Your search keyword '"Tim, Lämmermann"' showing total 60 results

1. Arp2/3 complex and the pentose phosphate pathway regulate late phases of neutrophil swarming

Author

Katharina M. Glaser, Jacob Doon-Ralls, Nicole Walters, Xilal Y. Rima, Angelika S. Rambold, Eduardo Réategui, and Tim Lämmermann

Subjects

Immunology, Science

Abstract

Summary: Neutrophil swarming is an essential process of the neutrophil response to many pathological conditions. Resultant neutrophil accumulations are hallmarks of acute tissue inflammation and infection, but little is known about their dynamic regulation. Technical limitations to spatiotemporally resolve individual cells in dense neutrophil clusters and manipulate these clusters in situ have hampered recent progress. We here adapted an in vitro swarming-on-a-chip platform for the use with confocal laser-scanning microscopy to unravel the complexity of single-cell responses during neutrophil crowding. Confocal sectioning allowed the live visualization of subcellular components, including mitochondria, cell membranes, cortical actin, and phagocytic cups, inside neutrophil clusters. Based on this experimental setup, we identify that chemical inhibition of the Arp2/3 complex causes cell death in crowding neutrophils. By visualizing spatiotemporal patterns of reactive oxygen species (ROS) production in developing neutrophil swarms, we further demonstrate a regulatory role of the metabolic pentose phosphate pathway for ROS production and neutrophil cluster growth.

Published

2024

2. Differential trafficking of ligands trogocytosed via CD28 versus CTLA4 promotes collective cellular control of co-stimulation

Author

Simon Zenke, Mauricio P. Sica, Florian Steinberg, Julia Braun, Alicia Zink, Alina Gavrilov, Alexander Hilger, Aditya Arra, Monika Brunner-Weinzierl, Roland Elling, Niklas Beyersdorf, Tim Lämmermann, Cristian R. Smulski, and Jan C. Rohr

Subjects

Science

Abstract

A number of costimulatory signals are critical to the activation and regulation of T cells, but how the availability or self-regulation of these occurs was previously unclear. Here the authors show a difference in the fate of ligands trogocytosed by CD28 or CTLA4 and link this to cellular control of costimulation.

Published

2022

3. Analyzing trogocytosis of T lymphocytes by flow cytometry and confocal microscopy

Author

Alicia Zink, Simon Zenke, Teresa Wiese, Niklas Beyersdorf, Tim Lämmermann, and Jan C. Rohr

Subjects

Cell Biology, Flow Cytometry/Mass Cytometry, Cell Membrane, Cell-based Assays, Immunology, Science (General), Q1-390

Abstract

Summary: Here, we present a protocol to examine the mechanisms underlying the intercellular transfer of transmembrane molecules, termed trogocytosis, and the fate of transferred molecules. We describe the steps needed from T lymphocyte isolation, via co-culture with cells expressing the ligand of interest, to cell harvest and subsequent staining for flow cytometry and confocal microscopy. Furthermore, we showcase critical parameters and pitfalls, which allow easy adaptation of the protocol to investigate trogocytosis of various cell surface receptors in different cell types.For complete details on the use and execution of this protocol, please refer to Zink and Rohr.1 : Publisher’s note: Undertaking any experimental protocol requires adherence to local institutional guidelines for laboratory safety and ethics.

Published

2023

4. 100 Hz ROCS microscopy correlated with fluorescence reveals cellular dynamics on different spatiotemporal scales

Author

Felix Jünger, Dominic Ruh, Dominik Strobel, Rebecca Michiels, Dominik Huber, Annette Brandel, Josef Madl, Alina Gavrilov, Michael Mihlan, Caterina Cora Daller, Eva A. Rog-Zielinska, Winfried Römer, Tim Lämmermann, and Alexander Rohrbach

Subjects

Science

Abstract

In live-cell microscopy, motion blur limits resolution and contrast. Here the authors use 100 Hz super-resolving Rotating Coherent Scattering (ROCS) microscopy on various dynamic biological systems, and time-window analysis to understand biological effects.

Published

2022

5. Combinatorial depletions of G-protein coupled receptor kinases in immune cells identify pleiotropic and cell type-specific functions

Author

Katharina M. Glaser, Teresa K. Tarrant, and Tim Lämmermann

Subjects

immune cell trafficking, leukocytes, G-protein coupled receptors, GRK, neutrophils, B cells, Immunologic diseases. Allergy, RC581-607

Abstract

G-protein coupled receptor kinases (GRKs) participate in the regulation of chemokine receptors by mediating receptor desensitization. They can be recruited to agonist-activated G-protein coupled receptors (GPCRs) and phosphorylate their intracellular parts, which eventually blocks signal propagation and often induces receptor internalization. However, there is growing evidence that GRKs can also control cellular functions beyond GPCR regulation. Immune cells commonly express two to four members of the GRK family (GRK2, GRK3, GRK5, GRK6) simultaneously, but we have very limited knowledge about their interplay in primary immune cells. In particular, we are missing comprehensive studies comparing the role of this GRK interplay for (a) multiple GPCRs within one leukocyte type, and (b) one specific GPCR between several immune cell subsets. To address this issue, we generated mouse models of single, combinatorial and complete GRK knockouts in four primary immune cell types (neutrophils, T cells, B cells and dendritic cells) and systematically addressed the functional consequences on GPCR-controlled cell migration and tissue localization. Our study shows that combinatorial depletions of GRKs have pleiotropic and cell-type specific effects in leukocytes, many of which could not be predicted. Neutrophils lacking all four GRK family members show increased chemotactic migration responses to a wide range of GPCR ligands, whereas combinatorial GRK depletions in other immune cell types lead to pro- and anti-migratory responses. Combined depletion of GRK2 and GRK6 in T cells and B cells shows distinct functional outcomes for (a) one GPCR type in different cell types, and (b) different GPCRs in one cell type. These GPCR-type and cell-type specific effects reflect in altered lymphocyte chemotaxis in vitro and localization in vivo. Lastly, we provide evidence that complete GRK deficiency impairs dendritic cell homeostasis, which unexpectedly results from defective dendritic cell differentiation and maturation in vitro and in vivo. Together, our findings demonstrate the complexity of GRK functions in immune cells, which go beyond GPCR desensitization in specific leukocyte types. Furthermore, they highlight the need for studying GRK functions in primary immune cells to address their specific roles in each leukocyte subset.

Published

2022

6. Neutrophils: Amoeboid Migration and Swarming Dynamics in Tissues

Author

Michael Mihlan, Katharina M. Glaser, Maximilian W. Epple, and Tim Lämmermann

Subjects

neutrophil, amoeboid migration, chemoattractants, swarming, inflammation, receptor desensitization, Biology (General), QH301-705.5

Abstract

Neutrophils are key cells of our innate immune response with essential roles for eliminating bacteria and fungi from tissues. They are also the prototype of an amoeboid migrating leukocyte. As one of the first blood-recruited immune cell types during inflammation and infection, these cells can invade almost any tissue compartment. Once in the tissue, neutrophils undergo rapid shape changes and migrate at speeds higher than most other immune cells. They move in a substrate-independent manner in interstitial spaces and do not follow predetermined tissue paths. Instead, neutrophil navigation is largely shaped by the chemokine and chemoattractant milieu around them. This highlights the decisive role of attractant-sensing G-protein coupled receptors (GPCRs) and downstream molecular pathways for controlling amoeboid neutrophil movement in tissues. A diverse repertoire of cell-surface expressed GPCRs makes neutrophils the perfect sentinel cell type to sense and detect danger-associated signals released from wounds, inflamed interstitium, dying cells, complement factors or directly from tissue-invading microbes. Moreover, neutrophils release attractants themselves, which allows communication and coordination between individual cells of a neutrophil population. GPCR-mediated positive feedback mechanisms were shown to underlie neutrophil swarming, a population response that amplifies the recruitment of amoeboid migrating neutrophils to sites of tissue injury and infection. Here we discuss recent findings and current concepts that counteract excessive neutrophil accumulation and swarm formation. In particular, we will focus on negative feedback control mechanisms that terminate neutrophil swarming to maintain the delicate balance between tissue surveillance, host protection and tissue destruction.

Published

2022

7. Macrophage network dynamics depend on haptokinesis for optimal local surveillance

Author

Neil Paterson and Tim Lämmermann

Subjects

macrophages, cell migration, integrins, tissue surveillance, efferocytosis, immune cells, Medicine, Science, Biology (General), QH301-705.5

Abstract

Macrophages are key immune cells with important roles for tissue surveillance in almost all mammalian organs. Cellular networks made up of many individual macrophages allow for optimal removal of dead cell material and pathogens in tissues. However, the critical determinants that underlie these population responses have not been systematically studied. Here, we investigated how cell shape and the motility of individual cells influences macrophage network responses in 3D culture settings and in mouse tissues. We show that surveying macrophage populations can tolerate lowered actomyosin contractility, but cannot easily compensate for a lack of integrin-mediated adhesion. Although integrins were dispensable for macrophage chemotactic responses, they were crucial to control cell movement and protrusiveness for optimal surveillance by a macrophage population. Our study reveals that β1 integrins are important for maintaining macrophage shape and network sampling efficiency in mammalian tissues, and sets macrophage motility strategies apart from the integrin-independent 3D migration modes of many other immune cell subsets.

Published

2022

8. Analyzing Inter-Leukocyte Communication and Migration In Vitro: Neutrophils Play an Essential Role in Monocyte Activation During Swarming

Author

Nicole Walters, Jingjing Zhang, Xilal Y. Rima, Luong T. H. Nguyen, Ronald N. Germain, Tim Lämmermann, and Eduardo Reátegui

Subjects

neutrophils (PMNs), monocytes, neutrophil swarming, intercellular communication, extracellular vesicles, Immunologic diseases. Allergy, RC581-607

Abstract

Neutrophils are known to be the first responders to infection or injury. However, as inflammation progresses, other leukocytes become increasingly important in inflammation propagation, tissue reconstruction, and inflammation resolution. In recent years, there has been an increase in publications that analyze neutrophil behavior in vitro, but there remains a gap in the literature for in vitro technologies that enable quantitatively measuring interactions between different types of human leukocytes. Here, we used an in vitro platform that mimics inflammation by inducing neutrophil swarming to analyze the behavior of various leukocytes in a swarming setting. Using human peripheral blood leukocytes isolated directly from whole blood, we found that myeloid cells and lymphoid cells had different migratory behaviors. Myeloid cells, which are predominately neutrophils, exhibited swarming behavior. This behavior was not seen with lymphoid cells. We perturbed the peripheral blood leukocyte system by adding exogenous leukotriene B4 (LTB4) to the medium. Notably, only the myeloid cell compartment was significantly changed by the addition of LTB4. Additionally, LTB4 had no significant impact on myeloid cell migration during the recruitment phase of swarming. To further investigate the myeloid cell compartment, we isolated neutrophils and monocytes to analyze their interaction on the platform. We found that neutrophils increase monocyte migration toward the bioparticle clusters, as measured through speed, chemotactic index, track straightness, and swarm size. These results were confirmed with in vivo mouse experiments, where monocyte accumulation only occurred when neutrophils were present. Additionally, we found that both neutrophils and monocytes release the monocyte chemoattractant proteins CCL2 and CCL3 in the presence of Staphylococcus aureus bioparticles. Furthermore, extracellular vesicles from swarming neutrophils caused monocyte activation. These findings suggest that neutrophils play an essential role in the onset of inflammation not only by sealing off the site of infection or injury, but also by recruiting additional leukocytes to the site.

