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2. CD14high CD16+ monocytes are the main producers of Interleukin-10 following clinical heart transplantation.

Author

Ludwig, Kristina, Chichelnitskiy, Evgeny, Kühne, Jenny F., Wiegmann, Bettina, Iske, Jasper, Ledwoch, Nadine, Ius, Fabio, Beushausen, Kerstin, Keil, Jana, Iordanidis, Susanne, Rojas, Sebastian V., Salman, Jawad, Knoefel, Ann-Kathrin, Haverich, Axel, Warnecke, Gregor, and Falk, Christine S.

Subjects
MONONUCLEAR leukocytes, HEART transplantation, MONOCYTES, LYMPHOCYTE subsets, HEART transplant recipients
Abstract

Introduction: Following heart transplantation, a cascade of immunological responses is initiated influencing the clinical outcome and long-term survival of the transplanted patients. The anti-inflammatory cytokine interleukin-10 (IL-10) was shown to be elevated in the blood of heart transplant recipients directly after transplantation but the releasing cell populations and the composition of lymphocyte subsets following transplantation have not been thoroughly studied. Methods: We identified immune cells by immunophenotyping and analyzed intracellular IL-10 production in peripheral blood mononuclear cells (PBMC) of heart transplanted patients (n= 17) before, directly after and 24h post heart transplantation. The cells were stimulated with lipopolysaccharide or PMA/Ionomycin to enhance cytokine production within leukocytes in vitro. Results and discussion: We demonstrate that intermediate monocytes (CD14highCD16+), but not CD8+ T cells, CD4+ T cells, CD56+ NK cells or CD20+ B cells appeared to be the major IL-10 producers within patients PBMC following heart transplantation. Consequently, the absolute monocyte count and the ratio of intermediate monocytes to classical monocytes (CD14+CD16-) were specifically increased in comparison to pre transplant levels. Hence, this population of monocytes, which has not been in the focus of heart transplantation so far, may be an important modulator of clinical outcome and long-term survival of heart transplant recipients. Alteration of blood-circulating monocytes towards a CD14highCD16+ phenotype could therefore shift the pro-inflammatory immune response towards induction of graft tolerance, and may pave the way for the optimization of immunosuppression. [ABSTRACT FROM AUTHOR]

Published
2023
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3. Infotainers, Mediators, or Watchdogs? Mapping the Field of News Podcasters and Their Role Conceptions in Germany, Austria, and Switzerland.

Author

Katzenberger, Vera, Schützeneder, Jonas, Grassl, Michael, and Keil, Jana

Subjects
PODCASTING, NATIVE advertising, INFORMATION dissemination, MASS media, WORK experience (Employment)
Abstract

News podcasts have emerged as a relevant medium, contributing to the collection, analysis, interpretation, and dissemination of information in mass media discourse. This paper presents an analysis of the sociodemographic backgrounds, professional profiles, role perceptions, and values of news podcasters based on an online survey of 195 participants in Austria, Germany, and Switzerland. The results reveal that news podcasters are predominantly male, middle-aged, and academically educated with no journalistic socialization or journalistic working experience. In terms of self-images and values, news podcasters emphasize the importance of education, information, and entertainment, while rejecting conventional concepts like criticism and control. Overall, they demonstrate a strong orientation towards the needs of their audiences and strive to be responsive to their preferences. Yet, the monetization of content through financing models such as sponsoring or native advertisement is not established on a broad scale. These findings shed light on the unique characteristics of news podcasters and provide insights into their status in a rapidly changing media environment. [ABSTRACT FROM AUTHOR]

Published
2023
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4. Immediate major dynamic changes in the T‐ and NK‐cell subset composition after cardiac transplantation.

