Showing total 43 results

1. Anti-angiogenesis: making the tumor vulnerable to the immune system

Author

Arjan W. Griffioen

Subjects

Cancer Research, Angiogenesis, medicine.medical_treatment, Immunology, Biology, Immune system, Immunity, Neoplasms, medicine, Animals, Humans, Immunology and Allergy, Cell adhesion, Neovascularization, Pathologic, Cell adhesion molecule, Soluble cell adhesion molecules, Cancer, Immunotherapy, medicine.disease, Cell biology, Oncology, Symposium Paper, Adhesion molecules, Cell Adhesion Molecules

Abstract

Ongoing angiogenesis has been shown to possess immune suppressive activity through several mechanisms. One of these mechanisms is the suppression of adhesion receptors, such as intercellular adhesion molecule-1, vascular cell adhesion molecule-1 and E-selectin-adhesion molecules involved in leukocyte interactions-on the vascular endothelium. This phenomenon, when happening to the tumor endothelium, supports tumor growth due to escape from immunity. Since angiogenesis has this immune suppressive effect, it has been hypothesized that inhibition of angiogenesis may circumvent this problem. In vitro and in vivo data now show that several angiogenesis inhibitors are able to normalize endothelial adhesion molecule expression in tumor blood vessels, restore leukocyte vessel wall interactions, and enhance the inflammatory infiltrate in tumors. It is suggested that such angiogenesis inhibitors can make tumors more vulnerable for the immune system and may therefore be applied to facilitate immunotherapy approaches for the treatment of cancer.

2. Cancer treatment: the combination of vaccination with other therapies

Author

Inge Marie Svane, Rikke Sørensen, Mads Hald Andersen, Per thor Straten, David Schrama, and Jürgen C. Becker

Subjects

Cancer Research, Population, Immunology, Antineoplastic Agents, Cancer Vaccines, Immune system, Antigen, Neoplasms, medicine, Cytotoxic T cell, Chemotherapy, Animals, Humans, Immunology and Allergy, Conventional treatment, education, Cancer, education.field_of_study, business.industry, Vaccination, FOXP3, medicine.disease, Combined Modality Therapy, Oncology, Symposium Paper, Cancer cell, Combination, Cancer research, business

Abstract

Harnessing of the immune system by the development of ‘therapeutic’ vaccines, for the battle against cancer has been the focus of tremendous research efforts over the past two decades. As an illustration of the impressive amounts of data gathered over the past years, numerous antigens expressed on the surface of cancer cells, have been characterized. To this end, recent years research has focussed on characterization of antigens that play an important role for the growth and survival of cancer cells. Anti-apoptotic molecules like survivin that enhance the survival of cancer cells and facilitate their escape from cytotoxic therapies represent prime vaccination candidates. The characterization of a high number of tumor antigens allow the concurrent or serial immunological targeting of different proteins associated with such cancer traits. Moreover, while vaccination in itself is a promising new approach to fight cancer, the combination with additional therapy could create a number of synergistic effects. Herein we discuss the possibilities and prospects of vaccination when combined with other treatments. In this regard, cell death upon drug exposure may be immunogenic or non-immunogenic depending on the specific chemotherapeutics. Also, chemotherapy represents one of several options available for clearance of CD4+ Foxp3+ regulatory T cells. Moreover, therapies based on monoclonal antibodies may have synergistic potential in combination with vaccination, both when used for targeting of tumor cells and endothelial cells. The efficacy of therapeutic vaccination against cancer will over the next few years be studied in settings taking advantage of strategies in which vaccination is combined with other treatment modalities. These combinations should be based on current knowledge not only regarding the biology of the cancer cell per se, but also considering how treatment may influence the malignant cell population as well as the immune system.

3. TARC and RANTES enhance antitumor immunity induced by the GM-CSF-transduced tumor vaccine in a mouse tumor model.

Author

Inoue, Hiroyuki, Iga, Mutsunori, Meng Xin, Asahi, Saori, Nakamura, Takafumi, Kurita, Ryo, Nakayama, Masaharu, Nakazaki, Yukoh, Takayama, Koichi, Nakanishi, Yoichi, and Tani, Kenzaburo

Subjects

GRANULOCYTE-macrophage colony-stimulating factor, GENETIC transduction, VACCINATION, IMMUNITY, IMMUNOLOGY, LABORATORY mice

Abstract

Transduction of the granulocyte-macrophage colony stimulating factor (GM-CSF) gene into mouse tumor cells abrogates their tumorigenicity in vivo. Our previous report demonstrated that gene transduction of GM-CSF with either TARC or RANTES chemokines suppressed in vivo tumor formation. In this paper, we examined whether the addition of either recombinant TARC or RANTES proteins to irradiated GM-CSF-transduced tumor vaccine cells enhanced antitumor immunity against established mouse tumor models to examine its future clinical application. Three million irradiated WEHI3B cells retrovirally transduced with murine GM-CSF cDNA in combination with either recombinant TARC or RANTES were subcutaneously inoculated into syngeneic WEHI3B-preestablished BALB/c mice. Vaccinations were well tolerated. Mice treated with GM-CSF-transduced cells and the chemokines demonstrated significantly longer survival than mice treated with GM-CSF-transduced cells alone. Splenocytes harvested from mice treated with the former vaccines produced higher levels of IL-4, IL-6, IFN-γ, and TNF-α, suggesting enhanced innate and adaptive immunity. Immunohistochemical analysis of tumor sections after vaccination revealed a more significant contribution of CD4+ and CD8+ T cells to tumor repression in the combined vaccine groups than controls. TARC and RANTES enhance the immunological antitumor effect induced by GM-CSF in mouse WEHI3B tumor models and may be clinically useful. [ABSTRACT FROM AUTHOR]

Published

2008

4. Anti-inflammatory pretreatment enables an efficient dendritic cell-based immunotherapy against established tumors.

Author

Chiarella, Paula, Vulcano, Marisa, Bruzzo, Juan, Vermeulen, Mónica, Vanzulli, Silvia, Maglioco, Andrea, Camerano, Gabriela, Palacios, Víctor, Fernández, Gabriela, Brando, Romina Fernández, Isturiz, Martín A., Dran, Graciela I., Bustuoabad, Oscar D., and Ruggiero, Raúl A.

