Your search keyword '"Arthur Liesz"' showing total 81 results

1. CD8+ T cells induce interferon-responsive oligodendrocytes and microglia in white matter aging

Author

Tuğberk Kaya, Nicola Mattugini, Lu Liu, Hao Ji, Ludovico Cantuti-Castelvetri, Jianping Wu, Martina Schifferer, Janos Groh, Rudolf Martini, Simon Besson-Girard, Seiji Kaji, Arthur Liesz, Ozgun Gokce, and Mikael Simons

Subjects

Mice, Oligodendroglia, General Neuroscience, Animals, ddc:610, Microglia, Interferons, CD8-Positive T-Lymphocytes, White Matter

Abstract

A hallmark of nervous system aging is a decline of white matter volume and function, but the underlying mechanisms leading to white matter pathology are unknown. In the present study, we found age-related alterations of oligodendrocyte cell state with a reduction in total oligodendrocyte density in aging murine white matter. Using single-cell RNA-sequencing, we identified interferon (IFN)-responsive oligodendrocytes, which localize in proximity to CD8+ T cells in aging white matter. Absence of functional lymphocytes decreased the number of IFN-responsive oligodendrocytes and rescued oligodendrocyte loss, whereas T-cell checkpoint inhibition worsened the aging response. In addition, we identified a subpopulation of lymphocyte-dependent, IFN-responsive microglia in the vicinity of the CD8+ T cells in aging white matter. In summary, we provide evidence that CD8+ T-cell-induced, IFN-responsive oligodendrocytes and microglia are important modifiers of white matter aging.

Published

2022

2. The role of circulating cell-free DNA as an inflammatory mediator after stroke

Author

Stefan Roth, Saskia R. Wernsdorf, and Arthur Liesz

Subjects

Immunology, Immunology and Allergy

Abstract

Stroke is the second leading cause of death worldwide and a leading cause of disability. Clinical and experimental studies highlighted the complex role of the immune system in the pathophysiology of stroke. Ischemic brain injury leads to the release of cell-free DNA, a damage-associated molecular pattern, which binds to pattern recognition receptors on immune cells such as toll-like receptors and cytosolic inflammasome sensors. The downstream signaling cascade then induces a rapid inflammatory response. In this review, we are highlighting the characteristics of cell-free DNA and how these can affect a local as well as a systemic response after stroke. For this purpose, we screened literature on clinical studies investigating cell-free DNA concentration and properties after brain ischemia. We report the current understanding for mechanisms of DNA uptake and sensing in the context of post-stroke inflammation. Moreover, we compare possible treatment options targeting cell-free DNA, DNA-sensing pathways, and the downstream mediators. Finally, we describe clinical implications of this inflammatory pathway for stroke patients, open questions, and potential future research directions.

Published

2023

3. Perspective Review of Myeloid Immune Cell Responses and Poststroke Immunosuppression

Author

Wanqing Xie, Alba Simats, Yunlu Guo, Tingting Huang, Xiaoyu Sun, Weijie Chen, Yuxuan Lin, Xin Wang, Zhongmeng Lai, Weifeng Yu, Arthur Liesz, and Peiying Li

Subjects

Advanced and Specialized Nursing, Neurology (clinical), Cardiology and Cardiovascular Medicine

Abstract

Ischemic stroke profoundly influences the peripheral immune system, which responds quickly to brain ischemia and participates in the evolution of poststroke neuroinflammation, while a period of systemic immunosuppression ensues. Poststroke immunosuppression brings harmful consequences, including increased infection rates and escalated death. As the most abundant cell population in the fast-responding innate immune system, myeloid cells including neutrophils and monocytes play an indispensable role in systemic immunosuppression after stroke. The change in myeloid response after stroke can be regulated by circulating DAMPs (damage-associated molecular patterns) and neuromodulatory mechanisms, which contain sympathetic nervous system, hypothalamic-pituitary-adrenal, and parasympathetic nervous system. In this review, we summarize the emerging roles and newly identified mechanisms underlying myeloid cell response in poststroke immunosuppression. Deeper understanding of the above points may pave the way for future development of novel therapeutic strategies to treat poststroke immunosuppression.

Published

2023

4. Stroke induces early recurrent vascular events by inflammasome-dependent atherosclerotic plaque rupture

Author

Arthur Liesz, Jiayu Cao, Stefan Roth, Sijia Zhang, Anna Kopczak, Marios Georgakis, Xinghai Li, Alexander Dutsch, Thomas Liman, Matthias Endres, David Brough, Jack Green, Saskia Wernsdorf, Christina Fürle, Olga Carofiglio, Jie Zhu, Yaw Asare, DEMDAS Study Group, Martin Dichgans, Hendrik Sager, and Gerrit Grosse

Abstract

The risk of early recurrent events after stroke remains high despite currently established secondary prevention strategies. Risk is particularly high in patients with atherosclerosis, with more than 10% of patients experiencing early recurrent events. However, despite the enormous medical burden of this clinical phenomenon, the underlying mechanisms leading to increased vascular risk and recurrent stroke are largely unknown. Here, using a novel mouse model of stroke-induced recurrent ischemia, we show that stroke leads to activation of the AIM2 inflammasome in vulnerable atherosclerotic plaques via an increase of circulating cell-free DNA from the ischemic tissue. Enhanced plaque inflammation post-stroke results in plaque destabilization and atherothrombosis, finally leading to arterio-arterial embolism and recurrent stroke within days after the index stroke. We confirm key steps of plaque destabilization also after experimental myocardial infarction and in carotid artery plaque samples from patients with acute stroke. Neutralization of cell-free DNA by DNase treatment or inhibition of inflammasome activation reduced the rate of stroke recurrence after experimental stroke. Our findings present an explanation for the high recurrence rate after incident ischemic events in atherosclerotic patients. The detailed mechanisms uncovered here provide so far clinically uncharted therapeutic targets for which we show high efficacy to prevent recurrent events. Targeting DNA-mediated inflammasome activation after remote tissue injury represents a promising avenue for further clinical development in the prevention of early recurrent events.

Published

2023

5. Author response: T cells modulate the microglial response to brain ischemia

Author

Corinne Benakis, Alba Simats, Sophie Tritschler, Steffanie Heindl, Simon Besson-Girard, Gemma Llovera, Kelsey Pinkham, Anna Kolz, Alessio Ricci, Fabian J Theis, Stefan Bittner, Özgün Gökce, Anneli Peters, and Arthur Liesz

Published

2022

6. Blocking P2X7 by intracerebroventricular injection of P2X7-specific nanobodies reduces stroke lesions

Author

Maximilian Wilmes, Carolina Pinto Espinoza, Peter Ludewig, Joschi Stabernack, Arthur Liesz, Annette Nicke, Mathias Gelderblom, Christian Gerloff, Simonetta Falzoni, Eva Tolosa, Francesco Di Virgilio, Björn Rissiek, Nikolaus Plesnilla, Friedrich Koch-Nolte, and Tim Magnus

Subjects

Receptors, Purinergic P2, General Neuroscience, Caspase 1, Interleukin-1beta, Immunology, Infarction, Middle Cerebral Artery, Single-Domain Antibodies, Stroke, Mice, Cellular and Molecular Neuroscience, Adenosine Triphosphate, Neurology, Animals, Calcium, Microglia, Receptors, Purinergic P2X7

Abstract

Background Previous studies have demonstrated that purinergic receptors could be therapeutic targets to modulate the inflammatory response in multiple models of brain diseases. However, tools for the selective and efficient targeting of these receptors are lacking. The development of new P2X7-specific nanobodies (nbs) has enabled us to effectively block the P2X7 channel. Methods Temporary middle cerebral artery occlusion (tMCAO) in wild-type (wt) and P2X7 transgenic (tg) mice was used to model ischemic stroke. Adenosine triphosphate (ATP) release was assessed in transgenic ATP sensor mice. Stroke size was measured after P2X7-specific nbs were injected intravenously (iv) and intracerebroventricularly (icv) directly before tMCAO surgery. In vitro cultured microglia were used to investigate calcium influx, pore formation via 4,6-diamidino-2-phenylindole (DAPI) uptake, caspase 1 activation and interleukin (IL)-1β release after incubation with the P2X7-specific nbs. Results Transgenic ATP sensor mice showed an increase in ATP release in the ischemic hemisphere compared to the contralateral hemisphere or the sham-treated mice up to 24 h after stroke. P2X7-overexpressing mice had a significantly greater stroke size 24 h after tMCAO surgery. In vitro experiments with primary microglial cells demonstrated that P2X7-specific nbs could inhibit ATP-triggered calcium influx and the formation of membrane pores, as measured by Fluo4 fluorescence or DAPI uptake. In microglia, we found lower caspase 1 activity and subsequently lower IL-1β release after P2X7-specific nb treatment. The intravenous injection of P2X7-specific nbs compared to isotype controls before tMCAO surgery did not result in a smaller stroke size. As demonstrated by fluorescence-activated cell sorting (FACS), after stroke, iv injected nbs bound to brain-infiltrated macrophages but not to brain resident microglia, indicating insufficient crossing of the blood–brain barrier of the nbs. Therefore, we directly icv injected the P2X7-specific nbs or the isotype nbs. After icv injection of 30 µg of P2X7 specific nbs, P2X7 specific nbs bound sufficiently to microglia and reduced stroke size. Conclusion Mechanistically, we can show that there is a substantial increase of ATP locally after stroke and that blockage of the ATP receptor P2X7 by icv injected P2X7-specific nbs can reduce ischemic tissue damage.

Published

2022

7. The gut-brain axis in ischemic stroke: its relevance in pathology and as a therapeutic target

Author

Corinne Benakis and Arthur Liesz

Subjects

General Computer Science

Abstract

The gut contains the largest reservoir of microorganisms of the human body, termed as the gut microbiota which emerges as a key pathophysiological factor in health and disease. The gut microbiota has been demonstrated to influence various brain functions along the “gut-brain axis”. Stroke leads to intestinal dysmotility and leakiness of the intestinal barrier which are associated with change of the gut microbiota composition and its interaction with the human host. Growing evidence over the past decade has demonstrated an important role of these post-stroke changes along the gut-brain axis to contribute to stroke pathology and be potentially druggable targets for future therapies. The impact of the gut microbiota on brain health and repair after stroke might be attributed to the diverse functions of gut bacteria in producing neuroactive compounds, modulating the host’s metabolism and immune status. Therefore, a better understanding on the gut-brain axis after stroke and its integration in a broader concept of stroke pathology could open up new avenues for stroke therapy. Here, we discuss current concepts from preclinical models and human studies on the bi-directional communication along the microbiota-gut-brain axis in stroke.

Published

2022

8. Discovery of an AIM2 inflammasome inhibitor for the treatment of DNA-driven inflammatory disease

Author

Jack P. Green, Lina Y. El-Sharkawy, Stefan Roth, Jie Zhu, Jiayu Cao, Andrew G. Leach, Arthur Liesz, Sally Freeman, and David Brough

Abstract

Inflammation driven by DNA sensors is now understood to be central to disease pathogenesis. Here we describe new inhibitors of pathogenic DNA sensing, primarily of the inflammasome forming sensor AIM2. Molecular modelling and biochemistry has revealed potent inhibitors of AIM2 that work by binding competitively to the DNA binding site. Though less potent, these AIM2 inhibitors, 4-sulfonic calixarenes, also inhibit DNA sensors cGAS and TLR9 demonstrating a broad utility against pathogenic DNA-driven inflammatory responses. The 4-sulfonic calixarenes inhibited AIM2 dependent post-stroke T cell death, highlighting a proof of concept that the 4-sulfonic calixarenes could be effective at combatting post-stroke immunosuppression. By extension, we propose a broad utility against DNA driven inflammation in disease. Finally, we reveal that the ancient drug suramin, by virtue of its structural similarities, is an excellent inhibitor of DNA-dependent inflammation and propose that suramin could be rapidly repurposed to meet an ever increasing clinical need.

