskar, Alexandra, Rieder, Dietmar, Salzer, Helin, Garczarczyk‐Asim, Dorota, Wang, Li, Abuduxikuer, Kuerbanjiang, Wang, Jian‐She, Scharrer, Anke, Faqeih, Eissa Ali, Aseeri, Ali T., Vodopiutz, Julia, Heilos, Andreas, Pichler, Judith, Huber, Wolf‐Dietrich, Müller, Thomas, Knisely, A. S., and Janecke, Andreas R.

Subjects
HEPATIC fibrosis, LIVER failure, CHILD patients, LIVER transplantation, LIVER diseases, GAMMA-glutamyltransferase
Abstract

Exome sequencing (ES) has identified biallelic kinesin family member 12 (KIF12) mutations as underlying neonatal cholestatic liver disease. We collected information on onset and progression of this entity. Among consecutively referred pediatric patients at our centers, diagnostic ES identified 4 patients with novel, biallelic KIF12 variants using the human GRCh38 reference sequence, as KIF12 remains incompletely annotated in the older reference sequence GRCh37. A review of these and of 21 reported patients with KIF12 variants found that presentation with elevated serum transaminase activity in the context of trivial respiratory infection, without clinical features of liver disease, was more common (n = 18) than manifest cholestatic disease progressing rapidly to liver transplantation (LT; n = 7). Onset of liver disease was at age <1 year in 15 patients; LT was more common in this group. Serum gamma‐glutamyl transpeptidase activity (GGT) was elevated in all patients, and total bilirubin was elevated in 15 patients. Liver fibrosis or cirrhosis was present in 14 of 18 patients who were biopsied. The 16 different pathogenic variants and 11 different KIF12 genotypes found were not correlated with age of onset or progression to LT. Identification of biallelic pathogenic KIF12 variants distinguishes KIF12‐related disease from other entities with elevated GGT. [ABSTRACT FROM AUTHOR]

Published
2024
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5. Torque teno viral load reflects immunosuppression in paediatric kidney-transplanted patients-a pilot study

Author

Uhl, Phoebe and Heilos, Andreas

Subjects
Kidneys -- Transplantation, TT virus infections -- Risk factors, Viremia -- Measurement, Graft rejection -- Risk factors, Pediatric research, Immunosuppression -- Patient outcomes, Health
Abstract

Background Chronic deterioration of kidney graft function is related to inadequate immunosuppression (IS). A novel tool to assess the individual net state of IS in transplanted patients might be the monitoring of Torque teno virus (TTV) viral load. TTV is a non-pathogen virus detectable in almost all individuals. TTV level in the peripheral blood has been linked to the immune-competence of its host and should thus reflect IS after solid organ transplantation. Methods TTV plasma load was quantified monthly by RT-PCR for a period of 1 year in 45 kidney-transplanted children. Post-transplant time was at least 3 months. The relation of the virus DNA levels to IS and transplant-specific clinical and laboratory parameters was analysed longitudinally. Results TTV DNA was detectable in 94.5% of the plasma samples. There was a significant association with the post-transplant follow-up time as well as with the type of IS regimen, with lower virus loads in patients after longer post-transplant time and mTOR inhibitor-based IS. Furthermore, a significant positive correlation with the dose of prednisolone and mycophenolate mofetil was found. Conclusions TTV levels show an association/correlation with the strength of IS. Further studies are needed in order to evaluate TTV measurement as a tool for IS monitoring for hard clinical outcomes such as presence of donor-specific antibodies, rejections or infections-common consequences of insufficient or too intense IS., Author(s): Phoebe Uhl [sup.1] , Andreas Heilos [sup.1] , Gregor Bond [sup.2] , Elias Meyer [sup.3] , Michael Böhm [sup.1] , Elisabeth Puchhammer-Stöckl [sup.4] , Klaus Arbeiter [sup.1] , Thomas [...]

Published
2021
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6. Muscle Fatigue Revisited – Insights From Optically Pumped Magnetometers

Author

Davide Sometti, Lorenzo Semeia, Sangyeob Baek, Hui Chen, Giulia Righetti, Juergen Dax, Cornelius Kronlage, Milena Kirchgässner, Alyssa Romano, Johanna Heilos, Deborah Staber, Julia Oppold, Thomas Middelmann, Christoph Braun, Philip Broser, and Justus Marquetand

Subjects
OPM, sEMG, magnetomyography, muscle fatigue, quantum sensors, Physiology, QP1-981
Abstract

So far, surface electromyography (sEMG) has been the method of choice to detect and evaluate muscle fatigue. However, recent advancements in non-cryogenic quantum sensors, such as optically pumped magnetometers (OPMs), enable interesting possibilities to flexibly record biomagnetic signals. Yet, a magnetomyographic investigation of muscular fatigue is still missing. Here, we simultaneously used sEMG (4 surface electrode) and OPM-based magnetomyography (OPM-MMG, 4 sensors) to detect muscle fatigue during a 3 × 1-min isometric contractions of the left rectus femoris muscle in 7 healthy participants. Both signals exhibited the characteristic spectral compression distinctive for muscle fatigue. OPM-MMG and sEMG slope values, used to quantify the spectral compression of the signals, were positively correlated, displaying similarity between the techniques. Additionally, the analysis of the different components of the magnetic field vector enabled speculations regarding the propagation of the muscle action potentials (MAPs). Altogether these results show the feasibility of the magnetomyographic approach with OPMs and propose a potential alternative to sEMG for the study of muscle fatigue.

Published
2021
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7. FHR-5 Serum Levels and CFHR5 Genetic Variations in Patients With Immune Complex-Mediated Membranoproliferative Glomerulonephritis and C3-Glomerulopathy

Author

Nóra Garam, Marcell Cserhalmi, Zoltán Prohászka, Ágnes Szilágyi, Nóra Veszeli, Edina Szabó, Barbara Uzonyi, Attila Iliás, Christof Aigner, Alice Schmidt, Martina Gaggl, Gere Sunder-Plassmann, Dóra Bajcsi, Jürgen Brunner, Alexandra Dumfarth, Daniel Cejka, Stefan Flaschberger, Hana Flögelova, Ágnes Haris, Ágnes Hartmann, Andreas Heilos, Thomas Mueller, Krisztina Rusai, Klaus Arbeiter, Johannes Hofer, Dániel Jakab, Mária Sinkó, Erika Szigeti, Csaba Bereczki, Viktor Janko, Kata Kelen, György S. Reusz, Attila J. Szabó, Nóra Klenk, Krisztina Kóbor, Nika Kojc, Maarten Knechtelsdorfer, Mario Laganovic, Adrian Catalin Lungu, Anamarija Meglic, Rina Rus, Tanja Kersnik Levart, Ernesta Macioniene, Marius Miglinas, Anna Pawłowska, Tomasz Stompór, Ludmila Podracka, Michael Rudnicki, Gert Mayer, Romana Rysava, Jana Reiterova, Marijan Saraga, Tomáš Seeman, Jakub Zieg, Eva Sládková, Natasa Stajic, Tamás Szabó, Andrei Capitanescu, Simona Stancu, Miroslav Tisljar, Kresimir Galesic, András Tislér, Inga Vainumäe, Martin Windpessl, Tomas Zaoral, Galia Zlatanova, Mihály Józsi, and Dorottya Csuka

Subjects
membranoproliferative glomerulonephritis, immune complex-mediated glomerulonephritis, C3 glomerulopathy, dense deposit disease (DDD), C3 glomerulonephritis (C3GN), Immunologic diseases. Allergy, RC581-607
Abstract

BackgroundFactor H-related protein 5 (FHR-5) is a member of the complement Factor H protein family. Due to the homology to Factor H, the main complement regulator of the alternative pathway, it may also be implicated in the pathomechanism of kidney diseases where Factor H and alternative pathway dysregulation play a role. Here, we report the first observational study on CFHR5 variations along with serum FHR-5 levels in immune complex-mediated membranoproliferative glomerulonephritis (IC-MPGN) and C3 glomerulopathy (C3G) patients together with the clinical, genetic, complement, and follow-up data.MethodsA total of 120 patients with a histologically proven diagnosis of IC-MPGN/C3G were enrolled in the study. FHR-5 serum levels were measured in ELISA, the CFHR5 gene was analyzed by Sanger sequencing, and selected variants were studied as recombinant proteins in ELISA and surface plasmon resonance (SPR).ResultsEight exonic CFHR5 variations in 14 patients (12.6%) were observed. Serum FHR-5 levels were lower in patients compared to controls. Low serum FHR-5 concentration at presentation associated with better renal survival during the follow-up period; furthermore, it showed clear association with signs of complement overactivation and clinically meaningful clusters.ConclusionsOur observations raise the possibility that the FHR-5 protein plays a fine-tuning role in the pathogenesis of IC-MPGN/C3G.

