Your search keyword '"Tatiana Jofra"' showing total 42 results

1. Case Report: Consistent disease manifestations with a staggered time course in two identical twins affected by adenosine deaminase 2 deficiency

Author

Federica Barzaghi, Maria Pia Cicalese, Matteo Zoccolillo, Immacolata Brigida, Matteo Barcella, Ivan Merelli, Claudia Sartirana, Monica Zanussi, Valeria Calbi, Maria Ester Bernardo, Francesca Tucci, Maddalena Migliavacca, Fabio Giglio, Matteo Doglio, Daniele Canarutto, Francesca Ferrua, Giulia Consiglieri, Giulia Prunotto, Francesco Saettini, Sonia Bonanomi, Patrizia Rovere-Querini, Giulia Di Colo, Tatiana Jofra, Georgia Fousteri, Federica Penco, Marco Gattorno, Michael S. Hershfield, Lucia Bongiovanni, Maurilio Ponzoni, Sarah Marktel, Raffaella Milani, Jacopo Peccatori, Fabio Ciceri, Alessandra Mortellaro, and Alessandro Aiuti

Subjects

ADA2, adenosine deaminase 2 deficiency, neutropenia, T large granular lymphocytes, TLGL, HSCT, Immunologic diseases. Allergy, RC581-607

Abstract

Deficiency of adenosine deaminase 2 (DADA2) is an autosomal recessive disease associated with a highly variable clinical presentation, including vasculitis, immunodeficiency, and hematologic manifestations, potentially progressing over time. The present study describes the long-term evolution of the immuno-hematological features and therapeutic challenge of two identical adult twin sisters affected by DADA2. The absence of plasmatic adenosine deaminase 2 (ADA2) activity in both twins suggested the diagnosis of DADA2, then confirmed by genetic analysis. Exon sequencing revealed a missense (p.Leu188Pro) mutation on the paternal ADA2 allele. While, whole genome sequencing identified an unreported deletion (IVS6_IVS7del*) on the maternal allele predicted to produce a transcript missing exon 7. The patients experienced the disease onset during childhood with early strokes (Patient 1 at two years, Patient 2 at eight years of age), subsequently followed by other shared DADA2-associated features, including neutropenia, hypogammaglobulinemia, reduced switched memory B cells, inverted CD4:CD8 ratio, increased naïve T cells, reduced follicular regulatory T cells, the almost complete absence of NK cells, T-large granular cell leukemia, and osteoporosis. Disease evolution differed: clinical manifestations presented several years earlier and were more pronounced in Patient 1 than in Patient 2. Due to G-CSF refractory life-threatening neutropenia, Patient 1 successfully underwent an urgent hematopoietic stem cell transplantation (HSCT) from a 9/10 matched unrelated donor. Patient 2 experienced a similar, although delayed, disease evolution and is currently on anti-TNF therapy and anti-infectious prophylaxis. The unique cases confirmed that heterozygous patients with null ADA2 activity deserve deep investigation for possible structural variants on a single allele. Moreover, this report emphasizes the importance of timely recognizing DADA2 at the onset to allow adequate follow-up and detection of disease progression. Finally, the therapeutic management in these identical twins raises significant concerns as they share a similar phenotype, with a delayed but almost predictable disease evolution in one of them, who could benefit from a prompt definitive treatment like elective allogeneic HSCT. Additional data are required to assess whether the absence of enzymatic activity at diagnosis is associated with hematological involvement and is also predictive of bone marrow dysfunction, encouraging early HSCT to improve functional outcomes.

Published

2022

2. Natural history of type 1 diabetes on an immunodysregulatory background with genetic alteration in B-cell activating factor receptor: A case report

Author

Biagio Di Lorenzo, Lucia Pacillo, Giulia Milardi, Tatiana Jofra, Silvia Di Cesare, Jolanda Gerosa, Ilaria Marzinotto, Ettore Zapparoli, Beatrice Rivalta, Cristina Cifaldi, Federica Barzaghi, Carmela Giancotta, Paola Zangari, Novella Rapini, Annalisa Deodati, Giada Amodio, Laura Passerini, Paola Carrera, Silvia Gregori, Paolo Palma, Andrea Finocchi, Vito Lampasona, Maria Pia Cicalese, Riccardo Schiaffini, Gigliola Di Matteo, Ivan Merelli, Matteo Barcella, Alessandro Aiuti, Lorenzo Piemonti, Caterina Cancrini, and Georgia Fousteri

Subjects

type 1 diabetes (T1D), common variable immunodeficiency (CVID), BAFFR mutation, islet autoimmunity, circulating T follicular helper cells (cTfh), Immunologic diseases. Allergy, RC581-607

Abstract

The immunological events leading to type 1 diabetes (T1D) are complex and heterogeneous, underscoring the necessity to study rare cases to improve our understanding. Here, we report the case of a 16-year-old patient who showed glycosuria during a regular checkup. Upon further evaluation, stage 2 T1D, autoimmune thrombocytopenic purpura (AITP), and common variable immunodeficiency (CVID) were diagnosed. The patient underwent low carb diet, losing > 8 kg, and was placed on Ig replacement therapy. Anti-CD20 monoclonal antibody (Rituximab, RTX) was administered 2 years after diagnosis to treat peripheral polyneuropathy, whereas an atypical mycobacteriosis manifested 4 years after diagnosis and was managed with prolonged antibiotic treatment. In the fifth year of monitoring, the patient progressed to insulin dependency despite ZnT8A autoantibody resolution and IA-2A and GADA autoantibody decline. The patient had low T1D genetic risk score (GRS = 0.22817) and absence of human leukocyte antigen (HLA) DR3/DR4-DQ8. Genetic analysis identified the monoallelic mutation H159Y in TNFRSF13C, a gene encoding B-cell activating factor receptor (BAFFR). Significant reduced blood B-cell numbers and BAFFR levels were observed in line with a dysregulation in BAFF–BAFFR signaling. The elevated frequency of PD-1+ dysfunctional Tfh cells composed predominantly by Th1 phenotype was observed at disease onset and during follow-up. This case report describes a patient progressing to T1D on a BAFFR-mediated immunodysregulatory background, suggesting a role of BAFF–BAFFR signaling in islet-specific tolerance and T1D progression.

Published

2022

3. Regulatory T cells from patients with end-stage organ disease can be isolated, expanded and cryopreserved according good manufacturing practice improving their function

Author

Francesca Ulbar, Tiziana Montemurro, Tatiana Jofra, Miriam Capri, Giorgia Comai, Valentina Bertuzzo, Cristiana Lavazza, Alessandra Mandelli, Mariele Viganò, Silvia Budelli, Maria Giulia Bacalini, Chiara Pirazzini, Paolo Garagnani, Valeria Giudice, Daria Sollazzo, Antonio Curti, Mario Arpinati, Gaetano La Manna, Matteo Cescon, Antonio Daniele Pinna, Claudio Franceschi, Manuela Battaglia, Rosaria Giordano, Lucia Catani, and Roberto Massimo Lemoli

Subjects

End stage organ disease, Regulatory T cells, Safety, Murine model, Medicine

Abstract

Abstract Background Here, we isolated, expanded and functionally characterized regulatory T cells (Tregs) from patients with end stage kidney and liver disease, waiting for kidney/liver transplantation (KT/LT), with the aim to establish a suitable method to obtain large numbers of immunomodulatory cells for adoptive immunotherapy post-transplantation. Methods We first established a preclinical protocol for expansion/isolation of Tregs from peripheral blood of LT/KT patients. We then scaled up and optimized such protocol according to good manufacturing practice (GMP) to obtain high numbers of purified Tregs which were phenotypically and functionally characterized in vitro and in vivo in a xenogeneic acute graft-versus-host disease (aGVHD) mouse model. Specifically, immunodepressed mice (NOD-SCID-gamma KO mice) received human effector T cells with or without GMP-produced Tregs to prevent the onset of xenogeneic GVHD. Results Our small scale Treg isolation/expansion protocol generated functional Tregs. Interestingly, cryopreservation/thawing did not impair phenotype/function and DNA methylation pattern of FOXP3 gene of the expanded Tregs. Fully functional Tregs were also isolated/expanded from KT and LT patients according to GMP. In the mouse model, GMP Tregs from LT or KT patient proved to be safe and show a trend toward reduced lethality of acute GVHD. Conclusions These data demonstrate that expanded/thawed GMP-Tregs from patients with end-stage organ disease are fully functional in vitro. Moreover, their infusion is safe and results in a trend toward reduced lethality of acute GVHD in vivo, further supporting Tregs-based adoptive immunotherapy in solid organ transplantation.

Published

2019

4. Murine Pancreatic Islets Transplantation under the Kidney Capsule

Author

Tatiana Jofra, Giuseppe Galvani, Fousteri Georgia, Gregori Silvia, Nicola Gagliani, and Manuela Battaglia

Subjects

Biology (General), QH301-705.5

Abstract

Type 1 diabetes (T1D) is an autoimmune disease caused by the lack of insulin-producing pancreatic beta cells leading to systemic hyperglycemia. Pancreatic islet transplantation is a valid therapeutic approach to restore insulin loss and to promote adequate glycemic control. Pancreatic islet transplantation in mice is an optimal preclinical model to identify new therapeutic strategies aiming at preventing rejection and optimizing post-transplant immuno-suppressive/-tolerogenic therapies. Islet transplantation in preclinical animal models can be performed in different sites such the kidney capsule, spleen, bone marrow and pancreas. This protocol describes murine islet transplantation under the kidney capsule. This is a widely accepted procedure for research purposes. Stress caused in the animals is minimal and it leads to reliable and reproducible results.

Published

2018

5. Extrinsic Protein Tyrosine Phosphatase Non-Receptor 22 Signals Contribute to CD8 T Cell Exhaustion and Promote Persistence of Chronic Lymphocytic Choriomeningitis Virus Infection

Author

Tatiana Jofra, Giuseppe Galvani, Mirela Kuka, Roberta Di Fonte, Bechara G. Mfarrej, Matteo Iannacone, Shahram Salek-Ardakani, Manuela Battaglia, and Georgia Fousteri

Subjects

protein tyrosine phosphatase non-receptor 22, persistent viral infection, T cell exhaustion, lymphocytic choriomeningitis virus clone 13, genetic predisposition, Immunologic diseases. Allergy, RC581-607

Abstract

A genetic variant of the protein tyrosine phosphatase non-receptor 22 (PTPN22) is associated with a wide range of autoimmune diseases; however, the reasons behind its prevalence in the general population remain not completely understood. Recent evidence highlights an important role of autoimmune susceptibility genetic variants in conferring resistance against certain pathogens. In this study, we examined the role of PTPN22 in persistent infection in mice lacking PTPN22 infected with lymphocytic choriomeningitis virus clone 13. We found that lack of PTPN22 in mice resulted in viral clearance 30 days after infection, which was reflected in their reduced weight loss and overall improved health. PTPN22−/− mice exhibited enhanced virus-specific CD8 and CD4 T cell numbers and functionality and reduced exhausted phenotype. Moreover, mixed bone marrow chimera studies demonstrated no differences in virus-specific CD8 T cell accumulation and function between the PTPN22+/+ and PTPN22−/− compartments, showing that the effects of PTPN22 on CD8 T cells are T cell-extrinsic. Together, these findings identify a CD8 T cell-extrinsic role for PTPN22 in weakening early CD8 T cell responses to collectively promote persistence of a chronic viral infection.

Published

2017

6. Combination of an Antigen-Specific Therapy and an Immunomodulatory Treatment to Simultaneous Block Recurrent Autoimmunity and Alloreactivity in Non-Obese Diabetic Mice.

