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1. Exonic knockout and knockin gene editing in hematopoietic stem and progenitor cells rescues RAG1 immunodeficiency

Author

Castiello, M, Brandas, C, Ferrari, S, Porcellini, S, Sacchetti, N, Canarutto, D, Draghici, E, Merelli, I, Barcella, M, Pelosi, G, Vavassori, V, Varesi, A, Jacob, A, Scala, S, Basso Ricci, L, Paulis, M, Strina, D, Di Verniere, M, Sergi Sergi, L, Serafini, M, Holland, S, Bergerson, J, De Ravin, S, Malech, H, Pala, F, Bosticardo, M, Brombin, C, Cugnata, F, Calzoni, E, Crooks, G, Notarangelo, L, Genovese, P, Naldini, L, Villa, A, Castiello, Maria Carmina, Brandas, Chiara, Ferrari, Samuele, Porcellini, Simona, Sacchetti, Nicolò, Canarutto, Daniele, Draghici, Elena, Merelli, Ivan, Barcella, Matteo, Pelosi, Gabriele, Vavassori, Valentina, Varesi, Angelica, Jacob, Aurelien, Scala, Serena, Basso Ricci, Luca, Paulis, Marianna, Strina, Dario, Di Verniere, Martina, Sergi Sergi, Lucia, Serafini, Marta, Holland, Steven M., Bergerson, Jenna R. E., De Ravin, Suk See, Malech, Harry L., Pala, Francesca, Bosticardo, Marita, Brombin, Chiara, Cugnata, Federica, Calzoni, Enrica, Crooks, Gay M., Notarangelo, Luigi D., Genovese, Pietro, Naldini, Luigi, Villa, Anna, Castiello, M, Brandas, C, Ferrari, S, Porcellini, S, Sacchetti, N, Canarutto, D, Draghici, E, Merelli, I, Barcella, M, Pelosi, G, Vavassori, V, Varesi, A, Jacob, A, Scala, S, Basso Ricci, L, Paulis, M, Strina, D, Di Verniere, M, Sergi Sergi, L, Serafini, M, Holland, S, Bergerson, J, De Ravin, S, Malech, H, Pala, F, Bosticardo, M, Brombin, C, Cugnata, F, Calzoni, E, Crooks, G, Notarangelo, L, Genovese, P, Naldini, L, Villa, A, Castiello, Maria Carmina, Brandas, Chiara, Ferrari, Samuele, Porcellini, Simona, Sacchetti, Nicolò, Canarutto, Daniele, Draghici, Elena, Merelli, Ivan, Barcella, Matteo, Pelosi, Gabriele, Vavassori, Valentina, Varesi, Angelica, Jacob, Aurelien, Scala, Serena, Basso Ricci, Luca, Paulis, Marianna, Strina, Dario, Di Verniere, Martina, Sergi Sergi, Lucia, Serafini, Marta, Holland, Steven M., Bergerson, Jenna R. E., De Ravin, Suk See, Malech, Harry L., Pala, Francesca, Bosticardo, Marita, Brombin, Chiara, Cugnata, Federica, Calzoni, Enrica, Crooks, Gay M., Notarangelo, Luigi D., Genovese, Pietro, Naldini, Luigi, and Villa, Anna

Abstract

Recombination activating genes (RAGs) are tightly regulated during lymphoid differentiation, and their mutations cause a spectrum of severe immunological disorders. Hematopoietic stem and progenitor cell (HSPC) transplantation is the treatment of choice but is limited by donor availability and toxicity. To overcome these issues, we developed gene editing strategies targeting a corrective sequence into the human RAG1 gene by homology-directed repair (HDR) and validated them by tailored two-dimensional, three-dimensional, and in vivo xenotransplant platforms to assess rescue of expression and function. Whereas integration into intron 1 of RAG1 achieved suboptimal correction, in-frame insertion into exon 2 drove physiologic human RAG1 expression and activity, allowing disruption of the dominant-negative effects of unrepaired hypomorphic alleles. Enhanced HDR-mediated gene editing enabled the correction of human RAG1 in HSPCs from patients with hypomorphic RAG1 mutations to overcome T and B cell differentiation blocks. Gene correction efficiency exceeded the minimal proportion of functional HSPCs required to rescue immunodeficiency in Rag1(-/- )mice, supporting the clinical translation of HSPC gene editing for the treatment of RAG1 deficiency.

Published
2024

2. Zeus Magnets Construction Status Report

Author

Oliva, A. Bonito, Bordin, F., Dormicchi, O., Gaggero, G., Losasso, M., Penco, R., Valle, N., Bruzzese, R., Spadoni, M., Sacchetti, N., Lin, Q., Sekiguchi, T., editor, and Shimamoto, S., editor

Published
1990
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3. Testing of full size high current superconductors in SULTAN III

Author

Blau, B., Rohleder, I., Vecsey, G., Pasotti, G., Ricci, M.V., Sacchetti, N., Bruzzone, P., Katheder, H., Mitchell, N., Bessette, D., and Duchateau, J.L.

