Your search keyword '"Anichini, Andrea"' showing total 312 results

301. Results of nimotuzumab and vinorelbine, radiation and re-irradiation for diffuse pontine glioma in childhood.

Author

Massimino M, Biassoni V, Miceli R, Schiavello E, Warmuth-Metz M, Modena P, Casanova M, Pecori E, Giangaspero F, Antonelli M, Buttarelli FR, Potepan P, Pollo B, Nunziata R, Spreafico F, Podda M, Anichini A, Clerici CA, Sardi I, De Cecco L, Bode U, Bach F, and Gandola L

Subjects

Adolescent, Antibodies, Monoclonal, Humanized adverse effects, Antibodies, Monoclonal, Humanized therapeutic use, Antineoplastic Agents, Phytogenic adverse effects, Antineoplastic Agents, Phytogenic therapeutic use, Brain Stem Neoplasms pathology, Child, Child, Preschool, Drug Therapy, Combination adverse effects, Female, Follow-Up Studies, Glioma pathology, Humans, Immunologic Factors adverse effects, Immunologic Factors therapeutic use, Magnetic Resonance Imaging, Male, Neoplasm Recurrence, Local radiotherapy, Pilot Projects, Retreatment, Survival Analysis, Treatment Outcome, Vinblastine adverse effects, Vinblastine analogs & derivatives, Vinblastine therapeutic use, Vinorelbine, Brain Stem Neoplasms therapy, Chemoradiotherapy, Glioma therapy

Abstract

Radiotherapy is the only treatment definitely indicated for diffuse pontine gliomas (DIPG). Findings on the role of EGFR signaling in the onset of childhood DIPG prompted the use of nimotuzumab, an anti-EGFR monoclonal antibody. Assuming a potential synergy with both radiotherapy and vinorelbine, a pilot phase 2 protocol was launched that combined nimotuzumab with concomitant radiation and vinorelbine. An amendment in July 2011 introduced re-irradiation at relapse. The primary endpoint for first-line treatment was objective response rate (CR + PR + SD) according to the RECIST. This report concerns the outcome of this strategy as a whole. Vinorelbine 20 mg/m(2) was administered weekly, with nimotuzumab 150 mg/m(2) in the first 12 weeks of treatment; radiotherapy was delivered from weeks 3 to 9, for a total dose of 54 Gy. Vinorelbine 25 mg/m(2) and nimotuzumab were given every other week thereafter until the tumor progressed or for up to 2 years. Re-irradiation consisted of 19.8 Gy, fractionated over 11 days. Baseline and latest MRIs were assessed blindly by an outside neuroradiologist. Twenty five children (mean age 7.4 years) were enrolled as of August 2009 (median follow-up 29 months). A response was observed in 24/25 patients (96 %). The nimotuzumab/vinorelbine combination was very well tolerated, with no acute side-effects. Eleven of 16 locally-relapsing patients were re-irradiated. One-year PFS and OS rates were 30 ± 10 % and 76 ± 9 %, respectively; 2-year OS was 27 ± 9 %; the median PFS and OS were 8.5 and 15 months, respectively. This strategy generated interesting results and warrants further investigation.

Published

2014

302. Role of macrophage targeting in the antitumor activity of trabectedin.

Author

Germano G, Frapolli R, Belgiovine C, Anselmo A, Pesce S, Liguori M, Erba E, Uboldi S, Zucchetti M, Pasqualini F, Nebuloni M, van Rooijen N, Mortarini R, Beltrame L, Marchini S, Fuso Nerini I, Sanfilippo R, Casali PG, Pilotti S, Galmarini CM, Anichini A, Mantovani A, D'Incalci M, and Allavena P

Subjects

Animals, Apoptosis drug effects, Blotting, Western, Carcinoma, Lewis Lung metabolism, Carcinoma, Lewis Lung pathology, Caspase 8 metabolism, Cell Proliferation, Female, Fibrosarcoma metabolism, Fibrosarcoma pathology, Flow Cytometry, Humans, Immunoenzyme Techniques, Macrophages metabolism, Macrophages pathology, Mice, Monocytes drug effects, Monocytes metabolism, Monocytes pathology, Myeloid Cells drug effects, Myeloid Cells metabolism, Myeloid Cells pathology, Neovascularization, Pathologic prevention & control, Ovarian Neoplasms metabolism, Ovarian Neoplasms pathology, Phagocytes drug effects, Phagocytes metabolism, Phagocytes pathology, Signal Transduction drug effects, Trabectedin, Tumor Cells, Cultured, Antineoplastic Agents, Alkylating therapeutic use, Carcinoma, Lewis Lung drug therapy, Dioxoles therapeutic use, Fibrosarcoma drug therapy, Macrophages drug effects, Ovarian Neoplasms drug therapy, Tetrahydroisoquinolines therapeutic use

