Your search keyword '"Tobias Stoeger"' showing total 158 results

1. Association of immune cell recruitment and BPD development

Author

Motaharehsadat Heydarian, Christian Schulz, Tobias Stoeger, and Anne Hilgendorff

Subjects

Neonate, Lung, Chronic lung disease, Bronchopulmonary dysplasia, Inflammation, Neutrophil, Pediatrics, RJ1-570

Abstract

Abstract In the neonatal lung, exposure to both prenatal and early postnatal risk factors converge into the development of injury and ultimately chronic disease, also known as bronchopulmonary dysplasia (BPD). The focus of many studies has been the characteristic inflammatory responses provoked by these exposures. Here, we review the relationship between immaturity and prenatal conditions, as well as postnatal exposure to mechanical ventilation and oxygen toxicity, with the imbalance of pro- and anti-inflammatory regulatory networks. In these conditions, cytokine release, protease activity, and sustained presence of innate immune cells in the lung result in pathologic processes contributing to lung injury. We highlight the recruitment and function of myeloid innate immune cells, in particular, neutrophils and monocyte/macrophages in the BPD lung in human patients and animal models. We also discuss dissimilarities between the infant and adult immune system as a basis for the development of novel therapeutic strategies.

Published

2022

2. Cytokine signaling converging on IL11 in ILD fibroblasts provokes aberrant epithelial differentiation signatures

Author

Miriam T. Kastlmeier, Erika Gonzalez-Rodriguez, Phoebe Cabanis, Eva M. Guenther, Ann-Christine König, Lianyong Han, Stefanie M. Hauck, Fenja See, Sara Asgharpour, Christina Bukas, Gerald Burgstaller, Marie Piraud, Mareike Lehmann, Rudolf A. Hatz, Jürgen Behr, Tobias Stoeger, Anne Hilgendorff, and Carola Voss

Subjects

cytokine, IL11, secretome, interstitial lung disease, organoids, human pluripotent stem cells, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionInterstitial lung disease (ILD) is a heterogenous group of lung disorders where destruction and incomplete regeneration of the lung parenchyma often results in persistent architectural distortion of the pulmonary scaffold. Continuous mesenchyme-centered, disease-relevant signaling likely initiates and perpetuates the fibrotic remodeling process, specifically targeting the epithelial cell compartment, thereby destroying the gas exchange area.MethodsWith the aim of identifying functional mediators of the lung mesenchymal-epithelial crosstalk with potential as new targets for therapeutic strategies, we developed a 3D organoid co-culture model based on human induced pluripotent stem cell-derived alveolar epithelial type 2 cells that form alveolar organoids in presence of lung fibroblasts from fibrotic-ILD patients, in our study referring to cases of pulmonary fibrosis, as well as control cell line (IMR-90).ResultsWhile organoid formation capacity and size was comparable in the presence of fibrotic-ILD or control lung fibroblasts, metabolic activity was significantly increased in fibrotic-ILD co-cultures. Alveolar organoids cultured with fibrotic-ILD fibroblasts further demonstrated reduced stem cell function as reflected by reduced Surfactant Protein C gene expression together with an aberrant basaloid-prone differentiation program indicated by elevated Cadherin 2, Bone Morphogenic Protein 4 and Vimentin transcription. To screen for key mediators of the misguided mesenchymal-to-epithelial crosstalk with a focus on disease-relevant inflammatory processes, we used mass spectrometry and characterized the secretome of end stage fibrotic-ILD lung fibroblasts in comparison to non-chronic lung disease (CLD) patient fibroblasts. Out of the over 2000 proteins detected by this experimental approach, 47 proteins were differentially abundant comparing fibrotic-ILD and non-CLD fibroblast secretome. The fibrotic-ILD secretome profile was dominated by chemokines, including CXCL1, CXCL3, and CXCL8, interfering with growth factor signaling orchestrated by Interleukin 11 (IL11), steering fibrogenic cell-cell communication, and proteins regulating extracellular matrix remodeling including epithelial-to-mesenchymal transition. When in turn treating alveolar organoids with IL11, we recapitulated the co-culture results obtained with primary fibrotic-ILD fibroblasts including changes in metabolic activity.ConclusionWe identified mediators likely contributing to the disease-perpetuating mesenchymal-to-epithelial crosstalk in ILD. In our alveolar organoid co-cultures, we were able to highlight the importance of fibroblast-initiated aberrant epithelial differentiation and confirmed IL11 as a key player in fibrotic-ILD pathogenesis by unbiased fibroblast secretome analysis.

Published

2023

3. Corrigendum: Monocyte signature as a predictor of chronic lung disease in the preterm infant

Author

Anita C. Windhorst, Motaharehsadat Heydarian, Maren Schwarz, Prajakta Oak, Kai Förster, Marion Frankenberger, Erika Gonzalez Rodriguez, Xin Zhang, Harald Ehrhardt, Christoph Hübener, Andreas W. Flemmer, Hamid Hossain, Tobias Stoeger, Christian Schulz, and Anne Hilgendorff

Subjects

bronchopulmonary dysplasia, monocytes, cytokines, preterm infants, prenatal injury, chronic lung disease, Immunologic diseases. Allergy, RC581-607

Published

2023

4. Monocyte signature as a predictor of chronic lung disease in the preterm infant

Author

Anita C. Windhorst, Motaharehsadat Heydarian, Maren Schwarz, Prajakta Oak, Kai Förster, Marion Frankenberger, Erika Gonzalez Rodriguez, Xin Zhang, Harald Ehrhardt, Christoph Hübener, Andreas W. Flemmer, Hamid Hossain, Tobias Stoeger, Christian Schulz, and Anne Hilgendorff

Subjects

bronchopulmonary dysplasia, monocytes, cytokines, preterm infants, prenatal injury, chronic lung disease, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionInflammation is a key driver of morbidity in the vulnerable preterm infant exposed to pre- and postnatal hazards and significantly contributes to chronic lung disease, i.e. bronchopulmonary dysplasia (BPD). However, the early changes in innate immunity associated with BPD development are incompletely understood.MethodsIn very immature preterm infants below 32 weeks gestational age (GA; n=30 infants), monocyte subtypes were identified by Flow Cytometry at birth and throughout the postnatal course including intracellular TNF expression upon LPS stimulation. Complementing these measurements, cytokine end growth factor expression profiles (Luminex® xMAP®; n=110 infants) as well as gene expression profiles (CodeLinkTM Human I Bioarray; n=22) were characterized at birth.ResultsThe abundance of monocyte subtypes differed between preterm and term neonates at birth. Specifically, CD14++CD16+ (intermediate) monocytes demonstrated a dependency on PMA and elevated levels of nonclassical (CD14+CD16++) monocytes characterized preterm infants with developing BPD. Postnatally, lung injury was associated with an increase in intermediate monocytes, while high levels of nonclassical monocytes persisted. Both subtypes were revealed as the main source of intracellular TNF-α expression in the preterm infant. We identified a cytokine and growth factor expression profile in cord blood specimen of preterm infants with developing BPD that corresponded to the disease-dependent regulation of monocyte abundances. Multivariate modeling of protein profiles revealed FGF2, sIL-2 Rα, MCP-1, MIP1a, and TNF-α as predictors of BPD when considering GA. Transcriptome analysis demonstrated genes predicting BPD to be overrepresented in inflammatory pathways with increased disease severity characterized by the regulation of immune and defense response pathways and upstream regulator analysis confirmed TNF-α, interleukin (IL) -6, and interferon α as the highest activated cytokines in more severe disease. Whereas all BPD cases showed downstream activation of chemotaxis and activation of inflammatory response pathways, more severe cases were characterized by an additional activation of reactive oxygen species (ROS) synthesis.DiscussionIn the present study, we identified the early postnatal presence of nonclassical (CD14+CD16++) and intermediate (CD14++CD16+) monocytes as a critical characteristic of BPD development including a specific response pattern of monocyte subtypes to lung injury. Pathophysiological insight was provided by the protein and transcriptome signature identified at birth, centered around monocyte and corresponding granulocyte activation and highlighting TNFα as a critical regulator in infants with developing BPD. The disease severity-dependent expression patterns could inform future diagnostic and treatment strategies targeting the monocytic cell and its progeny.

Published

2023

5. Editorial: Exploring impacts of combined exposures to particles and chemicals on immune reactions across living organisms

Author

Diana Boraschi, Albert Duschl, Iseult Lynch, and Tobias Stoeger

Subjects

immunotoxicity, nanoparticles, microplastics, microorganisms, chemicals, Toxicology. Poisons, RA1190-1270

Published

2023

6. The arginine methyltransferase PRMT7 promotes extravasation of monocytes resulting in tissue injury in COPD

Author

Gizem Günes Günsel, Thomas M. Conlon, Aicha Jeridi, Rinho Kim, Zeynep Ertüz, Niklas J. Lang, Meshal Ansari, Mariia Novikova, Dongsheng Jiang, Maximilian Strunz, Mariia Gaianova, Christine Hollauer, Christina Gabriel, Ilias Angelidis, Sebastian Doll, Jeanine C. Pestoni, Stephanie L. Edelmann, Marlene Sophia Kohlhepp, Adrien Guillot, Kevin Bassler, Hannelore P. Van Eeckhoutte, Özgecan Kayalar, Nur Konyalilar, Tamara Kanashova, Sophie Rodius, Carolina Ballester-López, Carlos M. Genes Robles, Natalia Smirnova, Markus Rehberg, Charu Agarwal, Ioanna Krikki, Benoit Piavaux, Stijn E. Verleden, Bart Vanaudenaerde, Melanie Königshoff, Gunnar Dittmar, Ken R. Bracke, Joachim L. Schultze, Henrik Watz, Oliver Eickelberg, Tobias Stoeger, Gerald Burgstaller, Frank Tacke, Vigo Heissmeyer, Yuval Rinkevich, Hasan Bayram, Herbert B. Schiller, Marcus Conrad, Robert Schneider, and Ali Önder Yildirim

Subjects

Science

Abstract

Chronic obstructive pulmonary disease is a progressive and incurable chronic condition that involves accumulation of inflammatory macrophages in the lung tissue. Authors here show in mouse models of lung disease that PRMT7, a protein arginine methyltransferase, is an important regulator of recruitment and the pro-inflammatory phenotype of macrophages.

Published

2022

7. Nanomaterial- and shape-dependency of TLR2 and TLR4 mediated signaling following pulmonary exposure to carbonaceous nanomaterials in mice

Author

Pernille Høgh Danielsen, Katja Maria Bendtsen, Kristina Bram Knudsen, Sarah Søs Poulsen, Tobias Stoeger, and Ulla Vogel

Subjects

Toll-like receptors, Nanomaterials, Inflammation, Acute phase response, Knockout mice, Toxicology. Poisons, RA1190-1270, Industrial hygiene. Industrial welfare, HD7260-7780.8

Abstract

Abstract Background Pulmonary exposure to high doses of engineered carbonaceous nanomaterials (NMs) is known to trigger inflammation in the lungs paralleled by an acute phase response. Toll-like receptors (TLRs), particularly TLR2 and TLR4, have recently been discussed as potential NM-sensors, initiating inflammation. Using Tlr2 and Tlr4 knock out (KO) mice, we addressed this hypothesis and compared the pattern of inflammation in lung and acute phase response in lung and liver 24 h after intratracheal instillation of three differently shaped carbonaceous NMs, spherical carbon black (CB), multi-walled carbon nanotubes (CNT), graphene oxide (GO) plates and bacterial lipopolysaccharide (LPS) as positive control. Results The LPS control confirmed a distinct TLR4-dependency as well as a pronounced contribution of TLR2 by reducing the levels of pulmonary inflammation to 30 and 60% of levels in wild type (WT) mice. At the doses chosen, all NM caused comparable neutrophil influxes into the lungs of WT mice, and reduced levels were only detected for GO-exposed Tlr2 KO mice (35%) and for CNT-exposed Tlr4 KO mice (65%). LPS-induced gene expression was strongly TLR4-dependent. CB-induced gene expression was unaffected by TLR status. Both GO and MWCNT-induced Saa1 expression was TLR4-dependent. GO-induced expression of Cxcl2, Cxcl5, Saa1 and Saa3 were TLR2-dependent. NM-mediated hepatic acute phase response in terms of liver gene expression of Saa1 and Lcn2 was shown to depend on TLR2 for all three NMs. TLR4, in contrast, was only relevant for the acute phase response caused by CNTs, and as expected by LPS. Conclusion TLR2 and TLR4 signaling was not involved in the acute inflammatory response caused by CB exposure, but contributed considerably to that of GO and CNTs, respectively. The strong involvement of TLR2 in the hepatic acute phase response caused by pulmonary exposure to all three NMs deserves further investigations.

