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1. An inflammatory Signature of Glucose Impairment in Cystic Fibrosis

Author

Montemari AL, Manco M, Fiocchi AG, Bartoli M, Facchiano F, Tabolacci C, Scatigna M, Ciciriello F, Alghisi F, Montemitro E, Carsetti R, Lucidi V, and Fiscarelli EV

Subjects
cystic fibrosis-related diabetes, cytokines, growth factors, immune mediators, impaired glucose tolerance, inflammation., Pathology, RB1-214, Therapeutics. Pharmacology, RM1-950
Abstract

Anna Lisa Montemari,1 Melania Manco,2 Alessandro Giovanni Fiocchi,3 Manuela Bartoli,4 Francesco Facchiano,5 Claudio Tabolacci,5 Maria Scatigna,6 Fabiana Ciciriello,3 Federico Alghisi,3 Enza Montemitro,3 Rita Carsetti,7 Vincenzina Lucidi,3 Ersilia Vita Fiscarelli1 1UOS Cystic Fibrosis Diagnostic, UOC Microbiology and Immunology Diagnostic, Bambino Gesù Children’s Hospital, IRCCS, Rome, Italy; 2Research Area for Multifactorial Diseases, Bambino Gesù Children’s Hospital, IRCCS, Rome, Italy; 3Cystic Fibrosis Unit, Department of Pediatrics Bambino Gesù Children’s Hospital, IRCCS, Rome, Italy; 4Department of Ophthalmology, Medical College of Georgia, Augusta University, Augusta, GA, USA; 5Department of Oncology and Molecular Medicine, Istituto Superiore Di Sanità, Rome, Italy; 6Department of Life, Health and Environmental Sciences, University of L’Aquila, L’Aquila, Italy; 7Diagnostic Immunology Unit, Department of Laboratories, B Cell Pathophysiology Unit, Immunology Research Area, Bambino Gesù Children’s Hospital, IRCCS, Rome, ItalyCorrespondence: Melania Manco, Bambino Gesù Children’s Hospital, IRCCS, piazza Sant’Onofrio 4, Rome, Italy, Tel +39 06 6859 2649, Fax +39 06 6859 2904, Email melania.manco@opbg.netObjective and Design: Cystic fibrosis-related diabetes (CFRD) is a severe complication associated with increased morbidity and mortality in cystic fibrosis (CF) patients. Extensive inflammatory state in CF leads to pancreas damage and insulin resistance with consequent altered glucose tolerance and CFRD development. The aim of the present study was to identify circulating levels of inflammatory markers specifically associated with impaired glucose tolerance (IGT) and overt CFRD in a sample of young adults with CF.Materials and Methods: Sixty-four CF outpatients, without evident active pulmonary exacerbation, infectious and autoimmune diseases, were enrolled in the study and the levels of 45 inflammatory serum mediators were measured through x magnetic bead panel multiplex technology.Results: Serum levels of PDGF-AA, CCL20/MIP3α, IFNα, CCL11/eotaxin, CXCL1/GROα, GMCSF, B7H1/PDL1, IL13, IL7, VEGF, and TGFα were all significantly (p< 0.05) elevated in patients according to glycemic status and directly correlated with glycated hemoglobin and C-reactive protein levels.Conclusion: Our findings suggest that increased levels of specific circulating inflammatory mediators are directly associated with impaired glucose tolerance in CF patients, thus, potentially implicating them in CFRD pathogenesis and warranting larger longitudinal studies to validate their monitoring as predictor of CFRD onset.Keywords: cystic fibrosis-related diabetes, cytokines, growth factors, immune mediators, impaired glucose tolerance, inflammation

Published
2022

4. GRAd-COV2 vaccine provides potent and durable humoral and cellular immunity to SARS-CoV-2 in randomized placebo-controlled phase 2 trial

Author

Capone, S, Fusco, F, Milleri, S, Borre, S, Carbonara, S, Lo Caputo, S, Leone, S, Gori, G, Maggi, P, Cascio, A, Lichtner, M, Cauda, R, Dal Zoppo, S, Cossu, M, Gori, A, Roda, S, Confalonieri, P, Bonora, S, Missale, G, Codeluppi, M, Mezzaroma, I, Capici, S, Pontali, E, Libanore, M, Diani, A, Lanini, S, Battella, S, Contino, A, Piano Mortari, E, Genova, F, Parente, G, Dragonetti, R, Colloca, S, Visani, L, Iannacone, C, Carsetti, R, Folgori, A, Camerini, R, Ziviani, L, Malescio, F, Turrini, I, Lawlor, R, Romano, A, Nunziata, M, Armato, S, Mazzeo, N, Carleo, M, Dell'Isola, C, Pisapia, R, Pontarelli, A, Olivani, A, Grasselli, S, Laccabue, D, Leoni, M, Paolillo, F, Mancini, A, Ruaro, B, Confalonieri, M, Salton, F, Mancarella, G, Marocco, R, De Masi, M, Belvisi, V, Lamonica, S, Cingolani, A, Seguiti, C, Brambilla, P, Ferraresi, A, Lupi, M, Ludovisi, S, Renisi, G, Massafra, R, Pellicciotta, M, Armiento, L, Vimercati, S, Piacenza, M, Bonfanti, P, Columpsi, P, Cazzaniga, M, Rovelli, C, Ceresini, M, Previtali, L, Trentini, L, Alcantarini, C, Rugge, W, Biffi, S, Poletti, F, Rostagno, R, Moglia, R, De Negri, F, Fini, E, Cangialosi, A, Bruno, S, Rizzo, M, Niglio, M, Stritto, A, Matano, A, Petruzziello, A, Valsecchi, P, Pieri, T, Altamura, M, Calamo, A, Giannelli, A, Menolascina, S, Di Bari, S, Mauro, V, Aronica, R, Segala, D, Cultrera, R, Sighinolfi, L, Abbott, M, Gizzi, A, Marascia, F, Valenti, G, Feasi, M, Bobbio, N, Del Puente, F, Nicosia, A, Frasca, M, Mazzoleni, M, Garofalo, N, Ammendola, V, Grazioli, F, Napolitano, F, Vitelli, A, Marcellini, V, Capone S., Fusco F. M., Milleri S., Borre S., Carbonara S., Lo Caputo S., Leone S., Gori G., Maggi P., Cascio A., Lichtner M., Cauda R., Dal Zoppo S., Cossu M. V., Gori A., Roda S., Confalonieri P., Bonora S., Missale G., Codeluppi M., Mezzaroma I., Capici S., Pontali E., Libanore M., Diani A., Lanini S., Battella S., Contino A. M., Piano Mortari E., Genova F., Parente G., Dragonetti R., Colloca S., Visani L., Iannacone C., Carsetti R., Folgori A., Camerini R., Ziviani L., Malescio F., Turrini I., Lawlor R., Romano A., Nunziata M., Armato S., Mazzeo N., Carleo M. A., Dell'Isola C., Pisapia R., Pontarelli A., Olivani A., Grasselli S., Laccabue D., Leoni M. C., Paolillo F., Mancini A., Ruaro B., Confalonieri M., Salton F., Mancarella G., Marocco R., De Masi M., Belvisi V., Lamonica S., Cingolani A., Seguiti C., Brambilla P., Ferraresi A., Lupi M., Ludovisi S., Renisi G., Massafra R., Pellicciotta M., Armiento L., Vimercati S., Piacenza M., Bonfanti P., Columpsi P., Cazzaniga M. E., Rovelli C., Ceresini M., Previtali L., Trentini L., Alcantarini C., Rugge W., Biffi S., Poletti F., Rostagno R., Moglia R., De Negri F., Fini E., Cangialosi A., Bruno S. R., Rizzo M., Niglio M., Stritto A. D., Matano A., Petruzziello A., Valsecchi P., Pieri T., Altamura M., Calamo A., Giannelli A., Menolascina S., Di Bari S., Mauro V., Aronica R., Segala D., Cultrera R., Sighinolfi L., Abbott M., Gizzi A., Marascia F. G., Valenti G., Feasi M., Bobbio N., Del Puente F., Nicosia A., Frasca M., Mazzoleni M., Garofalo N., Ammendola V., Grazioli F., Napolitano F., Vitelli A., Marcellini V., Capone, S, Fusco, F, Milleri, S, Borre, S, Carbonara, S, Lo Caputo, S, Leone, S, Gori, G, Maggi, P, Cascio, A, Lichtner, M, Cauda, R, Dal Zoppo, S, Cossu, M, Gori, A, Roda, S, Confalonieri, P, Bonora, S, Missale, G, Codeluppi, M, Mezzaroma, I, Capici, S, Pontali, E, Libanore, M, Diani, A, Lanini, S, Battella, S, Contino, A, Piano Mortari, E, Genova, F, Parente, G, Dragonetti, R, Colloca, S, Visani, L, Iannacone, C, Carsetti, R, Folgori, A, Camerini, R, Ziviani, L, Malescio, F, Turrini, I, Lawlor, R, Romano, A, Nunziata, M, Armato, S, Mazzeo, N, Carleo, M, Dell'Isola, C, Pisapia, R, Pontarelli, A, Olivani, A, Grasselli, S, Laccabue, D, Leoni, M, Paolillo, F, Mancini, A, Ruaro, B, Confalonieri, M, Salton, F, Mancarella, G, Marocco, R, De Masi, M, Belvisi, V, Lamonica, S, Cingolani, A, Seguiti, C, Brambilla, P, Ferraresi, A, Lupi, M, Ludovisi, S, Renisi, G, Massafra, R, Pellicciotta, M, Armiento, L, Vimercati, S, Piacenza, M, Bonfanti, P, Columpsi, P, Cazzaniga, M, Rovelli, C, Ceresini, M, Previtali, L, Trentini, L, Alcantarini, C, Rugge, W, Biffi, S, Poletti, F, Rostagno, R, Moglia, R, De Negri, F, Fini, E, Cangialosi, A, Bruno, S, Rizzo, M, Niglio, M, Stritto, A, Matano, A, Petruzziello, A, Valsecchi, P, Pieri, T, Altamura, M, Calamo, A, Giannelli, A, Menolascina, S, Di Bari, S, Mauro, V, Aronica, R, Segala, D, Cultrera, R, Sighinolfi, L, Abbott, M, Gizzi, A, Marascia, F, Valenti, G, Feasi, M, Bobbio, N, Del Puente, F, Nicosia, A, Frasca, M, Mazzoleni, M, Garofalo, N, Ammendola, V, Grazioli, F, Napolitano, F, Vitelli, A, Marcellini, V, Capone S., Fusco F. M., Milleri S., Borre S., Carbonara S., Lo Caputo S., Leone S., Gori G., Maggi P., Cascio A., Lichtner M., Cauda R., Dal Zoppo S., Cossu M. V., Gori A., Roda S., Confalonieri P., Bonora S., Missale G., Codeluppi M., Mezzaroma I., Capici S., Pontali E., Libanore M., Diani A., Lanini S., Battella S., Contino A. M., Piano Mortari E., Genova F., Parente G., Dragonetti R., Colloca S., Visani L., Iannacone C., Carsetti R., Folgori A., Camerini R., Ziviani L., Malescio F., Turrini I., Lawlor R., Romano A., Nunziata M., Armato S., Mazzeo N., Carleo M. A., Dell'Isola C., Pisapia R., Pontarelli A., Olivani A., Grasselli S., Laccabue D., Leoni M. C., Paolillo F., Mancini A., Ruaro B., Confalonieri M., Salton F., Mancarella G., Marocco R., De Masi M., Belvisi V., Lamonica S., Cingolani A., Seguiti C., Brambilla P., Ferraresi A., Lupi M., Ludovisi S., Renisi G., Massafra R., Pellicciotta M., Armiento L., Vimercati S., Piacenza M., Bonfanti P., Columpsi P., Cazzaniga M. E., Rovelli C., Ceresini M., Previtali L., Trentini L., Alcantarini C., Rugge W., Biffi S., Poletti F., Rostagno R., Moglia R., De Negri F., Fini E., Cangialosi A., Bruno S. R., Rizzo M., Niglio M., Stritto A. D., Matano A., Petruzziello A., Valsecchi P., Pieri T., Altamura M., Calamo A., Giannelli A., Menolascina S., Di Bari S., Mauro V., Aronica R., Segala D., Cultrera R., Sighinolfi L., Abbott M., Gizzi A., Marascia F. G., Valenti G., Feasi M., Bobbio N., Del Puente F., Nicosia A., Frasca M., Mazzoleni M., Garofalo N., Ammendola V., Grazioli F., Napolitano F., Vitelli A., and Marcellini V.

