Your search keyword '"Greiner JW"' showing total 161 results

1. NHS-IL12, a Tumor-Targeting Immunocytokine

Author

Greiner JW, Morillon II YM, and Schlom J

Subjects

interleukin-12, nhs-il12, immunotherapy, cancer, immuno-oncology, review., Immunologic diseases. Allergy, RC581-607

Abstract

John W Greiner, Y Maurice Morillon II, Jeffrey Schlom Laboratory of Tumor Immunology and Biology, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD, USACorrespondence: Jeffrey SchlomLaboratory of Tumor Immunology and Biology, Center for Cancer Research, National Cancer Institute, 10 Center Drive, Room 8B09, Bethesda, MD, 20892, USATel +1 240-858-3463Fax +1 240-541-4558Email schlomj@mail.nih.govAbstract: NHS-IL12 is a novel immunocytokine designed for delivery of IL-12 to the tumor microenvironment (TME). NHS-IL12 consists of two molecules of IL-12 fused to a human IgG1 (NHS76) recognizing DNA/histone complexes, which are often exposed in the necrotic portions of tumors. Preclinical studies demonstrated the tumor-targeting ability and longer plasma half-life for NHS-IL12 when compared with recombinant IL-12 (rIL-12). NHS-IL12 outperformed rIL-12 in enhancing the proliferation and activation of immune as well as antigen-presenting cells, resulting in a more robust primary immune response. NHS-IL12 also reduced the number and function of suppressive myeloid cells (myeloid derived suppressor cells/macrophages) within the TME. In a murine bladder tumor model, NHS-IL12 administration led to a coordinated increase in host immunity with a reduction of immunosuppressive myeloid cells in the TME resulting in substantial reduction in tumor growth. Several preclinical studies have demonstrated increased overall anti-tumor efficacy when NHS-IL12 was combined with either immune-based therapeutics or chemotherapeutic approaches.Keywords: interleukin-12, NHS-IL12, immunotherapy, cancer, immuno-oncology, review

Published

2021

2. Effect of the combined treatment with 5-fluorouracil, gamma-interferon or folinic acid on carcinoembryonic antigen expression in colon cancer cells

Author

Aquino A, Prete SP, Greiner JW, Giuliani A, Graziani G, Turriziani M, Masci G, Bonmassar E, De Vecchis L., DE FILIPPI, ROSARIA, Aquino, A, Prete, Sp, Greiner, Jw, Giuliani, A, Graziani, G, Turriziani, M, DE FILIPPI, Rosaria, Masci, G, Bonmassar, E, and De Vecchis, L.

Subjects

MONOCLONAL-ANTIBODY, Blotting, Western, Transplantation, Heterologous, Leucovorin, VACCINE, CARCINOMA-CELLS, LINES, NUCLEAR-RNA, COLORECTAL-CANCER, Interferon-gamma, Mice, Animals, Humans, RNA, Messenger, Mice, Inbred BALB C, Histocompatibility Antigens Class I, Settore BIO/14, HUMAN RECOMBINANT INTERFERONS, MESSENGER-RNA, IN-VITRO, GENE, Carcinoembryonic Antigen, Colonic Neoplasms, B7-1 Antigen, Female, Fluorouracil, HT29 Cells, Neoplasm Transplantation

Abstract

5-Fluorouracil (5-FU) and human recombinant gamma-interferon (gamma-IFN) were found to increase the expression of carcinoembryonic antigen (CEA) in human cancer cells in vitro. In the present study, the antimetabolite was associated with gamma-IFN or folinic acid (FA), a biochemical modulator of cellular metabolism of 5-FU, able to increase its antineoplastic activity. Treatment of two human colon cancer cell lines (HT-29 and WiDr) with 5-FU + gamma-IFN resulted in an increase of CEA expression higher than that obtainable with both agents alone, although no synergistic effects were obtained. This was demonstrated in terms of: (a) mRNA transcripts (HT-29); (b) cytoplasm and membrane CEA protein levels detected by Western blot analysis (HT-29); and (c) plasma membrane reactivity determined by flow cytometry analysis (HT-29 and WiDr). Moreover, 5-FU + gamma-IFN increased HLA class I molecules in the HT-29 cell membrane over that obtainable with gamma-IFN alone. In contrast, both agents did not induce the expression of the costimulatory molecule B7-1. Treatment with FA enhanced the antitumor effect of 5-FU but not its ability to augment CEA expression. This suggests that the FA-sensitive biochemical mechanism of action of 5-FU is not involved in its effect on CEA expression. In vivo studies showed, for the first time, that 5-FU, alone or combined with gamma-IFN, increases the amount of CEA protein over controls, either in cancer cells or in peripheral blood of nude mice bearing HT-29 cells. These results could be of potential diagnostic and/or therapeutic value when CEA protein is the target of humoral or cell-mediated immunity.

Published

1998

3. 85. Molecular and biological characteristics of a potentially novel human gastric tumor antigen

Author

Shimada, S, primary, Schlom, J, additional, Ogawa, M, additional, and Greiner, JW, additional

Published

1992

4. 153. Improved antinimor efficacy of a radiolabeled monoclonal antibody when combined with interferon-gamma

Author

Greiner, JW, primary, Nieroda, C, additional, Dansky-Ullmann, C, additional, and Schlom, J, additional

Published

1992

5. Physical activity and cancer prevention: pathways and targets for intervention.

Author

Rogers CJ, Colbert LH, Greiner JW, Perkins SN, and Hursting SD

Abstract

The prevalence of obesity, an established epidemiological risk factor for many cancers, has risen steadily for the past several decades in the US and many other countries. Particularly alarming are the increasing rates of obesity among children, portending continuing increases in the rates of obesity and obesity-related cancers for many years to come. Modulation of energy balance, via increased physical activity, has been shown in numerous comprehensive epidemiological reviews to reduce cancer risk. Unfortunately, the effects and mechanistic targets of physical activity interventions on the carcinogenesis process have not been thoroughly characterized. Studies to date suggest that exercise can exert its cancer-preventive effects at many stages during the process of carcinogenesis, including both tumour initiation and progression. As discussed in this review, exercise may be altering tumour initiation events by modifying carcinogen activation, specifically by enhancing the cytochrome P450 system and by enhancing selective enzymes in the carcinogen detoxification pathway, including, but not limited to, glutathione-S-transferases. Furthermore, exercise may reduce oxidative damage by increasing a variety of anti-oxidant enzymes, enhancing DNA repair systems and improving intracellular protein repair systems. In addition to altering processes related to tumour initiation, exercise may also exert a cancer-preventive effect by dampening the processes involved in the promotion and progression stages of carcinogenesis, including scavenging reactive oxygen species (ROS); altering cell proliferation, apoptosis and differentiation; decreasing inflammation; enhancing immune function; and suppressing angiogenesis. A paucity of data exists as to whether exercise may be working as an anti-promotion strategy via altering ROS in initiated or preneoplastic models; therefore, no conclusions can be made about this possible mechanism. The studies directly examining cell proliferation and apoptosis have shown that exercise can enhance both processes, which is difficult to interpret in the context of carcinogenesis. Studies examining the relationship between exercise and chronic inflammation suggest that exercise may reduce pro-inflammatory mediators and reduce the state of low-grade, chronic inflammation. Additionally, exercise has been shown to enhance components of the innate immune response (i.e. macrophage and natural killer cell function). Finally, only a limited number of studies have explored the relationship between exercise and angiogenesis; therefore, no conclusions can be made currently about the role of exercise in the angiogenesis process as it relates to tumour progression. In summary, exercise can alter biological processes that contribute to both anti-initiation and anti-progression events in the carcinogenesis process. However, more sophisticated, detailed studies are needed to examine each of the potential mechanisms contributing to an exercise-induced decrease in carcinogenesis in order to determine the minimum dose, duration and frequency of exercise needed to yield significant cancer-preventive effects, and whether exercise can be used prescriptively to reverse the obesity-induced physiological changes that increase cancer risk. [ABSTRACT FROM AUTHOR]

Published

2008

6. 85. Molecular and biological characteristics of a potentially novel human gastric tumor antigen

Author

Greiner Jw, J Schlom, Shinya Shimada, and M Ogawa

Subjects

Pharmacology, Antigen, business.industry, Cancer research, Medicine, Gastric tumor, General Medicine, business

Published

1992

7. IgEs targeted on tumor cells: therapeutic activity and potential in the design of tumor vaccines

Author

Reali, E., Greiner, J. W., Corti, A., Gould, H. J., Bottazzoli, F., Giovanni Paganelli, Schlom, J., Siccardi, A. G., Reali, E, Greiner, Jw, Corti, Angelo, Gould, Hj, Bottazzoli, F, Paganelli, G, Schlom, J, and Siccardi, Ag

Subjects

CD4-Positive T-Lymphocytes, Antibodies, Monoclonal, Neoplasms, Experimental, CD8-Positive T-Lymphocytes, Immunoglobulin E, Cancer Vaccines, Survival Analysis, Eosinophils, Mice, Inbred C57BL, Mice, Tumor Cells, Cultured, Animals, Female, Interleukin-5, Cell Division, Neoplasm Transplantation, T-Lymphocytes, Cytotoxic

Abstract

Surface-bound IgE play a central role in antiparasite immunity; to exploit IgE-driven immune mechanisms in tumor prevention and control, monoclonal IgEs of irrelevant specificity were loaded through biotin-avidin bridging onto tumor cells, either by systemic administration to tumor-bearing mice or pre-loading of tumor cells before inoculation. Here we show that systemic administration of biotinylated IgEs to mice bearing tumors pre-targeted with biotinylated antibodies and avidin significantly decreased tumor growth rate. In addition, as compared with IgC-loaded control cells, inoculation of suboptimal doses of IgE-loaded tumor cells suppressed tumor formation in a fraction of animals and induced protective host immunity by eliciting tumor-specific T-cell responses, Similarly, tumor vaccination experiments showed that irradiated tumor cells (IgE loaded by biotin-avidin bridging) conferred protective immunity at doses 100-fold lower than the corresponding control cells without IgE, Finally, in vivo depletion of eosinophils or T cells abrogated IgE-driven tumor growth inhibition. These results demonstrate that IgEs targeted on tumor cells not only possess a curative potential but also confer long-term antitumor immunity and that IgE-driven antitumor activity is not restricted to the activation of innate immunity effector mechanisms but also results from eosinophil-dependent priming of a T-cell-mediated adaptive immune response. This suggests a potential role for IgEs in the design of new cell-based tumor vaccines.

Published

2001

8. Macrophage colony-stimulating factor enhancement of antibody-dependent cellular cytotoxicity against human colon carcinoma cells

Author

Pierpaolo Correale, Kwong Y. Tsang, J W Greiner, Chen-Feng Qi, J. Schlom, C. Nieroda, R. De Filippi, Qi, Cf, Nieroda, C, DE FILIPPI, Rosaria, Greiner, Jw, Correale, P, Schlom, J, and Tsang, Ky

Subjects

Macrophage colony-stimulating factor, medicine.drug_class, medicine.medical_treatment, Immunology, Dose-Response Relationship, Immunologic, chemical and pharmacologic phenomena, Monoclonal antibody, Lymphocyte Depletion, Monocytes, Cancer immunotherapy, Adjuvants, Immunologic, medicine, Tumor Cells, Cultured, Immunology and Allergy, Macrophage, Humans, Neutralizing antibody, Cytotoxicity, Antibody-dependent cell-mediated cytotoxicity, biology, Chemistry, CD11 Antigens, Monocyte, Macrophage Colony-Stimulating Factor, Carcinoma, Antibody-Dependent Cell Cytotoxicity, Antibodies, Monoclonal, Molecular biology, CD56 Antigen, Recombinant Proteins, medicine.anatomical_structure, Colonic Neoplasms, biology.protein, Interleukin-4

Abstract

Antibody-dependent cellular cytotoxicity (ADCC) has been suggested to be an important defense mechanism against tumors. The effects of recombinant human macrophage colony-stimulating factor (rhM-CSF) on ADCC activity of human monocytes were investigated. Human peripheral monocytes were pre-incubated for 72 h with rhM-CSF at various concentrations (50, 100, 200, 400 U/ml) and then used as effector cells in a 24-h 111-Indium release assay. Human carcinoma cell lines LS-174T, CBS, and KLE were used as targets to react with anti-carcinoma monoclonal antibodies (mAbs: murine D612, murine CC49, and chimeric CC49). A significant increase in ADCC activity was observed after monocytes were incubated in 100-400 U/ml of human rhM-CSF. Variation in ADCC activity of monocytes among donors was observed. The enhancement of ADCC activity was blocked by the addition of a neutralizing antibody to rhM-CSF. Less D612 mAb was required for the rhM-CSF-treated monocytes to mediate an equivalent level of ADCC activity as compared to the untreated monocytes. Because of the low levels of rhM-CSF required in these studies to enhance ADCC, treatment of monocytes alone with comparable levels of rhM-CSF did not enhance antibody-independent cytotoxicity. Moreover, it is demonstrated here that recombinant human interleukin-4 (rhIL-4) and rhM-CSF can have a synergistic effect of monocyte-mediated ADCC on human tumor cells. These results thus indicate that rhM-CSF augments ADCC of human peripheral blood monocytes using mAbs to human carcinomas, suggesting a potential role for rhM-CSF in cancer immunotherapy.

Published

1995

9. Differential effects of recombinant interferon-alpha and 5-fluorouracil against colon cancer cells or against peripheral blood mononuclear cells

Author

Rosaria DE FILIPPI, Prete, S. P., Giuliani, A., Silvi, E., Yamaue, H., Nieroda, C. A., Greiner, J. W., Vecchis, L., Bonmassar, E., DE FILIPPI, Rosaria, Prete, Sp, Giuliani, A, Silvi, E, Yamaue, H, Nieroda, Ca, Greiner, Jw, De Vecchis, L, and Bonmassar, E.

