Your search keyword '"Forghieri, Fabio"' showing total 11 results

1. Identification and validation of diagnostic cut-offs of the ELISpot assay for the diagnosis of invasive aspergillosis in high-risk patients.

Author

Bettelli, Francesca, Vallerini, Daniela, Lagreca, Ivana, Barozzi, Patrizia, Riva, Giovanni, Nasillo, Vincenzo, Paolini, Ambra, D'Amico, Roberto, Forghieri, Fabio, Morselli, Monica, Pioli, Valeria, Gilioli, Andrea, Giusti, Davide, Messerotti, Andrea, Bresciani, Paola, Cuoghi, Angela, Colaci, Elisabetta, Marasca, Roberto, Pagano, Livio, and Candoni, Anna

Subjects

ASPERGILLOSIS, HEMATOLOGIC malignancies, T cells, SENSITIVITY & specificity (Statistics), INTERLEUKIN-10

Abstract

Objective: We investigated the performance of enzyme linked immunospot (ELISpot) assay for the diagnosis of invasive aspergillosis (IA) in high-risk patients with hematologic malignancies. Methods: We prospectively enrolled two cohorts of patients undergoing intensive myelosuppressive or immunosuppressive treatments at high risk for IA. ELISpot was performed to detect Aspergillus-specific T cells producing Interleukin-10. Results: In the discovery cohort, a derived cut-off of 40 spot forming cells (SFCs)/106 PBMCs has shown to correctly classify IA cases with a sensitivity and specificity of 89.5% and 88.6%, respectively. This cut-off is lowered to 25 SFC when considering the subset of possible IA patients, with sensitivity and specificity of 76% and 93%, respectively. The application of the 40 SFCs cut-off to the validation cohort resulted in a positivity rate of 83.3% in proven/probable cases and a negativity rate of 92.5% in possible/non-IA cases. Adopting the 25 SCFs cut-off, the assay resulted positive in 83.3% of proven/probable cases while it resulted negative in 66.7% of possible/non-IA cases. Conclusions: ELISpot shows promises in the diagnosis of IA and the possibility to use two distinct cut-offs with similar diagnostic performances according to patients' different pre-test probability of infection can widen its use in patients at risk. [ABSTRACT FROM AUTHOR]

Published

2024

2. Preclinical Validation of an Advanced Therapy Medicinal Product Based on Cytotoxic T Lymphocytes Specific for Mutated Nucleophosmin (NPM1 mut) for the Treatment of NPM1 mut -Acute Myeloid Leukemia.

Author

De Cicco, Marica, Lagreca, Ivana, Basso, Sabrina, Barozzi, Patrizia, Muscianisi, Stella, Bianco, Alba, Riva, Giovanni, Di Vincenzo, Sara, Pulvirenti, Chiara, Sapuppo, Davide, Siciliano, Mariangela, Rosti, Vittorio, Candoni, Anna, Zecca, Marco, Forghieri, Fabio, Luppi, Mario, and Comoli, Patrizia

Subjects

CYTOKINES, FLOW cytometry, CLINICAL drug trials, NUCLEOPHOSMIN, GENETIC mutation, MONONUCLEAR leukocytes, HUMAN research subjects, CELLULAR therapy, MANN Whitney U Test, INFORMED consent (Medical law), T-test (Statistics), IMMUNOPHENOTYPING, ENZYME-linked immunosorbent assay, CHI-squared test, DESCRIPTIVE statistics, RESEARCH funding, DRUG development, T cells, CELL surface antigens, HEMATOPOIETIC stem cells, HEMATOPOIETIC stem cell transplantation, DATA analysis software, IMMUNOTHERAPY, IMMUNODIAGNOSIS