Published

2022

9. T cells modulate the microglial response to brain ischemia

Author

Corinne Benakis, Alba Simats, Sophie Tritschler, Steffanie Heindl, Simon Besson-Girard, Gemma Llovera, Kelsey Pinkham, Anna Kolz, Alessio Ricci, Fabian J Theis, Stefan Bittner, Özgün Gökce, Anneli Peters, and Arthur Liesz

Subjects

T Cells, Immunology, Inflammation, Microglia, Mouse, Neuroscience, Single-cell Transcriptomics, Stroke, General Immunology and Microbiology, General Neuroscience, Humans, Brain, General Medicine, General Biochemistry, Genetics and Molecular Biology, Brain Ischemia, Signal Transduction

Abstract

Neuroinflammation after stroke is characterized by the activation of resident microglia and the invasion of circulating leukocytes into the brain. Although lymphocytes infiltrate the brain in small number, they have been consistently demonstrated to be the most potent leukocyte subpopulation contributing to secondary inflammatory brain injury. However, the exact mechanism of how this minimal number of lymphocytes can profoundly affect stroke outcome is still largely elusive. Here, using a mouse model for ischemic stroke, we demonstrated that early activation of microglia in response to stroke is differentially regulated by distinct T cell subpopulations – with TH1cells inducing a type I INF signaling in microglia and regulatory T cells (TREG) cells promoting microglial genes associated with chemotaxis. Acute treatment with engineered T cells overexpressing IL-10 administered into the cisterna magna after stroke induces a switch of microglial gene expression to a profile associated with pro-regenerative functions. Whereas microglia polarization by T cell subsets did not affect the acute development of the infarct volume, these findings substantiate the role of T cells in stroke by polarizing the microglial phenotype. Targeting T cell-microglia interactions can have direct translational relevance for further development of immune-targeted therapies for stroke and other neuroinflammatory conditions.

Published

2022

10. Discovery of an inhibitor of DNA-driven inflammation that preferentially targets the AIM2 inflammasome

Author

Jack P. Green, Lina Y. El-Sharkawy, Stefan Roth, Jie Zhu, Jiayu Cao, Andrew G. Leach, Arthur Liesz, Sally Freeman, and David Brough

Subjects

Multidisciplinary

Published

2023

11. Immunity in Stroke: The Next Frontier

Author

Ting Li and Arthur Liesz

Subjects

Inflammation, Stroke, Brain Injuries, Brain, Humans, Hematology, Brain Ischemia, Ischemic Stroke

Abstract

Translational stroke research has long been focusing on neuroprotective strategies to prevent secondary tissue injury and promote recovery after acute ischemic brain injury. The inflammatory response to stroke has more recently emerged as a key pathophysiological pathway contributing to stroke outcome. It is now accepted that the inflammatory response is functionally involved in all phases of the ischemic stroke pathophysiology. The immune response is therefore considered a breakthrough target for ischemic stroke treatment. On one side, stroke induces a local neuroinflammatory response, in which the inflammatory activation of glial, endothelial and brain-invading cells contributes to lesion progression after stroke. On the other side, ischemic brain injury perturbs systemic immune homeostasis and results in long-lasting changes of systemic immunity. Here, we briefly summarize current concepts in local neuroinflammation and the systemic immune responses after stroke, and highlight two promising therapeutic strategies for poststroke inflammation.

Published

2022

12. Implications of immune responses for ischemic brain injury and stroke recovery

Author

Dirk M. Hermann, Egor Dzyubenko, and Arthur Liesz

Subjects

Endocrine and Autonomic Systems, business.industry, medicine.medical_treatment, Immunology, Immunity, MEDLINE, Brain, Ischemic brain injury, Bioinformatics, Brain Ischemia, Stroke, Behavioral Neuroscience, Text mining, Immune system, Brain Injuries, medicine, Humans, business, Stroke recovery

Published

2021

13. The microbiome-gut-brain axis in acute and chronic brain diseases

Author

Camille Martin-Gallausiaux, Corinne Benakis, Paul Wilmes, Philip Melton, Arthur Liesz, and Jean-Pierre Trezzi

Subjects

Central Nervous System, 0301 basic medicine, Gut–brain axis, Central nervous system, Disease, Biology, 03 medical and health sciences, 0302 clinical medicine, Alzheimer Disease, medicine, Animals, Humans, Microbiome, General Neuroscience, Gastrointestinal Microbiome, Brain, Parkinson Disease, medicine.disease, 3. Good health, Stroke, 030104 developmental biology, medicine.anatomical_structure, Ageing, Alzheimer's disease, Neuroscience, 030217 neurology & neurosurgery, Function (biology)

Abstract

The gut microbiome - the largest reservoir of microorganisms of the human body - is emerging as an important player in neurodevelopment and ageing as well as in brain diseases including stroke, Alzheimer's disease and Parkinson's disease. The growing knowledge on mediators and triggered pathways has advanced our understanding of the interactions along the gut-brain axis. Gut bacteria produce neuroactive compounds and can modulate neuronal function, plasticity and behavior. Furthermore, intestinal microorganisms impact the host's metabolism and immune status which in turn affect neuronal pathways in the enteric and central nervous systems. Here, we discuss the recent insights from human studies and animal models on the bi-directional communication along the microbiome-gut-brain axis in both acute and chronic brain diseases.

Published

2020

14. T cells induce interferon-responsive oligodendrocytes during white matter aging

Author

Tuğberk Kaya, Nicola Mattugini, Lu Liu, Hao Ji, Simon Besson-Girard, Seiji Kaiji, Arthur Liesz, Ozgun Gokce, and Mikael Simons

Abstract

SUMMARYA hallmark of nervous system aging is a decline of white matter volume and function, but the underlying mechanisms leading to white matter pathology are unknown. Here, we found age-related alterations of oligodendrocytes with a reduction of total oligodendrocyte density in the aging murine white matter. Using single-cell RNA sequencing, we identify interferon-responsive oligodendrocytes, which localize in proximity of CD8+ T cells in the aging white matter. Absence of functional lymphocytes decreased oligodendrocyte reactivity and rescued oligodendrocyte loss, while T-cell checkpoint inhibition worsened the aging affect. In summary, we provide evidence that T cells induced interferon-responsive oligodendrocytes are important modifiers of white matter aging.

Published

2022

15. Reduced Acquisition Time [18F]GE-180 PET Scanning Protocol Replaces Gold-Standard Dynamic Acquisition in a Mouse Ischemic Stroke Model

Author

Artem Zatcepin, Steffanie Heindl, Ulrike Schillinger, Lena Kaiser, Simon Lindner, Peter Bartenstein, Anna Kopczak, Arthur Liesz, Matthias Brendel, and Sibylle I. Ziegler

Subjects

Medicine (General), R5-920, image-derived blood input function (IDIF), microglia, ddc:610, positron emission tomography (PET), General Medicine, GE-180 imaging, kinetic modeling, stroke, neuroinflammation, translocator protein (TSPO) imaging

Abstract

AimUnderstanding neuroinflammation after acute ischemic stroke is a crucial step on the way to an individualized post-stroke treatment. Microglia activation, an essential part of neuroinflammation, can be assessed using [18F]GE-180 18 kDa translocator protein positron emission tomography (TSPO-PET). However, the commonly used 60–90 min post-injection (p.i.) time window was not yet proven to be suitable for post-stroke neuroinflammation assessment. In this study, we compare semi-quantitative estimates derived from late time frames to quantitative estimates calculated using a full 0–90 min dynamic scan in a mouse photothrombotic stroke (PT) model.Materials and MethodsSix mice after PT and six sham mice were included in the study. For a half of the mice, we acquired four serial 0–90 min scans per mouse (analysis cohort) and calculated standardized uptake value ratios (SUVRs; cerebellar reference) for the PT volume of interest (VOI) in five late 10 min time frames as well as distribution volume ratios (DVRs) for the same VOI. We compared late static 10 min SUVRs and the 60–90 min time frame of the analysis cohort to the corresponding DVRs by linear fitting. The other half of the animals received a static 60–90 min scan and was used as a validation cohort. We extrapolated DVRs by using the static 60–90 min p.i. time window, which were compared to the DVRs of the analysis cohort.ResultsWe found high linear correlations between SUVRs and DVRs in the analysis cohort for all studied 10 min time frames, while the fits of the 60–70, 70–80, and 80–90 min p.i. time frames were the ones closest to the line of identity. For the 60–90 min time window, we observed an excellent linear correlation between SUVR and DVR regardless of the phenotype (PT vs. sham). The extrapolated DVRs of the validation cohort were not significantly different from the DVRs of the analysis group.ConclusionSimplified quantification by a reference tissue ratio of the late 60–90 min p.i. [18F]GE-180 PET image can replace full quantification of a dynamic scan for assessment of microglial activation in the mouse PT model.

Published

2022

16. Reduced Acquisition Time [

Author

Artem, Zatcepin, Steffanie, Heindl, Ulrike, Schillinger, Lena, Kaiser, Simon, Lindner, Peter, Bartenstein, Anna, Kopczak, Arthur, Liesz, Matthias, Brendel, and Sibylle I, Ziegler

Abstract

Understanding neuroinflammation after acute ischemic stroke is a crucial step on the way to an individualized post-stroke treatment. Microglia activation, an essential part of neuroinflammation, can be assessed using [Six mice after PT and six sham mice were included in the study. For a half of the mice, we acquired four serial 0-90 min scans per mouse (analysis cohort) and calculated standardized uptake value ratios (SUVRs; cerebellar reference) for the PT volume of interest (VOI) in five late 10 min time frames as well as distribution volume ratios (DVRs) for the same VOI. We compared late static 10 min SUVRs and the 60-90 min time frame of the analysis cohort to the corresponding DVRs by linear fitting. The other half of the animals received a static 60-90 min scan and was used as a validation cohort. We extrapolated DVRs by using the static 60-90 min p.i. time window, which were compared to the DVRs of the analysis cohort.We found high linear correlations between SUVRs and DVRs in the analysis cohort for all studied 10 min time frames, while the fits of the 60-70, 70-80, and 80-90 min p.i. time frames were the ones closest to the line of identity. For the 60-90 min time window, we observed an excellent linear correlation between SUVR and DVR regardless of the phenotype (PTSimplified quantification by a reference tissue ratio of the late 60-90 min p.i. [

Published

2021

17. Nanobody-Mediated Inhibition of P2X7 on Microglia Improves Stroke Outcome

Author

Maximilian Wilmes, Carolina Pinto Espinoza, Peter Ludewig, Arthur Liesz, Annette Nicke, Mathias Gelderblom, Christian Gerloff, Simonetta Falzoni, Eva Tolosa, Francesco Di Virgilio, Björn Rissiek, Nikolaus Plesnilla, Friedrich Koch-Nolte, and Tim Magnus