Subjects

Cytotoxicity, Immunologic, Immunity, Cellular, Drug Synergism, Lymphocyte Activation, Recombinant Proteins, Stimulation, Chemical, Antineoplastic Combined Chemotherapy Protocols, Colonic Neoplasms, Interferon Type I, Leukocytes, Mononuclear, Tumor Cells, Cultured, Humans, Fluorouracil, Phytohemagglutinins, Cell Division

Abstract

Comparative studies on the suppressive effects of recombinant interferon-alpha (IFN-alpha), 5-fluorouracil (5-FU), or IFN-alpha + 5-FU have been performed in vitro on colon carcinoma cells (HT-29 cell line) and PHA-stimulated mononuclear cells (MNC) of peripheral blood obtained from healthy donors. IFN-alpha was used at 500 U/ml against HT-29 cells and at 1000 U/ml against MNC on day 1 of culture; 5-FU was used at 250 microM against HT-29 and at 1400 microM against MNC on day 2 of culture. The results show that: (a) IFN-alpha inhibited MNC and HT-29 cells by 13.4% and 32.9%, respectively; (b) 5-FU inhibited MNC and HT-29 cells by 54.7% and 87.0%, respectively; (c) IFN-alpha + 5-FU resulted in a stronger inhibition of HT-29 cells (i.e., 96.1%). In contrast, that combination was significantly less suppressive than 5-FU alone when MNC were used as targets (i.e., 35.9% inhibition). Natural cell-mediated cytotoxic activity relative to 10(6) MNC was not markedly altered by all agents alone or in combination. Moreover, treatment with IFN-alpha, 5-FU or IFN-alpha + 5-FU resulted in a marked increase in the number of HT-29 cells positive for the CEA surface antigen. These data seem to provide further rational support of the clinical use of IFN-alpha + 5-FU in colorectal cancer, based on the differential toxicity of this drug combination on tumor versus normal immunocompetent cells.

Published

1994

10. Transfer of the IL-6 gene into a human colorectal carcinoma cell line and consequent enhancement of tumor antigen expression

Author

Jeffrey Schlom, F. J. Primus, Rosaria De Filippi, Syed V. S. Kashmiri, Chen F. Qi, Carol Nieroda, Kwong Y. Tsang, John W. Greiner, Benjamin Calvo, Tsang, Ky, Kashmiri, Sv, Qi, Cf, Nieroda, C, Calvo, B, DE FILIPPI, Rosaria, Greiner, Jw, Primus, Fj, and Schlom, J.

Subjects

medicine.medical_treatment, Immunology, Human leukocyte antigen, Transfection, Carcinoembryonic antigen, Antigen, Antigens, Neoplasm, HLA Antigens, medicine, Tumor Cells, Cultured, Immunology and Allergy, Humans, Receptors, Immunologic, Expression vector, biology, Interleukin-6, Carcinoma, Immunotherapy, DNA, Flow Cytometry, Intercellular Adhesion Molecule-1, Receptors, Interleukin-6, Tumor antigen, Carcinoembryonic Antigen, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, Genes, Cell culture, Liposomes, biology.protein, Cancer research, Colorectal Neoplasms, Cell Adhesion Molecules

Abstract

cDNA encoding the human IL gene (580 bp), inserted into a retroviral expression vector carrying neomycin resistance selective marker, was introduced into HT-29 human colon carcinoma cells by lipofection. Interleukin-6 activity was measured by ELISA and bioassay using B9 cells. Interleukin-6 secreted by transfected HT-29 cells was shown to be biologically active. The expression of the human tumor associated antigen CEA (carcinoembryonic antigen), HLA classes I and II, and ICAM-1 antigens in the transfected HT-29 cells were also analyzed by flow cytometry. Significant enhancement in the expression of CEA but not in the expression of HLA class I, HLA class II and ICAM-1 antigens, was observed in the transfected HT-29 cells as compared to the parental HT-29 cells. These results provide experimental evidence that enhancement of tumor antigen expression on tumor cells can be induced by IL-6 gene transfection, and suggest another potential role for the use of IL-6 gene transfer in the immunotherapy of human cancers.

Published

1993

11. A human T cell line engineered to secrete chimeric monoclonal antibody

Author

Syed V. S. Kashmiri, Chen-Feng Qi, R. De Filippi, J. Schlom, Benjamin Calvo, Liming Shu, John W. Greiner, Kwong Y. Tsang, C. A. Nieroda, Tsang, Ky, Kashmiri, Sv, DE FILIPPI, Rosaria, Qi, Cf, Calvo, B, Shu, L, Nieroda, Ca, Greiner, Jw, and Schlom, J.

Subjects

Cytotoxicity, Immunologic, Cancer Research, medicine.drug_class, T cell, medicine.medical_treatment, T-Lymphocytes, Immunology, Blotting, Western, Immunoglobulins, Biology, Monoclonal antibody, Transfection, Binding, Competitive, Cell Line, Immunophenotyping, medicine, Tumor Cells, Cultured, Immunology and Allergy, Humans, Pharmacology, Antibody-dependent cell-mediated cytotoxicity, Models, Genetic, Tumor-infiltrating lymphocytes, Antibodies, Monoclonal, Immunotherapy, Molecular biology, Chimeric antigen receptor, medicine.anatomical_structure, biology.protein, Antibody, Colorectal Neoplasms, Genetic Engineering

Abstract

Both monoclonal antibodies (MAbs) and human T cells have been used in human tumor immunotherapy protocols. Tumor-infiltrating lymphocytes (TILs) and MAbs that can mediate antibody-dependent cell-mediated cytotoxicity (ADCC) via human effector cells have shown antitumor effects in both animal models and clinical trials. One potential novel approach would be to combine these two modalities in the creation of a T cell capable of secreting antitumor immunoglobulins (Ig), in essence, creating an antitumor Ig "factory" at the tumor site. In the studies reported here, we have cloned the D612 MAb Ig genes and generated a chimeric D612 IgG1 containing the murine variable region and human constant region. D612 MAb has been shown to mediate lysis of human colon carcinomas via effector cell-mediated ADCC. We have demonstrated that following transfection, chimeric D612 can be expressed and secreted by the human T-cell line MOLT-4 at a rate of 0.25 micrograms/ml per 10(6) cells in 72 hours. The secreted Ig retained its antigen-binding properties as assayed by competition radioimmunoassay and also its ability to mediate ADCC against human tumor cells. To our knowledge, this is the first demonstration of the production of a chimeric IgG by human T cells and opens the possibility of a therapeutic approach in which TILs secrete humanized antitumor MAb capable of mediating ADCC at the tumor site.

Published

1993

12. Drug-induced changes of carcinoembryonic antigen expression in human cancer cells: Effect of 5-fluorouracil

Author

Prete, S. P., Aquino, A., Masci, G., Orlando, L., Giuliani, A., Santis, S., Vecchis, L., Filippi, R., Greiner, J. W., Bonmassar, E., GRAZIA GRAZIANI, Prete, Sp, Aquino, A, Masci, G, Orlando, L, Giuliani, A, De Santis, S, De Vecchis, L, DE FILIPPI, Rosaria, Greiner, Jw, Bonmassar, E, and Graziani, G.

Subjects

Messenger, antineoplastic activity, colon carcinoma, cancer cell culture, cancer chemotherapy, Tumor Cells, Cultured, cell growth, Humans, controlled study, dactinomycin, human, RNA, Messenger, antineoplastic agent, Neoplastic, cancer immunotherapy, Cultured, human cell, drug effect, article, genetic transcription, Settore BIO/14, interferon, Flow Cytometry, Tumor Cells, Carcinoembryonic Antigen, carcinoembryonic antibody, Gene Expression Regulation, Neoplastic, priority journal, Gene Expression Regulation, monoclonal antibody, concentration response, RNA, antigen expression, Fluorouracil, carcinoembryonic antigen, fluorouracil

Abstract

Previous studies showed that 5-fluorouracil (5-FU) is capable of enhancing the membrane reactivity of the human colon carcinoma cell line HT-29 with a monoclonal antibody (COL-1) directed against carcinoembryonic antigen (CEA). In the present study, we show that short-term exposure (i.e., 1 hr) of cancer cells to 5-FU mediates a marked increase of CEA expression, that is concentration-dependent and lasts up to day 5 after treatment. This phenomenon is the result of the drug-mediated enhancement of the CEA expression, but not of the selection of the CEA-positive cells operated by the antimetabolite. This is supported by the finding that the increase of the CEA expression detected by cytofluorimetric analysis is observed not only in the parental HT-29 line, but also in its C22.20 subclone, endowed with a low basal level of CEA and with chemosensitivity to 5-FU lower than that of the parental cell line. Moreover, increase of CEA expression occurs not only in the plasma membrane, but also in the cytosolic cellular compartment, as indicated by the results of Western blot analysis. Northern blot analysis of total RNA extracted from 5-FU-treated HT-29 or C22.20 cells shows an increase in the steady-state levels of CEA and CEA-related transcripts (e.g., biliary glycoprotein). Moreover 5-FU-mediated augmentation of the CEA transcript appears to be attributable mainly to enhanced transcription rather than to increased mRNA stability. It is concluded that induction of enhanced CEA protein expression in cancer cells treated with 5-FU could be of clinical interest for the development of immunochemotherapeutic protocols based on CEA protein as the target molecule.

13. Dacarbazine-induced immunogenicity of a murine leukemia is attenuated in cells transfected with mutated K-ras gene

Author

Testorelli, C., Bussini, S., Filippi, R., Marelli, O., Orlando, L., Greiner, J. W., Grohmann, U., Tentori, L., Giuliani, A., Bonmassar, E., GRAZIA GRAZIANI, Testorelli, C, Bussini, S, DE FILIPPI, Rosaria, Marelli, O, Orlando, L, Greiner, Jw, Grohmann, U, Tentori, L, Giuliani, A, Bonmassar, E, and Graziani, G.

Subjects

Mice, Inbred BALB C, triazenes, Histocompatibility Antigens Class I, leukemia, Settore BIO/14, Antineoplastic Agents, mutated oncogene, immunogenicity, Transfection, Dacarbazine, Mice, Genes, ras, Mice, Inbred DBA, K-ras, xenogenization, Animals, Leukemia L5178

Abstract

Strong immunogenicity is induced by antitumor triazene compounds in tumor cells through a mutagenic mechanism. A highly immunogenicDclone, isolated from a dacarbazine-treated L5178Y leukemia of DBA/2 mice, was transfected with K-ras mutated at codon 12 (i.e. ras(m12)). This transfected clone presents at least 2 mutations, one concerning K-ras gene, and the other affecting an unrelated gene, responsible for the generation of a highly immunogenic, MHC class I restricted non-self peptide. The results indicate that cells ofDclone transfected with ras(m12) were less immunogenic than cells of the same origin transfected with the vector alone. Moreover, ras(m12)-transfected cells showed lower levels of H-2K(d) gene expression with respect to those detectable in control cells. In addition, in vivo and in vitro sensitization againstDclone carrying mutated ras did not result in a strong cytotoxic T lymphocyte response against ras(m12)-transfected non immunogenic L5178y target cells. These preliminary results suggest that K-ras mutation could down-regulate the level of tumor immunogenicity, possibly acquired through a mutagenic process affecting other unrelated genes.

14. The Development of Next-generation PBMC Humanized Mice for Preclinical Investigation of Cancer Immunotherapeutic Agents.

Author

Morillon YM 2nd, Sabzevari A, Schlom J, and Greiner JW

Subjects

Animals, Antibodies, Monoclonal, Humanized immunology, Antibodies, Monoclonal, Humanized pharmacology, Antineoplastic Agents immunology, Antineoplastic Agents pharmacology, Disease Models, Animal, Humans, Leukocytes, Mononuclear drug effects, Mice, Neoplasms immunology, Neoplasms pathology, Immunity, Cellular drug effects, Immunotherapy, Leukocytes, Mononuclear immunology, Neoplasms drug therapy

Abstract

Investigation of the efficacy and mechanisms of human immuno-oncology agents has been hampered due to species-specific differences when utilizing preclinical mouse models. Peripheral blood mononuclear cell (PBMC) humanized mice provide a platform for investigating the modulation of the human immune-mediated antitumor response while circumventing the limitations of syngeneic model systems. Use of humanized mice has been stymied by model-specific limitations, some of which include the development of graft versus host disease, technical difficulty and cost associated with each humanized animal, and insufficient engraftment of some human immune subsets. Recent advances have addressed many of these limitations from which have emerged humanized models that are more clinically relevant. This review characterizes the expanded usage, advantages and limitations of humanized mice and provides insights into the development of the next generation of murine humanized models to further inform clinical applications of cancer immunotherapeutic agents., (Copyright© 2020, International Institute of Anticancer Research (Dr. George J. Delinasios), All rights reserved.)

Published

2020

15. The Use of a Humanized NSG-β2m -/- Model for Investigation of Immune and Anti-tumor Effects Mediated by the Bifunctional Immunotherapeutic Bintrafusp Alfa.