Published

2021

8. The role of tumor-associated macrophages and soluble mediators in pulmonary metastatic melanoma

Author

Kaifen Xiong, Min Qi, Tobias Stoeger, Jianglin Zhang, and Shanze Chen

Subjects

tumor-associated macrophages (TAMs), pulmonary metastatic melanoma, targeted therapy, soluble mediators, melanoma, Immunologic diseases. Allergy, RC581-607

Abstract

Skin malignant melanoma is a highly aggressive skin tumor, which is also a major cause of skin cancer-related mortality. It can spread from a relatively small primary tumor and metastasize to multiple locations, including lymph nodes, lungs, liver, bone, and brain. What’s more metastatic melanoma is the main cause of its high mortality. Among all organs, the lung is one of the most common distant metastatic sites of melanoma, and the mortality rate of melanoma lung metastasis is also very high. Elucidating the mechanisms involved in the pulmonary metastasis of cutaneous melanoma will not only help to provide possible explanations for its etiology and progression but may also help to provide potential new therapeutic targets for its treatment. Increasing evidence suggests that tumor-associated macrophages (TAMs) play an important regulatory role in the migration and metastasis of various malignant tumors. Tumor-targeted therapy, targeting tumor-associated macrophages is thus attracting attention, particularly for advanced tumors and metastatic tumors. However, the relevant role of tumor-associated macrophages in cutaneous melanoma lung metastasis is still unclear. This review will present an overview of the origin, classification, polarization, recruitment, regulation and targeting treatment of tumor-associated macrophages, as well as the soluble mediators involved in these processes and a summary of their possible role in lung metastasis from cutaneous malignant melanoma. This review particularly aims to provide insight into mechanisms and potential therapeutic targets to readers, interested in pulmonary metastasis melanoma.

Published

2022

9. Alveolar regeneration through a Krt8+ transitional stem cell state that persists in human lung fibrosis

Author

Maximilian Strunz, Lukas M. Simon, Meshal Ansari, Jaymin J. Kathiriya, Ilias Angelidis, Christoph H. Mayr, George Tsidiridis, Marius Lange, Laura F. Mattner, Min Yee, Paulina Ogar, Arunima Sengupta, Igor Kukhtevich, Robert Schneider, Zhongming Zhao, Carola Voss, Tobias Stoeger, Jens H. L. Neumann, Anne Hilgendorff, Jürgen Behr, Michael O’Reilly, Mareike Lehmann, Gerald Burgstaller, Melanie Königshoff, Harold A. Chapman, Fabian J. Theis, and Herbert B. Schiller

Subjects

Science

Abstract

Injury repair is characterized by the generation of transient cell states important for tissue recovery. Here, the authors present a single cell RNA-seq map of recovery from bleomycin lung injury in mice and uncover a Krt8+ transitional stem cell state that precedes the regeneration of AT1 cells and persists in human lung fibrosis.

Published

2020

10. Applications and Immunological Effects of Quantum Dots on Respiratory System

Author

Laibin Ren, Lingwei Wang, Markus Rehberg, Tobias Stoeger, Jianglin Zhang, and Shanze Chen

Subjects

quantum dot, respiratory system, biomedical applications, cytotoxicity, immunological effects, Immunologic diseases. Allergy, RC581-607

Abstract

Quantum dots (QDs), are one kind of nanoscale semiconductor crystals with specific electronic and optical properties, offering near-infrared mission and chemically active surfaces. Increasing interest for QDs exists in developing theranostics platforms for bioapplications such as imaging, drug delivery and therapy. Here we summarized QDs’ biomedical applications, toxicity, and immunological effects on the respiratory system. Bioapplications of QDs in lung include biomedical imaging, drug delivery, bio-sensing or diagnosis and therapy. Generically, toxic effects of nanoparticles are related to the generation of oxidative stresses with subsequent DNA damage and decreased lung cells viability in vitro and in vivo because of release of toxic metal ions or the features of QDs like its surface charge. Lastly, pulmonary immunological effects of QDs mainly include proinflammatory cytokines release and recruiting innate leukocytes or adaptive T cells.

Published

2022

11. Lung Organoids for Hazard Assessment of Nanomaterials

Author

Miriam T. Kastlmeier, Eva M. Guenther, Tobias Stoeger, and Carola Voss

Subjects

nanomaterial, pulmonary particle exposure, organoids, 3D in vitro models, pluripotent stem cells, respiratory toxicity, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Lung epithelial organoids for the hazard assessment of inhaled nanomaterials offer a promising improvement to in vitro culture systems used so far. Organoids grow in three-dimensional (3D) spheres and can be derived from either induced pluripotent stem cells (iPSC) or primary lung tissue stem cells from either human or mouse. In this perspective we will highlight advantages and disadvantages of traditional culture systems frequently used for testing nanomaterials and compare them to lung epithelial organoids. We also discuss the differences between tissue and iPSC-derived organoids and give an outlook in which direction the whole field could possibly go with these versatile tools.

Published

2022

12. Intense Innate Immune Responses and Severe Metabolic Disorders in Chicken Embryonic Visceral Tissues Caused by Infection with Highly Virulent Newcastle Disease Virus Compared to the Avirulent Virus: A Bioinformatics Analysis

Author

Shanyu Cheng, Xinxin Liu, Jiaqi Mu, Weiwen Yan, Mengjun Wang, Haoran Chai, Yuxin Sha, Shanshan Jiang, Sijie Wang, Yongning Ren, Chao Gao, Zhuang Ding, Tobias Stoeger, Erdene-Ochir Tseren-Ochir, Aleksandar Dodovski, Pastor Alfonso, Claro N. Mingala, and Renfu Yin

Subjects

Newcastle disease virus, chicken embryo, RNA-seq, virulence, host innate immune response, metabolism, Microbiology, QR1-502

Abstract

The highly virulent Newcastle disease virus (NDV) isolates typically result in severe systemic pathological changes and high mortality in Newcastle disease (ND) illness, whereas avirulent or low-virulence NDV strains can cause subclinical disease with no morbidity and even asymptomatic infections in birds. However, understanding the host’s innate immune responses to infection with either a highly virulent strain or an avirulent strain, and how this response may contribute to severe pathological damages and even mortality upon infection with the highly virulent strain, remain limited. Therefore, the differences in epigenetic and pathogenesis mechanisms between the highly virulent and avirulent strains were explored, by transcriptional profiling of chicken embryonic visceral tissues (CEVT), infected with either the highly virulent NA-1 strain or the avirulent vaccine LaSota strain using RNA-seq. In our current paper, severe systemic pathological changes and high mortality were only observed in chicken embryos infected with the highly virulent NA-1 strains, although the propagation of viruses exhibited no differences between NA-1 and LaSota. Furthermore, virulent NA-1 infection caused intense innate immune responses and severe metabolic disorders in chicken EVT at 36 h post-infection (hpi), instead of 24 hpi, based on the bioinformatics analysis results for the differentially expressed genes (DEGs) between NA-1 and LaSota groups. Notably, an acute hyperinflammatory response, characterized by upregulated inflammatory cytokines, an uncontrolled host immune defense with dysregulated innate immune response-related signaling pathways, as well as severe metabolic disorders with the reorganization of host–cell metabolism were involved in the host defense response to the CEVT infected with the highly virulent NA-1 strain compared to the avirulent vaccine LaSota strain. Taken together, these results indicate that not only the host’s uncontrolled immune response itself, but also the metabolic disorders with viruses hijacking host cell metabolism, may contribute to the pathogenesis of the highly virulent strain in ovo.

Published

2022

13. In vivo Dynamic Phase-Contrast X-ray Imaging using a Compact Light Source

Author

Regine Gradl, Martin Dierolf, Benedikt Günther, Lorenz Hehn, Winfried Möller, David Kutschke, Lin Yang, Martin Donnelley, Rhiannon Murrie, Alexander Erl, Tobias Stoeger, Bernhard Gleich, Klaus Achterhold, Otmar Schmid, Franz Pfeiffer, and Kaye Susannah Morgan

Subjects

Medicine, Science

Abstract

Abstract We describe the first dynamic and the first in vivo X-ray imaging studies successfully performed at a laser-undulator-based compact synchrotron light source. The X-ray properties of this source enable time-sequence propagation-based X-ray phase-contrast imaging. We focus here on non-invasive imaging for respiratory treatment development and physiological understanding. In small animals, we capture the regional delivery of respiratory treatment, and two measures of respiratory health that can reveal the effectiveness of a treatment; lung motion and mucociliary clearance. The results demonstrate the ability of this set-up to perform laboratory-based dynamic imaging, specifically in small animal models, and with the possibility of longitudinal studies.

Published

2018

14. Early pulmonary response is critical for extra-pulmonary carbon nanoparticle mediated effects: comparison of inhalation versus intra-arterial infusion exposures in mice

Author

Koustav Ganguly, Dariusch Ettehadieh, Swapna Upadhyay, Shinji Takenaka, Thure Adler, Erwin Karg, Fritz Krombach, Wolfgang G. Kreyling, Holger Schulz, Otmar Schmid, and Tobias Stoeger

Subjects

Inhaled soot, Ultrafine particulate matter, Inflammation, Lung, Heart, Aorta, Toxicology. Poisons, RA1190-1270, Industrial hygiene. Industrial welfare, HD7260-7780.8

Abstract

Abstract Background The death toll associated with inhaled ambient particulate matter (PM) is attributed mainly to cardio-vascular rather than pulmonary effects. However, it is unclear whether the key event for cardiovascular impairment is particle translocation from lung to circulation (direct effect) or indirect effects due to pulmonary particle-cell interactions. In this work, we addressed this issue by exposing healthy mice via inhalation and intra-arterial infusion (IAI) to carbon nanoparticles (CNP) as surrogate for soot, a major constituent of (ultrafine) urban PM. Methods Equivalent surface area CNP doses in the blood (30mm2 per animal) were applied by IAI or inhalation (lung-deposited dose 10,000mm2; accounting for 0.3% of lung-to-blood CNP translocation). Mice were analyzed for changes in hematology and molecular markers of endothelial/epithelial dysfunction, pro-inflammatory reactions, oxidative stress, and coagulation in lungs and extra-pulmonary organs after CNP inhalation (4 h and 24 h) and CNP infusion (4 h). For methodological reasons, we used two different CNP types (spark-discharge and Printex90), with very similar physicochemical properties [≥98 and ≥95% elemental carbon; 10 and 14 nm primary particle diameter; and 800 and 300 m2/g specific surface area] for inhalation and IAI respectively. Results Mild pulmonary inflammatory responses and significant systemic effects were observed following 4 h and 24 h CNP inhalation. Increased retention of activated leukocytes, secondary thrombocytosis, and pro-inflammatory responses in secondary organs were detected following 4 h and 24 h of CNP inhalation only. Interestingly, among the investigated extra-pulmonary tissues (i.e. aorta, heart, and liver); aorta revealed as the most susceptible extra-pulmonary target following inhalation exposure. Bypassing the lungs by IAI however did not induce any extra-pulmonary effects at 4 h as compared to inhalation. Conclusions Our findings indicate that extra-pulmonary effects due to CNP inhalation are dominated by indirect effects (particle-cell interactions in the lung) rather than direct effects (translocated CNPs) within the first hours after exposure. Hence, CNP translocation may not be the key event inducing early cardiovascular impairment following air pollution episodes. The considerable response detected in the aorta after CNP inhalation warrants more emphasis on this tissue in future studies.

