Your search keyword '"Pawel Durek"' showing total 111 results

1. Group 2 innate lymphoid cells are a non-redundant source of interleukin-5 required for development and function of murine B1 cells

Author

Karoline F. Troch, Manuel O. Jakob, Patrycja M. Forster, Katja J. Jarick, Jonathan Schreiber, Alexandra Preusser, Gabriela M. Guerra, Pawel Durek, Caroline Tizian, Nele Sterczyk, Sofia Helfrich, Claudia U. Duerr, David Voehringer, Mario Witkowski, David Artis, Tim Rollenske, Andrey A. Kruglov, Mir-Farzin Mashreghi, and Christoph S. N. Klose

Subjects

Science

Abstract

Abstract Tissue-resident immune cells, such as innate lymphoid cells, mediate protective or detrimental immune responses at barrier surfaces. Upon activation by stromal or epithelial cell-derived alarmins, group 2 innate lymphoid cells (ILC2s) are a rapid source of type 2 cytokines, such as IL-5. However, due to the overlap in effector functions, it remains unresolved whether ILC2s are an essential component of the type 2 response or whether their function can be compensated by other cells, such as T cells. Here we show a non-redundant role of ILC2s in supporting the development and function of B1 cells. We demonstrate that B1 cells fail to develop properly in the absence of ILC2s and identify the IL-33 receptor on ILC2s as an essential cell-intrinsic regulator of IL-5 production. Further, conditional deletion of Il5 in ILC2s results in defective B1 cell development and immunoglobulin production. Consequently, B1 cells with phosphatidylcholine specific B cell receptor rearrangements are diminished in ILC2-deficient mice. Thus, our data establish an essential function of ILC2s in supporting B1 cells and antibody production at barrier surfaces.

Published

2024

2. Recruitment of plasma cells from IL-21-dependent and IL-21-independent immune reactions to the bone marrow

Author

Marta Ferreira-Gomes, Yidan Chen, Pawel Durek, Hector Rincon-Arevalo, Frederik Heinrich, Laura Bauer, Franziska Szelinski, Gabriela Maria Guerra, Ana-Luisa Stefanski, Antonia Niedobitek, Annika Wiedemann, Marina Bondareva, Jacob Ritter, Katrin Lehmann, Sebastian Hardt, Christian Hipfl, Sascha Hein, Eberhard Hildt, Mareen Matz, Henrik E. Mei, Qingyu Cheng, Van Duc Dang, Mario Witkowski, Andreia C. Lino, Andrey Kruglov, Fritz Melchers, Carsten Perka, Eva V. Schrezenmeier, Andreas Hutloff, Andreas Radbruch, Thomas Dörner, and Mir-Farzin Mashreghi

Subjects

Science

Abstract

Abstract Bone marrow plasma cells (BMPC) are the correlate of humoral immunity, consistently releasing antibodies into the bloodstream. It remains unclear if BMPC reflect different activation environments or maturation of their precursors. Here we define human BMPC heterogeneity and track the recruitment of antibody-secreting cells (ASC) from SARS-CoV-2 vaccine immune reactions to the bone marrow (BM). Trajectories based on single-cell transcriptomes and repertoires of peripheral and BM ASC reveal sequential colonisation of BMPC compartments. In activated B cells, IL-21 suppresses CD19 expression, indicating that CD19low-BMPC are derived from follicular, while CD19high-BMPC originate from extrafollicular immune reactions. In primary immune reactions, both CD19low- and CD19high-BMPC compartments are populated. In secondary immune reactions, most BMPC are recruited to CD19high-BMPC compartments, reflecting their origin from extrafollicular reactivations of memory B cells. A pattern also observable in vaccinated-convalescent individuals and upon diphtheria/tetanus/pertussis recall-vaccination. Thus, BMPC diversity reflects the evolution of a given humoral immune response.

Published

2024

3. The miR-221/222 cluster regulates hematopoietic stem cell quiescence and multipotency by suppressing both Fos/AP-1/IEG pathway activation and stress-like differentiation to granulocytes.

Author

Peter K Jani, Georg Petkau, Yohei Kawano, Uwe Klemm, Gabriela Maria Guerra, Gitta Anne Heinz, Frederik Heinrich, Pawel Durek, Mir-Farzin Mashreghi, and Fritz Melchers

Subjects

Biology (General), QH301-705.5

Abstract

Throughout life, hematopoietic stem cells (HSCs), residing in bone marrow (BM), continuously regenerate erythroid/megakaryocytic, myeloid, and lymphoid cell lineages. This steady-state hematopoiesis from HSC and multipotent progenitors (MPPs) in BM can be perturbed by stress. The molecular controls of how stress can impact hematopoietic output remain poorly understood. MicroRNAs (miRNAs) as posttranscriptional regulators of gene expression have been found to control various functions in hematopoiesis. We find that the miR-221/222 cluster, which is expressed in HSC and in MPPs differentiating from them, perturbs steady-state hematopoiesis in ways comparable to stress. We compare pool sizes and single-cell transcriptomes of HSC and MPPs in unperturbed or stress-perturbed, miR-221/222-proficient or miR-221/222-deficient states. MiR-221/222 deficiency in hematopoietic cells was induced in C57BL/6J mice by conditional vav-cre-mediated deletion of the floxed miR-221/222 gene cluster. Social stress as well as miR-221/222 deficiency, alone or in combination, reduced HSC pools 3-fold and increased MPPs 1.5-fold. It also enhanced granulopoisis in the spleen. Furthermore, combined stress and miR-221/222 deficiency increased the erythroid/myeloid/granulocytic precursor pools in BM. Differential expression analyses of single-cell RNAseq transcriptomes of unperturbed and stressed, proficient HSC and MPPs detected more than 80 genes, selectively up-regulated in stressed cells, among them immediate early genes (IEGs). The same differential single-cell transcriptome analyses of unperturbed, miR-221/222-proficient with deficient HSC and MPPs identified Fos, Jun, JunB, Klf6, Nr4a1, Ier2, Zfp36-all IEGs-as well as CD74 and Ly6a as potential miRNA targets. Three of them, Klf6, Nr4a1, and Zfp36, have previously been found to influence myelogranulopoiesis. Together with increased levels of Jun, Fos forms increased amounts of the heterodimeric activator protein-1 (AP-1), which is known to control the expression of the selectively up-regulated expression of the IEGs. The comparisons of single-cell mRNA-deep sequencing analyses of socially stressed with miR-221/222-deficient HSC identify 5 of the 7 Fos/AP-1-controlled IEGs, Ier2, Jun, Junb, Klf6, and Zfp36, as common activators of HSC from quiescence. Combined with stress, miR-221/222 deficiency enhanced the Fos/AP-1/IEG pathway, extended it to MPPs, and increased the number of granulocyte precursors in BM, inducing selective up-regulation of genes encoding heat shock proteins Hspa5 and Hspa8, tubulin-cytoskeleton-organizing proteins Tuba1b, Tubb 4b and 5, and chromatin remodeling proteins H3f3b, H2afx, H2afz, and Hmgb2. Up-regulated in HSC, MPP1, and/or MPP2, they appear as potential regulators of stress-induced, miR-221/222-dependent increased granulocyte differentiation. Finally, stress by serial transplantations of miR-221/222-deficient HSC selectively exhausted their lymphoid differentiation capacities, while retaining their ability to home to BM and to differentiate to granulocytes. Thus, miR-221/222 maintains HSC quiescence and multipotency by suppressing Fos/AP-1/IEG-mediated activation and by suppressing enhanced stress-like differentiation to granulocytes. Since miR-221/222 is also expressed in human HSC, controlled induction of miR-221/222 in HSC should improve BM transplantations.

Published

2023

4. Distinct tissue niches direct lung immunopathology via CCL18 and CCL21 in severe COVID-19

Author

Ronja Mothes, Anna Pascual-Reguant, Ralf Koehler, Juliane Liebeskind, Alina Liebheit, Sandy Bauherr, Lars Philipsen, Carsten Dittmayer, Michael Laue, Regina von Manitius, Sefer Elezkurtaj, Pawel Durek, Frederik Heinrich, Gitta A. Heinz, Gabriela M. Guerra, Benedikt Obermayer, Jenny Meinhardt, Jana Ihlow, Josefine Radke, Frank L. Heppner, Philipp Enghard, Helena Stockmann, Tom Aschman, Julia Schneider, Victor M. Corman, Leif E. Sander, Mir-Farzin Mashreghi, Thomas Conrad, Andreas C. Hocke, Raluca A. Niesner, Helena Radbruch, and Anja E. Hauser

Subjects

Science

Abstract

Infection with SARS-CoV-2 has been linked with substantive inflammation, lung pathology and development of COVID-19. Here the authors spatially associate CCL18 and CCL21 in distinct tissue niches with lung pathology of severe COVID-19.

Published

2023

5. Questioning whether IgM Fc receptor (FcµR) is expressed by innate immune cells

Author

Christopher M. Skopnik, René Riedel, Richard K. Addo, Gitta Anne Heinz, Frederik Heinrich, Kazuhito Honjo, Pawel Durek, Philipp Enghard, Mir-Farzin Mashreghi, Andreas Radbruch, and Hiromi Kubagawa

Subjects

Science

Published

2022

6. Flow cytometry can reliably capture gut microbial composition in healthy adults as well as dysbiosis dynamics in patients with aggressive B-cell non-Hodgkin lymphoma

Author

Maren Schmiester, René Maier, René Riedel, Pawel Durek, Marco Frentsch, Stefan Kolling, Mir-Farzin Mashreghi, Robert Jenq, Liangliang Zhang, Christine B. Peterson, Lars Bullinger, Hyun-Dong Chang, and Il-Kang Na

Subjects

Flow cytmetry, microbiome, B-cell non-Hodgkin lymphoma, longitudinal, dysbiosis, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Modulation of commensal gut microbiota is increasingly recognized as a promising strategy to reduce mortality in patients with malignant diseases, but monitoring for dysbiosis is generally not routine clinical practice due to equipment, expertise and funding required for sequencing analysis. A low-threshold alternative is microbial diversity profiling by single-cell flow cytometry (FCM), which we compared to 16S rRNA sequencing in human fecal samples and employed to characterize longitudinal changes in the microbiome composition of patients with aggressive B-cell non-Hodgkin lymphoma undergoing chemoimmunotherapy. Diversity measures obtained from both methods were correlated and captured identical trends in microbial community structures, finding no difference in patients’ pretreatment alpha or beta diversity compared to healthy controls and a significant and progressive loss of alpha diversity during chemoimmunotherapy. Our results highlight the potential of FCM-based microbiome profiling as a reliable and accessible diagnostic tool that can provide novel insights into cancer therapy-associated dysbiosis dynamics.

