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43 results on '"CD40 Antigens"'

1. Plasma extracellular vesicles bearing PD-L1, CD40, CD40L or TNF-RII are significantly reduced after treatment of AIDS-NHL

Author

Martínez, Laura E, Lensing, Shelly, Chang, Di, Magpantay, Larry I, Mitsuyasu, Ronald, Ambinder, Richard F, Sparano, Joseph A, Martínez-Maza, Otoniel, and Epeldegui, Marta

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Hematology, Rare Diseases, Lymphoma, Clinical Research, Clinical Trials and Supportive Activities, Cancer, 2.1 Biological and endogenous factors, Aetiology, Acquired Immunodeficiency Syndrome, B7-H1 Antigen, CD40 Antigens, CD40 Ligand, Extracellular Vesicles, Humans, Lymphoma, AIDS-Related, Receptors, Tumor Necrosis Factor, Type II
Abstract

Emerging evidence shows that tumor cells secrete extracellular vesicles (EVs) that carry bioactive cell surface markers, such as programmed death-ligand 1 (PD-L1), which can modulate immune responses and inhibit anti-tumor responses, potentially playing a role in lymphomagenesis and in promoting the growth of these cancers. In this study, we investigated the role of EVs expressing cell surface molecules associated with B cell activation and immune regulation. We measured levels of EVs derived from plasma from 57 subjects with AIDS-related non-Hodgkin lymphoma (AIDS-NHL) enrolled in the AIDS Malignancies Consortium (AMC) 034 clinical trial at baseline and post-treatment with rituximab plus concurrent infusional EPOCH chemotherapy. We found that plasma levels of EVs expressing PD-L1, CD40, CD40L or TNF-RII were significantly reduced after cancer treatment. AIDS-NHL patients with the diffuse large B cell lymphoma (DLBCL) tumor subtype had decreased plasma levels of EVs bearing PD-L1, compared to those with Burkitt's lymphoma. CD40, CD40L and TNF-RII-expressing EVs showed a significant positive correlation with plasma levels of IL-10, CXCL13, sCD25, sTNF-RII and IL-18. Our results suggest that patients with AIDS-NHL have higher levels of EVs expressing PD-L1, CD40, CD40L or TNF-RII in circulation before cancer treatment and that levels of these EVs are associated with levels of biomarkers of microbial translocation and inflammation.

Published
2022

2. A cell‐penetrating CD40‐TRAF2,3 blocking peptide diminishes inflammation and neuronal loss after ischemia/reperfusion

Author

Portillo, Jose‐Andres C, Yu, Jin‐Sang, Hansen, Samuel, Kern, Timothy S, Subauste, M Cecilia, and Subauste, Carlos S

Subjects
Biomedical and Clinical Sciences, Immunology, Prevention, 2.1 Biological and endogenous factors, Aetiology, Animals, CD40 Antigens, Endothelial Cells, Female, Humans, Inflammation, Ischemia, Male, Mice, Neurons, Peptides, Reperfusion, Signal Transduction, TNF Receptor-Associated Factor 2, endothelial, muller cell, polymorphonuclear leukocyte, retina, toxoplasma, Biochemistry and Cell Biology, Physiology, Medical Physiology, Biochemistry & Molecular Biology, Biochemistry and cell biology, Medical physiology
Abstract

While the administration of anti-CD154 mAbs in mice validated the CD40-CD154 pathway as a target against inflammatory disorders, this approach caused thromboembolism in humans (unrelated to CD40 inhibition) and is expected to predispose to opportunistic infections. There is a need for alternative approaches to inhibit CD40 that avoid these complications. CD40 signals through TRAF2,3 and TRAF6-binding sites. Given that CD40-TRAF6 is the pathway that stimulates responses key for cell-mediated immunity against opportunistic pathogens, we examined the effects of pharmacologic inhibition of CD40-TRAF2,3 signaling. We used a model of ischemia/reperfusion (I/R)-induced retinopathy, a CD40-driven inflammatory disorder. Intravitreal administration of a cell-penetrating CD40-TRAF2,3 blocking peptide impaired ICAM-1 upregulation in retinal endothelial cells and CXCL1 upregulation in endothelial and Müller cells. The peptide reduced leukocyte infiltration, upregulation of NOS2/COX-2/TNF-α/IL-1β, and ameliorated neuronal loss, effects that mimic those observed after I/R in Cd40-/- mice. While a cell-penetrating CD40-TRAF6 blocking peptide also diminished I/R-induced inflammation, this peptide (but not the CD40-TRAF2,3 blocking peptide) impaired control of the opportunistic pathogen Toxoplasma gondii in the retina. Thus, inhibition of the CD40-TRAF2,3 pathway is a novel and potent approach to reduce CD40-induced inflammation, while likely diminishing the risk of opportunistic infections that would otherwise accompany CD40 inhibition.

Published
2021

3. Genetic modifiers of respiratory function in Duchenne muscular dystrophy.

Author

Bello, Luca, DAngelo, Grazia, Villa, Matteo, Fusto, Aurora, Vianello, Sara, Merlo, Beatrice, Sabbatini, Daniele, Barp, Andrea, Gandossini, Sandra, Magri, Francesca, Comi, Giacomo, Pedemonte, Marina, Tacchetti, Paola, Lanzillotta, Valentina, Trucco, Federica, DAmico, Adele, Bertini, Enrico, Astrea, Guja, Politano, Luisa, Masson, Riccardo, Baranello, Giovanni, Albamonte, Emilio, De Mattia, Elisa, Rao, Fabrizio, Sansone, Valeria, Previtali, Stefano, Messina, Sonia, Vita, Gian, Berardinelli, Angela, Mongini, Tiziana, Pini, Antonella, Pane, Marika, Mercuri, Eugenio, Vianello, Andrea, Bruno, Claudio, Hoffman, Eric, Morgenroth, Lauren, Gordish-Dressman, Heather, Pegoraro, Elena, and McDonald, Craig

Subjects
Adolescent, Adult, CD40 Antigens, Child, Child, Preschool, Dystrophin, Follow-Up Studies, Glucocorticoids, Humans, Male, Muscular Dystrophy, Duchenne, Osteopontin, Respiratory Function Tests, Respiratory Insufficiency, Retrospective Studies, Vital Capacity, Young Adult
Abstract

OBJECTIVE: Respiratory insufficiency is a major complication of Duchenne muscular dystrophy (DMD). Its progression shows considerable interindividual variability, which has been less thoroughly characterized and understood than in skeletal muscle. We collected pulmonary function testing (PFT) data from a large retrospective cohort followed at Centers collaborating in the Italian DMD Network. Furthermore, we analyzed PFT associations with different DMD mutation types, and with genetic variants in SPP1, LTBP4, CD40, and ACTN3, known to modify skeletal muscle weakness in DMD. Genetic association findings were independently validated in the Cooperative International Neuromuscular Research Group Duchenne Natural History Study (CINRG-DNHS). METHODS AND RESULTS: Generalized estimating equation analysis of 1852 PFTs from 327 Italian DMD patients, over an average follow-up time of 4.5 years, estimated that forced vital capacity (FVC) declined yearly by -4.2%, forced expiratory volume in 1 sec by -5.0%, and peak expiratory flow (PEF) by -2.9%. Glucocorticoid (GC) treatment was associated with higher values of all PFT measures (approximately + 15% across disease stages). Mutations situated 3 of DMD intron 44, thus predicted to alter the expression of short dystrophin isoforms, were associated with lower (approximately -6%) PFT values, a finding independently validated in the CINRG-DNHS. Deletions amenable to skipping of exon 51 and 53 were independently associated with worse PFT outcomes. A meta-analysis of the two cohorts identified detrimental effects of SPP1 rs28357094 and CD40 rs1883832 minor alleles on both FVC and PEF. INTERPRETATION: These findings support GC efficacy in delaying respiratory insufficiency, and will be useful for the design and interpretation of clinical trials focused on respiratory endpoints in DMD.

Published
2020

4. Further Evidence That the Soluble Urokinase Plasminogen Activator Receptor Does Not Directly Injure Mice or Human Podocytes.

Author

Harel, Efrat, Shoji, Jun, Abraham, Vivek, Miller, Loan, Laszik, Zoltan G, King, Andrew, Dobi, Dejan, Szabo, Gyula, Hann, Byron, Sarwal, Minnie M, Craik, Charles S, and Vincenti, Flavio

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Kidney Disease, Aetiology, 2.1 Biological and endogenous factors, Animals, Autoantibodies, Biopsy, CD40 Antigens, Cells, Cultured, Glomerulosclerosis, Focal Segmental, Humans, Kidney, Mice, Mice, Knockout, Podocytes, Primary Cell Culture, Receptors, Urokinase Plasminogen Activator, Recombinant Proteins, Medical and Health Sciences, Surgery, Clinical sciences, Immunology
Abstract

BackgroundThe role of the soluble urokinase plasminogen activator receptor (suPAR) in focal segmental glomerulosclerosis (FSGS) as the circulating factor or as a predictor of recurrence after transplantation remains controversial. Previously published studies in mice and isolated podocytes produced conflicting results on the effect of suPAR on podocyte injury, effacement of foot processes, and proteinuria. These discordant results were in part due to diverse experimental designs and different strains of mice. The aim of our study was to determine the reasons for the inconsistencies of the previous studies results with suPAR by using uniform methods and studies in different strains of mice.MethodsWe utilized a primary culture of human podocytes and 2 mouse models, the wild type (WT) and the urokinase plasminogen activator receptor (uPAR) KO (uPAR), in an attempt to resolve the reported conflicting results.ResultsIn both WT and uPAR mouse models, injection of recombinant uPAR, even at a high dose (100 μg), did not induce proteinuria, effacement of podocytes, or disruption of the cytoskeleton. Injection of suPAR resulted in its deposition exclusively in the glomerular endothelial cells and not in the podocytes of WT mice and was not detected at the uPAR KO mice. Kidneys from patients with recurrent FSGS had negative immunostaining for uPAR. We also evaluated the effect of recombinant uPAR on primary culture of human podocytes. uPAR did not result in podocytes damage.ConclusionssuPAR by itself is not the cause for direct podocyte injury, in vitro or in vivo. These findings suggest a more complex and still poorly understood role of suPAR in FSGS.

Published
2020

5. Proinflammatory cytokines and ARDS pulmonary edema fluid induce CD40 on human mesenchymal stromal cells—A potential mechanism for immune modulation

Author

Wilfong, Erin M, Croze, Roxanne, Fang, Xiaohui, Schwede, Matthew, Niemi, Erene, López, Giselle Y, Lee, Jae-Woo, Nakamura, Mary C, and Matthay, Michael A

Subjects
Biomedical and Clinical Sciences, Immunology, Stem Cell Research, Lung, Rare Diseases, Stem Cell Research - Nonembryonic - Human, Acute Respiratory Distress Syndrome, Bronchoalveolar Lavage Fluid, CD40 Antigens, Cell Adhesion Molecules, Cell Transdifferentiation, Cells, Cultured, Cyclooxygenase 2, Cytokines, Female, Humans, Lipopolysaccharides, Male, Mesenchymal Stem Cells, Respiratory Distress Syndrome, Transcription, Genetic, Up-Regulation, General Science & Technology
Abstract

Human mesenchymal stem/stromal cells (hMSCs) are a promising therapy for acute respiratory distress syndrome (ARDS) and other inflammatory conditions. While considerable research has focused on paracrine effects and mitochondrial transfer that improve lung fluid balance, hMSCs are well known to have immunomodulatory properties as well. Some of these immunomodulatory properties have been related to previously reported paracrine effectors such as indoleamine-2,3-dioxygenase (IDO), but these effects cannot fully account for cell-contact dependent immunomodulation. Here, we report that CD40 is upregulated on hMSCs under the same conditions previously reported to induce IDO. Further, CD40 transcription is also upregulated on hMSCs by ARDS pulmonary edema fluid but not by hydrostatic pulmonary edema fluid. Transcription of CD40, as well as paracrine effectors TSG6 and PTGS2 remained significantly upregulated for at least 12 hours after withdrawal of cytokine stimulation. Finally, induction of this immune phenotype altered the transdifferentiation of hMSCs, one of their hallmark properties. CD40 may play an important role in the immunomodulatory effects of hMSCs in ARDS and inflammation.

Published
2020

6. Proinflammatory cytokines and ARDS pulmonary edema fluid induce CD40 on human mesenchymal stromal cells-A potential mechanism for immune modulation.