Author

Georgia Fousteri, Tatiana Jofra, Roberta Di Fonte, and Manuela Battaglia

Subjects

Medicine, Science

Abstract

Restoration of endogenous insulin production by islet transplantation is considered a curative option for patients with type 1 diabetes. However, recurrent autoimmunity and alloreactivity cause graft rejection hindering successful transplantation. Here we tested whether transplant tolerance to allogeneic islets could be achieved in non-obese diabetic (NOD) mice by simultaneously tackling autoimmunity via antigen-specific immunization, and alloreactivity via granulocyte colony stimulating factor (G-CSF) and rapamycin (RAPA) treatment. Immunization with insB9-23 peptide alone or in combination with two islet peptides (IGRP206-214 and GAD524-543) in incomplete Freund's adjuvant (IFA) were tested for promoting syngeneic pancreatic islet engraftment in spontaneously diabetic NOD mice. Treatment with G-CSF/RAPA alone or in combination with insB9-23/IFA was examined for promoting allogeneic islet engraftment in the same mouse model. InsB9-23/IFA immunization significantly prolonged syngeneic pancreatic islet survival in NOD mice by a mechanism that necessitated the presence of CD4+CD25+ T regulatory (Treg) cells, while combination of three islet epitopes was less efficacious in controlling recurrent autoimmunity. G-CSF/RAPA treatment was unable to reverse T1D or control recurrent autoimmunity but significantly prolonged islet allograft survival in NOD mice. Blockade of interleukin-10 (IL-10) during G-CSF/RAPA treatment resulted in allograft rejection suggesting that IL-10-producing cells were fundamental to achieve transplant tolerance. G-CSF/RAPA treatment combined with insB9-23/IFA did not further increase the survival of allogeneic islets. Thus, insB9-23/IFA immunization controls recurrent autoimmunity and G-CSF/RAPA treatment limits alloreactivity, however their combination does not further promote allogeneic pancreatic islet engraftment in NOD mice.

Published

2015

7. Immune Depletion in Combination with Allogeneic Islets Permanently Restores Tolerance to Self-Antigens in Diabetic NOD Mice.

Author

Nicola Gagliani, Tatiana Jofra, Amanda L Posgai, Mark A Atkinson, and Manuela Battaglia

Subjects

Medicine, Science

Abstract

The destruction of beta cells in type 1 diabetes (T1D) results in loss of insulin production and glucose homeostasis. Treatment of non-obese diabetic (NOD) mice with immune-depleting/modulating agents (e.g., anti-CD3, murine anti-thymocyte-globulin (mATG)) can lead to diabetes reversal. However, for preclinical studies with these and other agents seeking to reverse disease at onset, the necessity for exogenous insulin administration is debated. Spontaneously diabetic NOD mice were treated with a short-course of mATG and insulin provided as drug therapy or by way of allogeneic islet implants. Herein we demonstrate that exogenous insulin administration is required to achieve disease reversal with mATG in NOD mice. Unexpectedly, we also observed that provision of insulin by way of allogeneic islet implantation in combination with mATG leads to a pronounced reversal of diabetes as well as restoration of tolerance to self-islets. Expansion/induction of regulatory cells was observed in NOD mice stably cured with mATG and allogeneic islets. These data suggest that transient provision of allogeneic insulin-producing islets might provide a temporary window for immune depletion to be more effective and instilling stable tolerance to endogenous beta cells. These findings support the use of a never before explored approach for preserving beta cell function in patients with recent onset T1D.

Published

2015

8. Reply to Comment on 'Stability of human rapamycin-expanded CD4+CD25+ T-regulatory cells' Haematologica 2011;96(9):1357–65

Author

Eleonora Tresoldi, Ilaria Dell’Albani, Angela Stabilini, Tatiana Jofra, Andrea Valle, Nicola Gagliani, Attilio Bondanza, Maria Grazia Roncarolo, and Manuela Battaglia

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Published

2012

9. Stability of human rapamycin-expanded CD4+CD25+ T regulatory cells

Author

Eleonora Tresoldi, Ilaria Dell’Albani, Angela Stabilini, Tatiana Jofra, Andrea Valle, Nicola Gagliani, Attilio Bondanza, Maria Grazia Roncarolo, and Manuela Battaglia

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Background The clinical use of ex vivo-expanded T-regulatory cells for the treatment of T-cell-mediated diseases has gained increasing momentum. However, the recent demonstration that FOXP3+ T-regulatory cells may contain interleukin-17–producing cells and that they can convert into effector cells once transferred in vivo raises significant doubts about their safety. We previously showed that rapamycin permits the ex vivo expansion of FOXP3+ T-regulatory cells while impairing the proliferation of non-T-regulatory cells. Here we investigated the Th17-cell content and the in vivo stability of rapamycin-expanded T-regulatory cells as pertinent aspects of cell-based therapy.Design and Methods T-regulatory-enriched cells were isolated from healthy volunteers and were expanded ex vivo with rapamycin with a pre-clinical applicable protocol. T-regulatory cells cultured with and without rapamycin were compared for their regulatory activity, content of pro-inflammatory cells and stability.Results We found that CD4+CCR6+CD161+ T cells (i.e., precursor/committed Th17 cells) contaminate the T-regulatory cells cultured ex vivo in the absence of rapamycin. In addition, Th17 cells do not expand when rapamycin-treated T-regulatory cells are exposed to a “Th17-favorable” environment. Rapamycin-expanded T-regulatory cells maintain their in vitro regulatory phenotype even after in vivo transfer into immunodeficient NOD-SCID mice despite being exposed to the irradiation-induced pro-inflammatory environment. Importantly, no additional rapamycin treatment, either in vitro or in vivo, is required to keep their phenotype fixed.Conclusions These data demonstrate that rapamycin secures ex vivo-expanded human T-regulatory cells and provide additional justification for their clinical use in future cell therapy-based trials.

Published

2011

10. Rapamycin combined with anti-CD45RB mAb and IL-10 or with G-CSF induces tolerance in a stringent mouse model of islet transplantation.

Author

Nicola Gagliani, Silvia Gregori, Tatiana Jofra, Andrea Valle, Angela Stabilini, David M Rothstein, Mark Atkinson, Maria Grazia Roncarolo, and Manuela Battaglia

Subjects

Medicine, Science

Abstract

A large pool of preexisting alloreactive effector T cells can cause allogeneic graft rejection following transplantation. However, it is possible to induce transplant tolerance by altering the balance between effector and regulatory T (Treg) cells. Among the various Treg-cell types, Foxp3(+)Treg and IL-10-producing T regulatory type 1 (Tr1) cells have frequently been associated with tolerance following transplantation in both mice and humans. Previously, we demonstrated that rapamycin+IL-10 promotes Tr1-cell-associated tolerance in Balb/c mice transplanted with C57BL/6 pancreatic islets. However, this same treatment was unsuccessful in C57BL/6 mice transplanted with Balb/c islets (classified as a stringent transplant model). We accordingly designed a protocol that would be effective in the latter transplant model by simultaneously depleting effector T cells and fostering production of Treg cells. We additionally developed and tested a clinically translatable protocol that used no depleting agent.Diabetic C57BL/6 mice were transplanted with Balb/c pancreatic islets. Recipient mice transiently treated with anti-CD45RB mAb+rapamycin+IL-10 developed antigen-specific tolerance. During treatment, Foxp3(+)Treg cells were momentarily enriched in the blood, followed by accumulation in the graft and draining lymph node, whereas CD4(+)IL-10(+)IL-4(-) T (i.e., Tr1) cells localized in the spleen. In long-term tolerant mice, only CD4(+)IL-10(+)IL-4(-) T cells remained enriched in the spleen and IL-10 was key in the maintenance of tolerance. Alternatively, recipient mice were treated with two compounds routinely used in the clinic (namely, rapamycin and G-CSF); this drug combination promoted tolerance associated with CD4(+)IL-10(+)IL-4(-) T cells.The anti-CD45RB mAb+rapamycin+IL-10 combined protocol promotes a state of tolerance that is IL-10 dependent. Moreover, the combination of rapamycin+G-CSF induces tolerance and such treatment could be readily translatable into the clinic.

Published

2011

11. Genetic determinants of type 1 diabetes in individuals with weak evidence of islet autoimmunity at disease onset

Author

Paola Carrera, Ilaria Marzinotto, Riccardo Bonfanti, Luca Massimino, Silvia Calzavara, Μariagrazia Favellato, Tatiana Jofra, Valeria De Giglio, Clara Bonura, Angela Stabilini, Valeria Favalli, Simone Bondesan, Maria Pia Cicalese, Andrea Laurenzi, Amelia Caretto, Giulio Frontino, Andrea Rigamonti, Chiara Molinari, Marina Scavini, Federica Sandullo, Ettore Zapparoli, Nicoletta Caridi, Silvia Bonfiglio, Valeria Castorani, Federica Ungaro, Alessandra Petrelli, Graziano Barera, Alessandro Aiuti, Emanuele Bosi, Manuela Battaglia, Lorenzo Piemonti, Vito Lampasona, and Georgia Fousteri

Subjects

Endocrinology, Diabetes and Metabolism, Internal Medicine

Published

2023

12. CXCR5‐CXCL13 axis markers in full‐term and preterm human neonates in the first weeks of life

Author

Alessandro Aiuti, Andrea Ronchi, Carlo Pietrasanta, Fabio Mosca, Lorenza Pugni, Tatiana Jofra, Pasqualina De Leo, Maria Pia Cicalese, Georgia Fousteri, Pietrasanta, C., De Leo, P., Jofra, T., Ronchi, A., Pugni, L., Mosca, F., Aiuti, A., Cicalese, M. P., and Fousteri, G.

Subjects

Receptors, CXCR5, 0301 basic medicine, Term Birth, Vaccine response, Immunology, Biology, CXCR5, Immunophenotyping, Sepsis, 03 medical and health sciences, 0302 clinical medicine, Text mining, medicine, Humans, Immunology and Allergy, CXCL13, Full Term, business.industry, Infant, Newborn, Germinal center, T-Lymphocytes, Helper-Inducer, medicine.disease, Chemokine CXCL13, Phenotype, 030104 developmental biology, Premature Birth, Disease Susceptibility, business, Biomarkers, 030215 immunology

Abstract

Term and preterm neonates have very few circulating Tfh-like cells (cTfh), and no circulating Tfr-like cells. Neonatal cTfh are CXCR5lo PD-1lo CD45RAhi , suggestive of a naive, possibly recently activated phenotype. CXCL13 is high at birth, but decreases rapidly in the first weeks of life. Overall, signs of GC activity in human neonates are weak, even in those born prematurely or after sepsis. Term and preterm neonates have very few circulating Tfh-like cells (cTfh), and no circulating Tfr-like cells. Neonatal cTfh are CXCR5(lo)PD-1(lo)CD45RA(hi), suggestive of a naive, possibly recently activated phenotype. CXCL13 is high at birth, but decreases rapidly in the first weeks of life. Overall, signs of GC activity in human neonates are weak, even in those born prematurely or after sepsis. (dagger)

Published

2021

13. Follicular helper T cell signature of replicative exhaustion, apoptosis, and senescence in common variable immunodeficiency