Subjects
Superconductors -- Research, Testing laboratories -- Research, Business, Electronics, Electronics and electrical industries
Abstract

The high field test facility SULTAN III in operation at PSI/Switzerland tests full size industrial prototype superconductors for fusion applications such as ITER. The facility provides a background field of up to 11 T over a length of 58 cm. A 50 kA superconducting transformer works as a very low noise current source which allows a criterion of 0.1 [micro]V/cm to determine the superconducting to normal transition. Three 3.6 m long cable-in-conduit conductors based on both NbTi and [Nb.sub.3]Sn, developed by different manufacturers, suitable for the central solenoid and toroidal field coils of ITER, have been tested so far. This paper presents the results of extensive measurements of critical current and current sharing temperature of the [Nb.sub.3]Sn conductors in the 8-11 T range for temperatures between 4.5 K and 11 K. Voltage versus current curves have been analyzed with respect to the n value. The manufacturing of a high quality joint between two [Nb.sub.3]Sn conductors after heat treatment is reported, together with some measurements of the joint resistance.

Published
1994

4. First performance tests of the 12T split coil test facility SULTAN III

Author

Blau, B., Aebli, E., Jakob, B., Pasztor, G., Rohleder, I., Trajkovic, D., Vecsey, G., Vogel, M., Corte, A. Della, Pasotti, G., Ricci, M., Sacchetti, N., Spadoni, M., and Balsamo, E.P.

Subjects
Testing laboratories -- Reports, Superconductivity -- Research, Business, Electronics, Electronics and electrical industries
Abstract

The Supraleitner Testanlage is a test facility at the Paul Scherrer Institute, Switzerland for validating full scale superconductors used as magnetic elements in fusion reactors. It contains a split coil system that generates magnetic fields of 12 T and more for testing superconductors with rated currents up to 50 kA between 4.5-7 K. A description of its first operational attempt is presented.

Published
1993

5. FINAL TESTS OF THE SULTAN 12T FACILITY IN THE SPLIT COIL CONFIGURATION

Author

BALSAMO, E.P., primary, CORTE, A. DELLA, additional, PASOTTI, G., additional, RICCI, M.V., additional, SPADONI, M., additional, SACCHETTI, N., additional, AEBLI, E., additional, BLAU, B., additional, JAKOB, B., additional, PASZTOR, G., additional, ROHLEDER, I., additional, VÉCSEY, G., additional, and VOGEL, M., additional

Published
1993
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6. Efficacy of lentivirus-mediated gene therapy in an Omenn syndrome recombination-activating gene 2 mouse model is not hindered by inflammation and immune dysregulation

Author

Capo, V, Castiello, M, Fontana, E, Penna, S, Bosticardo, M, Draghici, E, Poliani, L, Sergi Sergi, L, Rigoni, R, Cassani, B, Zanussi, M, Carrera, P, Uva, P, Dobbs, K, Sacchetti, N, Notarangelo, L, van Til, N, Wagemaker, G, Villa, A, Castiello, MC, Poliani, LP, Notarangelo, LD, van Til N. P., Capo, V, Castiello, M, Fontana, E, Penna, S, Bosticardo, M, Draghici, E, Poliani, L, Sergi Sergi, L, Rigoni, R, Cassani, B, Zanussi, M, Carrera, P, Uva, P, Dobbs, K, Sacchetti, N, Notarangelo, L, van Til, N, Wagemaker, G, Villa, A, Castiello, MC, Poliani, LP, Notarangelo, LD, and van Til N. P.

Abstract

Background: Omenn syndrome (OS) is a rare severe combined immunodeficiency associated with autoimmunity and caused by defects in lymphoid-specific V(D)J recombination. Most patients carry hypomorphic mutations in recombination-activating gene (RAG) 1 or 2. Hematopoietic stem cell transplantation is the standard treatment; however, gene therapy (GT) might represent a valid alternative, especially for patients lacking a matched donor. Objective: We sought to determine the efficacy of lentiviral vector (LV)–mediated GT in the murine model of OS (Rag2 R229Q/R229Q ) in correcting immunodeficiency and autoimmunity. Methods: Lineage-negative cells from mice with OS were transduced with an LV encoding the human RAG2 gene and injected into irradiated recipients with OS. Control mice underwent transplantation with wild-type or OS-untransduced lineage-negative cells. Immunophenotyping, T-dependent and T-independent antigen challenge, immune spectratyping, autoantibody detection, and detailed tissue immunohistochemical analyses were performed. Results: LV-mediated GT allowed immunologic reconstitution, although it was suboptimal compared with that seen in wild-type bone marrow (BM)−transplanted OS mice in peripheral blood and hematopoietic organs, such as the BM, thymus, and spleen. We observed in vivo variability in the efficacy of GT correlating with the levels of transduction achieved. Immunoglobulin levels and T-cell repertoire normalized, and gene-corrected mice responded properly to challenges in vivo. Autoimmune manifestations, such as skin infiltration and autoantibodies, dramatically improved in GT mice with a vector copy number/genome higher than 1 in the BM and 2 in the thymus. Conclusions: Our data show that LV-mediated GT for patients with OS significantly ameliorates the immunodeficiency, even in an inflammatory environment.

