21 results on '"Carolin Stump-Guthier"'
Search Results
2. The phosphoproteome of choroid plexus epithelial cells following infection with Neisseria meningitidis
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Rosanna Herold, Lea Denzer, Walter Muranyi, Carolin Stump-Guthier, Hiroshi Ishikawa, Horst Schroten, and Christian Schwerk
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blood-cerebrospinal fluid barrier ,host innate signaling ,host pathogen interaction ,phosphoproteome ,meningitis ,Neisseria meningitidis ,Microbiology ,QR1-502 - Abstract
The Gram-negative bacterium Neisseria meningitidis, which causes meningitis in humans, has been demonstrated to manipulate or alter host signalling pathways during infection of the central nervous system (CNS). However, these complex signalling networks are not completely understood. We investigate the phosphoproteome of an in vitro model of the blood-cerebrospinal fluid barrier (BCSFB) based on human epithelial choroid plexus (CP) papilloma (HIBCPP) cells during infection with the N. meningitidis serogroup B strain MC58 in presence and absence of the bacterial capsule. Interestingly, our data demonstrates a stronger impact on the phosphoproteome of the cells by the capsule-deficient mutant of MC58. Using enrichment analyses, potential pathways, molecular processes, biological processes, cellular components and kinases were determined to be regulated as a consequence of N. meningitidis infection of the BCSFB. Our data highlight a variety of protein regulations that are altered during infection of CP epithelial cells with N. meningitidis, with the regulation of several pathways and molecular events only being detected after infection with the capsule-deficient mutant. Mass spectrometry proteomics data are available via ProteomeXchange with identifier PXD038560.
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- 2023
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3. Protocol for the setup and use of a human choroid plexus endothelial-epithelial two-cell-type in vitro model
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Rosanna Herold, Julia Borkowski, Christian Schwerk, Carolin Stump-Guthier, Marko Lampe, Hiroshi Ishikawa, Walter Muranyi, and Horst Schroten
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Cell biology ,Cell culture ,Molecular biology ,Neuroscience ,Science (General) ,Q1-390 - Abstract
Summary: Choroid plexus, located in brain ventricles, is the site of blood-cerebrospinal fluid barrier that contains endothelial cells and an epithelial monolayer separated by stroma. We established a two-cell-type model of the human choroid plexus consisting of immortalized endothelial cells (iHCPEnC) and epithelial papilloma (HIBCPP) cells grown on opposite sides of filter supports. In this protocol, we describe the preparation of this model, the measurement of transepithelial electrical resistance (TEER), and immunofluorescence imaging-based analysis to determine the barrier function.For complete details on the use and execution of this protocol, please refer to Muranyi et al. (2022). : Publisher’s note: Undertaking any experimental protocol requires adherence to local institutional guidelines for laboratory safety and ethics.
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- 2022
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4. Immortalized human choroid plexus endothelial cells enable an advanced endothelial-epithelial two-cell type in vitro model of the choroid plexus
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Walter Muranyi, Christian Schwerk, Rosanna Herold, Carolin Stump-Guthier, Marko Lampe, Petra Fallier-Becker, Christel Weiß, Carsten Sticht, Hiroshi Ishikawa, and Horst Schroten
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Biological sciences ,Cell biology ,Biological sciences research methodologies ,Biology experimental methods ,Science - Abstract
Summary: The choroid plexus (CP) is a highly vascularized structure containing endothelial and epithelial cells located in the ventricular system of the central nervous system (CNS). The role of the fenestrated CP endothelium is under-researched and requires the generation of an immortalized CP endothelial cell line with preserved features. Transduction of primary human CP endothelial cells (HCPEnC) with the human telomerase reverse transcriptase (hTERT) resulted in immortalized HCPEnC (iHCPEnC), which grew as monolayer with contact inhibition, formed capillary-like tubes in Matrigel, and showed no colony growth in soft agar. iHCPEnC expressed pan-endothelial markers and presented characteristic plasmalemma vesicle-associated protein-containing structures. Cultivation of iHCPEnC and human epithelial CP papilloma (HIBCPP) cells on opposite sides of cell culture filter inserts generated an in vitro model with a consistently enhanced barrier function specifically by iHCPEnC. Overall, iHCPEnC present a tool that will contribute to the understanding of CP organ functions, especially endothelial-epithelial interplay.
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- 2022
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5. Distinct migratory pattern of naive and effector T cells through the blood–CSF barrier following Echovirus 30 infection
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Marie Wiatr, Carolin Stump-Guthier, Daniela Latorre, Stefanie Uhlig, Christel Weiss, Jorma Ilonen, Britta Engelhardt, Hiroshi Ishikawa, Christian Schwerk, Horst Schroten, Tobias Tenenbaum, and Henriette Rudolph
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Enterovirus ,Blood–cerebrospinal fluid barrier ,T cell migration ,Effector T cells ,Naive T cells ,Meningitis ,Neurology. Diseases of the nervous system ,RC346-429 - Abstract
Abstract Background Echovirus 30 (E-30) is one of the most frequently isolated pathogens in aseptic meningitis worldwide. To gain access to the central nervous system (CNS), E-30 and immune cells have to cross one of the two main barriers of the CNS, the epithelial blood–cerebrospinal fluid barrier (BCSFB) or the endothelial blood–brain barrier (BBB). In an in vitro model of the BCSFB, it has been shown that E-30 can infect human immortalized brain choroid plexus papilloma (HIBCPP) cells. Methods In this study we investigated the migration of different T cell subpopulations, naive and effector T cells, through HIBCPP cells during E-30 infection. Effects of E-30 infection and the migration process were evaluated via immunofluorescence and flow cytometry analysis, as well as transepithelial resistance and dextran flux measurement. Results Th1 effector cells and enterovirus-specific effector T cells migrated through HIBCPP cells more efficiently than naive CD4+ T cells following E-30 infection of HIBCPP cells. Among the different naive T cell populations, CD8+ T cells crossed the E-30-infected HIBCPP cell layer in a significantly higher number than CD4+ T cells. A large amount of effector T cells also remained attached to the basolateral side of the HIBCPP cells compared with naive T cells. Analysis of HIBCPP barrier function showed significant alteration after E-30 infection and trans- as well as paracellular migration of T cells independent of the respective subpopulation. Morphologic analysis of migrating T cells revealed that a polarized phenotype was induced by the chemokine CXCL12, but reversed to a round phenotype after E-30 infection. Further characterization of migrating Th1 effector cells revealed a downregulation of surface adhesion proteins such as LFA-1 PSGL-1, CD44, and CD49d. Conclusion Taken together these results suggest that naive CD8+ and Th1 effector cells are highly efficient to migrate through the BCSFB in an inflammatory environment. The T cell phenotype is modified during the migration process through HIBCPP cells.