Abstract

The ongoing severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) pandemic and heterologous immunization approaches implemented worldwide for booster doses call for diversified vaccine portfolios. GRAd-COV2 is a gorilla adenovirus-based COVID-19 vaccine candidate encoding prefusion-stabilized spike. The safety and immunogenicity of GRAd-COV2 is evaluated in a dose- and regimen-finding phase 2 trial (COVITAR study, ClinicalTrials.gov: NCT04791423) whereby 917 eligible participants are randomized to receive a single intramuscular GRAd-COV2 administration followed by placebo, or two vaccine injections, or two doses of placebo, spaced over 3 weeks. Here, we report that GRAd-COV2 is well tolerated and induces robust immune responses after a single immunization; a second administration increases binding and neutralizing antibody titers. Potent, variant of concern (VOC) cross-reactive spike-specific T cell response peaks after the first dose and is characterized by high frequencies of CD8s. T cells maintain immediate effector functions and high proliferative potential over time. Thus, GRAd vector is a valuable platform for genetic vaccine development, especially when robust CD8 response is needed.

Published
2023

5. GRAd-COV2 vaccine provides potent and durable humoral and cellular immunity to SARS-CoV-2 in randomized placebo-controlled phase 2 trial

Author

Capone S., Fusco F. M., Milleri S., Borre S., Carbonara S., Lo Caputo S., Leone S., Gori G., Maggi P., Cascio A., Lichtner M., Cauda R., Dal Zoppo S., Cossu M. V., Gori A., Roda S., Confalonieri P., Bonora S., Missale G., Codeluppi M., Mezzaroma I., Capici S., Pontali E., Libanore M., Diani A., Lanini S., Battella S., Contino A. M., Piano Mortari E., Genova F., Parente G., Dragonetti R., Colloca S., Visani L., Iannacone C., Carsetti R., Folgori A., Camerini R., Ziviani L., Malescio F., Turrini I., Lawlor R., Romano A., Nunziata M., Armato S., Mazzeo N., Carleo M. A., Dell'Isola C., Pisapia R., Pontarelli A., Olivani A., Grasselli S., Laccabue D., Leoni M. C., Paolillo F., Mancini A., Ruaro B., Confalonieri M., Salton F., Mancarella G., Marocco R., De Masi M., Belvisi V., Lamonica S., Cingolani A., Seguiti C., Brambilla P., Ferraresi A., Lupi M., Ludovisi S., Renisi G., Massafra R., Pellicciotta M., Armiento L., Vimercati S., Piacenza M., Bonfanti P., Columpsi P., Cazzaniga M. E., Rovelli C., Ceresini M., Previtali L., Trentini L., Alcantarini C., Rugge W., Biffi S., Poletti F., Rostagno R., Moglia R., De Negri F., Fini E., Cangialosi A., Bruno S. R., Rizzo M., Niglio M., Stritto A. D., Matano A., Petruzziello A., Valsecchi P., Pieri T., Altamura M., Calamo A., Giannelli A., Menolascina S., Di Bari S., Mauro V., Aronica R., Segala D., Cultrera R., Sighinolfi L., Abbott M., Gizzi A., Marascia F. G., Valenti G., Feasi M., Bobbio N., Del Puente F., Nicosia A., Frasca M., Mazzoleni M., Garofalo N., Ammendola V., Grazioli F., Napolitano F., Vitelli A., Marcellini V., Capone, Stefania, Fusco, Francesco M, Milleri, Stefano, Borrè, Silvio, Carbonara, Sergio, Lo Caputo, Sergio, Leone, Sebastiano, Gori, Giovanni, Maggi, Paolo, Cascio, Antonio, Lichtner, Miriam, Cauda, Roberto, Dal Zoppo, Sarah, Cossu, Maria V, Gori, Andrea, Roda, Silvia, Confalonieri, Paola, Bonora, Stefano, Missale, Gabriele, Codeluppi, Mauro, Mezzaroma, Ivano, Capici, Serena, Pontali, Emanuele, Libanore, Marco, Diani, Augusta, Lanini, Simone, Battella, Simone, Contino, Alessandra M, Piano Mortari, Eva, Genova, Francesco, Parente, Gessica, Dragonetti, Rosella, Colloca, Stefano, Visani, Luigi, Iannacone, Claudio, Carsetti, Rita, Folgori, Antonella, Camerini, Roberto, Capone, S, Fusco, F, Milleri, S, Borre, S, Carbonara, S, Lo Caputo, S, Leone, S, Gori, G, Maggi, P, Cascio, A, Lichtner, M, Cauda, R, Dal Zoppo, S, Cossu, M, Gori, A, Roda, S, Confalonieri, P, Bonora, S, Missale, G, Codeluppi, M, Mezzaroma, I, Capici, S, Pontali, E, Libanore, M, Diani, A, Lanini, S, Battella, S, Contino, A, Piano Mortari, E, Genova, F, Parente, G, Dragonetti, R, Colloca, S, Visani, L, Iannacone, C, Carsetti, R, Folgori, A, Camerini, R, Ziviani, L, Malescio, F, Turrini, I, Lawlor, R, Romano, A, Nunziata, M, Armato, S, Mazzeo, N, Carleo, M, Dell'Isola, C, Pisapia, R, Pontarelli, A, Olivani, A, Grasselli, S, Laccabue, D, Leoni, M, Paolillo, F, Mancini, A, Ruaro, B, Confalonieri, M, Salton, F, Mancarella, G, Marocco, R, De Masi, M, Belvisi, V, Lamonica, S, Cingolani, A, Seguiti, C, Brambilla, P, Ferraresi, A, Lupi, M, Ludovisi, S, Renisi, G, Massafra, R, Pellicciotta, M, Armiento, L, Vimercati, S, Piacenza, M, Bonfanti, P, Columpsi, P, Cazzaniga, M, Rovelli, C, Ceresini, M, Previtali, L, Trentini, L, Alcantarini, C, Rugge, W, Biffi, S, Poletti, F, Rostagno, R, Moglia, R, De Negri, F, Fini, E, Cangialosi, A, Bruno, S, Rizzo, M, Niglio, M, Stritto, A, Matano, A, Petruzziello, A, Valsecchi, P, Pieri, T, Altamura, M, Calamo, A, Giannelli, A, Menolascina, S, Di Bari, S, Mauro, V, Aronica, R, Segala, D, Cultrera, R, Sighinolfi, L, Abbott, M, Gizzi, A, Marascia, F, Valenti, G, Feasi, M, Bobbio, N, Del Puente, F, Nicosia, A, Frasca, M, Mazzoleni, M, Garofalo, N, Ammendola, V, Grazioli, F, Napolitano, F, Vitelli, A, and Marcellini, V

Subjects
immunological memory, phase 2 clinical trial, safety, Sars-CoV-2 vaccine, COVID-19, CD8, T cell response, simian adenoviral vector, General Biochemistry, Genetics and Molecular Biology, CD4, neutralizing antibodie
Abstract

The ongoing severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) pandemic and heterologous immunization approaches implemented worldwide for booster doses call for diversified vaccine portfolios. GRAd-COV2 is a gorilla adenovirus-based COVID-19 vaccine candidate encoding prefusion-stabilized spike. The safety and immunogenicity of GRAd-COV2 is evaluated in a dose- and regimen-finding phase 2 trial (COVITAR study, ClinicalTrials.gov: NCT04791423) whereby 917 eligible participants are randomized to receive a single intramuscular GRAd-COV2 administration followed by placebo, or two vaccine injections, or two doses of placebo, spaced over 3weeks. Here, we report that GRAd-COV2 is well tolerated and induces robust immune responses after a single immunization; a second administration increases binding and neutralizing antibody titers. Potent, variant of concern (VOC) cross-reactive spike-specific Tcell response peaks after the first dose and is characterized by high frequencies of CD8s. Tcells maintain immediate effector functions and high proliferative potential over time. Thus, GRAd vector is a valuable platform for genetic vaccine development, especially when robust CD8 response is needed.

