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1. Long-term follow-up of IPEX syndrome patients after different therapeutic strategies: An international multicenter retrospective study

Author

Barzaghi, F., Hernandez, L.C.A., Neven, B., Ricci, S., Kucuk, Z.Y., Bleesing, J.J., Nademi, Z., Slatter, M.A., Ulloa, E.R., Shcherbina, A., Roppelt, A., Worth, A., Silva, J., Aiuti, A., Murguia-Favela, L., Speckmann, C., Carneiro-Sampaio, M., Fernandes, J.F., Baris, S., Ozen, A., Karakoc-Aydiner, E., Kiykim, A., Schulz, A., Steinmann, S., Notarangelo, L.D., Gambineri, E., Lionetti, P., Shearer, W.T., Forbes, L.R., Martinez, C., Moshous, D., Blanche, S., Fisher, A., Ruemmele, F.M., Tissandier, C., Ouachee-Chardin, M., Rieux-Laucat, F., Cavazzana, M., Qasim, W., Lucarelli, B., Albert, M.H., Kobayashi, I., Alonso, L., Heredia, C.D. de, Kanegane, H., Lawitschka, A., Seo, J.J., Gonzalez-Vicent, M., Diaz, M.A., Goyal, R.K., Sauer, M.G., Yesilipek, A., Kim, M., Yilmaz-Demirdag, Y., Bhatia, M., Khlevner, J., Padilla, E.J.R., Martino, S., Montin, D., Neth, O., Molinos-Quintana, A., Valverde-Fernandez, J., Broides, A., Pinsk, V., Ballauf, A., Haerynck, F., Bordon, V., Dhooge, C., Garcia-Lloret, M.L., Bredius, R.G., Kawak, K., Haddad, E., Seidel, M.G., Duckers, G., Pai, S.Y., Dvorak, C.C., Ehl, S., Locatelli, F., Goldman, F., Gennery, A.R., Cowan, M.J., Roncarolo, M.G., Bacchetta, R., PIDTC, IEWP, European Soc Blood Marrow, Barzaghi, Federica, Hernandez, Laura Cristina Amaya, Neven, Benedicte, Ricci, Silvia, Kucuk, Zeynep Yesim, Bleesing, Jack J., Nademi, Zohreh, Slatter, Mary Anne, Ulloa, Erlinda Rose, Shcherbina, Anna, Roppelt, Anna, Worth, Austen, Silva, Juliana, Aiuti, Alessandro, Murguia-Favela, Luis, Speckmann, Carsten, Carneiro-Sampaio, Magda, Fernandes, Juliana Folloni, Baris, Safa, Ozen, Ahmet, Karakoc-Aydiner, Elif, Kiykim, Ayca, Schulz, Ansgar, Steinmann, Sandra, Notarangelo, Lucia Dora, Gambineri, Eleonora, Lionetti, Paolo, Shearer, William Thomas, Forbes, Lisa R., Martinez, Caridad, Moshous, Despina, Blanche, Stephane, Fisher, Alain, Ruemmele, Frank M., Tissandier, Come, Ouachee-Chardin, Marie, Rieux-Laucat, Frederic, Cavazzana, Marina, Qasim, Waseem, Lucarelli, Barbarella, Albert, Michael H., Kobayashi, Ichiro, Alonso, Laura, De Heredia, Cristina Diaz, Kanegane, Hirokazu, Lawitschka, Anita, Seo, Jong Jin, Gonzalez-Vicent, Marta, Diaz, Miguel Angel, Goyal, Rakesh Kumar, Sauer, Martin G., Yesilipek, Akif, Kim, Minsoo, Yilmaz-Demirdag, Yesim, Bhatia, Monica, Khlevner, Julie, Padilla, Erick J. Richmond, Martino, Silvana, Montin, Davide, Neth, Olaf, Molinos-Quintana, Agueda, Valverde-Fernandez, Justo, Broides, Arnon, Pinsk, Vered, Ballauf, Antje, Haerynck, Filomeen, Bordon, Victoria, Dhooge, Catharina, Garcia-Lloret, Maria Laura, Bredius, Robbert G., Kalwak, Krzysztof, Haddad, Elie, Seidel, Markus Gerhard, Duckers, Gregor, Pai, Sung-Yun, Dvorak, Christopher C., Ehl, Stephan, Locatelli, Franco, Goldman, Frederick, Gennery, Andrew Richard, Cowan, Mort J., Roncarolo, Maria-Grazia, Bacchetta, Rosa, Amaya Hernandez, Laura Cristina, Murguia-Favela, Lui, Shearer, William Thoma, Rieux-Laucat, Frédéric, Diaz De Heredia, Cristina, Richmond Padilla, Erick J., and Kałwak, Krzysztof

Subjects
0301 basic medicine, Male, Allergy, medicine.medical_treatment, Medizin, Disease, Hematopoietic stem cell transplantation, SIROLIMUS, Regenerative Medicine, primary immune deficiency, Medicine and Health Sciences, IPEX, Immunology and Allergy, 2.1 Biological and endogenous factors, Enteropathy, Aetiology, POLYENDOCRINOPATHY, Child, Pediatric, CÉLULAS-TRONCO, immunosuppression, Hematopoietic Stem Cell Transplantation, Genetic Diseases, X-Linked, Immunosuppression, Forkhead Transcription Factors, X-LINKED SYNDROME, Allografts, Survival Rate, surgical procedures, operative, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Immune System Diseases, Genetic Diseases, Child, Preschool, hematopoietic stem cell transplantation, Female, hematopoietic stem, neonatal diabetes, FOXP3, Primary Immune Deficiency, Treg cells, enteropathy, genetic autoimmunity, rapamycin, Type 1, Diarrhea, Adult, medicine.medical_specialty, Adolescent, Immunology, Neonatal onset, Article, Disease-Free Survival, 03 medical and health sciences, Neonatal diabete, Clinical Research, Internal medicine, IMMUNODYSREGULATION, medicine, Primary Immune Deficiency Treatment Consortium (PIDTC) and the Inborn Errors Working Party (IEWP) of the European Society for Blood and Marrow Transplantation, Diabetes Mellitus, Genetics, Humans, REGULATORY T-CELLS, cell transplantation, Preschool, Retrospective Studies, Immunosuppression Therapy, Transplantation, IMMUNE DYSREGULATION, business.industry, MUTATIONS, Infant, Retrospective cohort study, STEM-CELL TRANSPLANTATION, IPEX syndrome, X-Linked, medicine.disease, Stem Cell Research, BONE-MARROW-TRANSPLANTATION, Treg cell, FOXP3 MUTATIONS, Diabetes Mellitus, Type 1, 030104 developmental biology, ENGRAFTMENT, Mutation, business, Follow-Up Studies
Abstract

Background Immunodysregulation polyendocrinopathy enteropathy x-linked(IPEX) syndromeis a monogenic autoimmune disease caused by FOXP3 mutations. Because it is a rare disease, the natural history and response to treatments, including allogeneic hematopoietic stem cell transplantation (HSCT) and immunosuppression (IS), have not been thoroughly examined. Objective This analysis sought to evaluate disease onset, progression, and long-term outcome of the 2 main treatments in long-term IPEX survivors. Methods Clinical histories of 96 patients with a genetically proven IPEX syndrome were collected from 38 institutions worldwide and retrospectively analyzed. To investigate possible factors suitable to predict the outcome, an organ involvement (OI) scoring system was developed. Results We confirm neonatal onset with enteropathy, type 1 diabetes, and eczema. In addition, we found less common manifestations in delayed onset patients or during disease evolution. There is no correlation between the site of mutation and the disease course or outcome, and the same genotype can present with variable phenotypes. HSCT patients (n = 58) had a median follow-up of 2.7 years (range, 1 week-15 years). Patients receiving chronic IS (n = 34) had a median follow-up of 4 years (range, 2 months-25 years). The overall survival after HSCT was 73.2% (95% CI, 59.4-83.0) and after IS was 65.1% (95% CI, 62.8-95.8). The pretreatment OI score was the only significant predictor of overall survival after transplant (P = .035) but not under IS. Conclusions Patients receiving chronic IS were hampered by disease recurrence or complications, impacting long-term disease-free survival. When performed in patients with a low OI score, HSCT resulted in disease resolution with better quality of life, independent of age, donor source, or conditioning regimen., GRAPHICAL ABSTRACT