Abstract

BackgroundPrevious studies have demonstrated that purinergic receptors could be therapeutic targets to modulate the inflammatory response in multiple brain disease models. However, tools for the selective and efficient targeting of these receptors are scarce. The new development of P2X7-specific nanobodies (nbs) enables us to effectively block the P2X7-channel.MethodsTemporary middle cerebral artery occlusion (tMCAO) in wildtype and P2X7-transgenic mice was used as a model for ischemic stroke. ATP release was assessed in transgenic ATP sensor mice. Stroke size was measured without treatment and after injection of P2X7-specific nbs i.v. and i.c.v. directly before tMCAO-surgery. P2X7-GFP expressing transgenic mice were used to show immunhistochemically P2X7 distribution in the brain. In vitro cultured microglia were used to investigate calcium-influx, pore-formation via DAPI uptake, caspase 1 activation and IL-1b release after incubation with P2X7-specific nbs. ResultsATP sensor mice showed an increase of ATP-release in the ischemic hemisphere compared to the contralateral hemisphere or sham mice up to 24 h after stroke. We could further verify the role of the ATP-P2X7 axis in P2X7-overexpressing mice, which showed significantly greater stroke volumes after 24 h. In vitro experiments with primary microglia cells showed that P2X7-specific nanobodies were capable of dampening the ATP-trigged calcium-influx and formation of membrane pores measured by Fluo4 fluorescence or DAPI uptake. We found a lower caspase 1 activity and a subsequently lower IL-1b release. However, the intravenous (i.v.) injection of P2X7-specific nanobodies compared to isotype controls before the tMCAO-surgery did not result in smaller stroke size compared to isotype controls. As demonstrated by FACS, nbs had only reached brain infiltrating macrophages but not microglia. To reach microglia, we injected the P2X7-spezific nbs or the isotype directly intraventricularly (icv). 30 mg of P2X7-specific nbs proved efficient for microglial targeting, reducing post-stroke microglia activation and stroke size significantly.ConclusionHere, we demonstrate the importance of locally produced ATP for the tissue damage observed in ischemic stroke and we show the potential of icv injected P2X7-specific nbs to reduce ischemic tissue damage.

Published

2021

18. Coming to the Rescue: Regulatory T Cells for Promoting Recovery After Ischemic Stroke

Author

Yueman Zhang, Arthur Liesz, and Peiying Li

Subjects

Advanced and Specialized Nursing, Microglia, business.industry, Recovery of Function, biochemical phenomena, metabolism, and nutrition, T-Lymphocytes, Regulatory, Proinflammatory cytokine, medicine.anatomical_structure, Immune system, Immunology, Ischemic stroke, bacteria, Medicine, Animals, Humans, Neurology (clinical), Cardiology and Cardiovascular Medicine, business, Immune cell infiltration, Homeostasis, Ischemic Stroke

Abstract

Immune cell infiltration to the injured brain is a key component of the neuroinflammatory response after ischemic stroke. In contrast to the large amount of proinflammatory immune cells, regulatory T cells, are an important subgroup of T cells that are involved in maintaining immune homeostasis and suppress an overshooting immune reaction after stroke. Numerous previous reports have consistently demonstrated the beneficial role of this immunosuppressive immune cell population during the acute phase after experimental stroke by limiting inflammatory lesion progression. Two recent studies expanded now this concept and demonstrate that regulatory T cells-mediated effects also promote chronic recovery after stroke by promoting a proregenerative tissue environment. These recent findings suggest that boosting regulatory T cells could be beneficial beyond modulating the immediate neuroinflammatory response and improve chronic functional recovery.

Published

2021

19. CD8

Author

Tuğberk, Kaya, Nicola, Mattugini, Lu, Liu, Hao, Ji, Ludovico, Cantuti-Castelvetri, Jianping, Wu, Martina, Schifferer, Janos, Groh, Rudolf, Martini, Simon, Besson-Girard, Seiji, Kaji, Arthur, Liesz, Ozgun, Gokce, and Mikael, Simons

Subjects

Mice, Oligodendroglia, Animals, Microglia, Interferons, CD8-Positive T-Lymphocytes, White Matter

Abstract

A hallmark of nervous system aging is a decline of white matter volume and function, but the underlying mechanisms leading to white matter pathology are unknown. In the present study, we found age-related alterations of oligodendrocyte cell state with a reduction in total oligodendrocyte density in aging murine white matter. Using single-cell RNA-sequencing, we identified interferon (IFN)-responsive oligodendrocytes, which localize in proximity to CD8

Published

2021

20. T cells modulate the microglial response to brain ischemia

Author

Sophie Tritschler, Kelsey Pinkham, Corinne Benakis, Anneli Peters, Ozgun Gokce, Anna Kolz, Fabian J. Theis, Gemma Llovera, Alba Simats, Simon Besson-Girard, Steffanie Heindl, and Arthur Liesz

Subjects

Microglia, business.industry, T cell, medicine.disease, Phenotype, Brain ischemia, Crosstalk (biology), medicine.anatomical_structure, Gene expression, medicine, Cancer research, business, Stroke, Neuroinflammation

Abstract

Neuroinflammation after stroke is characterized by the activation of resident microglia and the invasion of circulating leukocytes into the brain. Although lymphocytes infiltrate the brain in small number, they have been consistently demonstrated to be the most potent leukocyte subpopulation contributing to secondary inflammatory brain injury. However, the exact mechanism how this minimal number of lymphocytes can profoundly affect stroke outcome is still largely elusive. Here, using a mouse model for ischemic stroke, we demonstrated that early activation of microglia in response to stroke is differentially regulated by distinct T cell subpopulations. Acute treatment with engineered T cells overexpressing IL-10 administered into the cisterna magna after stroke induces a switch of microglial gene expression to a profile associated with pro-regenerative functions. These findings substantiate the role of T cells in stroke with large impact on the cerebral inflammatory milieu by polarizing the microglial phenotype. Targeting T cell-microglia interactions can have direct translational relevance for further development of immune-targeted therapies for stroke and other neuroinflammatory conditions.SummaryThe crosstalk between brain infiltrating T cells and microglia in response to stroke remains elusive. Benakis et al. report that transcriptional signature of the stroke-associated microglia is reprogrammed by distinct T cell subpopulations. Engineered T cells overexpressing IL-10 administered four hours after stroke reinitiate microglial function inducing a pro-regenerative environment.

Published

2021

21. In vivo widefield calcium imaging of the mouse cortex for analysis of network connectivity in health and brain disease

Author

Martin Dichgans, J. Cramer, Marco Duering, Stefan Roth, Arthur Liesz, and Benno Gesierich

Subjects

Male, Computer science, Cognitive Neuroscience, Neuroimaging, 050105 experimental psychology, Mice, 03 medical and health sciences, Prosencephalon, 0302 clinical medicine, Calcium imaging, In vivo, Connectome, medicine, Animals, Focal brain injury, 0501 psychology and cognitive sciences, Stroke, Cerebral Cortex, Mouse cortex, medicine.diagnostic_test, Optical Imaging, 05 social sciences, Motor Cortex, medicine.disease, Brain disease, Mice, Inbred C57BL, Functional imaging, Disease Models, Animal, medicine.anatomical_structure, Neurology, Excitatory postsynaptic potential, Calcium, Female, Nerve Net, Functional magnetic resonance imaging, Neuroscience, 030217 neurology & neurosurgery, Preclinical imaging, Motor cortex

Abstract

The organization of brain areas in functionally connected networks, their dynamic changes, and perturbations in disease states are subject of extensive investigations. Research on functional networks in humans predominantly uses functional magnetic resonance imaging (fMRI). However, adopting fMRI and other functional imaging methods to mice, the most widely used model to study brain physiology and disease, poses major technical challenges and faces important limitations. Hence, there is great demand for alternative imaging modalities for network characterization. Here, we present a refined protocol for in vivo widefield calcium imaging of both cerebral hemispheres in mice expressing a calcium sensor in excitatory neurons. We implemented a stringent protocol for minimizing anesthesia and excluding movement artifacts which both imposed problems in previous approaches. We further adopted a method for unbiased identification of functional cortical areas using independent component analysis (ICA) on resting-state imaging data. Biological relevance of identified components was confirmed using stimulus-dependent cortical activation. To explore this novel approach in a model of focal brain injury, we induced photothrombotic lesions of the motor cortex, determined changes in inter- and intrahemispheric connectivity at multiple time points up to 56 days post-stroke and correlated them with behavioral deficits. We observed a severe loss in interhemispheric connectivity after stroke, which was partially restored in the chronic phase and associated with corresponding behavioral motor deficits. Taken together, we present an improved widefield calcium imaging tool accounting for anesthesia and movement artifacts, adopting an advanced analysis pipeline based on human fMRI algorithms and with superior sensitivity to recovery mechanisms in mouse models compared to behavioral tests. This tool will enable new studies on interhemispheric connectivity in murine models with comparability to human imaging studies for a wide spectrum of neuroscience applications in health and disease.

Published

2019

22. T cells in the post-ischemic brain: Troopers or paramedics?

Author

J. Cramer, Arthur Liesz, and Corinne Benakis

Subjects

0301 basic medicine, T-Lymphocytes, Lymphocyte, T cell, Immunology, Inflammation, Brain Ischemia, Brain ischemia, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, Animals, Humans, Immunology and Allergy, business.industry, Neurogenesis, medicine.disease, Acquired immune system, 030104 developmental biology, medicine.anatomical_structure, Neuroimmunology, Neurology, Neurology (clinical), medicine.symptom, business, Neuroscience, 030217 neurology & neurosurgery

Abstract

The immune system is intricately involved in brain development and physiological neuronal function. The influence of the adaptive immune system on several brain diseases has been described in great detail. In ischemic stroke, numerous studies have particularly demonstrated a key role for T cells during the acute phase after the brain injury. Recently, a critical role for T cells has also become more evident for the chronic phase after stroke in modulating delayed neuronal (dys-) function and recovery. Here, T cells may also affect various non-immunological pathways by interacting with brain-resident immune cells and modulating mechanisms such as neurogenesis and angiogenesis. This novel concept suggests T cells as potential therapeutic targets to modulate post-stroke regeneration.

Published

2019

23. Modeling Stroke in Mice: Transient Middle Cerebral Artery Occlusion via the External Carotid Artery

Author

Alba Simats, Arthur Liesz, and Gemma Llovera

Subjects

Middle Cerebral Artery, medicine.medical_specialty, General Chemical Engineering, External carotid artery, General Biochemistry, Genetics and Molecular Biology, Brain ischemia, Mice, Internal medicine, medicine.artery, Neuroplasticity, medicine, Animals, Humans, Middle cerebral artery occlusion, Stroke, General Immunology and Microbiology, business.industry, General Neuroscience, Reproducibility of Results, Infarction, Middle Cerebral Artery, Blood flow, medicine.disease, Disease Models, Animal, Clot lysis, Carotid Artery, External, Middle cerebral artery, Cardiology, business

Abstract

Stroke is the third most common cause of mortality and the leading cause of acquired adult disability in developed countries. To date, therapeutic options are limited to a small proportion of stroke patients within the first hours after stroke. Novel therapeutic strategies are being extensively investigated, especially to prolong the therapeutic time window. These current investigations include the study of important pathophysiological pathways after stroke, such as post-stroke inflammation, angiogenesis, neuronal plasticity, and regeneration. Over the last decade, there has been increasing concern about the poor reproducibility of experimental results and scientific findings among independent research groups. To overcome the so-called "replication crisis", detailed standardized models for all procedures are urgently needed. As an effort within the "ImmunoStroke" research consortium (https://immunostroke.de/), a standardized mouse model of transient middle cerebral artery occlusion (MCAo) is proposed. This model allows the complete restoration of the blood flow upon removal of the filament, simulating the therapeutic or spontaneous clot lysis that occurs in a large proportion of human strokes. The surgical procedure of this "filament" stroke model and tools for its functional analysis are demonstrated in the accompanying video.

