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2. Long-Term Drug Survival and Effectiveness of Secukinumab in Patients with Moderate to Severe Chronic Plaque Psoriasis: 42-Month Results from the SUPREME 2.0 Study

Author

Russo, Filomena, primary, Galluzzo, Marco, additional, Stingeni, Luca, additional, Persechino, Severino, additional, Zichichi, Leonardo, additional, Conti, Andrea, additional, Giofrè, Claudia, additional, Dini, Valentina, additional, Vispi, Martina, additional, Atzori, Laura, additional, Cattaneo, Angelo, additional, Parodi, Aurora, additional, Bardazzi, Federico, additional, Stinco, Giuseppe, additional, Dapavo, Paolo, additional, Girolomoni, Giampiero, additional, Musumeci, Maria Letizia, additional, Papini, Manuela, additional, Venturini, Marina, additional, Dastoli, Stefano, additional, Di Nuzzo, Sergio, additional, Fargnoli, Maria Concetta, additional, Pagnanelli, Gianluca, additional, Bernardini, Nicoletta, additional, Gambini, Daniele, additional, Malagoli, Piergiorgio, additional, Mazzatenta, Carlo, additional, Peris, Ketty, additional, Zalaudek, Iris, additional, Fabbrocini, Gabriella, additional, Loconsole, Francesco, additional, Vassallo, Camilla, additional, Pietroleonardo, Lucia, additional, Prignano, Francesca, additional, Franchi, Chiara, additional, Offidani, Anna Maria, additional, Bonifati, Claudio, additional, Di Lernia, Vito, additional, Gigante, Giovanni, additional, Bartezaghi, Marta, additional, Franchi, Matteo, additional, Ursoleo, Paola, additional, and Aloisi, Elisabetta, additional

Published
2023
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3. Long-Term Drug Survival and Effectiveness of Secukinumab in Patients with Moderate to Severe Chronic Plaque Psoriasis: 42-Month Results from the SUPREME 2.0 Study

Author

Russo,Filomena, Galluzzo,Marco, Stingeni,Luca, Persechino,Severino, Zichichi,Leonardo, Conti,Andrea, Giofrè,Claudia, Dini,Valentina, Vispi,Martina, Atzori,Laura, Cattaneo,Angelo, Parodi,Aurora, Bardazzi,Federico, Stinco,Giuseppe, Dapavo,Paolo, Girolomoni,Giampiero, Musumeci,Maria Letizia, Papini,Manuela, Venturini,Marina, Dastoli,Stefano, Di Nuzzo,Sergio, Fargnoli,Maria Concetta, Pagnanelli,Gianluca, Bernardini,Nicoletta, Gambini,Daniele, Malagoli,Piergiorgio, Mazzatenta,Carlo, Peris,Ketty, Zalaudek,Iris, Fabbrocini,Gabriella, Loconsole,Francesco, Vassallo,Camilla, Pietroleonardo,Lucia, Prignano,Francesca, Franchi,Chiara, Offidani,Anna Maria, Bonifati,Claudio, Di Lernia,Vito, Gigante,Giovanni, Bartezaghi,Marta, Franchi,Matteo, Ursoleo,Paola, Aloisi,Elisabetta, Russo,Filomena, Galluzzo,Marco, Stingeni,Luca, Persechino,Severino, Zichichi,Leonardo, Conti,Andrea, Giofrè,Claudia, Dini,Valentina, Vispi,Martina, Atzori,Laura, Cattaneo,Angelo, Parodi,Aurora, Bardazzi,Federico, Stinco,Giuseppe, Dapavo,Paolo, Girolomoni,Giampiero, Musumeci,Maria Letizia, Papini,Manuela, Venturini,Marina, Dastoli,Stefano, Di Nuzzo,Sergio, Fargnoli,Maria Concetta, Pagnanelli,Gianluca, Bernardini,Nicoletta, Gambini,Daniele, Malagoli,Piergiorgio, Mazzatenta,Carlo, Peris,Ketty, Zalaudek,Iris, Fabbrocini,Gabriella, Loconsole,Francesco, Vassallo,Camilla, Pietroleonardo,Lucia, Prignano,Francesca, Franchi,Chiara, Offidani,Anna Maria, Bonifati,Claudio, Di Lernia,Vito, Gigante,Giovanni, Bartezaghi,Marta, Franchi,Matteo, Ursoleo,Paola, and Aloisi,Elisabetta