Published

2022

7. Optimization of chondrocyte isolation from human articular cartilage to preserve the chondrocyte transcriptome

Author

Ping Shen, Peihua Wu, Tazio Maleitzke, Marie-Jacqueline Reisener, Gitta A. Heinz, Frederik Heinrich, Pawel Durek, Clemens Gwinner, Tobias Winkler, Matthias Pumberger, Carsten Perka, Mir-Farzin Mashreghi, and Max Löhning

Subjects

chondrocyte isolation, human articular cartilage, small chondrocytes, large chondrocytes, transcriptome preservation, single-cell RNA sequencing, Biotechnology, TP248.13-248.65

Abstract

The isolation of chondrocytes from human articular cartilage for single-cell RNA sequencing requires extensive and prolonged tissue digestion at 37 C. Modulations of the transcriptional activity likely take place during this period such that the transcriptomes of isolated human chondrocytes no longer match their original status in vivo. Here, we optimized the human chondrocyte isolation procedure to maximally preserve the in vivo transcriptome. Cartilage tissues were transferred into a hypoxia chamber (4% O2) immediately after being removed from OA patients and minced finely. Collagenase II at concentrations of 0.02%, 0.1%, 0.25%, 0.5%, 1%, and 2% was applied for 0.5, 1, 2, 4, and 18 h to digest the minced tissue. Actinomycin D (ActD) was added to test its capacity in stabilizing the transcriptome. Cell yield, viability, cell size, and transcriptome were determined using counter chamber, flow cytometry, and RNA sequencing (RNA-seq). Collagenase II at 2% concentration released small chondrocytes from cartilage matrix during the first digestion hour and started to release large cells thereafter, reaching a complete release at 4 h. During 4-h digestions, collagenase II at 2% and 1% but not at lower concentrations yielded maximal release also of the large chondrocyte population. RNA-seq analysis revealed that a 4-h digestion period with 1% or 2% collagenase II plus Actinomycin D optimally preserved the transcriptome. Thus, this study provides an isolation protocol for single chondrocytes from human articular cartilage optimized for transcriptome preservation and RNA-seq analysis.

Published

2022

8. SARS-CoV-2 in severe COVID-19 induces a TGF-β-dominated chronic immune response that does not target itself

Author

Marta Ferreira-Gomes, Andrey Kruglov, Pawel Durek, Frederik Heinrich, Caroline Tizian, Gitta Anne Heinz, Anna Pascual-Reguant, Weijie Du, Ronja Mothes, Chaofan Fan, Stefan Frischbutter, Katharina Habenicht, Lisa Budzinski, Justus Ninnemann, Peter K. Jani, Gabriela Maria Guerra, Katrin Lehmann, Mareen Matz, Lennard Ostendorf, Lukas Heiberger, Hyun-Dong Chang, Sandy Bauherr, Marcus Maurer, Günther Schönrich, Martin Raftery, Tilmann Kallinich, Marcus Alexander Mall, Stefan Angermair, Sascha Treskatsch, Thomas Dörner, Victor Max Corman, Andreas Diefenbach, Hans-Dieter Volk, Sefer Elezkurtaj, Thomas H. Winkler, Jun Dong, Anja Erika Hauser, Helena Radbruch, Mario Witkowski, Fritz Melchers, Andreas Radbruch, and Mir-Farzin Mashreghi

Subjects

Science

Abstract

Our understanding on the humoral immunity induced by SARS-CoV-2 is still lacking. Here the authors analyze B cell responses at the single cell level to find that, in severe COVID-19 patients, plasmablasts shift from IFN to TGFβ instruction to produce IgA antibodies that are not specific to dominant SARS-CoV-2 antigens.

Published

2021

9. Discrete populations of isotype-switched memory B lymphocytes are maintained in murine spleen and bone marrow

Author

René Riedel, Richard Addo, Marta Ferreira-Gomes, Gitta Anne Heinz, Frederik Heinrich, Jannis Kummer, Victor Greiff, Daniel Schulz, Cora Klaeden, Rebecca Cornelis, Ulrike Menzel, Stefan Kröger, Ulrik Stervbo, Ralf Köhler, Claudia Haftmann, Silvia Kühnel, Katrin Lehmann, Patrick Maschmeyer, Mairi McGrath, Sandra Naundorf, Stefanie Hahne, Özen Sercan-Alp, Francesco Siracusa, Jonathan Stefanowski, Melanie Weber, Kerstin Westendorf, Jakob Zimmermann, Anja E. Hauser, Sai T. Reddy, Pawel Durek, Hyun-Dong Chang, Mir-Farzin Mashreghi, and Andreas Radbruch

Subjects

Science

Abstract

Memory B cells are important for protecting the host from pathogen rechallenge, but their properties and locations remain ill-defined. Here the authors show, using single-cell transcriptomics and repertoire analyses, that mouse spleen and bone marrow host distinct populations of isotype-switched memory B cells to potentially optimize for rapid recall responses.

Published

2020

10. Prevention of EAE by tolerogenic vaccination with PEGylated antigenic peptides

Author

Jennifer Pfeil, Mario Simonetti, Uta Lauer, Bianca von Thülen, Pawel Durek, Christina Poulsen, Justyna Pawlowska, Matthias Kröger, Ralf Krähmer, Frank Leenders, Ute Hoffmann, and Alf Hamann

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Background: Therapeutic treatment options for chronic autoimmune disorders such as multiple sclerosis (MS) rely largely on the use of non-specific immunosuppressive drugs, which are not able to cure the disease. Presently, approaches to induce antigen-specific tolerance as a therapeutic approach; for example, by peptide-based tolerogenic ‘inverse’ vaccines have regained great interest. We have previously shown that coupling of peptides to carriers can enhance their capacity to induce regulatory T cells in vivo . Method: In this present study, we investigated whether the tolerogenic potential of immunodominant myelin T-cell epitopes can be improved by conjugation to the synthetic carrier polyethylene glycol (PEG) in an experimental autoimmune encephalomyelitis (EAE) mouse model for chronic MS (MOG C57BL/6). Results: Preventive administration of the PEGylated antigenic peptide could strongly suppress the development of EAE, accompanied by reduced immune cell infiltration in the central nervous system (CNS). Depletion of regulatory T cells (Tregs) abrogated the protective effect indicating that Tregs play a crucial role in induction of antigen-specific tolerance in EAE. Treatment during the acute phase of disease was safe and did not induce immune activation. However, treatment at the peak of disease did not affect the disease course, suggesting that either induction of Tregs does not occur in the highly inflamed situation, or that the immune system is refractory to regulation in this condition. Conclusion: PEGylation of antigenic peptides is an effective and feasible strategy to improve tolerogenic (Treg-inducing) peptide-based vaccines, but application for immunotherapy of overt disease might require modifications or combination therapies that simultaneously suppress effector mechanisms.

Published

2021

11. Tolerogenic Immunomodulation by PEGylated Antigenic Peptides

Author

Jennifer Pfeil, Mario Simonetti, Uta Lauer, Rudolf Volkmer, Bianca von Thülen, Pawel Durek, Ralf Krähmer, Frank Leenders, Alf Hamann, and Ute Hoffmann

Subjects

immune tolerance, autoimmunity, peptide vaccination, nanoparticles, regulatory T cells, Immunologic diseases. Allergy, RC581-607

Abstract

Current treatments for autoimmune disorders rely on non-specific immunomodulatory and global immunosuppressive drugs, which show a variable degree of efficiency and are often accompanied by side effects. In contrast, strategies aiming at inducing antigen-specific tolerance promise an exclusive specificity of the immunomodulation. However, although successful in experimental models, peptide-based tolerogenic “inverse” vaccines have largely failed to show efficacy in clinical trials. Recent studies showed that repetitive T cell epitopes, coupling of peptides to autologous cells, or peptides coupled to nanoparticles can improve the tolerogenic efficacy of peptides, suggesting that size and biophysical properties of antigen constructs affect the induction of tolerance. As these materials bear hurdles with respect to preparation or regulatory aspects, we wondered whether conjugation of peptides to the well-established and clinically proven synthetic material polyethylene glycol (PEG) might also work. We here coupled the T cell epitope OVA323–339 to polyethylene glycols of different size and structure and tested the impact of these nano-sized constructs on regulatory (Treg) and effector T cells in the DO11.10 adoptive transfer mouse model. Systemic vaccination with PEGylated peptides resulted in highly increased frequencies of Foxp3+ Tregs and reduced frequencies of antigen-specific T cells producing pro-inflammatory TNF compared to vaccination with the native peptide. PEGylation was found to extend the bioavailability of the model peptide. Both tolerogenicity and bioavailability were dependent on PEG size and structure. In conclusion, PEGylation of antigenic peptides is an effective and feasible strategy to improve Treg-inducing, peptide-based vaccines with potential use for the treatment of autoimmune diseases, allergies, and transplant rejection.

Published

2020

12. Stromal Cell-Contact Dependent PI3K and APRIL Induced NF-κB Signaling Prevent Mitochondrial- and ER Stress Induced Death of Memory Plasma Cells

Author

Rebecca Cornelis, Stefanie Hahne, Adriano Taddeo, Georg Petkau, Darya Malko, Pawel Durek, Manja Thiem, Lukas Heiberger, Lena Peter, Elodie Mohr, Cora Klaeden, Koji Tokoyoda, Francesco Siracusa, Bimba Franziska Hoyer, Falk Hiepe, Mir-Farzin Mashreghi, Fritz Melchers, Hyun-Dong Chang, and Andreas Radbruch

Subjects

long-lived memory PCs, bone marrow, stromal cell, FoxO, APRIL, PI3K/AKT, Biology (General), QH301-705.5

Abstract

Summary: The persistence of long-lived memory plasma cells in the bone marrow depends on survival factors available in the bone marrow, which are provided in niches organized by stromal cells. Using an ex vivo system in which we supply the known survival signals, direct cell contact to stromal cells, and the soluble cytokine a proliferation-inducing ligand (APRIL), we have elucidated the critical signaling pathways required for the survival of long-lived plasma cells. Integrin-mediated contact of bone marrow plasma cells with stromal cells activates the phosphatidylinositol 3-kinase (PI3K) signaling pathway, leading to critical inactivation of Forkhead-Box-Protein O1/3 (FoxO1/3) and preventing the activation of mitochondrial stress-associated effector caspases 3 and 7. Accordingly, inhibition of PI3K signaling in vivo ablates bone marrow plasma cells. APRIL signaling, by the nuclear factor κB (NF-κB) pathway, blocks activation of the endoplasmic-reticulum-stress-associated initiator caspase 12. Thus, stromal-cell-contact-induced PI3K and APRIL-induced NF-κB signaling provide the necessary and complementary signals to maintain bone marrow memory plasma cells.