Published

2017

15. The First Scube3 Mutant Mouse Line with Pleiotropic Phenotypic Alterations

Author

Helmut Fuchs, Sibylle Sabrautzki, Gerhard K. H. Przemeck, Stefanie Leuchtenberger, Bettina Lorenz-Depiereux, Lore Becker, Birgit Rathkolb, Marion Horsch, Lillian Garrett, Manuela A. Östereicher, Wolfgang Hans, Koichiro Abe, Nobuho Sagawa, Jan Rozman, Ingrid L. Vargas-Panesso, Michael Sandholzer, Thomas S. Lisse, Thure Adler, Juan Antonio Aguilar-Pimentel, Julia Calzada-Wack, Nicole Ehrhard, Ralf Elvert, Christine Gau, Sabine M. Hölter, Katja Micklich, Kristin Moreth, Cornelia Prehn, Oliver Puk, Ildiko Racz, Claudia Stoeger, Alexandra Vernaleken, Dian Michel, Susanne Diener, Thomas Wieland, Jerzy Adamski, Raffi Bekeredjian, Dirk H. Busch, John Favor, Jochen Graw, Martin Klingenspor, Christoph Lengger, Holger Maier, Frauke Neff, Markus Ollert, Tobias Stoeger, Ali Önder Yildirim, Tim M. Strom, Andreas Zimmer, Eckhard Wolf, Wolfgang Wurst, Thomas Klopstock, Johannes Beckers, Valerie Gailus-Durner, and Martin Hrabé de Angelis

Subjects

SCUBE3, systemic phenotype, pleitropy, Paget disease of bone (PDB), mouse model, Genetics, QH426-470

Abstract

The vertebrate Scube (Signal peptide, CUB, and EGF-like domain-containing protein) family consists of three independent members, Scube1–3, which encode secreted cell surface-associated membrane glycoproteins. Limited information about the general function of this gene family is available, and their roles during adulthood. Here, we present the first Scube3 mutant mouse line (Scube3N294K/N294K), which clearly shows phenotypic alterations by carrying a missense mutation in exon 8, and thus contributes to our understanding of SCUBE3 functions. We performed a detailed phenotypic characterization in the German Mouse Clinic (GMC). Scube3N294K/N294K mutants showed morphological abnormalities of the skeleton, alterations of parameters relevant for bone metabolism, changes in renal function, and hearing impairments. These findings correlate with characteristics of the rare metabolic bone disorder Paget disease of bone (PDB), associated with the chromosomal region of human SCUBE3. In addition, alterations in energy metabolism, behavior, and neurological functions were detected in Scube3N294K/N294K mice. The Scube3N294K/N294K mutant mouse line may serve as a new model for further studying the effect of impaired SCUBE3 gene function.

Published

2016

16. 'Novel' Triggers of Herpesvirus Reactivation and Their Potential Health Relevance

Author

Tobias Stoeger and Heiko Adler

Subjects

herpesvirus, reactivation, nanoparticle, non-canonical triggers, health relevance, Microbiology, QR1-502

Published

2019

17. S100a4 Is Secreted by Alternatively Activated Alveolar Macrophages and Promotes Activation of Lung Fibroblasts in Pulmonary Fibrosis

Author

Wei Zhang, Shinji Ohno, Beatrix Steer, Stephan Klee, Claudia A. Staab-Weijnitz, Darcy Wagner, Mareike Lehmann, Tobias Stoeger, Melanie Königshoff, and Heiko Adler

Subjects

S100A4, alternatively activated macrophages, lung fibrosis, fibroblast activation, fibroblast proliferation, M2 macrophages, Immunologic diseases. Allergy, RC581-607

Abstract

Idiopathic pulmonary fibrosis (IPF) is a devastating interstitial lung disease, characterized by damage of lung epithelial cells, excessive deposition of extracellular matrix in the lung interstitium, and enhanced activation and proliferation of fibroblasts. S100a4, also termed FSP-1 (fibroblast-specific protein-1), was previously considered as a marker of fibroblasts but recent findings in renal and liver fibrosis indicated that M2 macrophages are an important cellular source of S100a4. Thus, we hypothesized that also in pulmonary fibrosis, M2 macrophages produce and secrete S100a4, and that secreted S100a4 induces the proliferation and activation of fibroblasts. To prove this hypothesis, we comprehensively characterized two established mouse models of lung fibrosis: infection of IFN-γR−/− mice with MHV-68 and intratracheal application of bleomycin to C57BL/6 mice. We further provide in vitro data using primary macrophages and fibroblasts to investigate the mechanism by which S100A4 exerts its effects. Finally, we inhibit S100a4 in vivo in the bleomycin-induced lung fibrosis model by treatment with niclosamide. Our data suggest that S100a4 is produced and secreted by M2 polarized alveolar macrophages and enhances the proliferation and activation of lung fibroblasts. Inhibition of S100a4 might represent a potential therapeutic strategy for pulmonary fibrosis.

Published

2018

18. Enhanced Replication of Virulent Newcastle Disease Virus in Chicken Macrophages Is due to Polarized Activation of Cells by Inhibition of TLR7

Author

Pingze Zhang, Zhuang Ding, Xinxin Liu, Yanyu Chen, Junjiao Li, Zhi Tao, Yidong Fei, Cong Xue, Jing Qian, Xueli Wang, Qingmei Li, Tobias Stoeger, Jianjun Chen, Yuhai Bi, and Renfu Yin

Subjects

chicken macrophages, newcastle disease virus, toll-like receptor 7, macrophage polarized activation, virus growth, immune response, Immunologic diseases. Allergy, RC581-607

Abstract

Newcastle disease (ND), caused by infections with virulent strains of Newcastle disease virus (NDV), is one of the most important infectious disease affecting wild, peridomestic, and domestic birds worldwide. Vaccines constructed from live, low-virulence (lentogenic) viruses are the most accepted prevention and control strategies for combating ND in poultry across the globe. Avian macrophages are one of the first cell lines of defense against microbial infection, responding to signals in the microenvironment. Although macrophages are considered to be one of the main target cells for NDV infection in vivo, very little is known about the ability of NDV to infect chicken macrophages, and virulence mechanisms of NDV as well as the polarized activation patterns of macrophages and correlation with viral infection and replication. In the present study, a cell culture model (chicken bone marrow macrophage cell line HD11) and three different virulence and genotypes of NDV (including class II virulent NA-1, class II lentogenic LaSota, and class I lentogenic F55) were used to solve the above underlying questions. Our data indicated that all three NDV strains had similar replication rates during the early stages of infection. Virulent NDV titers were shown to increase compared to the other lentogenic strains, and this growth was associated with a strong upregulation of both pro-inflammatory M1-like markers/cytokines and anti-inflammatory M2-like markers/cytokines in chicken macrophages. Virulent NDV was found to block toll-like receptor (TLR) 7 expression, inducing higher expression of type I interferons in chicken macrophages at the late stage of viral infection. Only virulent NDV replication can be inhibited by pretreatment with TLR7 ligand. Overall, this study demonstrated that virulent NDV activates a M1-/M2-like mixed polarized activation of chicken macrophages by inhibition of TLR7, resulting in enhanced replication compared to lentogenic viruses.

Published

2018

19. Dispersal and Transmission of Avian Paramyxovirus Serotype 4 among Wild Birds and Domestic Poultry

Author

Renfu Yin, Pingze Zhang, Xinxin Liu, Yanyu Chen, Zhi Tao, Lili Ai, Junjiao Li, Yingying Yang, Mingxin Li, Cong Xue, Jing Qian, Xueli Wang, Jing Chen, Yong Li, Yanping Xiong, Jun Zhang, Tobias Stoeger, Yuhai Bi, Jianjun Chen, and Zhuang Ding

Subjects

APMV-4, intercontinental, wild birds, domestic poultry, dispersal, interspecies transmission, Microbiology, QR1-502

Abstract

Avian paramyxovirus serotype 4 (APMV-4) is found sporadically in wild birds worldwide, and it is an economically important poultry pathogen. Despite the existence of several published strains, very little is known about the distribution, host species, and transmission of APMV-4 strains. To better understand the relationships among these factors, we conducted an APMV-4 surveillance of wild birds and domestic poultry in six provinces of China suspected of being intercontinental flyways and sites of interspecies transmission. APMV-4 surveillance was conducted in 9,160 wild birds representing seven species, and 1,461 domestic poultry in live bird markets (LMBs) from December 2013 to June 2016. The rate of APMV-4 isolation was 0.10% (11/10,621), and viruses were isolated from swan geese, bean geese, cormorants, mallards, and chickens. Sequencing and phylogenetic analyses of the 11 isolated viruses indicated that all the isolates belonging to genotype I were epidemiologically connected with wild bird-origin viruses from the Ukraine and Italy. Moreover, chicken-origin APMV-4 strains isolated from the LBMs were highly similar to wild bird-origin viruses from nearby lakes with free-living wild birds. In additional, a hemagglutination-negative APMV-4 virus was identified. These findings, together with recent APMV-4 studies, suggest potential virus interspecies transmission between wild birds and domestic poultry, and reveal possible epidemiological intercontinental connections between APMV-4 transmission by wild birds.

Published

2017

20. INHALED AMBIENT PARTICULATE MATTER AND LUNG HEALTH BURDEN

Author

Swapna Upadhyay, Koustav Ganguly, and Tobias Stoeger

Subjects

particulate matter, particle pollution, chronic lung disease, lung function, pulmonary inflammation, Medicine, Diseases of the respiratory system, RC705-779

Abstract

Increased ambient particulate matter (PM) has been associated with various cardio-respiratory disorders and emergency room visits due to short-term and long-term exposures. However, most of the efforts correlating PM exposure with human health hazards have primarily focused on cardiovascular impairments, although the lung acts as the primary port of entry, and is therefore also the primary target organ. Emerging evidences have shown an association between increased PM and respiratory illness, particularly chronic lung diseases. PM10, PM2.5, ultrafine particles, or nanoparticles (NPs) are of interest in this regard. Particle surface area increases with decreasing size and surface related parameters such as oxidative potency, solubility, and bioavailability, and are widely regarded as the parameters determining particle toxicity. Factory utility smoke stacks, vehicle exhaust, wood, and biomass burning act as the primary sources for ambient PM, coupled with composition variability. Revolution of nanotechnology during the last decade brought forward concerns about NPs as a potential new health hazard as well. Epidemiological, clinical, and experimental studies suggest oxidative stress, inflammation, impaired inflammation resolution, and altered coagulation cascade homeostasis as the causative mechanisms of both pulmonary and cardiovascular impairments due to PM exposure. Children, the elderly, and individuals with pre-existing conditions are found to be the most vulnerable subjects. Respiratory symptoms of increased PM exposure include increased infection, pneumonia, chronic bronchitis, emphysema, exacerbation of asthma and chronic obstructive pulmonary disease, declined forced expiratory volume in 1 second, and forced vital capacity, apart from the classically known phenomenon of asbestosis, silicosis, mesothelioma, lung cancer, and pneumoconiosis.