Published
2021
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8. C4 nephritic factor in patients with immune-complex-mediated membranoproliferative glomerulonephritis and C3-glomerulopathy

Author

Nóra Garam, Zoltán Prohászka, Ágnes Szilágyi, Christof Aigner, Alice Schmidt, Martina Gaggl, Gere Sunder-Plassmann, Dóra Bajcsi, Jürgen Brunner, Alexandra Dumfarth, Daniel Cejka, Stefan Flaschberger, Hana Flögelova, Ágnes Haris, Ágnes Hartmann, Andreas Heilos, Thomas Mueller, Krisztina Rusai, Klaus Arbeiter, Johannes Hofer, Dániel Jakab, Mária Sinkó, Erika Szigeti, Csaba Bereczki, Viktor Janko, Kata Kelen, György S. Reusz, Attila J. Szabó, Nóra Klenk, Krisztina Kóbor, Nika Kojc, Maarten Knechtelsdorfer, Mario Laganovic, Adrian Catalin Lungu, Anamarija Meglic, Rina Rus, Tanja Kersnik-Levart, Ernesta Macioniene, Marius Miglinas, Anna Pawłowska, Tomasz Stompór, Ludmila Podracka, Michael Rudnicki, Gert Mayer, Romana Rysava, Jana Reiterova, Marijan Saraga, Tomáš Seeman, Jakub Zieg, Eva Sládková, Tamás Szabó, Andrei Capitanescu, Simona Stancu, Miroslav Tisljar, Kresimir Galesic, András Tislér, Inga Vainumäe, Martin Windpessl, Tomas Zaoral, Galia Zlatanova, and Dorottya Csuka

Subjects
C4 nephritic factor, C3 glomerulopathy, Membranoproliferative glomerulonephritis, C3 nephritic factor, Dense deposit disease, C3 glomerulonephritis, Medicine
Abstract

Abstract Background Acquired or genetic abnormalities of the complement alternative pathway are the primary cause of C3glomerulopathy(C3G) but may occur in immune-complex-mediated membranoproliferative glomerulonephritis (IC-MPGN) as well. Less is known about the presence and role of C4nephritic factor(C4NeF) which may stabilize the classical pathway C3-convertase. Our aim was to examine the presence of C4NeF and its connection with clinical features and with other pathogenic factors. Results One hunfe IC-MPGN/C3G patients were enrolled in the study. C4NeF activity was determined by hemolytic assay utilizing sensitized sheep erythrocytes. Seventeen patients were positive for C4NeF with lower prevalence of renal impairment and lower C4d level, and higher C3 nephritic factor (C3NeF) prevalence at time of diagnosis compared to C4NeF negative patients. Patients positive for both C3NeF and C4NeF had the lowest C3 levels and highest terminal pathway activation. End-stage renal disease did not develop in any of the C4NeF positive patients during follow-up period. Positivity to other complement autoantibodies (anti-C1q, anti-C3) was also linked to the presence of nephritic factors. Unsupervised, data-driven cluster analysis identified a group of patients with high prevalence of multiple complement autoantibodies, including C4NeF. Conclusions In conclusion, C4NeF may be a possible cause of complement dysregulation in approximately 10–15% of IC-MPGN/C3G patients.

Published
2019
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10. High-activity Classical and Alternative Complement Pathway Genotypes—Association With Donor-specific Antibody-triggered Injury and Renal Allograft Survival

Author

Mező, Blanka, Reindl-Schwaighofer, Roman, Eskandary, Farsad, Heinzel, Andreas, Wahrmann, Markus, Doberer, Konstantin, Heilos, Andreas, Bond, Gregor, Kläger, Johannes, Kozakowski, Nicolas, Haslacher, Helmuth, Oberbauer, Rainer, Viklický, Ondřej, Hrubá, Petra, Halloran, Philip F., Rusai, Krisztina, Prohászka, Zoltán, and Böhmig, Georg A.

Published
2020
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11. Intrinsic fluorescence of the clinically approved multikinase inhibitor nintedanib reveals lysosomal sequestration as resistance mechanism in FGFR-driven lung cancer

Author

Bernhard Englinger, Sebastian Kallus, Julia Senkiv, Daniela Heilos, Lisa Gabler, Sushilla van Schoonhoven, Alessio Terenzi, Patrick Moser, Christine Pirker, Gerald Timelthaler, Walter Jäger, Christian R. Kowol, Petra Heffeter, Michael Grusch, and Walter Berger

Subjects
FGFR1, Nintedanib, Fluorescence, Lysosomes, Resistance, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Abstract Background Studying the intracellular distribution of pharmacological agents, including anticancer compounds, is of central importance in biomedical research. It constitutes a prerequisite for a better understanding of the molecular mechanisms underlying drug action and resistance development. Hyperactivated fibroblast growth factor receptors (FGFRs) constitute a promising therapy target in several types of malignancies including lung cancer. The clinically approved small-molecule FGFR inhibitor nintedanib exerts strong cytotoxicity in FGFR-driven lung cancer cells. However, subcellular pharmacokinetics of this compound and its impact on therapeutic efficacy remain obscure. Methods 3-dimensional fluorescence spectroscopy was conducted to asses cell-free nintedanib fluorescence properties. MTT assay was used to determine the impact of the lysosome-targeting agents bafilomycin A1 and chloroquine combined with nintedanib on lung cancer cell viability. Flow cytometry and live cell as well as confocal microscopy were performed to analyze uptake kinetics as well as subcellular distribution of nintedanib. Western blot was conducted to investigate protein expression. Cryosections of subcutaneous tumor allografts were generated to detect intratumoral nintedanib in mice after oral drug administration. Results Here, we report for the first time drug-intrinsic fluorescence properties of nintedanib in living and fixed cancer cells as well as in cryosections derived from allograft tumors of orally treated mice. Using this feature in conjunction with flow cytometry and confocal microscopy allowed to determine cellular drug accumulation levels, impact of the ABCB1 efflux pump and to uncover nintedanib trapping into lysosomes. Lysosomal sequestration - resulting in an organelle-specific and pH-dependent nintedanib fluorescence - was identified as an intrinsic resistance mechanism in FGFR-driven lung cancer cells. Accordingly, combination of nintedanib with agents compromising lysosomal acidification (bafilomycin A1, chloroquine) exerted distinctly synergistic growth inhibitory effects. Conclusion Our findings provide a powerful tool to dissect molecular factors impacting organismal and intracellular pharmacokinetics of nintedanib. Regarding clinical application, prevention of lysosomal trapping via lysosome-alkalization might represent a promising strategy to circumvent cancer cell-intrinsic nintedanib resistance.

Published
2017
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15. C4 nephritic factor in patients with immune-complex-mediated membranoproliferative glomerulonephritis and C3-glomerulopathy

Author

Garam, Nóra, Prohászka, Zoltán, Szilágyi, Ágnes, Aigner, Christof, Schmidt, Alice, Gaggl, Martina, Sunder-Plassmann, Gere, Bajcsi, Dóra, Brunner, Jürgen, Dumfarth, Alexandra, Cejka, Daniel, Flaschberger, Stefan, Flögelova, Hana, Haris, Ágnes, Hartmann, Ágnes, Heilos, Andreas, Mueller, Thomas, Rusai, Krisztina, Arbeiter, Klaus, Hofer, Johannes, Jakab, Dániel, Sinkó, Mária, Szigeti, Erika, Bereczki, Csaba, Janko, Viktor, Kelen, Kata, Reusz, György S., Szabó, Attila J., Klenk, Nóra, Kóbor, Krisztina, Kojc, Nika, Knechtelsdorfer, Maarten, Laganovic, Mario, Lungu, Adrian Catalin, Meglic, Anamarija, Rus, Rina, Kersnik-Levart, Tanja, Macioniene, Ernesta, Miglinas, Marius, Pawłowska, Anna, Stompór, Tomasz, Podracka, Ludmila, Rudnicki, Michael, Mayer, Gert, Romana Rysava, Reiterova, Jana, Saraga, Marijan, Tomáš Seeman, Zieg, Jakub, Sládková, Eva, Szabó, Tamás, Capitanescu, Andrei, Stancu, Simona, Tisljar, Miroslav, Galesic, Kresimir, Tislér, András, Vainumäe, Inga, Windpessl, Martin, Zaoral, Tomas, Zlatanova, Galia, and Csuka, Dorottya

Published
2019
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16. ONLINE WEAR ANALYSIS OF CARD CLOTHINGS.