Published

2021

9. LC-MS-Based Targeted Metabolomics for FACS-Purified Rare Cells

Author

Katharina Schönberger, Michael Mitterer, Katharina Glaser, Manuel Stecher, Sebastian Hobitz, Dominik Schain-Zota, Konrad Schuldes, Tim Lämmermann, Angelika S. Rambold, Nina Cabezas-Wallscheid, and Joerg M. Buescher

Subjects

Analytical Chemistry

Abstract

Metabolism plays a fundamental role in regulating cellular functions and fate decisions. Liquid chromatography-mass spectrometry (LC-MS)-based targeted metabolomic approaches provide high-resolution insights into the metabolic state of a cell. However, the typical sample size is in the order of 105-107 cells and thus not compatible with rare cell populations, especially in the case of a prior flow cytometry-based purification step. Here, we present a comprehensively optimized protocol for targeted metabolomics on rare cell types, such as hematopoietic stem cells and mast cells. Only 5000 cells per sample are required to detect up to 80 metabolites above background. The use of regular-flow liquid chromatography allows for robust data acquisition, and the omission of drying or chemical derivatization avoids potential sources of error. Cell-type-specific differences are preserved while the addition of internal standards, generation of relevant background control samples, and targeted metabolite with quantifiers and qualifiers ensure high data quality. This protocol could help numerous studies to gain thorough insights into cellular metabolic profiles and simultaneously reduce the number of laboratory animals and the time-consuming and costly experiments associated with rare cell-type purification.

Published

2023

10. Slow integrin-dependent migration organizes networks of tissue-resident mast cells

Author

Lukas Kaltenbach, Paloma Martzloff, Sarah K. Bambach, Nadim Aizarani, Michael Mihlan, Alina Gavrilov, Katharina M. Glaser, Manuel Stecher, Roland Thünauer, Aude Thiriot, Klaus Heger, Katrin Kierdorf, Stephan Wienert, Ulrich H. von Andrian, Marc Schmidt-Supprian, Claus Nerlov, Frederick Klauschen, Axel Roers, Marc Bajénoff, Dominic Grün, Tim Lämmermann, Max Planck Institute of Immunobiology and Epigenetics (MPI-IE), Max-Planck-Gesellschaft, International Max Planck Research School for Immunobiology (IMPRS-IEM freburg), Faculty of Biology, University of Freiburg, Friedrich Miescher Institute for Biomedical Research (FMI), Novartis Research Foundation, Centre for Structural Systems Biology hamburg (Advanced Light and Fluorescence Microscopy Facility), Harvard Medical School [Boston] (HMS), The Ragon Institute of MGH, Department of Cancer Immunology, South San Francisco (Genentech), University of Freiburg [Freiburg], Centre for Integrative Biological Signalling Studies [Freiburg] (CIBSS), Center for Basics in NeuroModulation - Faculty Medicine - University of Freiburg (NeuroModulBasics), Charité - UniversitätsMedizin = Charité - University Hospital [Berlin], Center for Translational Cancer Research - Munich (TranslaTUM), MRC Weatherall Institute of Molecular Medicine - John Radcliffe Hospital, Ludwig-Maximilians University [Munich] (LMU), Berlin Institute for the Foundation of Learning and Data - Berlin (BIFOLD), UniversitätsKlinikum Heidelberg, Centre d'Immunologie de Marseille - Luminy (CIML), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Julius-Maximilians-Universität Würzburg (JMU), University of Würzburg = Universität Würzburg, and Helmholtz Institute for RNA‐based Infection Research (HIRI)

Subjects

Innate immune cells, [SDV]Life Sciences [q-bio], Immunology, Immunology and Allergy, Imaging the immune system, Cell migration

Abstract

Immune cell locomotion is associated with amoeboid migration, a flexible mode of movement, which depends on rapid cycles of actin polymerization and actomyosin contraction1. Many immune cells do not necessarily require integrins, the major family of adhesion receptors in mammals, to move productively through three-dimensional tissue spaces2,3. Instead, they can use alternative strategies to transmit their actin-driven forces to the substrate, explaining their migratory adaptation to changing external environments4–6. However, whether these generalized concepts apply to all immune cells is unclear. Here, we show that the movement of mast cells (immune cells with important roles during allergy and anaphylaxis) differs fundamentally from the widely applied paradigm of interstitial immune cell migration. We identify a crucial role for integrin-dependent adhesion in controlling mast cell movement and localization to anatomical niches rich in KIT ligand, the major mast cell growth and survival factor. Our findings show that substrate-dependent haptokinesis is an important mechanism for the tissue organization of resident immune cells.

Published

2023

11. Gut microbiota drives age-related oxidative stress and mitochondrial damage in microglia via the metabolite N6-carboxymethyllysine

Author

Omar Mossad, Bérénice Batut, Bahtiyar Yilmaz, Nikolaos Dokalis, Charlotte Mezö, Elisa Nent, Lara Susann Nabavi, Melanie Mayer, Feres José Mocayar Maron, Joerg M. Buescher, Mercedes Gomez de Agüero, Antal Szalay, Tim Lämmermann, Andrew J. Macpherson, Stephanie C. Ganal-Vonarburg, Rolf Backofen, Daniel Erny, Marco Prinz, and Thomas Blank

Subjects

General Neuroscience, digestive system

Abstract

Microglial function declines during aging. The interaction of microglia with the gut microbiota has been well characterized during development and adulthood but not in aging. Here, we compared microglial transcriptomes from young-adult and aged mice housed under germ-free and specific pathogen-free conditions and found that the microbiota influenced aging associated-changes in microglial gene expression. The absence of gut microbiota diminished oxidative stress and ameliorated mitochondrial dysfunction in microglia from the brains of aged mice. Unbiased metabolomic analyses of serum and brain tissue revealed the accumulation of N6-carboxymethyllysine (CML) in the microglia of the aging brain. CML mediated a burst of reactive oxygen species and impeded mitochondrial activity and ATP reservoirs in microglia. We validated the age-dependent rise in CML levels in the sera and brains of humans. Finally, a microbiota-dependent increase in intestinal permeability in aged mice mediated the elevated levels of CML. This study adds insight into how specific features of microglia from aged mice are regulated by the gut microbiota.

Published

2022

12. Slow integrin-dependent migration organizes networks of tissue-resident mast cells

Author

Sarah K. Bambach, Lukas Kaltenbach, Nadim Aizarani, Paloma Martzloff, Alina Gavrilov, Katharina M. Glaser, Roland Thünauer, Michael Mihlan, Manuel Stecher, Aude Thiriot, Stephan Wienert, Ulrich von Andrian, Marc Schmidt-Supprian, Claus Nerlov, Frederick Klauschen, Axel Roers, Marc Bajénoff, Dominic Grün, and Tim Lämmermann

Abstract

SUMMARYMany leukocytes use fast and flexible amoeboid migration strategies to move autonomously throughout tissues. Here, we show that the movement of mast cells (MCs), leukocytes with important roles during allergies and anaphylaxis, fundamentally differs from this rapid adhesion-free leukocyte migration. We identify a crucial role for integrin-dependent adhesion in controlling slow MC movement, which shapes the positioning and network-like tissue distribution of this long-lived immune cell type. In contrast to other immune and non-immune cells, MCs cannot compensate for the lack of integrin function by switching to another migration mode. Single-cell RNA-sequencing revealed a special role for integrins in defining a mature MC phenotype in the periarteriolar tissue space where several stromal cell types provide an anatomical niche rich in Kit ligand, the major MC growth and survival factor. Collectively, this study highlights substrate-dependent haptokinesis as an important mechanism for MC network formation and the tissue organization of resident immune cells.

Published

2022

13. Surprises from Intravital Imaging of the Innate Immune Response

Author

Michael Mihlan, Shima Safaiyan, Manuel Stecher, Neil Paterson, and Tim Lämmermann

Subjects

Inflammation, Mice, Intravital Microscopy, Macrophages, Animals, Cell Biology, Immunity, Innate, Developmental Biology

Abstract

Successful immune responses depend on the spatiotemporal coordination of immune cell migration, interactions, and effector functions in lymphoid and parenchymal tissues. Real-time intravital microscopy has revolutionized our understanding of the dynamic behavior of many immune cell types in the living tissues of several species. Observing immune cells in their native environment has revealed many unanticipated facets of their biology, which were not expected from experiments outside a living organism. Here we highlight both classic and more recent examples of surprising discoveries that critically relied on the use of live in vivo imaging. In particular, we focus on five major cell types of the innate immune response (macrophages, microglia, neutrophils, dendritic cells, and mast cells), and how studying their dynamics in mouse tissues has helped us advance our current knowledge of immune cell–mediated tissue homeostasis, host defense, and inflammation.

Published

2022

14. Macrophage network dynamics depend on haptokinesis for optimal local surveillance

Author

Tim Lämmermann and Neil Paterson

Subjects

Integrins, education.field_of_study, biology, General Immunology and Microbiology, Integrin beta1, Macrophages, General Neuroscience, Integrin, Population, Motility, Chemotaxis, General Medicine, Network dynamics, General Biochemistry, Genetics and Molecular Biology, Cell biology, Mice, Immune system, Cell Movement, T cell subset, biology.protein, Animals, Macrophage, education, Cell Shape

Abstract

Macrophages are key immune cells with important roles for tissue surveillance in almost all mammalian organs. Cellular networks made up of many individual macrophages allow for optimal removal of dead cell material and pathogens in tissues. However, the critical determinants that underlie these population responses have not been systematically studied. Here, we investigated how cell shape and the motility of individual cells influences macrophage network responses in 3D culture settings and in mouse tissues. We show that surveying macrophage populations can tolerate lowered actomyosin contractility, but cannot easily compensate for a lack of integrin-mediated adhesion. Although integrins were dispensable for macrophage chemotactic responses, they were crucial to control cell movement and protrusiveness for optimal surveillance by a macrophage population. Our study reveals that β1 integrins are important for maintaining macrophage shape and network sampling efficiency in mammalian tissues, and sets macrophage motility strategies apart from the integrin-independent 3D migration modes of many other immune cell subsets.Macrophages are immune cells in the body that remove dying cells and debris from tissues. They live in almost all the body’s organs, surveilling for signs of infection and destroying microbes. They also migrate to wound sites, where they can eliminate foreign particles and stop microbes from entering the body. To perform their surveillance role, macrophages need to work together as a team. They form a network, coordinating their movements to optimise the removal of particles and dead cells. How this happens is something of a mystery. As individuals, cells travel through tissues using a balance of several activities: they change their shape, they contract and relax, and they grab hold of their surroundings using proteins called integrins. It is thought that the choice between these types of movement may affect the rest of the network. To investigate, Paterson and Lämmermann genetically engineered mouse macrophages grown in the laboratory so they would not produce working integrins. These macrophages were able to contract and relax, but they could not attach to the proteins in the structures they were exploring. Paterson and Lämmermann then placed these macrophages in gels studded with proteins that mimic a biological matrix to observe their behaviour. When these macrophages were exposed to the chemicals that indicate the presence of a wound, they moved normally, changing shape and contracting and relaxing. Paterson and Lämmermann confirmed this normal behaviour for macrophages moving to sites of injuries in the tissue of living mice. However, when it came to surveillance, the macrophages’ abilities were seriously diminished, and they were unable to form an effective network to take up particles and dead cells. This work sheds light on how the movement of individual cells affects the entire immune surveillance network. A deeper understanding could lead to new insights into how to prevent inflammation. The next step is to map macrophage networks in healthy and diseased tissues to understand how cell movement affects surveillance under different conditions.