Published

2020

13. Deep Phenotyping of Urinary Leukocytes by Mass Cytometry Reveals a Leukocyte Signature for Early and Non-Invasive Prediction of Response to Treatment in Active Lupus Nephritis

Author

Martina Bertolo, Sabine Baumgart, Pawel Durek, Anette Peddinghaus, Henrik Mei, Thomas Rose, Philipp Enghard, and Andreas Grützkau

Subjects

systemic lupus – erythematosus, lupus nephritis, lupus nephritis biomarker, mass cytometry, urinary leukocytes, Immunologic diseases. Allergy, RC581-607

Abstract

Non-invasive biomarkers are necessary for diagnosis and monitoring disease activity in lupus nephritis (LN) to circumvent risks and limitations of renal biopsies. To identify new non-invasive cellular biomarkers in the urine sediment of LN patients, which may reflect kidney inflammation and can be used to predict treatment outcome, we performed in-depth urinary immune cell profiling by mass cytometry. We established a mass cytometric workflow to comparatively analyze the cellular composition of urine and peripheral blood (PB) in 13 patients with systemic lupus erythematosus (SLE) with active, biopsy-proven proliferative LN. Clinical and laboratory data were collected at the time of sampling and 6 months after induction of therapy in order to evaluate the clinical response of each patient. Six patients with different acute inflammatory renal diseases were included as comparison group. Leukocyte phenotypes and composition differed significantly between urine and paired PB samples. In urine, neutrophils and monocytes/macrophages were identified as the most prominent cell populations comprising together about 30%–83% of nucleated cells, while T and B lymphocytes, eosinophils, and natural killer (NK) cells were detectable at frequencies of

Published

2020

14. DNA copy number changes define spatial patterns of heterogeneity in colorectal cancer

Author

Soulafa Mamlouk, Liam Harold Childs, Daniela Aust, Daniel Heim, Friederike Melching, Cristiano Oliveira, Thomas Wolf, Pawel Durek, Dirk Schumacher, Hendrik Bläker, Moritz von Winterfeld, Bastian Gastl, Kerstin Möhr, Andrea Menne, Silke Zeugner, Torben Redmer, Dido Lenze, Sascha Tierling, Markus Möbs, Wilko Weichert, Gunnar Folprecht, Eric Blanc, Dieter Beule, Reinhold Schäfer, Markus Morkel, Frederick Klauschen, Ulf Leser, and Christine Sers

Subjects

Science

Abstract

The contribution of intra-tumour heterogeneity is increasingly associated with resistance to therapy. Here, the authors use genomic analyses to study heterogeneity in colorectal cancer and perform in-depth reconstruction of heterogeneity in one sample.

Published

2017

15. MicroRNA-31 Reduces the Motility of Proinflammatory T Helper 1 Lymphocytes

Author

Markus Bardua, Claudia Haftmann, Pawel Durek, Kerstin Westendorf, Antje Buttgereit, Cam Loan Tran, Mairi McGrath, Melanie Weber, Katrin Lehmann, Richard Kwasi Addo, Gitta Anne Heinz, Anna-Barbara Stittrich, Patrick Maschmeyer, Helena Radbruch, Michael Lohoff, Hyun-Dong Chang, Andreas Radbruch, and Mir-Farzin Mashreghi

Subjects

CD4, miR-31, miRNA, target identification, T cell migration, Th1 cells, Immunologic diseases. Allergy, RC581-607

Abstract

Proinflammatory type 1 T helper (Th1) cells are enriched in inflamed tissues and contribute to the maintenance of chronic inflammation in rheumatic diseases. Here we show that the microRNA- (miR-) 31 is upregulated in murine Th1 cells with a history of repeated reactivation and in memory Th cells isolated from the synovial fluid of patients with rheumatic joint disease. Knock-down of miR-31 resulted in the upregulation of genes associated with cytoskeletal rearrangement and motility and induced the expression of target genes involved in T cell activation, chemokine receptor– and integrin-signaling. Accordingly, inhibition of miR-31 resulted in increased migratory activity of repeatedly activated Th1 cells. The transcription factors T-bet and FOXO1 act as positive and negative regulators of T cell receptor (TCR)–mediated miR-31 expression, respectively. Taken together, our data show that a gene regulatory network involving miR-31, T-bet, and FOXO1 controls the migratory behavior of proinflammatory Th1 cells.

Published

2018

16. Inhibition or Stimulation of Ochratoxin A Synthesis on Inoculated Barley Triggered by Diffuse Coplanar Surface Barrier Discharge Plasma

Author

Julia Durek, Oliver Schlüter, Anne Roscher, Pawel Durek, and Antje Fröhling

Subjects

mycotoxin, ochratoxin A, Aspergillus niger, Penicillium verrucosum, cold atmospheric plasma, mold inhibition, Microbiology, QR1-502

Abstract

Ochratoxin A (OTA) is one of the most abundant food-contaminating mycotoxins. Besides their high toxicity, mycotoxins are highly stable to physical, chemical or biological detoxification. Therefore, the treatment with cold atmospheric plasma could be one approach to reduce the amount of mycotoxins in different products. The aim of this study was to determine the influence of cold atmospheric plasma on the inactivation of Aspergillus niger and Penicillium verrucosum inoculated on barley and their production of OTA. Inoculated barley was treated with plasma generated by dry air, CO2 or CO2 + O2 for 1 or 3 min and stored for up to two weeks at 9, 25, or 37°C. Three minutes of air plasma treatment effectively significantly reduced the total mold count of both microorganisms by 2.5–3 log cycles. The production of OTA from A. niger was only low, therefore the treatment effect was indistinguishable. The treatment of P. verrucosum on barley after an incubation of five days using a CO2 + O2 plasma resulted in a reduction of the OTA content from 49.0 (untreated) to 27.5 (1 min) and 23.8 ng/g (3 min), respectively. In contrast, CO2 plasma caused an increase of the OTA amount from 49.0 (untreated) to 55.8 (1 min) and 72.9 ng/g (3 min). Finally, the use of air plasma resulted likewise in a decrease of the OTA concentration from 56.9 (untreated) to 25.7 (1 min) and 20.2 ng/g (3 min), respectively. Reducing the incubation time before the treatment to 24 h caused in contrast an increase of the OTA content from 3.1 (untreated) to 29.1 (1 min) and 20.7 ng/g (3 min). Due to the high standard deviation, these changes were not significant, but the tendencies were clearly visible, showing the strong impact of the plasma gas on the OTA production. The results show, that even if the total mold count was reduced, under certain conditions the OTA amount was yet enhanced, probably due to a stress reaction of the mold. Concluding, the plasma gas and incubation conditions have to be considered to allow a successful inactivation of molds and in particular their toxic metabolites.

Published

2018

17. MicroRNA regulation in blood cells of renal transplanted patients with interstitial fibrosis/tubular atrophy and antibody-mediated rejection.

Author

Mareen Matz, Frederik Heinrich, Christine Lorkowski, Kaiyin Wu, Jens Klotsche, Qiang Zhang, Nils Lachmann, Pawel Durek, Klemens Budde, and Mir-Farzin Mashreghi

Subjects

Medicine, Science

Abstract

Interstitial fibrosis/tubular atrophy (IFTA) is associated with reduced allograft survival, whereas antibody-mediated rejection (ABMR) is the major cause for renal allograft failure. To identify specific microRNAs and their regulation involved in these processes, total RNA from blood cells of 16 kidney transplanted (KTx) patients with ABMR, stable graft function (SGF) and with T-cell mediated rejection (TCMR) was isolated. MicroRNA expression was determined by high-throughput sequencing. Differentially expressed candidate microRNAs were analyzed with RT-PCR in patients with SGF (n = 53), urinary tract infection (UTI) (n = 17), borderline rejection (BL) (n = 19), TCMR (n = 40), ABMR (n = 22) and IFTA (n = 30). From the 301 detected microRNAs, 64 were significantly regulated between the three cohorts. Selected candidate microRNAs miR-223-3p, miR-424-3p and miR-145-5p distinguished TCMR and ABMR from SGF, but not from other pathologies. Most importantly, miR-145-5p expression in IFTA patients was significantly downregulated and displayed a high diagnostic accuracy compared to SGF alone (AUC = 0.891) and compared to SGF, UTI, BL, TCMR and ABMR patients combined (AUC = 0.835), which was verified by cross-validation. The identification of miR-145-5p as IFTA specific marker in blood constitutes the basis for evaluating this potentially diagnostic microRNA as biomarker in studies including high numbers of patients and different pathologies and also the further analysis of fibrosis causing etiologies after kidney transplantation.

Published

2018

18. Network quantification of EGFR signaling unveils potential for targeted combination therapy

Author

Bertram Klinger, Anja Sieber, Raphaela Fritsche‐Guenther, Franziska Witzel, Leanne Berry, Dirk Schumacher, Yibing Yan, Pawel Durek, Mark Merchant, Reinhold Schäfer, Christine Sers, and Nils Blüthgen

Subjects

cancer, EGFR signaling, mathematical modeling, modular response analysis, signal transduction, Biology (General), QH301-705.5, Medicine (General), R5-920

Abstract

Abstract The epidermal growth factor receptor (EGFR) signaling network is activated in most solid tumors, and small‐molecule drugs targeting this network are increasingly available. However, often only specific combinations of inhibitors are effective. Therefore, the prediction of potent combinatorial treatments is a major challenge in targeted cancer therapy. In this study, we demonstrate how a model‐based evaluation of signaling data can assist in finding the most suitable treatment combination. We generated a perturbation data set by monitoring the response of RAS/PI3K signaling to combined stimulations and inhibitions in a panel of colorectal cancer cell lines, which we analyzed using mathematical models. We detected that a negative feedback involving EGFR mediates strong cross talk from ERK to AKT. Consequently, when inhibiting MAPK, AKT activity is increased in an EGFR‐dependent manner. Using the model, we predict that in contrast to single inhibition, combined inactivation of MEK and EGFR could inactivate both endpoints of RAS, ERK and AKT. We further could demonstrate that this combination blocked cell growth in BRAF‐ as well as KRAS‐mutated tumor cells, which we confirmed using a xenograft model.

