Your search keyword '"chemokine receptor CCR7"' showing total 30 results

1. Specialized Tfh cell subsets driving type-1 and type-2 humoral responses in lymphoid tissue

Author

Kumar, S, Basto, A, Ribeiro, F, Almeida, S, Campos, P, Peres, C, Pulvirenti, N, Al-Khalidi, S, Kilbey, A, Tosello, J, Piaggio, E, Russo, M, Gama-Carvalho, M, Coffelt, S, Roberts, E, Geginat, J, Florindo, H, Graca, L, Kumar S., Basto A. P., Ribeiro F., Almeida S. C. P., Campos P., Peres C., Pulvirenti N., Al-Khalidi S., Kilbey A., Tosello J., Piaggio E., Russo M., Gama-Carvalho M., Coffelt S. B., Roberts E. W., Geginat J., Florindo H. F., Graca L., Kumar, S, Basto, A, Ribeiro, F, Almeida, S, Campos, P, Peres, C, Pulvirenti, N, Al-Khalidi, S, Kilbey, A, Tosello, J, Piaggio, E, Russo, M, Gama-Carvalho, M, Coffelt, S, Roberts, E, Geginat, J, Florindo, H, Graca, L, Kumar S., Basto A. P., Ribeiro F., Almeida S. C. P., Campos P., Peres C., Pulvirenti N., Al-Khalidi S., Kilbey A., Tosello J., Piaggio E., Russo M., Gama-Carvalho M., Coffelt S. B., Roberts E. W., Geginat J., Florindo H. F., and Graca L.

Abstract

Effective antibody responses are essential to generate protective humoral immunity. Different inflammatory signals polarize T cells towards appropriate effector phenotypes during an infection or immunization. Th1 and Th2 cells have been associated with the polarization of humoral responses. However, T follicular helper cells (Tfh) have a unique ability to access the B cell follicle and support the germinal center (GC) responses by providing B cell help. We investigated the specialization of Tfh cells induced under type-1 and type-2 conditions. We first studied homogenous Tfh cell populations generated by adoptively transferred TCR-transgenic T cells in mice immunized with type-1 and type-2 adjuvants. Using a machine learning approach, we established a gene expression signature that discriminates Tfh cells polarized towards type-1 and type-2 response, defined as Tfh1 and Tfh2 cells. The distinct signatures of Tfh1 and Tfh2 cells were validated against datasets of Tfh cells induced following lymphocytic choriomeningitis virus (LCMV) or helminth infection. We generated single-cell and spatial transcriptomics datasets to dissect the heterogeneity of Tfh cells and their localization under the two immunizing conditions. Besides a distinct specialization of GC Tfh cells under the two immunizations and in different regions of the lymph nodes, we found a population of Gzmk+ Tfh cells specific for type-1 conditions. In human individuals, we could equally identify CMV-specific Tfh cells that expressed Gzmk. Our results show that Tfh cells acquire a specialized function under distinct types of immune responses and with particular properties within the B cell follicle and the GC.

Published

2024

2. Shifting CCR7 towards Its Monomeric Form Augments CCL19 Binding and Uptake.

Author

Gerken, Oliver J., Artinger, Marc, and Legler, Daniel F.

Subjects

*CHEMOKINE receptors, *G protein coupled receptors, *LUCIFERASES, *BINDING sites

Abstract

The chemokine receptor CCR7, together with its ligands, is responsible for the migration and positioning of adaptive immune cells, and hence critical for launching adaptive immune responses. CCR7 is also induced on certain cancer cells and contributes to metastasis formation. Thus, CCR7 expression and signalling must be tightly regulated for proper function. CCR7, like many other members of the G-protein coupled receptor superfamily, can form homodimers and oligomers. Notably, danger signals associated with pathogen encounter promote oligomerisation of CCR7 and is considered as one layer of regulating its function. Here, we assessed the dimerisation of human CCR7 and several single point mutations using split-luciferase complementation assays. We demonstrate that dimerisation-defective CCR7 mutants can be transported to the cell surface and elicit normal chemokine-driven G-protein activation. By contrast, we discovered that CCR7 mutants whose expression are shifted towards monomers significantly augment their capacities to bind and internalise fluorescently labelled CCL19. Modeling of the receptor suggests that dimerisation-defective CCR7 mutants render the extracellular loops more flexible and less structured, such that the chemokine recognition site located in the binding pocket might become more accessible to its ligand. Overall, we provide new insights into how the dimerisation state of CCR7 affects CCL19 binding and receptor trafficking. [ABSTRACT FROM AUTHOR]

Published

2022

3. CAL-1 as Cellular Model System to Study CCR7-Guided Human Dendritic Cell Migration.

Author

Uetz-von Allmen, Edith, Samson, Guerric P. B., Purvanov, Vladimir, Maeda, Takahiro, and Legler, Daniel F.

Subjects

CELL migration, DENDRITIC cells, CHEMOKINE receptors, CELL surface antigens, IMMUNOMODULATORS, CXCR4 receptors, CYTOTOXIC T cells

Abstract

Dendritic cells (DCs) are potent and versatile professional antigen-presenting cells and central for the induction of adaptive immunity. The ability to migrate and transport peripherally acquired antigens to draining lymph nodes for subsequent cognate T cell priming is a key feature of DCs. Consequently, DC-based immunotherapies are used to elicit tumor-antigen specific T cell responses in cancer patients. Understanding chemokine-guided DC migration is critical to explore DCs as cellular vaccines for immunotherapeutic approaches. Currently, research is hampered by the lack of appropriate human cellular model systems to effectively study spatio-temporal signaling and CCR7-driven migration of human DCs. Here, we report that the previously established human neoplastic cell line CAL-1 expresses the human DC surface antigens CD11c and HLA-DR together with co-stimulatory molecules. Importantly, if exposed for three days to GM-CSF, CAL-1 cells induce the endogenous expression of the chemokine receptor CCR7 upon encountering the clinically approved TLR7/8 agonist Resiquimod R848 and readily migrate along chemokine gradients. Further, we demonstrate that CAL-1 cells can be genetically modified to express fluorescent (GFP)-tagged reporter proteins to study and visualize signaling or can be gene-edited using CRISPR/Cas9. Hence, we herein present the human CAL-1 cell line as versatile and valuable cellular model system to effectively study human DC migration and signaling. [ABSTRACT FROM AUTHOR]

Published

2021

4. CAL-1 as Cellular Model System to Study CCR7-Guided Human Dendritic Cell Migration

Author

Edith Uetz-von Allmen, Guerric P. B. Samson, Vladimir Purvanov, Takahiro Maeda, and Daniel F. Legler

Subjects

human dendritic cell line, cell migration, chemokine receptor CCR7, CCL19, CCL21, chemotaxis, Immunologic diseases. Allergy, RC581-607

Abstract

Dendritic cells (DCs) are potent and versatile professional antigen-presenting cells and central for the induction of adaptive immunity. The ability to migrate and transport peripherally acquired antigens to draining lymph nodes for subsequent cognate T cell priming is a key feature of DCs. Consequently, DC-based immunotherapies are used to elicit tumor-antigen specific T cell responses in cancer patients. Understanding chemokine-guided DC migration is critical to explore DCs as cellular vaccines for immunotherapeutic approaches. Currently, research is hampered by the lack of appropriate human cellular model systems to effectively study spatio-temporal signaling and CCR7-driven migration of human DCs. Here, we report that the previously established human neoplastic cell line CAL-1 expresses the human DC surface antigens CD11c and HLA-DR together with co-stimulatory molecules. Importantly, if exposed for three days to GM-CSF, CAL-1 cells induce the endogenous expression of the chemokine receptor CCR7 upon encountering the clinically approved TLR7/8 agonist Resiquimod R848 and readily migrate along chemokine gradients. Further, we demonstrate that CAL-1 cells can be genetically modified to express fluorescent (GFP)-tagged reporter proteins to study and visualize signaling or can be gene-edited using CRISPR/Cas9. Hence, we herein present the human CAL-1 cell line as versatile and valuable cellular model system to effectively study human DC migration and signaling.

