Your search keyword '"Douglas C Palmer"' showing total 58 results

1. BACH2 regulates CD8(+) T cell differentiation by controlling access of AP-1 factors to enhancers

Author

Klaus Okkenhaug, Yuka Kanno, Luca Gattinoni, Han-Yu Shih, Peng Li, Giulia Fabozzi, Kylie M. Quinn, Yun Ji, Derek C. Macallan, Jun Zhu, Yoshiyuki Wakabayashi, Shashank J. Patel, Warren J. Leonard, Robert L. Eil, Akihiko Muto, Zhiya Yu, Christopher A. Klebanoff, Kazuhiko Igarashi, Douglas C. Palmer, Rosanne Spolski, Rahul Roychoudhuri, Jenny H. Pan, David Clever, Madhusudhanan Sukumar, Nicholas P. Restifo, John J. O'Shea, Roychoudhuri, Rahul [0000-0002-5392-1853], Okkenhaug, Klaus [0000-0002-9432-4051], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Cellular differentiation, Immunology, Oncogene Protein p65(gag-jun), Vaccinia virus, Biology, Adaptive Immunity, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Article, 03 medical and health sciences, Mice, Vaccinia, Immunology and Allergy, Cytotoxic T cell, Animals, Enhancer, Cells, Cultured, Mice, Knockout, Effector, Activator (genetics), T-cell receptor, Cell Differentiation, Acquired immune system, Mice, Inbred C57BL, Transcription Factor AP-1, 030104 developmental biology, Basic-Leucine Zipper Transcription Factors, Enhancer Elements, Genetic, Gene Expression Regulation, Cancer research, Signal transduction, Immunologic Memory, Signal Transduction

Abstract

T cell antigen receptor (TCR) signaling drives distinct responses depending upon the differentiation state and context of CD8+ T cells. We hypothesized that access of signal-dependent transcription factors (TFs) to enhancers is dynamically regulated to shape transcriptional responses to TCR signaling. We found that the TF BACH2 restrains terminal differentiation to enable generation of long-lived memory cells and protective immunity following viral infection. BACH2 was recruited to enhancers where it limited expression of TCR-driven genes by attenuating the availability of activator protein 1 (AP-1) sites to Jun family signal-dependent TFs. In naïve cells, this prevented TCR-driven induction of genes associated with terminal differentiation. Upon effector differentiation, reduced expression of BACH2 and its phosphorylation enabled unrestrained induction of TCR-driven effector programs.

Published

2018

2. Lineage relationship of CD8+ T cell subsets is revealed by progressive changes in the epigenetic landscape

Author

Douglas C. Palmer, John S. Tsang, Suresh Cuddapah, Christopher A. Klebanoff, Ena Wang, Joseph G. Crompton, Yun Ji, Manikandan Narayanan, Luca Gattinoni, Rahul Roychoudhuri, Keji Zhao, Francesco M. Marincola, Shashank J. Patel, Madhusudhanan Sukumar, Weiqun Peng, Wenjing Yang, and Nicholas P. Restifo

Subjects

Histone H3 Lysine 4, Epigenetics in learning and memory, Immunology, CD8-Positive T-Lymphocytes, Biology, Methylation, Chromatin remodeling, Epigenesis, Genetic, Histones, 03 medical and health sciences, 0302 clinical medicine, Animals, Immunology and Allergy, Cytotoxic T cell, Cell Lineage, Epigenetics, Promoter Regions, Genetic, Research Articles, 030304 developmental biology, Epigenomics, Genetics, 0303 health sciences, Gene Expression Profiling, Chromatin Assembly and Disassembly, Lymphocyte Subsets, Mice, Inbred C57BL, Enhancer Elements, Genetic, Infectious Diseases, Histone, biology.protein, H3K4me3, Immunologic Memory, Protein Processing, Post-Translational, 030215 immunology

Abstract

To better elucidate epigenetic mechanisms that correlate with the dynamic gene expression program observed upon T-cell differentiation, we investigated the genomic landscape of histone modifications in naive and memory CD8(+) T cells. Using a ChIP-Seq approach coupled with global gene expression profiling, we generated genome-wide histone H3 lysine 4 (H3K4me3) and H3 lysine 27 (H3K27me3) trimethylation maps in naive, T memory stem cells, central memory cells, and effector memory cells in order to gain insight into how histone architecture is remodeled during T cell differentiation. We show that H3K4me3 histone modifications are associated with activation of genes, while H3K27me3 is negatively correlated with gene expression at canonical loci and enhancers associated with T-cell metabolism, effector function, and memory. Our results also reveal histone modifications and gene expression signatures that distinguish the recently identified T memory stem cells from other CD8(+) T-cell subsets. Taken together, our results suggest that CD8(+) lymphocytes undergo chromatin remodeling in a progressive fashion. These findings have major implications for our understanding of peripheral T-cell ontogeny and the formation of immunological memory.

Published

2015

3. Akt Inhibition Enhances Expansion of Potent Tumor-Specific Lymphocytes with Memory Cell Characteristics

Author

Nicolas Acquavella, Robert L. Eil, Anthony J. Leonardi, Alena Gros, Sid P. Kerkar, David Clever, Joseph G. Crompton, Steven A. Rosenberg, Christopher A. Klebanoff, Trevor Upham, Ena Wang, Nicholas P. Restifo, Douglas C. Palmer, Douglas T. Fearon, Ryan D. Michalek, Mark S. Sundrud, Madhusudhanan Sukumar, Luca Gattinoni, Ken-ichi Hanada, Eric Tran, Rahul Roychoudhuri, Zhiya Yu, Pawel Muranski, and Francesco M. Marincola

Subjects

Cancer Research, Adoptive cell transfer, medicine.medical_treatment, Cell, Melanoma, Experimental, Mice, Transgenic, chemical and pharmacologic phenomena, Biology, Immunotherapy, Adoptive, Article, Cell therapy, Mice, Random Allocation, Lymphocytes, Tumor-Infiltrating, Mice, Inbred NOD, Tumor Cells, Cultured, medicine, Animals, Humans, Cytotoxic T cell, Melanoma, Protein Kinase Inhibitors, Protein kinase B, Cancer, Immunotherapy, medicine.disease, Mice, Inbred C57BL, medicine.anatomical_structure, Oncology, Immunology, Cancer research, Immunologic Memory, Proto-Oncogene Proteins c-akt

Abstract

Adoptive cell therapy (ACT) using autologous tumor-infiltrating lymphocytes (TIL) results in complete regression of advanced cancer in some patients, but the efficacy of this potentially curative therapy may be limited by poor persistence of TIL after adoptive transfer. Pharmacologic inhibition of the serine/threonine kinase Akt has recently been shown to promote immunologic memory in virus-specific murine models, but whether this approach enhances features of memory (e.g., long-term persistence) in TIL that are characteristically exhausted and senescent is not established. Here, we show that pharmacologic inhibition of Akt enables expansion of TIL with the transcriptional, metabolic, and functional properties characteristic of memory T cells. Consequently, Akt inhibition results in enhanced persistence of TIL after adoptive transfer into an immunodeficient animal model and augments antitumor immunity of CD8 T cells in a mouse model of cell-based immunotherapy. Pharmacologic inhibition of Akt represents a novel immunometabolomic approach to enhance the persistence of antitumor T cells and improve the efficacy of cell-based immunotherapy for metastatic cancer. Cancer Res; 75(2); 296–305. ©2014 AACR.

Published

2015

4. Cish actively silences TCR signaling in CD8+ T cells to maintain tumor tolerance

Author

Lakshmi Balagopalan, Christopher A. Klebanoff, Geoffrey Guittard, Madhusudhanan Sukumar, Robert L. Eil, Douglas C. Palmer, Zulmarie Franco, Luca Gattinoni, Nicholas P. Restifo, David Clever, Rajat Varma, Ena Wang, Lawrence E. Samelson, Joseph G. Crompton, Yun Ji, Shashank J. Patel, Anna Chichura, Rahul Roychoudhuri, Francesco M. Marincola, and Nicholas J. Van Panhuys

Subjects

inorganic chemicals, Mice, 129 Strain, medicine.medical_treatment, Immunology, Immunoblotting, Melanoma, Experimental, Receptors, Antigen, T-Cell, chemical and pharmacologic phenomena, Suppressor of Cytokine Signaling Proteins, Biology, CD8-Positive T-Lymphocytes, Immunotherapy, Adoptive, Article, Immune tolerance, Cancer immunotherapy, Cell Line, Tumor, medicine, Immune Tolerance, Tumor Microenvironment, otorhinolaryngologic diseases, Immunology and Allergy, Cytotoxic T cell, Animals, Humans, Avidity, CISH, Cells, Cultured, Research Articles, Cell Proliferation, Oligonucleotide Array Sequence Analysis, Mice, Knockout, Tumor microenvironment, Microscopy, Confocal, Phospholipase C gamma, Reverse Transcriptase Polymerase Chain Reaction, T-cell receptor, Mice, Inbred C57BL, Cancer research, sense organs, Transcriptome, CD8, psychological phenomena and processes, Protein Binding, Signal Transduction

Abstract

Palmer et al. find that Cish, a member of the SOCS family, is induced by TCR stimulation in CD8+ T cells and inhibits their functional avidity against tumor. The authors uncover a novel mechanism of suppression for a SOCS member., Improving the functional avidity of effector T cells is critical in overcoming inhibitory factors within the tumor microenvironment and eliciting tumor regression. We have found that Cish, a member of the suppressor of cytokine signaling (SOCS) family, is induced by TCR stimulation in CD8+ T cells and inhibits their functional avidity against tumors. Genetic deletion of Cish in CD8+ T cells enhances their expansion, functional avidity, and cytokine polyfunctionality, resulting in pronounced and durable regression of established tumors. Although Cish is commonly thought to block STAT5 activation, we found that the primary molecular basis of Cish suppression is through inhibition of TCR signaling. Cish physically interacts with the TCR intermediate PLC-γ1, targeting it for proteasomal degradation after TCR stimulation. These findings establish a novel targetable interaction that regulates the functional avidity of tumor-specific CD8+ T cells and can be manipulated to improve adoptive cancer immunotherapy.

Published

2015

5. Collapse of the Tumor Stroma is Triggered by IL-12 Induction of Fas

Author

Jenny H. Pan, Ling Zhang, Nicholas J. Van Panhuys, Nicholas P. Restifo, Richard A. Morgan, Steven A. Rosenberg, Zhiya Yu, Anthony J. Leonardi, Sid P. Kerkar, Douglas C. Palmer, and Joseph G. Crompton

Subjects

Stromal cell, Antigen presentation, Melanoma, Experimental, Mice, Transgenic, CD8-Positive T-Lymphocytes, Biology, Fas ligand, Mice, Interleukin 21, Drug Discovery, Genetics, Animals, Cytotoxic T cell, fas Receptor, Molecular Biology, Interleukin 3, Pharmacology, Dendritic Cells, Flow Cytometry, Interleukin-12, Mice, Inbred C57BL, Immunology, Cancer research, Interleukin 12, Molecular Medicine, Original Article, Female, CD8

Abstract

Engineering CD8⁺ T cells to deliver interleukin 12 (IL-12) to the tumor site can lead to striking improvements in the ability of adoptively transferred T cells to induce the regression of established murine cancers. We have recently shown that IL-12 triggers an acute inflammatory environment that reverses dysfunctional antigen presentation by myeloid-derived cells within tumors and leads to an increase in the infiltration of adoptively transferred antigen-specific CD8⁺ T cells. Here, we find that local delivery of IL-12 increased the expression of Fas within tumor-infiltrating macrophages, dendritic cells, and myeloid-derived suppressor cells (MDSC), and that these changes were abrogated in mice deficient in IL-12-receptor signaling. Importantly, upregulation of Fas in host mice played a critical role in the proliferation and antitumor activity of adoptively transferred IL-12-modified CD8⁺ T cells. We also observed higher percentages of myeloid-derived cell populations within tumors in Fas-deficient mice, indicating that tumor stromal destruction was dependent on the Fas death receptor. Taken together, these results describe the likely requirement for costimulatory reverse signaling through Fasl on T cells that successfully infiltrate tumors, a mechanism triggered by the induction of Fas expression on myeloid-derived cells by IL-12 and the subsequent collapse of the tumor stroma.

Published

2013

6. Retinoic acid controls the homeostasis of pre-cDC–derived splenic and intestinal dendritic cells

Author

Anthony J. Leonardi, Madhusudhanan Sukumar, Yasmine Belkaid, John R. Grainger, Christopher A. Klebanoff, Douglas C. Palmer, Sean P. Spencer, Christoph Wilhelm, Jinshan Wang, Christopher D. Scott, Gabriela A. Ferreyra, Rahul Roychoudhuri, Junfeng Sun, Joseph L. Napoli, Yun Ji, Parizad Torabi-Parizi, Nicholas P. Restifo, Pawel Muranski, Luca Gattinoni, Rongman Cai, Robert L. Danner, Jason A. Hall, and Zachary A. Borman

Subjects

Receptors, Retinoic Acid, Cellular differentiation, Retinoic acid, chemistry.chemical_compound, Mice, 0302 clinical medicine, Neoplasms, Immunology and Allergy, Homeostasis, Retinoid, Intestinal Mucosa, Vitamin A, 2. Zero hunger, 0303 health sciences, hemic and immune systems, Cell Differentiation, 3. Good health, Intestines, medicine.anatomical_structure, Phenotype, Organ Specificity, Female, Signal transduction, Whole-Body Irradiation, medicine.drug, Signal Transduction, medicine.drug_class, Cell Survival, Immunology, Spleen, chemical and pharmacologic phenomena, Tretinoin, Biology, Article, Immunophenotyping, 03 medical and health sciences, Immune system, medicine, Animals, Humans, 030304 developmental biology, Cell Proliferation, Histocompatibility Antigens Class II, Dendritic Cells, chemistry, 030215 immunology

Abstract

Retinoic acid is required to maintain pre-DC–derived CD11b+CD8α−Esamhigh dendritic cells (DCs) in the spleen and CD11b+CD103+ DCs in the gut., Dendritic cells (DCs) comprise distinct populations with specialized immune-regulatory functions. However, the environmental factors that determine the differentiation of these subsets remain poorly defined. Here, we report that retinoic acid (RA), a vitamin A derivative, controls the homeostasis of pre-DC (precursor of DC)–derived splenic CD11b+CD8α−Esamhigh DCs and the developmentally related CD11b+CD103+ subset within the gut. Whereas mice deprived of RA signaling significantly lost both of these populations, neither pre-DC–derived CD11b−CD8α+ and CD11b−CD103+ nor monocyte-derived CD11b+CD8α−Esamlow or CD11b+CD103− DC populations were deficient. In fate-tracking experiments, transfer of pre-DCs into RA-supplemented hosts resulted in near complete conversion of these cells into the CD11b+CD8α− subset, whereas transfer into vitamin A–deficient (VAD) hosts caused diversion to the CD11b−CD8α+ lineage. As vitamin A is an essential nutrient, we evaluated retinoid levels in mice and humans after radiation-induced mucosal injury and found this conditioning led to an acute VAD state. Consequently, radiation led to a selective loss of both RA-dependent DC subsets and impaired class II–restricted auto and antitumor immunity that could be rescued by supplemental RA. These findings establish a critical role for RA in regulating the homeostasis of pre-DC–derived DC subsets and have implications for the management of patients with immune deficiencies resulting from malnutrition and irradiation.