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- 2019
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6. The Choroid Plexus Is Permissive for a Preactivated Antigen-Experienced Memory B-Cell Subset in Multiple Sclerosis
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Jürgen Haas, Henriette Rudolph, Leonardo Costa, Simon Faller, Saskia Libicher, Cornelia Würthwein, Sven Jarius, Hiroshi Ishikawa, Carolin Stump-Guthier, Tobias Tenenbaum, Christian Schwerk, Horst Schroten, and Brigitte Wildemann
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multiple sclerosis ,blood-cerebrospinal fluid barrier ,B lymphocytes ,transmigration ,human ,Immunologic diseases. Allergy ,RC581-607 - Abstract
The role of B cells in multiple sclerosis (MS) is increasingly recognized. B cells undergo compartmentalized redistribution in blood and cerebrospinal fluid (CSF) during active MS, whereby memory B cells accumulate in the CSF. While B-cell trafficking across the blood–brain barrier has been intensely investigated, cellular diapedesis through the blood–CSF barrier (BCSFB) is incompletely understood. To investigate how B cells interact with the choroid plexus to transmigrate into the CSF we isolated circulating B cells from healthy donors (HC) and MS patients, utilized an inverted cell culture filter system of human choroid plexus papilloma (HIBCPP) cells to determine transmigration rates of B-cell subsets, immunofluorescence, and electron microscopy to analyze migration routes, and qRT-PCR to determine cytokines/chemokines mediating B-cell diapedesis. We also screened the transcriptome of intrathecal B cells from MS patients. We found, that spontaneous transmigration of HC- and MS-derived B cells was scant, yet increased significantly in response to B-cell specific chemokines CXCL-12/CXCL-13, was further boosted upon pre-activation and occurred via paracellular and transcellular pathways. Migrating cells exhibited upregulation of several genes involved in B-cell activation/migration and enhanced expression of chemokine receptors CXCR4/CXCR5, and were predominantly of isotype class switched memory phenotype. This antigen-experienced migratory subset displayed more pronounced chemotactic activities in MS than in HC and was retrieved in intrathecal B cells from patients with active MS. Trafficking of class-switched memory B cells was downscaled in a small cohort of natalizumab-exposed MS patients and the proportions of these phenotypes were reduced in peripheral blood yet were enriched intrathecally in patients who experienced recurrence of disease activity after withdrawal of natalizumab. Our findings highlight the relevance of the BCSFB as important gate for the entry of potentially harmful activated B cells into the CSF.
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- 2021
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7. Strain-dependent effects of clinical echovirus 30 outbreak isolates at the blood-CSF barrier
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Tobias Dahm, Ortwin Adams, Sindy Boettcher, Sabine Diedrich, Vasily Morozov, Grant Hansman, Petra Fallier-Becker, Sebastian Schädler, Claus J. Burkhardt, Christel Weiss, Carolin Stump-Guthier, Hiroshi Ishikawa, Horst Schroten, Christian Schwerk, Tobias Tenenbaum, and Henriette Rudolph
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Enterovirus ,Echovirus (E-30) ,Blood-cerebrospinal fluid barrier ,Outbreak strains ,Tight junction ,Genomic sequencing ,Neurology. Diseases of the nervous system ,RC346-429 - Abstract
Abstract Background Echovirus (E) 30 (E-30) meningitis is characterized by neuroinflammation involving immune cell pleocytosis at the protective barriers of the central nervous system (CNS). In this context, infection of the blood-cerebrospinal fluid barrier (BCSFB), which has been demonstrated to be involved in enteroviral CNS pathogenesis, may affect the tight junction (TJ) and adherens junction (AJ) function and morphology. Methods We used an in vitro human choroid plexus epithelial (HIBCPP) cell model to investigate the effect of three clinical outbreak strains (13-311, 13-759, and 14-397) isolated in Germany in 2013, and compared them to E-30 Bastianni. Conducting transepithelial electrical resistance (TEER), paracellular dextran flux measurement, quantitative real-time polymerase chain reaction (qPCR), western blot, and immunofluorescence analysis, we investigated TJ and AJ function and morphology as well as strain-specific E-30 infection patterns. Additionally, transmission electron and focused ion beam microscopy electron microscopy (FIB-SEM) was used to evaluate the mode of leukocyte transmigration. Genome sequencing and phylogenetic analyses were performed to discriminate potential genetic differences among the outbreak strains. Results We observed a significant strain-dependent decrease in TEER with strains E-30 Bastianni and 13-311, whereas paracellular dextran flux was only affected by E-30 Bastianni. Despite strong similarities among the outbreak strains in replication characteristics and particle distribution, strain 13-311 was the only outbreak isolate revealing comparable disruptive effects on TJ (Zonula Occludens (ZO) 1 and occludin) and AJ (E-cadherin) morphology to E-30 Bastianni. Notwithstanding significant junctional alterations upon E-30 infection, we observed both para- and transcellular leukocyte migration across HIBCPP cells. Complete genome sequencing revealed differences between the strains analyzed, but no explicit correlation with the observed strain-dependent effects on HIBCPP cells was possible. Conclusion The findings revealed distinct E-30 strain-specific effects on barrier integrity and junctional morphology. Despite E-30-induced barrier alterations leukocyte trafficking did not exclusively occur via the paracellular route.