Subjects

TUMOR treatment, ANTI-inflammatory agents, DENDRITIC cells, IMMUNOTHERAPY, IMMUNOLOGY

Abstract

Although animals can be immunized against the growth of some tumor implants, most of the attempts to use immunotherapy to cause the regression of animal and human tumors once they have become established have been disappointing even when strongly immunogenic tumors were used as target. In this paper, we demonstrate that the failure to achieve an efficient immunological treatment against an established strongly immunogenic murine fibrosarcoma was paralleled with the emergence of a state of immunological unresponsiveness (immunological eclipse) against tumor antigens observed when the tumor surpassed the critical size of 500 mm3. In turn, the onset of the immunological eclipse was coincidental with the onset of a systemic inflammatory condition characterized by a high number of circulating and splenic polymorphonucleated neutrophils (PMN) displaying activation and Gr1+Mac1+ phenotype and an increasing serum concentration of the pro-inflammatory cytokines TNF-α, IL-1β and IL-6 cytokines and C-reactive protein (CRP) and serum A amyloid (SAA) phase acute proteins. Treatment of tumor-bearing mice with a single low dose (0.75 mg/kg) of the synthetic corticoid dexamethasone (DX) significantly reduced all the systemic inflammatory parameters and simultaneously reversed the immunological eclipse, as evidenced by the restoration of specific T-cell-dependent concomitant immunity, ability of spleen cells to transfer anti-tumor activity and recovery of T-cell signal transduction molecules. Two other anti-inflammatory treatments by using indomethacin or dimeric TNF-α receptor, also partially reversed the immunological eclipse although the effect was not as striking as that observed with DX. The reversion of the immunological eclipse was not enough on its own to inhibit the primary growing tumor. However, when we used the two-step strategy of inoculating DX to reverse the eclipse and then dendritic cells loaded with tumor antigens (DC) as an immunization booster, a significant inhibition of the growth of both established tumors and remnant tumor cells after excision of large established tumors was observed, despite the fact that the vaccination alone (DC) had no effect or even enhanced tumor growth in certain circumstances. The two-step strategy of tumor immunotherapy that we present is based on the rationale that it is necessary to eliminate or ameliorate the immunological eclipse as a precondition to allow an otherwise ineffective anti-tumor immunological therapy to have a chance to be successful. [ABSTRACT FROM AUTHOR]

Published

2008

5. Expression of NK-associated receptors on cytotoxic T cells from melanoma patients: a two-edged sword?

Author

Tarazona, Raquel, Casado, Javier G., Soto, Rocío, DelaRosa, Olga, Peralbo, Esther, Rioja, Luis, Peña, José, and Solana, Rafael

Subjects

IMMUNOLOGY, NEUROENDOCRINE tumors, LYMPHOCYTES, MELANOMA

Abstract

The coexistence of tumor progression with a tumor-specific immune response constitutes a major paradox of tumor immunity. During the last decade, the presence of cytotoxic T lymphocytes (CTLs) recognising melanoma-associated antigens has been unequivocally demonstrated in numerous different in vivo and in vitro models. However, most often these melanoma-specific T lymphocytes do not control tumor growth. Several mechanisms that involve changes in melanoma phenotype and/or in T-cell differentiation and function could explain the inability of the immune response to control melanoma. In the last few years it has been demonstrated that cellular cytotoxicity is the result of a balance between activating signals triggered by the TCR and costimulatory molecules and inhibitory signals triggered by inhibitory receptors expressed by the CTL. Because the final outcome of the immune response against melanoma depends on the balance between activating and inhibitory signals, the expression de novo on melanoma cells of ligands for inhibitory NKRs and the down-regulation of costimulatory molecules may favor the escape of tumor cells from immunosurveillance. In this paper we review how altered expression of molecules required for T-cell costimulation could result in impaired lysis of melanoma. The modulation of antimelanoma T-cell responses by a group of receptors originally described on NK cells (NK-associated receptors) but which are now known also to be expressed on a subset of cytolytic effector cells is reviewed. We hypothesize that the expression of ligands for NKRs on melanoma cells may contribute to T-cell–mediated immune responses against melanoma either enhancing or inhibiting activation and differentiation to effector cells. Blocking inhibitory receptors or increasing activating receptors could result in new strategies to improve T-cell–mediated rejection of melanoma. [ABSTRACT FROM AUTHOR]

Published

2004

6. γ-Ray irradiation induces B7.1 costimulatory molecule neoexpression in various murine tumor cells.

Author

Morel, Arnaud, Fernandez, Nadine, de La Coste, A., Haddada, Hédi, Viguier, Mireille, Polla, Barbara S., Antoine, Bénédicte, and Kahn, A.

Abstract

The use of gene-modified tumor cells as a strategy for active immunotherapy is currently undergoing intensive fundamental and clinical research. Most clinical trials use γ-ray-irradiated tumor cells as vaccine, although little is known about the effects of irradiation on the immunogenicity of tumor cells. In particular, no data have been reported so far concerning the effects of γ-ray irradiation on the expression of B7 molecules in tumor cells. In this paper, we show a neoexpression of the B7.1 molecule after γ-ray irradiation in tumor cell lines from different tissues, while the B7.2 molecule remains unexpressed in all the cell lines tested. Furthermore, the induction of B7.1 molecule membrane expression after irradiation is shown to result from the neoexpression of B7.1 mRNA, and to be reproduced with H2O2 oxidative stress. These data could explain the enhanced immunogenicity of many tumor cells after irradiation, and could lead to new immunotherapy protocols. [ABSTRACT FROM AUTHOR]

Published

1998

7. CIMT meets Strategies for Immune Therapy: Mainz, Germany, 04–05 May 2006.

Author

Gouttefangeas, C., Britten, C., Badalians, E., and Pawelec, G.

Subjects

*CONFERENCES & conventions, *IMMUNOTHERAPY, *ONCOLOGY conferences, *IMMUNOLOGY, *TUMOR antigens, CONGRESSES

Abstract

Information about several papers discussed during the fourth international meeting of the Association for Immunotherapy of Cancer held in Germany is presented. Newly discovered tumor-associated antigens for antibody and T-cell based therapies were delivered and demonstrated. Various approaches and techniques targeting candidate antigens in immunotherapy were also discussed.

Published

2007

8. Comparison of the TCR ζ-chain with the FcR γ-chain in chimeric TCR constructs for T cell activation and apoptosis.

Author

Ren-Heidenreich, Lifen, Mordini, Ryan, Hayman, Thomas G., Siebenlist, Ruth, and LeFever, Ann

Subjects

T cell receptors, CELL receptors, T cells, CANCER treatment, CANCER, IMMUNOTHERAPY, IMMUNOLOGY

Abstract

A promising strategy for cancer treatment is adoptive gene therapy/immunotherapy by genetically modifying T cells with a chimeric T cell receptor (cTCR). When transduced T cells (T-bodies) specifically bind to tumor antigens through cTCR, they will become cytotoxic T lymphocytes (CTL) and lyse the tumor cells in a non-major histocompatibility complex (MHC)-restricted manner. Both the FcR γ-chain and the TCR ζ-chain have been used to construct such cTCR, and both have shown specific cytolytic functions against tumor cells. However, most researchers believe that the ζ-chain generates stronger cytolytic activities against tumor than the γ-chain and therefore would be a better candidate for cTCR construction. On the other hand, because of the lack of costimulation signaling in such constructs, the T-body might cause activation-induced T cell death (AICD) when bound to tumor antigens. Therefore, one can argue that the γ-chain might generate less AICD than the ζ-chain because the γ-chain has only one immunoreceptor tyrosine-based activation motif (ITAM), and the cytolytic activities can be therefore recycled. Two cTCR, GAHγ and GAHζ, were constructed and evaluated for cytokine production, specific cytolytic function and AICD in T-bodies after exposure to tumor cells. Using EGP-2-positive LS174T colorectal carcinoma cells as targets, there was no substantial difference observed between a γ-chain or ζ-chain as the T-body signaling moiety in terms of specific cytolytic functions and induced cytokine production. This paper also demonstrates that, in the absence of a costimulation system, tumor antigen may not trigger apoptosis of T cells transduced with a cTCR carrying either an FcR γ-chain or a TCR ζ-chain. These observations challenge current ideas about the role of ITAM in T cell activation. [ABSTRACT FROM AUTHOR]

Published

2002

9. Immunologic factors involved in the malignant transformation of endometriosis to endometriosis-associated ovarian carcinoma.

Author

Leenen, S., Hermens, M., de Vos van Steenwijk, P. J., Bekkers, R. L. M., and van Esch, E. M. G.

Subjects

IMMUNOMODULATORS, ENDOMETRIOSIS, CARCINOMA, KILLER cells, TREATMENT effectiveness

Abstract

Introduction: Endometriosis is a risk factor for low-grade serous, clear cell, and endometroid ovarian carcinoma. In both endometriosis and ovarian carcinoma, immunological factors are associated with clinical outcome. Chronic inflammation in endometriosis may be linked to tumorigenesis, but exact processes contributing to endometriosis-associated ovarian carcinoma remain unknown. This review aims to describe potential immunological factors involved in the malignant transformation of endometriosis into ovarian carcinoma. Methods: PubMed and Embase were searched from inception up to October 2020 for studies comparing immunological processes in endometriosis and endometriosis-associated ovarian carcinoma. Results: Detailed analysis of immune components in the malignant transformation of endometriosis into endometriosis-associated ovarian carcinoma is lacking. Altered levels of chemokines and cytokines as IL-6, IL-8, IL-10, and TNF-α are reported and the function, number and polarization of NK cells, dendritic cells, and monocytes differ between endometriosis and associated ovarian carcinoma compared to healthy tissue. In addition, altered inflammasome and complement systems, indicate a role for the immune system in the carcinogenesis of endometriosis. Conclusion: Chronic inflammation in endometriosis may potentially drive inflammation-induced carcinogenesis in endometriosis-associated ovarian carcinoma. Exact immunological pathways and cellular processes remain unknown and require more thorough investigation. [ABSTRACT FROM AUTHOR]

Published

2021

10. Acknowledgement to Reviewers in 2004.

Subjects

PERIODICAL publishing, IMMUNOLOGY, IMMUNOTHERAPY

Abstract

The article presents an index related to referees, who provide the authors with valuable criticism on the content and form of the papers that appear in the 2005 issue of the "Cancer Immunology Immunotherapy." Some of the referees are H. Aguila, E. Alvarez, R.J. Amato, E. Angevin, V.N. Anisimov, P. Arbuthnot, M. Aringer, H.K. Avraham, U. Bachrach and M. Baer.

Published

2005

11. Clinical evaluation of macrophages in cancer: role in treatment, modulation and challenges.

Author

Tremble, Liam, Forde, Patrick, and Soden, Declan

Subjects

TUMOR immunology, T cells, IMMUNOSUPPRESSION, MACROPHAGES, CANCER treatment

Abstract

The focus of immunotherapeutics has been placed firmly on anti-tumour T cell responses. Significant progress has been made in the treatment of both local and systemic malignancies, but low response rates and rising toxicities are limiting this approach. Advancements in the understanding of tumour immunology are opening up a new range of therapeutic targets, including immunosuppressive factors in the tumour microenvironment. Macrophages are a heterogeneous group of cells that have roles in innate and adaptive immunity and tissue repair, but become co-opted by tumours to support tumour growth, survival, metastasis and immunosuppression. Macrophages also support tumour resistance to conventional therapy. In preclinical models, interference with macrophage migration, macrophage depletion and macrophage re-education have all been shown to reduce tumour growth and support anti-tumour immune responses. Here we discuss the role of macrophages in prognosis and sensitivity to therapy, while examining the significant progress which has been made in modulating the behaviour of these cells in cancer patients. [ABSTRACT FROM AUTHOR]

Published

2017

12. Mass spectrometric analysis of the HLA class I peptidome of melanoma cell lines as a promising tool for the identification of putative tumor-associated HLA epitopes.

Author

Gloger, Andreas, Ritz, Danilo, Fugmann, Tim, and Neri, Dario

Subjects

CANCER immunotherapy, HLA histocompatibility antigens, TUMOR diagnosis, MELANOMA, TUMOR antigens, MASS spectrometry, IMMUNOLOGY

Abstract

Melanoma is one of the most immunogenic tumors, and extensive lists of potential tumor rejection antigens have been collected during the last decades. By isolating human leukocyte antigen (HLA) class I complexes from five melanoma cell lines (FM-82, FM-93/2, Mel-624, MeWo and SK-Mel-5) and sequencing HLA-eluted peptides by mass spectrometry, we identified over 10,000 unique peptides with high confidence. The majority of the peptides were 8-11 amino acids in length and were predicted to bind to the respective HLA alleles. Over 250 epitopes, corresponding to previously described tumor-associated antigens, were identified, suggesting that HLA peptidome analysis may facilitate the characterization of putative tumor rejection antigens. MeWo and SK-Mel-5 cell lines were further interrogated for neo-epitopes, revealing one peptide from MeWo cells carrying an amino acid mutation. We also observed a remarkable overlap between A*03:01 peptides eluted from Mel-624 cells and A*03:01 peptides recovered from soluble HLA complexes purified from two melanoma patients, shedding light on the similarity of the HLA peptidome in cell lines and in patient-derived material. The reliable characterization of the HLA class I peptidome in melanoma promises to facilitate the identification of tumor rejection antigens and the development of immunotherapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2016

13. Acknowledgement.

Subjects

IMMUNOLOGY, PUBLISHED articles, PUBLISHING, PERIODICAL articles, PERIODICAL publishing, PUBLICATIONS

Published

2016

14. Orchestrating an immune response against cancer with engineered immune cells expressing αβTCRs, CARs, and innate immune receptors: an immunological and regulatory challenge.

Author

Witte, Moniek, Kierkels, Guido, Straetemans, Trudy, Britten, Cedrik, and Kuball, Jürgen

Subjects

IMMUNE response, CANCER immunotherapy, NATURAL immunity, IMMUNOLOGY, HOMOGRAFTS, STEM cell transplantation

Abstract

Over half a century ago, the first allogeneic stem cell transplantation (allo-SCT) initiated cellular immunotherapy. For several decades, little progress was made, and toxicity of allo-SCT remained a major challenge. However, recent breakthroughs have opened new avenues to further develop this modality and to provide less toxic and equally efficient interventions for patients suffering from hematological or solid malignancies. Current novel cellular immune interventions include ex vivo expansion and adoptive transfer of tumor-infiltrating immune cells or administration of drugs which antagonize tolerizing mechanisms. Alternatively, transfer of immune cells engineered to express defined T cell receptors (TCRs) and chimeric antigen receptors (CARs) has shown its potential. A valuable addition to 'engineered' adaptive immunity has emerged recently through the improved understanding of how innate immune cells can attack cancer cells without substantial side effects. This has enabled the development of transplantation platforms with limited side effects allowing early immune interventions as well as the design of engineered immune cells expressing innate immune receptors. Here, we focus on innate immune interventions and their orchestration with TCR- and CAR-engineered immune cells. In addition, we discuss how the exploitation of the full potential of cellular immune interventions is influenced by regulatory frameworks. Finally, we highlight and discuss substantial differences in the current landscape of clinical trials in Europe as compared to the USA. The aim is to stimulate international efforts to support regulatory authorities and funding agencies, especially in Europe, to create an environment that will endorse the development of engineered immune cells for the benefit of patients. [ABSTRACT FROM AUTHOR]

