Your search keyword '"Neil C. Robson"' showing total 8 results

1. Presentation of tumour antigens by dendritic cells and challenges faced

Author

Max Schnurr, Sabine Hoves, Eugene Maraskovsky, and Neil C Robson

Subjects

Antigen Presentation, Clinical Trials as Topic, biology, medicine.medical_treatment, T cell, Immunology, Antigen presentation, Dendritic Cells, Immunotherapy, Major histocompatibility complex, medicine.anatomical_structure, Tumor Escape, Antigen, Antigens, Neoplasm, Neoplasms, medicine, biology.protein, Animals, Humans, Immunology and Allergy, Cytotoxic T cell, CD8

Abstract

The use of dendritic cells (DCs) for the generation of anti-tumour immunity has been the focus of a vast array of scientific and clinical studies. The ability of DCs to present protein tumour antigens (T-Ags) to CD4(+) and CD8(+) T cells is pivotal to the success of therapeutic cancer vaccines. DC's specialised capacity to cross-present exogenous Ags onto major histocompatibility (MHC) class I molecules for the generation of T-Ag-specific cytotoxic T lymphocytes (CTLs) has made these cells the focal point of vaccine-based immunotherapy of cancer. However, although DC-based strategies can induce T cell responses in cancer patients, recent reviews of clinical studies demonstrate that DC-based approaches have essentially failed to meet their clinical end points. These findings highlight the need to re-evaluate the DC-based vaccine strategies and incorporate recent advancements in DC biology and tumour immunology. The current review considers the issues related to how best to target the Ag-processing pathway of DCs, the role of adjuvants, the appropriate conditioning of the DCs and strategies to overcome tumour-mediated immune escape.

Published

2010

2. ISCOMATRIX Adjuvant Induces Efficient Cross-Presentation of Tumor Antigen by Dendritic Cells via Rapid Cytosolic Antigen Delivery and Processing via Tripeptidyl Peptidase II

Author

Neil C Robson, Eugene Maraskovsky, Max Schnurr, Hal Braley, Stefan Endres, Amanda Shin, Denise Airey, Jonathan Cebon, and Martin Orban

Subjects

Proteasome Endopeptidase Complex, medicine.medical_treatment, Immunology, Endosomes, Biology, Endocytosis, Aminopeptidases, Cancer Vaccines, Epitope, Cross-Priming, Cytosol, Adjuvants, Immunologic, Antigens, Neoplasm, medicine, Humans, Immunology and Allergy, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Myeloid Progenitor Cells, Phospholipids, Antigen Presentation, Hydrolysis, Quillaja, Serine Endopeptidases, Membrane Proteins, Tripeptidyl peptidase II, Cross-presentation, Cell Differentiation, Dendritic Cells, Saponins, Molecular biology, Immune complex, Tumor antigen, Cell biology, Drug Combinations, Protein Transport, CTL, Cholesterol, Lysosomes, Adjuvant, Signal Transduction

Abstract

Cancer vaccines aim to induce antitumor CTL responses, which require cross-presentation of tumor Ag to CTLs by dendritic cells (DCs). Adjuvants that facilitate cross-presentation of vaccine Ag are therefore key for inducing antitumor immunity. We previously reported that human DCs could not efficiently cross-present the full-length cancer/testis Ag NY-ESO-1 to CTL unless formulated as either an immune complex (NY-ESO-1/IC) or with ISCOMATRIX adjuvant. We now demonstrate that NY-ESO-1/ICs induce cross-presentation of HLA-A2- and HLA-Cw3-restricted epitopes via a proteasome-dependent pathway. In contrast, cross-presentation of NY-ESO-1/ISCOMATRIX vaccine was proteasome independent and required the cytosolic protease tripeptidyl peptidase II. Trafficking studies revealed that uptake of ICs and ISCOMATRIX vaccine by DCs occurred via endocytosis with delivery to lysosomes. Interestingly, ICs were retained in lysosomes, whereas ISCOMATRIX adjuvant induced rapid Ag translocation into the cytosol. Ag translocation was dependent on endosomal acidification and IL-4-driven differentiation of monocytes into DCs. This study demonstrates that Ag formulation determines Ag processing and supports a role for tripeptidyl peptidase II in cross-presentation of CTL epitopes restricted to diverse HLA alleles.

