Your search keyword '"antigen-presentation"' showing total 121 results

1. Triphenyl phosphate‐induced macrophages dysfunction by activation TLR4‐mediated ERK/NF‐κB pathway.

Author

Lin, Zeheng, Zhang, Wei, Li, Xing, Du, Bohai, Li, Tianlan, He, Haoqi, Lu, Xianzhu, Zhang, Chunmei, Liu, Yiwa, Ni, Jindong, Li, Li, and Shi, Ming

Subjects

MACROPHAGE activation, INFLAMMATORY mediators, FIREPROOFING agents, PHAGOCYTOSIS, IMMUNE system

Abstract

Triphenyl phosphate (TPHP) is one of the most widely used organic phosphorus flame retardants and is ubiquitous in the environment. Studies have been reported that TPHP may lead to obesity, neurotoxicity and reproductive toxicity, but its impact on the immune system is almost blank. The present study was aimed to investigate the potential immunotoxicity of TPHP on macrophages and its underlying mechanism. The results demonstrated for the first time that TPHP (12.5, 25, and 50 μM)‐induced F4/80+CD11c+ phenotype of RAW 264.7 macrophages, accompanied by increased mRNA levels of inflammatory mediators, antigen‐presenting genes (Cd80, Cd86, and H2‐Aa), and significantly enhanced the phagocytosis of macrophage. Meanwhile, TPHP increased the expression of Toll‐like receptor 4 (TLR4), and its co‐receptor CD14, leading to significant activation of the downstream ERK/NF‐κB pathway. However, co‐exposure of cells to TAK‐242, a TLR4 inhibitor, suppressed TPHP‐induced F4/80+CD11c+ phenotype, and down‐regulated inflammatory mediators and antigen‐presentation related genes, via blocked the TLR4/ERK/NF‐κB pathway. Taken together, our results suggested that TPHP could induce macrophage dysfunction through activating TLR4‐mediated ERK/NF‐κB signaling pathway, and it may be the potential reason for health‐threatening consequences. [ABSTRACT FROM AUTHOR]

Published

2023

2. Teleost fish IgM+ plasma-like cells possess IgM-secreting, phagocytic, and antigenpresenting capacities.

Author

Liting Wu, Yanjian Yang, Along Gao, Jun Li, and Jianmin Ye

Subjects

PLASMA cells, B cells, HUMORAL immunity, ENDOPLASMIC reticulum, MACROPHAGES

Abstract

Plasma cells are terminally differentiated antibody-secreting B lymphocytes that contribute to humoral immunity by producing large numbers of antibodies. Increasing evidence suggests that teleost fish B cells share certain characteristics with mammalian B1 B cells, including antibody-secreting, phagocytic, and antigen-presenting capacities. However, the difference between mature B cells and plasma cells remains unclear. In this study, we found that, based on their light-scattering characteristics, tilapia anterior kidney (AK) leukocytes can be categorized into two IgM+ B-cell subsets: the lymphoid (L) gate and granulocyte–monocyte/macrophage (G-M) subsets. G-M gate cells are more numerous than L-gate cells and have higher mean fluorescence, but lower forward scatter and side scatter. We analyzed the morphological and ultrastructural features of sorted IgM+ cells and found that L-gate IgM+ cells have a high nucleus–cytoplasm ratio and lymphocyte-like morphology, whereas G-M gate IgM+ cells have a small nucleus, more abundant endoplasmic reticulum, and a larger number of mitochondria, and have a plasma cell-like or macrophage-like morphology. To further characterize the cell types, we examined the specific patterns of expression of B-cell- and T-cell-related genes. We found that B-cell-specific genes were expressed by both L-gate and G-M gate IgM+ cells, and that G-M gate IgM+ cells secreted extremely high levels of IgM. However, T-cell-related genes were highly expressed only in L-gate IgM– cells. These results suggest that G-M gate IgM+ cells are similar to plasma-like cells, with high antibody-secreting capacity. Given that G-M gate cells include the granulocyte, monocyte, and macrophage cell types, but not B cells, monocyte/macrophage markers were used to investigate the cell types further. A macrophage receptor with a collagenous structure was frequently observed, and macrophage-expressed gene-1 was highly expressed, in the G-M gate IgM+ cells. Phagocytic capacity, as determined by ingestion of beads or bacteria, was significantly higher in G-M gate IgM+ cells than in L-gate IgM+ cells, as was antigen-processing capacity. Our findings show that tilapia AK leukocytes can be divided into two IgM+ B-cell subsets and that G-M gate IgM+ cells resemble plasma-like cells, having high antibody-secreting, phagocytic, and antigen-presenting capacities. Thus, this study increases our understanding of the functions of teleost fish plasmalike cells. [ABSTRACT FROM AUTHOR]

Published

2022

3. Teleost fish IgM+ plasma-like cells possess IgM-secreting, phagocytic, and antigen-presenting capacities

Author

Liting Wu, Yanjian Yang, Along Gao, Jun Li, and Jianmin Ye

Subjects

teleost fish, anterior kidney, IgM+ B cell, antibody-secreting, phagocytosis, antigen-presentation, Immunologic diseases. Allergy, RC581-607

Abstract

Plasma cells are terminally differentiated antibody-secreting B lymphocytes that contribute to humoral immunity by producing large numbers of antibodies. Increasing evidence suggests that teleost fish B cells share certain characteristics with mammalian B1 B cells, including antibody-secreting, phagocytic, and antigen-presenting capacities. However, the difference between mature B cells and plasma cells remains unclear. In this study, we found that, based on their light-scattering characteristics, tilapia anterior kidney (AK) leukocytes can be categorized into two IgM+ B-cell subsets: the lymphoid (L) gate and granulocyte–monocyte/macrophage (G-M) subsets. G-M gate cells are more numerous than L-gate cells and have higher mean fluorescence, but lower forward scatter and side scatter. We analyzed the morphological and ultrastructural features of sorted IgM+ cells and found that L-gate IgM+ cells have a high nucleus–cytoplasm ratio and lymphocyte-like morphology, whereas G-M gate IgM+ cells have a small nucleus, more abundant endoplasmic reticulum, and a larger number of mitochondria, and have a plasma cell-like or macrophage-like morphology. To further characterize the cell types, we examined the specific patterns of expression of B-cell- and T-cell-related genes. We found that B-cell-specific genes were expressed by both L-gate and G-M gate IgM+ cells, and that G-M gate IgM+ cells secreted extremely high levels of IgM. However, T-cell-related genes were highly expressed only in L-gate IgM– cells. These results suggest that G-M gate IgM+ cells are similar to plasma-like cells, with high antibody-secreting capacity. Given that G-M gate cells include the granulocyte, monocyte, and macrophage cell types, but not B cells, monocyte/macrophage markers were used to investigate the cell types further. A macrophage receptor with a collagenous structure was frequently observed, and macrophage-expressed gene-1 was highly expressed, in the G-M gate IgM+ cells. Phagocytic capacity, as determined by ingestion of beads or bacteria, was significantly higher in G-M gate IgM+ cells than in L-gate IgM+ cells, as was antigen-processing capacity. Our findings show that tilapia AK leukocytes can be divided into two IgM+ B-cell subsets and that G-M gate IgM+ cells resemble plasma-like cells, having high antibody-secreting, phagocytic, and antigen-presenting capacities. Thus, this study increases our understanding of the functions of teleost fish plasma-like cells.

Published

2022

4. Neutrophils-typical atypical antigen presenting cells?

Author

Polak, Dominika and Bohle, Barbara

Subjects

*ANTIGEN presenting cells, *T cell receptors, *T cells, *MAJOR histocompatibility complex, *ANTIMICROBIAL peptides, *REACTIVE oxygen species

Abstract

Neutrophils are the most abundant cells of the immune system and key in combating infections through phagocytosis, reactive oxygen species, neutrophil extracellular traps, and secretion of cytokines and antimicrobial peptides. Beyond this, they may influence the adaptive immune response by modulating CD4+ T cell responses. In response to cytokines, mainly GM-CSF, but also IFN-γ and TNF-α, neutrophils express major histocompatibility complex class II molecules on their surface. However, to function as antigen-presenting cells for CD4+ T cells, more requirements need to be fulfilled, like antigen internalization, processing into fragments containing T cell epitopes, and their presentation on the cell surface together with costimulatory molecules. Here, studies investigating the key features of antigen-presentation by neutrophils are summarized and discussed. Together, they provide evidence for a potential of neutrophils to specifically activate antigen-experienced CD4+ T cells. [ABSTRACT FROM AUTHOR]

Published

2022

5. Spotlight on TAP and its vital role in antigen presentation and cross-presentation.

Author

Mantel, Ian, Sadiq, Barzan A., and Blander, J. Magarian

Subjects

*ANTIGEN presentation, *T cells, *T cell receptors, *CYTOTOXIC T cells, *MAJOR histocompatibility complex, *ANTIGEN processing, *ONCOGENIC viruses, *PEPTIDES

Abstract

In the late 1980s and early 1990s, the hunt for a transporter molecule ostensibly responsible for the translocation of peptides across the endoplasmic reticulum (ER) membrane yielded the successful discovery of transporter associated with antigen processing (TAP) protein. TAP is a heterodimer complex comprised of TAP1 and TAP2, which utilizes ATP to transport cytosolic peptides into the ER across its membrane. In the ER, together with other components it forms the peptide loading complex (PLC), which directs loading of high affinity peptides onto nascent major histocompatibility complex class I (MHC-I) molecules that are then transported to the cell surface for presentation to CD8+ T cells. TAP also plays a crucial role in transporting peptides into phagosomes and endosomes during cross-presentation in dendritic cells (DCs). Because of the critical role that TAP plays in both classical MHC-I presentation and cross-presentation, its expression and function are often compromised by numerous types of cancers and viruses to evade recognition by cytotoxic CD8 T cells. Here we review the discovery and function of TAP with a major focus on its role in cross-presentation in DCs. We discuss a recently described emergency route of noncanonical cross-presentation that is mobilized in DCs upon TAP blockade to restore CD8 T cell cross-priming. We also discuss the various strategies employed by cancer cells and viruses to target TAP expression or function to evade immunosurveillance - along with some strategies by which the repertoire of peptides presented by cells which downregulate TAP can be targeted as a therapeutic strategy to mobilize a TAP-independent CD8 T cell response. Lastly, we discuss TAP polymorphisms and the role of TAP in inherited disorders. [ABSTRACT FROM AUTHOR]

Published

2022

6. LN Monocytes Limit DC-Poly I:C Induced Cytotoxic T Cell Response via IL-10 and Induction of Suppressor CD4 T Cells.

Author

Tewari, Anita, Prabagar, Miglena G., Gibbings, Sophie L., Rawat, Kavita, and Jakubzick, Claudia V.