Published
2018

2. Clinical features and follow-up in patients with 22q11.2 deletion syndrome

Author

Cancrini, C, Puliafito, P, Digilio, M, Soresina, A, Martino, S, Rondelli, R, Consolini, R, Ruga, E, Cardinale, F, Finocchi, A, Romiti, Ml, Martire, B, Bacchetta, R, Albano, V, Carotti, A, Specchia, F, Montin, D, Cirillo, E, Cocchi, G, Trizzino, A, Bossi, G, Milanesi, O, Azzari, C, Corsello, G, Pignata, C, Aiuti, A, Pietrogrande, M, Marino, B, Ugazio, A, Plebani, A, Rossi, P, Pierani, P, Gabrielli, A, Danieli, M, De Mattia, D, Sisto, C, Dammacco, F, Ranieri, G, Pession, A, Ricci, G, Minelli, P, Lougaris, V, Badolato, R, Cattaneo, R, Airò, P, Mura, R, Cossu, F, Del Giacco, S, Manconi, P, Consarino, C, Dello Russo, A, Miniero, R, Anastasio, E, Marino, S, Russo, G, Paganelli, R, Sperlì, D, Carpino, L, Aricò, M, Gambineri, E, Lippi, F, Canessa, C, Maggi, E, Romagnani, S, Matucci, A, Vultaggio, A, Gattorno, M, Castagnola, E, Nigro, G, Presta, G, Civino, A, Buzi, F, Gambaretto, G, Fasoli, S, Salpietro, C, Gallizzi, R, Dellepiane, R, Panisi, C, Fabio, G, Carrabba, M, Roncarolo, M, Biondi, A, Vallinoto, C, Poggi, V, Menna, G, Di Nardo, R, Sottile, R, Marone, G, Spadaro, G, Carli, M, Basso, G, Putti, C, Semenzato, G, Agostini, C, D'Angelo, P, Izzi, G, Bertolini, P, Zecca, M, Marseglia, G, Maccario, R, Felici, L, Favre, C, Vecchi, V, Sacchini, P, Rinaldi, G, Livadiotti, S, Simonetti, A, Stabile, A, Duse, M, Iacobini, M, Quinti, I, Fiorilli, M, Moschese, V, Cecere, F, D'Ambrosio, A, De Zan, G, Strafella, S, Tamaro, P, Rabusin, M, Tommasini, A, Tovo, P, De Carli, M, De Carli, S, Nespoli, L, Marinoni, M, Porcellini, A, Lunardi, C, Patuzzo, G, Boner, A, Degani, D, Cancrini, C, Puliafito, P, Digilio, Mc, Soresina, A, Martino, S, Rondelli, R, Consolini, R, Ruga, Em, Cardinale, F, Finocchi, A, Romiti, Ml, Martire, B, Bacchetta, R, Albano, V, Carotti, A, Specchia, F, Montin, D, Cirillo, E, Cocchi, G, Trizzino, A, Bossi, G, Milanesi, O, Azzari, C, Corsello, G, Pignata, C, Aiuti, Alessandro, Pietrogrande, Mc, Marino, B, Ugazio, Ag, Plebani, A, Rossi, P., Cancrini, Caterina, Puliafito, Pamela, Digilio, Maria Cristina, Soresina, Annarosa, Martino, Silvana, Rondelli, Roberto, Consolini, Rita, Ruga, Ezia Maria, Cardinale, Fabio, Finocchi, Andrea, Romiti, Maria Luisa, Martire, Baldassarre, Bacchetta, Rosa, Albano, Veronica, Carotti, Adriano, Specchia, Fernando, Montin, Davide, Cirillo, Emilia, Cocchi, Guido, Trizzino, Antonino, Bossi, Grazia, Milanesi, Ornella, Azzari, Chiara, Corsello, Giovanni, Pignata, Claudio, Pietrogrande, Maria Cristina, Marino, Bruno, Ugazio, Alberto Giovanni, Plebani, Alessandro, Rossi, Paolo, Aiuti, A, Rossi, P, Pierani, P, Gabrielli, A, Danieli, Mg, De Mattia, D, Sisto, C, Dammacco, F, Ranieri, G, Pession, A, Ricci, G, Minelli, P, Lougaris, V, Badolato, R, Cattaneo, R, Airò, P, Mura, Rm, Cossu, F, Del Giacco, S, Manconi, Pe, Consarino, C, Dello Russo, Am, Miniero, R, Anastasio, E, Marino, S, Russo, G, Paganelli, R, Sperlì, D, Carpino, L, Aricò, M, Gambineri, E, Lippi, F, Canessa, C, Maggi, E, Romagnani, S, Matucci, A, Vultaggio, A, Gattorno, M, Castagnola, E, Nigro, G, Presta, G, Civino, A, Buzi, F, Gambaretto, G, Fasoli, S, Salpietro, C, Gallizzi, R, Dellepiane, Rm, Panisi, C, Fabio, G, Carrabba, M, Pietrogrande, M, Roncarolo, Mg, Biondi, A, Vallinoto, C, Poggi, V, Menna, G, Di Nardo, R, Sottile, R, Marone, G, Spadaro, G, Carli, M, Basso, G, Putti, C, Semenzato, G, Agostini, C, D'Angelo, P, Izzi, G, Bertolini, P, Zecca, M, Marseglia, G, Maccario, R, Felici, L, Favre, C, Vecchi, V, Sacchini, P, Rinaldi, G, Livadiotti, S, Simonetti, A, Stabile, A, Duse, M, Iacobini, M, Quinti, I, Fiorilli, M, Moschese, V, Cecere, F, D'Ambrosio, A, De Zan, G, Strafella, S, Tamaro, Paolo, Rabusin, M, Tommasini, A, Tovo, P, De Carli, M, De Carli, S, Nespoli, L, Marinoni, M, Porcellini, A, Lunardi, C, Patuzzo, G, Boner, A, Degani, D., Cancrini, C., Pulisfito, P., Digilio, M. C., Soresina, A., Martino, S., Rondelli, R., Consolini, R., Ruga, E. M., C. a. r. d. i. n. a. l. e., F., Finocchi, A., Romiti, M. L., Martire, B., Bacchetta, R., Albano, V., Carotti, A., Specchia, F., Montin, D., Cocchi, G., Trizzino, A., Bossi, G., Milanesi, O., Azzari, C., Corsello, G., Aiuti, A., Pietrogrande, M. C., Marino, B., Ugazio, A. G., Plebani, A., Digilio, MC, Ruga, EM, Romiti, ML, trizzino, A, Aiuti, Pietrogrande, MC, and Ugazio, AG

Subjects
Male, Pediatrics, 22q11.2 deletion, Delayed Diagnosis, Time Factors, Chromosomes, Human, Pair 22, Developmental Disabilities, digeorge syndrome, Sex Factor, Severity of Illness Index, Retrospective Studie, DiGeorge syndrome, Early Diagnosi, Age Factor, Prospective Studies, Neonatal hypocalcemia, Prospective cohort study, Child, medicine.diagnostic_test, Delayed Diagnosi, Primary immune disorders, Age Factors, del 22q, MIM, Abnormalities, Multiple, Adolescent, Adult, Child, Preschool, DiGeorge Syndrome, Early Diagnosis, Female, Follow-Up Studies, Genetic Testing, Humans, Infant, Infant, Newborn, Monitoring, Physiologic, Retrospective Studies, Risk Assessment, Sex Factors, Young Adult, Disease Progression, Cohort, Abnormalities, Multiple, Pediatrics, Perinatology and Child Health, Human, medicine.medical_specialty, Time Factor, Monitoring, Developmental Disabilitie, Italian Association of Pediatric Haematology and Oncology, Context (language use), Chromosomes, Follow-Up Studie, Severity of illness, medicine, 22q11DS, 22q11.2 deletion syndrome, AIEOP, Mendelian Inheritance in Man, Preschool, Physiologic, Genetic testing, Settore MED/38 - Pediatria Generale e Specialistica, business.industry, Retrospective cohort study, medicine.disease, Newborn, Prospective Studie, Pair 22, business
Abstract

Objective To investigate the clinical manifestations at diagnosis and during follow-up in patients with 22q11.2 deletion syndrome to better define the natural history of the disease. Study design A retrospective and prospective multicenter study was conducted with 228 patients in the context of the Italian Network for Primary Immunodeficiencies. Clinical diagnosis was confirmed by cytogenetic or molecular analysis. Results The cohort consisted of 112 males and 116 females; median age at diagnosis was 4 months (range 0 to 36 years 10 months). The diagnosis was made before 2 years of age in 71% of patients, predominantly related to the presence of heart anomalies and neonatal hypocalcemia. In patients diagnosed after 2 years of age, clinical features such as speech and language impairment, developmental delay, minor cardiac defects, recurrent infections, and facial features were the main elements leading to diagnosis. During follow-up (available for 172 patients), the frequency of autoimmune manifestations ( P = .015) and speech disorders ( P = .002) increased. After a median follow-up of 43 months, the survival probability was 0.92 at 15 years from diagnosis. Conclusions Our data show a delay in the diagnosis of 22q11.2 deletion syndrome with noncardiac symptoms. This study provides guidelines for pediatricians and specialists for early identification of cases that can be confirmed by genetic testing, which would permit the provision of appropriate clinical management.

Published
2014

4. Autoantibodies to harmonin and villin are diagnostic markers in children with IPEX syndrome

Author

Lampasona V, Passerini L, Barzaghi F, Lombardoni C, Bazzigaluppi E, Brigatti C, Bacchetta R, BOSI , EMANUELE, Lampasona, V, Passerini, L, Barzaghi, F, Lombardoni, C, Bazzigaluppi, E, Brigatti, C, Bacchetta, R, and Bosi, Emanuele

Abstract

Autoantibodies to enterocyte antigens harmonin (75 kDa USH1C protein) and villin (actin-binding 95 kDa protein) are associated with the Immune dysregulation, Polyendocrinopathy, Enteropathy, X-linked (IPEX) syndrome. In this study we evaluated the diagnostic value of harmonin and villin autoantibodies in IPEX and IPEX-like syndromes. Harmonin and villin autoantibodies were measured by a novel Luminescent-Immuno-Precipitation-System (LIPS) quantitative assay, in patients with IPEX, IPEX-like syndrome, Primary Immunodeficiencies (PID) with enteropathy, all diagnosed by sequencing of the FOXP3 gene, and in type 1 diabetes (T1D), celiac disease and healthy blood donors as control groups. Harmonin and villin autoantibodies were detected in 12 (92%) and 6 (46%) of 13 IPEX patients, and in none of the IPEX-like, PID, T1D, celiac patients, respectively. All IPEX patients, including one case with late and atypical clinical presentation, had either harmonin and/or villin autoantibodies and tested positive for enterocyte antibodies by indirect immunofluorescence. When measured in IPEX patients in remission after immunosuppressive therapy or hematopoietic stem cell transplantation, harmonin and villin autoantibodies became undetectable or persisted at low titers in all cases but one in whom harmonin autoantibodies remained constantly high. In one patient, a peak of harmonin antibodies paralleled a relapse phase of enteropathy. Our study demonstrates that harmonin and villin autoantibodies, measured by LIPS, are sensitive and specific markers of IPEX, differentiate IPEX, including atypical cases, from other early childhood disorders associated with enteropathy, and are useful for screening and clinical monitoring of affected children.