Abstract

Simple Summary: Nearly 30% of adult acute myeloid leukemias (AML) harbor mutations of the nucleophosmin (NPM1) gene. These forms have a favorable outcome but, despite notable treatment advances, about 50% of patients still die of progressive disease. Thus, identification of new therapeutic opportunities is important to improve the prognosis. The aim of our study was to assess the feasibility of obtaining a cell therapy medicinal product specific for the mutated NPM1 protein from patients or healthy donors that could be employed to control leukemia and prevent hematologic relapse. We demonstrated that cytotoxic T cells specific for the mutated antigen can be reproducibly expanded, and these cells efficiently recognize and lyse leukemia blasts or other cell types carrying the NPM1-mutated antigen, without causing damage to normal hematopoietic cells. We believe that these T cells may integrate other therapy options in the treatment of patients with refractory or relapsed AML. Acute myeloid leukemia (AML) with nucleophosmin (NPM1) genetic mutations is the most common subtype in adult patients. Refractory or relapsed disease in unfit patients or after allogeneic hematopoietic stem cell transplantation (allo-HSCT) has a poor prognosis. NPM1-mutated protein, stably expressed on tumor cells but not on normal tissues, may serve as an ideal target for NPM1-mutated AML immunotherapy. The study aim was to investigate the feasibility of producing mutated-NPM1-specific cytotoxic T cells (CTLs) suitable for somatic cell therapy to prevent or treat hematologic relapse in patients with NPM1-mutated AML. T cells were expanded or primed from patient or donor peripheral blood mononuclear cells by NPM1-mutated protein-derived peptides, and tested for leukemia antigen-targeted cytotoxic activity, cytokine production and hematopoietic precursor inhibitory effect. We found that mutated-NPM1-specific CTLs, displaying specific cytokine production and high-level cytotoxicity against patients' leukemia blasts, and limited inhibitory activity in clonogenic assays, could be obtained from both patients and donors. The polyfunctional mutated-NPM1-specific CTLs included both CD8+ and CD4+ T cells endowed with strong lytic capacity. Our results suggest that mutated-NPM1-targeted CTLs may be a useful therapeutic option to control low-tumor burden relapse following conventional chemotherapy in older NPM1-mutated AML patients or eradicate persistent MRD after HSCT. [ABSTRACT FROM AUTHOR]

Published

2023

3. Mucorales-Specific T Cells in Patients with Hematologic Malignancies.

Author

Potenza, Leonardo, Vallerini, Daniela, Barozzi, Patrizia, Riva, Giovanni, Gilioli, Andrea, Forghieri, Fabio, Candoni, Anna, Cesaro, Simone, Quadrelli, Chiara, Maertens, Johan, Rossi, Giulio, Morselli, Monica, Codeluppi, Mauro, Mussini, Cristina, Colaci, Elisabetta, Messerotti, Andrea, Paolini, Ambra, Maccaferri, Monica, Fantuzzi, Valeria, and Del Giovane, Cinzia

Subjects

HEMATOLOGIC malignancies, MUCORALES, T cells, MUCORMYCOSIS, FEASIBILITY studies, IMMUNOASSAY, DIAGNOSIS, PATIENTS

Abstract

Background: Invasive mucormycosis (IM) is an emerging life-threatening fungal infection. It is difficult to obtain a definite diagnosis and to initiate timely intervention. Mucorales-specific T cells occur during the course of IM and are involved in the clearance of the infection. We have evaluated the feasibility of detecting Mucorales-specific T cells in hematological patients at risk for IM, and have correlated the detection of such cells with the clinical conditions of the patients. Methods and Findings: By using an enzyme linked immunospot assay, the presence of Mucorales-specific T cells in peripheral blood (PB) samples has been investigated at three time points during high-dose chemotherapy for hematologic malignancies. Mucorales-specific T cells producing interferon-γ, interleukin-10 and interleukin-4 were analysed in order to detect a correlation between the immune response and the clinical picture. Twenty-one (10.3%) of 204 patients, accounting for 32 (5.3%) of 598 PB samples, tested positive for Mucorales-specific T cells. Two groups could be identified. Group 1, including 15 patients without signs or symptoms of invasive fungal diseases (IFD), showed a predominance of Mucorales-specific T cells producing interferon-gamma. Group 2 included 6 patients with a clinical picture consistent with invasive fungal disease (IFD): 2 cases of proven IM and 4 cases of possible IFD. The proven patients had significantly higher number of Mucorales-specific T cells producing interleukin-10 and interleukin-4 and higher rates of positive samples by using derived diagnostic cut-offs when compared with the 15 patients without IFD. Conclusions: Mucorales-specific T cells can be detected and monitored in patients with hematologic malignancies at risk for IM. Mucorales-specific T cells polarized to the production of T helper type 2 cytokines are associated with proven IM and may be evaluated as a surrogate diagnostic marker for IM. [ABSTRACT FROM AUTHOR]

Published

2016

4. Characterization of Specific Immune Responses to Different Aspergillus Antigens during the Course of Invasive Aspergillosis in Hematologic Patients.