Published

2009

3. Directed evolution for improved secretion of cancer–testis antigen NY-ESO-1 from yeast

Author

Eugene Maraskovsky, Gerd Ritter, Shanshan W. Howland, Lloyd Old, Neil C Robson, Andrea Piatesi, K. Dane Wittrup, Christoph Renner, Jonathan Cebon, and James A. Rakestraw

Subjects

Male, Models, Molecular, medicine.drug_class, medicine.medical_treatment, Molecular Sequence Data, Saccharomyces cerevisiae, Biology, Monoclonal antibody, Epitope, Antigen, Cancer immunotherapy, Antigens, Neoplasm, Escherichia coli, medicine, Humans, Amino Acid Sequence, Sequence Homology, Amino Acid, Membrane Proteins, Molecular biology, Recombinant Proteins, Tumor antigen, Yeast, Cell biology, Genetic Techniques, Cancer/testis antigens, Directed Molecular Evolution, NY-ESO-1, Biotechnology

Abstract

NY-ESO-1 is a highly immunogenic tumor antigen and a promising vaccine candidate in cancer immunotherapy. Access to purified protein both for vaccine formulations and for monitoring antigen-specific immune responses is vital to vaccine development. Currently available recombinant Escherichia coli-derived NY-ESO-1 is isolated from inclusion bodies as a complex protein mixture and efforts to improve the purity of this antigen are required, especially for later-stage clinical trials. Using yeast cell surface display and fluorescence activated cell sorting techniques, we have engineered an NY-ESO-1 variant (NY-ESO-L5; C(75)A C(76)A C(78)A L(153)H) with a 100x improved display level on yeast compared to the wild-type protein. This mutant can be effectively produced as an Aga2p-fusion and purified in soluble form directly from the yeast cell wall. In the process, we have identified the epitope recognized by anti-NY-ESO-1 mAb E978 (79-87, GARGPESRL). The availability of an alternative expression host for this important antigen will help avoid artifactual false positive tests of patient immune response due to reaction against expression-host-specific contaminants.

Published

2006

4. Optimal effector functions in human natural killer cells rely upon autocrine bone morphogenetic protein signaling

Author

Angeles Vicente, Manuel Ramírez, Jonathan Cebon, Heng Wei, Ana Entrena, Alberto Varas, Neil C Robson, Víctor G. Martínez, Gustavo J. Melen, Laura Hidalgo, Andrew S. MacDonald, Rosa Sacedón, Tristan McAlpine, Eugene Maraskovsky, and Alexander T. Phythian-Adams

Subjects

Cancer Research, Effector, Cellular differentiation, medicine.medical_treatment, Cell Differentiation, Bone Morphogenetic Protein Receptors, Biology, Bone morphogenetic protein, Bone morphogenetic protein 2, Article, Cell biology, Killer Cells, Natural, Bone morphogenetic protein 6, Autocrine Communication, Cytokine, Oncology, Bone Morphogenetic Proteins, medicine, Humans, RNA, Messenger, Autocrine signalling, Interleukin 4, Signal Transduction

Abstract

Natural killer (NK) cells are critical for innate tumor immunity due to their specialized ability to recognize and kill neoplastically transformed cells. However, NK cells require a specific set of cytokine-mediated signals to achieve optimal effector function. Th1-associated cytokines promote effector functions that are inhibited by the prototypic Th2 cytokine IL4 and the TGFβ superfamily members TGFβ1 and activin-A. Interestingly, the largest subgroup of the TGFβ superfamily are the bone morphogenetic proteins (BMP), but the effects of BMP signaling on NK cell effector functions have not been evaluated. Here, we demonstrate that blood-circulating NK cells express type I and II BMP receptors, BMP-2 and BMP-6 ligands, and phosphorylated isoforms of Smad-1/-5/-8, which mediate BMP family member signaling. In opposition to the inhibitory effects of TGFβ1 or activin-A, autocrine BMP signaling was supportive to NK cell function. Mechanistic investigations in cytokine and TLR-L–activated NK cells revealed that BMP signaling optimized IFNγ and global cytokine and chemokine production, phenotypic activation and proliferation, and autologous dendritic cell activation and target cytotoxicity. Collectively, our findings identify a novel auto-activatory pathway that is essential for optimal NK cell effector function, one that might be therapeutically manipulated to help eradicate tumors. Cancer Res; 74(18); 5019–31. ©2014 AACR.

Published

2014

5. Development of prophylactic and therapeutic vaccines using the ISCOMATRIX adjuvant

Author

Eugene Maraskovsky, Debbie Drane, Nicholas S. Wilson, Jeff Boyle, Neil C Robson, and Max Schnurr

Subjects

T cell, medicine.medical_treatment, Immunology, Models, Biological, Immune system, Antigen, Adjuvants, Immunologic, Neoplasms, medicine, Immunology and Allergy, Cytotoxic T cell, Humans, Phospholipids, Vaccines, biology, business.industry, Immunogenicity, Cell Biology, Immunotherapy, Dendritic Cells, Saponins, Drug Combinations, medicine.anatomical_structure, Cholesterol, Virus Diseases, biology.protein, Antibody, business, Adjuvant

Abstract

Adjuvants are components that when added to subunit antigen (Ag) vaccines boost their immunogenicity and thus immune efficacy. However, there are few adjuvants that are approved for clinical use resulting in a critical need for the development of safe and effective adjuvants for use in both prophylactic and therapeutic vaccines. The paucity of appropriate adjuvants is more chronic for the development of therapeutic vaccines for cancer and chronic infectious disease, which need to induce cytotoxic T-cell responses via cross-presentation of the vaccine Ag by dendritic cells. The ISCOMATRIX adjuvant represents a unique adjuvant system that facilitates Ag delivery and presentation as well as immunomodulation to provide enhanced and accelerated immune responses. The immune responses generated are of broad specificity to the vaccine Ag, and include robust antibody responses of multiple subclasses as well as both CD4(+) and CD8(+) T-cell responses. Here we discuss our understanding of the mechanisms of action by which ISCOMATRIX adjuvant may facilitate these integrated immune responses and touch on insights gained through its clinical experience.

Published

2009

6. The Role of Dendritic Cells in Regulating Mucosal Immunity and Tolerance

Author

Allan McI. Mowat, Owain R. Millington, Lindsay J. McIntyre, Lucy Anne Parker, Neil C Robson, Anne M. Donachie, Fernando Gabriel Chirdo, and Helen Beacock-Sharp

Subjects

Lamina propria, medicine.medical_treatment, T cell, Priming (immunology), chemical and pharmacologic phenomena, Biology, Small intestine, Immune system, medicine.anatomical_structure, Antigen, Immunology, medicine, Adjuvant, Lymph node

Abstract

The intestinal immune system discriminates between invasive pathogens and antigens that are harmless, such as food proteins and commensal bacteria. The latter groups of antigens normally induce tolerance and a breakdown in this homeostatic process can lead to diseases such as coeliac disease or Crohn's disease. The nature ofthe intestinal immune response depends on how antigen is presented to CD4+ T cells by dendritic cells (DCs). Both oral tolerance and priming are influenced by the numbers and activation status of DCs in the gut and its draining lymphoid tissues, and our current work indicates that dietary proteins are taken up preferentially by DCs in the lamina propria of the small intestine. These then migrate to interact with antigen-specific CD4+ T cells in the mesenteric lymph node. In vivo and in vitro studies using purified lamina propria DCs suggest these may play a unique role in the regulation of intestinal immune responses. We propose that local DCs are the gatekeepers of the mucosal immune system, inducing tolerance under physiological conditions, but being sufficiently responsive to inflammatory stimuli to allow T cell priming and protective immunity when necessary. In addition, we will discuss evidence that adjuvant vectors such as ISCOMS may be effective mucosal vaccines due to an ability to activate intestinal DCs.

Published

2008

7. Activin-A: a novel dendritic cell-derived cytokine that potently attenuates CD40 ligand-specific cytokine and chemokine production

Author

Neil C Robson, Tracey Toy, Heng Wei, Tristan McAlpine, Kathy Wilson, David James Phillips, Weisan Chen, Damien Zanker, Naomi Kirkpatrick, Eugene Maraskovsky, Amanda Shin, Imke Helling, Vinochani Pillay, Suzanne Svobodova, and Jonathan Cebon

Subjects

Lipopolysaccharides, Chemokine, Follistatin, medicine.medical_treatment, Bone Morphogenetic Protein 7, Immunology, CD40 Ligand, chemical and pharmacologic phenomena, Receptors, Cell Surface, Bone Morphogenetic Protein 4, Cell Separation, Biology, CD8-Positive T-Lymphocytes, Biochemistry, Epitopes, Immune system, Transforming Growth Factor beta, medicine, Humans, Autocrine signalling, Cell Proliferation, Cell Biology, Hematology, Activin receptor, Dendritic cell, Dendritic Cells, Myostatin, Cell biology, Activins, Cytokine, Gene Expression Regulation, embryonic structures, Bone Morphogenetic Proteins, biology.protein, Tumor necrosis factor alpha, Chemokines, hormones, hormone substitutes, and hormone antagonists

Abstract

Activin-A is a transforming growth factor-beta (TGF-beta) superfamily member that plays a pivotal role in many developmental and reproductive processes. It is also involved in neuroprotection, apoptosis of tumor and some immune cells, wound healing, and cancer. Its role as an immune-regulating protein has not previously been described. Here we demonstrate for the first time that activin-A has potent autocrine effects on the capacity of human dendritic cells (DCs) to stimulate immune responses. Human monocyte-derived DCs (MoDCs) and the CD1c(+) and CD123(+) peripheral blood DC populations express both activin-A and the type I and II activin receptors. Furthermore, MoDCs and CD1c(+) myeloid DCs rapidly secrete high levels of activin-A after exposure to bacteria, specific toll-like receptor (TLR) ligands, or CD40 ligand (CD40L). Blocking autocrine activin-A signaling in DCs using its antagonist, follistatin, enhanced DC cytokine (IL-6, IL-10, IL-12p70, and tumor necrosis factor-alpha [TNF-alpha]) and chemokine (IL-8, IP-10, RANTES, and MCP-1) production during CD40L stimulation, but not TLR-4 ligation. Moreover, antagonizing DC-derived activin-A resulted in significantly enhanced expansion of viral antigen-specific effector CD8(+) T cells. These findings establish an immune-regulatory role for activin-A in DCs, highlighting the potential of antagonizing activin-A signaling in vivo to enhance vaccine immunogenicity.

Published

2007

8. The combined CTA1-DD/ISCOM adjuvant vector promotes priming of mucosal and systemic immunity to incorporated antigens by specific targeting of B cells

Author

Anja Helgeby, Anne M. Donachie, Allan McI. Mowat, Karin Schön, Nils Lycke, Helen Beackock-Sharp, Karin Lövgren, and Neil C Robson

Subjects

Cholera Toxin, T cell, medicine.medical_treatment, Recombinant Fusion Proteins, Immunology, Priming (immunology), Biology, Antibodies, Mice, Immune system, Th2 Cells, Adjuvants, Immunologic, medicine, Immunology and Allergy, Animals, Antigens, Immunity, Mucosal, B cell, B-Lymphocytes, Immunogenicity, ISCOM, Germinal center, Th1 Cells, medicine.anatomical_structure, Lymph Nodes, Adjuvant, ISCOMs

Abstract

The cholera toxin A1 (CTA1)-DD/QuilA-containing, immune-stimulating complex (ISCOM) vector is a rationally designed mucosal adjuvant that greatly potentiates humoral and cellular immune responses. It was developed to incorporate the distinctive properties of either adjuvant alone in a combination that exerted additive enhancing effects on mucosal immune responses. In this study we demonstrate that CTA1-DD and an unrelated Ag can be incorporated together into the ISCOM, resulting in greatly augmented immunogenicity of the Ag. To demonstrate its relevance for protection against infectious diseases, we tested the vector incorporating PR8 Ag from the influenza virus. After intranasal immunization we found that the immunogenicity of the PR8 proteins were significantly augmented by a mechanism that was enzyme dependent, because the presence of the enzymatically inactive CTA1R7K-DD mutant largely failed to enhance the response over that seen with ISCOMs alone. The combined vector was a highly effective enhancer of a broad range of immune responses, including specific serum Abs and balanced Th1 and Th2 CD4+ T cell priming as well as a strong mucosal IgA response. Unlike unmodified ISCOMs, Ag incorporated into the combined vector could be presented by B cells in vitro and in vivo as well as by dendritic cells; it also accumulated in B cell follicles of draining lymph nodes when given s.c. and stimulated much enhanced germinal center reactions. Strikingly, the enhanced adjuvant activity of the combined vector was absent in B cell-deficient mice, supporting the idea that B cells are important for the adjuvant effects of the combined CTA1-DD/ISCOM vector.