Published

2015

15. In memory of Professor Robert W. Baldwin: Editor-in-Chief of Cancer Immunology, Immunotherapy 1976-2003.

Subjects

OBITUARIES, COLLEGE teachers, CANCER immunotherapy, IMMUNOLOGY

Published

2012

16. Acknowledgement.

Subjects

PERIODICAL reviews, ACKNOWLEDGEMENTS (Academic dissertations), IMMUNOTHERAPY, IMMUNOLOGY, CANCER, PUBLISHING

Published

2012

17. Human NK cells in acute myeloid leukaemia patients: analysis of NK cell-activating receptors and their ligands.

Author

Sanchez-Correa, Beatriz, Morgado, Sara, Gayoso, Inmaculada, Bergua, Juan, Casado, Javier, Arcos, Maria, Bengochea, Maria, Duran, Esther, Solana, Rafael, and Tarazona, Raquel

Subjects

ACUTE myeloid leukemia treatment, KILLER cells, LIGANDS (Biochemistry), LEUKEMIA, CELL receptors, CELLULAR recognition, IMMUNOLOGY, PATIENTS

Abstract

Natural killer (NK) cell activation is strictly regulated to ensure that healthy cells are preserved, but tumour-transformed or virus-infected cells are recognized and eliminated. To carry out this selective killing, NK cells have an ample repertoire of receptors on their surface. Signalling by inhibitory and activating receptors by interaction with their ligands will determine whether the NK cell becomes activated and kills the target cell. Here, we show reduced expression of NKp46, NKp30, DNAM-1, CD244 and CD94/NKG2C activating receptors on NK cells from acute myeloid leukaemia patients. This reduction may be induced by chronic exposure to their ligands on leukaemic blasts. The analysis of ligands for NK cell-activating receptors showed that leukaemic blasts from the majority of patients express ligands for NK cell-activating receptors. DNAM-1 ligands are frequently expressed on blasts, whereas the expression of the NKG2D ligand MICA/B is found in half of the patients and CD48, a ligand for CD244, in only one-fourth of the patients. The decreased expression of NK cell-activating receptors and/or the heterogeneous expression of ligands for major receptors on leukaemic blasts can lead to an inadequate tumour immunosurveillance by NK cells. A better knowledge of the activating receptor repertoire on NK cells and their putative ligands on blasts together with the possibility to modulate their expression will open new possibilities for the use of NK cells in immunotherapy against leukaemia. [ABSTRACT FROM AUTHOR]

Published

2011

18. Monocyte-derived DC maturation strategies and related pathways: a transcriptional view.

Author

Castiello, Luciano, Sabatino, Marianna, Jin, Ping, Clayberger, Carol, Marincola, Francesco, Krensky, Alan, and Stroncek, David

Subjects

MONOCYTES, DENDRITIC cells, IMMUNE response, GENETIC transcription, DNA fingerprinting, PHENOTYPES, IMMUNOLOGY

Abstract

Ex vivo production of highly stimulator mature dendritic cells (DCs) for cellular therapy has been used to treat different pathological conditions with the aim of inducing a specific immune response. In the last decade, several protocols have been developed to mature monocyte-derived DCs: each one has led to the generation of DCs showing different phenotypes and stimulatory abilities, but it is not yet known which one is the best for inducing effective immune responses. We grouped several different maturation protocols according to the downstream pathways they activated and reviewed the shared features at a transcriptomic level to reveal the potential of DCs matured by each protocol to develop Th-polarized immune responses. [ABSTRACT FROM AUTHOR]

Published

2011

19. Acknowledgement.

Subjects

CANCER immunotherapy, IMMUNOLOGY, MEDICAL communication, AUTHORS

Published

2011

20. A phase II study of the cancer vaccine TG4010 alone and in combination with cytokines in patients with metastatic renal clear-cell carcinoma: clinical and immunological findings.

Author

Oudard, Stéphane, Rixe, Olivier, Beuselinck, Benoit, Linassier, Claude, Banu, Eugeniu, Machiels, Jean-Pascal, Baudard, Marion, Ringeisen, François, Velu, Thierry, Lefrere-Belda, Marie-Aude, Limacher, Jean-Marc, Fridman, W., Azizi, Michel, Acres, Bruce, and Tartour, Eric

Subjects

CANCER vaccines, CYTOKINES, METASTASIS, RENAL cell carcinoma, IMMUNOLOGY, IMMUNE response, SURVIVAL analysis (Biometry)

Abstract

MUC1 over-expression in renal clear-cell carcinoma (RCC) is associated with poor prognosis. This phase II study determined the efficacy and tolerability of TG4010, a cancer vaccine based on a modified vaccinia virus expressing MUC1 and interleukin-2, in combination with cytokines, as first-line therapy in metastatic RCC. Thirty-seven patients with progressive, MUC1-positive RCC received TG4010 10 pfu/inj weekly for 6 weeks, then every 3 weeks until progression, when TG4010 was continued in combination with interferon-α2a and interleukin-2. Assessments included clinical response (primary endpoint), safety, time to treatment failure (TTF), overall survival (OS), and immune response. No objective clinical responses occurred. Five of the 27 evaluable patients (18%) had stable disease for >6 months with TG4010 alone and six of 20 patients (30%) had stable disease for >6 months with TG4010 plus cytokines. Median TTF was 4.1, 3.6, and 9.3 months for monotherapy, combination therapy, and overall, respectively. Median OS was 19.3 months for all patients and 22.4 months combination therapy recipients. The most frequent TG4010-related adverse events were minor-to-moderate injection-site reactions, fatigue, and flu-like symptoms. Six of 28 patients showed a MUC1 CD4 T cell proliferative response during therapy. Anti-MUC1 CD8 T cells were detected before and after therapy in 3 and 4 patients, respectively. MUC1-specific CD8 T cell responses were associated with longer survival. Therapy with TG4010 plus cytokines appears to be feasible and well tolerated in patients with metastatic RCC. However, these data should be interpreted with caution, as additional prospective studies are necessary to clarify the clinical efficacy of this therapy. [ABSTRACT FROM AUTHOR]

Published

2011

21. Ninth international conference on progress in vaccination against cancer (PIVAC 9), 8–10 October 2009, Sofia, Bulgaria.

Author

Naumova, Elissaveta, McArdle, Stéphanie, and Pawelec, Graham

Subjects

CONFERENCES & conventions, CANCER vaccines, CANCER research, IMMUNOLOGY, CANCER immunotherapy

Abstract

The article presents information on the Ninth International Conference on Progress in Vaccination Against Cancer (PIVAC 9), organized during October 8-10, 2009, in SoWa, Bulgaria. The purpose of the annual event is to highlight new research related to cancer immunology and immunotherapy. Different sessions of the convention focused on tolerance, immunosuppression and tumour escape; interactions between chemotherapy and immunotherapy; and ways to improve cancer vaccines.

Published

2010

22. Acknowledgement.

Subjects

IMMUNOLOGY, DEDICATIONS

Abstract

People who author would like to thank for their assistance in the creation of the journal "Cancer Immunology Immunotherapy" are mentioned.

Published

2009

23. The European searchable tumour line database.

Author

Robinson, James, Roberts, Chrissy h., Dodi, I. Anthony, Madrigal, J. Alejandro, Pawelec, Graham, Wedel, Lilly, and Marsh, Steven G. E.