Published

2022

15. Author response: Macrophage network dynamics depend on haptokinesis for optimal local surveillance

Author

Neil Paterson and Tim Lämmermann

Published

2022

16. Specification of CNS macrophage subsets occurs postnatally in defined niches

Author

Takahiro Masuda, Lukas Amann, Gianni Monaco, Roman Sankowski, Ori Staszewski, Martin Krueger, Francesca Del Gaudio, Liqun He, Neil Paterson, Elisa Nent, Francisco Fernández-Klett, Ayato Yamasaki, Maximilian Frosch, Maximilian Fliegauf, Lance Fredrick Pahutan Bosch, Hatice Ulupinar, Nora Hagemeyer, Dietmar Schreiner, Cayce Dorrier, Makoto Tsuda, Claudia Grothe, Anne Joutel, Richard Daneman, Christer Betsholtz, Urban Lendahl, Klaus-Peter Knobeloch, Tim Lämmermann, Josef Priller, Katrin Kierdorf, and Marco Prinz

Subjects

Central Nervous System, Multidisciplinary, immunology [Central Nervous System], Pregnancy, Macrophages, Humans, Cell Lineage, Female, ddc:500, cytology [Macrophages], Microglia, Immunity, Innate, Yolk Sac

Abstract

All tissue-resident macrophages of the central nervous system (CNS)-including parenchymal microglia, as well as CNS-associated macrophages (CAMs1) such as meningeal and perivascular macrophages2-7-are part of the CNS endogenous innate immune system that acts as the first line of defence during infections or trauma2,8-10. It has been suggested that microglia and all subsets of CAMs are derived from prenatal cellular sources in the yolk sac that were defined as early erythromyeloid progenitors11-15. However, the precise ontogenetic relationships, the underlying transcriptional programs and the molecular signals that drive the development of distinct CAM subsets in situ are poorly understood. Here we show, using fate-mapping systems, single-cell profiling and cell-specific mutants, that only meningeal macrophages and microglia share a common prenatal progenitor. By contrast, perivascular macrophages originate from perinatal meningeal macrophages only after birth in an integrin-dependent manner. The establishment of perivascular macrophages critically requires the presence of arterial vascular smooth muscle cells. Together, our data reveal a precisely timed process in distinct anatomical niches for the establishment of macrophage subsets in the CNS.

Published

2022

17. Author Correction: Specification of CNS macrophage subsets occurs postnatally in defined niches

Author

Takahiro Masuda, Lukas Amann, Gianni Monaco, Roman Sankowski, Ori Staszewski, Martin Krueger, Francesca Del Gaudio, Liqun He, Neil Paterson, Elisa Nent, Francisco Fernández-Klett, Ayato Yamasaki, Maximilian Frosch, Maximilian Fliegauf, Lance Fredrick Pahutan Bosch, Hatice Ulupinar, Nora Hagemeyer, Dietmar Schreiner, Cayce Dorrier, Makoto Tsuda, Claudia Grothe, Anne Joutel, Richard Daneman, Christer Betsholtz, Urban Lendahl, Klaus-Peter Knobeloch, Tim Lämmermann, Josef Priller, Katrin Kierdorf, and Marco Prinz

Subjects

Multidisciplinary, ddc:500

Published

2022

18. Microbiota-dependent increase in δ-valerobetaine alters neuronal function and is responsible for age-related cognitive decline

Author

Omar Mossad, Elisa Nent, Sabrina Woltemate, Shani Folschweiller, Joerg M. Buescher, Daniel Schnepf, Daniel Erny, Peter Staeheli, Marlene Bartos, Antal Szalay, Bärbel Stecher, Marius Vital, Jonas F. Sauer, Tim Lämmermann, Marco Prinz, and Thomas Blank

Subjects

Aging, Neuroscience (miscellaneous), Geriatrics and Gerontology, digestive system

Abstract

Understanding the physiological origins of age-related cognitive decline is of critical importance given the rising age of the world’s population. Previous work in animal models has established a strong link between cognitive performance and the microbiota, and it is known that the microbiome undergoes profound remodeling in older adults. Despite growing evidence for the association between age-related cognitive decline and changes in the gut microbiome, the mechanisms underlying such interactions between the brain and the gut are poorly understood. Here, using fecal microbiota transplantation (FMT), we demonstrate that age-related remodeling of the gut microbiota leads to decline in cognitive function in mice and that this impairment can be rescued by transplantation of microbiota from young animals. Moreover, using a metabolomic approach, we found elevated concentrations of δ-valerobetaine, a gut microbiota-derived metabolite, in the blood and brain of aged mice and older adults. We then demonstrated that δ-valerobetaine is deleterious to learning and memory processes in mice. At the neuronal level, we showed that δ-valerobetaine modulates inhibitory synaptic transmission and neuronal network activity. Finally, we identified specific bacterial taxa that significantly correlate with δ-valerobetaine levels in the brain. Based on our findings, we propose that δ-valerobetaine contributes to microbiota-driven brain aging and that the associated mechanisms represent a promising target for countering age-related cognitive decline.

Published

2021

19. 100 Hz ROCS microscopy correlated with fluorescence reveals cellular dynamics on different spatiotemporal scales

Author

Felix Jünger, Dominic Ruh, Dominik Strobel, Rebecca Michiels, Dominik Huber, Annette Brandel, Josef Madl, Alina Gavrilov, Michael Mihlan, Caterina Cora Daller, Eva A. Rog-Zielinska, Winfried Römer, Tim Lämmermann, and Alexander Rohrbach

Subjects

Multidisciplinary, Microscopy, Fluorescence, General Physics and Astronomy, General Chemistry, Fibroblasts, General Biochemistry, Genetics and Molecular Biology, Actins, Lighting

Abstract

Fluorescence techniques dominate the field of live-cell microscopy, but bleaching and motion blur from too long integration times limit dynamic investigations of small objects. High contrast, label-free life-cell imaging of thousands of acquisitions at 160 nm resolution and 100 Hz is possible by Rotating Coherent Scattering (ROCS) microscopy, where intensity speckle patterns from all azimuthal illumination directions are added up within 10 ms. In combination with fluorescence, we demonstrate the performance of improved Total Internal Reflection (TIR)-ROCS with variable illumination including timescale decomposition and activity mapping at five different examples: millisecond reorganization of macrophage actin cortex structures, fast degranulation and pore opening in mast cells, nanotube dynamics between cardiomyocytes and fibroblasts, thermal noise driven binding behavior of virus-sized particles at cells, and, bacterial lectin dynamics at the cortex of lung cells. Using analysis methods we present here, we decipher how motion blur hides cellular structures and how slow structure motions cover decisive fast motions.

Published

2021

20. Differential trafficking of ligands trogocytosed via CD28 versus CTLA4 promotes collective cellular control of co-stimulation

Author

Simon Zenke, Mauricio P. Sica, Florian Steinberg, Julia Braun, Alicia Zink, Alina Gavrilov, Alexander Hilger, Aditya Arra, Monika Brunner-Weinzierl, Roland Elling, Niklas Beyersdorf, Tim Lämmermann, Cristian R. Smulski, and Jan C. Rohr

Subjects

Abatacept, Multidisciplinary, Immunoconjugates, CD28 Antigens, Antigens, CD, General Physics and Astronomy, CTLA-4 Antigen, General Chemistry, Ligands, General Biochemistry, Genetics and Molecular Biology

Abstract

Intercellular communication is crucial for collective regulation of cellular behaviors. While clustering T cells have been shown to mutually control the production of key communication signals, it is unclear whether they also jointly regulate their availability and degradation. Here we use newly developed reporter systems, bioinformatic analyses, protein structure modeling and genetic perturbations to assess this. We find that T cells utilize trogocytosis by competing antagonistic receptors to differentially control the abundance of immunoregulatory ligands. Specifically, ligands trogocytosed via CD28 are shuttled to the T cell surface, enabling them to co-stimulate neighboring T cells. In contrast, CTLA4-mediated trogocytosis targets ligands for degradation. Mechanistically, this fate separation is controlled by different acid-sensitivities of receptor-ligand interactions and by the receptor intracellular domains. The ability of CD28 and CTLA4 to confer different fates to trogocytosed ligands reveals an additional layer of collective regulation of cellular behaviors and promotes the robustness of population dynamics.

Published

2021

21. Neutrophils self-limit swarming to contain bacterial growth in vivo

Author

Teresa K. Tarrant, Sarah Eickhoff, Konrad Knöpper, Eduardo Reátegui, Maximilian W. Epple, Katharina M. Glaser, Ralf Baumeister, Matthias Gunzer, Wolfgang Kastenmüller, Ronald N. Germain, Daniel Irimia, Michael Mihlan, Tim Lämmermann, and Korbinian Kienle

Subjects

0303 health sciences, Cell signaling, Multidisciplinary, Innate immune system, biology, Neutrophils, Chemistry, Medizin, Swarming (honey bee), Chemotaxis, Inflammation, biology.organism_classification, Article, Cell aggregation, 3. Good health, Cell biology, 03 medical and health sciences, 0302 clinical medicine, medicine, medicine.symptom, Signal transduction, 030217 neurology & neurosurgery, Bacteria, 030304 developmental biology

Abstract

Stopping the swarmNeutrophils play a major role in the early immune response and are recruited in large numbers into inflamed and infected tissues. By secreting chemoattractants that bind G protein–coupled receptors (GPCRs) on neighboring cells, neutrophils coordinate their behavior as a swarm. Less clear is how this auto-amplifying swarming activity is ultimately turned off. Kienleet al.show that desensitization of these GPCRs by the same chemoattractants by GPCR-kinase 2 (GRK2) is one way in which these swarms are shut down (see the Perspective by Rocha-Gregg and Huttenlocher). Unexpectedly, mice with GRK2-deficient neutrophils showed impaired rather than enhanced bacterial clearance. The heightened scanning ability of GRK2-deficient neutrophils may come at the cost of suboptimal phagocytosis and containment of bacteria.Science, abe7729, this issue p.eabe7729; see also abj3065, p.1262