Published

2013

19. Human cytomegalovirus drives epigenetic imprinting of the IFNG locus in NKG2Chi natural killer cells.

Author

Merlin Luetke-Eversloh, Quirin Hammer, Pawel Durek, Karl Nordström, Gilles Gasparoni, Matthias Pink, Alf Hamann, Jörn Walter, Hyun-Dong Chang, Jun Dong, and Chiara Romagnani

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Memory type 1 T helper (T(H)1) cells are characterized by the stable expression of interferon (IFN)-γ as well as by the epigenetic imprinting of the IFNG locus. Among innate cells, NK cells play a crucial role in the defense against cytomegalovirus (CMV) and represent the main source of IFN-γ. Recently, it was shown that memory-like features can be observed in NK cell subsets after CMV infection. However, the molecular mechanisms underlying NK cell adaptive properties have not been completely defined. In the present study, we demonstrated that only NKG2Chi NK cells expanded in human CMV (HCMV) seropositive individuals underwent epigenetic remodeling of the IFNG conserved non-coding sequence (CNS) 1, similar to memory CD8(+) T cells or T(H)1 cells. The accessibility of the CNS1 was required to enhance IFN-γ transcriptional activity in response to NKG2C and 2B4 engagement, which led to consistent IFN-γ production in NKG2C(hi) NK cells. Thus, our data identify epigenetic imprinting of the IFNG locus as selective hallmark and crucial mechanism driving strong and stable IFN-γ expression in HCMV-specific NK cell expansions, providing a molecular basis for the regulation of adaptive features in innate cells.

Published

2014

20. Non-redundant functions of group 2 innate lymphoid cells

Author

Katja J. Jarick, Patrycja M. Topczewska, Manuel O. Jakob, Hiroshi Yano, Mohammad Arifuzzaman, Xuemei Gao, Sotiria Boulekou, Vladislava Stokic-Trtica, Pierre S. Leclère, Alexandra Preußer, Zoe A. Rompe, Anton Stamm, Amy M. Tsou, Coco Chu, Frederik R. Heinrich, Gabriela M. Guerra, Pawel Durek, Andranik Ivanov, Dieter Beule, Sofia Helfrich, Claudia U. Duerr, Anja A. Kühl, Christina Stehle, Chiara Romagnani, Mir-Farzin Mashreghi, Andreas Diefenbach, David Artis, and Christoph S. N. Klose

Subjects

Multidisciplinary

Published

2022

21. TNF hampers intestinal tissue repair in colitis by restricting IL-22 bioavailability

Author

Justus Ninnemann, Caroline Winsauer, Marina Bondareva, Anja A. Kühl, Laura Lozza, Pawel Durek, Donata Lissner, Britta Siegmund, Stefan H.E. Kaufmann, Mir-Farzin Mashreghi, Sergei A. Nedospasov, and Andrey A. Kruglov

Subjects

Inflammation, Colon, Tumor Necrosis Factor-alpha, Interleukins, Immunology, Biological Availability, Humans, Immunology and Allergy, Tumor Necrosis Factor Inhibitors, Intestinal Mucosa, Colitis, Inflammatory Bowel Diseases, digestive system diseases

Abstract

Successful treatment of chronic inflammatory diseases integrates both the cessation of inflammation and the induction of adequate tissue repair processes. Strikingly, targeting a single proinflammatory cytokine, tumor necrosis factor (TNF), induces both processes in a relevant cohort of inflammatory bowel disease (IBD) patients. However, the molecular mechanisms underlying intestinal repair following TNF blockade during IBD remain elusive. Using a novel humanized model of experimental colitis, we demonstrate that TNF interfered with the tissue repair program via induction of a soluble natural antagonist of IL-22 (IL-22Ra2; IL-22BP) in the colon and abrogated IL-22/STAT3-mediated mucosal repair during colitis. Furthermore, membrane-bound TNF expressed by T cells perpetuated colonic inflammation, while soluble TNF produced by epithelial cells (IECs) induced IL-22BP expression in colonic dendritic cells (DCs) and dampened IL-22-driven restitution of colonic epithelial functions. Finally, TNF induced IL-22BP expression in human monocyte-derived DCs and levels of IL22-BP correlated with TNF in sera of IBD patients. Thus, our data can explain how anti-TNF therapy induces mucosal healing by increasing IL-22 availability and implicates new therapeutic opportunities for IBD.

Published

2022

22. Resident memory CD4 + T lymphocytes mobilize from bone marrow to contribute to a systemic secondary immune reaction

Author

Carla Cendón, Weijie Du, Pawel Durek, Yuk‐Chien Liu, Tobias Alexander, Lindsay Serene, Xinyi Yang, Gilles Gasparoni, Abdulrahman Salhab, Karl Nordström, Tina Lai, Axel R. Schulz, Anna Rao, Gitta A. Heinz, Ana L. Stefanski, Anne Claußnitzer, Katherina Siewert, Thomas Dörner, Hyun‐Dong Chang, Hans‐Dieter Volk, Chiara Romagnani, Zhihai Qin, Sebastian Hardt, Carsten Perka, Simon Reinke, Jörn Walter, Mir‐Farzin Mashreghi, Kevin Thurley, Andreas Radbruch, and Jun Dong

Subjects

Immunology, Immunology and Allergy

Published

2022

23. Recruitment of plasma cells to the bone marrow in primary and secondary immune reactions

Author

Mir-Farzin Mashreghi, Marta Ferreira-Gomes, Pawel Durek, Yidan Chen, Hector Rincon-Arevalo, Frederik Heinrich, Franziska Szelinski, Gabriela Guerra, Ana-Luisa Stefanski, Antonia Niedobitek, Annika Wiedemann, Marina Bondareva, Jacob Ritter, Katrin Lehmann, Sebastian Hardt, Christian Hipfl, Sascha Hein, Eberhard Hildt, Mareen Matz, Henrik Mei, Qingyu Cheng, Van Duc Dang, Mario Witkowski, Andreia Lino, Andrey Kruglov, Fritz Melchers, Carsten Perka, Eva Schrezenmeier, Andreas Radbruch, and Thomas Dörner

Abstract

Bone marrow plasma cells (BMPC) emerge as a consequence of immune reactions and are considered the source of antibodies that protect against recurrent infectious diseases throughout life. Despite their importance, it remains unclear if these cells reflect different activation environments or the differentiation/maturation stages of their precursors. Here we track the recruitment of plasma cells, generated in primary and secondary immune reactions to SARS-CoV-2 spike protein vaccines, to the human bone marrow. Trajectories based on single cell transcriptomes and antigen-receptor clonotypes of antibody-secreting cells exiting the immune reaction and of those residing in the bone marrow, allow to follow the evolution of the immune response to these vaccines, leading to sequential colonization of these cells to different compartments (clans) of BMPC, and their establishment as long-lived (memory) plasma cells. In primary immune reactions, both CD19low (clans 1 and 4) and CD19high (clan 0) BMPC are generated. In secondary immune reactions, mostly CD19high BMPC of the largest compartment (clan 0) are generated, resulting from the reactivation of memory B lymphocytes. The latter is also observed in vaccinated convalescent individuals and upon recall vaccination against diphtheria/tetanus/pertussis (DTP). Thus, humoral immunological memory, i.e. serum antibodies secreted by long-lived memory BMPC, is generated already in the primary immune response, more so in the secondary, and it represents the evolution of the immune response.

Published

2023

24. MicroRNA-221/222-expression in HSC and MPP safeguards their quiescence and multipotency by downregulating stress-independent and dependent expression of IEG and of several myelo/granulopoiesis-enhancing target genes

Author

Peter K. Jani, Georg Petkau, Yohei Kawano, Uwe Klemm, Gabriela Maria Guerra, Gitta Anne Heinz, Frederik Heinrich, Pawel Durek, Mir-Farzin Mashreghi, and Fritz Melchers

Abstract

The microRNA cluster-221/222 is expressed in hematopoietic stem cells (HSC) and multipotent progenitors (MPP). To study its function in hematopoiesis, we generated mice, in which this cluster is selectively deleted by Vav-cre in HSC and, thus, in all hematopoietic cells. Fluorescence-activated cell sorting analyses of the lineage-negative HSC and MPP compartments in bone marrow at unperturbed, steady state hematopoiesis detect strong activation of HSC to MPP, as well as increased granulocytes in the periphery, induced by miR-221/222-deficiency. Short-term social stress on mice also activates HSC to MPP, but the time of stress is too short to detect further increases in granulocyte numbers. Single cell deep mRNA sequencing identifies Fos as direct, and Jun as well as six other immediate early genes (IEG) as indirect targets of miR-221/222 at unperturbed hematopoiesis. Three of these IEG - Klf6, Nr4a1 and Zfp36 - have previously been found to influence myelo/granulopoiesis. Short stress induces higher levels of the same, and an even larger number of IEGs, now also in MPP, indicating, that stress and miR-221/222 both activate HSC to MPP by IEG upregulation in perturbed hematopoiesis. Furthermore, combined stress and miR-221/222-deficiency rapidly increase numbers of myelo/granulocyte progenitors (MEP, GMP) in bone marrow. Additional indirect miR-221/222-targets become detectable in MPP, of which H3f3b has previously been found to influence myelopoiesis. In serial transplantations, miR-221/222-deficient HSC retain their capacity to home to, and become resident in bone marrow, but they loose their lymphopoietic capacities, thus their multipotency. Our results suggest, that miR-221/222-expression in HSC and MPP safeguards their quiescence and multipotency by downregulating the expression of IEG and of myelo/granulopoiesis-enhancing target genes. Since miR-221/222 is also expressed in human HSC and MPP, its expression should improve clinical settings of human bone marrow transplantations.

Published

2023

25. A type-1 immunity-restricted promoter of the IL-33 receptor gene directs antiviral T cell responses

Author

Max Löhning, Tobias Brunner, Sebastian Serve, Anna-Friederike Marx, Maria Dzamukova, Nayar Duran, Philippe Saikali, Christoph Kommer, Frederik Heinrich, Pawel Durek, Gitta Heinz, Thomas Höfer, Mir-Farzin Mashreghi, Ralf Kuehn, and Daniel Pinschewer

Abstract

The pleiotropic alarmin interleukin-33 (IL-33) drives type-1, type-2, and regulatory T-cell responses via its receptor ST2. Subset-specific differences in ST2 expression intensity and dynamics suggest that transcriptional regulation is key in orchestrating the context-dependent activity of IL-33-ST2 signaling in T-cell immunity. Here, we identify a previously unrecognized alternative promoter in mice and humans that is located far upstream of the curated ST2-coding gene and drives ST2 expression in type-1 immunity. Mice lacking this promoter exhibit a selective loss of ST2 expression in type-1- but not type-2-biased immune cells, resulting in impaired expansion of cytotoxic T cells (CTLs) and T-helper-1 cells upon viral infection. T-cell-intrinsic IL-33 signaling via type-1 promoter-driven ST2 is critical to generate a clonally diverse population of antiviral short-lived effector CTLs. Thus, lineage-specific alternative promoter usage directs alarmin responsiveness in T-cell subsets and offers opportunities for immune cell-specific targeting of the IL-33-ST2 axis in infections and inflammatory diseases.