Published
2018

7. The INFN Eloisatron Project: European Long Intersecting Storage Accelerator

Author

Aglietta, C., Alberini, K., Badino, G., Bari, G., Basile, M., Bassetti, M., Berbiers, J., Bertin, A., Boschi, E., Braginski, V., Bruzzese, R., Cabibbo, N., Romeo, G. Cara, Casaccia, R., Castagnoli, C., Castellina, A., Castelvetri, A., Cifarelli, L., Cindolo, F., Civita, M., Contin, A., D’Ali, G., Dardo, M., Del Papa, C., de Sabbata, V., Ferrario, L., Fulgione, W., Galassini, S., Galeotti, P., Gasperini, M., Giusti, P., Goldoni, R., Iacobucci, G., Laakso, I., Leo, A. R., Leo, M., Luches, G., Maccarrone, G., Marino, A., Massam, T., Melnikov, V. N., Meunier, R., Motta, F., Nania, R., Nassissi, V., Navarra, G., Palmonari, F., Papini, G., Passotti, G., Pelfer, P., Pocci, G., Prisco, G., Puglisi, M., Ricci, M., Rinaldi, G., Rizzuto, C., Rohrbach, F., Rotelli, P., Saavedra, O., Sacchetti, N., Sartorelli, G., Soliani, G., Spadoni, M., Steuer, M., Susinno, G., Tazzari, S., Thorne, K., Torelli, G., Trinchero, G. C., Vallania, P., Venturi, G., Vernetto, S., Villa, F., Vitale, A., Votano, L., Willutzky, M., Zichichi, A., Zichichi, Antonino, editor, and Villa, Francesco, editor

Published
1988
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11. A CONDUCTOR DESIGN FOR NET MACHINE

Author

Bruzzese, R., primary, Catitti, A., additional, Cerreta, R., additional, Della Corte, A., additional, Pasotti, G., additional, Ricci, M.V., additional, Sacchetti, N., additional, and Spadoni, M., additional

Published
1988
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14. First performance test of the 12 T split coil test facility SULTAN III

Author

Blau, B., primary, Aebli, E., additional, Jakob, B., additional, Pasztor, G., additional, Rohleder, I., additional, Trajkovic, D., additional, Vecsey, G., additional, Vogel, M., additional, Della Corte, A., additional, Pasotti, G., additional, Ricci, M., additional, Sacchetti, N., additional, Spadoni, M., additional, and Balsamo, E.P., additional

Published
1993
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24. Superconducting Nb3Sn diffusion layers

Author

Pasotti, G., Ricci, M. V., Sacchetti, N., Sacerdoti, G., and Spadoni, M.

Abstract

In the present work an experimental apparatus for the production of Nb3Sn superconducting ribbon is described. The fabrication method for these ribbons takes advantage of the diffusion process of tin into niobium. We give also some details of the technique by which the superconducting properties of Nb3Sn have been tested. A number of preliminary experimental results are discussed with the purpose of pointing out the main fabrication parameters which influence the superconducting properties. Finally future developments of this research program are outlined.

Published
1971
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29. ZEUS, A DETECTOR FOR HERA: LETTER OF INTENT

