Your search keyword '"Zanovello Paola"' showing total 9 results

1. Cytokines for the induction of antitumor effectors: The paradigm of Cytokine-Induced Killer (CIK) cells.

Author

Cappuzzello E, Sommaggio R, Zanovello P, and Rosato A

Subjects

Animals, Graft vs Host Disease immunology, Graft vs Host Disease therapy, Humans, Immunotherapy, Adoptive methods, Interferon-gamma immunology, Interleukin-2 immunology, Mice, NK Cell Lectin-Like Receptor Subfamily K immunology, NK Cell Lectin-Like Receptor Subfamily K metabolism, Neoplasms immunology, T-Lymphocytes immunology, Cytokine-Induced Killer Cells immunology, Cytokines immunology, Neoplasms therapy

Abstract

Cytokine-Induced killer (CIK) cells are raising growing interest in cellular antitumor therapy, as they can be easily expanded with a straightforward and inexpensive protocol, and are safe requiring only GMP-grade cytokines to obtain very high amounts of cytotoxic cells. CIK cells do not need antigen-specific stimuli to be activated and proliferate, as they recognize and destroy tumor cells in an HLA-independent fashion through the engagement of NKG2D. In several preclinical studies and clinical trials, CIK cells showed a reduced alloreactivity compared to conventional T cells, even when challenged across HLA-barriers; only in a few patients, a mild GVHD occurred after treatment with allogeneic CIK cells. Additionally, their antitumor activity can be redirected and further improved with chimeric antigen receptors, clinical-grade monoclonal antibodies or immune checkpoint inhibitors. The evidence obtained from a growing body of literature support CIK cells as a very promising cell population for adoptive immunotherapy. In this review, all these aspects will be addressed with a particular emphasis on the role of the cytokines involved in CIK cell generation, expansion and functionalization., (Copyright © 2017 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2017

2. Impact of γ-chain cytokines on EBV-specific T cell cultures.

Author

Merlo A, Turrini R, Trento C, Zanovello P, Dolcetti R, and Rosato A

Subjects

Animals, Biomarkers metabolism, CD4-Positive T-Lymphocytes cytology, CD4-Positive T-Lymphocytes immunology, CD4-Positive T-Lymphocytes virology, Cell Differentiation, Cell Proliferation, Cells, Cultured, Cytokines biosynthesis, Humans, Kinetics, Mice, Phenotype, T-Lymphocytes, Cytotoxic cytology, Cytokines immunology, Herpesvirus 4, Human immunology, T-Lymphocytes, Cytotoxic immunology, T-Lymphocytes, Cytotoxic virology

Abstract

Background: Recent preclinical adoptive immunotherapy studies in murine models prompt to employ "proper" rather than "as many as possible" antigen-specific T cells to gain better therapeutic results. Ideally, "proper" T cells are poorly differentiated in vitro, but retain the capacity to fully differentiate into effector cells in vivo, where they can undergo long-term survival and strong proliferation. Such requirements can be achieved by modifying culture conditions, namely using less "differentiating" cytokines than IL-2., Methods: To evaluate this issue in human T cell cultures, we exploited a well characterized and clinical-grade protocol finalized at generating EBV-specific CTL for adoptive immunotherapy. In particular, we studied the impact of IL-7, IL-15 and IL-21 compared to IL-2 on different aspects of T cell functionality, namely growth kinetics, differentiation/activation marker expression, cytokine production, and short-term and long-term cytotoxicity., Results: Results disclosed that the culture modifications we introduced in the standard protocol did not improve activity nor induce substantial changes in differentiation marker expression of EBV-specific CTL., Conclusions: Our data indicated that the addition of γ-chain cytokines other than IL-2 for the generation of EBV-specific T cell cultures did not produce the improvements expected on the basis of recent published literature. This fact was likely due to the intrinsic differences between murine and human models and highlights the need to design ad hoc protocols rather than simply modify the cytokines added in culture.

Published

2010

3. Polarized monocyte response to cytokine stimulation.

Author

Nagorsen D, Deola S, Smith K, Wang E, Monsurro V, Zanovello P, Marincola FM, and Panelli MC

Subjects

Adult, Cytokines classification, Female, Gene Expression Profiling, Gene Expression Regulation, Humans, Kinetics, Lipopolysaccharide Receptors analysis, Lipopolysaccharides pharmacology, Male, Matrix Metalloproteinases genetics, Matrix Metalloproteinases metabolism, Middle Aged, Monocytes drug effects, NF-kappa B metabolism, Oligonucleotide Array Sequence Analysis, Polymerase Chain Reaction methods, Transcription, Genetic drug effects, Cytokines pharmacology, Gene Expression, Monocytes immunology

Abstract

Background: Mononuclear phagocytes (MPs) stand at the crossroads between the induction of acute inflammation to recruit and activate immune effector cells and the downmodulation of the inflammatory process to contain collateral damage. This decision is extensively modulated by the cytokine microenvironment, which includes a broad array of cytokines whose direct effect on MPs remains largely unexplored. Therefore, we tested whether polarized responses of MPs to pathogens are related to the influence of selected cytokines or represent a mandatory molecular switch through which most cytokines operate., Results: Circulating CD14+ MPs were exposed to bacterial lipopolysaccharide (LPS) followed by exposure to an array of cytokines, chemokines and soluble factors involved in the immune response. Gene expression was studied by global transcript analysis. Two main classes of cytokines were identified that induced a classical or an alternative pathway of MP activation. Expression of genes affected by NFkappaB activation was most predictive of the two main classes, suggesting that this pathway is a fundamental target of cytokine regulation. As LPS itself induces a classical type of activation, the most dramatic modulation was observed toward the alternative pathway, suggesting that a broad array of cytokines may counteract the pro-inflammatory effects of bacterial components., Conclusions: This analysis is directly informative of the primary effect of individual cytokines on the early stages of LPS stimulation and, therefore, may be most informative of the way MP maturation may be polarized at the early stages of the immune response.

Published

2005

4. Impact of ϒ-chain cytokines on EBV-specific T cell cultures.

Author

Merlo, Anna, Turrini, Riccardo, Trento, Cristina, Zanovello, Paola, Dolcetti, Riccardo, and Rosato, Antonio

Subjects

CYTOKINES, T cells, IMMUNOTHERAPY, ANTIGENS, INTERLEUKIN-2

Abstract

Background: Recent preclinical adoptive immunotherapy studies in murine models prompt to employ "proper" rather than "as many as possible" antigen-specific T cells to gain better therapeutic results. Ideally, "proper" T cells are poorly differentiated in vitro, but retain the capacity to fully differentiate into effector cells in vivo, where they can undergo long-term survival and strong proliferation. Such requirements can be achieved by modifying culture conditions, namely using less "differentiating" cytokines than IL-2. Methods: To evaluate this issue in human T cell cultures, we exploited a well characterized and clinical-grade protocol finalized at generating EBV-specific CTL for adoptive immunotherapy. In particular, we studied the impact of IL-7, IL-15 and IL-21 compared to IL-2 on different aspects of T cell functionality, namely growth kinetics, differentiation/activation marker expression, cytokine production, and short-term and long-term cytotoxicity. Results: Results disclosed that the culture modifications we introduced in the standard protocol did not improve activity nor induce substantial changes in differentiation marker expression of EBV-specific CTL. Conclusions: Our data indicated that the addition of γ-chain cytokines other than IL-2 for the generation of EBV-specific T cell cultures did not produce the improvements expected on the basis of recent published literature. This fact was likely due to the intrinsic differences between murine and human models and highlights the need to design ad hoc protocols rather than simply modify the cytokines added in culture. [ABSTRACT FROM AUTHOR]

Published

2010

5. Leukocyte Infiltration in Cancer Creates an Unfavorable Environment for Antitumor Immune Responses: A Novel Target for Therapeutic Intervention.

Author

Bronte, Vincenzo, Cingarlini, Sara, Marigo, Ilaria, De Santo, Carmela, Gallina, Giovanna, Dolcetti, Luigi, Ugel, Stefano, Peranzoni, Elisa, Mandruzzato, Susanna, and Zanovello, Paola

Subjects

LEUKOCYTES, IMMUNOSUPPRESSION, IMMUNE response, CYTOKINES, FIBROBLASTS, CANCER

Abstract

The interaction between tumor cells and the nearby environment is being actively investigated to explore how this interplay affects the initiation and progression of cancer. Host-tumor relationship results in the production of pro-inflammatory cytokines and chemokines that promote the recruitment of leukocytes within and around developing neoplasms. Cancer cells, together with newly recruited tumor-infiltrating cells, can also activate fibroblast and vascular responses, thus resulting in a chronic microenvironment perturbation. In this complex scenario, interactions between innate and adaptive immune cells can be disturbed, leading to a failure of immune-mediated tumor recognition and destruction. On the basis of the recent awareness about tumor promotion and immune deregulation by immune/inflammatory cells, novel anti-cancer strategies can be exploited. [ABSTRACT FROM AUTHOR]

Published

2006

6. Retargeting cytokine-induced killer cell activity by CD16 engagement with clinical-grade antibodies.

Author

Cappuzzello, Elisa, Tosi, Anna, Zanovello, Paola, Sommaggio, Roberta, and Rosato, Antonio

Subjects

CYTOKINES, T cells, ANTINEOPLASTIC agents, CELL populations, IMMUNOTHERAPY, ANTIBODY-dependent cell cytotoxicity

Abstract

Cytokine-induced Killer (CIK) cells are a heterogeneous population ofex vivoexpanded T lymphocytes capable of MHC-unrestricted antitumor activity, which share phenotypic and functional features with both NK and T cells. Preclinical data and initial clinical studies demonstrated their high tolerabilityin vivo, supporting CIK cells as a promising cell population for adoptive cell immunotherapy. In this study, we report for the first time that CIK cells display a donor-dependent expression of CD16, which can be engaged by trastuzumab or cetuximab to exert a potent antibody-dependent cell-mediated cytotoxicity (ADCC) against ovarian and breast cancer cell lines, leading to an increased lytic activityin vitro, and an enhanced therapeutic efficacyin vivo. Thus, an efficient tumor antigen-specific retargeting can be achieved by a combination therapy with clinical-grade monoclonal antibodies already widely used in cancer therapy, and CIK cell populations that are easily expandable in very large numbers, inexpensive, safe and do not require genetic manipulations. Overall, these data provide a new therapeutic strategy for the treatment of Her2 and EGFR expressing tumors by adoptive cell therapy, which could find wide implementation and application, and could also be expanded to the use of additional therapeutic antibodies. [ABSTRACT FROM PUBLISHER]

Published

2016

7. miR-142-3p Prevents Macrophage Differentiation during Cancer-Induced Myelopoiesis.

Author

Sonda, Nada, Simonato, Francesca, Peranzoni, Elisa, Calì, Bianca, Bortoluzzi, Stefania, Bisognin, Andrea, Wang, Ena, Marincola, Francesco?M., Naldini, Luigi, Gentner, Bernhard, Trautwein, Christian, Sackett, Sara?Dutton, Zanovello, Paola, Molon, Barbara, and Bronte, Vincenzo

Subjects

*MACROPHAGES, *CELL differentiation, *CANCER invasiveness, *BIOACCUMULATION, *CYTOKINES, *MICRORNA

Abstract

Summary: Tumor progression is accompanied by an altered myelopoiesis causing the accumulation of immunosuppressive cells. Here, we showed that miR-142-3p downregulation promoted macrophage differentiation and determined the acquisition of their immunosuppressive function in tumor. Tumor-released cytokines signaling through gp130, the common subunit of the interleukin-6 cytokine receptor family, induced the LAP∗ isoform of C/EBPβ transcription factor, promoting macrophage generation. miR-142-3p downregulated gp130 by canonical binding to its messenger RNA (mRNA) 3' UTR and repressed C/EBPβ LAP∗ by noncanonical binding to its 5' mRNA coding sequence. Enforced miR expression impaired macrophage differentiation both in vitro and in vivo. Mice constitutively expressing miR-142-3p in the bone marrow showed a marked increase in survival following immunotherapy with tumor-specific T lymphocytes. By modulating a specific miR in bone marrow precursors, we thus demonstrated the feasibility of altering tumor-induced macrophage differentiation as a potent tool to improve the efficacy of cancer immunotherapy. [Copyright &y& Elsevier]

Published

2013

8. Tumor-Induced Tolerance and Immune Suppression Depend on the C/EBPβ Transcription Factor

Author

Marigo, Ilaria, Bosio, Erika, Solito, Samantha, Mesa, Circe, Fernandez, Audry, Dolcetti, Luigi, Ugel, Stefano, Sonda, Nada, Bicciato, Silvio, Falisi, Erika, Calabrese, Fiorella, Basso, Giuseppe, Zanovello, Paola, Cozzi, Emanuele, Mandruzzato, Susanna, and Bronte, Vincenzo

Subjects

*IMMUNOSUPPRESSION, *IMMUNOLOGICAL tolerance, *TRANSCRIPTION factors, *TUMOR growth, *CYTOKINES, *INTERLEUKIN-6, *IMMUNOREGULATION, *CELLULAR immunity

Abstract

Summary: Tumor growth is associated with a profound alteration in myelopoiesis, leading to recruitment of immunosuppressive cells known as myeloid-derived suppressor cells (MDSCs). We showed that among factors produced by various experimental tumors, the cytokines GM-CSF, G-CSF, and IL-6 allowed a rapid generation of MDSCs from precursors present in mouse and human bone marrow (BM). BM-MDSCs induced by GM-CSF+IL-6 possessed the highest tolerogenic activity, as revealed by the ability to impair the priming of CD8+ T cells and allow long term acceptance of pancreatic islet allografts. Cytokines inducing MDSCs acted on a common molecular pathway and the immunoregulatory activity of both tumor-induced and BM-derived MDSCs was entirely dependent on the C/EBPβ transcription factor. Adoptive transfer of tumor antigen-specific CD8+ T lymphocytes resulted in therapy of established tumors only in mice lacking C/EBPβ in the myeloid compartment, suggesting that C/EBPβ is a critical regulator of the immunosuppressive environment created by growing cancers. [Copyright &y& Elsevier]

Published

2010

9. Tumors induce a subset of inflammatory monocytes with immunosuppressive activity on CD8+ T cells.

Author

Gallina, Giovanna, Dolcetti, Luigi, Serafini, Paolo, de Santo, Carmela, Marigo, Ilaria, Colombo, Mario P., Basso, Giuseppe, Brombacher, Frank, Borrello, Ivan, Zanovello, Paola, Bicciato, Silvio, and Bronte, Vincenzo

Subjects

*SUPPRESSOR cells, *T cells, *TUMORS, *IMMUNOTHERAPY, *IMMUNODEFICIENCY, *MONOCYTES, *CYTOKINES, *ANTIGENS, *PHYSIOLOGY

Abstract

Active suppression of tumor-specific T lymphocytes can limit the efficacy of immune surveillance and immunotherapy. While tumor-recruited CD11b+ myeloid cells are known mediators of tumor-associated immune dysfunction, the true nature of these suppressive cells and the fine biochemical pathways governing their immunosuppressive activity remain elusive. Here we describe a population of circulating CD11b+IL-4 receptor alpha+ (CD11b+IL-4Ralpha+), inflammatory-type monocytes that is elicited by growing tumors and activated by IFN-gamma released from T lymphocytes. CD11b+IL-4Ralpha+ cells produced IL-13 and IFN-gamma and integrated the downstream signals of these cytokines to trigger the molecular pathways suppressing antigen-activated CD8+ T lymphocytes. Analogous immunosuppressive circuits were active in CD11b+ cells present within the tumor microenvironment. These suppressor cells challenge the current idea that tumor-conditioned immunosuppressive monocytes/macrophages are alternatively activated. Moreover, our data show how the inflammatory response elicited by tumors had detrimental effects on the adaptive immune system and suggest novel approaches for the treatment of tumor-induced immune dysfunctions. [ABSTRACT FROM AUTHOR]

Published

2006