Published

2021

24. Modeling Stroke in Mice: Focal Cortical Lesions by Photothrombosis

Author

Gemma Llovera, Kelsey Pinkham, and Arthur Liesz

Subjects

Rose Bengal, General Immunology and Microbiology, Stroke patient, business.industry, General Chemical Engineering, General Neuroscience, Regeneration (biology), Brain, medicine.disease, General Biochemistry, Genetics and Molecular Biology, Brain Ischemia, Surgical methods, Stroke, Brain ischemia, Disease Models, Animal, Mice, Invasive surgery, Neuroplasticity, Animals, Humans, Medicine, business, Neuroscience, Cause of death

Abstract

Stroke is a leading cause of death and acquired adult disability in developed countries. Despite extensive investigation for novel therapeutic strategies, there remain limited therapeutic options for stroke patients. Therefore, more research is needed for pathophysiological pathways such as post-stroke inflammation, angiogenesis, neuronal plasticity, and regeneration. Given the inability of in vitro models to reproduce the complexity of the brain, experimental stroke models are essential for the analysis and subsequent evaluation of novel drug targets for these mechanisms. In addition, detailed standardized models for all procedures are urgently needed to overcome the so-called replication crisis. As an effort within the ImmunoStroke research consortium, a standardized photothrombotic mouse model using an intraperitoneal injection of Rose Bengal and the illumination of the intact skull with a 561 nm laser is described. This model allows the performance of stroke in mice with allocation to any cortical region of the brain without invasive surgery; thus, enabling the study of stroke in various areas of the brain. In this video, the surgical methods of stroke induction in the photothrombotic model along with histological analysis are demonstrated.

Published

2021

25. Can static F-18-GE180 PET be a sufficient surrogate marker for post-stroke neuroinflammation in a mouse model?

Author

A Zatcepin, Steffanie Heindl, U Schillinger, Arthur Liesz, Peter Bartenstein, and Sibylle Ziegler

Subjects

Oncology, medicine.medical_specialty, business.industry, Surrogate endpoint, Internal medicine, Post stroke, Medicine, business, Neuroinflammation

Published

2021

26. Author response: Microbiota-derived short chain fatty acids modulate microglia and promote Aβ plaque deposition

Author

Harald Steiner, Frits Kamp, Finn Peters, Edith Winkler, Andrew J. Macpherson, Christian Haass, Arthur Liesz, Alessio Colombo, Aswin Verhoeven, Sabina Tahirovic, Vikramjeet Singh, Corinne Benakis, Martin Dichgans, Mercedes Gomez de Agüero, Steffanie Heindl, Jochen Herms, Rebecca Sadler, Martin Giera, Laura Sebastian Monasor, Samira Parhizkar, Stefan Roth, and Gemma Llovera

Subjects

medicine.anatomical_structure, Microglia, Chemistry, Biophysics, medicine, Deposition (chemistry)

Published

2021

27. Loss of TREM2 reduces hyperactivation of progranulin deficient microglia but not lysosomal pathology

Author

van Lengerich B, Janine Diehl-Schmid, Matthias Brendel, Haberl S, Anja Capell, Lina Riedl, Di Paolo G, Dominik Paquet, Vogt Ma, Katharina Bürger, Endy Weidinger, Christian Haass, Steffanie Heindl, Jung H. Suh, Julia K. Götzl, Anika Reifschneider, Arthur Liesz, Joseph W. Lewcock, Robinson S, Gnörich J, Brigitte Nuscher, Johannes Levin, Kathryn M. Monroe, A Zatcepin, Karin Wind, Julien Klimmt, Gernot Kleinberger, and Logan T

Subjects

Pathology, medicine.medical_specialty, Microglia, Hyperactivation, TREM2, business.industry, Neurodegeneration, Neurotoxicity, Frontotemporal lobar degeneration, medicine.disease, Neuroprotection, medicine.anatomical_structure, medicine, business, Haploinsufficiency

Abstract

GRN haploinsufficiency causes frontotemporal lobar degeneration and results in microglial hyperactivation, lysosomal dysfunction and TDP-43 deposition. To understand the contribution of microglial hyperactivation to pathology we evaluated genetic and pharmacological approaches suppressing TREM2 dependent transition of microglia from a homeostatic to a disease associated state. Trem2 deficiency in Grn KO mice led to a reduction of microglia activation. To explore antibody-mediated pharmacological modulation of TREM2-dependent microglial states, we identified antagonistic TREM2 antibodies. Treatment of macrophages from GRN-FTLD patients with these antibodies allowed a complete rescue of elevated levels of TREM2 together with increased shedding and reduction of TREM2 signaling. Furthermore, antibody-treated PGRN deficient hiMGL showed dampened microglial hyperactivation, reduced TREM2 signaling and phagocytic activity, however, lack of rescue of lysosomal dysfunction. Similarly, lysosomal dysfunction, lipid dysregulation and glucose hypometabolism of Grn KO mice were not rescued by TREM2 ablation. Furthermore, NfL, a biomarker for neurodegeneration, was elevated in the Grn/Trem2 KO. These findings suggest that microglia hyperactivation is not necessarily contributing to neurotoxicity, and instead demonstrates that TREM2 exhibits neuroprotective potential in this model.

Published

2021

28. Chronic T cell proliferation in brains after stroke could interfere with the efficacy of immunotherapies

Author

Adam Denes, Nicolai Franzmeier, Steffanie Heindl, Olga Carofiglio, Thomas Arzberger, Peter T. Nelson, Nikolett Lénárt, Alessio Ricci, Tibor Hortobágyi, Arthur Liesz, Dieter Edbauer, Qihui Zhou, and Ann M. Stowe

Subjects

0301 basic medicine, immunology [Brain Ischemia], Male, therapy [Stroke], Lymphocyte, Integrin alpha4, T-Lymphocytes, Autopsy, Brain Ischemia, immunology [T-Lymphocytes], 0302 clinical medicine, Neuroinflammation, pathology [Brain], drug effects [Neuronal Plasticity], Immunology and Allergy, immunology [Integrin alpha4], Stroke, Neuronal Plasticity, physiopathology [Stroke], biology, Natalizumab, Brain, Pathophysiology, 3. Good health, medicine.anatomical_structure, drug therapy [Brain Ischemia], immunology [Brain], Female, Immunotherapy, Antibody, drug effects [Recovery of Function], T cell, Immunology, pharmacology [Natalizumab], therapeutic use [Natalizumab], pathology [Brain Ischemia], 03 medical and health sciences, medicine, Animals, Humans, cardiovascular diseases, ddc:610, Lymphocyte Count, Cell Proliferation, business.industry, Brief Definitive Report, Recovery of Function, medicine.disease, Clinical trial, Mice, Inbred C57BL, 030104 developmental biology, biology.protein, business, 030217 neurology & neurosurgery, immunology [Stroke], Neuroscience

Abstract

Heindl et al. describe the local proliferation and clustering of T cells in the brain of mice and humans after stroke. This previously unrecognized phenomenon could explain why blocking cerebral leukocyte invasion might fail to improve long-term stroke recovery., Neuroinflammation is an emerging focus of translational stroke research. Preclinical studies have demonstrated a critical role for brain-invading lymphocytes in post-stroke pathophysiology. Reducing cerebral lymphocyte invasion by anti-CD49d antibodies consistently improves outcome in the acute phase after experimental stroke models. However, clinical trials testing this approach failed to show efficacy in stroke patients for the chronic outcome 3 mo after stroke. Here, we identify a potential mechanistic reason for this phenomenon by detecting chronic T cell accumulation—evading the systemic therapy—in the post-ischemic brain. We observed a persistent accumulation of T cells in mice and human autopsy samples for more than 1 mo after stroke. Cerebral T cell accumulation in the post-ischemic brain was driven by increased local T cell proliferation rather than by T cell invasion. This observation urges re-evaluation of current immunotherapeutic approaches, which target circulating lymphocytes for promoting recovery after stroke., Graphical Abstract

Published

2021

29. Detection of cytokine-induced sickness behavior after ischemic stroke by an optimized behavioral assessment battery

Author

J. Cramer, Rainer Malik, Stefan Roth, Arthur Liesz, and Jun Yang

Subjects

0301 basic medicine, Weakness, medicine.medical_specialty, medicine.medical_treatment, Immunology, Affect (psychology), Brain Ischemia, 03 medical and health sciences, Behavioral Neuroscience, Mice, 0302 clinical medicine, Physical medicine and rehabilitation, medicine, Animals, Humans, Stroke, Sickness behavior, Depression (differential diagnoses), Illness Behavior, Ischemic Stroke, Rehabilitation, Endocrine and Autonomic Systems, business.industry, Therapeutic effect, medicine.disease, 030104 developmental biology, Anxiety, Cytokines, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Stroke causes severe and long-lasting symptoms in patients. Besides focal deficits such as speech impairment and limb weakness, stroke also results in neuropsychiatric symptoms, including fatigue, anxiety, and depression, which are debilitating and often impair post-stroke rehabilitation. However, in experimental stroke research, the study of neuropsychiatric symptoms and their therapeutic targeting has so far been largely neglected, which can be mainly attributed to the lack of appropriate tools to investigate such deficits in mice. Here, we report that neuropsychiatric symptoms can be differentiated from focal deficits and specifically modulated independent of treating the primary lesion. In order to achieve this, we developed a novel behavior analysis tool by assessing test performance of various tests, combining outcome parameters to cover functional domains of focal and neuropsychiatric symptoms, and finally weighted results into a time point-specific score. This weighted score enabled us to clearly differentiate focal deficits and neuropsychiatric symptoms and detect these until the chronic phase after stroke. Using this analysis tool, we detected that neutralizing systemic cytokines (TNF-α, IL-1β and IL-6) specifically ameliorated neuropsychiatric symptoms but did not affect focal deficits or lesion volume. Hence, most conventional studies analyzing only focal deficits and lesion volume as primary outcome measures would have missed these significant and translationally relevant therapeutic effects. We anticipate that these findings will encourage more detailed analyses of neuropsychiatric symptoms particularly for anti-inflammatory therapies in stroke and that the presented weighted composite score will facilitate this development.