Author

Potenza, Leonardo, Vallerini, Daniela, Barozzi, Patrizia, Riva, Giovanni, Forghieri, Fabio, Beauvais, Anne, Beau, Remi, Candoni, Anna, Maertens, Johan, Rossi, Giulio, Morselli, Monica, Zanetti, Eleonora, Quadrelli, Chiara, Codeluppi, Mauro, Guaraldi, Giovanni, Pagano, Livio, Caira, Morena, Giovane, Cinzia Del, Maccaferri, Monica, and Stefani, Alessandro

Subjects

IMMUNE response, ASPERGILLUS, T cells, ENZYME-linked immunosorbent assay, CYTOKINES, CELL-mediated cytotoxicity, HEALTH outcome assessment

Abstract

Several studies in mouse model of invasive aspergillosis (IA) and in healthy donors have shown that different Aspergillus antigens may stimulate different adaptive immune responses. However, the occurrence of Aspergillus-specific T cells have not yet been reported in patients with the disease. In patients with IA, we have investigated during the infection: a) whether and how specific T-cell responses to different Aspergillus antigens occur and develop; b) which antigens elicit the highest frequencies of protective immune responses and, c) whether such protective T cells could be expanded ex-vivo. Forty hematologic patients have been studied, including 22 patients with IA and 18 controls. Specific T cells producing IL-10, IFN-γ, IL-4 and IL-17A have been characterized through enzyme linked immunospot and cytokine secretion assays on 88 peripheral blood (PB) samples, by using the following recombinant antigens: GEL1p, CRF1p, PEP1p, SOD1p, α1–3glucan, β1–3glucan, galactomannan. Specific T cells were expanded through short term culture. Aspergillus-specific T cells producing non-protective interleukin-10 (IL-10) and protective interferon-gamma (IFN-γ) have been detected to all the antigens only in IA patients. Lower numbers of specific T cells producing IL-4 and IL-17A have also been shown. Protective T cells targeted predominantly Aspergillus cell wall antigens, tended to increase during the IA course and to be associated with a better clinical outcome. Aspergillus-specific T cells could be successfully generated from the PB of 8 out of 8 patients with IA and included cytotoxic subsets able to lyse Aspergillus hyphae. Aspergillus specific T-cell responses contribute to the clearance of the pathogen in immunosuppressed patients with IA and Aspergillus cell wall antigens are those mainly targeted by protective immune responses. Cytotoxic specific T cells can be expanded from immunosuppressed patients even during the infection by using the above mentioned antigens. These findings may be exploited for immunotherapeutic purposes in patients with IA. [ABSTRACT FROM AUTHOR]

Published

2013

5. Neoantigen-Specific T-Cell Immune Responses: The Paradigm of NPM1 -Mutated Acute Myeloid Leukemia.

Author

Forghieri, Fabio, Riva, Giovanni, Lagreca, Ivana, Barozzi, Patrizia, Bettelli, Francesca, Paolini, Ambra, Nasillo, Vincenzo, Lusenti, Beatrice, Pioli, Valeria, Giusti, Davide, Gilioli, Andrea, Colasante, Corrado, Galassi, Laura, Catellani, Hillary, Donatelli, Francesca, Talami, Annalisa, Maffei, Rossana, Martinelli, Silvia, Potenza, Leonardo, and Marasca, Roberto

Subjects

*ACUTE myeloid leukemia, *CYTOTOXIC T cells, *IMMUNE checkpoint inhibitors, *IMMUNE response, *T cells, *THERAPEUTICS