Subjects

REGULATORY T cells, CYTOTOXIC T cells, INTERLEUKIN-10, MELANOMA, MONOCYTES, INFLAMMATORY mediators

Abstract

Every immune response has accelerators and brakes. Depending on the pathogen or injury, monocytes can play either role, promoting or resolving immunity. Poly I:C, a potent TLR3 ligand, licenses cross-presenting dendritic cells (DC1) to accelerate a robust cytotoxic T cells response against a foreign antigen. Poly I:C thus has promise as an adjuvant in cancer immunotherapy and viral subunit vaccines. Like DC1s, monocytes are also abundant in the LNs. They may act as either immune accelerators or brakes, depending on the inflammatory mediator they encounter. However, little is known about their contribution to adaptive immunity in the context of antigen and Poly I:C. Using monocyte-deficient and chimeric mice, we demonstrate that LN monocytes indirectly dampen a Poly I:C induced antigen-specific cytotoxic T cell response, exerting a "braking" function. This effect is mediated by IL-10 production and induction of suppressor CD4+ T cells. In a metastatic melanoma model, we show that a triple-combination prophylactic treatment consisting of anti-IL-10, tumor peptides and Poly I:C works because removing IL-10 counteracts the monocytic brake, resulting in significantly fewer tumors compared to mice treated with tumor peptides and Poly I:C alone. Finally, in human LN tissue, we observed that monocytes (unlike DCs) express high levels of IL-10, suggesting that anti-IL-10 may be an important addition to treatments. Overall, our data demonstrates that LN monocytes regulate the induction of a robust DC1-mediated immune response. Neutralization of either IL-10 or monocytes can augment Poly I:C-based treatments and enhance T cell cytotoxicity. [ABSTRACT FROM AUTHOR]

Published

2021

7. LN Monocytes Limit DC-Poly I:C Induced Cytotoxic T Cell Response via IL-10 and Induction of Suppressor CD4 T Cells

Author

Anita Tewari, Miglena G. Prabagar, Sophie L. Gibbings, Kavita Rawat, and Claudia V. Jakubzick

Subjects

dendritic cells, Ly6C+ monocytes, antigen-presentation, IL-10, cytotoxic T cells, Poly I:C, Immunologic diseases. Allergy, RC581-607

Abstract

Every immune response has accelerators and brakes. Depending on the pathogen or injury, monocytes can play either role, promoting or resolving immunity. Poly I:C, a potent TLR3 ligand, licenses cross-presenting dendritic cells (DC1) to accelerate a robust cytotoxic T cells response against a foreign antigen. Poly I:C thus has promise as an adjuvant in cancer immunotherapy and viral subunit vaccines. Like DC1s, monocytes are also abundant in the LNs. They may act as either immune accelerators or brakes, depending on the inflammatory mediator they encounter. However, little is known about their contribution to adaptive immunity in the context of antigen and Poly I:C. Using monocyte-deficient and chimeric mice, we demonstrate that LN monocytes indirectly dampen a Poly I:C induced antigen-specific cytotoxic T cell response, exerting a “braking” function. This effect is mediated by IL-10 production and induction of suppressor CD4+ T cells. In a metastatic melanoma model, we show that a triple-combination prophylactic treatment consisting of anti-IL-10, tumor peptides and Poly I:C works because removing IL-10 counteracts the monocytic brake, resulting in significantly fewer tumors compared to mice treated with tumor peptides and Poly I:C alone. Finally, in human LN tissue, we observed that monocytes (unlike DCs) express high levels of IL-10, suggesting that anti-IL-10 may be an important addition to treatments. Overall, our data demonstrates that LN monocytes regulate the induction of a robust DC1-mediated immune response. Neutralization of either IL-10 or monocytes can augment Poly I:C-based treatments and enhance T cell cytotoxicity.

Published

2021

8. CD169 Defines Activated CD14+ Monocytes With Enhanced CD8+ T Cell Activation Capacity

Author

Alsya J. Affandi, Katarzyna Olesek, Joanna Grabowska, Maarten K. Nijen Twilhaar, Ernesto Rodríguez, Anno Saris, Eline S. Zwart, Esther J. Nossent, Hakan Kalay, Michael de Kok, Geert Kazemier, Johannes Stöckl, Alfons J. M. van den Eertwegh, Tanja D. de Gruijl, Juan J. Garcia-Vallejo, Gert Storm, Yvette van Kooyk, and Joke M. M. den Haan

Subjects

monocyte, CD169, antigen-presentation, CD8+ T cell, nanovaccine, cancer, Immunologic diseases. Allergy, RC581-607

Abstract

Monocytes are antigen-presenting cells (APCs) that play diverse roles in promoting or regulating inflammatory responses, but their role in T cell stimulation is not well defined. In inflammatory conditions, monocytes frequently show increased expression of CD169/Siglec-1, a type-I interferon (IFN-I)-regulated protein. However, little is known about the phenotype and function of these CD169+ monocytes. Here, we have investigated the phenotype of human CD169+ monocytes in different diseases, their capacity to activate CD8+ T cells, and the potential for a targeted-vaccination approach. Using spectral flow cytometry, we detected CD169 expression by CD14+ CD16- classical and CD14+ CD16+ intermediate monocytes and unbiased analysis showed that they were distinct from dendritic cells, including the recently described CD14-expressing DC3. CD169+ monocytes expressed higher levels of co-stimulatory and HLA molecules, suggesting an increased activation state. IFNα treatment highly upregulated CD169 expression on CD14+ monocytes and boosted their capacity to cross-present antigen to CD8+ T cells. Furthermore, we observed CD169+ monocytes in virally-infected patients, including in the blood and bronchoalveolar lavage fluid of COVID-19 patients, as well as in the blood of patients with different types of cancers. Finally, we evaluated two CD169-targeting nanovaccine platforms, antibody-based and liposome-based, and we showed that CD169+ monocytes efficiently presented tumor-associated peptides gp100 and WT1 to antigen-specific CD8+ T cells. In conclusion, our data indicate that CD169+ monocytes are activated monocytes with enhanced CD8+ T cell stimulatory capacity and that they emerge as an interesting target in nanovaccine strategies, because of their presence in health and different diseases.

Published

2021

9. ADP‐heptose enables Helicobacter pylori to exploit macrophages as a survival niche by suppressing antigen‐presenting HLA‐II expression.

Author

Coletta, Sara, Battaggia, Greta, Della Bella, Chiara, Furlani, Matteo, Hauke, Martina, Faass, Larissa, D'Elios, Mario M., Josenhans, Christine, and de Bernard, Marina

Subjects

*HELICOBACTER pylori, *MACROPHAGES, *GASTRIC mucosa, *EPITHELIAL cells, *ANTIGEN presentation, *REGULATOR genes, *IMMUNE response

Abstract

The persistence of Helicobacter pylori in the human gastric mucosa implies that the immune response fails to clear the infection. We found that H. pylori compromises the antigen presentation ability of macrophages, because of the decline of the presenting molecules HLA‐II. Here, we reveal that the main bacterial factor responsible for this effect is ADP‐heptose, an intermediate metabolite in the biosynthetic pathway of lipopolysaccharide (LPS) that elicits a pro‐inflammatory response in gastric epithelial cells. In macrophages, it upregulates the expression of miR146b which, in turn, would downmodulate CIITA, the master regulator for HLA‐II genes. Hence, H. pylori, utilizing ADP‐heptose, exploits a specific arm of macrophage response to establish its survival niche in the face of the immune defense elicited in the gastric mucosa. [ABSTRACT FROM AUTHOR]

Published

2021

10. CD169 Defines Activated CD14+ Monocytes With Enhanced CD8+ T Cell Activation Capacity.

Author

Affandi, Alsya J., Olesek, Katarzyna, Grabowska, Joanna, Nijen Twilhaar, Maarten K., Rodríguez, Ernesto, Saris, Anno, Zwart, Eline S., Nossent, Esther J., Kalay, Hakan, de Kok, Michael, Kazemier, Geert, Stöckl, Johannes, van den Eertwegh, Alfons J. M., de Gruijl, Tanja D., Garcia-Vallejo, Juan J., Storm, Gert, van Kooyk, Yvette, and den Haan, Joke M. M.

Subjects

T cells, MONOCYTES, TYPE I interferons, COVID-19, ANTIGENS, HUMAN phenotype, T cell receptors

Abstract

Monocytes are antigen-presenting cells (APCs) that play diverse roles in promoting or regulating inflammatory responses, but their role in T cell stimulation is not well defined. In inflammatory conditions, monocytes frequently show increased expression of CD169/Siglec-1, a type-I interferon (IFN-I)-regulated protein. However, little is known about the phenotype and function of these CD169+ monocytes. Here, we have investigated the phenotype of human CD169+ monocytes in different diseases, their capacity to activate CD8+ T cells, and the potential for a targeted-vaccination approach. Using spectral flow cytometry, we detected CD169 expression by CD14+ CD16- classical and CD14+ CD16+ intermediate monocytes and unbiased analysis showed that they were distinct from dendritic cells, including the recently described CD14-expressing DC3. CD169+ monocytes expressed higher levels of co-stimulatory and HLA molecules, suggesting an increased activation state. IFNα treatment highly upregulated CD169 expression on CD14+ monocytes and boosted their capacity to cross-present antigen to CD8+ T cells. Furthermore, we observed CD169+ monocytes in virally-infected patients, including in the blood and bronchoalveolar lavage fluid of COVID-19 patients, as well as in the blood of patients with different types of cancers. Finally, we evaluated two CD169-targeting nanovaccine platforms, antibody-based and liposome-based, and we showed that CD169+ monocytes efficiently presented tumor-associated peptides gp100 and WT1 to antigen-specific CD8+ T cells. In conclusion, our data indicate that CD169+ monocytes are activated monocytes with enhanced CD8+ T cell stimulatory capacity and that they emerge as an interesting target in nanovaccine strategies, because of their presence in health and different diseases. [ABSTRACT FROM AUTHOR]

Published

2021

11. Impact of vitamin D on immune function: lessons learned from genome-wide analysis

Author

Chun, Rene F, Liu, Philip T, Modlin, Robert L, Adams, John S, and Hewison, Martin

Subjects

Biomedical and Clinical Sciences, Immunology, Clinical Research, Nutrition, Underpinning research, 1.1 Normal biological development and functioning, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, macrophage, dendritic cell, intracrine, antigen-presentation, antibacterial, CYP27B1, VDR, Physiology, Medical Physiology, Psychology, Biochemistry and cell biology, Medical physiology

Abstract

Immunomodulatory responses to the active form of vitamin D (1,25-dihydroxyvitamin D, 1,25D) have been recognized for many years, but it is only in the last 5 years that the potential role of this in normal human immune function has been recognized. Genome-wide analyses have played a pivotal role in redefining our perspective on vitamin D and immunity. The description of increased vitamin D receptor (VDR) and 1α-hydroxylase (CYP27B1) expression in macrophages following a pathogen challenge, has underlined the importance of intracrine vitamin D as key mediator of innate immune function. It is now clear that both macrophages and dendritic cells (DCs) are able to respond to 25-hydroxyvitamin D (25D), the major circulating vitamin D metabolite, thereby providing a link between the function of these cells and the variations in vitamin D status common to many humans. The identification of hundreds of primary 1,25D target genes in immune cells has also provided new insight into the role of vitamin D in the adaptive immune system, such as the modulation of antigen-presentation and T cells proliferation and phenotype, with the over-arching effects being to suppress inflammation and promote immune tolerance. In macrophages 1,25D promotes antimicrobial responses through the induction of antibacterial proteins, and stimulation of autophagy and autophagosome activity. In this way variations in 25D levels have the potential to influence both innate and adaptive immune responses. More recent genome-wide analyses have highlighted how cytokine signaling pathways can influence the intracrine vitamin D system and either enhance or abrogate responses to 25D. The current review will discuss the impact of intracrine vitamin D metabolism on both innate and adaptive immunity, whilst introducing the concept of disease-specific corruption of vitamin D metabolism and how this may alter the requirements for vitamin D in maintaining a healthy immune system in humans.