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- 2018
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8. Echovirus-30 Infection Alters Host Proteins in Lipid Rafts at the Cerebrospinal Fluid Barrier In Vitro
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Marie Wiatr, Simon Staubach, Ricardo Figueiredo, Carolin Stump-Guthier, Hiroshi Ishikawa, Christian Schwerk, Horst Schroten, Franz-Georg Hanisch, Henriette Rudolph, and Tobias Tenenbaum
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enterovirus ,Echovirus-30 ,lipid raft ,blood-cerebrospinal fluid barrier ,viral infection ,HIBCPP cells ,Biology (General) ,QH301-705.5 - Abstract
Echovirus-30 (E-30) is a non-polio enterovirus responsible for meningitis outbreaks in children worldwide. To gain access to the central nervous system (CNS), E-30 first has to cross the blood-brain barrier (BBB) or the blood-cerebrospinal fluid barrier (BCSFB). E-30 may use lipid rafts of the host cells to interact with and to invade the BCSFB. To study enteroviral infection of the BCSFB, an established in vitro model based on human immortalized brain choroid plexus papilloma (HIBCPP) cells has been used. Here, we investigated the impact of E-30 infection on the protein content of the lipid rafts at the BCSFB in vitro. Mass spectrometry analysis following E-30 infection versus uninfected conditions revealed differential abundancy in proteins implicated in cellular adhesion, cytoskeleton remodeling, and endocytosis/vesicle budding. Further, we evaluated the blocking of endocytosis via clathrin/dynamin blocking and its consequences for E-30 induced barrier disruption. Interestingly, blocking of endocytosis had no impact on the capacity of E-30 to induce loss of barrier properties in HIBCPP cells. Altogether, these data highlight the impact of E-30 on HIBCPP cells microdomain as an important factor for host cell alteration.
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- 2020
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9. Non-Typeable Haemophilus influenzae Invade Choroid Plexus Epithelial Cells in a Polar Fashion
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Christian Wegele, Carolin Stump-Guthier, Selina Moroniak, Christel Weiss, Manfred Rohde, Hiroshi Ishikawa, Horst Schroten, Christian Schwerk, Michael Karremann, and Julia Borkowski
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choroid plexus ,blood–cerebrospinal fluid barrier ,NTHI ,Haemophilus influenzae ,host pathogen interaction ,meningitis ,Biology (General) ,QH301-705.5 ,Chemistry ,QD1-999 - Abstract
Non-typeable Haemophilus influenzae (NTHI) is a pathogen of the human respiratory tract causing the majority of invasive H. influenzae infections. Severe invasive infections such as septicemia and meningitis occur rarely, but the lack of a protecting vaccine and the increasing antibiotic resistance of NTHI impede treatment and emphasize its relevance as a potential meningitis causing pathogen. Meningitis results from pathogens crossing blood–brain barriers and invading the immune privileged central nervous system (CNS). In this study, we addressed the potential of NTHI to enter the brain by invading cells of the choroid plexus (CP) prior to meningeal inflammation to enlighten NTHI pathophysiological mechanisms. A cell culture model of human CP epithelial cells, which form the blood–cerebrospinal fluid barrier (BCSFB) in vivo, was used to analyze adhesion and invasion by immunofluorescence and electron microscopy. NTHI invade CP cells in vitro in a polar fashion from the blood-facing side. Furthermore, NTHI invasion rates are increased compared to encapsulated HiB and HiF strains. Fimbriae occurrence attenuated adhesion and invasion. Thus, our findings underline the role of the BCSFB as a potential entry port for NTHI into the brain and provide strong evidence for a function of the CP during NTHI invasion into the CNS during the course of meningitis.
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- 2020
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10. Polar Infection of Echovirus-30 Causes Differential Barrier Affection and Gene Regulation at the Blood–Cerebrospinal Fluid Barrier
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Marie Wiatr, Ricardo Figueiredo, Carolin Stump-Guthier, Peter Winter, Hiroshi Ishikawa, Ortwin Adams, Christian Schwerk, Horst Schroten, Henriette Rudolph, and Tobias Tenenbaum
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blood–cerebrospinal fluid barrier ,Echovirus-30 ,meningitis ,polarity ,MACE RNA sequencing ,Biology (General) ,QH301-705.5 ,Chemistry ,QD1-999 - Abstract
Echovirus-30 (E-30) is responsible for the extensive global outbreaks of meningitis in children. To gain access to the central nervous system, E-30 first has to cross the epithelial blood–cerebrospinal fluid barrier. Several meningitis causing bacteria preferentially infect human choroid plexus papilloma (HIBCPP) cells in a polar fashion from the basolateral cell side. Here, we investigated the polar infection of HIBCPP cells with E-30. Both apical and basolateral infections caused a significant decrease in the transepithelial electrical resistance of HIBCPP cells. However, to reach the same impact on the barrier properties, the multiplicity of infection of the apical side had to be higher than that of the basolateral infection. Furthermore, the number of infected cells at respective time-points after basolateral infection was significantly higher compared to apical infection. Cytotoxic effects of E-30 on HIBCPP cells during basolateral infection were observed following prolonged infection and appeared more drastically compared to the apical infection. Gene expression profiles determined by massive analysis of cDNA ends revealed distinct regulation of specific genes depending on the side of HIBCPP cells’ infection. Altogether, our data highlights the polar effects of E-30 infection in a human in vitro model of the blood–cerebrospinal fluid barrier leading to central nervous system inflammation.