Author

Morillon YMI, Smalley Rumfield C, Pellom ST, Sabzevari A, Roller NT, Horn LA, Jochems C, Palena C, Greiner JW, and Schlom J

Abstract

The lack of serial biopsies in patients with a range of carcinomas has been one obstacle in our understanding of the mechanism of action of immuno-oncology agents as well as the elucidation of mechanisms of resistance to these novel therapeutics. While much information can be obtained from studies conducted with syngeneic mouse models, these models have limitations, including that both tumor and immune cells being targeted are murine and that many of the immuno-oncology agents being evaluated are human proteins, and thus multiple administrations are hampered by host xenogeneic responses. Some of these limitations are being overcome by the use of humanized mouse models where human peripheral blood mononuclear cells (PBMC) are engrafted into immunosuppressed mouse strains. Bintrafusp alfa (M7824) is an innovative first-in-class bifunctional fusion protein composed of the extracellular domain of the TGF-βRII to function as a TGF-β "trap" fused to a human IgG1 antibody blocking PD-L1. A phase I clinical trial of bintrafusp alfa showed promising anti-tumor efficacy in heavily pretreated advanced solid tumors, and multiple clinical studies are currently ongoing. There is still much to learn regarding the mechanism of action of bintrafusp alfa, including its effects on both human immune cells in the periphery and in the tumor microenvironment (TME), and any temporal effects upon multiple administrations. By using the NSG-β2m -/- mouse strain humanized with PBMC, we demonstrate here for the first time: (a) the effects of bintrafusp alfa administration on human immune cells in the periphery vs. the TME using three different human xenograft models; (b) temporal effects upon multiple administrations of bintrafusp alfa; (c) phenotypic changes induced in the TME, and (d) variations observed in the use of multiple different PBMC donors. Also discussed are the similarities and differences in the data thus far obtained employing murine syngeneic models, from clinical trials, and in the use of this humanized mouse model. The results described here may guide the future use of this agent or similar immunotherapy agents as monotherapies or in combination therapy studies., (Copyright © 2020 Morillon, Smalley Rumfield, Pellom, Sabzevari, Roller, Horn, Jochems, Palena, Greiner and Schlom.)

Published

2020

16. Temporal changes within the (bladder) tumor microenvironment that accompany the therapeutic effects of the immunocytokine NHS-IL12.

Author

Morillon YM 2nd, Su Z, Schlom J, and Greiner JW

Subjects

Animals, Disease Models, Animal, Female, Humans, Mice, Tumor Microenvironment, Immunoglobulin G genetics, Immunotherapy methods, Interleukin-12 genetics, Recombinant Fusion Proteins genetics, Urinary Bladder Neoplasms drug therapy

Abstract

Background: While significant strides in the treatment of metastatic bladder cancer have been made with immune checkpoint inhibitors, the treatment of carcinoma in situ and non-muscle invasive, non-metastatic (superficial) human urothelial carcinoma, also termed non-muscle invasive bladder cancer (NMIBC), remains intractable with bacillus Calmette-Guerin (BCG) employed as the standard of care. In this study, an immunocytokine, NHS-muIL12, which consists of two molecules of murine IL-12 fused to NHS76, a tumor necrosis-targeting human IgG1, was examined as an immunotherapeutic in an orthotopic MB49 luc bladder tumor model., Methods: The antitumor activity of systemic administration of NHS-muIL12 was investigated on MB49 luc tumors, an aggressive, bioluminescent orthotopic bladder cancer model. Temporal studies were carried out on MB49 luc bladder tumors harvested during various time points during NHS-muIL12 treatment and cellular changes associated with the reduction in tumor burden following NHS-muIL12 were determined by flow cytometry. Effects of those changes on the proliferation/activation of lymphoid cells were also determined., Results: Studies revealed a significant reduction in MB49 luc bladder tumor burden occurring between days 3 and 6 after the third and final systemic administration of NHS-muIL12. Temporal analyses of the MB49 luc bladder tumor microenvironment (TME) initially revealed a large accumulation of myeloid-derived suppressor cells (MDSCs) and macrophages that elicited potent immunosuppression. Immunosuppression was characterized by the inability of CD4 + and CD8 + T cells to respond to broad-based immune stimulants. NHS-muIL12 administration resulted in temporal-dependent reductions in the number of MDSCs, macrophages and tumor-associated TGF-β, which culminated in a re-ignition of CD4 + and CD8 + T cells to elicit potent antitumor responses against MB49 luc bladder tumors., Conclusions: These findings provide strong evidence that the systemic administration of an immunocytokine consisting of a tumor-targeting Ig through recognition of DNA and DNA-histone complexes coupled to muIL-12 can effectively target the bladder TME; this significantly reduces the myeloid cellular compartment and reverts an immunosuppressive to an immunopermissive TME, ultimately resulting in antitumor effects. These studies provide further rationale for the employment of NHS-IL12 as an immunomodulator and clinical immunotherapeutic for NMIBC.

Published

2019

17. Immunology, Immunotherapy, and Translating Basic Science into the Clinic for Bladder Cancer.

Author

Ingersoll MA, Li X, Inman BA, Greiner JW, Black PC, and Adam RM

Abstract

The Fourth Annual Albert Institute Bladder Cancer Care and Research Symposium was held from September 14th-16th in Houston, Texas. The symposium covered a range of topics relevant to bladder cancer, including basic science aspects of immunology and immunotherapy that inform clinical management; intravesical therapy for non-muscle invasive disease; understanding the nuances of carcinoma in situ ; and optimizing patient care and outcomes following therapy. The moving landscape of bladder cancer from an industry perspective was also discussed. In the following sections we discuss intrinsic and extrinsic factors, including the immune microenvironment and sex bias, in the context of bladder cancer; how these influence tumor development, progression, and treatment strategies; and how the interpretation of immune features in relation to molecular subtypes informs both treatment decisions and response. We conclude with a summary of key points that will need to be addressed to ensure best use of new knowledge in this area for improved clinical management of patients with bladder cancer.

Published

2018

18. Enhanced immunotherapy by combining a vaccine with a novel murine GITR ligand fusion protein.

Author

Morillon YM 2nd, Hammond SA, Durham NM, Schlom J, and Greiner JW

Abstract

Immunotherapy was significantly enhanced in a murine tumor model by combining a vaccine with a fusion protein designed to target the glucocorticoid-induced tumor necrosis factor (TNF) receptor related gene (GITR) on the surface of T cells. The recombinant poxvirus-based vaccine platform included Modified Vaccinia virus Ankara (rMVA) and fowlpox (rF) vectors as the driver immunogens both engineered to express the human carcinoembryonic antigen (CEA) and three murine costimulatory molecules B7.1, ICAM-1, LFA-3 (designated TRICOM). In previous studies, mice expressing human CEA as a transgene (CEA.Tg mice) vaccinated with rMVA/rF-CEA-TRICOM overcame CEA immune tolerance by inducing anti-CEA‒specific immunity and regression of CEA-expressing tumors. The murine GITR ligand fusion protein (mGITRL-FP) consisted of a mouse IgG2a Fc region, a yeast-derived coiled GCN4 pII and the extracellular GITR-binding domain of murine GITR ligand. The design maximized valency and the potential to agonize the GITR receptor. Combined treatment of the vaccine and mGITRL-FP mediated a more robust tumor regression, leading to sustained improvement in overall survival. The enhanced immunotherapeutic effect was linked to the generation of a strong CD8 + T cell antitumor immune response. A treatment schedule with mGITRL-FP administered prior to the priming rMVA-CEA-TRICOM vaccination was of paramount importance. The mechanism of action for the enhanced antitumor effects resided in the depletion of immune cells, particularly FoxP3 + regulatory T cells, that express high GITR levels following activation. The results provide evidence that targeting GITR with mGITRL-FP in concert with a cancer vaccine represents a potential novel approach to more effective immunotherapy., Competing Interests: CONFLICTS OF INTEREST NCI authors do not have any potential conflicts of interest to disclose. Scott A. Hammond and Nicholas M. Durham are employees of MedImmune.

Published

2017

19. Enhanced antitumor effects by combining an IL-12/anti-DNA fusion protein with avelumab, an anti-PD-L1 antibody.

Author

Fallon JK, Vandeveer AJ, Schlom J, and Greiner JW

Subjects

Animals, Antibodies, Monoclonal, Humanized, Disease Models, Animal, Drug Synergism, Enzyme-Linked Immunosorbent Assay, Enzyme-Linked Immunospot Assay, Immunohistochemistry, Interleukin-12 immunology, Interleukin-12 pharmacology, Lymphocyte Activation drug effects, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Transgenic, Neoplasms, Experimental immunology, Recombinant Fusion Proteins pharmacology, T-Lymphocytes drug effects, T-Lymphocytes immunology, Antibodies, Monoclonal pharmacology, Antineoplastic Agents pharmacology, Immunotherapy methods, Neoplasms, Experimental drug therapy

Abstract

The combined therapeutic potential of an immunocytokine designed to deliver IL-12 to the necrotic regions of solid tumors with an anti-PD-L1 antibody that disrupts the immunosuppressive PD-1/PD-L1 axis yielded a combinatorial benefit in multiple murine tumor models. The murine version of the immunocytokine, NHS-muIL12, consists of an antibody (NHS76) recognizing DNA/DNA-histone complexes, fused with two molecules of murine IL-12 (NHS-muIL12). By its recognition of exposed DNA, NHS-muIL12 targets IL-12 to the necrotic portions of tumors; it has a longer plasma half-life and better antitumor efficacy against murine tumors than recombinant murine IL-12. It is shown here that NHS-muIL12, in an IFN-γ‒dependent mechanism, upregulates mPD-L1 expression on mouse tumors, which could be construed as an immunosuppressive action. Yet concurrent therapy with NHS-muIL12 and an anti-PD-L1 antibody resulted in additive/synergistic antitumor effects in PD-L1‒expressing subcutaneously transplanted tumors (MC38, MB49) and in an intravesical bladder tumor model (MB49). Antitumor efficacy correlated with (a) with a higher frequency of tumor antigen-specific splenic CD8+ T cells and (b) enhanced T cell activation over a wide range of NHS-muIL12 concentrations. These findings suggest that combining NHS-muIL12 and an anti-PD-L1 antibody enhances T cell activation and T cell effector functions within the tumor microenvironment, significantly improving overall tumor regression. These results should provide the rationale to examine the combination of these agents in clinical studies.

Published

2017

20. An NK cell line (haNK) expressing high levels of granzyme and engineered to express the high affinity CD16 allele.

Author

Jochems C, Hodge JW, Fantini M, Fujii R, Morillon YM 2nd, Greiner JW, Padget MR, Tritsch SR, Tsang KY, Campbell KS, Klingemann H, Boissel L, Rabizadeh S, Soon-Shiong P, and Schlom J

Subjects

Animals, Antibody-Dependent Cell Cytotoxicity, B7-H1 Antigen analysis, Cell Line, Tumor, GPI-Linked Proteins genetics, GPI-Linked Proteins immunology, Genetic Engineering, Humans, Immunoglobulin G therapeutic use, Interleukin-2 genetics, Killer Cells, Natural enzymology, Killer Cells, Natural radiation effects, Male, Mice, Middle Aged, Receptors, IgG immunology, Adoptive Transfer, Granzymes immunology, Killer Cells, Natural immunology, Receptors, IgG genetics

Abstract

Natural killer (NK) cells are known to play a role in mediating innate immunity, in enhancing adaptive immune responses, and have been implicated in mediating anti-tumor responses via antibody-dependent cell-mediated cytotoxicity (ADCC) by reactivity of CD16 with the Fc region of human IgG1 antibodies. The NK-92 cell line, derived from a lymphoma patient, has previously been well characterized and adoptive transfer of irradiated NK-92 cells has demonstrated safety and shown preliminary evidence of clinical benefit in cancer patients. The NK-92 cell line, devoid of CD16, has now been engineered to express the high affinity (ha) CD16 V158 FcγRIIIa receptor, as well as engineered to express IL-2; IL-2 has been shown to replenish the granular stock of NK cells, leading to enhanced perforin- and granzyme-mediated lysis of tumor cells. The studies reported here show high levels of granzyme in haNK cells, and demonstrate the effects of irradiation of haNK cells on multiple phenotypic markers, viability, IL-2 production, and lysis of a spectrum of human tumor cells. Studies also compare endogenous irradiated haNK lysis of tumor cells with that of irradiated haNK-mediated ADCC using cetuximab, trastuzumab and pertuzumab monoclonal antibodies. These studies thus provide the rationale for the potential use of irradiated haNK cells in adoptive transfer studies for a range of human tumor types. Moreover, since only approximately 10% of humans are homozygous for the high affinity V CD16 allele, these studies also provide the rationale for the use of irradiated haNK cells in combination with IgG1 anti-tumor monoclonal antibodies.

Published

2016

21. Systemic Immunotherapy of Non-Muscle Invasive Mouse Bladder Cancer with Avelumab, an Anti-PD-L1 Immune Checkpoint Inhibitor.

Author

Vandeveer AJ, Fallon JK, Tighe R, Sabzevari H, Schlom J, and Greiner JW

Subjects

Adaptive Immunity, Animals, Antibodies, Monoclonal metabolism, Antibodies, Monoclonal pharmacology, Antibodies, Monoclonal, Humanized, Antineoplastic Agents metabolism, Antineoplastic Agents pharmacology, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Carcinoma, Transitional Cell immunology, Carcinoma, Transitional Cell pathology, Disease Models, Animal, Drug Evaluation, Preclinical methods, Female, Immune Tolerance immunology, Immunotherapy methods, Mice, Inbred C57BL, Mycobacterium bovis immunology, Neoplasm Transplantation, Urinary Bladder Neoplasms immunology, Urinary Bladder Neoplasms pathology, Antibodies, Monoclonal therapeutic use, Antineoplastic Agents therapeutic use, B7-H1 Antigen antagonists & inhibitors, Carcinoma, Transitional Cell drug therapy, Urinary Bladder Neoplasms drug therapy

Abstract

Bacillus Calmette-Guerin (BCG) is the standard of care for intravesical therapy for carcinoma in situ and non-muscle invasive, nonmetastatic human urothelial carcinoma. Although the responsiveness to this immunotherapeutic is believed to be linked with (i) a high number of somatic mutations and (ii) a large number of tumor-infiltrating lymphocytes, recent findings of the roles that inhibitory immune receptors and their ligands play in tumor evasion may provide insights into the limitations of the effectiveness of BCG and offer new targets for immune-based therapy. In this study, an aggressive, bioluminescent orthotopic bladder cancer model, MB49 tumor cells transfected with luciferase (MB49(luc)), was used to study the antitumor effects of avelumab, an antibody to PD-L1. MB49(luc) murine tumor cells form multifocal tumors on the mucosal wall of the bladder reminiscent of non-muscle invasive, nonmetastatic urothelial carcinomas. MB49(luc) bladder tumors are highly positive for the expression of PD-L1, and avelumab administration induced significant (P < 0.05) antitumor effects. These antitumor effects were more dependent on the presence of CD4 than CD8 T cells, as determined by in vivo immune cell depletions. The findings suggest that in this bladder tumor model, interruption of the immune-suppressive PD-1/PD-L1 complex releases a local adaptive immune response that, in turn, reduces tumor growth. This bladder tumor model can be used to further identify host antitumor immune mechanisms and evaluate combinations of immune-based therapies for carcinoma in situ and non-muscle invasive, nonmetastatic urothelial carcinoma, to provide the rationale for subsequent clinical studies. Cancer Immunol Res; 4(5); 452-62. ©2016 AACR., (©2016 American Association for Cancer Research.)

Published

2016

22. Identification and characterization of a cytotoxic T-lymphocyte agonist epitope of brachyury, a transcription factor involved in epithelial to mesenchymal transition and metastasis.

Author

Tucker JA, Jochems C, Boyerinas B, Fallon J, Greiner JW, Palena C, Rodell TC, Schlom J, and Tsang KY

Subjects

Animals, Cell Line, Tumor, Female, Humans, Mice, Mice, Transgenic, Neoplasm Metastasis, Neoplasms pathology, Neoplasms therapy, Epithelial-Mesenchymal Transition immunology, Epitopes, T-Lymphocyte immunology, Fetal Proteins immunology, Neoplasms immunology, T-Box Domain Proteins immunology, T-Lymphocytes, Cytotoxic immunology

Abstract

The transcription factor brachyury is a major driver of epithelial to mesenchymal transition in human carcinoma cells. It is overexpressed in several human tumor types versus normal adult tissues, except for testes and thyroid. Overexpression is associated with drug resistance and poor prognosis. Previous studies identified a brachyury HLA-A2 cytotoxic T-lymphocyte epitope. The studies reported here describe an enhancer epitope of brachyury. Compared to the native epitope, the agonist epitope: (a) has enhanced binding to MHC class I, (b) increased the IFN-γ production from brachyury-specific T cells, (c) generated brachyury-specific T cells with greater levels of perforin and increased proliferation, (d) generated T cells more proficient at lysing human carcinoma cells endogenously expressing the native epitope, and (e) achieved greater brachyury-specific T-cell responses in vivo in HLA-A2 transgenic mice. These studies also report the generation of a heat-killed recombinant Saccharomyces cerevisiae (yeast) vector expressing the full-length brachyury gene encoding the agonist epitope. Compared to yeast-brachyury (native) devoid of the agonist epitope, the yeast-brachyury (agonist) enhanced the activation of brachyury-specific T cells, which efficiently lysed human carcinoma cells. In addition to providing the rationale for the recombinant yeast-brachyury (agonist) as a potential vaccine in cancer therapy, these studies also provide the rationale for the use of the agonist in (a) dendritic cell (DC) vaccines, (b) adjuvant or liposomal vaccines, (c) recombinant viral and/or bacterial vaccines, (d) protein/polypeptide vaccines, (e) activation of T cells ex vivo in adoptive therapy protocols, and (f) generation of genetically engineered targeted T cells.

Published

2014

23. The immunocytokine NHS-IL12 as a potential cancer therapeutic.

Author

Fallon J, Tighe R, Kradjian G, Guzman W, Bernhardt A, Neuteboom B, Lan Y, Sabzevari H, Schlom J, and Greiner JW

Subjects

Animals, Antineoplastic Combined Chemotherapy Protocols immunology, Antineoplastic Combined Chemotherapy Protocols therapeutic use, CD8-Positive T-Lymphocytes, Cancer Vaccines administration & dosage, Cancer Vaccines therapeutic use, Cell Line, Tumor, Docetaxel, Female, Humans, Immunoglobulin G immunology, Immunoglobulin G therapeutic use, Immunomodulation, Indoles administration & dosage, Interleukin-12 immunology, Interleukin-12 therapeutic use, Lymphocyte Activation drug effects, Macaca fascicularis, Membrane Glycoproteins therapeutic use, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Protein Engineering, Pyrroles administration & dosage, Recombinant Fusion Proteins immunology, Recombinant Fusion Proteins therapeutic use, Sunitinib, Survival Rate, Taxoids administration & dosage, Tumor Burden, Antineoplastic Combined Chemotherapy Protocols pharmacology, Immunoglobulin G pharmacology, Interferon-gamma metabolism, Interleukin-12 pharmacology, Neoplasms, Experimental therapy, Recombinant Fusion Proteins pharmacology

Abstract

Targeted delivery of IL-12 might turn this cytokine into a safer, more effective cancer therapeutic. Here we describe a novel immunocytokine, NHS-IL12, consisting of two molecules of IL-12 fused to a tumor necrosis-targeting human IgG1 (NHS76). The addition of the human IgG1 moiety resulted in a longer plasma half-life of NHS-IL12 than recombinant IL-12, and a selective targeting to murine tumors in vivo. Data from both in vitro assays using human PBMCs and in vivo primate studies showed that IFN-gamma production by immune cells is attenuated following treatment with the immunocytokine, suggesting an improved toxicity profile than seen with recombinant IL-12 alone. NHS-IL12 was superior to recombinant IL-12 when evaluated as an anti-tumor agent in three murine tumor models. Mechanistic studies utilizing immune cell subset-depleting antibodies, flow cytometric methods, and in vitro cytotoxicity and ELISA assays all indicated that the anti-tumor effects of NHS-IL12 were primarily CD8+ T cell-dependent and likely IL-12-mediated. Combining NHS-IL12 treatment with a cancer vaccine, radiation, or chemotherapy resulted in greater anti-tumor effects than each individual therapy alone. These preclinical findings provide a rationale for the clinical testing of this immunocytokine, both as a single agent and in combination with vaccines, radiation and chemotherapy.

Published

2014

24. Therapeutic cancer vaccines.

Author

Schlom J, Hodge JW, Palena C, Tsang KY, Jochems C, Greiner JW, Farsaci B, Madan RA, Heery CR, and Gulley JL

Subjects

Animals, Biomarkers, Tumor physiology, Clinical Trials as Topic, Combined Modality Therapy, Disease Progression, Drug Resistance, Neoplasm, Humans, Molecular Targeted Therapy, Neoplasms pathology, Cancer Vaccines therapeutic use, Neoplasms therapy

Abstract

Therapeutic cancer vaccines have the potential of being integrated in the therapy of numerous cancer types and stages. The wide spectrum of vaccine platforms and vaccine targets is reviewed along with the potential for development of vaccines to target cancer cell "stemness," the epithelial-to-mesenchymal transition (EMT) phenotype, and drug-resistant populations. Preclinical and recent clinical studies are now revealing how vaccines can optimally be used with other immune-based therapies such as checkpoint inhibitors, and so-called nonimmune-based therapeutics, radiation, hormonal therapy, and certain small molecule targeted therapies; it is now being revealed that many of these traditional therapies can lyse tumor cells in a manner as to further potentiate the host immune response, alter the phenotype of nonlysed tumor cells to render them more susceptible to T-cell lysis, and/or shift the balance of effector:regulatory cells in a manner to enhance vaccine efficacy. The importance of the tumor microenvironment, the appropriate patient population, and clinical trial endpoints is also discussed in the context of optimizing patient benefit from vaccine-mediated therapy., (2014 Published by Elsevier Inc.)

Published

2014

25. Inhibition of TGF-β1 signaling promotes central memory T cell differentiation.

Author

Takai S, Schlom J, Tucker J, Tsang KY, and Greiner JW

Subjects

Adoptive Transfer, Animals, Blotting, Western, CD8-Positive T-Lymphocytes cytology, Enzyme-Linked Immunosorbent Assay, Female, Flow Cytometry, Mice, Mice, Inbred C57BL, Real-Time Polymerase Chain Reaction, CD8-Positive T-Lymphocytes immunology, Cell Differentiation immunology, Immunologic Memory immunology, Lymphocyte Activation immunology, Signal Transduction immunology, Transforming Growth Factor beta1 immunology

Abstract

This study affirmed that isolated CD8(+) T cells express mRNA and produce TGF-β following cognate peptide recognition. Blockage of endogenous TGF-β with either a TGF-β-blocking Ab or a small molecule inhibitor of TGF-βRI enhances the generation of CD62L(high)/CD44(high) central memory CD8(+) T cells accompanied with a robust recall response. Interestingly, the augmentation within the central memory T cell pool occurs in lieu of cellular proliferation or activation, but with the expected increase in the ratio of the Eomesoderm/T-bet transcriptional factors. Yet, the signal transduction pathway(s) seems to be noncanonical, independent of SMAD or mammalian target of rapamycin signaling. Enhancement of central memory generation by TGF-β blockade is also confirmed in human PBMCs. The findings underscore the role(s) that autocrine TGF-β plays in T cell homeostasis and, in particular, the balance of effector/memory and central/memory T cells. These results may provide a rationale to targeting TGF-β signaling to enhance Ag-specific CD8(+) T cell memory against a lethal infection or cancer.

Published

2013

26. Distinct effects of saracatinib on memory CD8+ T cell differentiation.

Author

Takai S, Sabzevari H, Farsaci B, Schlom J, and Greiner JW

Subjects

Animals, Antigens, Viral genetics, Antigens, Viral immunology, Antigens, Viral metabolism, CD8-Positive T-Lymphocytes enzymology, Cancer Vaccines genetics, Cancer Vaccines immunology, Cancer Vaccines metabolism, Cell Differentiation genetics, Cell Line, Tumor, Humans, Hyaluronan Receptors genetics, Hyaluronan Receptors immunology, Hyaluronan Receptors metabolism, Immunologic Memory genetics, Influenza A virus genetics, Influenza A virus immunology, Influenza A virus metabolism, Influenza Vaccines genetics, Influenza Vaccines immunology, Interferon-gamma genetics, Interferon-gamma immunology, Interferon-gamma metabolism, L-Selectin genetics, L-Selectin immunology, L-Selectin metabolism, Mice, Mice, Transgenic, Neoplasms, Experimental genetics, Neoplasms, Experimental immunology, Neoplasms, Experimental metabolism, Viral Proteins genetics, Viral Proteins immunology, Viral Proteins metabolism, src-Family Kinases antagonists & inhibitors, src-Family Kinases genetics, src-Family Kinases immunology, src-Family Kinases metabolism, Benzodioxoles pharmacology, CD8-Positive T-Lymphocytes immunology, Cell Differentiation drug effects, Immunologic Memory drug effects, Quinazolines pharmacology

Abstract

Immunologic memory involving CD8(+) T cells is a hallmark of an adaptive Ag-specific immune response and constitutes a critical component of protective immunity. Designing approaches that enhance long-term T cell memory would, for the most part, fortify vaccines and enhance host protection against infectious diseases and, perhaps, cancer immunotherapy. A better understanding of the cellular programs involved in the Ag-specific T cell response has led to new approaches that target the magnitude and quality of the memory T cell response. In this article, we show that T cells from TCR transgenic mice for the nucleoprotein of influenza virus NP68 exhibit the distinct phases--priming, expansion, contraction, and memory--of an Ag-specific T cell response when exposed in vitro to the cognate peptide. Saracatinib, a specific inhibitor of Src family kinases, administered at low doses during the expansion or contraction phases, increased CD62L(high)/CD44(high) central memory CD8(+) T cells and IFN-γ production but suppressed immunity when added during the priming phase. These effects by saracatinib were not accompanied by the expected decline of Src family kinases but were accompanied by Akt-mammalian target of rapamycin suppression and/or mediated via another pathway. Increased central memory cells by saracatinib were recapitulated in mice using a poxvirus-based influenza vaccine, thus underscoring the importance of dose and timing of the inhibitor in the context of memory T cell differentiation. Finally, vaccine plus saracatinib treatment showed better protection against tumor challenge. The immune-potentiating effects on CD8(+) T cells by a low dose of saracatinib might afford better protection from pathogens or cancer when combined with vaccine.

Published

2012

27. In vivo efficacy of a chitosan/IL-12 adjuvant system for protein-based vaccines.

Author

Heffernan MJ, Zaharoff DA, Fallon JK, Schlom J, and Greiner JW

Subjects

Animals, CD4-Positive T-Lymphocytes metabolism, Enzyme-Linked Immunosorbent Assay, Interferon-gamma metabolism, Mice, Mice, Inbred C57BL, Adjuvants, Immunologic metabolism, Chitosan immunology, Interleukin-12 immunology, Proteins immunology, Vaccines immunology

Abstract

Vaccines based on recombinant proteins require adjuvant systems in order to generate Th1-type immune responses. We have developed a vaccine adjuvant system using a viscous chitosan solution and interleukin (IL)-12, a Th1-inducing cytokine. The chitosan solution is designed to create a depot of antigen and IL-12 at a subcutaneous injection site. We measured the in vivo immune response of a vaccine containing 0.25, 1, or 4 μg murine IL-12 and 75 μg ovalbumin (OVA), formulated in a 1.5% chitosan glutamate solution. The chitosan/IL-12/OVA vaccine, in comparison to chitosan/OVA, IL-12/OVA, or OVA alone, elicited greater antigen-specific CD4(+) and CD8(+) T-cell responses, as determined by CD4(+) splenocyte proliferation, Th1 cytokine release, CD8(+) T-cell interferon-γ release, and MHC class I peptide pentamer staining. The combination of chitosan and IL-12 also enhanced IgG2a and IgG2b antibody responses to OVA. Co-formulation of chitosan and IL-12 thus promoted the generation of a Th1 immune response to a model protein vaccine., (Published by Elsevier Ltd.)

Published

2011

28. Detection of circulating tumor cells is improved by drug-induced antigen up-regulation: preclinical and clinical studies.

Author

Bonmassar L, Fossile E, Scoppola A, Graziani G, Prete SP, Formica V, Cappelletti D, De Vecchis L, Cardillo A, Concolino F, D'Atri S, Balduzzi A, Torino F, Caporaso P, Greiner JW, Bonmassar E, Roselli M, and Aquino A

Subjects

Aged, Aged, 80 and over, Animals, Antibodies, Monoclonal immunology, Antibodies, Monoclonal metabolism, Antimetabolites, Antineoplastic pharmacology, Carcinoembryonic Antigen metabolism, Cell Line, Tumor, Colonic Neoplasms immunology, Enzyme Inhibitors pharmacology, Female, Fluorouracil pharmacology, Humans, Immunoblotting, Immunomagnetic Separation, Keratin-19 metabolism, Male, Mice, Middle Aged, Neoplasm Metastasis, Neoplastic Cells, Circulating drug effects, Neoplastic Cells, Circulating metabolism, RNA, Messenger genetics, Reverse Transcriptase Polymerase Chain Reaction, Up-Regulation, Biomarkers, Tumor analysis, Carcinoembryonic Antigen genetics, Colonic Neoplasms blood, Keratin-19 genetics, Neoplastic Cells, Circulating pathology, Staurosporine pharmacology

Abstract

(51)Cr-prelabelled colon cancer cells (simulating 'circulating tumor cells', CTCs) were added to human peripheral blood and exposed to staurosporine (ST) to increase carcinoembryonic antigen (CEA) expression. CTCs were captured with immunomagnetic beads coated with Ber-EP4 monoclonal antibody, recognizing the common epithelial antigen present in the majority of cancer cells of epithelial origin, with capture efficiency of more than 80%. Moreover, ST treatment increased CEA expression without compromising Ber-EP4 capture efficiency. In a pilot clinical study on 37 patients, CTCs were captured using Ber-EP4 beads, and recognized by RT-PCR set for CEA or cytokeratin-19 (CK) mRNA detection. The results showed that: (a) the percentage of CEA-positive CTCs (CTC(CEA), 54.1%) was lower than that of CK-positive CTCs (CTC(CK), 70.3%); (b) in vitro ST treatment converted a significant number of CTC(CEA)-negative into CTC(CEA)-positive cases. Therefore, immunomagnetic capture combined with exposure to ST provides a feasible and sensitive technique for the detection of functionally-active CTCs responsive to ST-mediated CEA up-regulation.

Published

2010

29. Intratumoral immunotherapy of established solid tumors with chitosan/IL-12.

Author

Zaharoff DA, Hance KW, Rogers CJ, Schlom J, and Greiner JW

Subjects

Animals, Carcinoembryonic Antigen genetics, Cells, Cultured, Colorectal Neoplasms immunology, Cytotoxicity, Immunologic drug effects, Immunologic Memory, Interleukin-12 administration & dosage, Interleukin-12 adverse effects, Lymphocyte Depletion, Mice, Mice, Inbred C57BL, Mice, Transgenic, Neoplasm Transplantation, Pancreatic Neoplasms immunology, Remission Induction, Tumor Burden drug effects, Adjuvants, Immunologic administration & dosage, Chitosan administration & dosage, Colorectal Neoplasms therapy, Immunotherapy, Pancreatic Neoplasms therapy

Abstract

IL-12 is a potent antitumor cytokine that exhibits significant clinical toxicities after systemic administration. We hypothesized that intratumoral (i.t.) administration of IL-12 coformulated with the biodegradable polysaccharide chitosan could enhance the antitumor activity of IL-12 while limiting its systemic toxicity. Noninvasive imaging studies monitored local retention of IL-12, with and without chitosan coformulation, after i.t. injection. Antitumor efficacy of IL-12 alone and IL-12 coformulated with chitosan (chitosan/IL-12) was assessed in mice bearing established colorectal (MC32a) and pancreatic (Panc02) tumors. Additional studies involving depletion of immune cell subsets, tumor rechallenge, and CTL activity were designed to elucidate mechanisms of regression and tumor-specific immunity. Coformulation with chitosan increased local IL-12 retention from 1 to 2 days to 5 to 6 days. Weekly i.t. injections of IL-12 alone eradicated ≤10% of established MC32a and Panc02 tumors, while i.t. chitosan/IL-12 immunotherapy caused complete tumor regression in 80% to 100% of mice. Depletion of CD4(+) or Gr-1(+) cells had no impact on chitosan/IL-12-mediated tumor regression. However, CD8(+) or NK cell depletion completely abrogated antitumor activity. I.t. chitosan/IL-12 immunotherapy generated systemic tumor-specific immunity, as >80% of mice cured with i.t. chitosan/IL-12 immunotherapy were at least partially protected from tumor rechallenge. Furthermore, CTLs from spleens of cured mice lysed MC32a and gp70 peptide-loaded targets. Chitosan/IL-12 immunotherapy increased local retention of IL-12 in the tumor microenvironment, eradicated established, aggressive murine tumors, and generated systemic tumor-specific protective immunity. Chitosan/IL-12 is a well-tolerated, effective immunotherapy with considerable potential for clinical translation.

Published

2010

30. Intravesical immunotherapy of superficial bladder cancer with chitosan/interleukin-12.

Author

Zaharoff DA, Hoffman BS, Hooper HB, Benjamin CJ Jr, Khurana KK, Hance KW, Rogers CJ, Pinto PA, Schlom J, and Greiner JW

Subjects

Administration, Intravesical, Animals, BCG Vaccine administration & dosage, Carcinoma, Transitional Cell genetics, Carcinoma, Transitional Cell immunology, Cell Line, Tumor, Female, Immunohistochemistry, Interferon-gamma blood, Interferon-gamma urine, Interleukin-12 blood, Interleukin-12 urine, Luciferases biosynthesis, Luciferases genetics, Macrophages immunology, Mice, Mice, Inbred C57BL, Transfection, Urinary Bladder Neoplasms genetics, Urinary Bladder Neoplasms immunology, Carcinoma, Transitional Cell therapy, Chitosan administration & dosage, Interleukin-12 administration & dosage, Urinary Bladder Neoplasms therapy

Abstract

Intravesical BCG has been used successfully to treat superficial bladder cancer for three decades. However, 20% to 30% of patients will fail initial BCG therapy and 30% to 50% of patients will develop recurrent tumors within 5 years. Alternative or complementary strategies for the management of superficial bladder cancer are needed. Interleukin-12 (IL-12) is a potent T(H)1 cytokine with robust antitumor activity and the ability to potentiate immunologic memory. Unfortunately, intravesical IL-12 did not show antitumor efficacy in a recent clinical study of patients with recurrent superficial bladder cancer. We hypothesized that coformulation of IL-12 with chitosan, a biocompatible, mucoadhesive polysaccharide, could improve intravesical IL-12 delivery and provide an effective and durable alternative for the treatment of superficial bladder cancer. In antitumor studies, 88% to 100% of mice bearing orthotopic bladder tumors were cured after four intravesical treatments with chitosan/IL-12. In contrast, only 38% to 60% of mice treated with IL-12 alone and 0% treated with BCG were cured. Antitumor responses following chitosan/IL-12 treatments were durable and provided complete protection from intravesical tumor rechallenge. Urinary cytokine analysis showed that chitosan/IL-12 induced multiple T(H)1 cytokines at levels significantly higher than either IL-12 alone or BCG. Immunohistochemistry revealed moderate to intense tumor infiltration by T cells and macrophages following chitosan/IL-12 treatments. Bladder submucosa from cured mice contained residual populations of immune cells that returned to baseline levels after several months. Intravesical chitosan/IL-12 is a well-tolerated, effective immunotherapy that deserves further consideration for testing in humans for the management of superficial bladder cancer.

Published

2009

31. The antitumor and immunoadjuvant effects of IFN-alpha in combination with recombinant poxvirus vaccines.

Author

Hance KW, Rogers CJ, Zaharoff DA, Canter D, Schlom J, and Greiner JW

Subjects

Adenocarcinoma immunology, Animals, Cancer Vaccines genetics, Carcinoembryonic Antigen genetics, Cell Line, Tumor, Combined Modality Therapy, DNA, Recombinant analysis, Female, Histocompatibility Antigens Class I metabolism, Lymph Nodes drug effects, Lymph Nodes immunology, Mice, Mice, Inbred C57BL, Mice, Transgenic, Phenotype, Adenocarcinoma drug therapy, Adjuvants, Immunologic therapeutic use, Antineoplastic Agents therapeutic use, Cancer Vaccines therapeutic use, Fowlpox virus genetics, Interferon-alpha therapeutic use, Vaccinia virus genetics

Abstract

Purpose: IFN-alpha is a pleiotropic cytokine possessing immunomodulatory properties that may improve the efficacy of therapeutic cancer vaccines. The aim of this study was to evaluate the effectiveness and compatibility of combining recombinant IFN-alpha with poxvirus vaccines targeting the human carcinoembryonic antigen (CEA) in murine models of colorectal and pancreatic adenocarcinomas, where CEA is a self-antigen., Experimental Design: The phenotypic and functional effects of IFN-alpha were evaluated in the draining inguinal lymph nodes of tumor-free mice. We studied the effect of the site of IFN-alpha administration (local versus distal) on antigen-specific immune responses to poxvirus vaccination. Mechanistic studies were conducted to assess the efficacy of IFN-alpha and CEA-directed poxvirus vaccines in tumor-bearing CEA transgenic mice., Results: We identified a dose and schedule of IFN-alpha that induced a locoregional expansion of the draining inguinal lymph nodes and improved cellular cytotoxicity (natural killer and CD8(+)) and antigen presentation. Suppression of the vaccinia virus was avoided by administering IFN-alpha distal to the site of vaccination. The combination of IFN-alpha and vaccine inhibited tumor growth, improved survival, and elicited CEA-specific CTL responses in mice with CEA(+) adenocarcinomas. In mice with pancreatic tumors, IFN-alpha slowed tumor growth, induced CTL activity, and increased CD8(+) tumor-infiltrating lymphocytes., Conclusions: These data suggest that IFN-alpha can be used as a biological response modifier with antigen-directed poxvirus vaccines to yield significant therapeutic antitumor immune responses. This study provides the rationale and mechanistic insights to support a clinical trial of this immunotherapeutic strategy in patients with CEA-expressing carcinomas.

Published

2009

32. Exercise enhances vaccine-induced antigen-specific T cell responses.

Author

Rogers CJ, Zaharoff DA, Hance KW, Perkins SN, Hursting SD, Schlom J, and Greiner JW

Subjects

Animals, Body Composition, CD4-Positive T-Lymphocytes metabolism, Cell Proliferation, Cytokines biosynthesis, Cytokines immunology, Female, Lymphocyte Activation immunology, Mice, Mice, Inbred C57BL, Ovalbumin immunology, Substrate Specificity, CD4-Positive T-Lymphocytes immunology, Motor Activity, Vaccination

Abstract

Regular moderate exercise has been proposed to enhance immune function, but its effects on immunity and their consequences have not been well studied. Mice without (AL) or with access (AL+EX) to voluntary running wheels were vaccinated with a model antigen (ovalbumin (OVA)) via intranasal or subcutaneous routes to target the mucosal and systemic immune compartments, respectively. EX enhanced OVA-specific CD4(+) T cell cytokine production and proliferation in all lymphoid organs examined without changes in cell distribution in any organ. These results suggest that coupling moderate exercise with vaccination may enhance vaccine efficacy for the prevention and/or therapy of numerous diseases.

Published

2008

33. Vaccination with a recombinant Saccharomyces cerevisiae expressing a tumor antigen breaks immune tolerance and elicits therapeutic antitumor responses.

Author

Wansley EK, Chakraborty M, Hance KW, Bernstein MB, Boehm AL, Guo Z, Quick D, Franzusoff A, Greiner JW, Schlom J, and Hodge JW

Subjects

Animals, Antigens, Neoplasm metabolism, CD8-Positive T-Lymphocytes metabolism, Cancer Vaccines, Carcinoembryonic Antigen metabolism, Cell Proliferation, Female, Humans, Lymphocytes cytology, Mice, Mice, Inbred C57BL, Recombinant Proteins chemistry, Vaccines, DNA metabolism, Antigens, Neoplasm chemistry, Antineoplastic Agents pharmacology, Carcinoembryonic Antigen chemistry, Gene Expression Regulation, Immunotherapy methods, Saccharomyces cerevisiae metabolism, Vaccines, DNA chemistry

Abstract

Purpose: Saccharomyces cerevisiae, a nonpathogenic yeast, has been used previously as a vehicle to elicit immune responses to foreign antigens, and tumor-associated antigens, and has been shown to reduce tumor burden in mice. Studies were designed to determine if vaccination of human carcinoembryonic antigen (CEA)-transgenic (CEA-Tg) mice (where CEA is a self-antigen) with a recombinant S. cerevisiae construct expressing human CEA (yeast-CEA) elicits CEA-specific T-cell responses and antitumor activity., Experimental Design: CEA-Tg mice were vaccinated with yeast-CEA, and CD4(+) and CD8(+) T-cell responses were assessed after one and multiple administrations or vaccinations at multiple sites per administration. Antitumor activity was determined by tumor growth and overall survival in both pulmonary metastasis and s.c. pancreatic tumor models., Results: These studies demonstrate that recombinant yeast can break tolerance and that (a) yeast-CEA constructs elicit both CEA-specific CD4(+) and CD8(+) T-cell responses; (b) repeated yeast-CEA administration causes increased antigen-specific T-cell responses after each vaccination; (c) vaccination with yeast-CEA at multiple sites induces a greater T-cell response than the same dose given at a single site; and (d) tumor-bearing mice vaccinated with yeast-CEA show a reduction in tumor burden and increased overall survival compared to mock-treated or control yeast-vaccinated mice in both pulmonary metastasis and s.c. pancreatic tumor models., Conclusions: Vaccination with a heat-killed recombinant yeast expressing the tumor-associated antigen CEA induces CEA-specific immune responses, reduces tumor burden, and extends overall survival in CEA-Tg mice. These studies thus form the rationale for the incorporation of recombinant yeast-CEA and other recombinant yeast constructs in cancer immunotherapy protocols.