Author

Giulia Milardi, Biagio Di Lorenzo, Jolanda Gerosa, Federica Barzaghi, Gigliola Di Matteo, Maryam Omrani, Tatiana Jofra, Ivan Merelli, Matteo Barcella, Matteo Filippini, Anastasia Conti, Francesca Ferrua, Francesco Pozzo Giuffrida, Francesca Dionisio, Patrizia Rovere‐Querini, Sarah Marktel, Andrea Assanelli, Simona Piemontese, Immacolata Brigida, Matteo Zoccolillo, Emilia Cirillo, Giuliana Giardino, Maria Giovanna Danieli, Fernando Specchia, Lucia Pacillo, Silvia Di Cesare, Carmela Giancotta, Francesca Romano, Alessandro Matarese, Alfredo Antonio Chetta, Matteo Trimarchi, Andrea Laurenzi, Maurizio De Pellegrin, Silvia Darin, Davide Montin, Maddalena Marinoni, Rosa Maria Dellepiane, Valeria Sordi, Vassilios Lougaris, Angelo Vacca, Raffaella Melzi, Rita Nano, Chiara Azzari, Lucia Bongiovanni, Claudio Pignata, Caterina Cancrini, Alessandro Plebani, Lorenzo Piemonti, Constantinos Petrovas, Raffaella Di Micco, Maurilio Ponzoni, Alessandro Aiuti, Maria Pia Cicalese, Georgia Fousteri, Milardi, Giulia, Di Lorenzo, Biagio, Gerosa, Jolanda, Barzaghi, Federica, Di Matteo, Gigliola, Omrani, Maryam, Jofra, Tatiana, Merelli, Ivan, Barcella, Matteo, Filippini, Matteo, Conti, Anastasia, Ferrua, Francesca, Pozzo Giuffrida, Francesco, Dionisio, Francesca, Rovere-Querini, Patrizia, Marktel, Sarah, Assanelli, Andrea, Piemontese, Simona, Brigida, Immacolata, Zoccolillo, Matteo, Cirillo, Emilia, Giardino, Giuliana, Danieli, Maria Giovanna, Specchia, Fernando, Pacillo, Lucia, Di Cesare, Silvia, Giancotta, Carmela, Romano, Francesca, Matarese, Alessandro, Chetta, Alfredo Antonio, Trimarchi, Matteo, Laurenzi, Andrea, De Pellegrin, Maurizio, Darin, Silvia, Montin, Davide, Marinoni, Maddalena, Dellepiane, Rosa Maria, Sordi, Valeria, Lougaris, Vassilio, Vacca, Angelo, Melzi, Raffaella, Nano, Rita, Azzari, Chiara, Bongiovanni, Lucia, Pignata, Claudio, Cancrini, Caterina, Plebani, Alessandro, Piemonti, Lorenzo, Petrovas, Constantino, Di Micco, Raffaella, Ponzoni, Maurilio, Aiuti, Alessandro, Cicalese, Maria Pia, Fousteri, Georgia, and Giuffrida, Francesco Pozzo

Subjects

T cell exhaustion, B cells, B cell, T Follicular Helper Cells, Immunology, Programmed Cell Death 1 Receptor, Apoptosi, Apoptosis, T-Lymphocytes, Helper-Inducer, Common variable immunodeficiency, Common Variable Immunodeficiency, Settore MED/02, T-cell exhaustion, Immune aging, Humans, T follicular helper cells, Immunology and Allergy, T Follicular Helper Cell, immune aging, Human

Abstract

Common variable immunodeficiency (CVID) is the most frequent primary antibody deficiency whereby follicular helper T (Tfh) cells fail to establish productive responses with B cells in germinal centers. Here, we analyzed the frequency, phenotype, transcriptome and function of circulating Tfh (cTfh) cells in CVID patients displaying autoimmunity as an additional phenotype. A group of patients showed a high frequency of cTfh1 cells and a prominent expression of PD-1 and ICOS, as well as a cTfh mRNA signature consistent with highly activated, but exhausted, senescent and apoptotic cells. Plasmatic CXCL13 levels were elevated in this group and positively correlated with cTfh1 cell frequency and PD-1 levels. Monoallelic variants in RTEL1, a telomere length- and DNA repair-related gene, were identified in four patients belonging to this group. Their blood lymphocytes showed shortened telomeres, while their cTfh were more prone to apoptosis. These data point toward a novel pathogenetic mechanism in CVID, whereby alterations in DNA repair and telomere elongation might predispose to antibody deficiency. A Th1, highly activated but exhausted and apoptotic cTfh phenotype was associated with this form of CVID. This article is protected by copyright. All rights reserved.

Published

2022

14. Follicular helper T cell signature of replicative exhaustion, apoptosis and senescence in common variable immunodeficiency

Author

Chetta Aa, Georgia Fousteri, Sarah Marktel, Andrea Assanelli, Giuffrida Fp, Darin S, Zoccolillo M, Rita Nano, Andrea Laurenzi, Maria Giovanna Danieli, Simona Piemontese, Davide Montin, Carmela Giancotta, Barcella M, Dionisio F, Sordi, Chiara Azzari, Jolanda Gerosa, Matarese A, Lorenzo Bd, Matteo Trimarchi, Raffaella Melzi, Caterina Cancrini, Bongiovanni L, Claudio Pignata, Immacolata Brigida, Tatiana Jofra, Angelo Vacca, Lorenzo Piemonti, Maryam Omrani, Alessandro Aiuti, Silvia Di Cesare, Giuliana Giardino, Ivan Merelli, Alessandro Plebani, Maurilio Ponzoni, Constantinos Petrovas, Fernando Specchia, Pellegrin, M. P. Cicalese, Milardi G, Francesca Ferrua, Emilia Cirillo, Lougaris, Gigliola Di Matteo, Patrizia Rovere-Querini, Federica Barzaghi, Lucia Pacillo, Rosa Maria Dellepiane, and Romano F

Subjects

Senescence, T cell, Common variable immunodeficiency, Germinal center, Biology, medicine.disease, medicine.disease_cause, Telomere, Autoimmunity, Transcriptome, medicine.anatomical_structure, Immunology, medicine, CXCL13

Abstract

BackgroundCommon variable immunodeficiency (CVID) is the most frequent primary antibody deficiency. A significant number of CVID patients are affected by various manifestations of immune dysregulation such as autoimmunity. Follicular T cells cells are thought to support the development of CVID by providing inappropriate signals to B cells during the germinal center (GC) response.ObjectivesWe determined the possible role of follicular helper (Tfh) and follicular regulatory T (Tfr) cells in patients with CVID by phenotypic, molecular, and functional studies.MethodsWe analyzed the frequency, phenotype, transcriptome, and function of circulating Tfh cells in the peripheral blood of 27 CVID patients (11 pediatric and 16 adult) displaying autoimmunity as additional phenotype and compared them to 106 (39 pediatric and 67 adult) age-matched healthy controls. We applied Whole Exome Sequencing (WES) and Sanger sequencing to identify mutations that could account for the development of CVID and associate with Tfh alterations.ResultsA group of CVID patients (n=9) showed super-physiological frequency of Tfh1 cells and a prominent expression of PD-1 and ICOS, as well as a Tfh RNA signature consistent with highly active, but exhausted and apoptotic cells. Plasmatic CXCL13 levels were elevated in these patients and positively correlated with Tfh1 cell frequency, PD-1 levels, and an elevated frequency of CD21loCD38loautoreactive B cells. Monoallelic variants inRTEL1, a telomere length- and DNA repair-related gene, were ideintified in four patients belonging to this group. Lymphocytes with highly shortened telomeres, and a Tfh signature enriched in genes involved in telomere elongation and response to DNA damage were seen. Histopathological analysis of the spleen in one patient showed reduced amount and size of the GC that, unexpectedly, contained an increased number of Tfh cells.ConclusionThese data point toward a novel pathogenetic mechanism in a group of patients with CVID, whereby alterations in DNA repair and telomere elongation might be involved in GC B cells, and acquisition of a Th1, highly activated but exhausted and apoptotic phenotype by Tfh cells.

Published

2021

15. Experimental colitis in IL-10-deficient mice ameliorates in the absence of PTPN22

Author

Chiara Sorini, Marika Falcone, L De Giorgi, A Annoni, Tatiana Jofra, Georgia Fousteri, Ilaria Cosorich, Giuseppe Galvani, and A Vecchione

Subjects

Male, 0301 basic medicine, Chemokine CXCL1, Immunology, Protein tyrosine phosphatase, PTPN22, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, Animals, Immunology and Allergy, Receptors, Interleukin-10, Colitis, Receptor, business.industry, Dextran Sulfate, Interleukin-17, Interleukin, Protein Tyrosine Phosphatase, Non-Receptor Type 22, Inflammatory Bowel Diseases, medicine.disease, Interleukin-10, CXCL1, Disease Models, Animal, Interleukin 10, 030104 developmental biology, Editors’ Choice, Gene Knockdown Techniques, Th17 Cells, Female, business, 030215 immunology

Abstract

Summary Interleukin (IL)-10 plays a key role in controlling intestinal inflammation. IL-10-deficient mice and patients with mutations in IL-10 or its receptor, IL-10R, show increased susceptibility to inflammatory bowel diseases (IBD). Protein tyrosine phosphatase, non-receptor type 22 (PTPN22) controls immune cell activation and the equilibrium between regulatory and effector T cells, playing an important role in controlling immune homoeostasis of the gut. Here, we examined the role of PTPN22 in intestinal inflammation of IL-10-deficient (IL-10–/–) mice. We crossed IL-10–/– mice with PTPN22–/– mice to generate PTPN22–/–IL-10–/– double knock-out mice and induced colitis with dextran sodium sulphate (DSS). In line with previous reports, DSS-induced acute and chronic colitis was exacerbated in IL-10–/– mice compared to wild-type (WT) controls. However, PTPN22–/–IL-10–/– double knock-out mice developed milder disease compared to IL-10–/– mice. IL-17-promoting innate cytokines and T helper type 17 (Th17) cells were markedly increased in PTPN22–/–IL-10–/– mice, but did not provide a protctive function. CXCL1/KC was also increased in PTPN22–/–IL-10–/– mice, but therapeutic injection of CXCL1/KC in IL-10–/– mice did not ameliorate colitis. These results show that PTPN22 promotes intestinal inflammation in IL-10-deficient mice, suggesting that therapeutic targeting of PTPN22 might be beneficial in patients with IBD and mutations in IL-10 and IL-10R.

Published

2019

16. Persistence of circulating T-follicular helper cells after rituximab is associated with relapse of IgG4-related disease

Author

Gaia Mancuso, Emanuel Della-Torre, Tatiana Jofra, Lorenzo Dagna, Georgia Fousteri, Marco Lanzillotta, Maria Pia Cicalese, Giulia di Colo, Alessandro Aiuti, Mancuso, G., Jofra, T., Lanzillotta, M., Aiuti, A., Cicalese, M. P., di Colo, G., Dagna, L., Fousteri, G., and Della-Torre, E.

Subjects

Male, T Follicular Helper Cells, business.industry, Middle Aged, medicine.disease, Prognosis, Persistence (computer science), Treatment Outcome, Rheumatology, Recurrence, Antirheumatic Agents, Follicular phase, Immunology, Medicine, Humans, Pharmacology (medical), IgG4-related disease, Rituximab, Female, Immunoglobulin G4-Related Disease, business, medicine.drug, Aged

Published

2021

17. Reduced Follicular Regulatory T Cells in Spleen and Pancreatic Lymph Nodes of Patients With Type 1 Diabetes

Author

Andrea Vecchione, Maria Pia Cicalese, Mariagrazia Favellato, Raffaela Melzi, Constantinos Petrovas, Elio Ippolito, Giuseppe Galvani, Kimberly Shankwitz, Eleonora Bianconi, Alessandro Aiuti, Angela Stabilini, Nichole Danzl, Manuela Battaglia, Roberta Di Fonte, Lorenzo Piemonti, Georgia Fousteri, Francesca Ragogna, Pauline Grogan, Emanuele Bosi, Rita Nano, Andrea Laurenzi, Todd M. Brusko, Jolanda Gerosa, Giulia Milardi, Tatiana Jofra, Howie R Seay, Amelia Caretto, Andrew R Schultz, Vecchione, Andrea, Jofra, Tatiana, Gerosa, Jolanda, Shankwitz, Kimberly, Di Fonte, Roberta, Galvani, Giuseppe, Ippolito, Elio, Cicalese, Maria Pia, Schultz, Andrew R, Seay, Howie R, Favellato, Mariagrazia, Milardi, Giulia, Stabilini, Angela, Ragogna, Francesca, Grogan, Pauline, Bianconi, Eleonora, Laurenzi, Andrea, Caretto, Amelia, Nano, Rita, Melzi, Raffaela, Danzl, Nichole, Bosi, Emanuele, Piemonti, Lorenzo, Aiuti, Alessandro, Brusko, Todd, Petrovas, Constantino, Battaglia, Manuela, and Fousteri, Georgia

Subjects

Adult, Adoptive cell transfer, endocrine system, Endocrinology, Diabetes and Metabolism, Cell, Spleen, Mice, SCID, T-Lymphocytes, Regulatory, Pancreatic Lymph Node, Mice, Mice, Inbred NOD, Follicular phase, Internal Medicine, medicine, Animals, Humans, Lymphocyte Count, Pancreas, Cells, Cultured, Type 1 diabetes, business.industry, Autoantibody, Peripheral tolerance, medicine.disease, Mice, Inbred C57BL, medicine.anatomical_structure, Diabetes Mellitus, Type 1, Case-Control Studies, Immunology, Lymph Nodes, Immunology and Transplantation, business

Abstract

In the attempt to understand the origin of autoantibody (AAb) production in patients with and at-risk for T1D, multiple studies have analyzed and reported alterations in follicular helper T cells (Tfh) in presymptomatic AAb-positive subjects and patients with T1D. Yet, it is still not clear whether the regulatory counterpart of Tfh cells, represented by follicular regulatory T cells (Tfr), is similarly altered. To address this question, we performed analyses in peripheral blood, spleen and pancreatic lymph nodes (PLN) of organ donor subjects with T1D. Blood analyses were also performed in living AAb-negative and -positive subjects. While negligible differences in the frequency and phenotype of blood Tfr cells were observed between T1D, AAb-negative and AAb-positive adult subjects, the frequency of Tfr cells was significantly reduced in spleen and PLN of T1D as compared to non-diabetic controls. Furthermore, adoptive transfer of Tfr cells delayed disease development in a mouse model of T1D, a finding that could indicate that Tfr cells play an important role in peripheral tolerance and regulation of autoreactive Tfh cells. Together, our findings provide evidence of Tfr cell alterations within disease-relevant tissues in patients with T1D suggesting a role for Tfr cells in defective humoral tolerance and disease pathogenesis.