Published

2021

5. Shifting CCR7 towards Its Monomeric Form Augments CCL19 Binding and Uptake

Author

Oliver J. Gerken, Marc Artinger, and Daniel F. Legler

Subjects

chemokine receptor CCR7, receptor dimerisation, receptor trafficking, chemokine binding, signalling, GPCR, Cytology, QH573-671

Abstract

The chemokine receptor CCR7, together with its ligands, is responsible for the migration and positioning of adaptive immune cells, and hence critical for launching adaptive immune responses. CCR7 is also induced on certain cancer cells and contributes to metastasis formation. Thus, CCR7 expression and signalling must be tightly regulated for proper function. CCR7, like many other members of the G-protein coupled receptor superfamily, can form homodimers and oligomers. Notably, danger signals associated with pathogen encounter promote oligomerisation of CCR7 and is considered as one layer of regulating its function. Here, we assessed the dimerisation of human CCR7 and several single point mutations using split-luciferase complementation assays. We demonstrate that dimerisation-defective CCR7 mutants can be transported to the cell surface and elicit normal chemokine-driven G-protein activation. By contrast, we discovered that CCR7 mutants whose expression are shifted towards monomers significantly augment their capacities to bind and internalise fluorescently labelled CCL19. Modeling of the receptor suggests that dimerisation-defective CCR7 mutants render the extracellular loops more flexible and less structured, such that the chemokine recognition site located in the binding pocket might become more accessible to its ligand. Overall, we provide new insights into how the dimerisation state of CCR7 affects CCL19 binding and receptor trafficking.

Published

2022

6. Signs of immunosenescence correlate with poor outcome of mRNA COVID-19 vaccination in older adults

Author

Miguel Ángel Palacios-Pedrero, Janina M. Jansen, Cornelia Blume, Nils Stanislawski, Rebecca Jonczyk, Antonia Molle, Mariana Gonzalez Hernandez, Franziska K. Kaiser, Klaus Jung, Albert D. M. E. Osterhaus, Guus F. Rimmelzwaan, and Giulietta Saletti

Subjects

chemokine receptor CCR7, CD45RA antigen, tumor necrosis factor, neutralizing antibody, General Medicine, tozinameran, interleukin 2, immunoglobulin G, CD57 antigen, ddc:610, gamma interferon, Dewey Decimal Classification::600 | Technik::610 | Medizin, Gesundheit, SARS-CoV-2 antibody, coronavirus spike glycoprotein

Abstract

Vaccination against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is effective in preventing COVID-19 hospitalization and fatal outcome. However, several studies indicated that there is reduced vaccine effectiveness among older individuals, which is correlated with their general health status1,2. How and to what extent age-related immunological defects are responsible for the suboptimal vaccine responses observed in older individuals receiving SARS-CoV-2 messenger RNA vaccine, is unclear and not fully investigated1,3–5. In this observational study, we investigated adaptive immune responses in adults of various ages (22–99 years old) receiving 2 doses of the BNT162b2 mRNA vaccine. Vaccine-induced Spike-specific antibody, and T and memory B cell responses decreased with increasing age. These responses positively correlated with the percentages of peripheral naïve CD4+ and CD8+ T cells and negatively with CD8+ T cells expressing signs of immunosenescence. Older adults displayed a preferred T cell response to the S2 region of the Spike protein, which is relatively conserved and a target for cross-reactive T cells induced by human ‘common cold’ coronaviruses. Memory T cell responses to influenza virus were not affected by age-related changes, nor the SARS-CoV-2-specific response induced by infection. Collectively, we identified signs of immunosenescence correlating with the outcome of vaccination against a new viral antigen to which older adults are immunologically naïve. This knowledge is important for the management of COVID-19 infections in older adults.

Published

2022

7. Dendritic cell migration in inflammation and immunity

Author

Liu, Juan, Zhang, Xiaomin, Cheng, Yujie, and Cao, Xuetao

Published

2021

8. Dendritic cell migration in inflammation and immunity

Author

Xiaomin Zhang, Yujie Cheng, Juan Liu, and Xuetao Cao

Subjects

chemokine receptor CCR7, Chemokine, Receptors, CCR7, cell migration, Immunology, chemical and pharmacologic phenomena, Autoimmunity, Review Article, Adaptive Immunity, Communicable Diseases, Immune tolerance, Autoimmune Diseases, Immune system, Immunity, Cell Movement, Immunology and Allergy, Animals, Humans, Dendritic cell migration, Innate immunity, Inflammation, Innate immune system, biology, Cell migration, Dendritic Cells, Acquired immune system, Infectious Diseases, biology.protein, Chemokines

Abstract

Dendritic cells (DCs) are the key link between innate immunity and adaptive immunity and play crucial roles in both the promotion of immune defense and the maintenance of immune tolerance. The trafficking of distinct DC subsets across lymphoid and nonlymphoid tissues is essential for DC-dependent activation and regulation of inflammation and immunity. DC chemotaxis and migration are triggered by interactions between chemokines and their receptors and regulated by multiple intracellular mechanisms, such as protein modification, epigenetic reprogramming, metabolic remodeling, and cytoskeletal rearrangement, in a tissue-specific manner. Dysregulation of DC migration may lead to abnormal positioning or activation of DCs, resulting in an imbalance of immune responses and even immune pathologies, including autoimmune responses, infectious diseases, allergic diseases and tumors. New strategies targeting the migration of distinct DC subsets are being explored for the treatment of inflammatory and infectious diseases and the development of novel DC-based vaccines. In this review, we will discuss the migratory routes and immunological consequences of distinct DC subsets, the molecular basis and regulatory mechanisms of migratory signaling in DCs, and the association of DC migration with the pathogenesis of autoimmune and infectious diseases.

Published

2021

9. Signs of immunosenescence correlate with poor outcome of mRNA COVID-19 vaccination in older adults

Author

Palacios-Pedrero, Miguel Ángel, Jansen, Janina M., Blume, Cornelia, Stanislawski, Nils, Jonczyk, Rebecca, Molle, Antonia, Hernandez, Mariana Gonzalez, Kaiser, Franziska K., Jung, Klaus, Osterhaus, Albert D. M. E., Rimmelzwaan, Guus F., Saletti, Giulietta, Palacios-Pedrero, Miguel Ángel, Jansen, Janina M., Blume, Cornelia, Stanislawski, Nils, Jonczyk, Rebecca, Molle, Antonia, Hernandez, Mariana Gonzalez, Kaiser, Franziska K., Jung, Klaus, Osterhaus, Albert D. M. E., Rimmelzwaan, Guus F., and Saletti, Giulietta

Abstract

Vaccination against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is effective in preventing COVID-19 hospitalization and fatal outcome. However, several studies indicated that there is reduced vaccine effectiveness among older individuals, which is correlated with their general health status1,2. How and to what extent age-related immunological defects are responsible for the suboptimal vaccine responses observed in older individuals receiving SARS-CoV-2 messenger RNA vaccine, is unclear and not fully investigated1,3–5. In this observational study, we investigated adaptive immune responses in adults of various ages (22–99 years old) receiving 2 doses of the BNT162b2 mRNA vaccine. Vaccine-induced Spike-specific antibody, and T and memory B cell responses decreased with increasing age. These responses positively correlated with the percentages of peripheral naïve CD4+ and CD8+ T cells and negatively with CD8+ T cells expressing signs of immunosenescence. Older adults displayed a preferred T cell response to the S2 region of the Spike protein, which is relatively conserved and a target for cross-reactive T cells induced by human ‘common cold’ coronaviruses. Memory T cell responses to influenza virus were not affected by age-related changes, nor the SARS-CoV-2-specific response induced by infection. Collectively, we identified signs of immunosenescence correlating with the outcome of vaccination against a new viral antigen to which older adults are immunologically naïve. This knowledge is important for the management of COVID-19 infections in older adults.