Published
2013

7. Effetti di nano ZnO sull’intestino di embrioni di Xenopus laevis

Author

MANTECCA, PARIDE, MOSCHINI, ELISA, BONFANTI, PATRIZIA, COLOMBO, ANITA EMILIA, CAMATINI, MARINA CARLA, Fascio, U, Santo, N, Tremolada, P, Bacchetta, R., Mantecca, P, Moschini, E, Bonfanti, P, Colombo, A, Camatini, M, Fascio, U, Santo, N, Tremolada, P, and Bacchetta, R

Subjects
nano ZnO, Xenopus laevis, sviluppo embrionale, BIO/06 - ANATOMIA COMPARATA E CITOLOGIA
Published
2012

8. Do Surface Modifications Modulate Embryiotoxicity of nano ZnO?

Author

MOSCHINI, ELISA, COLOMBO, ANITA EMILIA, BONFANTI, PATRIZIA, CHIRICO, GIUSEPPE, CAMATINI, MARINA CARLA, MANTECCA, PARIDE, Calabri, L, Rettighieri, L, Bacchetta, R, Santo, N, Fascio, U, Moschini, E, Colombo, A, Bonfanti, P, Calabri, L, Rettighieri, L, Bacchetta, R, Santo, N, Fascio, U, Chirico, G, Camatini, M, and Mantecca, P

Subjects
nano ZnO, embryotoxicity, Xenopus laevis, BIO/06 - ANATOMIA COMPARATA E CITOLOGIA
Published
2012

10. Tossicità di nanoparticelle di Carbonio sullo sviluppo dell’anfibio Xenopus laevis

Author

Fascio, U, Santo, N, Bacchetta, R, Tremolada, P, CHIRICO, GIUSEPPE, CAMATINI, MARINA CARLA, COLOMBO, ANITA EMILIA, MOSCHINI, ELISA, MANTECCA, PARIDE, Fascio, U, Santo, N, Bacchetta, R, Tremolada, P, Chirico, G, Camatini, M, Colombo, A, Moschini, E, and Mantecca, P

Subjects
embriotossicità, nanoparticelle carbonio, Xenopus laevis, BIO/06 - ANATOMIA COMPARATA E CITOLOGIA
Published
2012

12. Mutations in the signal transducer and activator of transcription 3 (STAT3) and diagnostic guidelines for the Hyper-IgE syndrome

Author

Woellner, C., Gertz, M. E., Schaffer, A. A., Lagos, M., Perro, M., Glocker, E. -O, Pietrogrande, M. C., Cossu, F., Franco, J. L., Matamoros, N., Pietrucha, B., Heropolitanska-Pliszka, E., Yeganch, M., Moin, M., Espanol, T., Ehl, S., Gennery, A. R., Abinun, M., Breborowicz, A., Niehues, T., Kilic, S. S., Junker, A., Turvey, S. E., Plebani, A., Sanchez, B., Garty, B-Z, Pignata, C., Cancrini, C., Litzman, J., Sanal, O., Batimann, U., Bacchetta, R., Hsu, A. P., Davis, J. N., Hammarstrom, L., Davies, G. E., Eren, E., Arkwright, P. D., Moilanen, J. S., Viemann, D., Sujoy Khan, Marodi, L., Cant, A. J., Freeman, A. F., Puck, J. M., Holland, S. M., Grimbacher, B., Woellner, C., Gertz, E. M., Schäffer, A. A., Lagos, M., Perro, M., Glocker, E. O., Pietrogrande, M. C., Cossu, F., Franco, J. L., Matamoros, N., Pietrucha, B., Heropolitańska Pliszka, E., Yeganeh, M., Moin, M., Español, T., Ehl, S., Gennery, A. R., Abinun, M., Bręborowicz, A., Niehues, T., Kilic, S. S., Junker, A., Turvey, S. E., Plebani, A., Sánchez, B., Garty, B. Z., Pignata, Claudio, Cancrini, C., Litzman, J., Sanal, O., Baumann, U., Bacchetta, R., Hsu, A. P., Davis, J. N., Hammarström, L., Davies, E. G., Eren, E., Arkwright, P. D., Moilanen, J. S., Viemann, D., Khan, S., Maródi, L., Cant, A. J., Freeman, A. F., Puck, J. M., Holland, S. H., and Grimbacher, B.

Subjects
Hyper-IgE syndrome, STAT3 mutation, TH17 cell, Job syndrome, diagnostic guideline, HIES, Immunodeficiencies
Abstract

BACKGROUND: The hyper-IgE syndrome (HIES) is a primary immunodeficiency characterized by infections of the lung and skin, elevated serum IgE, and involvement of the soft and bony tissues. Recently, HIES has been associated with heterozygous dominant-negative mutations in the signal transducer and activator of transcription 3 (STAT3) and severe reductions of T(H)17 cells. OBJECTIVE: To determine whether there is a correlation between the genotype and the phenotype of patients with HIES and to establish diagnostic criteria to distinguish between STAT3 mutated and STAT3 wild-type patients. METHODS: We collected clinical data, determined T(H)17 cell numbers, and sequenced STAT3 in 100 patients with a strong clinical suspicion of HIES and serum IgE >1000 IU/mL. We explored diagnostic criteria by using a machine-learning approach to identify which features best predict a STAT3 mutation. RESULTS: In 64 patients, we identified 31 different STAT3 mutations, 18 of which were novel. These included mutations at splice sites and outside the previously implicated DNA-binding and Src homology 2 domains. A combination of 5 clinical features predicted STAT3 mutations with 85% accuracy. T(H)17 cells were profoundly reduced in patients harboring STAT3 mutations, whereas 10 of 13 patients without mutations had low (1000IU/mL plus a weighted score of clinical features >30 based on recurrent pneumonia, newborn rash, pathologic bone fractures, characteristic face, and high palate. Probable: These characteristics plus lack of T(H)17 cells or a family history for definitive HIES. Definitive: These characteristics plus a dominant-negative heterozygous mutation in STAT3.

Published
2010

13. Intensified immunosuppression with ATG reduces graft failure without affecting immune reconstitution or infections in high-risk beta thalassaemia patients after HLA-identical sibling HSCT

Author

Biral E, Cappelli B, Zugna D, Chiesa R, Biffi A, Zito L, Fleischhauer K, Bacchetta R, Fumagalli L, Di Serio C, Roncarolo MG, Aiuti A, Marktel S., CICERI , FABIO, Biral, E, Cappelli, B, Zugna, D, Chiesa, R, Biffi, A, Zito, L, Fleischhauer, K, Bacchetta, R, Fumagalli, L, Di Serio, C, Ciceri, Fabio, Roncarolo, Mg, Aiuti, A, and Marktel, S.

Published
2010

14. Interleukin-10 Anergized Donor T Cell Infusion Improves Immune Reconstitution without Severe Graft-Versus-Host-Disease After Haploidentical Hematopoietic Stem Cell Transplantation

Author

Bacchetta R, Sartirana C, Lucarelli B, Miqueu P, Stanghellini MTL, Greco R, Velardi A, Aversa F, Martelli MF, Gregori S, Zappone E, Fleischhauer K, Bernardi M, Peccatori J, Roncarolo MG, CICERI , FABIO, Bacchetta, R, Sartirana, C, Lucarelli, B, Miqueu, P, Stanghellini, Mtl, Greco, R, Velardi, A, Aversa, F, Martelli, Mf, Gregori, S, Zappone, E, Fleischhauer, K, Bernardi, M, Peccatori, J, Ciceri, Fabio, and Roncarolo, Mg

Published
2009

15. Termporal, quantitative and functional characteristics of single-KIR positive alloreactive natural killer cell recovery account for impaired graft-versus-leukemia activity after haploidentical hematopoietic stem cell transplantation

Author

VAGO L, FORNO B, SORMANI M. P, CROCCHIOLO R, ZINO E, DI TERLIZZI S, LUPO STANGHELLINI M. T, MAZZI B, PERNA S. K, BONDANZA A, MIDDLETON D, PALINI A, BERNARDI M, BACCHETTA R, PECCATORI J, ROSSINI S, RONCAROLO M. G, BORDIGNON , CLAUDIO, BONINI C, CICERI, FABIO, AND K. FLEISCHHAUER, Vago, L, Forno, B, SORMANI M., P, Crocchiolo, R, Zino, E, DI TERLIZZI, S, LUPO STANGHELLINI M., T, Mazzi, B, PERNA S., K, Bondanza, A, Middleton, D, Palini, A, Bernardi, M, Bacchetta, R, Peccatori, J, Rossini, S, RONCAROLO M., G, Bordignon, Claudio, Bonini, C, Ciceri, Fabio, and AND K., Fleischhauer

Published
2008

16. Diagnostic criteria for the hyper IgE recurrent infection syndrome/Job’s syndrome/STAT3 deficiency

Author

Woellner C., Gertz E.m., Schaeffer A.A., Lagos M., Perro M., Pietrogrande M.C., Cossu F., Franco J.L., Matamoros N., Pietrucha B., Heropolianska Pliszka E., Yeganeh M., Espanol T., Ehl S., Gennery A.r., Abinun M., Breborowics A., Niehues T., Kilic S.S., Junker A., Turvey S., Plebani A., Sanchez B., Garty B.Z., Cancrini C., Litzman J., Sanal O., Baumann U., Bacchetta R., Hsu A., Hammarstrom L., Davies E.G., Eren E., Arkwright P.D., Moilanen J.S., Viemann D., Khan S., Marodi L., Cant A.M., Puck J.M., Holland S.M., Grimbacher B., PIGNATA, CLAUDIO, Woellner, C., Gertz, E. m., Schaeffer, A. A., Lagos, M., Perro, M., Pietrogrande, M. C., Cossu, F., Franco, J. L., Matamoros, N., Pietrucha, B., Heropolianska Pliszka, E., Yeganeh, M., Espanol, T., Ehl, S., Gennery, A. r., Abinun, M., Breborowics, A., Niehues, T., Kilic, S. S., Junker, A., Turvey, S., Plebani, A., Sanchez, B., Garty, B. Z., Pignata, Claudio, Cancrini, C., Litzman, J., Sanal, O., Baumann, U., Bacchetta, R., Hsu, A., Hammarstrom, L., Davies, E. G., Eren, E., Arkwright, P. D., Moilanen, J. S., Viemann, D., Khan, S., Marodi, L., Cant, A. M., Puck, J. M., Holland, S. M., and Grimbacher, B.

Published
2008

20. Type 1 T regulatory cells

Author

RONCAROLO , MARIA GRAZIA, BACCHETTA R., BORDIGNON , CLAUDIO, NARULA S., LEVINGS M. K., Roncarolo, MARIA GRAZIA, Bacchetta, R., Bordignon, Claudio, Narula, S., and Levings, M. K.