Published
2023

6. Persistent B cell memory after SARS-CoV-2 vaccination is functional during breakthrough infections

Author

Terreri, S., Piano Mortari, E., Vinci, M. R., Russo, C., Alteri, C., Albano, C., Colavita, F., Gramigna, G., Agrati, C., Linardos, G., Coltella, L., Colagrossi, L., Deriu, G., Ciofi Degli Atti, M., Rizzo, C., Scarsella, M., Brugaletta, R., Camisa, V., Santoro, A., Roscilli, G., Pavoni, E., Muzi, A., Magnavita, N., Scutari, R., Villani, A., Raponi, M., Locatelli, F., Perno, C. F., Zaffina, S., Carsetti, R., Piano Mortari E., Vinci M. R., Deriu G., Camisa V., Muzi A., Magnavita N. (ORCID:0000-0002-0988-7344), Villani A., Locatelli F. (ORCID:0000-0002-1268-0125), Zaffina S. (ORCID:0000-0002-8858-5423), Carsetti R., Terreri, S., Piano Mortari, E., Vinci, M. R., Russo, C., Alteri, C., Albano, C., Colavita, F., Gramigna, G., Agrati, C., Linardos, G., Coltella, L., Colagrossi, L., Deriu, G., Ciofi Degli Atti, M., Rizzo, C., Scarsella, M., Brugaletta, R., Camisa, V., Santoro, A., Roscilli, G., Pavoni, E., Muzi, A., Magnavita, N., Scutari, R., Villani, A., Raponi, M., Locatelli, F., Perno, C. F., Zaffina, S., Carsetti, R., Piano Mortari E., Vinci M. R., Deriu G., Camisa V., Muzi A., Magnavita N. (ORCID:0000-0002-0988-7344), Villani A., Locatelli F. (ORCID:0000-0002-1268-0125), Zaffina S. (ORCID:0000-0002-8858-5423), and Carsetti R.

Abstract

Breakthrough SARS-CoV-2 infections in fully vaccinated individuals are considered a consequence of waning immunity. Serum antibodies represent the most measurable outcome of vaccine-induced B cell memory. When antibodies decline, memory B cells are expected to persist and perform their function, preventing clinical disease. We investigated whether BNT162b2 mRNA vaccine induces durable and functional B cell memory in vivo against SARS-CoV-2 3, 6, and 9 months after the second dose in a cohort of health care workers (HCWs). While we observed physiological decline of SARS-CoV-2-specific antibodies, memory B cells persist and increase until 9 months after immunization. HCWs with breakthrough infections had no signs of waning immunity. In 3–4 days, memory B cells responded to SARS-CoV-2 infection by producing high levels of specific antibodies in the serum and anti-Spike IgA in the saliva. Antibodies to the viral nucleoprotein were produced with the slow kinetics typical of the response to a novel antigen.

Published
2022

8. Inflammatory and senescence-associated mediators affect the persistence of humoral response to COVID-19 mRNA vaccination in transfusion-dependent beta-thalassemic patients

Author

Bordoni, V., Casale, M., Pinto, V. M., Carsetti, R., Gianesin, B., Gamberini, M. R., Mazdai, L., Barella, S., Denotti, A. R., Colavita, F., Perrotta, S., Maggio, A., Pitrolo, L., Quintino, S., Caminati, M., Mazzi, F., Ceolan, J., De Franceschi, L., Forni, G. L., Locatelli, Franco, Agrati, C., Locatelli F. (ORCID:0000-0002-7976-3654), Bordoni, V., Casale, M., Pinto, V. M., Carsetti, R., Gianesin, B., Gamberini, M. R., Mazdai, L., Barella, S., Denotti, A. R., Colavita, F., Perrotta, S., Maggio, A., Pitrolo, L., Quintino, S., Caminati, M., Mazzi, F., Ceolan, J., De Franceschi, L., Forni, G. L., Locatelli, Franco, Agrati, C., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

N/A

Published
2023

9. The molecular mechanism of B cell activation by toll-like receptor protein RP-105.

Author

Chan, VW, Mecklenbräuker, I, Su, I, Texido, G, Leitges, M, Carsetti, R, Lowell, CA, Rajewsky, K, Miyake, K, and Tarakhovsky, A

Subjects
Spleen, B-Lymphocytes, Cells, Cultured, Animals, Mice, Knockout, Mice, Calcium, Protein Kinases, Mitogen-Activated Protein Kinase Kinases, Protein Kinase C, src-Family Kinases, Immunoglobulin M, Membrane Glycoproteins, Drosophila Proteins, Membrane Proteins, Receptors, Cell Surface, Flow Cytometry, Signal Transduction, Cell Division, Enzyme Activation, Phosphorylation, Toll-Like Receptors, RP-105, B lymphocytes, signal transduction, mice, Cells, Cultured, Knockout, Receptors, Cell Surface, Medical and Health Sciences, Immunology
Abstract

The B cell-specific transmembrane protein RP-105 belongs to the family of Drosophila toll-like proteins which are likely to trigger innate immune responses in mice and man. Here we demonstrate that the Src-family protein tyrosine kinase Lyn, protein kinase C beta I/II (PKCbetaI/II), and Erk2-specific mitogen-activated protein (MAP) kinase kinase (MEK) are essential and probably functionally connected elements of the RP-105-mediated signaling cascade in B cells. We also find that negative regulation of RP-105-mediated activation of MAP kinases by membrane immunoglobulin may account for the phenomenon of antigen receptor-mediated arrest of RP-105-mediated B cell proliferation.

Published
1998

10. The response to BTN62b2 booster doses demonstrates that serum antibodies do not predict the establishment of immune B-cell memory in common variable immune deficiencies

Author

Piano Mortari, E., primary, Pulvirenti, F., additional, Marcellini, V., additional, Terreri, S., additional, Fernandez Salinas, A., additional, Ferrari, S., additional, Di Napoli, G., additional, Guadagnolo, D., additional, Sculco, E., additional, Albano, C., additional, Guercio, M., additional, Di Cecca, S., additional, Milito, C., additional, Garzi, G., additional, Pesce, A.M., additional, Bonanni, L., additional, Sinibaldi, M., additional, Di Cecilia, S., additional, Agrati, C., additional, Quintarelli, C., additional, Zaffina, S., additional, Locatelli, F., additional, Carsetti, R., additional, and Quinti, I., additional

Published
2022
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11. The Immune Response to SARS-CoV-2 Vaccination: Insights Learned From Adult Patients With Common Variable Immune Deficiency

Author

Quinti, I., Locatelli, Franco, Carsetti, R., Locatelli F. (ORCID:0000-0002-7976-3654), Quinti, I., Locatelli, Franco, Carsetti, R., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

CVID patients have an increased susceptibility to vaccine-preventable infections. The question on the potential benefits of immunization of CVID patients against SARS-CoV-2 offered the possibility to analyze the defective mechanisms of immune responses to a novel antigen. In CVID, as in immunocompetent subjects, the role of B and T cells is different between infected and vaccinated individuals. Upon vaccination, variable anti-Spike IgG responses have been found in different CVID cohorts. Immunization with two doses of mRNA vaccine did not generate Spike-specific classical memory B cells (MBCs) but atypical memory B cells (ATM) with low binding capacity to Spike protein. Spike-specific T-cells responses were also induced in CVID patients with a variable frequency, differently from specific T cells produced after multiple exposures to viral antigens following influenza virus immunization and infection. The immune response elicited by SARS-CoV-2 infection was enhanced by subsequent immunization underlying the need to immunize convalescent COVID-19 CVID patients after recovery. In particular, immunization after SARS-Cov-2 infection generated Spike-specific classical memory B cells (MBCs) with low binding capacity to Spike protein and Spike-specific antibodies in a high percentage of CVID patients. The search for a strategy to elicit an adequate immune response post-vaccination in CVID patients is necessary. Since reinfection with SARS-CoV-2 has been documented, at present SARS-CoV-2 positive CVID patients might benefit from new preventing strategy based on administration of anti-SARS-CoV-2 monoclonal antibodies.

Published
2022

12. The immune response as a double-edged sword: The lesson learnt during the COVID-19 pandemic

Author

Agrati, C., Carsetti, R., Bordoni, V., Sacchi, A., Quintarelli, C., Locatelli, Franco, Ippolito, G., Capobianchi, M. R., Locatelli F. (ORCID:0000-0002-7976-3654), Agrati, C., Carsetti, R., Bordoni, V., Sacchi, A., Quintarelli, C., Locatelli, Franco, Ippolito, G., Capobianchi, M. R., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

The COVID-19 pandemic has represented an unprecedented challenge for the humanity, and scientists around the world provided a huge effort to elucidate critical aspects in the fight against the pathogen, useful in designing public health strategies, vaccines and therapeutic approaches. One of the first pieces of evidence characterizing the SARS-CoV-2 infection has been its breadth of clinical presentation, ranging from asymptomatic to severe/deadly disease, and the indication of the key role played by the immune response in influencing disease severity. This review is aimed at summarizing what the SARS-CoV-2 infection taught us about the immune response, highlighting its features of a double-edged sword mediating both protective and pathogenic processes. We will discuss the protective role of soluble and cellular innate immunity and the detrimental power of a hyper-inflammation-shaped immune response, resulting in tissue injury and immunothrombotic events. We will review the importance of B- and T-cell immunity in reducing the clinical severity and their ability to cross-recognize viral variants.

Published
2022

13. Case Report: Precision COVID-19 Immunization Strategy to Overcome Individual Fragility: A Case of Generalized Lipodystrophy Type 4

Author

Zaffina, S., Piano Mortari, E., Di Prinzio, R. R., Cappa, M., Novelli, A., Agolini, E., Raponi, M., Dallapiccola, B., Locatelli, Franco, Perno, C. F., Carsetti, R., Locatelli F. (ORCID:0000-0002-7976-3654), Zaffina, S., Piano Mortari, E., Di Prinzio, R. R., Cappa, M., Novelli, A., Agolini, E., Raponi, M., Dallapiccola, B., Locatelli, Franco, Perno, C. F., Carsetti, R., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

A 48-year-old patient affected with congenital generalized lipodystrophy type 4 failed to respond to two doses of the BNT162b2 vaccine, consisting of lipid nanoparticle encapsulated mRNA. As the disease is caused by biallelic variants of CAVIN1, a molecule indispensable for lipid endocytosis and regulation, we complemented the vaccination cycle with a single dose of the Ad26.COV2 vaccine. Adenovirus-based vaccine entry is mediated by the interaction with adenovirus receptors and transport occurs in clathrin-coated pits. Ten days after Ad26.COV2 administration, S- and RBD-specific antibodies and high-affinity memory B cells increased significantly to values close to those observed in Health Care Worker controls.