Published

2021

18. Author response for 'CXCR5‐CXCL13 axis markers in full‐term and preterm human neonates in the first weeks of life'

Author

Andrea Ronchi, Pasqualina De Leo, Tatiana Jofra, Fabio Mosca, Georgia Fousteri, Lorenza Pugni, Alessandro Aiuti, Carlo Pietrasanta, and Maria Pia Cicalese

Subjects

Pediatrics, medicine.medical_specialty, medicine, Biology, Full Term

Published

2020

19. Key role of macrophages in tolerance induction via T regulatory type 1 (Tr1) cells

Author

Bechara Mfarrej, Nicola Gagliani, Manuela Battaglia, Georgia Fousteri, Cristina Morsiani, Tatiana Jofra, Mfarrej B., Jofra T., Morsiani C., Gagliani N., Fousteri G., and Battaglia M.

Subjects

0301 basic medicine, regulatory T cell, Macrophage, Immunology, Islets of Langerhans Transplantation, Spleen, T-Lymphocytes, Regulatory, Diabetes Mellitus, Experimental, 03 medical and health sciences, Mice, 0302 clinical medicine, In vivo, Insulin-Secreting Cells, Granulocyte Colony-Stimulating Factor, medicine, Immunology and Allergy, Animals, Humans, Transplantation, Homologous, Sirolimu, Transplantation, Homologou, Cells, Cultured, Sirolimus, Mice, Inbred BALB C, tolerance, Animal, Chemistry, Pancreatic islets, Macrophages, Interleukin, Peripheral tolerance, Original Articles, Th1 Cells, Cell biology, Transplantation, Mice, Inbred C57BL, Tolerance induction, Disease Models, Animal, Th1 Cell, 030104 developmental biology, medicine.anatomical_structure, Insulin-Secreting Cell, Transplantation Tolerance, transplantation, Human, 030215 immunology

Abstract

Summary T regulatory type 1 (Tr1) cells are a class of regulatory T cells (Tregs) participating in peripheral tolerance, hence the rationale behind their testing in clinical trials in different disease settings. One of their applications is tolerance induction to allogeneic islets for long-term diabetes-free survival. Currently the cellular and molecular mechanisms that promote Tr1-cell induction in vivo remain poorly understood. We employed a mouse model of transplant tolerance where treatment with granulocyte colony-stimulating factor (G-CSF)/rapamycin induces permanent engraftment of allogeneic pancreatic islets in C57BL/6 mice via Tr1 cells. The innate composition of graft and spleen cells in tolerant mice was analyzed by flow cytometry. Graft phagocytic cells were co-cultured with CD4+ T cells in vitro to test their ability to induce Tr1-cell induction. Graft phagocytic cells were depleted in vivo at different time-points during G-CSF/rapamycin treatment, to identify their role in Tr1-cell induction and consequently in graft survival. In the spleen, the site of Tr1-cell induction, no differences in the frequencies of macrophages or dendritic cells (DC) were observed. In the graft, the site of antigen uptake, a high proportion of macrophages and not DC was detected in tolerant but not in rejecting mice. Graft-infiltrating macrophages of G-CSF/rapamycin-treated mice had an M2 phenotype, characterized by higher CD206 expression and interleukin (IL)-10 production, whereas splenic macrophages only had an increased CD206 expression. Graft-infiltrating cells from G-CSF/rapamycin-treated mice-induced Tr1-cell expansion in vitro. Furthermore, Tr1-cell induction was perturbed upon in-vivo depletion of phagocytic cells, early and not late during treatment, leading to graft loss suggesting that macrophages play a key role in tolerance induction mediated by Tr1 cells. Taken together, in this mouse model of Tr1-cell induced tolerance to allogeneic islets, M2 macrophages infiltrating the graft upon G-CSF/rapamycin treatment are key for Tr1-cell induction. This work provides mechanistic insight into pharmacologically induced Tr1-cell expansion in vivo in this stringent model of allogeneic transplantation.

Published

2020

20. A Prevalent CXCR3+ Phenotype of Circulating Follicular Helper T Cells Indicates Humoral Dysregulation in Children with Down Syndrome

Author

Andrea Vecchione, Micaela Santini, Cristiana Trimarchi, Pasqualina De Leo, Maria Pia Cicalese, Maddalena Marinoni, Giorgio Ottaviano, Tatiana Jofra, Massimo Agosti, Georgia Fousteri, Jolanda Gerosa, Alessandro Aiuti, Maurizio De Pellegrin, Ottaviano, Giorgio, Gerosa, Jolanda, Santini, Micaela, De Leo, Pasqualina, Vecchione, Andrea, Jofra, Tatiana, Trimarchi, Cristiana, De Pellegrin, Maurizio, Agosti, Massimo, Aiuti, Alessandro, Marinoni, Maddalena, Cicalese, Maria Pia, and Fousteri, Georgia

Subjects

Male, Down syndrome, Receptors, CXCR3, Adolescent, T cell, Immunology, CXCR3, medicine.disease_cause, Autoimmunity, Autoimmune Diseases, follicular helper T cells, T-Lymphocyte Subsets, Follicular phase, medicine, Immunology and Allergy, Humans, Child, follicular helper T cell, Th1-Th2 Balance, Cells, Cultured, Respiratory tract infections, business.industry, Cell Differentiation, T-Lymphocytes, Helper-Inducer, medicine.disease, Germinal Center, Phenotype, Immunity, Humoral, medicine.anatomical_structure, follicular regulatory T cells, Humoral immunity, Blood Circulation, germinal center response, Female, follicular regulatory T cell, business

Abstract

Patients with Down syndrome (DS) are characterized by increased susceptibility to autoimmunity and respiratory tract infections that are suggestive of humoral immunity impairment. Here, we sought to determine the follicular helper (Tfh) and follicular regulatory (Tfr) T cell profile in the blood of children with DS. Blood was collected from 24 children with DS, nine of which had autoimmune diseases. Children with DS showed skewed Tfh differentiation towards the CXCR3+ phenotype: Tfh1 and Tfh1/17 subsets were increased, while Tfh2 and Tfh17 subsets were reduced. While no differences in the percentage of Tfr cells were seen, the ratio of Tfh1 and CXCR3+PD-1+ subsets to Tfr cells was significantly increased in the affected children. The excessive polarization towards a CXCR3+ phenotype in children with DS suggests that re-calibration of Tfh subset skewing could potentially offer new therapeutic opportunities for these patients. Patients with Down syndrome (DS) are characterized by increased susceptibility to autoimmunity and respiratory tract infections that are suggestive of humoral immunity impairment. Here, we sought to determine the follicular helper (Tfh) and follicular regulatory (Tfr) T cell profile in the blood of children with DS. Blood was collected from 24 children with DS, nine of which had autoimmune diseases. Children with DS showed skewed Tfh differentiation towards the CXCR3+ phenotype: Tfh1 and Tfh1/17 subsets were increased, while Tfh2 and Tfh17 subsets were reduced. While no differences in the percentage of Tfr cells were seen, the ratio of Tfh1 and CXCR3+PD-1+ subsets to Tfr cells was significantly increased in the affected children. The excessive polarization towards a CXCR3+ phenotype in children with DS suggests that re-calibration of Tfh subset skewing could potentially offer new therapeutic opportunities for these patients.

Published

2020

21. Tr1 cell immunotherapy promotes transplant tolerance via de novo Tr1 cell induction in mice and is safe and effective during acute viral infection

Author

Georgia Fousteri, Matteo Iannacone, Manuela Battaglia, Giuseppe Galvani, Roberta Di Fonte, Tatiana Jofra, and Mirela Kuka

Subjects

0301 basic medicine, Tr1 cell, Effector, viruses, medicine.medical_treatment, Immunology, Immunotherapy, Biology, Lymphocytic choriomeningitis, medicine.disease, Viral infection, Virus, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine, Immunology and Allergy, Pancreatic islet transplantation, CD8, 030215 immunology

Abstract

Tr1 cell therapy is considered an emerging approach to improve transplant tolerance and enhance allogeneic graft survival. However, it remains unclear how Tr1 cells promote transplant tolerance and whether they will be safe and stable in the face of an acute viral infection. By employing a mouse model of pancreatic islet transplantation, we report that Tr1 cell therapy promoted transplant tolerance via de novo induction of Tr1 cells in the recipients. Acute viral infection with lymphocytic choriomeningitis virus (LCMV) had no impact on Tr1 cell number and function, neither on the Tr1 cells infused nor on the ones induced, and that was reflected in the robust maintenance of the graft. Moreover, Tr1 cell immunotherapy had no detrimental effect on CD8 and CD4 anti-LCMV effector T-cell responses and viral control. Together, these data suggest that Tr1 cells did not convert to effector cells during acute infection with LCMV, maintained transplant tolerance and did not inhibit antiviral immunity.

Published

2018

22. Regulatory T cells from patients with end-stage organ disease can be isolated, expanded and cryopreserved according good manufacturing practice improving their function

Author

Roberto M. Lemoli, Maria Giulia Bacalini, Antonio Curti, Gaetano La Manna, Matteo Cescon, Claudio Franceschi, Cristiana Lavazza, Tatiana Jofra, Valeria Giudice, Antonio Daniele Pinna, Manuela Battaglia, Giorgia Comai, Miriam Capri, Francesca Ulbar, Valentina Rosa Bertuzzo, Mariele Viganò, Paolo Garagnani, Chiara Pirazzini, Lucia Catani, Daria Sollazzo, Alessandra Mandelli, Mario Arpinati, Tiziana Montemurro, Rosaria Giordano, Silvia Budelli, Ulbar F., Montemurro T., Jofra T., Capri M., Comai G., Bertuzzo V., Lavazza C., Mandelli A., Vigano M., Budelli S., Bacalini M.G., Pirazzini C., Garagnani P., Giudice V., Sollazzo D., Curti A., Arpinati M., La Manna G., Cescon M., Pinna A.D., Franceschi C., Battaglia M., Giordano R., Catani L., and Lemoli R.M.