Abstract

The C-terminal aminoacidic sequence from NPM1-mutated protein, absent in normal human tissues, may serve as a leukemia-specific antigen and can be considered an ideal target for NPM1-mutated acute myeloid leukemia (AML) immunotherapy. Different in silico instruments and in vitro/ex vivo immunological platforms have identified the most immunogenic epitopes from NPM1-mutated protein. Spontaneous development of endogenous NPM1-mutated-specific cytotoxic T cells has been observed in patients, potentially contributing to remission maintenance and prolonged survival. Genetically engineered T cells, namely CAR-T or TCR-transduced T cells, directed against NPM1-mutated peptides bound to HLA could prospectively represent a promising therapeutic approach. Although either adoptive or vaccine-based immunotherapies are unlikely to be highly effective in patients with full-blown leukemia, these strategies, potentially in combination with immune-checkpoint inhibitors, could be promising in maintaining remission or preemptively eradicating persistent measurable residual disease, mainly in patients ineligible for allogeneic hematopoietic stem cell transplant (HSCT). Alternatively, neoantigen-specific donor lymphocyte infusion derived from healthy donors and targeting NPM1-mutated protein to selectively elicit graft-versus-leukemia effect may represent an attractive option in subjects experiencing post-HSCT relapse. Future studies are warranted to further investigate dynamics of NPM1-mutated-specific immunity and explore whether novel individualized immunotherapies may have potential clinical utility in NPM1-mutated AML patients. [ABSTRACT FROM AUTHOR]

Published

2021

6. Long-term molecular remission with persistence of BCR- ABL1-specific cytotoxic T cells following imatinib withdrawal in an elderly patient with Philadelphia-positive ALL.

Author

Riva, Giovanni, Luppi, Mario, Lagreca, Ivana, Barozzi, Patrizia, Quadrelli, Chiara, Vallerini, Daniela, Zanetti, Eleonora, Basso, Sabrina, Forghieri, Fabio, Morselli, Monica, Maccaferri, Monica, Paolini, Ambra, Fantuzzi, Valeria, Messerotti, Andrea, Maffei, Rossana, Iacobucci, Ilaria, Martinelli, Giovanni, Marasca, Roberto, Narni, Franco, and Comoli, Patrizia

Subjects

LYMPHOBLASTIC leukemia diagnosis, LYMPHOBLASTIC leukemia, DRUG therapy, IMATINIB, STEROID drugs, PATIENTS

Abstract

The article presents a case study of a 75-year-old woman who was diagnosed with Philadelphia-positive acute lymphoblastic leukaemia (Ph+ALL). She underwent treatment with Imatinib with steroids, obtaining rapid complete molecular remission (CMR), and after a period of eight years of Imatinib withdrawal, reports concluded that that the withdrawal of Imatinib therapy could be safely performed in Ph+ALL patients exhibiting long-term CMR.

Published

2014

7. Inflammatory Microenvironment and Specific T Cells in Myeloproliferative Neoplasms: Immunopathogenesis and Novel Immunotherapies.

Author

Nasillo, Vincenzo, Riva, Giovanni, Paolini, Ambra, Forghieri, Fabio, Roncati, Luca, Lusenti, Beatrice, Maccaferri, Monica, Messerotti, Andrea, Pioli, Valeria, Gilioli, Andrea, Bettelli, Francesca, Giusti, Davide, Barozzi, Patrizia, Lagreca, Ivana, Maffei, Rossana, Marasca, Roberto, Potenza, Leonardo, Comoli, Patrizia, Manfredini, Rossella, and Maiorana, Antonino

Subjects

KILLER cells, SUPPRESSOR cells, HEMATOPOIETIC stem cells, SOMATIC mutation, CYTOTOXIC T cells, DENDRITIC cells, MONOCYTES, MYELOPROLIFERATIVE neoplasms, PHILADELPHIA chromosome