Published
2022

14. Impaired memory B-cell response to the Pfizer-BioNTech COVID-19 vaccine in patients with common variable immunodeficiency

Author

Fernandez Salinas, A., Piano Mortari, E., Terreri, S., Milito, C., Zaffina, S., Perno, C. F., Locatelli, Franco, Quinti, I., Carsetti, R., Locatelli F. (ORCID:0000-0002-7976-3654), Fernandez Salinas, A., Piano Mortari, E., Terreri, S., Milito, C., Zaffina, S., Perno, C. F., Locatelli, Franco, Quinti, I., Carsetti, R., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

no abstract

Published
2022

15. The BNT162b2 vaccine induces humoral and cellular immune memory to SARS-CoV-2 Wuhan strain and the Omicron variant in children 5 to 11 years of age

Author

Cinicola, B. L., Piano Mortari, E., Zicari, A. M., Agrati, C., Bordoni, V., Albano, C., Fedele, G., Schiavoni, I., Leone, P., Fiore, S., Capponi, M., Conti, M. G., Petrarca, L., Stefanelli, P., Spalice, A., Midulla, F., Palamara, A. T., Quinti, I., Locatelli, Franco, Carsetti, R., Locatelli F. (ORCID:0000-0002-7976-3654), Cinicola, B. L., Piano Mortari, E., Zicari, A. M., Agrati, C., Bordoni, V., Albano, C., Fedele, G., Schiavoni, I., Leone, P., Fiore, S., Capponi, M., Conti, M. G., Petrarca, L., Stefanelli, P., Spalice, A., Midulla, F., Palamara, A. T., Quinti, I., Locatelli, Franco, Carsetti, R., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

SARS-CoV-2 mRNA vaccines prevent severe COVID-19 by generating immune memory, comprising specific antibodies and memory B and T cells. Although children are at low risk of severe COVID-19, the spreading of highly transmissible variants has led to increasing in COVID-19 cases and hospitalizations also in the youngest, but vaccine coverage remains low. Immunogenicity to mRNA vaccines has not been extensively studied in children 5 to 11 years old. In particular, cellular immunity to the wild-type strain (Wuhan) and the cross-reactive response to the Omicron variant of concern has not been investigated. We assessed the humoral and cellular immune response to the SARS-CoV-2 BNT162b2 vaccine in 27 healthy children. We demonstrated that vaccination induced a potent humoral and cellular immune response in all vaccinees. By using spike-specific memory B cells as a measurable imprint of a previous infection, we found that 50% of the children had signs of a past, undiagnosed infection before vaccination. Children with pre-existent immune memory generated significantly increased levels of specific antibodies, and memory T and B cells, directed against not only the wild type virus but also the omicron variant.

Published
2022

18. COVID-19 - pathogenesis and immunological findings across the clinical manifestation spectrum

Author

Carsetti, R., Quinti, I., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Carsetti, R., Quinti, I., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Purpose of reviewThe wide spectrum of COVID-19 clinical manifestations demonstrates the determinant role played by the individual immune response to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) in the course of the disease. Thanks to the large number of published data, we are beginning to understand the logic of the human response to a virus adapted to bat immunity.Recent findingsImpairment of types I and III interferon responses may facilitate the occurrence of severe COVID-19 with reduced antiviral activity associated to potent inflammation. The human T and B-cell germline repertoire contain the specificities able to react against SARS-CoV-2 antigens. Although inflammation disrupts the structure of germinal centers, memory T and B cells can be found in the blood of patients after mild and severe COVID 19.SummaryFurther studies are indispensable to better understand the human immune response to SARS-CoV-2. The diversity of the individual reaction may contribute to explain the clinical manifestation spectrum. Immunological memory can be demonstrated in patients, convalescent from mild, moderate, or severe COVID-19, but we do not know whether asymptomatic individuals have memory of the virus. Tailored vaccination protocols may be needed for individuals with previous SAS-CoV-2 infection.

Published
2021

19. SARS-CoV-2 Vaccine Induced Atypical Immune Responses in Antibody Defects: Everybody Does their Best

Author

Salinas, A. F., Mortari, E. P., Terreri, S., Quintarelli, C., Pulvirenti, F., Di Cecca, S., Guercio, M., Milito, C., Bonanni, L., Auria, S., Romaggioli, L., Cusano, G., Albano, C., Zaffina, S., Perno, C. F., Spadaro, G., Locatelli, Franco, Carsetti, R., Quinti, I., Locatelli F. (ORCID:0000-0002-7976-3654), Salinas, A. F., Mortari, E. P., Terreri, S., Quintarelli, C., Pulvirenti, F., Di Cecca, S., Guercio, M., Milito, C., Bonanni, L., Auria, S., Romaggioli, L., Cusano, G., Albano, C., Zaffina, S., Perno, C. F., Spadaro, G., Locatelli, Franco, Carsetti, R., Quinti, I., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Background: Data on immune responses to SARS-CoV-2 in patients with Primary Antibody Deficiencies (PAD) are limited to infected patients and to heterogeneous cohorts after immunization. Methods: Forty-one patients with Common Variable Immune Deficiencies (CVID), six patients with X-linked Agammaglobulinemia (XLA), and 28 healthy age-matched controls (HD) were analyzed for anti-Spike and anti-receptor binding domain (RBD) antibody production, generation of Spike-specific memory B-cells, and Spike-specific T-cells before vaccination and one week after the second dose of BNT162b2 vaccine. Results: The vaccine induced Spike-specific IgG and IgA antibody responses in all HD and in 20% of SARS-CoV-2 naive CVID patients. Anti-Spike IgG were detectable before vaccination in 4 out 7 CVID previously infected with SARS-CoV-2 and were boosted in six out of seven patients by the subsequent immunization raising higher levels than patients naïve to infection. While HD generated Spike-specific memory B-cells, and RBD-specific B-cells, CVID generated Spike-specific atypical B-cells, while RBD-specific B-cells were undetectable in all patients, indicating the incapability to generate this new specificity. Specific T-cell responses were evident in all HD and defective in 30% of CVID. All but one patient with XLA responded by specific T-cell only. Conclusion: In PAD patients, early atypical immune responses after BNT162b2 immunization occurred, possibly by extra-follicular or incomplete germinal center reactions. If these responses to vaccination might result in a partial protection from infection or reinfection is now unknown. Our data suggests that SARS-CoV-2 infection more effectively primes the immune response than the immunization alone, possibly suggesting the need for a third vaccine dose for patients not previously infected.

Published
2021

20. B cell response induced by SARS-CoV-2 infection is boosted by the BNT162b2 vaccine in primary antibody deficiencies

Author

Pulvirenti, F., Salinas, A. F., Milito, C., Terreri, S., Mortari, E. P., Quintarelli, C., Di Cecca, S., Lagnese, G., Punziano, A., Guercio, M., Bonanni, L., Auria, S., Villani, F., Albano, C., Locatelli, Franco, Spadaro, G., Carsetti, R., Quinti, I., Locatelli F. (ORCID:0000-0002-7976-3654), Pulvirenti, F., Salinas, A. F., Milito, C., Terreri, S., Mortari, E. P., Quintarelli, C., Di Cecca, S., Lagnese, G., Punziano, A., Guercio, M., Bonanni, L., Auria, S., Villani, F., Albano, C., Locatelli, Franco, Spadaro, G., Carsetti, R., Quinti, I., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Background: Patients with primary antibody deficiencies are at risk in the current COVID-19 pandemic due to their impaired response to infection and vaccination. Specifically, patients with common variable immunodeficiency (CVID) generated poor spike-specific antibody and T cell responses after immunization. Methods: Thirty-four CVID convalescent patients after SARS-CoV-2 infection, 38 CVID patients immunized with two doses of the BNT162b2 vaccine, and 20 SARS-CoV-2 CVID convalescents later and immunized with BNT162b2 were analyzed for the anti-spike IgG production and the generation of spike-specific memory B cells and T cells. Results: Spike-specific IgG was induced more frequently after infection than after vaccination (82% vs. 34%). The antibody response was boosted in convalescents by vaccination. Although immunized patients generated atypical memory B cells possibly by extra-follicular or incomplete germinal center reactions, convalescents responded to infection by generating spike-specific memory B cells that were improved by the subsequent immunization. Poor spike-specific T cell responses were measured independently from the immunological challenge. Conclusions: SARS-CoV-2 infection primed a more efficient classical memory B cell response, whereas the BNT162b2 vaccine induced non-canonical B cell responses in CVID. Natural infection responses were boosted by subsequent immunization, suggesting the possibility to further stimulate the immune response by additional vaccine doses in CVID.

Published
2021

21. Highly specific memory b cells generation after the 2nd dose of bnt162b2 vaccine compensate for the decline of serum antibodies and absence of mucosal iga

Author

Mortari, E. P., Russo, C., Vinci, Maria Rosaria, Terreri, S., Salinas, A. F., Piccioni, L., Alteri, C., Colagrossi, L., Coltella, L., Ranno, S., Linardos, G., Agosta, Marilena, Albano, C., Agrati, C., Castilletti, C., Meschi, S., Romania, P., Roscilli, G., Pavoni, E., Camisa, Vincenzo, Santoro, A., Brugaletta, R., Magnavita, Nicola, Ruggiero, Antonio, Cotugno, N., Amodio, D., Atti, M. L. C. D., Giorgio, D., Russo, N., Salvatori, G., Corsetti, T., Locatelli, Federica, Perno, C. F., Zaffina, Salvatore, Carsetti, Rita, Vinci M. R., Agosta M., Camisa V., Magnavita N. (ORCID:0000-0002-0988-7344), Ruggiero A. (ORCID:0000-0002-6052-3511), Locatelli F. (ORCID:0000-0002-1268-0125), Zaffina S. (ORCID:0000-0002-8858-5423), Carsetti R., Mortari, E. P., Russo, C., Vinci, Maria Rosaria, Terreri, S., Salinas, A. F., Piccioni, L., Alteri, C., Colagrossi, L., Coltella, L., Ranno, S., Linardos, G., Agosta, Marilena, Albano, C., Agrati, C., Castilletti, C., Meschi, S., Romania, P., Roscilli, G., Pavoni, E., Camisa, Vincenzo, Santoro, A., Brugaletta, R., Magnavita, Nicola, Ruggiero, Antonio, Cotugno, N., Amodio, D., Atti, M. L. C. D., Giorgio, D., Russo, N., Salvatori, G., Corsetti, T., Locatelli, Federica, Perno, C. F., Zaffina, Salvatore, Carsetti, Rita, Vinci M. R., Agosta M., Camisa V., Magnavita N. (ORCID:0000-0002-0988-7344), Ruggiero A. (ORCID:0000-0002-6052-3511), Locatelli F. (ORCID:0000-0002-1268-0125), Zaffina S. (ORCID:0000-0002-8858-5423), and Carsetti R.