Published

2008

34. Targeted delivery of murine IFN-gamma using a recombinant fowlpox virus: NK cell recruitment to regional lymph nodes and priming of tumor-specific host immunity.

Author

Zeytin H, Reali E, Zaharoff DA, Rogers CJ, Schlom J, and Greiner JW

Subjects

Animals, Cancer Vaccines administration & dosage, Cell Line, Tumor, Cell Movement, Cytotoxicity, Immunologic, DNA, Recombinant administration & dosage, Female, Genetic Vectors, Immunologic Factors administration & dosage, Injections, Interferon-gamma biosynthesis, Interferon-gamma blood, Mice, Mice, Inbred C57BL, Neoplasms, Experimental immunology, Neoplasms, Experimental prevention & control, Recombinant Proteins administration & dosage, T-Lymphocytes, Cytotoxic immunology, Cancer Vaccines immunology, Fowlpox virus genetics, Immunologic Factors genetics, Interferon-gamma genetics, Killer Cells, Natural immunology, Lymph Nodes immunology

Abstract

Interferon-gamma (IFN-gamma) is a proinflammatory cytokine that also acts as a potent immunomodulatory agent. In this study, a replication-deficient recombinant avian (fowlpox) virus was engineered to express the murine IFN-gamma gene (rF-MuIFN-gamma) with the rationale of delivering concentrated levels of the cytokine to a local tissue microenvironment. Subcutaneous (s.c.) rF-MuIFN-gamma administration resulted in IFN-gamma production that (1) was restricted to the tissue microenvironment of the injection site and (2) was biologically active, as evidenced by a significant increase of class I MHC expression levels in s.c. growing tumors following rF-MuIFN-gamma administration. Infection of a highly tumorigenic murine cell line, MC38, with rF-MuIFN-gamma functioned as an effective tumor cell-based vaccine by protecting mice from the formation of primary tumors and from subsequent tumor challenge. The cell-based vaccine was completely ineffective if mice were vaccinated with MC38 cells either pretreated with rIFN-gamma or infected with the wild-type fowlpox virus (FP-WT). Analysis of the regional lymph nodes draining the site of injection of the rF-MuIFN-gamma-based tumor cell vaccine revealed the presence of tumor-specific cell lysis (CTL) as well as a significant amount of lysis directed at natural killer (NK)-sensitive YAC-1 cells. Flow cytometric analyses coupled with functional assays confirmed the sustained presence of NK1.1(+) cells within those draining lymph nodes for up to 5 days after rF-MuIFN-gamma injection. Mice treated with NK cell-depleting antibodies prior to the injection of the rF-MuIFN-gamma-infected MC38 tumor cells were not protected from primary tumor growth; analysis of the lymph nodes draining the injection site in NK-depleted mice revealed an accompanying loss of the tumor-specific CTL activity. The findings provide evidence that NK cells, known for their contributions to host innate immunity, also provide immunoregulatory signals required for the development of an adaptive immune response, which, in turn, protected vaccinated mice against tumor growth.

Published

2008

35. Energy restriction and exercise differentially enhance components of systemic and mucosal immunity in mice.

Author

Rogers CJ, Berrigan D, Zaharoff DA, Hance KW, Patel AC, Perkins SN, Schlom J, Greiner JW, and Hursting SD

Subjects

Animals, Body Composition, Female, Mice, Mice, Inbred C57BL, Organ Size, Peyer's Patches cytology, Peyer's Patches metabolism, Spleen anatomy & histology, T-Lymphocytes, Energy Intake physiology, Immunity, Mucosal immunology, Motor Activity physiology

Abstract

The prevalence of obesity, an established risk factor for several chronic diseases, including cancer, has risen dramatically over the past 4 decades. Dietary change and/or increased physical activity are the most commonly recommended lifestyle-based strategies for preventing or reversing obesity. One of several physiological systems that may be enhanced by dietary change and exercise is the immune system. In this study, we examined the effects of energy restriction (ER; 30% reduction relative to control energy intake) and/or exercise (EX; voluntary wheel running) on systemic and mucosal immune function. Female C57BL/6 mice were randomized into 4 treatment conditions: 1) controls consumed ad libitum (AL); 2) AL with access to running wheels (AL + EX); 3) 30% ER; and 4) 30% ER with access to running wheels (ER + EX). Both ER and EX reduced spleen weight and the number of splenic T and B lymphocytes (P < 0.05). ER enhanced natural killer (NK) cell function, but reduced concanavalin A (Con A)-induced T-cell proliferation (P < 0.05). In contrast, EX enhanced Con A-induced proliferation and cytokine production from Peyer's patch cells (P < 0.05). These data suggest that ER and EX enhance some, but not all, components of the immune system and are likely working via different biological mechanisms to regulate NK and T-cell function.

Published

2008

36. Chitosan solution enhances the immunoadjuvant properties of GM-CSF.

Author

Zaharoff DA, Rogers CJ, Hance KW, Schlom J, and Greiner JW

Subjects

Adjuvants, Immunologic administration & dosage, Animals, Antigen Presentation immunology, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Cell Proliferation, Cytotoxicity Tests, Immunologic, Delayed-Action Preparations administration & dosage, Dendritic Cells immunology, Female, Gene Expression, Granulocyte-Macrophage Colony-Stimulating Factor administration & dosage, Histocompatibility Antigens Class II genetics, Injections, Subcutaneous, Lymph Nodes immunology, Lymphocyte Subsets immunology, Mice, T-Lymphocytes, Cytotoxic immunology, Chitosan immunology, Granulocyte-Macrophage Colony-Stimulating Factor immunology

Abstract

Sustained, local delivery of immunomodulatory cytokines is under investigation for its ability to enhance vaccine and anti-tumor responses both clinically and preclinically. This study evaluates the ability of chitosan, a biocompatible polysaccharide, to (1) control the dissemination of a cytokine, GM-CSF, and (2) enhance the immunoadjuvant properties of GM-CSF. While cytokines have previously been delivered in lipid-based adjuvants and other vehicles, these do not have the clinical safety profile or unique properties of chitosan. We found that chitosan solution maintained a measurable depot of recombinant GM-CSF (rGM-CSF) at a subcutaneous injection site for up to 9 days. In contrast, when delivered in a saline vehicle, rGM-CSF was undetectable in 12-24h. Furthermore, a single s.c. injection of 20 microg rGM-CSF in chitosan solution (chitosan/rGM-CSF(20 microg)) transiently expanded lymph nodes up to 4.6-fold and increased the number of MHC class II expressing cells and dendritic cells by 7.4-fold and 6.8-fold, respectively. These increases were significantly greater than those measured when rGM-CSF was administered in saline at the standard preclinical dose and schedule, i.e. 4 daily s.c. injections of 20 microg. Furthermore, lymph node cells from mice injected with chitosan/rGM-CSF(20 microg) induced greater allogeneic T cell proliferation, indicating enhanced antigen presenting capability, than lymph node cells from mice injected with rGM-CSF alone. Finally, in vaccination experiments, chitosan/rGM-CSF was superior to either chitosan or rGM-CSF alone in enhancing the induction of antigen-specific CD4(+) proliferation, peptide-specific CD8(+) pentamer staining and cytotoxic T cell lysis. Altogether, chitosan/rGM-CSF outperformed standard rGM-CSF administrations in dendritic cell recruitment, antigen presentation and vaccine enhancement. We conclude that chitosan solution is a promising delivery platform for the sustained, local delivery of rGM-CSF.

Published

2007

37. Combination of physical activity, nutrition, or other metabolic factors and vaccine response.

Author

Hance KW, Rogers CJ, Hursting SD, and Greiner JW

Subjects

Combined Modality Therapy, Energy Intake immunology, Humans, Immunity, Innate, Neoplasms complications, Neoplasms immunology, Obesity complications, Obesity immunology, Risk Factors, Cancer Vaccines, Diet, Exercise, Neoplasms prevention & control

Abstract

A number of lifestyle factors that reduce cancer risk in the primary prevention setting may be potential new targets for use in combination with cancer vaccines. This review discusses the modulation of energy balance (physical activity, calorie restriction, and obesity prevention), and the supplementation with natural and synthetic analogs of vitamins A and E, as potential interventions for use in combination with cancer vaccines. Additionally, the pharmacologic manipulation of nutrient metabolism in the tumor microenvironment (e.g., arachidonic acid, arginine, tryptophan, and glucose metabolism) is discussed. This review includes a brief overview of the role of each agent in primary cancer prevention; outlines the effects of these agents on immune function, specifically adaptive and/or anti-tumor immune mechanisms, when known; and discusses the potential use of these interventions in combination with therapeutic cancer vaccines. Modulation of energy balance through exercise and strategies targeting nutrient metabolism in the tumor microenvironment represent the most promising interventions to partner with therapeutic cancer vaccines. Additionally, the use of vitamin E succinate and the retinoid X receptor-directed rexinoids in combination with cancer vaccines offer promise. In summary, a number of energy balance- and nutrition-related interventions are viable candidates for further study in combination with cancer vaccines.

Published

2007

38. Chitosan solution enhances both humoral and cell-mediated immune responses to subcutaneous vaccination.

Author

Zaharoff DA, Rogers CJ, Hance KW, Schlom J, and Greiner JW

Subjects

Aluminum Hydroxide immunology, Animals, CD4-Positive T-Lymphocytes immunology, Chitosan pharmacokinetics, Enzyme-Linked Immunosorbent Assay, Female, Freund's Adjuvant, Histocytochemistry, Hypersensitivity, Delayed, Injections, Subcutaneous, Lipids, Lymph Nodes cytology, Lymphocyte Activation, Mice, Mice, Inbred C57BL, Models, Animal, Skin pathology, Vaccines administration & dosage, beta-Galactosidase immunology, Adjuvants, Immunologic, Antibodies blood, Chitosan immunology, Vaccination, Vaccines immunology

Abstract

The development of safe, novel adjuvants is necessary to maximize the efficacy of new and/or available vaccines. Chitosan is a non-toxic, biocompatible, biodegradable, natural polysaccharide derived from the exoskeletons of crustaceans and insects. Chitosan's biodegradability, immunological activity and high viscosity make it an excellent candidate as a depot/adjuvant for parenteral vaccination. To this end, we explored chitosan solution as an adjuvant for subcutaneous vaccination of mice with a model protein antigen. We found that chitosan enhanced antigen-specific antibody titers over five-fold and antigen-specific splenic CD4+ proliferation over six-fold. Strong increases in antibody titers together with robust delayed-type hypersensitivity (DTH) responses revealed that chitosan induced both humoral and cell-mediated immune responses. When compared with traditional vaccine adjuvants, chitosan was equipotent to incomplete Freund's adjuvant (IFA) and superior to aluminum hydroxide. Mechanistic studies revealed that chitosan exhibited at least two characteristics that may allow it to function as an immune adjuvant. First, the viscous chitosan solution created an antigen depot. More specifically, less than 9% of a protein antigen, when delivered in saline, remained at the injection site after 8 h. However, more than 60% of a protein antigen delivered in chitosan remained at the injection site for 7 days. Second, chitosan induced a transient 67% cellular expansion in draining lymph nodes. The expansion peaked between 14 and 21 days after chitosan injection and diminished as the polysaccharide was degraded. These mechanistic studies, taken together with the enhancement of a vaccine response, demonstrate that chitosan is a promising and safe platform for parenteral vaccine delivery.

Published

2007

39. TRICOM vector based cancer vaccines.

Author

Garnett CT, Greiner JW, Tsang KY, Kudo-Saito C, Grosenbach DW, Chakraborty M, Gulley JL, Arlen PM, Schlom J, and Hodge JW

Subjects

Animals, Clinical Trials as Topic, Combined Modality Therapy, Humans, Neoplasms physiopathology, Neoplasms prevention & control, Neoplasms radiotherapy, Signal Transduction drug effects, T-Lymphocytes immunology, Vaccination, Vaccines, Synthetic therapeutic use, Cancer Vaccines therapeutic use, Immunotherapy methods, Neoplasms therapy

Abstract

For the immune system to mount an effective antitumor T-cell response, an adequate number of T-cells specific for the antigens expressed by the malignancy must be activated [1]. Since most antigens expressed by tumors are "self"-antigens, tumor antigens often lack endogenous immunogenicity and thus do not sufficiently activate T-cells to levels that can mediate tumor eradication. In addition, virtually all solid tumor cells lack the costimulatory molecules necessary to activate tumor-specific T-cells. Approaches that stimulate immune responses to these tumor antigens have the potential to alter this poor responsiveness. This theory has promoted the use of active immunotherapy to generate immune responses against tumor-associated antigens (TAAs) for the treatment of cancer. As one such vaccine strategy, we have utilized poxviruses as delivery vehicles for TAAs in combination with T-cell costimulatory molecules. Initial studies have demonstrated that the insertion of costimulatory molecule trangenes into viral vectors, along with a TAA transgene, greatly enhances the immune response to the antigen. Using this approach, a TRIad of COstimulatory Molecules (TRICOM; B7-1, ICAM-1 and LFA-3) has been shown to enhance T-cell responses to TAAs to levels far greater than any one or two of the costimulatory molecules in combination. In this article, preclinical findings and recent clinical applications of TRICOM-based vaccines as a cancer immunotherapy are reviewed.