Published

2022

10. Effects of Chemokines on Tumor Metastasis

Author

Takeuchi, Hiroya, Kitago, Minoru, Hoon, David S. B., Rosen, Steven T., editor, and Leong, Stanley P. L., editor

Published

2007

11. Inflammatory chemokines: their role in tumor growth and progression

Author

Balkwill, Frances R., Parnham, Michael J., editor, Morgan, Douglas W., editor, Forssmann, Ulf J., editor, and Nakada, Marian T., editor

Published

2004

12. Shifting CCR7 towards its monomeric form augments CCL19 binding and uptake

Author

Gerken, Oliver J, Artinger, Marc, and Legler, Daniel F

Subjects

Receptors, CCR7, Chemokine CCL21, 610 Medicine & health, hemic and immune systems, chemical and pharmacologic phenomena, General Medicine, Ligands, chemokine receptor CCR7, receptor dimerisation, receptor trafficking, chemokine binding, signalling, GPCR, immune system diseases, ddc:570, Chemokine CCL19, Humans, Protein Binding, Signal Transduction

Abstract

The chemokine receptor CCR7, together with its ligands, is responsible for the migration and positioning of adaptive immune cells, and hence critical for launching adaptive immune responses. CCR7 is also induced on certain cancer cells and contributes to metastasis formation. Thus, CCR7 expression and signalling must be tightly regulated for proper function. CCR7, like many other members of the G-protein coupled receptor superfamily, can form homodimers and oligomers. Notably, danger signals associated with pathogen encounter promote oligomerisation of CCR7 and is considered as one layer of regulating its function. Here, we assessed the dimerisation of human CCR7 and several single point mutations using split-luciferase complementation assays. We demonstrate that dimerisation-defective CCR7 mutants can be transported to the cell surface and elicit normal chemokine-driven G-protein activation. By contrast, we discovered that CCR7 mutants whose expression are shifted towards monomers significantly augment their capacities to bind and internalise fluorescently labelled CCL19. Modeling of the receptor suggests that dimerisation-defective CCR7 mutants render the extracellular loops more flexible and less structured, such that the chemokine recognition site located in the binding pocket might become more accessible to its ligand. Overall, we provide new insights into how the dimerisation state of CCR7 affects CCL19 binding and receptor trafficking.

Published

2022

13. Functional Subsets of Memory T Cells Identified by CCR7 Expression

Author

Sallusto, F., Langenkamp, A., Geginat, J., Lanzavecchia, A., Compans, R. W., editor, Cooper, M., editor, Hogle, J. M., editor, Ito, Y., editor, Koprowski, H., editor, Melchers, F., editor, Oldstone, M., editor, Olsnes, S., editor, Potter, M., editor, Saedler, H., editor, Vogt, P. K., editor, Wagner, H., editor, and Melchers, Fritz, editor

Published

2000

14. Converse regulation of CCR7-driven human dendritic cell migration by prostaglandin E2 and liver X receptor activation.

Author

Bruckner, Markus, Dickel, Denise, Singer, Eva, and Legler, Daniel F.

Abstract

Migration and homing of DCs to lymphoid organs is pivotal for inducing adaptive immunity and tolerance. DC homing depends on the chemokine receptor CCR7. However, expression of CCR7 alone is not sufficient for effective DC migration. A second signal, mediated by prostaglandin E2 (PGE2), is critical for the development of a migratory DC phenotype. PGE2 is important for inducing efficient immune responses, but, if deregulated, contributes to chronic inflammation, autoimmune diseases through Th17-cell development and tumorigenesis. In contrast, activation of liver X receptor ( LXR)α has recently been shown to interfere with CCR7 expression and migration of DCs resulting in a reduced immune response. Here, we demonstrate that PGE2 downregulates LXRα expression in human monocyte derived as well as ex vivo DCs. Moreover, PGE2 stimulation dampens LXR activation, auto-regulation and LXR-mediated gene transcription. Consequently, we show that PGE2 enhances CCR7 expression and migration of LXR-activated DCs. Furthermore, we provide evidence that PGE2 signaling and LXR activation specifically elicit converse effects on CCR7 expression and DC migration. In contrast, production of MMP9, CCL4, COX-2, and IL-23 is solely regulated by PGE2, but not by LXR activation, offering new perspectives for therapeutic interventions. [ABSTRACT FROM AUTHOR]

Published

2012

15. Nasal and pulmonary vaccine delivery using particulate carriers

Author

Yimei Jia, Lakshmi Krishnan, and Abdelwahab Omri

Subjects

chemokine receptor CCR7, medicine.medical_treatment, Haemophilus infection, Pharmaceutical Science, Drug Delivery Systems, vaccine, Haemophilus influenzae type b vaccine, pneumococcal infection, T lymphocyte, diphtheria pertussis poliomyelitis tetanus Haemophilus influenzae type b vaccine, Medicine, CD8+ T lymphocyte, Respiratory system, polylactic acid, Lung, innate immunity, Vaccines, inhalation, tumor necrosis factor alpha, biology, pertussis, Immunogenicity, Vaccination, adaptive immunity, chitosan nanoparticle, diphtheria vaccine, Respiratory pathogens, severe acute respiratory syndrome vaccine, tuberculosis, virus like agent, liposome, gamma interferon, Antibody, influenza, Adjuvant, DNA vaccine, interleukin 18, polymer, respiratory tract infection, measles mumps rubella vaccine, nanoemulsion, Respiratory Mucosa, severe acute respiratory syndrome, interleukin 2, diphtheria pertussis tetanus vaccine, Immune system, Adjuvants, Immunologic, measles vaccine, ISCOM, Animals, Humans, measles, influenza A (H5N1), Antigens, Immunity, Mucosal, BCG vaccine, CD4+ T lymphocyte, B lymphocyte, cross presentation, business.industry, cholera toxin, virosome, Vaccine delivery, Pneumococcus vaccine, Nasal Mucosa, antigen presenting cell, macrogol, Immunology, biology.protein, mucosal immunity, interleukin 12, Local immunity, influenza vaccine, chickenpox measles mumps rubella vaccine, polyethyleneimine, business, gold nanoparticle

Abstract

Introduction: Many human pathogens cause respiratory illness by colonizing and invading the respiratory mucosal surfaces. Preventing infection at local sites via mucosally active vaccines is a promising and rational approach for vaccine development. However, stimulating mucosal immunity is often challenging. Particulate adjuvants that can specifically target mucosal immune cells offer a promising opportunity to stimulate local immunity at the nasal and/or pulmonary mucosal surfaces.Areas covered: This review analyzes the common causes of respiratory infections, the challenges in the induction of mucosal and systemic responses and current pulmonary and nasal mucosal vaccination strategies. The ability of various particulate adjuvant formulations, including lipid-based particles, polymers and other particulate systems, to be effectively utilized for mucosal vaccine delivery is discussed.Expert opinion: Induction of antibody and cell-mediated mucosal immunity that can effectively combat respiratory pathogens remains a challenge. Particulate delivery systems can be developed to target mucosal immune cells and effectively present antigen to evoke a rapid and long-term local immunity in the respiratory mucosa. In particular, particulate delivery systems offer the versatility of being formulated with multiple adjuvants and antigenic cargo, and can be tailored to effectively prime immune responses across the mucosal barrier. The opportunity for rational design of novel subunit particulate vaccines is emerging.

Published

2015

16. Induced regulatory T cells are phenotypically unstable and do not protect mice from rapidly progressive glomerulonephritis.

Author

Ghali J.R., Kitching A.R., Holdsworth S.R., Alikhan M.A., Ghali J.R., Kitching A.R., Holdsworth S.R., and Alikhan M.A.