Published

2014

21. The Emergence of Avian Orthoavulavirus 13 in Wild Migratory Waterfowl in China Revealed the Existence of Diversified Trailer Region Sequences and HN Gene Lengths within this Serotype

Author

Yidong Fei, Xinxin Liu, Jiaqi Mu, Junjiao Li, Xibing Yu, Jin Chang, Yuhai Bi, Tobias Stoeger, Abdul Wajid, Denys Muzyka, Kirill Sharshov, Alexander Shestopalov, Alongkorn Amonsin, Jianjun Chen, Zhuang Ding, and Renfu Yin

Subjects

avian orthoavulavirus 13, migratory waterfowl, HN gene, trailer, genetic relationships, Microbiology, QR1-502

Abstract

Avian orthoavulavirus 13 (AOAV-13), also named avian paramyxovirus 13 (APMV-13), has been found sporadically in wild birds around the world ever since the discovery of AOAV-13 (AOAV-13/wild goose/Shimane/67/2000) in a wild goose from Japan in 2000. However, there are no reports of AOAV-13 in China. In the present study, a novel AOAV-13 virus (AOAV-13/wild goose/China/Hubei/V93-1/2015), isolated from a wild migratory waterfowl in a wetland of Hubei province of China, during active surveillance from 2013 to 2018, was biologically and genetically characterized. Phylogenetic analyses demonstrated a very close genetic relationship among all AOAV-13 strains, as revealed by very few genetic variations. Moreover, pathogenicity tests indicated that the V93-1 strain is a low virulent virus for chickens. However, the genome of the V93-1 virus was found to be 16,158 nucleotides (nt) in length, which is 12 nt or 162 nt longer than the other AOAV-13 strains that have been reported to date. The length difference of 12 nt in strain V93-1 is due to the existence of three repeats of the conserved sequence, “AAAAAT”, in the 5′-end trailer of the genome. Moreover, the HN gene of the V93-1 virus is 2070 nt in size, encoding 610 aa, which is the same size as the AOAV-13 strain from Japan, whereas that of two strains from Ukraine and Kazakhstan are 2080 nt in length, encoding 579 aa. We describe a novel AOAV-13 in migratory waterfowl in China, which suggests that diversified trailer region sequences and HN gene lengths exist within serotype AOAV-13, and highlight the need for its constant surveillance in poultry from live animal markets, and especially migratory birds.

Published

2019

22. Macrophage Cellular Adaptation, Localization and Imaging of Different Size Polystyrene Particles

Author

Furong Tian, Adriele Prina-Mello, Giovani Estrada, Andrea Beyerle, Winfried Möller, Holger Schulz, Wolfgang Kreyling, and Tobias Stoeger

Subjects

polystyreneparticles, macrophage, adaption, localization, imaging, Biology (General), QH301-705.5, Medicine

Abstract

Several studies have tackled the evaluation of the biocompatibility of nanomaterials in cell and tissue. Nonetheless to date, a quantitative technique for the assessment of the total intracellular nanocarrier dose administered has not been introduced. In this paper we develop two rapid and sensitive assays for the measurement of internalized nanomaterials in macrophages to be applied as vehicular carriers for drug delivery and contrast imaging applications. Five commercially available polystyrene particles with different diameters (from 20 to 1000 nm) were used and imaged by using a 3dimensional confocal imaging techniques. The two proposed assays are: “volumetric” assay which evaluate the spherical volume of internalized particles and 2) “max-flat” assay which evaluate the total differential area between cells and internalized particles. These two assays were then compared to a reference method. Among these three assays, the “max-flat” assay was found to be the most reliable and accurate to quantify and investigate the total content of internalized nanomaterials. The “max-flat” assay also allowed for a 3dimensional subcellular investigation of the adaptation and localization mechanisms between cytoskeleton and internalized materials, which may help to further increase the selectivity and delivery of active and passive biopolymers. Therefore, we believe that the here presented assays could become a useful tool to address many biomaterials questions, especially where the key issue is the quantitative assessment of dose effect issues related to the sizedependence response of nanomaterials.

Published

2009

23. Comparative hazard identification by a single dose lung exposure of zinc oxide and silver nanomaterials in mice.

Author

Ilse Gosens, Ali Kermanizadeh, Nicklas Raun Jacobsen, Anke-Gabriele Lenz, Bas Bokkers, Wim H de Jong, Petra Krystek, Lang Tran, Vicki Stone, Håkan Wallin, Tobias Stoeger, and Flemming R Cassee

Subjects

Medicine, Science

Abstract

Comparative hazard identification of nanomaterials (NMs) can aid in the prioritisation for further toxicity testing. Here, we assessed the acute lung, systemic and liver responses in C57BL/6N mice for three NMs to provide a hazard ranking. A silver (Ag), non-functionalised zinc oxide (ZnO) and a triethoxycaprylylsilane functionalised ZnO NM suspended in water with 2% mouse serum were examined 24 hours following a single intratracheal instillation (I.T.). An acute pulmonary inflammation was noted (marked by a polymorphonuclear neutrophil influx) with cell damage (LDH and total protein) in broncho-alveolar lavage fluid (BALF) after administration of both non-functionalised and functionalised ZnO. The latter also induced systemic inflammation measured as an increase in blood neutrophils and a decrease in blood lymphocytes. Exposure to Ag NM was not accompanied by pulmonary inflammation or cytotoxicity, or by systemic inflammation. A decrease in glutathione levels was demonstrated in the liver following exposure to high doses of all three nanomaterials irrespective of any noticeable inflammatory or cytotoxic effects in the lung. By applying benchmark dose (BMD) modeling statistics to compare potencies of the NMs, we rank functionalised ZnO ranked the highest based on the largest number of affected endpoints, as well as the strongest responses observed after 24 hours. The non-functionalised ZnO NM gave an almost similar response, whereas Ag NM did not cause an acute response at similar doses.

Published

2015

24. Pleiotropic functions for transcription factor zscan10.

Author

Petra Kraus, Sivakamasundari V, Hong Bing Yu, Xing Xing, Siew Lan Lim, Thure Adler, Juan Antonio Aguilar Pimentel, Lore Becker, Alexander Bohla, Lillian Garrett, Wolfgang Hans, Sabine M Hölter, Eva Janas, Kristin Moreth, Cornelia Prehn, Oliver Puk, Birgit Rathkolb, Jan Rozman, Jerzy Adamski, Raffi Bekeredjian, Dirk H Busch, Jochen Graw, Martin Klingenspor, Thomas Klopstock, Frauke Neff, Markus Ollert, Tobias Stoeger, Ali Önder Yildrim, Oliver Eickelberg, Eckhard Wolf, Wolfgang Wurst, Helmut Fuchs, Valérie Gailus-Durner, Martin Hrabě de Angelis, Thomas Lufkin, and Lawrence W Stanton

Subjects

Medicine, Science

Abstract

The transcription factor Zscan10 had been attributed a role as a pluripotency factor in embryonic stem cells based on its interaction with Oct4 and Sox2 in in vitro assays. Here we suggest a potential role of Zscan10 in controlling progenitor cell populations in vivo. Mice homozygous for a Zscan10 mutation exhibit reduced weight, mild hypoplasia in the spleen, heart and long bones and phenocopy an eye malformation previously described for Sox2 hypomorphs. Phenotypic abnormalities are supported by the nature of Zscan10 expression in midgestation embryos and adults suggesting a role for Zscan10 in either maintaining progenitor cell subpopulation or impacting on fate choice decisions thereof.

Published

2014

25. Mouse nuclear myosin I knock-out shows interchangeability and redundancy of myosin isoforms in the cell nucleus.

Author

Tomáš Venit, Rastislav Dzijak, Alžběta Kalendová, Michal Kahle, Jana Rohožková, Volker Schmidt, Thomas Rülicke, Birgit Rathkolb, Wolfgang Hans, Alexander Bohla, Oliver Eickelberg, Tobias Stoeger, Eckhard Wolf, Ali Önder Yildirim, Valérie Gailus-Durner, Helmut Fuchs, Martin Hrabě de Angelis, and Pavel Hozák

Subjects

Medicine, Science

Abstract

BACKGROUND: Nuclear myosin I (NM1) is a nuclear isoform of the well-known "cytoplasmic" Myosin 1c protein (Myo1c). Located on the 11(th) chromosome in mice, NM1 results from an alternative start of transcription of the Myo1c gene adding an extra 16 amino acids at the N-terminus. Previous studies revealed its roles in RNA Polymerase I and RNA Polymerase II transcription, chromatin remodeling, and chromosomal movements. Its nuclear localization signal is localized in the middle of the molecule and therefore directs both Myosin 1c isoforms to the nucleus. METHODOLOGY/PRINCIPAL FINDINGS: In order to trace specific functions of the NM1 isoform, we generated mice lacking the NM1 start codon without affecting the cytoplasmic Myo1c protein. Mutant mice were analyzed in a comprehensive phenotypic screen in cooperation with the German Mouse Clinic. Strikingly, no obvious phenotype related to previously described functions has been observed. However, we found minor changes in bone mineral density and the number and size of red blood cells in knock-out mice, which are most probably not related to previously described functions of NM1 in the nucleus. In Myo1c/NM1 depleted U2OS cells, the level of Pol I transcription was restored by overexpression of shRNA-resistant mouse Myo1c. Moreover, we found Myo1c interacting with Pol II. The ratio between Myo1c and NM1 proteins were similar in the nucleus and deletion of NM1 did not cause any compensatory overexpression of Myo1c protein. CONCLUSION/SIGNIFICANCE: We observed that Myo1c can replace NM1 in its nuclear functions. Amount of both proteins is nearly equal and NM1 knock-out does not cause any compensatory overexpression of Myo1c. We therefore suggest that both isoforms can substitute each other in nuclear processes.

Published

2013

26. Cytokine profiles in asthma families depend on age and phenotype.

Author

Katrin Pukelsheim, Tobias Stoeger, David Kutschke, Koustav Ganguly, and Matthias Wjst

Subjects

Medicine, Science

Abstract

BACKGROUND: Circulating cytokine patterns may be relevant for the diagnosis of asthma, for the discrimination of certain phenotypes, and prognostic factors for exacerbation of disease. METHODOLOGY/PRINCIPAL FINDINGS: In this study we investigated serum samples from 944 individuals of 218 asthma-affected families by a multiplex, microsphere based system detecting at high sensitivity eleven asthma associated mediators: eotaxin (CCL11), granulocyte macrophage stimulating factor (GM-CSF), interferon gamma (IFNγ), interleukin-4 (IL-4), IL-5, IL-8, IL-10, IL-12 (p40), IL-13, IL-17 and tumor necrosis factor alpha (TNFα). Single cytokine levels were largely similar between asthmatic and healthy individuals when analysing asthma as single disease entity. Regulatory differences between parental and pediatric asthma were reflected by six of the eleven mediators analyzed (eotaxin, IL-4, IL-5, IL-10, IL-12, TNFα). IL-12 (p40) and IL-5 were the best predictor for extrinsic asthma in children with an increased odds ratio of 2.85 and 1.96 per log pg/ml increase (IL-12 (p40): 1.2-6.8, p=0.019, and IL-5: 1.2-2.5, p=0.025). Frequent asthma attacks in children are associated with elevated IL-5 serum levels (p=0.013). Cytokine patterns seem to be individually balanced in both, healthy and diseased adults and children, with various cytokines correlating among each other (IL-17 and IFNγ (rs=0.67), IL-4 and IL-5 (rs=0.55), IFNγ and GM-CSF (rs=0.54)). CONCLUSION/SIGNIFICANCE: Our data support mainly an age- but also an asthma phenotype-dependent systemic immune regulation.