Published

2021

22. T Cells: Bridge-and-Channel Commute to the White Pulp

Author

Tim Lämmermann and Michael Sixt

Subjects

0301 basic medicine, White pulp, T-Lymphocytes, Immunology, T cells, Biology, Article, GPCRs, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, medicine, Immunology and Allergy, bridging channels, Immunity, lymphocyte trafficking, Marginal zone, vascular-guided migration, Cell biology, 030104 developmental biology, Infectious Diseases, Bridge (graph theory), medicine.anatomical_structure, 030220 oncology & carcinogenesis, intravital imaging, spleen, Lymph Nodes, Lymph, Intravital microscopy

Abstract

Summary Lymphocyte homeostasis and immune surveillance require that T and B cells continuously recirculate between secondary lymphoid organs. Here, we used intravital microscopy to define lymphocyte trafficking routes within the spleen, an environment of open blood circulation and shear forces unlike other lymphoid organs. Upon release from arterioles into the red pulp sinuses, T cells latched onto perivascular stromal cells in a manner that was independent of the chemokine receptor CCR7 but sensitive to Gi protein-coupled receptor inhibitors. This latching sheltered T cells from blood flow and enabled unidirectional migration to the bridging channels and then to T zones, entry into which required CCR7. Inflammatory responses modified the chemotactic cues along the perivascular homing paths, leading to rapid block of entry. Our findings reveal a role for vascular structures in lymphocyte recirculation through the spleen, indicating the existence of separate entry and exit routes and that of a checkpoint located at the gate to the T zone., Graphical Abstract, Highlights • Perivascular pathways support T cell entry into splenic T zones, but not egress from them • Attachment to the homing paths requires activation of GPCRs other than CCR7 • CCR7 mediates one-directional migration and entry into T zones • Inflammation leads to modification of the homing paths and to rapid block of entry, Lymphocyte recirculation between secondary lymphoid organs is critical for their function and for immune homeostasis. Using intravital imaging, Chauveau et al. reveal that a network of perivascular pathways supports T cell migration into splenic T zones and describe a dynamic multi-step cascade of entry.

Published

2020

23. Positive feedback amplification in swarming immune cell populations

Author

Katharina M. Glaser, Tim Lämmermann, and Michael Mihlan

Subjects

Cell type, Neutrophils, Population, Cell, Swarming (honey bee), Motility, Biology, 010402 general chemistry, 01 natural sciences, Feedback, 03 medical and health sciences, Mice, Immune system, medicine, Animals, education, Zebrafish, 030304 developmental biology, 0303 health sciences, education.field_of_study, Chemotaxis, Cell Biology, biochemical phenomena, metabolism, and nutrition, 0104 chemical sciences, Cell biology, medicine.anatomical_structure, bacteria, Intracellular

Abstract

Several immune cell types (neutrophils, eosinophils, T cells, and innate-like lymphocytes) display coordinated migration patterns when a population, formed of individually responding cells, moves through inflamed or infected tissues. “Swarming” refers to the process in which a population of migrating leukocytes switches from random motility to highly directed chemotaxis to form local cell clusters. Positive feedback amplification underlies this behavior and results from intercellular communication in the immune cell population. We here highlight recent findings on neutrophil swarming from mouse models, zebrafish larvae, and in vitro platforms for human cells, which together advanced our understanding of the principles and molecular mechanisms that shape immune cell swarming.

Published

2021

24. Gut microbiota drives age-related oxidative stress and mitochondrial damage in microglia via the metabolite N

Author

Omar, Mossad, Bérénice, Batut, Bahtiyar, Yilmaz, Nikolaos, Dokalis, Charlotte, Mezö, Elisa, Nent, Lara Susann, Nabavi, Melanie, Mayer, Feres José Mocayar, Maron, Joerg M, Buescher, Mercedes Gomez, de Agüero, Antal, Szalay, Tim, Lämmermann, Andrew J, Macpherson, Stephanie C, Ganal-Vonarburg, Rolf, Backofen, Daniel, Erny, Marco, Prinz, and Thomas, Blank

Subjects

Mice, Oxidative Stress, Lysine, Animals, Microglia, Gastrointestinal Microbiome

Abstract

Microglial function declines during aging. The interaction of microglia with the gut microbiota has been well characterized during development and adulthood but not in aging. Here, we compared microglial transcriptomes from young-adult and aged mice housed under germ-free and specific pathogen-free conditions and found that the microbiota influenced aging associated-changes in microglial gene expression. The absence of gut microbiota diminished oxidative stress and ameliorated mitochondrial dysfunction in microglia from the brains of aged mice. Unbiased metabolomic analyses of serum and brain tissue revealed the accumulation of N

Published

2021

25. Age-related changes in the local milieu of inflamed tissues cause aberrant neutrophil trafficking and subsequent remote organ damage

Author

Jennifer V. Bodkin, Tim Lämmermann, Matthew Golding, Ulrich H. von Andrian, Natalia Reglero-Real, Anna Barkaway, Cleo L. Bishop, Régis Joulia, Rebecca S. Saleeb, Mathieu-Benoit Voisin, Monja Stein, Robin N. Poston, Tamara Girbl, Charlotte Owen-Woods, David Voehringer, Tchern Lenn, Aude Thiriot, Laura Vázquez-Martínez, Axel Roers, Antal Rot, Johan Duchene, Sussan Nourshargh, and Loïc Rolas

Subjects

0301 basic medicine, Male, Pathology, medicine.medical_specialty, Chemokine, Aging, Endothelium, endothelium, Neutrophils, Chemokine CXCL1, Immunology, Inflammation, chemokines, mast cells, Biology, Article, Receptors, Interleukin-8B, 03 medical and health sciences, Chemokine receptor, Mice, 0302 clinical medicine, Venules, medicine, Immunology and Allergy, Animals, CXC chemokine receptors, Lung, CXCR2, diapedesis, Endothelial Cells, Biological Transport, CXCL1, Endothelial stem cell, Mice, Inbred C57BL, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Intercellular Junctions, 030220 oncology & carcinogenesis, biology.protein, Female, Endothelium, Vascular, medicine.symptom, Intravital microscopy, ACKR1, extravasation

Abstract

Summary Aging is associated with dysregulated immune functions. Here, we investigated the impact of age on neutrophil diapedesis. Using confocal intravital microscopy, we found that in aged mice, neutrophils adhered to vascular endothelium in inflamed tissues but exhibited a high frequency of reverse transendothelial migration (rTEM). This retrograde breaching of the endothelium by neutrophils was governed by enhanced production of the chemokine CXCL1 from mast cells that localized at endothelial cell (EC) junctions. Increased EC expression of the atypical chemokine receptor 1 (ACKR1) supported this pro-inflammatory milieu in aged venules. Accumulation of CXCL1 caused desensitization of the chemokine receptor CXCR2 on neutrophils and loss of neutrophil directional motility within EC junctions. Fluorescent tracking revealed that in aged mice, neutrophils undergoing rTEM re-entered the circulation and disseminated to the lungs where they caused vascular leakage. Thus, neutrophils stemming from a local inflammatory site contribute to remote organ damage, with implication to the dysregulated systemic inflammation associated with aging., Graphical abstract, Highlights • Aged mice show high levels of neutrophil reverse transendothelial migration (rTEM) • Mast cells (MC) and MC-derived CXCL1 drive neutrophil rTEM in inflamed aged tissues • Intensified endothelial ACKR1-CXCL1 axis promotes neutrophil CXCR2 internalization • Aged lungs program rTEM neutrophils toward an activated and noxious phenotype, Aging is a critical risk factor for inflammatory disorders. Barkaway, Rolas et al. show that inflamed aged tissues present a high frequency of neutrophil reverse transendothelial migration (rTEM) back into the circulation in a mast cell-dependent manner. rTEM neutrophils are retained in aged lungs and programmed toward an activated phenotype, capable of inducing tissue damage.

Published

2020

26. Upregulation of VCAM-1 in lymphatic collectors supports dendritic cell entry and rapid migration to lymph nodes in inflammation

Author

Mona C. Friess, Cornelia Halin, Morgan Campbell Hunter, Philipp Schineis, Jorge Arasa, Carlotta Tacconi, Neil Paterson, Michael Detmar, Victor Collado-Diaz, Tim Lämmermann, Friedemann Kiefer, Takashi Nagasawa, Taija Makinen, Markus Moser, Ioannis Kritikos, Jessica Danielly Medina-Sanchez, and Elena C. Sigmund

Subjects

Transcriptional Activation, Receptors, CCR7, Immunology, Integrin, Vascular Cell Adhesion Molecule-1, Innate immunity and inflammation, Inflammation, C-C chemokine receptor type 7, Basement Membrane, Article, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Cell Movement, Cardiovascular Biology, medicine, otorhinolaryngologic diseases, Immunology and Allergy, Animals, Humans, VCAM-1, 030304 developmental biology, Lymphatic Vessels, Skin, Basement membrane, 0303 health sciences, biology, integumentary system, Chemistry, Integrin beta1, Endothelial Cells, hemic and immune systems, Dendritic cell, Dendritic Cells, 3. Good health, Cell biology, Up-Regulation, Mice, Inbred C57BL, stomatognathic diseases, Lymphatic system, medicine.anatomical_structure, biology.protein, Female, Lymph, Lymph Nodes, medicine.symptom, 030215 immunology

Abstract

Dendritic cells (DCs) are thought to enter afferent lymphatics exclusively through lymphatic capillaries. This study reveals that in inflammation, DCs additionally enter downstream of capillaries into contracting collectors, allowing for a more rapid migration to draining lymph nodes., Dendritic cell (DC) migration to draining lymph nodes (dLNs) is a slow process that is believed to begin with DCs approaching and entering into afferent lymphatic capillaries. From capillaries, DCs slowly crawl into lymphatic collectors, where lymph flow induced by collector contraction supports DC detachment and thereafter rapid, passive transport to dLNs. Performing a transcriptomics analysis of dermal endothelial cells, we found that inflammation induces the degradation of the basement membrane (BM) surrounding lymphatic collectors and preferential up-regulation of the DC trafficking molecule VCAM-1 in collectors. In crawl-in experiments performed in ear skin explants, DCs entered collectors in a CCR7- and β1 integrin–dependent manner. In vivo, loss of β1-integrins in DCs or of VCAM-1 in lymphatic collectors had the greatest impact on DC migration to dLNs at early time points when migration kinetics favor the accumulation of rapidly migrating collector DCs rather than slower capillary DCs. Taken together, our findings identify collector entry as a critical mechanism enabling rapid DC migration to dLNs in inflammation., Graphical Abstract

Published

2020

27. Neutrophils provide cellular communication between ileum and mesenteric lymph nodes at graft-versus-host disease onset

Author

Zhan Gao, Jan Hülsdünker, Katja J. Ottmüller, Sandra Duquesne, Geoffrey R. Hill, Oliver S. Thomas, Hannes P. Neeff, Brian T. Fife, Marie Follo, Robert Zeiser, Heide Dierbach, Bruce R. Blazar, Georg Häcker, Gabriele Prinz, Motoko Koyama, Andreas Beilhack, Ali Al-Ahmad, Tim Lämmermann, Susanne Kirschnek, and Martin J. Blaser