Abstract

There is widespread interest in macrophages as a therapeutic target in cancer. Here, we demonstrate that trabectedin, a recently approved chemotherapeutic agent, induces rapid apoptosis exclusively in mononuclear phagocytes. In four mouse tumor models, trabectedin caused selective depletion of monocytes/macrophages in blood, spleens, and tumors, with an associated reduction of angiogenesis. By using trabectedin-resistant tumor cells and myeloid cell transfer or depletion experiments, we demonstrate that cytotoxicity on mononuclear phagocytes is a key component of its antitumor activity. Monocyte depletion, including tumor-associated macrophages, was observed in treated tumor patients. Trabectedin activates caspase-8-dependent apoptosis; selectivity for monocytes versus neutrophils and lymphocytes is due to differential expression of signaling and decoy TRAIL receptors. This unexpected property may be exploited in different therapeutic strategies., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

303. Peptides with dual binding specificity for HLA-A2 and HLA-E are encoded by alternatively spliced isoforms of the antioxidant enzyme peroxiredoxin 5.

Author

Sensi M, Pietra G, Molla A, Nicolini G, Vegetti C, Bersani I, Millo E, Weiss E, Moretta L, Mingari MC, and Anichini A

Subjects

Alternative Splicing, Amino Acid Motifs immunology, Antigens, Neoplasm genetics, Antigens, Neoplasm immunology, Antioxidants metabolism, Catalytic Domain, Cell Line, Tumor, Clone Cells, Cysteine deficiency, Humans, Immunity, Cellular, Killer Cells, Natural metabolism, Melanoma genetics, Melanoma metabolism, Oxidative Stress immunology, Peptides chemistry, Peptides immunology, Peptides metabolism, Peroxiredoxins genetics, Peroxiredoxins immunology, Protein Binding, Protein Isoforms genetics, Protein Isoforms immunology, Protein Stability drug effects, Sequence Deletion, T-Lymphocytes, Cytotoxic immunology, T-Lymphocytes, Cytotoxic metabolism, HLA-E Antigens, Antigens, Neoplasm metabolism, HLA Antigens metabolism, HLA-A2 Antigen metabolism, Histocompatibility Antigens Class I metabolism, Killer Cells, Natural immunology, Melanoma immunology, Peroxiredoxins metabolism, Protein Isoforms metabolism

Abstract

Peptides with dual binding specificity for classical HLA class I and non-classical HLA-E molecules have been identified in virus-encoded proteins, but not in cellular proteins from normal or neoplastic cells. Expression screening of a melanoma cDNA library with a CTL clone recognizing an HLA-A2-restricted tumor-specific epitope encoded by mutant peroxiredoxin 5 (Prdx5), a stress-inducible peroxidase, led to the identification of two alternatively spliced isoforms of the same gene. These isoforms, which lack the catalytic cysteine fundamental for enzymatic activity, showed widespread expression in neoplastic and normal tissues but were unstable at the protein level, being detectable, following transient transfection, only after lactacystin treatment to inhibit proteasomal degradation. Isoform-specific sequences which formed, respectively, as result of exon 1 splicing to either exon 3 or 4, encoded two distinct nonapeptides (AMAPIKTHL and AMAPIKVRL, not present in the full-length protein) with anchor residues for HLA-A2 and HLA-E molecules and able to stabilize HLA-A2 and HLA-E cell surface expression. HLA-E+ targets, loaded with these peptides, were not recognized by NK cells expressing CD94/NKG2A inhibitory or CD94/NKG2C activatory receptors. However, both peptides were recognized, although with low avidity, by HLA-E-restricted CD8+ CTL. The nonapeptide AMAPIKVRL was used to elicit HLA-A2-restricted CTL clones that killed peptide-pulsed lymphoblastoid cell lines and melanoma cells expressing the corresponding Prdx5 isoform. Our results suggest that alternatively spliced isoforms of Prdx5, through the generation of HLA-E- and HLA-A2-restricted peptides may be part of immune-mediated stress response contributing to the detection and elimination of damaged normal or neoplastic cells.

Published

2009

304. The effect of artificial antigen-presenting cells with preclustered anti-CD28/-CD3/-LFA-1 monoclonal antibodies on the induction of ex vivo expansion of functional human antitumor T cells.

Author

Zappasodi R, Di Nicola M, Carlo-Stella C, Mortarini R, Molla A, Vegetti C, Albani S, Anichini A, and Gianni AM

Subjects

Antigens, Neoplasm immunology, Cell Differentiation, Cells, Cultured, Humans, Immunophenotyping, MART-1 Antigen, Neoplasm Proteins immunology, Phenotype, T-Lymphocytes cytology, Antibodies, Monoclonal immunology, Antigen-Presenting Cells immunology, CD28 Antigens immunology, CD3 Complex immunology, Lymphocyte Function-Associated Antigen-1 immunology, Neoplasms immunology, T-Lymphocytes immunology

Abstract

Background: Adoptive cell therapy with ex vivo expanded autologous antitumor cytotoxic T lymphocytes represents an important therapeutic option as an anticancer strategy. In order to identify a reliable method for producing adequate amounts of functional antitumor cytotoxic T lymphocytes with a potentially long in vivo lifespan, we tested the T-cell expansion efficiency of a new artificial antigen-presenting cell-based system., Design and Methods: Our artificial antigen-presenting cells were generated with activating (anti-CD3), co-stimulating (anti-CD28) and adhesion (anti-LFA-1) biotinylated monoclonal antibodies preclustered in microdomains held on a liposome scaffold by neutravidin rafts. The co-localization of T-cell ligands in microdomains and the targeting of an adhesion protein, increasing the efficiency of immunological synapse formation, represent the novelties of our system. The activity of our artificial antigen-presenting cells was compared with that of anti-CD3/-CD28 coated immunomagnetic microbeads and immobilized anti-CD3 monoclonal antibody (OKT3 clone), the only two commercially available artificial systems., Results: Our artificial antigen-presenting cells expanded both polyclonal T cells and MART-1-specific CD8(+) T cells in a more efficient manner than the other systems. Stimulation with artificial antigen-presenting cells allows for the generation of viable T cells displaying an immunophenotype consistent with in vivo potential for persistence, without increasing the frequency of regulatory T cells. The starting specificity of anti MART-1 CD8(+) T cells was preserved after stimulation with artificial antigen-presenting cells and it was statistically greater when compared to the activity of the same cells expanded with the other systems. Finally, our artificial antigen-presenting cells proved to be suitable for large-scale application, minimizing the volume and the costs of T-cell expansion., Conclusions: Our artificial antigen-presenting cells might represent an efficient tool to rapidly obtain a sufficient number of functional T cells for adoptive immunotherapy in patients with cancer.

Published

2008

305. APAF-1 signaling in human melanoma.

Author

Anichini A, Mortarini R, Sensi M, and Zanon M

Subjects

Apoptotic Protease-Activating Factor 1, Humans, Intracellular Signaling Peptides and Proteins chemistry, Intracellular Signaling Peptides and Proteins genetics, Melanoma drug therapy, Proteins chemistry, Proteins genetics, Apoptosis, Intracellular Signaling Peptides and Proteins physiology, Melanoma pathology, Proteins physiology, Signal Transduction physiology

Abstract

Acquired resistance to mechanisms of programmed cell death is one of the hallmarks of cancer. Human melanoma, in advanced stage, is hardly curable, due to development of several strategies that impair apoptosis induced by the death receptor and the mitochondrial pathways of apoptosis. Among these apoptosis escape strategies, one is based on inactivation of pro-apoptotic factors such as Apoptotic Protease Activating Factor-1 (APAF-1). APAF-1 couples cytochrome c release from the mitochondria to caspase-9 activation and has been considered a central adaptor in the intrinsic pathway of programmed cell death. Inactivation of APAF-1 in human melanoma may impair the mitochondrial pathway of apoptosis induced by chemotherapeutic drugs that activate the p53 pathway, thus contributing to the development of chemoresistance. In-vivo, loss of expression of APAF-1 is associated with tumor progression, suggesting that APAF-1 inactivation may provide a selective survival advantage to neoplastic cells. However, recent results have indicated the existence of APAF-1-independent pathways of caspase activation and apoptosis in normal and neoplastic cells. Moreover, it has been found that expression of APAF-1 is not necessary for the apoptotic response of melanoma cells to different pro-apoptotic drugs. The emerging picture from results obtained in melanoma and other human tumors is that the relevance of the APAF-1 pathway in programmed cell death is cell-context-dependent and related to the specificity of the pro-apoptotic-stimuli.

Published

2006

306. Skewed T-cell differentiation in patients with indolent non-Hodgkin lymphoma reversed by ex vivo T-cell culture with gammac cytokines.

Author

Anichini A, Mortarini R, Romagnoli L, Baldassari P, Cabras A, Carlo-Stella C, Gianni AM, and Di Nicola M

Subjects

Adult, Bone Marrow immunology, Bone Marrow pathology, Humans, Interferon-gamma immunology, Interleukin Receptor Common gamma Subunit, Lymph Nodes cytology, Lymph Nodes immunology, Lymph Nodes pathology, Lymphoma, B-Cell metabolism, Lymphoma, B-Cell pathology, Receptors, Interleukin-7 metabolism, T-Lymphocytes cytology, T-Lymphocytes metabolism, T-Lymphocytes, Cytotoxic cytology, Th2 Cells immunology, Th2 Cells metabolism, Tumor Cells, Cultured, Cell Differentiation, Cytokines immunology, Lymphoma, B-Cell immunology, Receptors, Interleukin-7 immunology, T-Lymphocytes immunology, T-Lymphocytes, Cytotoxic immunology

Abstract

The unfavorable clinical evolution in indolent non-Hodgkin lymphomas suggests defective control of neoplastic growth by the immune system. To address this issue, we evaluated phenotype, function, and maturation profile of CD4(+) and CD8(+) T cells from peripheral-blood, lymph nodes, or bone marrow of patients with B-cell non-Hodgkin lymphoma (NHL) at diagnosis. T cells from these patients frequently showed an activated but apoptosis-prone phenotype with low frequency of tumor-reactive T cells showing a TH2/Tc2 functional profile in the response to autologous tumor. In peripheral blood or in lymph nodes and bone marrow, and, in comparison to healthy donors, patients' T cells showed a skewed differentiation toward Tnaive and Tcentral memory stages, with low expression of granzyme B and perforin. T-cell culture with autologous tumor in the presence of IL-2, IL-15, and autologous bone marrow-derived cells led to massive T-cell expansion and to differentiation of cytotoxic factor(+) CD8(+) T cells releasing IFN-gamma and killing autologous B-cell tumor in an HLA-class I-restricted fashion. These results suggest impaired T-cell differentiation to effector stage in patients with B-cell NHL, but indicate that T-cell responsiveness to gammac cytokines is retained, thus allowing to promote generation of antitumor T cells for immune intervention.

Published

2006

307. The paradox of T-cell-mediated antitumor immunity in spite of poor clinical outcome in human melanoma.

Author

Anichini A, Vegetti C, and Mortarini R

Subjects

Antigens, Differentiation immunology, Antigens, Neoplasm immunology, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Cancer Vaccines therapeutic use, Cell Differentiation, Clinical Trials as Topic, Disease Progression, Humans, Lymphocytes, Tumor-Infiltrating immunology, Melanoma pathology, Melanoma therapy, Models, Immunological, Neoplasm Metastasis, Neoplasm Staging, Treatment Failure, Melanoma immunology, T-Lymphocyte Subsets immunology, Tumor Escape immunology

Abstract

Human melanoma is hardly ever curable at an advanced stage, but overwhelming evidence from untreated or vaccinated patients indicates that this tumor is highly antigenic and frequently immunogenic. Here, we review recent results indicating that CD8(+) T cell-mediated antitumor immunity is activated at the systemic and tumor level in the early clinical stages (AJCC stages I and II) and continues to be promoted, in a fraction of patients, even in metastatic disease (stages III and IV). This evidence was obtained by looking at frequency, differentiation phenotype, and function of antitumor T cells in periphery and tumor site of melanoma patients. On the other hand, the paradox of immunity in spite of poor clinical evolution of the disease, points toward a model of concurrent evolution of immunity and tumor escape. As melanoma progresses to metastatic disease, powerful mechanisms of tumor evasion from immune recognition, and of immunosuppression, are activated, thus tilting the balance between immunity and escape in favor of tumor resistance to host defense. Nevertheless, recent developments in our understanding of regulation of T cell-mediated immunity can provide clues to the prospects for improved immunotherapy approaches. By integrating the information from basic research in immunology, from murine tumor models, and from trials of immunotherapy, we discuss how the most relevant steps of the antitumor response should be manipulated with greater efficacy by future clinical trials.

Published

2004

308. Dendritic cell viability is decreased after phagocytosis of apoptotic tumor cells induced by staurosporine or vaccinia virus infection.

Author

Di Nicola M, Napoli S, Anichini A, Mortarini R, Romagnoli L, Magni M, Matteucci P, Baldassarri P, Bersani I, Carlo-Stella C, and Gianni AM

Subjects

Antigen Presentation, Antigens, Neoplasm immunology, Apoptosis radiation effects, B-Lymphocytes pathology, B-Lymphocytes radiation effects, Cancer Vaccines, Coculture Techniques, Culture Media, Conditioned pharmacology, Humans, Interferon-gamma pharmacology, Leukemia, Lymphocytic, Chronic, B-Cell pathology, Lymphoma, Follicular pathology, Monocytes cytology, Monocytes drug effects, T-Lymphocytes immunology, Tumor Cells, Cultured drug effects, Tumor Cells, Cultured immunology, Tumor Cells, Cultured radiation effects, Tumor Cells, Cultured virology, Vaccination, Apoptosis drug effects, B-Lymphocytes drug effects, B-Lymphocytes virology, Dendritic Cells cytology, Phagocytosis, Staurosporine pharmacology, Ultraviolet Rays, Vaccinia virus physiology

Abstract

Background and Objectives: Dendritic cells (DC) primed with tumor antigens can effectively mediate the regression of a variety of established solid malignancies in both murine and human models. Several experimental studies indicate that apoptotic bodies are an optimal source of tumor antigens for ex vivo priming of DC. However, the clinical use of killed tumor cells as a source of antigens will require an optimal methodology to induce effective tumor cell apoptosis., Design and Methods: The goal of this study was to compare the efficiency of three agents for inducing neoplastic B lymphocyte apoptosis; staurosporine, infection by modified vaccinia (MVA) viral particles and ultraviolet C (UVC) radiation., Results: The three methods were finely tuned to induce apoptosis in more than 90% of tumor cells after 24 hours of exposure. However, the viability of monocyte-derived DC, loaded with B-cell tumor apoptotic bodies induced by staurosporine or MVA viral particles, decreased dramatically within 48 hours after phagocytosis of the killed neoplastic cells. The persistence of the apoptosis-inducing agents in the apoptotic bodies and not in the tumor supernatant, was responsible for the observed damage to DC viability. In contrast, DC viability was not affected after uptake of tumor cells killed through UVC-irradiation. Furthermore, B-lymphoblastic cell line (LCL)-specific T cells were reactivated by DC loaded with apoptotic bodies induced by UVC-rays., Interpretation and Conclusions: Since the method used to induce tumor cell apoptosis might be detrimental to DC viability, these findings should be considered when designing anticancer vaccination programs.

Published

2003

309. Clinical protocol. Immunization of patients with malignant melanoma with autologous CD34(+) cell-derived dendritic cells transduced ex vivo with a recombinant replication-deficient vaccinia vector encoding the human tyrosinase gene: a phase I trial.

Author

Di Nicola M, Carlo-Stella C, Anichini A, Mortarini R, Guidetti A, Tragni G, Gallino F, Del Vecchio M, Ravagnani F, Morelli D, Chaplin P, Arndtz N, Sutter G, Drexler I, Parmiani G, Cascinelli N, and Gianni AM

Subjects

Adolescent, Adult, Antigens, CD34 metabolism, Clinical Protocols, Female, Gene Transfer Techniques, Humans, Immunization, Male, Transduction, Genetic, Vaccinia virus immunology, Cancer Vaccines immunology, Dendritic Cells immunology, Genetic Vectors, Melanoma immunology, Monophenol Monooxygenase genetics

Published

2003

310. Differentiation of CD8+ T cells from tumor-invaded and tumor-free lymph nodes of melanoma patients: role of common gamma-chain cytokines.

Author

Anichini A, Scarito A, Molla A, Parmiani G, and Mortarini R

Subjects

Antigens, Neoplasm, Antigens, Viral immunology, CD8-Positive T-Lymphocytes cytology, CD8-Positive T-Lymphocytes metabolism, Cell Differentiation immunology, Cells, Cultured, Epitopes, T-Lymphocyte immunology, Humans, Interleukin Receptor Common gamma Subunit, Interleukin-15 physiology, Interleukin-2 physiology, Lymph Nodes cytology, Lymph Nodes immunology, Lymphocytes, Tumor-Infiltrating metabolism, Lymphocytes, Tumor-Infiltrating virology, MART-1 Antigen, Melanoma pathology, Melanoma virology, Neoplasm Proteins immunology, Receptors, CCR7, Receptors, Chemokine biosynthesis, T-Lymphocyte Subsets cytology, T-Lymphocyte Subsets immunology, T-Lymphocyte Subsets pathology, Tumor Cells, Cultured, CD8-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes pathology, Lymph Nodes pathology, Lymphocytes, Tumor-Infiltrating immunology, Lymphocytes, Tumor-Infiltrating pathology, Melanoma immunology, Receptors, Interleukin-7 physiology

Abstract

Differentiation of CD8(+) T cells at the tumor site toward effector and memory stages may represent a key step for the efficacy of antitumor response developing naturally or induced through immunotherapy. To address this issue, CD8(+) T lymphocytes from tumor-invaded (n = 142) and tumor-free (n = 42) lymph nodes removed from the same nodal basin of melanoma patients were analyzed for the expression of CCR7, CD45RA, perforin, and granzyme B. By hierarchical cluster analysis, CD8(+) T cells from all tumor-free lymph nodes and from 56% of the tumor-invaded lymph node samples fell in the same cluster, characterized mainly by CCR7(+) CD45RA(+/-) cytotoxic factor(-) cells. The remaining three clusters contained only samples from tumor-invaded lymph nodes and showed a progressive shift of the CD8(+) T cell population toward CCR7(-) CD45RA(-/+) perforin(+) granzyme B(+) differentiation stages. Distinct CD8(+) T cell maturation stages, as defined by CCR7 vs CD45RA and by functional assays, were identified even in melanoma- or viral Ag-specific T cells from invaded lymph nodes by HLA tetramer analysis. Culture for 7 days of CCR7(+) perforin(-) CD8(+) T cells from tumor-invaded lymph nodes with IL-2 or IL-15, but not IL-7, promoted, mainly in CCR7(+)CD45RA(-) cells, proliferation coupled to differentiation to the CCR7(-) perforin(+) stage and acquisition of melanoma Ag-specific effector functions. Taken together, these results indicate that CD8(+) T cells differentiated toward CCR7(-) cytotoxic factor(+) stages are present in tumor-invaded, but not in tumor-free, lymph nodes of a relevant fraction of melanoma patients and suggest that cytokines such as IL-2 and IL-15 may be exploited to promote Ag-independent maturation of anti-tumor CD8(+) T cells.

Published

2003

311. Lack of terminally differentiated tumor-specific CD8+ T cells at tumor site in spite of antitumor immunity to self-antigens in human metastatic melanoma.

Author

Mortarini R, Piris A, Maurichi A, Molla A, Bersani I, Bono A, Bartoli C, Santinami M, Lombardo C, Ravagnani F, Cascinelli N, Parmiani G, and Anichini A

Subjects

Antigens, Neoplasm immunology, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes cytology, Cell Differentiation immunology, Epitopes, T-Lymphocyte immunology, Granzymes, HLA-A Antigens immunology, HLA-A2 Antigen, Humans, Immunologic Memory, Leukocyte Common Antigens immunology, Lymph Nodes immunology, Lymph Nodes pathology, MART-1 Antigen, Melanoma pathology, Melanoma secondary, Membrane Glycoproteins biosynthesis, Membrane Glycoproteins immunology, Monophenol Monooxygenase immunology, Neoplasm Proteins immunology, Neoplasm Staging, Peptide Fragments immunology, Perforin, Pore Forming Cytotoxic Proteins, Proteins immunology, Receptors, CCR7, Receptors, Chemokine immunology, Serine Endopeptidases biosynthesis, gp100 Melanoma Antigen, Autoantigens immunology, CD8-Positive T-Lymphocytes immunology, Melanoma immunology, Membrane Proteins