Published

2010

27. Cytokine signaling converging onIL11in ILD fibroblasts provokes aberrant epithelial differentiation signatures

Author

Miriam T. Kastlmeier, Erika Gonzalez Rodriguez, Phoebe Cabanis, Eva M. Guenther, Ann-Christine König, Lianyong Han, Stefanie M. Hauck, Fenja See, Sara Asgharpour, Christina Bukas, Gerald Burgstaller, Marie Piraud, Mareike Lehmann, Rudolf A. Hatz, Jürgen Behr, Tobias Stoeger, Anne Hilgendorff, and Carola Voss

Abstract

Interstitial lung disease (ILD) is a heterogenous group of lung disorders where destruction and incomplete regeneration of the lung parenchyma often results in persistent architectural distortion of the pulmonary scaffold. Continuous mesenchyme-centered, disease-relevant signaling likely initiates and perpetuates the fibrotic remodeling process, specifically targeting the epithelial cell compartment, thereby destroying the gas exchange area.With the aim of identifying functionally relevant mediators of the lung mesenchymal-epithelial crosstalk that hold potential as new targets for therapeutic strategies, we developed a 3D organoid co-culture model based on human induced pluripotent stem cell-derived alveolar epithelial type 2 cells that form alveolar organoids in presence of lung fibroblasts from ILD patients as well as a control cell line (IMR-90). While organoid formation capacity and size was comparable in the presence of ILD or control lung fibroblasts, metabolic activity was significantly increased in ILD co-cultures. Alveolar organoids cultured with ILD fibroblasts further demonstrated reduced stem cell function as reflected by reducedSurfactant Protein Cgene expression together with an aberrant basaloid-prone differentiation program indicated by elevatedCadherin 2, Bone Morphogenic Protein 4andVimentintranscription.In order to screen for key mediators of the misguided mesenchymal-to-epithelial crosstalk with a focus on disease-relevant inflammatory processes, we used mass spectrometry and characterized the secretome of end stage ILD lung fibroblasts in comparison to non-chronic lung disease (CLD) patient fibroblasts. Out of the over 2000 proteins detected by this experimental approach, 47 proteins were differentially abundant comparing ILD and non-CLD fibroblast secretome.The ILD secretome profile was dominated by chemokines, includingCXCL1, CXCL3, andCXCL8, interfering with growth factor signaling orchestrated byInterleukin 11 (IL11), steering fibrogenic cell-cell communication, and proteins regulating extracellular matrix remodeling including epithelial-to-mesenchymal transition. When in turn treating alveolar organoids withIL11, we recapitulated the co-culture results obtained with primary ILD fibroblasts including changes in metabolic activity.In summary, we identified mediators likely contributing to the disease-perpetuating mesenchymal-to-epithelial crosstalk in ILD. In our alveolar organoid co-cultures, we were able to highlight the importance of fibroblast-initiated aberrant epithelial differentiation and confirmedIL11as a key player in ILD pathogenesis by unbiased ILD fibroblast secretome analysis.Abstract Figure

Published

2022

28. 89 Lung Single Cell Transcriptomics to Guide the Development of AOP Anchored Cell-Based Assays in Response to Nanoparticle Exposure

Author

Lianyong Han, Carola Voss, Meshal Ansari, Maximilian Strunz, Ilias Angelidis, Verena Haefner, Christoph Mayr, Carolina Ballester, Qiongliang Liu, Ali Oender Yildirim, Thomas Conlon, Ulla Voger, Markus Rehberg, Herbert B Schiller, and Tobias Stoeger

Subjects

Public Health, Environmental and Occupational Health

Abstract

Inhaled nanoparticles (NP) can cause acute and chronic inflammation. Here we seek to identify NP-specific cellular perturbation pathways and the underlying key cell types to inform adverse outcome pathway (AOP) anchored in vitro studies, by single cell transcriptomics. We exposed mice intratracheally to carbon black (CNP), tangled double-walled (DWCNT) and rigid, multi-walled carbon nanotubes (MWCNT). All lungs underwent single-cell RNA sequencing (scRNA-seq), histology and BAL analysis. At the chosen doses all NPs caused comparable airspace neutrophilia at 12h, which increased until d6 for the CNTs but remained elevated until d28 only for MWCNT, indicating the key event (KE) acute and chronic inflammation. Comparing scRNA-seq and BAL cytokine levels at 12h, differentiated the fate of inflammation NP specifically. In agreement with airspace neutrophilia, CNP uniquely triggered GM-CSF and CXCL1 release, with Csf2 and Cxcl1 mRNAs being expressed mainly in alveolar epithelial cells. DWCNT caused CCL2, -3 and -4 release involving interstitial macrophages and monocytes, associated with acute high lung monocyte and at d6 high BAL macrophage numbers. MWCNT in contrast caused ample BAL cytokine increases involving different cell types and specifically caused a Th2 cytokine response (CCL11, IL10), a crucial KE of fibrosis AOPs. MWCNT triggered cell communication analysis uncovered NP-specific networks including epithelial cells, fibroblasts, macrophages, dendritic cells and endothelial cells. Our study uncovers early NP-specific cell perturbations and identified first specific cellular response pattern to guide AOP predictive cell-based testing strategies. Further analysis of the cellular dynamics shall enhance our understanding of NP specific cell circuits and related pathologies.

Published

2023

29. 131 Alveolar Macrophage Degranulation Initiates the Spatially Restricted Innate Immune Response During Ventilator-Assisted Nanoparticle Inhalation

Author

Qiongliang Liu, Lin Yang, Chenxi Li, Otmar Schmid, Tobias Stoeger, and Markus Rehberg

Subjects

Public Health, Environmental and Occupational Health

Abstract

To visualize and measure in real-time the cellular pulmonary innate immune response elicited by inhaled NPs, we apply state-of-the-art intravital microscopy on the alveolar region of the murine lung. Fluorescent carboxyl-quantum-dot-NPs (deposited dose of 16 cm2/g) applied via ventilator-assisted inhalation accumulated within seconds as distinct fluorescent spots at the alveolar walls. Already at 30min, cQD-NPs elicited an increase in microvascular neutrophil numbers as compared to controls, which subsequently transmigrated into the alveolar space. This early immune response was not specific to cQD-NPs, since a comparable increase in neutrophil numbers was also observed upon inhalation of a bioequivalent dose of carbon black NPs, a typical component of urban air pollution. AMs actively accumulated cQD-NPs over time, starting few minutes after inhalation. Significantly more neutrophils were attracted in proximity to cQD-NP-laden AMs, as compared to NP-free AMs or control areas with epithelial associated cQD-NP. Prior airway application of a cellular degranulation inhibitor prevented cQD-NP and CNP induced neutrophil recruitment at 2h and 24 h after inhalation. Inhibition of Fcγ-receptor mediated AM cQD-NP uptake by prior application of anti-CD64 mAbs or neutralizing of TNFα by anti-TNFα mAbs in the airspace, abolished this early immune response. Importantly, initial ImageStream flow cytometry analysis of BAL samples indicated an increase of macrophage-derived microvesicles upon NP inhalation. Taken together, our data links NP-induced AM degranulation and cytokine release to the rapid and site-specific recruitment of neutrophils, suggesting this process to be a key event in mounting the immune response upon NP inhalation.

Published

2023

30. 140 A Framework for Grouping Inhaled Multi-Component Nanomaterials to Streamline Hazard Assessment

Author

Vicki Stone, Agnes Oomen, Helinor Johnston, Danail Hristozov, Otmar Schmidt, Tobias Stoeger, Juan Antonio Tamayo Ramos, Santiago Aparicio, and Fiona Murphy

Subjects

Public Health, Environmental and Occupational Health

Abstract

The GRACIOUS Framework (www.h2020gracious.eu) supports the grouping of nanomaterials to streamline hazard testing of nanomaterials. The GRACIOUS Framework includes a template to generate grouping hypotheses based upon use and life cycle stage (to inform exposure route), physicochemical properties (what they are), fate or toxicokinetics (where they go) and hazard (what they do). The gathering of evidence to test these hypotheses was supported by tailored Integrated Approaches to Testing and Assessment (IATAs). Subsequent NMBP-16 projects have developed the hypothesis template further for multicomponent nanomaterials. Modifications include additional information requirements to accommodate the complexity of composition (what they are) and enhanced properties, with an aim to incorporate the relationship of these to the mechanism of hazard. Furthermore, the template considers potential for the components to dissociate, disintegrate or dissolve, with different kinetics, leading to a complex exposure scenario both in lung lining fluid and inside cells. This knowledge informs the hazard assessment (whether hazard is driven by the intact multicomponent nanomaterial or various components) and whether interactions between the components may lead to antagonism, synergism or potentiation of response. Hazard assessment outcome can then inform Safe-by-Design modifications. The template has been adapted to formulate clear questions needed to test all aspects of the hypothesis, with these questions being used to formulate the IATA. Case studies of different multicomponent nanomaterials are being used to inform the design process, and demonstrate its usefulness. Funding acknowledgement European Commission Horizon 2020 for GRACIOUS, SUNSHINE, HARMLESS and DIAGONAL, Grant Agreement No. 760840, 952924, 953183 953152 respectively.

Published

2023

31. 86 Persistent Macrophage Depletion and Arrested Replenishment is Dependent on Carbon Nanotube type as Shown by Single Cell Transcriptomics

Author

Carola Voss, Lianyong Han, Meshal Ansari, Qiongliang Liu, Carol Ballester-Lopez, Thomas M Conlon, Verena Haefner, Maximilian Strunz, Ilias Angelidis, Christoph Mayr, Markus Rehberg, Ali Önder Yildirim, Herbert B Schiller, and Tobias Stoeger

Subjects

Public Health, Environmental and Occupational Health

Abstract

Inhalation of carbon nanomaterials (NMs) can cause severe health effects, including chronic inflammation and fibrosis. We aim for a better understanding of NM specific cellular perturbation patterns. Therefore, we exposed mice intratracheally to soot like carbon black, tangled double-walled (DWCNT) and rigid, multi-walled carbon nanotubes (MWCNT). All lungs underwent single cell RNA sequencing and BAL analysis at 12h, 6d and 28d. At the chosen doses, all NMs caused comparable airspace neutrophilia at 12h, which increased until d6 for CNTs and remained elevated until d28 for MWCNT. We observed a significant increase in total BAL macrophages, however, exclusively after 6d CNT instillation. This d6 peak coincided with the loss of F4/80+/CD11c+/CD11b- alveolar macrophages (AMs) for MWCNTs, and to a lesser extent DWCNTs, in lung FACS. In parallel, we noticed the pulmonary accumulation of a transitional macrophage population at d6 uniquely after MWCNT instillation, and not DWCNTs. According to RNA velocity analysis, blood monocytes differentiate into Lyve1-/CD163- interstitial macrophages and subsequently give rise to this transitional population which fails to replenish the CD11c+/SiglecFhigh AM pool. These cells show high similarity with the initiating monocyte-derived macrophage population necessary for bleomycin- and asbestos-induced lung fibrosis (Misharin et al.,JEM,2017.214(8)). The pro-fibrotic role of this population also has been demonstrated in context of SARsCoV2 infection-associated acute respiratory distress (Wendisch et al.,Cell,2021.184(26)). We summarize, that this transitional cell population are monocyte-derived AM precursors, which lack the ability to differentiate into mature AMs being the decisive mechanism for MWCNT induced, not resolving lung fibrosis.