Abstract

Regulatory T (Treg) cells are a suppressive CD4+ T-cell subset. We generated induced Treg (iTreg) cells and explored their therapeutic potential in a murine model of rapidly progressive glomerulonephritis. Polyclonal naive CD4+ T cells were cultured in vitro with interleukin-2 (IL-2), transforming growth factor-beta1, all-trans-retinoic acid and monoclonal antibodies against interferon-gamma and IL-4, generating Foxp3+ iTreg cells. To enhance their suppressive phenotype, iTreg cultures were modified with the addition of a monoclonal antibody against IL-12p40 or by using RORgammat-/- CD4+ T cells. Induced Treg cells were transferred into models of delayed-type hypersensitivity and experimental glomerulonephritis. The iTreg cells exhibited comparable surface receptor expression and in vitro suppressive ability to natural Treg cells, but did not regulate antigen-specific delayed-type hypersensitivity or systemic inflammatory immune responses, losing Foxp3 expression in vivo. In glomerulonephritis, transferred iTreg cells did not prevent renal injury or modulate systemic T helper type 1 immune responses. Induced Treg cells cultured with anti-IL-12p40 had an enhanced suppressive phenotype in vitro and regulated dermal delayed-type hypersensitivity in vivo, but were not protective against renal injury, losing Foxp3 expression, especially in the transferred cells recruited to the kidney. Use of RORgammat-/- CD4+ T cells or iTreg cells generated from sensitized CD4+ Foxp3- cells did not regulate renal or systemic inflammatory responses in vivo. In conclusion, iTreg cells suppress T-cell proliferation in vitro, but do not regulate experimental glomerulonephritis, being unstable in this inflammatory milieu in vivo.Copyright © 2016 John Wiley & Sons Ltd

Published

2017

17. Converse regulation of CCR7-driven human dendritic cell migration by prostaglandin E(2) and liver X receptor activation

Author

Bruckner, Markus, Dickel, Denise, Singer, Eva, and Legler, Daniel

Subjects

prostaglandin E2, Chemokine receptor CCR7, ddc:570, monocyte-derived DCs, hemic and immune systems, chemical and pharmacologic phenomena, lipids (amino acids, peptides, and proteins), migration, liver X receptor

Abstract

Migration and homing of DCs to lymphoid organs is pivotal for inducing adaptive immunity and tolerance. DC homing depends on the chemokine receptor CCR7. However, expression of CCR7 alone is not sufficient for effective DC migration. A second signal, mediated by prostaglandin E2 (PGE2), is critical for the development of a migratory DC phenotype. PGE2 is important for inducing efficient immune responses, but, if deregulated, contributes to chronic inflammation, autoimmune diseases through Th17-cell development and tumorigenesis. In contrast, activation of liver X receptor (LXR)α has recently been shown to interfere with CCR7 expression and migration of DCs resulting in a reduced immune response. Here, we demonstrate that PGE2 downregulates LXRα expression in human monocyte derived as well as ex vivo DCs. Moreover, PGE2 stimulation dampens LXR activation, auto-regulation and LXR-mediated gene transcription. Consequently, we show that PGE2 enhances CCR7 expression and migration of LXR-activated DCs. Furthermore, we provide evidence that PGE2 signaling and LXR activation specifically elicit converse effects on CCR7 expression and DC migration. In contrast, production of MMP9, CCL4, COX-2, and IL-23 is solely regulated by PGE2, but not by LXR activation, offering new perspectives for therapeutic interventions.

Published

2012

18. Chemokine receptors CXCR4 and CCR7 promote metastasis by preventing anoikis in cancer cells

Author

Marina Kochetkova, Shaun R. McColl, Sharad Kumar, Kochetkova, M., Kumar, S, and McColl, S. R.

Subjects

chemokine receptor CCR7, Receptors, CCR7, Receptors, CXCR4, bcl-X Protein, Apoptosis, Breast Neoplasms, C-C chemokine receptor type 7, Mice, SCID, Metastasis, Mice, Chemokine receptor, Cell Line, Tumor, Animals, Humans, Medicine, Anoikis, Neoplasm Metastasis, Molecular Biology, Adaptor Proteins, Signal Transducing, Chemokine CCL21, business.industry, chemokine receptor CXCR4, Cancer, Cell Biology, medicine.disease, Chemokine CXCL12, Extracellular Matrix, immunoglobulin enhancer binding protein, Gene Knockdown Techniques, Cancer cell, Immunology, Cancer research, Female, RNA Interference, Signal transduction, business, Signal Transduction, CCL21

Abstract

Chemokine receptors are essential mediators of the metastatic spread in various cancer types; however their precise function in the development of secondary tumors remains poorly understood. We report here a novel property of the chemokine receptors CXCR4 and CCR7 in inhibiting detachment-induced cell death - anoikis, which is believed to be one of the major blocks in the metastatic spread of various neoplasms. Activation of these chemokine receptors by their respective ligands, CXCL12 and CCL21 specifically reduced the sensitivity of metastatic breast cancer cells to anoikis by a distinct mechanism of selective regulation of pro-apoptotic Bmf and anti-apoptotic Bcl-xL proteins. Consequently, functional CXCR4 and CCR7 increased cell survival in the absence of correct ECM attachment both in vitro and in vivo. We also demonstrated that preventing chemokine-induced reduction in Bmf levels significantly attenuated breast cancer metastasis in an experimental mouse model. These results provide evidence for a previously unknown axis in malignant tumors, which connects chemokine receptors with deregulated apoptosis in the absence of the appropriate cell - ECM interaction and may offer novel targets for therapeutic intervention for the treatment of metastatic breast and potentially other tumors. Refereed/Peer-reviewed

Published

2009

19. Cutting Edge: Activity of Human Adult Microglia in Response to CC Chemokine Ligand 21

Subjects

chemokine receptor CCR7, gamma interferon inducible protein 10, microglia, animal cell, protein binding, immune response, animal tissue, immunocytochemistry, controlled study, human, chemotaxis, lymphoid tissue, protein expression, mouse, nonhuman, beta chemokine, secondary lymphoid tissue chemokine, adult, human cell, chemokine receptor CXCR3, article, hemic and immune systems, monokine, nucleotide sequence, human tissue, unclassified drug, priority journal, CXCL9 chemokine, cell function, gamma interferon, signal transduction

Abstract

The approximately 50 known chemokines are classified in distinct subfamilies: CXC, CC, CX3C, and C. Although the signaling of chemokines often is promiscuous, signaling events between members of these distinct chemokine classes are hardly observed. The only known exception so far is the murine CC chemokine ligand (CCL)21 (secondary lymphoid tissue chemokine, Exodus-2, 6Ckine), which binds and activates the murine CXC chemokine receptor CXCR3. However, this exception has not been found in humans. In this study, we provide evidence that human CCL21 is a functional ligand for endogenously expressed CXCR3 in human adult microglia. In absence of CCR7 expression, CCL21 induced chemotaxis of human microglia with efficiency similar to the CXCR3 ligands CXC chemokine ligand 9 (monokine induced by IFN-3γ) and CXC chemokine ligand 10 (IFN-γ-inducible protein-10). Because human CCL21 did not show any effects in CXCR3-transfected HEK293 cells, it is indicated that CXCR3 signaling depends on the cellular background in which the CXCR3 is expressed.