Author

FISCHER, HOLGER, HEILOS, KATHARINA, THAL, DANIEL, FAASEN, ANDRÉ, and HOFMANN, MARCEL

Subjects
GLASS fibers, PRODUCTION planning, INDUSTRY 4.0, CLOTHING & dress, FIBERS
Abstract

The processing of abrasive fibres in the carding process, in particular high-performance fibres such as glass, carbon or aramid fibres, can cause increased wear of the card clothing. In the FutureTex project 'HPFGarnitur', the wear of card clothing was investigated and an online wear measurement system has been developed. The aim of the project was both, to optimize the clothings to enable gentler processing of the fibres, and to develop a digital monitoring system to observe the degree of wear of the clothings, which offers a new possibility for maintenance prediction and production planning in the sense of Industry 4.0. [ABSTRACT FROM AUTHOR]

Published
2023
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20. Torque teno viral load reflects immunosuppression in paediatric kidney-transplanted patients—a pilot study

Author

Phoebe Uhl, Michael Böhm, Klaus Arbeiter, Andreas Heilos, Krisztina Rusai, Elisabeth Puchhammer-Stöckl, Thomas Müller-Sacherer, Gregor Bond, Dagmar Csaicsich, Christoph Aufricht, and Elias L. Meyer

Subjects
0301 basic medicine, Nephrology, medicine.medical_specialty, Torque teno virus, medicine.medical_treatment, TTV, Pilot Projects, Immunologic monitoring, 030230 surgery, Kidney, Gastroenterology, Virus, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Child, Immunosuppression Therapy, Transplantation, business.industry, Immunosuppression, Viral Load, Anellovirus, Kidney Transplantation, Paediatric kidney transplantation, Regimen, 030104 developmental biology, DNA, Viral, Pediatrics, Perinatology and Child Health, Prednisolone, Original Article, business, Viral load, Immunosuppressive Agents, Biomarkers, medicine.drug
Abstract

Background Chronic deterioration of kidney graft function is related to inadequate immunosuppression (IS). A novel tool to assess the individual net state of IS in transplanted patients might be the monitoring of Torque teno virus (TTV) viral load. TTV is a non-pathogen virus detectable in almost all individuals. TTV level in the peripheral blood has been linked to the immune-competence of its host and should thus reflect IS after solid organ transplantation. Methods TTV plasma load was quantified monthly by RT-PCR for a period of 1 year in 45 kidney-transplanted children. Post-transplant time was at least 3 months. The relation of the virus DNA levels to IS and transplant-specific clinical and laboratory parameters was analysed longitudinally. Results TTV DNA was detectable in 94.5% of the plasma samples. There was a significant association with the post-transplant follow-up time as well as with the type of IS regimen, with lower virus loads in patients after longer post-transplant time and mTOR inhibitor–based IS. Furthermore, a significant positive correlation with the dose of prednisolone and mycophenolate mofetil was found. Conclusions TTV levels show an association/correlation with the strength of IS. Further studies are needed in order to evaluate TTV measurement as a tool for IS monitoring for hard clinical outcomes such as presence of donor-specific antibodies, rejections or infections—common consequences of insufficient or too intense IS.

Published
2020

21. Muscle Fatigue Revisited – Insights From Optically Pumped Magnetometers

Author

Sometti, Davide, primary, Semeia, Lorenzo, additional, Baek, Sangyeob, additional, Chen, Hui, additional, Righetti, Giulia, additional, Dax, Juergen, additional, Kronlage, Cornelius, additional, Kirchgässner, Milena, additional, Romano, Alyssa, additional, Heilos, Johanna, additional, Staber, Deborah, additional, Oppold, Julia, additional, Middelmann, Thomas, additional, Braun, Christoph, additional, Broser, Philip, additional, and Marquetand, Justus, additional

Published
2021
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22. RecyCarb: Process Optimization and On-Line Monitoring in the Recycling of Carbon Fibre Waste for the Re-Use in High-Grade Fibre Reinforced Plastics

Author

Marcel Hofmann, Andrea Miene, Katharina Heilos, and Holger Fischer

Subjects
Materials science, Mechanics of Materials, business.industry, Mechanical Engineering, General Materials Science, Process optimization, Line (text file), Process engineering, business
Abstract

Within the project ‘RecyCarb’ a qualified value-added chain for recycled carbon fibres (rCF) to enable their high-quality and sustainable re-use in sophisticated fibre-reinforced composites was established. A team of four industrial partners and two research institutes closed the technological gap between the actual rCF available on the market and the functional re-use as reinforcing elements in high-quality components. Process optimisation, initiation of a reliable scheme of quality assurance and a process integrated quality monitoring were the main aspects of this project. Besides different kinds of carbon fibre waste, different nonwoven processes (web formation and bonding methods) and an online fibre orientation analysis were investigated. This project focuses a variety of several application markets, e.g. sports equipment, medical technologies or automotive, shown by developed demonstrators.

Published
2019
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23. The Natural Fungal Metabolite Beauvericin Exerts Anticancer Activity In Vivo: A Pre-Clinical Pilot Study

Author

Daniela Heilos, Yelko Rodríguez-Carrasco, Bernhard Englinger, Gerald Timelthaler, Sushilla van Schoonhoven, Michael Sulyok, Simon Boecker, Roderich D. Süssmuth, Petra Heffeter, Rosa Lemmens-Gruber, Rita Dornetshuber-Fleiss, and Walter Berger

Subjects
cyclohexadepsipeptide, beauvericin, cervix carcinoma, colorectal carcinoma, therapy, Medicine
Abstract

Recently, in vitro anti-cancer properties of beauvericin, a fungal metabolite were shown in various cancer cell lines. In this study, we assessed the specificity of this effect by comparing beauvericin cytotoxicity in malignant versus non-malignant cells. Moreover, we tested in vivo anticancer effects of beauvericin by treating BALB/c and CB-17/SCID mice bearing murine CT-26 or human KB-3-1-grafted tumors, respectively. Tumor size and weight were measured and histological sections were evaluated by Ki-67 and H/E staining as well as TdT-mediated-dUTP-nick-end (TUNEL) labeling. Beauvericin levels were determined in various tissues and body fluids by LC-MS/MS. In addition to a more pronounced activity against malignant cells, we detected decreased tumor volumes and weights in beauvericin-treated mice compared to controls in both the allo- and the xenograft model without any adverse effects. No significant differences were detected concerning percentages of proliferating and mitotic cells in tumor sections from treated and untreated mice. However, a significant increase of necrotic areas within whole tumor sections of beauvericin-treated mice was found in both models corresponding to an enhanced number of TUNEL-positive, i.e., apoptotic, cells. Furthermore, moderate beauvericin accumulation was detected in tumor tissues. In conclusion, we suggest beauvericin as a promising novel natural compound for anticancer therapy.

Published
2017
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25. Muscle fatigue revisited - Insights from optically pumped magnetometers

Author

Justus Marquetand, Christoph Braun, Romano A, Baek S, Davide Sometti, Dax J, Chen H, Righetti G, Kirchgässner M, Middelmann T, Lorenzo Semeia, Staber D, Cornelius Kronlage, Broser P, Oppold J, and Heilos J

Subjects
Materials science, Muscle fatigue, medicine.diagnostic_test, Magnetometer, Isometric exercise, Rectus femoris muscle, Electromyography, Neurophysiology, Signal, law.invention, law, Muscular fatigue, medicine, Biomedical engineering
Abstract

Muscle fatigue is well characterized electromyographically, nevertheless only information about summed potential differences is detectable. In contrast, recently developed quantum sensors optically pumped magnetometers (OPMs) offer the advantage of recording both the electrical current propagation in the muscle as well as its geometry, by measuring the magnetic field generated by the muscular action potentials. Magnetomyographic investigation of muscle fatigue is still lacking and it is an open question whether fatigue is characterized similarly in magnetomyography (MMG) compared to electromyography (EMG). Herein, we investigated the muscle fatigue during a 3×1-min strong isometric contraction of the rectus femoris muscle of 12 healthy subjects using simultaneous EMG-MMG (4-channel surface EMG and 4 OPM along the rectus femoris muscle).Both EMG and MMG showed the characteristic frequency decrease in the signal magnitude during isometric contraction, which is typical for muscle fatigue. In addition, it was shown that the main part of this frequency decrease seems to occur in the circular component of the magnetic field around the muscle fibers and less longitudinally along the muscle fibers. Overall, these results show not only that magnetomyography is capable of reproducing the electromyographic standards in identifying muscular fatigue, but it also adds relevant information about the spatial characterization of the signal. Therefore, OPM-MMG offers new insights for the study of muscular activity and might serve as a new, supplementary neurophysiological method.

Published
2021
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26. FHR-5 Serum Levels and CFHR5 Genetic Variations in Patients With Immune Complex-Mediated Membranoproliferative Glomerulonephritis and C3-Glomerulopathy

Author

Garam, Nóra, primary, Cserhalmi, Marcell, additional, Prohászka, Zoltán, additional, Szilágyi, Ágnes, additional, Veszeli, Nóra, additional, Szabó, Edina, additional, Uzonyi, Barbara, additional, Iliás, Attila, additional, Aigner, Christof, additional, Schmidt, Alice, additional, Gaggl, Martina, additional, Sunder-Plassmann, Gere, additional, Bajcsi, Dóra, additional, Brunner, Jürgen, additional, Dumfarth, Alexandra, additional, Cejka, Daniel, additional, Flaschberger, Stefan, additional, Flögelova, Hana, additional, Haris, Ágnes, additional, Hartmann, Ágnes, additional, Heilos, Andreas, additional, Mueller, Thomas, additional, Rusai, Krisztina, additional, Arbeiter, Klaus, additional, Hofer, Johannes, additional, Jakab, Dániel, additional, Sinkó, Mária, additional, Szigeti, Erika, additional, Bereczki, Csaba, additional, Janko, Viktor, additional, Kelen, Kata, additional, Reusz, György S., additional, Szabó, Attila J., additional, Klenk, Nóra, additional, Kóbor, Krisztina, additional, Kojc, Nika, additional, Knechtelsdorfer, Maarten, additional, Laganovic, Mario, additional, Lungu, Adrian Catalin, additional, Meglic, Anamarija, additional, Rus, Rina, additional, Kersnik Levart, Tanja, additional, Macioniene, Ernesta, additional, Miglinas, Marius, additional, Pawłowska, Anna, additional, Stompór, Tomasz, additional, Podracka, Ludmila, additional, Rudnicki, Michael, additional, Mayer, Gert, additional, Rysava, Romana, additional, Reiterova, Jana, additional, Saraga, Marijan, additional, Seeman, Tomáš, additional, Zieg, Jakub, additional, Sládková, Eva, additional, Stajic, Natasa, additional, Szabó, Tamás, additional, Capitanescu, Andrei, additional, Stancu, Simona, additional, Tisljar, Miroslav, additional, Galesic, Kresimir, additional, Tislér, András, additional, Vainumäe, Inga, additional, Windpessl, Martin, additional, Zaoral, Tomas, additional, Zlatanova, Galia, additional, Józsi, Mihály, additional, and Csuka, Dorottya, additional