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- 2020
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11. Invasion of the choroid plexus epithelium byNeisseria meningitidisis differently mediated by Arp2/3 signaling and possibly by dynamin dependent on the presence of the capsule
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Carolin Stump-Guthier, Horst Schroten, Christel Weiss, Gina Sünwoldt, Hiroshi Ishikawa, Rüdiger Adam, Rosanna Herold, and Christian Schwerk
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Dynamins ,Microbiology (medical) ,Capsules ,Neisseria meningitidis ,medicine.disease_cause ,Actin-Related Protein 2-3 Complex ,Epithelium ,medicine ,Choroid Plexus Epithelium ,Humans ,Immunology and Allergy ,Cytoskeleton ,Cells, Cultured ,Actin ,Dynamin ,Virulence ,General Immunology and Microbiology ,Chemistry ,Epithelial Cells ,General Medicine ,Actins ,Endocytosis ,Cell biology ,Meningococcal Infections ,src-Family Kinases ,Infectious Diseases ,medicine.anatomical_structure ,Blood-Brain Barrier ,Choroid Plexus ,Host-Pathogen Interactions ,Choroid plexus ,Signal transduction ,Signal Transduction - Abstract
Neisseria meningitis (Nm) is a human-specific bacterial pathogen that can cause sepsis and meningitis. To cause meningitis Nm must enter the central nervous system (CNS) across one of the barriers between the blood and the brain. We have previously shown that a capsule-depleted Serogroup B strain of Nm displays enhanced invasion into human choroid plexus (CP) epithelial papilloma (HIBCPP) cells, which represent an in vitro model of the blood–cerebrospinal fluid barrier (BCSFB). Still, the processes involved during CNS invasion by Nm, especially the role of host cell actin cytoskeleton remodeling, are not investigated in detail. Here, we demonstrate that invasion into CP epithelial cells by encapsulated and capsule-depleted Nm is mediated by distinct host cell pathways. Whereas a Serogroup B wild-type strain enters HIBCPP cells by a possibly dynamin-independent, but actin related protein 2/3 (Arp2/3)-dependent mechanism, invasion by a capsule-depleted mutant is reduced by the dynamin inhibitor dynasore and Arp2/3-independent. Both wild-type and mutant bacteria require Src kinase activity for entry into HIBCPP cells. Our data show that Nm can employ different mechanisms for invasion into the CP epithelium dependent on the presence of a capsule.
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- 2021
12. Immortalized human choroid plexus endothelial cells enable an advanced endothelial-epithelial two-cell type
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Walter, Muranyi, Christian, Schwerk, Rosanna, Herold, Carolin, Stump-Guthier, Marko, Lampe, Petra, Fallier-Becker, Christel, Weiß, Carsten, Sticht, Hiroshi, Ishikawa, and Horst, Schroten
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The choroid plexus (CP) is a highly vascularized structure containing endothelial and epithelial cells located in the ventricular system of the central nervous system (CNS). The role of the fenestrated CP endothelium is under-researched and requires the generation of an immortalized CP endothelial cell line with preserved features. Transduction of primary human CP endothelial cells (HCPEnC) with the human telomerase reverse transcriptase (hTERT) resulted in immortalized HCPEnC (iHCPEnC), which grew as monolayer with contact inhibition, formed capillary-like tubes in Matrigel, and showed no colony growth in soft agar. iHCPEnC expressed pan-endothelial markers and presented characteristic plasmalemma vesicle-associated protein-containing structures. Cultivation of iHCPEnC and human epithelial CP papilloma (HIBCPP) cells on opposite sides of cell culture filter inserts generated an
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- 2021
13. Echovirus-30 Infection Alters Host Proteins in Lipid Rafts at the Cerebrospinal Fluid Barrier In Vitro
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Simon Staubach, Henriette Rudolph, Tobias Tenenbaum, Ricardo Figueiredo, Carolin Stump-Guthier, Franz-Georg Hanisch, Christian Schwerk, Horst Schroten, Hiroshi Ishikawa, and Marie Wiatr
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0301 basic medicine ,Microbiology (medical) ,Medizin ,Endocytosis ,Microbiology ,Clathrin ,Article ,03 medical and health sciences ,0302 clinical medicine ,Virology ,ddc:610 ,HIBCPP cells ,Cell adhesion ,Cytoskeleton ,lcsh:QH301-705.5 ,Lipid raft ,Dynamin ,biology ,Chemistry ,enterovirus ,Lipid microdomain ,In vitro ,Cell biology ,lipid raft ,030104 developmental biology ,lcsh:Biology (General) ,Echovirus-30 ,biology.protein ,viral infection ,030217 neurology & neurosurgery ,blood-cerebrospinal fluid barrier - Abstract
Echovirus-30 (E-30) is a non-polio enterovirus responsible for meningitis outbreaks in children worldwide. To gain access to the central nervous system (CNS), E-30 first has to cross the blood-brain barrier (BBB) or the blood-cerebrospinal fluid barrier (BCSFB). E-30 may use lipid rafts of the host cells to interact with and to invade the BCSFB. To study enteroviral infection of the BCSFB, an established in vitro model based on human immortalized brain choroid plexus papilloma (HIBCPP) cells has been used. Here, we investigated the impact of E-30 infection on the protein content of the lipid rafts at the BCSFB in vitro. Mass spectrometry analysis following E-30 infection versus uninfected conditions revealed differential abundancy in proteins implicated in cellular adhesion, cytoskeleton remodeling, and endocytosis/vesicle budding. Further, we evaluated the blocking of endocytosis via clathrin/dynamin blocking and its consequences for E-30 induced barrier disruption. Interestingly, blocking of endocytosis had no impact on the capacity of E-30 to induce loss of barrier properties in HIBCPP cells. Altogether, these data highlight the impact of E-30 on HIBCPP cells microdomain as an important factor for host cell alteration.