Published
2001

21. La memoria immunologica

Author

Bacchetta R, Cattaneo F, BATTAGLIA, MARCO MARIA, RONCAROLO , MARIA GRAZIA, Bacchetta, R, Cattaneo, F, Battaglia, MARCO MARIA, and Roncarolo, MARIA GRAZIA

Published
2001

22. Transplantation in patients with SCID: mismatched related stem cells or unrelated cord blood?

Author

Fernandes, Jf, Rocha, V, Labopin, M, Neven, B, Moshous, D, Gennery, Ar, Friedrich, W, Porta, F, Diaz de Heredia, C, Wall, D, Bertrand, Y, Veys, P, Slatter, M, Schulz, A, Chan, Kw, Grimley, M, Ayas, M, Gungor, T, Ebell, W, Bonfim, C, Kalwak, K, Taupin, P, Blanche, S, Gaspar, Hb, Landais, P, Fischer, A, Gluckman, E, Cavazzana Calvo, M, Eurocord, Inborn Errors Working Party of European Group for Blood, Marrow Transplantation: Ahmed, A, Auiti, A, Biffi, A, Cant, A, Fasth, A, Gennery, A, Hassan, A, Lankester, A, O'Mera, A, Plabani, A, Rovelli, A, Salmon, A, Scarselli, A, Thrasher, A, Van Royen, A, Villa, A, Wawer, A, Wahadneh, A, Worth, A, Belohradsky, B, Wolska, B, Gaspar, B, Bonfirm, C, Booth, C, Klein, C, Messina, C, Peters, C, Steward, C, Lindemans, C, Schuetz, C, de Heredia Rubio CD, Bensoussan, D, Gleadow, D, Lilic, D, Gambineri, Eleonora, Smith, E, Aerts, F, Caracseghi, F, Roberts, G, Davies, G, Al Mousa, H, Jossanc, H, Ozsahim, H, Hirsch, I, Meyts, I, Tezcan, I, Mueller, I, Andresc, I, Boelens, J, Fernandes, J, Folloni, J, Keuhl, J, Reichenbach, J, Stary, J, Wachowiak, J, Xu Bayford, J, Cunha, Jm, Ehlert, J, Rao, K, Sykora, K, Andais, L, Brown, L, Dal Cortivo, L, Griffith, L, Notarangelo, L, Abinun, M, Albert, M, Bierings, M, Bouchet, M, Cavazzana, M, Hirschfield, M, Cowan, M, Hoenig, M, Loubser, M, Roncarolo, M, Sauer, M, Schneider, M, Verstegen, M, Schroeder, M, Essink, M, Yesilipek, M, Entz Werle, N, Mahlaoui, N, Schlautmann, N, Taylor, N, Vanroyen, N, Walffraat, N, Sanal, O, Amrolia, P, Bordigoni, P, De Coppi, P, Frange, P, Orchard, P, Sedlacek, P, Shaw, P, Stephensky, P, Bacchetta, R, Bredius, R, Formankova, R, Gale, R, Seger, R, Wynn, R, Corbacioglu, S, Ehl, S, Hacein Bey, S, Hambleton, S, Mohsen, S, Mueller, S, Pai, Sy, Espanol, T, Flood, T, Guengoer, T, Bordon, V, Ormoor, V, Pashano, V, Courteille, V, Czogala, W, Qasim, W, Camci, Y, and Nademi, Z.

Subjects
Male, medicine.medical_specialty, Transplantation Conditioning, medicine.medical_treatment, Immunology, Graft vs Host Disease, Kaplan-Meier Estimate, Cord Blood Stem Cell Transplantation, Hematopoietic stem cell transplantation, Biochemistry, Gastroenterology, SCID HSCT, Internal medicine, medicine, Humans, Proportional Hazards Models, Retrospective Studies, Preparative Regimen, Severe combined immunodeficiency, business.industry, Umbilical Cord Blood Transplantation, Incidence, Hematopoietic Stem Cell Transplantation, Infant, Newborn, Infant, Cell Biology, Hematology, medicine.disease, Surgery, Transplantation, Treatment Outcome, Child, Preschool, Histocompatibility, Cord blood, Female, Severe Combined Immunodeficiency, business
Abstract

Pediatric patients with SCID constitute medical emergencies. In the absence of an HLA-identical hematopoietic stem cell (HSC) donor, mismatched related-donor transplantation (MMRDT) or unrelated-donor umbilical cord blood transplantation (UCBT) are valuable treatment options. To help transplantation centers choose the best treatment option, we retrospectively compared outcomes after 175 MMRDTs and 74 UCBTs in patients with SCID or Omenn syndrome. Median follow-up time was 83 months and 58 months for UCBT and MMRDT, respectively. Most UCB recipients received a myeloablative conditioning regimen; most MMRDT recipients did not. UCB recipients presented a higher frequency of complete donor chimerism (P = .04) and faster total lymphocyte count recovery (P = .04) without any statistically significance with the preparative regimen they received. The MMRDT and UCBT groups did not differ in terms of T-cell engraftment, CD4+ and CD3+ cell recoveries, while Ig replacement therapy was discontinued sooner after UCBT (adjusted P = .02). There was a trend toward a greater incidence of grades II-IV acute GVHD (P = .06) and more chronic GVHD (P = .03) after UCBT. The estimated 5-year overall survival rates were 62% ± 4% after MMRDT and 57% ± 6% after UCBT. For children with SCID and no HLA-identical sibling donor, both UCBT and MMRDT represent available HSC sources for transplantation with quite similar outcomes.

Published
2012

23. Natural killer cell clones can efficiently process and present protein antigens

Author

Roncarolo, M. G., Bigler, M., Haanen, J. B., Yssel, H., Bacchetta, R., de Vries, J. E., Spits, H., and Other departments

Subjects
Immunology, Immunology and Allergy
Abstract

NK cell clones obtained from three different donors were tested for their ability to present soluble proteins to Ag-specific T cell clones. All NK clones were CD2+CD3-CD56+, whereas the expression of CD16 varied from clone to clone. The NK cell clones were able to process and present tetanus toxoid (TT) to TT-specific T cell clones in a class II HLA restricted manner. The capacity of NK cell clones to function as APC was also observed using the house dust mite allergen Der p I and the Der p I-derived peptide Val89-Cys117. As with EBV-transformed B cell line, NK cell clones could present the peptide 3-13 derived from the 65-kDa heat shock protein of Mycobacterium leprae, but they were unable to present the whole M. leprae Ag. Freshly isolated NK cells, IL-2-activated NK cells, and NK cell lines expanded in vitro could also process and present TT. The ability of the different NK populations to act as accessory cells correlated with their levels of class II HLA expression. These data demonstrate that NK cell clones can efficiently function as APC, however they may be restricted in the types of Ag that they can process.

Published
1991
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25. Host-reactive CD4+ and CD8+ T cell clones isolated from a human chimera produce IL-5, IL-2, IFN-gamma and granulocyte/macrophage-colony-stimulating factor but not IL-4

Author

Bacchetta, R., de Waal Malefijt, R., Yssel, H., Abrams, J., de Vries, J. E., Spits, H., Roncarolo, M. G., and Other departments

Subjects
Immunology, Immunology and Allergy
Abstract

In the present study, we investigated the lymphokine production patterns in a series of CD4+ and CD8+ host-reactive T cell clones isolated from PBL of a SCID patient, who was immunologically reconstituted by two allogeneic fetal liver and thymus transplantations 13 years ago. We demonstrate that these donor-derived T cell clones, specifically reacting with the MHC Ag expressed on the recipient cells, do not produce IL-4 and do not express IL-4 mRNA upon Ag or polyclonal stimulations. In contrast, CD4+ tetanus toxin-specific T cell clones isolated from the same patient and having the same HLA phenotype produced normal amounts of IL-4 upon activation. These data suggest that the failure to produce IL-4 is a specific characteristic of these host-reactive clones and is not due to a genetic defect of the transplanted cells. Furthermore, different modes of activation resulted in simultaneous production of IL-5, IL-2, IFN-gamma, granulocyte/macrophage-CSF, and transcription of the TNF-beta gene by the host-reactive clones, indicating that the lack of IL-4 production is not related to the mode of activation. The finding that some of these clones produce significant levels of IL-5 but no IL-4 indicates that the IL-4 and IL-5 genes are not always coexpressed in activated human T cells.

Published
1990
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27. DYSFUNCTIONAL CYTOKINE PRODUCTION BY HOST-REACTIVE T-CELL - CLONES ISOLATED FROM A CHIMERIC SEVERE COMBINED IMMUNODEFICIENCY PATIENT TRANSPLANTED WITH HAPLOIDENTICAL BONE-MARROW

Author

BACCHETTA R, PARKMAN R, MCMAHON M, WEINBERG K, BIGLER M, DEVRIES JE, RONCAROLO , MARIA GRAZIA, Bacchetta, R, Parkman, R, Mcmahon, M, Weinberg, K, Bigler, M, Devries, Je, and Roncarolo, MARIA GRAZIA

Abstract

We have investigated the mechanism of tolerance in a patient with severe combined immunodeficiency (SCID) transplanted with HLA-haploidentical, T cell-depleted bone marrow cells obtained from the mother. At 4 years after transplantation, T cells, natural killer (NK) cells, and a small percentage (2%) of B cells were found to be of donor origin, whereas monocytes and the majority of B cells remained of host origin. In primary mixed lymphocyte cultures (MLC). the engrafted T cells of the donor did not proliferate in response to the host cells, whereas untransplanted donor T cells showed good proliferative responses. However, CD4(+) and CD8(+) T-cell clones of donor origin with specificity for class II and class I HLA determinants of the host were isolated. CD8(+), host-reactive T-cell clones displayed normal cytotoxic activity after stimulation with the host cells, but proliferative responses of CD4(+), host-reactive T-cell clones were considerably reduced. In addition, both CD8(+) and CD4(+), host-reactive T-cell clones produced very low to undetectable levels of interleukin-2 (IL-2), IL-4, IL-5, IL-10, interferon-gamma, and granulocyte-macrophage colony-stimulating factor after specific antigenic activation, which may be responsible for their nonresponsive state in vivo. Expression of the CD3 zeta subunit of the T-cell receptor (TcR) was normal, and after stimulation via CD3, Raf-1 and p42 mitogen activated protein (MAP) kinase were phosphorylated, indicating that this part of the signaling pathway after triggering of the TcR/CD3 complex is present. These results, together with our previous observation that dysfunctional, host-reactive T-cell clones can be isolated in SCID patients transplanted with fetal liver stem cells, demonstrate that lack of clonal deletion of host-reactive T cells is a general phenomenon after HLA-mismatched stem cell transplantation. (C) 1995 by The American Society of Hematology.

Published
1995

29. Role of IL-10 in transplantation tolerance

Author

RONCAROLO , MARIA GRAZIA, Bacchetta R, Touraine JL, de Waal Malefyt R, de Vries JE, J.L. Touraine, J. Traeger, H. Bétuel, J.M. Dubernard, J.P. Revillard and C. Dupuy, Roncarolo, MARIA GRAZIA, Bacchetta, R, Touraine, Jl, de Waal Malefyt, R, and de Vries, Je

Published
1994

30. Human Ig production and isotype switching in severe combined immunodeficient-human mice

Author

Bart Vandekerckhove, Jones D, Punnonen J, Schols D, Hc, Lin, Duncan B, Bacchetta R, Je, Vries, Mg, Roncarolo, Vandekerckhove, Bae, Jones, D, Punnonen, J, Schols, D, Lin, Hc, Duncan, B, Bacchetta, R, Devries, Je, and Roncarolo, MARIA GRAZIA

Subjects
B-Lymphocytes, Chimera, Immunology, Mice, SCID, Thymus Gland, Lymphocyte Subsets, Clone Cells, Immunoglobulin Isotypes, Mice, Immunoglobulin M, Fetal Tissue Transplantation, Immunoglobulin G, Antibody Formation, Immunology and Allergy, Animals, Humans
Abstract

Severe combined immunodeficient (SCID) mice were transplanted with different human fetal organs (SCID-hu mice), including thymus, liver, spleen, and omentum, and the serum levels of human IgM, IgG, IgE, and IgA were measured. In all SCID-hu mice significant levels (up to 590 ng/ml) of IgM were detected, irrespective of the organs transplanted. In contrast, IgG was present (up to 530 ng/ml) only when the fetal thymus was transplanted together with the fetal liver, indicating that the presence of human T cells is a prerequisite for in vivo isotype switching by human B cells in SCID-hu mice. Additional transplantation of fetal spleen did not significantly increase IgG levels. Human IgA and IgE were never detected in the serum of these SCID-hu mice. The peak of IgM and IgG production was observed 4 months after transplantation. At that time, analysis by IEF showed that human IgG present in SCID-hu serum was at least oligoclonal. Furthermore, all IgG subclasses were represented in the human IgG pool. Human B cells were undetectable in the peripheral blood, spleen, and bone marrow of-these SCID-hu mice; in contrast, B cells expressing CD19 could be isolated from the SCID-hu thymus. Considerable proportions of the CD19+ B cells coexpressed CD5, CD7, CD10, CD40, and CD2. These B cells spontaneously produced IgM and IgG in vitro and could be induced to switch to IgE-producing cells when cocultured with cloned activated CD4+ T cells in the presence of IL-4. Collectively, these data demonstrate that functionally mature B cells able to produce IgM and IgG in vivo, and IgE in vitro, are present in the SCID-hu human thymus.

Published
1993

31. FETAL LIVER-TRANSPLANTATION - BIOLOGY AND CLINICAL-RESULTS

Author

TOURAINE JL, BACCHETTA R, RAUDRANT D, REBAUD A, LAPLACE S, CESBRON P, GEBUHRER L, ZABOT MT, TOURAINE F, FRAPPAZ D, SOUILLET G, VULLO C., RONCAROLO , MARIA GRAZIA, Touraine, Jl, Roncarolo, MARIA GRAZIA, Bacchetta, R, Raudrant, D, Rebaud, A, Laplace, S, Cesbron, P, Gebuhrer, L, Zabot, Mt, Touraine, F, Frappaz, D, Souillet, G, and Vullo, C.

Abstract

Over the last 18 years, we have developed the transplantation of fetal liver cells to treat severe immunodeficiencies, hematological disorders and inborn errors of metabolism. Post-natally, this treatment is successful in two-third of patients and it is therefore very valuable, especially when there is no perfectly matched donor for a bone marrow transplant. Since 1 988 we have carried out these fetal liver transplants (FLTs) in utero, immediately after prenatal diagnosis. Engraftment and reconstitution have been obtained, and several advantages appear to be associated with in utero FLT : increased probability of graft take, ideal isolation of the patient (in the maternal uterus) and optimal environment for the differentiation of the transplanted fetal liver cells (in the fetal host).

Published
1993

32. Depth effects on zebra mussel reproduction

Author

Mantecca, P., Vailati, G., Garibaldi, L., and Bacchetta, R.

Subjects
Settore BIO/06 - Anatomia Comparata e Citologia, Depth, Dreissena polymorpha, Gametogenesis, Histology, Reproduction
Published
2003

33. T-CELL REPERTOIRE AND TOLERANCE AFTER FETAL STEM-CELL TRANSPLANTATION

Author

RONCAROLO , MARIA GRAZIA, BACCHETTA R., Roncarolo, MARIA GRAZIA, and Bacchetta, R.

Abstract

We studied the T cell repertoire and the mechanism of tolerance in two patients with severe combined immunodeficiency transplanted with HLA mismatched fetal liver stem cells. They are 17 and 5 years old now, healthy, and show normal immunoresponses to recall antigens. Their T cells are of donor origin, whereas monocytes and B cells remained of the host. The NK cells have different sources since in one patient they derive from the donor and in the other one from the host. Despite the HLA mismatch between donor and host cells, no acute or chronic graft-versus-host disease was observed. In vitro experiments with PBMC showed specific nonresponsiveness for the HLA antigens expressed by the host cells. However, an extensive clonal analysis showed that CD4+ and CD8+ host-reactive T cell clones recognizing class II and class I HLA molecules of the host, respectively, were present in the peripheral blood of both patients. Limiting dilution experiments indicated that the frequency of CD8+ host-reactive cells was in the same range as that observed for alloreactive T cells. In contrast, no donor reactive CD8+ T cells could be isolated. Host-reactive CD4+ and CD8+ T cell clones were normal in their capacity to produce IL-2, IFN-gamma, GM-CSF and IL-5, but they failed completely to synthesize IL-4. In addition, CD4+ T cell clones from patient RV secreted very high levels of IL-10. Interestingly, exogenous IL-10 was able to inhibit the proliferative responses of the CD4+ host-reactive T cell clones. Our data demonstrate that host-reactive cells are not deleted from the donor T cell repertoire following allogenic fetal liver stem cell transplantation. Therefore, in vivo tolerance between the host and the donor is maintained by a peripheral autoregulatory mechanism in which cytokines may play a role.

Published
1992

34. A SCID PATIENT RECONSTITUTED WITH HLA-INCOMPATIBLE FETAL STEM-CELLS AS A MODEL FOR STUDYING TRANSPLANTATION TOLERANCE

Author

RONCAROLO , MARIA GRAZIA, BACCHETTA R, BIGLER M, TOURAINE JL, DEVRIES JE, SPITS H., Roncarolo, MARIA GRAZIA, Bacchetta, R, Bigler, M, Touraine, Jl, Devries, Je, and Spits, H.

Abstract

We studied a severe combined immunodeficiency (SCID) patient who received transplantations with completely HLA-mismatched fetal liver and thymus from two different donors. The patient is now 14 years old, healthy and shows normal immunoresponses to recall antigens. His T cells are of donor origin, whereas the monocytes, B cells, and natural killer (NK) cells are of the recipient. The successful immunological reconstitution raised questions as to how T and B cells could collaborate across an HLA barrier and how tolerance was achieved. We have shown that tetanus toxin-specific T cell clones isolated from this patient recognized this antigen in the context of host and not of donor HLA-DR, indicating that those cells were educated in the host environment, presumably the thymus. Despite this, an unexpectedly high frequency of host-reactive clones was found that could recognize MHC antigens of the host. It was particularly striking that CD8+ CTL clones were obtained that recognized class I MHC antigens on the host cells. Nevertheless, the patient did not show any sign of acute or chronic graft-versus-host disease (GVHD). These data indicated that no or only incomplete clonal deletion had taken place in this patient and suggest the presence of a peripheral suppressor mechanism. Thus far, we have no indication for the existence of suppressor T cells. Inasmuch as it was found that host-reactive T cells fail to produce IL-4, which is exceptional for CD4+ T cells, we are exploring the possibility that abnormal cytokine production patterns of host-reactive T cells are associated with suppression of these cells in vivo.

Published
1991

35. NATURAL-KILLER-CELL CLONES CAN EFFICIENTLY PROCESS AND PRESENT PROTEIN ANTIGENS

Author

RONCAROLO , MARIA GRAZIA, BIGLER M, HAANEN JBA, YSSEL H, BACCHETTA R, DEVRIES JE, SPITS H., Roncarolo, MARIA GRAZIA, Bigler, M, Haanen, Jba, Yssel, H, Bacchetta, R, Devries, Je, and Spits, H.

Abstract

NK cell clones obtained from three different donors were tested for their ability to present soluble proteins to Ag-specific T cell clones. All NK clones were CD2+CD3-CD56+, whereas the expression of CD16 varied from clone to clone. The NK cell clones were able to process and present tetanus toxoid (TT) to TT-specific T cell clones in a class II HLA restricted manner. The capacity of NK cell clones to function as APC was also observed using the house dust mite allergen Der p I and the Der p I-derived peptide Val89-Cys117. As with EBV-transformed B cell line, NK cell clones could present the peptide 313 derived from the 65-kDa heat shock protein of Mycobacterium leprae, but they were unable to present the whole M. leprae Ag. Freshly isolated NK cells, IL-2-activated NK cells, and NK cell lines expanded in vitro could also process and present TT. The ability of the different NK populations to act as accessory cells correlated with their levels of class II HLA expression. These data demonstrate that NK cell clones can efficiently function as APC, however they may be restricted in the types of Ag that they can process.

Published
1991

36. Host-reactive CD4+ and CD8+ T cell clones isolated from a human chimera produce IL-5, IL-2, IFN-γ and granulocyte/macrophage-colony-stimulating factor but not IL-4

Author

Bacchetta, R., De Waal Malefijt, R. , Yssel, H. , Abrams, De Vries, J. E. , Spits, RONCAROLO , MARIA GRAZIA, Bacchetta, R., De Waal, Malefijt, R., Yssel, H., Abram, De, Vrie, J. E., Spit, and Roncarolo, MARIA GRAZIA

Abstract

In the present study, we investigated the lymphokine production patterns in a series of CD4+ and CD8+ host-reactive T cell clones isolated from PBL of a SCID patient, who was immunologically reconstituted by two allogeneic fetal liver and thymus transplantations 13 years ago. We demonstrate that these donor-derived T cell clones, specifically reacting with the MHC Ag expressed on the recipient cells, do not produce IL-4 and do not express IL-4 mRNA upon Ag or polyclonal stimulations. In contrast, CD4+ tetanus toxin-specific T cell clones isolated from the same patient and having the same HLA phenotype produced normal amounts of IL-4 upon activation. These data suggest that the failure to produce IL-4 is a specific characteristic of these host-reactive clones and is not due to a genetic defect of the transplanted cells. Furthermore, different modes of activation resulted in simultaneous production of IL-5, IL-2, IFN-γ, granulocyte/macrophage-CSF, and transcription of the TNF-β gene by the host-reactive clones, indicating that the lack of IL-4 production is not related to the mode of activation. The finding that some of these clones produce significant levels of IL-5 but no IL-4 indicates that the IL-4 and IL-5 genes are not always coexpressed in activated human T cells.