Published

2004

20. Cutting Edge: Activity of Human Adult Microglia in Response to CC Chemokine Ligand 21

Author

Hendrikus Boddeke, Sandra Hulshof, Ineke M. Dijkstra, Paul van der Valk, Knut Biber, Translational Immunology Groningen (TRIGR), and Molecular Neuroscience and Ageing Research (MOLAR)

Subjects

chemokine receptor CCR7, gamma interferon inducible protein 10, animal cell, protein binding, C-C chemokine receptor type 6, Ligands, immune response, Mice, Chemokine receptor, immunocytochemistry, Immunology and Allergy, CXC chemokine receptors, Cells, Cultured, beta chemokine, Reverse Transcriptase Polymerase Chain Reaction, Chemotaxis, article, Brain, hemic and immune systems, unclassified drug, CXCL2, priority journal, Chemokines, CC, CXCL9, Receptors, Chemokine, gamma interferon, Microglia, Signal Transduction, Adult, Receptors, CCR7, Receptors, CXCR3, Immunology, Biology, Transfection, animal tissue, Cell Line, Animals, Humans, controlled study, human, CXCL13, lymphoid tissue, protein expression, mouse, Inflammation, nonhuman, Chemokine CCL21, secondary lymphoid tissue chemokine, human cell, chemokine receptor CXCR3, monokine, nucleotide sequence, Molecular biology, human tissue, CXCL9 chemokine, XCL2, cell function, CCL21

Abstract

The approximately 50 known chemokines are classified in distinct subfamilies: CXC, CC, CX3C, and C. Although the signaling of chemokines often is promiscuous, signaling events between members of these distinct chemokine classes are hardly observed. The only known exception so far is the murine CC chemokine ligand (CCL)21 (secondary lymphoid tissue chemokine, Exodus-2, 6Ckine), which binds and activates the murine CXC chemokine receptor CXCR3. However, this exception has not been found in humans. In this study, we provide evidence that human CCL21 is a functional ligand for endogenously expressed CXCR3 in human adult microglia. In absence of CCR7 expression, CCL21 induced chemotaxis of human microglia with efficiency similar to the CXCR3 ligands CXC chemokine ligand 9 (monokine induced by IFN-γ) and CXC chemokine ligand 10 (IFN-γ-inducible protein-10). Because human CCL21 did not show any effects in CXCR3-transfected HEK293 cells, it is indicated that CXCR3 signaling depends on the cellular background in which the CXCR3 is expressed.

Published

2004

21. T Lymphocyte Antigen 4-Modified Dendritic Cell Therapy for Asthmatic Mice Guided by the CCR7 Chemokine Receptor

Author

Yan Chen, Yongming Wang, and Zhou Fu

Subjects

chemokine receptor CCR7, medicine.medical_treatment, Lymphocyte, precision-guided immunotherapy, C-C chemokine receptor type 7, lcsh:Chemistry, Chemokine receptor, Mice, immune system diseases, Cell Movement, CTLA-4 Antigen, lcsh:QH301-705.5, Spectroscopy, the cytotoxic T lymphocyte antigen 4 (CTLA4), Mice, Inbred BALB C, hemic and immune systems, General Medicine, Computer Science Applications, medicine.anatomical_structure, Cytokine, Female, Immunotherapy, Receptors, CCR7, Immunoglobulin gamma-Chains, Genetic Vectors, chemical and pharmacologic phenomena, Biology, Catalysis, Article, Adenoviridae, Inorganic Chemistry, Interferon-gamma, medicine, dendritic cells (DCs), Animals, Physical and Theoretical Chemistry, Molecular Biology, Organic Chemistry, Dendritic Cells, recombinant viral vectors, asthma, Immunoglobulin Fc Fragments, lcsh:Biology (General), lcsh:QD1-999, Immunology, Humoral immunity, Interleukin-4, CC chemokine receptors, CD80

Abstract

The CD80/CD86-CD28 axis is a critical pathway for immuno-corrective therapy, and the cytotoxic T lymphocyte antigen 4 (CTLA4) is a promising immunosuppressor targeting the CD80/CD86-CD28 axis, however, its use for asthma therapy needs further optimization. A human CTLA4 fused with the IgCγ Fc (CTLA4Ig) and mouse CC chemokine receptor type7 (CCR7) coding sequences were inserted into a recombinant adenovirus (rAdV) vector to generate rAdV-CTLA4Ig and rAdV-CCR7. The naive dendritic cells (DCs) were infected with these rAdVs to ensure CCR7 and CTLA4Ig expression. The therapeutic effects of modified DCs were evaluated. rAdV-CTLA4Ig and rAdV-CCR7 infected DCs improved all asthma symptoms. Inflammatory cell infiltration and cytokine analysis showed that rAdV-CTLA4Ig and rAdV-CCR7-modified DC therapy reduced the number of eosinophils and lymphocyte and neutrophil infiltration in the lung. Interestingly, assessment of the humoral immunity showed that the IL-4 and IFNγ levels of the rAdV-CTLA4Ig and rAdV-CCR7-modified DC-treated mice decreased significantly and did not reverse the Th1/Th2 balance. DCs expressing CCR7 displayed guidance ability for DC migration, primarily for DCs in the inflammatory lung. Additionally, the rAdVs caused an inflammatory response by inducing DC differentiation, inflammatory cell infiltration and changes in cytokines, however, mice transplanted with rAdV-green fluorescent protein (GFP)-infected DCs displayed no asthma manifestations. In conclusion, CTLA4Ig-modified DCs exhibited a therapeutic effect on asthma, and CCR7 may guide DC homing. The combination of these two molecules may be a model for precision-guided immunotherapy.

Published

2014

22. A mechanistic role for leptin in human dendritic cell migration: differences between ileum and colon in health and Crohn's disease

Author

Andrew J. Stagg, Elizabeth R. Mann, A Jones, N R English, Aravinth U. Murugananthan, Hafid O. Al-Hassi, Michael A. Kamm, David Bernardo, Stella C. Knight, Alex I. Blakemore, Naila Arebi, and Ailsa Hart

Subjects

Leptin, CHEMOKINE RECEPTOR CCR7, Adipose tissue, C-C chemokine receptor type 7, Antigens, CD40, Crohn Disease, Cell Movement, Antigens, CD80, Immunology and Allergy, Mesenteric lymph nodes, digestive, oral, and skin physiology, hemic and immune systems, 11 Medical And Health Sciences, Antigens, CD86, medicine.anatomical_structure, ADIPOSE-TISSUE, Cellular Microenvironment, B7-1 Antigen, Receptors, Leptin, SIGNALING PATHWAY, medicine.symptom, Life Sciences & Biomedicine, STAT3 Transcription Factor, medicine.medical_specialty, Receptors, CCR7, INTESTINAL INFLAMMATION, Colon, Immunology, Adipokine, Inflammation, chemical and pharmacologic phenomena, Biology, Article, STIMULATORY CAPACITY, MATURATION, Ileum, Internal medicine, medicine, Humans, CD40 Antigens, Dendritic cell migration, Leptin receptor, Science & Technology, CYTOKINE PRODUCTION, IN-VITRO, Dendritic Cells, 06 Biological Sciences, MESENTERIC LYMPH-NODES, Endocrinology, Case-Control Studies, B7-2 Antigen, INFLAMMATORY-BOWEL-DISEASE

Abstract

Dendritic cells (DC) migrate to lymph nodes on expression of C-C motif chemokine receptor 7 (CCR7) and control immune activity. Leptin, an immunomodulatory adipokine, functions via leptin receptors, signaling via the long isoform of receptor, LepRb. Leptin promotes DC maturation and increases CCR7 expression on blood DC. Increased mesenteric fat and leptin occur early in Crohn's disease (CD), suggesting leptin-mediated change in intestinal CCR7 expression on DC as a pro-inflammatory mechanism. We have demonstrated CCR7 expression and capacity to migrate to its ligand macrophage inflammatory protein 3beta in normal human ileal DC but not colonic or blood DC. In CD, functional CCR7 was expressed on DC from all sites. Only DC populations containing CCR7-expressing cells produced LepRb; in vitro exposure to leptin also increased expression of functional CCR7 in intestinal DC in a dose-dependent manner. In conclusion, leptin may regulate DC migration from gut, in homeostatic and inflammatory conditions, providing a link between mesenteric obesity and inflammation.

Published

2012

23. LXR agonist suppresses atherosclerotic lesion growth and promotes lesion regression in apoE*3Leiden mice: Time course and mechanisms

Author

Verschuren, L., Vries de Weij, J. van der, Zadelaar, A.S.M., Kleemann, R., Kooistra, T., and TNO Kwaliteit van Leven

Subjects

chemokine receptor CCR7, Biomedical Research, fluorinated hydrocarbon, Hydrocarbons, Fluorinated, cell receptor, cholesterol blood level, Apolipoprotein E3, Receptors, Cytoplasmic and Nuclear, cholesterol diet, ABCG1 protein, mouse, Mice, Liver-X-receptor, TO-901317, n (2,2,2 trifluoroethyl) n [4 (2,2,2 trifluoro 1 hydroxy 1 trifluoromethylethyl)phenyl]benzenesulfonamide, animal, genetics, n (2,2,2 trifluoroethyl) n [4 [2,2,2 trifluoro 1 hydroxy 1 (trifluoromethoxy)ethyl]phenyl]benzenesulfonamide, Hermes antigen, Sulfonamides, ABC transporter A1, disease course, Anticholesteremic Agents, lipoprotein, hypocholesterolemic agent, endothelial leukocyte adhesion molecule 1, Intercellular Adhesion Molecule-1, Antigens, CD44, intercellular adhesion molecule 1, DNA-Binding Proteins, immunoglobulin enhancer binding protein, female, priority journal, Health, immunohistochemistry, monocyte, lipids (amino acids, peptides, and proteins), ABC transporter, triacylglycerol, E-Selectin, drug potency, liver X receptor, endothelium, Lipoproteins, animal experiment, Mice, Transgenic, macrophage, remission, lipid, sulfonamide, drug mechanism, Animals, controlled study, protein expression, mouse, ABC transporter G1, Inflammation, Serum Amyloid A Protein, nonhuman, drug potentiation, Macrophages, animal model, cholesterol, serum amyloid A, cell adhesion, Atherosclerosis, triacylglycerol blood level, DNA binding protein, liver X receptor agonist, transgenic mouse, apolipoprotein E3 (Leidein), pathology, ATP-Binding Cassette Transporters, cell adhesion molecule, metabolism

Abstract

The aim of this study was to define the anti-atherosclerotic role of liver-X-receptors (LXRs) under lesion progressive and lesion regressive conditions, to establish a temporal line of events, and to gain insights into the mechanisms underlying the anti-atherogenic potency of LXRs. We used apoE*3Leiden (E3L) mice to comprehensively and time-dependently dissect how T0901317, an LXR-agonist, inhibits initiation and progression of atherosclerotic lesions and regresses existing lipid- and macrophage-rich lesions. T0901317 suppresses lesion evolution and promotes lesion regression regarding lesion number, area, and severity. Quantitative plasma and vessel wall analyses corroborated by immunohistochemical evaluation of the aortic lesions revealed that under progressive (high-cholesterol diet) as well as regressive (cholesterol-free diet) conditions T0901317: i) significantly increases plasma triglyceride and total cholesterol levels; ii) does not affect the systemic inflammation marker, Serum amyloid A (SAA); iii) suppresses endothelial monocyte adhesion; and iv) induces the expression of the cholesterol efflux-related genes apolipoprotein E (apoE), ATP binding cassette (ABC) transporters ABCA1 and ABCG1. Furthermore, under progressive conditions, T0901317 suppresses the vascular inflammatory status (NF-κB) and the vascular expression of adhesion molecules [E-selectin, intercellular adhesion molecule (ICAM)-1, and CD44], lowers lesional macrophage accumulation, and blocks lesion evolution at the transition from lesional stage II to III. Under regressive conditions, T0901317 induces lesional macrophage disappearance and increases the expression of the chemokine receptor CCR7, a factor functionally required for regression. The LXR-agonist T0901317 retards vascular lesion development and promotes lesion regression at several levels. The findings support that vascular LXR is a potential anti-atherosclerotic target. Copyright © 2009 by the American Society for Biochemistry and Molecular Biology, Inc.

Published

2009

24. LXR agonist suppresses atherosclerotic lesion growth and promotes lesion regression in apoE*3Leiden mice: Time course and mechanisms

Subjects

chemokine receptor CCR7, Biomedical Research, fluorinated hydrocarbon, Cytoplasmic and Nuclear, cell receptor, cholesterol blood level, Apolipoprotein E3, cholesterol diet, Transgenic, Mice, Liver-X-receptor, Fluorinated, TO-901317, Receptors, animal, genetics, CD44, Hermes antigen, Sulfonamides, ABC transporter A1, disease course, Anticholesteremic Agents, lipoprotein, 2 trifluoro 1 hydroxy 1 (trifluoromethoxy)ethyl]phenyl]benzenesulfonamide, hypocholesterolemic agent, endothelial leukocyte adhesion molecule 1, Intercellular Adhesion Molecule-1, intercellular adhesion molecule 1, DNA-Binding Proteins, immunoglobulin enhancer binding protein, female, priority journal, Health, immunohistochemistry, monocyte, lipids (amino acids, peptides, and proteins), ABC transporter, triacylglycerol, E-Selectin, drug potency, liver X receptor, n (2, endothelium, Lipoproteins, animal experiment, macrophage, 2 trifluoroethyl) n [4 [2, remission, lipid, sulfonamide, drug mechanism, Animals, controlled study, ABCG1 protein, Antigens, protein expression, mouse, ABC transporter G1, Inflammation, Serum Amyloid A Protein, nonhuman, drug potentiation, Macrophages, animal model, 2 trifluoroethyl) n [4 (2, cholesterol, serum amyloid A, cell adhesion, Atherosclerosis, triacylglycerol blood level, DNA binding protein, Hydrocarbons, liver X receptor agonist, transgenic mouse, 2 trifluoro 1 hydroxy 1 trifluoromethylethyl)phenyl]benzenesulfonamide, apolipoprotein E3 (Leidein), pathology, ATP-Binding Cassette Transporters, cell adhesion molecule, metabolism

Abstract

The aim of this study was to define the anti-atherosclerotic role of liver-X-receptors (LXRs) under lesion progressive and lesion regressive conditions, to establish a temporal line of events, and to gain insights into the mechanisms underlying the anti-atherogenic potency of LXRs. We used apoE*3Leiden (E3L) mice to comprehensively and time-dependently dissect how T0901317, an LXR-agonist, inhibits initiation and progression of atherosclerotic lesions and regresses existing lipid- and macrophage-rich lesions. T0901317 suppresses lesion evolution and promotes lesion regression regarding lesion number, area, and severity. Quantitative plasma and vessel wall analyses corroborated by immunohistochemical evaluation of the aortic lesions revealed that under progressive (high-cholesterol diet) as well as regressive (cholesterol-free diet) conditions T0901317: i) significantly increases plasma triglyceride and total cholesterol levels; ii) does not affect the systemic inflammation marker, Serum amyloid A (SAA); iii) suppresses endothelial monocyte adhesion; and iv) induces the expression of the cholesterol efflux-related genes apolipoprotein E (apoE), ATP binding cassette (ABC) transporters ABCA1 and ABCG1. Furthermore, under progressive conditions, T0901317 suppresses the vascular inflammatory status (NF-κB) and the vascular expression of adhesion molecules [E-selectin, intercellular adhesion molecule (ICAM)-1, and CD44], lowers lesional macrophage accumulation, and blocks lesion evolution at the transition from lesional stage II to III. Under regressive conditions, T0901317 induces lesional macrophage disappearance and increases the expression of the chemokine receptor CCR7, a factor functionally required for regression. The LXR-agonist T0901317 retards vascular lesion development and promotes lesion regression at several levels. The findings support that vascular LXR is a potential anti-atherosclerotic target. Copyright © 2009 by the American Society for Biochemistry and Molecular Biology, Inc.

Published

2009

25. Monocyte-derived dendritic cells loaded with a mixture of apoptotic/ necrotic melanoma cells efficiently cross-present gp100 and MART-1 antigens to specific CD8+ T lymphocytes

Author

von Euw, E.M., Barrio, M.M., Furman, D., Bianchini, M., Levy, E.M., Yee, C., Li, Y., Wainstok, R., and Mordoh, J.

Subjects

chemokine receptor CCR7, cell cloning, HLA antigen class 3, Time Factors, HLA antigen class 2, cell migration, HLA antigen class 1, B7 antigen, glycoprotein gp 100, cell maturation, radiation exposure, Apoptosis, cytotoxic T lymphocyte, CD8-Positive T-Lymphocytes, Monocytes, CD40 antigen, fluorescence activated cell sorting, necrosis, immunology, Epitopes, cell motion, Cell Movement, dendritic cell vaccine, membrane protein, CD8+ T lymphocyte, CD83 antigen, Melanoma, time, epitope, Membrane Glycoproteins, HLA A antigen, drug effect, article, SILV protein, human, phagocytosis, Cell Differentiation, melan A, CCR7 protein, human, ultrastructure, Interleukin-12, unclassified drug, Interleukin-10, Neoplasm Proteins, cell death, cell surface, cytokine release, dextran, monocyte, gamma interferon, cancer vaccine, coculture, gp100 Melanoma Antigen, melanoma cell, Receptors, CCR7, in vitro study, HLA antigen, cell kinetics, dendritic cell, fluorescein isothiocyanate, CD86 antigen, Cross-Priming, MART-1 Antigen, tumor protein, Antigens, Neoplasm, Cell Line, Tumor, Humans, controlled study, human, electron microscopy, cross presentation, human cell, chemokine, gamma radiation, tumor cell line, Dendritic Cells, vaccination, gamma irradiation, Coculture Techniques, Gamma Rays, cytology, antigen specificity, Chemokine CCL19, interleukin 12, macrophage inflammatory protein 3beta, melanocyte protein Pmel 17, antigen expression, cell vacuole, pathology, interleukin 10, tumor antigen, MLANA protein, human, upregulation

Abstract

Background: In the present study, we demonstrate, in rigorous fashion, that human monocyte-derived immature dendritic cells (DCs) can efficiently cross-present tumor-associated antigens when co-cultured with a mixture of human melanoma cells rendered apoptotic/necrotic by γ irradiation (Apo-Nec cells). Methods: We evaluated the phagocytosis of Apo-Nec cells by FACS after PKH26 and PKH67 staining of DCs and Apo-Nec cells at different times of coculture. The kinetics of the process was also followed by electron microscopy. DCs maturation was also studied monitoring the expression of specific markers, migration towards specific chemokines and the ability to cross-present in vitro the native melanoma-associated Ags MelanA/MART-1 and gp100. Results: Apo-Nec cells were efficiently phagocytosed by immature DCs (iDC) (55 ± 10.5%) at 12 hs of coculture. By 12-24 hs we observed digested Apo-Nec cells inside DCs and large empty vacuoles as part of the cellular processing. Loading with Apo-Nec cells induced DCs maturation to levels achieved using LPS treatment, as measured by: i) the decrease in FITC - Dextran uptake (iDC: 81 ± 5%; DC/Apo-Nec 33 ± 12%); ii) the cell surface up-regulation of CD80, CD86, CD83, CCR7, CD40, HLA-I and HLA-II and iii) an increased in vitro migration towards MIP-3β. DC/Apo-Nec isolated from HLA-A*0201 donors were able to induce >600 pg/ml IFN-γ secretion of CTL clones specific for MelanA/MART-1 and gp100 Ags after 6 hs and up to 48 hs of coculture, demonstrating efficient cross-presentation of the native Ags. Intracellular IL-12 was detected in DC/Apo-Nec 24 hs post-coculture while IL-10 did not change. Conclusion: We conclude thatthe use of a mixture of four apoptotic/ necrotic melanoma cell lines is a suitable source of native melanoma Ags that provides maturation signals for DCs, increases migration to MIP-3β and allows Ag cross-presentation. This strategy could be exploited for vaccination of melanoma patients. © 2007 von Euw et al; licensee BioMed Central Ltd. Fil:von Euw, E.M. Universidad de Buenos Aires. Facultad de Ciencias Exactas y Naturales; Argentina. Fil:Barrio, M.M. Universidad de Buenos Aires. Facultad de Ciencias Exactas y Naturales; Argentina. Fil:Levy, E.M. Universidad de Buenos Aires. Facultad de Ciencias Exactas y Naturales; Argentina.

Published

2007

26. Skin irritants and contact sensitizers induce Langerhans cell migration and maturation at irritant concentration

Subjects

Contact allergen, Contact allergy, chemical and pharmacologic phenomena, Dermatitis, Immunopathology, Langerhans cell, Explant, Article, Tissue Culture Techniques, Skin allergy, Chemokine receptor CCR7, Cell Movement, Maturation, T6 antigen, Contact sensitization, Contact, Hypersensitivity reaction, Humans, Cell migration, Human tissue, Quantitative analysis, CD83 antigen, Migration, Irritant agent, Skin, integumentary system, Skin irritation, hemic and immune systems, Cell Differentiation, Allergens, Cell count, Skin Irritancy Tests, Immunohistochemistry, Occupational, Skin culture, Langerhans Cells, Irritants, Lymph node, Female, Lymph Nodes, Cell maturation, Controlled study, Dendritic cell, Human

Abstract

Skin irritants and contact allergens reduce the number of Langerhans cells (LCs). It has been assumed that this reduction is due their migration to the draining lymph node (LN) for initiating immune sensitization in a host. Skin irritation, however, as opposed to contact allergy is not considered to be an immunological disease. Nevertheless, skin irritants are also known for their adjuvant-like effects on contact allergy, resulting in skin hypersensitivity reactions like toxic dermatitis. The human organotypic skin explant culture (hOSEC) model is used to study the characteristics of chemical-induced migration of CD1a+ LCs out of the epidermis in relation to irritancy or toxicity. We analysed cells emigrating out of hOSEC for CD1a+ LCs, CD83+ mature dendritic cells (DCs) and CCR7+ LN homing cells. After exposure to a toxic concentration of a non-immunogenic irritant, an increase of CD1a+CD83+ LCs was found in the culture medium. A non-toxic concentration of an sensitizer induced an increase of CD1a+ cells. About 50% of skin emigrating CD1a+ LCs were CD83- (immature) but all were CCR7+. Skin irritation by both non-allergenic and allergenic compounds induces LC migration and maturation. In contrast, only allergenic compounds induced LC migration with partial maturation at subtoxic concentration. This effectively demonstrates that irritation is physiologically needed stimuli for inducing LC maturation. © Blackwell Munksgaard, 2006.

Published

2006

27. Skin irritants and contact sensitizers induce Langerhans cell migration and maturation at irritant concentration

Author

Jacobs, J.J.L., Lehé, C.L., Hasegawa, H., Elliott, G.R., Das, P.K., and TNO Defensie en Veiligheid

Subjects

Contact allergen, Contact allergy, chemical and pharmacologic phenomena, Immunopathology, Dermatitis, Contact, Langerhans cell, Explant, Article, Tissue Culture Techniques, Skin allergy, Chemokine receptor CCR7, Cell Movement, Maturation, T6 antigen, Contact sensitization, Hypersensitivity reaction, Humans, Cell migration, Human tissue, Quantitative analysis, CD83 antigen, Migration, Irritant agent, Skin, integumentary system, Skin irritation, hemic and immune systems, Cell Differentiation, Allergens, Cell count, Skin Irritancy Tests, Immunohistochemistry, Skin culture, Dermatitis, Occupational, Langerhans Cells, Irritants, Lymph node, Female, Lymph Nodes, Cell maturation, Controlled study, Dendritic cell, Human

Abstract

Skin irritants and contact allergens reduce the number of Langerhans cells (LCs). It has been assumed that this reduction is due their migration to the draining lymph node (LN) for initiating immune sensitization in a host. Skin irritation, however, as opposed to contact allergy is not considered to be an immunological disease. Nevertheless, skin irritants are also known for their adjuvant-like effects on contact allergy, resulting in skin hypersensitivity reactions like toxic dermatitis. The human organotypic skin explant culture (hOSEC) model is used to study the characteristics of chemical-induced migration of CD1a+ LCs out of the epidermis in relation to irritancy or toxicity. We analysed cells emigrating out of hOSEC for CD1a+ LCs, CD83+ mature dendritic cells (DCs) and CCR7+ LN homing cells. After exposure to a toxic concentration of a non-immunogenic irritant, an increase of CD1a+CD83+ LCs was found in the culture medium. A non-toxic concentration of an sensitizer induced an increase of CD1a+ cells. About 50% of skin emigrating CD1a+ LCs were CD83- (immature) but all were CCR7+. Skin irritation by both non-allergenic and allergenic compounds induces LC migration and maturation. In contrast, only allergenic compounds induced LC migration with partial maturation at subtoxic concentration. This effectively demonstrates that irritation is physiologically needed stimuli for inducing LC maturation. © Blackwell Munksgaard, 2006.

Published

2006

28. Involvement of beta-chemokines in the development of inflammatory demyelination.

Author

Banisor, Ileana, Leist, Thomas P, Kalman, Bernadette, Banisor, Ileana, Leist, Thomas P, and Kalman, Bernadette

Abstract

The importance of beta-chemokines (or CC chemokine ligands - CCL) in the development of inflammatory lesions in the central nervous system of patients with multiple sclerosis and rodents with experimental allergic encephalomyelitis is strongly supported by descriptive studies and experimental models. Our recent genetic scans in families identified haplotypes in the genes of CCL2, CCL3 and CCL11-CCL8-CCL13 which showed association with multiple sclerosis. Complementing the genetic associations, we also detected a distinct regional expression regulation for CCL2, CCL7 and CCL8 in correlation with chronic inflammation in multiple sclerosis brains. These observations are in consensus with previous studies, and add new data to support the involvement of CCL2, CCL7, CCL8 and CCL3 in the development of inflammatory demyelination. Along with our own data, here we review the literature implicating CCLs and their receptors (CCRs) in multiple sclerosis and experimental allergic encephalomyelitis. The survey reflects that the field is in a rapid expansion, and highlights some of the pathways which might be suitable to pharmaceutical interventions.

Published

2005

29. Interaction between MALAT-1, CCR7 and correlated genes in oral squamous cell carcinoma.

Author

Xu Z, Han X, Tang Z, Tian G, Gao J, and Xu X

Abstract

Objective: This study focuses on the feasible molecular mechanism of the interaction between MALAT-1, CCR7 and related genes in oral squamous cell carcinoma, to find new target molecules that can block the lymph node metastasis., Methods: The expression of MALAT-1, miRNA-320s, SRSF1, YB-1 and CCR7 were detected in T3/T4-phase OSCC tissues of two groups with or without lymph node metastasis using real-time qPCR. CO-IP and western blot to test the interaction of RNAs (MALAT-1, miRNA-320s) with SRSF1 protein or YB-1 were evaluated by CO-IP, Western blot and real-time qPCR. The expression change of chemokine receptor CCR7 were investigated using CO-IP, Western blot and real-time qPCR after silencing miRNA-320d (one of the miRNA-320s family members) by transfection of miRNA mimics to explore related signaling pathway., Results: The expression levels of MALAT-1 SRSF1 and CCR7 in OSCC tissues with were differentially higher compared with those of samples without lymph node metastasis as well as para-carcinoma tissues, exclusive of miRNA-320d. Moreover, it is confirmed that the target RNA (MALAT-1, miRNA-320s) and SRSF1 protein can combine with each other, based on the statistically significant difference compared with negative control group ( P <0.05). In addition, the expression of CCR7 was higher than the negative control group after silencing miRNA-320d., Conclusion: SRSF1 is likely to mediate the interactive relationship between MALAT-1 and miRNA-320d. CCR7 expression can be distinctly increased by silencing miRNA-320d. The effect of long-chain non-coding RNA MALAT-1 on chemokine receptor CCR7 and possibly further influence on lymph node metastasis of oral squamous cell carcinoma are revealed in molecular level to offer help for prevention and treatment of OSCC in future., Competing Interests: None., (IJCEP Copyright © 2017.)

Published

2017

30. Dry eye-induced CCR7+CD11b+ cell lymph node homing is induced by COX-2 activities.

Author

Ji YW, Seo Y, Choi W, Yeo A, Noh H, Kim EK, and Lee HK

Subjects

Animals, Cell Proliferation, Cornea pathology, Cyclooxygenase 2 metabolism, Disease Models, Animal, Dry Eye Syndromes genetics, Dry Eye Syndromes metabolism, Female, Flow Cytometry, Immunohistochemistry, Lymph Nodes immunology, Lymph Nodes metabolism, Mice, Mice, Inbred C57BL, Real-Time Polymerase Chain Reaction, Receptors, CCR7 metabolism, Receptors, Lymphocyte Homing immunology, Receptors, Lymphocyte Homing metabolism, CD11b Antigen immunology, Cornea metabolism, Cyclooxygenase 2 genetics, Dry Eye Syndromes immunology, Gene Expression Regulation, RNA, Messenger genetics, Receptors, CCR7 immunology

Abstract

Purpose: We aimed to determine the role of CCR7+CD11b+ cell lymph node (LN) homing and T-cell differentiation in dry eye (DE)-induced immunopathogenesis and investigate the therapeutic effects of cyclooxygenase-2 (COX-2) and prostaglandin E2/eicosanoid-prostanoid (PGE2/EP) inhibitors against DE., Methods: Six-week-old female C57BL/6 mice were housed in a controlled-environment chamber and administered topical selective COX-2 inhibitors or EP2 antagonists. Expression of major histocompatibility complex (MHC)-IIhigh, CD11b+, CCR7+, IFN-γ+, IL-17+, and CD4+ in the corneas and draining LNs was evaluated using flow cytometry. Mixed lymphocyte reactions (MLRs) with carboxyfluorescein diacetate succinimidyl ester labeling and intracellular cytokine staining were used to verify DE-induced corneal dendritic cell function. mRNA expression of COX-2, EPs, and proinflammatory cytokines in ocular surface was evaluated using quantitative RT-PCR and immunohistochemical staining., Results: Dry eye significantly increased MHC-IIhighCD11b+ and CCR7+CD11b+ cells in the cornea and LNs, and MLR revealed CCR7+CD11b+ cells from DE corneas stimulated IL-17+CD4+ cell proliferation. mRNA levels of COX-2, EP2, IFN-γ, TNF-α, IL-6, and IL-17 were significantly higher in DE ocular surface but were suppressed by topical COX-2 inhibitors and EP2-specific blockers. Immunohistochemical staining showed COX-2 and matrix metalloproteinase expression in DE corneal epithelia that was diminished by both topical treatments. Furthermore, both topical treatments significantly reduced frequencies of MHC-IIhigh, CD11b+, and CCR7+CD11b+ cells in the corneas and LNs, but also IL-17+CD4+ cells in LNs., Conclusions: Topical COX-2/EP2 treatment reduces CCR7+CD11b+ cells on the ocular surface with inhibition of cellular LN homing and suppresses Th17 immune response, suggesting the COX-2/PGE2/EP axis contributes to immuno-inflammatory pathogenesis on the ocular surface and may be a novel therapeutic target in DE., (Copyright 2014 The Association for Research in Vision and Ophthalmology, Inc.)

Published

2014