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- 2020
14. Capsule and fimbriae modulate the invasion of Haemophilus influenzae in a human blood-cerebrospinal fluid barrier model
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Julia Borkowski, Carolin Stump-Guthier, Christel Weiss, Svenja Häuser, Horst Schroten, Rüdiger Adam, Christian Wegele, Christian Schwerk, Hiroshi Ishikawa, Manfred Rohde, and HZI,Helmholtz-Zentrum für Infektionsforschung GmbH, Inhoffenstr. 7,38124 Braunschweig, Germany.
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0301 basic medicine ,Microbiology (medical) ,Haemophilus Infections ,Phagocytosis ,030106 microbiology ,Fimbria ,Choroid plexus ,Biology ,medicine.disease_cause ,Microbiology ,Bacterial Adhesion ,Haemophilus influenzae ,03 medical and health sciences ,Cerebrospinal fluid ,Blood-cerebrospinal fluid barrier ,medicine ,Humans ,Meningitis ,Bacterial Capsules ,Epithelial Cells ,General Medicine ,medicine.disease ,Choroid plexus papilloma ,Antibody opsonization ,030104 developmental biology ,Infectious Diseases ,Blood-Brain Barrier ,Fimbriae, Bacterial ,Host-Pathogen Interactions ,Host pathogen interaction - Abstract
The Gram-negative bacterium Haemophilus influenzae (H. influenzae) can commensally colonize the upper respiratory tract, but also cause life threatening disease including epiglottitis, sepsis and meningitis. The H. influenzae capsule protects the bacteria against both phagocytosis and opsonization. Encapsulated H. influenzae strains are classified into serotypes ranging from a to f dependent on their distinct polysaccharide capsule. Due to the implementation of vaccination the incidence of invasive H. influenzae type b (Hib) infections has strongly decreased and infections with other capsulated types, including H. influenzae type f (Hif), are emerging. The pathogenesis of H. influenzae meningitis is not clarified. To enter the central nervous system (CNS) the bacteria generally have to cross either the blood-brain barrier (BBB) or the blood-cerebrospinal fluid barrier (BSCFB). Using a cell culture model of the BCSFB based on human choroid plexus papilloma (HIBCPP) cells and different H. influenzae strains we investigated whether Hib and Hif invade the cells, and if invasion differs between encapsulated vs. capsular-deficient and fimbriated vs. non-fimbriated variants. We find that Hib can adhere to and invade into HIBCPP cells. Invasion occurs in a strongly polar fashion, since the bacteria enter the cells preferentially from the basolateral "blood "side. Fimbriae and capsule attenuate invasion into choroid plexus (CP) epithelial cells, and capsulation can influence the bacterial distribution pattern. Finally, analysis of clinical Hib and Hif isolates confirms the detected invasive properties of H. influenzae. Our data point to roles of capsule and fimbriae during invasion of CP epithelial cells.
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- 2018
15. Distinct migratory pattern of naive and effector T cells through the blood–CSF barrier following Echovirus 30 infection
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Christian Schwerk, Stefanie Uhlig, Carolin Stump-Guthier, Christel Weiss, Britta Engelhardt, Marie Wiatr, Hiroshi Ishikawa, Horst Schroten, Jorma Ilonen, Daniela Latorre, Henriette Rudolph, and Tobias Tenenbaum
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Chemokine ,Naive T cell ,T-Lymphocytes ,T cell ,Immunology ,Echovirus Infections ,Blood–cerebrospinal fluid barrier ,T cell migration ,lcsh:RC346-429 ,03 medical and health sciences ,Cellular and Molecular Neuroscience ,0302 clinical medicine ,Immune system ,Enterovirus ,Effector T cells ,Naive T cells ,Meningitis ,Cell Movement ,Tumor Cells, Cultured ,medicine ,Humans ,lcsh:Neurology. Diseases of the nervous system ,030304 developmental biology ,0303 health sciences ,biology ,Effector ,Chemistry ,Research ,General Neuroscience ,CD44 ,3. Good health ,Cell biology ,medicine.anatomical_structure ,Neurology ,Blood-Brain Barrier ,Choroid Plexus ,biology.protein ,030217 neurology & neurosurgery ,CD8 - Abstract
BackgroundEchovirus 30 (E-30) is one of the most frequently isolated pathogens in aseptic meningitis worldwide. To gain access to the central nervous system (CNS), E-30 and immune cells have to cross one of the two main barriers of the CNS, the epithelial blood–cerebrospinal fluid barrier (BCSFB) or the endothelial blood–brain barrier (BBB). In an in vitro model of the BCSFB, it has been shown that E-30 can infect human immortalized brain choroid plexus papilloma (HIBCPP) cells.MethodsIn this study we investigated the migration of different T cell subpopulations, naive and effector T cells, through HIBCPP cells during E-30 infection. Effects of E-30 infection and the migration process were evaluated via immunofluorescence and flow cytometry analysis, as well as transepithelial resistance and dextran flux measurement.ResultsTh1 effector cells and enterovirus-specific effector T cells migrated through HIBCPP cells more efficiently than naive CD4+T cells following E-30 infection of HIBCPP cells. Among the different naive T cell populations, CD8+T cells crossed the E-30-infected HIBCPP cell layer in a significantly higher number than CD4+T cells. A large amount of effector T cells also remained attached to the basolateral side of the HIBCPP cells compared with naive T cells. Analysis of HIBCPP barrier function showed significant alteration after E-30 infection and trans- as well as paracellular migration of T cells independent of the respective subpopulation. Morphologic analysis of migrating T cells revealed that a polarized phenotype was induced by the chemokine CXCL12, but reversed to a round phenotype after E-30 infection. Further characterization of migrating Th1 effector cells revealed a downregulation of surface adhesion proteins such as LFA-1 PSGL-1, CD44, and CD49d.ConclusionTaken together these results suggest that naive CD8+and Th1 effector cells are highly efficient to migrate through the BCSFB in an inflammatory environment. The T cell phenotype is modified during the migration process through HIBCPP cells.