Published
1990

38. Measurement of the t(t)over-bar production cross section in p(p)over-bar collisions at root s=1.8 TeV

Author

Affolder, T, Akimoto, H, Akopian, A, Albrow, MG, Amaral, P, Amendolia, SR, Amidei, D, Anikeev, K, Antos, J, Apollinari, G, Arisawa, T, Asakawa, T, Ashmanskas, W, Azfar, F, Azzi-Bacchetta, R, Bacchetta, N, Bailey, MW, Bailey, S, de Barbaro, P, Barbaro-Galtieri, A, Barnes, VE, Barnett, BA, Baroiant, S, Barone, M, Bauer, G, Bedeschi, F, Belforte, S, Bell, WH, Bellettini, G, Bellinger, J, Benjamin, D, Bensinger, J, Beretvas, A, Berge, JP, Berryhill, J, Bevensee, B, Bhatti, A, Binkley, M, Bisello, D, Bishai, M, Blair, RE, Blocker, C, Bloom, K, Blumenfeld, B, Blusk, SR, Bocci, A, Bodek, A, Bokhari, W, Bolla, G, Bonushkin, Y, Bortoletto, D, Boudreau, J, Brandl, A, van den Brink, S, Bromberg, C, Brozovic, M, Bruner, N, Buckley-Geer, E, Budagov, J, Budd, HS, Burkett, K, Busetto, G, Byon-Wagner, A, Byrum, KL, Calafiura, P, Campbell, M, Carithers, W, Carlson, J, Carlsmith, D, Caskey, W, Cassada, J, Castro, A, Cauz, D, Cerri, A, Chan, AW, Chang, PS, Chang, PT, Chapman, J, Chen, C, Chen, YC, Cheng, MT, Chertok, M, Chiarelli, G, Chirikov-Zorin, I, Chlachidze, G, Chlebana, F, Christofek, L, Chu, ML, Chung, YS, Ciobanu, CI, Clark, AG, Connolly, A, Conway, J, Cordelli, M, Cranshaw, J, Cronin-Hennessy, D, Cropp, R, Culbertson, R, Dagenhart, D, D'Auria, S, DeJongh, F, Dell'Agnello, S, Dell'Orso, M, Demortier, L, Deninno, M, Derwent, PF, Devlin, T, Dittmann, JR, Donati, S, Done, J, Dorigo, T, Eddy, N, Einsweiler, K, Elias, JE, Engels, E, Erbacher, R, Errede, D, Errede, S, Fan, Q, Feild, RG, Fernandez, JP, Ferretti, C, Field, RD, Fiori, I, Flaugher, B, Foster, GW, Franklin, M, Freeman, J, Friedman, J, Fukui, Y, Furic, I, Galeotti, S, Gallinaro, M, Gao, T, Garcia-Sciveres, M, Garfinkel, AF, Gatti, P, Gay, C, Gerdes, DW, Giannetti, P, Giromini, P, Glagolev, V, Glenzinski, D, Gold, M, Goldstein, J, Gordon, A, Gorelov, I, Goshaw, AT, Gotra, Y, Goulianos, K, Green, C, Grim, G, Gris, P, Groer, L, Grosso-Pilcher, C, Guenther, M, Guillian, G, da Costa, JG, Haas, RM, Haber, C, Hafen, E, Hahn, SR, Hall, C, Handa, T, Handler, R, Hao, W, Happacher, F, Hara, K, Hardman, AD, Harris, RM, Hartmann, F, Hatakeyama, K, Hauser, J, Heinrich, J, Heiss, A, Herndon, M, Hill, C, Hoffman, KD, Holck, C, Hollebeek, R, Holloway, L, Hughes, R, Huston, J, Huth, J, Ikeda, H, Incandela, J, Introzzi, G, Iwai, J, Iwata, Y, James, E, Jones, M, Joshi, U, Kambara, H, Kamon, T, Kaneko, T, Karr, K, Kasha, H, Kato, Y, Keaffaber, TA, Kelley, K, Kelly, M, Kennedy, RD, Kephart, R, Khazins, D, Kikuchi, T, Kilminster, B, Kim, BJ, Kim, DH, Kim, HS, Kim, MJ, Kim, SH, Kim, YK, Kirby, M, Kirk, M, Kirsch, L, Klimenko, S, Koehn, P, Kongeter, A, Kondo, K, Konigsberg, J, Kordas, K, Korn, A, Korytov, A, Kovacs, E, Kroll, J, Kruse, M, Kuhlmann, SE, Kurino, K, Kuwabara, T, Laasanen, AT, Lai, N, Lami, S, Lammel, S, Lamoureux, JI, Lancaster, J, Lancaster, M, Lander, R, Latino, G, LeCompte, T, Lee, AM, Lee, K, Leone, S, Lewis, JD, Lindgren, M, Liu, JB, Liu, YC, Litvintsev, DO, Lobban, O, Lockyer, N, Loken, J, Loreti, M, Lucchesi, D, Lukens, P, Lusin, S, Lyons, L, Lys, J, Madrak, R, Maeshima, K, Maksimovic, P, Malferrari, L, Mangano, M, Mariotti, M, Martignon, G, Martin, A, Matthews, JAJ, Mayer, J, Mazzanti, P, McFarland, KS, McIntyre, P, McKigney, E, Menguzzato, M, Menzione, A, Mesropian, C, Meyer, A, Miao, T, Miller, R, Miller, JS, Minato, H, Miscetti, S, Mishina, M, Mitselmakher, G, Moggi, N, Moore, E, Moore, R, Morita, Y, Moulik, T, Mulhearn, M, Mukherjee, A, Muller, T, Munar, A, Murat, P, Murgia, S, Nachtman, J, Nagaslaev, V, Nahn, S, Nakada, H, Nakaya, T, Nakano, I, Nelson, C, Nelson, T, Neu, C, Neuberger, D, Newman-Holmes, C, Ngan, CYR, Niu, H, Nodulman, L, Nomerotski, A, Oh, SH, Ohmoto, T, Ohsugi, T, Oishi, R, Okusawa, T, Olsen, J, Orejudos, W, Pagliarone, C, Palmonari, F, Paoletti, R, Papadimitriou, V, Pappas, SP, Partos, D, Patrick, J, Pauletta, G, Paulini, M, Paus, C, Pescara, L, Phillips, TJ, Piacentino, G, Pitts, KT, Pompos, A, Pondrom, L, Pope, G, Popovic, M, Prokoshin, F, Proudfoot, J, Ptohos, F, Pukhov, O, Punzi, G, Ragan, K, Rakitine, A, Reher, D, Reichold, A, Ribon, A, Riegler, W, Rimondi, F, Ristori, L, Riveline, M, Robertson, WJ, Robinson, A, Rodrigo, T, Rolli, S, Rosenson, L, Roser, R, Rossin, R, Roy, A, Safonov, A, St Denis, R, Sakumoto, WK, Saltzberg, D, Sanchez, C, Sansoni, A, Santi, L, Sato, H, Savard, P, Schlabach, P, Schmidt, EE, Schmidt, MP, Schmitt, M, Scodellaro, L, Scott, A, Scribano, A, Segler, S, Seidel, S, Seiya, Y, Semenov, A, Semeria, F, Shah, T, Shapiro, MD, Shepard, PF, Shibayama, T, Shimojima, M, Shochet, M, Sidoti, A, Siegrist, J, Sill, A, Sinervo, P, Singh, P, Slaughter, AJ, Sliwa, K, Smith, C, Snider, FD, Solodsky, A, Spalding, J, Speer, T, Sphicas, P, Spinella, F, Spiropulu, M, Spiegel, L, Steele, J, Stefanini, A, Strologas, J, Strumia, F, Stuart, D, Sumorok, K, Suzuki, T, Takano, T, Takashima, R, Takikawa, K, Tamburello, P, Tanaka, M, Tannenbaum, B, Taylor, W, Tecchio, M, Tesarek, R, Teng, PK, Terashi, K, Tether, S, Thompson, AS, Thurman-Keup, R, Tipton, P, Tkaczyk, S, Toback, D, Tollefson, K, Tollestrup, A, Toyoda, H, Trischuk, W, de Troconiz, JF, Tseng, J, Turini, N, Ukegawa, F, Vaiciulis, T, Valls, J, Vejcik, S, Velev, G, Vidal, R, Vilar, R, Volobouev, I, Vucinic, D, Wagner, RG, Wagner, RL, Wahl, J, Wallace, NB, Walsh, AM, Wang, C, Wang, MJ, Watanabe, T, Waters, D, Watts, T, Webb, R, Wenzel, H, Wester, WC, Wicklund, AB, Wicklund, E, Wilkes, T, Williams, HH, Wilson, P, Winer, BL, Winn, D, Wolbers, S, Wolinski, D, Wolinski, J, Wolinski, S, Worm, S, Wu, X, Wyss, J, Yagil, A, Yao, W, Yeh, GP, Yeh, P, Yoh, J, Yosef, C, Yoshida, T, Yu, I, Yu, S, Yu, Z, Zanetti, A, Zetti, F, Zucchelli, S, and Collaboration, CDF

Subjects
HADRONIC COLLISIONS, COLLIDER DETECTOR, (P)OVER-BAR-P COLLISIONS, TOP-QUARK PRODUCTION, ALPHA-S CALCULATION, FINAL-STATES, EVENTS, CDF, FERMILAB, ORDER, High Energy Physics::Phenomenology, SILICON VERTEX DETECTOR, T%28B%29OVER-BAR%22">Q(Q)OVER-BAR->T(B)OVER-BAR, PHYSICS, High Energy Physics::Experiment, QC
Abstract

We update the measurement of the t (t) over bar production cross section using the CDF detector at the Fermilab Tevatron. This measurement uses t (t) over bar decays to the final states e + nu + jets and mu + nu + jets. We search for b quarks from t decays via secondary-vertex identification or the identification of semileptonic decays of the b and cascade c quarks. The background to the t (t) over bar production is determined primarily through a Monte Carlo simulation. However, we calibrate the simulation and evaluate its uncertainty using several independent data samples. For a top quark mass of 175 GeV/c(2), we measure sigma (t (t) over bar)-=5.1 +/- 1.5 pb and sigma (t (t) over bar)=9.2 +/- 4.3 pb using the secondary vertex and the lepton tagging algorithms, respectively. Finally, we combine these results with those from other t (t) over bar decay channels and obtain sigma (t (t) over bar)-= 6.5 (+1.7)(-1.4)pb

Published
1998

41. A SCID patient reconstituted with HLA-incompatible fetal stem cells as a model for studying transplantation tolerance