Subjects

ONLINE databases, MELANOMA, CELL lines, NEUROENDOCRINE tumors, TUMOR treatment, IMMUNOGLOBULINS, GENE expression, IMMUNOLOGY

Abstract

The European Searchable Tumour line Database (ESTDAB) () is a freely available and fully searchable database of melanoma-derived cell lines, which have been characterised for over 250 immunologically relevant markers by a consortium of European scientists. The database is linked to a cell bank, which can provide melanoma cell lines to non-profit investigators for a nominal handling charge. All cells are fully HLA typed at the genomic and surface expression levels. The expression of a number of surface antigens, apoptotic markers, tumour-associated antigens and extracellular matrix proteins has also been determined. Cytokine secretion has been tested and polymorphisms in cytokine genes have been identified. Glycans at the cell surface were identified and glycosyltransferase activity quantified. Cell lines with a particular constellation of these parameters can be sought online via the ESTDAB interface, which is included as part of the Immuno-Polymorphism Database (IPD) section of the European Bioinformatics Institute’s (EBI) website. [ABSTRACT FROM AUTHOR]

Published

2009

24. Expression of adhesion molecules and ligands for activating and costimulatory receptors involved in cell-mediated cytotoxicity in a large panel of human melanoma cell lines.

Author

Casado, Javier G., Pawelec, Graham, Morgado, Sara, Sanchez-Correa, Beatriz, Delgado, Elena, Gayoso, Inmaculada, Duran, Esther, Solana, Rafael, and Tarazona, Raquel

Subjects

CELL adhesion molecules, NEUROENDOCRINE tumors, CELL lines, THERAPEUTICS, IMMUNOLOGY

Abstract

Knowledge of the interactions between MHC-unrestricted cytotoxic effector cells and solid tumour cells is essential for introducing more effective NK cell-based immunotherapy protocols into clinical practise. Here, to begin to obtain an overview of the possible universe of molecules that could be involved in the interactions between immune effector cells and melanoma, we analyse the surface expression of adhesion and costimulatory molecules and of ligands for NK-activating receptors on a large panel of cell lines from the “European Searchable Tumour Cell Line and Data Bank” (ESTDAB, ) and discuss their potential role in the immune response against this tumour. We show that most melanoma cell lines express not only adhesion molecules that are likely to favour their interaction with cells of the immune system, but also their interaction with endothelial cells potentially increasing their invasiveness and metastatic capacity. A high percentage of melanoma cell lines also express ligands for the NK-activating receptor NKG2D; whereas, the majority express MICA/B molecules, ULBP expression, however, was rarely found. In addition to these molecules, we also found that CD155 (poliovirus receptor, PVR) is expressed by the majority of melanoma cell lines, whereas CD112 (Nectin-2) expression was rare. These molecules are DNAM-1 ligands, a costimulatory molecule involved in NK cell-mediated cytotoxicity and cytokine production that also mediates costimulatory signals for triggering naïve T cell differentiation. The phenotypical characterisation of adhesion molecules and ligands for receptors involved in cell cytotoxicity on a large series of melanoma cell lines will contribute to the identification of markers useful for the development of new immunotherapy strategies. [ABSTRACT FROM AUTHOR]

Published

2009

25. Dendritic cell vaccination and immune monitoring.

Author

Aarntzen, E. H. J. G., Figdor, C. G., Adema, G. J., Punt, C. J. A., and De Vries, I. J. M.

Subjects

DENDRITIC cells, MELANOMA, TUMOR antigens, CANCER vaccines, IMMUNOLOGY, T cells, PATIENTS

Abstract

We exploited dendritic cells (DC) to vaccinate melanoma patients. We recently demonstrated a statistical significant correlation between favorable clinical outcome and the presence of vaccine-related tumor antigen-specific T cells in delayed type hypersensitivity (DTH) skin biopsies. However, favorable clinical outcome is only observed in a minority of the treated patients. Therefore, it is obvious that current DC-based protocols need to be improved. For this reason, we study in small proof of principle trials the fate, interactions and effectiveness of the injected DC. [ABSTRACT FROM AUTHOR]

Published

2008

26. Tumor destruction using electrochemotherapy followed by CpG oligodeoxynucleotide injection induces distant tumor responses.

Author

Roux, Stephan, Bernat, Claire, Al-Sakere, Bassim, Ghiringhelli, François, Opolon, Paule, Carpentier, Antoine F., Zitvogel, Laurence, Mir, Lluis M., and Robert, Caroline

Subjects

DRUG therapy, TUMORS, TUMOR antigens, IMMUNITY, IMMUNE response, IMMUNOLOGY

Abstract

Electrochemotherapy (ECT) is an effective local therapy of human cutaneous cancers but has no effect on distant untreated tumors. We addressed whether tumor-associated antigens released after ECT could induce an efficient systemic immunity when associated with an appropriate immunoadjuvant. We first studied the nature of the cellular recruitment and the expression of various toll-like receptors (TLRs) in tumors treated by ECT. We found that ECT induced a massive recruitment of CD11c and CD11b positive cells in the tumors and a strong increase of TLR9 expression. We then tested antitumor effects of the combination: ECT followed by TLR-9 ligands, CpG oligodeoxynucleotides (CpG ODN), in three murine tumor models. We found that this combination triggered both potent local synergistic antitumor effects, on the ipsi-lateral ECT-treated tumor, and more interestingly, a systemic antitumor response on the contra-lateral untreated tumor, in the three models. The systemic protection was T-cell dependent as it was not observed in nude littermates. The combination induced tumor-specific T cell effectors in the tumor-draining lymph nodes and in the spleen which secreted significantly more gamma-interferon upon activation than with ECT or CpG ODN alone. Our data show that ECT and CpG ODN synergize and induce a significant increase of the local effect and a systemic T-dependent antitumor response. Such combination constitutes a potential innovative vaccination strategy using in situ tumor-associated antigens that could eventually be translated into the clinic. [ABSTRACT FROM AUTHOR]

Published

2008

27. Pilot study of mutant ras peptide-based vaccine as an adjuvant treatment in pancreatic and colorectal cancers.

Author

Toubaji, Antoun, Achtar, Moujahed, Provenzano, Maurizio, Herrin, Vincent E., Behrens, Robert, Hamilton, Michael, Bernstein, Sarah, Venzon, David, Gause, Barry, Marincola, Francesco, and Khleif, Samir N.

Subjects

RAS oncogenes, IMMUNOTHERAPY, ADJUVANT treatment of cancer, PANCREATIC cancer, COLON cancer, IMMUNE response, IMMUNOLOGY

Abstract

There is mounting evidence describing the immunosuppressive role of bulky metastatic disease, thus countering the therapeutic effects of tumor vaccine. Therefore, adjuvant immunotherapy may have a better impact on clinical outcome. In this phase II clinical trial, we aimed to test the feasibility of using a specific mutant ras peptide vaccine as an adjuvant immunotherapy in pancreatic and colorectal cancer patients. Twelve patients with no evidence of disease (NED), five pancreatic and seven colorectal cancer patients were vaccinated subcutaneously with 13-mer mutant ras peptide, corresponding to their tumor’s ras mutation. Vaccinations were given every 4 weeks, up to a total of six vaccines. No serious acute or delayed systemic side effects were seen. We detected specific immune responses to the relevant mutant ras peptide by measuring IFN-gamma mRNA expression by quantitative real-time PCR. Five out of eleven patients showed a positive immune response. Furthermore, the five pancreatic cancer patients have shown a mean disease-free survival (DFS) of 35.2+ months and a mean overall survival (OS) of 44.4+ months. The seven colorectal cancer patients have shown a mean disease-free survival (DFS) of 27.2+ months and a mean overall survival (OS) of 41.5+ months. In this study, we found that it is feasible to use mutant ras vaccine in the adjuvant setting. This vaccine is safe, can induce specific immune responses, and it appears to have a positive outcome in overall survival. Therefore, we believe that such an approach warrants further investigation in combination with other therapies. [ABSTRACT FROM AUTHOR]

Published

2008

28. Clinical impact of HLA class I expression in rectal cancer.

Author

Speetjens, Frank M., de Bruin, Elza C., Morreau, Hans, Zeestraten, Eliane C.M., Putter, Hein, Han van Krieken, J., van Buren, Maaike M., van Velzen, Monique, Geeske Dekker-Ensink, N., van de Velde, Cornelis J.H., and Kuppen, Peter J.K.

Subjects

RECTAL cancer, HLA histocompatibility antigens, TISSUES, IMMUNOHISTOCHEMISTRY, IMMUNOGLOBULINS, PROGNOSIS

Abstract

To determine the clinical impact of human leukocyte antigen (HLA) class I expression in irradiated and non-irradiated rectal carcinomas. Tumor samples in tissue micro array format were collected from 1,135 patients. HLA class I expression was assessed after immunohistochemical staining with two antibodies (HCA2 and HC10). Tumors were split into two groups: (1) tumors with >50% of tumor cells expressing HLA class I (high) and (2) tumors with ≤50% of tumor cells expressing HLA class I (low). No difference in distribution or prognosis of HLA class I expression was found between irradiated and non-irradiated patients. Patients with low expression of HLA class I (15% of all patients) showed an independent significantly worse prognosis with regard to overall survival and disease-free survival. HLA class I expression had no effect on cancer-specific survival or recurrence-free survival. Down-regulation of HLA class I in rectal cancer is associated with poor prognosis. In contrast to our results, previous reports on HLA class I expression in colorectal cancer described a large population of patients with HLA class I negative tumors, having a good prognosis. This difference might be explained by the fact that a large proportion of HLA negative colon tumors are microsatellite instable (MSI). MSI tumors are associated with a better prognosis than microsatellite stable (MSS). As rectal tumors are mainly MSS, our results suggest that it is both, oncogenic pathway and HLA class I expression, that dictates patient’s prognosis in colorectal cancer. Therefore, to prevent confounding in future prognostic analysis on the impact of HLA expression in colorectal tumors, separate analysis of MSI and MSS tumors should be performed. [ABSTRACT FROM AUTHOR]

Published

2008

29. The role of CD4+ T cell help in cancer immunity and the formulation of novel cancer vaccines.

Author

Assudani, Deepak P., Horton, Roger B. V., Mathieu, Morgan G., McArdle, Stephanie E. B., and Rees, Robert C.

Subjects

CANCER treatment, IMMUNE response, IMMUNOLOGY, CANCER vaccines, T cells, CONFERENCES & conventions

Abstract

Recent years have seen the unprecedented surge of interest in the role of CD4+ T cells and the role they play in the development of the immune response. In this symposium review, we examine the evidence for this and discuss their functions, particularly in respect to the cancer immunology, including CD4+CD25+ cells (Treg). [ABSTRACT FROM AUTHOR]

Published

2007

30. Virology- and immunology-based gene therapy for cancer.

Author

Tagawa, Masatoshi, Kawamura, Kiyoko, Shimozato, Osamu, Guangyu Ma, Quanhai Li, Suzuki, Nobuo, Shimada, Hideaki, and Ochiai, Takenori

Subjects

VIROLOGY, IMMUNOLOGY, CANCER treatment, GENE therapy, GENETIC engineering, TUMOR growth

Abstract

Current strategies for cancer gene therapy consist mainly of direct inhibition of tumor cell growth and activation of systemic host defense mechanisms. Conventional chemotherapy and radiotherapy, even considered to be temporally suppressing tumor growth, suppress immune responses; therefore, we examined potential clinical feasibility of virus-mediated tumor destruction, which can rather enhance immunity. We showed that human tumors were more susceptible to adenoviruses (Ad) in which the E1A expression was controlled by a putative tumor promoter than normal cells, and that a replication of the Ad was greater in tumor cells than in normal cells. We also demonstrated that the intratumoral injection of the Ad bearing a tumor promoter inhibited the subsequent tumor growth in vivo. The E1A expression was detected in the tumors injected with the Ad but not in non-tumorous tissues of the same mice. The Ad modified to show the regulated E1A expression is thereby oncolytic in nature. Antitumor immune responses are initiated after the acquisition of putative tumor antigen(s) by dendritic cells (DCs); therefore, enhanced antigen presentation is a crucial step for the early phase of cell-mediated immunity. Destruction of tumors can release the tumor antigens and DCs come to recognize them thereafter. We found that the stimulation of Fas expressed on DCs with Fas ligand (FasL) did not induce apoptosis of DCs but rather enhanced the antigen presentation. Activation of DCs induced production of a number of cytokines, and we showed that the interleukin-12 family secreted from tumors could induce systemic antitumor immunity. We presume that the administration of oncolytic Ad, which can destroy local tumors and subsequently make the putative tumor antigen(s) released from the tumors, stimulation of DCs with the Fas/FasL signal pathway and secretion of DCs-derived cytokines coordinately produce synergistic antitumor effects and that a combinatory application of these procedures can be a possible therapeutic strategy for cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2006

31. The use of reverse immunology to identify HLA-A2 binding epitopes in Tie-2.

Author

Ramage, Judith M., Spendlove, Ian, Rees, Robert, Moss, Robert S., and Durrant, Lindy G.

Subjects

HLA histocompatibility antigens, EPITOPES, IMMUNOLOGY, CANCER vaccines, CANCER treatment

Abstract

A potential target for a cancer vaccine would be receptors, such as Tie-2 which are over expressed on tumour endothelium. Using computer aided motif predictions for possible HLA class I epitopes, we have identified peptides from Tie-2 that should bind with a range of affinities to HLA-A*0201. No direct correlation between predicted values and actual binding affinities was observed. Although, the programs did produce a number of false positives, two epitopes were predicted that bound with relatively high affinity when compared with an influenza peptide. We have previously identified a Tie-2 epitope and shown that it was only immunogenic when we substituted preferred amino acids at key anchor residues to increase binding affinity. In this study we used a similar approach to generate modified epitopes. When HLA-A2 transgenic mice were immunised with peptides, CTL killing of the target cells was only achieved when the wild type epitope was presented at moderate levels. Moreover, the efficiency of immunisation was increased when we linked CD4 epitopes to CD8 epitopes. Caution should therefore be employed in the use of both reverse immunology and anchor modification of CTL epitopes in the identification of CTL epitopes for cancer vaccines. [ABSTRACT FROM AUTHOR]

Published

2006

32. Acknowledgement to Reviewers.

Subjects

PUBLISHING, IMMUNOLOGY, MEDICAL sciences, PERIODICALS

Abstract

This article presents a list of several authors, who reviewed various articles published in the journal "Cancer Immunology, Immunotherapy." Some of the authors are, F. Balkwill, H. Bartsch, J. Bennett, T. Gajeswski, K. Matta, G. Parmiani, and others.