Author

Iske, Jasper, Wiegmann, Bettina, Ius, Fabio, Chichelnitskiy, Evgeny, Ludwig, Kristina, Kühne, Jenny F., Hitz, Anna Maria, Beushausen, Kerstin, Keil, Jana, Iordanidis, Susanne, Rojas, Sebastián V., Sommer, Wiebke, Salman, Jawad, Haverich, Axel, Warnecke, Gregor, and Falk, Christine S

Subjects
HEART transplantation, LYMPHOCYTE subsets, KILLER cells, IMMUNOLOGIC memory, T cells, REJECTION (Psychology)
Abstract

Early kinetics of lymphocyte subsets involved in tolerance and rejection following heart transplantation (HTx) are barely defined. Here, we aimed to delineate the early alloimmune response immediately after HTx. Therefore, blood samples from 23 heart‐transplanted patients were collected before (pre‐), immediately (T0), 24 hours (T24), and 3 weeks (3 wks) after HTx. Immunophenotyping was performed using flow cytometry. A significant increase was detected for terminally differentiated (TEMRA) CD4+ or CD8+ T cells and CD56dimCD16+ NK cells immediately after HTx linked to a decrease in naïve CD8+ and CM CD4+ T as well as CD56brightCD16− NK cells, returning to baseline levels at T24. More detailed analyses revealed increased CD69+CD25− and diminished CD69−CD25−CD4+ or CD8+ T‐cell proportions at T0 associated with decreasing S1PR1 expression. Passenger T and NK cells were found at low frequencies only in several patients at T0 and did not correlate with lymphocyte alterations. Collectively, these results suggest an immediate, transient shift toward memory T and NK cells following HTx. Opposite migratory properties of naïve versus memory T and NK cells occurring in the early phase after HTx could underlie these observations and may impinge on the development of allo‐specific immune responses. [ABSTRACT FROM AUTHOR]

Published
2023
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7. Third SARS-CoV-2 vaccination and breakthrough infections enhance humoral and cellular immunity against variants of concern.

Author

Ruhl, Louisa, Kühne, Jenny F., Beushausen, Kerstin, Keil, Jana, Christoph, Stella, Sauer, Jasper, and Falk, Christine S.

Subjects
BREAKTHROUGH infections, CELLULAR immunity, SARS-CoV-2, SARS-CoV-2 Omicron variant, IMMUNOLOGIC memory, PSYCHONEUROIMMUNOLOGY, BODY dysmorphic disorder
Abstract

Introduction: SARS-CoV-2 vaccination is the leading strategy to prevent severe courses after SARS-CoV-2 infection. In our study, we analyzed humoral and cellular immune responses in detail to three consecutive homologous or heterologous SARS-CoV-2 vaccinations and breakthrough infections. Methods: Peripheral blood samples of n=20 individuals were analyzed in the time course of three SARS-CoV-2 vaccinations and/or breakthrough infection. S1-, RBD-, S2- and N-specific IgG antibodies were quantified using Luminexbased multiplex assays and electrochemiluminescence multiplex assays for surrogate neutralization in plasma. Changes in cellular immune components were determined via flow cytometry of whole blood samples. Results: All individuals (n=20) responded to vaccination with increasing S1-/RBD-/S2-specific IgG levels, whereas specific plasma IgA displayed individual variability. The third dose increased antibody inhibitory capacity (AIC) against immune-escape variants Beta and Omicron BA.1 independently of age. The mRNA-primed vaccination induced IgG and IgA immunity more efficiently, whereas vectorprimed individuals displayed higher levels of memory T and B cells. Vaccinees showed SARS-CoV-2-specific T cell responses, which were further improved and specified afterOmicron breakthrough infections in parallel to the appearance of new variant-specific antibodies. Discussion: In conclusion, the third vaccination was essential to increase IgG levels, mandatory to boost AIC against immune-escape variants, and induced SARS-CoV-2-specific T cells. Breakthrough infection with Omicron generates additional spike specificities covering all known variants. [ABSTRACT FROM AUTHOR]

Published
2023
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8. Donor NK and T Cells in the Periphery of Lung Transplant Recipients Contain High Frequencies of Killer Cell Immunoglobulin-Like Receptor-Positive Subsets.

Author

Hitz, Anna-Maria, Bläsing, Kim-Alina, Wiegmann, Bettina, Bellmàs-Sanz, Ramon, Chichelnitskiy, Evgeny, Wandrer, Franziska, Horn, Lisa-Marie, Neudörfl, Christine, Keil, Jana, Beushausen, Kerstin, Ius, Fabio, Sommer, Wiebke, Avsar, Murat, Kühn, Christian, Tudorache, Igor, Salman, Jawad, Siemeni, Thierry, Haverich, Axel, Warnecke, Gregor, and Falk, Christine S.

Subjects
KILLER cells, T cells, LUNG transplantation, KILLER cell receptors, GRAFT survival
Abstract

Introduction: For end-stage lung diseases, double lung transplantation (DLTx) is the ultimate curative treatment option. However, acute and chronic rejection and chronic dysfunction are major limitations in thoracic transplantation medicine. Thus, a better understanding of the contribution of immune responses early after DLTx is urgently needed. Passenger cells, derived from donor lungs and migrating into the recipient periphery, are comprised primarily by NK and T cells. Here, we aimed at characterizing the expression of killer cell immunoglobulin-like receptors (KIR) on donor and recipient NK and T cells in recipient blood after DLTx. Furthermore, we investigated the functional status and capacity of donor vs. recipient NK cells. Methods: Peripheral blood samples of 51 DLTx recipients were analyzed pre Tx and at T0, T24 and 3wk post Tx for the presence of HLA-mismatched donor NK and T cells, their KIR repertoire as well as activation status using flow cytometry. Results: Within the first 3 weeks after DLTx, donor NK and T cells were detected in all patients with a peak at T0. An increase of the KIR2DL/S1-positive subset was found within the donor NK cell repertoire. Moreover, donor NK cells showed significantly higher frequencies of KIR2DL/S1-positive cells (p<0.01) 3wk post DLTx compared to recipient NK cells. This effect was also observed in donor KIR+ T cells 3wk after DLTx with higher proportions of KIR2DL/S1 (p<0.05) and KIR3DL/S1 (p<0.01) positive T cells. Higher activation levels of donor NK and T cells (p<0.001) were detected compared to recipient cells via CD25 expression as well as a higher degranulation capacity upon activation by K562 target cells. Conclusion: Higher frequencies of donor NK and T cells expressing KIR compared to recipient NK and T cells argue for their origin in the lung as a part of a highly specialized immunocompetent compartment. Despite KIR expression, higher activation levels of donor NK and T cells in the periphery of recipients suggest their pre-activation during the ex situ phase. Taken together, donor NK and T cells are likely to have a regulatory effect in the balance between tolerance and rejection and, hence, graft survival after DLTx. [ABSTRACT FROM AUTHOR]

Published
2021
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10. Defining the Inflammatory Microenvironment in the Human Cochlea by Perilymph Analysis: Toward Liquid Biopsy of the Cochlea.

Author

Warnecke, Athanasia, Prenzler, Nils K., Schmitt, Heike, Daemen, Kerstin, Keil, Jana, Dursin, Martin, Lenarz, Thomas, and Falk, Christine S.

Subjects
BONE conduction, COCHLEA, DEAF people, PROTEIN microarrays, LIQUID analysis, INNER ear
Abstract

The molecular pathomechanisms in the majority of patients suffering from acute or progressive sensorineural hearing loss cannot be determined yet. The size and the complex architecture of the cochlea make biopsy and in-depth histological analyses impossible without severe damage of the organ. Thus, histopathology correlated to inner disease is only possible after death. The establishment of a technique for perilymph sampling during cochlear implantation may enable a liquid biopsy and characterization of the cochlear microenvironment. Inflammatory processes may not only participate in disease onset and progression in the inner ear, but may also control performance of the implant. However, little is known about cytokines and chemokines in the human inner ear as predictive markers for cochlear implant performance. First attempts to use multiplex protein arrays for inflammatory markers were successful for the identification of cytokines, chemokines, and endothelial markers present in the human perilymph. Moreover, unsupervised cluster and principal component analyses were used to group patients by lead cytokines and to correlate certain proteins to clinical data. Endothelial and epithelial factors were detected at higher concentrations than typical pro-inflammatory cytokines such as TNF-a or IL-6. Significant differences in VEGF family members have been observed comparing patients with deafness to patients with residual hearing with significantly reduced VEGF-D levels in patients with deafness. In addition, there is a trend toward higher IGFBP-1 levels in these patients. Hence, endothelial and epithelial factors in combination with cytokines may present robust biomarker candidates and will be investigated in future studies in more detail. Thus, multiplex protein arrays are feasible in very small perilymph samples allowing a qualitative and quantitative analysis of inflammatory markers. More results are required to advance this method for elucidating the development and course of specific inner ear diseases or for perioperative characterization of cochlear implant patients. [ABSTRACT FROM AUTHOR]

Published
2019
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11. NK Cells of Kidney Transplant Recipients Display an Activated Phenotype that Is Influenced by Immunosuppression and Pathological Staging.

Author

Hoffmann, Ulrike, Neudörfl, Christine, Daemen, Kerstin, Keil, Jana, Stevanovic-Meyer, Maja, Lehner, Frank, Haller, Hermann, Blume, Cornelia, and Falk, Christine S.

Subjects
KILLER cells, KIDNEY transplantation, PHENOTYPES, IMMUNOSUPPRESSION, CYTOKINES
Abstract

To explore phenotype and function of NK cells in kidney transplant recipients, we investigated the peripheral NK cell repertoire, capacity to respond to various stimuli and impact of immunosuppressive drugs on NK cell activity in kidney transplant recipients. CD56dim NK cells of kidney transplanted patients displayed an activated phenotype characterized by significantly decreased surface expression of CD16 (p=0.0003), CD226 (p<0.0001), CD161 (p=0.0139) and simultaneously increased expression of activation markers like HLA-DR (p=0.0011) and CD25 (p=0.0015). Upon in vitro stimulation via Ca++-dependent signals, down-modulation of CD16 was associated with induction of interferon (IFN)-γ expression. CD16 modulation and secretion of NFAT-dependent cytokines such as IFN-γ, TNF-α, IL-10 and IL-31 were significantly suppressed by treatment of isolated NK cells with calcineurin inhibitors but not with mTOR inhibitors. In kidney transplant recipients, IFN-γ production was retained in response to HLA class I-negative target cells and to non-specific stimuli, respectively. However, secretion of other cytokines like IL-13, IL-17, IL-22 and IL-31 was significantly reduced compared to healthy donors. In contrast to suppression of cytokine expression at the transcriptional level, cytotoxin release, i.e. perforin, granzyme A/B, was not affected by immunosuppression in vitro and in vivo in patients as well as in healthy donors. Thus, immunosuppressive treatment affects NK cell function at the level of NFAT-dependent gene expression whereby calcineurin inhibitors primarily impair cytokine secretion while mTOR inhibitors have only marginal effects. Taken together, NK cells may serve as indicators for immunosuppression and may facilitate a personalized adjustment of immunosuppressive medication in kidney transplant recipients. [ABSTRACT FROM AUTHOR]

Published
2015
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12. A systems biological approach suggests that transcriptional feedback regulation by dual-specificity phosphatase 6 shapes extracellular signal-related kinase activity in RAS-transformed fibroblasts.

Author

Blüthgen, Nils, Legewie, Stefan, Kielbasa, Szymon M., Schramme, Anja, Tchernitsa, Oleg, Keil, Jana, Solf, Andrea, Vingron, Martin, Schäfer, Reinhold, Herzel, Hanspeter, and Sers, Christine

Subjects
PHOSPHATASES, MATHEMATICAL models, MITOGEN-activated protein kinases, CELL determination, CELL transformation, SYSTEMS biology
Abstract

Mitogen-activated protein kinase (MAPK) signaling determines crucial cell fate decisions in most cell types, and mediates cellular transformation in many types of cancer. The activity of MAPK is controlled by reversible phosphorylation, and the quantitative characteristics of MAPK activation determine the cellular response. Many systems biological studies have analyzed the activation kinetics and the dose–response behavior of the MAPK signaling pathway. Here we investigate how the pathway activity is controlled by transcriptional feedback loops. Initially, we predict that MAPK signaling regulates phosphatases, by integrating promoter sequence data and ontology-based classification of gene function. From this, we deduce that MAPK signaling might be controlled by transcriptional negative feedback regulation via dual-specificity phosphatases (DUSPs), and implement a mathematical model to further test this hypothesis. Using time-resolved measurements of pathway activity and gene expression, we employ a model selection approach, and select DUSP6 as a highly likely candidate for shaping the activity of the MAPK pathway during cellular transformation caused by oncogenic RAS. Two predictions from the model were confirmed: first, feedback regulation requires that DUSP6 mRNA and protein are unstable; and second, the activation kinetics of MAPK are ultrasensitive. Taken together, an integrated systems biological approach reveals that transcriptional negative feedback controls the kinetics and the extent of MAPK activation under both physiological and pathological conditions. [ABSTRACT FROM AUTHOR]

Published
2009
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13. Leading performance: A moderated mediation analysis at the team level.

Author

Keil, Jana, Rigotti, Thomas, and Otto, Kathleen

Abstract

Fostering team performance is an important leadership function. The underlying processes, however, are not well understood. We approach this question by integrating innovation research principles. Our multi-source study was conducted in two-waves in different German organizations and departments with a total of 609 employees in 84 teams. Regression analyses revealed that two team climate for innovation dimensions, (1) vision and (2) task orientation, mediate the relationship between transformational leadership and one year later team performance. This effect was stronger for teams with low autonomy. In these teams, (3) participative safety was a significant mediator as well. (4) Support for innovation, one of the strongest predictors for innovation, was not significant. Ways to enhance transformational leadership and team climate for innovation dimensions especially under circumstances when team members have little autonomy are discussed. [ABSTRACT FROM AUTHOR]

Published
2017
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14. Immune monitoring after pediatric liver transplantation - the prospective ChilSFree cohort study.

Author

Goldschmidt, Imeke, Karch, André, Mikolajczyk, Rafael, Mutschler, Frauke, Junge, Norman, Pfister, Eva Doreen, Möhring, Tamara, d'Antiga, Lorenzo, McKiernan, Patrick, Kelly, Deirdre, Debray, Dominique, McLin, Valérie, Pawlowska, Joanna, Hierro, Loreto, Daemen, Kerstin, Keil, Jana, Falk, Christine, and Baumann, Ulrich

Subjects
IMMUNOSUPPRESSIVE agents, TRANSPLANTATION of organs, tissues, etc., IMMUNOSUPPRESSION, HOMEOSTASIS, LIVER transplantation, IMMUNE response, CHRONIC kidney failure, BIOPSY, CHEMOKINES, COMPARATIVE studies, CYTOKINES, GRAFT rejection, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, POSTOPERATIVE period, RESEARCH, RESEARCH funding, EVALUATION research, VASCULAR endothelial growth factors, SURGERY
Abstract

Background: Although trough levels of immunosuppressive drugs are largely used to monitor immunosuppressive therapy after solid organ transplantation, there is still no established tool that allows for a validated assessment of functional degree of immunosuppression or the identification of clinically relevant over- or under-immunosuppression, depending on graft homeostasis. Reliable non-invasive markers to predict biopsy proven acute rejection (BPAR) do not exist. Literature data suggest that longitudinal measurements of immune markers might be predictive of BPAR, but data in children are scarce. We therefore propose an observational prospective cohort study focusing on immune monitoring in children after liver transplantation. We aim to describe immune function in a cohort of children before and during the first year after liver transplantation and plan to investigate how the immune function profile is associated with clinical and laboratory findings.Methods: In an international multicenter prospective approach, children with end-stage liver disease who undergo liver transplantation are enrolled to the study and receive extensive immune monitoring before and at 1, 2, 3, 4 weeks and 3, 6, 12 months after transplantation, and whenever a clinically indicated liver biopsy is scheduled. Blood samples are analyzed for immune cell numbers and circulating levels of cytokines, chemokines and factors of angiogenesis reflecting immune cell activation. Statistical analysis will focus on the identification of trajectorial patterns of immune reactivity predictive for systemic non-inflammatory states, infectious complications or BPAR using joint modelling approaches.Discussion: The ChilSFree study will help to understand the immune response after pLTx in different states of infection or rejection. It may provide insight into response mechanisms eventually facilitating immune tolerance towards the graft. Our analysis may yield an applicable immune panel for non-invasive early detection of acute cellular rejection, with the prospect of individually tailoring immunosuppressive therapy. The international collaborative set-up of this study allows for an appropriate sample size which is otherwise difficult to achieve in the field of pediatric liver transplantation. [ABSTRACT FROM AUTHOR]

Published
2018
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