Published

2013

7. Repression of the DNA-binding inhibitor Id3 by Blimp-1 limits the formation of memory CD8+ T cells

Author

Madhusudhanan Sukumar, Christopher A. Klebanoff, Nicholas P. Restifo, Zoltan Pos, Mahadev Rao, Robert Reger, Ena Wang, Zhiya Yu, Yun Ji, Pawel Muranski, Douglas C. Palmer, Zachary A. Borman, Luca Gattinoni, Francesco M. Marincola, and David S. Schrump

Subjects

Regulation of gene expression, Cell culture, Effector, Cellular differentiation, Immunology, Immunology and Allergy, Cytotoxic T cell, Biology, Psychological repression, Transcription factor, Molecular biology, CD8

Abstract

The transcriptional repressor Blimp-1 promotes the differentiation of CD8(+) T cells into short-lived effector cells (SLECs) that express the lectin-like receptor KLRG-1, but how it operates remains poorly defined. Here we show that Blimp-1 bound to and repressed the promoter of the gene encoding the DNA-binding inhibitor Id3 in SLECs. Repression of Id3 by Blimp-1 was dispensable for SLEC development but limited the ability of SLECs to persist as memory cells. Enforced expression of Id3 was sufficient to restore SLEC survival and enhanced recall responses. Id3 function was mediated in part through inhibition of the transcriptional activity of E2A and induction of genes regulating genome stability. Our findings identify the Blimp-1-Id3-E2A axis as a key molecular switch that determines whether effector CD8(+) T cells are programmed to die or enter the memory pool.

Published

2011

8. Determinants of Successful CD8+ T-Cell Adoptive Immunotherapy for Large Established Tumors in Mice

Author

Christian S. Hinrichs, Steven E. Finkelstein, Sid P. Kerkar, Steven A. Rosenberg, Luca Gattinoni, Douglas C. Palmer, Pawel Muranski, Yun Ji, Christopher D. Scott, Nicholas P. Restifo, Christopher A. Klebanoff, and Zachary A. Borman

Subjects

Interleukin 2, Cancer Research, Adoptive cell transfer, medicine.medical_treatment, Melanoma, Experimental, Mice, Transgenic, CD8-Positive T-Lymphocytes, Biology, Cancer Vaccines, Immunotherapy, Adoptive, Article, Mice, Antigen, Cell Line, Tumor, medicine, Animals, Cytotoxic T cell, Interleukin-15, Dose-Response Relationship, Drug, Interleukin-7, Interleukins, Melanoma, Cell Differentiation, Immunotherapy, medicine.disease, Tumor Burden, Mice, Inbred C57BL, Treatment Outcome, Cytokine, Oncology, Interleukin 15, Immunology, Cytokines, Interleukin-2, Regression Analysis, Immunologic Memory, medicine.drug

Abstract

Purpose: Adoptive cell transfer (ACT) of tumor infiltrating or genetically engineered T cells can cause durable responses in patients with metastatic cancer. Multiple clinically modifiable parameters can comprise this therapy, including cell dose and phenotype, in vivo antigen restimulation, and common gamma-chain (γc) cytokine support. However, the relative contributions of each these individual components to the magnitude of the antitumor response have yet to be quantified. Experimental Design: To systematically and quantitatively appraise each of these variables, we employed the Pmel-1 mouse model treating large, established B16 melanoma tumors. In addition to cell dose and magnitude of in vivo antigen restimulation, we also evaluated the relative efficacy of central memory (TCM), effector memory (TEM), and stem cell memory (TSCM) subsets on the strength of tumor regression as well as the dose and type of clinically available γc cytokines, including IL-2, IL-7, IL-15, and IL-21. Results: We found that cell dose, T-cell differentiation status, and viral vaccine titer each were correlated strongly and significantly with the magnitude of tumor regression. Surprisingly, although the total number of IL-2 doses was correlated with tumor regression, no significant benefit to prolonged (≥6 doses) administration was observed. Moreover, the specific type and dose of γc cytokine only moderately correlated with response. Conclusion: Collectively, these findings elucidate some of the key determinants of successful ACT immunotherapy for the treatment of cancer in mice and further show that γc cytokines offer a similar ability to effectively drive antitumor T-cell function in vivo. Clin Cancer Res; 17(16); 5343–52. ©2011 AACR.

Published

2011

9. Transplantation of mouse HSCs genetically modified to express a CD4-restricted TCR results in long-term immunity that destroys tumors and initiates spontaneous autoimmunity

Author

Jon N. Marsh, Hal E. Broxmeyer, Nicholas P. Restifo, Christopher E. Touloukian, Nicholas D. Klemen, Kenneth Cornetta, Giao Hangoc, Andrew G. Brandmaier, Douglas C. Palmer, Sung P. Ha, and Garrett Kinnebrew

Subjects

CD4-Positive T-Lymphocytes, Genetically modified mouse, Adoptive cell transfer, medicine.medical_treatment, T cell, Receptors, Antigen, T-Cell, Vitiligo, Autoimmunity, Mice, Transgenic, Mice, SCID, In Vitro Techniques, Biology, Autoimmune Diseases, Mice, Melanocyte differentiation, Mice, Inbred NOD, Transduction, Genetic, Cell Line, Tumor, HLA-DR4 Antigen, medicine, Animals, Humans, T-cell receptor, Hematopoietic Stem Cell Transplantation, Neoplasms, Experimental, General Medicine, Immunotherapy, Mice, Inbred C57BL, Transplantation, medicine.anatomical_structure, Immunology, Cancer research, CD8, Research Article

Abstract

The development of effective cancer immunotherapies has been consistently hampered by several factors, including an inability to instigate long-term effective functional antitumor immunity. This is particularly true for immunotherapies that focus on the adoptive transfer of activated or genetically modified mature CD8+ T cells. In this study, we sought to alter and enhance long-term host immunity by genetically modifying, then transplanting, mouse HSCs. We first cloned a previously identified tumor-reactive HLA-DR4–restricted CD4+ TCR specific for the melanocyte differentiation antigen tyrosinase-related protein 1 (Tyrp1), then constructed both a high-expression lentivirus vector and a TCR-transgenic mouse expressing the genes encoding this TCR. Using these tools, we demonstrated that both mouse and human HSCs established durable, high-efficiency TCR gene transfer following long-term transplantation into lethally irradiated mice transgenic for HLA-DR4. Recipients of genetically modified mouse HSCs developed spontaneous autoimmune vitiligo that was associated with the presence of a Th1-polarized memory effector CD4+ T cell population that expressed the Tyrp1-specific TCR. Most importantly, large numbers of CD4+ T cells expressing the Tyrp1-specific TCR were detected in secondary HLA-DR4–transgenic transplant recipients, and these mice were able to destroy subcutaneously administered melanoma cells without the aid of vaccination, immune modulation, or cytokine administration. These results demonstrate the creation of what we believe to be a novel translational model of durable lentiviral gene transfer that results in long-term effective immunity.

Published

2010

10. Tumor-Specific CD8+ T Cells Expressing Interleukin-12 Eradicate Established Cancers in Lymphodepleted Hosts

Author

Ling Zhang, Sid P. Kerkar, Douglas C. Palmer, Luis Sanchez-Perez, Zhiya Yu, Pawel Muranski, Steven A. Rosenberg, Luca Gattinoni, Andrew Kaiser, Giorgio Trinchieri, Zachary A. Borman, Robert Reger, Nicholas P. Restifo, Andrea Boni, and Richard A. Morgan

Subjects

Cancer Research, Adoptive cell transfer, medicine.medical_treatment, Melanoma, Experimental, Mice, Transgenic, CD8-Positive T-Lymphocytes, Biology, Protein Engineering, Immunotherapy, Adoptive, Article, Mice, Lymphocytes, Tumor-Infiltrating, Transduction, Genetic, medicine, Animals, Cytotoxic T cell, Tumor microenvironment, Interleukin, FOXP3, Immunotherapy, Flow Cytometry, Interleukin-12, Mice, Inbred C57BL, Retroviridae, Oncology, Immunology, Interleukin 12, Female, CD8

Abstract

T-cell–based immunotherapies can be effective in the treatment of large vascularized tumors, but they rely on adoptive transfer of substantial numbers (∼20 million) of tumor-specific T cells administered together with vaccination and high-dose interleukin (IL)-2. In this study, we report that ∼10,000 T cells gene-engineered to express a single-chain IL-12 molecule can be therapeutically effective against established tumors in the absence of exogenous IL-2 and vaccine. Although IL-12–engineered cells did not perist long-term in hosts, they exhibited enhanced functionality and were detected in higher numbers intratumorally along with increased numbers of endogenous natural killer and CD8+ T cells just before regression. Importantly, transferred T cells isolated from tumors stably overproduced supraphysiologic amounts of IL-12, and the therapeutic effect of IL-12 produced within the tumor microenvironment could not be mimicked with high doses of exogenously provided IL-12. Furthermore, antitumor effects could be recapitulated by engineering wild-type open-repertoire splenocytes to express both the single-chain IL-12 and a recombinant tumor-specific T-cell receptor (TCR), but only when individual cells expressed both the TCR and IL-12, indicating that arrested migration of T cells at the tumor site was required for their activities. Successful tumor eradication was dependent on a lymphodepleting preconditioning regimen that reduced the number of intratumoral CD4+ Foxp3+ T regulatory cells. Our findings reveal an approach to genetically modify T cells to reduce the cell number needed, eliminate the need for vaccines or systemic IL-2, and improve immunotherapy efficacy based on adoptive transfer of gene-engineered T cells. Cancer Res; 70(17); 6725–34. ©2010 AACR.

Published

2010

11. IFN-γ-receptor signaling ameliorates transplant vasculopathy through attenuation of CD8+T-cell-mediated injury of vascular endothelial cells

Author

Matthias W. Hoffmann, Daniel S. Engeler, Yinghua Tian, Douglas C. Palmer, Sonja Firner, Burkhard Ludewig, Pierre-Alain Clavien, Simone Miller, Philippe Krebs, Nicholas P. Restifo, and Beatrice Bolinger

Subjects

Graft Rejection, Male, Adoptive cell transfer, Immunology, Priming (immunology), Enzyme-Linked Immunosorbent Assay, Mice, Transgenic, Cell Separation, CD8-Positive T-Lymphocytes, Article, Mice, Downregulation and upregulation, PD-L1, Animals, Immunology and Allergy, Cytotoxic T cell, Receptor, Receptors, Interferon, Feedback, Physiological, biology, Reverse Transcriptase Polymerase Chain Reaction, Endothelial Cells, Flow Cytometry, Adoptive Transfer, Mice, Inbred C57BL, Transplantation, biology.protein, Cancer research, Heart Transplantation, Female, CD8, Signal Transduction

Abstract

Occlusive transplant vasculopathy (TV) is the major cause for chronic graft rejection. Since endothelial cells (EC) are the first graft cells encountered by activated host lymphocytes, it is important to delineate the molecular mechanisms that coordinate the interaction of EC with activated T cells. Here, the interaction of CD8(+) T cells with Ag-presenting EC in vivo was examined using a transgenic heart transplantation model with beta-galactosidase (beta-gal) expression exclusively in EC (Tie2-LacZ hearts). We found that priming with beta-gal peptide-loaded DC failed to generate a strong systemic IFN-gamma response, but elicited pronounced TV in both IFN-gamma receptor (IFNGR)-competent, and ifngr(-/-) Tie2-LacZ hearts. In contrast, stimulation of EC-specific CD8(+) T cells with beta-gal-recombinant mouse cytomegalovirus (MCMV-LacZ) in recipients of ifngr(+/+) Tie2-LacZ hearts did not precipitate significant TV. However, MCMV-LacZ infection of recipients of ifngr(-/-) Tie2-LacZ hearts led to massive activation of beta-gal-specific CD8 T cells, and led to development of fulminant TV. Further analyses revealed that the strong systemic IFN-gamma "storm" associated with MCMV infection induced upregulation of programmed death-1 ligand 1 (PD-L1) on EC, and subsequent attenuation of programmed death-1 (PD-1)-expressing EC-specific CD8(+) T cells. Thus, IFNGR signaling in ECs activates a potent peripheral negative feedback circuit that protects vascularized grafts from occlusive TV.

Published

2010

12. Suppressors of cytokine signaling (SOCS) in T cell differentiation, maturation, and function

Author

Nicholas P. Restifo and Douglas C. Palmer

Subjects

medicine.medical_treatment, T cell, Cellular differentiation, Immunology, Suppressor of Cytokine Signaling Proteins, Biology, Communicable Diseases, Immunotherapy, Adoptive, Suppressor of cytokine signalling, Article, Autoimmune Diseases, T-Lymphocyte Subsets, Neoplasms, medicine, Animals, Humans, Immunology and Allergy, IL-2 receptor, Cell Differentiation, Immunotherapy, Lymphoid Progenitor Cells, Cell biology, Cytokine, medicine.anatomical_structure, T cell differentiation, Immunologic Memory, CD8, Signal Transduction

Abstract

Cytokines are key modulators of T cell biology, but their influence can be attenuated by suppressors of cytokine signaling (SOCS), a family of proteins consisting of eight members, SOCS1-7 and CIS. SOCS proteins regulate cytokine signals that control the polarization of CD4(+) T cells into Th1, Th2, Th17, and T regulatory cell lineages, the maturation of CD8(+) T cells from naïve to "stem-cell memory" (Tscm), central memory (Tcm), and effector memory (Tem) states, and the activation of these lymphocytes. Understanding how SOCS family members regulate T cell maturation, differentiation, and function might prove critical in improving adoptive immunotherapy for cancer and therapies aimed at treating autoimmune and infectious diseases.