Published

2001

33. Binding parameters of antibodies: pseudo-affinity and other misconceptions.

Author

Mattes, M. Jules

Subjects

MONOCLONAL antibodies, IMMUNOGLOBULINS, IMMUNOTHERAPY, IMMUNOLOGY, ANTIGENS, IMMUNITY

Abstract

In order to evaluate and compare monoclonal antibodies (Abs), functional affinities are generally determined. While the equations that define affinity relate to monovalent interactions, it has been considered that the binding of Abs to multivalent antigens such as the cell surface could be described by an apparent, or functional affinity. We demonstrate here that this concept is incorrect, since the binding interactions that occur cannot be described in terms of a functional affinity, and the values that are obtained serve only to obscure the true interactions. Bivalent Ab binding must be considered to be an irreversible reaction, in most cases. A correct understanding of Ab binding will be useful in the further development of Abs for therapeutic purposes. [ABSTRACT FROM AUTHOR]

Published

2005

34. Harnessing host immune responses to preneoplasia: promise and challenges.

Author

Dhodapkar, Madhav

Subjects

IMMUNE response, PRECANCEROUS conditions, PLASMA cell diseases, IMMUNOLOGY, IMMUNE system, RISK assessment

Abstract

Preneoplastic lesions are more common than clinical cancer and define a population at increased risk for the development of malignancy. Recent studies suggest that the immune system has the capacity to recognize these lesions, and enrichment of preneoplasia-specific immune effectors can be detected in the tumor bed of some preneoplastic lesions such as monoclonal gammopathies. Here, I discuss the promise and challenges of harnessing the immune response against preneoplasia. Approaches to boost the natural host response to these lesions may have a major impact on reducing net cancer burden. [ABSTRACT FROM AUTHOR]

Published

2005

35. A listing of human tumor antigens recognized by T cells: March 2004 update.

Author

Novellino, Luisa, Castelli, Chiara, and Parmiani, Giorgio

Subjects

TUMOR antigens, T cells, TUMOR markers, CANCER immunology, ONCOLOGY, IMMUNOLOGY

Abstract

The technological advances occurred in the last few years have led to a great increase in the number of tumor associated antigens (TAA) that are currently available for clinical applications. In this review we provide a comprehensive list of human tumor antigens as reported in the literature updated at Feburary 2004. The list includes all T cell-defined epitopes, while excluding analogs or artificially modified epitopes, as well as virus-encoded and antibodies-recognized antigens. TAAs are listed in alphabetical order along with the epitope sequence and the HLA allele which restricts recognition by T cells. Data on the tissue distribution of each antigen are also provided together with an extensive bibliography that allows a rapid search for any additional information may be needed on each single antigen or epitope. Overall, the updated list is a database tool for clinicians, scientists and students who have an interest in the field of tumor immunology and immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2005

36. Prognostic value of the CD4+/CD8+ ratio of tumour infiltrating lymphocytes in colorectal cancer and HLA-DR expression on tumour cells.

Author

Diederichsen, Axel C. P., Hjelmborg, J. v. B., Christensen, Per B., Zeuthen, Jesper, and Fenger, Claus

Subjects

COLON cancer, LYMPHOCYTES, CANCER cells, HLA histocompatibility antigens, CANCER, IMMUNOTHERAPY, IMMUNOLOGY

Abstract

The purpose of this study was to clarify whether HLA-DR expression of colorectal tumour cells or the CD4+/CD8+ ratio of the tumour infiltrating lymphocytes is significantly associated with the prognosis of colorectal cancer. Using flow cytometry, we studied the tumour cell expression of the HLA class II in 70 enzymatically dissociated colorectal cancers and the phenotype of tumour infiltrating lymphocytes (TILs) in 41 cases. There was no trend in 5-year survival between three levels (low, medium, high) of HLA-DR expression on the tumour cells. Patients with low CD4+/CD8+ ratios had a better clinical course, with significantly higher 5-year survival, p=0.046, independent of the Dukes stage and age. Our results have implications for tumour immunology; colorectal cancer cells might be a target for cytotoxic T-lymphocytes, however the tumour cells are not able to initiate an immune response. Stimulation of the immune system could possible be obtained using dendritic cells cultured in vitro and loaded with tumour antigens. [ABSTRACT FROM AUTHOR]

Published

2003

37. Prediction of an HLA-DR-binding peptide derived from Wilms' tumour 1 protein and demonstration of in vitro immunogenicity of WT1(124–138)-pulsed dendritic cells generated according to an optimised protocol.

Author

Knights, Ashley, Zaniou, Angeliki, Rees, Robert C., Pawelec, Graham, and Müller, Ludmila

Subjects

TUMORS, MAJOR histocompatibility complex, IMMUNOTHERAPY, THERAPEUTICS, CLINICAL immunology, IMMUNOLOGY, HOMEOPATHY

Abstract

The Wilms' tumour 1 (WT1) protein is over-expressed in several types of cancer including leukaemias and might therefore constitute a novel target for immunotherapy. Recently, human leucocyte antigen (HLA) class I-binding WT1 peptides have been identified and shown to stimulate CD8+ T cells in vitro. For maximal CD8 cell efficacy, CD4+ helper T cells responding to major histocompatibility complex (MHC) class II-binding epitopes are required. Here, we report that scanning the WT1 protein sequence using an evidence-based predictive computer algorithm (SYFPEITHI) yielded a peptide WT1(124–138) predicted to bind the HLA-DRB1*0401 molecule with high affinity. Moreover, synthetic WT1(124–138)-peptide-pulsed dendritic cells (DC), generated according to a protocol optimised in the present study, sensitised T cells in vitro to proliferate and secrete interferon-γ (IFN-γ) when rechallenged with specific peptide-pulsed DC, but not with peripheral blood mononuclear cells (PBMC). These results suggest that the WT1 protein may yield epitopes immunogenic to CD4 as well as CD8 T cells, and therefore constitute a novel potential target for specific immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2002

38. Induction of Tc2 cells with specificity for prostate-specific antigen from patients with hormone-refractory prostate cancer.

Author

Perambakam, Supriya, Bao-Hua Xue, Sosman, Jeffrey A., and Peace, David J.