Published

2023

26. Computer-assisted curation of a human regulatory core network from the biological literature.

Author

Philippe Thomas 0002, Pawel Durek, Illés Solt, Bertram Klinger, Franziska Witzel, Pascal Schulthess, Yvonne Mayer, Domonkos Tikk, Nils Blüthgen, and Ulf Leser

Published

2015

27. Untimely TGFβ responses in COVID-19 limit antiviral functions of NK cells

Author

Gitta Anne Heinz, Josefine Radke, Sophie Mc Ewen, V. Moos, Jobst Roehmel, Tilmann Kallinich, Pawel Durek, Daniela Niemeyer, Leif G. Hanitsch, Florian Kurth, Thordis Hohnstein, Uwe Kölsch, Mario Witkowski, Philipp Nawrath, Marcus A. Mall, Frederik Heinrich, Leif E. Sander, Stefan Frischbutter, Mir-Farzin Mashreghi, Tom Aschman, Emanuela Marcenaro, Victor M. Corman, Edoardo Viviano, Sascha Treskatsch, Andreas Diefenbach, Marta Ferreira-Gomes, Marcus Maurer, Christian Meisel, Caroline Tizian, Robert Lorenz Chua, Claudia U. Duerr, Stefan Angermair, Andrey Kruglov, Helena Radbruch, Birgit Sawitzki, Silvia Zocche, Christian Conrad, Andreas Radbruch, Irene Mattiola, Joseph A. Trapani, Thomas Schneider, Christian Drosten, Terry Jones, and Kristina Allers

Subjects

Multidisciplinary, Innate immune system, Effector, medicine.medical_treatment, Cell, Innate lymphoid cell, Biology, Virus, Cell biology, medicine.anatomical_structure, Cytokine, Viral replication, medicine, Cytotoxic T cell

Abstract

SARS-CoV-2 is a single-stranded RNA virus that causes coronavirus disease 2019 (COVID-19). Given its acute and often self-limiting course, components of the innate immune system are likely central in controlling virus replication thereby determining clinical outcome. Natural killer (NK) cells are innate lymphocytes with notable activity against a broad range of viruses, including RNA viruses1,2. NK cell function may be altered during COVID-19 despite increased representation of NK cells with an activated and ‘adaptive’ phenotype3,4. Here we show that viral load decline in COVID-19 correlates with NK cell status and that NK cells can control SARS-CoV-2 replication by recognizing infected target cells. In severe COVID-19, NK cells show remarkable defects in virus control, cytokine production and cell-mediated cytotoxicity despite high expression of cytotoxic effector molecules. Single-cell RNA-sequencing (scRNA-seq) of NK cells along the time course of the entire COVID-19 disease spectrum reveals a unique gene expression signature. Transcriptional networks of interferon-driven NK cell activation are superimposed by a dominant TGFβ response signature with reduced expression of genes related to cell-cell adhesion, granule exocytosis and cell-mediated cytotoxicity. In severe COVID-19, serum levels of TGFβ peak during the first 2 weeks of infection, and serum obtained from these patients profoundly inhibits NK cell function in a TGFβ-dependent manner. Our data reveal that untimely production of TGFβ is a hallmark of severe COVID-19 and may inhibit NK cell function and early virus control.

Published

2021

28. T-bet and RORα control lymph node formation by regulating embryonic innate lymphoid cell differentiation

Author

Carolin Ulbricht, Pawel Durek, Claire Willis, Daniela Finke, Dominika W Gajdasik, Timo Rückert, Chiara Romagnani, Remi Fiancette, David R. Withers, Jakob Zimmermann, Mir-Farzin Mashreghi, Hyun-Dong Chang, Christina Stehle, and Anja E. Hauser

Subjects

Immunology, Embryogenesis, Innate lymphoid cell, chemical and pharmacologic phenomena, hemic and immune systems, Biology, Embryonic stem cell, Cell biology, medicine.anatomical_structure, Lymphatic system, RAR-related orphan receptor gamma, medicine, Immunology and Allergy, Progenitor cell, Lymph node, Transcription factor

Abstract

The generation of lymphoid tissues during embryogenesis relies on group 3 innate lymphoid cells (ILC3) displaying lymphoid tissue inducer (LTi) activity and expressing the master transcription factor RORγt. Accordingly, RORγt-deficient mice lack ILC3 and lymphoid structures, including lymph nodes (LN). Whereas T-bet affects differentiation and functions of ILC3 postnatally, the role of T-bet in regulating fetal ILC3 and LN formation remains completely unknown. Using multiple mouse models and single-cell analyses of fetal ILCs and ILC progenitors (ILCP), here we identify a key role for T-bet during embryogenesis and show that its deficiency rescues LN formation in RORγt-deficient mice. Mechanistically, T-bet deletion skews the differentiation fate of fetal ILCs and promotes the accumulation of PLZFhi ILCP expressing central LTi molecules in a RORα-dependent fashion. Our data unveil an unexpected role for T-bet and RORα during embryonic ILC function and highlight that RORγt is crucial in counteracting the suppressive effects of T-bet.

Published

2021

29. Combining segmental bulk- and single-cell RNA-sequencing to define the chondrocyte gene expression signature in the murine knee joint

Author

Frederik F. Heinrich, Pawel Durek, Vikram Sunkara, Annemarie Lang, Gitta Anne Heinz, Mir-Farzin Mashreghi, and Ali Mobasheri

Subjects

Cartilage, Articular, Male, 0301 basic medicine, Cell, Population, Biomedical Engineering, RNA-Seq, Biology, Chondrocyte, Transcriptome, Mice, 03 medical and health sciences, Chondrocytes, 0302 clinical medicine, Rheumatology, Gene expression, medicine, Animals, Orthopedics and Sports Medicine, education, Gene, 030203 arthritis & rheumatology, education.field_of_study, Sequence Analysis, RNA, Cartilage, Endochondral bone growth, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, RNA

Abstract

ObjectiveDue to the small size of the murine knee joint, extracting the chondrocyte transcriptome from articular cartilage (AC) is a major technical challenge. In this study, we demonstrate a new and pragmatic approach of combining bulk RNA-sequencing (RNA-seq) and single cell (sc)RNA-seq to address this problem.DesignWe propose a new cutting strategy of the murine femur which produces three segments with a predictable mixed cell populations, where one segment contains AC and growth plate (GP) chondrocytes, another contains GP chondrocytes, and the last segment contains only bone and bone marrow. We analysed the bulk RNA-seq of the different segments to find common and distinct genes between the segments. Then, the segment containing AC chondrocytes was digested and analysed via scRNA-seq.ResultsDifferential expression analysis using bulk RNA-seq identified 350 candidate chondrocyte gene in the AC segment. Gene set enrichment analysis of these genes revealed biological processes related- and non-related to chondrocytes, including, cartilage development (adj. p-value: 3.45E-17) and endochondral bone growth (adj. p-value 1.22E-4), respectively. ScRNA-seq of the AC segment found a cluster of 131 cells containing mainly chondrocytes. This cluster had 759 differentially expressed genes which enriched for extracellular matrix organisation (adj. p-value 7.76E-40) and other joint development processes. The intersection of the gene sets of bulk- and scRNA-seq contained 75 genes, where all but ten genes were previously implicated in cartilage homeostasis or osteoarthritis (OA) progression.ConclusionsOur approach has the potential to detect the scarce disease phenotypes of chondrocytes in murine OA models.

Published

2021

30. Antigen‐driven PD‐1 + TOX + BHLHE40 + and PD‐1 + TOX + EOMES + T lymphocytes regulate juvenile idiopathic arthritis in situ

Author

Bas Vastert, Alessio Mazzoni, Lorenz Elias Wirth, Tilmann Kallinich, Francesco Giudici, Francesco Annunziato, Pawel Durek, Philipp Enghard, Patrick Maschmeyer, Mir-Farzin Mashreghi, Katrin Lehmann, Sae Lim von Stuckrad, Femke van Wijk, Cam Loan Tran, Andreas Radbruch, Imme Sakwa, Christopher Mark Skopnik, Marcus A. Mall, René Riedel, Hyun-Dong Chang, Lisanne Lutter, Gitta Anne Heinz, Rolando Cimaz, and Frederik Heinrich

Subjects

0301 basic medicine, education.field_of_study, biology, Immunology, Population, T-cell receptor, Arthritis, Inflammation, medicine.disease, Major histocompatibility complex, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Immune system, Antigen, medicine, biology.protein, Immunology and Allergy, medicine.symptom, education, CD8, 030215 immunology

Abstract

T lymphocytes accumulate in inflamed tissues of patients with chronic inflammatory diseases (CIDs) and express pro-inflammatory cytokines upon re-stimulation in vitro. Further, a significant genetic linkage to MHC genes suggests that T lymphocytes play an important role in the pathogenesis of CIDs including juvenile idiopathic arthritis (JIA). However, the functions of T lymphocytes in established disease remain elusive. Here we dissect the transcriptional and the clonal heterogeneity of synovial T lymphocytes in JIA patients by single-cell RNA sequencing combined with T cell receptor profiling on the same cells. We identify clonally expanded subpopulations of T lymphocytes expressing genes reflecting recent activation by antigen in situ. A PD-1+ TOX+ EOMES+ population of CD4+ T lymphocytes expressed immune regulatory genes and chemoattractant genes for myeloid cells. A PD-1+ TOX+ BHLHE40+ population of CD4+ , and a mirror population of CD8+ T lymphocytes expressed genes driving inflammation, and genes supporting B lymphocyte activation in situ. This analysis points out that multiple types of T lymphocytes have to be targeted for therapeutic regeneration of tolerance in arthritis.

Published

2021

31. PhosPhAt: the Arabidopsis thaliana phosphorylation site database. An update.

Author

Pawel Durek, Robert Schmidt, Joshua L. Heazlewood, Alexandra Jones, Daniel MacLean, Axel Nagel, Birgit Kersten, and Waltraud X. Schulze

Published

2010

32. Targeting CD38 with Daratumumab in Refractory Systemic Lupus Erythematosus

Author

Falk Hiepe, Frederik Heinrich, Marie Burns, Lennard Ostendorf, Tobias Alexander, Gerd R Burmester, Andreas Radbruch, Panagiotis Garantziotis, Philipp Enghard, Robert Biesen, Fabian Knebel, Pawel Durek, Henrik E. Mei, Udo Schneider, Mir-Farzin Mashreghi, Ulrich Richter, and Gitta Anne Heinz

Subjects

Lupus erythematosus, Systemic lupus erythematosus, biology, business.industry, medicine.medical_treatment, Autoantibody, Daratumumab, Immunosuppression, General Medicine, 030204 cardiovascular system & hematology, medicine.disease, Belimumab, 03 medical and health sciences, 0302 clinical medicine, Monoclonal, Immunology, biology.protein, Medicine, 030212 general & internal medicine, Antibody, business, medicine.drug

Abstract

Daratumumab, a human monoclonal antibody that targets CD38, depletes plasma cells and is approved for the treatment of multiple myeloma. Long-lived plasma cells are implicated in the pathogenesis of systemic lupus erythematosus because they secrete autoantibodies, but they are unresponsive to standard immunosuppression. We describe the use of daratumumab that induced substantial clinical responses in two patients with life-threatening lupus, with the clinical responses sustained by maintenance therapy with belimumab, an antibody to B-cell activating factor. Significant depletion of long-lived plasma cells, reduction of interferon type I activity, and down-regulation of T-cell transcripts associated with chronic inflammation were documented. (Supported by the Deutsche Forschungsgemeinschaft and others.).