Author

Roncarolo, M. G., Bacchetta, R., Bigler, M., Touraine, J. L., de Vries, J. E., Spits, H., and Other departments

Abstract

We studied a severe combined immunodeficiency (SCID) patient who received transplantations with completely HLA-mismatched fetal liver and thymus from two different donors. The patient is now 14 years old, healthy and shows normal immunoresponses to recall antigens. His T cells are of donor origin, whereas the monocytes, B cells, and natural killer (NK) cells are of the recipient. The successful immunological reconstitution raised questions as to how T and B cells could collaborate across an HLA barrier and how tolerance was achieved. We have shown that tetanus toxin-specific T cell clones isolated from this patient recognized this antigen in the context of host and not of donor HLA-DR, indicating that those cells were educated in the host environment, presumably the thymus. Despite this, an unexpectedly high frequency of host-reactive clones was found that could recognize MHC antigens of the host. It was particularly striking that CD8+ CTL clones were obtained that recognized class I MHC antigens on the host cells. Nevertheless, the patient did not show any sign of acute or chronic graft-versus-host disease (GVHD). These data indicated that no or only incomplete clonal deletion had taken place in this patient and suggest the presence of a peripheral suppressor mechanism. Thus far, we have no indication for the existence of suppressor T cells. Inasmuch as it was found that host-reactive T cells fail to produce IL-4, which is exceptional for CD4+ T cells, we are exploring the possibility that abnormal cytokine production patterns of host-reactive T cells are associated with suppression of these cells in vivo

Published
1991

42. Anti-infective prophylaxis for primary immunodeficiencies: what is done in Italian Primary Immunodeficiency Network centers (IPINet) and review of the literature

Author

Moschese, V., Martire, B., Soresina, A., Chini, L., Graziani, S., Monteferrario, E., Bacchetta, R., Cancrini, C., Fiorilli, M., Gambineri, E., Pession, A., Pignata, C., Quinti, I., Rondelli, R., PAOLO ROSSI, Ugazio, A. G., Plebani, A., Pietrogrande, M. C., Moschese, V., Martire, B., Soresina, A., Chini, L., Graziani, S., Monteferrario, E., Bacchetta, R., Cancrini, C., Fiorilli, M., Gambineri, E., Pession, A., Pignata, Claudio, Quinti, I., Rondelli, R., Rossi, P., Ugazio, A. G., Plebani, A., Pietrogrande, M. C., Moschese V, Martire B, Soresina A, Chini L, Graziani S, Monteferrario E, Bacchetta R, Cancrini C, Fiorilli M, Gambineri E, Pession A, Pignata C, Quinti I, Rondelli R, Rossi P, Ugazio AG, Plebani A, and Pietrogrande MC

Subjects
Settore MED/38 - Pediatria Generale e Specialistica, Humans, Granulomatous Disease, Chronic, X-Linked Combined Immunodeficiency Diseases, Antibiotic Prophylaxis, Immunologic Deficiency Syndromes, IgA Deficiency, DiGeorge Syndrome, Common Variable Immunodeficiency, CHRONIC GRANULOMATOUS-DISEASE, X-LINKED AGAMMAGLOBULINEMIA, WISKOTT-ALDRICH-SYNDROME, TERM-FOLLOW-UP, LARGE COHORT, CLINICAL IMMUNOLOGY, ANTIBODY DEFICIENCY, T-CELLS, PULMONARY, HYPOGAMMAGLOBULINEMIA, ipinet-aieop, primary immunodeficiencies, antimicrobial prophylaxis, infections, Granulomatous Disease, Chronic
Abstract

Primary immunodeficiencies (PIDs) are rare diseases characterized by an increased susceptibility to infections. Early diagnosis and appropriate treatment are critical for reducing morbidity and mortality. Based on available data, the efficacy of antibiotic administration for the prophylaxis of infections remains uncertain, and recommendations supporting this practice are poor. The use of antimicrobial prophylaxis is mainly based on single institution-specific experience without controlled measurements of patient safety and quality health outcomes. To address this issue an Italian Network on Primary Immunodeficiencies (IPINet) has been set up in 1999 within the Italian Association of Pediatric Hematology and Oncology (AIEOP) to increase the awareness of these disorders among physicians. Further, diagnostic and treatment guideline recommendations have been established to standardize the best clinical assistance to all patients, including antibiotic prophylaxis, and for a national epidemiologic monitoring of PIDs. The aim of this review is not only to give a scientific update on the use of antimicrobial prophylaxis in selected congenital immunological disorders but also to draw a picture of this practice in the context of the Italian Primary Immunodeficiency Network (IPINet). Controlled multicenter studies are necessary to establish if, when and how you should start an efficacious antimicrobial prophylaxis.

43. Antigen recognition by MHC-incompatible cells of a human mismatched chimera

Author

RONCAROLO , MARIA GRAZIA, Yssel, H., Touraine, J. L., Bacchetta, R., Gebuhrer, L., De Vries, J. E. , Spits, Roncarolo, MARIA GRAZIA, Yssel, H., Touraine, J. L., Bacchetta, R., Gebuhrer, L., De, Vrie, and J. E., Spits

Abstract

Tetanus toxin (TT)-specific T cell clones of donor origin were obtained from a patient with severe combined immunodeficiency (SCID) successfully reconstituted by transplantation of allogeneic fetal liver and thymus cells from two different donors performed 10 yr ago. A series of these clones recognized TT in the context of 'allo' class II HLA determinants expressed by recipient APC. The restriction element of two T cell clones with the HLA phenotype of the first donor (HLA-DR1,8) and one T cell clone with the HLA phenotype of the second transplant (HLA-DR3,9) was HLA-DR4 of the recipient, whereas other T cell clones derived from the second transplant recognized TT in the context of HLA-DR5 of the recipient's APC. These latter T cell clones were not able to proliferate in response to TT when autologous APC were used. These data demonstrate that recipient and donor cells having different HLA phenotypes could cooperate across the allogeneic barrier and that MHC restriction of antigen (Ag) recognition is independent from the MHC genotype of the T cells but is influenced by the environment in which the T cells mature. We also isolated T cell clones that were able to recognize processed TT presented by all allogeneic EBV cell lines tested, indicating that the Ag specificity of these clones was not restricted by a particular class II MHC molecule. The Ag-specific proliferative response of one of these clones could be blocked by anti-class II MHC mAbs. These results demonstrate that in addition to Ag recognition in the context of specific class II MHC Ags, other types of Ag-specific responses may occur in this human chimera. It is not clear whether this 'allo' plus Ag recognition is the result of education of transplanted fetal cells in the host thymus. Taking into consideration our previous findings indicating that alloreactive T cell clones specific for the recipient cells could be isolated in vitro from the PBL of the same patient, our data suggest that the mechanism for deletion of self-reactive clones and the generation of MHC-restricted responses are different.

Published
1988

44. CITOCHINE E VACCINAZIONI

Author

RONCAROLO , MARIA GRAZIA, BACCHETTA R., AUTORI VARI, Roncarolo, MARIA GRAZIA, and Bacchetta, R.

47. Treatment with rapamycin can restore regulatory T-cell function in IPEX patients

Author

Pier Alberto Testoni, Rosalia Curto, Federica Barzaghi, Olaf Neth, Maria Grazia Roncarolo, Alessandro Aiuti, Francesca Tucci, Claudia Sartirana, Laura Passerini, Rosa Bacchetta, Vito Lampasona, Graziano Barera, Daniele Zama, Maria Pia Cicalese, Elena Bazzigaluppi, Manfred Hoenig, Ansgar Schulz, Alberto Mariani, Sven Olek, Luca Albarello, Ivana Rabbone, Emanuele Bosi, Markus G. Seidel, Passerini, L., Barzaghi, F., Curto, R., Sartirana, C., Barera, G., Tucci, F., Albarello, L., Mariani, A., Testoni, P. A., Bazzigaluppi, E., Bosi, E., Lampasona, V., Neth, O., Zama, D., Hoenig, M., Schulz, A., Seidel, M. G., Rabbone, I., Olek, S., Roncarolo, M. G., Cicalese, M. P., Aiuti, A., Bacchetta, R., Passerini L., Barzaghi F., Curto R., Sartirana C., Barera G., Tucci F., Albarello L., Mariani A., Testoni P.A., Bazzigaluppi E., Bosi E., Lampasona V., Neth O., Zama D., Hoenig M., Schulz A., Seidel M.G., Rabbone I., Olek S., Roncarolo M.G., Cicalese M.P., Aiuti A., and Bacchetta R.

Subjects
Male, 0301 basic medicine, regulatory T cell, medicine.medical_treatment, Hematopoietic stem cell transplantation, Lymphocyte Activation, medicine.disease_cause, T-Lymphocytes, Regulatory, regulatory T cells, Autoimmunity, Immunosuppressive Agent, 0302 clinical medicine, Cell Movement, IPEX, Immunology and Allergy, Sirolimu, Child, Cells, Cultured, autoimmunity, FOXP3, Forkhead Transcription Factors, Genetic Diseases, X-Linked, hemic and immune systems, EBI3, Regulatory T cells, suppression, Minor Histocompatibility Antigen, medicine.anatomical_structure, Immune System Diseases, mTOR, Immunosuppressive Agents, Human, Diarrhea, Ebi3, Immune System Disease, Regulatory T cell, Immunology, chemical and pharmacologic phenomena, Minor Histocompatibility Antigens, 03 medical and health sciences, TIGIT, Glucocorticoid-Induced TNFR-Related Protein, Immune Tolerance, medicine, Humans, GITR, Sirolimus, rapamycin, business.industry, Interleukins, Forkhead Transcription Factor, Interleukin, IPEX syndrome, medicine.disease, Diabetes Mellitus, Type 1, 030104 developmental biology, Gene Expression Regulation, CTLA-4, Mutation, Cancer research, business, 030215 immunology
Abstract

[Background] Immune-dysregulation, polyendocrinopathy, enteropathy, X-linked (IPEX) syndrome is a lethal disease caused by mutations in a transcription factor critical for the function of thymus-derived regulatory T (Treg) cells (ie, FOXP3), resulting in impaired Treg function and autoimmunity. At present, hematopoietic stem cell transplantation is the therapy of choice for patients with IPEX syndrome. If not available, multiple immunosuppressive regimens have been used with poor disease-free survival at long-term follow-up. Rapamycin has been shown to suppress peripheral T cells while sparing Treg cells expressing wild-type FOXP3, thereby proving beneficial in the clinical setting of immune dysregulation. However, the mechanisms of immunosuppression selective to Treg cells in patients with IPEX syndrome are unclear., [Objective] We sought to determine the cellular and molecular basis of the clinical benefit observed under rapamycin treatment in 6 patients with IPEX syndrome with different FOXP3 mutations., [Methods] Phenotype and function of FOXP3-mutated Treg cells from rapamycin-treated patients with IPEX syndrome were tested by flow cytometry and in vitro suppression assays, and the gene expression profile of rapamycin-conditioned Treg cells by droplet-digital PCR., [Results] Clinical and histologic improvements in patients correlated with partially restored Treg function, independent of FOXP3 expression or Treg frequency. Expression of TNF-receptor-superfamily-member 18 (TNFRSF18, glucocorticoid-induced TNF-receptor–related) and EBV-induced-3 (EBI3, an IL-35 subunit) in patients’ Treg cells increased during treatment as compared with that of Treg cells from untreated healthy subjects. Furthermore inhibition of glucocorticoid-induced TNF-receptor–related and Ebi3 partially reverted in vitro suppression by in vivo rapamycin-conditioned Treg cells., [Conclusions] Rapamycin is able to affect Treg suppressive function via a FOXP3-independent mechanism, thus sustaining the clinical improvement observed in patients with IPEX syndrome under rapamycin treatment.