Subjects

Male, 0301 basic medicine, Cell Transplantation, medicine.medical_treatment, lcsh:Medicine, Graft vs Host Disease, Mice, SCID, Liver transplantation, T-Lymphocytes, Regulatory, Cryopreservation, Mice, Liver disease, 0302 clinical medicine, Mice, Inbred NOD, End stage organ disease, Mice, Knockout, Kidney, Liver Diseases, Forkhead Transcription Factors, hemic and immune systems, Regulatory T cells, General Medicine, Middle Aged, Phenotype, medicine.anatomical_structure, 030220 oncology & carcinogenesis, DNA methylation, Female, Immunotherapy, Safety, Adult, chemical and pharmacologic phenomena, General Biochemistry, Genetics and Molecular Biology, End stage renal disease, 03 medical and health sciences, In vivo, medicine, Animals, Humans, Aged, business.industry, Research, lcsh:R, End stage organ disease, Murine model, Regulatory T cells, Safety, DNA Methylation, medicine.disease, In vitro, 030104 developmental biology, Immunology, Kidney Failure, Chronic, Murine model, business, Regulatory T cell

Abstract

Background Here, we isolated, expanded and functionally characterized regulatory T cells (Tregs) from patients with end stage kidney and liver disease, waiting for kidney/liver transplantation (KT/LT), with the aim to establish a suitable method to obtain large numbers of immunomodulatory cells for adoptive immunotherapy post-transplantation. Methods We first established a preclinical protocol for expansion/isolation of Tregs from peripheral blood of LT/KT patients. We then scaled up and optimized such protocol according to good manufacturing practice (GMP) to obtain high numbers of purified Tregs which were phenotypically and functionally characterized in vitro and in vivo in a xenogeneic acute graft-versus-host disease (aGVHD) mouse model. Specifically, immunodepressed mice (NOD-SCID-gamma KO mice) received human effector T cells with or without GMP-produced Tregs to prevent the onset of xenogeneic GVHD. Results Our small scale Treg isolation/expansion protocol generated functional Tregs. Interestingly, cryopreservation/thawing did not impair phenotype/function and DNA methylation pattern of FOXP3 gene of the expanded Tregs. Fully functional Tregs were also isolated/expanded from KT and LT patients according to GMP. In the mouse model, GMP Tregs from LT or KT patient proved to be safe and show a trend toward reduced lethality of acute GVHD. Conclusions These data demonstrate that expanded/thawed GMP-Tregs from patients with end-stage organ disease are fully functional in vitro. Moreover, their infusion is safe and results in a trend toward reduced lethality of acute GVHD in vivo, further supporting Tregs-based adoptive immunotherapy in solid organ transplantation. Electronic supplementary material The online version of this article (10.1186/s12967-019-2004-2) contains supplementary material, which is available to authorized users.

Published

2019

23. Reduced PD-1 expression on circulating follicular and conventional FOXP3

Author

Andrea, Vecchione, Roberta, Di Fonte, Jolanda, Gerosa, Tatiana, Jofra, Maria Pia, Cicalese, Vincenzo, Napoleone, Elio, Ippolito, Giuseppe, Galvani, Francesca, Ragogna, Angela, Stabilini, Eleonora, Bianconi, Pauline, Grogan, Clara, Bonura, Riccardo, Bonfanti, Giulio, Frontino, Rita, Nano, Raffaela, Melzi, Maurizio, De Pellegrin, Andrea, Laurenzi, Franco, Meschi, Graziano, Barera, Andrea, Rigamonti, Rita, Indirli, Emanuele, Bosi, Lorenzo, Piemonti, Alessandro, Aiuti, Manuela, Battaglia, and Georgia, Fousteri

Subjects

Male, Receptors, CXCR5, Adolescent, Programmed Cell Death 1 Receptor, Forkhead Transcription Factors, T-Lymphocytes, Regulatory, Islets of Langerhans, Diabetes Mellitus, Type 1, Mice, Inbred NOD, Child, Preschool, Disease Progression, Animals, Humans, Female, Child, Autoantibodies, Hair

Abstract

Autoantibodies (AAbs) are a hallmark of Type 1 diabetes (T1D). Alterations in the frequency and phenotype of follicular helper (Tfh) T cells have been previously documented in patients with type 1 diabetes (T1D), but the contribution of follicular regulatory T (Treg) cells, which are responsible for suppressing AAb development, is less clear. Here, we investigated the frequency and activation status of follicular (CXCR5

Published

2019

24. POS1356 PERSISTENCE OF TFH CELLS AFTER RITUXIMAB IS ASSOCIATED WITH IGG4-RELATED DISEASE RELAPSE

Author

Gaia Mancuso, Jolanda Gerosa, Lorenzo Dagna, Tatiana Jofra, Georgia Fousteri, G. Di Colo, E. Della Torre, and Marco Lanzillotta

Subjects

medicine.diagnostic_test, business.industry, medicine.drug_class, Immunology, Germinal center, Monoclonal antibody, medicine.disease, Peripheral blood mononuclear cell, General Biochemistry, Genetics and Molecular Biology, Flow cytometry, Rheumatology, Follicular phase, Immunology and Allergy, Medicine, IgG4-related disease, Rituximab, CXCL13, business, medicine.drug

Abstract

Background:Clinical improvement after B-cell depletion with rituxmab suggests a prominent pathogenic role of B-lymphcytes in IgG4-related disease (IgG4-RD). IgG4-RD, however, relapses in most cases together with re-expansion of clonally divergent plasmablasts indicating that treatment with rituximab does not completely abrogates T follicular helper (Tfh)-cells dependent germinal center reactions leading to de-novo plasmablast differentiation.Objectives:In the present work we aim to study the effects of B-cell depletion therapy with rituximab on circulating Tfh cells and on the levels of CXCL13 - a chemotactic factor for B-lymphocytes produced by Tfh cells - in patients with IgG4-RD.Methods:Thirty patients with IgG4-RD, diagnosed according to the “Consensus Statement on the Pathology of IgG4-RD” and fulfilling the “2019 ACR/EULAR Classification Criteria” were included in the present study. Ten patients with relapsing disease were treated with the anti-CD20 monoclonal antibody rituximab (two 1g infuxions 15 days apart). Peripheral blood mononuclear cells and serum were collected before rituximab and three months after infusion. Tfh cells subsets in the peripheral blood were measured by flow cytometry and CXCL13 plasma levels were measured by ELISA assay.Results:No changes in total Tfh cells and Tfh cells subsets were observed three months after rituximab neither in absolute counts nor in percentage of CD4+ T cells. In particular, no difference in Tfh1, Tfh2, Tfh17, T follicular regulatory and highly functional Tfh cells counts was observed before and after treatment. The serum level of CXCL13 was significantly higher in active untreated IgG4-RD patients compared to healthy controls (151.94 pg/ml vs 66.98 pg/ml, p value = 0.0026), but was not affected by rituximab treatment (p value = 0.41).Conclusion:In relapsing patients with IgG4-RD rituximab does not affect circulating Tfh cells numbers and serum levels of CXCL13. Persistence of Tfh cells after rituximab and reconstitution of germinal center reactions likely drives IgG4-RD flare.References:[1]Lanzillotta M, Mancuso G, Della-Torre E. Advances in the diagnosis and management of IgG4 related disease. BMJ. 2020 Jun 16;369:m1067. doi: 10.1136/bmj.m1067. PMID: 32546500.[2]Lanzillotta M, Della-Torre E, Stone JH. Roles of Plasmablasts and B Cells in IgG4-Related Disease: Implications for Therapy and Early Treatment Outcomes. Curr Top Microbiol Immunol. 2017;401:85-92. doi: 10.1007/82_2016_58. PMID: 28091934.[3]Campochiaro C, Ramirez GA, Bozzolo EP, Lanzillotta M, Berti A, Baldissera E, Dagna L, Praderio L, Scotti R, Tresoldi M, Roveri L, Mariani A, Balzano G, Castoldi R, Doglioni C, Sabbadini MG, Della-Torre E. IgG4-related disease in Italy: clinical features and outcomes of a large cohort of patients. Scand J Rheumatol. 2016;45(2):135-45. doi: 10.3109/03009742.2015.1055796. Epub 2015 Sep 23. PMID: 26398142.[4]Mattoo H, Mahajan VS, Della-Torre E, Sekigami Y, Carruthers M, Wallace ZS, Deshpande V, Stone JH, Pillai S. De novo oligoclonal expansions of circulating plasmablasts in active and relapsing IgG4-related disease. J Allergy Clin Immunol. 2014 Sep;134(3):679-87. doi: 10.1016/j.jaci.2014.03.034. Epub 2014 May 6. PMID: 24815737; PMCID: PMC4149918.Disclosure of Interests:None declared

Published

2021

25. Protein tyrosine phosphatase PTPN22 has dual roles in promoting pathogen versus homeostatic‐driven CD8 T‐cell responses

Author

Tarun E. Hutchinson, Farhad Dastmalchi, Giuseppe Galvani, Georgia Fousteri, Shahram Salek-Ardakani, Tatiana Jofra, Manuela Battaglia, and Roberta Di Fonte

Subjects

musculoskeletal diseases, 0301 basic medicine, Immunology, Protein tyrosine phosphatase, CD8-Positive T-Lymphocytes, Lymphocytic Choriomeningitis, Biology, Lymphocyte Activation, 03 medical and health sciences, 0302 clinical medicine, immune system diseases, Interferon, medicine, Animals, Homeostasis, Lymphocytic choriomeningitis virus, Immunology and Allergy, Cytotoxic T cell, IL-2 receptor, Phosphorylation, skin and connective tissue diseases, Cell Proliferation, ZAP70, Protein Tyrosine Phosphatase, Non-Receptor Type 22, Cell Biology, eye diseases, Up-Regulation, Cell biology, Mice, Inbred C57BL, STAT1 Transcription Factor, 030104 developmental biology, Interferon Type I, Cytokines, Signal transduction, Biomarkers, CD8, Signal Transduction, 030215 immunology, medicine.drug

Abstract

PTPN22 (protein tyrosine phosphatase non receptor 22) encodes a tyrosine phosphatase that functions as a key regulator of immune homeostasis. In particular, PTPN22 inhibits T-cell receptor signaling and selectively promotes type I interferon responses in myeloid cells. To date, there is little information on the CD8 T-cell-intrinsic role of PTPN22 in response to a viral pathogen. We unexpectedly found that PTPN22-deficient virus-specific CD8 T cells failed to accumulate in wild-type hosts after lymphocytic choriomeningitis virus infection. Lack of PTPN22 expression altered CD8 T-cell activation and antiviral cytokine production, but did not significantly affect the composition of effector and memory cell precursors. Most significantly, in vivo, PTPN22-deficient CD8 T cells showed a profound defect in upregulating STAT-1 after lymphocytic choriomeningitis virus infection and considerably less phosphorylation of STAT-1 in response to IFN-α treatment in vitro compared with their wild-type counterparts. In stark contrast, following transfer into lymphopenic mice, CD8 T-cell expansion and central-like phenotype, was considerably increased in the absence of PTPN22. Collectively, our results suggest that PTPN22 has dual roles in T-cell clonal expansion and effector function; whereas it promotes antigen-driven responses during acute infection by positively regulating interferon signaling in T cells, PTPN22 inhibits homeostatic-driven proliferation.

Published

2016

26. Tr1 cell immunotherapy promotes transplant tolerance via de novo Tr1 cell induction in mice and is safe and effective during acute viral infection

Author

Tatiana, Jofra, Roberta, Di Fonte, Giuseppe, Galvani, Mirela, Kuka, Matteo, Iannacone, Manuela, Battaglia, Georgia, Fousteri, Jofra, Tatiana, Di Fonte, Roberta, Galvani, Giuseppe, Kuka, Mirela, Iannacone, Matteo, Battaglia, Manuela, and Fousteri, Georgia.

Subjects

Mice, Inbred BALB C, Islets of Langerhans Transplantation, CD8-Positive T-Lymphocytes, Lymphocytic Choriomeningitis, Immunotherapy, Adoptive, T-Lymphocytes, Regulatory, Mice, Inbred C57BL, Islets of Langerhans, Mice, Diabetes Mellitus, Type 1, Models, Animal, Immune Tolerance, Animals, Lymphocytic choriomeningitis virus

Abstract

Tr1 cell therapy is considered an emerging approach to improve transplant tolerance and enhance allogeneic graft survival. However, it remains unclear how Tr1 cells promote transplant tolerance and whether they will be safe and stable in the face of an acute viral infection. By employing a mouse model of pancreatic islet transplantation, we report that Tr1 cell therapy promoted transplant tolerance via de novo induction of Tr1 cells in the recipients. Acute viral infection with lymphocytic choriomeningitis virus (LCMV) had no impact on Tr1 cell number and function, neither on the Tr1 cells infused nor on the ones induced, and that was reflected in the robust maintenance of the graft. Moreover, Tr1 cell immunotherapy had no detrimental effect on CD8 and CD4 anti-LCMV effector T-cell responses and viral control. Together, these data suggest that Tr1 cells did not convert to effector cells during acute infection with LCMV, maintained transplant tolerance and did not inhibit antiviral immunity.