Published

2009

13. Programming tumor-reactive effector memory CD8+ T cells in vitro obviates the requirement for in vivo vaccination

Author

Zhiya Yu, Douglas C. Palmer, Luca Gattinoni, Christopher A. Klebanoff, Nicholas P. Restifo, and Leroy N. Hwang

Subjects

CD3 Complex, Immunology, Melanoma, Experimental, Genes, MHC Class I, Mice, Transgenic, Cell Separation, CD8-Positive T-Lymphocytes, In Vitro Techniques, Major histocompatibility complex, Cancer Vaccines, Biochemistry, Major Histocompatibility Complex, Interferon-gamma, Mice, CD28 Antigens, Interferon, Neoplasms, MHC class I, medicine, Animals, Cytotoxic T cell, Interferon gamma, IL-2 receptor, Immunobiology, biology, Cell Biology, Hematology, T lymphocyte, Flow Cytometry, Cell biology, Phenotype, biology.protein, CD8, medicine.drug

Abstract

Naive and memory CD8+ T cells can undergo programmed activation and expansion in response to a short T-cell receptor stimulus, but the extent to which in vitro programming can qualitatively substitute for an in vivo antigen stimulation remains unknown. We show that self-/tumor-reactive effector memory CD8+ T cells (TEM) programmed in vitro either with peptide-pulsed antigen-presenting cells or plate-bound anti-CD3/anti-CD28 embark on a highly stereotyped response of in vivo clonal expansion and tumor destruction nearly identical to that of vaccine-stimulated TEM cells. This programmed response was associated with an interval of antigen-independent interferon-γ (IFN-γ) release that facilitated the dynamic expression of the major histocompatibility complex class I restriction element H-2Db on responding tumor cells, leading to recognition and subsequent tumor lysis. Delaying cell transfer for more than 24 hours after stimulation or infusion of cells deficient in IFN-γ entirely abrogated the benefit of the programmed response, whereas transfer of cells unable to respond to IFN-γ had no detriment to antitumor immunity. These findings extend the phenomenon of a programmable effector response to memory CD8+ T cells and have major implications for the design of current adoptive-cell transfer trials.

Published

2009

14. Tumor-specific Th17-polarized cells eradicate large established melanoma

Author

Pawel Muranski, Lionel Feigenbaum, Luca Gattinoni, Christopher E. Touloukian, Andrea Boni, Krzysztof Ptak, Claudia Wrzesinski, Nicholas P. Restifo, Douglas C. Palmer, Lydie Cassard, Chrystal M. Paulos, Chi-Chao Chan, Paul A. Antony, Andrew Kaiser, Keith W. Kerstann, Kari R. Irvine, and Christian S. Hinrichs

Subjects

CD4-Positive T-Lymphocytes, Cytotoxicity, Immunologic, Adoptive cell transfer, medicine.medical_treatment, Immunology, Mice, Transgenic, T-Cell Antigen Receptor Specificity, Pregnancy Proteins, Biology, Biochemistry, Epitope, Interferon-gamma, Mice, Interleukin 21, Antigen, T-Lymphocyte Subsets, Cell Line, Tumor, MHC class I, medicine, Animals, Cytotoxic T cell, IL-2 receptor, Melanoma, Immunobiology, Cell Biology, Hematology, Immunotherapy, Mice, Inbred C57BL, Interferon Type I, Cancer research, biology.protein

Abstract

CD4+ T cells can differentiate into multiple effector subsets, but the potential roles of these subsets in anti-tumor immunity have not been fully explored. Seeking to study the impact of CD4+ T cell polarization on tumor rejection in a model mimicking human disease, we generated a new MHC class II-restricted, T-cell receptor (TCR) transgenic mouse model in which CD4+ T cells recognize a novel epitope in tyrosinase-related protein 1 (TRP-1), an antigen expressed by normal melanocytes and B16 murine melanoma. Cells could be robustly polarized into Th0, Th1, and Th17 subtypes in vitro, as evidenced by cytokine, chemokine, and adhesion molecule profiles and by surface markers, suggesting the potential for differential effector function in vivo. Contrary to the current view that Th1 cells are most important in tumor rejection, we found that Th17-polarized cells better mediated destruction of advanced B16 melanoma. Their therapeutic effect was critically dependent on interferon-γ (IFN-γ) production, whereas depletion of interleukin (IL)–17A and IL-23 had little impact. Taken together, these data indicate that the appropriate in vitro polarization of effector CD4+ T cells is decisive for successful tumor eradication. This principle should be considered in designing clinical trials involving adoptive transfer–based immunotherapy of human malignancies.

Published

2008

15. CD4+T Cells Are Programmed to Differentiate Before Entry into Division

Author

Ronald N. Germain, Nicholas J. Van Panhuys, and Douglas C. Palmer

Subjects

Interleukin 21, Naive T cell, Cellular differentiation, T-cell receptor, Immunology, Priming (immunology), FOXP3, IL-2 receptor, Biology, Acquired immune system, Cell biology

Abstract

In order to provide a protective host response to a vast array of invading pathological microorganisms the ability of naïve CD4+T cells to differentiate into discrete effector subsets, each able to mediate specific aspects of immunity is a central tenet of the adaptive immune response. T helper (Th) 1 cells mediate protection against intracellular pathogens, such as bacterial and viral infections, whereas Th2 cells mediate protective responses against extracellular pathogens such as helminthic parasites. Additionally, naive T cells may be induced to differentiate into T regulatory (Treg) cells, with Treg cells serving as an immunological checkpoint to dampen the immune response and protect against inappropriate activation of the immune system. As in the case of autoimmune diseases where aberrant Th1 cell differentiation occurs in response to self antigens or in the case of asthma and allergic responses where aberrant Th2 cell differentiation occurs in response to non-self environmental antigens. In order to activate naïve T cells and induce them to differentiate to combat a specific invading pathogen dendritic cells (DC), which are present throughout the body serving as cellular sentinels constantly surveying there surrounding for evidence of infection must be activated. Activation of DC occurs through ligand mediated activation of pathogen associated molecular pattern receptors or danger associated molecular pattern receptors. Allowing for the engagement of specific downstream patterns of effector molecule regulation that play an instructive role in the decision making process which occurs during the activation, division and differentiation of naïve T cells. Current dogma suggests that the generation of differentiated effector CD4+T cells takes place over a 3–4 day period following the initial engagement of the T cell receptor (TCR). Activation of CD4+T cells is thought to occur in three distinct functional phases, priming, proliferation and differentiation. Through the use of an in vitro culture system that allows for precise control of the factors which regulate the activation of naïve CD4+T cells we initially assessed the requirements for cytokine signaling vs. strength of TCR signaling during differentiation. Here, we determined that Th2 differentiation can be driven following activation with a weak TCR stimuli in the absence of additional cytokine inputs, indicating that Th2 differentiation occurs through a default endogenous pathway following activation. Whereas, Th1 differentiation required both a strong TCR signal and the presence of an instructive cytokine, in this case IFNg in order for differentiation to occur. We additionally investigated the kinetics of upregulation of the master transcription factors that regulate commitment to a specific T-helper phenotype. CD4+T cells acquire the disposition to commit to either Th1, Th2 or Treg lineages very soon after activation >24 hr and prior to the induction of division, as evidenced by increased expression of the master transcription factor proteins Tbet, GATA3 or Foxp3. Further, we show that entrance into cellular division is not required for the induction of a full program of differentiation to occur. By interrupting the activation of naïve CD4+T cells at different time points following stimulation through the use of anti-MHCII antibody. We were able to probe the effects that both alteration of TCR signal strength and alteration of TCR signal length have on the induction of differentiation as compared to division. This approach allowed us to demonstrate that TCR signaling is responsible for two distinct activation programs, whereby the strength of signal that a naïve T cell receives working in concert with or without cytokine at an early phase can induce Th1 or Th2 differentiation respectively. Whereas the length of the TCR signal can be construed as a secondary component of activation which controls the ability of CD4+T cells to enter into division. Here, we determined that at low concentrations of antigen TCR signaling must occur for 2 hr. Demonstrating that the signal delivered through the TCR represents not only an essential component for inducing an immune response through the initial activation of naïve CD4+T cells, but also acts as a rheostat that is able to determine both the strength and the length of TCR signal received. In turn controlling cellular decision making by dictating the outcome of differentiation and whether a cell will enter into cycle. As such these results have important implications for the rational design of vaccination strategies, in order to modulate components of TCR signaling cascade to direct an optimal response against the target vaccine antigens.

Published

2016

16. Hematopoietic stem cells promote the expansion and function of adoptively transferred antitumor CD8+ T cells

Author

Steven A. Rosenberg, Andrew Kaiser, Claudia Wrzesinski, Douglas C. Palmer, Zhiya Yu, Chrystal M. Paulos, Luca Gattinoni, and Nicholas P. Restifo

Subjects

Adoptive cell transfer, biology, T-Lymphocytes, medicine.medical_treatment, Hematopoietic Stem Cell Transplantation, General Medicine, Hematopoietic stem cell transplantation, Hematopoietic Stem Cells, Immunotherapy, Adoptive, Lymphocyte Depletion, Haematopoiesis, Immune system, Neoplasms, Immunology, MHC class I, medicine, biology.protein, Cancer research, Animals, Humans, Cytotoxic T cell, Stem cell, CD8, Research Article

Abstract

Depleting host immune elements with nonmyeloablative regimens prior to the adoptive transfer of tumor-specific CD8 + T cells significantly enhances tumor treatment. In the current study, superior antitumor efficacy was achieved by further increasing the intensity of lymphodepletion to a level that required HSC transplantation. Surprisingly, the HSC transplant and not the increased lymphodepletion caused a robust expansion of adoptively transferred tumor-specific CD8 + T cells. The HSC-driven cell expansion of effector, but not of naive, CD8 + T cells was independent of in vivo restimulation by MHC class I-expressing APCs. Simultaneously, HSCs also facilitated the reconstitution of the host lymphoid compartment, including inhibitory elements, not merely via the production of progeny cells but by enhancing the expansion of cells that had survived lymphodepletion. Profound lymphodepletion, by myeloablation or by genetic means, focused the nonspecific HSC boost preferentially toward the transferred tumor-specific T cells, leading to successful tumor treatment. These findings indicate that CD8 + T cell-mediated tumor responses can be efficiently driven by HSCs in the myeloablative setting and have substantial implications for the design of new antitumor immunotherapies.

Published

2007

17. Cish actively silences tcr signaling in CD8+ T cells to maintain tumor tolerance

Author

Lakshmi Balagopalan, Christopher A. Klebanoff, Lawrence E. Samelson, Geoff Guittard, Madhusudhanan Sukumar, Robert L. Eil, David Clever, Shashank J. Patel, Douglas C. Palmer, Nicholas P. Restifo, Rahul Roychoudhuri, and Zulmarie Franco

Subjects

Pharmacology, Cancer Research, Tumor microenvironment, Effector, medicine.medical_treatment, Immunology, T-cell receptor, chemical and pharmacologic phenomena, Biology, Cytokine, Oncology, Cancer immunotherapy, Poster Presentation, medicine, Cancer research, Molecular Medicine, Immunology and Allergy, Cytotoxic T cell, Avidity, CISH

Abstract

Meeting abstracts Improving the functional avidity of effector T cells is critical in overcoming inhibitory factors within the tumor microenvironment and eliciting tumor regression. We have found that Cish, a member of the Suppressor of Cytokine Signaling (SOCS) family, is induced by TCR

Published

2015

18. CTLA-4 dysregulation of self/tumor-reactive CD8+ T-cell function is CD4+ T-cell dependent

Author

Nicholas P. Restifo, Douglas C. Palmer, Paul A. Antony, Steven A. Rosenberg, David M. Heimann, Anju Ranganathan, Marc R. Theoret, Luca Gattinoni, and Deborah R. Surman

Subjects

CD4-Positive T-Lymphocytes, Immunology, Vitiligo, Autoimmunity, CD8-Positive T-Lymphocytes, Biology, Lymphocyte Activation, Biochemistry, Lymphocyte Depletion, Autoimmune Diseases, Mice, Interleukin 21, Antigens, CD, Neoplasms, Animals, Cytotoxic T cell, CTLA-4 Antigen, IL-2 receptor, Antigen-presenting cell, Cell Proliferation, Immunobiology, Homeodomain Proteins, Mice, Knockout, Peripheral tolerance, Cell Biology, Hematology, Natural killer T cell, Antigens, Differentiation, CTLA-4, Cancer research, CD8

Abstract

Cytotoxic T lymphocyte–associated antigen 4 (CTLA-4) maintains peripheral tolerance by suppressing T-cell activation and proliferation but its precise role in vivo remains unclear. We sought to elucidate the impact of CTLA-4 expression on self/tumor-reactive CD8+ T cells by using the glycoprotein (gp) 100–specific T-cell receptor (TCR) transgenic mouse, pmel-1. pmel-1 CLTA-4–/– mice developed profound, accelerated autoimmune vitiligo. This enhanced autoimmunity was associated with a small but highly activated CD8+ T-cell population and large numbers of CD4+ T cells not expressing the transgenic TCR. Adoptive transfer of pmel-1 CLTA-4–/– CD8+ T cells did not mediate superior antitumor immunity in the settings of either large established tumors or tumor challenge, suggesting that the mere absence of CTLA-4–mediated inhibition on CD8+ T cells did not directly promote enhancement of their effector functions. Removal of CD4+ T cells by crossing the pmel-1 CLTA-4–/– mouse onto a Rag-1–/– background resulted in the complete abrogation of CD8+ T-cell activation and autoimmune manifestations. The effects of CD4+ CLTA-4–/– T cells were dependent on the absence of CTLA-4 on CD8+ T cells. These results indicated that CD8+ CLTA-4–/– T-cell–mediated autoimmunity and tumor immunity required CD4+ T cells in which the function was dysregulated by the absence of CTLA-4–mediated negative costimulation.

Published

2006

19. Cross-priming utilizes antigen not available to the direct presentation pathway

Author

Douglas C. Palmer, Keri B. Donohue, Nicholas P. Restifo, Christopher C. Norbury, Eric F. Tewalt, Jean M. Grant, and Marc R. Theoret

Subjects

Immunology, Antigen presentation, Receptors, Antigen, T-Cell, Antigen-Presenting Cells, Mice, Transgenic, CD8-Positive T-Lymphocytes, Major histocompatibility complex, Cell Line, Mice, Cross-Priming, Antigen, Neoplasms, Animals, Immunology and Allergy, Cytotoxic T cell, Antigens, Cycloheximide, Antigen-presenting cell, Protein Synthesis Inhibitors, Antigen Presentation, CD40, biology, Antigen processing, T-cell receptor, Original Articles, Flow Cytometry, Adoptive Transfer, Cell biology, Mice, Inbred C57BL, Electroporation, Virus Diseases, biology.protein

Abstract

CD8+ T cells play a crucial role in protective immunity to viruses and tumours. Antiviral CD8+ T cells are initially activated by professional antigen presenting cells (pAPCs) that are directly infected by viruses (direct-priming) or following uptake of exogenous antigen transferred from virus-infected or tumour cells (cross-priming). In order to efficiently target each of these antigen-processing pathways during vaccine design, it is necessary to delineate the properties of the natural substrates for either of these antigen-processing pathways. In this study, we utilized a novel T-cell receptor (TCR) transgenic mouse to examine the requirement for both antigen synthesis and synthesis of other cellular factors during direct or cross-priming. We found that direct presentation required ongoing synthesis of antigen, but that cross-priming favoured long-lived antigens and did not require ongoing antigen production. Even after prolonged blockade of protein synthesis in the donor cell, cross-priming was unaffected. In contrast, direct-presentation was almost undetectable in the absence of antigen neosynthesis and required ongoing protein synthesis. This suggests that the direct- and cross-priming pathways may utilize differing pools of antigen, an observation that has far-reaching implications for the rational design of vaccines aimed at the generation of protective CD8+ T cells.