Abstract

Specific memory B cells and antibodies are a reliable read-out of vaccine efficacy. We analysed these biomarkers after one and two doses of BNT162b2 vaccine. The second dose significantly increases the level of highly specific memory B cells and antibodies. Two months after the second dose, specific antibody levels decline, but highly specific memory B cells continue to increase, thus predicting a sustained protection from COVID-19. We show that although mucosal IgA is not induced by the vaccination, memory B cells migrate in response to inflammation and secrete IgA at mucosal sites. We show that the first vaccine dose may lead to an insufficient number of highly specific memory B cells and low concentration of serum antibodies, thus leaving vaccinees without the immune robustness needed to ensure viral elimination and herd immunity. We also clarify that the reduction of serum antibodies does not diminish the force and duration of the immune protection induced by vaccination. The vaccine does not induce sterilizing immunity. Infection after vaccination may be caused by the lack of local preventive immunity because of the absence of mucosal IgA.

Published
2021

22. Evolution of Human Memory B Cells From Childhood to Old Age

Author

Ciocca, M., Zaffina, Salvatore, Fernandez Salinas, A., Bocci, C., Palomba, P., Conti, M. G., Terreri, S., Frisullo, Giovanni, Giorda, E., Scarsella, M., Brugaletta, R., Vinci, Maria Rosaria, Magnavita, Nicola, Carsetti, Rita, Piano Mortari, E., Zaffina S. (ORCID:0000-0002-8858-5423), Frisullo G., Vinci M. R., Magnavita N. (ORCID:0000-0002-0988-7344), Carsetti R., Ciocca, M., Zaffina, Salvatore, Fernandez Salinas, A., Bocci, C., Palomba, P., Conti, M. G., Terreri, S., Frisullo, Giovanni, Giorda, E., Scarsella, M., Brugaletta, R., Vinci, Maria Rosaria, Magnavita, Nicola, Carsetti, Rita, Piano Mortari, E., Zaffina S. (ORCID:0000-0002-8858-5423), Frisullo G., Vinci M. R., Magnavita N. (ORCID:0000-0002-0988-7344), and Carsetti R.

Abstract

High quality medical assistance and preventive strategies, including pursuing a healthy lifestyle, result in a progressively growing percentage of older people. The population and workforce is aging in all countries of the world. It is widely recognized that older individuals show an increased susceptibility to infections and a reduced response to vaccination suggesting that the aged immune system is less able to react and consequently protect the organism. The SARS-CoV-2 pandemic is dramatically showing us that the organism reacts to novel pathogens in an age-dependent manner. The decline of the immune system observed in aging remains unclear. We aimed to understand the role of B cells. We analyzed peripheral blood from children (4-18 years); young people (23-60 years) and elderly people (65-91 years) by flow cytometry. We also measured antibody secretion by ELISA following a T-independent stimulation. Here we show that the elderly have a significant reduction of CD27dull memory B cells, a population that bridges innate and adaptive immune functions. In older people, memory B cells are mostly high specialized antigen-selected CD27bright. Moreover, after in vitro stimulation with CpG, B cells from older individuals produced significantly fewer IgM and IgA antibodies compared to younger individuals. Aging is a complex process characterized by a functional decline in multiple physiological systems. The immune system of older people is well equipped to react to often encountered antigens but has a low ability to respond to new pathogens.

Published
2021

23. Recurrence, Reactivation, or Inflammatory Rebound of SARS-CoV-2 Infection With Acute Vestibular Symptoms: A Case Report and Revision of Literature

Author

Zaffina, Salvatore, Lanteri, P., Gilardi, F., Garbarino, Sergio, Santoro, A., Vinci, Maria Rosaria, Carsetti, Rita, Scorpecci, A., Raponi, M., Magnavita, Nicola, Camisa, Vincenzo, Zaffina S. (ORCID:0000-0002-8858-5423), Garbarino S., Vinci M. R., Carsetti R., Magnavita N. (ORCID:0000-0002-0988-7344), Camisa V., Zaffina, Salvatore, Lanteri, P., Gilardi, F., Garbarino, Sergio, Santoro, A., Vinci, Maria Rosaria, Carsetti, Rita, Scorpecci, A., Raponi, M., Magnavita, Nicola, Camisa, Vincenzo, Zaffina S. (ORCID:0000-0002-8858-5423), Garbarino S., Vinci M. R., Carsetti R., Magnavita N. (ORCID:0000-0002-0988-7344), and Camisa V.

Abstract

A case of recurrent coronavirus disease 2019 (COVID-19) with neurovestibular symptoms was reported. In March 2020, a physician working in an Italian pediatric hospital had flu-like symptoms with anosmia and dysgeusia, and following a reverse transcription PCR (RT/PCR) test with a nasopharyngeal swab tested positive for SARS-CoV-2. After home quarantine, 21 days from the beginning of the symptoms, the patient tested negative in two subsequent swabs and was declared healed and readmitted to work. Serological testing showed a low level of immunoglobulin G (IgG) antibody title and absence of immunoglobulin M (IgM). However, 2 weeks later, before resuming work, the patient complained of acute vestibular syndrome, and the RT/PCR test with mucosal swab turned positive. On the basis of the literature examined and reviewed for recurrence cases and vestibular symptoms during COVID-19, to our knowledge this case is the first case of recurrence with vestibular impairment as a neurological symptom, and we defined it as probably a viral reactivation. The PCR retest positivity cannot differentiate re-infectivity, relapse, and dead-viral RNA detection. Serological antibody testing and viral genome sequencing could be always performed in recurrence cases.

Published
2021

26. The immune system of children: the key to understanding SARS-CoV-2 susceptibility?

Author

Carsetti, R., Quintarelli, C., Quinti, I., Piano Mortari, E., Zumla, A., Ippolito, G., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Carsetti, R., Quintarelli, C., Quinti, I., Piano Mortari, E., Zumla, A., Ippolito, G., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

no abstract available

Published
2020

27. HLA allele frequencies and susceptibility to COVID-19 in a group of 99 Italian patients

Author

Novelli, A., Andreani, M., Biancolella, M., Liberatoscioli, L., Passarelli, C., Colona, V. L., Rogliani, P., Leonardis, F., Campana, A., Carsetti, R., Andreoni, M., Bernardini, S., Novelli, G., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Novelli, A., Andreani, M., Biancolella, M., Liberatoscioli, L., Passarelli, C., Colona, V. L., Rogliani, P., Leonardis, F., Campana, A., Carsetti, R., Andreoni, M., Bernardini, S., Novelli, G., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

With the aim to individuate alleles that may reflect a higher susceptibility to the disease, in the present study we analyzed the HLA allele frequency distribution in a group of 99 Italian patients affected by a severe or extremely severe form of COVID-19. After the application of Bonferroni's correction for multiple tests, a significant association was found for HLA-DRB1*15:01, -DQB1*06:02 and -B*27:07, after comparing the results to a reference group of 1017 Italian individuals, previously typed in our laboratory. The increased frequencies observed may contribute to identify potential markers of susceptibility to the disease, although controversial results on the role of single HLA alleles in COVID-19 patients have been recently reported.

Published
2020

28. The Interplay between CD27dull and CD27bright B Cells Ensures the Flexibility, Stability, and Resilience of Human B Cell Memory

Author

Grimsholm, O., Piano Mortari, E., Davydov, A. N., Shugay, M., Obraztsova, A. S., Bocci, C., Marasco, E., Marcellini, V., Aranburu, A., Farroni, C., Silvestris, D. A., Cristofoletti, C., Giorda, E., Scarsella, M., Cascioli, S., Barresi, S., Lougaris, V., Plebani, A., Cancrini, C., Finocchi, A., Moschese, V., Valentini, D., Vallone, C., Signore, F., de Vincentiis, G., Zaffina, S., Russo, G., Gallo, A., Locatelli, Franco, Tozzi, A. E., Tartaglia, M., Chudakov, D. M., Carsetti, R., Locatelli F. (ORCID:0000-0002-7976-3654), Grimsholm, O., Piano Mortari, E., Davydov, A. N., Shugay, M., Obraztsova, A. S., Bocci, C., Marasco, E., Marcellini, V., Aranburu, A., Farroni, C., Silvestris, D. A., Cristofoletti, C., Giorda, E., Scarsella, M., Cascioli, S., Barresi, S., Lougaris, V., Plebani, A., Cancrini, C., Finocchi, A., Moschese, V., Valentini, D., Vallone, C., Signore, F., de Vincentiis, G., Zaffina, S., Russo, G., Gallo, A., Locatelli, Franco, Tozzi, A. E., Tartaglia, M., Chudakov, D. M., Carsetti, R., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Grimsholm et al. show that CD27dull and CD27bright represent sequential MBC developmental stages. T cell- and germinal center (GC)-independent CD27dull MBCs are the plastic source of strongly selected and GC-dependent CD27bright MBCs. CD27dull MBCs, able to expand and differentiate in response to change, ensure stability and flexibility of human B cell memory.

