Your search keyword '"Marcus Gereke"' showing total 26 results

1. Evaluation of PRRSv specific, maternally derived and induced immune response in Ingelvac PRRSFLEX EU vaccinated piglets in the presence of maternally transferred immunity.

Author

Christian Kraft, Rimma Hennies, Karla Dreckmann, Marta Noguera, Poul Henning Rathkjen, Michael Gassel, and Marcus Gereke

Subjects

Medicine, Science

Abstract

In this study, we analyzed PRRS virus (PRRSv) specific lymphocyte function in piglets vaccinated with Ingelvac PRRSFLEX EU® at two and three weeks of age in the presence of homologous maternal immunity. Complete analysis of maternal immunity to PRRSv was evaluated postpartum, as well as passive transfer of antibodies and T cells to the piglet through colostrum intake and before and after challenge with a heterologous PRRSv at ten weeks of age. Maternal-derived antibodies were detected in piglets but declined quickly after weaning. However, vaccinated animals restored PRRSv-specific antibody levels by anamnestic response to vaccination. Cell analysis in colostrum and milk revealed presence of PRRSv-specific immune cells at suckling with higher concentrations found in colostrum than in milk. In addition, colostrum and milk contained PRRSv-specific IgA and IgG that may contribute to protection of newborn piglets. Despite the presence of PRRSv-specific Peripheral Blood Mononuclear cells (PBMCs) in colostrum and milk, no PRRSv-specific cells could be detected from blood of the piglets at one or two weeks of life. Nevertheless, cellular immunity was detectable in pre-challenged piglets up to 7 weeks after vaccination while the non-vaccinated control group showed no interferon (IFN) γ response to PRRSv stimulation. After challenge, all piglets developed a PRRSv-specific IFNγ-response, which was more robust at significantly higher levels in vaccinated animals compared to the primary response to PRRSv in non-vaccinated animals. Cytokine analysis in the lung lumen showed a reduction of pro-inflammatory responses to PRRSv challenge in vaccinated animals, especially reduced interferon (IFN) α levels. In conclusion, vaccination of maternally positive piglets at 2 and 3 weeks of age with Ingelvac PRRSFLEX EU induced a humoral and cellular immune response to PRRSv and provided protection against virulent, heterologous PRRSv challenge.

Published

2019

2. Gamma secretase dependent release of the CD44 cytoplasmic tail upregulates IFI16 in cd44-/- tumor cells, MEFs and macrophages.

Author

Kristin Schultz, Christina Grieger Lindner, Yong Li, Pavel Urbánek, Anne Ruschel, Kerstin Minnich, Dunja Bruder, Marcus Gereke, Antonio Sechi, and Peter Herrlich

Subjects

Medicine, Science

Abstract

The adhesion molecule and co-receptor of receptor tyrosine kinases, CD44, is expressed in all cells of the immune system, but also in numerous non-immune cells. CD44 plays roles in the cellular response to different pathogens. The molecular actions of CD44 during these processes are by and large still unknown. The CD44 molecule undergoes a sequential proteolytic cleavage which leads to the release of a soluble intracellular domain (CD44-ICD). Previous reports had shown that the CD44-ICD is taken up into the nucleus where it enhances transcription of specific target genes. By RNA profiling we identified a CD44-dependent transcriptional increase of interferon-responsive genes, among them IFI16. IFI16 is important in the innate immune response. It senses and binds pathogenic DNA and, together with cGAS, activates the cGAS-cGAMP-STING pathway and induces the expression of genes relevant for the response, e.g. IFN-β. Our results show that the enhancement of IFI16 expression depended on CD44 cleavage. A CD44-negative tumor cell line, embryonic fibroblasts and bone marrow-derived macrophages from cd44-/- mice were reduced in their response to IFN-γ, to viral DNA fragments and to Listeria monocytogenes infection. We could rescue the deficiency of CD44 negative RPM-MC cells and cd44-/- MEFs by expressing only the soluble CD44-ICD in the absence of any other CD44 domain. Expression of the CD44-ICD carrying a mutation that prevented the uptake into the nucleus, could not rescue the absence of CD44. This molecular aspect of regulation by CD44 may explain part of the immune phenotypes of mice with cd44 gene disruption.

Published

2018

3. Attenuation of immune-mediated influenza pneumonia by targeting the inducible co-stimulator (ICOS) molecule on T cells.

Author

Priya Sakthivel, Marcus Gereke, Angele Breithaupt, Dietmar Fuchs, Luca Gigliotti, Achim D Gruber, Umberto Dianzani, and Dunja Bruder

Subjects

Medicine, Science

Abstract

Inducible Co-stimulator (ICOS) plays a critical role in mediating T cell differentiation and function and is considered a key player in balancing T effector and T regulatory (Treg) cell responses. Here we show that activation of the ICOS signalling pathway during acute influenza A virus (IAV) infection by application of an agonistic ICOS antibody reduced the frequency of CD8+ T cells in the respiratory tract of IAV infected animals and delayed pathogen elimination. In line with this, immune-mediated influenza pneumonia was significantly ameliorated in mice that received ICOS agonist as indicated by significantly reduced alveolar infiltrations and bronchointerstitial pneumonia, while at the same time virus-related pathology remained unaffected. Importantly, ICOS agonist treatment resulted in expansion of CD4+Foxp3+ Tregs in IAV infected mice, which was associated with elevated levels of the immunosuppressive cytokine IL-10 in the alveolar space. Together, our findings suggest a prominent role of ICOS signaling during acute IAV infection by increasing the Treg/CD8+ T cell ratio with beneficial outcome on immune-mediated pneumonia and underline the suitability of ICOS as potential therapeutic target for immune intervention in those infectious conditions characterized by strong immunopathology rather than virus-mediated cytopathic effects.

Published

2014

4. Increased susceptibility for superinfection with Streptococcus pneumoniae during influenza virus infection is not caused by TLR7-mediated lymphopenia.

Author

Sabine Stegemann, Sofia Dahlberg, Andrea Kröger, Marcus Gereke, Dunja Bruder, Birgitta Henriques-Normark, and Matthias Gunzer

Subjects

Medicine, Science

Abstract

Influenza A virus (IAV) causes respiratory tract infections leading to recurring epidemics with high rates of morbidity and mortality. In the past century IAV induced several world-wide pandemics, the most aggressive occurring in 1918 with a death toll of 20-50 million cases. However, infection with IAV alone is rarely fatal. Instead, death associated with IAV is usually mediated by superinfection with bacteria, mainly Streptococcus pneumoniae. The reasons for this increased susceptibility to bacterial superinfection have not been fully elucidated. We previously demonstrated that triggering of TLR7 causes immune incompetence in mice by induction of lymphopenia. IAV is recognized by TLR7 and infections can lead to lymphopenia. Since lymphocytes are critical to protect from S. pneumoniae it has long been speculated that IAV-induced lymphopenia might mediate increased susceptibility to superinfection. Here we show that sub-lethal pre-infections of mice with IAV-PR8/A/34 strongly increased their mortality in non-lethal SP infections, surprisingly despite the absence of detectable lymphopenia. In contrast to SP-infection alone co-infected animals were unable to control the exponential growth of SP. However, lymphopenia forced by TLR7-triggering or antibody-mediated neutropenia did not increase SP-susceptibility or compromise the ability to control SP growth. Thus, the immune-incompetence caused by transient lympho- or leukopenia is not sufficient to inhibit potent antibacterial responses of the host and mechanisms distinct from leukodepletion must account for increased bacterial superinfection during viral defence.

Published

2009

5. Mucosal CD8+ T cell responses induced by an MCMV based vaccine vector confer protection against influenza challenge

Author

Marcus Gereke, Jennifer D. Oduro, Ulrike Heise, Astrid Krmpotić, Julia D. Boehme, Carlos A. Guzmán, Lisa Borkner, Thomas Ebensen, Luka Cicin-Sain, Xiaoyan Zheng, Marina C. Pils, Dunja Bruder, and HZI,Helmholtz-Zentrum für Infektionsforschung GmbH, Inhoffenstr. 7,38124 Braunschweig, Germany.