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- 2019
16. Delta-Like Ligand 4 Modulates Liver Damage by Down-Regulating Chemokine Expression
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Youming Li, Frank Lammert, Q. Li, Ogyi Park, Steven Dooley, Junhao Hu, Hai Li, Chengfu Xu, A Müller, Matthias P. Ebert, Roman Liebe, Hong Lei Weng, Stefan Munker, Jun Li, Teng Feng, Iryna Ilkavets, Carolin Stump-Guthier, Peter R. Mertens, Chaohui Yu, Vincent Zimmer, Zhe Shen, Hellmut G. Augustin, Christoph Meyer, Y Liu, Bedair Dewidar, Bin Gao, and Peter ten Dijke
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0301 basic medicine ,Male ,Chemokine ,Pathology ,medicine.medical_specialty ,Blotting, Western ,Notch signaling pathway ,Down-Regulation ,Inflammation ,Enzyme-Linked Immunosorbent Assay ,Real-Time Polymerase Chain Reaction ,Pathology and Forensic Medicine ,03 medical and health sciences ,Liver disease ,Mice ,0302 clinical medicine ,Massive Hepatic Necrosis ,medicine ,Animals ,Humans ,education ,Chemokine CCL2 ,education.field_of_study ,Delta-like ligand 4 ,biology ,Bile duct ,Liver Diseases ,Intracellular Signaling Peptides and Proteins ,Membrane Proteins ,Regular Article ,medicine.disease ,Immunohistochemistry ,Mice, Inbred C57BL ,030104 developmental biology ,medicine.anatomical_structure ,Hepatic stellate cell ,biology.protein ,Cancer research ,cardiovascular system ,030211 gastroenterology & hepatology ,Female ,medicine.symptom ,Chemokines - Abstract
Disrupting Notch signaling ameliorates experimental liver fibrosis. However, the role of individual Notch ligands in liver damage is unknown. We investigated the effects of Delta-like ligand 4 (Dll4) in liver disease. DLL4 expression was measured in 31 human liver tissues by immunohistochemistry. Dll4 function was examined in carbon tetrachloride– and bile duct ligation–challenged mouse models in vivo and evaluated in hepatic stellate cells, hepatocytes, and Kupffer cells in vitro . DLL4 was expressed in patients' Kupffer and liver sinusoidal endothelial cells. Recombinant Dll4 protein (rDll4) ameliorated hepatocyte apoptosis, inflammation, and fibrosis in mice after carbon tetrachloride challenge. In vitro , rDll4 significantly decreased lipopolysaccharide-dependent chemokine expression in both Kupffer and hepatic stellate cells. In bile duct ligation mice, rDll4 induced massive hepatic necrosis, resulting in the death of all animals within 1 week. Inflammatory cell infiltration and chemokine ligand 2 (Ccl2) expression were significantly reduced in rDll4-receiving bile duct ligation mice. Recombinant Ccl2 rescued bile duct ligation mice from rDll4-mediated death. In patients with acute-on-chronic liver failure, DLL4 expression was inversely associated with CCL2 abundance. Mechanistically, Dll4 regulated Ccl2 expression via NF-κB. Taken together, Dll4 modulates liver inflammatory response by down-regulating chemokine expression. rDll4 application results in opposing outcomes in two models of liver damage. Loss of DLL4 may be associated with CCL2-mediated cytokine storm in patients with acute-on-chronic liver failure.