Published
2021
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27. Muscle fatigue revisited - Insights from optically pumped magnetometers

Author

Sometti, Davide, Semeia, Lorenzo, Baek, Sangyeob, Chen, Hui, Righetti, Giulia, Dax, Juergen, Kronlage, Cornelius, Kirchgässner, Milena, Romano, Alyssa, Heilos, Johanna, Staber, Deborah, Oppold, Julia, Middelmann, Thomas, Braun, Christoph, Broser, Philip, and Marquetand, Justus

Subjects
sEMG, Physiology, OPM, muscle fatigue, Magnetomyography, Muscle Fatigue, Opm, Quantum Sensors, Semg, magnetomyography, quantum sensors, Original Research
Abstract

So far, surface electromyography (sEMG) has been the method of choice to detect and evaluate muscle fatigue. However, recent advancements in non-cryogenic quantum sensors, such as optically pumped magnetometers (OPMs), enable interesting possibilities to flexibly record biomagnetic signals. Yet, a magnetomyographic investigation of muscular fatigue is still missing. Here, we simultaneously used sEMG (4 surface electrode) and OPM-based magnetomyography (OPM-MMG, 4 sensors) to detect muscle fatigue during a 3 × 1-min isometric contractions of the left rectus femoris muscle in 7 healthy participants. Both signals exhibited the characteristic spectral compression distinctive for muscle fatigue. OPM-MMG and sEMG slope values, used to quantify the spectral compression of the signals, were positively correlated, displaying similarity between the techniques. Additionally, the analysis of the different components of the magnetic field vector enabled speculations regarding the propagation of the muscle action potentials (MAPs). Altogether these results show the feasibility of the magnetomyographic approach with OPMs and propose a potential alternative to sEMG for the study of muscle fatigue.

Published
2021

28. Recessive NOS1AP variants impair actin remodeling and cause glomerulopathy in humans and mice

Author

Amar J. Majmundar, Daniela A. Braun, Verena Klämbt, Youying Mao, Ali Amar, Ihsan Ullah, Florian Buerger, Caroline M. Kolvenbach, Neveen A. Soliman, Ker Sin Tan, Ana C. Onuchic-Whitford, Rufeng Dai, Friedhelm Hildebrandt, Shirlee Shril, Julie D. Forman-Kay, Chin Heng Chen, Marwa M. Nabhan, Andreas Heilos, Daanya Salmanullah, Richard P. Lifton, Kaitlyn Eddy, Konstantin Deutsch, Michelle Scurr, Renate Kain, Isabel Ottlewski, Melissa H. Little, Ronen Schneider, Thomas A. Forbes, Nina Mann, Makiko Nakayama, Eugen Widmeier, Seymour Rosen, Sara E. Howden, Amy Kolb, Thomas M. Kitzler, Shrikant Mane, Ethan W. Lai, Mickael Krzeminski, and Christoph Aufricht

Subjects
0303 health sciences, Gene knockdown, Multidisciplinary, Podosome, 030232 urology & nephrology, Actin remodeling, Glomerulosclerosis, macromolecular substances, Biology, medicine.disease, 3. Good health, Cell biology, Podocyte, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Glomerulopathy, medicine, Filopodia, Exome sequencing, 030304 developmental biology
Abstract

Nephrotic syndrome (NS) is a leading cause of chronic kidney disease. We found recessive NOS1AP variants in two families with early-onset NS by exome sequencing. Overexpression of wild-type (WT) NOS1AP, but not cDNA constructs bearing patient variants, increased active CDC42 and promoted filopodia and podosome formation. Pharmacologic inhibition of CDC42 or its effectors, formin proteins, reduced NOS1AP-induced filopodia formation. NOS1AP knockdown reduced podocyte migration rate (PMR), which was rescued by overexpression of WT Nos1ap but not by constructs bearing patient variants. PMR in NOS1AP knockdown podocytes was also rescued by constitutively active CDC42Q61L or the formin DIAPH3 Modeling a NOS1AP patient variant in knock-in human kidney organoids revealed malformed glomeruli with increased apoptosis. Nos1apEx3-/Ex3- mice recapitulated the human phenotype, exhibiting proteinuria, foot process effacement, and glomerulosclerosis. These findings demonstrate that recessive NOS1AP variants impair CDC42/DIAPH-dependent actin remodeling, cause aberrant organoid glomerulogenesis, and lead to a glomerulopathy in humans and mice.

Published
2021
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29. Recessive NOS1AP variants impair actin remodeling and cause glomerulopathy in humans and mice

Author

Majmundar, AJ, Buerger, F, Forbes, TA, Klambt, V, Schneider, R, Deutsch, K, Kitzler, TM, Howden, SE, Scurr, M, Tan, KS, Krzeminski, M, Widmeier, E, Braun, DA, Lai, E, Ullah, I, Amar, A, Kolb, A, Eddy, K, Chen, CH, Salmanullah, D, Dai, R, Nakayama, M, Ottlewski, I, Kolvenbach, CM, Onuchic-Whitford, AC, Mao, Y, Mann, N, Nabhan, MM, Rosen, S, Forman-Kay, JD, Soliman, NA, Heilos, A, Kain, R, Aufricht, C, Mane, S, Lifton, RP, Shril, S, Little, MH, Hildebrandt, F, Majmundar, AJ, Buerger, F, Forbes, TA, Klambt, V, Schneider, R, Deutsch, K, Kitzler, TM, Howden, SE, Scurr, M, Tan, KS, Krzeminski, M, Widmeier, E, Braun, DA, Lai, E, Ullah, I, Amar, A, Kolb, A, Eddy, K, Chen, CH, Salmanullah, D, Dai, R, Nakayama, M, Ottlewski, I, Kolvenbach, CM, Onuchic-Whitford, AC, Mao, Y, Mann, N, Nabhan, MM, Rosen, S, Forman-Kay, JD, Soliman, NA, Heilos, A, Kain, R, Aufricht, C, Mane, S, Lifton, RP, Shril, S, Little, MH, and Hildebrandt, F

Abstract

Nephrotic syndrome (NS) is a leading cause of chronic kidney disease. We found recessive NOS1AP variants in two families with early-onset NS by exome sequencing. Overexpression of wild-type (WT) NOS1AP, but not cDNA constructs bearing patient variants, increased active CDC42 and promoted filopodia and podosome formation. Pharmacologic inhibition of CDC42 or its effectors, formin proteins, reduced NOS1AP-induced filopodia formation. NOS1AP knockdown reduced podocyte migration rate (PMR), which was rescued by overexpression of WT Nos1ap but not by constructs bearing patient variants. PMR in NOS1AP knockdown podocytes was also rescued by constitutively active CDC42Q61L or the formin DIAPH3 Modeling a NOS1AP patient variant in knock-in human kidney organoids revealed malformed glomeruli with increased apoptosis. Nos1apEx3-/Ex3- mice recapitulated the human phenotype, exhibiting proteinuria, foot process effacement, and glomerulosclerosis. These findings demonstrate that recessive NOS1AP variants impair CDC42/DIAPH-dependent actin remodeling, cause aberrant organoid glomerulogenesis, and lead to a glomerulopathy in humans and mice.

Published
2021

31. EVI1 inhibits apoptosis induced by antileukemic drugs via upregulation of CDKN1A/p21/WAF in human myeloid cells.

Author

Anna Rommer, Birgit Steinmetz, Friederike Herbst, Hubert Hackl, Petra Heffeter, Daniela Heilos, Martin Filipits, Katarina Steinleitner, Shayda Hemmati, Irene Herbacek, Ilse Schwarzinger, Katharina Hartl, Pieter Rondou, Hanno Glimm, Kadin Karakaya, Alwin Krämer, Walter Berger, and Rotraud Wieser

Subjects
Medicine, Science
Abstract

Overexpression of ecotropic viral integration site 1 (EVI1) is associated with aggressive disease in acute myeloid leukemia (AML). Despite of its clinical importance, little is known about the mechanism through which EVI1 confers resistance to antileukemic drugs. Here, we show that a human myeloid cell line constitutively overexpressing EVI1 after infection with a retroviral vector (U937_EVI1) was partially resistant to etoposide and daunorubicin as compared to empty vector infected control cells (U937_vec). Similarly, inducible expression of EVI1 in HL-60 cells decreased their sensitivity to daunorubicin. Gene expression microarray analyses of U937_EVI1 and U937_vec cells cultured in the absence or presence of etoposide showed that 77 and 419 genes were regulated by EVI1 and etoposide, respectively. Notably, mRNA levels of 26 of these genes were altered by both stimuli, indicating that EVI1 regulated genes were strongly enriched among etoposide regulated genes and vice versa. One of the genes that were induced by both EVI1 and etoposide was CDKN1A/p21/WAF, which in addition to its function as a cell cycle regulator plays an important role in conferring chemotherapy resistance in various tumor types. Indeed, overexpression of CDKN1A in U937 cells mimicked the phenotype of EVI1 overexpression, similarly conferring partial resistance to antileukemic drugs.