Published

2018

27. Murine Pancreatic Islets Transplantation under the Kidney Capsule

Author

Gregori Silvia, Manuela Battaglia, Tatiana Jofra, Nicola Gagliani, Fousteri Georgia, and Giuseppe Galvani

Subjects

endocrine system, Type 1 diabetes, geography, geography.geographical_feature_category, endocrine system diseases, business.industry, Strategy and Management, Mechanical Engineering, Pancreatic islets, Insulin, medicine.medical_treatment, Metals and Alloys, medicine.disease, Islet, Industrial and Manufacturing Engineering, Transplantation, medicine.anatomical_structure, Methods Article, medicine, Cancer research, Pancreatic islet transplantation, Bone marrow, Pancreas, business

Abstract

Type 1 diabetes (T1D) is an autoimmune disease caused by the lack of insulin-producing pancreatic beta cells leading to systemic hyperglycemia. Pancreatic islet transplantation is a valid therapeutic approach to restore insulin loss and to promote adequate glycemic control. Pancreatic islet transplantation in mice is an optimal preclinical model to identify new therapeutic strategies aiming at preventing rejection and optimizing post-transplant immuno-suppressive/-tolerogenic therapies. Islet transplantation in preclinical animal models can be performed in different sites such the kidney capsule, spleen, bone marrow and pancreas. This protocol describes murine islet transplantation under the kidney capsule. This is a widely accepted procedure for research purposes. Stress caused in the animals is minimal and it leads to reliable and reproducible results.

Published

2017

28. Lack of the protein tyrosine phosphatase PTPN22 strengthens transplant tolerance to pancreatic islets in mice

Author

Cristina Morsiani, Tatiana Jofra, Manuela Battaglia, Roberta Di Fonte, Georgia Fousteri, Nicola Gagliani, Angela Stabilini, Fousteri, Georgia, Jofra, Tatiana, Di Fonte, Roberta, Gagliani, Nicola, Morsiani, Cristina, Stabilini, Angela, and Battaglia, Manuela

Subjects

Blood Glucose, endocrine system diseases, Endocrinology, Diabetes and Metabolism, Islets of Langerhans Transplantation, Autoimmunity, Protein tyrosine phosphatase, medicine.disease_cause, T-Lymphocytes, Regulatory, Mice, Risk Factors, immune system diseases, skin and connective tissue diseases, Mice, Knockout, Mice, Inbred BALB C, Mice, Inbred C3H, FOXP3, Forkhead Transcription Factors, PTPN22, Adoptive Transfer, Tr1 cell, medicine.anatomical_structure, Transplantation Tolerance, Pancreatic islet transplantation, Signal Transduction, musculoskeletal diseases, T cell, Mice, Transgenic, G-CSF, Biology, Islets of Langerhans, Transplant tolerance, Internal Medicine, medicine, Animals, Rapamycin, Alloreactivity, B cell, Animal, Risk Factor, Pancreatic islets, Islets of Langerhan, Protein Tyrosine Phosphatase, Non-Receptor Type 22, Forkhead Transcription Factor, Treg cell, eye diseases, Mice, Inbred C57BL, Immunology

Abstract

Aims/hypothesis: Protein tyrosine phosphatase non-receptor 22 (PTPN22) plays a central role in T cell, B cell and innate immune cell signalling. A genetic variation in Ptpn22 is considered a major risk factor for the development of type 1 diabetes and has been the subject of extensive study. While several reports have addressed how Ptpn22 might predispose to autoimmunity, its involvement in other immune-mediated diseases, such as allograft rejection, has not been explored. Methods: To address a possible function for Ptpn22 in allograft rejection, we used a mouse model of pancreatic islet transplantation. We performed transplant tolerance experiments and determined how PTPN22 shapes tolerance induction and maintenance. Results: Ptpn22−/− recipient mice generate higher numbers of alloreactive T cells after allogeneic pancreatic islet transplantation compared with wild-type (WT) mice, but reject grafts with similar kinetics. This is not only due to their well-documented increase in forkhead box protein P3 (FOXP3)+ T regulatory (Treg) cells but also to the expansion of T regulatory type 1 (Tr1) cells caused by the lack of PTPN22. In addition, a tolerogenic treatment known to induce transplant tolerance in WT mice via Tr1 cell generation is more effective in Ptpn22−/− mice as a consequence of boosting both Tr1 and FOXP3+ Treg cells. Conclusions/interpretation: A lack of PTPN22 strengthens transplant tolerance to pancreatic islets by expanding both FOXP3+ Treg and Tr1 cells. These data suggest that targeting PTPN22 could serve to boost transplant tolerance.

Published

2015

29. Heterogeneous CD3 Expression Levels in Differing T Cell Subsets Correlate with the In Vivo Anti-CD3–Mediated T Cell Modulation

Author

Andrea Valle, Eliane Piaggio, Nicolas Cagnard, Manuela Battaglia, Tatiana Jofra, Angela Stabilini, Nicola Gagliani, Santosh Anand, Giulia Barbagiovanni, Louis Pérol, and Audrey Baeyens

Subjects

CD4-Positive T-Lymphocytes, Male, Adolescent, CD3 Complex, T cell, Immunology, CD8-Positive T-Lymphocytes, Biology, Antibodies, Monoclonal, Humanized, Lymphocyte Depletion, Genetic Heterogeneity, Mice, Young Adult, Interleukin 21, Mice, Inbred NOD, T-Lymphocyte Subsets, Immune Tolerance, medicine, Animals, Humans, Hypoglycemic Agents, Immunologic Factors, Immunology and Allergy, Cytotoxic T cell, IL-2 receptor, Child, Antigen-presenting cell, ZAP70, FOXP3, Forkhead Transcription Factors, Natural killer T cell, Cell biology, Diabetes Mellitus, Type 1, medicine.anatomical_structure, Gene Expression Regulation, Child, Preschool, Female, Signal Transduction

Abstract

The tolerogenic anti-CD3ε monoclonal Abs (anti-CD3) are promising compounds for the treatment of type 1 diabetes. Anti-CD3 administration induces transient T cell depletion both in preclinical and in clinical studies. Notably, the said depletion mainly affects CD4+ but not CD8+ T cells. Moreover, type 1 diabetes reversal in preclinical models is accompanied by the selective expansion of CD4+Foxp3+ T regulatory (Treg) cells, which are fundamental for the long-term maintenance of anti-CD3–mediated tolerance. The mechanisms that lead to this immune-shaping by affecting mainly CD4+ T effector cells while sparing CD4+Foxp3+ Treg cells have still to be fully elucidated. This study shows that CD3 expression levels differ from one T cell subset to another. CD4+Foxp3− T cells contain higher amounts of CD3 molecules than do CD4+Foxp3+ and CD8+ T cells in both mice and humans. The said differences correlate with the anti-CD3–mediated immune resetting that occurs in vivo after anti-CD3 administration in diabetic NOD mice. Additionally, transcriptome analysis demonstrates that CD4+Foxp3+ Treg cells are significantly less responsive than are CD4+Foxp3− T cells to anti-CD3 treatment at a molecular level. Thus, heterogeneity in CD3 expression seems to confer to the various T cell subsets differing susceptibility to the in vivo tolerogenic anti-CD3–mediated modulation. These data shed new light on the molecular mechanism that underlies anti-CD3–mediated immune resetting and thus may open new opportunities to improve this promising treatment.

Published

2015

30. PTPN22 controls virally-induced autoimmune diabetes by modulating cytotoxic T lymphocyte responses in an epitope-specific manner

Author

Mirela Kuka, Tatiana Jofra, Matteo Iannacone, Manuela Battaglia, Roberta Di Fonte, and Georgia Fousteri

Subjects

Male, endocrine system diseases, T cell, Immunology, Epitopes, T-Lymphocyte, Autoimmunity, Spleen, Biology, Lymphocyte Activation, Lymphocytic choriomeningitis, medicine.disease_cause, T-Lymphocytes, Regulatory, Epitope, Diabetes Mellitus, Experimental, Proinflammatory cytokine, Mice, Mice, Inbred NOD, immune system diseases, medicine, Animals, Lymphocytic choriomeningitis virus, Immunology and Allergy, Cytotoxic T cell, Pancreas, Mice, Knockout, Effector, Protein Tyrosine Phosphatase, Non-Receptor Type 22, medicine.disease, Mice, Inbred C57BL, Diabetes Mellitus, Type 1, medicine.anatomical_structure, Female, Lymph Nodes, Immunologic Memory, T-Lymphocytes, Cytotoxic

Abstract

Ptpn22 is one of the most potent autoimmunity predisposing genes and strongly associates with type 1 diabetes (T1D). Previous studies showed that non-obese diabetic mice with reduced expression levels of Ptpn22 are protected from T1D due to increased number of T regulatory (Treg) cells. We report that lack of Ptpn22 exacerbates virally-induced T1D in female rat insulin promoter lymphocytic choriomeningitis virus (RIP-LCMV-GP) mice, while maintaining higher number of Treg cells throughout the antiviral response in the blood and spleen but not in the pancreatic lymph nodes. GP 33–41 -specific pentamer-positive cytotoxic lymphocytes (CTLs) are numerically reduced in the absence of Ptpn22 at the expansion and contraction phase but reach wild-type levels at the memory phase. However, they show similar effector function and even a subtle increase in the production of IL-2. In contrast, NP 396–404 -specific CTLs develop normally at all phases but display enhanced effector function. Lack of Ptpn22 also augments the memory proinflammatory response of GP 61–80 CD4 T cells. Hence, lack of Ptpn22 largely augments antiviral effector T cell responses, suggesting that caution should be taken when targeting Ptpn22 to treat autoimmune diseases where viral infections are considered environmental triggers.

Published

2015

31. Extrinsic Protein Tyrosine Phosphatase Non-Receptor 22 Signals Contribute to CD8 T Cell Exhaustion and Promote Persistence of Chronic Lymphocytic Choriomeningitis Virus Infection

Author

Shahram Salek-Ardakani, Manuela Battaglia, Roberta Di Fonte, Tatiana Jofra, Matteo Iannacone, Georgia Fousteri, Bechara Mfarrej, Mirela Kuka, Giuseppe Galvani, Jofra, Tatiana, Galvani, Giuseppe, Kuka, Mirela, Di Fonte, Roberta, Mfarrej, Bechara G., Iannacone, Matteo, Salek-Ardakani, Shahram, Battaglia, Manuela, and Fousteri, Georgia

Subjects

lcsh:Immunologic diseases. Allergy, musculoskeletal diseases, 0301 basic medicine, Lymphocytic choriomeningitis virus clone 13, endocrine system diseases, Immunology, Population, Protein tyrosine phosphatase, protein tyrosine phosphatase non-receptor 22, Biology, PTPN22, 03 medical and health sciences, Chimera (genetics), 0302 clinical medicine, immune system diseases, Genetic predisposition, Immunology and Allergy, Cytotoxic T cell, skin and connective tissue diseases, education, Receptor, Original Research, T cell exhaustion, education.field_of_study, persistent viral infection, Protein tyrosine phosphatase non-receptor 22, Persistent viral infection, Virology, eye diseases, lymphocytic choriomeningitis virus clone 13, 030104 developmental biology, lcsh:RC581-607, genetic predisposition, CD8, 030215 immunology

Abstract

A genetic variant of the protein tyrosine phosphatase non-receptor 22 (PTPN22) is associated with a wide range of autoimmune diseases; however, the reasons behind its prevalence in the general population remain not completely understood. Recent evidence highlights an important role of autoimmune susceptibility genetic variants in conferring resistance against certain pathogens. In this study, we examined the role of PTPN22 in persistent infection in mice lacking PTPN22 infected with lymphocytic choriomeningitis virus clone 13. We found that lack of PTPN22 in mice resulted in viral clearance 30 days after infection, which was reflected in their reduced weight loss and overall improved health. PTPN22−/− mice exhibited enhanced virus-specific CD8 and CD4 T cell numbers and functionality and reduced exhausted phenotype. Moreover, mixed bone marrow chimera studies demonstrated no differences in virus-specific CD8 T cell accumulation and function between the PTPN22+/+ and PTPN22−/− compartments, showing that the effects of PTPN22 on CD8 T cells are T cell-extrinsic. Together, these findings identify a CD8 T cell-extrinsic role for PTPN22 in weakening early CD8 T cell responses to collectively promote persistence of a chronic viral infection.