Abstract

Filomena Russo,1 Marco Galluzzo,2,3 Luca Stingeni,4 Severino Persechino,5 Leonardo Zichichi,6 Andrea Conti,7 Claudia Giofrè,8 Valentina Dini,9 Martina Vispi,10 Laura Atzori,11 Angelo Cattaneo,12 Aurora Parodi,13 Federico Bardazzi,14 Giuseppe Stinco,15 Paolo Dapavo,16 Giampiero Girolomoni,17 Maria Letizia Musumeci,18 Manuela Papini,19 Marina Venturini,20 Stefano Dastoli,21 Sergio Di Nuzzo,22 Maria Concetta Fargnoli,23 Gianluca Pagnanelli,24 Nicoletta Bernardini,25 Daniele Mario Gambini,26 Piergiorgio Malagoli,27 Carlo Mazzatenta,28 Ketty Peris,29 Iris Zalaudek,30 Gabriella Fabbrocini31 ,†Francesco Loconsole,32 Camilla Vassallo,33 Lucia Pietroleonardo,34 Francesca Prignano,35 Chiara Franchi,36 Anna Maria Offidani,37 Claudio Bonifati,38 Vito Di Lernia,39 Giovanni Gigante,40 Marta Silvia Bartezaghi,40 Matteo Franchi,41,42 Paola Ursoleo,40 Elisabetta Aloisi40 1Dermatology Section, Department of Medical, Surgical and Neurological Science, University of Siena, S. Maria Alle Scotte Hospital, Siena, Italy; 2Department of Systems Medicine, University of Rome “Tor Vergata”, Rome, Italy; 3Dermatology Unit, Fondazione Policlinico “Tor Vergata”, Rome, Italy; 4Section of Dermatology, Department of Medicine and Surgery, University of Perugia, Perugia, Italy; 5Dermatology Unit, NESMOS Department, Faculty of Medicine & Psychology, Sapienza University of Rome, Sant’Andrea University Hospital, Rome, Italy; 6Unit of Dermatology, San Antonio Abate Hospital, Trapani, Italy; 7Section of Dermatology, Department of Specialized Medicine, University of Modena and Reggio Emilia, Modena, Italy; 8U.O.C. Dermatologia, A.O. Papardo, Messina, Italy; 9Section of Dermatology, Department of Medicine and Oncology, University of Pisa, Pisa, Italy; 10Dermatology Unit, Misericordia Hospital, Grosseto, Italy; 11Dermatology Unit, Department of Medical Sciences and Public Health, University of Cagliari, Cagliari, Italy; 12Dermatology Unit, Fondazione IRCCS Cà Granda Ospedale Maggiore Policl

Published
2023

4. Efficacy and Safety of Secukinumab in Elderly Patients with Moderate to Severe Plaque-Type Psoriasis: Post-Hoc Analysis of the SUPREME Study

Author

Talamonti,Marina, Russo,Filomena, Malara,Giovanna, Hansel,Katharina, Papini,Manuela, Cattaneo,Angelo, Parodi,Aurora, Chiricozzi,Andrea, Malagoli,Piergiorgio, Bardazzi,Federico, Brazzelli,Valeria, Dapavo,Paolo, Gisondi,Paolo, Zane,Cristina, Potenza,Concetta, Cantoresi,Franca, Fargnoli,Maria Concetta, Trevisini,Sara, Brianti,Pina, Pescitelli,Leonardo, Gigante,Giovanni, Bartezaghi,Marta, Caputo,Luisa, Aloisi,Elisabetta, Costanzo,Antonio, Talamonti,Marina, Russo,Filomena, Malara,Giovanna, Hansel,Katharina, Papini,Manuela, Cattaneo,Angelo, Parodi,Aurora, Chiricozzi,Andrea, Malagoli,Piergiorgio, Bardazzi,Federico, Brazzelli,Valeria, Dapavo,Paolo, Gisondi,Paolo, Zane,Cristina, Potenza,Concetta, Cantoresi,Franca, Fargnoli,Maria Concetta, Trevisini,Sara, Brianti,Pina, Pescitelli,Leonardo, Gigante,Giovanni, Bartezaghi,Marta, Caputo,Luisa, Aloisi,Elisabetta, and Costanzo,Antonio