Author

Edwards, K., Kapitza, H., Smith, G., Conetti, S., Corriveau, F., Hamel, L. A., Leroy, C., Marchionni, A., Nilsson, A., Patel, P., Stairs, D., Bailey, David C., Bracker, Stephen B., Hartner, G., Kumar, R., Levman, G., Luste, G., Macfarlane, D., Martin, J., Orr, R., Prentice, J., Stacey, B., Yoon, T. S., Frisken, William R., Fukunaga, C., Bock, B., Diekmann, B., Hartmann, H., Heinloth, K., Jakob, H. P., Kolanoski, H., Odingen, R., Paul, E., Sauerwein, R., Schlosser, A., Wedemeyer, R., Anders, B., Bernardi, E., Drews, G., Fohrmann, R., Gather, K., Hultschig, H., Joos, P., Klanner, R., Klima, B., Kotz, U., Kowalski, H., Ladage, A., Lohr, B., Luke, D., Mess, K. H., Mattig, Peter, Notz, D., Schutte, W., Selonke, F., Trines, D., Wolf, G., Bamberger, A., Heck, W., Runge, K., Wulker, M., Beckmann, R., Behrens, U., Bruckmann, H., Holm, U., Pegel, C., Vogel, W., Wick, K., Hilger, E., Kruger, J., Lohrmann, E., Poelz, G., Schmueser, Peter, Wiik, B. H., Backer, A., Holder, M., Mattern, H., Roderburg, E., Walenta, A., Zech, Gunter, Eisenberg, Y., Karshon, U., Montag, A., Revel, D., Ronat, E. E., Alberini, C., Basile, M., Cara Romeo, G., Castelvetri, A., Cifarelli, L., Cindolo, F., Contin, A., Del Papa, C., Focardi, S., Galli, D., giuseppe iacobucci, Maccarrone, G., Massam, T., Meunier, R., Motta, F., Nania, R., Palmonari, F., Rinaldi, G., Sartorelli, G., Zichichi, A., Calabrese, R., Dalpiaz, P., Ferretti Dalpiaz, P., Petrucci, F., Savrie, M., Borchi, E., Gennaro, S., Macii, R., Pelfer, P., Casaccia, R., Laakso, I., Rindi, A., Sgamma, F., Susinno, G. C., Votano, L., Scrimaglio, R., Rotelli, P., Scarsella, A., Acerbi, E., Baccaglioni, G., Cecchet, G., Groppi, F., Liguori, G., Pensotti, S., Rancoita, P. G., Rossi, L., Carlin, R., Dosselli, U., Gasparini, F., Limentani, S., Morandin, M., Posocco, M., Stanco, L., Voci, C., D Ali, G., Pasquale, S., Sacchetti, N., Ricci, M., Spadoni, M., Pasotti, G., Bruzzese, R., Aglietta, C., Badino, G., Bergamasco, L., Castagnoli, C., Castellina, A., Cini, G., Dardo, M., Ferrero, M. I., Fulgione, W., Galeotti, P., Navarra, G., Saavedra, O., Trinchero, G. C., Vallania, P., Vernetto, S., Daum, C., Engelen, J., Hoogland, W., Paar, H., Tenner, A., Tiecke, H., Wiggers, L., Wigmans, R., Kittel, W., Metzger, W., Burkot, W., Chwastowski, J., Dwurazny, A., Eskreys, A., Niziol, B., Zachara, M., Zawiejski, L., Kisielewska, D., Suszycki, L., Abramowicz, H., Dominik, W., Genser, K., Lipniacka, A., Nassalski, J., Nowak, R., Pawlak, J., Sandacz, A., Tymieniecka, T., Walczak, R., Wroblewski, A. K., Zakrzewski, Janusz Andrzej, Barreiro, F., Ros, E., Foster, B., Gilmore, R., Gooch, T., Kwan, W. L., Malos, J., Smith, V. J., Tapper, R. J., Wood, A. T., Miller, D. B., Bullock, F. W., Jones, T. W., Lush, G. J., Fitch, P. J., Bowler, M. G., Cashmore, R. J., Cobb, J. H., Devenish, R. C. E., Heath, G., Perkins, D. H., Salmon, G. L., Hart, J. C., Hasell, D. K., Mccubbin, N. A., Roberts, J. H. C., Saxon, D. H., Derrick, M., Kooijman, P., Musgrave, B., Sugano, K., Lee, Won-Yong, Seto, R., Sippach, W., Tzanakos, G., O Halloran, T., Wiss, J., Velde, J., Ling, T. Y., Romanowski, T., Oh, B. Y., Smith, G. A., Whitmore, J., Mcdonald, K., Mo, L., Nunamaker, T. A., Camerini, U., Fry, W. F., Loveless, R. J., March, R. H., Morse, R. M., and Reeder, D. D.