Subjects

0301 basic medicine, Neutrophils, T cell, Immunology, Graft vs Host Disease, chemical and pharmacologic phenomena, Cell Communication, Major histocompatibility complex, Biochemistry, Pathogenesis, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, Ileum, medicine, Animals, Mesenteric lymph nodes, Mesentery, Protein Kinase Inhibitors, Mice, Knockout, Mice, Inbred BALB C, Innate immune system, biology, business.industry, Janus Kinase 1, Cell Biology, Hematology, Janus Kinase 2, medicine.disease, 030104 developmental biology, Graft-versus-host disease, medicine.anatomical_structure, Neutrophil Infiltration, Acute Disease, biology.protein, Lymph Nodes, Cell activation, business, 030215 immunology

Abstract

Conditioning-induced damage of the intestinal tract plays a critical role during the onset of acute graft-versus-host disease (GVHD). Therapeutic interference with these early events of GVHD is difficult, and currently used immunosuppressive drugs mainly target donor T cells. However, not donor T cells but neutrophils reach the sites of tissue injury first, and therefore could be a potential target for GVHD prevention. A detailed analysis of neutrophil fate during acute GVHD and the effect on T cells is difficult because of the short lifespan of this cell type. By using a novel photoconverter reporter system, we show that neutrophils that had been photoconverted in the ileum postconditioning later migrated to mesenteric lymph nodes (mLN). This neutrophil migration was dependent on the intestinal microflora. In the mLN, neutrophils colocalized with T cells and presented antigen on major histocompatibility complex (MHC)-II, thereby affecting T cell expansion. Pharmacological JAK1/JAK2 inhibition reduced neutrophil influx into the mLN and MHC-II expression, thereby interfering with an early event in acute GVHD pathogenesis. In agreement with this finding, neutrophil depletion reduced acute GVHD. We conclude that neutrophils are attracted to the ileum, where the intestinal barrier is disrupted, and then migrate to the mLN, where they participate in alloantigen presentation. JAK1/JAK2-inhibition can interfere with this process, which provides a potential therapeutic strategy to prevent early events of tissue damage-related innate immune cell activation and, ultimately, GVHD.

Published

2018

28. Platelet Serotonin Aggravates Myocardial Ischemia/Reperfusion Injury via Neutrophil Degranulation

Author

Christoph Koentges, Tim Lämmermann, Korbinian Kienle, Claudia Schoenichen, Daniel Duerschmied, Ludwig Dorner, Benoît Ho-Tin-Noé, Carmen Härdtner, Daniela Stallmann, Claus Normann, Ingo Ahrens, Véronique Ollivier, Paul Walther, Klaus Ley, Maximilian Mauler, Heiko Bugger, Maximilian Schell, Christopher Wippel, Ingo Hilgendorf, Christoph Bode, Dennis Wolf, Thilo Witsch, Timoteo Marchini, and Nadine Herr

Subjects

Inflammation, 030204 cardiovascular system & hematology, Pharmacology, Article, 03 medical and health sciences, 0302 clinical medicine, INFLAMMATION, Physiology (medical), purl.org/becyt/ford/3.2 [https], medicine, Platelet, REACTIVE OXYGEN SPECIES, REPERFUSION INJURY, Thrombus, NEUTROPHILS, 030304 developmental biology, 0303 health sciences, business.industry, SEROTONIN, Degranulation, medicine.disease, INTEGRINS, Hemostasis, Neutrophil degranulation, purl.org/becyt/ford/3 [https], Serotonin, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Reperfusion injury, BLOOD PLATELETS

Abstract

Background: Platelets store large amounts of serotonin that they release during thrombus formation or acute inflammation. This facilitates hemostasis and modulates the inflammatory response. Methods: Infarct size, heart function, and inflammatory cell composition were analyzed in mouse models of myocardial reperfusion injury with genetic and pharmacological depletion of platelet serotonin. These studies were complemented by in vitro serotonin stimulation assays of platelets and leukocytes in mice and men, and by measuring plasma serotonin levels and leukocyte activation in patients with acute coronary syndrome. Results: Platelet-derived serotonin induced neutrophil degranulation with release of myeloperoxidase and hydrogen peroxide (H2O2) and increased expression of membrane-bound leukocyte adhesion molecule CD11b, leading to enhanced inflammation in the infarct area and reduced myocardial salvage. In patients hospitalized with acute coronary syndrome, plasmatic serotonin levels correlated with CD11b expression on neutrophils and myeloperoxidase plasma levels. Long-term serotonin reuptake inhibition - reported to protect patients with depression from cardiovascular events - resulted in the depletion of platelet serotonin stores in mice. These mice displayed a reduction in neutrophil degranulation and preserved cardiac function. In line, patients with depression using serotonin reuptake inhibition, presented with suppressed levels of CD11b surface expression on neutrophils and lower myeloperoxidase levels in blood. Conclusions: Taken together, we identify serotonin as a potent therapeutic target in neutrophil-dependent thromboinflammation during myocardial reperfusion injury. Fil: Mauler, Maximilian. No especifíca; Fil: Herr, Nadine. No especifíca; Fil: Schoenichen, Claudia. No especifíca; Fil: Witsch, Thilo. No especifíca; Fil: Marchini, Timoteo Oscar. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Houssay. Instituto de Bioquímica y Medicina Molecular. Universidad de Buenos Aires. Facultad Medicina. Instituto de Bioquímica y Medicina Molecular; Argentina Fil: Härdtner, Carmen. No especifíca; Fil: Koentges, Christoph. No especifíca; Fil: Kienle, Korbinian. Max Planck Institute Of Immunobiology And Epigenetics; Alemania Fil: Ollivier, Véronique. Inserm; Francia Fil: Schell, Maximilian. No especifíca; Fil: Dorner, Ludwig. No especifíca; Fil: Wippel, Christopher. No especifíca; Fil: Stallmann, Daniela. No especifíca; Fil: Normann, Claus. No especifíca; Fil: Bugger, Heiko. No especifíca; Fil: Walther, Paul. Universitat Ulm; Alemania Fil: Wolf, Dennis. La Jolla Institute for Allergy and Immunology; Estados Unidos Fil: Ahrens, Ingo. No especifíca; Fil: Lämmermann, Tim. Max Planck Institute Of Immunobiology And Epigenetics; Alemania Fil: Ho-Tin-Noé, Benoît. Inserm; Francia Fil: Ley, Klaus. La Jolla Institute for Allergy and Immunology; Estados Unidos Fil: Bode, Christoph. No especifíca; Fil: Hilgendorf, Ingo. No especifíca; Fil: Duerschmied, Daniel. No especifíca

Published

2019

29. A Subset of Skin Macrophages Contributes to the Seruveillance and Regeneration of Local Nerves

Author

Anne Kathrin Lösslein, Claudia Waskow, Sebastian Baasch, Melanie Meyer-Luehmann, Patrice Zeis, Kourosh Gharun, Neil Paterson, Nora Hagemeyer, Tim Lämmermann, Julia Kolter, Reinhild Feuerstein, Philipp Henneke, Dominic Grün, Marco Prinz, Lukas Amann, Paolo d'Errico, Takahiro Masuda, and Claus-Werner Franzke

Subjects

0301 basic medicine, Cell type, Immunology, CX3C Chemokine Receptor 1, Biology, Immunophenotyping, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Dermis, Fate mapping, medicine, Immunology and Allergy, Animals, Axon, Immunologic Surveillance, Skin, Regeneration (biology), Macrophages, Cell Differentiation, Cell biology, Nerve Regeneration, Haematopoiesis, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Animals, Newborn, 030220 oncology & carcinogenesis, Stem cell, Biomarkers

Abstract

Summary The skin comprises tissue macrophages as the most abundant resident immune cell type. Their diverse tasks including resistance against invading pathogens, attraction of bypassing immune cells from vessels, and tissue repair require dynamic specification. Here, we delineated the postnatal development of dermal macrophages and their differentiation into subsets by adapting single-cell transcriptomics, fate mapping, and imaging. Thereby we identified a phenotypically and transcriptionally distinct subset of prenatally seeded dermal macrophages that self-maintained with very low postnatal exchange by hematopoietic stem cells. These macrophages specifically interacted with sensory nerves and surveilled and trimmed the myelin sheath. Overall, resident dermal macrophages contributed to axon sprouting after mechanical injury. In summary, our data show long-lasting functional specification of macrophages in the dermis that is driven by stepwise adaptation to guiding structures and ensures codevelopment of ontogenetically distinct cells within the same compartment.

Published

2019

30. Neutrophil swarming: an essential process of the neutrophil tissue response

Author

Korbinian Kienle and Tim Lämmermann

Subjects

0301 basic medicine, Neutrophils, Sterile inflammation, Immunology, Swarming (honey bee), Biology, 03 medical and health sciences, Cell Movement, medicine, Animals, Humans, Immunology and Allergy, Inflammation, Innate immune system, Chemotaxis, medicine.disease, Immunity, Innate, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Neutrophil Infiltration, Infiltration (medical), Intracellular, Intravital microscopy, Blood vessel

Abstract

Summary Neutrophil infiltration into inflamed and infected tissues is a fundamental process of the innate immune response. While neutrophil interactions with the blood vessel wall have been intensely studied over the last decades, neutrophil dynamics beyond the vasculature have for a long time remained poorly investigated. Recent intravital microscopy studies of neutrophil populations directly at the site of tissue damage or microbial invasion have changed our perspective on neutrophil responses within tissues. Swarm-like migration patterns of neutrophils, referred to as ‘neutrophil swarming’, have been detected in diverse tissues under conditions of sterile inflammation and infection with various pathogens, including bacteria, fungi, and parasites. Current work has begun to unravel the molecular pathways choreographing the sequential phases of highly coordinated chemotaxis followed by neutrophil accumulation and the formation of substantial neutrophil clusters. It is now clear that intercellular communication among neutrophils amplifies their recruitment in a feed-forward manner, which provides them with a level of self-organization during neutrophil swarming. This review will summarize recent developments and current concepts on neutrophil swarming, an important process of the neutrophil tissue response with a critical role in maintaining the balance between host protection and inflammation-driven tissue destruction.