Published

2006

40. Costimulatory molecules as adjuvants for immunotherapy.

Author

Hodge JW, Greiner JW, Tsang KY, Sabzevari H, Kudo-Saito C, Grosenbach DW, Gulley JL, Arlen PM, Marshall JL, Panicali D, and Schlom J

Subjects

Animals, B7-1 Antigen metabolism, CD58 Antigens metabolism, Cancer Vaccines, Clinical Trials as Topic, Cytokines metabolism, Genetic Vectors, Granulocyte-Macrophage Colony-Stimulating Factor metabolism, Humans, Intercellular Adhesion Molecule-1 metabolism, Neoplasms therapy, Poxviridae genetics, Signal Transduction, T-Lymphocytes metabolism, Transgenes, Adjuvants, Immunologic therapeutic use, Immunotherapy methods, Neoplasms prevention & control

Abstract

Tumor-associated antigens (TAAs) are by definition either weakly immunogenic or functionally nonimmunogenic. Therefore, efforts have concentrated on the development of vaccine strategies in which the presentation of TAAs to the immune system results in far greater activation of T cells than that occurring naturally in the host. Several strategies are being explored in our laboratory and others to enhance the immunogenicity of TAAs. These are: (a) placing the gene coding for the tumor antigen, as a transgene, into poxvirus vectors. (b) The use of diversified prime and boost vaccine strategies employing two different types of poxvirus vectors. (c) The use of T-cell costimulation; accomplished by placing transgenes for different T-cell costimulation molecules into viral vectors along with the transgenes for the TAA. (d) Altering the amino acid sequence of the TAA to enhance the host immune response. (e) The use of cytokines, and in particular GM-CSF, as a biologic adjuvant. This review will focus on the current state of the use of costimulatory molecules as adjuvants for immunotherapy, and in particular, as immunomodulators for cancer vaccines.

Published

2006

41. Mouse models expressing human carcinoembryonic antigen (CEA) as a transgene: evaluation of CEA-based cancer vaccines.

Author

Hance KW, Zeytin HE, and Greiner JW

Subjects

Animals, Cancer Vaccines genetics, Cancer Vaccines immunology, Carcinoembryonic Antigen genetics, Humans, Mice, Mice, Transgenic, Neoplasms, Experimental immunology, Neoplasms, Experimental secondary, Survival Rate, Cancer Vaccines therapeutic use, Carcinoembryonic Antigen immunology, Disease Models, Animal, Neoplasms, Experimental therapy

Abstract

In recent years, investigators have carried out several studies designed to evaluate whether human tumor-associated antigens might be exploited as targets for active specific immunotherapy, specifically human cancer vaccines. Not too long ago such an approach would have been met with considerable skepticism because the immune system was believed to be a rigid discriminator between self and non-self which, in turn, protected the host from a variety of pathogens. That viewpoint has been challenged in recent years by a series of studies indicating that antigenic determinants of self have not induced absolute host immune tolerance. Moreover, under specific conditions that evoke danger signals, peptides from self-antigen can be processed by the antigen-presenting cellular machinery, loaded onto the major histocompatibility antigen groove to serve as targets for immune intervention. Those findings provide the rationale to investigate a wide range of tumor-associated antigens, including differentiation antigens, oncogenes, and tumor suppressor genes as possible immune-based targets. One of those tumor-associated antigens is the carcinoembryonic antigen (CEA). Described almost 40 years ago, CEA is a M(r) 180-200,000 oncofetal antigen that is one of the more widely studied human tumor-associated antigens. This review will provide: (i) a brief overview of the CEA gene family, (ii) a summary of early preclinical findings on overcoming immune tolerance to CEA, and (iii) the rationale to develop mouse models which spontaneously develop gastrointestinal tumors and express the CEA transgene. Those models have been used extensively in the study of overcoming host immune tolerance to CEA, a self, tumor-associated antigen, and the experimental findings have served as the rationale for the design of early clinical trials to evaluate CEA-based cancer vaccines.

Published

2005

42. Comparative studies of Avipox-GM-CSF versus recombinant GM-CSF protein as immune adjuvants with different vaccine platforms.

Author

Reali E, Canter D, Zeytin H, Schlom J, and Greiner JW

Subjects

Animals, Female, Granulocyte-Macrophage Colony-Stimulating Factor blood, Granulocyte-Macrophage Colony-Stimulating Factor immunology, Mice, Recombinant Proteins administration & dosage, Recombinant Proteins immunology, T-Lymphocytes, Cytotoxic immunology, Avipoxvirus genetics, Granulocyte-Macrophage Colony-Stimulating Factor administration & dosage

Abstract

Granulocyte-macrophage colony-stimulating factor (GM-CSF) is a potent immune stimulant when administered with different vaccines. Optimal use of GM-CSF resides in its ability to act locally to stimulate the proliferation and maturation of professional antigen-presenting cells (APCs) (i.e., Langerhans' cells) at the injection site. GM-CSF was engineered into a replication-incompetent recombinant avian (fowlpox) virus (rF-GM-CSF) and a single subcutaneous injection resulted in a sustained enrichment of activated dendritic cells within the regional draining lymph nodes. Those changes were attributed to local GM-CSF production at the injection site by rF-GM-CSF-infected cells. Studies were carried out in which mice were administered different types of beta-galactosidase (beta-gal)-based vaccines--whole protein, peptide, recombinant poxviruses--and GM-CSF was administered either as a single injection of rF-GM-CSF or four daily bolus injections of the recombinant protein. The use of rF-GM-CSF either improved the immune adjuvant effect, as observed for poxvirus-based vaccines, or was equivalent to rGM-CSF, as observed with the beta-gal protein vaccine. It is important to note that with either the replication-competent (vaccinia) or replication-incompetent (fowlpox) vaccines expressing LacZ, strong CTL responses directed against beta-gal were induced only when rF-GM-CSF was used as the immune adjuvant. Engineering GM-CSF into a recombinant fowlpox virus offers an excellent vehicle for the delivery of this cytokine as an immune adjuvant with specific vaccine platforms. In particular, delivery of GM-CSF via the rF-GM-CSF construct would be preferred over bolus injections of rGM-CSF when used as an immune adjuvant with whole protein or recombinant poxvirus-based vaccines. The study underscores the importance of defining the appropriate delivery form of an immune adjuvant, such as GM-CSF, relative to the immunization strategy to maximize the host immune responses against a specific antigen.

Published

2005

43. Combination of a poxvirus-based vaccine with a cyclooxygenase-2 inhibitor (celecoxib) elicits antitumor immunity and long-term survival in CEA.Tg/MIN mice.

Author

Zeytin HE, Patel AC, Rogers CJ, Canter D, Hursting SD, Schlom J, and Greiner JW

Subjects

Animals, B-Lymphocytes drug effects, B-Lymphocytes immunology, Cancer Vaccines immunology, Carcinoembryonic Antigen genetics, Celecoxib, Colorectal Neoplasms enzymology, Combined Modality Therapy, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors administration & dosage, Diet, Epitopes immunology, Female, Humans, Killer Cells, Natural drug effects, Killer Cells, Natural immunology, Membrane Proteins, Mice, Mice, Inbred C57BL, Mice, Knockout, Prostaglandin-Endoperoxide Synthases, Pyrazoles, T-Lymphocytes drug effects, T-Lymphocytes immunology, Transgenes, Cancer Vaccines administration & dosage, Carcinoembryonic Antigen immunology, Colorectal Neoplasms immunology, Colorectal Neoplasms therapy, Isoenzymes antagonists & inhibitors, Poxviridae immunology, Sulfonamides administration & dosage

Abstract

The present study was designed to determine whether: (a) chronic administration of dietary celecoxib (Celebrex), a potent nonsteroidal anti-inflammatory drug, which targets the cyclooxygenase-2 (COX-2) enzyme, negatively impacts host immunity; and (b) celecoxib can be coupled with a poxvirus-based vaccine to impact tumor burden in a murine tumor model of spontaneous adenomatous polyposis coli. Naive mice fed the celecoxib-supplemented diets developed eosinophilia with lowered plasma prostaglandin E(2) levels and reduced COX-2 mRNA expression levels in their splenic T cells. Responses of splenic T, B, and natural killer cells to broad-based and antigen-specific stimuli were, for the most part, unchanged in those mice as well as COX-2 knockout mice; exceptions included: (a) reduced IFN-gamma production by concanavalin A- or antigen-stimulated T cells; and (b) heightened lipopolysaccharide response of naive B cells from mice fed a diet supplemented with 1000 ppm of celecoxib. When transgenic mice that express the human carcinoembryonic antigen (CEA) gene (CEA transgenic) were bred with mice bearing a mutation in the Apc(Delta850) gene (multiple intestinal neoplasia mice), the progeny (CEA transgenic/multiple intestinal neoplasia) spontaneously develop multiple intestinal neoplasms that overexpress CEA and COX-2. Beginning at 30 days of age, the administration of a diversified prime/boost recombinant CEA-poxvirus-based vaccine regimen or celecoxib (1000 ppm)-supplemented diet reduced the number of intestinal neoplasms by 54% and 65%, respectively. Combining the CEA-based vaccine with the celecoxib-supplemented diet reduced tumor burden by 95% and significantly improved overall long-term survival. Both tumor reduction and improved overall survival were achieved without any evidence of autoimmunity directed at CEA-expressing or other normal tissues. Celecoxib is prescribed for the treatment of familial adenomatous polyposis in humans, and the CEA-based vaccines have been well tolerated and capable of eliciting anti-CEA host immune responses in early clinical studies. The results suggest that the administration of a recombinant poxvirus-based vaccine is compatible with celecoxib, and this combined chemoimmuno-based approach might lead to an additive therapeutic antitumor benefit not only in patients diagnosed with familial adenomatous polyposis but, perhaps, in other preventive settings in which COX-2 overexpression is associated with progression from premalignancy to neoplasia.

Published

2004

44. Combinatorial vaccine strategies and the use of molecular arrays to characterize T-cell activation.

Author

Schlom J, Palena C, Greiner JW, Tsang KY, Grosenbach DW, Sabzevari H, Gulley JL, Arlen PM, Kass E, and Hodge JW

Subjects

Adjuvants, Immunologic administration & dosage, Animals, Antibody Affinity, Antigens, Neoplasm genetics, Cancer Vaccines genetics, Clinical Trials as Topic, Epitopes immunology, Granulocyte-Macrophage Colony-Stimulating Factor administration & dosage, Humans, Mice, Mice, Transgenic, Cancer Vaccines immunology, Lymphocyte Activation, T-Lymphocytes immunology, Vaccines, Synthetic immunology

Published

2004

45. Enhanced expression of lymphotactin by CD8+ T cells is selectively induced by enhancer agonist peptides of tumor-associated antigens.

Author

Palena C, Arlen P, Zeytin H, Greiner JW, Schlom J, and Tsang KY

Subjects

Animals, Antigen Presentation immunology, B-Lymphocytes immunology, CD8-Positive T-Lymphocytes drug effects, CD8-Positive T-Lymphocytes immunology, Carcinoembryonic Antigen immunology, Cell Line, Chemokines, C genetics, Cluster Analysis, Coculture Techniques, Concanavalin A pharmacology, Down-Regulation, Epitopes, T-Lymphocyte chemistry, Gene Expression Regulation drug effects, Gene Expression Regulation immunology, Humans, Immunodominant Epitopes chemistry, Immunodominant Epitopes immunology, Interferon-gamma genetics, Interferon-gamma metabolism, Lymphocyte Activation immunology, Lymphocytes drug effects, Lymphocytes immunology, Mice, Mice, Knockout, Mucin-1 immunology, Oligonucleotide Array Sequence Analysis, Peptide Fragments chemistry, Peptide Fragments pharmacology, Proteins analysis, Spleen cytology, T-Lymphocytes, Cytotoxic immunology, Up-Regulation, Antigens, Neoplasm immunology, CD8-Positive T-Lymphocytes metabolism, Chemokines, C metabolism, Epitopes, T-Lymphocyte immunology, Peptide Fragments immunology

Abstract

Human tumor-associated antigens (TAAs) are weak immunogens. One strategy for increasing the immunogenicity of TAAs is to generate altered peptide ligands. In the studies reported here, microarray technology has been used to compare gene expression profiles of a human T cell line that was derived from the peripheral blood of a cancer patient vaccinated with a carcinoembryonic antigen (CEA)-based vaccine. We compared the gene expression profiles of this CEA-specific CD8 T cell line when (a) stimulated with the native peptide used to derive this line vs. no peptide, and (b) stimulated with its TCR enhancer agonist epitope vs. no peptide. The results demonstrate that the effect on the T cell line, when stimulated with the agonist peptide, is not an enhanced quantitative expression of the same genes or gene sets induced by the native peptide, but is rather a nearly reciprocal upregulation of different gene sets. The gene for the chemokine lymphotactin, which was overexpressed only in T cells stimulated with the agonist peptide, stood out above all others. This finding was extended using other T cell lines, and another set of agonist and native peptides from another TAA. ELISPOT and ELISA assays for lymphotactin confirmed and extended these findings. These studies suggest a potential role for lymphotactin in the T-cell activation processes and subsequent anti-tumor events.