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- 2016
17. A Choroid Plexus Epithelial Cell-based Model of the Human Blood-Cerebrospinal Fluid Barrier to Study Bacterial Infection from the Basolateral Side
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Tobias Tenenbaum, Hiroshi Ishikawa, Horst Schroten, Carolin Stump-Guthier, Julia Borkowski, Christian Schwerk, and Stefanie Dinner
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0301 basic medicine ,Pathology ,medicine.medical_specialty ,General Chemical Engineering ,Cell ,Ventricular system ,General Biochemistry, Genetics and Molecular Biology ,Tight Junctions ,03 medical and health sciences ,Cerebrospinal fluid ,medicine ,Humans ,General Immunology and Microbiology ,Tight junction ,business.industry ,General Neuroscience ,Epithelial Cells ,Bacterial Infections ,medicine.disease ,Choroid plexus papilloma ,Epithelium ,Cell biology ,030104 developmental biology ,medicine.anatomical_structure ,Blood-Brain Barrier ,Cell culture ,Choroid Plexus ,Medicine ,Choroid plexus ,business - Abstract
The epithelial cells of the choroid plexus (CP), located in the ventricular system of the brain, form the blood-cerebrospinal fluid barrier (BCSFB). The BCSFB functions in separating the cerebrospinal fluid (CSF) from the blood and restricting the molecular exchange to a minimum extent. An in vitro model of the BCSFB is based on cells derived from a human choroid plexus papilloma (HIBCPP). HIBCPP cells display typical barrier functions including formation of tight junctions (TJs), development of a transepithelial electrical resistance (TEER), as well as minor permeabilities for macromolecules. There are several pathogens that can enter the central nervous system (CNS) via the BCSFB and subsequently cause severe disease like meningitis. One of these pathogens is Neisseria meningitidis (N. meningitidis), a human-specific bacterium. Employing the HIBCPP cells in an inverted cell culture filter insert system enables to study interactions of pathogens with cells of the BCSFB from the basolateral cell side, which is relevant in vivo. In this article, we describe seeding and culturing of HIBCPP cells on cell culture inserts. Further, infection of the cells with N. meningitidis along with analysis of invaded and adhered bacteria via double immunofluorescence is demonstrated. As the cells of the CP are also involved in other diseases, including neurodegenerative disorders like Alzheimer`s disease and Multiple Sclerosis, as well as during the brain metastasis of tumor cells, the model system can also be applied in other fields of research. It provides the potential to decipher molecular mechanisms and to identify novel therapeutic targets.
- Published
- 2016
18. Mitogen-activated protein kinases are required for effective infection of human choroid plexus epithelial cells by Listeria monocytogenes
- Author
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Christian Schwerk, Julian Kaltschmidt, Svetlana Hetjens, Carolin Stump-Guthier, Tobias Tenenbaum, Hiroshi Ishikawa, Stefanie Dinner, and Horst Schroten
- Subjects
0301 basic medicine ,MAPK/ERK pathway ,Chemokine ,p38 mitogen-activated protein kinases ,Immunology ,Biology ,medicine.disease_cause ,Endocytosis ,Microbiology ,03 medical and health sciences ,Listeria monocytogenes ,medicine ,Humans ,Internalin ,Epithelial Cells ,Virology ,030104 developmental biology ,Infectious Diseases ,Mitogen-activated protein kinase ,Choroid Plexus ,Host-Pathogen Interactions ,biology.protein ,Choroid plexus ,Mitogen-Activated Protein Kinases - Abstract
Listeria monocytogenes, a Gram-positive bacterium, can cause meningitis after invading the human central nervous system. The blood-cerebrospinal fluid barrier (BCSFB), located at the epithelium of the choroid plexus, is a possible entry site for L. monocytogenes into the brain, and in vitro L. monocytogenes invades human choroid plexus epithelial papilloma (HIBCPP) cells. Although host cell signal transduction subsequent to infection by L. monocytogenes has been investigated, the role of mitogen-activated protein kinases (MAPK) is not clarified yet. We show that infection with L. monocytogenes causes activation of the MAPKs Erk1/2 and p38 preferentially when bacteria are added to the physiologically more relevant basolateral side of HIBCPP cells. Deletion of the listerial virulence factors Internalin (InlA) and InlB reduces MAPK activation. Whereas inhibition of either Erk1/2 or p38 signaling significantly attenuates infection of HIBCPP cells with L. monocytogenes, simultaneous inhibition of both MAPK pathways shows an additive effect, and Erk1/2 and p38 are involved in regulation of cytokine and chemokine expression following infection. Blocking of endocytosis with the synthetic dynamin inhibitor dynasore strongly abrogates infection of HIBCPP cells with L. monocytogenes. Concurrent inhibition of MAPK signaling further reduces infection, suggesting MAPKs mediate infection with L. monocytogenes during inhibition of dynamin-mediated endocytosis.
- Published
- 2016
19. Neutrophil extracellular trap formation in the Streptococcus suis-infected cerebrospinal fluid compartment
- Author
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Nicole, de Buhr, Friederike, Reuner, Ariane, Neumann, Carolin, Stump-Guthier, Tobias, Tenenbaum, Horst, Schroten, Hiroshi, Ishikawa, Kristin, Müller, Andreas, Beineke, Isabel, Hennig-Pauka, Thomas, Gutsmann, Peter, Valentin-Weigand, Christoph G, Baums, and Maren, von Köckritz-Blickwede
- Subjects
Swine Diseases ,Deoxyribonucleases ,Microbial Viability ,Streptococcus suis ,Neutrophils ,Swine ,Cell Culture Techniques ,Extracellular Traps ,Animals, Newborn ,Blood-Brain Barrier ,Cathelicidins ,Streptococcal Infections ,Animals ,Cerebrospinal Fluid - Abstract
Streptococcus suis is an important meningitis-causing pathogen in pigs and humans. Neutrophil extracellular traps (NETs) have been identified as host defense mechanism against different pathogens. Here, NETs were detected in the cerebrospinal fluid (CSF) of S. suis-infected piglets despite the presence of active nucleases. To study NET-formation and NET-degradation after transmigration of S. suis and neutrophils through the choroid plexus epithelial cell barrier, a previously described model of the human blood-CSF barrier was used. NETs and respective entrapment of streptococci were recorded in the "CSF compartment" despite the presence of active nucleases. Comparative analysis of S. suis wildtype and different S. suis nuclease mutants did not reveal significant differences in NET-formation or bacterial survival. Interestingly, transcript expression of the human cathelicidin LL-37, a NET-stabilizing factor, increased after transmigration of neutrophils through the choroid plexus epithelial cell barrier. In good accordance, the porcine cathelicidin PR-39 was significantly increased in CSF of piglets with meningitis. Furthermore, we confirmed that PR-39 is associated with NETs in infected CSF and inhibits neutrophil DNA degradation by bacterial nucleases. In conclusion, neutrophils form NETs after breaching the infected choroid plexus epithelium, and those NETs may be protected by antimicrobial peptides against bacterial nucleases.