Published

2006

20. Removal of homeostatic cytokine sinks by lymphodepletion enhances the efficacy of adoptively transferred tumor-specific CD8+ T cells

Author

Claudia Wrzesinski, David M. Heimann, Paul J. Spiess, Christopher A. Klebanoff, Douglas C. Palmer, Steven A. Rosenberg, Nicholas P. Restifo, Steven E. Finkelstein, Paul A. Antony, Charles D. Surh, Leroy N. Hwang, Zhiya Yu, and Luca Gattinoni

Subjects

T cell, Immunology, Autoimmunity, CD8-Positive T-Lymphocytes, Biology, T-Lymphocytes, Regulatory, Mice, Interleukin 21, Cell Line, Tumor, Lymphopenia, Neoplasms, medicine, Animals, Immunology and Allergy, Cytotoxic T cell, IL-2 receptor, Antigen-presenting cell, Vaccination, Brief Definitive Report, Peripheral tolerance, Natural killer T cell, Adoptive Transfer, Cell biology, Mice, Inbred C57BL, medicine.anatomical_structure, Cytokines, Female, Whole-Body Irradiation, CD8

Abstract

Depletion of immune elements before adoptive cell transfer (ACT) can dramatically improve the antitumor efficacy of transferred CD8+ T cells, but the specific mechanisms that contribute to this enhanced immunity remain poorly defined. Elimination of CD4+CD25+ regulatory T (T reg) cells has been proposed as a key mechanism by which lymphodepletion augments ACT-based immunotherapy. We found that even in the genetic absence of T reg cells, a nonmyeloablative regimen substantially augmented CD8+ T cell reactivity to self-tissue and tumor. Surprisingly, enhanced antitumor efficacy and autoimmunity was caused by increased function rather than increased numbers of tumor-reactive T cells, as would be expected by homeostatic mechanisms. The γC cytokines IL-7 and IL-15 were required for augmenting T cell functionality and antitumor activity. Removal of γC cytokine–responsive endogenous cells using antibody or genetic means resulted in the enhanced antitumor responses similar to those seen after nonmyeloablative conditioning. These data indicate that lymphodepletion removes endogenous cellular elements that act as sinks for cytokines that are capable of augmenting the activity of self/tumor-reactive CD8+ T cells. Thus, the restricted availability of homeostatic cytokines can be a contributing factor to peripheral tolerance, as well as a limiting resource for the effectiveness of tumor-specific T cells.

Published

2005

21. Central memory self/tumor-reactive CD8 + T cells confer superior antitumor immunity compared with effector memory T cells

Author

Luca Gattinoni, Steven A. Rosenberg, Christopher A. Klebanoff, Thomas A. Waldmann, Douglas C. Palmer, Parizad Torabi-Parizi, Samuel T Hwang, Nicholas P. Restifo, Steven E. Finkelstein, Keith W. Kerstann, Paul A. Antony, and Adela R. Cardones

Subjects

Interleukin 2, Lymphoid Tissue, T cell, medicine.medical_treatment, Mice, Transgenic, CD8-Positive T-Lymphocytes, Biology, Mice, Interleukin 21, Cell Line, Tumor, Neoplasms, medicine, Animals, Cytotoxic T cell, IL-2 receptor, Interleukin-15, Mice, Knockout, Multidisciplinary, Immunotherapy, Active, Immunotherapy, Biological Sciences, Flow Cytometry, Microarray Analysis, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Interleukin 15, Immunology, Cancer research, Interleukin-2, Immunologic Memory, CD8, medicine.drug

Abstract

Central memory CD8 + T cells (T CM ) and effector memory CD8 + T cells (T EM ) are found in humans and mice; however, their relative contributions to host immunity have only recently been examined in vivo . Further, the ability of T CM to treat an established tumor or infection has yet to be evaluated. To address the therapeutic potential of different tumor-reactive CD8 + T cell memory subsets, we used an established model for the in vitro generation of T CM and T EM by using IL-15 and IL-2, respectively. Adoptively transferred T CM exhibited a potent in vivo recall response when combined with tumor-antigen vaccination and exogenous IL-2, leading to the eradication of large established tumors. By contrast, T EM were far less effective on a per-cell basis. Microarray analysis revealed that the signature of highly in vivo effective antitumor T cells included the overexpression of genes responsible for trafficking to secondary lymphoid tissues. This gene expression profile correctly predicted the in vitro and in vivo lymphoid-homing attributes of tumor-reactive T cells. Furthermore, we found that homing to secondary lymphoid tissue is required for optimal tumor treatment. Our findings indicated that highly in vivo effective antitumor T cells were those that initially targeted secondary lymphoid tissue, rather than tumor sites, as had previously been postulated. Thus, tumor-reactive CD8 + T cell populations with the phenotypic and functional attributes of T CM may be superior to T EM /effector T cells for adoptive immunotherapies using concomitant tumor-antigen vaccination.

Published

2005

22. Vaccine-Stimulated, Adoptively Transferred CD8+ T Cells Traffic Indiscriminately and Ubiquitously while Mediating Specific Tumor Destruction

Author

Claudia Wrzesinski, Shahram Farid, Nicholas P. Restifo, Sanjeeve Balasubramaniam, Marc R. Theoret, Douglas C. Palmer, Leroy N. Hwang, James Chih-Hsin Yang, Christopher A. Klebanoff, Luca Gattinoni, Ken-ichi Hanada, Allan L. Goldstein, and Zhiya Yu

Subjects

biology, CD30, medicine.medical_treatment, T cell, Melanoma, Immunology, Immunotherapy, medicine.disease, Interleukin 21, medicine.anatomical_structure, Perforin, biology.protein, Cancer research, medicine, Immunology and Allergy, Cytotoxic T cell, CD8

Abstract

It has been suggested that antitumor T cells specifically traffic to the tumor site, where they effect tumor destruction. To test whether tumor-reactive CD8+ T cells specifically home to tumor, we assessed the trafficking of gp100-specific pmel-1 cells to large, vascularized tumors that express or do not express the target Ag. Activation of tumor-specific CD8+ pmel-1 T cells with IL-2 and vaccination with an altered peptide ligand caused regression of gp100-positive tumors (B16), but not gp100-negative tumors (methylcholanthrene 205), implanted on opposing flanks of the same mouse. Surprisingly, we found approximately equal and very large numbers of pmel-1 T cells (>25% of all lymphocytes) infiltrating both Ag-positive and Ag-negative tumors. We also found evidence of massive infiltration and proliferation of activated antitumor pmel-1 cells in a variety of peripheral tissues, including lymph nodes, liver, spleen, and lungs, but not peripheral blood. Most importantly, evidence for T cell function, as measured by production of IFN-γ, release of perforin, and activation of caspase-3 in target cells, was confined to Ag-expressing tumor. We thus conclude that CD8+ T cell-mediated destruction of tumor is the result of specific T cell triggering at the tumor site. The ability to induce ubiquitous homing and specific tumor destruction may be important in the case of noninflammatory metastatic tumor foci.

Published

2004

23. Tumor Regression and Autoimmunity after Reversal of a Functionally Tolerant State of Self-reactive CD8+ T Cells

Author

Paul J. Spiess, Christopher A. Klebanoff, Deborah R. Surman, Laurina A. de Jong, David M. Heimann, Florry A. Vyth-Dreese, Willem W. Overwijk, Zhiya Yu, Steven A. Rosenberg, Ada M. Kruisbeek, Steven E. Finkelstein, Douglas C. Palmer, Paul A. Antony, Leroy N. Hwang, Trees A. M. Dellemijn, Nicholas P. Restifo, Lionel Feigenbaum, and Marc R. Theoret

Subjects

Adoptive cell transfer, T cell, Immunology, Melanoma, Experimental, Receptors, Antigen, T-Cell, Autoimmunity, Mice, Transgenic, Streptamer, Biology, CD8-Positive T-Lymphocytes, Article, Major Histocompatibility Complex, Interleukin 21, Interferon-gamma, Mice, medicine, Immune Tolerance, Immunology and Allergy, Cytotoxic T cell, Animals, Humans, Antigen-presenting cell, adoptive cell transfer, Membrane Glycoproteins, IL-2, Histocompatibility Antigens Class I, Vaccination, Natural killer T cell, Adoptive Transfer, Tumor antigen, Neoplasm Proteins, Mice, Inbred C57BL, Survival Rate, medicine.anatomical_structure, recombinant poxvirus, Self Tolerance, Interleukin-2, immunotherapy, T cell epitope, gp100 Melanoma Antigen

Abstract

Many tumor-associated antigens are derived from nonmutated “self” proteins. T cells infiltrating tumor deposits recognize self-antigens presented by tumor cells and can be expanded in vivo with vaccination. These T cells exist in a functionally tolerant state, as they rarely result in tumor eradication. We found that tumor growth and lethality were unchanged in mice even after adoptive transfer of large numbers of T cells specific for an MHC class I–restricted epitope of the self/tumor antigen gp100. We sought to develop new strategies that would reverse the functionally tolerant state of self/tumor antigen-reactive T cells and enable the destruction of large (with products of perpendicular diameters of >50 mm2), subcutaneous, unmanipulated, poorly immunogenic B16 tumors that were established for up to 14 d before the start of treatment. We have defined three elements that are all strictly necessary to induce tumor regression in this model: (a) adoptive transfer of tumor-specific T cells; (b) T cell stimulation through antigen-specific vaccination with an altered peptide ligand, rather than the native self-peptide; and (c) coadministration of a T cell growth and activation factor. Cells, vaccination, or cyto-kine given alone or any two in combination were insufficient to induce tumor destruction. Autoimmune vitiligo was observed in mice cured of their disease. These findings illustrate that adoptive transfer of T cells and IL-2 can augment the function of a cancer vaccine. Furthermore, these data represent the first demonstration of complete cures of large, established, poorly immunogenic, unmanipulated solid tumors using T cells specific for a true self/tumor antigen and form the basis for a new approach to the treatment of patients with cancer.

Published

2003

24. Enhanced T-cell activation and differentiation in lymphocytes from transgenic mice expressing ubiquitination-resistant 2KR LAT molecules

Author

Connie L. Sommers, S L Epstein, Nicholas P. Restifo, Ana B. Rodríguez-Peña, Phyllis B. Silver, Robert L. Kortum, Julio Gomez-Rodriguez, Geoffrey Guittard, Zhiya Yu, Yasmine Belkaid, J A Misplon, Lawrence E. Samelson, Elizabeth A. Wohlfert, Lionel Feigenbaum, Douglas C. Palmer, Lakshmi Balagopalan, Rachel R. Caspi, Instituto Nacional del Cáncer (España), Instituto de Salud Carlos III, and Ministerio de Economía y Competitividad (España)

Subjects

Genetically modified mouse, medicine.medical_treatment, T cell, Transgene, viruses, Receptors, Antigen, T-Cell, Linker for Activation of T cells, Mice, Transgenic, chemical and pharmacologic phenomena, Biology, Lymphocyte Activation, Article, Mice, Genetics, medicine, Animals, Lymphocytes, skin and connective tissue diseases, Molecular Biology, Adaptor Proteins, Signal Transducing, Effector, T-cell receptor, Ubiquitination, Signal transducing adaptor protein, Membrane Proteins, Cell Differentiation, biochemical phenomena, metabolism, and nutrition, Phosphoproteins, Cell biology, Cytokine, medicine.anatomical_structure, Amino Acid Substitution, Immunology, Molecular Medicine, sense organs

Abstract

Linker for activation of T cells (LAT) is critical for the propagation of T-cell signals upon T-cell receptor (TCR) activation. Previous studies demonstrated that substitution of LAT lysines with arginines (2KR LAT) resulted in decreased LAT ubiquitination and elevated T-cell signaling, indicating that LAT ubiquitination is a molecular checkpoint for attenuation of T-cell signaling. To investigate the role of LAT ubiquitination in vivo, we have generated transgenic mice expressing WT and ubiquitin-defective 2KR LAT. On TCR stimulation of T cells from these mice, proximal signaling and cytokine production was elevated in 2KR versus wild-type (WT) LAT mice. Enhanced cytolytic activity as well as T-helper responses were observed on LAT expression, which were further elevated by 2KR LAT expression. Despite greater T-effector function, WT or 2KR LAT expression did not have any effect on clearance of certain pathogens or tumors. Our data support the model that lack of tumor clearance is due to increased differentiation and acquisition of effector phenotype that is associated with suboptimal immunity in an immunotherapy model. Thus, our data further reinforce the role of LAT ubiquitination in TCR signaling and uncovers a novel role for LAT in driving T-cell differentiation., This research was supported by the Intramural Research Program of the National Institutes of Health, National Cancer Institute, Center for Cancer Research. Ana B Rodríguez-Peña was additionally supported by Fondo de Investigaciones Sanitarias, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad, Spain.