Published
2013
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32. Recessive

Author

Amar J, Majmundar, Florian, Buerger, Thomas A, Forbes, Verena, Klämbt, Ronen, Schneider, Konstantin, Deutsch, Thomas M, Kitzler, Sara E, Howden, Michelle, Scurr, Ker Sin, Tan, Mickaël, Krzeminski, Eugen, Widmeier, Daniela A, Braun, Ethan, Lai, Ihsan, Ullah, Ali, Amar, Amy, Kolb, Kaitlyn, Eddy, Chin Heng, Chen, Daanya, Salmanullah, Rufeng, Dai, Makiko, Nakayama, Isabel, Ottlewski, Caroline M, Kolvenbach, Ana C, Onuchic-Whitford, Youying, Mao, Nina, Mann, Marwa M, Nabhan, Seymour, Rosen, Julie D, Forman-Kay, Neveen A, Soliman, Andreas, Heilos, Renate, Kain, Christoph, Aufricht, Shrikant, Mane, Richard P, Lifton, Shirlee, Shril, Melissa H, Little, and Friedhelm, Hildebrandt

Subjects
Mice, Nephrotic Syndrome, Podocytes, Animals, Formins, Humans, Kidney Diseases, Actins, Adaptor Proteins, Signal Transducing
Abstract

Nephrotic syndrome (NS) is a leading cause of chronic kidney disease. We found recessive

Published
2020

33. CFHR5 Genetic Variations and Serum Levels in Patients with Immune-Complex-Mediated Membranoproliferative Glomerulonephritis and C3-Glomerulopathy

Author

Attila Szabo, Barbara Uzonyi, Ágnes Szilágyi, Krešimir Galešić, Dóra Bajcsi, Gere Sunder-Plassmann, Mária Sinkó, Ernesta Macioniene, Anna Pawłowska, Nóra Klenk, Johannes Hofer, Marcell Cserhalmi, Klaus Arbeiter, Tanja Kersnik-Levart, Marius Miglinas, Dorottya Csuka, Ágnes Hartmann, Galia Zlatanova, Kata Kelen, Tomáš Seeman, Andreas Heilos, Marijan Saraga, Eva Sládková, Krisztina Rusai, Gert Mayer, Martin Windpessl, Erika Szigeti, Jana Reiterova, Ludmila Podracka, Nóra Veszeli, Edina Szabó, Martina Gaggl, Mario Laganović, Tamás Szabó, Tomasz Stompór, Stefan Flaschberger, Daniel Cejka, Rina Rus, Nika Kojc, Maarten Knechtelsdorfer, Nóra Garam, Miroslav Tisljar, András Tislér, Michael A. Rudnicki, Christof Aigner, Ágnes Haris, Natasa Stajic, Anamarija Meglic, Hana Flögelová, Jürgen Brunner, Simona Stancu, György Reusz, Attila Iliás, Jakub Zieg, Adrian Catalin Lungu, Viktor Janko, Thomas Mueller, Dániel Jakab, Inga Vainumäe, Krisztina Kóbor, Tomas Zaoral, Mihály Józsi, Csaba Bereczki, Romana Rysava, Alice Schmidt, Andrei Capitanescu, Zoltán Prohászka, and Alexandra Dumfarth

Subjects
Glomerulopathy, business.industry, embryonic structures, Genetic variation, Immunology, Membranoproliferative glomerulonephritis, medicine, In patient, medicine.disease, business, CFHR5, Immune complex
Abstract

Background: Factor H-related-5 (FHR-5) is a member of the complement Factor H protein family. Due to the homology to Factor H, the main complement regulator of the alternative pathway, it may also be implicated in pathomechanism of kidney diseases where Factor H and alternative pathway dysregulation play a role. Here, we report the first observational study on CFHR5 variations along with serum FHR-5 levels in immune-complex-mediated membranoproliferative glomerulonephritis (IC-MPGN) and C3 glomerulopathy (C3G) patients together with the clinical, genetic, complement and follow-up data.Results: 120 patients with a histologically-proven diagnosis of IC-MPGN/C3G were enrolled in the study. FHR-5 serum levels were measured in ELISA, the CFHR5 gene was analyzed by Sanger-sequencing, and selected mutants were studied as recombinant proteins in ELISA and SPR.Eight relevant CFHR5 variations in 14 patients (11.7%) were observed, 5 of them identified as pathogenic for C3G. The FHR-5G278S and FHR-5R356H mutations altered the interaction of FHR-5 with C3b, when compared to the FHR-5WT. Serum FHR-5 levels were lower in patients compared to controls. Low serum FHR-5 concentration at presentation associated with better renal survival during the follow-up period, furthermore, it showed clear association with signs of hypocomplementemia and clinically meaningful clusters.Conclusions: Our observations support the hypothesis that FHR-5 protein and its genetic alterations play a role in the pathogenesis of IC-MPGN/C3G.

Published
2020
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34. High-activity Classical and Alternative Complement Pathway Genotypes—Association With Donor-specific Antibody-triggered Injury and Renal Allograft Survival

Author

Roman Reindl-Schwaighofer, Andreas Heilos, Krisztina Rusai, Philip F. Halloran, Ondřej Viklický, Andreas Heinzel, Petra Hruba, Konstantin Doberer, Zoltán Prohászka, Georg A. Böhmig, Rainer Oberbauer, Blanka Mező, Helmuth Haslacher, Nicolas Kozakowski, Gregor Bond, Johannes Kläger, Markus Wahrmann, and Farsad Eskandary

Subjects
0303 health sciences, Transplantation, Kidney, biology, business.industry, Hazard ratio, 030232 urology & nephrology, Complement factor B, Kidney Transplantation, 3. Good health, 03 medical and health sciences, Classical complement pathway, 0302 clinical medicine, medicine.anatomical_structure, Interquartile range, Immunology, Cohort, biology.protein, Alternative complement pathway, ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, Medicine, Antibody, business, 030304 developmental biology
Abstract

Supplemental Digital Content is available in the text., Background. Complement may contribute to donor-specific antibody (DSA)-triggered transplant injury. Here, we investigated whether the intrinsic strength of classical pathway and alternative pathway (AP) relates to the pathogenicity of DSA. Methods. Classical pathway and AP high-activity genotypes were defined according to C4 gene copy number and the presence of functional polymorphisms in C3 (C3102G), factor B (fB32R), and factor H (fH62V) genes. Associations of these genotypes with blood complement profiles and morphologic/molecular rejection features were evaluated in a cohort of 83 DSA-positive patients (antibody-mediated rejection [AMR], n = 47) identified upon cross-sectional screening of 741 kidney allograft recipients ≥180 days posttransplantation. Associations with long-term graft survival were evaluated in a larger kidney transplant cohort (n = 660) not enriched for a specific type of rejection. Results. In the cohort of DSA-positive subjects, the number of C4 gene copies was related to C4 protein levels in serum and capillary C4d staining, but not AMR activity. Patients with a high-activity AP complotype, which was associated with complement consumption in serum, showed enhanced microcirculation inflammation (median glomerulitis plus peritubular capillaritis score, 2 [interquartile range, 0–4 versus 1 0–2]; P = 0.037). In the larger transplant cohort, this complotype was associated with a slightly increased risk of graft loss (hazard ratio, 1.52; 95% confidence interval, 1.02-2.25; P = 0.038 and multivariable Cox model, 1.55; 1.04-2.32; P = 0.031). Conclusions. Our study suggests a contribution of complement genetics to the phenotypic presentation of AMR. Future studies will have to clarify whether a possible association of AP strength with graft survival relates to enhanced antibody-triggered injury.