Author

Wilfong, Erin M, Croze, Roxanne, Fang, Xiaohui, Schwede, Matthew, Niemi, Erene, López, Giselle Y, Lee, Jae-Woo, Nakamura, Mary C, and Matthay, Michael A

Subjects
Cells, Cultured, Mesenchymal Stem Cells, Bronchoalveolar Lavage Fluid, Humans, Lipopolysaccharides, Cell Adhesion Molecules, Cytokines, Transcription, Genetic, Up-Regulation, Female, Male, Cyclooxygenase 2, Cell Transdifferentiation, CD40 Antigens, Respiratory Distress Syndrome, Cells, Cultured, Transcription, Genetic, General Science & Technology
Abstract

Human mesenchymal stem/stromal cells (hMSCs) are a promising therapy for acute respiratory distress syndrome (ARDS) and other inflammatory conditions. While considerable research has focused on paracrine effects and mitochondrial transfer that improve lung fluid balance, hMSCs are well known to have immunomodulatory properties as well. Some of these immunomodulatory properties have been related to previously reported paracrine effectors such as indoleamine-2,3-dioxygenase (IDO), but these effects cannot fully account for cell-contact dependent immunomodulation. Here, we report that CD40 is upregulated on hMSCs under the same conditions previously reported to induce IDO. Further, CD40 transcription is also upregulated on hMSCs by ARDS pulmonary edema fluid but not by hydrostatic pulmonary edema fluid. Transcription of CD40, as well as paracrine effectors TSG6 and PTGS2 remained significantly upregulated for at least 12 hours after withdrawal of cytokine stimulation. Finally, induction of this immune phenotype altered the transdifferentiation of hMSCs, one of their hallmark properties. CD40 may play an important role in the immunomodulatory effects of hMSCs in ARDS and inflammation.

Published
2020

7. Differential cell-intrinsic regulations of germinal center B and T cells by miR-146a and miR-146b.

Author

Cho, Sunglim, Lee, Hyang-Mi, Yu, I-Shing, Choi, Youn, Huang, Hsi-Yuan, Hashemifar, Somaye, Lin, Ling-Li, Chen, Mei-Chi, Afanasiev, Nikita, Khan, Aly, Lin, Shu-Wha, Rudensky, Alexander, Crotty, Shane, and Lu, Li-Fan

Subjects
Animals, Autoantibodies, Autoimmunity, B-Lymphocytes, Bone Marrow Cells, CD40 Antigens, Cell Differentiation, Gene Expression Regulation, Germinal Center, Immunity, Humoral, Interleukin-4, Mice, Mice, Transgenic, MicroRNAs, Primary Cell Culture, Protein Isoforms, Signal Transduction, T-Lymphocytes, Helper-Inducer
Abstract

Reciprocal interactions between B and follicular T helper (Tfh) cells orchestrate the germinal center (GC) reaction, a hallmark of humoral immunity. Abnormal GC responses could lead to the production of pathogenic autoantibodies and the development of autoimmunity. Here we show that miR-146a controls GC responses by targeting multiple CD40 signaling pathway components in B cells; by contrast, loss of miR-146a in T cells does not alter humoral responses. However, specific deletion of both miR-146a and its paralog, miR-146b, in T cells increases Tfh cell numbers and enhanced GC reactions. Thus, our data reveal differential cell-intrinsic regulations of GC B and Tfh cells by miR-146a and miR-146b. Together, members of the miR-146 family serve as crucial molecular brakes to coordinately control GC reactions to generate protective humoral responses without eliciting unwanted autoimmunity.

Published
2018

8. CD40 Mediates Maturation of Thymic Dendritic Cells Driven by Self-Reactive CD4+ Thymocytes and Supports Development of Natural Regulatory T Cells

Author

Oh, Jaehak, Wu, Nan, Barczak, Andrea J, Barbeau, Rebecca, Erle, David J, and Shin, Jeoung-Sook

Subjects
HIV/AIDS, Animals, CD4-Positive T-Lymphocytes, CD40 Antigens, Cell Differentiation, Dendritic Cells, Mice, Self Tolerance, Signal Transduction, T-Lymphocytes, Regulatory, Thymocytes, Thymus Gland, Immunology
Abstract

Thymic dendritic cells (tDCs) play an important role in central tolerance by eliminating self-reactive thymocytes or differentiating them to regulatory T (Treg) cells. However, the molecular and cellular mechanisms underlying these functions are not completely understood. We found that mouse tDCs undergo maturation following cognate interaction with self-reactive CD4+ thymocytes and that this maturation is dependent on CD40 signaling. Ablation of CD40 expression in tDCs resulted in a significant reduction in the number of Treg cells in association with a significant reduction in the number of mature tDCs. In addition, CD40-deficient DCs failed to fully mature upon cognate interaction with CD4+ thymocytes in vitro and failed to differentiate them into Treg cells to a sufficient number. These findings suggest that tDCs mature and potentiate Treg cell development in feedback response to self-reactive CD4+ thymocytes.

Published
2018

9. Exogenous IL-33 Restores Dendritic Cell Activation and Maturation in Established Cancer.

Author

Dominguez, Donye, Ye, Cong, Geng, Zhe, Chen, Siqi, Fan, Jie, Qin, Lei, Long, Alan, Wang, Long, Zhang, Zhuoli, Zhang, Yi, Fang, Deyu, Kuzel, Timothy M, and Zhang, Bin

Subjects
Dendritic Cells, CD8-Positive T-Lymphocytes, Tumor Cells, Cultured, Animals, Mice, Inbred C57BL, Mice, Neoplasms, Experimental, Proto-Oncogene Proteins B-raf, Recombinant Proteins, Cytotoxicity, Immunologic, STAT1 Transcription Factor, PTEN Phosphohydrolase, Myeloid Differentiation Factor 88, Interleukin-33, Interleukin-1 Receptor-Like 1 Protein, CD40 Antigens, Biotechnology, Vaccine Related, Immunization, Cancer, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Immunology
Abstract

The role of IL-33, particularly in tumor growth and tumor immunity, remains ill-defined. We show that exogenous IL-33 can induce robust antitumor effect through a CD8+ T cell-dependent mechanism. Systemic administration of rIL-33 alone was sufficient to inhibit growth of established tumors in transplant and de novo melanoma tumorigenesis models. Notably, in addition to a direct action on CD8+ T cell expansion and IFN-γ production, rIL-33 therapy activated myeloid dendritic cells (mDCs) in tumor-bearing mice, restored antitumor T cell activity, and increased Ag cross-presentation within the tumor microenvironment. Furthermore, combination therapy consisting of rIL-33 and agonistic anti-CD40 Abs demonstrated synergistic antitumor activity. Specifically, MyD88, an essential component of the IL-33 signaling pathway, was required for the IL-33-mediated increase in mDC number and upregulation in expression of costimulatory molecules. Importantly, we identified that the IL-33 receptor ST2, MyD88, and STAT1 cooperate to induce costimulatory molecule expression on mDCs in response to rIL-33. Thus, our study revealed a novel IL-33-ST2-MyD88-STAT1 axis that restores mDC activation and maturation in established cancer and, thereby, the magnitude of antitumor immune responses, suggesting a potential use of rIL-33 as a new immunotherapy option to treat established cancer.

Published
2017

10. CD40 in Retinal Müller Cells Induces P2X7-Dependent Cytokine Expression in Macrophages/Microglia in Diabetic Mice and Development of Early Experimental Diabetic Retinopathy

Author

Portillo, Jose-Andres C, Corcino, Yalitza Lopez, Miao, Yanling, Tang, Jie, Sheibani, Nader, Kern, Timothy S, Dubyak, George R, and Subauste, Carlos S

Subjects
Biomedical and Clinical Sciences, Ophthalmology and Optometry, Eye Disease and Disorders of Vision, Diabetes, 2.1 Biological and endogenous factors, Aetiology, Metabolic and endocrine, Animals, CD40 Antigens, Capillaries, Cytokines, Diabetes Mellitus, Experimental, Diabetic Retinopathy, Ependymoglial Cells, Inflammation, Intercellular Adhesion Molecule-1, Interleukin-1beta, Leukostasis, Macrophages, Male, Mice, Mice, Knockout, Microglia, Myeloid Cells, Nitric Oxide Synthase Type II, Purinergic P2X Receptor Antagonists, Receptors, Purinergic P2X7, Tumor Necrosis Factor-alpha, Type C Phospholipases, Medical and Health Sciences, Endocrinology & Metabolism, Biomedical and clinical sciences
Abstract

Müller cells and macrophages/microglia are likely important for the development of diabetic retinopathy; however, the interplay between these cells in this disease is not well understood. An inflammatory process is linked to the onset of experimental diabetic retinopathy. CD40 deficiency impairs this process and prevents diabetic retinopathy. Using mice with CD40 expression restricted to Müller cells, we identified a mechanism by which Müller cells trigger proinflammatory cytokine expression in myeloid cells. During diabetes, mice with CD40 expressed in Müller cells upregulated retinal tumor necrosis factor-α (TNF-α), interleukin 1β (IL-1β), intracellular adhesion molecule 1 (ICAM-1), and nitric oxide synthase (NOS2), developed leukostasis and capillary degeneration. However, CD40 did not cause TNF-α or IL-1β secretion in Müller cells. TNF-α was not detected in Müller cells from diabetic mice with CD40+ Müller cells. Rather, TNF-α was upregulated in macrophages/microglia. CD40 ligation in Müller cells triggered phospholipase C-dependent ATP release that caused P2X7-dependent production of TNF-α and IL-1β by macrophages. P2X7-/- mice and mice treated with a P2X7 inhibitor were protected from diabetes-induced TNF-α, IL-1β, ICAM-1, and NOS2 upregulation. Our studies indicate that CD40 in Müller cells is sufficient to upregulate retinal inflammatory markers and appears to promote experimental diabetic retinopathy and that Müller cells orchestrate inflammatory responses in myeloid cells through a CD40-ATP-P2X7 pathway.

Published
2017

11. Loss of CD40 attenuates experimental diabetes-induced retinal inflammation but does not protect mice from electroretinogram defects

Author

Samuels, Ivy S, Portillo, Jose-Andres C, Miao, Yanling, Kern, Timothy S, and Subauste, Carlos S

Subjects
Biomedical and Clinical Sciences, Ophthalmology and Optometry, Prevention, Eye Disease and Disorders of Vision, Diabetes, Neurosciences, Aetiology, 2.1 Biological and endogenous factors, Metabolic and endocrine, Eye, Animals, CD40 Antigens, Diabetes Mellitus, Experimental, Diabetic Retinopathy, Electroretinography, Female, Intercellular Adhesion Molecule-1, Interleukin-1beta, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Nitric Oxide Synthase Type II, RNA, Messenger, Real-Time Polymerase Chain Reaction, Retina, Retinitis, Tumor Necrosis Factor-alpha, Up-Regulation, CD40, Diabetic retinopathy, Electroretinogram, Inflammation, Medical and Health Sciences, Psychology and Cognitive Sciences, Neurology & Neurosurgery, Ophthalmology and optometry
Abstract

Chronic low grade inflammation is considered to contribute to the development of experimental diabetic retinopathy (DR). We recently demonstrated that lack of CD40 in mice ameliorates the upregulation of inflammatory molecules in the diabetic retina and prevented capillary degeneration, a hallmark of experimental diabetic retinopathy. Herein, we investigated the contribution of CD40 to diabetes-induced reductions in retinal function via the electroretinogram (ERG) to determine if inflammation plays a role in the development of ERG defects associated with diabetes. We demonstrate that diabetic CD40-/- mice are not protected from reduction to the ERG b-wave despite failing to upregulate inflammatory molecules in the retina. Our data therefore supports the hypothesis that retinal dysfunction found in diabetics occurs independent of the induction of inflammatory processes.

Published
2017

12. CD40-Mediated NF-κB Activation in B Cells Is Increased in Multiple Sclerosis and Modulated by Therapeutics

Author

Chen, Ding, Ireland, Sara J, Remington, Gina, Alvarez, Enrique, Racke, Michael K, Greenberg, Benjamin, Frohman, Elliot M, and Monson, Nancy L

Subjects
Neurodegenerative, Brain Disorders, Multiple Sclerosis, Autoimmune Disease, Neurosciences, 2.1 Biological and endogenous factors, Aetiology, Neurological, Aged, B-Lymphocytes, CD40 Antigens, Drug Therapy, Combination, Extracellular Signal-Regulated MAP Kinases, Female, Glatiramer Acetate, Humans, Immunologic Memory, Interferon beta-1a, Lymphocyte Activation, MAP Kinase Signaling System, Male, Middle Aged, Mycophenolic Acid, Phosphorylation, Transcription Factor RelA, Immunology
Abstract

CD40 interacts with CD40L and plays an essential role in immune regulation and homeostasis. Recent research findings, however, support a pathogenic role of CD40 in a number of autoimmune diseases. We previously showed that memory B cells from relapsing-remitting multiple sclerosis (RRMS) patients exhibited enhanced proliferation with CD40 stimulation compared with healthy donors. In this study, we used a multiparameter phosflow approach to analyze the phosphorylation status of NF-κB and three major MAPKs (P38, ERK, and JNK), the essential components of signaling pathways downstream of CD40 engagement in B cells from MS patients. We found that memory and naive B cells from RRMS and secondary progressive MS patients exhibited a significantly elevated level of phosphorylated NF-κB (p-P65) following CD40 stimulation compared with healthy donor controls. Combination therapy with IFN-β-1a (Avonex) and mycophenolate mofetil (Cellcept) modulated the hyperphosphorylation of P65 in B cells of RRMS patients at levels similar to healthy donor controls. Lower disease activity after the combination therapy correlated with the reduced phosphorylation of P65 following CD40 stimulation in treated patients. Additionally, glatiramer acetate treatment also significantly reduced CD40-mediated P65 phosphorylation in RRMS patients, suggesting that reducing CD40-mediated p-P65 induction may be a general mechanism by which some current therapies modulate MS disease.