Subjects

RNA viruses, Muromegalovirus, Cellular immunity, Physiology, Epitopes, T-Lymphocyte, CD8-Positive T-Lymphocytes, medicine.disease_cause, Biochemistry, Epitope, Mice, 0302 clinical medicine, Spectrum Analysis Techniques, Influenza A Virus, H1N1 Subtype, Immune Physiology, Cellular types, Influenza A virus, Cytotoxic T cell, Biology (General), Immune Response, Lung, CD8(+) T-CELLS, MURINE CYTOMEGALOVIRUS-INFECTION, RESIDENT MEMORY, RESPIRATORY-INFECTION, EXPRESSION DEFINES, CMV INFECTION, TISSUE, VIRUS, IMMUNITY, CLEARANCE, Pathology and laboratory medicine, Mice, Inbred BALB C, Vaccines, Synthetic, 0303 health sciences, Immune System Proteins, Chemotaxis, Immune cells, 030302 biochemistry & molecular biology, virus diseases, Medical microbiology, Flow Cytometry, 3. Good health, Vaccination, Cell Motility, Spectrophotometry, Influenza Vaccines, Viruses, White blood cells, Female, Cytophotometry, Pathogens, Chemokines, BIOMEDICINA I ZDRAVSTVO. Temeljne medicinske znanosti, Research Article, Cell biology, Blood cells, QH301-705.5, Genetic Vectors, Immunology, T cells, Cytotoxic T cells, Respiratory Mucosa, Biology, Research and Analysis Methods, Microbiology, Virus, Antibodies, Cell Line, 03 medical and health sciences, Immune system, Immunity, Virology, Influenza, Human, medicine, Genetics, Influenza viruses, Animals, Humans, Amino Acid Sequence, Immunity, Mucosal, Molecular Biology, Administration, Intranasal, 030304 developmental biology, Medicine and health sciences, Biology and life sciences, BIOMEDICINE AND HEALTHCARE. Basic Medical Sciences, Organisms, Viral pathogens, Proteins, Gene Products, env, RC581-607, Peptide Fragments, Microbial pathogens, Animal cells, Immunization, NIH 3T3 Cells, Parasitology, Immunologic diseases. Allergy, Spleen, CD8, 030215 immunology, Orthomyxoviruses

Abstract

Cytomegalovirus (CMV) is a ubiquitous β-herpesvirus that establishes life-long latent infection in a high percentage of the population worldwide. CMV induces the strongest and most durable CD8+ T cell response known in human clinical medicine. Due to its unique properties, the virus represents a promising candidate vaccine vector for the induction of persistent cellular immunity. To take advantage of this, we constructed a recombinant murine CMV (MCMV) expressing an MHC-I restricted epitope from influenza A virus (IAV) H1N1 within the immediate early 2 (ie2) gene. Only mice that were immunized intranasally (i.n.) were capable of controlling IAV infection, despite the greater potency of the intraperitoneally (i.p.) vaccination in inducing a systemic IAV-specific CD8+ T cell response. The protective capacity of the i.n. immunization was associated with its ability to induce IAV-specific tissue-resident memory CD8+ T (CD8TRM) cells in the lungs. Our data demonstrate that the protective effect exerted by the i.n. immunization was critically mediated by antigen-specific CD8+ T cells. CD8TRM cells promoted the induction of IFNγ and chemokines that facilitate the recruitment of antigen-specific CD8+ T cells to the lungs. Overall, our results showed that locally applied MCMV vectors could induce mucosal immunity at sites of entry, providing superior immune protection against respiratory infections., Author summary Vaccines against influenza typically induce immune responses based on antibodies, small molecules that recognize the virus particles outside of cells and neutralize them before they infect a cell. However, influenza rapidly evolves, escaping immune recognition, and the fastest evolution is seen in the part of the virus that is recognized by antibodies. Therefore, every year we are confronted with new flu strains that are not recognized by our antibodies against the strains from previous years. The other branch of the immune system is made of killer T cells, which recognize infected cells and target them for killing. Influenza does not rapidly evolve to escape T cell killing; thus, vaccines inducing T-cell responses to influenza might provide long-term protection. We introduced an antigen from influenza into the murine cytomegalovirus (MCMV) and used it as a vaccine vector inducing killer T-cell responses of unparalleled strength. Our vector controls influenza replication and provides relief to infected mice, but only if we administered it through the nose, to activate killer T cells that will persist in the lungs close to the airways. Therefore, our data show that the subset of lung-resident killer T cells is sufficient to protect against influenza.

Published

2019

6. ADAP plays a pivotal role in CD4+ T cell activation but is only marginally involved in CD8+ T cell activation, differentiation, and immunity to pathogens

Author

Burkhart Schraven, Stefanie Kliche, Gerald P. Parzmair, Michaela Annemann, Annegret Reinhold, Lisa Podlasly, Oxana Haberkorn, Marcus Gereke, and Dunja Bruder

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, T cell, Immunology, Integrin, Mice, Transgenic, CD8-Positive T-Lymphocytes, Biology, Lymphocyte Activation, Proinflammatory cytokine, Epitopes, Interferon-gamma, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Cell Adhesion, medicine, Animals, Immunology and Allergy, Cytotoxic T cell, Adaptor Proteins, Signal Transducing, Cell Proliferation, Immunity, Degranulation, Signal transducing adaptor protein, Cell Differentiation, Cell Biology, Adoptive Transfer, Listeria monocytogenes, Lymphocyte Subsets, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, biology.protein, Receptors, Chemokine, Signal transduction, CD8, 030215 immunology

Abstract

The adhesion and degranulation promoting adaptor protein (ADAP) is a multifunctional scaffold involved in many different signaling pathways that are important for the function of T cells, including the inside-out and outside-in signaling of integrins, the activation of NF-κB, and the subsequent production of proinflammatory cytokines (e.g., IFN-γ and IL-2). Strikingly, despite its well-established role in T cells, previous studies did not distinguish between CD4+ and CD8+ T cells, and thus, it is unknown whether ADAP fulfills equally important functions in both T cell subsets. We show here that despite comparable ADAP expression levels in CD4+ and CD8+ T cells, their function is differentially dependent on ADAP. Whereas in vitro TCR-stimulation experiments revealed that activation, proliferation, and adhesion are severely compromised in CD4+ T cells lacking ADAP, their CD8+ counterparts are hardly affected by ADAP deficiency. Accordingly, antigen-specific in vivo stimulation of adoptively transferred CD8+ T cells during Listeria monocytogenes (Lm) and influenza A virus (IAV) infection revealed only moderate effects of ADAP deficiency in terms of CD8+ T cell activation, proliferation, and differentiation, which, however, did not impair pathogen-specific immunity. Thus, we show for the first time that ADAP fulfills different functions in CD4+ and CD8+ T cells, with CD8+ T cells being less dependent on ADAP. Our data identify ADAP as a potential molecular target for T cell subset-specific therapeutic interventions.

