Your search keyword '"Manghisi, B"' showing total 13 results

1. Idiopathic erythrocytosis: a germline disease?

Author

Elli, E. M., Mauri, M., D’Aliberti, D., Crespiatico, I., Fontana, D., Redaelli, S., Pelucchi, S., Spinelli, S., Manghisi, B., Cavalca, F., Aroldi, A., Ripamonti, A., Ferrari, S., Palamini, S., Mottadelli, F., Massimino, L., Ramazzotti, D., Cazzaniga, G., Piperno, A., Gambacorti-Passerini, C., and Piazza, R.

Published

2024

2. First-hit SETBP1 mutations cause a myeloproliferative disorder with bone marrow fibrosis

Author

Crespiatico, I, Zaghi, M, Mastini, C, D'Aliberti, D, Mauri, M, Mercado, C, Fontana, D, Spinelli, S, Crippa, V, Inzoli, E, Manghisi, B, Civettini, I, Ramazzotti, D, Sangiorgio, V, Gengotti, M, Brambilla, V, Aroldi, A, Banfi, F, Barone, C, Orsenigo, R, Riera, L, Riminucci, M, Corsi, A, Breccia, M, Morotti, A, Cilloni, D, Roccaro, A, Sacco, A, Stagno, F, Serafini, M, Mottadelli, F, Cazzaniga, G, Pagni, F, Chiarle, R, Azzoni, E, Sessa, A, Gambacorti Passerini, C, Elli, E, Mologni, L, Piazza, R, Crespiatico I., Zaghi M., Mastini C., D'Aliberti D., Mauri M., Mercado C. M., Fontana D., Spinelli S., Crippa V., Inzoli E., Manghisi B., Civettini I., Ramazzotti D., Sangiorgio V., Gengotti M., Brambilla V., Aroldi A., Banfi F., Barone C., Orsenigo R., Riera L., Riminucci M., Corsi A., Breccia M., Morotti A., Cilloni D., Roccaro A., Sacco A., Stagno F., Serafini M., Mottadelli F., Cazzaniga G., Pagni F., Chiarle R., Azzoni E., Sessa A., Gambacorti Passerini C., Elli E. M., Mologni L., Piazza R., Crespiatico, I, Zaghi, M, Mastini, C, D'Aliberti, D, Mauri, M, Mercado, C, Fontana, D, Spinelli, S, Crippa, V, Inzoli, E, Manghisi, B, Civettini, I, Ramazzotti, D, Sangiorgio, V, Gengotti, M, Brambilla, V, Aroldi, A, Banfi, F, Barone, C, Orsenigo, R, Riera, L, Riminucci, M, Corsi, A, Breccia, M, Morotti, A, Cilloni, D, Roccaro, A, Sacco, A, Stagno, F, Serafini, M, Mottadelli, F, Cazzaniga, G, Pagni, F, Chiarle, R, Azzoni, E, Sessa, A, Gambacorti Passerini, C, Elli, E, Mologni, L, Piazza, R, Crespiatico I., Zaghi M., Mastini C., D'Aliberti D., Mauri M., Mercado C. M., Fontana D., Spinelli S., Crippa V., Inzoli E., Manghisi B., Civettini I., Ramazzotti D., Sangiorgio V., Gengotti M., Brambilla V., Aroldi A., Banfi F., Barone C., Orsenigo R., Riera L., Riminucci M., Corsi A., Breccia M., Morotti A., Cilloni D., Roccaro A., Sacco A., Stagno F., Serafini M., Mottadelli F., Cazzaniga G., Pagni F., Chiarle R., Azzoni E., Sessa A., Gambacorti Passerini C., Elli E. M., Mologni L., and Piazza R.