Abstract

Marina Talamonti,1 Filomena Russo,2 Giovanna Malara,3,4 Katharina Hansel,5 Manuela Papini,6 Angelo Cattaneo,7 Aurora Parodi,8 Andrea Chiricozzi,9,10 Piergiorgio Malagoli,11 Federico Bardazzi,12 Valeria Brazzelli,13 Paolo Dapavo,14 Paolo Gisondi,15 Cristina Zane,16 Concetta Potenza,17 Franca Cantoresi,18 Maria Concetta Fargnoli,19 Sara Trevisini,20 Pina Brianti,21 Leonardo Pescitelli,22 Giovanni Gigante,23 Marta Bartezaghi,23 Luisa Caputo,23 Elisabetta Aloisi,23 Antonio Costanzo24,25 On behalf of the SUPREME Study Group1Dermatology, University of Rome Tor Vergata, Rome, Italy; 2Department of Medical, Surgical and Neurological Science, Dermatology Section, University of Siena, S. Maria alle Scotte Hospital, Siena, Italy; 3Dermatology Unit, Hospital “Bianchi Melacrino Morelli”, Reggio, Calabria, Italy; 4Department of Dermatology, Papardo Hospital, Messina, Italy; 5Section of Dermatology, Department of Medicine and Surgery, University of Perugia, Perugia, Italy; 6Dermatologic Clinic of Terni, Department of Medicine and Surgery, University of Perugia, Perugia, Italy; 7U.O. Dermatologia, Fondazione IRCCS Ca’ Granda - Ospedale Maggiore Policlinico, Milano, Italy; 8Di.S.Sal. Section of Dermatology, Ospedale Policlinico San Martino, University of Genova, Genova GE, 16132, Italy; 9UOC di Dermatologia, Dipartimento di Scienze Mediche e Chirurgiche, Fondazione Policlinico Universitario A. Gemelli - IRCCS, Rome, Italy; 10Dermatologia, Dipartimento di Medicina e Chirurgia Traslazionale, Università Cattolica del Sacro Cuore, Rome, Italy; 11Psocare Unit, I.R.C.C.S Policlinico San Donato, Milano, Italy; 12Dermatology Unit, IRCCS Azienda Ospedaliero-Universitaria di Bologna, Bologna, Italy; 13Dermatology, Fondazione IRCCS Policlinico San Matteo and University of Pavia, Pavia, Italy; 14Department of Biomedical Science and Human Oncology, Second Dermatologic Clinic, University of Torino, Torino, Italy; 15Section of Dermatology and Venereology, Department of Medicine, University

Published
2023

5. Efficacy of Secukinumab in Psoriasis: Post Hoc Gender-Wise Analysis of the SUPREME Study

Author

Stingeni,Luca, Malara,Giovanna, Conti,Andrea, Di Costanzo,Luisa, Carrera,Carlo Giovanni, Burlando,Martina, Malagoli,Piergiorgio, Musumeci,Maria Letizia, Bardazzi,Federico, Brazzelli,Valeria, Amerio,Paolo, De Simone,Clara, Trevisini,Sara, Balato,Anna, Megna,Matteo, Loconsole,Francesco, De Felice,Catia, Bartezaghi,Marta, Rausa,Alice, Aloisi,Elisabetta, Orsenigo,Roberto, Costanzo,Antonio, Stingeni,Luca, Malara,Giovanna, Conti,Andrea, Di Costanzo,Luisa, Carrera,Carlo Giovanni, Burlando,Martina, Malagoli,Piergiorgio, Musumeci,Maria Letizia, Bardazzi,Federico, Brazzelli,Valeria, Amerio,Paolo, De Simone,Clara, Trevisini,Sara, Balato,Anna, Megna,Matteo, Loconsole,Francesco, De Felice,Catia, Bartezaghi,Marta, Rausa,Alice, Aloisi,Elisabetta, Orsenigo,Roberto, and Costanzo,Antonio