Published

2016

7. Type IIFNs induce anti-tumor polarization of tumor associated neutrophils in mice and human

Author

Ching-Fang Wu, Sven Brandau, Lisa Andzinski, Maren von Köckritz-Blickwede, Jadwiga Jablonska, Bastian Schilling, Stephanie Stahnke, Siegfried Weiss, Marcus Gereke, and Nadine Kasnitz

Subjects

0301 basic medicine, Antitumor activity, Cancer Research, Lung, medicine.diagnostic_test, Melanoma, Neutrophil extracellular traps, Biology, medicine.disease, Phenotype, Flow cytometry, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Oncology, Immunology, medicine, Infiltration (medical), Interferon type I, medicine.drug

Abstract

The importance of tumor associated neutrophils (TANs) in cancer development is in the meantime well established. Numerous of clinical data document the adverse prognostic effects of neutrophil infiltration in solid tumors. However, certain tumor therapies need functional neutrophils to be effective, suggesting altered neutrophil polarization associated with different outcomes for cancer patients. Therefore, modulation of neutrophilic phenotypes represents a potent therapeutic option, but factors mediating neutrophil polarization are still poorly defined. In this manuscript we provide evidence that type I IFNs alter neutrophilic phenotype into anti-tumor, both in mice and human. In the absence of IFN-β, pro-tumor properties, such as reduced tumor cytotoxicity with low neutrophil extracellular traps (NETs) expression, low ICAM1 and TNF-α expression, dominated neutrophil phenotypes in primary lesion and premetastatic lung. Interestingly, such neutrophils have significantly prolonged life-span. Notably, interferon therapy in mice altered TAN polarization towards anti-tumor N1. Similar changes in neutrophil activation could be observed in melanoma patients undergoing type I IFN therapy. Altogether, these data highlight the therapeutic potential of interferons, suggesting optimization of its clinical use as potent anti-tumor agent.

Published

2015

8. Targeted antigen delivery to dendritic cells elicits robust antiviral T cell-mediated immunity in the liver

Author

Thomas Ebensen, Carlos A. Guzmán, Peggy Riese, Marcus Gereke, Lars Philipsen, Robert Klopfleisch, Andreas Müller, Percy A. Knolle, Achim D. Gruber, Sabine Stegemann-Koniszewski, Stefan Lienenklaus, Dunja Bruder, Dirk Wohlleber, Julia Volckmar, and Helmholtz-Zentrum für Infektionsforschung GmbH, Inhoffenstr.7, 38124 Braunschweig, Germany.

Subjects

0301 basic medicine, Ovalbumin, Hepatitis C virus, T cell, Receptors, Cell Surface, Biology, CD8-Positive T-Lymphocytes, medicine.disease_cause, T cell mediated immunity, Virus, Article, Minor Histocompatibility Antigens, 03 medical and health sciences, Cross-Priming, In vivo, Immunity, Antigens, CD, medicine, Animals, Lectins, C-Type, Viral hepatitis, Lymphocyte activation, Multidisciplinary, Toll-Like Receptors, Dendritic Cells, Virology, Mice, Inbred C57BL, TLR2, 030104 developmental biology, medicine.anatomical_structure, Liver, Viral infection, Immunology, Female, Immunization, CD8

Abstract

Hepatotropic viruses such as hepatitis C virus cause life-threatening chronic liver infections in millions of people worldwide. Targeted in vivo antigen-delivery to cross-presenting dendritic cells (DCs) has proven to be extraordinarily efficient in stimulating antigen-specific T cell responses. To determine whether this approach would as well be suitable to induce local antiviral effector T cells in the liver we compared different vaccine formulations based on either the targeting of DEC-205 or TLR2/6 on cross-presenting DCs or formulations not involving in vivo DC targeting. As read-outs we used in vivo hepatotropic adenovirus challenge, histology and automated multidimensional fluorescence microscopy (MELC). We show that targeted in vivo antigen delivery to cross-presenting DCs is highly effective in inducing antiviral CTLs capable of eliminating virus-infected hepatocytes, while control vaccine formulation not involving DC targeting failed to induce immunity against hepatotropic virus. Moreover, we observed distinct patterns of CD8+ T cell interaction with virus-infected and apoptotic hepatocytes in the two DC-targeting groups suggesting that the different vaccine formulations may stimulate distinct types of effector functions. Our findings represent an important step toward the future development of vaccines against hepatotropic viruses and the treatment of patients with hepatic virus infection after liver transplantation to avoid reinfection.

Published

2017

9. Evaluation of PRRSv specific, maternally derived and induced immune response in Ingelvac PRRSFLEX EU vaccinated piglets in the presence of maternally transferred immunity

Author

Poul H. Rathkjen, Marcus Gereke, K. Dreckmann, Rimma Hennies, Michael Gassel, Marta Noguera, and Christian Kraft

Subjects

Cellular immunity, Swine, Physiology, viruses, animal diseases, Lymphocyte, Antibodies, Viral, Biochemistry, Cell-Mediated Immunity, fluids and secretions, Immune Physiology, Medicine and Health Sciences, Public and Occupational Health, Enzyme-Linked Immunoassays, Lung, Breast Milk, Mammals, Immunity, Cellular, Vaccines, Innate Immune System, Immune System Proteins, Multidisciplinary, Vaccination, Eukaryota, virus diseases, respiratory system, Vaccination and Immunization, Body Fluids, Milk, Infectious Diseases, medicine.anatomical_structure, Vertebrates, Cytokines, Medicine, Female, Inflammation Mediators, Anatomy, Antibody, Bronchoalveolar Lavage Fluid, Research Article, Infectious Disease Control, Science, Immunology, Biology, Breast milk, Research and Analysis Methods, Antibodies, Beverages, Interferon-gamma, Immune system, Species Specificity, Immunity, medicine, Animals, Porcine respiratory and reproductive syndrome virus, Viremia, Immunoassays, Nutrition, Colostrum, Organisms, Biology and Life Sciences, Proteins, Molecular Development, Immunity, Humoral, Immunoglobulin A, Diet, Animals, Newborn, Immunoglobulin G, Immune System, Antibody Formation, Amniotes, Immunologic Techniques, biology.protein, Preventive Medicine, Immunity, Maternally-Acquired, Developmental Biology

Abstract

In this study, we analyzed PRRS virus (PRRSv) specific lymphocyte function in piglets vaccinated with Ingelvac PRRSFLEX EU® at two and three weeks of age in the presence of homologous maternal immunity. Complete analysis of maternal immunity to PRRSv was evaluated postpartum, as well as passive transfer of antibodies and T cells to the piglet through colostrum intake and before and after challenge with a heterologous PRRSv at ten weeks of age. Maternal-derived antibodies were detected in piglets but declined quickly after weaning. However, vaccinated animals restored PRRSv-specific antibody levels by anamnestic response to vaccination. Cell analysis in colostrum and milk revealed presence of PRRSv-specific immune cells at suckling with higher concentrations found in colostrum than in milk. In addition, colostrum and milk contained PRRSv-specific IgA and IgG that may contribute to protection of newborn piglets. Despite the presence of PRRSv-specific Peripheral Blood Mononuclear cells (PBMCs) in colostrum and milk, no PRRSv-specific cells could be detected from blood of the piglets at one or two weeks of life. Nevertheless, cellular immunity was detectable in pre-challenged piglets up to 7 weeks after vaccination while the non-vaccinated control group showed no interferon (IFN) γ response to PRRSv stimulation. After challenge, all piglets developed a PRRSv-specific IFNγ-response, which was more robust at significantly higher levels in vaccinated animals compared to the primary response to PRRSv in non-vaccinated animals. Cytokine analysis in the lung lumen showed a reduction of pro-inflammatory responses to PRRSv challenge in vaccinated animals, especially reduced interferon (IFN) α levels. In conclusion, vaccination of maternally positive piglets at 2 and 3 weeks of age with Ingelvac PRRSFLEX EU induced a humoral and cellular immune response to PRRSv and provided protection against virulent, heterologous PRRSv challenge.

Published

2019

10. Cellular-FLIP, Raji isoform (c-FLIPR) modulates cell death induction upon T-cell activation and infection

Author

Nana Ueffing, Frida Ewald, Dunja Bruder, Marc Schuster, Tanja Telieps, Yvonne Rauter, Marcus Gereke, Ingo Schmitz, Dorthe von Smolinski, Michaela Annemann, and Achim D. Gruber

Subjects

Genetically modified mouse, Transgene, T cell, Immunology, HEK 293 cells, Biology, Fas receptor, Cell biology, Haematopoiesis, medicine.anatomical_structure, Immune system, Apoptosis, medicine, Immunology and Allergy

Abstract

Dysregulation of apoptosis caused by an imbalance of pro- and anti-apoptotic protein expression can lead to cancer, neurodegenerative, and autoimmune diseases. Cellular-FLIP (c-FLIP) proteins inhibit apoptosis directly at the death-inducing signaling complex of death receptors, such as CD95, and have been linked to apoptosis regulation during immune responses. While the isoforms c-FLIPL and c-FLIPS are well characterized, the function of c-FLIPR remains poorly understood. Here, we demonstrate the induction of endogenous murine c-FLIPR in activated lymphocytes for the first time. To analyze c-FLIPR function in vivo, we generated transgenic mice expressing murine c-FLIPR specifically in hematopoietic cells. As expected, lymphocytes from c-FLIPR transgenic mice were protected against CD95-induced apoptosis in vitro. In the steady state, transgenic mice had normal cell numbers and unaltered frequencies of B cells and T-cell subsets in lymphoid organs. However, when challenged with Listeria monocytogenes, c-FLIPR transgenic mice showed less liver necrosis and better bacterial clearance compared with infected wild-type mice. We conclude that c-FLIPR expression in hematopoietic cells supports an efficient immune response against bacterial infections.

Published

2013

11. Alveolar Type II Epithelial Cells Contribute to the Anti-Influenza A Virus Response in the Lung by Integrating Pathogen- and Microenvironment-Derived Signals

Author

Sabine Stegemann-Koniszewski, Robert Geffers, Andreas Jeron, Matthias Gunzer, Marcus Gereke, Dunja Bruder, Andrea Kröger, and Helmholtz Centre for infection research, Inhoffenstr. 7, 38124 Braunschweig, Germany.

Subjects

0301 basic medicine, Population, Antigen presentation, Medizin, Biology, medicine.disease_cause, Microbiology, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Orthomyxoviridae Infections, Interferon, Immunity, Virology, medicine, Influenza A virus, Leukocytes, Animals, education, Lung, education.field_of_study, Effector, Gene Expression Profiling, QR1-502, Disease Models, Animal, 030104 developmental biology, 030220 oncology & carcinogenesis, Alveolar Epithelial Cells, Immunology, Interferons, Ex vivo, medicine.drug, Research Article

Abstract

Influenza A virus (IAV) periodically causes substantial morbidity and mortality in the human population. In the lower lung, the primary targets for IAV replication are type II alveolar epithelial cells (AECII), which are increasingly recognized for their immunological potential. So far, little is known about their reaction to IAV and their contribution to respiratory antiviral immunity in vivo. Therefore, we characterized the AECII response during early IAV infection by analyzing transcriptional regulation in cells sorted from the lungs of infected mice. We detected rapid and extensive regulation of gene expression in AECII following in vivo IAV infection. The comparison to transcriptional regulation in lung tissue revealed a strong contribution of AECII to the respiratory response. IAV infection triggered the expression of a plethora of antiviral factors and immune mediators in AECII with a high prevalence for interferon-stimulated genes. Functional pathway analyses revealed high activity in pathogen recognition, immune cell recruitment, and antigen presentation. Ultimately, our analyses of transcriptional regulation in AECII and lung tissue as well as interferon I/III levels and cell recruitment indicated AECII to integrate signals provided by direct pathogen recognition and surrounding cells. Ex vivo analysis of AECII proved a powerful tool to increase our understanding of their role in respiratory immune responses, and our results clearly show that AECII need to be considered a part of the surveillance and effector system of the lower respiratory tract., IMPORTANCE In order to confront the health hazard posed by IAV, we need to complete our understanding of its pathogenesis. AECII are primary targets for IAV replication in the lung, and while we are beginning to understand their importance for respiratory immunity, the in vivo AECII response during IAV infection has not been analyzed. In contrast to studies addressing the response of AECII infected with IAV ex vivo, we have performed detailed gene transcriptional profiling of AECII isolated from the lungs of infected mice. Thereby, we have identified an exceptionally rapid and versatile response to IAV infection that is shaped by pathogen-derived as well as microenvironment-derived signals and aims at the induction of antiviral measures and the recruitment and activation of immune cells. In conclusion, our study presents AECII as active players in antiviral defense in vivo that need to be considered part of the sentinel and effector immune system of the lung.

Published

2016

12. Abscisic Acid: A Phytohormone and Mammalian Cytokine as Novel Pharmacon with Potential for Future Development into Clinical Applications

Author

Niharika Sharma, Priya Sakthivel, Dunja Bruder, Philipp Klahn, and Marcus Gereke

Subjects

0301 basic medicine, medicine.medical_treatment, Cell, Inflammation, Disease, Biology, Bioinformatics, Biochemistry, Regenerative medicine, Communicable Diseases, 03 medical and health sciences, chemistry.chemical_compound, Immune system, Drug Discovery, medicine, Animals, Humans, Abscisic acid, Pharmacon, Pharmacology, organic chemicals, fungi, Organic Chemistry, Anti-Inflammatory Agents, Non-Steroidal, food and beverages, Mesenchymal Stem Cells, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Cytokine, chemistry, Molecular Medicine, medicine.symptom, Abscisic Acid

Abstract

The isoprenoid stress-associated phytohormone abscisic acid (ABA) has recently been recognized to possess multifaceted biological functions in mammals and to exert potent curative effects in a number of clinically relevant human diseases. Studies with human specimens have unequivocally shown that ABA retains its stress-related functional attributes, previously identified in plants, which contribute to enhanced inflammatory defense mechanisms in mammals. Besides, studies performed in animal models revealed prominent anti-inflammatory properties of ABA as indicated by a marked reduction of immune cell infiltrates at the sites of inflammation. Thus, ABA treatment ultimately leads to the profound improvement of both non-communicable and communicable diseases which are associated with an overall alleviated course of inflammation. In addition to its action on the mammalian immune system, ABA was also shown to exert diverse physiological functions on non-immune components. One of the most remarkable features of ABA is to stimulate and expand mesenchymal stem cells, which may open a new avenue for its potential use in the field of regenerative medicine. Furthermore, ABA has been reported to play an important role in the maintenance of glycemic control. In this review, we summarize current understanding of the significance of ABA in the mammalian system, its prophylactic and therapeutic effects in various disease settings and the future directions for the development of ABA as novel drug candidate for the improved treatment of inflammatory and infectious human diseases.

Published

2016

13. CD8+ T Cells Responding to Alveolar Self-Antigen Lack CD25 Expression and Fail to Precipitate Autoimmunity

Author

Milena J. Tosiek, Marcus Gereke, Dunja Bruder, Jan Buer, Sophie R. Bader, and Achim D. Gruber

Subjects

Cytotoxicity, Immunologic, Pulmonary and Respiratory Medicine, T cell, Clinical Biochemistry, Medizin, Mice, Transgenic, CD8-Positive T-Lymphocytes, Biology, pulmonary inflammation, Autoantigens, chronic obstructive pulmonary disease, Mice, Interleukin 21, Antigen, medicine, Animals, Cytotoxic T cell, IL-2 receptor, Molecular Biology, Cell Proliferation, Mice, Inbred BALB C, autoimmunity, Interleukin-2 Receptor alpha Subunit, Peripheral tolerance, Cell Differentiation, Cell Biology, CD8+ T lymphocytes, Natural killer T cell, Adoptive Transfer, peripheral tolerance, Pulmonary Alveoli, medicine.anatomical_structure, Immunology, Interleukin 12, Interleukin-2, Inflammation Mediators, Signal Transduction

Abstract

Although the contribution of CD8(+) T cells to the pathogenesis of noncommunicable lung diseases has become increasingly appreciated, our knowledge about the mechanisms controlling self-reactive CD8(+) T cells in the respiratory tract remains largely elusive. The outcome of the encounter between pulmonary self-antigen and naive CD8(+) T cells, in the presence or absence of inflammation, was traced after adoptive transfer of fluorescence-labeled CD8(+) T cells specific for the neo-self-antigen influenza A hemagglutinin into transgenic mice expressing hemagglutinin specifically in alveolar type II epithelial cells in order: to study the outcome of alveolar antigen encounter in the steady state and under inflammatory conditions; to define the phenotype and fate of CD8(+) T cells primed in the respiratory tract; and, finally, to correlate these findings with the onset of autoimmunity in the lung. We found that CD8(+) T cells remain ignorant in the steady state, whereas transient proliferation of self-reactive CD8(+) T cells is induced by forced maturation or licensing of dendritic cells, increases in the antigenic threshold, and targeted release of alveolar self-antigen by epithelial injury. However, these cells fail to acquire effector functions, lack the expression of the high-affinity IL-2 receptor CD25, and do not precipitate autoimmunity in the lung. We conclude that inadvertent activation of CD8(+) T cells in the lung is prevented in the absence of "danger signals," whereas tissue damage after infection or noninfectious inflammation creates an environment that allows the priming of previously ignorant T cells. Failure in effector cell differentiation after abortive priming, however, precludes the establishment of self-perpetuating autoimmunity in the lung.

Published

2012

14. Impact of enzymatic tissue disintegration on the level of surface molecule expression and immune cell function

Author

Andrea Autengruber, Marcus Gereke, Gesine Prof. Dr. Hansen, Dunja Bruder, and Christian Hennig

Subjects

chemistry.chemical_classification, medicine.diagnostic_test, Biology, In vitro, Flow cytometry, Cell biology, Immune system, Enzyme, chemistry, Dispase, Immunology, medicine, Collagenase, Liberation, Original Article, CD8, medicine.drug

Abstract

Immunological characterization of immune cells that reside in specific anatomic compartments often requires their isolation from the respective tissue on the basis of enzymatic tissue disintegration. Applying enzymatic digestion of primary splenocytes, we evaluated the impact of collagenase and dispase, two enzymes that are commonly used for the liberation of immune cells from tissues, on the detectability of 48 immunologically relevant surface molecules that are frequently used for flow cytometric identification, isolation, and characterization of immune cell subsets. Whereas collagenase treatment had only minor effects on surface expression of most molecules tested, dispase treatment considerably affected antibody-mediated detectability of the majority of surface markers in subsequent FACS analyses. This effect was long lasting and, in case of high-dose dispase treatment, evident for the majority of surface molecules even after 24 h of in vitro culture. Of note, high-dose dispase treatment not only affected surface expression of certain molecules but also impaired antigen-specific proliferation of CD4(+) and CD8(+) T cells. Together, our data indicate that enzymatic tissue disintegration can have profound effects on the expression of a variety of cell-surface molecules with direct consequences for phenotypic analysis, FACS- and MACS-based target cell isolation, and immune cell function in cell culture experiments.

Published

2012

15. Therapeutic Intervention in Cancer and Chronic Viral Infections: Antibody Mediated Manipulation of PD-1/PD-L1 Interaction

Author

Priya Sakthivel, Dunja Bruder, and Marcus Gereke

Subjects

Pharmacology, business.industry, medicine.medical_treatment, T cell, Programmed Cell Death 1 Receptor, Peripheral tolerance, General Medicine, Immunotherapy, Antibodies, B7-H1 Antigen, T cell mediated immunity, Immune system, medicine.anatomical_structure, Virus Diseases, Neoplasms, Chronic Disease, Immunology, medicine, Humans, Drug Therapy, Combination, IL-2 receptor, business, Viral load, CD8

Abstract

Programmed Death-1 (PD-1) is a negative regulator of T cell activation and proliferation that mediates suppressive action by binding to its ligands PD-L1 and PD-L2. The well-established immunosuppressive properties of PD-1/PD-L1 interaction resulting in the re-establishment of peripheral tolerance makes PD-1 an interesting target for therapeutic intervention in cancer patients. In addition to its relevance in tumor-specific immunity, recent studies demonstrate that PD-1 expression on T cells correlates with viral load in HIV and HCV infected patients and further identified PD-1 expression as a marker for exhausted virus-specific CD8+ T cells. In particular, PD-1+CD8+ T cells show impaired effector functions and PD-1 associated T cell exhaustion could be restored by blocking the PD-1/PD-L1 interaction. This results in recovery of virus-specific CD8+ T cell mediated immunity, suggesting that interrupting PD-1 signaling using an antagonistic antibody restores T-cell effector functions. Thus, immunotherapy based on the blockade of PD-1/PD-L1 interaction does not only result in breakdown of effector T-cell tolerance to tumor antigens, but in addition also represents a promising therapeutic strategy for reactivation of virus-specific effector T cells to exert pathogen eradication in chronic viral infections. In this review, we give a comprehensive overview about the immunological functions of PD-1 mediated signaling in T cells with special emphasis on its immune regulatory functions in the context of cancer and chronic viral infections. Moreover, we will summarize recent data obtained in animal models, in-vitro preclinical approaches in patients and their implementation in clinical trials for treating patients with cancer and chronic viral infections.

Published

2012

16. Respiratory Bordetella bronchiseptica Carriage is Associated with Broad Phenotypic Alterations of Peripheral CD4+CD25+ T Cells and Differentially Affects Immune Responses to Secondary Non-Infectious and Infectious Stimuli in Mice

Author

Julia D. Boehme, Marcus Gereke, Robert Geffers, Carlos A. Guzmán, Andreas Jeron, Jens Schreiber, Dunja Bruder, Sabine Stegemann-Koniszewski, Tetyana Yevsa, Julia Volckmar, and HZI,Helmholtz-Zentrum für Infektionsforschung GmbH, Inhoffenstr. 7,38124 Braunschweig, Germany.

Subjects

0301 basic medicine, Adaptive Immunity, T-Lymphocytes, Regulatory, regulatory T cells, lcsh:Chemistry, Mice, 0302 clinical medicine, IL-2 receptor, Respiratory system, Respiratory Tract Infections, lcsh:QH301-705.5, Spectroscopy, Mice, Inbred BALB C, Bordetella bronchiseptica, Coinfection, FOXP3, General Medicine, Antibodies, Bacterial, Computer Science Applications, medicine.anatomical_structure, Carrier State, respiratory microbial carriage, polymicrobial interactions, T cell, Secondary infection, Biology, CD5 Antigens, respiratory immune regulation, Article, Catalysis, Inorganic Chemistry, 03 medical and health sciences, Immune system, medicine, Animals, influenza A virus, Physical and Theoretical Chemistry, Molecular Biology, Bordetella Infections, Organic Chemistry, vaccination, biology.organism_classification, Listeria monocytogenes, secondary infections, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Immunology, 030215 immunology, Respiratory tract

Abstract

The respiratory tract is constantly exposed to the environment and displays a favorable niche for colonizing microorganisms. However, the effects of respiratory bacterial carriage on the immune system and its implications for secondary responses remain largely unclear. We have employed respiratory carriage with Bordetella bronchiseptica as the underlying model to comprehensively address effects on subsequent immune responses. Carriage was associated with the stimulation of Bordetella-specific CD4+, CD8+, and CD4+CD25+Foxp3+ T cell responses, and broad transcriptional activation was observed in CD4+CD25+ T cells. Importantly, transfer of leukocytes from carriers to acutely B. bronchiseptica infected mice, resulted in a significantly increased bacterial burden in the recipient&rsquo, s upper respiratory tract. In contrast, we found that respiratory B. bronchiseptica carriage resulted in a significant benefit for the host in systemic infection with Listeria monocytogenes. Adaptive responses to vaccination and influenza A virus infection, were unaffected by B. bronchiseptica carriage. These data showed that there were significant immune modulatory processes triggered by B. bronchiseptica carriage, that differentially affect subsequent immune responses. Therefore, our results demonstrated the complexity of immune regulation induced by respiratory bacterial carriage, which can be beneficial or detrimental to the host, depending on the pathogen and the considered compartment.