Published

2016

31. Quorum Regulation via Nested Antagonistic Feedback Circuits Mediated by the Receptors CD28 and CTLA-4 Confers Robustness to T Cell Population Dynamics

Author

Margriet Palm, Audrey Gérard, Philippa Meiser, Julia Braun, Simon Zenke, Jan Rohr, Niklas Beyersdorf, Stephan Ehl, Tim Lämmermann, Joost B. Beltman, Alina Gavrilov, Jan P. Böttcher, and Ton N. Schumacher

Subjects

0301 basic medicine, Cell Count, feedback, Cell Communication, robustness, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Mice, 0302 clinical medicine, CD80, T lymphocyte, population dynamics, Immunology and Allergy, CTLA-4 Antigen, Receptor, education.field_of_study, CD28, Intercellular Adhesion Molecule-1, Cell biology, Infectious Diseases, medicine.anatomical_structure, Cell Tracking, 030220 oncology & carcinogenesis, B7-1 Antigen, Cell type, Cell Survival, T cell, Immunology, Population, Mice, Transgenic, Biology, Cell Line, 03 medical and health sciences, CD28 Antigens, quorum regulation, medicine, Animals, education, CD86, IL-2, Robustness (evolution), Dendritic Cells, Models, Theoretical, Mice, Inbred C57BL, 030104 developmental biology, Interleukin-2, CTLA-4, B7-2 Antigen

Abstract

T cell responses upon infection display a remarkably reproducible pattern of expansion, contraction, and memory formation. If the robustness of this pattern builds entirely on signals derived from other cell types or if activated T cells themselves contribute to the orchestration of these population dynamics-akin to bacterial quorum regulation-is unclear. Here, we examined this question using time-lapse microscopy, genetic perturbation, bioinformatic predictions, and mathematical modeling. We found that ICAM-1-mediated cell clustering enabled CD8+ T cells to collectively regulate the balance between proliferation and apoptosis. Mechanistically, T cell expressed CD80 and CD86 interacted with the receptors CD28 and CTLA-4 on neighboring T cells; these interactions fed two nested antagonistic feedback circuits that regulated interleukin 2 production in a manner dependent on T cell density as confirmed by in vivo modulation of this network. Thus, CD8+ T cell-population-intrinsic mechanisms regulate cellular behavior, thereby promoting robustness of population dynamics.

Published

2020

32. Resident Macrophages Cloak Tissue Microlesions to Prevent Neutrophil-Driven Inflammatory Damage

Author

Andrew J. Martins, Tim Lämmermann, Ronald N. Germain, Stefan Uderhardt, and John S. Tsang

Subjects

Neutrophils, Sialic Acid Binding Ig-like Lectin 1, Confocal, Muscle Fibers, Skeletal, Biology, General Biochemistry, Genetics and Molecular Biology, Neutrophil Activation, 03 medical and health sciences, Mice, 0302 clinical medicine, Parenchyma, medicine, Alarmins, Animals, Cell damage, Tissue homeostasis, 030304 developmental biology, Inflammation, Mice, Knockout, 0303 health sciences, Macrophages, Cell injury, Chemotaxis, Intravital Imaging, medicine.disease, Endocytosis, Cell biology, Mice, Inbred C57BL, Microscopy, Fluorescence, Collateral damage, 030217 neurology & neurosurgery

Abstract

Summary Neutrophils are attracted to and generate dense swarms at sites of cell damage in diverse tissues, often extending the local disruption of organ architecture produced by the initial insult. Whether the inflammatory damage resulting from such neutrophil accumulation is an inescapable consequence of parenchymal cell death has not been explored. Using a combination of dynamic intravital imaging and confocal multiplex microscopy, we report here that tissue-resident macrophages rapidly sense the death of individual cells and extend membrane processes that sequester the damage, a process that prevents initiation of the feedforward chemoattractant signaling cascade that results in neutrophil swarms. Through this "cloaking" mechanism, the resident macrophages prevent neutrophil-mediated inflammatory damage, maintaining tissue homeostasis in the face of local cell injury that occurs on a regular basis in many organs because of mechanical and other stresses. Video Abstract

Published

2018

33. Cochaperone Mzb1 is a key effector of Blimp1 in plasma cell differentiation and β1-integrin function

Author

Stephen L. Nutt, Senthilkumar Ramamoorthy, Abhinav Pandey, Rudolf Grosschedl, Tim Lämmermann, Ekaterina Lupar, and Virginia Andreani

Subjects

0301 basic medicine, Stromal cell, Blimp1, plasma cell, integrin, Cellular differentiation, Plasma Cells, Bone Marrow Cells, Plasma cell, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Immunology and Inflammation, Mzb1, Plasma cell differentiation, medicine, Animals, Secretion, Mice, Knockout, Multidisciplinary, Chemistry, Integrin beta1, Cell Differentiation, Biological Sciences, Marginal zone, Cell biology, 030104 developmental biology, medicine.anatomical_structure, PNAS Plus, Immunoglobulin M, Bone marrow, Positive Regulatory Domain I-Binding Factor 1, Grp94, 030215 immunology, Molecular Chaperones

Abstract

Significance Antibody-secreting plasma cells are effectors of the humoral immune response. Transcription factor Blimp1 (Prdm1) is essential for the generation and function of plasma cells, and it regulates many genes, including Mzb1 (pERp1). Mzb1 protein is localized in the endoplasmic reticulum and acts as a cochaperone for the substrate-specific chaperone Grp94 (gp96). By the analysis of Mzb1−/−Prdm1+/gfp mice, we find that Mzb1 is required for T cell-independent immune responses and differentiation of plasma cells. In Mzb1−/−Prdm1+/gfp mice, we also observe impaired β1-integrin activation and trafficking of plasma cells to the bone marrow. Notably, we show that Mzb1 accounts for many of the Blimp1-associated downstream functions, suggesting that Mzb1 is a key effector of the Blimp1 regulatory network in plasma cells., Plasma cell differentiation involves coordinated changes in gene expression and functional properties of B cells. Here, we study the role of Mzb1, a Grp94 cochaperone that is expressed in marginal zone (MZ) B cells and during the terminal differentiation of B cells to antibody-secreting cells. By analyzing Mzb1−/−Prdm1+/gfp mice, we find that Mzb1 is specifically required for the differentiation and function of antibody-secreting cells in a T cell-independent immune response. We find that Mzb1-deficiency mimics, in part, the phenotype of Blimp1 deficiency, including the impaired secretion of IgM and the deregulation of Blimp1 target genes. In addition, we find that Mzb1−/− plasmablasts show a reduced activation of β1-integrin, which contributes to the impaired plasmablast differentiation and migration of antibody-secreting cells to the bone marrow. Thus, Mzb1 function is required for multiple aspects of plasma cell differentiation.

Published

2018

34. Platelets, On Your Marks, Get Set, Migrate!

Author

Tim Lämmermann and Sarah K. Bambach

Subjects

0301 basic medicine, Blood Platelets, Pathology, medicine.medical_specialty, Fibrin, Integrins, biology, Bacteria, Integrin, Thrombosis, medicine.disease, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, biology.protein, medicine, Humans, Platelet, Thrombus, 030215 immunology

Abstract

The idea that anucleate platelets display autonomous migration has long been viewed with skepticism. Gaertner et al. provide in vivo evidence that platelets undergo active migration at sites of thrombus formation and in inflamed liver sinusoids. Integrin-dependent migration allows platelets to scavenge and bundle fibrin-bound material, including intravascular bacteria.

Published

2017

35. Continuous volumetric imaging via an optical phase-locked ultrasound lens

Author

Lingjie Kong, Charles P. Lin, Jianyong Tang, Tim Lämmermann, Ronald N. Germain, Justin P. Little, Yang Yu, and Meng Cui

Subjects

Optics and Photonics, Materials science, Neutrophils, Green Fluorescent Proteins, Phase (waves), Mice, Transgenic, Image processing, Biochemistry, Article, law.invention, Mice, law, Oscillometry, Microscopy, Image Processing, Computer-Assisted, Fluorescence microscope, Animals, Molecular Biology, Cerebral Cortex, business.industry, Lasers, Ultrasound, Neurosciences, Brain, Dendritic Cells, Cell Biology, Laser, Lens (optics), Microscopy, Fluorescence, Multiphoton, Microscopy, Fluorescence, Immune System, Calibration, Calcium, Lymph Nodes, Microglia, business, Algorithms, Preclinical imaging, Biotechnology, Biomedical engineering

Abstract

In vivo imaging at high spatiotemporal resolution holds the key to the fundamental understanding of complex biological systems. Integrating an optical phase-locked ultrasound lens into a conventional two-photon fluorescence microscope, we achieved microsecond scale axial scanning, which enabled high-speed volumetric imaging. We applied this system to multicolor volumetric imaging of fast processes, including calcium dynamics in the cerebral cortex of behaving mice, and transient morphology changes and trafficking of immune cells.

Published

2015

36. Cell migration: Arraying neutrophils in swarms

Author

Tim Lämmermann

Subjects

0301 basic medicine, Chemistry, Collective cell migration, Biomedical Engineering, Medicine (miscellaneous), Bioengineering, Cell migration, Computer Science Applications, Cell biology, 03 medical and health sciences, 030104 developmental biology, Immunology, Microscale chemistry, Biotechnology

Abstract

Microscale arrays of protein–polysaccharide clusters enable the functional characterization of human-neutrophil migration.

Published

2017

37. Tuning of Antigen Sensitivity by T Cell Receptor-Dependent Negative Feedback Controls T Cell Effector Function in Inflamed Tissues

Author

Tetsuya Honda, Jackson G. Egen, Parizad Torabi-Parizi, Ronald N. Germain, Wolfgang Kastenmüller, and Tim Lämmermann

Subjects

Effector, medicine.medical_treatment, T cell, T-cell receptor, Antigen presentation, Immunology, Biology, Cell biology, Immune system, Cytokine, medicine.anatomical_structure, Infectious Diseases, Antigen, medicine, Immunology and Allergy, Receptor

Abstract

Activated T cells must mediate effector responses sufficient to clear pathogens while avoiding excessive tissue damage. Here we have combined dynamic intravital microscopy with ex vivo assessments of T cell cytokine responses to generate a detailed spatiotemporal picture of CD4+ T cell effector regulation in the skin. In response to antigen, effector T cells arrested transiently on antigen presenting cells, briefly producing cytokine and then resuming migration. Antigen recognition led to PD-1 upregulation of the programmed death-1 (PD-1) glycoprotein by T cells and blocking its canonical ligand, programmed death-ligand 1 (PD-L1), lengthened the duration of migration arrest and cytokine production, showing that PD-1 interaction with PD-L1 is a major negative feedback regulator of antigen responsiveness. We speculate that the immune system employs a mechanism involving T cell recruitment, transient activation, and rapid desensitization, allowing the T cell response to rapidly adjust to changes in antigen presentation and minimize collateral injury to the host.