Published

2023

32. 54 Impact of Carbon Nanoparticle–Triggered Gammaherpesvirus Reactivation on Lung Immunity and Diseases

Author

Eva M Guenther, Verena Haefner, Lianyong Han, Carola Voss, Ali Oender Yildirim, Heiko Adler, and Tobias Stoeger

Subjects

Public Health, Environmental and Occupational Health

Abstract

Inhalation of environmental particles and herpesvirus infection are ubiquitous in our society. Herpesviruses persist lifelong in the host in a latent state, which can be exited by stress-induced reactivation with production of lytic virus. Our previous investigations show that pulmonary exposure to carbon nanoparticles (CNP) triggers reactivation of latent murine gammaherpesvirus 68 (MHV-68) in mouse lungs, mainly localizing to CD11b+ infiltrating macrophages and dependent on p38 MAPK signaling. Furthermore, we observed that a two-time repeated CNP administration to latently infected mice resulted in alveolar damage leading to progressive emphysema. However, the underlying adverse mechanisms causing alveolar damage and the corresponding cell communication upon CNP exposure in latently infected lungs is still unclear. To investigate this, we developed a 3D lung organoid culture from primary murine epithelial cells in combination with persistently MHV-68 infected macrophages. This model enables us to detect reactivation and cytokine release upon CNP exposure, and to gain insights into the cellular communication of epithelial cells and macrophages, to understand the mechanisms underlying reactivation-triggered damage. In parallel, adverse effects of this second hit scenario on the alveolar epithelium and subsequent disease development get investigated in vivo. Latently infected mice are exposed to CNP up to 5 times, and virus reactivation and further epithelial damage is analyzed. By uncovering molecular mechanisms underlying the adverse effects and elucidating the communication occurring in vitro and in vivo we want to identify potential targets to prevent exacerbation of lung diseases caused by these two omnipresent factors, herpesvirus infection and ambient particle exposure.

Published

2023

33. Real time in vivo investigation of the innate immune response during ventilator-assisted nanoparticle inhalation

Author

Qiongliang Liu, Yang Lin, Chenxi Li, Otmar Schmid, Tobias Stoeger, and Markus Rehberg

Published

2022

34. Rescue of STAT3 Function in Hyper-IgE Syndrome Using Adenine Base Editing

Author

Michelle Plummer, Miriam T Kastlmeier, Renate Effner, Anna Pertek, Riccardo Berutti, Tobias Stoeger, Ellen D. Renner, Thomas Meitinger, Amina Sayed, Ejona Rusha, Florian Giesert, Thomas Volz, Beate Hagl, Carola Voss, Micha Drukker, Andreas C. Eberherr, Elisabeth Graf, Christine Wolf, Tim M. Strom, Andre Maaske, and Alena Buyx

Subjects

STAT3 Transcription Factor, Heterozygote, Induced Pluripotent Stem Cells, Immunoglobulin E, Genetics, Humans, Medicine, Clustered Regularly Interspaced Short Palindromic Repeats, Base (exponentiation), STAT3, Gene Editing, Whole Genome Sequencing, biology, business.industry, Adenine, High-Throughput Nucleotide Sequencing, Cell Differentiation, Fibroblasts, medicine.disease, Lung disease, Mutation, Immunology, biology.protein, Primary immunodeficiency, CRISPR-Cas Systems, business, Job Syndrome, Function (biology), Biotechnology

Abstract

STAT3-hyper IgE syndrome (STAT3-HIES) is a primary immunodeficiency presenting with destructive lung disease along with other symptoms. CRISPR-Cas9-mediated adenine base editors (ABEs) have the potential to correct one of the most common STAT3-HIES causing heterozygous

Published

2021

35. 45 Behavior and Effect of Nanoparticles on Neutrophil Recruitment in the Pulmonary Microcirculation

Author

Chenxi Li, Qiongliang Liu, Tobias Stoeger, and Markus Rehberg

Subjects

Public Health, Environmental and Occupational Health

Abstract

NP exposure is frequently associated with adverse cardiovascular effects. A small fraction of NP deposited in lung has been shown to penetrate into the blood circulation. However, the interactions and effects of NP in the pulmonary microcirculation under healthy and pathophysiologic conditions such as LPS-induced acute lung injury are largely unknown. To visualize and quantify NP dynamics and pulmonary vascular innate immune responses elicited by different surface-modified NPs in real time, we applied state-of-the-art intra-vital microscopy in the alveolar region of murine lungs. I.v. injected polyethylene-glycol-amine (aPEG)-QDs and carboxyl-QDs exhibited a half-life time of 30 and 6 mins in the microcirculation and did not permanently interact with vessel wall. Blood flow velocity was significantly decreased after aPEG-QDs application in healthy mice, but did not further decrease the reduced microcirculatory perfusion after LPS treatment. In healthy mice, aPEG-QDs elicited a significant increase in neutrophil number in alveolar micro-vessels from 30 min upon application compared to controls, whereas cQDs induced only a slight neutrophil increment. Accordingly, the crawling velocity of neutrophils in pulmonary micro-vessels was significantly reduced after aPEG-QDs application. No effect of QDs on neutrophil number and crawling was detected in the LPS group. Importantly, neutrophil recruitment by aPEG-QDs was diminished by prior i.v. application of anti-TNFa, anti-E-selectin and anti-LFA-1 blocking antibodies. Taken together our data suggest that aPEG-QDs induced microvascular inflammation involving TNFa secretion, expression of the vascular cell adhesion molecule E-selectin and neutrophil integrin LFA-1, whereas QDs application did not alter LPS-dependent microvascular inflammation.

Published

2023

36. 60 Multimodal Imaging and Artificial Intelligence Unveil Hot-Spot Deposition, Bronchial/Alveolar Dose and Cellular Fate of Biopersistent Nanoparticles in the Lung

Author

Lin Yang, Qiongliang Liu, Pramod Kumar, Arunima Sengupta, Ali Farnoud, Ruolin Shen, Darya Trofimova, Sebastian Ziegler, David Kutschke, Wolfgang Kreyling, Marie Piraud, Fabian Isensee, Gerald Burgstaller, Markus Rehberg, Tobias Stoeger, and Otmar Schmid

Subjects

Public Health, Environmental and Occupational Health

Abstract

Pulmonary delivery is not only of increasing importance to exploit local therapy for lung diseases like COVID-19, but also plays an essential role in interpreting health impact of inhaled hazardous (nano-)materials. Deciphering of biodistribution, biokinetics, and cell-mediated immunity of pulmonary delivered nanoparticles (NPs) remains insufficient. We applied state-of-the-art multimodal imaging and deep learning pipelines to elucidate the intricate deposition profiles and the fate of biopersistent NPs in the lung within cellular resolution. Spatially resolved delivery characteristics like inter- and intra-acinar distribution pattern and regional NP dosage were revealed by tissue-clearing light-sheet fluorescence microscopy for six common routes of pulmonary delivery, i.e., intranasal & oropharyngeal aspiration, intubated instillation, microsprayer application, ventilator-assisted & nose-only aerosol inhalation. Artificial intelligence-driven entire airway 3D segmentation (convolutional neural network) enabled accurate dosimetry of bronchial versus acinar/alveolar NP dose (B/A: 0.04 to 0.18 depending on delivery route) rather than the conventionally simplified 2D central-to-peripheral ratio (C/P: 1.32 to 3.79). Moreover, longitudinal 3D imaging revealed similar intra-acinar NP kinetics independent of delivery route. Inhaled NP relocation from the alveolar-epithelium to interstitium was traditionally claimed as the consequence of passive diffusion/transportation of NPs. This study, however, revealed that acinar NP transport can be attributed to the phagocytosis and migration of tissue-resident macrophages (TRMs) as evidenced by complementary analytical approaches (intravital microscopy, ex vivo 4D live-tissue microscopy, in situ immunofluorescence, ex vivo NP-lung interaction model, flow cytometry). Overall, this study elucidates holistic NP-lung delivery and biokinetics features and TRM immunity on the fate of biopersistent NPs.

Published

2023

37. Reactivation of latent virus infection links air pollutants to chronic lung disease

Author

Verena Haefner, Lianyong Han, David Kutschke, Beatrix Steer, Ali Oender Yildirim, Heiko Adler, and Tobias Stoeger

Published

2022

38. Ferroptosis, induced by macrophages drives COPD pathogenesis

Author

Aicha Jeridi, Gizem Günes Günsel, Mariia Novikava, Sebastian Doll, Niklas J. Lang, Stijin E. Verleden, Markus Rehberg, Tobias Stoeger, Herbert B. Schiller, Marcus Conrad, Thomas M. Conlon, and Ali Önder Yildirim

Published

2022

39. Environmental Nanoparticle Exposure Triggers Herpesvirus Reactivation via MAPK Signaling Pathway

Author

Lianyong Han, Verena Haefner, David Kutschke, Anna Fuchs, Beatrix Steer, Martin Irmler, Johannes Beckers, Heiko Adler, and Tobias Stoeger

Published

2022

40. Course of lung inflammation and injury caused by nanoparticle inhalation depends on material specific cellular perturbation pattern

Author

Carola Voss, Meshal Ansari, Maximilian Strunz, Ilias Angelidis, Verena Haefner, Christoph Mayr, Carol Ballester-Lopez, Qiongliang Liu, Lianyong Han, Thomas M Conlon, Herbert B Schiller, and Tobias Stoeger

Published

2022

41. Chronic Pseudomonas aeruginosa Lung Infection Is IL-1R Independent, but Relies on MyD88 Signaling

Author

Dieudonnée Togbe, Jean-Claude Sirard, Corinne Panek, Jennifer Palomo, Marc Le Bert, Hana Čipčić Paljetak, Herbert B. Schiller, François Huaux, Thomas Secher, Tiffany Marchiol, Valérie F. J. Quesniaux, Tobias Stoeger, François Erard, Claire Mackowiak, Isabelle Couillin, Bernhard Ryffel, Louis Fauconnier, F. Savigny, Delphine Sedda, Alessandra Bragonzi, Immunologie et Neurogénétique Expérimentales et Moléculaires (INEM), Université d'Orléans (UO)-Centre National de la Recherche Scientifique (CNRS), Artimmune SAS, University of Zagreb, Artimmune, privé, Centre d’Etude des Pathologies Respiratoires (CEPR), UMR 1100 (CEPR), Université de Tours (UT)-Institut National de la Santé et de la Recherche Médicale (INSERM), IRCCS Ospedale San Raffaele [Milan, Italy], Université libre de Bruxelles (ULB), German Research Center for Environmental Health - Helmholtz Center München (GmbH), Centre d’Infection et d’Immunité de Lille - INSERM U 1019 - UMR 9017 - UMR 8204 (CIIL), Institut Pasteur de Lille, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lille-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)-Centre National de la Recherche Scientifique (CNRS), This work was supported by the Région Centre (ResPig project), CNRS of Orléans (France), and European funding in Région Centre-Val de Loire (FEDER 2016-00110366 BIO-TARGET, EX005756 BIO-TARGET II, and EUROFéRI EX010381)., Centre National de la Recherche Scientifique (CNRS)-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)-Université de Lille-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut Pasteur de Lille, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP), Université de Tours-Institut National de la Santé et de la Recherche Médicale (INSERM), and Sirard, Jean-Claude

Subjects

Cell type, Myeloid, keratinocyte-derived chemokine, Pseudomonas aeruginosa, chronic lung infection, MyD88 signaling, [SDV]Life Sciences [q-bio], Immunology, MPO, knockout, Inflammation, medicine.disease_cause, Cystic fibrosis, Proinflammatory cytokine, Epithelial Damage, 03 medical and health sciences, 0302 clinical medicine, medicine, Immunology and Allergy, 030304 developmental biology, 0303 health sciences, biology, business.industry, KO, General Medicine, medicine.disease, 3. Good health, [SDV] Life Sciences [q-bio], myeloperoxidase, medicine.anatomical_structure, Myeloperoxidase, biology.protein, medicine.symptom, business, 030215 immunology

Abstract

Cystic fibrosis is associated with chronic Pseudomonas aeruginosa colonization and inflammation. The role of MyD88, the shared adapter protein of the proinflammatory TLR and IL-1R families, in chronic P. aeruginosa biofilm lung infection is unknown. We report that chronic lung infection with the clinical P. aeruginosa RP73 strain is associated with uncontrolled lung infection in complete MyD88-deficient mice with epithelial damage, inflammation, and rapid death. Then, we investigated whether alveolar or myeloid cells contribute to heightened sensitivity to infection. Using cell-specific, MyD88-deficient mice, we uncover that the MyD88 pathway in myeloid or alveolar epithelial cells is dispensable, suggesting that other cell types may control the high sensitivity of MyD88-deficient mice. By contrast, IL-1R1–deficient mice control chronic P. aeruginosa RP73 infection and IL-1β Ab blockade did not reduce host resistance. Therefore, the IL-1R1/MyD88 pathway is not involved, but other IL-1R or TLR family members need to be investigated. Our data strongly suggest that IL-1 targeted neutralizing therapies used to treat inflammatory diseases in patients unlikely reduce host resistance to chronic P. aeruginosa infection.

Published

2021

42. Nanomaterial- and shape-dependency of TLR2 and TLR4 mediated signaling following pulmonary exposure to carbonaceous nanomaterials in mice

Author

Kristina Bram Knudsen, Tobias Stoeger, Katja Maria Bendtsen, Pernille Høgh Danielsen, Ulla Vogel, and Sarah S. Poulsen

Subjects

Lipopolysaccharide, Health, Toxicology and Mutagenesis, Acute phase response, Inflammation, 02 engineering and technology, Pharmacology, Toxicology, 03 medical and health sciences, chemistry.chemical_compound, Mice, RA1190-1270, medicine, Animals, Receptor, Lung, Acute Phase Response, Knockout Mice, Nanomaterials, Toll-like Receptors, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Nanotubes, Carbon, Research, Acute-phase protein, General Medicine, HD7260-7780.8, 021001 nanoscience & nanotechnology, Toll-Like Receptor 2, 3. Good health, Toll-like receptors, Mice, Inbred C57BL, Toll-Like Receptor 4, TLR2, medicine.anatomical_structure, chemistry, Toxicology. Poisons, Knockout mouse, TLR4, Industrial hygiene. Industrial welfare, medicine.symptom, 0210 nano-technology, Knockout mice

Abstract

Background Pulmonary exposure to high doses of engineered carbonaceous nanomaterials (NMs) is known to trigger inflammation in the lungs paralleled by an acute phase response. Toll-like receptors (TLRs), particularly TLR2 and TLR4, have recently been discussed as potential NM-sensors, initiating inflammation. Using Tlr2 and Tlr4 knock out (KO) mice, we addressed this hypothesis and compared the pattern of inflammation in lung and acute phase response in lung and liver 24 h after intratracheal instillation of three differently shaped carbonaceous NMs, spherical carbon black (CB), multi-walled carbon nanotubes (CNT), graphene oxide (GO) plates and bacterial lipopolysaccharide (LPS) as positive control. Results The LPS control confirmed a distinct TLR4-dependency as well as a pronounced contribution of TLR2 by reducing the levels of pulmonary inflammation to 30 and 60% of levels in wild type (WT) mice. At the doses chosen, all NM caused comparable neutrophil influxes into the lungs of WT mice, and reduced levels were only detected for GO-exposed Tlr2 KO mice (35%) and for CNT-exposed Tlr4 KO mice (65%). LPS-induced gene expression was strongly TLR4-dependent. CB-induced gene expression was unaffected by TLR status. Both GO and MWCNT-induced Saa1 expression was TLR4-dependent. GO-induced expression of Cxcl2, Cxcl5, Saa1 and Saa3 were TLR2-dependent. NM-mediated hepatic acute phase response in terms of liver gene expression of Saa1 and Lcn2 was shown to depend on TLR2 for all three NMs. TLR4, in contrast, was only relevant for the acute phase response caused by CNTs, and as expected by LPS. Conclusion TLR2 and TLR4 signaling was not involved in the acute inflammatory response caused by CB exposure, but contributed considerably to that of GO and CNTs, respectively. The strong involvement of TLR2 in the hepatic acute phase response caused by pulmonary exposure to all three NMs deserves further investigations.

Published

2021

43. Chronic

Author

Claire, Mackowiak, Tiffany, Marchiol, Hana Cipcic, Paljetak, Louis, Fauconnier, Jennifer, Palomo, Thomas, Secher, Corinne, Panek, Delphine, Sedda, Florence, Savigny, Francois, Erard, Alessandra, Bragonzi, Francois, Huaux, Tobias, Stoeger, Herbert B, Schiller, Jean-Claude, Sirard, Marc, Le Bert, Isabelle, Couillin, Valerie F J, Quesniaux, Dieudonnée, Togbe, and Bernhard, Ryffel

Subjects

Mice, Knockout, Receptors, Interleukin-1 Type I, Interleukin-1beta, Toll-Like Receptors, Immunity, Innate, Mice, Inbred C57BL, Mice, Myeloid Differentiation Factor 88, Pseudomonas aeruginosa, Animals, Humans, Pseudomonas Infections, Lung, Signal Transduction

Abstract

Cystic fibrosis is associated with chronic

Published

2020

44. Acute Phase Response as a Biological Mechanism-of-Action of (Nano)particle-Induced Cardiovascular Disease

Author

Vadim Zhernovkov, Herbert B. Schiller, Niels Hadrup, Nicklas Raun Jacobsen, Sabina Halappanavar, Ulla Vogel, Meshal Ansari, Sarah S. Poulsen, Maximilian Strunz, Carola Voss, Anne T. Saber, Boris N. Kholodenko, and Tobias Stoeger

Subjects

Occupational disease, 02 engineering and technology, Disease, 010402 general chemistry, Bioinformatics, 01 natural sciences, Biomaterials, SDG 3 - Good Health and Well-being, medicine, Humans, General Materials Science, Particle Size, Acute-Phase Reaction, Lung cancer, Lung, Inhalation Exposure, Inhalation, biology, business.industry, Atherosclerosis, Cardiovascular Diseases, C-reactive Protein, Nanoparticles, Occupational Exposure, Serum Amyloid A, C-reactive protein, Acute-phase protein, General Chemistry, 021001 nanoscience & nanotechnology, medicine.disease, 3. Good health, 0104 chemical sciences, Occupational Diseases, Mechanism of action, biology.protein, Particulate Matter, medicine.symptom, 0210 nano-technology, business, Risk assessment, Biotechnology

Abstract

Inhaled nanoparticles constitute a potential health hazard due to their size-dependent lung deposition and large surface to mass ratio. Exposure to high levels contributes to the risk of developing respiratory and cardiovascular diseases, as well as of lung cancer. Particle-induced acute phase response may be an important mechanism of action of particle-induced cardiovascular disease. Here, the authors review new important scientific evidence showing causal relationships between inhalation of particle and nanomaterials, induction of acute phase response, and risk of cardiovascular disease. Particle-induced acute phase response provides a means for risk assessment of particle-induced cardiovascular disease and underscores cardiovascular disease as an occupational disease.

Published

2020

45. Biological and phylogenetic characterization of a novel hemagglutination-negative avian avulavirus 6 isolated from wild waterfowl in China

Author

Zhe Liu, Yidong Fei, Yanyu Chen, Zhuang Ding, Renfu Yin, Junjiao Li, Xinxin Liu, Tobias Stoeger, Jianjun Chen, and Yuhai Bi

Subjects

0301 basic medicine, Serotype, China, Genotype, Zoology, Animals, Wild, Biology, Serogroup, Aavv-6, Domestic Poultry, Intercontinental Transmission, Wild Bird, Feces, 03 medical and health sciences, Phylogenetics, Waterfowl, Animals, Avulavirus, Phylogeny, Poultry Diseases, General Veterinary, General Immunology and Microbiology, Phylogenetic tree, Bird Diseases, business.industry, Avulavirus Infections, Hemagglutination, intercontinental transmission, domestic poultry, Hemagglutination Tests, General Medicine, Poultry farming, biology.organism_classification, Ducks, 030104 developmental biology, wild bird, Rapid Communications, Animals, Domestic, Influenza in Birds, Cloaca, business, Chickens, Rapid Communication, AAvV‐6

Abstract

Up to now only nine whole genome sequences of avian avulavirus 6 (AAvV‐6) had been documented in the world since the first discovery of AAvV‐6 (AAvV‐6/duck/HongKong/18/199/77) at a domestic duck in 1977 from Hong Kong of China. Very limited information is known about the regularities of transmission, genetic and biological characteristics of AAvV‐6 because of the lower isolation rate and mild losses for poultry industry. To better further explore the relationships among above factors, an AAvV‐6 epidemiological surveillance of domestic poultry and wild birds in six provinces of China suspected of sites of inter‐species transmission and being intercontinental flyways during the year 2013–2017 was conducted. Therefore, 9,872 faecal samples from wild birds and 1,642 cloacal and tracheal swab samples from clinically healthy poultry of live bird market (LBM) were collected respectively. However, only one novel hemagglutination‐negative AAvV‐6 isolate (AAvV‐6/mallard/Hubei/2015) was isolated from a fresh faecal sample obtained from mallard at a wetland of Hubei province. Sequencing and phylogenetic analyses of this AAvV‐6 isolate (AAvV‐6/mallard/Hubei/2015) indicated that this isolate grouping to genotype I were epidemiological intercontinentally linked with viruses from the wild birds in Europe and America. Meanwhile, at least two genotypes (I and II) are existed within serotype AAvV‐6. In additional, this novel hemagglutination‐negative AAvV‐6 isolate in chicken embryos restored its hemagglutination when pre‐treated with trypsin. These findings, together with data from other AAvV‐6, suggest potential epidemiological intercontinental spreads among AAvV‐6 transmission by wild migratory birds, and reveal potential threats to wild birds and domestic poultry worldwide.

Published

2018

46. In vivo Dynamic Phase-Contrast X-ray Imaging using a Compact Light Source

Author

Kaye S. Morgan, Lorenz Hehn, Benedikt Günther, Lin Yang, Winfried Möller, Martin Dierolf, Regine Gradl, David Kutschke, Otmar Schmid, Martin Donnelley, Rhiannon P. Murrie, Tobias Stoeger, Alexander Erl, Bernhard Gleich, Franz Pfeiffer, and Klaus Achterhold

Subjects

0301 basic medicine, 030103 biophysics, Multidisciplinary, Materials science, Focus (geometry), Mucociliary clearance, Dynamic imaging, Phase-contrast X-ray imaging, Science, 02 engineering and technology, Synchrotron light source, 021001 nanoscience & nanotechnology, Article, 3. Good health, ddc, 03 medical and health sciences, Light source, In vivo, Medicine, 0210 nano-technology, Respiratory health, Biomedical engineering

Abstract

We describe the first dynamic and the first in vivo X-ray imaging studies successfully performed at a laser-undulator-based compact synchrotron light source. The X-ray properties of this source enable time-sequence propagation-based X-ray phase-contrast imaging. We focus here on non-invasive imaging for respiratory treatment development and physiological understanding. In small animals, we capture the regional delivery of respiratory treatment, and two measures of respiratory health that can reveal the effectiveness of a treatment; lung motion and mucociliary clearance. The results demonstrate the ability of this set-up to perform laboratory-based dynamic imaging, specifically in small animal models, and with the possibility of longitudinal studies.