Published

2020

30. Microbiota-derived short chain fatty acids promote Aβ plaque deposition

Author

Rebecca Sadler, Martin Giera, Martin Dichgans, Mercedes Gomez de Agüero, Jochen Herms, Stefan Roth, Christian Haass, Edith Winkler, Alessio Colombo, Finn Peters, Frits Kamp, Andrew J. Macpherson, Laura Sebastian Monasor, Arthur Liesz, Samira Parhizkar, Sabina Tahirovic, Steffanie Heindl, Gemma Llovera, Aswin Verhoeven, Vikramjeet Singh, Corinne Benakis, and Harald Steiner

Subjects

Apolipoprotein E, medicine.medical_specialty, Endocrinology, Downregulation and upregulation, Chemistry, Internal medicine, digestive, oral, and skin physiology, Plasma concentration, medicine, digestive system, Aβ deposition, Gut microbiome

Abstract

Previous studies have identified a crucial role of the gut microbiome in modifying Alzheimer’s disease (AD) progression. However, the mechanisms of microbiome-brain interaction in AD, including the microbial mediators and their cellular targets in the brain, were so far unknown. Here, we identify microbiota-derived short chain fatty acids (SCFA) as key metabolites along the gut-brain axis in AD. Germ-free (GF) AD mice exhibit a substantially reduced Aβ plaque load and markedly reduced SCFA plasma concentrations; conversely, SCFA supplementation to GF AD mice was sufficient to increase the Aβ plaque load to levels of conventionally colonized animals. While Aβ generation was only mildly affected, we observed strong microglial activation and upregulation of ApoE upon the SCFA supplementation. Taken together, our results demonstrate that microbiota-derived SCFA are the key mediators along the gut-brain axis resulting in increased microglial activation, ApoE upregulation and Aβ deposition.

Published

2020

31. Fibrillar Aβ triggers microglial proteome alterations and dysfunction in Alzheimer mouse models

Author

Michael Willem, Jasmin König, Sabina Tahirovic, Matthias Prestel, Stefan Roth, Jochen Herms, Alessio Colombo, Gaye Tanrioever, Anke Piechotta, Stefan F. Lichtenthaler, Laura Sebastian Monasor, Anna Berghofer, Arthur Liesz, Stephan A. Müller, Christian Haass, Takashi Saito, and Takaomi C. Saido

Subjects

Male, 0301 basic medicine, Mouse, Proteome, QH301-705.5, Science, Phagocytosis, microglia, Mice, Transgenic, Biology, General Biochemistry, Genetics and Molecular Biology, neuroinflammation, Amyloid beta-Protein Precursor, Mice, 03 medical and health sciences, 0302 clinical medicine, proteomic signatures, Alzheimer Disease, medicine, Animals, Gene Knock-In Techniques, Functional studies, Biology (General), Neuroinflammation, Amyloid beta-Peptides, General Immunology and Microbiology, Microglia, General Neuroscience, phagocytosis, General Medicine, Alzheimer's disease, Phenotype, Aβ deposition, Tools and Resources, 3. Good health, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Potential biomarkers, Medicine, Female, ddc:600, Neuroscience, 030217 neurology & neurosurgery

Abstract

Microglial dysfunction is a key pathological feature of Alzheimer's disease (AD), but little is known about proteome-wide changes in microglia during the course of AD and their functional consequences. Here, we performed an in-depth and time-resolved proteomic characterization of microglia in two mouse models of amyloid β (Aβ) pathology, the overexpression APPPS1 and the knock-in APP-NL-G-F (APP-KI) model. We identified a large panel of Microglial Aβ Response Proteins (MARPs) that reflect heterogeneity of microglial alterations during early, middle and advanced stages of Aβ deposition and occur earlier in the APPPS1 mice. Strikingly, the kinetic differences in proteomic profiles correlated with the presence of fibrillar Aβ, rather than dystrophic neurites, suggesting that fibrillar Aβ may trigger the AD-associated microglial phenotype and the observed functional decline. The identified microglial proteomic fingerprints of AD provide a valuable resource for functional studies of novel molecular targets and potential biomarkers for monitoring AD progression or therapeutic efficacy., eLife digest Alzheimer’s disease is a progressive, irreversible brain disorder. Patients with Alzheimer’s have problems with memory and other mental skills, which lead to more severe cognitive decline and, eventually, premature death. This is due to increasing numbers of nerve cells in the brain dying over time. A distinctive feature of Alzheimer’s is the abnormally high accumulation of a protein called amyloid-β, which forms distinctive clumps in the brain termed ‘plaques’. The brain has a type of cells called the microglia that identify infections, toxic material and damaged cells, and prevent these from building up by clearing them away. In Alzheimer’s disease, however, the microglia do not work properly, which is thought to contribute to the accumulation of amyloid-β plaques. This means that people with mutations in the genes important for the microglia activity are also at higher risk of developing the disease. Although problems with the microglia play an important role in Alzheimer’s, researchers still do not fully understand why microglia stop working in the first place. It is also not known exactly when and how the microglia change as Alzheimer’s disease progresses. To unravel this mystery, Sebastian Monasor, Müller et al. carried out a detailed study of the molecular ‘fingerprints’ of microglia at each key stage of Alzheimer’s disease. The experiments used microglia cells from two different strains of genetically altered mice, both of which develop the hallmarks of Alzheimer’s disease, including amyloid-β plaques, at similar rates. Analysis of the proteins in microglia cells from both strains revealed distinctive, large-scale changes corresponding to successive stages of the disease – reflecting the gradual accumulation of plaques. Obvious defects in microglia function also appeared soon after plaques started to build up. Microscopy imaging of the brain tissue showed that although amyloid-β plaques appeared at the same time, they looked different in each mouse strain. In one, plaques were more compact, while in the other, plaques appeared ‘fluffier’, like cotton wool. In mice with more compacted plaques, microglia recognized the plaques earlier and stopped working sooner, suggesting that plaque structure and microglia defects could be linked. These results shed new light on the role of microglia and their changing protein ‘signals’ during the different stages of Alzheimer’s disease. In the future, this information could help identify people at risk for the disease, so that they can be treated as soon as possible, and to design new therapies to make microglia work again.

Published

2020

32. Author response: Fibrillar Aβ triggers microglial proteome alterations and dysfunction in Alzheimer mouse models

Author

Anke Piechotta, Michael Willem, Sabina Tahirovic, Takaomi C. Saido, Alessio Colombo, Stefan F. Lichtenthaler, Jasmin König, Anna Berghofer, Jochen Herms, Laura Sebastian Monasor, Gaye Tanrioever, Stefan Roth, Matthias Prestel, Stephan A. Müller, Christian Haass, Takashi Saito, and Arthur Liesz

Subjects

Proteome, Biology, Neuroscience

Published

2020

33. Single-cell profiling of CNS border compartment leukocytes reveals that B cells and their progenitors reside in non-diseased meninges

Author

Thomas Seidenbecher, Sandra Martín-Salamanca, Jan-Kolja Strecker, Xiaolin Li, Jens Minnerup, Arthur Liesz, Michael Heming, Christian Thomas, Sven G. Meuth, Maike Hartlehnert, Anna-Lena Börsch, I-Na Lu, Alessio Ricci, Andrés Hidalgo, David Schafflick, Mathias Pawlak, Jolien Wolbert, Heinz Wiendl, and Gerd Meyer zu Hörste

Subjects

Pathology, medicine.medical_specialty, B-Lymphocytes, Myeloid, General Neuroscience, Dura mater, Precursor Cells, B-Lymphoid, Meninges, Biology, Rats, Mice, medicine.anatomical_structure, Cerebrospinal fluid, medicine, Animals, Choroid plexus, Bone marrow, Single-Cell Analysis, Neuroscience, B cell, Neuroinflammation

Abstract

The CNS is ensheathed by the meninges and cerebrospinal fluid, and recent findings suggest that these CNS-associated border tissues have complex immunological functions. Unlike myeloid lineage cells, lymphocytes in border compartments have yet to be thoroughly characterized. Based on single-cell transcriptomics, we here identified a highly location-specific composition and expression profile of tissue-resident leukocytes in CNS parenchyma, pia-enriched subdural meninges, dura mater, choroid plexus and cerebrospinal fluid. The dura layer of the meninges contained a large population of B cells under homeostatic conditions in mice and rats. Murine dura B cells exhibited slow turnover and long-term tissue residency, and they matured in experimental neuroinflammation. The dura also contained B lineage progenitors at the pro-B cell stage typically not found outside of bone marrow, without direct influx from the periphery or the skull bone marrow. This identified the dura as an unexpected site of B cell residence and potentially of development in both homeostasis and neuroinflammation.

Published

2020

34. Microglia monitor and protect neuronal function through specialized somatic purinergic junctions

Author

Gábor Tamás, István Katona, Katinka Ujvári, Gábor Molnár, Balázs Pósfai, Bernadett Martinecz, Tibor Hortobágyi, Zsuzsanna Környei, Róbert Szipőcs, Barbara Orsolits, Marco Duering, Mária Baranyi, Zsófia Maglóczky, Zsolt Lele, Anett D. Schwarcz, Nikolett Lénárt, Arthur Liesz, Rebeka Fekete, Ferenc Erdélyi, Krisztina Tóth, Adam Denes, Michael M. Tamkun, Eszter Szabadits, Steffanie Heindl, Csaba Cserép, Gábor Szabó, Zsófia I. László, Beáta Sperlágh, László Csiba, and Benno Gesierich

Subjects

Somatic cell, Cell Communication, Biology, Neuroprotection, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, P2Y12, Shab Potassium Channels, medicine, Animals, Humans, 030304 developmental biology, Neurons, 0303 health sciences, Multidisciplinary, Microglia, Purinergic receptor, Brain, Human brain, Purinergic signalling, Receptors, Purinergic P2Y12, Mitochondria, medicine.anatomical_structure, HEK293 Cells, Intercellular Junctions, Brain Injuries, Calcium, Signal transduction, Neuroscience, 030217 neurology & neurosurgery, Signal Transduction

Abstract

Microglia take control Changes in the activity of microglia, the primary immune cells of the central nervous system, are linked with major human diseases, including stroke, epilepsy, psychiatric disorders, and neurodegeneration. Cserép et al. identified a specialized morphofunctional communication site between microglial processes and neuronal cell bodies in the mouse and the human brain (see the Perspective by Nimmerjahn). These junctions are formed at specific areas of the neuronal somatic membranes and possess a distinctive nanoarchitecture and specialized molecular composition linked to mitochondrial signaling. The junctions appear to provide a major site for microglia-neuron communication and may help to mediate the neuroprotective effects of microglia after acute brain injury. Science , this issue p. 528 ; see also p. 510

Published

2020

35. Panoptic imaging of transparent mice reveals whole-body neuronal projections and skull–meninges connections

Author

Arthur Liesz, Shan Zhao, Martin Kerschensteiner, Chenchen Pan, Hanno Steinke, Arnaldo Parra-Damas, Ruiyao Cai, Corinne Benakis, Markus Rempfler, Ali Ertürk, Mihail Ivilinov Todorov, Harsharan S. Bhatia, Sabine Liebscher, Anna L.R. Xavier, Bjoern H. Menze, Benjamin T. Kress, Benjamin Förstera, Delphine Theodorou, Ingo Bechmann, Leander Mrowka, and Alireza Ghasemigharagoz

Subjects

0301 basic medicine, Nervous system, Mice, Transgenic, Biology, Article, Mice, 03 medical and health sciences, Immunolabeling, Meninges, 0302 clinical medicine, Peripheral nerve, Brain meninges, medicine, Animals, Whole Body Imaging, Rest (music), Neurons, General Neuroscience, Skull, 030104 developmental biology, medicine.anatomical_structure, Whole body, Neuroscience, 030217 neurology & neurosurgery

Abstract

Analysis of entire transparent rodent bodies after clearing could provide holistic biological information in health and disease, but reliable imaging and quantification of fluorescent protein signals deep inside the tissues has remained a challenge. Here, we developed vDISCO, a pressure-driven, nanobody-based whole-body immunolabeling technology to enhance the signal of fluorescent proteins by up to two orders of magnitude. This allowed us to image and quantify subcellular details through bones, skin and highly autofluorescent tissues of intact transparent mice. For the first time, we visualized whole-body neuronal projections in adult mice. We assessed CNS trauma effects in the whole body and found degeneration of peripheral nerve terminals in the torso. Furthermore, vDISCO revealed short vascular connections between skull marrow and brain meninges, which were filled with immune cells upon stroke. Thus, our new approach enables unbiased comprehensive studies of the interactions between the nervous system and the rest of the body.