Published
2020

35. Contributor contact details

Author

Jansohn, P., primary, Mom, André J.A., additional, Desideri, U., additional, Kappis, W., additional, Flohr, P., additional, Schnieder, M., additional, Sommer, T., additional, Sundén, B., additional, Gellert, B., additional, Konter, M., additional, Bossman, H.-P., additional, Prade, B., additional, Razak, A.M.Y., additional, Álvarez Tejedor, T., additional, Singh, R., additional, Pilidis, P., additional, Huth, M., additional, Heilos, A., additional, Soothill, C.D., additional, Bialkowski, M.T., additional, Guidati, G.L., additional, Zagorskiy, A., additional, and Andrews, G.E., additional

Published
2013
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37. Recessive NOS1AP variants impair actin remodeling and cause glomerulopathy in humans and mice

Author

Majmundar, Amar J., primary, Buerger, Florian, additional, Forbes, Thomas A., additional, Klämbt, Verena, additional, Schneider, Ronen, additional, Deutsch, Konstantin, additional, Kitzler, Thomas M., additional, Howden, Sara E., additional, Scurr, Michelle, additional, Tan, Ker Sin, additional, Krzeminski, Mickaël, additional, Widmeier, Eugen, additional, Braun, Daniela A., additional, Lai, Ethan, additional, Ullah, Ihsan, additional, Amar, Ali, additional, Kolb, Amy, additional, Eddy, Kaitlyn, additional, Chen, Chin Heng, additional, Salmanullah, Daanya, additional, Dai, Rufeng, additional, Nakayama, Makiko, additional, Ottlewski, Isabel, additional, Kolvenbach, Caroline M., additional, Onuchic-Whitford, Ana C., additional, Mao, Youying, additional, Mann, Nina, additional, Nabhan, Marwa M., additional, Rosen, Seymour, additional, Forman-Kay, Julie D., additional, Soliman, Neveen A., additional, Heilos, Andreas, additional, Kain, Renate, additional, Aufricht, Christoph, additional, Mane, Shrikant, additional, Lifton, Richard P., additional, Shril, Shirlee, additional, Little, Melissa H., additional, and Hildebrandt, Friedhelm, additional

Published
2021
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38. Changed genome heterochromatinization upon prolonged activation of the Raf/ERK signaling pathway.

Author

Catherine Martin, Songbi Chen, Daniela Heilos, Guido Sauer, Jessica Hunt, Alexander George Shaw, Paul Francis George Sims, Dean Andrew Jackson, and Josip Lovrić

Subjects
Medicine, Science
Abstract

The Raf/ERK (Extracellular Signal Regulated Kinase) signal transduction pathway controls numerous cellular processes, including growth, differentiation, cellular transformation and senescence. ERK activation is thought to involve complex spatial and temporal regulation, to achieve a high degree of specificity, though precisely how this is achieved remains to be confirmed. We report here that prolonged activation of a conditional form of c-Raf-1 (BXB-ER) leads to profound changes in the level and distribution of a heterochromatic histone mark. In mouse fibroblasts, the heterochromatic trimethylation of lysine 9 in histone H3 (H3K9Me3) is normally confined to pericentromeric regions. However, following ERK activation a genome-wide redistribution of H3K9Me3 correlates with loss of the histone modification from chromocentres and the appearance of numerous punctuate sites throughout the interphase nucleus. These epigenetic changes during interphase correlate with altered chromosome structure during mitosis, where robust H3K9Me3 signals appear within telomeric heterochromatin. This pattern of heterochromatinization is distinct from previously described oncogene induced senescence associated heterochromatin foci (SAHF), which are excluded from telomeres. The H3K9Me3 histone mark is known to bind the major heterochromatin protein HP1 and we show that the alterations in the distribution of this histone epistate correlate with redistribution of HP1β throughout the nucleus. Interestingly while ERK activation is fully reversible, the observed chromatin changes induced by epigenetic modifications are not reversible once established. We describe for the first time a link from prolonged ERK activation to stable changes in genome organization through redistribution of heterochromatic domains involving the telomeres. These epigenetic changes provide a possible mechanism through which prolonged activation of Raf/ERK can lead to growth arrest or the induction of differentiation, senescence and cancer.

Published
2010
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40. Torque teno viral load reflects immunosuppression in paediatric kidney-transplanted patients—a pilot study

Author

Uhl, Phoebe, primary, Heilos, Andreas, additional, Bond, Gregor, additional, Meyer, Elias, additional, Böhm, Michael, additional, Puchhammer-Stöckl, Elisabeth, additional, Arbeiter, Klaus, additional, Müller-Sacherer, Thomas, additional, Csaicsich, Dagmar, additional, Aufricht, Christoph, additional, and Rusai, Krisztina, additional

Published
2020
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41. CFHR5 Genetic Variations and Serum Levels in Patients with Immune-Complex-Mediated Membranoproliferative Glomerulonephritis and C3-Glomerulopathy

Author

Garam, Nóra, primary, Cserhalmi, Marcell, additional, Prohászka, Zoltán, additional, Szilágyi, Ágnes, additional, Veszeli, Nóra, additional, Szabó, Edina, additional, Uzonyi, Barbara, additional, Iliás, Attila, additional, Aigner, Christof, additional, Schmidt, Alice, additional, Gaggl, Martina, additional, Sunder-Plassmann, Gere, additional, Bajcsi, Dóra, additional, Brunner, Jürgen, additional, Dumfarth, Alexandra, additional, Cejka, Daniel, additional, Flaschberger, Stefan, additional, Flögelova, Hana, additional, Haris, Ágnes, additional, Hartmann, Ágnes, additional, Heilos, Andreas, additional, Mueller, Thomas, additional, Rusai, Krisztina, additional, Arbeiter, Klaus, additional, Hofer, Johannes, additional, Jakab, Dániel, additional, Sinkó, Mária, additional, Szigeti, Erika, additional, Bereczki, Csaba, additional, Janko, Viktor, additional, Kelen, Kata, additional, Reusz, György S., additional, Szabó, Attila J., additional, Klenk, Nóra, additional, Kóbor, Krisztina, additional, Kojc, Nika, additional, Knechtelsdorfer, Maarten, additional, Laganovic, Mario, additional, Lungu, Adrian Catalin, additional, Meglic, Anamarija, additional, Rus, Rina, additional, Kersnik-Levart, Tanja, additional, Macioniene, Ernesta, additional, Miglinas, Marius, additional, Pawłowska, Anna, additional, Stompór, Tomasz, additional, Podracka, Ludmila, additional, Rudnicki, Michael, additional, Mayer, Gert, additional, Rysava, Romana, additional, Reiterova, Jana, additional, Saraga, Marijan, additional, Seeman, Tomáš, additional, Zieg, Jakub, additional, Sládková, Eva, additional, Stajic, Natasa, additional, Szabó, Tamás, additional, Capitanescu, Andrei, additional, Stancu, Simona, additional, Tisljar, Miroslav, additional, Galesic, Kresimir, additional, Tislér, András, additional, Vainumäe, Inga, additional, Windpessl, Martin, additional, Zaoral, Tomas, additional, Zlatanova, Galia, additional, Józsi, Mihály, additional, and Csuka, Dorottya, additional

Published
2020
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42. Validation of distinct pathogenic patterns in a cohort of membranoproliferative glomerulonephritis patients by cluster analysis

Author

Dániel Jakab, Ágnes Szilágyi, Gert Mayer, Nóra Garam, Miroslav Tisljar, Viktor Janko, Attila Szabo, Inga Vainumäe, Christof Aigner, Ágnes Hartmann, Simona Stancu, Galia Zlatanova, Tamás Szabó, Marius Miglinas, András Tislér, Krisztina Kóbor, Tomáš Seeman, Mária Sinkó, Alice Schmidt, Stefan Flaschberger, Hana Flögelová, Nika Kojc, Klaus Arbeiter, Jana Reiterova, Tomas Zaoral, Michael A. Rudnicki, Gere Sunder-Plassmann, Romana Rysava, Jürgen Brunner, Maarten Knechtelsdorfer, Daniel Cejka, Ágnes Haris, György Reusz, Krešimir Galešić, Mario Laganović, Tomasz Stompór, Anna Pawłowska, Anamarija Meglic, Eva Sládková, Dorottya Csuka, Andrei Capitanescu, Tanja Kersnik-Levart, Zoltán Prohászka, Rina Rus, Adrian Catalin Lungu, Csaba Bereczki, Marijan Saraga, Thomas Mueller, Ernesta Macioniene, Andreas Heilos, Krisztina Rusai, Kata Kelen, Erika Szigeti, Alexandra Dumfarth, Dóra Bajcsi, Ludmila Podracka, Martina Gaggl, Jakub Zieg, Nóra Klenk, Johannes Hofer, and Martin Windpessl

Subjects
C3 Glomerulonephritis, 030232 urology & nephrology, Late onset, C3-glomerulopathy, C3-glomerulonephritis, 03 medical and health sciences, Nephritic syndrome, 0302 clinical medicine, Membranoproliferative glomerulonephritis, medicine, complement, 030304 developmental biology, 0303 health sciences, Transplantation, dense deposit disease, membranoproliferative glomerulonephritis, business.industry, Incidence (epidemiology), Original Articles, medicine.disease, Nephrology, Immunology, Cohort, Age of onset, Complement membrane attack complex, business
Abstract

Background A novel data-driven cluster analysis identified distinct pathogenic patterns in C3-glomerulopathies and immune complex-mediated membranoproliferative glomerulonephritis. Our aim was to replicate these observations in an independent cohort and elucidate disease pathophysiology with detailed analysis of functional complement markers. Methods A total of 92 patients with clinical, histological, complement and genetic data were involved in the study, and hierarchical cluster analysis was done by Ward method, where four clusters were generated. Results High levels of sC5b-9 (soluble membrane attack complex), low serum C3 levels and young age at onset (13 years) were characteristic for Cluster 1 with a high prevalence of likely pathogenic variations (LPVs) and C3 nephritic factor, whereas for Cluster 2—which is not reliable because of the small number of cases—strong immunoglobulin G staining, low C3 levels and high prevalence of nephritic syndrome at disease onset were observed. Low plasma sC5b-9 levels, decreased C3 levels and high prevalence of LPV and sclerotic glomeruli were present in Cluster 3, and patients with late onset of the disease (median: 39.5 years) and near-normal C3 levels in Cluster 4. A significant difference was observed in the incidence of end-stage renal disease during follow-up between the different clusters. Patients in Clusters 3–4 had worse renal survival than patients in Clusters 1–2. Conclusions Our results confirm the main findings of the original cluster analysis and indicate that the observed, distinct pathogenic patterns are replicated in our cohort. Further investigations are necessary to analyse the distinct biological and pathogenic processes in these patient groups.