30. THE ZEUS DETECTOR: TECHNICAL PROPOSAL

Author

Wolf, G., Edwards, K., Kapitza, H., Smith, G., Conetti, S., Francois Corriveau, Hamel, L. A., Legault, A., Leroy, C., Marchionni, A., Nilsson, A., Patel, P., Stairs, D., Bailey, David C., Bracker, Stephen B., Hartner, G., Kumar, R., Levman, G., Luste, G., Macfarlane, D., Martin, J., Orr, R., Prentice, J., Stacey, B., Yoon, T. S., Frisken, William R., Fukunaga, C., Bock, B., Diekmann, B., Hartmann, H., Heinloth, K., Jakob, H. P., Kolanoski, H., Odingen, R., Paul, E., Sauerwein, R., Schlosser, A., Wedemeyer, R., Anders, B., Bernardi, E., Drews, G., Fohrmann, R., Gather, K., Hultschig, H., Joos, P., Klanner, R., Klima, B., Kotz, U., Kowalski, H., Ladage, A., Lohr, B., Luke, D., Mess, K. H., Notz, D., Rohde, M., Schutte, W., Selonke, F., Trines, D., Bamberger, A., Runge, K., Wulker, M., Beckmann, R., Behrens, U., Bruckmann, H., Holm, U., Pegel, C., Vogel, W., Wick, K., Dierks, K., Hilger, E., Kruger, J., Lohrmann, E., Poelz, G., Schmueser, Peter, Wiik, B. H., Backer, A., Holder, M., Mattern, D., Roderburg, E., Walenta, A., Zech, Gunter, Eisenberg, Y., Karshon, U., Montag, A., Revel, D., Ronat, E. E., Wainer, N., Alberini, C., Bari, G., Basile, M., Cara Romeo, G., Castelvetri, A., Cifarelli, L., Contin, A., Del Papa, C., Galli, D., Iacobucci, G., Janik, R. R., Maccarrone, G., Massam, T., Motta, F., Nania, R., O Shea, V., Palmonari, F., Prisco, G., Rinaldi, G., Sartorelli, G., Willutzky, M., Zichichi, A., Barbagli, G., Borchi, E., Burlamacchi, P., Cirri, G., Cordero, A., Gennaro, S., Del Puglia, A., Lombardini, L., Macii, R., Pelfer, P., Tesi, M., Zoli, M., Anzivino, G., Casaccia, R., Cindolo, F., Laakso, I., Qian, S., Rindi, A., Sgamma, F., Susinno, G. C., Votano, L., Di Sciascio, G., Scrimaglio, R., Rocco Semeraro, G., Rotelli, P., Acerbi, E., Baccaglioni, G., Groppi, F., Pensotti, S., Rancoita, P. G., Rossi, L., Simeoni, C., Stanziani, M., Carlin, R., Dosselli, U., Gasparini, F., Limentani, S., Morandin, M., Posocco, M., Stanco, L., Voci, C., D Ali, G., Pasquale, S., Bruzzese, R., Pasotti, G., Ricci, M., Sacchetti, N., Spadoni, M., D Agostini, G., Gaspero, Mario, Marini, G., Nigro, A., Aglietta, C., Badino, G., Bergamasco, L., Castagnoli, C., Castellina, A., Cini, G., Dardo, M., Ferrero, M. I., Fulgione, W., Galeotti, P., Morello, C., Navarra, G., Periale, L., Saavedra, O., Trinchero, G. C., Vallania, P., Vernetto, S., Daum, C., Engelen, J., Hoogland, W., Paar, H., Tenner, A., Tiecke, H., Wiggers, L., Wigmans, R., Burkot, W., Chwastowski, J., Dwurazny, A., Eskreys, A., Niziol, B., Zachara, M., Zawiejski, L., Eskreys, K., Jelen, K., Kisielewska, D., Suszycki, L., Abramowicz, H., Dominik, W., Genser, K., Lipniacka, A., Nassalski, J., Nowak, R., Pawlak, J., Sandacz, A., Stopczynski, A., Tkaczyk, S., Tymieniecka, T., Walczak, R., Wroblewski, A. K., Zakrzewski, Janusz Andrzej, Barreiro, F., Ros, E., Foster, B., Gilmore, R., Gooch, T., Kwan, W. L., Malos, J., Smith, V. J., Tapper, R. J., Hassard, J., Miller, D. B., Mobayyen, M., Bullock, F. W., Jones, T. W., Lush, G. J., Fitch, P. J., Bowler, M. G., Cashmore, R. J., Cobb, J. H., Devenish, R. C. E., Harnew, N., Heath, G., Salmon, G. L., Hart, J. C., Hassel, D. K., Mccubbin, N. A., Roberts, J. H. C., Saxon, D. H., Derrick, M., Kooijman, P., Musgrave, B., Sugano, K., Lee, Won-Yong, Mishra, S., Sciulli, F., Seto, R., Sippach, W., Smith, W., Tzanakos, G., O Halloran, T., Wiss, J., Ling, T. Y., Romanowski, T., Oh, B. Y., Smith, G. A., Whitmore, J., Ficenec, J., Mo, L., Nunamaker, T. A., Prosper, H., Camerini, U., Fry, W. F., Loveless, R. J., March, R. H., Morse, R. M., and Reeder, D. D.

31. Status-Report on the 12-Split Coil Test Facility Sultan

Author

Blau, B., Aebli, E., Jakob, B., Pasztor, G., Vecsey, G., Dellacorte, A., Pasotti, G., Sacchetti, N., and Spadoni, M.

Abstract

The third phase of upgrading of the superconductor test facility SULTAN into a split coil system (SULTAN III) is in progress. SULTAN III - a joint project of ENEA (Italy) and PSI (Switzerland) - consists of two coil packages, each containing three concentrically mounted superconducting solenoids. Together they will produce a field of nearly 12T between the two coil packages, inside a solenoid bore of 58 cm. The outermost 6T coils have NbTi conductors, whereas the inner 9T and 12T coils are made of A-15 cables. All Nb3Sn coils are manufactured by the react-and-wind technique. The split coil arrangement, in connection with a sophisticated sample insert containing a 50 kA superconducting transformer, will allow testing of short samples of high current carrying superconductors, e.g. for fusion applications. The sample insert was designed to allow changing the samples within a few hours without warming up the whole magnet system. This paper will deal with the present status and potential of the Split Coil Test Facility SULTAN III.