Published

2018

17. CD4 T Lymphocyte–mediated Lung Disease

Author

Robert Geffers, Richard I. Enelow, Jan Buer, Astrid M. Westendorf, Achim D. Gruber, Marcus Gereke, and Dunja Bruder

Subjects

CD4-Positive T-Lymphocytes, Pulmonary and Respiratory Medicine, T cell, Genes, MHC Class II, Autoimmunity, Mice, Transgenic, Inflammation, Critical Care and Intensive Care Medicine, Major histocompatibility complex, Autoimmune Diseases, Mice, Antigen, Intensive care, medicine, Animals, biology, business.industry, Gene Expression Profiling, T-cell receptor, Peripheral tolerance, T lymphocyte, Pulmonary Surfactant-Associated Protein C, Hemagglutinins, Self Tolerance, medicine.anatomical_structure, Chronic Disease, Immunology, biology.protein, medicine.symptom, Lung Diseases, Interstitial, business

Abstract

Although considerable evidence indicates a role for CD4(+) T lymphocytes (T cells) in airway inflammation, little data exist regarding the mechanisms underlying the induction and regulation of CD4(+) T cell reactivity to lung-specific antigens. To dissect the immunologic and molecular mechanisms of CD4(+) T cell dysregulation, reactivity to a self-antigen expressed in the lung of mice bearing a major histocompatibility complex class-II-restricted T cell receptor specific for this antigen was studied. Transgenic mice developed a progressive interstitial pneumonitis characterized by massive lymphocytic and plasmacytic infiltration of interalveolar septa, a clinical picture closely resembling some of the interstitial lung diseases. Pulmonary inflammation reached a plateau state in older mice with prominent formation of lymphoid follicles but reduced interstitial infiltration. Extensive immunologic characterization of self-reactive CD4(+) T cells isolated from the inflamed lung suggested the induction of regulatory T cells in the site of inflammation. Moreover, inflammation was accompanied by broad changes in the gene expression pattern toward a profile partially resembling that of activated, but strikingly, also that of regulatory CD4(+) T cells. Together our data provide important insights into functional and molecular alterations being associated with the induction and/or regulation of T cell-mediated pulmonary inflammation.

Published

2004

18. Attenuation of immune-mediated influenza pneumonia by targeting the inducible co-stimulator (ICOS) molecule on T cells

Author

Achim D. Gruber, Priya Sakthivel, Angele Breithaupt, Luca Gigliotti, Marcus Gereke, Dietmar Fuchs, Dunja Bruder, and Umberto Dianzani

Subjects

Viral Diseases, Infectious Disease Control, medicine.medical_treatment, T cell, Immunology, lcsh:Medicine, Biology, CD8-Positive T-Lymphocytes, medicine.disease_cause, Inducible T-Cell Co-Stimulator Protein, Immunomodulation, Mice, Immune system, Orthomyxoviridae Infections, medicine, Influenza A virus, Medicine and Health Sciences, Cytotoxic T cell, Animals, Humans, Molecular Targeted Therapy, lcsh:Science, Lung, Immunity to Infections, Multidisciplinary, lcsh:R, FOXP3, Biology and Life Sciences, Pneumonia, Interleukin-10, Interleukin 10, Cytokine, medicine.anatomical_structure, Infectious Diseases, Female, Clinical Immunology, lcsh:Q, CD8, Research Article

Abstract

Inducible Co-stimulator (ICOS) plays a critical role in mediating T cell differentiation and function and is considered a key player in balancing T effector and T regulatory (Treg) cell responses. Here we show that activation of the ICOS signalling pathway during acute influenza A virus (IAV) infection by application of an agonistic ICOS antibody reduced the frequency of CD8+ T cells in the respiratory tract of IAV infected animals and delayed pathogen elimination. In line with this, immune-mediated influenza pneumonia was significantly ameliorated in mice that received ICOS agonist as indicated by significantly reduced alveolar infiltrations and bronchointerstitial pneumonia, while at the same time virus-related pathology remained unaffected. Importantly, ICOS agonist treatment resulted in expansion of CD4+Foxp3+ Tregs in IAV infected mice, which was associated with elevated levels of the immunosuppressive cytokine IL-10 in the alveolar space. Together, our findings suggest a prominent role of ICOS signaling during acute IAV infection by increasing the Treg/CD8+ T cell ratio with beneficial outcome on immune- mediated pneumonia and underline the suitability of ICOS as potential therapeutic target for immune intervention in those infectious conditions characterized by strong immunopathology rather than virus-mediated cytopathic effects.

Published

2014

19. TLR7 contributes to the rapid progression but not to the overall fatal outcome of secondary pneumococcal disease following influenza A virus infection

Author

Shizuo Akira, Matthias Gunzer, Bastian Pasche, Birgitta Henriques-Normark, Sofia Orrskog, Stefan Lienenklaus, Achim D. Gruber, Sabine Stegemann-Koniszewski, Sophie R. Bader, Dunja Bruder, Siegfried Weiss, Marcus Gereke, and Immune Regulation Group, Helmholtz Centre for Infection Research, Braunschweig, Germany.

Subjects

Fatal outcome, Medizin, Biology, medicine.disease_cause, Virus, Pneumococcal Infections, Madin Darby Canine Kidney Cells, Mice, Dogs, Phagocytosis, Streptococcus pneumoniae, Influenza, Human, medicine, Influenza A virus, Immunology and Allergy, Animals, Humans, Receptor, Mice, Knockout, Innate immune system, Membrane Glycoproteins, virus diseases, TLR7, Interferon-beta, Virology, Mice, Inbred C57BL, Toll-Like Receptor 7, Superinfection, Immunology, Disease Progression, Bacterial superinfection, Research Article

Abstract

Increased risk for bacterial superinfections substantially contributes to the mortality caused by influenza A virus (IAV) epidemics. While the mechanistic basis for this lethal synergism is still insufficiently understood, immune modulation through the viral infection has been shown to be involved. Since the pattern-recognition receptor (PRR) toll-like receptor 7 (TLR7) is a major sensor for the viral genome, we studied how IAV recognition by TLR7 influences the development of secondary pneumococcal infection. In a mouse model of IAV, TLR7-deficient hosts induced a potent antiviral response and showed unchanged survival. In secondary pneumococcal infection during acute influenza, TLR7ko mice showed a fatal outcome similar to wild-type (WT) hosts, despite significantly delayed disease progression. Also, when bacterial superinfection occurred after virus clearance, WT and TLR7-deficient hosts showed similar mortality, even though we found the phagocytic activity of alveolar macrophages isolated from IAV-pre-infected hosts to be enhanced in TLR7ko over WT mice. Thus, we show that a virus-sensing PRR modulates the progression of secondary pneumococcal infection following IAV. However, the fatal overall outcome in WT as well as TLR7ko hosts suggests that processes distinct from TLR7-triggering override the contribution of this single PRR.

Published

2013

20. Flow Cytometric Isolation of Primary Murine Type II Alveolar Epithelial Cells for Functional and Molecular Studies

Author

Dunja Bruder, Sabine Stegemann-Koniszewski, Lothar Gröbe, Marcus Gereke, Andreas Jeron, and Andrea Autengruber

Subjects

Cell type, medicine.medical_treatment, General Chemical Engineering, Population, Cell, Immunology, Biology, CD19, General Biochemistry, Genetics and Molecular Biology, Flow cytometry, Mice, medicine, Animals, education, education.field_of_study, medicine.diagnostic_test, General Immunology and Microbiology, General Neuroscience, Epithelial Cells, Cell sorting, Flow Cytometry, Cell biology, Pulmonary Alveoli, Cytokine, medicine.anatomical_structure, Cell culture, biology.protein

Abstract

Throughout the last years, the contribution of alveolar type II epithelial cells (AECII) to various aspects of immune regulation in the lung has been increasingly recognized. AECII have been shown to participate in cytokine production in inflamed airways and to even act as antigen-presenting cells in both infection and T-cell mediated autoimmunity (1-8). Therefore, they are especially interesting also in clinical contexts such as airway hyper-reactivity to foreign and self-antigens as well as infections that directly or indirectly target AECII. However, our understanding of the detailed immunologic functions served by alveolar type II epithelial cells in the healthy lung as well as in inflammation remains fragmentary. Many studies regarding AECII function are performed using mouse or human alveolar epithelial cell lines (9-12). Working with cell lines certainly offers a range of benefits, such as the availability of large numbers of cells for extensive analyses. However, we believe the use of primary murine AECII allows a better understanding of the role of this cell type in complex processes like infection or autoimmune inflammation. Primary murine AECII can be isolated directly from animals suffering from such respiratory conditions, meaning they have been subject to all additional extrinsic factors playing a role in the analyzed setting. As an example, viable AECII can be isolated from mice intranasally infected with influenza A virus, which primarily targets these cells for replication (13). Importantly, through ex vivo infection of AECII isolated from healthy mice, studies of the cellular responses mounted upon infection can be further extended. Our protocol for the isolation of primary murine AECII is based on enzymatic digestion of the mouse lung followed by labeling of the resulting cell suspension with antibodies specific for CD11c, CD11b, F4/80, CD19, CD45 and CD16/CD32. Granular AECII are then identified as the unlabeled and sideward scatter high (SSC(high)) cell population and are separated by fluorescence activated cell sorting (3). In comparison to alternative methods of isolating primary epithelial cells from mouse lungs, our protocol for flow cytometric isolation of AECII by negative selection yields untouched, highly viable and pure AECII in relatively short time. Additionally, and in contrast to conventional methods of isolation by panning and depletion of lymphocytes via binding of antibody-coupled magnetic beads (14, 15), flow cytometric cell-sorting allows discrimination by means of cell size and granularity. Given that instrumentation for flow cytometric cell sorting is available, the described procedure can be applied at relatively low costs. Next to standard antibodies and enzymes for lung disintegration, no additional reagents such as magnetic beads are required. The isolated cells are suitable for a wide range of functional and molecular studies, which include in vitro culture and T-cell stimulation assays as well as transcriptome, proteome or secretome analyses (3, 4).

Published

2012

21. New insights into the molecular pathology of radiation-induced pneumopathy

Author

Therese Eldh, Ute Fischer, Klaus Schulze-Osthoff, David Köhler, Federica Cappuccini, Marcus Gereke, Dunja Bruder, Verena Jendrossek, Martin Stuschke, Holger Jastrow, and Institute of Cell Biology (Cancer Research), University Hospital Essen, Germany.

Subjects

Pathology, medicine.medical_specialty, Pulmonary Fibrosis, Medizin, Apoptosis, Radiation Dosage, Mice, Random Allocation, Immune system, Fibrosis, Reference Values, Albumins, Medicine, Animals, Radiology, Nuclear Medicine and imaging, Pathology, Molecular, Lung, Pneumonitis, Peroxidase, Analysis of Variance, medicine.diagnostic_test, business.industry, Dose-Response Relationship, Radiation, Hematology, respiratory system, Total body irradiation, Thorax, medicine.disease, respiratory tract diseases, Mice, Inbred C57BL, Radiation Pneumonitis, Disease Models, Animal, Bronchoalveolar lavage, medicine.anatomical_structure, Oncology, Immunohistochemistry, Cytokines, business, Bronchoalveolar Lavage Fluid, Whole-Body Irradiation

Abstract

Background and purpose Pneumonitis and fibrosis constitute dose-limiting side effects of thorax or total body irradiation. An improved understanding of the underlying mechanisms is a prerequisite for the development of effective radioprotective strategies. Here we characterized the behavior of resident and immune cells in a murine model of radiation-induced pneumopathy. Materials and methods Wild type (WT) or RAG-2 deficient C57BL/6 mice received 15 Gray of (hemi)-thorax irradiation in a single dose. Bronchoalveolar lavage fluid (BALF) and lung tissue were collected at defined time points post-irradiation for the determination of apoptosis, microvascular injury, and histological and immunohistochemical analyses. Results Higher albumin levels and increased apoptosis were detected in the BALF 21days after irradiation, indicative for delayed damage to resident cells. Irradiation also induced time-dependent changes in the BALF cytokine profile, the recruitment of activated T-cells into the lung and the formation of lipid-loaded resident cells. Lung fibrosis occurred earlier in RAG-2 −/− mice, which lack mature T and B cells, compared to WT mice. Conclusions Thorax irradiation triggers a delayed disturbance of tissue integrity and lipid metabolism in the lung. Activated T-lymphocytes infiltrating the lung tissue upon thorax irradiation participate in the protection of the lung from radiation-induced fibrosis.

Published

2011

22. Na+/H+ exchanger isoform NHE3 and NHERF adaptor protein expression, localization and function in the small and large intestine of CD45RB high transfer colitis

Author

Mingmin Chen, Marcus Gereke, Brigitte Riederer, Maria Lünnemann, Sunil Yeruva, Julia Goldstein, Dunja Bruder, Ursula Seidler, Anurag K. Singh, and Michael P. Manns

Subjects

Gene isoform, Chemistry, Signal transducing adaptor protein, medicine.disease, Biochemistry, Cell biology, Sodium–hydrogen antiporter, medicine.anatomical_structure, Genetics, medicine, Large intestine, Colitis, Molecular Biology, Function (biology), Biotechnology

Published

2009

23. Phenotypic alterations in type II alveolar epithelial cells in CD4+ T cell mediated lung inflammation

Author

Marcus Gereke, Silvia Prettin, Dunja Bruder, Stefanie Deppenmeier, Michael Kasper, Richard I. Enelow, Jan Buer, Lothar Gröbe, Achim D. Gruber, and Helmholtz Center for Infection Research, Inhoffenstr. 7, D-38124 Braunschweig, Germany

Subjects

Pulmonary and Respiratory Medicine, CD4-Positive T-Lymphocytes, Chemokine, medicine.medical_treatment, T cell, Mice, Transgenic, Inflammation, Respiratory Mucosa, Lung injury, Immunophenotyping, Alveolar cells, Mice, Antigen, medicine, Animals, Lung, lcsh:RC705-779, Mice, Inbred BALB C, biology, Research, T-cell receptor, lcsh:Diseases of the respiratory system, respiratory system, Pulmonary Alveoli, Cytokine, medicine.anatomical_structure, Gene Expression Regulation, Immunology, biology.protein, Cancer research, medicine.symptom

Abstract

Background Although the contribution of alveolar type II epithelial cell (AEC II) activities in various aspects of respiratory immune regulation has become increasingly appreciated, our understanding of the contribution of AEC II transcriptosome in immunopathologic lung injury remains poorly understood. We have previously established a mouse model for chronic T cell-mediated pulmonary inflammation in which influenza hemagglutinin (HA) is expressed as a transgene in AEC II, in mice expressing a transgenic T cell receptor specific for a class II-restricted epitope of HA. Pulmonary inflammation in these mice occurs as a result of CD4+ T cell recognition of alveolar antigen. This model was utilized to assess the profile of inflammatory mediators expressed by alveolar epithelial target cells triggered by antigen-specific recognition in CD4+ T cell-mediated lung inflammation. Methods We established a method that allows the flow cytometric negative selection and isolation of primary AEC II of high viability and purity. Genome wide transcriptional profiling was performed on mRNA isolated from AEC II isolated from healthy mice and from mice with acute and chronic CD4+ T cell-mediated pulmonary inflammation. Results T cell-mediated inflammation was associated with expression of a broad array of cytokine and chemokine genes by AEC II cell, indicating a potential contribution of epithelial-derived chemoattractants to the inflammatory cell parenchymal infiltration. Morphologically, there was an increase in the size of activated epithelial cells, and on the molecular level, comparative transcriptome analyses of AEC II from inflamed versus normal lungs provide a detailed characterization of the specific inflammatory genes expressed in AEC II induced in the context of CD4+ T cell-mediated pneumonitis. Conclusion An important contribution of AEC II gene expression to the orchestration and regulation of interstitial pneumonitis is suggested by the panoply of inflammatory genes expressed by this cell population, and this may provide insight into the molecular pathogenesis of pulmonary inflammatory states. CD4+ T cell recognition of antigen presented by AEC II cells appears to be a potent trigger for activation of the alveolar cell inflammatory transcriptosome.