Published
2020

29. Partial T cell defects and expanded CD56bright NK cells in an SCID patient carrying hypomorphic mutation in the IL2RG gene

Author

Cifaldi, C., Cotugno, N., Di Cesare, S., Giliani, S., Di Matteo, G., Amodio, D., Piano Mortari, E., Chiriaco, M., Buonsenso, D., Zangari, P., Pagliara, D., Gaspari, S., Carsetti, R., Palma, P., Finocchi, A., Locatelli, Franco, Rossi, P., Doria, M., Cancrini, C., Locatelli F. (ORCID:0000-0002-7976-3654), Cifaldi, C., Cotugno, N., Di Cesare, S., Giliani, S., Di Matteo, G., Amodio, D., Piano Mortari, E., Chiriaco, M., Buonsenso, D., Zangari, P., Pagliara, D., Gaspari, S., Carsetti, R., Palma, P., Finocchi, A., Locatelli, Franco, Rossi, P., Doria, M., Cancrini, C., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

X-linked severe combined immunodeficiency (X-SCID) caused by full mutation of the IL2RG gene leads to T− B+ NK− phenotype and is usually associated with severe opportunistic infections, diarrhea, and failure to thrive. When IL2RG hypomorphic mutation occurs, diagnosis could be delayed and challenging since only moderate reduction of T and NK cells may be present. Here, we explored phenotypic insights and the impact of the p.R222C hypomorphic mutation (IL2RGR222C) in distinct cell subsets in an 8-month-old patient with atypical X-SCID. We found reduced CD4+ T cell counts, a decreased frequency of naïve CD4+ and CD8+ T cells, and an expansion of B cells. Ex vivo STAT5 phosphorylation was impaired in CD4+CD45RO+ T cells, yet compensated by supraphysiological doses of IL-2. Sanger sequencing on purified cell subsets showed a partial reversion of the mutation in total CD3+ cells, specifically in recent thymic emigrants (RTE), effector memory (EM), and CD45RA+ terminally differentiated EM (EMRA) CD4+ T cells. Of note, patient's NK cells had a normal frequency compared to age-matched healthy subjects, but displayed an expansion of CD56bright cells with higher perforin content and cytotoxic potential, associated with accumulation of NK-cell stimulatory cytokines (IL-2, IL-7, IL-15). Overall, this report highlights an alteration in the NK-cell compartment that, together with the high disease-phenotype variability, should be considered in the suspicion of X-SCID with hypomorphic IL2RG mutation.

Published
2020

30. Different Innate and Adaptive Immune Responses to SARS-CoV-2 Infection of Asymptomatic, Mild, and Severe Cases

Author

Carsetti, R., Zaffina, S., Piano Mortari, E., Terreri, S., Corrente, F., Capponi, C., Palomba, P., Mirabella, M., Cascioli, S., Palange, P., Cuccaro, I., Milito, C., Zumla, A., Maeurer, M., Camisa, V., Vinci, M. R., Santoro, A., Cimini, E., Marchioni, L., Nicastri, E., Palmieri, F., Agrati, C., Ippolito, G., Porzio, O., Concato, C., Onetti Muda, A., Raponi, M., Quintarelli, C., Quinti, I., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Carsetti, R., Zaffina, S., Piano Mortari, E., Terreri, S., Corrente, F., Capponi, C., Palomba, P., Mirabella, M., Cascioli, S., Palange, P., Cuccaro, I., Milito, C., Zumla, A., Maeurer, M., Camisa, V., Vinci, M. R., Santoro, A., Cimini, E., Marchioni, L., Nicastri, E., Palmieri, F., Agrati, C., Ippolito, G., Porzio, O., Concato, C., Onetti Muda, A., Raponi, M., Quintarelli, C., Quinti, I., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

SARS-CoV-2 is a novel coronavirus, not encountered before by humans. The wide spectrum of clinical expression of SARS-CoV-2 illness suggests that individual immune responses to SARS-CoV-2 play a crucial role in determining the clinical course after first infection. Immunological studies have focused on patients with moderate to severe disease, demonstrating excessive inflammation in tissues and organ damage. In order to understand the basis of the protective immune response in COVID-19, we performed a longitudinal follow-up, flow-cytometric and serological analysis of innate and adaptive immunity in 64 adults with a spectrum of clinical presentations: 28 healthy SARS-CoV-2-negative contacts of COVID-19 cases; 20 asymptomatic SARS-CoV-2-infected cases; eight patients with Mild COVID-19 disease and eight cases of Severe COVID-19 disease. Our data show that high frequency of NK cells and early and transient increase of specific IgA, IgM and, to a lower extent, IgG are associated with asymptomatic SARS-CoV-2 infection. By contrast, monocyte expansion and high and persistent levels of IgA and IgG, produced relatively late in the course of the infection, characterize severe disease. Modest increase of monocytes and different kinetics of antibodies are detected in mild COVID-19. The importance of innate NK cells and the short-lived antibody response of asymptomatic individuals and patients with mild disease suggest that only severe COVID-19 may result in protective memory established by the adaptive immune response.

Published
2020

33. A clinical, histopathological and laboratory study of 19 consecutive Italian paediatric patients with chilblain‐like lesions: lights and shadows on the relationship with COVID‐19 infection

Author

El Hachem, M., primary, Diociaiuti, A., additional, Concato, C., additional, Carsetti, R., additional, Carnevale, C., additional, Ciofi Degli Atti, M., additional, Giovannelli, L., additional, Latella, E., additional, Porzio, O., additional, Rossi, S., additional, Stracuzzi, A., additional, Zaffina, S., additional, Onetti Muda, A., additional, Zambruno, G., additional, and Alaggio, R., additional

Published
2020
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35. A novel disorder involving dyshematopoiesis, inflammation, and HLH due to aberrant CDC42 function

Author

Lam, M. T., Coppola, S., Krumbach, O. H. F., Prencipe, G., Insalaco, A., Cifaldi, C., Brigida, I., Zara, E., Scala, S., Di Cesare, S., Martinelli, S., Di Rocco, M., Pascarella, A., Niceta, M., Pantaleoni, F., Ciolfi, A., Netter, P., Carisey, A. F., Diehl, M., Akbarzadeh, M., Cont, F., Merli, P., Pastore, A., Mortera, S. L., Camerini, S., Farina, L., Buchholzer, M., Pannone, L., Cao, T. N., Coban-Akdemir, Z. H., Jhangiani, S. N., Muzny, D. M., Gibbs, R. A., Basso-Ricci, L., Chiriaco, M., Dvorsky, R., Putignani, L., Carsetti, R., Janning, P., Stray-Pedersen, A., Erichsen, H. C., Horne, A. C., Bryceson, Y. T., Torralba-Raga, L., Ramme, K., Rosti, V., Bracaglia, C., Messia, V., Palma, P., Finocchi, A., Locatelli, Franco, Chinn, I. K., Lupski, J. R., Mace, E. M., Cancrini, C., Aiuti, A., Ahmadian, M. R., Orange, J. S., De Benedetti, F., Tartaglia, M., Locatelli F. (ORCID:0000-0002-7976-3654), Lam, M. T., Coppola, S., Krumbach, O. H. F., Prencipe, G., Insalaco, A., Cifaldi, C., Brigida, I., Zara, E., Scala, S., Di Cesare, S., Martinelli, S., Di Rocco, M., Pascarella, A., Niceta, M., Pantaleoni, F., Ciolfi, A., Netter, P., Carisey, A. F., Diehl, M., Akbarzadeh, M., Cont, F., Merli, P., Pastore, A., Mortera, S. L., Camerini, S., Farina, L., Buchholzer, M., Pannone, L., Cao, T. N., Coban-Akdemir, Z. H., Jhangiani, S. N., Muzny, D. M., Gibbs, R. A., Basso-Ricci, L., Chiriaco, M., Dvorsky, R., Putignani, L., Carsetti, R., Janning, P., Stray-Pedersen, A., Erichsen, H. C., Horne, A. C., Bryceson, Y. T., Torralba-Raga, L., Ramme, K., Rosti, V., Bracaglia, C., Messia, V., Palma, P., Finocchi, A., Locatelli, Franco, Chinn, I. K., Lupski, J. R., Mace, E. M., Cancrini, C., Aiuti, A., Ahmadian, M. R., Orange, J. S., De Benedetti, F., Tartaglia, M., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Hemophagocytic lymphohistiocytosis (HLH) is characterized by immune dysregulation due to inadequate restraint of overactivated immune cells and is associated with a variable clinical spectrum having overlap with more common pathophysiologies. HLH is difficult to diagnose and can be part of inflammatory syndromes. Here, we identify a novel hematological/autoinflammatory condition (NOCARH syndrome) in four unrelated patients with superimposable features, including neonatal-onset cytopenia with dyshematopoiesis, autoinflammation, rash, and HLH. Patients shared the same de novo CDC42 mutation (Chr1:22417990C>T, p.R186C) and altered hematopoietic compartment, immune dysregulation, and inflammation. CDC42 mutations had been associated with syndromic neurodevelopmental disorders. In vitro and in vivo assays documented unique effects of p.R186C on CDC42 localization and function, correlating with the distinctiveness of the trait. Emapalumab was critical to the survival of one patient, who underwent successful bone marrow transplantation. Early recognition of the disorder and establishment of treatment followed by bone marrow transplant are important to survival.

Published
2019

36. Metaproteomic investigation to assess gut microbiota shaping in newborn mice: A combined taxonomic, functional and quantitative approach

Author

Mortera, Sl, Soggiu, A, Vernocchi, P, Del Chierico, F, Piras, C, Carsetti, R, Marzano, V, Britti, D, Urbani, Andrea, Roncada, P, Putignani, Lorenza, Urbani, A (ORCID:0000-0001-9168-3174), Putignani, L, Mortera, Sl, Soggiu, A, Vernocchi, P, Del Chierico, F, Piras, C, Carsetti, R, Marzano, V, Britti, D, Urbani, Andrea, Roncada, P, Putignani, Lorenza, Urbani, A (ORCID:0000-0001-9168-3174), and Putignani, L

Abstract

Breastfeeding is nowadays known to be one of the most critical factors contributing to the development of an efficient immune system. In the last decade, a consistent number of pieces of evidence demonstrated the relationship between a healthy organism and its gut microbiota. However, this link is still not fully understood and requires further investigation. We recently adopted a murine model to describe the impact of either maternal milk or parental genetic background, on the composition of the gut microbial population in the first weeks of life. A metaproteomic approach to such complex environments is a big challenge that requires a strong effort in both data production and analysis, including the set-up of dedicated multitasking bioinformatics pipelines. Herein we present an LC-MS/MS based investigation to monitor mouse gut microbiota in the early life, aiming at characterizing its functions and metabolic activities together with a taxonomic description in terms of operational taxonomic units. We provided a quantitative evaluation of bacterial metaproteins, taking into account differential expression results in relation to the functional and taxonomic classification, particularly with proteins from orthologues groups. This allowed the reduction of the bias arising from the presence of a high number of shared peptides, and proteins, among different bacterial species. We also focused on host mucosal proteome and its modulation, according to different microbiota composition.