33. THE FORCED FLOW HIGH FIELD TEST FACILITY SULTAN

Author

Horvath, I., primary, Vécsey, G., additional, Weymuth, P., additional, Zellweger, J., additional, Balsamo, E. P., additional, Pasotti, G., additional, Ricci, M. V., additional, Sacchetti, N., additional, Spadoni, M., additional, Elen, J. D., additional, Franken, W. M.P., additional, and Roeterdink, J. A., additional

Published
1984
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41. Efficacy Of Lentivirus-Mediated Gene Therapy In An Omenn Syndrome Recombination-Activating Gene 2 Mouse Model Is Not Hindered By Inflammation And Immune Dysregulation

Author

Anna Villa, Paola Carrera, Marita Bosticardo, Elena Fontana, Maria Carmina Castiello, Sara Penna, Monica Zanussi, Lucia Sergi Sergi, Elena Draghici, Luigi Poliani, Nicolò Sacchetti, Gerard Wagemaker, Valentina Capo, Barbara Cassani, Luigi D. Notarangelo, Niek P. van Til, Kerry Dobbs, Rosita Rigoni, Paolo Uva, İç Hastalıkları, Hematology, Capo, V, Castiello, M, Fontana, E, Penna, S, Bosticardo, M, Draghici, E, Poliani, L, Sergi Sergi, L, Rigoni, R, Cassani, B, Zanussi, M, Carrera, P, Uva, P, Dobbs, K, Sacchetti, N, Notarangelo, L, van Til, N, Wagemaker, G, and Villa, A

Subjects
Male, 0301 basic medicine, Rag gene, Allergy, T-Lymphocytes, Genetic enhancement, Immunology, Autoimmunity, Mice, Transgenic, Article, Gene therapy, Lentiviral vector, Omenn syndrome, Rag genes, Immunology and Allergy, 03 medical and health sciences, RAG2, medicine, Animals, Lymphocyte Count, Immunodeficiency, Inflammation, B-Lymphocytes, Severe combined immunodeficiency, business.industry, Lentivirus, Genetic Therapy, medicine.disease, Autoimmune regulator, 3. Good health, DNA-Binding Proteins, Mice, Inbred C57BL, Transplantation, Disease Models, Animal, 030104 developmental biology, Primary immunodeficiency, Female, Severe Combined Immunodeficiency, business
Abstract

Background Omenn syndrome (OS) is a rare severe combined immunodeficiency associated with autoimmunity and caused by defects in lymphoid-specific V(D)J recombination. Most patients carry hypomorphic mutations in recombination-activating gene ( RAG ) 1 or 2. Hematopoietic stem cell transplantation is the standard treatment; however, gene therapy (GT) might represent a valid alternative, especially for patients lacking a matched donor. Objective We sought to determine the efficacy of lentiviral vector (LV)–mediated GT in the murine model of OS (Rag2 R229Q/R229Q ) in correcting immunodeficiency and autoimmunity. Methods Lineage-negative cells from mice with OS were transduced with an LV encoding the human RAG2 gene and injected into irradiated recipients with OS. Control mice underwent transplantation with wild-type or OS-untransduced lineage-negative cells. Immunophenotyping, T-dependent and T-independent antigen challenge, immune spectratyping, autoantibody detection, and detailed tissue immunohistochemical analyses were performed. Results LV-mediated GT allowed immunologic reconstitution, although it was suboptimal compared with that seen in wild-type bone marrow (BM)−transplanted OS mice in peripheral blood and hematopoietic organs, such as the BM, thymus, and spleen. We observed in vivo variability in the efficacy of GT correlating with the levels of transduction achieved. Immunoglobulin levels and T-cell repertoire normalized, and gene-corrected mice responded properly to challenges in vivo . Autoimmune manifestations, such as skin infiltration and autoantibodies, dramatically improved in GT mice with a vector copy number/genome higher than 1 in the BM and 2 in the thymus. Conclusions Our data show that LV-mediated GT for patients with OS significantly ameliorates the immunodeficiency, even in an inflammatory environment.

Published
2018

46. Exonic knockout and knockin gene editing in hematopoietic stem and progenitor cells rescues RAG1 immunodeficiency.

Author

Castiello MC, Brandas C, Ferrari S, Porcellini S, Sacchetti N, Canarutto D, Draghici E, Merelli I, Barcella M, Pelosi G, Vavassori V, Varesi A, Jacob A, Scala S, Basso Ricci L, Paulis M, Strina D, Di Verniere M, Sergi Sergi L, Serafini M, Holland SM, Bergerson JRE, De Ravin SS, Malech HL, Pala F, Bosticardo M, Brombin C, Cugnata F, Calzoni E, Crooks GM, Notarangelo LD, Genovese P, Naldini L, and Villa A

Subjects
Animals, Humans, Mice, Exons, Hematopoietic Stem Cells metabolism, Homeodomain Proteins genetics, Homeodomain Proteins metabolism, Gene Editing methods, Hematopoietic Stem Cell Transplantation
Abstract

Recombination activating genes ( RAGs ) are tightly regulated during lymphoid differentiation, and their mutations cause a spectrum of severe immunological disorders. Hematopoietic stem and progenitor cell (HSPC) transplantation is the treatment of choice but is limited by donor availability and toxicity. To overcome these issues, we developed gene editing strategies targeting a corrective sequence into the human RAG1 gene by homology-directed repair (HDR) and validated them by tailored two-dimensional, three-dimensional, and in vivo xenotransplant platforms to assess rescue of expression and function. Whereas integration into intron 1 of RAG1 achieved suboptimal correction, in-frame insertion into exon 2 drove physiologic human RAG1 expression and activity, allowing disruption of the dominant-negative effects of unrepaired hypomorphic alleles. Enhanced HDR-mediated gene editing enabled the correction of human RAG1 in HSPCs from patients with hypomorphic RAG1 mutations to overcome T and B cell differentiation blocks. Gene correction efficiency exceeded the minimal proportion of functional HSPCs required to rescue immunodeficiency in Rag1 -/- mice, supporting the clinical translation of HSPC gene editing for the treatment of RAG1 deficiency.