Published

2017

32. Transplant Tolerance to Pancreatic Islets Is Initiated in the Graft and Sustained in the Spleen

Author

Adriana Polachini do Valle, Silvia Gregori, Richard A. Flavell, Cristina Morsiani, Mark A. Atkinson, Manuela Battaglia, Masahito Kamanaka, S. Deng, Maria Grazia Roncarolo, Nicola Gagliani, Tatiana Jofra, David M. Rothstein, Angela Stabilini, Gagliani, N, Jofra, T, Valle, A, Stabilini, A, Morsiani, C, Gregori, S, Deng, S, Rothstein, Dm, Atkinson, M, Kamanaka, M, Flavell, Ra, Roncarolo, MARIA GRAZIA, Battaglia, MARCO MARIA, N. Gagliani, T. Jofra, A. Valle, A. Stabilini, C. Morsiani, S. Gregori, S. Deng, D. M. Rothstein, M. Atkinson, M. Kamanaka, R. A. Flavell, M. G. Roncarolo, and M. Battaglia

Subjects

CD4-Positive T-Lymphocytes, Cell type, Adoptive cell transfer, Allogeneic transplantation, Islets of Langerhans Transplantation, chemical and pharmacologic phenomena, Spleen, T-Lymphocytes, Regulatory, Graft, Islets of Langerhans, Mice, Immune system, medicine, Animals, Transplantation, Homologous, Immunology and Allergy, Pharmacology (medical), Mice, Inbred BALB C, Transplantation, business.industry, Pancreatic islets, Graft Survival, Allograft Tolerance, Antibodies, Monoclonal, FOXP3, Forkhead Transcription Factors, hemic and immune systems, T REGULATORY CELLS, Adoptive Transfer, Mice, Inbred C57BL, transplant tolerance, medicine.anatomical_structure, CD4 Antigens, Immunology, Leukocyte Common Antigens, Transplantation Tolerance, spleen, business

Abstract

The immune system is comprised of several CD4(+) T regulatory (Treg) cell types, of which two, the Foxp3(+) Treg and T regulatory type 1 (Tr1) cells, have frequently been associated with transplant tolerance. However, whether and how these two Treg-cell types synergize to promote allograft tolerance remains unknown. We previously developed a mouse model of allogeneic transplantation in which a specific immunomodulatory treatment leads to transplant tolerance through both Foxp3(+) Treg and Tr1 cells. Here, we show that Foxp3(+) Treg cells exert their regulatory function within the allograft and initiate engraftment locally and in a non-antigen (Ag) specific manner. Whereas CD4(+) CD25(-) T cells, which contain Tr1 cells, act from the spleen and are key to the maintenance of long-term tolerance. Importantly, the role of Foxp3(+) Treg and Tr1 cells is not redundant once they are simultaneously expanded/induced in the same host. Moreover, our data show that long-term tolerance induced by Foxp3(+) Treg-cell transfer is sustained by splenic Tr1 cells and functionally moves from the allograft to the spleen.

Published

2013

33. Transplant Site Influences the Immune Response After Islet Transplantation: Bone Marrow Versus Liver

Author

Antonio Citro, Elisa Cantarelli, Georgia Fousteri, Anna Mondino, Alessia Mercalli, Raffaella Melzi, Lorenzo Piemonti, Erica Dugnani, Tatiana Jofra, Silvia Pellegrini, Pathology/molecular and cellular medicine, Cantarelli, E., Citro, A., Pellegrini, S., Mercalli, A., Melzi, R., Dugnani, E., Jofra, T., Fousteri, G., Mondino, A., and Piemonti, Lorenzo

Subjects

0301 basic medicine, Liver surgery, Graft Rejection, Male, Isoantigens, T-Lymphocytes, Islets of Langerhans Transplantation, Adaptive Immunity, Isoantibodies, 03 medical and health sciences, Mice, Immune system, Bone Marrow, medicine, Journal Article, Animals, Comparative Study, Liver immunology, Transplantation, geography, Mice, Inbred BALB C, geography.geographical_feature_category, business.industry, Acquired immune system, Islet, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Liver, Immunology, Drug Therapy, Combination, Bone marrow, business, Biomarkers, Immunosuppressive Agents

Abstract

Background. The aim of this study was to characterize the immune response against intrabone marrow (BM-Tx) or intraliver (liver-Tx) transplanted islets in the presence or in the absence of immunosuppression. Methods. Less (C57BL/6 in Balb/c) and highly (Balb/c in C57BL/6) stringent major histocompatibility complex fully mismatched mouse models were used to evaluate the alloimmune response. Single antigen-mismatched mouse model (C57BL/6 RIP-GP in C57BL/6) was used to evaluate the antigen-specific immune response.Mice received tacrolimus (FK-506, 0.1mg/kg per day)/mycophenolate mofetil (MMF, 60mg/kg per day), and anti-CD3 (50 ?g/day) either alone or in combination. Results. Transplant site did not impact the timing nor the kinetics of the alloimmune and single antigen-specificmemory Tcell responses in the absence of immunosuppression or in the presence of MMF/FK-506 combination. On the other hand, the median time to graft rejection was 28 ± 5.2 days and 16 ± 2.6 days (P = 0.14) in the presence of anti-CD3 treatment, 50 ± 12.5 days and 10 ± 1.3 days (P = 0.003) in the presence of anti-CD3/ MMF/FK-506 treatment for liver-Tx and BM-Tx, respectively. Anti-CD3 did not differentially reach BM and liver tissues but was more effective in reducing graft associated Tcell responses in liver-Tx than in BM-Tx. Conclusions. Islets infused in the BM appear less protected from the adaptive immune response in the presence of the anti-CD3 treatment. This result raises some concerns over the potential of the BM as a site for islet allotransplantation. Copyright © 2017 Wolters Kluwer Health, Inc. All rights reserved.

Published

2016

34. Antigen-Specific Dependence of Tr1-Cell Therapy in Preclinical Models of Islet Transplant

Author

Manuela Battaglia, Angela Stabilini, Maria Grazia Roncarolo, Mark A. Atkinson, Tatiana Jofra, Andrea Valle, Nicola Gagliani, Gagliani, N, Jofra, T, Stabilini, A, Valle, A, Atkinson, M, Roncarolo, MARIA GRAZIA, and Battaglia, MARCO MARIA

Subjects

Blood Glucose, CD4-Positive T-Lymphocytes, Graft Rejection, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Islets of Langerhans Transplantation, Enzyme-Linked Immunosorbent Assay, Biology, T-Lymphocytes, Regulatory, Diabetes Mellitus, Experimental, Cell therapy, Mice, Antigen, Internal Medicine, medicine, Animals, Type 1 diabetes, geography, Mice, Inbred BALB C, Mice, Inbred C3H, geography.geographical_feature_category, Immunosuppression, medicine.disease, Islet, Rats, Transplantation, Mice, Inbred C57BL, Disease Models, Animal, Immunology, CD4 Antigens, Experimental pathology, Pancreatic islet transplantation, Original Article, Female, Immunology and Transplantation

Abstract

OBJECTIVE In type 1 diabetes, allogeneic pancreatic islet transplant restores insulin production, but life-threatening immunosuppression is required to avoid graft rejection. Induction of antigen (Ag)–specific tolerance by cell therapy with regulatory T-cells (Tregs) represents an attractive alternative approach but its therapeutic efficacy in islet transplant remains to be determined. Among the different subsets of CD4+ Tregs, the T inducible regulatory type 1 (Tr1) cells can be generated from naive T-cells in the presence of interleukin-10 (IL-10) and represent one promising therapeutic choice. This study was designed to define the efficacy of Tr1-cell therapy in preclinical models of islet transplant. RESEARCH DESIGN AND METHODS Non–Ag-specific polyclonal Tr1 cells and donor Ag-specific Tr1 cells were transferred, in the absence of any pharmacological treatment, in two distinct mouse models of islet transplant. The two models differed in their therapeutic stringency, based on the mean rejection time of untreated mice that underwent a transplant. RESULTS Transfer of polyclonal Tr1 cells engendered graft tolerance only in the nonstringent mouse model. Conversely, cell therapy with Ag-specific Tr1 cells induced an IL-10–dependent tolerance in the stringent mouse model of islet transplant. The therapeutic advantage of Ag-specific Tr1 cells over polyclonal Tr1 cells was due to their donor Ag specificity. CONCLUSIONS These results demonstrate that Tr1-cell therapy leads to tolerance in settings of islet transplant and that its therapeutic efficacy is highly dependent on the antigen specificity of these cells.

Published

2009

35. Rapamycin Prevents and Breaks the Anti-CD3–Induced Tolerance in NOD Mice

Author

Manuela Battaglia, Mark A. Atkinson, Tatiana Jofra, Angela Stabilini, Maria Grazia Roncarolo, Andrea Valle, Valle, A, Jofra, T, Stabilini, A, Atkinson, M, Roncarolo, MARIA GRAZIA, and Battaglia, MARCO MARIA

Subjects

Blood Glucose, CD3 Complex, Ratón, Endocrinology, Diabetes and Metabolism, Disease, Biology, Antibodies, Immune tolerance, Therapeutic approach, Mice, Mice, Inbred NOD, Diabetes mellitus, Internal Medicine, medicine, Immune Tolerance, Animals, NOD mice, Sirolimus, Type 1 diabetes, Brief Report, medicine.disease, Disease Models, Animal, Diabetes Mellitus, Type 1, Immunology, Female, Immunology and Transplantation, Immunosuppressive Agents, medicine.drug

Abstract

OBJECTIVE Non–Fc-binding anti-CD3–specific antibodies represent a promising therapy for preserving C-peptide production in subjects with recent-onset type 1 diabetes. However, the mechanisms by which anti-CD3 exerts its beneficial effect are still poorly understood, and it is questionable whether this therapeutic approach will prove durable with regard to its ability to impart metabolic preservation without additional actions designed to maintain immunological tolerance. We used the NOD mouse model to test whether rapamycin, a compound well-known for its immunomodulatory activity in mice and humans, could increase the therapeutic effectiveness of anti-CD3 treatment in type 1 diabetes. RESEARCH DESIGN AND METHODS Rapamycin was administered to diabetic NOD mice simultaneously with anti-CD3 or to NOD mice cured by anti-CD3 therapy. The ability of this combined therapy to revert type 1 diabetes and maintain a state of long-term tolerance was monitored and compared with that of anti-CD3 therapy alone. RESULTS Rapamycin inhibited the ability of anti-CD3 to revert disease without affecting the frequency/phenotype of T-cells. Rapamycin also reinstated diabetes in mice whose disease was previously reversed by anti-CD3. Withdrawal of rapamycin in these latter animals promptly restored a normoglycemic state. CONCLUSIONS Our findings indicate that, when combined with anti-CD3, rapamycin exerts a detrimental effect on the disease outcome in NOD mice for as long as it is administered. These results suggest strong caution with regard to combining these treatments in type 1 diabetic patients.