Published

2020

33. Local CCL18 and CCL21 expand lung fibrovascular niches and recruit lymphocytes, leading to tertiary lymphoid structure formation in prolonged COVID-19

Author

Ronja Mothes, Anna Pascual-Reguant, Ralf Koehler, Juliane Liebeskind, Alina Liebheit, Sandy Bauherr, Carsten Dittmayer, Michael Laue, Regina von Manitius, Sefer Elezkurtaj, Pawel Durek, Frederik Heinrich, Gitta Anne Heinz, Gabriela Maria Guerra, Benedikt Obermayer, Jenny Meinhardt, Jana Ihlow, Josefine Radke, Frank L. Heppner, Philipp Enghard, Helena Stockmann, Tom Aschman, Julia Schneider, Victor Corman, Leif Erik Sander, Mir-Farzin Mashreghi, Thomas Conrad, Andreas Hocke, Raluca A. Niesner, Helena Radbruch, and Anja E. Hauser

Abstract

Post-acute lung sequelae of COVID-19 are challenging many survivors across the world, yet the mechanisms behind are poorly understood. Our results delineate an inflammatory cascade of events occurring along disease progression within fibrovascular niches. It is initiated by endothelial dysfunction, followed by heme scavenging of CD163+ macrophages and production of CCL18. This chemokine synergizes with local CCL21 upregulation to influence the stromal composition favoring endothelial to mesenchymal transition. The local immune response is further modulated via recruitment of CCR7+ T cells into the expanding fibrovascular niche and imprinting an exhausted, T follicular helper–like phenotype in these cells. Eventually, this culminates in the formation of tertiary lymphoid structures, further perpetuating chronic inflammation. Thus, our work presents misdirected immune-stromal interaction mechanisms promoting a self-sustained and non-resolving local immune response that extends beyond active viral infection and leads to profound tissue repurposing and chronic inflammation.

Published

2022

34. Resident memory CD4

Author

Carla, Cendón, Weijie, Du, Pawel, Durek, Yuk-Chien, Liu, Tobias, Alexander, Lindsay, Serene, Xinyi, Yang, Gilles, Gasparoni, Abdulrahman, Salhab, Karl, Nordström, Tina, Lai, Axel R, Schulz, Anna, Rao, Gitta A, Heinz, Ana L, Stefanski, Anne, Claußnitzer, Katherina, Siewert, Thomas, Dörner, Hyun-Dong, Chang, Hans-Dieter, Volk, Chiara, Romagnani, Zhihai, Qin, Sebastian, Hardt, Carsten, Perka, Simon, Reinke, Jörn, Walter, Mir-Farzin, Mashreghi, Kevin, Thurley, Andreas, Radbruch, and Jun, Dong

Subjects

CD4-Positive T-Lymphocytes, Vaccines, Bone Marrow, Humans, CD8-Positive T-Lymphocytes, Immunologic Memory

Abstract

Resident memory T lymphocytes (T

Published

2022

35. B Cell Numbers Predict Humoral and Cellular Response Upon SARS-CoV-2 Vaccination Among Patients Treated With Rituximab

Author

Katja Kotsch, Hector Rincon-Arevalo, Frederik Heinrich, Marta Ferreira Gomes, Kirsten Karberg, Bernd Jahrsdoerfer, Gerd R Burmester, Fabian Proft, Hubert Schrezenmeier, Andreia C. Lino, Hildrun Haibel, Ana-Luisa Stefanski, Yidan Chen, Gabriella Maria Guerra, Anne Claussnitzer, Franziska Szelinski, Eva Schrezenmeier, Arne Sattler, Jacob Ritter, Mir-Farzin Mashreghi, Thomas Doerner, Carolin Ludwig, Andreas Radbruch, and Pawel Durek

Subjects

SARS–CoV-2, business.industry, Arthritis, Vaccination, Immunology, medicine.disease, Immune system, medicine.anatomical_structure, Rheumatology, Rheumatoid arthritis, Plasma cell differentiation, medicine, Cytotoxic T cell, Immunology and Allergy, Rituximab, Seroconversion, business, B cell, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::610 Medizin und Gesundheit, medicine.drug

Abstract

Objective: Patients with autoimmune inflammatory rheumatic diseases receiving rituximab (RTX) therapy are at higher risk of poor COVID-19 outcomes and show substantially impaired humoral immune response to anti-SARS-CoV-2 vaccine. However, the complex relationship between antigen-specific B cells and T cells and the level of B cell repopulation necessary to achieve anti-vaccine responses remain largely unknown. Methods: Antibody responses to SARS-CoV-2 vaccines and induction of antigen-specific B and CD4/CD8 T cell subsets were studied in 19 patients with rheumatoid arthritis (RA) or antineutrophil cytoplasmic antibody-associated vasculitis receiving RTX, 12 patients with RA receiving other therapies, and 30 healthy controls after SARS-CoV-2 vaccination with either messenger RNA or vector-based vaccines. Results: A minimum of 10 B cells per microliter (0.4% of lymphocytes) in the peripheral circulation appeared to be required for RTX-treated patients to mount seroconversion to anti-S1 IgG upon SARS-CoV-2 vaccination. RTX-treated patients who lacked IgG seroconversion showed reduced receptor-binding domain-positive B cells (P = 0.0005), a lower frequency of Tfh-like cells (P = 0.0481), as well as fewer activated CD4 (P = 0.0036) and CD8 T cells (P = 0.0308) compared to RTX-treated patients who achieved IgG seroconversion. Functionally relevant B cell depletion resulted in impaired interferon-γ secretion by spike-specific CD4 T cells (P = 0.0112, r = 0.5342). In contrast, antigen-specific CD8 T cells were reduced in both RA patients and RTX-treated patients, independently of IgG formation. Conclusion: In RTX-treated patients, a minimum of 10 B cells per microliter in the peripheral circulation is a candidate biomarker for a high likelihood of an appropriate cellular and humoral response after SARS-CoV-2 vaccination. Mechanistically, the data emphasize the crucial role of costimulatory B cell functions for the proper induction of CD4 responses propagating vaccine-specific B cell and plasma cell differentiation.

Published

2022

36. PhosPhAt: a database of phosphorylation sites in Arabidopsis thaliana and a plant-specific phosphorylation site predictor.

Author

Joshua L. Heazlewood, Pawel Durek, Jan Hummel, Joachim Selbig, Wolfram Weckwerth, Dirk Walther 0001, and Waltraud X. Schulze

Published

2008

37. Protection against autoimmunity is driven by thymic epithelial cell–mediated regulation of Tregdevelopment

Author

Ari Waisman, Pawel Durek, Nicole Puertas, Mir-Farzin Mashreghi, Marianne R. Spalinger, Stefan Floess, Mirjam Lutz, Ekaterina Friebel, Benedict Becher, Florian Ingelfinger, Florian Mair, Ana Amorim, Claudia Haftmann, Stefanie Schärli, Pascale Zwicky, Burkhard Becher, Jochen Huehn, René Riedel, Jan Kisielow, and Brian P. Leung

Subjects

medicine.anatomical_structure, T cell, Immunology, Thymic epithelial cell, medicine, Cancer research, General Medicine, Biology, medicine.disease_cause, Autoimmunity

Abstract

Medullary thymic epithelial cells (mTECs) are key antigen-presenting cells mediating T cell tolerance to prevent harmful autoimmunity. mTECs both negatively select self-reactive T cells and promote...

Published

2021

38. Protection against autoimmunity is driven by thymic epithelial cell-mediated regulation of T

Author

Claudia, Haftmann, Pascale, Zwicky, Florian, Ingelfinger, Florian, Mair, Stefan, Floess, René, Riedel, Pawel, Durek, Marianne R, Spalinger, Ekaterina, Friebel, Brian P, Leung, Mirjam, Lutz, Nicole, Puertas, Ana, Amorim, Stefanie, Schärli, Benedict, Becher, Jan, Kisielow, Ari, Waisman, Mir-Farzin, Mashreghi, Jochen, Huehn, and Burkhard, Becher

Subjects

Mice, Inbred C57BL, Mice, Knockout, Mice, Mice, Congenic, Animals, Humans, Autoimmunity, Epithelial Cells, Forkhead Transcription Factors, Thymus Gland, Protein Serine-Threonine Kinases, T-Lymphocytes, Regulatory

Abstract

Medullary thymic epithelial cells (mTECs) are key antigen-presenting cells mediating T cell tolerance to prevent harmful autoimmunity. mTECs both negatively select self-reactive T cells and promote the development of thymic regulatory T cells (tT

Published

2021

39. Induction of cross-reactive antibody responses against the RBD domain of the spike protein of SARS-CoV-2 by commensal microbiota

Author

Caroline Tizian, Hyun-Dong Chang, Philipp Enghard, Edoardo Viviano, Andreas Diefenbach, Toni Sempert, Mario Witkowski, Katharina Johanna Sehmsdorf, Thomas Doerner, Sascha Treskatsch, Harald Pruess, Stefan Angermair, Martin Raftery, Mir-Farzin Mashreghi, Ivan V. Smirnov, Elisa Sanchez-Sendin, Andreas Radbruch, Justus Ninnemann, Lisa Budzinski, Eva Schrezenmeier, Jakob Kreye, Selin Yilmaz, Pawel Durek, Gitta Anne Heinz, Momsen Reincke, Marina Bondareva, Vadim M. Govorun, Andrey Kruglov, Silvia Zocche, Daria Matyushkina, and Guenther Schoenrich

Subjects

biology, Streptococcus, Human microbiome, Veillonella, medicine.disease_cause, biology.organism_classification, Microbiology, Streptococcus salivarius, Antigen, Monoclonal, medicine, biology.protein, Antibody, Bacteria

Abstract

The commensal microflora is a source for multiple antigens that may induce cross-reactive antibodies against host proteins and pathogens. However, whether commensal bacteria can induce cross-reactive antibodies against SARS-CoV-2 remains unknown. Here we report that several commensal bacteria contribute to the generation of cross-reactive IgA antibodies against the receptor-binding domain (RBD) of the SARS-CoV-2 Spike protein. We identified SARS-CoV-2 unexposed individuals with RBD-binding IgA antibodies at their mucosal surfaces. Conversely, neutralising monoclonal anti-RBD antibodies recognised distinct commensal bacterial species. Some of these bacteria, such as Streptococcus salivarius, induced a cross-reactive anti-RBD antibodies upon supplementation in mice. Conversely, severely ill COVID-19 patients showed reduction of Streptococcus and Veillonella in their oropharynx and feces and a reduction of anti-RBD IgA at mucosal surfaces. Altogether, distinct microbial species of the human microbiota can induce secretory IgA antibodies cross-reactive for the RBD of SARS-CoV-2.

Published

2021

40. Single‐cell transcriptomes of murine bone marrow stromal cells reveal niche‐associated heterogeneity

Author

Gitta Anne Heinz, Frederik Heinrich, Max Löhning, Katrin Lehmann, Mir-Farzin Mashreghi, Markus Bardua, Anja E. Hauser, Daniel Schulz, Andreas Radbruch, Özen Sercan-Alp, Cam Loan Tran, Richard K. Addo, Mareen Matz, Hyun-Dong Chang, Pawel Durek, and Andrey Kruglov

Subjects

Stromal cell, bone marrow, medicine.medical_treatment, Short Communication, Immunology, Bone Marrow Cells, Biology, single cell sequencing, Transcriptome, Mice, Immune system, hematopoietic cells, B-Cell Activating Factor, medicine, Immunology and Allergy, Animals, Basic, Cells, Cultured, Interleukin-15, Sequence Analysis, RNA, Interleukin-7, Mesenchymal stem cell, Mesenchymal Stem Cells, Hematopoietic Stem Cells, cytokines, Cell biology, Short Communication|Basic, Mice, Inbred C57BL, Haematopoiesis, Cytokine, medicine.anatomical_structure, Single cell sequencing, Systems immunology, Bone marrow, Stromal Cells

Abstract

Bone marrow (BM) stromal cells are important in the development and maintenance of cells of the immune system. Using single cell RNA sequencing, we here explore the functional and phenotypic heterogeneity of individual transcriptomes of 1167 murine BM mesenchymal stromal cells. These cells exhibit a tremendous heterogeneity of gene expression, which precludes the identification of defined subpopulations. However, according to the expression of 108 genes involved in the communication of stromal cells with hematopoietic cells, we have identified 14 non‐overlapping subpopulations, with distinct cytokine or chemokine gene expression signatures. With respect to the maintenance of subsets of immune memory cells by stromal cells, we identified distinct subpopulations expressing Il7, Il15 and Tnfsf13b. Together, this study provides a comprehensive dissection of the BM stromal heterogeneity at the single cell transcriptome level and provides a basis to understand their lifestyle and their role as organizers of niches for the long‐term maintenance of immune cells.

Published

2019

41. Impaired antigen-specific memory B cell and plasma cell responses including lack of specific IgG upon SARS-CoV-2 BNT162b2 vaccination among Kidney Transplant and Dialysis patients

Author

Alexander Potekhin, Andreia C. Lino, Arne Sattler, Katja Kotsch, Hubert Schrezenmeier, Frederik Heinrich, Fabian Halleck, Mira Choi, Klemens Budde, Franziska Szelinski, Eva Schrezenmeier, Mir-Farzin Mashreghi, Hector Rincon-Arevalo, Andreas Radbruch, Carolin Ludwig, Pawel Durek, Bernd Jahrsdoerfer, Thomas Doerner, Ana-Luisa Stefanski, Marta Ferreira-Gomes, Kai-Uwe Eckardt, Yidan Chen, Gabriela Maria Guerra, Gerd R Burmester, and Ulrike Weber

Subjects

business.industry, T cell, medicine.medical_treatment, Naive B cell, Germinal center, Immunosuppression, Plasma cell, medicine.disease, medicine.anatomical_structure, Immunology, medicine, Memory B cell, business, Kidney transplantation, B cell

Abstract

Patients with kidney failure are at increased risk during the COVID-19 pandemic and effective vaccinations are needed. It is not known how efficient mRNA vaccines mount B and plasma cell responses in dialysis patients (DP) or kidney transplant recipients (KTR) compared to healthy controls (HC). We studied humoral and B cell responses of 25 HC, 44 DP and 40 KTR. Markedly impaired anti-BNT162b2 responses were identified among KTR and DP compared to 100% seroconversion in HC. In DP, the response was delayed (3-4 weeks after boost) and reduced with anti-S1 IgG positivity in 31 (70.5%) and anti-S1 IgA in 30 (68.2%) of 44, respectively. In contrast, KTR did not develop IgG response except one patient who had prior unrecognized infection and developed anti-S1 IgG. The majority of antigen-specific B cells (RBD+) were identified in the plasmablast or post-switch memory B cell compartments in HC, whereas these RBD+ B cells were enriched among pre-switch and naïve B cells from DP and KTR. Single cell transcriptome and CITE-seq analyses found reduced frequencies of plasmablasts, TCF7+CD27+GZMK+ T cells and proliferating MKI67-expressing lymphocytes among KTR non-responders. Importantly, the frequency and absolute number of antigen-specific circulating plasmablasts in the whole cohort correlated with the Ig response, a characteristic not reported for other vaccinations. In conclusion, this data indicate that lack of T cell help related to immunosuppression results in impaired germinal center differentiation of B and plasma cell memory. There is an urgent need to improve vaccination protocols in patients after kidney transplantation or on chronic dialysis.One Sentence SummaryKidney transplant recipients and dialysis patients show a markedly diminished humoral response and impaired molecular B cell memory formation upon vaccination with BNT162b2.

Published

2021

42. Antigen‐driven PD‐1 + TOX + BHLHE40 + and PD‐1 + TOX + EOMES + T lymphocytes regulate juvenile idiopathic arthritis in situ

Author

Patrick Maschmeyer, Gitta Anne Heinz, Christopher Mark Skopnik, Lisanne Lutter, Alessio Mazzoni, Frederik Heinrich, Sae Lim Stuckrad, Lorenz Elias Wirth, Cam Loan Tran, René Riedel, Katrin Lehmann, Imme Sakwa, Rolando Cimaz, Francesco Giudici, Marcus Alexander Mall, Philipp Enghard, Bas Vastert, Hyun‐Dong Chang, Pawel Durek, Francesco Annunziato, Femke Wijk, Andreas Radbruch, Tilmann Kallinich

Published

2021

43. Detection and characterization of 3D-signature phosphorylation site motifs and their contribution towards improved phosphorylation site prediction in proteins.

Author

Pawel Durek, Christian Schudoma, Wolfram Weckwerth, Joachim Selbig, and Dirk Walther 0001

Published

2009

44. T-bet and RORα control lymph node formation by regulating embryonic innate lymphoid cell differentiation

Author

Christina, Stehle, Timo, Rückert, Rémi, Fiancette, Dominika W, Gajdasik, Claire, Willis, Carolin, Ulbricht, Pawel, Durek, Mir-Farzin, Mashreghi, Daniela, Finke, Anja Erika, Hauser, David R, Withers, Hyun-Dong, Chang, Jakob, Zimmermann, and Chiara, Romagnani

Subjects

Mice, Lymphoid Tissue, Animals, Cell Differentiation, Cell Lineage, Female, Nuclear Receptor Subfamily 1, Group F, Member 1, Lymph Nodes, Lymphocytes, T-Lymphocytes, Helper-Inducer, Nuclear Receptor Subfamily 1, Group F, Member 3, T-Box Domain Proteins, Immunity, Innate

Abstract

The generation of lymphoid tissues during embryogenesis relies on group 3 innate lymphoid cells (ILC3) displaying lymphoid tissue inducer (LTi) activity and expressing the master transcription factor RORγt. Accordingly, RORγt-deficient mice lack ILC3 and lymphoid structures, including lymph nodes (LN). Whereas T-bet affects differentiation and functions of ILC3 postnatally, the role of T-bet in regulating fetal ILC3 and LN formation remains completely unknown. Using multiple mouse models and single-cell analyses of fetal ILCs and ILC progenitors (ILCP), here we identify a key role for T-bet during embryogenesis and show that its deficiency rescues LN formation in RORγt-deficient mice. Mechanistically, T-bet deletion skews the differentiation fate of fetal ILCs and promotes the accumulation of PLZF

Published

2020

45. Author response for 'Antigen‐driven PD‐1 + TOX + BHLHE40 + and PD‐1 + TOX + EOMES + T lymphocytes regulate juvenile idiopathic arthritis in situ'

Author

Gitta Anne Heinz, Katrin Lehmann, Frederik Heinrich, Lisanne Lutter, Imme Sakwa, Patrick Maschmeyer, Christopher Mark Skopnik, Philipp Enghard, Sae Lim von Stuckrad, Rolando Cimaz, Femke van Wijk, Tilmann Kallinich, Cam Loan Tran, Pawel Durek, Bas Vastert, René Riedel, Alessio Mazzoni, Francesco Annunziato, Hyun-Dong Chang, Lorenz Elias Wirth, Marcus A. Mall, Mir-Farzin Mashreghi, Francesco Giudici, and Andreas Radbruch

Subjects

In situ, Antigen, Immunology, medicine, Juvenile, Arthritis, Biology, medicine.disease

Published

2020

46. Antigen-driven PD-1

Author

Patrick, Maschmeyer, Gitta Anne, Heinz, Christopher Mark, Skopnik, Lisanne, Lutter, Alessio, Mazzoni, Frederik, Heinrich, Sae Lim, von Stuckrad, Lorenz Elias, Wirth, Cam Loan, Tran, René, Riedel, Katrin, Lehmann, Imme, Sakwa, Rolando, Cimaz, Francesco, Giudici, Marcus Alexander, Mall, Philipp, Enghard, Bas, Vastert, Hyun-Dong, Chang, Pawel, Durek, Francesco, Annunziato, Femke, van Wijk, Andreas, Radbruch, Tilmann, Kallinich, and Mir-Farzin, Mashreghi

Subjects

CD4-Positive T-Lymphocytes, Homeodomain Proteins, Gene Expression Profiling, T-Lymphocytes, Programmed Cell Death 1 Receptor, High Mobility Group Proteins, Receptors, Antigen, T-Cell, CD8-Positive T-Lymphocytes, Arthritis, Juvenile, Basic Helix-Loop-Helix Transcription Factors, Humans, RNA-Seq, Antigens, Single-Cell Analysis, T-Box Domain Proteins, Transcriptome, Cells, Cultured

Abstract

T lymphocytes accumulate in inflamed tissues of patients with chronic inflammatory diseases (CIDs) and express pro-inflammatory cytokines upon re-stimulation in vitro. Further, a significant genetic linkage to MHC genes suggests that T lymphocytes play an important role in the pathogenesis of CIDs including juvenile idiopathic arthritis (JIA). However, the functions of T lymphocytes in established disease remain elusive. Here we dissect the transcriptional and the clonal heterogeneity of synovial T lymphocytes in JIA patients by single-cell RNA sequencing combined with T cell receptor profiling on the same cells. We identify clonally expanded subpopulations of T lymphocytes expressing genes reflecting recent activation by antigen in situ. A PD-1