Subjects

CANCER treatment, PROSTATE-specific antigen, TUMOR antigens, T cells, LYMPHOCYTES, IMMUNE response, IMMUNOLOGY

Abstract

Prostate-specific antigen (PSA) is a potentially useful antigen for targeted T-cell immunotherapy of prostate cancer (CaP). Our laboratory has identified a synthetic nonamer peptide (PSA 146–154) homologue of PSA, which binds to the prevalent human leukocyte antigen, HLA-A2, and elicits specific cytotoxic T-lymphocyte (CTL) responses from normal individuals of the HLA-A2 phenotype. In the present study, we report on the induction of CTL from peripheral blood mononuclear cells (PBMC) of patients with hormone-refractory CaP, which exhibit the same specificity. T-cell lines were established from two patients by stimulation of PBMC with PSA 146–154 peptide in vitro. The T-cell lines exhibited specific cytolytic activity against T2 cells pulsed with PSA 146–154 peptide, but not a control HLA-A2 binding peptide (HIV-RT 476–484) via chromium release assay (CRA). The T-cell lines also showed PSA 146–154 peptide-specific IL-4 responses, but no detectable interferon-gamma (IFN-γ) responses via enzyme-linked immuno-spot assays. Magnetic immuno-selection studies of one of the T-cell lines demonstrated that both cytolytic and interleukin-4 (IL-4) responses were mediated by CD8+, but not by CD4+ T cells. This Tc2 line was further characterized for the ability to recognize endogenously processed PSA epitopes. The line specifically secreted IL-4 in response to HLA-A2+ target cells transfected to express PSA and specifically lysed the PSA+ target cells, but not control transfected cells. The results indicate that the PSA 146–154 peptide emulates a naturally processed and presented peptide epitope of PSA that is within the T-cell repertoire of HLA-A2+ patients with CaP. [ABSTRACT FROM AUTHOR]

Published

2002

39. Immune response to E7 protein of human papillomavirus type 16 anchored on the cell surface.

Author

Nemeckova, Sarka, Stranska, Ruzena, Subrtova, Jana, Kutinova, Luda, Otahal, Pavel, Hainz, Petr, Maresova, Lucie, Sroller, Vojtech, Hamsikova, Eva, and Vonka, Vladimir

Subjects

IMMUNE response, IMMUNOLOGY, PROTEINS, PAPILLOMAVIRUSES, GENES, VIRUSES

Abstract

To target the E7 protein of human papilloma virus 16 to the cell surface, a fusion gene was constructed. It encodes the signal peptide, part of the immunoglobulin (IgG)-like domain, the transmembrane anchor of vaccinia virus (VV) hemagglutinin (HA), and the complete E7-coding sequence. The fusion gene was expressed under the HA late promoter by a recombinant VV, designated VV-E7-HA. The E7-HA protein was displayed on the surface of cells infected with the recombinant virus and was more stable than unmodified E7. The biological properties of the VV-E7-HA virus were compared with those of a VV-E7 virus that expressed the unmodified E7 and with a VV expressing the Sig-E7-LAMP fusion protein. While the first two of these recombinants were based on VV strain Praha, the third was derived from the WR strain of VV. Infection of mice with the VV-E7-HA virus induced the formation of E7-specific antibodies with the predominance of the IgG2a isotype, whereas the other two viruses did not induce the formation of E7-specific antibodies. Unlike the other two viruses, VV-E7-HA did not induce a response of cytotoxic T lymphocytes or Th1 cells and did not protect mice against the growth of E7-expressing tumors. Thus, VV-E7-HA induced a differently polarized immune response to the E7 protein than the other two viruses. [ABSTRACT FROM AUTHOR]

Published

2002

40. Augmentation of MHC class I antigen presentation via heat shock protein expression by hyperthermia.

Author

Ito, Akira, Shinkai, Masashige, Honda, Hiroyuki, Wakabayashi, Toshihiko, Yoshida, Jun, and Kobayashi, Takeshi

Subjects

IMMUNITY, ANTIGENS, CELL adhesion molecules, IMMUNOGLOBULINS, BIOMOLECULES, IMMUNOLOGY, AUTOIMMUNITY

Abstract

Heat shock proteins are recognized as significant participants in immune reactions. In this study, we have demonstrated that the cell surface presentation of MHC class I antigen was increased in tandem with increased heat shock protein 70 (HSP70) expression and the immunogenicity of rat T-9 glioma cells was enhanced by hyperthermia. T-9 cells showed growth inhibition for 24 h after the heat treatment at 43 °C for 1 h in vitro, but then resumed a normal growth rate. HSP70 expression reached a maximum at 24 h after heating. Flow cytometric analysis revealed a significant increase in MHC class I antigen on the surface of the heated cells. The augmentation of MHC class I surface expression started 24 h after heating and reached a maximum 48 h after heating. The expression of other immunologic mediators, such as intracellular adhesion molecule-1 (ICAM-1) and MHC class II antigens, did not increase. In an in vivo experiment using immunocompetent syngeneic rats (F344), growth of the heated T-9 cells, with augmentation of MHC class I antigen surface expression, was significantly inhibited, while the cells grew progressively in nude rats (F344/N Jcl-rnu). Furthermore, compared with lymphocytes from non-immunized (PBS only injection) rats or rats injected with non-heated T-9 cells, the splenic lymphocytes of the rats in which the heated T-9 cells were injected displayed specific cytotoxicity against T-9 cells. These results suggest that HSP70 is an important modulator of tumor cell immunogenicity, and that hyperthermic treatment of tumor cells can induce the host antitumor immunity via the expression of HSP70. These results may benefit further efforts on developing novel cancer immunotherapies based on hyperthermia. [ABSTRACT FROM AUTHOR]

Published

2001

41. Tumour-induced suppression of immune response and its correction.

Author

Banat, G.-A., Christ, O., Cochlovius, B., Pralle, H. B., and Zöller, M.

Subjects

IMMUNE response, IMMUNOLOGY, LYMPHOCYTES, LEUCOCYTES, CELL death, T cells, IMMUNE system

Abstract

Immunosuppressive features of tumour cells are a major obstacle for immunotherapy of cancer. We recently noted that RENCA cells effectively interfere with the in vivo activation of RENCA-specific T cells. To unravel the underlying mechanism, we evaluated the influence of RENCA cells on a mixed-lymphocyte/ tumour reaction as well as an allogeneic mixed-lymphocyte reaction. We observed that RENCA cells were not directly immunosuppressive. Instead, they initiated deviation of an immune response in at least two independent directions: (i) expansion of a population of NK1.1+/CD3+ cells, which was accompanied by elimination of mainly CD4+ lymphocytes, and (ii) production of a leukocyte-derived inhibitory factor. Expression of the costimulatory molecule B7.1 by RENCA cells prevented induction of anergy, while expression of MHC class II molecules prevented expansion of NK1.1+ cells, which was accompanied by a significant decrease in cell death. Hence, an unimpaired response was observed only when RENCA cells expressed B7.1 plus MHC class II molecules. Thus, even if a tumour itself is not immunosuppressive, it can induce a strong deviation of the immune response. It is concluded that the first contact between elements of the immune system and the tumour cell can confer a severe bias on immunoregulatory circuits. [ABSTRACT FROM AUTHOR]

Published

2001

42. Acknowledgement to Reviewers in 2003.

Subjects

PUBLISHING, IMMUNOLOGY, PERIODICALS

Abstract

Presents an acknowledgement for the reviewers of the 2003 issue of "Cancer Immunology Immunotherapy."

Published

2004

43. Michael Rawling Price: an appreciation.

Author

Baldwin, R. W.

Subjects

MEDICAL research, CANCER research, IMMUNOLOGY, TUMORS, LABORATORIES

Abstract

This article profiles immunologist Mike Price. Price died on November 200 had a long and distinguished career in tumor immunology. He joined the Cancer research Campaign Laboratories, university of Nottingham in 1969 as a graduate research student and after a research career more than 30 years was recently promoted to a full Professorship in the University. Mike Price was an enthusiastic supporter of education cancer research community. he was scientific secretary of the European Association for Cancer Research from its early begriming in the 1970s.

Published

2001