Published
2020
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48. Forkhead box protein 3 (FOXP3) mutations lead to increased TH17 cell numbers and regulatory T-cell instability

Author

Federica Barzaghi, Sara Di Nunzio, Sven Olek, Mario Amendola, Rosa Bacchetta, Maria G. Roncarolo, Mario Abinun, Alberto Tommasini, Marco Cipolli, Massimiliano Cecconi, Laura Passerini, Luigi Naldini, Silvia Vignola, Sophie Hambleton, Luisa Guidi, Approches génétiques intégrées et nouvelles thérapies pour les maladies rares (INTEGRARE), Université d'Évry-Val-d'Essonne (UEVE)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris-Saclay-Généthon, Passerini, L, Olek, S, Di Nunzio, S, Barzaghi, F, Hambleton, S, Abinun, M, Tommasini, A, Vignola, S, Cipolli, M, Amendola, M, Naldini, L, Guidi, L, Cecconi, M, Roncarolo, M G, Bacchetta, R, Naldini, Luigi, Roncarolo, MARIA GRAZIA, and Bacchetta, R.

Subjects
Male, [SDV.BIO]Life Sciences [q-bio]/Biotechnology, Regulatory T cell, Immunology, Cell, Autoimmune/genetics, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Biology, Forkhead Transcription Factors/genetics, Gene Expression Regulation/genetics, Genetic Diseases, X-Linked/genetics, Humans, Immunologic Deficiency Syndromes/genetics, Polyendocrinopathies, medicine, Forkhead Box, Immunology and Allergy, Polyendocrinopathies, Autoimmune, ComputingMilieux_MISCELLANEOUS, Immunologic Deficiency Syndromes, FOXP3, Forkhead Transcription Factors, Genetic Diseases, X-Linked, [SDV.MHEP.HEM]Life Sciences [q-bio]/Human health and pathology/Hematology, Intestinal Diseases, medicine.anatomical_structure, Gene Expression Regulation, Mutation (genetic algorithm), Mutation, Cancer research
Abstract

International audience

Published
2011
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49. Clinical heterogeneity and diagnostic delay of autoimmune polyendocrinopathy-candidiasis-ectodermal dystrophy syndrome

Author

Alberto Vitali, Federica Ortolani, Roberto Rusconi, Srdjan Pasic, Rosa Bacchetta, Fabio Buzi, Donatella Capalbo, Annarosa Soresina, Andrea Taddio, Vassilios Lougaris, Claudio Pignata, Lucia Dora Notarangelo, Mariacarolina Salerno, Małgorzata Pac, Giorgio Radetti, Monique de Vroede, Giuseppe Maggiore, Silvana Martino, Sanal Ozden, Raffaele Badolato, Nella Augusta Greggio, Giovanna Weber, Cinzia Mazza, Alessandro Plebani, Sara Sebnem Kilic, Luigi D. Notarangelo, Mazza, C., Buzi, Paola, Ortolani, F., Karabchuk, Vitali, Notarangelo, L. D., Weber, G., Bacchetta, R., Soresina, A., Lougaris, V., Greggio, N., Taddio, A., Pasic, S., de Vroede, M., Pac, M., Kilic, S. S., Ozden, S., Rusconi, R., Martino, S., Capalbo, D., Salerno, M., Pignata, C., Radetti, G., Maggiore, G., Plebani, A., Notarangelo, Ld., Badolato, R., Çocuk Sağlığı ve Hastalıkları, Buzi, F., Vitali, A., Greggio, N. A., Taddio, Andrea, Uludağ Üniversitesi/Tıp Fakültesi/Pediatri Anabilim Dalı., Kılıç, Sara Şebnem, AAH-1658-2021, Mazza, C, Buzi, F, Ortolani, F, Vitali, A, Notarangelo, Ld, Weber, Giovanna, Bacchetta, R, Soresina, A, Lougaris, V, Greggio, Na, Taddio, A, Pasic, S, de Vroede, M, Pac, M, Kilic, S, Ozden, S, Rusconi, R, Martino, S, Capalbo, D, Salerno, M, Pignata, C, Radetti, G, Maggiore, G, and Plebani, A

Subjects
Time Factors, Autoimmunity, Endocrinopathy, Disease, Type-1, medicine.disease_cause, Mucocutaneous Candidiasis, Homozygosity, Genetic heterogeneity, 0302 clinical medicine, Immunology and Allergy, Autoimmune polyendocrinopathy candidiasis ectodermal dystrophy, Chronic mucocutaneous candidiasis, Child, Polyendocrinopathies, Autoimmune, Priority journal, 0303 health sciences, Heterozygosity, Candidiasis, Genetic analysis, Homozygote, Autoimmune polyendocrinopathy, Middle Aged, Autoimmune regulator, Common, 3. Good health, Child, Preschool, APECED, diagnostic tool, children, Mutations, diagnostic tool, Human, Adult, Heterozygote, animal structures, Adolescent, Clinical article, Immunology, Socio-culturale, 030209 endocrinology & metabolism, APECED, DIAGNOSIS, DIAGNOSIS, Article, 03 medical and health sciences, Young Adult, children, medicine, Humans, Gene mutation, Preschool, Autoantibodies, 030304 developmental biology, Gene amplification, Hepatitis, business.industry, Protein, Dystrophy, Disease type-ı, medicine.disease, Polyendocrinopathies, Autoimmune regulator protein, Preschool child, Regulator aire gene, Type 1 Autoimmune Polyendocrinopathy Syndrome, Regulator, Central Tolerance, Mutation, Genetic association, School child, business, Autoimmune, APECED
Abstract

Autoimmune polyendocrinopathy-candidiasis-ectodermal dystrophy (APECED) is a rare autosomal recessive organ-specific autoimmune disorder that is characterized by a variable combination of (i) chronic mucocutaneous candidiasis, (ii) polyendocrinopathy and/or hepatitis and (iii) dystrophy of the dental enamel and nails. We analyzed the AIRE (autoimmune regulator) gene in subjects who presented any symptom that has been associated with APECED, including candidiasis and autoimmune endocrinopathy. We observed that 83.3% of patients presented at least two of the three typical manifestations of APECED, while the remaining 16.7% of patients showed other signs of the disease. Analysis of the genetic diagnosis of these subjects revealed that a considerable delay occurs in the majority of patients between the appearance of symptoms and the diagnosis. Overall, the mean diagnostic delay in our patients was 10.2 years. These results suggest that molecular analysis of AIRE should be performed in patients with relapsing mucocutaneous candidiasis for early identification of APECED. Fondazione Cariplo Fondazione Telethon European Commission (FP7 HLH-cure) (201461) Ministry of Education, Universities and Research (MIUR) Research Projects of National Relevance (PRIN) (2007ACZMMZ_005) Seventh Framework Programme (201461)

Published
2011

50. Ectopic FOXP3 Expression Preserves Primitive Features Of Human Hematopoietic Stem Cells While Impairing Functional T Cell Differentiation

Author

Maria Grazia Roncarolo, Rosa Bacchetta, Laura Passerini, Fabio Russo, Luigi Naldini, F. R. Santoni de Sio, M. M. Valente, Santoni De Sio, F. R., Passerini, L., Valente, M. M., Russo, F., Naldini, L., Roncarolo, M. G., and Bacchetta, R.

Subjects
0301 basic medicine, Regulatory T cell, Cellular differentiation, T-Lymphocytes, lcsh:Medicine, Biology, Article, Immune tolerance, 03 medical and health sciences, Mice, medicine, Animals, Humans, lcsh:Science, Cells, Cultured, Regulation of gene expression, Multidisciplinary, Animal, lcsh:R, FOXP3, Forkhead Transcription Factors, Hematopoietic Stem Cell, Cell Differentiation, hemic and immune systems, Anatomy, Forkhead Transcription Factor, IPEX syndrome, medicine.disease, Hematopoietic Stem Cells, Cell biology, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, T-Lymphocyte, lcsh:Q, Stem cell, Human
Abstract

FOXP3 is the transcription factor ruling regulatory T cell function and maintenance of peripheral immune tolerance, and mutations in its coding gene causes IPEX autoimmune syndrome. FOXP3 is also a cell-cycle inhibitor and onco-suppressor in different cell types. In this work, we investigate the effect of ectopic FOXP3 expression on HSC differentiation and we challenged this approach as a possible HSC-based gene therapy for IPEX. FOXP3-expressing HSC showed reduced proliferation ability and increased maintenance of primitive markers in vitro in both liquid and OP9-ΔL1 co-cultures. When transplanted into immunodeficient mice, FOXP3-expressing HSC showed significantly enhanced engraftment ability. This was due to a pronounced increase in the frequency of repopulating cells, as assessed by extreme limiting dilution assay. Likely underlying the increased repopulating ability, FOXP3 expressing HSC showed significantly enhanced expression of genes controlling stemness features. However, peripheral T cells developed in the FOXP3-humanized mice were quantitatively reduced and hyporesponsive to cytokine and polyclonal stimulation. Our findings reveal unpredicted effects of FOXP3 in the biology of HSC and may provide new tools to manipulate primitive features in HSC for clinical applications. Moreover, they formally prove the need of preserving endogenous FOXP3 regulation for an HSC-based gene therapy approach for IPEX syndrome.

Published
2017
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