Published
2024
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47. Efficacy and safety of anti-CD45-saporin as conditioning agent for RAG deficiency.

Author

Castiello MC, Bosticardo M, Sacchetti N, Calzoni E, Fontana E, Yamazaki Y, Draghici E, Corsino C, Bortolomai I, Sereni L, Yu HH, Uva P, Palchaudhuri R, Scadden DT, Villa A, and Notarangelo LD

Subjects
Allografts, Animals, Antibodies, Monoclonal adverse effects, Homeodomain Proteins immunology, Immunoconjugates adverse effects, Leukocyte Common Antigens genetics, Leukocyte Common Antigens immunology, Mice, Mice, Knockout, Saporins adverse effects, Severe Combined Immunodeficiency genetics, Severe Combined Immunodeficiency immunology, Antibodies, Monoclonal pharmacology, Bone Marrow Transplantation, Homeodomain Proteins genetics, Immunoconjugates pharmacology, Leukocyte Common Antigens antagonists & inhibitors, Saporins pharmacology, Severe Combined Immunodeficiency therapy, Transplantation Conditioning
Abstract

Background: Mutations in the recombinase-activating genes cause severe immunodeficiency, with a spectrum of phenotypes ranging from severe combined immunodeficiency to immune dysregulation. Hematopoietic stem cell transplantation is the only curative option, but a high risk of graft failure and poor immune reconstitution have been observed in the absence of myeloablation., Objectives: Our aim was to improve multilineage engraftment; we tested nongenotoxic conditioning with anti-CD45 mAbs conjugated with saporin CD45 (CD45-SAP)., Methods: Rag1-KO and Rag1-F971L mice, which represent models of severe combined immune deficiency and combined immune deficiency with immune dysregulation, respectively, were conditioned with CD45-SAP, CD45-SAP plus 2 Gy of total body irradiation (TBI), 2 Gy of TBI, 8 Gy of TBI, or no conditioning and treated by using transplantation with lineage-negative bone marrow cells from wild-type mice. Flow cytometry and immunohistochemistry were used to assess engraftment and immune reconstitution. Antibody responses to 2,4,6-trinitrophenyl-conjugated keyhole limpet hemocyanin were measured by ELISA, and presence of autoantibody was detected by microarray., Results: Conditioning with CD45-SAP enabled high levels of multilineage engraftment in both Rag1 mutant models, allowed overcoming of B- and T-cell differentiation blocks and thymic epithelial cell defects, and induced robust cellular and humoral immunity in the periphery., Conclusions: Conditioning with CD45-SAP allows multilineage engraftment and robust immune reconstitution in mice with either null or hypomorphic Rag mutations while preserving thymic epithelial cell homeostasis., (Published by Elsevier Inc.)

Published
2021
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48. Artificial thymic organoids represent a reliable tool to study T-cell differentiation in patients with severe T-cell lymphopenia.

Author

Bosticardo M, Pala F, Calzoni E, Delmonte OM, Dobbs K, Gardner CL, Sacchetti N, Kawai T, Garabedian EK, Draper D, Bergerson JRE, DeRavin SS, Freeman AF, Güngör T, Hartog N, Holland SM, Kohn DB, Malech HL, Markert ML, Weinacht KG, Villa A, Seet CS, Montel-Hagen A, Crooks GM, and Notarangelo LD

Subjects
Antigens, CD34, Cell Differentiation, Humans, Organoids, Hematopoietic Stem Cells, Lymphopenia
Abstract

The study of early T-cell development in humans is challenging because of limited availability of thymic samples and the limitations of in vitro T-cell differentiation assays. We used an artificial thymic organoid (ATO) platform generated by aggregating a DLL4-expressing stromal cell line (MS5-hDLL4) with CD34+ cells isolated from bone marrow or mobilized peripheral blood to study T-cell development from CD34+ cells of patients carrying hematopoietic intrinsic or thymic defects that cause T-cell lymphopenia. We found that AK2 deficiency is associated with decreased cell viability and an early block in T-cell development. We observed a similar defect in a patient carrying a null IL2RG mutation. In contrast, CD34+ cells from a patient carrying a missense IL2RG mutation reached full T-cell maturation, although cell numbers were significantly lower than in controls. CD34+ cells from patients carrying RAG mutations were able to differentiate to CD4+CD8+ cells, but not to CD3+TCRαβ+ cells. Finally, normal T-cell differentiation was observed in a patient with complete DiGeorge syndrome, consistent with the extra-hematopoietic nature of the defect. The ATO system may help determine whether T-cell deficiency reflects hematopoietic or thymic intrinsic abnormalities and define the exact stage at which T-cell differentiation is blocked.

Published
2020
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49. Efficacy of lentivirus-mediated gene therapy in an Omenn syndrome recombination-activating gene 2 mouse model is not hindered by inflammation and immune dysregulation.

Author

Capo V, Castiello MC, Fontana E, Penna S, Bosticardo M, Draghici E, Poliani LP, Sergi Sergi L, Rigoni R, Cassani B, Zanussi M, Carrera P, Uva P, Dobbs K, Sacchetti N, Notarangelo LD, van Til NP, Wagemaker G, and Villa A

Subjects
Animals, Autoimmunity, B-Lymphocytes immunology, Disease Models, Animal, Female, Inflammation immunology, Inflammation therapy, Lymphocyte Count, Male, Mice, Inbred C57BL, Mice, Transgenic, Severe Combined Immunodeficiency immunology, T-Lymphocytes immunology, DNA-Binding Proteins genetics, Genetic Therapy, Lentivirus genetics, Severe Combined Immunodeficiency therapy
Abstract

Background: Omenn syndrome (OS) is a rare severe combined immunodeficiency associated with autoimmunity and caused by defects in lymphoid-specific V(D)J recombination. Most patients carry hypomorphic mutations in recombination-activating gene (RAG) 1 or 2. Hematopoietic stem cell transplantation is the standard treatment; however, gene therapy (GT) might represent a valid alternative, especially for patients lacking a matched donor., Objective: We sought to determine the efficacy of lentiviral vector (LV)-mediated GT in the murine model of OS (Rag2 R229Q/R229Q ) in correcting immunodeficiency and autoimmunity., Methods: Lineage-negative cells from mice with OS were transduced with an LV encoding the human RAG2 gene and injected into irradiated recipients with OS. Control mice underwent transplantation with wild-type or OS-untransduced lineage-negative cells. Immunophenotyping, T-dependent and T-independent antigen challenge, immune spectratyping, autoantibody detection, and detailed tissue immunohistochemical analyses were performed., Results: LV-mediated GT allowed immunologic reconstitution, although it was suboptimal compared with that seen in wild-type bone marrow (BM)-transplanted OS mice in peripheral blood and hematopoietic organs, such as the BM, thymus, and spleen. We observed in vivo variability in the efficacy of GT correlating with the levels of transduction achieved. Immunoglobulin levels and T-cell repertoire normalized, and gene-corrected mice responded properly to challenges in vivo. Autoimmune manifestations, such as skin infiltration and autoantibodies, dramatically improved in GT mice with a vector copy number/genome higher than 1 in the BM and 2 in the thymus., Conclusions: Our data show that LV-mediated GT for patients with OS significantly ameliorates the immunodeficiency, even in an inflammatory environment., (Copyright © 2017 American Academy of Allergy, Asthma & Immunology. Published by Elsevier Inc. All rights reserved.)

Published
2018
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50. A retinoic acid-dependent stroma-leukemia crosstalk promotes chronic lymphocytic leukemia progression.

Author

Farinello D, Wozińska M, Lenti E, Genovese L, Bianchessi S, Migliori E, Sacchetti N, di Lillo A, Bertilaccio MTS, de Lalla C, Valsecchi R, Gleave SB, Lligé D, Scielzo C, Mauri L, Ciampa MG, Scarfò L, Bernardi R, Lazarevic D, Gonzalez-Farre B, Bongiovanni L, Campo E, Cerutti A, Ponzoni M, Pattini L, Caligaris-Cappio F, Ghia P, and Brendolan A

Subjects
Animals, Cell Line, Chemokine CXCL13 metabolism, Coculture Techniques, Disease Progression, Female, Gene Expression Regulation, Neoplastic, Leukemia, Lymphocytic, Chronic, B-Cell metabolism, Male, Mice, Inbred C57BL, Signal Transduction, Survival Analysis, Tretinoin metabolism, Tumor Microenvironment, Leukemia, Lymphocytic, Chronic, B-Cell pathology, Stromal Cells pathology, Tretinoin physiology
Abstract

In chronic lymphocytic leukemia (CLL), the non-hematopoietic stromal microenvironment plays a critical role in promoting tumor cell recruitment, activation, survival, and expansion. However, the nature of the stromal cells and molecular pathways involved remain largely unknown. Here, we demonstrate that leukemic B lymphocytes induce the activation of retinoid acid synthesis and signaling in the microenvironment. Inhibition of RA-signaling in stromal cells causes deregulation of genes associated with adhesion, tissue organization and chemokine secretion including the B-cell chemokine CXCL13. Notably, reducing retinoic acid precursors from the diet or inhibiting RA-signaling through retinoid-antagonist therapy prolong survival by preventing dissemination of leukemia cells into lymphoid tissues. Furthermore, mouse and human leukemia cells could be distinguished from normal B-cells by their increased expression of Rarγ2 and RXRα, respectively. These findings establish a role for retinoids in murine CLL pathogenesis, and provide new therapeutic strategies to target the microenvironment and to control disease progression.

Published
2018
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