Published
2019

39. The Vici syndrome protein EPG5 regulates intracellular nucleic acid trafficking linking autophagy to innate and adaptive immunity

Author

Piano Mortari, E., Folgiero, V., Marcellini, V., Romania, P., Bellacchio, E., D'Alicandro, V., Bocci, C., Carrozzo, R., Martinelli, D., Petrini, S., Axiotis, E., Farroni, C., Locatelli, Franco, Schara, U., Pilz, D. T., Jungbluth, H., Dionisi-Vici, C., Carsetti, R., Locatelli F. (ORCID:0000-0002-7976-3654), Piano Mortari, E., Folgiero, V., Marcellini, V., Romania, P., Bellacchio, E., D'Alicandro, V., Bocci, C., Carrozzo, R., Martinelli, D., Petrini, S., Axiotis, E., Farroni, C., Locatelli, Franco, Schara, U., Pilz, D. T., Jungbluth, H., Dionisi-Vici, C., Carsetti, R., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Vici syndrome is a human inherited multi-system disorder caused by recessive mutations in EPG5, encoding the EPG5 protein that mediates the fusion of autophagosomes with lysosomes. Immunodeficiency characterized by lack of memory B cells and increased susceptibility to infection is an integral part of the condition, but the role of EPG5 in the immune system remains unknown. Here we show that EPG5 is indispensable for the transport of the TLR9 ligand CpG to the late endosomal-lysosomal compartment, and for TLR9-initiated signaling, a step essential for the survival of human memory B cells and their ultimate differentiation into plasma cells. Moreover, the predicted structure of EPG5 includes a membrane remodeling domain and a karyopherin-like domain, thus explaining its function as a carrier between separate vesicular compartments. Our findings indicate that EPG5, by controlling nucleic acids intracellular trafficking, links macroautophagy/autophagy to innate and adaptive immunity.

Published
2018

40. Are SARS‐CoV‐2 IgA antibodies in paediatric patients with chilblain‐like lesions indicative of COVID‐19 asymptomatic or paucisymptomatic infection?

Author

Diociaiuti, A., Giancristoforo, S., Terreri, S., Corbeddu, M., Concato, C., Ciofi Degli Atti, M., Zambruno, G., Carsetti, R., and El Hachem, M.

Subjects
CHILD patients, COVID-19, SARS-CoV-2, IMMUNOGLOBULIN A, IMMUNOGLOBULINS
Abstract

Are SARS-CoV-2 IgA antibodies in paediatric patients with chilblain-like lesions indicative of COVID-19 asymptomatic or paucisymptomatic infection? Dear Editor, Acral chilblain-like lesions in young patients are one of the commonest skin manifestations reported during COVID-19 pandemic.1-3 Despite the temporal and spatial correlation between the outbreak of pernio-like and the pandemic, the relationship with COVID-19 remains uncertain. Three patients of group B reported flu-like symptoms 3-4 weeks before skin lesion onset, and a single patient developed chilblain after proving positive to SARS-CoV-2. [Extracted from the article]

Published
2021
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41. Infants hospitalized for Bordetella pertussis infection commonly have respiratory viral coinfections

Author

Frassanito, Antonella, Nenna, Raffaella, Nicolai, Ambra, Pierangeli, Alessandra, Tozzi, A. E., Stefanelli, P., Carsetti, R., Concato, C., Schiavoni, I., Midulla, Fabio, DI MATTIA, Greta, Pandolfi, Elisabetta, Gesualdo, Francesco, Agricola, Eleonora, Russo, Luisa, Ferretti, Beatrice, Campagna, Ilaria, Villani, Alberto, Gonfiantini, Michaela Veronika, Marcellini, Valentina, Vennarucci, Valentina Spuri, Buttinelli, Gabriele, and Fedele, Giorgio

Subjects
Male, 0301 basic medicine, Bordetella pertussis, Pediatrics, Rhinovirus, Whooping Cough, child, pertussis, respiratory virus, severity, infectious diseases, Respiratory virus, medicine.disease_cause, Severity of Illness Index, 0302 clinical medicine, Medical microbiology, 030212 general & internal medicine, Respiratory system, Child, Respiratory Tract Infections, biology, Settore MED/38, Parainfluenza Virus 2, Human, Hospitalization, Infectious Diseases, Child, Preschool, Coinfection, RNA, Viral, Female, Nasal Cavity, Research Article, medicine.medical_specialty, 030106 microbiology, Real-Time Polymerase Chain Reaction, Severity, Virus, lcsh:Infectious and parasitic diseases, 03 medical and health sciences, Pertussis, medicine, Humans, lcsh:RC109-216, Retrospective Studies, business.industry, Infant, biology.organism_classification, medicine.disease, Parainfluenza Virus 1, Human, Coronavirus, Respiratory Syncytial Virus, Human, Immunology, Tropical medicine, business
Abstract

Background Whether viral coinfections cause more severe disease than Bordetella pertussis (B. pertussis) alone remains unclear. We compared clinical disease severity and sought clinical and demographic differences between infants with B. pertussis infection alone and those with respiratory viral coinfections. We also analyzed how respiratory infections were distributed during the 2 years study. Methods We enrolled 53 infants with pertussis younger than 180 days (median age 58 days, range 17–109 days, 64.1% boys), hospitalized in the Pediatric Departments at “Sapienza” University Rome and Bambino Gesù Children’s Hospital from August 2012 to November 2014. We tested in naso-pharyngeal washings B. pertussis and 14 respiratory viruses with real-time reverse-transcriptase-polymerase chain reaction. Clinical data were obtained from hospital records and demographic characteristics collected using a structured questionnaire. Results 28/53 infants had B. pertussis alone and 25 viral coinfection: 10 human rhinovirus (9 alone and 1 in coinfection with parainfluenza virus), 3 human coronavirus, 2 respiratory syncytial virus. No differences were observed in clinical disease severity between infants with B. pertussis infection alone and those with coinfections. Infants with B. pertussis alone were younger than infants with coinfections, and less often breastfeed at admission. Conclusions In this descriptive study, no associations between clinical severity and pertussis with or without co-infections were found. Trial registration Policlinico Umberto I: protocol 213/14, 3085/13.02.2014, retrospectively registered. Bambino Gesù Children’s Hospital: protocol n. RF-2010-2317709.

Published
2017
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42. Does Breastfeeding Protect Young Infants From Pertussis? Case-control Study and Immunologic Evaluation

Author

Pandolfi, E, Gesualdo, F, Carloni, E, Villani, A, Midulla, Fabio, Carsetti, R, Stefanelli, P, Fedele, G, Tozzi, Ae, and Pertussis Study Group

Subjects
Microbiology (medical), Male, Bordetella pertussis, medicine.medical_specialty, Pediatrics, Whooping Cough, breastfeeding, Breastfeeding, Breast milk, Pertussis toxin, immunology, 03 medical and health sciences, 0302 clinical medicine, prevention, Nasopharyngeal aspirate, 030225 pediatrics, Internal medicine, medicine, Humans, 030212 general & internal medicine, biology, Milk, Human, business.industry, pertussis, Case-control study, Infant, Newborn, Infant, Odds ratio, biology.organism_classification, Antibodies, Bacterial, Settore MED/38, Immunoglobulin A, Infectious Diseases, Breast Feeding, Italy, Case-Control Studies, Immunoglobulin G, Pediatrics, Perinatology and Child Health, biology.protein, Female, Antibody, business
Abstract

BACKGROUND Pertussis infection can be severe in unvaccinated infants. A case-control study was conducted to investigate the potential role of breastfeeding in protecting young, unvaccinated infants from pertussis. METHODS Hospitalized infants

Published
2017

43. Parents as source of pertussis transmission in hospitalized young infants

Author

Fedele, G., Carollo, M., Palazzo, R., Stefanelli, P., Pandolfi, E., Gesualdo, F., Tozzi, A. E., Carsetti, R., Villani, A., Nicolai, A., Midulla, F., Ausiello, C. M., The Pertussis Study Group, Leone, P., Schiavoni, I., Buttinelli, G., Gonfiantini, M. V., Agricola, E., Russo, L., Ferretti, B., Campagna, I., Marcellini, V., Concato, C., Frassanito, A., Nenna, R., Di Mattia, G., and Rizzo, C

Subjects
0301 basic medicine, Microbiology (medical), Male, Parents, medicine.medical_specialty, Pediatrics, Whooping Cough, 030106 microbiology, Prevalence, serology, infant, pertussis, source of infection, law.invention, Young infants, 03 medical and health sciences, law, Seroepidemiologic Studies, Epidemiology, medicine, Humans, Family Health, business.industry, Infant, Newborn, General Medicine, Antibodies, Bacterial, Settore MED/38, Infectious Disease Transmission, Vertical, Infectious Diseases, Transmission (mechanics), Case-Control Studies, Immunoglobulin G, Female, Antitoxins, business, Disease transmission
Abstract

This study was planned to collect evidences of familial pertussis transmission to infants younger than 6 months of age. Understanding the dynamics of transmission of pertussis in families is essential to plan effective prevention strategies that could be integrated in pertussis control.The seroprevalence of IgG antibodies to pertussis toxin (PT-IgG) and prolonged cough symptoms were evaluated in parents of 55 infants aged6 months hospitalized for confirmed pertussis. Parents of 33 infants with lower respiratory tract infection (LRTI) and parents of 57 healthy infants admitted as outpatients for hip ultrasound examination (HE) were enrolled as controls.Parents of pertussis cases had PT-IgG levels significantly higher as compared to LRTI and HE parents. More than 40 % were compatible as transmitters of pertussis to their babies, since they had a level of PT-IgG ≥ 100 IU/ml, which is considered diagnostic for a recent pertussis episode. Based on serology, the percentage of pertussis cases that had at least one parent as source of infection was 49.1 %. When cough symptoms were taken into account, the percentage of parents putative transmitters of the infection to their infants increased to 56.4 %.Parents are scarcely aware of the household transmission of pertussis to their newborns. Our study highlights the need to advise parents about the likelihood of transmission to the newborn and to be particularly aware of coughing symptoms in the household. Since infection can be asymptomatic, a serological survey of family members should also be considered.