- Published
- 2015
20. Neisseria meningitidis elicits a pro-inflammatory response involving IκBζ in a human blood-cerebrospinal fluid barrier model
- Author
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Julia, Borkowski, Li, Li, Ulrike, Steinmann, Natascha, Quednau, Carolin, Stump-Guthier, Christel, Weiss, Peter, Findeisen, Norbert, Gretz, Hiroshi, Ishikawa, Tobias, Tenenbaum, Horst, Schroten, and Christian, Schwerk
- Subjects
Analysis of Variance ,Host-pathogen interactions ,Cell Survival ,Gene Expression Profiling ,Research ,Toll-Like Receptors ,NF-kappa B ,Enzyme-Linked Immunosorbent Assay ,Epithelial Cells ,Choroid plexus ,Cellular immune response ,Neisseria meningitidis ,Microarray ,Up-Regulation ,Blood-Brain Barrier ,Cell Line, Tumor ,Blood-cerebrospinal fluid barrier ,Cytokines ,Humans ,Papilloma, Choroid Plexus ,Transcriptomics ,Oligonucleotide Array Sequence Analysis - Abstract
Background The human-specific, Gram-negative bacterium Neisseria meningitidis (Nm) is a leading cause of bacterial meningitis worldwide. The blood-cerebrospinal fluid barrier (BCSFB), which is constituted by the epithelial cells of the choroid plexus (CP), has been suggested as one of the potential entry sites of Nm into the CSF and can contribute to the inflammatory response during infectious diseases of the brain. Toll-like receptors (TLRs) are involved in mediating signal transduction caused by the pathogens. Methods Using a recently established in vitro model of the human BCSFB based on human malignant CP papilloma (HIBCPP) cells we investigated the cellular response of HIBCPP cells challenged with the meningitis-causing Nm strain, MC58, employing transcriptome and RT-PCR analysis, cytokine bead array, and enzyme-linked immunosorbent assay (ELISA). In comparison, we analyzed the answer to the closely related unencapsulated carrier isolate Nm α14. The presence of TLRs in HIBCPP and their role during signal transduction caused by Nm was studied by RT-PCR and the use of specific agonists and mutant bacteria. Results We observed a stronger transcriptional response after infection with strain MC58, in particular with its capsule-deficient mutant MC58siaD−, which correlated with bacterial invasion levels. Expression evaluation and Gene Set Enrichment Analysis pointed to a NFκB-mediated pro-inflammatory immune response involving up-regulation of the transcription factor IκBζ. Infected cells secreted significant levels of pro-inflammatory chemokines and cytokines, including, among others, IL8, CXCL1-3, and the IκBζ target gene product IL6. The expression profile of pattern recognition receptors in HIBCPP cells and the response to specific agonists indicates that TLR2/TLR6, rather than TLR4 or TLR2/TLR1, is involved in the cellular reaction following Nm infection. Conclusions Our data show that Nm can initiate a pro-inflammatory response in human CP epithelial cells probably involving TLR2/TLR6 signaling and the transcriptional regulator IκBζ. Electronic supplementary material The online version of this article (doi:10.1186/s12974-014-0163-x) contains supplementary material, which is available to authorized users.
- Published
- 2014
21. Neutrophil extracellular trap formation in theStreptococcus suis-infected cerebrospinal fluid compartment
- Author
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Nicole de Buhr, Peter Valentin-Weigand, Tobias Tenenbaum, Friederike Reuner, Maren von Köckritz-Blickwede, Hiroshi Ishikawa, Christoph Georg Baums, Horst Schroten, K. Müller, Isabel Hennig-Pauka, Ariane Neumann, Carolin Stump-Guthier, Andreas Beineke, and Thomas Gutsmann
- Subjects
0301 basic medicine ,medicine.medical_treatment ,030106 microbiology ,Immunology ,Antimicrobial peptides ,Streptococcus suis ,Neutrophil extracellular traps ,Biology ,Blood–brain barrier ,biology.organism_classification ,Microbiology ,Cathelicidin ,03 medical and health sciences ,030104 developmental biology ,Cerebrospinal fluid ,medicine.anatomical_structure ,Virology ,Choroid Plexus Epithelium ,medicine ,Choroid plexus - Abstract
Streptococcus suis is an important meningitis-causing pathogen in pigs and humans. Neutrophil extracellular traps (NETs) have been identified as host defense mechanism against different pathogens. Here, NETs were detected in the cerebrospinal fluid (CSF) of S. suis-infected piglets despite the presence of active nucleases. To study NET-formation and NET-degradation after transmigration of S. suis and neutrophils through the choroid plexus epithelial cell barrier, a previously described model of the human blood-CSF barrier was used. NETs and respective entrapment of streptococci were recorded in the "CSF compartment" despite the presence of active nucleases. Comparative analysis of S. suis wildtype and different S. suis nuclease mutants did not reveal significant differences in NET-formation or bacterial survival. Interestingly, transcript expression of the human cathelicidin LL-37, a NET-stabilizing factor, increased after transmigration of neutrophils through the choroid plexus epithelial cell barrier. In good accordance, the porcine cathelicidin PR-39 was significantly increased in CSF of piglets with meningitis. Furthermore, we confirmed that PR-39 is associated with NETs in infected CSF and inhibits neutrophil DNA degradation by bacterial nucleases. In conclusion, neutrophils form NETs after breaching the infected choroid plexus epithelium, and those NETs may be protected by antimicrobial peptides against bacterial nucleases.
- Published
- 2016
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