Abstract

The Philadelphia-negative myeloproliferative neoplasms (MPNs) are malignancies of the hematopoietic stem cell (HSC) arising as a consequence of clonal proliferation driven by somatically acquired driver mutations in discrete genes (JAK2, CALR, MPL). In recent years, along with the advances in molecular characterization, the role of immune dysregulation has been achieving increasing relevance in the pathogenesis and evolution of MPNs. In particular, a growing number of studies have shown that MPNs are often associated with detrimental cytokine milieu, expansion of the monocyte/macrophage compartment and myeloid-derived suppressor cells, as well as altered functions of T cells, dendritic cells and NK cells. Moreover, akin to solid tumors and other hematological malignancies, MPNs are able to evade T cell immune surveillance by engaging the PD-1/PD-L1 axis, whose pharmacological blockade with checkpoint inhibitors can successfully restore effective antitumor responses. A further interesting cue is provided by the recent discovery of the high immunogenic potential of JAK2V617F and CALR exon 9 mutations, that could be harnessed as intriguing targets for innovative adoptive immunotherapies. This review focuses on the recent insights in the immunological dysfunctions contributing to the pathogenesis of MPNs and outlines the potential impact of related immunotherapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2021

8. BCR-ABL-specific T-cell therapy in Ph+ ALL patients on tyrosine-kinase inhibitors.

Author

Comoli, Patrizia, Basso, Sabrina, Riva, Giovanni, Barozzi, Patrizia, Guido, Llaria, Gurrado, Antonella, Quartuccio, Giuseppe, Rubert, Laura, Lagreca, Ivana, Vallerini, Daniela, Forghieri, Fabio, Morselli, Monica, Bresciani, Paola, Cuoghi, Angela, Paolini, Ambra, Colaci, Elisabetta, Marasca, Roberto, Cuneo, Antonio, Lughetti, Lorenzo, and Trenti, Tommaso

Subjects

*T cells, *PROTEIN-tyrosine kinase inhibitors, *T-cell lymphoma, *BONE marrow, *LYMPHOBLASTIC leukemia, *HEMATOLOGY, *PATIENTS, *THERAPEUTICS

Abstract

Although the emergence of bone marrow (BM)–resident p190BCR-ABL–specific T lymphocytes has been correlated with hematologic and cytogenetic remissions in patients with Philadelphia chromosome–positive acute lymphoblastic leukemia (Ph+ ALL) undergoing maintenance tyrosine-kinase inhibitor treatment, little is known about the possibility of culturing these cells ex vivo and using them in T-cell therapy strategies. We investigated the feasibility of expanding/priming p190BCR-ABL–specific T cells in vitro by stimulation with dendritic cells pulsed with p190BCR-ABL peptides derived from the BCR-ABL junctional region and alternative splicing, and of adoptively administering them to patients with relapsed disease. We report on the feasibility of producing clinical-grade BCR-ABL–specific cytotoxic T lymphocytes (CTLs), endowed with antileukemia activity, from Ph+ ALL patients and healthy donors. We treated 3 patients with Ph+ ALL with autologous or allogeneic p190BCR-ABL–specific CTLs. No postinfusion toxicity was observed, except for a grade II skin graft-versus-host disease in the patient treated for hematologic relapse. All patients achieved a molecular or hematologic complete remission (CR) after T-cell therapy, upon emergence of p190BCR-ABL–specific T cells in the BM. Our results show that p190BCR-ABL–specific CTLs are capable of controlling treatment-refractory Ph+ ALL in vivo, and support the development of adoptive immunotherapeutic approaches with BCR-ABL CTLs in Ph+ ALL. [ABSTRACT FROM AUTHOR]

Published

2017

9. How I treat HHV8/KSHV-related diseases in posttransplant patients.

Author

Riva, Giovanni, Luppi, Mario, Barozzi, Patrizia, Forghieri, Fabio, and Potenza, Leonardo

Subjects

*HERPESVIRUS diseases, *TRANSPLANTATION of organs, tissues, etc., *KAPOSI'S sarcoma, *LYMPHOPROLIFERATIVE disorders, *T cells, *MTOR protein, *CASTLEMAN'S disease, *PATIENTS