Published
2017

44. The Vici syndrome protein EPG5 regulates intracellular nucleic acid trafficking linking autophagy to innate and adaptive immunity

Author

Piano Mortari, E., primary, Folgiero, V., additional, Marcellini, V., additional, Romania, P., additional, Bellacchio, E., additional, D'Alicandro, V., additional, Bocci, C., additional, Carrozzo, R., additional, Martinelli, D., additional, Petrini, S., additional, Axiotis, E., additional, Farroni, C., additional, Locatelli, F., additional, Schara, U., additional, Pilz, D.T., additional, Jungbluth, H., additional, Dionisi-Vici, C., additional, and Carsetti, R., additional

Published
2018
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47. TLR9 signaling in patients with ectodermal dysplasia and immunodeficiency associated with Nuclear Factor Essential Modulator (NEMO) mutations

Author

GIARDINO, GIULIANA, NADDEI, ROBERTA, CIRILLO, EMILIA, GALLO, VERA, PIGNATA, CLAUDIO, Esposito T., Fusco F., Quinti I., Ursini M. V., Carsetti R., Giardino, Giuliana, Naddei, Roberta, Cirillo, Emilia, Gallo, Vera, Esposito, T., Fusco, F., Quinti, I., Ursini, M. V., Carsetti, R., and Pignata, Claudio

Abstract

Background: Hypohidrotic ectodermal dysplasia (HED) is a group of disorders of ectodermal tissues, resulting from mutations in the ectodysplasin-A (EDA) pathway. Hypomorphic mutations in the NF-?B essential modulator (NEMO) result in HED with immunodeficiency (HED-ID, OMIM 300291), characterized by susceptibility to encapsulated bacteria, mycobacteria, and herpes virus infections. Objective: To analyze B-cell compartment and TLR9 signaling in HED-ID patients. Methods: Two HED-ID patients and a patient with HED caused by EDA gene mutation (XLHED) to confirm the implication of NFkB in this pathway were studied. Results: In HED-ID, differently from XLHED, only few B cells acquired the phenotype of IgM memory and differentiated into plasma cells upon TLR9 stimulation. Memory B cells did not produce IgG and IgA, and only small amounts of IgM in vitro. Conclusion: In HED-ID patients, TLR9 signaling is abnormal, in keeping with the lack of IgM memory B cells and natural antibodies. In individuals at a high risk of developing pneumococcal diseases, increased susceptibility to Streptococcus pneumonia infections and poor response to polysaccharide antigens have been associated with the lack of IgM memory B cells, required for the T-independent response toward encapsulated bacteria, whose differentiation from transitional B cells is under TLR9 control. This finding helps explain the susceptibility to infections by encapsulated bacteria.

Published
2014

48. Humoral alteration in 22q11.2 deletion syndrome patients

Author

Cancrini, C., Di Cesare, S., Puliafito, P., Montin, D., Rondelli, R., Soresina, A., Pignata, C., Pietrogrande, M., Carsetti, R., PAOLO ROSSI, Cancrini, C., Di Cesare, S., Puliafito, P., Montin, D., Rondelli, R., Soresina, A., Pignata, Claudio, Pietrogrande, M., Carsetti, R., and Rossi, P.

Abstract

Objective: To investigate humoral compartment at diagnosis and during follow-up in patients with 22q11.2 Deletion Syndrome (22q11DS). Methods: A retrospective and prospective multicenter study was conducted with 165 patients in the context of the Italian Network for Primary Immunodeficiencies. Patients were investigated for serum immunoglobulin, testing specific antibody titers to recall antigens and proliferative responses to phytohemagglutinin (PHA) and OKT3. Lymphocyte subsets were assessed by flow cytometric analysis. Results: The cohort consisted of 96 males and 69 females; median age at diagnosis was 4 months (range 0 to 35 years). Eighty out of 165 patients had a history of recurrent and/or severe infections and 41% patients received at least one prophylactic treatment. During follow-up the frequency of autoimmune manifestations increased, severe infections and antibiotic prophylaxis decreased. We reported hypogammaglobulinemia in 34% of patients at diagnosis, confirmed during follow-up. Total lymphocytes and T-cells subsets were decreased in most of 22q11DS patients, although these immunological abnormalities did not correlate to risk of infections. Lymphocyte proliferation in response to mitogens and antigens was normal/ in the lower levels of normality, in most of patients. Our preliminary data showed a decrease of B cell memory. Conclusions: Not only T-cell but also B- cell compartment should be routinely investigated in 22q11DS patients with an history of recurrent infections and autoimmune manifestations. These data could help to better define, in these patients, follow-up and clinical management with a specific antimicrobial treatment and/or intravenous immunoglobulin therapy.

Published
2014

49. Chronic mucocutaneous candidiasis, recurrent herpetic infections and suppurative eyelid infections in a patient carrying a novel gain-of-function mutation in the STAT1 DNA-binding domain

Author

GIARDINO, GIULIANA, CIRILLO, EMILIA, GALLO, VERA, D'ASSANTE, ROBERTA, RUGGIERO, GIUSEPPINA, PIGNATA, CLAUDIO, Paciolla M., Ursini M. V., Carsetti R., Puel A., Giardino, Giuliana, Cirillo, Emilia, Gallo, Vera, D'Assante, Roberta, Paciolla, M., Ruggiero, Giuseppina, Ursini, M. V., Carsetti, R., Puel, A., and Pignata, Claudio

Abstract

Chronic mucocutaneous candidiasis (CMCC) is characterized by noninvasive persistent Candida infections. Gain-of-function mutations in signal transducer and activator of transcription 1 (STAT1) cause impaired STAT1 dephosphorylation, diminished IL-17-producing T-cells, and CMCC. We report on a 17-year-old boy with CMCC. At 7 years of age he developed mucocutaneous candidiasis. At 8 years he suffered from severe varicella infection and since 11 he experienced recurrent herpetic infections involving genitals and limbs, recurrent abscesses and suppurative eyelid infections. Familial history was negative. The physical examination revealed oral thrush, onichomycosis, suppurative eyelid infection (figure), furunculosis and parodontitis. Azole-sensitive Candida Albicans grew from oral lesions, nails and esophageal mucosa cultures. Prophylactic treatment with fluconazole resulted in a decrease of frequency and severity of fungal infections. Laboratory evaluation revealed normal white blood cell, T- and B-lymphocyte counts, T-lymphocyte proliferation, Ig and IgG subclasses serum levels and responses to vaccines. HIV serology was negative and IgE levels were persistently elevated (684 KU/L). Transitional (8.2%), mature (79.8%) and memory (12%) B cell levels were normal. Memory B cells mostly included IgM and only few switched cells (88 and 12%, respectively). CD4 and CD8 naïve and memory T cells were normal. IL-17-producing T-cell numbers were 0%. Toll like receptor stimulation resulted in high levels of IL-10, IL1 beta, TNF alpha, IFN-gamma, IL-6 and IL-8. Full-length sequencing of STAT1 genomic DNA identified a T387A heterozygous mutations in the DNA-binding domain, not identified in the unaffected parents. This mutation has not been previously reported.

Published
2014

50. Identification of Endothelin-1 and NR4A2 as CD133-regulated genes in colon cancer cells

Author

Puglisi, Maria Ausiliatrice, Barba, Maria Cristina, Corbi, Maddalena, Errico, Mf, Giorda, E, Saulnier, Nathalie, Boninsegna Lucarelli, Alma, Piscaglia, Ac, Carsetti, R, Cittadini, Achille Renato Maria, Gasbarrini, Antonio, Sgambato, Alessandro, and Barba, Marta

Subjects
Nuclear Receptor Subfamily 4, Member 2, Blotting, Western, Cell Separation, Biology, Immunophenotyping, Pathology and Forensic Medicine, Side population, Antigen, Settore MED/04 - PATOLOGIA GENERALE, Antigens, CD, Cancer stem cell, Nuclear Receptor Subfamily 4, Group A, Member 2, Gene expression, Humans, AC133 Antigen, Antigens, Group A, Glycoproteins, Regulation of gene expression, Neoplastic, Endothelin-1, Blotting, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Flow Cytometry, Molecular biology, CD, Gene Expression Regulation, Neoplastic, Gene expression profiling, Gene Expression Regulation, Cell culture, Colonic Neoplasms, embryonic structures, Neoplastic Stem Cells, Caco-2 Cells, Peptides, Western
Abstract

Several in vitro assays have been proposed to identify cancer stem cells (CSCs), including immunophenotyping, sphere assay and side population (SP) assay. CD133 antigen has been proposed as a CSC marker in colon cancer (CC). However, no functional data are available to date and conflicting results have been reported regarding its role as true CSC marker. Here we set out to identify a molecular signature associated with potential CSC. CD133(+) cells isolated from the CaCo-2 CC cell line were analysed by microarray molecular profiling compared to CD133(-) counterparts. Various differentially expressed genes were identified and the most relevant transcripts found to be over-expressed in CD133(+) cells were evaluated by quantitative RT-PCR in the CD133(+) fractions isolated from several CC cell lines. In the attempt to find a correlation between putative CSCs, isolated by means of CD133 immunophenotyping and the SP approach, we demonstrated a significant enrichment of CD133(+) cells within the SP fraction of CC cells, and comparison of the gene expression profiles revealed that Endothelin-1 (END-1) and nuclear receptor subfamily 4, group A, member 2 (NR4A2) transcripts are highly expressed in both CD133(+) and SP fractions of CC cells. Moreover, depletion of CD133 by siRNA induced a significant attenuation of END-1 and NR4A2 expression levels in CaCo-2 cells, while expression of all three molecules decreased during sodium butyrate-induced differentiation. In conclusion, we have identified a molecular signature associated with potential CSCs and showed for the first time the existence of a functional relationship between CD133, END-1 and NR4A2 expression in colon cancer cells.

Published
2011
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