Published

2015

25. Type I cytokines synergize with oncogene inhibition to induce tumor growth arrest

Author

Marcus Bosenberg, Zulmarie Franco, Rahul Roychoudhuri, Liqiang Xi, Gautam U. Mehta, Hui Liu, Nicolas Acquavella, David Clever, Joseph G. Crompton, David F. Stroncek, Douglas C. Palmer, Mark Raffeld, James J. Morrow, Ena Wang, Christopher A. Klebanoff, Luca Gattinoni, Ken-ichi Hanada, Chyi-Chia Richard Lee, Alena Gros, Yun Ji, Zhiya Yu, Holger Pflicke, Melody E. Roelke-Parker, Madhusudhanan Sukumar, Ian S. Goldlust, Francesco M. Marincola, and Nicholas P. Restifo

Subjects

Proto-Oncogene Proteins B-raf, Cancer Research, Adoptive cell transfer, Indoles, medicine.medical_treatment, Immunology, Mice, Transgenic, Biology, CD8-Positive T-Lymphocytes, Immunotherapy, Adoptive, Mice, Immune system, Cell Line, Tumor, medicine, Animals, Humans, Neoplasm Metastasis, Vemurafenib, Melanoma, Sulfonamides, Oncogene, Immunotherapy, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Mutation, Disease Progression, Cytokines, Tumor necrosis factor alpha, Female, V600E, medicine.drug, Signal Transduction

Abstract

Both targeted inhibition of oncogenic driver mutations and immune-based therapies show efficacy in treatment of patients with metastatic cancer, but responses can be either short lived or incompletely effective. Oncogene inhibition can augment the efficacy of immune-based therapy, but mechanisms by which these two interventions might cooperate are incompletely resolved. Using a novel transplantable BRAFV600E-mutant murine melanoma model (SB-3123), we explored potential mechanisms of synergy between the selective BRAFV600E inhibitor vemurafenib and adoptive cell transfer (ACT)–based immunotherapy. We found that vemurafenib cooperated with ACT to delay melanoma progression without significantly affecting tumor infiltration or effector function of endogenous or adoptively transferred CD8+ T cells, as previously observed. Instead, we found that the T-cell cytokines IFNγ and TNFα synergized with vemurafenib to induce cell-cycle arrest of tumor cells in vitro. This combinatorial effect was recapitulated in human melanoma–derived cell lines and was restricted to cancers bearing a BRAFV600E mutation. Molecular profiling of treated SB-3123 indicated that the provision of vemurafenib promoted the sensitization of SB-3123 to the antiproliferative effects of T-cell effector cytokines. The unexpected finding that immune cytokines synergize with oncogene inhibitors to induce growth arrest has major implications for understanding cancer biology at the intersection of oncogenic and immune signaling and provides a basis for design of combinatorial therapeutic approaches for patients with metastatic cancer. Cancer Immunol Res; 3(1); 37–47. ©2014 AACR. See related commentary by Riddell, p. 23

Published

2014

26. MicroRNA-155 is required for effector CD8+ T cell responses to virus infection and cancer

Author

Rachel Perret, Dietmar Zehn, Luca Gattinoni, Caroline Boudousquié, Pedro Romero, Yun Ji, Daniel T. Utzschneider, Thelma M. Escobar, Douglas C. Palmer, Bruno Salaun, Gwennaëlle C. Monnot, Alena Donda, Jan C. Dudda, Nicholas P. Restifo, Estelle Merck, Stefan A. Muljo, Michael Hebeisen, Werner Held, and Nathalie Rufer

Subjects

Cytotoxicity, Immunologic, Adoptive cell transfer, medicine.medical_treatment, Immunology, Melanoma, Experimental, Apoptosis, Mice, Transgenic, Suppressor of Cytokine Signaling Proteins, Biology, CD8-Positive T-Lymphocytes, Lymphocytic Choriomeningitis, Virus Replication, Virus, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Suppressor of Cytokine Signaling 1 Protein, medicine, Immunology and Allergy, Cytotoxic T cell, Gene silencing, Animals, Humans, Lymphocytic choriomeningitis virus, RNA, Small Interfering, B cell, Cells, Cultured, 030304 developmental biology, Cell Proliferation, 0303 health sciences, Mice, Inbred BALB C, Effector, Adoptive Transfer, 3. Good health, Mice, Inbred C57BL, MicroRNAs, Infectious Diseases, Cytokine, medicine.anatomical_structure, Cancer research, Cytokines, STAT6 Transcription Factor, 030215 immunology

Abstract

Summary MicroRNAs (miRNAs) regulate the function of several immune cells, but their role in promoting CD8 + T cell immunity remains unknown. Here we report that miRNA-155 is required for CD8 + T cell responses to both virus and cancer. In the absence of miRNA-155, accumulation of effector CD8 + T cells was severely reduced during acute and chronic viral infections and control of virus replication was impaired. Similarly, Mir155 −/− CD8 + T cells were ineffective at controlling tumor growth, whereas miRNA-155 overexpression enhanced the antitumor response. miRNA-155 deficiency resulted in accumulation of suppressor of cytokine signaling-1 (SOCS-1) causing defective cytokine signaling through STAT5. Consistently, enforced expression of SOCS-1 in CD8 + T cells phenocopied the miRNA-155 deficiency, whereas SOCS-1 silencing augmented tumor destruction. These findings identify miRNA-155 and its target SOCS-1 as key regulators of effector CD8 + T cells that can be modulated to potentiate immunotherapies for infectious diseases and cancer.

Published

2013

27. Oxygen Sensing by T Cells Establishes an Immunologically Tolerant Metastatic Niche

Author

Jenny H. Pan, Zhiya Yu, Anthony T. Phan, Heather D. Hickman, Madhusudhanan Sukumar, David Clever, Nicholas P. Restifo, Michael H. Askenase, Yasmine Belkaid, Luca Gattinoni, Douglas C. Palmer, Robert L. Eil, Christopher A. Klebanoff, Ananda W. Goldrath, Michael G. Constantinides, Rahul Roychoudhuri, and John Goulding

Subjects

0301 basic medicine, Adoptive cell transfer, Effector, Biology, medicine.disease, General Biochemistry, Genetics and Molecular Biology, 3. Good health, Metastasis, 03 medical and health sciences, 030104 developmental biology, Immune system, Circulating tumor cell, Antigen, hemic and lymphatic diseases, Immunology, Cancer cell, medicine, CD8

Abstract

Summary Cancer cells must evade immune responses at distant sites to establish metastases. The lung is a frequent site for metastasis. We hypothesized that lung-specific immunoregulatory mechanisms create an immunologically permissive environment for tumor colonization. We found that T-cell-intrinsic expression of the oxygen-sensing prolyl-hydroxylase (PHD) proteins is required to maintain local tolerance against innocuous antigens in the lung but powerfully licenses colonization by circulating tumor cells. PHD proteins limit pulmonary type helper (Th)-1 responses, promote CD4 + -regulatory T (T reg ) cell induction, and restrain CD8 + T cell effector function. Tumor colonization is accompanied by PHD-protein-dependent induction of pulmonary T reg cells and suppression of IFN-γ-dependent tumor clearance. T-cell-intrinsic deletion or pharmacological inhibition of PHD proteins limits tumor colonization of the lung and improves the efficacy of adoptive cell transfer immunotherapy. Collectively, PHD proteins function in T cells to coordinate distinct immunoregulatory programs within the lung that are permissive to cancer metastasis. PaperClip

Published

2016

28. Th17 cells are long-lived and retain a stem cell-like molecular signature

Author

Sid P. Kerkar, Zachary A. Borman, Douglas C. Palmer, Gabriela A. Ferreyra, Wei Shen, Steven J. Kern, Yun Ji, Luis Sanchez-Perez, Zhiya Yu, Pawel Muranski, Chi-Chao Chan, Christopher A. Klebanoff, Nicholas P. Restifo, Madhusudhanan Sukumar, Luca Gattinoni, Paul A. Antony, Scott K. Durum, Robert L. Danner, Lionel Feigenbaum, Arian Laurence, Robert Reger, and Rahul Roychoudhuri

Subjects

Cell Survival, Cellular differentiation, Immunology, Stem cell theory of aging, Mice, Transgenic, Biology, Article, Mice, NK-92, Cancer stem cell, T-Lymphocyte Subsets, Neoplasms, Immunology and Allergy, Animals, Induced stem cells, Gene Expression Profiling, Stem Cells, Interleukin-17, Cell Differentiation, Th1 Cells, Cell biology, Tumor Necrosis Factor Receptor Superfamily, Member 7, Endothelial stem cell, Infectious Diseases, Th17 Cells, Stem cell, Adult stem cell

Abstract

SummaryTh17 cells have been described as short lived, but this view is at odds with their capacity to trigger protracted damage to normal and transformed tissues. We report that Th17 cells, despite displaying low expression of CD27 and other phenotypic markers of terminal differentiation, efficiently eradicated tumors and caused autoimmunity, were long lived, and maintained a core molecular signature resembling early memory CD8+ cells with stem cell-like properties. In addition, we found that Th17 cells had high expression of Tcf7, a direct target of the Wnt and β-catenin signaling axis, and accumulated β-catenin, a feature observed in stem cells. In vivo, Th17 cells gave rise to Th1-like effector cell progeny and also self-renewed and persisted as IL-17A-secreting cells. Multipotency was required for Th17 cell-mediated tumor eradication because effector cells deficient in IFN-γ or IL-17A had impaired activity. Thus, Th17 cells are not always short lived and are a less-differentiated subset capable of superior persistence and functionality.

Published

2011

29. Human effector CD8+ T cells derived from naive rather than memory subsets possess superior traits for adoptive immunotherapy

Author

Sid P. Kerkar, Shicheng Yang, Christopher A. Klebanoff, Luca Gattinoni, Christopher D. Scott, Richard A. Morgan, Nicholas P. Restifo, Zhiya Yu, Pawel Muranski, Steven A. Rosenberg, Paul F. Robbins, Jianping Huang, Laura A. Johnson, Douglas C. Palmer, Christian S. Hinrichs, William R. Burns, and Zachary A. Borman

Subjects

Cell Survival, Cellular differentiation, medicine.medical_treatment, Immunology, Population, Genetic Vectors, Gene Expression, Biology, CD8-Positive T-Lymphocytes, Biochemistry, Immunotherapy, Adoptive, T-Lymphocyte Subsets, Transduction, Genetic, Cell Line, Tumor, medicine, Cytotoxic T cell, Humans, IL-2 receptor, education, Cells, Cultured, Cell Proliferation, education.field_of_study, Cluster of differentiation, Effector, Cell Differentiation, Cell Biology, Hematology, Immunotherapy, Gene Therapy, Telomere, Flow Cytometry, Tumor Necrosis Factor Receptor Superfamily, Member 7, Retroviridae, Cytokines, Immunologic Memory, CD8

Abstract

Cluster of differentiation (CD)8+ T cells exist as naive, central memory, and effector memory subsets, and any of these populations can be genetically engineered into tumor-reactive effector cells for adoptive immunotherapy. However, the optimal subset from which to derive effector CD8+ T cells for patient treatments is controversial and understudied. We investigated human CD8+ T cells and found that naive cells were not only the most abundant subset but also the population most capable of in vitro expansion and T-cell receptor transgene expression. Despite increased expansion, naive-derived cells displayed minimal effector differentiation, a quality associated with greater efficacy after cell infusion. Similarly, the markers of terminal differentiation, killer cell lectin-like receptor G1 and CD57, were expressed at lower levels in cells of naive origin. Finally, naive-derived effector cells expressed higher CD27 and retained longer telomeres, characteristics that suggest greater proliferative potential and that have been linked to greater efficacy in clinical trials. Thus, these data suggest that naive cells resist terminal differentiation, or “exhaustion,” maintain high replicative potential, and therefore may be the superior subset for use in adoptive immunotherapy.

Published

2011

30. Increased intensity lymphodepletion enhances tumor treatment efficacy of adoptively transferred tumor-specific T cells

Author

Douglas C. Palmer, Luca Gattinoni, Claudia Wrzesinski, Steven A. Rosenberg, Zhiya Yu, Pawel Muranski, Nicholas P. Restifo, Andrew Kaiser, and Chrystal M. Paulos

Subjects

Cancer Research, Adoptive cell transfer, medicine.medical_treatment, T-Lymphocytes, Immunology, Mice, Transgenic, Cell Separation, Article, Lymphocyte Depletion, Mice, T-Lymphocyte Subsets, Neoplasms, Immunology and Allergy, Medicine, Cytotoxic T cell, Animals, Pharmacology, Innate immune system, business.industry, Hematopoietic stem cell, Immunotherapy, Total body irradiation, Flow Cytometry, Adoptive Transfer, Transplantation, medicine.anatomical_structure, Cancer research, business, CD8, Whole-Body Irradiation

Abstract

Lymphodepletion before adoptive cell transfer (ACT)-based immunotherapies can enhance anti-tumor responses by augmenting innate immunity, by increasing access to homeostatic cytokines, and by depressing the numbers of regulatory T cells and myeloid-derived suppressor cells. Although it is clear that high-dose total body irradiation given together with hematopoietic stem cell (HSC) transplantation effectively enhances ACT, the relationship between the intensity of lymphodepletion and tumor treatment efficacy has not been systematically studied. Using the pmel-1 mouse model of self/tumor-reactive CD8 T cells, we observed a strong correlation between the intensity of the conditioning regimen and the efficacy of ACT-based treatments using linear regression analysis. This was the case for preparative total body irradiation administered either as a single dose (R=0.97, P

Published

2010

31. Adoptively transferred effector cells derived from naive rather than central memory CD8+ T cells mediate superior antitumor immunity

Author

Nicholas P. Restifo, Lydie Cassard, Douglas C. Palmer, Warren J. Leonard, Steven A. Rosenberg, Steven J. Kern, Zhiya Yu, Pawel Muranski, Christian S. Hinrichs, Robert L. Danner, Zachary A. Borman, Robert Reger, Luca Gattinoni, Yun Ji, Carol Logun, Rosanne Spolski, and Luis Sanchez-Perez

Subjects

Primates, Adoptive cell transfer, Receptors, Antigen, T-Cell, Biology, CD8-Positive T-Lymphocytes, Autoantigens, Immunotherapy, Adoptive, Immunophenotyping, Animals, Genetically Modified, Interleukin 21, Antigen, Neoplasms, Cytotoxic T cell, Animals, Humans, IL-2 receptor, Multidisciplinary, Effector, Neoplasms, Experimental, Biological Sciences, Natural killer T cell, Adoptive Transfer, Cell biology, Survival Rate, Immunology, Immunologic Memory, CD8

Abstract

Effector cells derived from central memory CD8 + T cells were reported to engraft and survive better than those derived from effector memory populations, suggesting that they are superior for use in adoptive immunotherapy studies. However, previous studies did not evaluate the relative efficacy of effector cells derived from naïve T cells. We sought to investigate the efficacy of tumor-specific effector cells derived from naïve or central memory T-cell subsets using transgenic or retrovirally transduced T cells engineered to express a tumor-specific T-cell receptor. We found that naïve, rather than central memory T cells, gave rise to an effector population that mediated superior antitumor immunity upon adoptive transfer. Effector cells developed from naïve T cells lost the expression of CD62L more rapidly than those derived from central memory T cells, but did not acquire the expression of KLRG-1, a marker for terminal differentiation and replicative senescence. Consistent with this KLRG-1 − phenotype, naïve-derived cells were capable of a greater proliferative burst and had enhanced cytokine production after adoptive transfer. These results indicate that insertion of genes that confer antitumor specificity into naïve rather than central memory CD8 + T cells may allow superior efficacy upon adoptive transfer.