Published

2018

36. <scp>CCL</scp>23: a new<scp>CC</scp>chemokine involved in human brain damage

Author

Alejandro Bustamante, Arthur Liesz, Dolors Giralt, Gemma Llovera, Joan Montaner, X Wang, Y Jiang, Laura Ramiro, Anna Rosell, Elena Martínez-Sáez, Francesc Canals, Alba Simats, Teresa García-Berrocoso, and Anna Penalba

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Neutrophils, Ischemia, Inflammation, Brain damage, Gastroenterology, CCL6, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Internal Medicine, medicine, Animals, Humans, Rats, Wistar, Stroke, Aged, Aged, 80 and over, Neurons, business.industry, Human brain, Macrophage Inflammatory Proteins, Prognosis, medicine.disease, Up-Regulation, Mice, Inbred C57BL, Disease Models, Animal, Early Diagnosis, 030104 developmental biology, medicine.anatomical_structure, Case-Control Studies, Chemokines, CC, Biomarker (medicine), Female, Chemokines, medicine.symptom, business, CCL23, Biomarkers, 030217 neurology & neurosurgery, Follow-Up Studies

Abstract

BACKGROUND CCL23 role in the inflammatory response after acute brain injuries remains elusive. Here, we evaluated whether CCL23 blood levels associate with acquired cerebral lesions and determined CCL23 predictive capacity for assessing stroke prognosis. We used preclinical models to study the CCL23 homologous chemokines in rodents, CCL9 and CCL6. METHODS Baseline CCL23 blood levels were determined on 245 individuals, including ischaemic strokes (IS), stroke mimics and controls. Temporal profile of circulating CCL23 was explored from baseline to 24 h in 20 of the IS. In an independent cohort of 120 IS with a 3-month follow-up, CCL23 blood levels were included in logistic regression models to predict IS outcome. CCL9/CCL6 cerebral expression was evaluated in rodent models of brain damage. Both chemokines were also profiled in circulation and histologically located on brain following ischaemia. RESULTS Baseline CCL23 blood levels did not discriminate IS, but permitted an accurate discrimination of patients presenting acute brain lesions (P = 0.003). IS exhibited a continuous increase from baseline to 24 h in circulating CCL23 (P

Published

2018

37. A macrophage-T cell coculture model for severe tissue injury-induced T cell death

Author

Jiayu Cao, Arthur Liesz, Stefan Roth, and Jie Zhu

Subjects

Male, Science (General), Inflammasomes, T-Lymphocytes, T cell, Immunology, General Biochemistry, Genetics and Molecular Biology, Q1-390, Mice, 03 medical and health sciences, 0302 clinical medicine, Health Sciences, Protocol, medicine, Animals, Macrophage, 030304 developmental biology, 0303 health sciences, Cell Death, General Immunology and Microbiology, Chemistry, Macrophages, General Neuroscience, Models, Immunological, Cell Biology, Coculture Techniques, 3. Good health, Mice, Inbred C57BL, medicine.anatomical_structure, Cell isolation, Cancer research, Wounds and Injuries, Female, Cell culture, Spleen, 030217 neurology & neurosurgery

Abstract

Summary A key observation of tissue injury, such as stroke and burn, is a state of systemic immunosuppression characterized by loss of T cells and rise of infections. Here, we present an in vitro model for cell-cell interactions between innate (macrophages) and adaptive (T cells) immune cells. This protocol facilitates bone marrow-derived macrophages (BMDMs) and splenic T cells in a coculture model. The procedure mimics injury-induced T cell death, which is driven by inflammasome activation in macrophages. For complete details on the use and execution of this protocol, please refer to Roth et al. (2021)., Graphical abstract, Highlights • Coculture model of murine bone marrow-derived macrophages and splenic T cells • Modeling immune cell-cell interactions between innate and lymphoid immune cells • Analysis of cell death receptor-ligand interactions between macrophages and T cells • Serum from mice with severe tissue injury as initial stimulus for the coculture, A key observation of tissue injury, such as stroke and burn, is a state of systemic immunosuppression characterized by loss of T cells and rise of infections. Here, we present an in vitro model for cell-cell interactions between innate (macrophages) and adaptive (T cells) immune cells. This protocol facilitates bone marrow-derived macrophages (BMDMs) and splenic T cells in a coculture model. The procedure mimics injury-induced T cell death, which is driven by inflammasome activation in macrophages.

Published

2021

38. Microbiota differences between commercial breeders impacts the post-stroke immune response

Author

David Brea, Josef Anrather, Rebecca Sadler, Arthur Liesz, Bärbel Stecher, Corinne Benakis, Vikramjeet Singh, and Debora Garzetti

Subjects

Male, 0301 basic medicine, T-Lymphocytes, T cell, Segmented filamentous bacteria, Immunology, Population, Gut flora, Lymphocyte Activation, 03 medical and health sciences, Behavioral Neuroscience, 0302 clinical medicine, Immune system, CD28 Antigens, medicine, Animals, education, Stroke, Neuroinflammation, education.field_of_study, biology, Endocrine and Autonomic Systems, Reproducibility of Results, CD28, medicine.disease, biology.organism_classification, Gastrointestinal Microbiome, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Encephalitis, Female, Immunotherapy, 030217 neurology & neurosurgery

Abstract

Experimental reproducibility between laboratories is a major translational obstacle worldwide, particularly in studies investigating immunomodulatory therapies in relation to brain disease. In recent years increasing attention has been drawn towards the gut microbiota as a key factor in immune cell polarization. Moreover, manipulation of the gut microbiota has been found effective in a diverse range of brain disorders. Within this study we aimed to test the impact of microbiota differences between mice from different sources on the post-stroke neuroinflammatory response. With this rationale, we have investigated the correlation between microbiota differences and the immune response in mice from three commercial breeders with the same genetic background (C57BL/6). While overall bacterial load was comparable, we detected substantial differences in species diversity and microbiota composition on lower taxonomic levels. Specifically, we investigated segmented filamentous bacteria (SFB)-which have been shown to promote T cell polarization-and found that they were absent in mice from one breeder but abundant in others. Our experiments revealed a breeder specific correlation between SFB presence and the ratio of Treg to Th17 cells. Moreover, recolonization of SFB-negative mice with SFB resulted in a T cell shift which mimicked the ratios found in SFB-positive mice. We then investigated the response to a known experimental immunotherapeutic approach, CD28 superagonist (CD28SA), which has been previously shown to expand the Treg population. CD28SA treatment had differing effects between mice from different breeders and was found to be ineffective at inducing Treg expansion in SFB-free mice. These changes directly corresponded to stroke outcome as mice lacking SFB had significantly larger brain infarcts. This study demonstrates the major impact of microbiota differences on T cell polarization in mice during ischemic stroke conditions, and following immunomodulatory therapies.

Published

2017

39. Microglia monitor and protect neuronal function via specialized somatic purinergic junctions

Author

Adam Denes, Bernadett Martinecz, István Katona, Steffanie Heindl, Balázs Pósfai, Róbert Szipőcs, Marco Duering, Arthur Liesz, Barbara Orsolits, László Csiba, Zsolt Lele, Katinka Ujvári, Anett D. Schwarcz, Csaba Cserép, Ferenc Erdélyi, Rebeka Fekete, Benno Gesierich, Gábor Molnár, Gábor Tamás, Tibor Hortobágyi, Zsófia I. László, Zsófia Maglóczky, Gábor Szabó, and Nikolett Lénárt

Subjects

0303 health sciences, Microglia, Somatic cell, Purinergic receptor, Human brain, Purinergic signalling, Biology, Mitochondrion, Neuroprotection, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, nervous system, medicine, Neuroscience, 030217 neurology & neurosurgery, Homeostasis, 030304 developmental biology

Abstract

Microglia are the main immune cells in the brain with emerging roles in brain homeostasis and neurological diseases, while mechanisms underlying microglia-neuron communication remain elusive. Here, we identify a novel site of interaction between neuronal cell bodies and microglial processes in mouse and human brain. Somatic microglia-neuron junctions possess specialized nanoarchitecture optimized for purinergic signaling. Activity of neuronal mitochondria is linked with microglial junction formation, which is rapidly induced in response to neuronal activation and blocked by inhibition of P2Y12-receptors (P2Y12R). Brain injury-induced changes at somatic junctions trigger P2Y12R-dependent microglial neuroprotection, regulating neuronal calcium load and functional connectivity. Collectively, our results suggest that microglial processes at these junctions are in ideal position to monitor and protect neuronal functions in both the healthy and injured brain.One-sentence summaryNeuronal cell bodies possess specialized, pre-formed sites, through which microglia monitor their status and exert neuroprotection.

Published

2019

40. Young microglia restore amyloid plaque clearance of aged microglia

Author

Michael Willem, Christian Haass, Anna Daria, Arthur Liesz, Sabina Tahirovic, Gemma Llovera, Heike Hampel, and Alessio Colombo

Subjects

0301 basic medicine, Amyloid, Phagocytosis, metabolism [Microglia], Biology, General Biochemistry, Genetics and Molecular Biology, pathology [Alzheimer Disease], Mice, 03 medical and health sciences, Organ Culture Techniques, 0302 clinical medicine, pathology [Brain], ddc:570, medicine, Conditioned medium, Animals, Molecular Biology, Neuroinflammation, Cell Proliferation, General Immunology and Microbiology, Microglia, Cell growth, General Neuroscience, Neurodegeneration, medicine.disease, Coculture Techniques, metabolism [Plaque, Amyloid], physiology [Microglia], Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Culture Media, Conditioned, Immunology, Alzheimer's disease, 030217 neurology & neurosurgery

Abstract

Alzheimer′s disease (AD) is characterized by deposition of amyloid plaques, neurofibrillary tangles, and neuroinflammation. In order to study microglial contribution to amyloid plaque phagocytosis, we developed a novel ex vivo model by co‐culturing organotypic brain slices from up to 20‐month‐old, amyloid‐bearing AD mouse model (APPPS1) and young, neonatal wild‐type (WT) mice. Surprisingly, co‐culturing resulted in proliferation, recruitment, and clustering of old microglial cells around amyloid plaques and clearance of the plaque halo. Depletion of either old or young microglial cells prevented amyloid plaque clearance, indicating a synergistic effect of both populations. Exposing old microglial cells to conditioned media of young microglia or addition of granulocyte‐macrophage colony‐stimulating factor (GM‐CSF) was sufficient to induce microglial proliferation and reduce amyloid plaque size. Our data suggest that microglial dysfunction in AD may be reversible and their phagocytic ability can be modulated to limit amyloid accumulation. This novel ex vivo model provides a valuable system for identification, screening, and testing of compounds aimed to therapeutically reinforce microglial phagocytosis. ![][1] Phagocytic function of aged microglial cells in amyloid plaque‐bearing tissue is not irreversibly impaired, but can be restored through factors secreted by young microglia. Microglia function in Aβ clearance and reducing the amyloid burden highlights the need for development of therapeutic approaches modulating microglial activity. [1]: /embed/graphic-1.gif