Abstract

SETBP1 mutations are found in various clonal myeloid disorders. However, it is unclear whether they can initiate leukemia, because SETBP1 mutations typically appear as later events during oncogenesis. To answer this question, we generated a mouse model expressing mutated SETBP1 in hematopoietic tissue: this model showed profound alterations in the differentiation program of hematopoietic progenitors and developed a myeloid neoplasm with megakaryocytic dysplasia, splenomegaly, and bone marrow fibrosis, prompting us to investigate SETBP1 mutations in a cohort of 36 triple-negative primary myelofibrosis (TN-PMF) cases. We identified 2 distinct subgroups, one carrying SETBP1 mutations and the other completely devoid of somatic variants. Clinically, a striking difference in disease aggressiveness was noted, with patients with SETBP1 mutation showing a much worse clinical course. In contrast to myelodysplastic/myeloproliferative neoplasms, in which SETBP1 mutations are mostly found as a late clonal event, single-cell clonal hierarchy reconstruction in 3 patients with TN-PMF from our cohort revealed SETBP1 to be a very early event, suggesting that the phenotype of the different SETBP1+ disorders may be shaped by the opposite hierarchy of the same clonal SETBP1 variants.

Published

2024

3. Idiopathic erythrocytosis: a germline disease?

Author

Elli, E, Mauri, M, D’Aliberti, D, Crespiatico, I, Fontana, D, Redaelli, S, Pelucchi, S, Spinelli, S, Manghisi, B, Cavalca, F, Aroldi, A, Ripamonti, A, Ferrari, S, Palamini, S, Mottadelli, F, Massimino, L, Ramazzotti, D, Cazzaniga, G, Piperno, A, Gambacorti-Passerini, C, Piazza, R, Elli, E. M., Mauri, M., D’Aliberti, D., Crespiatico, I., Fontana, D., Redaelli, S., Pelucchi, S., Spinelli, S., Manghisi, B., Cavalca, F., Aroldi, A., Ripamonti, A., Ferrari, S., Palamini, S., Mottadelli, F., Massimino, L., Ramazzotti, D., Cazzaniga, G., Piperno, A., Gambacorti-Passerini, C., Piazza, R., Elli, E, Mauri, M, D’Aliberti, D, Crespiatico, I, Fontana, D, Redaelli, S, Pelucchi, S, Spinelli, S, Manghisi, B, Cavalca, F, Aroldi, A, Ripamonti, A, Ferrari, S, Palamini, S, Mottadelli, F, Massimino, L, Ramazzotti, D, Cazzaniga, G, Piperno, A, Gambacorti-Passerini, C, Piazza, R, Elli, E. M., Mauri, M., D’Aliberti, D., Crespiatico, I., Fontana, D., Redaelli, S., Pelucchi, S., Spinelli, S., Manghisi, B., Cavalca, F., Aroldi, A., Ripamonti, A., Ferrari, S., Palamini, S., Mottadelli, F., Massimino, L., Ramazzotti, D., Cazzaniga, G., Piperno, A., Gambacorti-Passerini, C., and Piazza, R.

Abstract

Polycythemia Vera (PV) is typically caused by V617F or exon 12 JAK2 mutations. Little is known about Polycythemia cases where no JAK2 variants can be detected, and no other causes identified. This condition is defined as idiopathic erythrocytosis (IE). We evaluated clinical-laboratory parameters of a cohort of 56 IE patients and we determined their molecular profile at diagnosis with paired blood/buccal-DNA exome-sequencing coupled with a high-depth targeted OncoPanel to identify a possible underling germline or somatic cause. We demonstrated that most of our cohort (40/56: 71.4%) showed no evidence of clonal hematopoiesis, suggesting that IE is, in large part, a germline disorder. We identified 20 low mutation burden somatic variants (Variant allelic fraction, VAF, < 10%) in only 14 (25%) patients, principally involving DNMT3A and TET2. Only 2 patients presented high mutation burden somatic variants, involving DNMT3A, TET2, ASXL1 and WT1. We identified recurrent germline variants in 42 (75%) patients occurring mainly in JAK/STAT, Hypoxia and Iron metabolism pathways, among them: JAK3-V722I and HIF1A-P582S; a high fraction of patients (48.2%) resulted also mutated in homeostatic iron regulatory gene HFE-H63D or C282Y. By generating cellular models, we showed that JAK3-V722I causes activation of the JAK-STAT5 axis and upregulation of EPAS1/HIF2A, while HIF1A-P582S causes suppression of hepcidin mRNA synthesis, suggesting a major role for these variants in the onset of IE.