Published

2014

12. Interplay of Na+ Balance and Immunobiology of Dendritic Cells

Author

Patrick Neubert, Agnes Schröder, Dominik N. Müller, and Jonathan Jantsch

Subjects

dendritic cells, Na+ balance, antigen-presentation, Nfat5, kidney, skin microenvironment, Immunologic diseases. Allergy, RC581-607

Abstract

Local Na+ balance emerges as an important factor of tissue microenvironment. On the one hand, immune cells impact on local Na+ levels. On the other hand, Na+ availability is able to influence immune responses. In contrast to macrophages, our knowledge of dendritic cells (DCs) in this state of affair is rather limited. Current evidence suggests that the impact of increased Na+ on DCs is context dependent. Moreover, it is conceivable that DC immunobiology might also be influenced by Na+-rich-diet-induced changes of the gut microbiome.

Published

2019

13. Morphological characteristic and functional dependencies of dendritic cell in developing rabbit lung during fetal and neonatal life.

Author

Mokhtar, Doaa M. and Hussein, Marwa M.

Subjects

*CELL morphology, *ANTIGEN presentation, *LUNGS, *DENDRITES, *DENDRITIC cells, *RABBITS, *ENDOCYTOSIS

Abstract

Recently, pulmonary DC deserved the attention of researchers and clinicians as it was implicated in many diseases afflicting human lungs. However, there are no available data about the morphological or functional features of pulmonary dendritic cells in fetal or early neonatal life. The present study aimed to demonstrate the morphological development of DCs using light-, electron-microscopy, and immunohistochemistry. DCs showed strong immunoreactivity for both CD8 and CD56. Moreover, DCs strongly expressed CD34, VEGF, NSE, and connexin-43 within the developing pulmonary tissue. By SEM, DCs were polyhedral in shape with short cell processes in fetal life. By the advancement of the age, DCs became more numerous and exhibited rounded to oval cell bodies with many fine dendrites. TEM revealed that at early fetal life, DCs were characterized by their heterochromatic indented nuclei, few cell processes and few organelles. With the advancement of age, DCs showed dendrite-like processes and displayed signs of high endocytic activities with releasing of secretory materials. At late fetal life, DCs showed an obvious increase in the nuclear/cytoplasmic ratio and they exhibited a unique connection with type II pneumocytes and pulmonary endothelium by gap junction. In the early neonate, the DCs cells were seen in association with T-lymphocytes, neutrophils, telocytes (TCs), and air-blood barrier. They possessed many fine dendrites, the characteristic Birbeck granules and many vesicles. DCs may contribute to apoptosis, endocytosis, and angiogenesis. The difference in the maturation status may reflect different roles for DCs in the lung. The immature DCs may have an antigen-uptake role through endocytosis, while mature DCs may involve in antigen presentation to T-cells. • The present study demonstrate the morphological development of DCs in rabbit' lungs at the fetal and postnatal life. • DCs showed immunoreactivity for CD8, CD56, CD34, VEGF, NSE, and connexin-43 within the developing pulmonary tissue. • DCs may contribute to apoptosis, endocytosis, and angiogenesis. • Immature DCs may have an antigen-uptake role, while mature DCs may involve in antigen presentation to T-cells. [ABSTRACT FROM AUTHOR]

Published

2019

14. MHC Class I Stability is Modulated by Cell Surface Sialylation in Human Dendritic Cells

Author

Zélia Silva, Tiago Ferro, Danielle Almeida, Helena Soares, José Alexandre Ferreira, Fanny M. Deschepper, Paul J. Hensbergen, Martina Pirro, Sandra J. van Vliet, Sebastian Springer, and Paula A. Videira

Subjects

dendritic-cells, antigen-presentation, mhc-i, immunogenicity, t-cell response, cancer-vaccines, Pharmacy and materia medica, RS1-441

Abstract

Maturation of human Dendritic Cells (DCs) is characterized by increased expression of antigen presentation molecules, and overall decreased levels of sialic acid at cell surface. Here, we aimed to identify sialylated proteins at DC surface and comprehend their role and modulation. Mass spectrometry analysis of DC’s proteins, pulled down by a sialic acid binding lectin, identified molecules of the major human histocompatibility complex class I (MHC-I), known as human leucocyte antigen (HLA). After desialylation, DCs showed significantly higher reactivity with antibodies specific for properly folded MHC-I-β2-microglobulin complex and for β2-microglobulin but showed significant lower reactivity with an antibody specific for free MHC-I heavy chain. Similar results for antibody reactivities were observed for TAP2-deficient lymphoblastoid T2 cells, which express HLA-A*02:01. Using fluorescent peptide specifically fitting the groove of HLA-A*02:01, instead of antibody staining, also showed higher peptide binding on desialylated cells, confirming higher surface expression of MHC-I complex. A decay assay showed that desialylation doubled the half-life of MHC-I molecules at cell surface in both DCs and T2 cells. The biological impact of DC´s desialylation was evaluated in co-cultures with autologous T cells, showing higher number and earlier immunological synapses, and consequent significantly increased production of IFN-γ by T cells. In summary, sialic acid content modulates the expression and stability of complex MHC-I, which may account for the improved DC-T synapses.

Published

2020

15. Recent advances in understanding basophil functions in vivo [version 1; referees: 5 approved]

Author

David Voehringer

Subjects

Review, Articles, Allergy & Hypersensitivity, Antigen Processing & Recognition, Autoimmunity, Clinical Immunology, Immune & Inflammatory Rheumatic Diseases (incl. Arthritis), Immunomodulation, Innate Immunity, Leukocyte Development, Leukocyte Signaling & Gene Expression, basophil, transcription factors, antigen-presentation, inflammatory response, allergy

Abstract

Basophils are mainly known as pro-inflammatory effector cells associated with allergy and helminth infections. Although they were identified over 130 years ago, their in vivo functions are still poorly understood. New insights into basophil development and function have been gained by the development of various transgenic mouse lines and staining techniques to detect and purify these cells from different organs. Several studies over the past few years have identified unexpected functions for basophils, including immunomodulatory properties and interactions with other immune cells. Here, I summarize and discuss the main findings.

Published

2017

16. Blockade of PD-1/PD-L1 Pathway Enhances the Antigen-Presenting Capacity of Fibrocytes

Author

Afroj, Tania, Mitsuhashi, Atsushi, Ogino, Hirokazu, Saijo, Atsuro, Otsuka, Kenji, Yoneda, Hiroto, Tobiume, Makoto, Nguyen, Na Thi, Goto, Hisatsugu, Koyama, Kazuya, Sugimoto, Masamichi, Kondoh, Osamu, Nokihara, Hiroshi, and Nishioka, Yasuhiko

Subjects

PD-1/PD-L1 Blockade, Antigen-presentation, Fibrocytes, CD8+ T-cells, Cancer immunotherapy

Abstract

Fibrocytes, a distinct population of collagen-producing, monocyte-derived cells, are involved in wound healing as well as fibrotic diseases. Recently, fibrocytes have been revealed to play a role in the tumor microenvironment, particularly under antiangiogenic therapy. In addition, combination cancer immunotherapy with immune checkpoint inhibitor and antiangiogenic agents have been developed for various cancers in the clinical setting, although the immunological background is not clear. In the current study, we aimed to determine the function of fibrocytes in tumor immunity induced by immune checkpoint inhibitor therapy. Human and murine fibrocytes were generated from PBMCs and lungs, respectively. The expression of costimulatory and inhibitory molecules on fibrocytes was examined by flow cytometry. The stimulation of CD8+ T cells by fibrocytes was examined in MLRs with a 3H-thymidine incorporation assay. Fibrocytes expressed CD80low and CD86high as a costimulatory molecule, and expressed PD-L1high, but not PD-L2, as a coinhibitory molecule.Without any stimulation, fibrocytes strongly enhanced the proliferation of CD8+ T cells in mice and humans. Treatment with anti-CD86 and -CD54 Abs inhibited the growth of CD8+ T cells induced by fibrocytes. Anti–PD-L1 Ab further enhanced the proliferation of CD8+ T cells, even in the OVA-specific MLR with OT-1Rag-/- mice. Importantly, fibrocytes derived from PBMCs of patients with lung adenocarcinoma or murine MC38 tumors augmented the proliferation of CD8+ T cells with PD-L1 blockade. These results suggest that fibrocytes infiltrating tumor sites may play a role in the antitumor immunity mediated by CD8+ T cells when the activity is further enhanced by PD-L1/PD-1 blockade.

Published

2021

17. Contact sensitizers trigger human CD1-autoreactive T-cell responses.

Author

Betts, Richard J., Perkovic, Adrijana, Mahapatra, Subhashree, Del Bufalo, Aurélia, Camara, Kaddy, Howell, Amy R., Martinozzi Teissier, Silvia, De Libero, Gennaro, and Mori, Lucia

Abstract

Allergic contact dermatitis is a primarily T-cell-mediated inflammatory skin disease induced by exposure to small molecular-weight haptens, which covalently bind to proteins. The abundance of cutaneous T cells that recognize CD1a antigen-presenting molecules raises the possibility that MHC-independent antigen presentation may be relevant in some hapten-driven immune responses. Here we examine the ability of contact sensitizers to influence CD1-restricted immunity. Exposure of human antigen-presenting cells such as monocyte-derived dendritic cells and THP-1 cells to the prototypical contact sensitizer dinitrochlorobenzene potentiated the response of CD1a- and CD1d-autoreactive T cells, which released a vast array of cytokines in a CD1- and TCR-dependent manner. The potentiating effects of dinitrochlorobenzene depended upon newly synthesized CD1 molecules and the presence of endogenous stimulatory lipids. Further examination of a broad panel of contact sensitizers revealed 1,4-benzoquinone, resorcinol, isoeugenol, and cinnamaldehyde to activate the same type of CD1-restricted responses. These findings provide a basis for the antigen-specific activation of skin-associated CD1-restricted T cells by small molecules and may have implications for contact sensitizer-induced inflammatory skin diseases. [ABSTRACT FROM AUTHOR]

Published

2017

18. Of self-lipids, CD1-restricted T cells, and contact sensitization.

Author

Casorati, Giulia and Dellabona, Paolo

Abstract

Contact hypersensitivity (CHS) in rodents and contact dermatitis in humans are long-known pathological conditions caused by MHC-restricted T-cell responses. These responses are triggered upon T-cell recognition of neo-antigenic determinants, which are generated by a variety of environmental contact sensitizer (CS) chemicals associating with self-proteins to comprise these neo-antigens. In this issue of the European Journal of Immunology, Betts et al. [ Eur. J. Immunol. 2017. 47: 1171-1180] provide intriguing data implying that common small molecule CSs such as dinitrochlorobenzene can also recruit and activate autoreactive CD1-restricted T cells specific for cell-endogenous lipids, which are enriched in human skin. The effects of dinitrochlorobenzene on CD1 T-cell recruitment and function were dependent on newly synthesized CD1 molecules and the presence of endogenous lipids. These findings shed new light on unanticipated mechanisms that have potential clinical relevance on a common and highly distressing disease state. [ABSTRACT FROM AUTHOR]

Published

2017

19. Piperine, a Pungent Alkaloid from Black Pepper, Inhibits B Lymphocyte Activation and Effector Functions.

Author

Soutar, David A., Doucette, Carolyn D., Liwski, Robert S., and Hoskin, David W.