Published

2009

32. Viral sequestration of antigen subverts cross presentation to CD8(+) T cells

Author

Christopher C. Norbury, Eric F. Tewalt, Nicholas P. Restifo, Neal D. Heuss, Dale S. Gregerson, Jean M. Grant, Erica L. Granger, and Douglas C. Palmer

Subjects

lcsh:Immunologic diseases. Allergy, viruses, Immunology, Antigen presentation, Antigen-Presenting Cells, Vaccinia virus, CD8-Positive T-Lymphocytes, Virology/Immune Evasion, Major histocompatibility complex, Microbiology, Cell Line, 03 medical and health sciences, Cross-Priming, 0302 clinical medicine, Antigen, Immunology/Immunity to Infections, Virology, Genetics, Animals, Humans, Cytotoxic T cell, Antigen-presenting cell, Antigens, Viral, Molecular Biology, lcsh:QH301-705.5, 030304 developmental biology, Antigen Presentation, 0303 health sciences, biology, Antigen processing, Histocompatibility Antigens Class I, T-cell receptor, Histocompatibility Antigens Class II, Cross-presentation, 3. Good health, lcsh:Biology (General), Immunology/Antigen Processing and Recognition, biology.protein, Parasitology, Virology/Host Antiviral Responses, lcsh:RC581-607, Research Article, 030215 immunology

Abstract

Virus-specific CD8+ T cells (TCD8+) are initially triggered by peptide-MHC Class I complexes on the surface of professional antigen presenting cells (pAPC). Peptide-MHC complexes are produced by two spatially distinct pathways during virus infection. Endogenous antigens synthesized within virus-infected pAPC are presented via the direct-presentation pathway. Many viruses have developed strategies to subvert direct presentation. When direct presentation is blocked, the cross-presentation pathway, in which antigen is transferred from virus-infected cells to uninfected pAPC, is thought to compensate and allow the generation of effector TCD8+. Direct presentation of vaccinia virus (VACV) antigens driven by late promoters does not occur, as an abortive infection of pAPC prevents production of these late antigens. This lack of direct presentation results in a greatly diminished or ablated TCD8+ response to late antigens. We demonstrate that late poxvirus antigens do not enter the cross-presentation pathway, even when identical antigens driven by early promoters access this pathway efficiently. The mechanism mediating this novel means of viral modulation of antigen presentation involves the sequestration of late antigens within virus factories. Early antigens and cellular antigens are cross-presented from virus-infected cells, as are late antigens that are targeted to compartments outside of the virus factories. This virus-mediated blockade specifically targets the cross-presentation pathway, since late antigen that is not cross-presented efficiently enters the MHC Class II presentation pathway. These data are the first to describe an evasion mechanism employed by pathogens to prevent entry into the cross-presentation pathway. In the absence of direct presentation, this evasion mechanism leads to a complete ablation of the TCD8+ response and a potential replicative advantage for the virus. Such mechanisms of viral modulation of antigen presentation must also be taken into account during the rational design of antiviral vaccines., Author Summary Understanding the pathways by which protective immunity is mediated against viral pathogens is essential to allow the design of effective vaccines. No effective vaccine has been designed to activate killer cells of the immune system expressing CD8, although CD8+ T cells are the most effective cells at modulating anti-viral immunity. We have studied the process that activates the CD8+ T cell to better understand how the cells are triggered so future vaccines might readily activate these cells. CD8+ T cells are activated following recognition of small peptides derived from a virus that binds to a cell surface MHC molecule. Many viruses have evolved to prevent the presentation of these peptide-MHC complexes to CD8+ T cells. However, the immune system avoids these viral “evasion” mechanisms by allowing virus-derived peptides to be generated from viral proteins that are taken up by uninfected cells, a process termed “cross presentation”. We have shown that a poxvirus can specifically prevent the presentation of its proteins by uninfected cells, the first demonstration of evasion of cross presentation. This knowledge is vital in the use of certain viral vectors during vaccine design and adds to the numerous ways in which viruses can evade the immune system.

Published

2009

33. Adoptive transfer of allogeneic tumor-specific T cells mediates effective regression of large tumors across major histocompatibility barriers

Author

Claudia Wrzesinski, Chrystal M. Paulos, Steven A. Rosenberg, Nicholas P. Restifo, Lydie Cassard, Chi-Chao Chan, Luca Gattinoni, Douglas C. Palmer, Christian S. Hinrichs, Pawel Muranski, and Andrea Boni

Subjects

Adoptive cell transfer, Immunology, Melanoma, Experimental, Graft vs Host Disease, Mice, Transgenic, Major histocompatibility complex, Biochemistry, Major Histocompatibility Complex, Mice, Lymphocytes, Tumor-Infiltrating, Antigen, Animals, Transplantation, Homologous, Cells, Cultured, Preparative Regimen, Mice, Inbred BALB C, Mice, Inbred C3H, Transplantation, biology, Graft vs Tumor Effect, Remission Induction, Cell Biology, Hematology, T lymphocyte, Total body irradiation, Adoptive Transfer, Tumor Burden, Mice, Inbred C57BL, Allogeneic Lymphocyte, Mice, Inbred DBA, Blood Group Incompatibility, biology.protein, Female, CD8

Abstract

Graft-versus-tumor effects can be achieved after allogeneic bone marrow transplantation in patients with malignancies of the kidney or hematopoietic system but are often accompanied by severe graft-versus-host-disease (GVHD). We sought to maximize graft-versus-tumor while minimizing GVHD using tumor-specific allogeneic effector T cells rather than open-repertoire T cells. We transferred allogeneic CD8+ pmel-1 or CD4+ TRP-1 T cells specific for the melanoma-associated antigens, glycoprotein 100 (gp100) and tyrosinase-related protein-1 (TRP-1), respectively, into B16-melanoma–bearing mice. Mice receiving a preparative regimen of nonmyeloablating (5 Gy) total body irradiation experienced the rapid rejection of tumor-specific allogeneic lymphocytes with no impact on tumor growth. However, when mice were given more intense total body irradiation conditioning regimens combined with autologous bone marrow transplantation, adoptively transferred allogeneic tumor-specific T lymphocytes persisted at detectable levels for several weeks and mediated significant regression of large, vascularized tumors. We found that the risk of GVHD was low when tumor-specific T cells were transferred and significant toxicity was observed only when substantial numbers of open repertoire allogeneic naive T cells were mixed with the tumor-specific lymphocytes. Taken together, these data indicate that the use of tumor-specific allogeneic CD8+ T cells or CD4+ can result in significant antitumor effects in the absence of measurable GVHD.

Published

2008

34. TSCOT+ thymic epithelial cell-mediated sensitive CD4 tolerance by direct presentation

Author

Hyo Sun Shin, Douglas C. Palmer, Deokjae Lee, Graham Anderson, Soo Jung Yang, Mincheol Kim, Marc R. Theoret, Moon Gyo Kim, Eric J. Jenkinson, Seunghyuk Lee, Kee Nyung Lee, Nicholas P. Restifo, Gwanghee Lee, and Sejin Ahn

Subjects

CD4-Positive T-Lymphocytes, Stromal cell, QH301-705.5, Immunology, Antigen-Presenting Cells, Mice, Transgenic, Thymus Gland, Lymphocyte Activation, General Biochemistry, Genetics and Molecular Biology, Immune tolerance, Mice, Antigen, Immune Tolerance, Animals, Cytotoxic T cell, Biology (General), Antigen-presenting cell, CD40, Symporters, General Immunology and Microbiology, biology, General Neuroscience, Cell Differentiation, Epithelial Cells, Dendritic Cells, Molecular biology, Primer, Lac Operon, biology.protein, Stromal Cells, Central tolerance, General Agricultural and Biological Sciences, CD80

Abstract

Although much effort has been directed at dissecting the mechanisms of central tolerance, the role of thymic stromal cells remains elusive. In order to further characterize this event, we developed a mouse model restricting LacZ to thymic stromal cotransporter (TSCOT)-expressing thymic stromal cells (TDLacZ). The thymus of this mouse contains approximately 4,300 TSCOT+ cells, each expressing several thousand molecules of the LacZ antigen. TSCOT+ cells express the cortical marker CDR1, CD40, CD80, CD54, and major histocompatibility complex class II (MHCII). When examining endogenous responses directed against LacZ, we observed significant tolerance. This was evidenced in a diverse T cell repertoire as measured by both a CD4 T cell proliferation assay and an antigen-specific antibody isotype analysis. This tolerance process was at least partially independent of Autoimmune Regulatory Element gene expression. When TDLacZ mice were crossed to a novel CD4 T cell receptor (TCR) transgenic reactive against LacZ (BgII), there was a complete deletion of double-positive thymocytes. Fetal thymic reaggregate culture of CD45- and UEA-depleted thymic stromal cells from TDLacZ and sorted TCR-bearing thymocytes excluded the possibility of cross presentation by thymic dendritic cells and medullary epithelial cells for the deletion. Overall, these results demonstrate that the introduction of a neoantigen into TSCOT-expressing cells can efficiently establish complete tolerance and suggest a possible application for the deletion of antigen-specific T cells by antigen introduction into TSCOT+ cells.

Published

2008

35. Effective tumor treatment targeting a melanoma/melanocyte-associated antigen triggers severe ocular autoimmunity

Author

Luca Gattinoni, Steven E. Finkelstein, Chrystal M. Paulos, Douglas C. Palmer, Steven A. Rosenberg, Christopher A. Klebanoff, Zhiya Yu, Robert N. Fariss, Chi-Chao Chan, Nicholas P. Restifo, Daniel J. Powell, Claudia Wrzesinski, Robert B. Nussenblatt, and Christian S. Hinrichs

Subjects

Adoptive cell transfer, medicine.medical_treatment, Autoimmunity, CD8-Positive T-Lymphocytes, medicine.disease_cause, Eye, Mice, Immune system, Antigen, Cancer immunotherapy, Antigens, Neoplasm, Neoplasms, MHC class I, medicine, Animals, Humans, Receptors, Interferon, Multidisciplinary, biology, Melanoma, Histocompatibility Antigens Class I, Immunotherapy, Biological Sciences, medicine.disease, Up-Regulation, Immunology, biology.protein

Abstract

Nonmutated tissue differentiation antigens expressed by tumors are attractive targets for cancer immunotherapy, but the consequences of a highly effective antitumor immune response on self-tissue have not been fully characterized. We found that the infusion ofex vivoexpanded adoptively transferred melanoma/melanocyte-specific CD8+T cells that mediated robust tumor killing also induced autoimmune destruction of melanocytes in the eye. This severe autoimmunity was associated with the up-regulation of MHC class I molecules in the eye and high levels of IFN-γ derived from both adoptively transferred CD8+T cells and host cells. Furthermore, ocular autoimmunity required the presence of the IFN-γ receptor on target tissues. Data compiled from >200 eyes and tumors in 10 independently performed experiments revealed a highly significant correlation (P< 0.0001) between the efficacy of tumor immunotherapy and the severity of ocular autoimmunity. Administration of high doses of steroids locally mitigated ocular autoimmunity without impairing the antitumor effect. These findings have particular importance for immunotherapies directed against self-antigens and highlight the need for targeting unique tumor antigens not expressed in critical tissues.

Published

2008

36. IL-2 and IL-21 confer opposing differentiation programs to CD8+ T cells for adoptive immunotherapy

Author

Christian S. Hinrichs, Christopher A. Klebanoff, Keith W. Kerstann, Douglas C. Palmer, Nicholas P. Restifo, Luca Gattinoni, Chrystal M. Paulos, Rosanne Spolski, Steven A. Rosenberg, and Warren J. Leonard

Subjects

Interleukin 2, Adoptive cell transfer, Cellular differentiation, Immunology, Eomesodermin, Gene Expression, Mice, Transgenic, Biology, CD8-Positive T-Lymphocytes, Biochemistry, Immunotherapy, Adoptive, Granzymes, Interleukin 21, Mice, T-Lymphocyte Subsets, medicine, Cytotoxic T cell, Animals, IL-2 receptor, Oligonucleotide Array Sequence Analysis, Immunobiology, Interleukin-15, Reverse Transcriptase Polymerase Chain Reaction, Interleukins, Cell Differentiation, Cell Biology, Hematology, Flow Cytometry, Cell biology, Hyaluronan Receptors, Interleukin-2, CD8, medicine.drug

Abstract

IL-2 and IL-21 are closely related cytokines that might have arisen by gene duplication. Both cytokines promote the function of effector CD8+ T cells, but their distinct effects on antigen-driven differentiation of naive CD8+ T cells into effector CD8+ T cells are not clearly understood. We found that antigen-induced expression of Eomesodermin (Eomes) and maturation of naive CD8+ T cells into granzyme B- and CD44-expressing effector CD8+ T cells was enhanced by IL-2, but, unexpectedly, suppressed by IL-21. Furthermore, IL-21 repressed expression of IL-2Ra and inhibited IL-2–mediated acquisition of a cytolytic CD8+ T-cell phenotype. Despite its inhibitory effects, IL-21 did not induce anergy, but instead potently enhanced the capacity of cells to mediate tumor regression upon adoptive transfer. In contrast, IL-2 impaired the subsequent antitumor function of transferred cells. Gene expression studies revealed a distinct IL-21 program that was characterized phenotypically by increased expression of L-selectin and functionally by enhanced antitumor immunity that was not reversed by secondary in vitro stimulation with antigen and IL-2. Thus, the efficacy of CD8+ T cells for adoptive immunotherapy can be influenced by opposing differentiation programs conferred by IL-2 and IL-21, a finding with important implications for the development of cellular cancer therapies.

Published

2008

37. Immunologic ignorance of vascular endothelial cells expressing minor histocompatibility antigen

Author

Yinghua Tian, Daniel S. Engeler, Douglas C. Palmer, Elke Scandella, Burkhard Ludewig, Beatrice Bolinger, Nicholas P. Restifo, Simone Miller, Pierre-Alain Clavien, Philippe Krebs, University of Zurich, and Ludewig, B

Subjects

Adoptive cell transfer, 2403 Immunology, 1303 Biochemistry, Endothelium, Immunology, Antigen presentation, 2720 Hematology, CD11c, 610 Medicine & health, Cell Biology, Hematology, Biology, medicine.disease, Biochemistry, Hemostasis, Thrombosis, and Vascular Biology, Transplant rejection, Transplantation, 1307 Cell Biology, medicine.anatomical_structure, 10022 Division of Surgical Research, medicine, Minor histocompatibility antigen, CD8, 10217 Clinic for Visceral and Transplantation Surgery

Abstract

Endothelial cells (ECs) presenting minor histocompatibility antigen (mhAg) are major target cells for alloreactive effector CD8+ T cells during chronic transplant rejection and graft-versus-host disease (GVHD). The contribution of ECs to T-cell activation, however, is still a controversial issue. In this study, we have assessed the antigen-presenting capacity of ECs in vivo using a transgenic mouse model with beta-galactosidase (β-gal) expression confined to the vascular endothelium (Tie2-LacZ mice). In a GVHD-like setting with adoptive transfer of β-gal–specific T-cell receptor–transgenic T cells, β-gal expression by ECs was not sufficient to either activate or tolerize CD8+ T cells. Likewise, transplantation of fully vascularized heart or liver grafts from Tie2-LacZ mice into nontransgenic recipients did not suffice to activate β-gal–specific CD8+ T cells, indicating that CD8+ T-cell responses against mhAg cannot be initiated by ECs. Moreover, we could show that spontaneous activation of β-gal–specific CD8+ T cells in Tie2-LacZ mice was exclusively dependent on CD11c+ dendritic cells (DCs), demonstrating that mhAgs presented by ECs remain immunologically ignored unless presentation by DCs is granted.

Published

2008

38. T-Cell Receptor Gene Therapy of Established Tumors in a Murine Melanoma Model

Author

Moniek A. de Witte, Cyrille J. Cohen, John B. A. G. Haanen, Ton N. Schumacher, Cary Hsu, Steven A. Rosenberg, Annelies Jorritsma, Douglas C. Palmer, Luca Gattinoni, Richard A. Morgan, John D. Abad, Chrystal M. Paulos, Claudia Wrzensinski, Willem W. Overwijk, and Nicholas P. Restifo

Subjects

Cancer Research, T cell, medicine.medical_treatment, Receptors, Antigen, T-Cell, alpha-beta, Immunology, Genetic Vectors, Melanoma, Experimental, Receptors, Antigen, T-Cell, chemical and pharmacologic phenomena, Mice, Transgenic, Biology, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Transfection, Immunotherapy, Adoptive, Article, Viral vector, Immunophenotyping, Interferon-gamma, Mice, Antigen, Cell Line, Tumor, medicine, Immunology and Allergy, Animals, Lymphocytes, Pharmacology, Membrane Glycoproteins, Melanoma, T-cell receptor, Immunotherapy, T lymphocyte, Genetic Therapy, medicine.disease, Tumor antigen, Coculture Techniques, Mice, Inbred C57BL, medicine.anatomical_structure, Spleen, gp100 Melanoma Antigen

Abstract

Adoptive cell transfer therapy using tumor-infiltrating lymphocytes for patients with metastatic melanoma has demonstrated significant objective response rates. One major limitation of these current therapies is the frequent inability to isolate tumor-reactive lymphocytes for treatment. Genetic engineering of peripheral blood lymphocytes with retroviral vectors encoding tumor antigen-specific T-cell receptors (TCRs) bypasses this restriction. To evaluate the efficacy of TCR gene therapy, a murine treatment model was developed. A retroviral vector was constructed encoding the pmel-1 TCR genes targeting the B16 melanoma antigen, gp100. Transduction of C57BL/6 lymphocytes resulted in efficient pmel-1 TCR expression. Lymphocytes transduced with this retrovirus specifically recognized gp100-pulsed target cells as measured by interferon-gamma secretion assays. Upon transfer into B16 tumor-bearing mice, the genetically engineered lymphocytes significantly slowed tumor development. The effectiveness of tumor treatment was directly correlated with the number of TCR-engineered T cells administered. These results demonstrated that TCR gene therapy targeting a native tumor antigen significantly delayed the growth of established tumors. When C57BL/6 lymphocytes were added to antigen-reactive pmel-1 T cells, a reduction in the ability of pmel-1 T cell to treat B16 melanomas was seen, suggesting that untransduced cells may be deleterious to TCR gene therapy. This model may be a powerful tool for evaluating future TCR gene transfer-based strategies.

Published

2008

39. Toll-like receptors in tumor immunotherapy

Author

Steven A. Rosenberg, Douglas C. Palmer, Lydie Cassard, Christian S. Hinrichs, Andrea Boni, Claudia Wrzesinski, Nicholas P. Restifo, Chrystal M. Paulos, Luca Gattinoni, Zhiya Yu, Pawel Muranski, Andrew Kaiser, Paul A. Antony, and Luis Sanchez-Perez

Subjects

Cancer Research, Adoptive cell transfer, medicine.medical_treatment, T-Lymphocytes, Immunotherapy, Adoptive, Lymphocyte Depletion, Article, Mice, Immune system, Neoplasms, medicine, Animals, Humans, Receptor, Toll-like receptor, Innate immune system, business.industry, Melanoma, Toll-Like Receptors, Immunotherapy, Total body irradiation, medicine.disease, Intestines, Oncology, Immunology, business, Whole-Body Irradiation

Abstract

Lymphodepletion with chemotherapeutic agents or total body irradiation (TBI) before adoptive transfer of tumor-specific T cells is a critical advancement in the treatment of patients with melanoma. More than 50% of patients that are refractory to other treatments experience an objective or curative response with this approach. Emerging data indicate that the key mechanisms underlying how TBI augments the functions of adoptively transferred T cells include (a) the depletion of regulatory T cells (Treg) and myeloid-derived suppressor cells that limit the function and proliferation of adoptively transferred cells; (b) the removal of immune cells that act as “sinks” for homeostatic cytokines, whose levels increase after lymphodepletion; and (c) the activation of the innate immune system via Toll-like receptor 4 signaling, which is engaged by microbial lipopolysaccharide that translocated across the radiation-injured gut. Here, we review these mechanisms and focus on the effect of Toll-like receptor agonists in adoptive immunotherapy. We also discuss alternate regimens to chemotherapy or TBI, which might be used to safely treat patients with advanced disease and promote tumor regression.

Published

2007

40. Sensitization of B16 tumor cells with a CXCR4 antagonist increases the efficacy of immunotherapy for established lung metastases

Author

Chih Hung Lee, Samuel T Hwang, Julia Wang, Douglas C. Palmer, Nicholas P. Restifo, Takashi Kakinuma, and Hong Zhang

Subjects

Cytotoxicity, Immunologic, Cancer Research, Receptors, CXCR4, Lung Neoplasms, Cyclophosphamide, medicine.medical_treatment, Melanoma, Experimental, chemical and pharmacologic phenomena, Apoptosis, Mice, SCID, Article, Mice, Immune system, Antigen, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Humans, B-Lymphocytes, CXCR4 antagonist, business.industry, Melanoma, Antibodies, Monoclonal, Drug Synergism, Immunotherapy, medicine.disease, Chemokine CXCL12, Mice, Inbred C57BL, Oncology, Cancer cell, Immunology, Cancer research, Female, business, Peptides, Chemokines, CXC, CD8, Neoplasm Transplantation, medicine.drug, T-Lymphocytes, Cytotoxic

Abstract

Expression of the chemokine receptor CXCR4 by tumor cells promotes metastasis, possibly by activating prosurvival signals that render cancer cells resistant to immune attack. Inhibition of CXCR4 with a peptide antagonist, T22, blocks metastatic implantation of CXCR4-transduced B16 (CXCR4-luc-B16) melanoma cells in lung, but not the outgrowth of established metastases, raising the question of how T22 can best be used in a clinical setting. Herein, whereas the treatment of CXCR4-luc-B16 cells in vitro with the CXCR4 ligand CXCL12 did not reduce killing induced by cisplatin or cyclophosphamide, CXCL12 markedly reduced Fas-dependent killing by gp100-specific (pmel-1) CD8+ T cells. T22 pretreatment restored sensitivity of CXCR4-luc-B16 cells to pmel-1 killing, even in the presence of CXCL12. Two immune-augmenting regimens were used in combination with T22 to treat experimental lung metastases. First, low-dose cyclophosphamide treatment (100 mg/kg) on day 5 in combination with T22 (days 4–7) yielded a ∼70% reduction of B16 metastatic tumor burden in the lungs compared with cyclophosphamide treatment alone (P < 0.001). Furthermore, whereas anti–CTL antigen 4 (CTLA4) monoclonal antibody (mAb; or T22 treatment) alone had little effect on established B16 metastases, pretreatment with T22 (in combination with anti-CTLA4 mAb) resulted in a 50% reduction in lung tumor burden (P = 0.02). Thus, in vitro, CXCR4 antagonism with T22 renders B16 cells susceptible to killing by antigen-specific T cells. In vivo, T22 synergizes with cyclophosphamide or anti-CTLA4 mAb in the treatment of established lung metastases, suggesting a novel strategy for augmenting the efficacy of immunotherapy. [Mol Cancer Ther 2006;5(10):2592–9]

Published

2006

41. The in vivo expansion rate of properly stimulated transferred CD8+ T cells exceeds that of an aggressively growing mouse tumor

Author

Leroy N. Hwang, Zhiya Yu, Nicholas P. Restifo, and Douglas C. Palmer

Subjects

Interleukin 2, Cancer Research, Adoptive cell transfer, Skin Neoplasms, Lymphocyte, Population, Mice, Transgenic, Biology, CD8-Positive T-Lymphocytes, Ligands, Cancer Vaccines, Immunotherapy, Adoptive, Article, Mice, medicine, Cytotoxic T cell, Animals, education, Melanoma, Cell Proliferation, education.field_of_study, Cell growth, T lymphocyte, Mice, Inbred C57BL, Kinetics, medicine.anatomical_structure, Oncology, Immunology, Cancer research, Interleukin-2, Immunization, CD8, medicine.drug

Abstract

It has been hypothesized that rapidly dividing tumor cells can outpace adoptively transferred antitumor lymphocytes when tumors are large. However, this hypothesis is at odds with clinical observations indicating that bulky tumors can be destroyed by small numbers of adoptively transferred antitumor T cells. We sought to measure the relative growth rates of T cells and tumor cells in a model using transgenic CD8+ T cells specific for the gp10025-33 H-2Db epitope (called pmel-1) to treat large, well-established s.c. B16 melanoma. We tested the effect of the immunization using an altered peptide ligand vaccine alone or in combination with interleukin-2 (IL-2) by analyzing the kinetics of T-cell expansion using direct enumeration. We found that pmel-1 T cells proliferated explosively during a 5-day period following transfer. Calculations from net changes in population suggest that, at the peak of cell division, pmel-1 T cells divide at a rate of 5.3 hours per cell division, which was much faster than B16 tumor cells during optimal growth (24.9 hours per cell division). These results clearly indicate that the notion of a kinetic “race” between the tumor and the lymphocyte is no contest when adoptively transferred cells are stimulated with immunization and IL-2. When appropriately stimulated, tumor-reactive T-cell expansion can far exceed the growth of even an aggressively growing mouse tumor. (Cancer Res 2006; 66(2): 1132-8)

Published

2006

42. Glucocorticoids do not inhibit antitumor activity of activated CD8+ T cells

Author

Christian S. Hinrichs, Douglas C. Palmer, Nicholas P. Restifo, and Steven A. Rosenberg

Subjects

Interleukin 2, Cancer Research, Adoptive cell transfer, T cell, medicine.medical_treatment, Immunology, Melanoma, Experimental, Mice, Transgenic, Pharmacology, CD8-Positive T-Lymphocytes, Immunotherapy, Adoptive, Dexamethasone, Article, Mice, Interferon, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Lymphocyte Count, Cell Proliferation, Membrane Glycoproteins, business.industry, Immunotherapy, Mice, Inbred C57BL, medicine.anatomical_structure, Interleukin-2, Female, business, Glucocorticoid, CD8, Immunosuppressive Agents, Neoplasm Transplantation, Spleen, medicine.drug, gp100 Melanoma Antigen

Abstract

From the National Cancer Institute (NCI), National Institutes of Health (NIH), Bethesda, Maryland. Summary Glucocorticoids are potent immunosuppressive drugs that are generally withheld from cancer patients receiving immunotherapy. We sought to test the hypothesis that glucocorticoids might interfere with the function of cells after adoptive transfer. We gave dexamethasone, a potent synthetic glucocorticoid, to B16 melanoma–bearing mice receiving the adoptive cell transfer (ACT) of pmel-1 T-cell receptor transgenic CD8 + cells. Dexamethasone caused a profound lymphodepletion but, surprisingly, did not alter the antitumor efficacy of ACT-based regimens whether given before, during, or after ACT. Although dexamethasone radically decreased the number of native CD8 + splenocytes in recipient mice, it did not affect the numbers of CD8 + pmel-1 cells derived from ACT in these mice. In vitro proliferation assays revealed acute inhibition of naive pmel-1 CD8 + cells by dexamethasone without significant effect on activated cells. In vitro interferon (IFN)-γ release from activated pmel-1 CD8 + cells showed partial inhibition by dexamethasone, but this effect was relatively minor when compared with the near-complete inhibition of naive cells. Thus, glucocorticoids had a profound inhibitory effect on naive CD8 + T cells but had little impact on the proliferation and function of activated CD8 + pmel-1 T cells. Finally, because glucocorticoids had no effect on tumor regression in this model, it may be possible to use glucocorticoids in some patients receiving ACT-based immunotherapy regimens.

Published

2005

43. CD8+ T cell immunity against a tumor/self-antigen is augmented by CD4 T helper cells and hindered by naturally occurring T regulatory cells

Author

Willem W. Overwijk, Nicholas P. Restifo, Steven A. Rosenberg, Ciriaco A. Piccirillo, Deborah R. Surman, Paul A. Antony, Douglas C. Palmer, Christopher A. Klebanoff, Steven E. Finkelstein, Akgul Akpinarli, Paul J. Speiss, and Chi-Chao Chan

Subjects

CD4-Positive T-Lymphocytes, T cell, Immunology, Melanoma, Experimental, Mice, Transgenic, Biology, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Immunotherapy, Adoptive, T-Lymphocytes, Regulatory, Article, Interleukin 21, Mice, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Homeostasis, IL-2 receptor, Antigen-presenting cell, Cell Proliferation, Mice, Knockout, CD40, Membrane Glycoproteins, Receptors, Interleukin-2, Natural killer T cell, Immunity, Innate, Neoplasm Proteins, Mice, Inbred C57BL, medicine.anatomical_structure, Self Tolerance, Cancer research, Interleukin 12, biology.protein, Interleukin-2, Transplantation Tolerance, Tumor Escape, gp100 Melanoma Antigen

Abstract

CD4+ T cells control the effector function, memory, and maintenance of CD8+ T cells. Paradoxically, we found that absence of CD4+ T cells enhanced adoptive immunotherapy of cancer when using CD8+ T cells directed against a persisting tumor/self-Ag. However, adoptive transfer of CD4+CD25− Th cells (Th cells) with tumor/self-reactive CD8+ T cells and vaccination into CD4+ T cell-deficient hosts induced autoimmunity and regression of established melanoma. Transfer of CD4+ T cells that contained a mixture of Th and CD4+CD25+ T regulatory cells (Treg cells) or Treg cells alone prevented effective adoptive immunotherapy. Maintenance of CD8+ T cell numbers and function was dependent on Th cells that were capable of IL-2 production because therapy failed when Th cells were derived from IL-2−/− mice. These findings reveal that Th cells can help break tolerance to a persisting self-Ag and treat established tumors through an IL-2-dependent mechanism, but requires simultaneous absence of naturally occurring Treg cells to be effective.