Published

2014

38. In the eye of the neutrophil swarm - navigation signals that bring neutrophils together in inflamed and infected tissues

Author

Tim Lämmermann

Subjects

0301 basic medicine, Programmed cell death, Chemokine, Neutrophils, Immunology, Cell, Swarming (honey bee), Inflammation, Infections, 03 medical and health sciences, Paracrine signalling, medicine, Animals, Humans, Immunology and Allergy, biology, Chemotaxis, Cell Biology, Immunity, Innate, 030104 developmental biology, medicine.anatomical_structure, Neutrophil Infiltration, biology.protein, medicine.symptom, Intracellular

Abstract

Neutrophils are sentinel cells that express in higher vertebrates >30 chemokine and chemoattractant receptors to sense and quickly react to tissue damage signals. Intravital microscopy studies in mouse models of wounding, inflammation, and infection have revealed that neutrophils form cell swarms at local sites of tissue injury and cell death. This swarming response is choreographed by chemokines, lipids, and other chemoattractants, controlling sequential phases of highly coordinated chemotaxis, intercellular signal relay, and cluster formation among neutrophils. This review will give a brief overview about the basic principles and key molecules that have led to the refined multistep model of how neutrophils come together to isolate sites of tissue injury and microbial invasion from healthy tissue. Whereas auto- and paracrine signaling among neutrophils during later phases of swarming can provide a level of self-organization for robust navigation in diverse inflammatory settings, guidance factors from primary tissue lesions, resident bystander cells, and dying cells regulate the initial phases of the swarming response. This review will discuss how the specific environmental context and mixture of attractants at the locally inflamed site can lead to variants of the multistep attraction model and influence the extent of neutrophil swarming, ranging from accumulations of only few individual cells to the aggregation of several hundreds of neutrophils, as found in abscesses. Given the critical roles of neutrophils in both host protection and tissue destruction, novel insights on neutrophil swarming might provide useful for the therapeutic modulation of neutrophil-dependent inflammatory processes.

Published

2016

39. Immobilized Chemokine Fields and Soluble Chemokine Gradients Cooperatively Shape Migration Patterns of Dendritic Cells

Author

Tim Lämmermann, Julien Polleux, Gerold Schuler, Manfred B. Lutz, Markus Bruckner, Reinhold Förster, Daniel F. Legler, Joachim P. Spatz, Kathrin Schumann, Michael Sixt, and Lydia Sorokin

Subjects

Chemokine, endocrine system, Integrins, Receptors, CCR7, PROTEINS, Surface Properties, Integrin, Fluoroimmunoassay, Immunology, C-C chemokine receptor type 7, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Cell Movement, ddc:570, Animals, Immunology and Allergy, MOLIMMUNO, Cell adhesion, CXCL16, Cells, Cultured, 030304 developmental biology, Mice, Knockout, 0303 health sciences, biology, Chemokine CCL21, CCL19, Dendritic Cells, biochemical phenomena, metabolism, and nutrition, Cells, Immobilized, Recombinant Proteins, Cell biology, Mice, Inbred C57BL, Reticulin, Infectious Diseases, Solubility, biology.protein, bacteria, Chemokine CCL19, Lymph Nodes, CCL25, Chemokines, 030215 immunology, CCL21

Abstract

SummaryChemokines orchestrate immune cell trafficking by eliciting either directed or random migration and by activating integrins in order to induce cell adhesion. Analyzing dendritic cell (DC) migration, we showed that these distinct cellular responses depended on the mode of chemokine presentation within tissues. The surface-immobilized form of the chemokine CCL21, the heparan sulfate-anchoring ligand of the CC-chemokine receptor 7 (CCR7), caused random movement of DCs that was confined to the chemokine-presenting surface because it triggered integrin-mediated adhesion. Upon direct contact with CCL21, DCs truncated the anchoring residues of CCL21, thereby releasing it from the solid phase. Soluble CCL21 functionally resembles the second CCR7 ligand, CCL19, which lacks anchoring residues and forms soluble gradients. Both soluble CCR7 ligands triggered chemotactic movement, but not surface adhesion. Adhesive random migration and directional steering cooperate to produce dynamic but spatially restricted locomotion patterns closely resembling the cellular dynamics observed in secondary lymphoid organs.PaperClip

Published

2010

40. Cytohesin-1 controls the activation of RhoA and modulates integrin-dependent adhesion and migration of dendritic cells

Author

Thomas Quast, Tim Lämmermann, Christian Weber, Ronen Alon, Jessica Grell, Cora Schild, Reinhold Förster, Michael Sixt, Katrin Dreck, Barbara Tappertzhofen, Waldemar Kolanus, Niklas Czeloth, and Line Fraemohs

Subjects

Integrins, Chemokine, RHOA, Immunology, Integrin, Biochemistry, Mice, Cell Movement, Cell Adhesion, Animals, Guanine Nucleotide Exchange Factors, Humans, Antigen-presenting cell, Cells, Cultured, biology, Cell adhesion molecule, Cell Differentiation, Cell migration, Dendritic Cells, Cell Biology, Hematology, Dendritic cell, Cell biology, Enzyme Activation, CD18 Antigens, biology.protein, RNA Interference, Guanine nucleotide exchange factor, rhoA GTP-Binding Protein

Abstract

Adhesion and motility of mammalian leukocytes are essential requirements for innate and adaptive immune defense mechanisms. We show here that the guanine nucleotide exchange factor cytohesin-1, which had previously been demonstrated to be an important component of beta-2 integrin activation in lymphocytes, regulates the activation of the small GTPase RhoA in primary dendritic cells (DCs). Cytohesin-1 and RhoA are both required for the induction of chemokine-dependent conformational changes of the integrin beta-2 subunit of DCs during adhesion under physiological flow conditions. Furthermore, use of RNAi in murine bone marrow DCs (BM-DCs) revealed that interference with cytohesin-1 signaling impairs migration of wild-type dendritic cells in complex 3D environments and in vivo. This phenotype was not observed in the complete absence of integrins. We thus demonstrate an essential role of cytohesin-1/RhoA during ameboid migration in the presence of integrins and further suggest that DCs without integrins switch to a different migration mode.

Published

2009

41. The multiple faces of leukocyte interstitial migration

Author

Ronald N. Germain and Tim Lämmermann

Subjects

Leukocyte migration, Cell signaling, Immunology, Immunity, Motility, Chemotaxis, Inflammation, Cell Communication, Biology, medicine.disease, Article, Cell biology, Cellular Microenvironment, Cell Movement, medicine, Leukocytes, Immunology and Allergy, Animals, Humans, medicine.symptom, Cytoskeleton, Infiltration (medical), Actin

Abstract

Spatiotemporal control of leukocyte dynamics within tissues is critical for successful innate and adaptive immune responses. Homeostatic trafficking and coordinated infiltration into and within sites of inflammation and infection rely on signaling in response to extracellular cues that in turn controls a variety of intracellular protein networks regulating leukocyte motility, migration, chemotaxis, positioning, and cell–cell interaction. In contrast to mesenchymal cells, leukocytes migrate in an amoeboid fashion by rapid cycles of actin polymerization and actomyosin contraction, and their migration in tissues is generally referred to as low adhesive and nonproteolytic. The interplay of actin network expansion, contraction, and adhesion shapes the exact mode of amoeboid migration, and in this review, we explore how leukocyte subsets potentially harness the same basic biomechanical mechanisms in a cell-type-specific manner. Most of our detailed understanding of these processes derives from in vitro migration studies in three-dimensional gels and confined spaces that mimic geometrical aspects of physiological tissues. We summarize these in vitro results and then critically compare them to data from intravital imaging of leukocyte interstitial migration in mouse tissues. We outline the technical challenges of obtaining conclusive mechanistic results from intravital studies, discuss leukocyte migration strategies in vivo, and present examples of mode switching during physiological interstitial migration. These findings are also placed in the context of leukocyte migration defects in primary immunodeficiencies. This overview of both in vitro and in vivo studies highlights recent progress in understanding the molecular and biophysical mechanisms that shape robust leukocyte migration responses in physiologically complex and heterogeneous environments.

Published

2014

42. Neutrophil swarms require LTB4 and integrins at sites of cell death in vivo

Author

Tim Lämmermann, Philippe V. Afonso, Ji Ming Wang, Carole A. Parent, Bastian R. Angermann, Wolfgang Kastenmüller, and Ronald N. Germain

Subjects

Male, Integrins, Neutrophils, Leukotriene B4, Integrin, Population, Article, Receptors, G-Protein-Coupled, Mice, chemistry.chemical_compound, Dermis, medicine, Animals, education, Skin, Wound Healing, education.field_of_study, Multidisciplinary, Innate immune system, Cell Death, Chemotactic Factors, biology, Macrophages, Chemotaxis, Immunity, Innate, Cell biology, Chemotaxis, Leukocyte, medicine.anatomical_structure, Neutrophil Infiltration, chemistry, Pseudomonas aeruginosa, Immunology, biology.protein, Female, Collagen, Lymph Nodes, Wound healing, Intracellular

Abstract

Neutrophil recruitment from blood to extravascular sites of sterile or infectious tissue damage is a hallmark of early innate immune responses, and the molecular events leading to cell exit from the bloodstream have been well defined1,2. Once outside the vessel, individual neutrophils often show extremely coordinated chemotaxis and cluster formation reminiscent of the swarming behaviour of insects3,4,5,6,7,8,9,10,11. The molecular players that direct this response at the single-cell and population levels within the complexity of an inflamed tissue are unknown. Using two-photon intravital microscopy in mouse models of sterile injury and infection, we show a critical role for intercellular signal relay among neutrophils mediated by the lipid leukotriene B4, which acutely amplifies local cell death signals to enhance the radius of highly directed interstitial neutrophil recruitment. Integrin receptors are dispensable for long-distance migration12, but have a previously unappreciated role in maintaining dense cellular clusters when congregating neutrophils rearrange the collagenous fibre network of the dermis to form a collagen-free zone at the wound centre. In this newly formed environment, integrins, in concert with neutrophil-derived leukotriene B4 and other chemoattractants, promote local neutrophil interaction while forming a tight wound seal. This wound seal has borders that cease to grow in kinetic concert with late recruitment of monocytes and macrophages at the edge of the displaced collagen fibres. Together, these data provide an initial molecular map of the factors that contribute to neutrophil swarming in the extravascular space of a damaged tissue. They reveal how local events are propagated over large-range distances, and how auto-signalling produces coordinated, self-organized neutrophil-swarming behaviour that isolates the wound or infectious site from surrounding viable tissue.

Published

2013

43. Extracellular matrix of secondary lymphoid organs impacts on B-cell fate and survival

Author

Thomas Winkler, Julia Rolf, John F. Kearney, Elisabeth Georges-Labouesse, Zerina Lokmic, Jian Song, Xueli Zhang, Markus A. Rüegg, Arnoud Sonnenberg, Nathalie Horn, Melanie Jane Hannocks, Chuan Wu, Tim Lämmermann, Susanna Cardell, Rupert Hallmann, and Lydia Sorokin

Subjects

Stromal cell, Cell Survival, T cell, Population, Integrin, Biology, Extracellular matrix, Mice, 03 medical and health sciences, 0302 clinical medicine, Bone Marrow, Cell Movement, Laminin, medicine, Animals, Agrin, education, B cell, 030304 developmental biology, Mice, Knockout, B-Lymphocytes, 0303 health sciences, education.field_of_study, Multidisciplinary, Integrin alpha6beta1, Marginal zone, Extracellular Matrix, Cell biology, medicine.anatomical_structure, PNAS Plus, Immunology, biology.protein, Spleen, 030217 neurology & neurosurgery

Abstract

We describe a unique extracellular matrix (ECM) niche in the spleen, the marginal zone (MZ), characterized by the basement membrane glycoproteins, laminin α5 and agrin, that promotes formation of a specialized population of MZ B lymphocytes that respond rapidly to blood-borne antigens. Mice with reduced laminin α5 expression show reduced MZ B cells and increased numbers of newly formed (NF) transitional B cells that migrate from the bone marrow, without changes in other immune or stromal cell compartments. Transient integrin α6β1-mediated interaction of NF B cells with laminin α5 in the MZ supports the MZ B-cell population, their long-term survival, and antibody response. Data suggest that the unique 3D structure and biochemical composition of the ECM of lymphoid organs impacts on immune cell fate.