Published

2016

41. Interfering with the Chronic Immune Response Rescues Chronic Degeneration After Traumatic Brain Injury

Author

Karpagam Srinivasan, Maj Hedehus, Sara L. Dominguez, Arthur Liesz, Susanne Mentz, Kimberly Scearce-Levie, Morgan Sheng, David V. Hansen, Ali Ertürk, Lisa Neumaier, Erik E Stout, Franziska Krammer, and Gemma Llovera

Subjects

Male, 0301 basic medicine, Time Factors, Traumatic brain injury, Dendritic Spines, CX3C Chemokine Receptor 1, Mice, Transgenic, Inflammation, Brain damage, Motor Activity, Bioinformatics, Mice, 03 medical and health sciences, Epilepsy, 0302 clinical medicine, Brain Injuries, Traumatic, CX3CR1, medicine, Animals, Dementia, Neuroinflammation, Neurons, business.industry, General Neuroscience, Calcium-Binding Proteins, Microfilament Proteins, Neurodegeneration, Brain, Recovery of Function, Articles, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Chronic Disease, Nerve Degeneration, Exploratory Behavior, Female, Receptors, Chemokine, medicine.symptom, business, Neuroscience, Psychomotor Performance, 030217 neurology & neurosurgery

Abstract

After traumatic brain injury (TBI), neurons surviving the initial insult can undergo chronic (secondary) degeneration via poorly understood mechanisms, resulting in long-term cognitive impairment. Although a neuroinflammatory response is promptly activated after TBI, it is unknown whether it has a significant role in chronic phases of TBI (>1 year after injury). Using a closed-head injury model of TBI in mice, we showed by MRI scans that TBI caused substantial degeneration at the lesion site within a few weeks and these did not expand significantly thereafter. However, chronic alterations in neurons were observed, with reduced dendritic spine density lasting >1 year after injury. In parallel, we found a long-lasting inflammatory response throughout the entire brain. Deletion of one allele of CX3CR1, a chemokine receptor, limited infiltration of peripheral immune cells and largely prevented the chronic degeneration of the injured brain and provided a better functional recovery in female, but not male, mice. Therefore, targeting persistent neuroinflammation presents a new therapeutic option to reduce chronic neurodegeneration.SIGNIFICANCE STATEMENTTraumatic brain injury (TBI) often causes chronic neurological problems including epilepsy, neuropsychiatric disorders, and dementia through unknown mechanisms. Our study demonstrates that inflammatory cells invading the brain lead to secondary brain damage. Sex-specific amelioration of chronic neuroinflammation rescues the brain degeneration and results in improved motor functions. Therefore, this study pinpoints an effective therapeutic approach to preventing secondary complications after TBI.

Published

2016

42. Inadequate food and water intake determine mortality following stroke in mice

Author

Joshua Shrouder, Uta Mamrak, Stefan Roth, Athanasios Lourbopoulos, Matilde Balbi, Arthur Liesz, Nikolaus Plesnila, and Farida Hellal

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Drinking, Hypoglycemia, Neuroprotection, Eating, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine.artery, medicine, Animals, Water intake, Stroke, Survival analysis, Nutritional Support, business.industry, Mortality rate, Original Articles, medicine.disease, Infarct size, Survival Analysis, Surgery, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Neurology, Middle cerebral artery, Cardiology, Neurology (clinical), Cardiology and Cardiovascular Medicine, business, 030217 neurology & neurosurgery

Abstract

Experimental stroke models producing clinically relevant functional deficits are often associated with high mortality. Because the mechanisms that underlie post-stroke mortality are largely unknown, results obtained using these models are often difficult to interpret, thereby limiting their translational potential. Given that specific forms of post-stroke care reduce mortality in patients, we hypothesized that inadequate food and water intake may underlie mortality following experimental stroke. C57BL/6 mice were subjected to 1 h of intraluminal filament middle cerebral artery occlusion. Nutritional support beginning on the second day after filament middle cerebral artery occlusion reduced the 14-day mortality rate from 59% to 15%. The surviving mice in the post-stroke support group had the same infarct size as non-surviving control mice, suggesting that post-stroke care was not neuroprotective and that inadequate food and/or water intake are the main reasons for filament middle cerebral artery occlusion–induced mortality. This notion was supported by the presence of significant hypoglycemia, ketonemia, and dehydration in control mice. Taken together, these data suggest that post–filament middle cerebral artery occlusion mortality in mice is not primarily caused by ischemic brain damage, but secondarily by inadequate food and/or water intake. Thus, providing nutritional support following filament middle cerebral artery occlusion greatly minimizes mortality bias and allows the study of long-term morphological and functional sequelae of stroke in mice.

Published

2016

43. Panoptic vDISCO imaging reveals neuronal connectivity, remote trauma effects and meningeal vessels in intact transparent mice

Author

Markus Rempfler, Arthur Liesz, Shan Zhao, Martin Kerschensteiner, Anna L.R. Xavier, Harsharan S. Bhatia, Bjoern H. Menze, Foerstera B, Benjamin T. Kress, Corinne Benakis, Ali Ertürk, Leander Mrowka, Ruiyao Cai, Mihail Ivilinov Todorov, Chenchen Pan, Alireza Ghasemigharagoz, M. Nedergaard, and Delphine Theodorou

Subjects

Nervous system, Immunolabeling, Skull, medicine.anatomical_structure, Meningeal lymphatic vessels, medicine, Biology, Brain trauma, Neuroscience, Clearance

Abstract

Analysis of entire transparent rodent bodies could provide holistic information on biological systems in health and disease. However, it has been challenging to reliably image and quantify signal from endogenously expressed fluorescent proteins in large cleared mouse bodies due to the low signal contrast. Here, we devised a pressure driven, nanobody based whole-body immunolabeling technology to enhance the signal of fluorescent proteins by up to two orders of magnitude. This allowed us to image subcellular details in transparent mouse bodies through bones and highly autofluorescent tissues, and perform quantifications. We visualized for the first-time whole-body neuronal connectivity of an entire adult mouse and discovered that brain trauma induces degeneration of peripheral axons. We also imaged meningeal lymphatic vessels and immune cells through the intact skull and vertebra in naive animals and trauma models. Thus, our new approach can provide an unbiased holistic view of biological events affecting the nervous system and the rest of the body.

Published

2018

44. The gut microbiome primes a cerebroprotective immune response after stroke

Author

Rebecca Sadler, Steffanie Heindl, Corinne Benakis, Arthur Liesz, Vikramjeet Singh, Stefan Roth, and Gemma Llovera

Subjects

0301 basic medicine, T-Lymphocytes, Brief Communication, 03 medical and health sciences, Mice, 0302 clinical medicine, Bacterial colonization, Immune system, Stroke outcome, medicine, Animals, Microbiome, cardiovascular diseases, Stroke, Neuroinflammation, Inflammation, Microglia, business.industry, Immunity, Protective Factors, medicine.disease, Gut microbiome, Neuroprotection, Gastrointestinal Microbiome, 030104 developmental biology, medicine.anatomical_structure, Neurology, Immunology, Neurology (clinical), Cardiology and Cardiovascular Medicine, business, 030217 neurology & neurosurgery

Abstract

Microbiome alterations have been shown to affect stroke outcome. However, to what extent the presence of a gut microbiome per se is affecting post-stroke neuroinflammation has not been tested. By comparing germfree mice with recolonized (Ex-GF) and conventional SPF mice, we were able to demonstrate that bacterial colonization reduces stroke volumes. Bacterial colonization increased cerebral expression of cytokines as well as microglia/macrophage cell counts in contrast to improved stroke outcome. Interestingly, the microbiome-mediated brain protection was absent in lymphocyte-deficient mice. These findings support the concept of lymphocyte-driven protective neuroinflammation after stroke under control of the microbiome.

Published

2018

45. Brain-released alarmins and stress response synergize in accelerating atherosclerosis progression after stroke

Author

Marco Bianchi, Maxime Gauberti, Stefan Roth, Antoine P. Fournier, Arthur Liesz, Britta Engelhardt, Lesca M. Holdt, Christof Haffner, Steffen Tiedt, Arie Geerlof, Denis Vivien, Vikramjeet Singh, Lisa Schindler, Helena Erlandsson Harris, Jürgen Bernhagen, Martin Dichgans, Daniel J. Antoine, Georg Huber, Antoine Anfray, Cyrille Orset, Roth, Stefan, Singh, Vikramjeet, Tiedt, Steffen, Schindler, Lisa, Huber, Georg, Geerlof, Arie, Antoine, Daniel J., Anfray, Antoine, Orset, Cyrille, Gauberti, Maxime, Fournier, Antoine, Holdt, Lesca M., Harris, Helena Erlandsson, Engelhardt, Britta, Bianchi, Marco E., Vivien, Deni, Haffner, Christof, Bernhagen, Jürgen, Dichgans, Martin, and Liesz, Arthur

Subjects

0301 basic medicine, Inflammation, RAGE (receptor), Endothelial activation, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Glycation, medicine, Alarmins, Animals, 610 Medicine & health, Receptor, Stroke, Medicine (all), Monocyte, Brain, General Medicine, Atherosclerosis, medicine.disease, Immunity, Innate, Plaque, Atherosclerotic, 030104 developmental biology, medicine.anatomical_structure, Cancer research, 570 Life sciences, biology, medicine.symptom, 030217 neurology & neurosurgery

Abstract

Stroke induces a multiphasic systemic immune response, but the consequences of this response on atherosclerosis-a major source of recurrent vascular events-have not been thoroughly investigated. We show that stroke exacerbates atheroprogression via alarmin-mediated propagation of vascular inflammation. The prototypic brain-released alarmin high-mobility group box 1 protein induced monocyte and endothelial activation via the receptor for advanced glycation end products (RAGE)-signaling cascade and increased plaque load and vulnerability. Recruitment of activated monocytes via the CC-chemokine ligand 2-CC-chemokine receptor type 2 pathway was critical in stroke-induced vascular inflammation. Neutralization of circulating alarmins or knockdown of RAGE attenuated atheroprogression. Blockage of. 3-adrenoreceptors attenuated the egress of myeloid monocytes after stroke, whereas neutralization of circulating alarmins was required to reduce systemic monocyte activation and aortic invasion. Our findings identify a synergistic effect of the sympathetic stress response and alarmin-driven inflammation via RAGE as a critical mechanism of exacerbated atheroprogression after stroke.

Published

2018

46. Abstract TP259: Tryptophan Metabolism Affects the Intestinal Immune Response After Stroke

Author

Rebecca Sadler, Corinne Benakis, Stefan Roth, Vikramjeet Singh, and Arthur Liesz

Subjects

Advanced and Specialized Nursing, medicine.medical_specialty, biology, business.industry, Metabolite, Cell, Aryl hydrocarbon receptor, Small intestine, chemistry.chemical_compound, Immune system, Endocrinology, medicine.anatomical_structure, Integrin alpha M, chemistry, Downregulation and upregulation, Internal medicine, medicine, biology.protein, Neurology (clinical), Cardiology and Cardiovascular Medicine, business, Kynurenine

Abstract

Introduction: The gut microbiota influences the severity of brain injury through regulation of intestinal immune homeostasis. However, molecular cues involved in microbiota-immune interaction after stroke are unknown. Metabolites have a pivotal role in connecting commensals to the immune response. Specifically, bacteria-derived metabolites of tryptophan catabolism activate the transcription factor aryl hydrocarbon receptor (AhR) which regulates T cell polarization directly or via tolerogenic function of dendritic cells (DCs). Hypothesis: Since adaptive immune cells are involved in stroke, we hypothesize that modulation of tryptophan metabolism–orchestrated by bacteria–modifies T cell differentiation and influences stroke outcome. Methods: Stroke is induced by the occlusion of the middle cerebral artery (MCAO) in C57BL6 mice. Blood and the distal small intestine are sampled for the detection of tryptophan metabolites and quantified by metagenomics or mRNA expression. Immune cells are isolated from the intestine and analyzed by flow cytometry. Stroke outcome is measured by infarct volumetry and behaviour tests. Results: Tryptophan catabolism was augmented in mice subjected to stroke-induced dysbiosis–shown by a) an increase of the most proximal metabolite kynurenine and a concomitant decrease of tryptophan and b) an upregulation of mRNA expression of the rate-limiting enzyme involved in tryptophan’s breakdown. This was paralleled by an increase of AhR mRNA in the ileum after MCAO. To test the implication of AhR on the tolerogenic function of DCs, we used AhR-DCs knock-out mice. We found that CD103+CD11b+ DCs lacking AhR were downregulated after stroke compared to wild-type (WT) mice. Interestingly, polarization state of T cells was modified in DCs lacking AhR (regulatory versus Th17 cell ratio). This could influence the central nervous system immune response and induce protection after stroke, as suggested by a reduction of infarct volume observed 3 days after stroke in AhR-DCs knock-out mice compared to WT mice. Conclusion: These findings suggest that stroke-induced dysbiosis leads to an increase of tryptophan catabolism, and that AhR depletion in DCs influences immune cell polarization and stroke outcome.

Published

2018

47. Acquired Immunoglobulin G deficiency in stroke patients and experimental brain ischemia

Author

Kerstin Hofmann, Roland Veltkamp, Stefan Roth, Markus Zorn, Arthur Liesz, and Li Sun

Subjects

Male, Pathology, medicine.medical_specialty, Time Factors, medicine.medical_treatment, Sensitivity and Specificity, Severity of Illness Index, Statistics, Nonparametric, Transient Hypogammaglobulinemia, Brain ischemia, Hypogammaglobulinemia, Excretion, Mice, Developmental Neuroscience, medicine, Animals, Humans, Biotinylation, IgG Deficiency, Stroke, Aged, Analysis of Variance, biology, business.industry, Immunosuppression, Middle Aged, medicine.disease, Disease Models, Animal, Neurology, Ischemic Attack, Transient, Brain Injuries, Immunoglobulin G, Luminescent Measurements, Immunology, biology.protein, Female, IgG deficiency, Antibody, business

Abstract

Background and purpose Acute brain injuries induce a systemic immune depression syndrome (SIDS) that predisposes patients to bacterial infections. While cellular compartments of this syndrome have been well characterized, the contribution of humoral immune mechanisms and particularly immunoglobulins to SIDS has not been investigated so far. Methods We determined serum immunoglobulin levels and infectious complications at several time points in 159 ischemic and hemorrhagic stroke patients. Additionally, findings were verified in a transient middle cerebral artery occlusion model. A novel immunoassay was established to analyze the IgG excretion ratio in mice. Results We identified a transient IgG reduction in patients suffering from substantial ischemic or hemorrhagic brain injuries. The IgG-reduction was associated with subsequent bacterial infections. Similarly, transient hypogammaglobulinemia was detected in a murine stroke model. We then used this animal model to further distinguish the mechanism of the IgG reduction by an IgG transfer paradigm. Excretional loss rather than deficient production of IgG was demonstrated to underlay hypogammaglobulinemia. Conclusions This is the first report of transient hypogammaglobulinemia after ischemic and hemorrhagic stroke suggesting involvement in infectious complications. These findings pave the road for further studies investigating post-stroke hypogammaglobulinemia as a druggable target for stroke-induced complications.

Published

2015

48. Amplification of Regulatory T Cells Using a CD28 Superagonist Reduces Brain Damage After Ischemic Stroke in Mice

Author

Thomas Hünig, Roland Veltkamp, Arthur Liesz, Shin-Young Na, and Eva Mracsko

Subjects

Advanced and Specialized Nursing, Pathology, medicine.medical_specialty, business.industry, Ischemia, CD28, Spleen, Brain damage, medicine.disease, Brain ischemia, medicine.anatomical_structure, medicine.artery, Middle cerebral artery, Medicine, Immunohistochemistry, Neurology (clinical), medicine.symptom, Cardiology and Cardiovascular Medicine, business, Stroke

Abstract

Background and Purpose— Neuroinflammation plays an important role in ischemic brain injury. Regulatory T cells (Treg) are important endogenous immune modulators. We tested the hypothesis that Treg amplification with a CD28 superagonistic monoclonal antibody (CD28SA) reduces brain damage in murine cerebral ischemia. Methods— Cerebral ischemia was induced by coagulation of the distal middle cerebral artery or by 60 minutes filament occlusion of the proximal middle cerebral artery in C57BL6 mice. 150 μg CD28SA was injected intraperitoneally 3 or 6 hours after ischemia onset. Outcome was determined by infarct volumetry and behavioral testing. Brain-infiltrating leukocyte subpopulations were analyzed by flow cytometry and immunohistochemistry 3 and 7 days after middle cerebral artery occlusion. Results— CD28SA reduced infarct size in both models and attenuated functional deficit 7 days after stroke induction. Mice treated with CD28SA increased numbers of Treg in spleen and brain. Tregs were functionally active and migrated into the brain where they accumulated and proliferated in the peri-infarct area. More than 60% of brain infiltrating Treg produced interleukin-10 in CD28SA compared with 30% in control. Conclusions— In vivo expansion and amplification of Treg by CD28SA attenuates the inflammatory response and improves outcome after experimental stroke.

Published

2015

49. The Role of T Cells in Post-stroke Regeneration

Author

J. Cramer and Arthur Liesz

Subjects

business.industry, T cell, Lymphocyte, Regeneration (biology), Neurogenesis, medicine.disease, Acquired immune system, Brain ischemia, medicine.anatomical_structure, Neuroimmunology, Immune system, Medicine, business, Neuroscience

Abstract

The interaction of the immune system with the brain is necessary for development and surveillance of the healthy brain. The influence of the adaptive immune system on several brain diseases has been described in great detail. In ischemic stroke, a growing body of evidence has demonstrated a key role for T cells in the acute phase after stroke. Pro- and anti-inflammatory T cell subpopulations impact in this early phase the inflammatory milieu and directly affect secondary lesion progression and neuronal injury. Recently, a functional role for T cells has also become more evident also in delayed neuronal (dys-)function and late-phase recovery after stroke. Here, T cells may also affect various non-immunological pathways involved in tissue repair, neuronal plasticity and functional recovery. These pleiotropic effects of T cells on mechanisms such as neurogenesis and angiogenesis suggest T cells as potential therapeutic target to modulate post-stroke regeneration. This chapter will provide a comprehensive overview of the current knowledge about the role of T cells in stroke with a particular focus on regenerative processes in the chronic phase.

Published

2017

50. RNA-Seq Identifies Circulating miR-125a-5p, miR-125b-5p, and miR-143-3p as Potential Biomarkers for Acute Ischemic Stroke

Author

Steffen Tiedt, Franziska Dorn, Rainer Malik, Nikolaus Plesnila, Martin Dichgans, Knut Krohn, Nicola Schieferdecker, Lesca M. Holdt, Julia Böck, Marco Duering, Veronika Kautzky, Matthias Prestel, Bernd H. Northoff, Matthias Klein, Arthur Liesz, Ivelina Stoycheva, and Daniel Teupser

Subjects

0301 basic medicine, Oncology, Male, Pathology, Time Factors, Physiology, law.invention, Brain Ischemia, 0302 clinical medicine, law, Stroke, Polymerase chain reaction, Aged, 80 and over, biology, Area under the curve, Middle Aged, Prognosis, 3. Good health, Area Under Curve, Female, medicine.symptom, Cardiology and Cardiovascular Medicine, Genetic Markers, medicine.medical_specialty, Enolase, Real-Time Polymerase Chain Reaction, 03 medical and health sciences, Predictive Value of Tests, Internal medicine, microRNA, medicine, Humans, Interleukin 6, Aged, business.industry, Interleukin-6, Sequence Analysis, RNA, Reproducibility of Results, Hypoxia (medical), medicine.disease, Circulating MicroRNA, MicroRNAs, 030104 developmental biology, Early Diagnosis, ROC Curve, Case-Control Studies, Phosphopyruvate Hydratase, biology.protein, business, Tomography, X-Ray Computed, 030217 neurology & neurosurgery

Abstract

Rationale: Currently, there are no blood-based biomarkers with clinical utility for acute ischemic stroke (IS). MicroRNAs show promise as disease markers because of their cell type–specific expression patterns and stability in peripheral blood. Objective: To identify circulating microRNAs associated with acute IS, determine their temporal course up to 90 days post-stroke, and explore their utility as an early diagnostic marker. Methods and Results: We used RNA sequencing to study expression changes of circulating microRNAs in a discovery sample of 20 patients with IS and 20 matched healthy control subjects. We further applied quantitative real-time polymerase chain reaction in independent samples for validation (40 patients with IS and 40 matched controls), replication (200 patients with IS, 100 healthy control subjects), and in 72 patients with transient ischemic attacks. Sampling of patient plasma was done immediately upon hospital arrival. We identified, validated, and replicated 3 differentially expressed microRNAs, which were upregulated in patients with IS compared with both healthy control subjects (miR-125a-5p [1.8-fold; P =1.5×10 −6 ], miR-125b-5p [2.5-fold; P =5.6×10 −6 ], and miR-143-3p [4.8-fold; P =7.8×10 −9 ]) and patients with transient ischemic attack (miR-125a-5p: P =0.003; miR-125b-5p: P =0.003; miR-143-3p: P =0.005). Longitudinal analysis of expression levels up to 90 days after stroke revealed a normalization to control levels for miR-125b-5p and miR-143-3p starting at day 2 while miR-125a-5p remained elevated. Levels of all 3 microRNAs depended on platelet numbers in a platelet spike-in experiment but were unaffected by chemical hypoxia in Neuro2a cells and in experimental stroke models. In a random forest classification, miR-125a-5p, miR-125b-5p, and miR-143-3p differentiated between healthy control subjects and patients with IS with an area under the curve of 0.90 (sensitivity: 85.6%; specificity: 76.3%), which was superior to multimodal cranial computed tomography obtained for routine diagnostics (sensitivity: 72.5%) and previously reported biomarkers of acute IS (neuron-specific enolase: area under the curve=0.69; interleukin 6: area under the curve=0.82). Conclusions: A set of circulating microRNAs (miR-125a-5p, miR-125b-5p, and miR-143-3p) associates with acute IS and might have clinical utility as an early diagnostic marker.

Published

2017