Published
2019

44. C4 nephritic factor in patients with immune-complex-mediated membranoproliferative glomerulonephritis and C3-glomerulopathy

Author

Ágnes Szilágyi, Christof Aigner, Attila Szabo, Tanja Kersnik-Levart, Dorottya Csuka, Ágnes Haris, Alice Schmidt, Rina Rus, Stefan Flaschberger, Ernesta Macioniene, Hana Flögelová, Anamarija Meglic, Ludmila Podracka, Gere Sunder-Plassmann, Alexandra Dumfarth, Martina Gaggl, Andrei Capitanescu, Viktor Janko, Anna Pawłowska, Gert Mayer, Thomas Mueller, Ágnes Hartmann, András Tislér, Kata Kelen, Erika Szigeti, Galia Zlatanova, Martin Windpessl, Tamás Szabó, Klaus Arbeiter, Mario Laganović, György Reusz, Romana Rysava, Krisztina Kóbor, Jakub Zieg, Daniel Cejka, Michael A. Rudnicki, Andreas Heilos, Krisztina Rusai, Dániel Jakab, Tomas Zaoral, Nóra Klenk, Johannes Hofer, Nóra Garam, Krešimir Galešić, Jürgen Brunner, Miroslav Tisljar, Marius Miglinas, Mária Sinkó, Csaba Bereczki, Inga Vainumäe, Nika Kojc, Marijan Saraga, Tomáš Seeman, Simona Stancu, Eva Sládková, Jana Reiterova, Zoltán Prohászka, Maarten Knechtelsdorfer, Adrian Catalin Lungu, Tomasz Stompór, and Dóra Bajcsi

Subjects
0301 basic medicine, Adult, Male, Adolescent, C3 Glomerulonephritis, Glomerulonephritis, Membranoproliferative, 030232 urology & nephrology, lcsh:Medicine, Disease, C4 nephritic factor, 03 medical and health sciences, Classical complement pathway, Young Adult, 0302 clinical medicine, C3 glomerulonephritis, Glomerulopathy, Membranoproliferative glomerulonephritis, Medicine, Humans, Pharmacology (medical), C3 glomerulopathy, C3 nephritic factor, Genetics (clinical), Autoantibodies, Complement C3 Nephritic Factor, Dense deposit disease, business.industry, Research, lcsh:R, Autoantibody, General Medicine, Complement System Proteins, medicine.disease, Immune complex, 030104 developmental biology, Immunology, Alternative complement pathway, Female, Kidney Diseases, business
Abstract

Background Acquired or genetic abnormalities of the complement alternative pathway are the primary cause of C3glomerulopathy(C3G) but may occur in immune-complex-mediated membranoproliferative glomerulonephritis (IC-MPGN) as well. Less is known about the presence and role of C4nephritic factor(C4NeF) which may stabilize the classical pathway C3-convertase. Our aim was to examine the presence of C4NeF and its connection with clinical features and with other pathogenic factors. Results One hunfe IC-MPGN/C3G patients were enrolled in the study. C4NeF activity was determined by hemolytic assay utilizing sensitized sheep erythrocytes. Seventeen patients were positive for C4NeF with lower prevalence of renal impairment and lower C4d level, and higher C3 nephritic factor (C3NeF) prevalence at time of diagnosis compared to C4NeF negative patients. Patients positive for both C3NeF and C4NeF had the lowest C3 levels and highest terminal pathway activation. End-stage renal disease did not develop in any of the C4NeF positive patients during follow-up period. Positivity to other complement autoantibodies (anti-C1q, anti-C3) was also linked to the presence of nephritic factors. Unsupervised, data-driven cluster analysis identified a group of patients with high prevalence of multiple complement autoantibodies, including C4NeF. Conclusions In conclusion, C4NeF may be a possible cause of complement dysregulation in approximately 10–15% of IC-MPGN/C3G patients.

Published
2019

45. Mechanistische Untersuchungen zur Inhibition von Cathepsin B und Rhodesain mit niedermolekularen Inhibitoren

Author

Heilos, Anna

Subjects
540 Chemie und zugeordnete Wissenschaften, Inhibitor, ddc:540, Cysteinproteasen
Abstract

Cysteine proteases play a crucial role in medical chemistry concerning various fields reaching from more common ailments like cancer and hepatitis to less noted tropical diseases, namely the so-called African Sleeping Sickness (Human Arfican Trypanosomiasis). Detailed knowledge about the catalytic function of these systems is highly desirable for drug research in the respective areas. In this work, the inhibition mechanisms of the two cysteine proteases cathepsin B and rhodesain with respectively one low-molecular inhibitor class were investigated in detail, using computational methods. In order to sufficiently describe macromolecular systems, molecular mechanics based methods (MM) and quantum mechanical based method (QM), as well as hybrid methods (QM/MM) combining those two approaches, were applied. For Cathespin B, carbamate-based molecules were investigated as potential inhibitors for the cysteine protease. The results indicate, that water-bridged proton-transfer reactions play a crucial role for the inhibition. The energetically most favoured pathway (according to the calculations) includes an elimination reaction following an E1cB mechanism with a subsequent carbamylation of the active site amino acid cysteine. Nitroalkene derivatives were investigated as inhibitors for rhodesain. The investigation of structurally similar inhibitors showed, that even small steric differences can crucially influence the inhibition potential of the components. Furthermore, the impact of a fluorination of the nitroalkene inhibitors on the inhibition mechanism was investigated. According to experimental data measured from the working group of professor Schirmeister in Mainz, fluorinated nitroalkenes show – in contrast to the unfluorinated compounds – a time dependent inhibition efficiency. The calculations of the systems indicate, that the fluorination impacts the non-covalent interactions of the inhibitors with the enzymatic environment of the enzyme which results in a different inhibition behaviour., Cysteinproteasen spielen eine wichtige Rolle in der medizinischen Chemie. Nicht nur im Bereich bekannterer Krankheiten wie Krebs oder Hepatitis, sondern auch bezüglich weniger verbreiteter, tropischer Krankheiten wie der sogenannten afrikanischen Schlafkrankheit (Afrikanische Trypanosomiasis) haben diese Enzyme eine große Bedeutung. Im Bereich der Wirkstofffindung ist ein detailliertes Wissen über die katalytische Funktion der an einer Krankheit beteiligten Enzyme unabdingbar .In der vorliegenden Arbeit wurden die Inhibitionsmechanismen der beiden Cysteinproteasen Cathepsin B und Rhodesain in Verbindung mit zwei niedermolekularen Inhibitorklassen anhand theoretischer Berechnungen untersucht. Um die makromolekularen Systeme ausreichend genau beschreiben zu können, wurden neben molekularmechanischen (MM) und quantenmechanischen (QM) Ansätzen auch Hybridmethoden verwendet, welche beide Ansätze (QM/MM) verbinden. Für Cathepsin B wurden Carbamat-basierte Moleküle als potenzielle Inhibitoren der Cysteinprotease untersucht. Die Ergebnisse weisen darauf hin, dass wasser-verbrückte Protonentransferreaktionen eine entscheidende Rolle für die Inhibition spielen. Der laut den Rechnungen energetisch günstigste Mechanismus beinhaltet eine Eliminierungsreaktion nach einem E1cB Mechanismus gefolgt von der Carbamylierung der Aminosäure Cystein in der aktiven Tasche des Enzyms. Nitroalken-Derivate wurden als potenzielle Rhodesain Inhibitoren untersucht. Der Vergleich strukturell ähnlicher Verbindungen weist darauf hin, dass schon kleine sterische Veränderungen einen großen Einfluss auf das Inhibitionspotenzial der Nitroalkene haben können. Außerdem wurde der Einfluss einer Fluorierung der Inhibitoren anhand von Berechnungen untersucht. Messungen der Arbeitsgruppe von Prof. Schirmeister in Mainz zu fluorierten und unfluorierten Nitroalkenen zeigen, dass die fluorierten Verbindungen ein zeitabhängiges Inhibitionspotenzial in Rhodesain aufweisen. Die Berechnungen der Systeme deuten darauf hin, dass die Fluorierung die nicht-kovalenten Wechselwirkungen der Inhibitoren mit der enzymatischen Umgebung des Systems beeinflussen, was zu einem unterschiedlichen Inhibitionsverhalten führt.