Published

2020

47. SARS-CoV-2 in severe COVID-19 induces a TGF-β-dominated chronic immune response that does not target itself

Author

Hyun-Dong Chang, Mareen Matz, Weijie Du, Günther Schönrich, Lukas Heiberger, Marta Ferreira-Gomes, Thomas Dörner, Sascha Treskatsch, Gitta Anne Heinz, Lisa Budzinski, Lennard Ostendorf, Frederik Heinrich, Caroline Tizian, Jun Dong, Andreas Radbruch, Katharina Habenicht, Anna Pascual-Reguant, Helena Radbruch, Péter K. Jani, Sandy Bauherr, Mir-Farzin Mashreghi, Sefer Elezkurtaj, Anja E. Hauser, Katrin Lehmann, Andreas Diefenbach, Thomas Winkler, Martin Raftery, Gabriela Maria Guerra, Hans-Dieter Volk, Mario Witkowski, Ronja Mothes, Marcus A. Mall, Tilmann Kallinich, Pawel Durek, Victor M. Corman, Fritz Melchers, Andrey Kruglov, Stefan Frischbutter, Chaofan Fan, Marcus Maurer, Stefan Angermair, and Justus Ninnemann

Subjects

0301 basic medicine, Male, General Physics and Astronomy, Antibodies, Viral, Pathogenesis, 0302 clinical medicine, Transforming Growth Factor beta, Gene expression, Medicine, skin and connective tissue diseases, Aged, 80 and over, Multidisciplinary, biology, Middle Aged, Acquired immune system, Spike Glycoprotein, Coronavirus, Female, Antibody, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::610 Medizin und Gesundheit, Adult, Science, Plasma Cells, General Biochemistry, Genetics and Molecular Biology, Article, Antibodies, 03 medical and health sciences, Immune system, Antigen, Intensive care, Humans, ddc:610, Seroconversion, Aged, business.industry, SARS-CoV-2, Interleukins, fungi, COVID-19, General Chemistry, Antimicrobial responses, biochemical phenomena, metabolism, and nutrition, Immunoglobulin A, body regions, 030104 developmental biology, Viral infection, Immunoglobulin G, Immunology, biology.protein, Next-generation sequencing, business, 030215 immunology

Abstract

The pathogenesis of severe COVID-19 reflects an inefficient immune reaction to SARS-CoV-2. Here we analyze, at the single cell level, plasmablasts egressed into the blood to study the dynamics of adaptive immune response in COVID-19 patients requiring intensive care. Before seroconversion in response to SARS-CoV-2 spike protein, peripheral plasmablasts display a type 1 interferon-induced gene expression signature; however, following seroconversion, plasmablasts lose this signature, express instead gene signatures induced by IL-21 and TGF-β, and produce mostly IgG1 and IgA1. In the sustained immune reaction from COVID-19 patients, plasmablasts shift to the expression of IgA2, thereby reflecting an instruction by TGF-β. Despite their continued presence in the blood, plasmablasts are not found in the lungs of deceased COVID-19 patients, nor does patient IgA2 binds to the dominant antigens of SARS-CoV-2. Our results thus suggest that, in severe COVID-19, SARS-CoV-2 triggers a chronic immune reaction that is instructed by TGF-β, and is distracted from itself., Our understanding on the humoral immunity induced by SARS-CoV-2 is still lacking. Here the authors analyze B cell responses at the single cell level to find that, in severe COVID-19 patients, plasmablasts shift from IFN to TGFβ instruction to produce IgA antibodies that are not specific to dominant SARS-CoV-2 antigens.

Published

2020

48. Prevention of EAE by PEGylated Antigenic Peptides

Author

Uta Lauer, Bianca von Thülen, Mario Simonetti, Matthias Kröger, Pawel Durek, Ralf Krähmer, Frank Leenders, Ute Hoffmann, Jennifer Pfeil, Christina Poulsen, Justyna Pawlowska, and Alf Hamann

Subjects

Effector, business.industry, Multiple sclerosis, Central nervous system, Experimental autoimmune encephalomyelitis, medicine.disease, Myelin, medicine.anatomical_structure, Immune system, In vivo, Immunology, PEGylation, Medicine, business

Abstract

The treatment of autoimmune disorders such as multiple sclerosis (MS) so far relies largely on the use of non-specific immunosuppressive drugs, which are not able to cure the disease. Presently, approaches to induce antigen-specific tolerance e.g. by peptide-based tolerogenic “inverse” vaccines regain interest. We previously have shown that coupling of peptides to carriers can enhance their capacity to induce regulatory T cells in vivo. We here investigated in an experimental autoimmune encephalomyelitis (EAE) model for chronic MS (MOG C57BL/6) whether the tolerogenic potential of immunodominant myelin T cell epitopes can be improved by conjugation to the synthetic carrier polyethylene glycol (PEG). Indeed, preventive administration of the PEGylated antigenic peptide could almost completely protect mice from EAE development, which was accompanied by reduced immune cell infiltration in the central nervous system (CNS). Depletion of Tregs abrogated the protective effect indicating that Tregs play a crucial role in induction of antigen-specific tolerance in EAE. Treatment during the acute phase was safe and did not induce immune activation. However, treatment at the peak of disease was not affecting the disease course, suggesting that either induction of Tregs is not occurring in the highly inflamed situation, or that the immune system is refractory to regulation in this condition. Thus, PEGylation of antigenic peptides is an effective and feasible strategy to improve tolerogenic (Treg-inducing) peptide-based vaccines, but application in overt disease might require modifications or combination therapies that simultaneously suppress effector mechanisms.

Published

2020

49. In severe COVID-19, SARS-CoV-2 induces a chronic, TGF-β-dominated adaptive immune response

Author

Sascha Treskatsch, Mir-Farzin Mashreghi, Katharina Habenicht, Caroline Tizian, Stefan Angermair, Andrey Kruglov, Tilmann Kallinich, Fan C, Stefan Frischbutter, Lisa Budzinski, Thomas Dörner, Dong J, Lukas Heiberger, Günther Schönrich, Pawel Durek, Katrin Lehmann, Justus Ninnemann, Anne Heinz G, Thomas Winkler, Lennard Ostendorf, Mareen Matz, Alexander Mall M, Erika Hauser A, Fritz Melchers, Mario Witkowski, Andreas Radbruch, Marcus Maurer, Andreas Diefenbach, Hans-Dieter Volk, Ronja Mothes, Gabriela Maria Guerra, Martin Raftery, Du W, Max Corman, Marta Ferreira-Gomes, Sefer Elezkurtaj, Péter K. Jani, Helena Radbruch, Sandy Bauherr, H.-D. Chang, Pascual-Reguant A, and Frederik Heinrich

Subjects

Antigen, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Gene expression, Immunology, Seroconversion, Biology, Acquired immune system, Peripheral, Transforming growth factor

Abstract

Here we have analyzed the dynamics of the adaptive immune response triggered by SARS-CoV-2 in severely affected COVID-19 patients, as reflected by activated B cells egressing into the blood, at the single cell level. Early on, before seroconversion in response to SARS-CoV-2 spike protein, activated peripheral B cells displayed a type 1 interferon-induced gene expression signature. After seroconversion, activated B cells lost this signature, expressed IL-21- and TGF-β-induced gene expression signatures, and mostly IgG1 and IgA1. In the sustained immune reaction of the COVID-19 patients, until day 59, activated peripheral B cells shifted to expression of IgA2, reflecting instruction by TGF-β. Despite the continued generation of activated B cells, those cells were not found in the lungs of deceased COVID-19 patients, nor did the IgA2 bind to dominant antigens of SARS-CoV-2. In severe COVID-19, SARS-CoV-2 thus triggers a chronic immune reaction distracted from itself and instructed by TGF-β.

Published

2020

50. Discrete populations of isotype-switched memory B lymphocytes are maintained in murine spleen and bone marrow

Author

Stefanie Hahne, Katrin Lehmann, Claudia Haftmann, Jannis Kummer, Melanie Weber, Silvia Kühnel, Daniel Schulz, Stefan Kröger, Ralf Köhler, Richard K. Addo, Jakob Zimmermann, Ulrike Menzel, Frederik Heinrich, Andreas Radbruch, Patrick Maschmeyer, Rebecca Cornelis, Anja E. Hauser, Sai T. Reddy, Francesco Siracusa, Gitta Anne Heinz, Ulrik Stervbo, Özen Sercan-Alp, Mir-Farzin Mashreghi, Jonathan Stefanowski, Pawel Durek, René Riedel, Hyun-Dong Chang, Victor Greiff, Marta Ferreira-Gomes, Cora Klaeden, Mairi McGrath, Kerstin Westendorf, and Sandra Naundorf

Subjects

0301 basic medicine, General Physics and Astronomy, Immunological memory, Transcriptome, 0302 clinical medicine, 610 Medicine & health, lcsh:Science, education.field_of_study, B-Lymphocytes, Multidisciplinary, Cell Cycle, RNA sequencing, Isotype, medicine.anatomical_structure, Antibody, Stromal cell, Science, B-cell receptor, Population, Receptors, Antigen, B-Cell, Vascular Cell Adhesion Molecule-1, Spleen, Animals, Wild, Bone Marrow Cells, Mice, Transgenic, Biology, General Biochemistry, Genetics and Molecular Biology, Article, Antibodies, 03 medical and health sciences, Antigen, Adjuvants, Immunologic, medicine, Animals, ddc:610, education, B cell, Cell Proliferation, B cells, General Chemistry, Immunoglobulin Class Switching, B-1 cell, Mice, Inbred C57BL, 030104 developmental biology, Gene Expression Regulation, Immunology, biology.protein, lcsh:Q, Bone marrow, Stromal Cells, 610 Medizin und Gesundheit, Immunologic Memory, 030215 immunology

Abstract

At present, it is not clear how memory B lymphocytes are maintained over time, and whether only as circulating cells or also residing in particular tissues. Here we describe distinct populations of isotype-switched memory B lymphocytes (Bsm) of murine spleen and bone marrow, identified according to individual transcriptional signature and B cell receptor repertoire. A population of marginal zone-like cells is located exclusively in the spleen, while a population of quiescent Bsm is found only in the bone marrow. Three further resident populations, present in spleen and bone marrow, represent transitional and follicular B cells and B1 cells, respectively. A population representing 10-20% of spleen and bone marrow memory B cells is the only one qualifying as circulating. In the bone marrow, all cells individually dock onto VCAM1+ stromal cells and, reminiscent of resident memory T and plasma cells, are void of activation, proliferation and mobility., Nature Communications, 11 (1), ISSN:2041-1723

Published

2020