Abstract

Luca Stingeni,1 Giovanna Malara,2,3 Andrea Conti,4 Luisa Di Costanzo,5 Carlo Giovanni Carrera,6 Martina Burlando,7 Piergiorgio Malagoli,8 Maria Letizia Musumeci,9 Federico Bardazzi,10 Valeria Brazzelli,11 Paolo Amerio,12 Clara De Simone,13,14 Sara Trevisini,15 Anna Balato,16 Matteo Megna,17 Francesco Loconsole,18 Catia De Felice,19 Marta Bartezaghi,20 Alice Rausa,20 Elisabetta Aloisi,20 Roberto Orsenigo,20 Antonio Costanzo21,22 On behalf of the SUPREME Study Group1Dermatology Section, Medical and Surgical Department, University of Perugia, Perugia, Italy; 2Dermatology Unit, Hospital “Bianchi Melacrino Morelli”, Reggio Calabria, Italy; 3Department of Dermatology, Papardo Hospital, Messina, Italy; 4Dermatologic Unit, Department of Surgery, Infermi Hospital, AUSL Romagna, Rimini, Italy; 5Department of Dermatology, “Gaetano Rummo” Hospital, Benevento UOC Dermatologia, AO G. Rummo, Benevento, Italy; 6U.O. Dermatologia, Fondazione IRCCS Ca’ Granda - Ospedale Maggiore Policlinico, Milano, Italy; 7IRCCS San Martino Polyclinic Hospital, Di.S.Sal. Section of Dermatology, Genoa, Italy; 8Dermatology Unit IRCCS Policlinico San Donato, Milan, Italy; 9Dermatology Clinic, University of Catania, Catania, Italy; 10Division of Dermatology, University Hospital Policlinico “S. Orsola-Malpighi”, Bologna, Italy; 11Institute of Dermatology, Foundation IRCCS Policlinico San Matteo and University of Pavia, Pavia, Italy; 12Dermatologic Clinic, G. D’Annunzio University, Chieti, Italy; 13Istituto di Dermatologia, Università Cattolica del Sacro Cuore, Rome, Italy; 14Fondazione Policlinico Universitario A. Gemelli – IRCCS, Rome, Italy; 15Dermatology Department, University of Trieste, Trieste, Italy; 16Dermatology Unit, University of Campania “Luigi Vanvitelli”, Naples, Italy; 17Section of Dermatology, Department of Clinical Medicine and Surgery, University of Naples Federico II, Naples, Italy; 18Department of Biomedical Sciences and Human Oncology, University of Bari, Bari

Published
2023

6. Long-Term Drug Survival and Effectiveness of Secukinumab in Patients with Moderate to Severe Chronic Plaque Psoriasis: 42-Month Results from the SUPREME 2.0 Study

Author

Russo, F, Galluzzo, M, Stingeni, L, Persechino, S, Zichichi, L, Conti, A, Giofrè, C, Dini, V, Vispi, M, Atzori, L, Cattaneo, A, Parodi, A, Bardazzi, F, Stinco, G, Dapavo, P, Girolomoni, G, Musumeci, M, Papini, M, Venturini, M, Dastoli, S, Di Nuzzo, S, Fargnoli, M, Pagnanelli, G, Bernardini, N, Gambini, D, Malagoli, P, Mazzatenta, C, Peris, K, Zalaudek, I, Fabbrocini, G, Loconsole, F, Vassallo, C, Pietroleonardo, L, Prignano, F, Franchi, C, Offidani, A, Bonifati, C, Di Lernia, V, Gigante, G, Bartezaghi, M, Franchi, M, Ursoleo, P, Aloisi, E, Russo, Filomena, Galluzzo, Marco, Stingeni, Luca, Persechino, Severino, Zichichi, Leonardo, Conti, Andrea, Giofrè, Claudia, Dini, Valentina, Vispi, Martina, Atzori, Laura, Cattaneo, Angelo, Parodi, Aurora, Bardazzi, Federico, Stinco, Giuseppe, Dapavo, Paolo, Girolomoni, Giampiero, Musumeci, Maria Letizia, Papini, Manuela, Venturini, Marina, Dastoli, Stefano, Di Nuzzo, Sergio, Fargnoli, Maria Concetta, Pagnanelli, Gianluca, Bernardini, Nicoletta, Gambini, Daniele, Malagoli, Piergiorgio, Mazzatenta, Carlo, Peris, Ketty, Zalaudek, Iris, Fabbrocini, Gabriella, Loconsole, Francesco, Vassallo, Camilla, Pietroleonardo, Lucia, Prignano, Francesca, Franchi, Chiara, Offidani, Anna Maria, Bonifati, Claudio, Di Lernia, Vito, Gigante, Giovanni, Bartezaghi, Marta, Franchi, Matteo, Ursoleo, Paola, Aloisi, Elisabetta, Russo, F, Galluzzo, M, Stingeni, L, Persechino, S, Zichichi, L, Conti, A, Giofrè, C, Dini, V, Vispi, M, Atzori, L, Cattaneo, A, Parodi, A, Bardazzi, F, Stinco, G, Dapavo, P, Girolomoni, G, Musumeci, M, Papini, M, Venturini, M, Dastoli, S, Di Nuzzo, S, Fargnoli, M, Pagnanelli, G, Bernardini, N, Gambini, D, Malagoli, P, Mazzatenta, C, Peris, K, Zalaudek, I, Fabbrocini, G, Loconsole, F, Vassallo, C, Pietroleonardo, L, Prignano, F, Franchi, C, Offidani, A, Bonifati, C, Di Lernia, V, Gigante, G, Bartezaghi, M, Franchi, M, Ursoleo, P, Aloisi, E, Russo, Filomena, Galluzzo, Marco, Stingeni, Luca, Persechino, Severino, Zichichi, Leonardo, Conti, Andrea, Giofrè, Claudia, Dini, Valentina, Vispi, Martina, Atzori, Laura, Cattaneo, Angelo, Parodi, Aurora, Bardazzi, Federico, Stinco, Giuseppe, Dapavo, Paolo, Girolomoni, Giampiero, Musumeci, Maria Letizia, Papini, Manuela, Venturini, Marina, Dastoli, Stefano, Di Nuzzo, Sergio, Fargnoli, Maria Concetta, Pagnanelli, Gianluca, Bernardini, Nicoletta, Gambini, Daniele, Malagoli, Piergiorgio, Mazzatenta, Carlo, Peris, Ketty, Zalaudek, Iris, Fabbrocini, Gabriella, Loconsole, Francesco, Vassallo, Camilla, Pietroleonardo, Lucia, Prignano, Francesca, Franchi, Chiara, Offidani, Anna Maria, Bonifati, Claudio, Di Lernia, Vito, Gigante, Giovanni, Bartezaghi, Marta, Franchi, Matteo, Ursoleo, Paola, and Aloisi, Elisabetta