Published
2019

46. Intrinsic fluorescence of the clinically approved multikinase inhibitor nintedanib reveals lysosomal sequestration as resistance mechanism in FGFR-driven lung cancer

Author

Englinger, Bernhard, Kallus, Sebastian, Senkiv, Julia, Heilos, Daniela, Gabler, Lisa, van Schoonhoven, Sushilla, Terenzi, Alessio, Moser, Patrick, Pirker, Christine, Timelthaler, Gerald, Jäger, Walter, Kowol, Christian R., Heffeter, Petra, Grusch, Michael, Berger, Walter, Englinger B., Kallus S., Senkiv J., Heilos D., Gabler L., Van Schoonhoven S., Terenzi A., Moser P., Pirker C., Timelthaler G., Jager W., Kowol C.R., Heffeter P., Grusch M., and Berger W.

Subjects
Indoles, Lung Neoplasms, Nintedanib, Resistance, lcsh:RC254-282, Fluorescence, Mice, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, Animals, Humans, Phosphorylation, Lung, Cell Proliferation, Antineoplastic Combined Chemotherapy Protocol, Animal, Research, Drug Synergism, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Lysosome, Receptors, Fibroblast Growth Factor, Xenograft Model Antitumor Assays, Lung Neoplasm, FGFR1, Indole, Settore CHIM/03 - Chimica Generale E Inorganica, Macrolides, Macrolide, Lysosomes, Human, Signal Transduction
Abstract

Background Studying the intracellular distribution of pharmacological agents, including anticancer compounds, is of central importance in biomedical research. It constitutes a prerequisite for a better understanding of the molecular mechanisms underlying drug action and resistance development. Hyperactivated fibroblast growth factor receptors (FGFRs) constitute a promising therapy target in several types of malignancies including lung cancer. The clinically approved small-molecule FGFR inhibitor nintedanib exerts strong cytotoxicity in FGFR-driven lung cancer cells. However, subcellular pharmacokinetics of this compound and its impact on therapeutic efficacy remain obscure. Methods 3-dimensional fluorescence spectroscopy was conducted to asses cell-free nintedanib fluorescence properties. MTT assay was used to determine the impact of the lysosome-targeting agents bafilomycin A1 and chloroquine combined with nintedanib on lung cancer cell viability. Flow cytometry and live cell as well as confocal microscopy were performed to analyze uptake kinetics as well as subcellular distribution of nintedanib. Western blot was conducted to investigate protein expression. Cryosections of subcutaneous tumor allografts were generated to detect intratumoral nintedanib in mice after oral drug administration. Results Here, we report for the first time drug-intrinsic fluorescence properties of nintedanib in living and fixed cancer cells as well as in cryosections derived from allograft tumors of orally treated mice. Using this feature in conjunction with flow cytometry and confocal microscopy allowed to determine cellular drug accumulation levels, impact of the ABCB1 efflux pump and to uncover nintedanib trapping into lysosomes. Lysosomal sequestration - resulting in an organelle-specific and pH-dependent nintedanib fluorescence - was identified as an intrinsic resistance mechanism in FGFR-driven lung cancer cells. Accordingly, combination of nintedanib with agents compromising lysosomal acidification (bafilomycin A1, chloroquine) exerted distinctly synergistic growth inhibitory effects. Conclusion Our findings provide a powerful tool to dissect molecular factors impacting organismal and intracellular pharmacokinetics of nintedanib. Regarding clinical application, prevention of lysosomal trapping via lysosome-alkalization might represent a promising strategy to circumvent cancer cell-intrinsic nintedanib resistance. Electronic supplementary material The online version of this article (10.1186/s13046-017-0592-3) contains supplementary material, which is available to authorized users.

Published
2017

47. Vergasung fester und flüssiger Brennstoffe

Author

Jaan Hellat, Jürgen Karg, Andreas Heilos, and Michael Huth

Abstract

Gasturbinen werden bis heute noch fast ausschlieslich zur Verstromung von Erdgas oder Heizol eingesetzt. Die Vorschaltung einer Vergasungsanlage ermoglicht auch die Nutzung von festen oder flussigen Brennstoffen wie Kohle oder Raffinerieruckstanden, die sonst nicht direkt in einer Gasturbine bzw. GuD-Anlagemit hohem Wirkungsgrad umgesetzt werden konnten. Diese Kopplung aus Vergasungsanlage mit nachgeschalteter Gasreinigung und anschliesender Nutzung des gereinigten Synthesegases (Syngas) in einer GuD-Anlage wird als IGCC-Kraftwerk (IGCC = Integrated Gasification Combined Cycle) bezeichnet.

Published
2018
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49. Altered membrane rigidity via enhanced endogenous cholesterol synthesis drives cancer cell resistance to destruxins

Author

Ursula Windberger, Sushilla van Schoonhoven, Shahid Iqbal, Bernhard Englinger, Thomas Mohr, Walter Jäger, Hermann Stuppner, Judith Taibon, Clemens Röhrl, Dina Baier, Tanja Eberhart, Rosa Lemmens-Gruber, Kristaps Klavins, Rita Dornetshuber-Fleiss, Michaela Schwaiger, Christine Pirker, Daniela Heilos, Walter Berger, Sonja Sturm, and Gunda Koellensperger

Subjects
0301 basic medicine, Cell type, Oxysterol, Cholesterol, Cell, cell membrane alterations, Cell biology, Cell membrane, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, destruxins, Oncology, chemistry, 030220 oncology & carcinogenesis, mycotoxins, Cancer cell, medicine, Mevalonate pathway, cholesterol synthesis pathway, Mode of action, Research Paper, cancer cell resistance
Abstract

Destruxins, secondary metabolites of entomopathogenic fungi, exert a wide variety of interesting characteristics ranging from antiviral to anticancer effects. Although their mode of action was evaluated previously, the molecular mechanisms of resistance development are unknown. Hence, we have established destruxin-resistant sublines of HCT116 colon carcinoma cells by selection with the most prevalent derivatives, destruxin (dtx)A, dtxB and dtxE. Various cell biological and molecular techniques were applied to elucidate the regulatory mechanisms underlying these acquired and highly stable destruxin resistance phenotypes. Interestingly, well-known chemoresistance-mediating ABC efflux transporters were not the major players. Instead, in dtxA- and dtxB-resistant cells a hyper-activated mevalonate pathway was uncovered resulting in increased de-novo cholesterol synthesis rates and elevated levels of lanosterol, cholesterol as well as several oxysterol metabolites. Accordingly, inhibition of the mevalonate pathway at two different steps, using either statins or zoledronic acid, significantly reduced acquired but also intrinsic destruxin resistance. Vice versa, cholesterol supplementation protected destruxin-sensitive cells against their cytotoxic activity. Additionally, an increased cell membrane adhesiveness of dtxA-resistant as compared to parental cells was detected by atomic force microscopy. This was paralleled by a dramatically reduced ionophoric capacity of dtxA in resistant cells when cultured in absence but not in presence of statins. Summarizing, our results suggest a reduced ionophoric activity of destruxins due to cholesterol-mediated plasma membrane re-organization as molecular mechanism underlying acquired destruxin resistance in human colon cancer cells. Whether this mechanism might be valid also in other cell types and organisms exposed to destruxins e.g. as bio-insecticides needs to be evaluated.

Published
2018

50. Validation of distinct pathogenic patterns in a cohort of membranoproliferative glomerulonephritis patients by cluster analysis

Author

Garam, Nóra, primary, Prohászka, Zoltán, primary, Szilágyi, Ágnes, primary, Aigner, Christof, primary, Schmidt, Alice, primary, Gaggl, Martina, primary, Sunder-Plassmann, Gere, primary, Bajcsi, Dóra, primary, Brunner, Jürgen, primary, Dumfarth, Alexandra, primary, Cejka, Daniel, primary, Flaschberger, Stefan, primary, Flögelova, Hana, primary, Haris, Ágnes, primary, Hartmann, Ágnes, primary, Heilos, Andreas, primary, Mueller, Thomas, primary, Rusai, Krisztina, primary, Arbeiter, Klaus, primary, Hofer, Johannes, primary, Jakab, Dániel, primary, Sinkó, Mária, primary, Szigeti, Erika, primary, Bereczki, Csaba, primary, Janko, Viktor, primary, Kelen, Kata, primary, Reusz, György S, primary, Szabó, Attila J, primary, Klenk, Nóra, primary, Kóbor, Krisztina, primary, Kojc, Nika, primary, Knechtelsdorfer, Maarten, primary, Laganovic, Mario, primary, Lungu, Adrian Catalin, primary, Meglic, Anamarija, primary, Rus, Rina, primary, Kersnik-Levart, Tanja, primary, Macioniene, Ernesta, primary, Miglinas, Marius, primary, Pawłowska, Anna, primary, Stompór, Tomasz, primary, Podracka, Ludmila, primary, Rudnicki, Michael, primary, Mayer, Gert, primary, Rysava, Romana, primary, Reiterova, Jana, primary, Saraga, Marijan, primary, Seeman, Tomáš, primary, Zieg, Jakub, primary, Sládková, Eva, primary, Szabó, Tamás, primary, Capitanescu, Andrei, primary, Stancu, Simona, primary, Tisljar, Miroslav, primary, Galesic, Kresimir, primary, Tislér, András, primary, Vainumäe, Inga, primary, Windpessl, Martin, primary, Zaoral, Tomas, primary, Zlatanova, Galia, primary, and Csuka, Dorottya, primary

Published
2019
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