Published

2024

4. Communicating the diagnosis of a hematological neoplastic disease to patients’ minor children: a multicenter prospective study

Author

Manghisi, B, Borin, L, Monaco, M, Sacco, G, Antolini, L, Mantegazza, R, Barichello, M, Mazza, U, Zappasodi, P, Onida, F, Arcaini, L, Cairoli, R, Gambacorti Passerini, C, Manghisi, Beatrice, Borin, Lorenza, Monaco, Maria Rosaria, Sacco, Gaia Giulia Angela, Antolini, Laura, Mantegazza, Raffaele, Barichello, Monica, Mazza, Umberto, Zappasodi, Patrizia, Onida, Francesco, Arcaini, Luca, Cairoli, Roberto, Gambacorti Passerini, Carlo, Manghisi, B, Borin, L, Monaco, M, Sacco, G, Antolini, L, Mantegazza, R, Barichello, M, Mazza, U, Zappasodi, P, Onida, F, Arcaini, L, Cairoli, R, Gambacorti Passerini, C, Manghisi, Beatrice, Borin, Lorenza, Monaco, Maria Rosaria, Sacco, Gaia Giulia Angela, Antolini, Laura, Mantegazza, Raffaele, Barichello, Monica, Mazza, Umberto, Zappasodi, Patrizia, Onida, Francesco, Arcaini, Luca, Cairoli, Roberto, and Gambacorti Passerini, Carlo

Abstract

Background When a hematological malignancy is diagnosed, the whole family carries the burden of the disease; parents often try to protect minor children from suffering by avoiding communication about their disease. Since 2009, patients with minors at the Adult Hematology Division at San Gerardo Hospital (Monza) can take part in the "Emanuela Project": children can visit parents and talk with psychologists and hematologists, who explain the disease through simple metaphors.Materials and Methods The EMY STUDY aimed to evaluate the impact of illness-related communication on children's behavior, comparing Monza's experience with other Hematology Units, where the communication is delegated to parents or psychological support. Questionnaires exploring the children's main behaviors (school performance, appetite, sleeping patterns, attachment to family figures, and family dialogue) were administered to both sick (SP) and healthy (HP) parents. From 2017 to 2021, 32 patients were enrolled, 20 from Monza and 12 from other hospitals; 84 questionnaires were globally collected.Results In Monza's group, no major changes in children's behavior were observed and an open dialogue about the disease was often possible. Disease communication is considered crucial and perceived as a responsibility of parents together with a professional figure, mainly the hematologist. Patients were satisfied with "Emanuela Project," reporting positive effects on doctor-patient relationship. Difficulties in separation were significantly higher at other hospitals (P = .019) than in Monza. While at other centers communication is considered parents' responsibility, Monza's patients emphasize the role of professional figures (P = .007). Differently from other hospitals, the role of the hematologist is crucial to Monza's patients (P = .001).Conclusion Disease communication to patients' offspring is a crucial moment in the process of care, and the hematologist can play a major role in this difficult task, with