Published

2013

44. Cancer-associated epithelial cell adhesion molecule (EpCAM; CD326) enables epidermal Langerhans cell motility and migration in vivo

Author

Daniel H. Kaplan, Lino Tessarollo, Mark C. Udey, Xu Feng, Ronald N. Germain, Tim Lämmermann, Botond Z. Igyártó, and Maria R. Gaiser

Subjects

chemistry.chemical_compound, Multidisciplinary, Epidermis (botany), chemistry, Cell adhesion molecule, In vivo, Conditional gene knockout, Motility, Chemotaxis, Epithelial cell adhesion molecule, Adhesion, Biology, Cell biology

Abstract

After activation, Langerhans cells (LC), a distinct subpopulation of epidermis-resident dendritic cells, migrate from skin to lymph nodes where they regulate the magnitude and quality of immune responses initiated by epicutaneously applied antigens. Modulation of LC–keratinocyte adhesion is likely to be central to regulation of LC migration. LC express high levels of epithelial cell adhesion molecule (EpCAM; CD326), a cell-surface protein that is characteristic of some epithelia and many carcinomas and that has been implicated in intercellular adhesion and metastasis. To gain insight into EpCAM function in a physiologic context in vivo, we generated conditional knockout mice with EpCAM-deficient LC and characterized them. Epidermis from these mice contained increased numbers of LC with normal levels of MHC and costimulatory molecules and T-cell–stimulatory activity in vitro. Migration of EpCAM-deficient LC from skin explants was inhibited, but chemotaxis of dissociated LC was not. Correspondingly, the ability of contact allergen-stimulated, EpCAM-deficient LC to exit epidermis in vivo was delayed, and strikingly fewer hapten-bearing LC subsequently accumulated in lymph nodes. Attenuated migration of EpCAM-deficient LC resulted in enhanced contact hypersensitivity responses as previously described in LC-deficient mice. Intravital microscopy revealed reduced translocation and dendrite motility in EpCAM-deficient LC in vivo in contact allergen-treated mice. These results conclusively link EpCAM expression to LC motility/migration and LC migration to immune regulation. EpCAM appears to promote LC migration from epidermis by decreasing LC–keratinocyte adhesion and may modulate intercellular adhesion and cell movement within in epithelia during development and carcinogenesis in an analogous fashion.

Published

2012

45. In vitro analysis of chemotactic leukocyte migration in 3D environments

Author

Michael, Sixt and Tim, Lämmermann

Subjects

Microscopy, Staining and Labeling, Cell Culture Techniques, Dendritic Cells, Time-Lapse Imaging, Chemotaxis, Leukocyte, Mice, Cell Migration Assays, Leukocyte, Leukocytes, Animals, Collagen, Single-Cell Analysis, Gels, Cells, Cultured

Abstract

Cell migration on two-dimensional (2D) substrates follows entirely different rules than cell migration in three-dimensional (3D) environments. This is especially relevant for leukocytes that are able to migrate in the absence of adhesion receptors within the confined geometry of artificial 3D extracellular matrix scaffolds and within the interstitial space in vivo. Here, we describe in detail a simple and economical protocol to visualize dendritic cell migration in 3D collagen scaffolds along chemotactic gradients. This method can be adapted to other cell types and may serve as a physiologically relevant paradigm for the directed locomotion of most amoeboid cells.

Published

2011

46. In Vitro Analysis of Chemotactic Leukocyte Migration in 3D Environments

Author

Michael Sixt and Tim Lämmermann

Subjects

Extracellular matrix, Leukocyte migration, Cell type, Single-cell analysis, Chemistry, Motility, Cell migration, Chemotaxis, Dendritic cell migration, Cell biology

Abstract

Cell migration on two-dimensional (2D) substrates follows entirely different rules than cell migration in three-dimensional (3D) environments. This is especially relevant for leukocytes that are able to migrate in the absence of adhesion receptors within the confined geometry of artificial 3D extracellular matrix scaffolds and within the interstitial space in vivo. Here, we describe in detail a simple and economical protocol to visualize dendritic cell migration in 3D collagen scaffolds along chemotactic gradients. This method can be adapted to other cell types and may serve as a physiologically relevant paradigm for the directed locomotion of most amoeboid cells.

Published

2011

47. Adaptive force transmission in amoeboid cell migration

Author

Matthieu Piel, Michele Weber, Joachim P. Spatz, Michael Sixt, Jörg Renkawitz, Kathrin Schumann, Holger Pflicke, Julien Polleux, and Tim Lämmermann

Subjects

Integrins, biology, Chemotaxis, Integrin, Dendritic Cells, Cell Biology, macromolecular substances, Adaptation, Physiological, Actins, Substrate Specificity, Cell biology, Mice, Membrane, Polymerization, Cell surface receptor, biology.protein, Animals, Chemokine CCL19, Pseudopodia, Bleb (cell biology), Cells, Cultured, Actin

Abstract

The leading front of a cell can either protrude as an actin-free membrane bleb that is inflated by actomyosin-driven contractile forces, or as an actin-rich pseudopodium, a site where polymerizing actin filaments push out the membrane1, 2, 3. Pushing filaments can only cause the membrane to protrude if the expanding actin network experiences a retrograde counter-force, which is usually provided by transmembrane receptors of the integrin family4. Here we show that chemotactic dendritic cells mechanically adapt to the adhesive properties of their substrate by switching between integrin-mediated and integrin-independent locomotion. We found that on engaging the integrin–actin clutch, actin polymerization was entirely turned into protrusion, whereas on disengagement actin underwent slippage and retrograde flow. Remarkably, accelerated retrograde flow was balanced by an increased actin polymerization rate; therefore, cell shape and protrusion velocity remained constant on alternating substrates. Due to this adaptive response in polymerization dynamics, tracks of adhesive substrate did not dictate the path of the cells. Instead, directional guidance was exclusively provided by a soluble gradient of chemoattractant, which endowed these 'amoeboid' cells with extraordinary flexibility, enabling them to traverse almost every type of tissue.

Published

2009

48. Mechanical modes of 'amoeboid' cell migration

Author

Michael Sixt and Tim Lämmermann

Subjects

Force generation, Amoeboid movement, Cell type, Eukaryota, Amoeboid cell migration, Motility, Cell Biology, Cell movement, Biology, Biomechanical Phenomena, Cell biology, Cell Movement, Cell Adhesion, Animals, Humans, Cell adhesion, Swimming, Actin, Muscle Contraction

Abstract

The morphological term 'amoeboid' migration subsumes a number of rather distinct biophysical modes of cellular locomotion that range from blebbing motility to entirely actin-polymerization-based gliding. Here, we discuss the diverse principles of force generation and force transduction that lead to the distinct amoeboid phenotypes. We argue that shifting the balance between actin protrusion, actomyosin contraction, and adhesion to the extracellular substrate can explain the different modes of amoeboid movement and that blebbing and gliding are barely extreme variants of one common migration strategy. Depending on the cell type, physiological conditions or experimental manipulation, amoeboid cells can adopt the distinct mechanical modes of amoeboid migration.

Published

2009

49. Cdc42-dependent leading edge coordination is essential for interstitial dendritic cell migration

Author

Cord Brakebusch, Xunwei Wu, Michael Sixt, Karin Hirsch, Tim Lämmermann, and Jörg Renkawitz

Subjects

Mice, Knockout, Immunology, Motility, Cell Differentiation, Cell migration, Dendritic Cells, Cell Biology, Hematology, macromolecular substances, Biology, Actin cytoskeleton, Biochemistry, Interstitial cell, Cell biology, Extracellular matrix, Mice, Cell Movement, Animals, Chemokine CCL19, cdc42 GTP-Binding Protein, Cytoskeleton, Dendritic cell migration, Cells, Cultured, Actin

Abstract

Mature dendritic cells (DCs) moving from the skin to the lymph node are a prototypic example of rapidly migrating amoeboid leukocytes. Interstitial DC migration is directionally guided by chemokines, but independent of specific adhesive interactions with the tissue as well as pericellular proteolysis. Instead, the protrusive flow of the actin cytoskeleton directly drives a basal mode of locomotion that is occasionally supported by actomyosin contractions at the trailing edge to propel the cell's rigid nucleus. We here delete the small GTPase Cdc42 in DCs and find that actin flow and actomyosin contraction are still initiated in response to chemotactic cues. Accordingly, the cells are able to polarize and form protrusions. However, in the absence of Cdc42 the protrusions are temporally and spatially dysregulated, which leads to impaired leading edge coordination. Although this defect still allows the cells to move on 2-dimensional surfaces, their in vivo motility is completely abrogated. We show that this difference is entirely caused by the geometric complexity of the environment, as multiple competing protrusions lead to instantaneous entanglement within 3-dimensional extracellular matrix scaffolds. This demonstrates that the decisive factor for migrating DCs is not specific interaction with the extracellular environment, but adequate coordination of cytoskeletal flow.

Published

2009

50. Rapid leukocyte migration by integrin-independent flowing and squeezing

Author

Karin Hirsch, Tim Lämmermann, David R. Critchley, Michael Sixt, Markus Keller, Bernhard L. Bader, Tim Worbs, Reinhold Förster, Susan J. Monkley, Reinhard Fässler, and Roland Wedlich-Söldner

Subjects

Leukocyte migration, Integrins, Time Factors, Integrin, Mice, Cell Movement, Cell Adhesion, Leukocytes, Animals, Cytoskeleton, Cell adhesion, Dendritic cell migration, Cell Shape, Actin, Cell Nucleus, Myosin Type II, Multidisciplinary, biology, Chemistry, Chemotaxis, Dendritic Cells, Actins, Cell biology, biology.protein, Lymph Nodes, Leukocyte chemotaxis

Abstract

All metazoan cells carry transmembrane receptors of the integrin family, which couple the contractile force of the actomyosin cytoskeleton to the extracellular environment. In agreement with this principle, rapidly migrating leukocytes use integrin-mediated adhesion when moving over two-dimensional surfaces. As migration on two-dimensional substrates naturally overemphasizes the role of adhesion, the contribution of integrins during three-dimensional movement of leukocytes within tissues has remained controversial. We studied the interplay between adhesive, contractile and protrusive forces during interstitial leukocyte chemotaxis in vivo and in vitro. We ablated all integrin heterodimers from murine leukocytes, and show here that functional integrins do not contribute to migration in three-dimensional environments. Instead, these cells migrate by the sole force of actin-network expansion, which promotes protrusive flowing of the leading edge. Myosin II-dependent contraction is only required on passage through narrow gaps, where a squeezing contraction of the trailing edge propels the rigid nucleus.

Published

2008