Published

2003

46. Vaccine-based therapy directed against carcinoembryonic antigen demonstrates antitumor activity on spontaneous intestinal tumors in the absence of autoimmunity.

Author

Greiner JW, Zeytin H, Anver MR, and Schlom J

Subjects

Adjuvants, Immunologic pharmacology, Animals, Autoimmunity immunology, B7-1 Antigen genetics, B7-1 Antigen immunology, Body Weight immunology, CD58 Antigens genetics, CD58 Antigens immunology, Cancer Vaccines genetics, Cancer Vaccines therapeutic use, Carcinoembryonic Antigen genetics, Female, Granulocyte-Macrophage Colony-Stimulating Factor pharmacology, Hematocrit, Humans, Immunohistochemistry, Intercellular Adhesion Molecule-1 genetics, Intercellular Adhesion Molecule-1 immunology, Intestinal Neoplasms genetics, Intestinal Neoplasms pathology, Intestinal Neoplasms prevention & control, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Cancer Vaccines immunology, Carcinoembryonic Antigen immunology, Intestinal Neoplasms immunology

Abstract

By virtue of its tissue-specific expression, carcinoembryonic antigen (CEA) is an important self, tumor-associated antigen, which is expressed by different human adenocarcinomas and also serves as a target for active-specific immunotherapy. Similar to humans, CEA expression in mice transgenic for the human CEA gene (CEA.Tg) occurs predominantly along the gastrointestinal tract. CEA.Tg mice were crossed with mice bearing a mutation in the Apc gene (MIN mice), and the CEA.Tg/MIN progeny developed multiple intestinal neoplasms, which overexpress CEA to levels that are reminiscent of those reported for tubulovillous intestinal adenomas from patients. CEA.Tg/MIN mice were vaccinated with an aggressive diversified prime/boost vaccine regimen: (a) a primary vaccine consisting of recombinant vaccinia virus-expressing CEA and a triad of costimulatory molecules (TRICOM): B7.1, ICAM-1, and LFA-3 (rV-CEA-TRICOM); and (b) a booster vaccine using CEA-TRICOM in a recombinant avipox (fowlpox) virus (rF-CEA-TRICOM). Granulocyte/macrophage colony-stimulating factor was administered as a biological adjuvant with all vaccinations, either as a recombinant protein (with rV-CEA-TRICOM) or as a recombinant avipox virus (with rF-CEA-TRICOM). That vaccine regimen generated strong CEA-specific host immune responses in CEA.Tg/MIN mice, which resulted in (a) a delayed onset of adult anemia and weight loss, (b) a significant reduction in the number of intestinal tumors, and (c) improved overall survival. No evidence of autoimmunity directed against normal tissues expressing CEA was observed in mice in which the CEA-based vaccine significantly reduced intestinal tumor load. The CEA.Tg/MIN mice present a clinically relevant model in which different CEA-based vaccine strategies can be tested on the spontaneous onset of intestinal tumorigenesis.

Published

2002

47. Identification of an interferon-gamma-inducible carcinoembryonic antigen (CEA) CD8(+) T-cell epitope, which mediates tumor killing in CEA transgenic mice.

Author

Schmitz J, Reali E, Hodge JW, Patel A, Davis G, Schlom J, and Greiner JW

Subjects

Adenocarcinoma therapy, Animals, Cytotoxicity, Immunologic immunology, Humans, Interferon-gamma immunology, Mice, Mice, Transgenic, Neoplasms, Experimental therapy, Adenocarcinoma immunology, Carcinoembryonic Antigen immunology, Epitopes, T-Lymphocyte immunology, Immunotherapy, Adoptive methods, Interferon-gamma pharmacology, Neoplasms, Experimental immunology, T-Lymphocytes, Cytotoxic immunology

Abstract

This study describes a CD8(+) T-cell line specific for a MHC class I-restricted carcinoembryonic antigen (CEA) epitope, residues 526-533, isolated from CEA transgenic (CEA.Tg) mice immunized with a recombinant vaccinia-CEA vaccine. Incubation of splenocytes from the immune CEA.Tg mice with the CEA(526-533) peptide resulted in the outgrowth of low-avidity CD8(+) T cells, which produced IFN-gamma and mediated perforin-dependent tumor cell lysis. However, the CEA peptide-specific T cells killed CEA-expressing murine colorectal tumor cells only after pretreatment of the targets with murine IFN-gamma (muIFN-gamma), and lysis was H-2D(b)-restricted and involved the Fas-FasL-mediated cytotoxic pathway. When the CEA peptide-specific T cells were used as in vivo effectors in adoptive T-cell transfer studies, muIFN-gamma treatment of the CEA.Tg mice was again required for T-cell-dependent growth suppression of CEA-expressing metastatic tumors. The results indicate that (a) vaccination of mice carrying the human CEA gene with recombinant vaccinia-CEA generates a CEA epitope-specific, CD8-dependent CTL response, (b) CEA, a normal, tissue-specific antigen, can also serve as a target for antitumor immunity after the adoptive transfer of CEA peptide-specific T cells, and (c) muIFN-gamma might be an effective cancer vaccine adjuvant by virtue of its ability to augment the susceptibility of tumor targets to cell-mediated lysis.

Published

2002

48. Carcinoembryonic antigen as a target for specific antitumor immunotherapy of head and neck cancer.

Author

Kass ES, Greiner JW, Kantor JA, Tsang KY, Guadagni F, Chen Z, Clark B, De Pascalis R, Schlom J, and Van Waes C

Subjects

Carcinoembryonic Antigen biosynthesis, Carcinoma, Squamous Cell metabolism, HLA-A2 Antigen immunology, Head and Neck Neoplasms metabolism, Humans, Immunohistochemistry, T-Lymphocytes, Cytotoxic immunology, Carcinoembryonic Antigen immunology, Carcinoma, Squamous Cell immunology, Carcinoma, Squamous Cell therapy, Head and Neck Neoplasms immunology, Head and Neck Neoplasms therapy, Immunotherapy, Adoptive methods

Abstract

Human carcinoembryonic antigen (CEA) is an oncofetal glycoprotein overexpression of which by gastrointestinal carcinomas is well known. Expression of CEA in head and neck cancer (HNC) is not widely recognized. It is important to note that most of these studies used polyclonal antibodies that may have cross-reactivity with CEA-related antigens. Currently, CEA is being evaluated in preclinical and clinical studies as a target for specific immunotherapy against gastrointestinal adenocarcinomas that express the antigen. This study was conducted to evaluate CEA as a potential target for specific immunotherapy against HNC. Immunohistochemical analysis of tumor tissue from 69 cases of squamous cell carcinoma (SCC) of the head and neck using a CEA-specific monoclonal antibody (COL-1) showed the majority to be positive for CEA. Tumor cell lines derived from human HNC were screened for CEA transcripts using nested reverse transcription-PCR. Constitutive expression of CEA mRNA was detected in 7 of 10 HNC lines. CEA protein was detectable in lysates from all 7 of the lines by quantitative fluoroimmunometry. SDS-PAGE/Western blot analysis of cell lysates from these lines showed a COL-1 immunoreactive product with a molecular weight equivalent to that of CEA. Cell surface expression of CEA was low for the SCC lines; however, there was moderate to strong cytoplasmic staining intensity for all of the CEA(+) HNC lines by immunocytochemistry. Additional supportive evidence for CEA as a target was demonstrated by the presence of cytolytic activity of an HLA-A2-restricted/CEA-epitope-specific human CTL against a CEA-overexpressing HNC-derived SCC line. These results suggest that CEA may be considered as a possible target for specific vaccine-mediated immunotherapy against HNCs.

Published

2002

49. Pharmacological modulation of carcinoembryonic antigen in human cancer cells: studies with staurosporine.

Author

Prete SP, Cappelletti D, Baier S, Nasuti P, Guadagni F, De Vecchis L, Greiner JW, Bonmassar E, Graziani G, and Aquino A

Subjects

Cell Membrane drug effects, Cell Membrane metabolism, Cytosol drug effects, Cytosol metabolism, Gene Expression Regulation drug effects, Gene Expression Regulation physiology, Humans, Tumor Cells, Cultured drug effects, Tumor Cells, Cultured metabolism, Carcinoembryonic Antigen biosynthesis, Staurosporine pharmacology

Abstract

Preliminary studies, performed in our laboratory, showed that staurosporine (ST), a protein-kinase (PK) inhibitor, increases the expression of the carcinoembryonic antigen (CEA) in a human colon cancer cell line. The present study explores the cellular and molecular effects of ST on the CEA expression in breast cancer MCF-7 line and in a number of colon cancer cell lines characterized by the different basal levels of the antigen, including two cloned sublines (i.e. C22.20 and C6.6, expressing low and high CEA levels, respectively). In all cases, increase of the CEA expression was observed at drug concentrations devoid of marked cytostatic effects (e.g. 5 nM) and was accompanied by the enhanced CEA shedding in the supernatant. Moreover, the increase of the CEA levels both occurred in the cell membranes and in the cytosolic compartments and appeared to be the result of the enhanced CEA gene transcription. Similar results have been previously obtained with interferon-gamma. However, ST treatment, different from interferon-gamma, did not up-regulate the level of the HLA class I molecules. A preliminary investigation also showed that other PKC inhibitors did not substantially modulate the CEA expression. Therefore, the biochemical mechanism underlying the effect of ST should not be correlated with that involved in the PKC inhibition. The present study suggests that ST and, presumably, its analogs used in the cancer treatment could enhance the CEA expression on neoplastic cells in patients affected by the CEA-positive malignancies. This appears to be of potential clinical interest for the development of new immunotherapeutic or diagnostic approaches based on the pharmacological modulation of this antigenic marker.

Published

2002

50. Detection of blood-borne cells in colorectal cancer patients by nested reverse transcription-polymerase chain reaction for carcinoembryonic antigen messenger RNA: longitudinal analyses and demonstration of its potential importance as an adjunct to multiple serum markers.

Author

Guadagni F, Kantor J, Aloe S, Carone MD, Spila A, D'Alessandro R, Abbolito MR, Cosimelli M, Graziano F, Carboni F, Carlini S, Perri P, Sciarretta F, Greiner JW, Kashmiri SV, Steinberg SM, Roselli M, and Schlom J

Subjects

Adenocarcinoma genetics, Adenocarcinoma immunology, Adenocarcinoma pathology, Adult, Aged, Aged, 80 and over, Antigens, Tumor-Associated, Carbohydrate blood, Antigens, Tumor-Associated, Carbohydrate genetics, Biomarkers, Tumor genetics, CA-19-9 Antigen blood, CA-19-9 Antigen genetics, Carcinoembryonic Antigen biosynthesis, Carcinoembryonic Antigen blood, Colorectal Neoplasms genetics, Colorectal Neoplasms immunology, Colorectal Neoplasms pathology, Female, Humans, Immunohistochemistry, Longitudinal Studies, Male, Middle Aged, Neoplastic Cells, Circulating metabolism, RNA, Messenger genetics, Sensitivity and Specificity, Adenocarcinoma blood, Biomarkers, Tumor blood, Carcinoembryonic Antigen genetics, Colorectal Neoplasms blood, Neoplastic Cells, Circulating immunology, RNA, Messenger blood, Reverse Transcriptase Polymerase Chain Reaction

Abstract

The use of reverse transcription-PCR (RT-PCR) to analyze cells in the blood of cancer patients for the detection of mRNA expressed in tumor cells has implications for both the prognosis and the monitoring of cancer patients for the efficacy of established or experimental therapies. Carcinoembryonic antigen (CEA) is expressed on approximately 95% of colorectal, gastric, and pancreatic tumors, and on the majority of breast, non-small cell lung, and head and neck carcinomas. CEA shed in serum is useful as a marker in only approximately 50% of colorectal cancer patients and rarely is shed by some other carcinoma types. RT-PCR has been used previously to detect CEA mRNA in cells in the blood and lymph nodes of cancer patients. Under the assay conditions validated in the studies reported here, 34 of 51 (67%) patients with different stages of colorectal cancer had blood cells that were positive by RT-PCR for CEA mRNA, whereas none of 18 patients with colonic polyps were positive; 2 of 60 apparently healthy individuals (who were age and sex matched with the carcinoma patients and were part of a colon cancer screening program as controls) were marginally positive. The results of CEA PCR in the blood of the carcinoma patients and the other groups showed strong statistical correlation with the disease (P2 < 0.0001). Analyses were carried out to detect both serum CEA protein levels and CEA mRNA in blood cells of colorectal carcinoma patients by RT-PCR. For all stages of disease, 18 of 51 patients (35%) were positive for serum CEA, whereas 35 of 51 (69%) were positive by RT-PCR. More importantly, only 5 of 23 (20%) of stage B and C colorectal cancer patients were positive for serum CEA, whereas 16 of 23 (70%) were positive by RT-PCR. The use of two other serum markers (CA19.9 and CA72-4) for colorectal cancer in combination with serum CEA scored two additional patients as positive; both were positive by RT-PCR for CEA mRNA. Pilot long-term longitudinal studies conducted before and after surgery identified some patients with CEA mRNA in blood cells that were negative for all serum markers, who eventually developed clinical metastatic disease. The studies reported here are the first to correlate RT-PCR results for CEA mRNA in blood cells with one or more serum markers for patients with different stages of colorectal cancer, and are the first long-term longitudinal studies to use RT-PCR to detect CEA mRNA in blood cells of cancer patients. Larger cohorts will be required in future studies to define the impact, if any, of this technology on prognosis and/or disease monitoring.

Published

2001