Abstract

Activation of CTL-mediated antitumor immunity to self-epitopes expressed by neoplastic cells is thought to be prevented, at any stage of tumor progression, by tolerance mechanisms. In contrast, in 74 American Joint Committee on Cancer stages I-IV melanoma patients, we found that development of lymph node metastases is a key event triggering CD8(+) T-cell-mediated immunity to self-epitopes encoded by melanocyte differentiation antigens. This was shown by the increased peripheral precursor frequency to Melan-A/Mart-1, gp100, and tyrosinase epitopes in stage III and IV compared with stage I and II patients, and by accumulation of functional memory T cells directed to Melan-A/Mart-1(26-35) in tumor-invaded lymph nodes. However, in tumor-invaded lymph nodes of most patients, CD8(+) T cells directed to melanocyte differentiation antigens or to tumor-restricted antigens (MAGE-3 and NY-ESO-1 epitopes), showed a CCR7(+) CD45RA(+) CD27(+) CD28(+) perforin(-) "precursor" phenotype. Only in 7 of 23 cases antigen-specific CD8(+) T cells in invaded lymph nodes showed a predominant CCR7(-) CD45RA(-) CD27(+) CD28(-) perforin(+) "preterminally differentiated" phenotype. In the latter subset of patients, by immunohistochemistry in lymph node lesions, we found that CD8(+) T lymphocytes intermingling with the neoplastic tissue expressed a CCR7(-) CD45RO(+)/RA(-) phenotype, whereas CD4(+) lymphocytes did not infiltrate the tumor. Furthermore, perforin and granzyme B were expressed on a higher fraction of the CD8(+) cells surrounding the invading tumor compared with the lymphocytes infiltrating the neoplastic tissue. In addition, no evidence for tumor regression was found in such metastatic lesions, as documented by absence of neoplastic cell necrosis or apoptosis. These data indicate that neoplastic cells in the lymph nodes and/or increased tumor burden in metastatic disease activate CD8(+) T-cell-mediated antitumor immunity to self-epitopes. However, the paucity of terminally differentiated CD8(+) T cells at tumor site suggests that immunotherapy strategies may require not only the boosting of tumor immunity, but also effective means to promote CD8(+) T-cell differentiation in the neoplastic tissue.

Published

2003

312. T-cell response to unique and shared antigens and vaccination of cancer patients.

Author

Parmiani G, Sensi M, Castelli C, Rivoltini L, and Anichini A

Subjects

Cancer Vaccines therapeutic use, Humans, Melanoma drug therapy, Melanoma pathology, Neoplasm Metastasis, Vaccination, Antigens, Neoplasm immunology, Melanoma immunology, T-Lymphocytes immunology

Abstract

Most vaccination studies of cancer patients find no clear association between clinical and immunological responses to the vaccine. We discuss the possible kinetics of the T cell response in melanoma patients against unique or shared tumor antigens. We hypothesize that a response against unique antigens prevails during primary melanoma growth, causing the selection of tumor cells lacking most of these antigens unless these are necessary to maintain the neoplastic state. After a subset of tumor cells metastasize to the lymph nodes, T cells are activated against previously ignored shared, differentiation-like antigens, owing to a new environment where pro-inflammatory cytokines can be present. The development of a T cell response to such normal epitopes then associates with tumor growth, but remains clinically inefficient. We predict that two immunologically different subsets of melanoma patients may exist, one that mounted an early immune response against melanoma antigens and one that did not. A paradox may emerge when vaccination is attempted in these two groups of subjects, with the second group being more prone to develop an effective immune response if the vaccine is potent enough to activate naive T cells, while the first has probably already eliminated most of the tumor antigens potentially recognizable by the host T cells owing to the previous selection made by the immune response developed early during tumor growth. Thus, it is likely that the subgroup of metastatic patients with a high frequency of anti-melanoma memory T cells may not show a clinical response to vaccination.

Published

2002