Published

2024

5. DNA Damage Response (DDR) Is Associated With Treatment-free Remission in Chronic Myeloid Leukemia Patients

Author

Malighetti, F, Arosio, G, Manfroni, C, Mauri, M, Villa, M, Manghisi, B, Inzoli, E, Rindone, G, Zambrotta, G, Civettini, I, Guglielmana, V, Ramazzotti, D, Giudici, G, Bombelli, S, Perego, R, Piazza, R, Mologni, L, Gambacorti-Passerini, C, Malighetti, Federica, Arosio, Giulia, Manfroni, Chiara, Mauri, Mario, Villa, Matteo, Manghisi, Beatrice, Inzoli, Elena, Rindone, Giovanni, Zambrotta, Giovanni P M, Civettini, Ivan, Guglielmana, Veronica, Ramazzotti, Daniele, Giudici, Giovanni, Bombelli, Silvia, Perego, Roberto, Piazza, Rocco, Mologni, Luca, Gambacorti-Passerini, Carlo, Malighetti, F, Arosio, G, Manfroni, C, Mauri, M, Villa, M, Manghisi, B, Inzoli, E, Rindone, G, Zambrotta, G, Civettini, I, Guglielmana, V, Ramazzotti, D, Giudici, G, Bombelli, S, Perego, R, Piazza, R, Mologni, L, Gambacorti-Passerini, C, Malighetti, Federica, Arosio, Giulia, Manfroni, Chiara, Mauri, Mario, Villa, Matteo, Manghisi, Beatrice, Inzoli, Elena, Rindone, Giovanni, Zambrotta, Giovanni P M, Civettini, Ivan, Guglielmana, Veronica, Ramazzotti, Daniele, Giudici, Giovanni, Bombelli, Silvia, Perego, Roberto, Piazza, Rocco, Mologni, Luca, and Gambacorti-Passerini, Carlo

Published

2023

6. Clinical and Molecular features of the patients with Idiopathic Erythrocytosis

Author

Elli, E, Mauri, M, D’Aliberti, D, Crespiatico, I, Fontana, D, Redaelli, S, Pelucchi, S, Manghisi, B, Cavalca, F, Ripamonti, A, Brioschi, F, Palamini, S, Mottadelli, F, Ramazzotti, D, Piperno, A, Gambacorti Passerini, C, Piazza, R, Elli, E, Mauri, M, D’Aliberti, D, Crespiatico, I, Fontana, D, Redaelli, S, Pelucchi, S, Manghisi, B, Cavalca, F, Ripamonti, A, Brioschi, F, Palamini, S, Mottadelli, F, Ramazzotti, D, Piperno, A, Gambacorti Passerini, C, and Piazza, R

Subjects

Idiopathic Erythrocytosis

Published

2022

7. Humoral and cellular immune response in patients with hematological disorders after two doses of BNT162b2 mRNA COVID-19 vaccine: A single-center prospective observational study (NCT05074706)

Author

Bossi, E, Aroldi, A, Borin, L, Verga, L, Fontana, D, Cocito, F, Manghisi, B, Rindone, G, Cavalca, F, Ripamonti, A, Raggi, M, Malandrin, S, Cavallero, A, Antolini, L, Bonardi, D, Piazza, R, Gambacorti-Passerini, C, Bossi, Elisa, Aroldi, Andrea, Borin, Lorenza Maria, Verga, Luisa, Fontana, Diletta, Cocito, Federica, Manghisi, Beatrice, Rindone, Giovanni, Cavalca, Fabrizio, Ripamonti, Alessia, Raggi, Monica, Malandrin, Sergio Maria Ivano, Cavallero, Annalisa, Antolini, Laura, Bonardi, Diego, Piazza, Rocco Giovanni, Gambacorti-Passerini, Carlo, Bossi, E, Aroldi, A, Borin, L, Verga, L, Fontana, D, Cocito, F, Manghisi, B, Rindone, G, Cavalca, F, Ripamonti, A, Raggi, M, Malandrin, S, Cavallero, A, Antolini, L, Bonardi, D, Piazza, R, Gambacorti-Passerini, C, Bossi, Elisa, Aroldi, Andrea, Borin, Lorenza Maria, Verga, Luisa, Fontana, Diletta, Cocito, Federica, Manghisi, Beatrice, Rindone, Giovanni, Cavalca, Fabrizio, Ripamonti, Alessia, Raggi, Monica, Malandrin, Sergio Maria Ivano, Cavallero, Annalisa, Antolini, Laura, Bonardi, Diego, Piazza, Rocco Giovanni, and Gambacorti-Passerini, Carlo

Abstract

Hematological patients at higher risk of severe COVID-19 were excluded from the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) vaccine trials. In this single-center observational prospective study (NCT05074706), we evaluate immune response in the hematological patients followed at the Hematological Division of San Gerardo Hospital, Monza (Italy) deemed to be severely immunosuppressed after vaccination with two doses of the BNT162b2 vaccine. Anti-SARS-CoV-2 immunoglobulin G titers above the cutoff value of 33.8 BAU/ml were detected in 303 (80.2%) out of the 378 patients enrolled. Patients with lymphoproliferative disorders had a significant lower probability of immunization (43.2% vs. 88.4%, p < 0.001). Patients treated with anti-CD20 showed a significantly lower probability of immunization compared to all other treatments (21.4%, p < 0.0001). Among 69 patients who failed seroconversion, 15 patients (22.7%) showed a positive T-cell response. Patients previously treated with anti-CD20 were 2.4 times more likely to test positive for T-cell responses (p = 0.014). Within a follow-up of 9 months from the second COVID-19 vaccination, symptomatic SARS-CoV-2 infections were reported by 20 patients (5.3%) and four of them required hospitalization. Successful serological or T-cell-mediated immunization conferred protection from symptomatic COVID-19. Patients treated with anti-CD20 who were not seroconverted after vaccination might still be protected from COVID-19 due to the T-cell immune response.

Published

2022

8. DNA Damage Response (DDR) Is Associated With Treatment-free Remission in Chronic Myeloid Leukemia Patients

Author

Federica Malighetti, Giulia Arosio, Chiara Manfroni, Mario Mauri, Matteo Villa, Beatrice Manghisi, Elena Inzoli, Giovanni Rindone, Giovanni P. M. Zambrotta, Ivan Civettini, Veronica Guglielmana, Daniele Ramazzotti, Giovanni Giudici, Silvia Bombelli, Roberto Perego, Rocco Piazza, Luca Mologni, Carlo Gambacorti-Passerini, Malighetti, F, Arosio, G, Manfroni, C, Mauri, M, Villa, M, Manghisi, B, Inzoli, E, Rindone, G, Zambrotta, G, Civettini, I, Guglielmana, V, Ramazzotti, D, Giudici, G, Bombelli, S, Perego, R, Piazza, R, Mologni, L, and Gambacorti-Passerini, C

Subjects

Chronic Myeloid Leukemia, Hematology

Published

2023

9. Humoral and cellular immune response in patients with hematological disorders after two doses of BNT162b2 mRNA COVID-19 vaccine: A single-center prospective observational study (NCT05074706)

Author

Elisa Bossi, Andrea Aroldi, Lorenza Maria Borin, Luisa Verga, Diletta Fontana, Federica Cocito, Beatrice Manghisi, Giovanni Rindone, Fabrizio Cavalca, Alessia Ripamonti, Monica Raggi, Sergio Maria Ivano Malandrin, Annalisa Cavallero, Laura Antolini, Diego Bonardi, Rocco Giovanni Piazza, Carlo Gambacorti‐Passerini, Bossi, E, Aroldi, A, Borin, L, Verga, L, Fontana, D, Cocito, F, Manghisi, B, Rindone, G, Cavalca, F, Ripamonti, A, Raggi, M, Malandrin, S, Cavallero, A, Antolini, L, Bonardi, D, Piazza, R, and Gambacorti-Passerini, C

Subjects

mRNA vaccine, COVID‐19, hematological disorder, cellular immune response, seroconversion