Published

2007

24. The Mechanism of Type I Interferon-Mediated Polarization of Tumor-Associated Neutrophils in Mice and Human

Author

Jadwiga Jablonska, Nadine Kasnitz, Lisa Andzinski, Ching-Fang Wu, Lothar Kanz, Maren von Köckritz-Blickwede, Marcus Gereke, Bastian Schilling, Edyta Zyla, Siegfried Weiss, Julia Skokowa, Karl Welte, Sven Brandau, Mozhgan Dehghan Harati, and Stephanie Stahnke

Subjects

Chemokine, Tumor microenvironment, Immunology, Nicotinamide phosphoribosyltransferase, Inflammation, Cell Biology, Hematology, MMP9, Biology, Biochemistry, S100A9, chemistry.chemical_compound, Blood serum, chemistry, Interferon, medicine, biology.protein, Cancer research, medicine.symptom, medicine.drug

Abstract

Neutrophils are the most abundant cells of all white blood cells and play a key role in host inflammatory responses. Importantly, inflammation has been associated with increased susceptibility for cancer and neutrophils, as a crucial component of this process, play essential role in inflammation-driven tumorigenesis. Neutrophils also represent an independent prognostic marker in a broad variety of neoplasias. The tumor microenvironment represents a special niche that is extremely influencing infiltrating immune cells. The concept of immune cell polarization was first described for macrophages (anti-tumor M1/pro-tumor M2). Recently neutrophil polarization has been postulated. Neutrophils appear to have diverse phenotypes in the tumor microenvironment i.e. tumor promoting (N2) or inhibiting (N1). Previously, we could show that significantly elevated numbers of neutrophils accumulate in tumors of mice that lack endogenous type I IFNs (Ifnb1-/-). Such tumor associated neutrophils (TANs) do not only efficiently support tumor angiogenesis and growth by up-regulating pro-angiogenic molecules (VEGF and MMP9), but also secrete higher amounts of neutrophil-attracting chemokines and display prolonged survival, compared to their WT counterparts thus representing pro-tumor N2 phenotype. Moreover, we could show that these N2 neutrophils efficiently support metastatic processes, due to up-regulation of pro-metastatic proteins, like Bv8, MMP9, S100A8 and S100A9, and due to impaired tumor cell killing. Treatment of such cells with rmIFNb reversed such an effect leading to anti-tumor N1 polarization. Here, we add further evidence emphasizing the importance of type I IFNs for neutrophil polarization in tumor microenvironment and reveal possible mechanism responsible for this phenomenon. In Ifnb1-/- mice, we observe a significant down-regulation of anti-tumor neutrophil markers, like ICAM1 and TNF-α. Moreover, neutrophils show reduced formation of NETs, accompanied by lower tumor killing capacity. Under these conditions, massively enhanced neutrophil turnover in combination with accumulation of immature neutrophils is observed. Importantly, therapeutic intervention in both Ifnb1-/- and WT mice using low dose IFN-β, induced anti-tumor activation of neutrophils. Correspondingly, in human melanoma patients undergoing type I IFN therapy, neutrophil anti-tumor characteristics were augmented, compared to untreated patients, suggesting effective outcome of this therapy. Further, we evaluated the mechanism of prolonged neutrophil survival in the absence of endogenous IFN-β. Importantly, we found that G-CSF mRNA expression levels in Ifnb1-/- neutrophils from different anatomical compartments as well as G-CSF blood serum levels were markedly up-regulated in such mice. G-CSF-expression levels were strongly reduced when the Ifnb1-/- neutrophils were incubated with rmIFN-β suggesting involvement of type I interferons in G-CSF down-regulation. Notably, we could recently show that G-CSF induces synthesis of enzyme Nicotinamide phosphoribosyltransferase (NAMPT), which is a rate-limiting enzyme converting nicotinamide (NA) into NAD+ that in turn activates NAD+ -dependent protein deacetylases sirtuins (SIRTs). NAMPT serves as an inhibitor of neutrophil apoptosis and as neutrophil chemoattractant by upregulation of CXCL8. It is a potent pro-inflammatory factor (upregulation of ROS release) and pro-angiogenic factor (smooth muscle maturation). At the same time, NAMPT was found to be strongly overexpressed in tumors and serum of leukemia patients. Analysis of NAMPT and SIRTs levels in tumor bearing Ifnb1-/- mice revealed highly upregulated levels of NAMPT and SIRT1 in blood neutrophils of these animals, in comparison to WT mice, which was in line with elevated levels of G-CSF. It also correlates with enhanced tumor angiogenesis, growth and metastasis. Based on these observations, we identified a new mechanism of interferon-mediated activation of pro-tumor neutrophils. Since tumor associated neutrophils represent a highly potent therapeutic target, these data highlight the therapeutic potential of interferons and NAMPT inhibitors, suggesting optimization of their clinical use as potent anti-tumor agent. Disclosures No relevant conflicts of interest to declare.

Published

2015

25. Immune regulation in CD8+ T cell-mediated pulmonary disease

Author

Milena J. Tosiek, Dunja Bruder, Achim D. Gruber, and Marcus Gereke

Subjects

business.industry, Immunology, Immune regulation, Immunology and Allergy, Medicine, Cytotoxic T cell, Pulmonary disease, Hematology, business, Molecular Biology, Biochemistry

Published

2009

26. 885 Preserved Abundance But Functional Dysregulation of Na+/H+ Exchanger Isoform NHE3 in the Small and Large Intestine in CD45RBhigh Transfer Colitis Mice with Diarrhea

Author

Anurag K. Singh, Michael P. Manns, Maria Lünnemann, Dunja Bruder, Sunil Yeruva, Brigitte Riederer, Mingmin Chen, Ursula Seidler, Julia Goldstein, and Marcus Gereke

Subjects

Gene isoform, medicine.medical_specialty, Hepatology, business.industry, Incidence (epidemiology), Gastroenterology, Diclofenac Sodium, medicine.disease, Sodium–hydrogen antiporter, Diarrhea, medicine.anatomical_structure, Biochemistry, Internal medicine, Medicine, Rebamipide, Large intestine, medicine.symptom, Colitis, business, medicine.drug

Abstract

G A A b st ra ct s before and after medication were analyzed for small intestinal injuries. NSAID treatment significantly increased the mean number of mucosal breaks and reddened lesions per subject in the Control-group, from 0.1±0.3 to 15.8±71.5 and from 4.0±3.9 to 10.0±10.3 respectively; but only up from 0.1±0.3 to 4.2±7.8 and from 5.4±6.3 to 9.2±6.6 in the Rebamipide-group. The percentage of subjects with at least one mucosal break at post-treatment was also higher in the Control-group (63%) than in the Rebamipide-group (47%); (NS). The percentage of subjects with post-treatment increases in reddened lesions ≥ 10 was significantly higher in the Control-group (46%) than in the Rebamipide-group (14%); (P=0.04). Conclusion: Rebamipide administration reduced the incidence of small intestinal lesions induced by twoweek administration of diclofenac sodium. Further studies are warranted to determine whether a higher rebamipide dosage can further protect against NSAID-induced small intestinal mucosal breaks.

Published

2009