Published

2005

44. Sinks, suppressors and antigen presenters: how lymphodepletion enhances T cell-mediated tumor immunotherapy

Author

Christopher A. Klebanoff, Nicholas P. Restifo, Paul A. Antony, Douglas C. Palmer, and Hung T. Khong

Subjects

Adoptive cell transfer, medicine.medical_treatment, T cell, T-Lymphocytes, Immunology, Antigen-Presenting Cells, Biology, Lymphocyte Activation, Immunotherapy, Adoptive, Lymphocyte Depletion, Article, Immune tolerance, Cancer immunotherapy, Neoplasms, medicine, Immune Tolerance, Immunology and Allergy, Animals, Humans, IL-2 receptor, Antigen-presenting cell, Clinical Trials as Topic, Receptors, Interleukin-7, Interleukins, Models, Immunological, Immunotherapy, medicine.anatomical_structure, Treatment Outcome, Cell activation, Interleukin Receptor Common gamma Subunit

Abstract

Lymphodepletion followed by adoptive cell transfer (ACT) of autologous, tumor-reactive T cells boosts antitumor immunotherapeutic activity in mouse and in humans. In the most recent clinical trials, lymphodepletion together with ACT has an objective response rate of 50% in patients with solid metastatic tumors. The mechanisms underlying this recent advance in cancer immunotherapy are beginning to be elucidated and include: the elimination of cellular cytokine ‘sinks’ for homeostatic γC-cytokines, such as interleukin-7 (IL-7), IL-15 and possibly IL-21, which activate and expand tumor-reactive T cells; the impairment of CD4+CD25+ regulatory T (Treg) cells that suppress tumor-reactive T cells; and the induction of tumor apoptosis and necrosis in conjunction with antigen-presenting cell activation. Knowledge of these factors could be exploited therapeutically to improve the in vivo function of adoptively transferred, tumor-reactive T cells for the treatment of cancer.

Published

2005

45. Acquisition of full effector function in vitro paradoxically impairs the in vivo antitumor efficacy of adoptively transferred CD8+ T cells

Author

Luca Gattinoni, Douglas C. Palmer, Zhiya Yu, Steven A. Rosenberg, Marc R. Theoret, Christopher A. Klebanoff, Steven E. Finkelstein, Claudia Wrzesinski, Keith W. Kerstann, and Nicholas P. Restifo

Subjects

Interleukin 2, Cell Survival, medicine.medical_treatment, T cell, Melanoma, Experimental, Receptors, Lymphocyte Homing, Apoptosis, Biology, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Immunotherapy, Adoptive, Interleukin 21, Mice, T-Lymphocyte Subsets, medicine, Cytotoxic T cell, Animals, IL-2 receptor, Antigen-presenting cell, Cellular Senescence, Cell Proliferation, General Medicine, Immunotherapy, medicine.anatomical_structure, Immunology, Cancer research, Commentary, Interleukin-2, CD8, medicine.drug

Abstract

T cell differentiation is a progressive process characterized by phenotypic and functional changes. By transferring tumor-specific CD8+ T cells into tumor-bearing mice at various stages of differentiation, we evaluated their efficacy for adoptive immunotherapy. We found that administration of naive and early effector T cells, in combination with active immunization and IL-2, resulted in the eradication of large, established tumors. Despite enhanced in vitro antitumor properties, more-differentiated effector T cells were less effective for in vivo tumor treatment. Several events may underlie this paradoxical phenomenon: (a) downregulation of lymphoid-homing and costimulatory molecules; (b) inability to produce IL-2 and access homeostatic cytokines; and (c) entry into a proapoptotic and replicative senescent state. While the progressive acquisition of terminal effector properties is characterized by pronounced in vitro tumor killing, in vivo T cell activation, proliferation, and survival are progressively impaired. These findings suggest that the current methodology for selecting T cells for transfer is inadequate and provide new criteria for the generation and the screening of optimal lymphocyte populations for adoptive immunotherapy.

Published

2005

46. Bedside to bench and back again: how animal models are guiding the development of new immunotherapies for cancer

Author

Paul J. Spiess, Leroy N. Hwang, Deborah R. Surman, Steven E. Finkelstein, Paul A. Antony, Claudia Wrzesiniski, David M. Heimann, Steven A. Rosenberg, Zhiya Yu, Christopher A. Klebanoff, Luca Gattinoni, Douglas C. Palmer, Christian S. Hinrichs, and Nicholas P. Restifo

Subjects

Adoptive cell transfer, medicine.medical_treatment, T-Lymphocytes, Immunology, Major histocompatibility complex, Article, Mice, Antigen, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Neoplasm Metastasis, Melanoma, biology, business.industry, T-cell receptor, Cancer, Cell Biology, Immunotherapy, medicine.disease, Adoptive Transfer, Disease Models, Animal, biology.protein, business

Abstract

Immunotherapy using adoptive cell transfer is a promising approach that can result in the regression of bulky, invasive cancer in some patients. However, currently available therapies remain less successful than desired. To study the mechanisms of action and possible improvements in cell-transfer therapies, we use a murine model system with analogous components to the treatment of patients. T cell receptor transgenic CD8+ T cells (pmel-1) specifically recognizing the melanocyte differentiation antigen gp100 are adoptively transferred into lympho-depleted mice bearing large, established, 14-day subcutaneous B16 melanoma (0.5–1 cm in diameter) on the day of treatment. Adoptive cell transfer in combination with interleukin interleukin-2 or interleukin-15 cytokine administration and vaccination using an altered form of the target antigen, gp100, can result in the complete and durable regression of large tumor burdens. Complete responders frequently develop autoimmunity with vitiligo at the former tumor site that often spreads to involve the whole coat. These findings have important implications for the design of immunotherapy trials in humans.

Published

2004

47. Inflammatory mediator production in swine following endotoxin challenge with or without co-administration of dexamethasone

Author

Michael J. Myers, Douglas C. Palmer, Lynn O. Post, and Dorothy E. Farrell

Subjects

Lipopolysaccharides, medicine.medical_specialty, Lipopolysaccharide, medicine.drug_class, Swine, Immunology, Biology, Nitric Oxide, Neopterin, Dexamethasone, Nitric oxide, chemistry.chemical_compound, Internal medicine, medicine, Immunology and Allergy, Animals, Nitrite, Pharmacology, Tumor Necrosis Factor-alpha, Interleukins, Systemic Inflammatory Response Syndrome, Disease Models, Animal, Endocrinology, chemistry, Toxicity, Injections, Intravenous, Corticosteroid, Tumor necrosis factor alpha, Inflammation Mediators, Biomarkers, medicine.drug

Abstract

The inflammatory response in swine challenged with lipopolysaccharide (LPS) has only been partially characterized. As swine are increasingly used in biomedical research, it is important to determine if they respond to endotoxin challenge in a manner similar to other model systems. Accordingly, 24 Poland China x Landrace barrows were treated with saline, LPS, dexamethasone, or LPS and dexamethasone, with six animals in each treatment group. The kinetics of TNFalpha, IL-1beta, IL-6, IL-8, IL-10, nitric oxide (nitrate/nitrite), and neopterin production in swine plasma were examined at 1, 3, 6, 9, and 24 h after acute LPS challenge. Lipopolysaccharide increased plasma TNFalpha levels, which peaked 1 h post-challenge. Dexamethasone decreased LPS-induced TNFalpha by approximately 60%. Plasma IL-6 levels peaked 3 h post-LPS challenge, returning to basal levels by 9 h. Swine given both LPS and dexamethasone had minimal IL-6 levels. Control and dexamethasone-only treated animals never exhibited systemic TNFalpha or IL-6 levels. Lipopolysaccharide increased plasma IL-10 1 h after challenge. Dexamethasone did not alter plasma IL-10 levels in LPS-challenged swine. Interleukin-1beta was constitutively present in plasma and was not altered by any combination of treatments. Plasma IL-8 was not observed in any treatment group. Plasma nitrate/nitrite levels were maximal 24 h post-challenge. Dexamethasone treatment prevented increases in plasma nitrate/nitrite levels in LPS-treated animals. Lipopolysaccharide induced levels of neopterin; dexamethasone served to further increase plasma neopterin levels in LPS-challenged animals. The discordant regulation of inflammatory mediators suggests that the immunological responses by swine to LPS are distinct from the responses seen in rodent and human studies.

Published

2003

48. Cish attenuates proximal TCR-signaling and CD8+ T cell immunity

Author

Nicholas P. Restifo, Douglas C. Palmer, Lawrence E. Samelson, Geoffery Guittard, and Shashank J. Patel

Subjects

Pharmacology, Cancer Research, Tcr signaling, business.industry, Immunology, T-cell receptor, hemic and immune systems, chemical and pharmacologic phenomena, Oncology, Immunity, Poster Presentation, Molecular Medicine, Immunology and Allergy, Cytotoxic T cell, Medicine, business, CISH, CD8

Abstract

Meeting abstracts CD8+ T cells are potent killers of infected cells and tumors, specifically recognizing their targets through the T cell receptor (TCR). While much has been revealed about the activation of TCR signaling, negative regulation of this pathway remains incompletely elucidated. We

Published

2014

49. Identification of the Genomic Insertion Site of Pmel-1 TCR α and β Transgenes by Next-Generation Sequencing

Author

Natalie Abrams, Yun Ji, Wei Zhu, Parthav Jailwala, Zulmarie Franco, Douglas C. Palmer, Rahul Roychoudhuri, Nicholas P. Restifo, Luca Gattinoni, Zhiya Yu, Eric A. Stahlberg, and Eddie Salinas

Subjects

Genetically modified mouse, Receptors, Antigen, T-Cell, alpha-beta, Transgene, Genetic Vectors, Molecular Sequence Data, Immunology, Gene Dosage, lcsh:Medicine, Gene Expression, Mutagenesis (molecular biology technique), Mice, Transgenic, CD8-Positive T-Lymphocytes, Biology, Research and Analysis Methods, Gene dosage, DNA sequencing, law.invention, Mice, Model Organisms, law, Medicine and Health Sciences, Animals, Humans, Transgenes, lcsh:Science, Genotyping, Polymerase chain reaction, Whole genome sequencing, Genetics, Multidisciplinary, Base Sequence, lcsh:R, Chromosome Mapping, High-Throughput Nucleotide Sequencing, Biology and Life Sciences, Computational Biology, Mutagenesis, Insertional, Oncology, Chromosomes, Human, Pair 2, lcsh:Q, gp100 Melanoma Antigen, Research Article

Abstract

The pmel-1 T cell receptor transgenic mouse has been extensively employed as an ideal model system to study the mechanisms of tumor immunology, CD8+ T cell differentiation, autoimmunity and adoptive immunotherapy. The 'zygosity' of the transgene affects the transgene expression levels and may compromise optimal breeding scheme design. However, the integration sites for the pmel-1 mouse have remained uncharacterized. This is also true for many other commonly used transgenic mice created before the modern era of rapid and inexpensive next-generation sequencing. Here, we show that whole genome sequencing can be used to determine the exact pmel-1 genomic integration site, even with relatively 'shallow' (8X) coverage. The results were used to develop a validated polymerase chain reaction-based genotyping assay. For the first time, we provide a quick and convenient polymerase chain reaction method to determine the dosage of pmel-1 transgene for this freely and publically available mouse resource. We also demonstrate that next-generation sequencing provides a feasible approach for mapping foreign DNA integration sites, even when information of the original vector sequences is only partially known.

Published

2014

50. IFN-gamma production by adoptively transferred CD8+ T lymphocytes and host cells contributes to successful tumor immunotherapy

Author

Paul A. Antony, Paul J. Spiess, Nicholas P. Restifo, Christopher A. Klebanoff, Leroy N. Hwang, Douglas C. Palmer, Luca Gattinoni, David M. Heimann, Steven A. Rosenberg, Steven E. Finkelstein, and Christian S. Hinrichs

Subjects

Adoptive cell transfer, business.industry, Melanoma, medicine.medical_treatment, Immunotherapy, Active immunization, medicine.disease, In vitro, Cytokine, In vivo, Immunology, medicine, Cancer research, Surgery, business, CD8

Abstract

Introduction: Adoptively transferred antigen-specific CD8+ T-cells can specifically produce IFN-gamma in response to tumor stimulation. We hypothesized that IFN-gamma production solely by adoptively transferred T-cells was required for anti-tumor efficacy. Methods: A murine model with analogous components to the treatment of patients was established. CD8+ T-cell receptor gp100-specific transgenic mice (Pmel-1) were crossed with IFN-gamma knockout mice (IFN-gamma−/−). Pmel-1 and Pmel-1IFN-gamma−/− cells were analyzed in vitro. In vivo function was assessed by adoptive transfer of Pmel-1 or Pmel-1IFN-gamma−/− cells into wild-type C57BL/6 or IFN-gamma−/− mice bearing large, established subcutaneous B16 melanoma (> 50mm 2 ). Cell transfer was undertaken in combination with active immunization with fowlpox virus encoding human gp100 (rFPVhgp100) plus interleukin-2 (IL-2). Tumor size (rank-sum test) and survival (Kaplan-Meier) were analyzed. Results: Pmel-1IFN-gamma−/− cells did not produce IFN-gamma, in vitro; yet, Pmel-1 and Pmel-1IFN-gamma−/− cells were able to produce GM-CSF, TNF-alpha, MIP-1alpha, and RANTES. Adoptive transfer of Pmel-1+rFPVhgp100+IL-2 led to the regression of large tumor burden in both wild-type and IFN-gamma−/− hosts. Pmel-1IFN-gamma−/− T-lymphocytes were less efficacious in a wild-type host. However, when Pmel-1IFN-gamma−/− cells were employed into IFN-gamma−/− hosts, therapeutic efficacy was abrogated with tumor growth similar to no treatment controls. Conclusions: These data suggest that IFN-gamma is essential for treatment of large, established melanoma, but this cytokine is not necessarily produced solely by adoptively transferred antigen specific T-lymphocytes and may be provided by the host's cells. These findings have important implications for the design of immunotherapy trials in humans.

Published

2004