Published
2016

13. Association Study of Exon Variants in the NF-κB and TGFβ Pathways Identifies CD40 as a Modifier of Duchenne Muscular Dystrophy.

Author

Bello, Luca, Flanigan, Kevin, Weiss, Robert, Spitali, Pietro, Aartsma-Rus, Annemieke, Muntoni, Francesco, Zaharieva, Irina, Ferlini, Alessandra, Mercuri, Eugenio, Tuffery-Giraud, Sylvie, Claustres, Mireille, Straub, Volker, Lochmüller, Hanns, Barp, Andrea, Vianello, Sara, Pegoraro, Elena, Punetha, Jaya, Gordish-Dressman, Heather, Giri, Mamta, Hoffman, Eric, and McDonald, Craig

Subjects
Adolescent, Alleles, CD40 Antigens, Case-Control Studies, Child, Dystrophin, Exons, Genes, Modifier, Genome-Wide Association Study, Glucocorticoids, Humans, Latent TGF-beta Binding Proteins, Muscular Dystrophy, Duchenne, Mutation, NF-kappa B, Osteopontin, Polymorphism, Single Nucleotide, Transforming Growth Factor beta, White People
Abstract

The expressivity of Mendelian diseases can be influenced by factors independent from the pathogenic mutation: in Duchenne muscular dystrophy (DMD), for instance, age at loss of ambulation (LoA) varies between individuals whose DMD mutations all abolish dystrophin expression. This suggests the existence of trans-acting variants in modifier genes. Common single nucleotide polymorphisms (SNPs) in candidate genes (SPP1, encoding osteopontin, and LTBP4, encoding latent transforming growth factor β [TGFβ]-binding protein 4) have been established as DMD modifiers. We performed a genome-wide association study of age at LoA in a sub-cohort of European or European American ancestry (n = 109) from the Cooperative International Research Group Duchenne Natural History Study (CINRG-DNHS). We focused on protein-altering variants (Exome Chip) and included glucocorticoid treatment as a covariate. As expected, due to the small population size, no SNPs displayed an exome-wide significant p value (< 1.8 × 10-6). Subsequently, we prioritized 438 SNPs in the vicinities of 384 genes implicated in DMD-related pathways, i.e., the nuclear-factor-κB and TGFβ pathways. The minor allele at rs1883832, in the 5-untranslated region of CD40, was associated with earlier LoA (p = 3.5 × 10-5). This allele diminishes the expression of CD40, a co-stimulatory molecule for T cell polarization. We validated this association in multiple independent DMD cohorts (United Dystrophinopathy Project, Bio-NMD, and Padova, total n = 660), establishing this locus as a DMD modifier. This finding points to cell-mediated immunity as a relevant pathogenetic mechanism and potential therapeutic target in DMD.

Published
2016

14. Gut dendritic cell activation links an altered colonic microbiome to mucosal and systemic T-cell activation in untreated HIV-1 infection

Author

Dillon, SM, Lee, EJ, Kotter, CV, Austin, GL, Gianella, S, Siewe, B, Smith, DM, Landay, AL, McManus, MC, Robertson, CE, Frank, DN, McCarter, MD, and Wilson, CC

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Microbiome, Clinical Research, Sexually Transmitted Infections, HIV/AIDS, 2.1 Biological and endogenous factors, Infection, Oral and gastrointestinal, Adult, Antigens, CD, Antigens, CD1, CD4-Positive T-Lymphocytes, CD40 Antigens, CD8-Positive T-Lymphocytes, Case-Control Studies, Cell Lineage, Colon, Dendritic Cells, Female, Gastrointestinal Microbiome, Gene Expression Regulation, Glycoproteins, HIV Infections, HIV-1, Humans, Immunoglobulins, Interferon-gamma, Lymphocyte Activation, Male, Membrane Glycoproteins, Middle Aged, Mucous Membrane, Prevotella, Ruminococcus, Signal Transduction, Viral Load, CD83 Antigen, Biological Sciences, Medical and Health Sciences
Abstract

HIV-1-associated disruption of intestinal homeostasis is a major factor contributing to chronic immune activation and inflammation. Dendritic cells (DCs) are crucial in maintaining intestinal homeostasis, but the impact of HIV-1 infection on intestinal DC number and function has not been extensively studied. We compared the frequency and activation/maturation status of colonic myeloid DC (mDC) subsets (CD1c(+) and CD1c(neg)) and plasmacytoid DCs in untreated HIV-1-infected subjects with uninfected controls. Colonic mDCs in HIV-1-infected subjects had increased CD40 but decreased CD83 expression, and CD40 expression on CD1c(+) mDCs positively correlated with mucosal HIV-1 viral load, with mucosal and systemic cytokine production, and with frequencies of activated colon and blood T cells. Percentage of CD83(+)CD1c(+) mDCs negatively correlated with frequencies of interferon-γ-producing colon CD4(+) and CD8(+) T cells. CD40 expression on CD1c(+) mDCs positively associated with abundance of high prevalence mucosal Prevotella copri and Prevotella stercorea but negatively associated with a number of low prevalence mucosal species, including Rumminococcus bromii. CD1c(+) mDC cytokine production was greater in response to in vitro stimulation with Prevotella species relative to R. bromii. These findings suggest that, during HIV infection, colonic mDCs become activated upon exposure to mucosal pathobiont bacteria leading to mucosal and systemic immune activation.

Published
2016

15. Gut dendritic cell activation links an altered colonic microbiome to mucosal and systemic T-cell activation in untreated HIV-1 infection

Author

Dillon, SM, Lee, EJ, Kotter, CV, Austin, GL, Gianella, S, Siewe, B, Smith, DM, Landay, AL, McManus, MC, Robertson, CE, Frank, DN, McCarter, MD, and Wilson, CC

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Clinical Research, HIV/AIDS, Digestive Diseases, Infectious Diseases, Emerging Infectious Diseases, Aetiology, 2.1 Biological and endogenous factors, Infection, Inflammatory and immune system, Adult, Antigens, CD, Antigens, CD1, CD4-Positive T-Lymphocytes, CD40 Antigens, CD8-Positive T-Lymphocytes, Case-Control Studies, Cell Lineage, Colon, Dendritic Cells, Female, Gastrointestinal Microbiome, Gene Expression Regulation, Glycoproteins, HIV Infections, HIV-1, Humans, Immunoglobulins, Interferon-gamma, Lymphocyte Activation, Male, Membrane Glycoproteins, Middle Aged, Mucous Membrane, Prevotella, Ruminococcus, Signal Transduction, Viral Load, Biological Sciences, Medical and Health Sciences
Abstract

HIV-1-associated disruption of intestinal homeostasis is a major factor contributing to chronic immune activation and inflammation. Dendritic cells (DCs) are crucial in maintaining intestinal homeostasis, but the impact of HIV-1 infection on intestinal DC number and function has not been extensively studied. We compared the frequency and activation/maturation status of colonic myeloid DC (mDC) subsets (CD1c(+) and CD1c(neg)) and plasmacytoid DCs in untreated HIV-1-infected subjects with uninfected controls. Colonic mDCs in HIV-1-infected subjects had increased CD40 but decreased CD83 expression, and CD40 expression on CD1c(+) mDCs positively correlated with mucosal HIV-1 viral load, with mucosal and systemic cytokine production, and with frequencies of activated colon and blood T cells. Percentage of CD83(+)CD1c(+) mDCs negatively correlated with frequencies of interferon-γ-producing colon CD4(+) and CD8(+) T cells. CD40 expression on CD1c(+) mDCs positively associated with abundance of high prevalence mucosal Prevotella copri and Prevotella stercorea but negatively associated with a number of low prevalence mucosal species, including Rumminococcus bromii. CD1c(+) mDC cytokine production was greater in response to in vitro stimulation with Prevotella species relative to R. bromii. These findings suggest that, during HIV infection, colonic mDCs become activated upon exposure to mucosal pathobiont bacteria leading to mucosal and systemic immune activation.

Published
2016

16. Gut dendritic cell activation links an altered colonic microbiome to mucosal and systemic T-cell activation in untreated HIV-1 infection.

Author

Dillon, SM, Lee, EJ, Kotter, CV, Austin, GL, Gianella, S, Siewe, B, Smith, DM, Landay, AL, McManus, MC, Robertson, CE, Frank, DN, McCarter, MD, and Wilson, CC

Subjects
Colon, Mucous Membrane, Dendritic Cells, CD4-Positive T-Lymphocytes, CD8-Positive T-Lymphocytes, Humans, Prevotella, Ruminococcus, HIV-1, HIV Infections, Glycoproteins, Immunoglobulins, Membrane Glycoproteins, Antigens, CD, Antigens, CD1, Viral Load, Case-Control Studies, Lymphocyte Activation, Signal Transduction, Gene Expression Regulation, Cell Lineage, Adult, Middle Aged, Female, Male, Interferon-gamma, Gastrointestinal Microbiome, CD40 Antigens, Infectious Diseases, Digestive Diseases, HIV/AIDS, Clinical Research, Emerging Infectious Diseases, 2.1 Biological and endogenous factors, Inflammatory and Immune System, Infection, Antigens, CD, CD1, CD40, Immunology, Biological Sciences, Medical and Health Sciences
Abstract

HIV-1-associated disruption of intestinal homeostasis is a major factor contributing to chronic immune activation and inflammation. Dendritic cells (DCs) are crucial in maintaining intestinal homeostasis, but the impact of HIV-1 infection on intestinal DC number and function has not been extensively studied. We compared the frequency and activation/maturation status of colonic myeloid DC (mDC) subsets (CD1c(+) and CD1c(neg)) and plasmacytoid DCs in untreated HIV-1-infected subjects with uninfected controls. Colonic mDCs in HIV-1-infected subjects had increased CD40 but decreased CD83 expression, and CD40 expression on CD1c(+) mDCs positively correlated with mucosal HIV-1 viral load, with mucosal and systemic cytokine production, and with frequencies of activated colon and blood T cells. Percentage of CD83(+)CD1c(+) mDCs negatively correlated with frequencies of interferon-γ-producing colon CD4(+) and CD8(+) T cells. CD40 expression on CD1c(+) mDCs positively associated with abundance of high prevalence mucosal Prevotella copri and Prevotella stercorea but negatively associated with a number of low prevalence mucosal species, including Rumminococcus bromii. CD1c(+) mDC cytokine production was greater in response to in vitro stimulation with Prevotella species relative to R. bromii. These findings suggest that, during HIV infection, colonic mDCs become activated upon exposure to mucosal pathobiont bacteria leading to mucosal and systemic immune activation.