Published

2009

36. Combination of an Antigen-Specific Therapy and an Immunomodulatory Treatment to Simultaneous Block Recurrent Autoimmunity and Alloreactivity in Non-Obese Diabetic Mice

Author

Manuela Battaglia, Roberta Di Fonte, Georgia Fousteri, and Tatiana Jofra

Subjects

Graft Rejection, endocrine system, medicine.medical_treatment, Islets of Langerhans Transplantation, lcsh:Medicine, Autoimmunity, Nod, medicine.disease_cause, Immunomodulation, Mice, Inbred NOD, Granulocyte Colony-Stimulating Factor, medicine, Animals, IL-2 receptor, lcsh:Science, NOD mice, Sirolimus, geography, Mice, Inbred BALB C, Multidisciplinary, geography.geographical_feature_category, business.industry, lcsh:R, Immunotherapy, medicine.disease, Islet, Transplant rejection, Transplantation, Immunology, lcsh:Q, Immunization, business, Immunosuppressive Agents, Research Article

Abstract

Restoration of endogenous insulin production by islet transplantation is considered a curative option for patients with type 1 diabetes. However, recurrent autoimmunity and alloreactivity cause graft rejection hindering successful transplantation. Here we tested whether transplant tolerance to allogeneic islets could be achieved in non-obese diabetic (NOD) mice by simultaneously tackling autoimmunity via antigen-specific immunization, and alloreactivity via granulocyte colony stimulating factor (G-CSF) and rapamycin (RAPA) treatment. Immunization with insB9-23 peptide alone or in combination with two islet peptides (IGRP206-214 and GAD524-543) in incomplete Freund's adjuvant (IFA) were tested for promoting syngeneic pancreatic islet engraftment in spontaneously diabetic NOD mice. Treatment with G-CSF/RAPA alone or in combination with insB9-23/IFA was examined for promoting allogeneic islet engraftment in the same mouse model. InsB9-23/IFA immunization significantly prolonged syngeneic pancreatic islet survival in NOD mice by a mechanism that necessitated the presence of CD4+CD25+ T regulatory (Treg) cells, while combination of three islet epitopes was less efficacious in controlling recurrent autoimmunity. G-CSF/RAPA treatment was unable to reverse T1D or control recurrent autoimmunity but significantly prolonged islet allograft survival in NOD mice. Blockade of interleukin-10 (IL-10) during G-CSF/RAPA treatment resulted in allograft rejection suggesting that IL-10-producing cells were fundamental to achieve transplant tolerance. G-CSF/RAPA treatment combined with insB9-23/IFA did not further increase the survival of allogeneic islets. Thus, insB9-23/IFA immunization controls recurrent autoimmunity and G-CSF/RAPA treatment limits alloreactivity, however their combination does not further promote allogeneic pancreatic islet engraftment in NOD mice.

Published

2015

37. Immune Depletion in Combination with Allogeneic Islets Permanently Restores Tolerance to Self-Antigens in Diabetic NOD Mice

Author

Mark A. Atkinson, Tatiana Jofra, Nicola Gagliani, Amanda L. Posgai, and Manuela Battaglia

Subjects

medicine.medical_specialty, medicine.medical_treatment, lcsh:Medicine, Nod, Biology, Autoantigens, Immune tolerance, Mice, Mice, Inbred NOD, Insulin-Secreting Cells, Internal medicine, Diabetes mellitus, Immune Tolerance, medicine, Animals, Humans, Insulin, Transplantation, Homologous, Glucose homeostasis, lcsh:Science, Antilymphocyte Serum, NOD mice, Type 1 diabetes, geography, Multidisciplinary, geography.geographical_feature_category, lcsh:R, Antibodies, Monoclonal, medicine.disease, Islet, Diabetes Mellitus, Type 1, Glucose, Endocrinology, Immunology, lcsh:Q, Research Article

Abstract

The destruction of beta cells in type 1 diabetes (T1D) results in loss of insulin production and glucose homeostasis. Treatment of non-obese diabetic (NOD) mice with immune-depleting/modulating agents (e.g., anti-CD3, murine anti-thymocyte-globulin (mATG)) can lead to diabetes reversal. However, for preclinical studies with these and other agents seeking to reverse disease at onset, the necessity for exogenous insulin administration is debated. Spontaneously diabetic NOD mice were treated with a short-course of mATG and insulin provided as drug therapy or by way of allogeneic islet implants. Herein we demonstrate that exogenous insulin administration is required to achieve disease reversal with mATG in NOD mice. Unexpectedly, we also observed that provision of insulin by way of allogeneic islet implantation in combination with mATG leads to a pronounced reversal of diabetes as well as restoration of tolerance to self-islets. Expansion/induction of regulatory cells was observed in NOD mice stably cured with mATG and allogeneic islets. These data suggest that transient provision of allogeneic insulin-producing islets might provide a temporary window for immune depletion to be more effective and instilling stable tolerance to endogenous beta cells. These findings support the use of a never before explored approach for preserving beta cell function in patients with recent onset T1D.

Published

2015

38. The protein tyrosine phosphatase PTPN22 controls forkhead box protein 3 T regulatory cell induction but is dispensable for T helper type 1 cell polarization

Author

Nunzio Bottini, Andrea Laurenzi, Stephanie M. Stanford, Tatiana Jofra, Manuela Battaglia, Georgia Fousteri, and I. Debernardis

Subjects

CD4-Positive T-Lymphocytes, Immunology, Receptors, Antigen, T-Cell, chemical and pharmacologic phenomena, Biology, T-Lymphocytes, Regulatory, Interleukin 21, Mice, Immunology and Allergy, Cytotoxic T cell, Animals, Humans, IL-2 receptor, Antigen-presenting cell, Mice, Knockout, CD40, ZAP70, hemic and immune systems, Cell Differentiation, Forkhead Transcription Factors, Protein Tyrosine Phosphatase, Non-Receptor Type 22, Original Articles, Th1 Cells, Natural killer T cell, Cell biology, Mice, Inbred C57BL, biology.protein, CD8

Abstract

Summary Protein tyrosine phosphatases (PTPs) regulate T cell receptor (TCR) signalling and thus have a role in T cell differentiation. Here we tested whether the autoimmune predisposing gene PTPN22 encoding for a PTP that inhibits TCR signalling affects the generation of forkhead box protein 3 (FoxP3)+ T regulatory (Treg) cells and T helper type 1 (Th1) cells. Murine CD4+ T cells isolated from Ptpn22 knock-out (Ptpn22 KO) mice cultured in Treg cell polarizing conditions showed increased sensitivity to TCR activation compared to wild-type (WT) cells, and subsequently reduced FoxP3 expression at optimal-to-high levels of activation. However, at lower levels of TCR activation, Ptpn22 KO CD4+ T cells showed enhanced expression of FoxP3. Similar experiments in humans revealed that at optimal levels of TCR activation PTPN22 knock-down by specific oligonucleotides compromises the differentiation of naive CD4+ T cells into Treg cells. Notably, in vivo Treg cell conversion experiments in mice showed delayed kinetic but overall increased frequency and number of Treg cells in the absence of Ptpn22. In contrast, the in vitro and in vivo generation of Th1 cells was comparable between WT and Ptpn22 KO mice, thus suggesting PTPN22 as a FoxP3-specific regulating factor. Together, these results propose PTPN22 as a key factor in setting the proper threshold for FoxP3+ Treg cell differentiation.

Published

2014

39. Reply to Comment on 'Stability of human rapamycin-expanded CD4(+)CD25(+) T-regulatory cells' Haematologica 2011;96(9):1357-65

Author

Andrea Valle, Maria Grazia Roncarolo, Eleonora Tresoldi, Attilio Bondanza, Nicola Gagliani, Ilaria Dell’Albani, Manuela Battaglia, Tatiana Jofra, Angela Stabilini, Tresoldi, E, Dell'Albani, I, Stabilini, A, Jofra, T, Valle, A, Gagliani, N, Bondanza, Attilio, Roncarolo, MARIA GRAZIA, and Battaglia, MARCO MARIA

Subjects

Cd4 cd25, Online-Only Articles, Stability (learning theory), Hematology, Psychology, Neuroscience, Treg cell

Abstract

We have read the letter by He and Lv[1][1] and we think the issues raised by the authors are not pertinent to our published work. Specifically, He and Lv raise three issues. 1. They claim that we cannot conclude from our study that rapamycin has an intrinsic role in the stability of Treg cells. We

Published

2012

40. Rapamycin combined with anti-CD45RB mAb and IL-10 or with G-CSF induces tolerance in a stringent mouse model of islet transplantation

Author

David M. Rothstein, Maria Grazia Roncarolo, Andrea Valle, Nicola Gagliani, Manuela Battaglia, Angela Stabilini, Tatiana Jofra, Mark A. Atkinson, Silvia Gregori, Gagliani, N, Gregori, S, Jofra, T, Valle, A, Stabilini, A, Rothstein, Dm, Atkinson, M, Roncarolo, MARIA GRAZIA, and Battaglia, MARCO MARIA

Subjects

Time Factors, Mouse, Islets of Langerhans Transplantation, lcsh:Medicine, T-Lymphocytes, Regulatory, Immune tolerance, Epitopes, Mice, Granulocyte Colony-Stimulating Factor, lcsh:Science, Immune Response, Mice, Inbred BALB C, Multidisciplinary, T Cells, FOXP3, Antibodies, Monoclonal, Forkhead Transcription Factors, Animal Models, Transplant rejection, Interleukin-10, Interleukin 10, medicine.anatomical_structure, CD4 Antigens, Models, Animal, Medicine, Drug Therapy, Combination, Female, medicine.drug, Research Article, Immune Cells, Immunology, Spleen, Biology, Microbiology, Model Organisms, medicine, Immune Tolerance, Animals, Humans, Transplantation, Homologous, Sirolimus, Transplantation, Pancreatic islets, lcsh:R, Interleukin-2 Receptor alpha Subunit, Immunity, Immunoregulation, Immunologic Subspecialties, medicine.disease, Mice, Inbred C57BL, Cancer research, Leukocyte Common Antigens, lcsh:Q, Clinical Immunology

Abstract

Background: A large pool of preexisting alloreactive effector T cells can cause allogeneic graft rejection following transplantation. However, it is possible to induce transplant tolerance by altering the balance between effector and regulatory T (Treg) cells. Among the various Treg-cell types, Foxp3 +Treg and IL-10-producing T regulatory type 1 (Tr1) cells have frequently been associated with tolerance following transplantation in both mice and humans. Previously, we demonstrated that rapamycin+IL-10 promotes Tr1-cell-associated tolerance in Balb/c mice transplanted with C57BL/6 pancreatic islets. However, this same treatment was unsuccessful in C57BL/6 mice transplanted with Balb/c islets (classified as a stringent transplant model). We accordingly designed a protocol that would be effective in the latter transplant model by simultaneously depleting effector T cells and fostering production of Treg cells. We additionally developed and tested a clinically translatable protocol that used no depleting agent. Methodology/Principal Findings: Diabetic C57BL/6 mice were transplanted with Balb/c pancreatic islets. Recipient mice transiently treated with anti-CD45RB mAb+rapamycin+IL-10 developed antigen-specific tolerance. During treatment, Foxp3 +Treg cells were momentarily enriched in the blood, followed by accumulation in the graft and draining lymph node, whereas CD4 +IL-10 +IL-4 - T (i.e., Tr1) cells localized in the spleen. In long-term tolerant mice, only CD4 +IL-10 +IL-4 - T cells remained enriched in the spleen and IL-10 was key in the maintenance of tolerance. Alternatively, recipient mice were treated with two compounds routinely used in the clinic (namely, rapamycin and G-CSF); this drug combination promoted tolerance associated with CD4 +IL-10 +IL-4 - T cells. Conclusions/Significance: The anti-CD45RB mAb+rapamycin+IL-10 combined protocol promotes a state of tolerance that is IL-10 dependent. Moreover, the combination of rapamycin+G-CSF induces tolerance and such treatment could be readily translatable into the clinic. © 2011 Gagliani et al.

Published

2011

41. A New Combined Therapy (anti-CD45RB mAb + rapamycin + IL-10) Able to Induce Active Long-term Tolerance in a Stringent Pre-clinical Model of Allogeneic Islet Transplantation

Author

Manuela Battaglia, Tatiana Jofra, Silvia Gregori, Nicola Gagliani, and Maria Grazia Roncarolo

Subjects

geography, geography.geographical_feature_category, business.industry, medicine.drug_class, Immunology, Monoclonal antibody, Islet, Transplantation, Interleukin 10, Immunology and Allergy, Combined therapy, Medicine, business

Published

2008

42. Bone Marrow Versus Liver

Author

Elisa Cantarelli, Antonio Citro, Silvia Pellegrini, Alessia Mercalli, Raffaella Melzi, Erica Dugnani, Tatiana Jofra, Georgia Fousteri, Anna Mondino, and Lorenzo Piemonti