Abstract

Hematological patients at higher risk of severe COVID-19 were excluded from the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) vaccine trials. In this single-center observational prospective study (NCT05074706), we evaluate immune response in the hematological patients followed at the Hematological Division of San Gerardo Hospital, Monza (Italy) deemed to be severely immunosuppressed after vaccination with two doses of the BNT162b2 vaccine. Anti-SARS-CoV-2 immunoglobulin G titers above the cutoff value of 33.8 BAU/ml were detected in 303 (80.2%) out of the 378 patients enrolled. Patients with lymphoproliferative disorders had a significant lower probability of immunization (43.2% vs. 88.4%, p < 0.001). Patients treated with anti-CD20 showed a significantly lower probability of immunization compared to all other treatments (21.4%, p < 0.0001). Among 69 patients who failed seroconversion, 15 patients (22.7%) showed a positive T-cell response. Patients previously treated with anti-CD20 were 2.4 times more likely to test positive for T-cell responses (p = 0.014). Within a follow-up of 9 months from the second COVID-19 vaccination, symptomatic SARS-CoV-2 infections were reported by 20 patients (5.3%) and four of them required hospitalization. Successful serological or T-cell-mediated immunization conferred protection from symptomatic COVID-19. Patients treated with anti-CD20 who were not seroconverted after vaccination might still be protected from COVID-19 due to the T-cell immune response.

Published

2022

10. Communicating the diagnosis of a hematological neoplastic disease to patients' minor children: a multicenter prospective study.

Author

Manghisi B, Borin L, Monaco MR, Sacco GGA, Antolini L, Mantegazza R, Barichello M, Mazza U, Zappasodi P, Onida F, Arcaini L, Cairoli R, and Gambacorti Passerini C

Subjects

Humans, Male, Female, Prospective Studies, Child, Adolescent, Surveys and Questionnaires, Communication, Child, Preschool, Adult, Parents psychology, Hematologic Neoplasms psychology

Abstract

Background: When a hematological malignancy is diagnosed, the whole family carries the burden of the disease; parents often try to protect minor children from suffering by avoiding communication about their disease. Since 2009, patients with minors at the Adult Hematology Division at San Gerardo Hospital (Monza) can take part in the "Emanuela Project": children can visit parents and talk with psychologists and hematologists, who explain the disease through simple metaphors., Materials and Methods: The EMY STUDY aimed to evaluate the impact of illness-related communication on children's behavior, comparing Monza's experience with other Hematology Units, where the communication is delegated to parents or psychological support. Questionnaires exploring the children's main behaviors (school performance, appetite, sleeping patterns, attachment to family figures, and family dialogue) were administered to both sick (SP) and healthy (HP) parents. From 2017 to 2021, 32 patients were enrolled, 20 from Monza and 12 from other hospitals; 84 questionnaires were globally collected., Results: In Monza's group, no major changes in children's behavior were observed and an open dialogue about the disease was often possible. Disease communication is considered crucial and perceived as a responsibility of parents together with a professional figure, mainly the hematologist. Patients were satisfied with "Emanuela Project," reporting positive effects on doctor-patient relationship. Difficulties in separation were significantly higher at other hospitals (P = .019) than in Monza. While at other centers communication is considered parents' responsibility, Monza's patients emphasize the role of professional figures (P = .007). Differently from other hospitals, the role of the hematologist is crucial to Monza's patients (P = .001)., Conclusion: Disease communication to patients' offspring is a crucial moment in the process of care, and the hematologist can play a major role in this difficult task, with potential positive effects both on children's well-being and on doctor-patient relationship., (© The Author(s) 2024. Published by Oxford University Press.)

Published

2024

11. First-hit SETBP1 mutations cause a myeloproliferative disorder with bone marrow fibrosis.

Author

Crespiatico I, Zaghi M, Mastini C, D'Aliberti D, Mauri M, Mercado CM, Fontana D, Spinelli S, Crippa V, Inzoli E, Manghisi B, Civettini I, Ramazzotti D, Sangiorgio V, Gengotti M, Brambilla V, Aroldi A, Banfi F, Barone C, Orsenigo R, Riera L, Riminucci M, Corsi A, Breccia M, Morotti A, Cilloni D, Roccaro A, Sacco A, Stagno F, Serafini M, Mottadelli F, Cazzaniga G, Pagni F, Chiarle R, Azzoni E, Sessa A, Gambacorti-Passerini C, Elli EM, Mologni L, and Piazza R

Subjects

Animals, Mice, Humans, Mutation, Carrier Proteins genetics, Nuclear Proteins genetics, Primary Myelofibrosis genetics, Myeloproliferative Disorders genetics, Myelodysplastic-Myeloproliferative Diseases, Hematopoietic System

Abstract

Abstract: SETBP1 mutations are found in various clonal myeloid disorders. However, it is unclear whether they can initiate leukemia, because SETBP1 mutations typically appear as later events during oncogenesis. To answer this question, we generated a mouse model expressing mutated SETBP1 in hematopoietic tissue: this model showed profound alterations in the differentiation program of hematopoietic progenitors and developed a myeloid neoplasm with megakaryocytic dysplasia, splenomegaly, and bone marrow fibrosis, prompting us to investigate SETBP1 mutations in a cohort of 36 triple-negative primary myelofibrosis (TN-PMF) cases. We identified 2 distinct subgroups, one carrying SETBP1 mutations and the other completely devoid of somatic variants. Clinically, a striking difference in disease aggressiveness was noted, with patients with SETBP1 mutation showing a much worse clinical course. In contrast to myelodysplastic/myeloproliferative neoplasms, in which SETBP1 mutations are mostly found as a late clonal event, single-cell clonal hierarchy reconstruction in 3 patients with TN-PMF from our cohort revealed SETBP1 to be a very early event, suggesting that the phenotype of the different SETBP1+ disorders may be shaped by the opposite hierarchy of the same clonal SETBP1 variants., (© 2024 American Society of Hematology. Published by Elsevier Inc. All rights are reserved, including those for text and data mining, AI training, and similar technologies.)

Published

2024

12. DNA Damage Response (DDR) Is Associated With Treatment-free Remission in Chronic Myeloid Leukemia Patients.

Author

Malighetti F, Arosio G, Manfroni C, Mauri M, Villa M, Manghisi B, Inzoli E, Rindone G, Zambrotta GPM, Civettini I, Guglielmana V, Ramazzotti D, Giudici G, Bombelli S, Perego R, Piazza R, Mologni L, and Gambacorti-Passerini C

Published

2023

13. Humoral and cellular immune response in patients with hematological disorders after two doses of BNT162b2 mRNA COVID-19 vaccine: A single-center prospective observational study (NCT05074706).

Author

Bossi E, Aroldi A, Borin LM, Verga L, Fontana D, Cocito F, Manghisi B, Rindone G, Cavalca F, Ripamonti A, Raggi M, Malandrin SMI, Cavallero A, Antolini L, Bonardi D, Piazza RG, and Gambacorti-Passerini C

Abstract

Hematological patients at higher risk of severe COVID-19 were excluded from the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) vaccine trials. In this single-center observational prospective study (NCT05074706), we evaluate immune response in the hematological patients followed at the Hematological Division of San Gerardo Hospital, Monza (Italy) deemed to be severely immunosuppressed after vaccination with two doses of the BNT162b2 vaccine. Anti-SARS-CoV-2 immunoglobulin G titers above the cutoff value of 33.8 BAU/ml were detected in 303 (80.2%) out of the 378 patients enrolled. Patients with lymphoproliferative disorders had a significant lower probability of immunization (43.2% vs. 88.4%, p  < 0.001). Patients treated with anti-CD20 showed a significantly lower probability of immunization compared to all other treatments (21.4%, p  < 0.0001). Among 69 patients who failed seroconversion, 15 patients (22.7%) showed a positive T-cell response. Patients previously treated with anti-CD20 were 2.4 times more likely to test positive for T-cell responses ( p  = 0.014). Within a follow-up of 9 months from the second COVID-19 vaccination, symptomatic SARS-CoV-2 infections were reported by 20 patients (5.3%) and four of them required hospitalization. Successful serological or T-cell-mediated immunization conferred protection from symptomatic COVID-19. Patients treated with anti-CD20 who were not seroconverted after vaccination might still be protected from COVID-19 due to the T-cell immune response., Competing Interests: The authors declare they have no conflicts of interest in relation to the work described., (© 2022 The Authors. eJHaem published by British Society for Haematology and John Wiley & Sons Ltd.)

Published

2022