Published

2018

47. Detrimental effects of microplastic exposure on normal and asthmatic pulmonary physiology

Author

Michael Lo, Xiao Lin, Ji Shuqin, James K. H. Fang, Lingwei Wang, Tobias Stoeger, Ziyi Lin, Ting-Fung Chan, Chen Qiu, Guobing Chen, Lei Li, Liang Gao, Keng Po Lai, Kuo Lu, and Shanze Chen

Subjects

Programmed cell death, Environmental Engineering, Microplastics, Health, Toxicology and Mutagenesis, Phagocytosis, 0211 other engineering and technologies, Inflammation, 02 engineering and technology, 010501 environmental sciences, 01 natural sciences, Mice, Immune system, Cellular stress response, Microplastic, Asthma, Respiratory System, Health Risk, Transcriptome, medicine, Animals, Environmental Chemistry, Macrophage, Lung, Waste Management and Disposal, 0105 earth and related environmental sciences, Mice, Inbred BALB C, 021110 strategic, defence & security studies, medicine.diagnostic_test, business.industry, Pollution, Bronchoalveolar lavage, Immunology, Tumor necrosis factor alpha, medicine.symptom, business, Bronchoalveolar Lavage Fluid, Plastics

Abstract

Concerns that airborne microplastics (MP) may be detrimental to human health are rising. However, research on the effects of MP on the respiratory system are limited. We tested the effect of MP exposure on both normal and asthmatic pulmonary physiology in mice. We show that MP exposure caused pulmonary inflammatory cell infiltration, bronchoalveolar macrophage aggregation, increased TNF-alpha level in bronchoalveolar lavage fluid (BALF), and increased plasma IgG1 production in normal mice. MP exposure also affected asthma symptoms by increasing mucus production and inflammatory cell infiltration with notable macrophage aggregation. Further, we found co-labeling of macrophage markers with MP incorporating fluorescence, which indicates phagocytosis of the MP by macrophages. A comparative transcriptomic analysis showed that MP exposure altered clusters of genes related to immune response, cellular stress response, and programmed cell death. A bioinformatics analysis further uncovered the molecular mechanism whereby MP stimulated production of tumor necrosis factor and immunoglobulins to activate a group of transmembrane B-cell antigens, leading to the modulation of cellular stress and programmed cell death in the asthma model. In summary, we show that MP exposure had detrimental effects on the respiratory system in both healthy and asthmatic mice, which calls for urgent discourse and action to mitigate environmental microplastic pollutants.

Published

2021

48. Inhibition of LTβR signalling activates WNT-induced regeneration in lung

Author

Zeynep Ertüz, Giorgi Beroshvili, Dominik Pfister, Adrien Guillot, Oliver Eickelberg, Mathias Heikenwalder, Eric Goffin, Reinoud Gosens, Gerald Burgstaller, Danijela Heide, Maximilian Strunz, Fabian J. Theis, Mareike Lehmann, Martin A. Lopez, Michael Boutros, Aicha Jeridi, Darcy E. Wagner, Yan Hu, Marlene Kohlhepp, Tracy O'Connor, Lore Becker, Frank Tacke, Thomas M. Conlon, Meshal Ansari, Indrabahadur Singh, Christoph Mayr, Martin Hrabé de Angelis, Tobias Stoeger, Emmanuel Dejardin, Hani N. Alsafadi, Melanie Königshoff, Sandra Prokosch, Chiara Ciminieri, Michael Dudek, Bernard Pirotte, Herbert B. Schiller, Johannes Beckers, Maja C. Funk, Percy A. Knolle, Martin Irmler, Stijn E. Verleden, Michael Lindner, Gizem Gunes, Rita Costa, Jenny Hetzer, Gerrit John-Schuster, Jakob Janzen, Ali Önder Yildirim, Groningen Research Institute for Asthma and COPD (GRIAC), Molecular Pharmacology, and Nanomedicine & Drug Targeting

Subjects

0301 basic medicine, Aging, Apoptosis, Adaptive Immunity, Article, 03 medical and health sciences, Mice, Pulmonary Disease, Chronic Obstructive, 0302 clinical medicine, Fibrosis, Lymphotoxin beta Receptor, Smoke, medicine, Animals, Humans, Regeneration, Progenitor cell, Lung, beta Catenin, Emphysema, Multidisciplinary, Innate immune system, business.industry, Regeneration (biology), Stem Cells, Wnt signaling pathway, NF-kappa B, Acquired immune system, medicine.disease, Epithelium, Immunity, Innate, 3. Good health, Mice, Inbred C57BL, Wnt Proteins, 030104 developmental biology, Lymphotoxin, medicine.anatomical_structure, 030228 respiratory system, Alveolar Epithelial Cells, Cancer research, Female, business, Engineering sciences. Technology, Signal Transduction

Abstract

Blockade of lymphotoxin beta-receptor (LT beta R) signalling restores WNT signalling and epithelial repair in a model of chronic obstructive pulmonary disease. Lymphotoxin beta-receptor (LT beta R) signalling promotes lymphoid neogenesis and the development of tertiary lymphoid structures(1,2), which are associated with severe chronic inflammatory diseases that span several organ systems(3-6). How LT beta R signalling drives chronic tissue damage particularly in the lung, the mechanism(s) that regulate this process, and whether LT beta R blockade might be of therapeutic value have remained unclear. Here we demonstrate increased expression of LT beta R ligands in adaptive and innate immune cells, enhanced non-canonical NF-kappa B signalling, and enriched LT beta R target gene expression in lung epithelial cells from patients with smoking-associated chronic obstructive pulmonary disease (COPD) and from mice chronically exposed to cigarette smoke. Therapeutic inhibition of LT beta R signalling in young and aged mice disrupted smoking-related inducible bronchus-associated lymphoid tissue, induced regeneration of lung tissue, and reverted airway fibrosis and systemic muscle wasting. Mechanistically, blockade of LT beta R signalling dampened epithelial non-canonical activation of NF-kappa B, reduced TGF beta signalling in airways, and induced regeneration by preventing epithelial cell death and activating WNT/beta-catenin signalling in alveolar epithelial progenitor cells. These findings suggest that inhibition of LT beta R signalling represents a viable therapeutic option that combines prevention of tertiary lymphoid structures(1) and inhibition of apoptosis with tissue-regenerative strategies.

Published

2019

49. In vivo x-ray imaging of the respiratory system using synchrotron sources and a compact light source

Author

Mark Gardner, Nigel Farrow, Freda Werdiger, Martin Dierolf, Kaye S. Morgan, Christoph Jud, David Kutschke, Lin Yang, Regine Gradl, Alexandra McCarron, Martin Donnelley, Patricia Cmielewski, Melanie A. Kimm, Tobias Stoeger, Benedikt Günther, Helena Haas, Franz Pfeiffer, Otmar Schmid, Klaus Achterhold, and David Parsons

Subjects

Physics, business.industry, Attenuation, Biomedical Imaging, Respiratory Imaging, Talbot-lau Grating Interferometry, X-ray Phase Contrast, X-ray, Synchrotron radiation, Signal, Synchrotron, law.invention, Optics, Beamline, law, Medical imaging, business, Australian Synchrotron

Abstract

Bright synchrotron x-ray sources enable imaging with short exposure times, and hence in a high-speed image sequence. These x-ray movies can capture not only sample structure, but also how the sample changes with time, how it functions. The use of a synchrotron x-ray source also provides high spatial coherence, which facilitates the capture of not only a conventional attenuation-based x-ray image, but also phase-contrast and dark-field signals. These signals are strongest from air/tissue interfaces, which means that they are particularly useful for examining the respiratory system. We have performed a range of x-ray imaging studies that look at lung function, airway surface function, inhaled and instilled treatment delivery, and treatment effect in live small animal models [Morgan, 2019]. These have utilized a range of optical set-ups and phase-contrast imaging methods in order to be sensitive to the relevant sample features, and be compatible with high-speed imaging. For example, we have used a grating interferometer to measure how the airsacs in the lung inflate during inhalation, via changes in the dark-field signal [Gradl, 2018], a single-exposure, single-grid set-up to capture changes in the liquid lining of the airways [Morgan, 2015] and propagation-based phase contrast to image clearance of inhaled debris [Donnelley, 2019]. Studies have also utilized a range of analysis methods to extract how the sample features change within a time-sequence of two-dimensional projections or three-dimensional volumes. While these imaging studies began in large-scale synchrotron facilities, we have recently performed these kinds of studies at an inverse-Compton-based compact synchrotron, the Munich Compact Light Source (MuCLS) [Gradl, 2018b]. 1. Morgan, Kaye, et al., “Methods for dynamic synchrotron X-ray imaging of live animals.”, under review 01/2019. 2. Gradl, R., et al. "Dynamic in vivo chest x-ray dark-field imaging in mice." IEEE Transactions on Medical Imaging (2018). 3. Morgan, Kaye S., et al. "In vivo X-ray imaging reveals improved airway surface hydration after a therapy designed for cystic fibrosis." American Journal of Respiratory and Critical Care Medicine 190.4 (2014): 469-472. 4. Donnelley, Martin, et al. "Live-pig-airway surface imaging and whole-pig CT at the Australian Synchrotron Imaging and Medical Beamline." Journal of Synchrotron Radiation 26.1 (2019). 5. Gradl, Regine, et al. "In vivo Dynamic Phase-Contrast X-ray Imaging using a Compact Light Source." Scientific Reports 8.1 (2018b): 6788.

Published

2019

50. The Emergence of Avian Orthoavulavirus 13 in Wild Migratory Waterfowl in China Revealed the Existence of Diversified Trailer Region Sequences and HN Gene Lengths within this Serotype

Author

Jianjun Chen, Yuhai Bi, Alongkorn Amonsin, Alexander Shestopalov, Abdul Wajid, Yidong Fei, Zhuang Ding, Xibing Yu, Renfu Yin, Jin Chang, Tobias Stoeger, Xinxin Liu, Denys Muzyka, Kirill Sharshov, Jiaqi Mu, and Junjiao Li

Subjects

0301 basic medicine, Serotype, China, medicine.medical_specialty, 030106 microbiology, lcsh:QR1-502, Zoology, Animals, Wild, Genome, Viral, avian orthoavulavirus 13, Serogroup, lcsh:Microbiology, Conserved sequence, migratory waterfowl, 03 medical and health sciences, Goose, genetic relationships, Phylogenetics, Virology, biology.animal, Molecular genetics, Geese, Genetic variation, Waterfowl, medicine, Animals, Avulavirus, Phylogeny, HN Protein, biology, Phylogenetic tree, Avulavirus Infections, Brief Report, HN gene, Sequence Analysis, DNA, biology.organism_classification, Ducks, Avian Orthoavulavirus 13, Migratory Waterfowl, Hn Gene, Trailer, Genetic Relationships, 030104 developmental biology, Infectious Diseases, RNA, Viral, Animal Migration, Chickens, trailer

Abstract

Avian orthoavulavirus 13 (AOAV-13), also named avian paramyxovirus 13 (APMV-13), has been found sporadically in wild birds around the world ever since the discovery of AOAV-13 (AOAV-13/wild goose/Shimane/67/2000) in a wild goose from Japan in 2000. However, there are no reports of AOAV-13 in China. In the present study, a novel AOAV-13 virus (AOAV-13/wild goose/China/Hubei/V93-1/2015), isolated from a wild migratory waterfowl in a wetland of Hubei province of China, during active surveillance from 2013 to 2018, was biologically and genetically characterized. Phylogenetic analyses demonstrated a very close genetic relationship among all AOAV-13 strains, as revealed by very few genetic variations. Moreover, pathogenicity tests indicated that the V93-1 strain is a low virulent virus for chickens. However, the genome of the V93-1 virus was found to be 16,158 nucleotides (nt) in length, which is 12 nt or 162 nt longer than the other AOAV-13 strains that have been reported to date. The length difference of 12 nt in strain V93-1 is due to the existence of three repeats of the conserved sequence, “AAAAAT”, in the 5′-end trailer of the genome. Moreover, the HN gene of the V93-1 virus is 2070 nt in size, encoding 610 aa, which is the same size as the AOAV-13 strain from Japan, whereas that of two strains from Ukraine and Kazakhstan are 2080 nt in length, encoding 579 aa. We describe a novel AOAV-13 in migratory waterfowl in China, which suggests that diversified trailer region sequences and HN gene lengths exist within serotype AOAV-13, and highlight the need for its constant surveillance in poultry from live animal markets, and especially migratory birds.

Published

2019