Abstract

Posttransplantation human herpesvirus-8 (HHV8)/Kaposi sarcoma herpesvirus (KSHV) primary infection and/or reactivations are associated with uncommon and sometimes fatal, neoplastic, and non-neoplastic diseases. HHV8-related clinical manifestations notably range from Kaposi sarcoma (KS) to either primary effusion lymphoma or multicentric Castleman disease B-cell malignancies, and from polyclonal HHV8-positive plasmacytic lymphoproliferative disorders to bone marrow failure and peripheral cytopenias, associated or not with hemophagocytic syndromes, and to acute hepatitis syndromes. We reviewed the patient series reported in the literature and summarized clinical management aspects, in terms of diagnosis, follow-up, and treatment. We described typical clinical presentations and histopathologic diagnostic features of these diseases, and we discussed the role of HHV8-specific serologic, molecular, and immunologic assays, particularly focusing on recent data from HHV8-specific T-cell monitoring in posttransplantation KS patients. We finally discussed actual therapeutic options, namely, the reduction or discontinuation of immunosuppressive therapy or the switch from calcineurin inhibitors to mTOR inhibitors, as alternatives to antineoplastic chemotherapy, along with the use of antiherpesvirus agents as prophylactic or therapeutic measures, and treatment with rituximab in posttrans-plantation multicentric Castleman disease patients and non-neoplastic HHV8-associated syndromes. [ABSTRACT FROM AUTHOR]

Published

2012

10. Mucorales-specific T cells emerge in the course of invasive mucormycosis and may be used as a surrogate diagnostic marker in high-risk patients.

Author

Potenza, Leonardo, Vallerini, Daniela, Barozzi, Patrizia, Riva, Giovanni, Forghieri, Fabio, Zanetti, Eleonora, Quadrelli, Chiara, Candoni, Anna, Maertens, Johan, Rossi, Giulio, Morselli, Monica, Codeluppi, Mauro, Paolini, Ambra, Maccaferri, Monica, Giovane, Cinzia Del, D'Amico, Roberto, Rumpianesi, Fabio, Pecorari, Monica, Cavalleri, Francesca, and Marasca, Roberto

Subjects

*MUCORALES, *T cells, *MUCORMYCOSIS, *BIOMARKERS, *MYCOSES, *PREVENTION

Abstract

Mucorales-specific T cells were investigated in 28 hematologic patients during the course of their treatment. Three developed proven invasive mucormycosis (IM), 17 had infections of known origin but other than IM, and 8 never had fever during the period of observation. Mucorales-specific T cells could be detected only in patients with IM, both at diagnosis and throughout the entire course of the IM, but neither before nor for long after resolution of the infection. Such T cells predominantly produced IL-4, IFN-γ, IL-10, and to a lesser extent IL-17 and belonged to either CD4+ or CD8+ subsets. The specific T cells that produced IFN-γ were able to directly induce damage to Mucorales hyphae. None of the 25 patients without IM had Mucorales-specific T cells. Specific T cells contribute to human immune responses against fungi of the order Mucorales and could be evaluated as a surrogate diagnostic marker of IM. [ABSTRACT FROM AUTHOR]

Published

2011

11. Mucorales-Specific T Cells in Patients with Hematologic Malignancies

Author

Leonardo Potenza, Daniela Vallerini, Patrizia Barozzi, Giovanni Riva, Andrea Gilioli, Fabio Forghieri, Anna Candoni, Simone Cesaro, Chiara Quadrelli, Johan Maertens, Giulio Rossi, Monica Morselli, Mauro Codeluppi, Cristina Mussini, Elisabetta Colaci, Andrea Messerotti, Ambra Paolini, Monica Maccaferri, Valeria Fantuzzi, Cinzia Del Giovane, Alessandro Stefani, Uliano Morandi, Rossana Maffei, Roberto Marasca, Franco Narni, Renato Fanin, Patrizia Comoli, Luigina Romani, Anne Beauvais, Pier Luigi Viale, Jean Paul Latgè, Russell E Lewis, Mario Luppi, Papp, Tamás, Potenza, Leonardo, Vallerini, Daniela, Barozzi, Patrizia, Riva, Giovanni, Gilioli, Andrea, Forghieri, Fabio, Candoni, Anna, Cesaro, Simone, Quadrelli, Chiara, Maertens, Johan, Rossi, Giulio, Morselli, Monica, Codeluppi, Mauro, Mussini, Cristina, Colaci, Elisabetta, Messerotti, Andrea, Paolini, Ambra, Maccaferri, Monica, Fantuzzi, Valeria, DEL GIOVANE, Cinzia, Stefani, Alessandro, Morandi, Uliano, Maffei, Rossana, Marasca, Roberto, Narni, Franco, Fanin, Renato, Comoli, Patrizia, Romani, Luigina, Beauvais, Anne, Viale, Pierluigi, Latgè, Jean Paul, Lewis, RUSSEL EDWARD, and Luppi, Mario

Subjects

Mucorale, Myeloid, Genetics and Molecular Biology (all), 0301 basic medicine, Male, Physiology, Cancer Treatment, lcsh:Medicine, Mucormycosi, Biochemistry, Hematologic Cancers and Related Disorders, White Blood Cells, Animal Cells, Immune Physiology, Medicine and Health Sciences, Enzyme-Linked Immunoassays, lcsh:Science, Immune Response, Innate Immune System, Leukemia, Multidisciplinary, biology, T Cells, Pharmaceutics, Medicine (all), Fungal Diseases, Hematology, Middle Aged, Myeloid Leukemia, Mucormycosis, early diagnosis, T-specific cells, Interleukin 10, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Infectious Diseases, Oncology, Mucorales, Cytokines, Cancer Therapy, Female, Cellular Types, Human, Research Article, early diagnosis, Acute Myeloid Leukemia, Adult, Adolescent, T-specific cells, Immune Cells, Aged, Humans, Mucormycosis, Th2 Cells, Young Adult, Immunocompromised Host, Agricultural and Biological Sciences (all), Biochemistry, Genetics and Molecular Biology (all), 030106 microbiology, Immunology, Acute, Research and Analysis Methods, 03 medical and health sciences, Pharmacotherapy, Immune system, Drug Therapy, Diagnostic Medicine, Leukemias, medicine, Chemotherapy, Th2 Cell, Immunoassays, Interleukin 4, Blood Cells, business.industry, lcsh:R, High-Dose Chemotherapy, Biology and Life Sciences, Cancers and Neoplasms, Cell Biology, Molecular Development, medicine.disease, biology.organism_classification, Radiography, 030104 developmental biology, Immune System, Immunologic Techniques, lcsh:Q, business, Developmental Biology

Abstract

BACKGROUND: Invasive mucormycosis (IM) is an emerging life-threatening fungal infection. It is difficult to obtain a definite diagnosis and to initiate timely intervention. Mucorales-specific T cells occur during the course of IM and are involved in the clearance of the infection. We have evaluated the feasibility of detecting Mucorales-specific T cells in hematological patients at risk for IM, and have correlated the detection of such cells with the clinical conditions of the patients. METHODS AND FINDINGS: By using an enzyme linked immunospot assay, the presence of Mucorales-specific T cells in peripheral blood (PB) samples has been investigated at three time points during high-dose chemotherapy for hematologic malignancies. Mucorales-specific T cells producing interferon-γ, interleukin-10 and interleukin-4 were analysed in order to detect a correlation between the immune response and the clinical picture. Twenty-one (10.3%) of 204 patients, accounting for 32 (5.3%) of 598 PB samples, tested positive for Mucorales-specific T cells. Two groups could be identified. Group 1, including 15 patients without signs or symptoms of invasive fungal diseases (IFD), showed a predominance of Mucorales-specific T cells producing interferon-gamma. Group 2 included 6 patients with a clinical picture consistent with invasive fungal disease (IFD): 2 cases of proven IM and 4 cases of possible IFD. The proven patients had significantly higher number of Mucorales-specific T cells producing interleukin-10 and interleukin-4 and higher rates of positive samples by using derived diagnostic cut-offs when compared with the 15 patients without IFD. CONCLUSIONS: Mucorales-specific T cells can be detected and monitored in patients with hematologic malignancies at risk for IM. Mucorales-specific T cells polarized to the production of T helper type 2 cytokines are associated with proven IM and may be evaluated as a surrogate diagnostic marker for IM. ispartof: PLoS One vol:11 issue:2 ispartof: location:United States status: published

Published

2016