Subjects

ALKALOIDS, AMIDES, ANIMAL experimentation, B cells, CELL culture, CELL physiology, HETEROCYCLIC compounds, IMMUNOLOGY technique, INTERLEUKINS, MICE, PIPERIDINE, PLANTS, T cells, PHARMACODYNAMICS, PHYSIOLOGY

Abstract

Piperine has several well-documented anti-inflammatory properties; however, little is known regarding its effect on humoral immunity. In this study, we describe the immunosuppressive effect of piperine on B lymphocytes, which are integral to the humoral immune response. Mouse B cells were cultured in the absence or presence of non-cytotoxic concentrations (25, 50, and 100 μM) of piperine during T-dependent or T-independent stimulation. Piperine inhibited B cell proliferation by causing G0/G1 phase cell cycle arrest in association with reduced expression of cyclin D2 and D3. The inhibitory effect of piperine was not mediated through transient receptor potential vanilloid-1 ion channel (TRPV1) because piperine also inhibited the proliferation of B cells from TRPV1-deficient mice. Expression of class II major histocompatibility complex molecules and costimulatory CD40 and CD86 on B lymphocytes was reduced in the presence of piperine, as was B cell-mediated antigen presentation to syngeneic T cells. In addition, piperine inhibited B cell synthesis of interleukin (IL)-6 and IL-10 cytokines, as well as IgM, IgG2b, and IgG3 immunoglobulins. The inhibitory effect of piperine on B lymphocyte activation and effector function warrants further investigation for possible application in the treatment of pathologies related to inappropriate humoral immune responses. Copyright © 2017 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2017

20. The Diverse Roles of γδ T Cells in Cancer: From Rapid Immunity to Aggressive Lymphoma

Author

Susann Schönefeldt, Tamara Wais, Marco Herling, Satu Mustjoki, Vasileios Bekiaris, Richard Moriggl, Heidi A. Neubauer, HUS Comprehensive Cancer Center, Department of Clinical Chemistry and Hematology, Clinicum, Department of Oncology, Hematologian yksikkö, Digital Precision Cancer Medicine (iCAN), and TRIMM - Translational Immunology Research Program

Subjects

FUSION TRANSCRIPT, Cancer Research, 3122 Cancers, Cancer immunity, Review, ANTIGEN-PRESENTATION, γδ T-cell lymphoma, γδ T cells, Targeted therapy, 03 medical and health sciences, ALPHA-BETA-T, 0302 clinical medicine, SDG 3 - Good Health and Well-being, cancer immunity, ddc:570, ANTITUMOR IMMUNITY, gamma delta T cells, SUPPRESSOR-CELLS, THYMIC DEVELOPMENT, γδ T-cell transformation, RC254-282, 030304 developmental biology, gamma delta T-cell transformation, LYMPHOCYTIC-LEUKEMIA, 0303 health sciences, IFN-GAMMA, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, targeted therapy, MEVALONATE METABOLITES, DENDRITIC-CELLS, 3. Good health, immunotherapy, Oncology, gamma delta T-cell lymphoma, Immunotherapy, 030215 immunology

Abstract

Simple Summary:& nbsp;gamma delta T cells play important roles in cancer immunity. Their rapid activation and cytotoxic nature make them promising candidates for use in cell-based immunotherapies; however, under certain conditions, they can induce pro-tumour functions. Furthermore, upon transformation, gamma delta T cells can develop into aggressive lymphomas with a poor prognosis and no curative therapeutic options. Here, we provide a comprehensive summary of our current knowledge on the complex roles of gamma delta T cells in cancer. We discuss their anti- and pro-tumour functions in both solid and blood cancers, highlighting the key subsets involved and their potential utility in anti-cancer immunotherapy. We also discuss the mechanisms of gamma delta T-cell transformation, summarising the resulting gamma delta T-cell leukaemia/lymphoma entities and their genetic and molecular profiles, as well as current and future treatment strategies.& nbsp;gamma delta T cells are unique players in shaping immune responses, lying at the intersection between innate and adaptive immunity. Unlike conventional alpha beta T cells, gamma delta T cells largely populate non-lymphoid peripheral tissues, demonstrating tissue specificity, and they respond to ligands in an MHC-independent manner. gamma delta T cells display rapid activation and effector functions, with a capacity for cytotoxic anti-tumour responses and production of inflammatory cytokines such as IFN-gamma or IL-17. Their rapid cytotoxic nature makes them attractive cells for use in anti-cancer immunotherapies. However, upon transformation, gamma delta T cells can give rise to highly aggressive lymphomas. These rare malignancies often display poor patient survival, and no curative therapies exist. In this review, we discuss the diverse roles of gamma delta T cells in immune surveillance and response, with a particular focus on cancer immunity. We summarise the intriguing dichotomy between pro- and anti-tumour functions of gamma delta T cells in solid and haematological cancers, highlighting the key subsets involved. Finally, we discuss potential drivers of gamma delta T-cell transformation, summarising the main gamma delta T-cell lymphoma/leukaemia entities, their clinical features, recent advances in mapping their molecular and genomic landscapes, current treatment strategies and potential future targeting options.

Published

2021

21. LN Monocytes Limit DC-Poly I:C Induced Cytotoxic T Cell Response via IL-10 and Induction of Suppressor CD4 T Cells

Author

Sophie L. Gibbings, Miglena Prabagar, Kavita Rawat, Anita Tewari, and Claudia Jakubzick

Subjects

Poly I:C, CD4-Positive T-Lymphocytes, Receptors, CCR2, medicine.medical_treatment, Antigen presentation, Immunology, Melanoma, Experimental, Monocytes, Mice, Immune system, Cancer immunotherapy, Antigen, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Humans, dendritic cells, Original Research, Chemistry, cytotoxic T cells, antigen-presentation, RC581-607, Acquired immune system, Interleukin-10, double-stranded RNA, Mice, Inbred C57BL, Interleukin 10, Poly I-C, TLR3, IL-10, Cancer research, suppressor CD4+ T cells, Lymph Nodes, Immunologic diseases. Allergy, Ly6C+ monocytes, T-Lymphocytes, Cytotoxic

Abstract

Every immune response has accelerators and brakes. Depending on the pathogen or injury, monocytes can play either role, promoting or resolving immunity. Poly I:C, a potent TLR3 ligand, licenses cross-presenting dendritic cells (DC1) to accelerate a robust cytotoxic T cells response against a foreign antigen. Poly I:C thus has promise as an adjuvant in cancer immunotherapy and viral subunit vaccines. Like DC1s, monocytes are also abundant in the LNs. They may act as either immune accelerators or brakes, depending on the inflammatory mediator they encounter. However, little is known about their contribution to adaptive immunity in the context of antigen and Poly I:C. Using monocyte-deficient and chimeric mice, we demonstrate that LN monocytes indirectly dampen a Poly I:C induced antigen-specific cytotoxic T cell response, exerting a “braking” function. This effect is mediated by IL-10 production and induction of suppressor CD4+ T cells. In a metastatic melanoma model, we show that a triple-combination prophylactic treatment consisting of anti-IL-10, tumor peptides and Poly I:C works because removing IL-10 counteracts the monocytic brake, resulting in significantly fewer tumors compared to mice treated with tumor peptides and Poly I:C alone. Finally, in human LN tissue, we observed that monocytes (unlike DCs) express high levels of IL-10, suggesting that anti-IL-10 may be an important addition to treatments. Overall, our data demonstrates that LN monocytes regulate the induction of a robust DC1-mediated immune response. Neutralization of either IL-10 or monocytes can augment Poly I:C-based treatments and enhance T cell cytotoxicity.

Published

2021

22. Antigen presenting cells: Professionals, amateurs, and spectators in the 'long game' of lung immunity.

Author

Hargrave, Kerrie E., MacLeod, Megan K.L., and Worrell, Julie C.

Subjects

*ANTIGEN presenting cells, *LUNGS, *DENDRITIC cells, *IMMUNOLOGIC memory, *T cells, *EPITHELIAL cells, *CELL physiology, *IMMUNITY

Abstract

The lung is frequently and repeatedly exposed to invading pathogens and thus requires constant immunosurveillance. Professional antigen presenting cells (APCs), including dendritic cells, engulf invading pathogens and present their peptides via major histocompatibility complexes (MHC) I and II, to CD8 or CD4 T cells. Epithelial cells and stromal cells (including fibroblasts) provide more than structural support, they are increasingly recognised as key players in the immune response, acting as non-professional APCs through interactions with antigen experienced T cells that migrate to the lung. The importance of the contributions of non-professional and professional APCs to T cell function in vivo , is currently unclear. This review summarises the roles of professional and non-professional APCs in lung immunity, at the steady state and following viral insult, with particular emphasis on their ability to interact with and influence T cells. • The lung contains various populations of professional and non‑professional antigen presenting cells. • Memory T cell reactivation by diverse antigen-presenting cells may drive distinct functional responses post infection. • Using specific APC subsets to facilitate targeted reactivation of memory T cells may enhance vaccine efficacy. [ABSTRACT FROM AUTHOR]

Published

2022

23. Recognition of microbial glycolipids by Natural Killer T cells

Author

Dirk Michael Zajonc and Enrico eGirardi

Subjects

Glycolipids, tcr, Microbes, NKT cells, antigen-presentation, CD1d, Immunologic diseases. Allergy, RC581-607

Abstract

T cells can recognize microbial antigens when presented by dedicated antigen-presenting molecules. While peptides are presented by classical members of the Major Histocompatibility (MHC) family (MHC I and II), lipids, glycolipids and lipopeptides can be presented by the non-classical MHC member CD1. The best studied subset of lipid-reactive T cells are Type I Natural killer T (iNKT) cells that recognize a variety of different antigens when presented by the non-classical MHCI homolog CD1d. iNKT cells have been shown to be important for the protection against various microbial pathogens, including B. burgdorferi the causative agents of Lyme disease and S. pneumoniae, which causes pneumococcal meningitis and community-acquired pneumonia. Both pathogens carry microbial glycolipids that can trigger the T cell antigen receptor (TCR), leading to iNKT cell activation. iNKT cells have an evolutionary conserved TCR alpha chain, yet retain the ability to recognize structurally diverse glycolipids. They do so using a conserved recognition mode, in which the TCR enforces a conserved binding orientation on CD1d. TCR binding is accompanied by structural changes within the TCR binding site of CD1d, as well as the glycolipid antigen itself. In addition to direct recognition of microbial antigens, iNKT cells can also be activated by a combination of cytokines (IL-12/IL-18) and TCR stimulation. Many microbes carry TLR antigens and microbial infections can lead to TLR activation. The subsequent cytokine response in turn lower the threshold of TCR mediated iNKT cell activation, especially when weak microbial or even self-antigens are presented during the cause of the infection. In summary, iNKT cells can be directly activated through TCR triggering of strong antigens, while cytokines produced by the innate immune response may be necessary for TCR triggering and iNKT cell activation in the presence of weak antigens. Here we will review the molecular basis of iNKT cell recognition of glyc

Published

2015

24. Linarin down-regulates phagocytosis, pro-inflammatory cytokine production, and activation marker expression in RAW264.7 macrophages.