Published
2016

17. Gene expression and TB pathogenesis in rhesus macaques: TR4, CD40, CD40L, FAS (CD95), and TNF are host genetic markers in peripheral blood mononuclear cells that are associated with severity of TB lesions

Author

Roodgar, Morteza, Ross, Cody T, Tarara, Ross, Lowenstine, Linda, Dandekar, Satya, and Smith, David Glenn

Subjects
Microbiology, Biological Sciences, Bioinformatics and Computational Biology, Genetics, Infectious Diseases, Tuberculosis, Lung, HIV/AIDS, Rare Diseases, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Animals, CD40 Antigens, CD40 Ligand, Cluster Analysis, Gene Expression, Gene Expression Profiling, Genetic Association Studies, Genetic Markers, Genetic Predisposition to Disease, Host-Pathogen Interactions, Leukocytes, Mononuclear, Macaca mulatta, Monkey Diseases, Mycobacterium tuberculosis, Receptors, Thyroid Hormone, Severity of Illness Index, Tumor Necrosis Factors, fas Receptor, Rhesus macaques, Gene expression, Host genes, Histopathologic lesions, TR4, IFNE, Bioinformatics and computational biology
Abstract

Tuberculosis (TB) pathologic lesions in rhesus macaques resemble those in humans. The expression levels of several host TB candidate genes in the peripheral blood mononuclear cells (PBMCs) of six rhesus macaques experimentally infected with Mycobacterium tuberculosis were quantified pre-infection and at several dates post-infection. Quantitative measures of TB histopathology in the lungs including: granuloma count, granuloma size, volume of granulomatous and non-granulomatous lesions, and direct bacterial load, were used as the outcomes of a multi-level Bayesian regression model in which expression levels of host genes at various dates were used as predictors. The results indicate that the expression levels of TR4, CD40, CD40L, FAS (CD95) and TNF in PBMC were associated with quantitative measures of the severity of TB histopathologic lesions in the lungs of the study animals. Moreover, no reliable association between the expression levels of IFNE in PBMCs and the severity of TB lesions in the lungs of the study animals was found. In conclusion, PBMC expression profiles derived from the above-listed host genes might be appropriate biomarkers for probabilistic diagnosis and/or prognosis of TB severity in rhesus macaques.

Published
2015

18. Allogeneic IgG combined with dendritic cell stimuli induce antitumour T-cell immunity.

Author

Carmi, Yaron, Linde, Ian, Burt, Bryan, Prestwood, Tyler, Perlman, Nicola, Davidson, Matthew, Kenkel, Justin, Segal, Ehud, Pusapati, Ganesh, Bhattacharya, Nupur, Engleman, Edgar, and Spitzer, Matthew

Subjects
Animals, Antibodies, Neoplasm, Antigens, Neoplasm, CD40 Antigens, Dendritic Cells, Disease Models, Animal, Female, Immunoglobulin G, Isoantibodies, Lymphocyte Activation, Male, Mice, Neoplasm Metastasis, Neoplasm Transplantation, Neoplasms, Receptors, IgG, T-Lymphocytes, Tumor Necrosis Factor-alpha
Abstract

Whereas cancers grow within host tissues and evade host immunity through immune-editing and immunosuppression, tumours are rarely transmissible between individuals. Much like transplanted allogeneic organs, allogeneic tumours are reliably rejected by host T cells, even when the tumour and host share the same major histocompatibility complex alleles, the most potent determinants of transplant rejection. How such tumour-eradicating immunity is initiated remains unknown, although elucidating this process could provide the basis for inducing similar responses against naturally arising tumours. Here we find that allogeneic tumour rejection is initiated in mice by naturally occurring tumour-binding IgG antibodies, which enable dendritic cells (DCs) to internalize tumour antigens and subsequently activate tumour-reactive T cells. We exploited this mechanism to treat autologous and autochthonous tumours successfully. Either systemic administration of DCs loaded with allogeneic-IgG-coated tumour cells or intratumoral injection of allogeneic IgG in combination with DC stimuli induced potent T-cell-mediated antitumour immune responses, resulting in tumour eradication in mouse models of melanoma, pancreas, lung and breast cancer. Moreover, this strategy led to eradication of distant tumours and metastases, as well as the injected primary tumours. To assess the clinical relevance of these findings, we studied antibodies and cells from patients with lung cancer. T cells from these patients responded vigorously to autologous tumour antigens after culture with allogeneic-IgG-loaded DCs, recapitulating our findings in mice. These results reveal that tumour-binding allogeneic IgG can induce powerful antitumour immunity that can be exploited for cancer immunotherapy.

Published
2015

19. Allogeneic IgG combined with dendritic cell stimuli induce antitumour T-cell immunity

Author

Carmi, Yaron, Spitzer, Matthew H, Linde, Ian L, Burt, Bryan M, Prestwood, Tyler R, Perlman, Nicola, Davidson, Matthew G, Kenkel, Justin A, Segal, Ehud, Pusapati, Ganesh V, Bhattacharya, Nupur, and Engleman, Edgar G

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Cancer, Inflammatory and immune system, Animals, Antibodies, Neoplasm, Antigens, Neoplasm, CD40 Antigens, Dendritic Cells, Disease Models, Animal, Female, Immunoglobulin G, Isoantibodies, Lymphocyte Activation, Male, Mice, Neoplasm Metastasis, Neoplasm Transplantation, Neoplasms, Receptors, IgG, T-Lymphocytes, Tumor Necrosis Factor-alpha, General Science & Technology
Abstract

Whereas cancers grow within host tissues and evade host immunity through immune-editing and immunosuppression, tumours are rarely transmissible between individuals. Much like transplanted allogeneic organs, allogeneic tumours are reliably rejected by host T cells, even when the tumour and host share the same major histocompatibility complex alleles, the most potent determinants of transplant rejection. How such tumour-eradicating immunity is initiated remains unknown, although elucidating this process could provide the basis for inducing similar responses against naturally arising tumours. Here we find that allogeneic tumour rejection is initiated in mice by naturally occurring tumour-binding IgG antibodies, which enable dendritic cells (DCs) to internalize tumour antigens and subsequently activate tumour-reactive T cells. We exploited this mechanism to treat autologous and autochthonous tumours successfully. Either systemic administration of DCs loaded with allogeneic-IgG-coated tumour cells or intratumoral injection of allogeneic IgG in combination with DC stimuli induced potent T-cell-mediated antitumour immune responses, resulting in tumour eradication in mouse models of melanoma, pancreas, lung and breast cancer. Moreover, this strategy led to eradication of distant tumours and metastases, as well as the injected primary tumours. To assess the clinical relevance of these findings, we studied antibodies and cells from patients with lung cancer. T cells from these patients responded vigorously to autologous tumour antigens after culture with allogeneic-IgG-loaded DCs, recapitulating our findings in mice. These results reveal that tumour-binding allogeneic IgG can induce powerful antitumour immunity that can be exploited for cancer immunotherapy.

Published
2015

20. Allogeneic IgG combined with dendritic cell stimuli induce antitumour T-cell immunity.

Author

Carmi, Yaron, Spitzer, Matthew H, Linde, Ian L, Burt, Bryan M, Prestwood, Tyler R, Perlman, Nicola, Davidson, Matthew G, Kenkel, Justin A, Segal, Ehud, Pusapati, Ganesh V, Bhattacharya, Nupur, and Engleman, Edgar G

Subjects
Dendritic Cells, T-Lymphocytes, Animals, Mice, Neoplasms, Neoplasm Metastasis, Disease Models, Animal, Tumor Necrosis Factor-alpha, Immunoglobulin G, Receptors, IgG, Antibodies, Neoplasm, Isoantibodies, Antigens, Neoplasm, Lymphocyte Activation, Neoplasm Transplantation, Female, Male, CD40 Antigens, Disease Models, Animal, Antigens, CD40, Receptors, IgG, Antibodies, Neoplasm, Cancer, Transplantation, 5.2 Cellular and gene therapies, Inflammatory and Immune System, General Science & Technology
Abstract

Whereas cancers grow within host tissues and evade host immunity through immune-editing and immunosuppression, tumours are rarely transmissible between individuals. Much like transplanted allogeneic organs, allogeneic tumours are reliably rejected by host T cells, even when the tumour and host share the same major histocompatibility complex alleles, the most potent determinants of transplant rejection. How such tumour-eradicating immunity is initiated remains unknown, although elucidating this process could provide the basis for inducing similar responses against naturally arising tumours. Here we find that allogeneic tumour rejection is initiated in mice by naturally occurring tumour-binding IgG antibodies, which enable dendritic cells (DCs) to internalize tumour antigens and subsequently activate tumour-reactive T cells. We exploited this mechanism to treat autologous and autochthonous tumours successfully. Either systemic administration of DCs loaded with allogeneic-IgG-coated tumour cells or intratumoral injection of allogeneic IgG in combination with DC stimuli induced potent T-cell-mediated antitumour immune responses, resulting in tumour eradication in mouse models of melanoma, pancreas, lung and breast cancer. Moreover, this strategy led to eradication of distant tumours and metastases, as well as the injected primary tumours. To assess the clinical relevance of these findings, we studied antibodies and cells from patients with lung cancer. T cells from these patients responded vigorously to autologous tumour antigens after culture with allogeneic-IgG-loaded DCs, recapitulating our findings in mice. These results reveal that tumour-binding allogeneic IgG can induce powerful antitumour immunity that can be exploited for cancer immunotherapy.

Published
2015

21. B cell TLR1/2, TLR4, TLR7 and TLR9 interact in induction of class switch DNA recombination: Modulation by BCR and CD40, and relevance to T-independent antibody responses

Author

Pone, Egest J, Lou, Zheng, Lam, Tonika, Greenberg, Milton L, Wang, Rui, Xu, Zhenming, and Casali, Paolo

Subjects
Genetics, Vaccine Related, Prevention, Biotechnology, 2.1 Biological and endogenous factors, Aetiology, 1.1 Normal biological development and functioning, Underpinning research, Animals, B-Lymphocytes, CD40 Antigens, CD40 Ligand, Calcium, Cell Differentiation, Cytokines, Gene Expression Regulation, Imidazoles, Immunoglobulin Class Switching, Immunoglobulin G, Lipopeptides, Lipopolysaccharides, Membrane Glycoproteins, Mice, Mice, Inbred C57BL, Receptor Cross-Talk, Receptors, Antigen, B-Cell, Recombination, Genetic, Signal Transduction, Toll-Like Receptor 1, Toll-Like Receptor 2, Toll-Like Receptor 4, Toll-Like Receptor 7, Toll-Like Receptor 9, Antibody, B cells, B cell receptor, CpG, class switch DNA recombination, lipopolysaccharides, T-independent antibody response, Toll-like receptor, Immunology
Abstract

Ig class switch DNA recombination (CSR) in B cells is crucial to the maturation of antibody responses. It requires IgH germline IH-CH transcription and expression of AID, both of which are induced by engagement of CD40 or dual engagement of a Toll-like receptor (TLR) and B cell receptor (BCR). Here, we have addressed cross-regulation between two different TLRs or between a TLR and CD40 in CSR induction by using a B cell stimulation system involving lipopolysaccharides (LPS). LPS-mediated long-term primary class-switched antibody responses and memory-like antibody responses in vivo and induced generation of class-switched B cells and plasma cells in vitro. Consistent with the requirement for dual TLR and BCR engagement in CSR induction, LPS, which engages TLR4 through its lipid A moiety, triggered cytosolic Ca2+ flux in B cells through its BCR-engaging polysaccharidic moiety. In the presence of BCR crosslinking, LPS synergized with a TLR1/2 ligand (Pam3CSK4) in CSR induction, but much less efficiently with a TLR7 (R-848) or TLR9 (CpG) ligand. In the absence of BCR crosslinking, R-848 and CpG, which per se induced marginal CSR, virtually abrogated CSR to IgG1, IgG2a, IgG2b, IgG3 and/or IgA, as induced by LPS or CD154 (CD40 ligand) plus IL-4, IFN-γ or TGF-β, and reduced secretion of class-switched Igs, without affecting B cell proliferation or IgM expression. The CSR inhibition by TLR9 was associated with the reduction in AID expression and/or IgH germline IH-S-CH transcription, and required co-stimulation of B cells by CpG with LPS or CD154. Unexpectedly, B cells also failed to undergo CSR or plasma cell differentiation when co-stimulated by LPS and CD154. Overall, by addressing the interaction of TLR1/2, TLR4, TLR7 and TLR9 in the induction of CSR and modulation of TLR-dependent CSR by BCR and CD40, our study suggests the complexity of how different stimuli cross-regulate an important B cell differentiation process and an important role of TLRs in inducing effective T-independent antibody responses to microbial pathogens, allergens and vaccines.

Published
2015

22. Proinflammatory Responses Induced by CD40 in Retinal Endothelial and Müller Cells are Inhibited by Blocking CD40-Traf2,3 or CD40-Traf6 SignalingCD40-Traf and Retinal Cells

Author

Portillo, Jose-Andres C, Schwartz, Isaac, Zarini, Simona, Bapputty, Reena, Kern, Timothy S, Gubitosi-Klug, Rose A, Murphy, Robert C, Subauste, M Cecilia, and Subauste, Carlos S

Subjects
Biomedical and Clinical Sciences, Ophthalmology and Optometry, Eye Disease and Disorders of Vision, Diabetes, Aetiology, 2.1 Biological and endogenous factors, Analysis of Variance, Animals, Biomarkers, CD40 Antigens, Cells, Cultured, Chemokine CCL2, Diabetes Mellitus, Experimental, Dinoprostone, Endothelial Cells, Ependymoglial Cells, Humans, Intercellular Adhesion Molecule-1, Mice, Rats, Retina, Signal Transduction, Tumor Necrosis Factor Receptor-Associated Peptides and Proteins, Vascular Endothelial Growth Factor A, CD40, chemokine, diabetes, intercellular adhesion molecules, Biological Sciences, Medical and Health Sciences, Ophthalmology & Optometry, Ophthalmology and optometry
Abstract

PurposeThe cell surface receptor CD40 is required for the development of retinopathies induced by diabetes and ischemia/reperfusion. The purpose of this study was to identify signaling pathways by which CD40 triggers proinflammatory responses in retinal cells, since this may lead to pharmacologic targeting of these pathways as novel therapy against retinopathies.MethodsRetinal endothelial and Müller cells were transduced with vectors that encode wild-type CD40 or CD40 with mutations in sites that recruit TNF receptor associated factors (TRAF): TRAF2,3 (ΔT2,3), TRAF6 (ΔT6), or TRAF2,3 plus TRAF6 (ΔT2,3,6). Cells also were incubated with CD40-TRAF2,3 or CD40-TRAF6 blocking peptides. We assessed intercellular adhesion molecule-1 (ICAM-1), CD40, monocyte chemoattractant protein-1 (MCP-1), VEGF, and prostaglandin E₂ (PGE₂) by fluorescence-activated cell sorting (FACS), ELISA, or mass spectrometry. Mice (B6 and CD40(-/-)) were made diabetic using streptozotocin. The MCP-1 mRNA was assessed by real-time PCR.ResultsThe CD40-mediated ICAM-1 upregulation in endothelial and Müller cells was markedly inhibited by expression of CD40 ΔT2,3 or CD40 ΔT6. The CD40 was required for MCP-1 mRNA upregulation in the retina of diabetic mice. The CD40 stimulation of endothelial and Müller cells enhanced MCP-1 production that was markedly diminished by CD40 ΔT2,3 or CD40 ΔT6. Similar results were obtained in cells incubated with CD40-TRAF2,3 or CD40-TRAF6 blocking peptides. The CD40 ligation upregulated PGE₂ and VEGF production by Müller cells, that was inhibited by CD40 ΔT2,3 or CD40 ΔT6. All cellular responses tested were obliterated by expression of CD40 ΔT2,3,6.ConclusionsBlockade of a single CD40-TRAF pathway was sufficient to impair ICAM-1, MCP-1, PGE₂, and VEGF upregulation in retinal endothelial and/or Müller cells. Blockade of CD40-TRAF signaling may control retinopathies.

Published
2014

23. Type II Toxoplasma gondii Induction of CD40 on Infected Macrophages Enhances Interleukin-12 Responses

Author

Morgado, Pedro, Sudarshana, Dattanand M, Gov, Lanny, Harker, Katherine S, Lam, Tonika, Casali, Paolo, Boyle, Jon P, and Lodoen, Melissa B

Subjects
Vaccine Related, Biodefense, Biotechnology, Foodborne Illness, Infectious Diseases, Genetics, Prevention, Emerging Infectious Diseases, 2.2 Factors relating to the physical environment, 2.1 Biological and endogenous factors, Aetiology, Infection, Animals, Antigens, Protozoan, CD40 Antigens, Cells, Cultured, Humans, Interleukin-12, Macrophages, Protozoan Proteins, Toxoplasma, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Microbiology
Abstract

Toxoplasma gondii is an obligate intracellular parasite that can cause severe neurological disease in infected humans. CD40 is a receptor on macrophages that plays a critical role in controlling T. gondii infection. We examined the regulation of CD40 on the surface of T. gondii-infected bone marrow-derived macrophages (BMdMs). T. gondii induced CD40 expression both at the transcript level and on the cell surface, and interestingly, the effect was parasite strain specific: CD40 levels were dramatically increased in type II T. gondii-infected BMdMs compared to type I- or type III-infected cells. Type II induction of CD40 was specific to cells harboring intracellular parasites and detectable as early as 6 h postinfection (hpi) at the transcript level. CD40 protein expression peaked at 18 hpi. Using forward genetics with progeny from a type II × type III cross, we found that CD40 induction mapped to a region of chromosome X that included the gene encoding the dense granule protein 15 (GRA15). Using type I parasites stably expressing the type II allele of GRA15 (GRA15II), we found that type I GRA15II parasites induced the expression of CD40 on infected cells in an NF-κB-dependent manner. In addition, stable expression of hemagglutinin-tagged GRA15II in THP-1 cells resulted in CD40 upregulation in the absence of infection. Since CD40 signaling contributes to interleukin-12 (IL-12) production, we examined IL-12 from infected macrophages and found that CD40L engagement of CD40 amplified the IL-12 response in type II-infected cells. These data indicate that GRA15II induction of CD40 promotes parasite immunity through the production of IL-12.

Published
2014

24. A circulating antibody panel for pretransplant prediction of FSGS recurrence after kidney transplantation

Author

Delville, Marianne, Sigdel, Tara K, Wei, Changli, Li, Jing, Hsieh, Szu-Chuan, Fornoni, Alessia, Burke, George W, Bruneval, Patrick, Naesens, Maarten, Jackson, Annette, Alachkar, Nada, Canaud, Guillaume, Legendre, Christophe, Anglicheau, Dany, Reiser, Jochen, and Sarwal, Minnie M

Subjects
Clinical Research, Rare Diseases, Kidney Disease, Transplantation, Aetiology, 2.1 Biological and endogenous factors, Renal and urogenital, Adult, Antibodies, CD40 Antigens, Case-Control Studies, Enzyme-Linked Immunosorbent Assay, Female, Glomerulosclerosis, Focal Segmental, Humans, Kidney Transplantation, Male, Recurrence, Biological Sciences, Medical and Health Sciences
Abstract

Recurrence of focal segmental glomerulosclerosis (rFSGS) after kidney transplantation is a cause of accelerated graft loss. To evaluate pathogenic antibodies (Abs) in rFSGS, we processed 141 serum samples from 64 patients with and without primary rFSGS and 34 non-FSGS control patients transplanted at four hospitals. We screened about 9000 antigens in pretransplant sera and selected 10 Abs targeting glomerular antigens for enzyme-linked immunosorbent assay (ELISA) validation. A panel of seven Abs (CD40, PTPRO, CGB5, FAS, P2RY11, SNRPB2, and APOL2) could predict posttransplant FSGS recurrence with 92% accuracy. Pretransplant elevation of anti-CD40 Ab alone had the best correlation (78% accuracy) with rFSGS risk after transplantation. Epitope mapping of CD40 with customized peptide arrays and rFSGS sera demonstrated altered immunogenicity of the extracellular CD40 domain in rFSGS. Immunohistochemistry of CD40 demonstrated a differential expression in FSGS compared to non-FSGS controls. Anti-CD40 Abs purified from rFSGS patients were particularly pathogenic in human podocyte cultures. Injection of anti-CD40/rFSGS Ab enhanced suPAR (soluble urokinase receptor)-mediated proteinuria in wild-type mice, yet no sensitizing effect was noted in mice deficient in CD40 or in wild-type mice that received blocking Ab to CD40. In conclusion, a panel of seven Abs can help identify primary FSGS patients at high risk of recurrence before transplantation. Intrarenal CD40 (and possibly other specific glomerular antigens) is an important contributor to FSGS disease pathogenesis. Human trials of anti-CD40 therapies are warranted to evaluate their efficacy for preventing rFSGS and improving graft survival.

Published
2014

25. Combination of an agonistic anti-CD40 monoclonal antibody and the COX-2 inhibitor celecoxib induces anti-glioma effects by promotion of type-1 immunity in myeloid cells and T-cells

Author

Kosaka, Akemi, Ohkuri, Takayuki, and Okada, Hideho

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Rare Diseases, Cancer, Brain Cancer, Biotechnology, Neurosciences, Brain Disorders, 2.1 Biological and endogenous factors, Aetiology, Animals, Antibodies, Monoclonal, Antineoplastic Combined Chemotherapy Protocols, CD40 Antigens, Celecoxib, Cyclooxygenase 2 Inhibitors, Female, Glioma, Mice, Mice, Inbred C57BL, Myeloid Cells, Pyrazoles, Rats, Sulfonamides, T-Lymphocytes, Cytotoxic, Transfection, Oncology and carcinogenesis
Abstract

Malignant gliomas are heavily infiltrated by immature myeloid cells that mediate immunosuppression. Agonistic CD40 monoclonal antibody (mAb) has been shown to activate myeloid cells and promote antitumor immunity. Our previous study has also demonstrated blockade of cyclooxygenase-2 (COX-2) reduces immunosuppressive myeloid cells, thereby suppressing glioma development in mice. We therefore hypothesized that a combinatory strategy to modulate myeloid cells via two distinct pathways, i.e., CD40/CD40L stimulation and COX-2 blockade, would enhance anti-glioma immunity. We used three different mouse glioma models to evaluate therapeutic effects and underlying mechanisms of a combination regimen with an agonist CD40 mAb and the COX-2 inhibitor celecoxib. Treatment of glioma-bearing mice with the combination therapy significantly prolonged survival compared with either anti-CD40 mAb or celecoxib alone. The combination regimen promoted maturation of CD11b(+) cells in both spleen and brain, and enhanced Cxcl10 while suppressing Arg1 in CD11b(+)Gr-1(+) cells in the brain. Anti-glioma activity of the combination regimen was T-cell dependent because depletion of CD4(+) and CD8(+) cells in vivo abrogated the anti-glioma effects. Furthermore, the combination therapy significantly increased the frequency of CD8(+) T-cells, enhanced IFN-γ-production and reduced CD4(+)CD25(+)Foxp3(+) T regulatory cells in the brain, and induced tumor-antigen-specific T-cell responses in lymph nodes. Our findings suggest that the combination therapy of anti-CD40 mAb with celecoxib enhances anti-glioma activities via promotion of type-1 immunity both in myeloid cells and T-cells.

Published
2014

26. Regulatory T Cells and Myeloid-Derived Suppressor Cells in the Tumor Microenvironment Undergo Fas-Dependent Cell Death during IL-2/αCD40 Therapy

Author

Weiss, Jonathan M, Subleski, Jeff J, Back, Tim, Chen, Xin, Watkins, Stephanie K, Yagita, Hideo, Sayers, Thomas J, Murphy, William J, and Wiltrout, Robert H

Subjects
Vaccine Related, Cancer, Clinical Research, Immunization, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Animals, Antineoplastic Agents, CD40 Antigens, CD8-Positive T-Lymphocytes, Cell Death, Cell Line, Tumor, Interleukin-2, Mice, Mice, Inbred BALB C, Mice, Knockout, Myeloid Cells, Neoplasms, Experimental, Proto-Oncogene Proteins c-bcl-2, T-Lymphocytes, Regulatory, Tumor Microenvironment, fas Receptor, Immunology
Abstract

Fas ligand expression in certain tumors has been proposed to contribute to immunosuppression and poor prognosis. However, immunotherapeutic approaches may elicit the Fas-mediated elimination of immunosuppressive regulatory T cells (Tregs) and myeloid-derived suppressor cells (MDSCs) within tumors that represent major obstacles for cancer immunotherapy. Previously, we showed that IL-2 and agonistic CD40 Ab (αCD40) elicited synergistic antitumor responses coincident with the efficient removal of Tregs and MDSCs. We demonstrate in this study in two murine tumor models that Treg and MDSC loss within the tumor microenvironment after IL-2/αCD40 occurs through a Fas-dependent cell death pathway. Among tumor-infiltrating leukocytes, CD8(+) T cells, neutrophils, and immature myeloid cells expressed Fas ligand after treatment. Fas was expressed by tumor-associated Tregs and immature myeloid cells, including MDSCs. Tregs and MDSCs in the tumor microenvironment expressed active caspases after IL-2/αCD40 therapy and, in contrast with effector T cells, Tregs significantly downregulated Bcl-2 expression. In contrast, Tregs and MDSCs proliferated and expanded in the spleen after treatment. Adoptive transfer of Fas-deficient Tregs or MDSCs into wild-type, Treg-, or MDSC-depleted hosts resulted in the persistence of Tregs or MDSCs and the loss of antitumor efficacy in response to IL-2/αCD40. These results demonstrate the importance of Fas-mediated Treg/MDSC removal for successful antitumor immunotherapy. Our results suggest that immunotherapeutic strategies that include exploiting Treg and MDSC susceptibility to Fas-mediated apoptosis hold promise for treatment of cancer.

Published
2014

27. Bystander activation and anti-tumor effects of CD8+ T cells following Interleukin-2 based immunotherapy is independent of CD4+ T cell help.

Author

Monjazeb, Arta M, Tietze, Julia K, Grossenbacher, Steven K, Hsiao, Hui-Hua, Zamora, Anthony E, Mirsoian, Annie, Koehn, Brent, Blazar, Bruce R, Weiss, Jonathan M, Wiltrout, Robert H, Sckisel, Gail D, and Murphy, William J

Subjects
CD4-Positive T-Lymphocytes, CD8-Positive T-Lymphocytes, Animals, Mice, Inbred C57BL, Mice, Antineoplastic Combined Chemotherapy Protocols, Interleukins, Interleukin-2, Cytokines, Immunotherapy, Flow Cytometry, Signal Transduction, Cell Proliferation, Models, Immunological, Programmed Cell Death 1 Receptor, CD4 Antigens, CD40 Antigens, General Science & Technology
Abstract

We have previously demonstrated that immunotherapy combining agonistic anti-CD40 and IL-2 (IT) results in synergistic anti-tumor effects. IT induces expansion of highly cytolytic, antigen-independent "bystander-activated" (CD8(+)CD44high) T cells displaying a CD25(-)NKG2D(+) phenotype in a cytokine dependent manner, which were responsible for the anti-tumor effects. While much attention has focused on CD4(+) T cell help for antigen-specific CD8(+) T cell expansion, little is known regarding the role of CD4(+) T cells in antigen-nonspecific bystander-memory CD8(+) T cell expansion. Utilizing CD4 deficient mouse models, we observed a significant expansion of bystander-memory T cells following IT which was similar to the non-CD4 depleted mice. Expanded bystander-memory CD8(+) T cells upregulated PD-1 in the absence of CD4(+) T cells which has been published as a hallmark of exhaustion and dysfunction in helpless CD8(+) T cells. Interestingly, compared to CD8(+) T cells from CD4 replete hosts, these bystander expanded cells displayed comparable (or enhanced) cytokine production, lytic ability, and in vivo anti-tumor effects suggesting no functional impairment or exhaustion and were enriched in an effector phenotype. There was no acceleration of the post-IT contraction phase of the bystander memory CD8(+) response in CD4-depleted mice. The response was independent of IL-21 signaling. These results suggest that, in contrast to antigen-specific CD8(+) T cell expansion, CD4(+) T cell help is not necessary for expansion and activation of antigen-nonspecific bystander-memory CD8(+) T cells following IT, but may play a role in regulating conversion of these cells from a central memory to effector phenotype. Additionally, the expression of PD-1 in this model appears to be a marker of effector function and not exhaustion.

Published
2014

28. Bystander Activation and Anti-Tumor Effects of CD8+ T Cells Following Interleukin-2 Based Immunotherapy Is Independent of CD4+ T Cell Help

Author

Monjazeb, Arta M, Tietze, Julia K, Grossenbacher, Steven K, Hsiao, Hui-Hua, Zamora, Anthony E, Mirsoian, Annie, Koehn, Brent, Blazar, Bruce R, Weiss, Jonathan M, Wiltrout, Robert H, Sckisel, Gail D, and Murphy, William J

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Vaccine Related, 2.1 Biological and endogenous factors, Aetiology, Animals, Antineoplastic Combined Chemotherapy Protocols, CD4 Antigens, CD4-Positive T-Lymphocytes, CD40 Antigens, CD8-Positive T-Lymphocytes, Cell Proliferation, Cytokines, Flow Cytometry, Immunotherapy, Interleukin-2, Interleukins, Mice, Mice, Inbred C57BL, Models, Immunological, Programmed Cell Death 1 Receptor, Signal Transduction, General Science & Technology
Abstract

We have previously demonstrated that immunotherapy combining agonistic anti-CD40 and IL-2 (IT) results in synergistic anti-tumor effects. IT induces expansion of highly cytolytic, antigen-independent "bystander-activated" (CD8(+)CD44high) T cells displaying a CD25(-)NKG2D(+) phenotype in a cytokine dependent manner, which were responsible for the anti-tumor effects. While much attention has focused on CD4(+) T cell help for antigen-specific CD8(+) T cell expansion, little is known regarding the role of CD4(+) T cells in antigen-nonspecific bystander-memory CD8(+) T cell expansion. Utilizing CD4 deficient mouse models, we observed a significant expansion of bystander-memory T cells following IT which was similar to the non-CD4 depleted mice. Expanded bystander-memory CD8(+) T cells upregulated PD-1 in the absence of CD4(+) T cells which has been published as a hallmark of exhaustion and dysfunction in helpless CD8(+) T cells. Interestingly, compared to CD8(+) T cells from CD4 replete hosts, these bystander expanded cells displayed comparable (or enhanced) cytokine production, lytic ability, and in vivo anti-tumor effects suggesting no functional impairment or exhaustion and were enriched in an effector phenotype. There was no acceleration of the post-IT contraction phase of the bystander memory CD8(+) response in CD4-depleted mice. The response was independent of IL-21 signaling. These results suggest that, in contrast to antigen-specific CD8(+) T cell expansion, CD4(+) T cell help is not necessary for expansion and activation of antigen-nonspecific bystander-memory CD8(+) T cells following IT, but may play a role in regulating conversion of these cells from a central memory to effector phenotype. Additionally, the expression of PD-1 in this model appears to be a marker of effector function and not exhaustion.

Published
2014

29. Aging predisposes to acute inflammatory induced pathology after tumor immunotherapy

Author

Bouchlaka, Myriam N, Sckisel, Gail D, Chen, Mingyi, Mirsoian, Annie, Zamora, Anthony E, Maverakis, Emanual, Wilkins, Danice EC, Alderson, Kory L, Hsiao, Hui-Hua, Weiss, Jonathan M, Monjazeb, Arta M, Hesdorffer, Charles, Ferrucci, Luigi, Longo, Dan L, Blazar, Bruce R, Wiltrout, Robert H, Redelman, Doug, Taub, Dennis D, and Murphy, William J

Subjects
Aging, Immunization, Cancer, Vaccine Related, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Animals, CD40 Antigens, Cytokines, Dose-Response Relationship, Drug, Female, Humans, Immunotherapy, Inflammation, Inflammation Mediators, Lipopolysaccharides, Liver, Macrophages, Mice, Mice, Inbred C57BL, Neoplasms, Survival Analysis, Tumor Necrosis Factor-alpha, Medical and Health Sciences, Immunology
Abstract

Cancer commonly occurs in the elderly and immunotherapy (IT) is being increasingly applied to this population. However, the majority of preclinical mouse tumor models assessing potential efficacy and toxicities of therapeutics use young mice. We assessed the impact of age on responses to systemic immune stimulation. In contrast to young mice, systemic cancer IT regimens or LPS given to aged mice resulted in rapid and lethal toxicities affecting multiple organs correlating with heightened proinflammatory cytokines systemically and within the parenchymal tissues. This inflammatory response and increased morbidity with age was independent of T cells or NK cells. However, prior in vivo depletion of macrophages in aged mice resulted in lesser cytokine levels, increased survival, and decreased liver histopathology. Furthermore, macrophages from aged mice and normal human elderly volunteers displayed heightened TNF and IL-6 production upon in vitro stimulation. Treatment of both TNF knockout mice and in vivo TNF blockade in aged mice resulted in significant increases in survival and lessened pathology. Importantly, TNF blockade in tumor-bearing, aged mice receiving IT displayed significant anti-tumor effects. These data demonstrate the critical role of macrophages in the age-associated hyper-inflammatory cytokine responses to systemic immunostimulation and underscore the importance of performing preclinical assessments in aged mice.

Published
2013

30. Aging predisposes to acute inflammatory induced pathology after tumor immunotherapy.

Author

Bouchlaka, Myriam N, Sckisel, Gail D, Chen, Mingyi, Mirsoian, Annie, Zamora, Anthony E, Maverakis, Emanual, Wilkins, Danice EC, Alderson, Kory L, Hsiao, Hui-Hua, Weiss, Jonathan M, Monjazeb, Arta M, Hesdorffer, Charles, Ferrucci, Luigi, Longo, Dan L, Blazar, Bruce R, Wiltrout, Robert H, Redelman, Doug, Taub, Dennis D, and Murphy, William J

Subjects
Liver, Macrophages, Animals, Mice, Inbred C57BL, Humans, Mice, Neoplasms, Inflammation, Lipopolysaccharides, Tumor Necrosis Factor-alpha, Inflammation Mediators, Cytokines, Immunotherapy, Survival Analysis, Aging, Dose-Response Relationship, Drug, Female, CD40 Antigens, Immunology, Medical and Health Sciences
Abstract

Cancer commonly occurs in the elderly and immunotherapy (IT) is being increasingly applied to this population. However, the majority of preclinical mouse tumor models assessing potential efficacy and toxicities of therapeutics use young mice. We assessed the impact of age on responses to systemic immune stimulation. In contrast to young mice, systemic cancer IT regimens or LPS given to aged mice resulted in rapid and lethal toxicities affecting multiple organs correlating with heightened proinflammatory cytokines systemically and within the parenchymal tissues. This inflammatory response and increased morbidity with age was independent of T cells or NK cells. However, prior in vivo depletion of macrophages in aged mice resulted in lesser cytokine levels, increased survival, and decreased liver histopathology. Furthermore, macrophages from aged mice and normal human elderly volunteers displayed heightened TNF and IL-6 production upon in vitro stimulation. Treatment of both TNF knockout mice and in vivo TNF blockade in aged mice resulted in significant increases in survival and lessened pathology. Importantly, TNF blockade in tumor-bearing, aged mice receiving IT displayed significant anti-tumor effects. These data demonstrate the critical role of macrophages in the age-associated hyper-inflammatory cytokine responses to systemic immunostimulation and underscore the importance of performing preclinical assessments in aged mice.

Published
2013

31. Developmental maturation of innate immune cell function correlates with susceptibility to central nervous system autoimmunity

Author

Hertzenberg, Deetje, Lehmann‐Horn, Klaus, Kinzel, Silke, Husterer, Veronika, Cravens, Petra D, Kieseier, Bernd C, Hemmer, Bernhard, Brück, Wolfgang, Zamvil, Scott S, Stüve, Olaf, and Weber, Martin S

Subjects
Biomedical and Clinical Sciences, Immunology, Emerging Infectious Diseases, Brain Disorders, Neurodegenerative, Prevention, Neurosciences, Autoimmune Disease, Multiple Sclerosis, 1.1 Normal biological development and functioning, 2.1 Biological and endogenous factors, Aetiology, Underpinning research, Inflammatory and immune system, Adoptive Transfer, Age Factors, Animals, Antigen-Presenting Cells, Autoimmunity, CD40 Antigens, Cell Differentiation, Cell Proliferation, Central Nervous System, Cytokines, Dendritic Cells, Encephalomyelitis, Autoimmune, Experimental, Female, Histocompatibility Antigens Class II, Immunity, Innate, Interleukin-10, Lymphocyte Activation, Mice, Mice, Inbred C57BL, Myeloid Cells, Th1 Cells, Th17 Cells, Age, Experimental autoimmune encephalomyelitis, Innate immunity, Multiple sclerosis, Susceptibility
Abstract

MS is an inflammatory CNS disorder, which typically occurs in early adulthood and rarely in children. Here we tested whether functional maturation of innate immune cells may determine susceptibility to CNS autoimmune disease in EAE. Two-week-old mice were resistant to active EAE, which causes fulminant paralysis in adult mice; this resistance was associated with an impaired development of Th1 and Th17 cells. Resistant, young mice had higher frequencies of myeloid-derived suppressor cells and plasma-cytoid DCs. Furthermore, myeloid APCs and B cells from young mice expressed lower levels of MHC class II and CD40, produced decreased amounts of proinflammatory cytokines, and released enhanced levels of anti-inflammatory IL-10. When used as APCs, splenocytes from 2-week-old mice failed to differentiate naive T cells into Th1 and Th17 cells irrespective of the T-cell donor's age, and promoted development of Treg cells and Th2 cells instead. Adoptive transfer of adult APCs restored the ability of 2-week-old mice to generate encephalitogenic T cells and develop EAE. Collectively, these findings indicate that the innate immune compartment functionally matures during development, which may be a prerequisite for development of T-cell-mediated CNS autoimmune disease.

Published
2013

32. Cancer immunoediting by the innate immune system in the absence of adaptive immunity

Author

O’Sullivan, Timothy, Saddawi-Konefka, Robert, Vermi, William, Koebel, Catherine M, Arthur, Cora, White, J Michael, Uppaluri, Ravi, Andrews, Daniel M, Ngiow, Shin Foong, Teng, Michele WL, Smyth, Mark J, Schreiber, Robert D, and Bui, Jack D

Subjects
Cancer, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Adaptive Immunity, Animals, CD40 Antigens, Cell Line, Tumor, DNA-Binding Proteins, Genetic Predisposition to Disease, Histocompatibility Antigens Class II, Immunity, Innate, Immunomodulation, Interferon-gamma, Interleukin Receptor Common gamma Subunit, Killer Cells, Natural, Macrophages, Mice, Mice, Knockout, Neoplasms, Phenotype, Sarcoma, Transplantation, Isogeneic, Medical and Health Sciences, Immunology
Abstract

Cancer immunoediting is the process whereby immune cells protect against cancer formation by sculpting the immunogenicity of developing tumors. Although the full process depends on innate and adaptive immunity, it remains unclear whether innate immunity alone is capable of immunoediting. To determine whether the innate immune system can edit tumor cells in the absence of adaptive immunity, we compared the incidence and immunogenicity of 3'methylcholanthrene-induced sarcomas in syngeneic wild-type, RAG2(-/-), and RAG2(-/-)x γc(-/-) mice. We found that innate immune cells could manifest cancer immunoediting activity in the absence of adaptive immunity. This activity required natural killer (NK) cells and interferon γ (IFN-γ), which mediated the induction of M1 macrophages. M1 macrophages could be elicited by administration of CD40 agonists, thereby restoring editing activity in RAG2(-/-)x γc(-/-) mice. Our results suggest that in the absence of adaptive immunity, NK cell production of IFN-γ induces M1 macrophages, which act as important effectors during cancer immunoediting.

Published
2012

33. Cancer immunoediting by the innate immune system in the absence of adaptive immunity.

Author

O'Sullivan, Timothy, Saddawi-Konefka, Robert, Vermi, William, Koebel, Catherine M, Arthur, Cora, White, J Michael, Uppaluri, Ravi, Andrews, Daniel M, Ngiow, Shin Foong, Teng, Michele WL, Smyth, Mark J, Schreiber, Robert D, and Bui, Jack D

Subjects
Killer Cells, Natural, Cell Line, Tumor, Macrophages, Animals, Mice, Knockout, Mice, Neoplasms, Sarcoma, Genetic Predisposition to Disease, DNA-Binding Proteins, Antigens, CD40, Histocompatibility Antigens Class II, Transplantation, Isogeneic, Phenotype, Interleukin Receptor Common gamma Subunit, Immunity, Innate, Interferon-gamma, Adaptive Immunity, Immunomodulation, CD40 Antigens, Cell Line, Tumor, Immunity, Innate, Killer Cells, Natural, Knockout, Transplantation, Isogeneic, Medical and Health Sciences, Immunology
Abstract

Cancer immunoediting is the process whereby immune cells protect against cancer formation by sculpting the immunogenicity of developing tumors. Although the full process depends on innate and adaptive immunity, it remains unclear whether innate immunity alone is capable of immunoediting. To determine whether the innate immune system can edit tumor cells in the absence of adaptive immunity, we compared the incidence and immunogenicity of 3'methylcholanthrene-induced sarcomas in syngeneic wild-type, RAG2(-/-), and RAG2(-/-)x γc(-/-) mice. We found that innate immune cells could manifest cancer immunoediting activity in the absence of adaptive immunity. This activity required natural killer (NK) cells and interferon γ (IFN-γ), which mediated the induction of M1 macrophages. M1 macrophages could be elicited by administration of CD40 agonists, thereby restoring editing activity in RAG2(-/-)x γc(-/-) mice. Our results suggest that in the absence of adaptive immunity, NK cell production of IFN-γ induces M1 macrophages, which act as important effectors during cancer immunoediting.

Published
2012

34. BCR-signalling synergizes with TLR-signalling for induction of AID and immunoglobulin class-switching through the non-canonical NF-κB pathway.

Author

Pone, Egest J, Zhang, Jinsong, Mai, Thach, White, Clayton A, Li, Guideng, Sakakura, John K, Patel, Pina J, Al-Qahtani, Ahmed, Zan, Hong, Xu, Zhenming, and Casali, Paolo

Subjects
B-Lymphocytes, Cells, Cultured, Animals, Mice, Inbred C57BL, Mice, Knockout, Mice, Cytidine Deaminase, Immunoglobulin G, NF-kappa B, Antigens, CD40, Signal Transduction, Immunoglobulin Class Switching, Up-Regulation, Toll-Like Receptors, Antigens, CD79, CD40 Antigens, CD79 Antigens, Genetics, Vaccine Related, Biotechnology, Cancer, Cells, Cultured, Inbred C57BL, Knockout, Antigens, CD40, CD79
Abstract

By diversifying antibody biological effector functions, class switch DNA recombination has a central role in the maturation of the antibody response. Here we show that BCR-signalling synergizes with Toll-like receptor (TLR) signalling to induce class switch DNA recombination. BCR-signalling activates the non-canonical NF-κB pathway and enhances the TLR-dependent canonical NF-κB pathway, thereby inducing activation-induced cytidine deaminase (AID), which is critical for class switch DNA recombination. Escherichia coli lipopolysaccharide (LPS) triggers dual TLR4/BCR-signalling and induces hallmarks of BCR-signalling, including CD79a phosphorylation and Ca(2+) mobilization, and activates both the NF-κB pathways to induce AID and class switch DNA recombination in a PI(3)K p85α-dependent fashion. CD40-signalling activates the two NF-κB pathways to induce AID and class switch DNA recombination independent of BCR-signalling. Finally, dual BCR/TLR-engaging NP-lipopolysaccharide effectively elicits class-switched NP-specific IgG3 and IgG2b in mice. Thus, by integrating signals of the non-canonical and canonical NF-κB pathways, BCR and TLRs synergize to induce AID and T-cell-independent class switch DNA recombination.

Published
2012

35. BCR-signalling synergizes with TLR-signalling for induction of AID and immunoglobulin class-switching through the non-canonical NF-κB pathway

Author

Pone, Egest J, Zhang, Jinsong, Mai, Thach, White, Clayton A, Li, Guideng, Sakakura, John K, Patel, Pina J, Al-Qahtani, Ahmed, Zan, Hong, Xu, Zhenming, and Casali, Paolo

Subjects
Biotechnology, Vaccine Related, Genetics, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Cancer, Animals, B-Lymphocytes, CD40 Antigens, CD79 Antigens, Cells, Cultured, Cytidine Deaminase, Immunoglobulin Class Switching, Immunoglobulin G, Mice, Mice, Inbred C57BL, Mice, Knockout, NF-kappa B, Signal Transduction, Toll-Like Receptors, Up-Regulation
Abstract

By diversifying antibody biological effector functions, class switch DNA recombination has a central role in the maturation of the antibody response. Here we show that BCR-signalling synergizes with Toll-like receptor (TLR) signalling to induce class switch DNA recombination. BCR-signalling activates the non-canonical NF-κB pathway and enhances the TLR-dependent canonical NF-κB pathway, thereby inducing activation-induced cytidine deaminase (AID), which is critical for class switch DNA recombination. Escherichia coli lipopolysaccharide (LPS) triggers dual TLR4/BCR-signalling and induces hallmarks of BCR-signalling, including CD79a phosphorylation and Ca(2+) mobilization, and activates both the NF-κB pathways to induce AID and class switch DNA recombination in a PI(3)K p85α-dependent fashion. CD40-signalling activates the two NF-κB pathways to induce AID and class switch DNA recombination independent of BCR-signalling. Finally, dual BCR/TLR-engaging NP-lipopolysaccharide effectively elicits class-switched NP-specific IgG3 and IgG2b in mice. Thus, by integrating signals of the non-canonical and canonical NF-κB pathways, BCR and TLRs synergize to induce AID and T-cell-independent class switch DNA recombination.

Published
2012

36. HIV-1 inhibits autophagy in bystander macrophage/monocytic cells through Src-Akt and STAT3.

Author

Van Grol, Jennifer, Subauste, Cecilia, Andrade, Rosa M, Fujinaga, Koh, Nelson, Julie, and Subauste, Carlos S

Subjects
Monocytes, Cells, Cultured, Cell Line, Macrophages, Humans, Toxoplasma, HIV-1, Sirolimus, Antigens, CD40, Immunoblotting, Autophagy, STAT3 Transcription Factor, Proto-Oncogene Proteins c-akt, CD40 Antigens, Cells, Cultured, General Science & Technology
Abstract

Autophagy is a homeostatic mechanism of lysosomal degradation. Defective autophagy has been linked to various disorders such as impaired control of pathogens and neurodegeneration. Autophagy is regulated by a complex array of signaling pathways that act upstream of autophagy proteins. Little is known about the role of altered regulatory signaling in disorders associated with defective autophagy. In particular, it is not known if pathogens inhibit autophagy by modulation of upstream regulatory pathways. Cells infected with HIV-1 blocked rapamycin-induced autophagy and CD40-induced autophagic killing of Toxoplasma gondii in bystander (non-HIV-1 infected) macrophage/monocytic cells. Blockade of autophagy was dependent on Src-Akt and STAT3 triggered by HIV-1 Tat and IL-10. Neutralization of the upstream receptors VEGFR, beta-integrin or CXCR4, as well as of HIV-1 Tat or IL-10 restored autophagy in macrophage/monocytic cells exposed to HIV-1-infected cells. Defective autophagic killing of T. gondii was detected in monocyte-derived macrophages from a subset of HIV-1(+) patients. This defect was also reverted by neutralization of Tat or IL-10. These studies revealed that a pathogen can impair autophagy in non-infected cells by activating counter-regulatory pathways. The fact that pharmacologic manipulation of cell signaling restored autophagy in cells exposed to HIV-1-infected cells raises the possibility of therapeutic manipulation of cell signaling to restore autophagy in HIV-1 infection.

Published
2010

37. HIV-1 Inhibits Autophagy in Bystander Macrophage/Monocytic Cells through Src-Akt and STAT3

Author

Van Grol, Jennifer, Subauste, Cecilia, Andrade, Rosa M, Fujinaga, Koh, Nelson, Julie, and Subauste, Carlos S

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Immunology, Medical Microbiology, HIV/AIDS, Infectious Diseases, Aetiology, 2.1 Biological and endogenous factors, Infection, Autophagy, CD40 Antigens, Cell Line, Cells, Cultured, HIV-1, Humans, Immunoblotting, Macrophages, Monocytes, Proto-Oncogene Proteins c-akt, STAT3 Transcription Factor, Sirolimus, Toxoplasma, General Science & Technology
Abstract

Autophagy is a homeostatic mechanism of lysosomal degradation. Defective autophagy has been linked to various disorders such as impaired control of pathogens and neurodegeneration. Autophagy is regulated by a complex array of signaling pathways that act upstream of autophagy proteins. Little is known about the role of altered regulatory signaling in disorders associated with defective autophagy. In particular, it is not known if pathogens inhibit autophagy by modulation of upstream regulatory pathways. Cells infected with HIV-1 blocked rapamycin-induced autophagy and CD40-induced autophagic killing of Toxoplasma gondii in bystander (non-HIV-1 infected) macrophage/monocytic cells. Blockade of autophagy was dependent on Src-Akt and STAT3 triggered by HIV-1 Tat and IL-10. Neutralization of the upstream receptors VEGFR, beta-integrin or CXCR4, as well as of HIV-1 Tat or IL-10 restored autophagy in macrophage/monocytic cells exposed to HIV-1-infected cells. Defective autophagic killing of T. gondii was detected in monocyte-derived macrophages from a subset of HIV-1(+) patients. This defect was also reverted by neutralization of Tat or IL-10. These studies revealed that a pathogen can impair autophagy in non-infected cells by activating counter-regulatory pathways. The fact that pharmacologic manipulation of cell signaling restored autophagy in cells exposed to HIV-1-infected cells raises the possibility of therapeutic manipulation of cell signaling to restore autophagy in HIV-1 infection.