Abstract

Purpose: SUPREME, a phase IIIb study conducted in Italy, demonstrated safety and high efficacy of secukinumab for up to 72 weeks in patients with moderate-to-severe plaque-type psoriasis. SUPREME 2.0 study aimed to provide real-world data on the long-term drug survival and effectiveness of secukinumab beyond 72 weeks. Patients and Methods: SUPREME 2.0 is a retrospective observational chart review study conducted in patients previously enrolled in SUPREME study. After the end of the SUPREME study, eligible patients continued treatment as per clinical practice, and their effectiveness and drug survival data were retrieved from medical charts. Results: Of the 415 patients enrolled in the SUPREME study, 297 were included in SUPREME 2.0; of which, 210 (70.7%) continued secukinumab treatment throughout the 42-month observation period. Patients in the biologic-naïve cohort had higher drug survival than those in the biologic-experienced cohort (74.9% vs 61.7%), while HLA-Cw6–positive and HLA-Cw6–negative patients showed similar drug survival (69.3% and 71.9%). After 42 months, Psoriasis Area and Severity Index (PASI) 90 was achieved by 79.6% of patients overall; with a similar proportion of biologic-naïve and biologic-experienced patients achieving PASI90 (79.8% and 79.1%). The mean absolute PASI score reduced from 21.94 to 1.38 in the overall population, 21.90 to 1.24 in biologic-naïve and 22.03 to 1.77 in biologic-experienced patients after 42 months. The decrease in the absolute PASI score was comparable between HLA-Cw6–positive and HLA–Cw6-negative patients. The baseline Dermatology Life Quality Index scores also decreased in the overall patients (10.5 to 2.32) and across all study sub-groups after 42 months. Safety was consistent with the known profile of secukinumab, with no new findings. Conclusion: In this real-world cohort study, secukinumab showed consistently high long-term drug survival and effectiveness with a favourable safety profile.

Published
2023

7. Efficacy and Safety of Secukinumab in Elderly Patients with Moderate to Severe Plaque-Type Psoriasis: Post-Hoc Analysis of the SUPREME Study

Author

Talamonti, Marina, primary, Russo, Filomena, additional, Malara, Giovanna, additional, Hansel, Katharina, additional, Papini, Manuela, additional, Cattaneo, Angelo, additional, Parodi, Aurora, additional, Chiricozzi, Andrea, additional, Malagoli, Piergiorgio, additional, Bardazzi, Federico, additional, Brazzelli, Valeria, additional, Dapavo, Paolo, additional, Gisondi, Paolo, additional, Zane, Cristina, additional, Potenza, