Your search keyword '"Bettina Wiegmann"' showing total 4 results

1. CD14highCD16+ monocytes are the main producers of Interleukin-10 following clinical heart transplantation

Author

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

Subjects

heart transplantation, organ transplantation, ischemia-reperfusion injury, interleukin-10, monocytes, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionFollowing 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.MethodsWe 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 discussionWe 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.

Published

2023

2. Pushing the boundaries of innovation: the potential of ex vivo organ perfusion from an interdisciplinary point of view

Author

Jasper Iske, Andreas Schroeter, Samuel Knoedler, Timo Z. Nazari-Shafti, Leonard Wert, Maximilian J. Roesel, Felix Hennig, Adelheid Niehaus, Christian Kuehn, Fabio Ius, Volkmar Falk, Moritz Schmelzle, Arjang Ruhparwar, Axel Haverich, Christoph Knosalla, Stefan G. Tullius, Florian W. R. Vondran, and Bettina Wiegmann

Subjects

transplantation, transplantation heart, ex vivo organ perfusion, machine perfusion, ex vivo machine perfusion, organ modification, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Ex vivo machine perfusion (EVMP) is an emerging technique for preserving explanted solid organs with primary application in allogeneic organ transplantation. EVMP has been established as an alternative to the standard of care static-cold preservation, allowing for prolonged preservation and real-time monitoring of organ quality while reducing/preventing ischemia–reperfusion injury. Moreover, it has paved the way to involve expanded criteria donors, e.g., after circulatory death, thus expanding the donor organ pool. Ongoing improvements in EVMP protocols, especially expanding the duration of preservation, paved the way for its broader application, in particular for reconditioning and modification of diseased organs and tumor and infection therapies and regenerative approaches. Moreover, implementing EVMP for in vivo-like preclinical studies improving disease modeling raises significant interest, while providing an ideal interface for bioengineering and genetic manipulation. These approaches can be applied not only in an allogeneic and xenogeneic transplant setting but also in an autologous setting, where patients can be on temporary organ support while the diseased organs are treated ex vivo, followed by reimplantation of the cured organ. This review provides a comprehensive overview of the differences and similarities in abdominal (kidney and liver) and thoracic (lung and heart) EVMP, focusing on the organ-specific components and preservation techniques, specifically on the composition of perfusion solutions and their supplements and perfusion temperatures and flow conditions. Novel treatment opportunities beyond organ transplantation and limitations of abdominal and thoracic EVMP are delineated to identify complementary interdisciplinary approaches for the application and development of this technique.

Published

2023

3. Trends, Advantages and Disadvantages in Combined Extracorporeal Lung and Kidney Support From a Technical Point of View

Author

Ana Martins Costa, Frank Halfwerk, Bettina Wiegmann, Michael Neidlin, and Jutta Arens

Subjects

veno-venous ECMO, continuous RRT, extracorporeal life support, artificial kidney, artificial lung, artificial organ, Medical technology, R855-855.5

Abstract

Extracorporeal membrane oxygenation (ECMO) provides pulmonary and/or cardiac support for critically ill patients. Due to their diseases, they are at high risk of developing acute kidney injury. In that case, continuous renal replacement therapy (CRRT) is applied to provide renal support and fluid management. The ECMO and CRRT circuits can be combined by an integrated or parallel approach. So far, all methods used for combined extracorporeal lung and kidney support present serious drawbacks. This includes not only high risks of circuit related complications such as bleeding, thrombus formation, and hemolysis, but also increase in technical workload and health care costs. In this sense, the development of a novel optimized artificial lung device with integrated renal support could offer important treatment benefits. Therefore, we conducted a review to provide technical background on existing techniques for extracorporeal lung and kidney support and give insight on important aspects to be addressed in the development of this novel highly integrated artificial lung device.

Published

2022

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

Author

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

Subjects

lung transplantation, passenger leukocytes, NK cells, T cells, killer cell immunoglobulin-like receptor, primary graft dysfunction, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionFor 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.MethodsPeripheral 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.ResultsWithin 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

Published

2021