Published
2010

38. An Early CD4+ T Cell–dependent Immunoglobulin A Response to Influenza Infection in the Absence of Key Cognate T–B Interactions

Author

Sangster, Mark Y, Riberdy, Janice M, Gonzalez, Maricela, Topham, David J, Baumgarth, Nicole, and Doherty, Peter C

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Influenza, Vaccine Related, Infectious Diseases, Prevention, Pneumonia & Influenza, HIV/AIDS, Biodefense, Emerging Infectious Diseases, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Infection, Animals, Antibodies, Viral, B-Lymphocytes, CD4-Positive T-Lymphocytes, CD40 Antigens, Cell Communication, Histocompatibility Antigens Class II, Immunoglobulin A, Immunoglobulin G, Immunologic Memory, Lymphocyte Activation, Mice, Mice, Inbred C57BL, Orthomyxoviridae Infections, T-Lymphocytes, B lymphocytes, T lymphocytes, antibody formation, immunoglobulin A, mucosal immunity, Medical and Health Sciences, Biomedical and clinical sciences, Health sciences
Abstract

Contact-mediated interactions between CD4+ T cells and B cells are considered crucial for T cell-dependent B cell responses. To investigate the ability of activated CD4+ T cells to drive in vivo B cell responses in the absence of key cognate T-B interactions, we constructed radiation bone marrow chimeras in which CD4+ T cells would be activated by wild-type (WT) dendritic cells, but would interact with B cells that lacked expression of either major histocompatibility complex class II (MHC II) or CD40. B cell responses were assessed after influenza virus infection of the respiratory tract, which elicits a vigorous, CD4+ T cell-dependent antibody response in WT mice. The influenza-specific antibody response was strongly reduced in MHC II knockout and CD40 knockout mice. MHC II-deficient and CD40-deficient B cells in the chimera environment also produced little virus-specific immunoglobulin (Ig)M and IgG, but generated a strong virus-specific IgA response with virus-neutralizing activity. The IgA response was entirely influenza specific, in contrast to the IgG2a response, which had a substantial nonvirus-specific component. Our study demonstrates a CD4+ T cell-dependent, antiviral IgA response that is generated in the absence of B cell signaling via MHC II or CD40, and is restricted exclusively to virus-specific B cells.

Published
2003

39. An early CD4+ T cell-dependent immunoglobulin A response to influenza infection in the absence of key cognate T-B interactions.

Author

Sangster, Mark Y, Riberdy, Janice M, Gonzalez, Maricela, Topham, David J, Baumgarth, Nicole, and Doherty, Peter C

Subjects
B-Lymphocytes, T-Lymphocytes, CD4-Positive T-Lymphocytes, Animals, Mice, Inbred C57BL, Mice, Orthomyxoviridae Infections, Immunoglobulin A, Immunoglobulin G, Antigens, CD40, Antibodies, Viral, Histocompatibility Antigens Class II, Lymphocyte Activation, Cell Communication, Immunologic Memory, CD40 Antigens, B lymphocytes, T lymphocytes, antibody formation, immunoglobulin A, mucosal immunity, Antibodies, Viral, Inbred C57BL, Medical and Health Sciences, Immunology
Abstract

Contact-mediated interactions between CD4+ T cells and B cells are considered crucial for T cell-dependent B cell responses. To investigate the ability of activated CD4+ T cells to drive in vivo B cell responses in the absence of key cognate T-B interactions, we constructed radiation bone marrow chimeras in which CD4+ T cells would be activated by wild-type (WT) dendritic cells, but would interact with B cells that lacked expression of either major histocompatibility complex class II (MHC II) or CD40. B cell responses were assessed after influenza virus infection of the respiratory tract, which elicits a vigorous, CD4+ T cell-dependent antibody response in WT mice. The influenza-specific antibody response was strongly reduced in MHC II knockout and CD40 knockout mice. MHC II-deficient and CD40-deficient B cells in the chimera environment also produced little virus-specific immunoglobulin (Ig)M and IgG, but generated a strong virus-specific IgA response with virus-neutralizing activity. The IgA response was entirely influenza specific, in contrast to the IgG2a response, which had a substantial nonvirus-specific component. Our study demonstrates a CD4+ T cell-dependent, antiviral IgA response that is generated in the absence of B cell signaling via MHC II or CD40, and is restricted exclusively to virus-specific B cells.

Published
2003

40. Constitutive CD8 expression allows inefficient maturation of CD4+ helper T cells in class II major histocompatibility complex mutant mice.

Author

Robey, E, Itano, A, Fanslow, WC, and Fowlkes, BJ

Subjects
HIV/AIDS, Inflammatory and immune system, Animals, Antigens, CD, Antigens, Differentiation, B-Lymphocyte, CD4 Antigens, CD40 Antigens, CD8 Antigens, Flow Cytometry, Gene Expression, Genes, MHC Class II, Histocompatibility Antigens Class II, Lymph Nodes, Lymphocyte Activation, Mice, Mice, Mutant Strains, Mice, Transgenic, T-Lymphocytes, Helper-Inducer, Thymus Gland, Medical and Health Sciences, Immunology
Abstract

Although mature CD4+ T cells bear T cell receptors (TCRs) that recognize class II major histocompatibility complex (MHC) and mature CD8+ T cells bear TCRs that recognize class I MHC, it is possible that the initial commitment of an immature thymocyte to a CD4 or CD8 lineage is made without regard to the specificity of the TCR. According to this model, CD4+ cells with class I TCR do not mature because the CD8 coreceptor is required for class I MHC recognition and positive selection. If this model is correct, constitutive expression of CD8 should allow CD4+ T cells with class I-specific TCRs to develop. In this report, we show that mature peripheral CD4+ cells are present in class II MHC-deficient mice that express a constitutive CD8.1 transgene. These cells share a number of properties with the major class II MHC-selected CD4 population, including the ability to express CD40 ligand upon activation. Although mature CD4 cells are also detectable in the thymus of class II MHC mutant/CD8.1 transgenic mice, they represent a small fraction of the mature CD4 cells found in mice that express class II MHC. These results indicate that some T cells choose the CD4 helper lineage independent of their antigen receptor specificity; however, the inefficiency of generating class I-specific CD4 cells leaves open the possibility that an instructive signal generated upon MHC recognition may bias lineage commitment.

Published
1994

41. Constitutive CD8 expression allows inefficient maturation of CD4+ helper T cells in class II major histocompatibility complex mutant mice.

Author

ROBEY, Ellen, Itano, A, Fanslow, W, and Fowlkes, B

Subjects
Animals, Antigens, CD, Antigens, Differentiation, B-Lymphocyte, CD4 Antigens, CD40 Antigens, CD8 Antigens, Flow Cytometry, Gene Expression, Genes, MHC Class II, Histocompatibility Antigens Class II, Lymph Nodes, Lymphocyte Activation, Mice, Mice, Mutant Strains, Mice, Transgenic, T-Lymphocytes, Helper-Inducer, Thymus Gland
Abstract

Although mature CD4+ T cells bear T cell receptors (TCRs) that recognize class II major histocompatibility complex (MHC) and mature CD8+ T cells bear TCRs that recognize class I MHC, it is possible that the initial commitment of an immature thymocyte to a CD4 or CD8 lineage is made without regard to the specificity of the TCR. According to this model, CD4+ cells with class I TCR do not mature because the CD8 coreceptor is required for class I MHC recognition and positive selection. If this model is correct, constitutive expression of CD8 should allow CD4+ T cells with class I-specific TCRs to develop. In this report, we show that mature peripheral CD4+ cells are present in class II MHC-deficient mice that express a constitutive CD8.1 transgene. These cells share a number of properties with the major class II MHC-selected CD4 population, including the ability to express CD40 ligand upon activation. Although mature CD4 cells are also detectable in the thymus of class II MHC mutant/CD8.1 transgenic mice, they represent a small fraction of the mature CD4 cells found in mice that express class II MHC. These results indicate that some T cells choose the CD4 helper lineage independent of their antigen receptor specificity; however, the inefficiency of generating class I-specific CD4 cells leaves open the possibility that an instructive signal generated upon MHC recognition may bias lineage commitment.

Published
1994

42. Activated T cells induce expression of B7/BB1 on normal or leukemic B cells through a CD40-dependent signal.

Author

Ranheim, EA and Kipps, TJ

Subjects
Hematology, 2.1 Biological and endogenous factors, Aetiology, Animals, Antigens, CD, Antigens, Differentiation, B-Lymphocyte, Antigens, Surface, B-Lymphocytes, B7-1 Antigen, CD40 Antigens, Cell Adhesion Molecules, Cells, Cultured, Humans, Intercellular Adhesion Molecule-1, Kinetics, Leukemia, Lymphocyte Activation, Mice, Phenotype, Signal Transduction, T-Lymphocytes, Medical and Health Sciences, Immunology
Abstract

Cognate interactions between antigen-presenting B and T cells play crucial roles in immunologic responses. T cells that have been activated via the crosslinking of CD3 are able to induce B cell proliferation and immunoglobulin secretion in a major histocompatibility complex-unrestricted and contact-dependent manner. We find that such activated human CD4+ T cells, but not control Ig-treated T cells, may induce normal or leukemic B cells to express B7/BB1 and significantly higher levels of CD54 intercellular adhesion molecule 1 via a process that also requires direct cell-cell contact. To discern what cell surface molecule(s) may be responsible for signalling B cells to express B7/BB1, we added various monoclonal antibodies (mAbs) specific for T or B cell accessory molecules or control mAbs to cocultures of alpha-CD3-activated T cells and resting B cells. We find that only alpha-CD40 mAbs can significantly inhibit the increased expression of B7/BB1, suggesting that the ligand for CD40 expressed on activated T cells may be an important inducer of B7/BB1 expression. Subsequent experiments in fact demonstrate that alpha-CD40 mAbs, but not control mAbs, induce changes in B cell phenotype similar to those induced by activated T cells when the mAbs are presented on Fc gamma RII (CDw32)-expressing L cells. These phenotypic changes have significant effects on B cell function. Whereas chronic lymphocytic leukemia (CLL) B cells normally are very poor stimulators in allogeneic mixed lymphocyte reactions (MLRs), CLL-B cells preactivated via CD40 crosslinking are significantly better presenters of alloantigen, affecting up to 30-fold-greater stimulation of T cell proliferation than that induced by control treated or nontreated CLL-B cells. Similarly, the MLR of T cells stimulated by allogeneic nonleukemic B cells can be enhanced significantly if the stimulator B cells are preactivated via CD40 crosslinking. The enhanced MLR generated by such preactivated B cells may be inhibited by blocking B7/BB1-CD28 interaction with CTLA4Ig. These studies demonstrate a novel, CD40-dependent pathway for inducing B cell expression of B7/BB1 and enhancing B cell antigen-presenting cell activity that can be initiated via cell-cell contact with alpha-CD3-stimulated CD4+ T cells.

Published
1993

43. Activated T cells induce expression of B7/BB1 on normal or leukemic B cells through a CD40-dependent signal.

Author

Ranheim, EA and Kipps, TJ

Subjects
B-Lymphocytes, T-Lymphocytes, Cells, Cultured, Animals, Humans, Mice, Leukemia, Cell Adhesion Molecules, Intercellular Adhesion Molecule-1, Antigens, CD, Antigens, Differentiation, B-Lymphocyte, Antigens, Surface, Lymphocyte Activation, Signal Transduction, Kinetics, Phenotype, B7-1 Antigen, CD40 Antigens, Antigens, CD, Differentiation, B-Lymphocyte, Surface, Cells, Cultured, Medical and Health Sciences, Immunology
Abstract

Cognate interactions between antigen-presenting B and T cells play crucial roles in immunologic responses. T cells that have been activated via the crosslinking of CD3 are able to induce B cell proliferation and immunoglobulin secretion in a major histocompatibility complex-unrestricted and contact-dependent manner. We find that such activated human CD4+ T cells, but not control Ig-treated T cells, may induce normal or leukemic B cells to express B7/BB1 and significantly higher levels of CD54 intercellular adhesion molecule 1 via a process that also requires direct cell-cell contact. To discern what cell surface molecule(s) may be responsible for signalling B cells to express B7/BB1, we added various monoclonal antibodies (mAbs) specific for T or B cell accessory molecules or control mAbs to cocultures of alpha-CD3-activated T cells and resting B cells. We find that only alpha-CD40 mAbs can significantly inhibit the increased expression of B7/BB1, suggesting that the ligand for CD40 expressed on activated T cells may be an important inducer of B7/BB1 expression. Subsequent experiments in fact demonstrate that alpha-CD40 mAbs, but not control mAbs, induce changes in B cell phenotype similar to those induced by activated T cells when the mAbs are presented on Fc gamma RII (CDw32)-expressing L cells. These phenotypic changes have significant effects on B cell function. Whereas chronic lymphocytic leukemia (CLL) B cells normally are very poor stimulators in allogeneic mixed lymphocyte reactions (MLRs), CLL-B cells preactivated via CD40 crosslinking are significantly better presenters of alloantigen, affecting up to 30-fold-greater stimulation of T cell proliferation than that induced by control treated or nontreated CLL-B cells. Similarly, the MLR of T cells stimulated by allogeneic nonleukemic B cells can be enhanced significantly if the stimulator B cells are preactivated via CD40 crosslinking. The enhanced MLR generated by such preactivated B cells may be inhibited by blocking B7/BB1-CD28 interaction with CTLA4Ig. These studies demonstrate a novel, CD40-dependent pathway for inducing B cell expression of B7/BB1 and enhancing B cell antigen-presenting cell activity that can be initiated via cell-cell contact with alpha-CD3-stimulated CD4+ T cells.

Published
1993

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