Author

Kim, Bomi, Lee, Jong, Seo, Myung-Ji, Eom, Seok, and Kim, Wooki

Abstract

Plant-extracted flavonoid glycosides have been reported to be bioactive compounds with pleiotropic functions, including antioxidant, anti-inflammatory, and anti-cancer effects. This study investigated the anti-inflammatory role of linarin (acacetin-7-rutinoside, which is found in Chrysanthemum indicum (Gam-Guk) and Dendranthema zawadskii (Gu-Jul-Cho)), on lipopolysaccharide-stimulated RAW264.7 macrophages. Linarin treatments exhibited no cytotoxicity up to a concentration of 30 μM, as assessed by MTT assay. The production of nitric oxide, an inflammatory mediator, was decreased by addition of linarin. The secretion of pro-inflammatory cytokines, interleukin-1β and interleukin-6, was significantly decreased in a dose-dependent manner. Linarin also decreased the phagocytic ability of macrophages following co-culture with fluorescent beads. In addition, expression levels of antigenpresenting surface markers, MHC II and CD80, were suppressed by linarin. Taken together, these results indicate that the flavonoid glycoside linarin has an anti-inflammatory effect, in part through the suppression of phagocytosis, cytokine production, and antigen presentation in macrophages. [ABSTRACT FROM AUTHOR]

Published

2016

25. Single-walled carbon nanotubes disturbed the immune and metabolic regulation function 13-weeks after a single intratracheal instillation.

Author

Park, Eun-Jung, Hong, Young-Shick, Lee, Byoung-Seok, Yoon, Cheolho, Jeong, Uiseok, and Kim, Younghun

Subjects

*CARBON nanotubes, *IMMUNE response, *INTRATRACHEAL drug administration, *METABOLIC regulation, *GENE expression, *GLUCOSE metabolism, *PROTEIN metabolism

Abstract

Due to their unique physicochemical properties, the potential health effects of single-walled carbon nanotubes (SWCNTs) have attracted continuous attention together with their extensive application. In this study, we aimed to identify local and systemic health effects following pulmonary persistence of SWCNTs. As expected, SWCNTs remained in the lung for 13 weeks after a single intratracheal instillation (50, 100, and 200 μg/kg). In the lung, the total number of cells and the percentages of lymphocytes and neutrophils significantly increased at 200 μg/kg compared to the control, and the Th1-polarized immune response was induced accompanying enhanced expression of tissue damage-related genes and increased release of chemokines. Additionally, SWCNTs enhanced the expression of antigen presentation-related proteins on the surface of antigen-presenting cells, however, maturation of dendritic cells was inhibited by their persistence. As compared to the control, a significant increase in the percentage of neutrophils and a remarkable decrease of BUN and potassium level were observed in the blood of mice treated with the highest dose. This was accompanied by the down-regulation of the expression of antigen presentation-related proteins on splenocytes. Moreover, protein and glucose metabolism were disturbed with an up-regulation of fatty acid β-oxidation. Taken together, we conclude that SWCNTs may induce adverse health effects by disturbing immune and metabolic regulation functions in the body. Therefore, careful application of SWCNTs is necessary for the enforcement of safety in nano-industries. [ABSTRACT FROM AUTHOR]

Published

2016

26. The role of dendritic cell alterations in susceptibility to hospital-acquired infections during critical-illness related immunosuppression.

Author

Roquilly, Antoine and Villadangos, Jose A.

Subjects

*DENDRITIC cells, *DISEASE susceptibility, *IMMUNOSUPPRESSION, *SYSTEMIC inflammatory response syndrome, *NOSOCOMIAL infections, *PATIENTS

Abstract

Systemic inflammatory response syndrome (SIRS) is a common condition in critically ill patients. SIRS is characterized by alteration of both innate and adaptive immunity and causes protracted immunosupression, exposing the patients to severe secondary infections. Dendritic cells (DCs), which play a pivotal role bridging innate and T cell-dependent immunity, exhibit prolonged alterations after SIRS. In an early phase, SIRS causes depletion or systemic activation of immature DCs in parenchymal tissues and lymphoid organs, leading to impaired pathogen detection and presentation. Later on, newly formed DCs acquire a poorly immunogenic phenotype, with poor capacity to capture, process and/or present antigens and to stimulate T cells. Here, we review the studies that describe alterations in DC function post-SIRS. Knowledge about the molecular mechanisms involved are still scarce but their understanding might open new therapeutic avenues to prevent or reduce protracted immunosuppression in critically-ill patients. [ABSTRACT FROM AUTHOR]

Published

2015

27. ADP-heptose enables Helicobacter pylori to exploit macrophages as a survival niche by suppressing antigen-presenting HLA-II expression

Author

Greta Battaggia, Mario Milco D'Elios, Larissa Faass, Chiara Della Bella, Sara Coletta, Martina Hauke, Matteo Furlani, Christine Josenhans, and Marina de Bernard

Subjects

antigen-presentation, Helicobacter pylori, HLA-II, immunoevasion, macrophages, Antigen Presentation, Gene Expression Regulation, Heptoses, Histocompatibility Antigens Class II, Humans, Macrophages, Nuclear Proteins, Trans-Activators, Lipopolysaccharide, Antigen presentation, Biophysics, Biology, Biochemistry, chemistry.chemical_compound, Immune system, Antigen, Structural Biology, Genetics, Gastric mucosa, medicine, CIITA, Macrophage, Molecular Biology, Cell Biology, biology.organism_classification, medicine.anatomical_structure, chemistry, Immunology

Abstract

The persistence of Helicobacter pylori in the human gastric mucosa implies that the immune response fails to clear the infection. We found that H. pylori compromises the antigen presentation ability of macrophages, because of the decline of the presenting molecules HLA-II. Here, we reveal that the main bacterial factor responsible for this effect is ADP-heptose, an intermediate metabolite in the biosynthetic pathway of lipopolysaccharide (LPS) that elicits a pro-inflammatory response in gastric epithelial cells. In macrophages, it upregulates the expression of miR146b which, in turn, would downmodulate CIITA, the master regulator for HLA-II genes. Hence, H. pylori, utilizing ADP-heptose, exploits a specific arm of macrophage response to establish its survival niche in the face of the immune defense elicited in the gastric mucosa.

Published

2021

28. Engineering dendritic cell vaccines to improve cancer immunotherapy

Author

Michele De Palma and Caleb R. Perez

Subjects

0301 basic medicine, T-Lymphocytes, medicine.medical_treatment, Cellular differentiation, Cell Culture Techniques, General Physics and Astronomy, Cancer immunotherapy, Cell Separation, 0302 clinical medicine, Neoplasms, lcsh:Science, Multidisciplinary, Cell Differentiation, antigen-presentation, hemic and immune systems, kinase 3 ligand, Acquired immune system, ifn-gamma, 3. Good health, 030220 oncology & carcinogenesis, Perspective, Tumour immunology, Immunotherapy, Science, chemical and pharmacologic phenomena, Tumor immunity, in-vitro, melanoma patients, Cancer Vaccines, General Biochemistry, Genetics and Molecular Biology, lymph-nodes, 03 medical and health sciences, Cancer Medicine, medicine, Animals, Humans, cd8(+), human blood, cross-presentation, Rational design, Dendritic Cells, General Chemistry, Dendritic cell, Dc vaccine, 030104 developmental biology, responses, lcsh:Q, Neuroscience

Abstract

At the interface between the innate and adaptive immune system, dendritic cells (DCs) play key roles in tumour immunity and hold a hitherto unrealized potential for cancer immunotherapy. Here we review the role of distinct DC subsets in the tumour microenvironment, with special emphasis on conventional type 1 DCs. Integrating new knowledge of DC biology and advancements in cell engineering, we provide a blueprint for the rational design of optimized DC vaccines for personalized cancer medicine., Dendritic cells (DCs) have been explored as a promising strategy for cancer immunotherapy. In this Perspective, the authors discuss the different types of DCs and their therapeutic potential in the context of vaccines for personalized cancer therapy.

Published

2019

29. Expanded human blood-derived γδT cells display potent antigen-presentation functions

Author

Mohd Wajid Ali Khan, Stuart M Curbishley, Hung-Chang eChen, Andrew D Thomas, Hanspeter ePircher, Domenico eMavilio, Neil M Steven, Matthias eEberl, and Bernhard eMoser

Subjects

Immunotherapy, Vaccine, antigen-presentation, γδ T cells, γδT cells, Immunologic diseases. Allergy, RC581-607

Abstract

Cell-based immunotherapy strategies target tumors directly (via cytolytic effector cells) or aim at mobilizing endogenous anti-tumor immunity. The latter approach includes dendritic cells (DC), most frequently in the form of in vitro cultured peripheral blood monocytes-derived DC. Human blood γδT cells are selective for a single class of non-peptide agonists (phosphoantigens) and develop into potent antigen-presenting cells (APC), termed γδT-APC, within 1-3 days of in vitro culture. Availability of large numbers of γδT-APC would be advantageous for use as a novel cellular vaccine. We here report optimal γδT cell expansion (>107 cells/ml blood) when peripheral blood mononuclear cells (PBMC) from healthy individuals and melanoma patients were stimulated with zoledronate and then cultured for 14 days in the presence of IL-2 and IL-15, yielding γδT cell cultures of variable purity (77±21% and 56±26%, respectively). They resembled effector-memory &#945&#946T (TEM) cells and retained full functionality as assessed by in vitro tumor cell killing as well as secretion of proinflammatory cytokines (IFNγ, TNF&#945) and cell proliferation in response to stimulation with phosphoantigens. Importantly, day 14 γδT cells expressed numerous APC-related cell surface markers and, in agreement, displayed potent in vitro APC functions. Day 14 γδT cells from PBMC of patients with cancer were equally effective as their counterparts derived from blood of healthy individuals and triggered potent CD8+ &#945&#946T cell responses following processing and cross-presentation of simple (influenza M1) and complex (tuberculin purified protein derivative) protein antigens. Of note, and in clear contrast to peripheral blood γδT cells, the ability of day 14 γδT cells to trigger antigen-specific &#945&#946T cell responses did not depend on re-stimulation. We conclude that day 14 γδT cell cultures provide a convenient source of autologous APC for use in immunotherapy of patients with various cancers

Published

2014

30. Impact of vitamin D on immune function: lessons learned from genome-wide analysis

Author

Rene F Chun, Philip T Liu, Robert L Modlin, John S Adams, and Martin eHewison

Subjects

dendritic cell, macrophage, Antibacterial, antigen-presentation, intracrine, VDR, Physiology, QP1-981

Abstract

Immunomodulatory responses to the active form of vitamin D (1,25-dihydroxyvitamin D, 1,25D) have been recognized for many years, but it is only in the last five years that the potential role of this in normal human immune function has been recognized. Genome-wide analyses have played a pivotal role in redefining our perspective on vitamin D and immunity. The description of increased vitamin D receptor (VDR) and 1α-hydroxylase (CYP27B1) expression in macrophages following a pathogen challenge, has underlined the importance of intracrine vitamin D as key mediator of innate immune function. It is now clear that both macrophages and DCs are able to respond to 25-hydroxyvitamin D (25D), the major circulating vitamin D metabolite, thereby providing a link between the function of these cells and the variations in vitamin D status common to many humans. The identification of hundreds of primary 1,25D target genes in immune cells has also provided new insight into the role of vitamin D in the adaptive immune system, such as the modulation of antigen-presentation and T cells proliferation and phenotype, with the over-arching effects being to suppress inflammation and promote immune tolerance. In macrophages 1,25D promotes antimicrobial responses through the induction of antibacterial proteins, and stimulation of autophagy and autophagosome activity. In this way variations in 25D levels have the potential to influence both innate and adaptive immune responses. More recent genome-wide analyses have highlighted how cytokine signaling pathways can influence the intracrine vitamin D system and either enhance or abrogate responses to 25D. The current review will discuss the impact of intracrine vitamin D metabolism on both innate and adaptive immunity, whilst introducing the concept of disease-specific corruption of vitamin D metabolism and how this may alter the requirements for vitamin D in maintaining a healthy immune system in humans.

Published

2014

31. Chiral-Selective Antigen-Presentation by Supramolecular Chiral Polymer Micelles.

Author

Jiang H, Liu R, Wang L, Wang X, Zhang M, Lin S, Cao Z, Wu F, Liu Y, and Liu J

Subjects

Animals, Mice, Antigen Presentation, Micelles, Polyethyleneimine, Antigens, Polymers chemistry, COVID-19, Neoplasms

Abstract

Chirality is ubiquitous in biological systems, which is closely related to biological functions, life processes, and even the pathogenesis of diseases. However, the interface between the chirality of synthetic materials and organisms, particularly the immune system, remains poorly understood. Here, supramolecular chiral polymer micelles (SCPMs) are prepared by complexing antigenic proteins with chiral amino acid-modified polyethyleneimine. The introduction of chirality not only reduces the toxicity of cationic polymer, but also benefits cell uptake and antigen presentation. Especially, D-chirality presents the lowest cytotoxicity, while promoting the highest expression level of costimulatory molecules on dendritic cells compared to L-chirality and achirality. The superiority of D-chirality to stimulate dendritic cell maturation is supported by immunization with D-SCPMs, which achieves significant antigen-specific proliferation of T cells in the spleen, lymph nodes, and tumor of mice. Chirality-mediated antigen processing and presentation are demonstrated by D-SCPMs self-assembled from chiral alkaline histidine or neutral phenylalanine modified polyethyleneimine and tumor associated ovalbumin or severe acute respiratory syndrome coronavirus 2 spike 1 antigenic protein. Immunoactivation enabled by D-chirality opens a window to prepare potent nanotherapeutics for disease prevention and treatment., (© 2022 Wiley-VCH GmbH.)

Published

2023

32. Chronic pulmonary accumulation of iron oxide nanoparticles induced Th1-type immune response stimulating the function of antigen-presenting cells.

Author

Park, Eun-Jung, Oh, Seung Yun, Lee, Sang Jin, Lee, Kyuhong, Kim, Younghun, Lee, Byoung-Seok, and Kim, Jong Sung

Subjects

*IRON oxide nanoparticles, *PULMONARY toxicology, *BIOACCUMULATION, *IMMUNE response, *ANTIGEN presenting cells, *ADVERSE health care events, *IMMUNOMODULATORS

Abstract

Although there is growing evidence that suggests that pulmonary exposure to nanoparticles causes adverse health effects by modulating immune system of the body, available information is very limited. In this study, we investigated immune response following chronic pulmonary accumulation of iron oxide nanoparticles (FeNPs, Fe 2 O 3 ). FeNPs have a needle-like shape in suspension (101.3±4.2 nm). On day 90 after a single intratracheal instillation (0.5, 1, and 2 mg/kg), the FeNPs remained in the lung and particle-laden macrophages were clearly observed in the BAL fluid of the treated-mice. The number of total cells and proportions of neutrophils and lymphocytes significantly increased at 2 mg/kg dose, and the percentage of apoptotic cells and LDH release increased in a dose-dependent manner. We also found that Th1-polarized inflammatory response was induced in the lung of the treated group accompanying the elevated secretion of chemokines, including GM-CSF, MCP-1, and MIP-1. Additionally, FeNPs enhanced the expression of antigen presentation-related proteins, including CD80, CD86, and MHC class II, on antigen-presenting cells in BAL fluid. Taken together, we suggest that chronic pulmonary accumulation of FeNPs may induce Th1-polarized immune response augmenting the function of antigen-presenting cells in the lung. [ABSTRACT FROM AUTHOR]

Published

2015

33. ADP-heptose enables Helicobacter pylori to exploit macrophages as a survival niche by suppressing antigen-presenting HLA-II expression

Author

Coletta, S., Battaggia, G., Della Bella, C., Furlani, M., Hauke, M., Faass, L., D'Elios, M. M., Josenhans, C., and de Bernard, M.

Subjects

antigen-presentation, Helicobacter pylori, HLA-II, immunoevasion, macrophages, Antigen Presentation, Gene Expression Regulation, Heptoses, Histocompatibility Antigens Class II, Humans, Macrophages, Nuclear Proteins, Trans-Activators

Published

2021

34. TOLEROGENIC AND ACTIVATORY PLASMACYTOID DENDRITIC CELLS IN AUTOIMMUNITY

Author

Leslie eGuery and Stephanie eHugues

Subjects

Autoimmunity, tolerance, plasmacytoid dendritic cells, antigen-presentation, type-I IFNs, Immunologic diseases. Allergy, RC581-607

Abstract

Plasmacytoid dendritic cells (pDCs) are a particular subset of DCs that link innate and adaptive immunity. They are responsible for the substantial production of type 1 interferon (IFN-I) in response to viral RNA or DNA through activation of TLR7 and 9. Furthermore, pDCs present antigens and induce naïve T cell differentiation. It has been demonstrated that pDCs can induce immunogenic T cell responses through differentiation of cytotoxic CD8+ T cells and effector CD4+ T cells. Conversely, pDCs exhibit strong tolerogenic functions by inducing CD8+ T cell deletion, CD4+ T cell anergy, and Treg differentiation. However, since IFN-I produced by pDCs efficiently activates and recruits conventional DCs, B cells, T cells and NK cells, pDCs also indirectly affect the nature and the amplitude of adaptive immune responses. As a consequence, the precise role of antigen-presenting functions of pDCs in adaptive immunity has been difficult to dissect in vivo. Additionally, different experimental procedures led to conflicting results regarding the outcome of T cell responses induced by pDCs. During the development of autoimmunity, pDCs have been shown to play both immunogenic and tolerogenic functions depending on disease, disease progression and the experimental conditions. In this review, we will discuss the relative contribution of innate and adaptive pDC functions in modulating T cell responses, particularly during the development of autoimmunity.

Published

2013

35. Expanded human blood-derived γδT cells display potent antigen-presentation functions.

Author

Khan, Mohd Wajid A., Curbishley, Stuart M., Hung-Chang Chen, Thomas, Andrew D., Pircher, Hanspeter, Mavilio, Domenico, Steven, Neil M., Eberl, Matthias, and Moser, Bernhard

Subjects

T cells, ANTIGENS, VACCINE research, IMMUNOTHERAPY, PEPTIDES, TUMORS

Abstract

Cell-based immunotherapy strategies target tumors directly (via cytolytic effector cells) or aim at mobilizing endogenous anti-tumor immunity. The latter approach includes dendritic cells (DC) most frequently in the form of in vitro cultured peripheral blood monocytesderived DC. Human blood γδT cells are selective for a single class of non-peptide agonists ("phosphoantigens") and develop into potent antigen-presenting cells (APC), termed gdTAPC within 1-3 days of in vitro culture. Availability of large numbers of γδT-APC would be advantageous for use as a novel cellular vaccine. We here report optimal gdT cell expansion (>107 cells/ml blood) when peripheral blood mononuclear cells (PBMC) from healthy individuals and melanoma patients were stimulated with zoledronate and then cultured for 14 days in the presence of IL-2 and IL-15, yielding gdT cell cultures of variable purity (77±21 and 56±26%, respectively). They resembled effector memory αβT (TEM) cells and retained full functionality as assessed by in vitro tumor cell killing as well as secretion of pro-inflammatory cytokines (IFNg,TNFα) and cell proliferation in response to stimulation with phosphoantigens. Importantly, day 14 γδT cells expressed numerous APC-related cell surface markers and, in agreement, displayed potent in vitro APC functions. Day 14 γδT cells from PBMC of patients with cancer were equally effective as their counterparts derived from blood of healthy individuals and triggered potent CD8C αβT cell responses following processing and cross-presentation of simple (influenza M1) and complex (tuberculin purified protein derivative) protein antigens. Of note, and in clear contrast to peripheral blood γδT cells, the ability of day 14 γδT cells to trigger antigen-specific abT cell responses did not depend on re-stimulation.We conclude that day 14 gdT cell cultures provide a convenient source of autologous APC for use in immunotherapy of patients with various cancers. [ABSTRACT FROM AUTHOR]

Published

2014

36. Productive replication of Middle East respiratory syndrome coronavirus in monocyte-derived dendritic cells modulates innate immune response.

Author

Chu, Hin, Zhou, Jie, Ho-Yin Wong, Bosco, Li, Cun, Cheng, Zhong-Shan, Lin, Xiang, Kwok-Man Poon, Vincent, Sun, Tianhao, Choi-Yi Lau, Candy, Fuk-Woo Chan, Jasper, Kai-Wang To, Kelvin, Chan, Kwok-Hung, Lu, Liwei, Zheng, Bo-Jian, and Yuen, Kwok-Yung

Subjects

*MERS coronavirus, *VIRAL replication, *DENDRITIC cells, *NATURAL immunity, *IMMUNE response, *PNEUMONIA

Abstract

Abstract: The Middle East respiratory syndrome coronavirus (MERS-CoV) closely resembled severe acute respiratory syndrome coronavirus (SARS-CoV) in disease manifestation as rapidly progressive acute pneumonia with multi-organ dysfunction. Using monocyte-derived-dendritic cells (Mo-DCs), we discovered fundamental discrepancies in the outcome of MERS‐CoV‐ and SARS-CoV-infection. First, MERS-CoV productively infected Mo-DCs while SARS-CoV-infection was abortive. Second, MERS-CoV induced significantly higher levels of IFN-γ, IP-10, IL-12, and RANTES expression than SARS-CoV. Third, MERS-CoV-infection induced higher surface expression of MHC class II (HLA-DR) and the co-stimulatory molecule CD86 than SARS-CoV-infection. Overall, our data suggests that the dendritic cell can serve as an important target of viral replication and a vehicle for dissemination. MERS-CoV-infection in DCs results in the production of a rich combination of cytokines and chemokines, and modulates innate immune response differently from that of SARS-CoV-infection. Our findings may help to explain the apparent discrepancy in the pathogenicity between MERS-CoV and SARS-CoV. [Copyright &y& Elsevier]

Published

2014

37. Impact of vitamin D on immune function: lessons learned from genome-wide analysis.

Author

Chun, Rene F., Liu, Philip T., Modlin, Robert L., Adams, John S., and Hewison, Martin

Subjects

PHYSIOLOGICAL effects of vitamin D, IMMUNE system, IMMUNOREGULATION, IMMUNITY, METABOLISM

Abstract

Immunomodulatory responses to the active form of vitamin D (1,25-dihydroxyvitamin D, 1,25D) have been recognized for many years, but it is only in the last 5 years that the potential role of this in normal human immune function has been recognized. Genome-wide analyses have played a pivotal role in redefining our perspective on vitamin D and immunity. The description of increased vitamin D receptor (VDR) and 1α-hydroxylase (CYP27B1) expression in macrophages following a pathogen challenge, has underlined the importance of intracrine vitamin D as key mediator of innate immune function. It is now clear that both macrophages and dendritic cells (DCs) are able to respond to 25-hydroxyvitamin D (25D), the major circulating vitamin D metabolite, thereby providing a link between the function of these cells and the variations in vitamin D status common to many humans. The identification of hundreds of primary 1,25D target genes in immune cells has also provided new insight into the role of vitamin D in the adaptive immune system, such as the modulation of antigen-presentation and T cells proliferation and phenotype, with the over-arching effects being to suppress inflammation and promote immune tolerance. In macrophages 1,25D promotes antimicrobial responses through the induction of antibacterial proteins, and stimulation of autophagy and autophagosome activity. In this way variations in 25D levels have the potential to influence both innate and adaptive immune responses. More recent genome-wide analyses have highlighted how cytokine signaling pathways can influence the intracrine vitamin D system and either enhance or abrogate responses to 25D. The current review will discuss the impact of intracrine vitamin D metabolism on both innate and adaptive immunity, whilst introducing the concept of disease-specific corruption of vitamin D metabolism and how this may alter the requirements for vitamin D in maintaining a healthy immune system in humans. [ABSTRACT FROM AUTHOR]

Published

2014

38. MHC class I stability is modulated by cell surface sialylation in human dendritic cells

Author

Sandra J. van Vliet, Martina Pirro, Tiago Ferro, José Alexandre Ferreira, Danielle Almeida, Zélia Silva, Paula A. Videira, Helena Soares, Fanny M. Deschepper, Sebastian Springer, Paul J. Hensbergen, UCIBIO - Applied Molecular Biosciences Unit, DCV - Departamento de Ciências da Vida, NOVA Medical School|Faculdade de Ciências Médicas (NMS|FCM), Centro de Estudos de Doenças Crónicas (CEDOC), and Molecular cell biology and Immunology

Subjects

Antigen presentation, cancer-vaccines, lcsh:RS1-441, Pharmaceutical Science, Peptide binding, Sialic acid binding, Human leukocyte antigen, immunogenicity, Major histocompatibility complex, Article, lcsh:Pharmacy and materia medica, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Antigen-presentation, SDG 3 - Good Health and Well-being, MHC class I, MHC-I, dendritic-cells, dendritic-cells, antigen-presentation, MHC-I, immunogenicity, T-cell response, 030304 developmental biology, 0303 health sciences, biology, antigen-presentation, Immunogenicity, 3. Good health, Sialic acid, Cell biology, Dendritic-cells, chemistry, T-cell response, 030220 oncology & carcinogenesis, Cancer-vaccines, biology.protein, Antibody

Abstract

Maturation of human Dendritic Cells (DCs) is characterized by increased expression of antigen presentation molecules, and overall decreased levels of sialic acid at cell surface. Here, we aimed to identify sialylated proteins at DC surface and comprehend their role and modulation. Mass spectrometry analysis of DC&rsquo, s proteins, pulled down by a sialic acid binding lectin, identified molecules of the major human histocompatibility complex class I (MHC-I), known as human leucocyte antigen (HLA). After desialylation, DCs showed significantly higher reactivity with antibodies specific for properly folded MHC-I-&beta, 2-microglobulin complex and for &beta, 2-microglobulin but showed significant lower reactivity with an antibody specific for free MHC-I heavy chain. Similar results for antibody reactivities were observed for TAP2-deficient lymphoblastoid T2 cells, which express HLA-A*02:01. Using fluorescent peptide specifically fitting the groove of HLA-A*02:01, instead of antibody staining, also showed higher peptide binding on desialylated cells, confirming higher surface expression of MHC-I complex. A decay assay showed that desialylation doubled the half-life of MHC-I molecules at cell surface in both DCs and T2 cells. The biological impact of DC&acute, s desialylation was evaluated in co-cultures with autologous T cells, showing higher number and earlier immunological synapses, and consequent significantly increased production of IFN-&gamma, by T cells. In summary, sialic acid content modulates the expression and stability of complex MHC-I, which may account for the improved DC-T synapses.

Published

2020

39. Teleost fish IgM + plasma-like cells possess IgM-secreting, phagocytic, and antigen-presenting capacities.

Author

Wu L, Yang Y, Gao A, Li J, and Ye J

Subjects

Animals, Antigens, B-Lymphocytes, Immunoglobulin M, Mammals, Phagocytes metabolism, Tilapia

Abstract

Plasma cells are terminally differentiated antibody-secreting B lymphocytes that contribute to humoral immunity by producing large numbers of antibodies. Increasing evidence suggests that teleost fish B cells share certain characteristics with mammalian B1 B cells, including antibody-secreting, phagocytic, and antigen-presenting capacities. However, the difference between mature B cells and plasma cells remains unclear. In this study, we found that, based on their light-scattering characteristics, tilapia anterior kidney (AK) leukocytes can be categorized into two IgM + B-cell subsets: the lymphoid (L) gate and granulocyte-monocyte/macrophage (G-M) subsets. G-M gate cells are more numerous than L-gate cells and have higher mean fluorescence, but lower forward scatter and side scatter. We analyzed the morphological and ultrastructural features of sorted IgM + cells and found that L-gate IgM + cells have a high nucleus-cytoplasm ratio and lymphocyte-like morphology, whereas G-M gate IgM + cells have a small nucleus, more abundant endoplasmic reticulum, and a larger number of mitochondria, and have a plasma cell-like or macrophage-like morphology. To further characterize the cell types, we examined the specific patterns of expression of B-cell- and T-cell-related genes. We found that B-cell-specific genes were expressed by both L-gate and G-M gate IgM + cells, and that G-M gate IgM + cells secreted extremely high levels of IgM. However, T-cell-related genes were highly expressed only in L-gate IgM - cells. These results suggest that G-M gate IgM + cells are similar to plasma-like cells, with high antibody-secreting capacity. Given that G-M gate cells include the granulocyte, monocyte, and macrophage cell types, but not B cells, monocyte/macrophage markers were used to investigate the cell types further. A macrophage receptor with a collagenous structure was frequently observed, and macrophage-expressed gene-1 was highly expressed, in the G-M gate IgM + cells. Phagocytic capacity, as determined by ingestion of beads or bacteria, was significantly higher in G-M gate IgM + cells than in L-gate IgM + cells, as was antigen-processing capacity. Our findings show that tilapia AK leukocytes can be divided into two IgM + B-cell subsets and that G-M gate IgM + cells resemble plasma-like cells, having high antibody-secreting, phagocytic, and antigen-presenting capacities. Thus, this study increases our understanding of the functions of teleost fish plasma-like cells., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Wu, Yang, Gao, Li and Ye.)

Published

2022

40. CD1b Tetramers Identify T Cells that Recognize Natural and Synthetic Diacylated Sulfoglycolipids from Mycobacterium tuberculosis

Author

Momin Khan, Varinder K. Aggarwal, Ryan O. Emerson, Zuzanna Z. Moleda, Adriaan J. Minnaard, Martine Gilleron, D. Branch Moody, Charlotte A. James, Peter Reinink, Josephine F. Reijneveld, Dale I. Godfrey, Thomas J. Scriba, Michael N. T. Souter, Eleonora Diamanti, Krystle K. Q. Yu, Chetan Seshadri, Ildiko Van Rhijn, Stefanie Lenz, Daniel G. Pellicci, Vijayendar R. Yedulla, Jacques Prandi, Chemical Biology 2, Department of Engineering Mathematics, University of Bristol, University of Bristol [Bristol], Institut de pharmacologie et de biologie structurale (IPBS), Centre National de la Recherche Scientifique (CNRS)-Université Toulouse III - Paul Sabatier (UT3), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées, and University of Cape Town

Subjects

Models, Molecular, 0301 basic medicine, Acylation, T-Lymphocytes, [SDV]Life Sciences [q-bio], Clinical Biochemistry, Lymphocyte Activation, 01 natural sciences, Biochemistry, Antigens, CD1, Drug Discovery, Receptor, ComputingMilieux_MISCELLANEOUS, lipid antigen, antigen-presentation, 3. Good health, Cell biology, tuberculosis, Molecular Medicine, mycobacteria, Antigen presentation, T cells, CD1, Biology, Article, Cell Line, Mycobacterium tuberculosis, 03 medical and health sciences, Glycolipid, Antigen, Journal Article, Humans, Tuberculosis, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, human, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM], Molecular Biology, Pharmacology, Antigens, Bacterial, 010405 organic chemistry, T-cell receptor, biology.organism_classification, 0104 chemical sciences, 030104 developmental biology, Cell culture, Glycolipids, Protein Multimerization, T cell receptor

Abstract

Mycobacterial cell wall lipids bind the conserved CD1 family of antigen-presenting molecules and activate T cells via their T cell receptors (TCRs). Sulfoglycolipids (SGLs) are uniquely synthesized by Mycobacterium tuberculosis, but tools to study SGL-specific T cells in humans are lacking. We designed a novel hybrid synthesis of a naturally occurring SGL, generated CD1b tetramers loaded with natural or synthetic SGL analogs, and studied the molecular requirements for TCR binding and T cell activation. Two T cell lines derived using natural SGLs are activated by synthetic analogs independently of lipid chain length and hydroxylation, but differentially by saturation status. By contrast, two T cell lines derived using an unsaturated SGL synthetic analog were not activated by the natural antigen. Our data provide a bioequivalence hierarchy of synthetic SGL analogs and SGL-loaded CD1b tetramers. These reagents can now be applied to large-scale translational studies investigating the diagnostic potential of SGL-specific T cell responses or SGL-based vaccines. Sulfoglycolipids (SGLs) are uniquely synthesized by Mycobacterium tuberculosis (Mtb) and recognized by human T cells. James, Yu et al. describe a new hybrid synthesis for key antigenic determinants of SGLs and the development of SGL-specific tetramers that can now be applied to large-scale translational studies.

Published

2018

41. Activation of PAF-receptor induces regulatory dendritic cells through PGE2 and IL-10.

Author

Koga, Marianna M., Bizzarro, Bruna, Sá-Nunes, Anderson, Rios, Francisco J.O., and Jancar, Sonia

Abstract

Abstract: Activation of the platelet-activating factor receptor (PAFR) in macrophages is associated with suppressor phenotype. Here, we investigated the PAFR in murine dendritic cells (DC). Bone marrow-derived dendritic cells (BALB/c) were cultured with GM-CSF and maturation was induced by LPS. The PAFR antagonists (WEB2086, WEB2170, PCA4248) and the prostaglandin (PG) synthesis inhibitors (indomethacin, nimesulide and NS-398) were added before LPS. Mature and immature DCs expressed PAFR. LPS increased MHCII, CD40, CD80, CD86, CCR7 and induced IL-10, IL-12, COX-2 and PGE2 expression. IL-10, COX-2 and PGE2 levels were reduced by PAFR antagonists and increased by cPAF. The IL-10 production was independent of PGs. Mature DCs induced antigen-specific lymphocyte proliferation. PAFR antagonists or PG-synthesis inhibitors significantly increased lymphocyte proliferation. It is proposed that PAF has a central role in regulatory DC differentiation through potentiation of IL-10 and PGE2 production. [Copyright &y& Elsevier]

Published

2013

42. Antimalarials: Reversing the autoimmune “mal-area”?

Author

Shrivastava, Arun and Khanna, Dhanita

Published

2012

43. Immunology and pathogenesis of childhood TB.

Author

Jones, Christine, Whittaker, Elizabeth, Bamford, Alasdair, and Kampmann, Beate

Subjects

TUBERCULOSIS microbiology, AGE distribution, MYCOBACTERIUM tuberculosis, TUBERCULOSIS

Published

2011

44. A Cre-loxP based system for studying horizontal gene transfer

Author

Bergsmedh, Anna, Ehnfors, Jacob, Spetz, Anna-Lena, and Holmgren, Lars

Subjects

*GENETIC transformation, *DNA, *ANTIGENS, *NUCLEOPROTEINS

Abstract

Abstract: We have previously shown that DNA can be transferred to phagocytosing cells via the uptake of apoptotic cells. We report a model system that facilitates study of antigen presentation of genes transferred specifically via horizontal gene transfer. Constructs were generated encoding the LacZ gene or the influenza A nucleoprotein silenced by a STOP sequence flanked by two loxP sites. These reporter genes were demonstrated to be silent in donor cells and become activated after phagocytosis of Cre-expressing fibroblasts or macrophages. These results provide a model system for studying the influence of horizontally transferred antigens on activation of the immune system. [Copyright &y& Elsevier]

Published

2007

45. The cellular response in neuroinflammation: The role of leukocytes, microglia and astrocytes in neuronal death and survival

Author

Carson, Monica J., Cameron Thrash, J., and Walter, Barbara

Subjects

*NEUROLOGY, *INFLAMMATION, *CELLS, *NEURONS, *MICROGLIA

Abstract

Abstract: Neuroinflammation is a complex integration of the responses of all cells present within the CNS, including the neurons, macroglia, microglia and the infiltrating leukocytes. The initiating insult, environmental factors, genetic background and age/past experiences all combine to modulate the integrated response of this complex neuroinflammatory circuit. Here, we explore how these factors interact to lead to either neuroprotective versus neurotoxic inflammatory responses. We specifically focus on microglia and astrocytic regulation of autoreactive T cell responses. [Copyright &y& Elsevier]

Published

2006

46. How T lymphocytes recognize lipid antigens

Author

De Libero, Gennaro and Mori, Lucia

Subjects

*ANTIGENS, *LYMPHOCYTES, *STEROIDS, *MOLECULES

Abstract

Abstract: Recognition of lipid antigens by T lymphocytes is well established. Lipids are recognized by T cells when presented in association with CD1 antigen-presenting molecules. Both microbial and self lipids stimulate specific T lymphocytes, thus participating in immune reactions during infections and autoimmune diseases. The immune system uses a variety of strategies to solubilise lipid antigens, to facilitate their internalization, processing, and loading on CD1 molecules. Recent studies in the field of lipid antigen presentation have revealed new mechanisms which allow the immune system to sense lipids as stimulatory antigens. [Copyright &y& Elsevier]

Published

2006

47. Microglia and the control of autoreactive T cell responses

Author

Melchior, Benoit, Puntambekar, Shweta S., and Carson, Monica J.

Subjects

*MICROGLIA, *T cells, *VIRUS diseases, *DENDRITIC cells

Abstract

Abstract: Microglial activation is one of the earliest and most prominent features of nearly all CNS neuropathologies often occurring prior to other indicators of overt neuropathology. Whether microglial activation in seemingly healthy CNS tissue during the early stages of several is a response to early stages of neuronal or glial distress or an early sign of microglial dysfunction causing subsequent neurodegeneration is unknown. Here we characterize and discuss how changes in the CNS microenvironment (neuronal activity/viability, glial activation) lead to specific forms of microglial activation. Specifically, we examine the potential role that TREM-2 expressing microglia may play in regulating the effector function of autoreactive T cell responses. Thus, we suggest that ubiquitous suppression of microglial activation during CNS inflammatory disorders rather than targeted manipulation of microglial activation, may in the end be maladaptive leading to incomplete remission of symptoms. [Copyright &y& Elsevier]

Published

2006

48. Effects of Cyclophilin A on Myeloblastic Cell Line KG-1 Derived Dendritic Like Cells (DLC) Through p38 MAP Kinase Activation1,2

Author

Bharadwaj, Uddalak, Zhang, Rongxin, Yang, Hui, Li, Min, Doan, Linh X., Chen, Changyi, and Yao, Qizhi

Subjects

*IMMUNOREGULATION, *CYTOKINES, *LYMPHOCYTES, *DENDRITIC cells, *PYRIMIDINE nucleotides

Abstract

Background: Cyclophilin A (CypA) is a ubiquitously distributed intracellular protein as well as a secreted protein and has recently been reported to be an immunomodulatory molecule. The objective of this study was to determine the effect of CypA on dendritic cell (DC) differentiation, activation, and functional maturation. The role of p38 MAP kinase in DC functions was also investigated. Materials and methods: KG1 cells (CD34+ human myeloblastic cell line) were treated with cytokines (GM-CSF+IL-4) and/or CypA and expression of cell surface markers was analyzed by FACS analysis. The antigen-uptake capacity of different DCs was determined by FITC-dextran uptake assay. Antigen-presentation capacity of DCs was determined by allogeneic mixed lymphocyte reaction (MLR) by [3H] thymidine incorporation assay. To assess the T cell polarization stimulated by KG1 derived DCs, various Th1 and Th2 cytokines secreted by allostimulated CD4+ and CD8+ T cells were determined by Bioplex cytokine assay. Total and phosphorylated p38 MAPK activity in CypA treated DCs was detected by Bioplex p38 total and phosphoprotein assay. Results: During the differentiation of KG1 cells to immature DCs, cell surface expression of CD11b was increased by 30.6% for CypA alone, 55% for CypA plus cytokines, and 44% for cytokines alone. Similarly, CypA alone increased the cell surface expression of CD11c by 59% as compared to CypA plus cytokines (68%) and cytokines alone (50%). CypA up-regulated the antigen uptake capacity of the immature DCs to a greater extent (5 times) as compared to cytokines alone (2.5 times). Moreover, CypA augmented the capacity of DCs to present antigens to allogenic CD8+ T cells, and also increased the secretion of Th1 type cytokines TNF-α and IFN-γ from the allogenic CD4+ T cells. Furthermore, CypA induced the phosphorylation and hence activation of MAP kinase p38. Pre-treatment with SB-203580, a p38 inhibitor, significantly reduced MLR stimulatory capacity of CypA-induced DCs in both CD8+ and CD4+ T cells (P < 0.05). Conclusions: CypA enhances DC differentiation and maturation by up-regulating CD11b and CD11c expression. CypA can also augment DC antigen uptake and antigen presentation, which may be mediated by the p38 signaling pathway. [Copyright &y& Elsevier]

Published

2005

49. Regulation of the humanleukocyte-derived arginine aminopeptidase endoplasmic reticulum-aminopeptidase 2gene by interferon-γ.

Author

Tanioka, Toshihiro, Hattori, Akira, Mizutani, Shigehiko, and Tsujimoto, Masafumi

Subjects

*LEUCOCYTES, *ARGININE, *AMINOPEPTIDASES, *ENDOPLASMIC reticulum, *PEPTIDES, *LEUCINE

Abstract

The leukocyte-derived arginine aminopeptidase (L-RAP) is the second aminopeptidase localized in the endoplasmic reticulum (ER) processing antigenic peptides presented to major histocompatibility complex (MHC) class I molecules. In this study, the genomic organization of the gene encoding human L-RAP was determined and the regulatory mechanism of its expression was elucidated.The entire genomic structure of theL-RAPgene is similar to bothplacental leucine aminopeptidase(P-LAP) andadipocyte-derived leucine aminopeptidase(A-LAP) genes, confirming the close relationship of these three enzymes. Interferon (IFN)-γ up-regulates the expression of theL-RAPgene. Deletion and site-directed mutagenic analyses of the 5′-flanking region of theL-RAPgene and electrophoretic mobility shift assay indicated that while interferon regulatory factor (IRF)-2 is important in the basal condition, IRF-1 is the primary regulator of IFN-γ-mediated augmentation of the gene expression. In addition, PU.1, a member of the E26 transformation-specificfamily of transcription factors, also plays a role in the regulation of gene expression. The maximum expression of the gene was achieved by coexpression of IRF-1 and PU.1 in HEK293 cells and IRF-2 suppressed the IRF-1-mediated enhancement of gene expression, suggesting that IFN-γ-inducedL-RAPgene expression is cooperatively regulated by IRFs and PU.1 transcription factors. [ABSTRACT FROM AUTHOR]

Published

2005

50. Development of new strategies to prevent type 1 diabetes: the role of animal models.

Author

Hänninen, Arno, Hamilton-Williams, Emma, and Kurts, Christian

Subjects

DIABETES, CARBOHYDRATE intolerance, ENDOCRINE diseases, NUTRITION disorders, AUTOANTIBODIES, IMMUNOGLOBULINS

Abstract

Type 1 diabetes is an immune-mediated disease typically preceded by a long preclinical stage during which a growing number of islet-cell-specific autoantibodies appear in the serum. Although antigen-specific T lymphocytes and cytokines rather than these autoantibodies are the likely executors of β-cell-destruction, these autoantibodies reflect the existence of autoimmunity that targets islet β-cells. Abrogation of this autoimmunity during the preclinical stage would be the key to the prevention of type 1 diabetes. However, the quest of protecting islet-cells from the immune attack requires detailed knowledge of mechanisms that control islet-inflammation and β-cell-destruction, and of mechanisms that control immune tolerance to peripheral self-antigens in general. This knowledge can only be obtained through further innovative research in experimental animal models. In this review, we will first examine how research in non-obese diabetic mice has already led to promising new strategies of diabetes prevention now being tested in human clinical trials. Thereafter, we will discuss how recent advances in understanding the mechanisms that control immune response to peripheral self-antigens such as β-cell antigens may help to develop even more selective and effective strategies to prevent diabetes in the future. [ABSTRACT FROM AUTHOR]

Published

2003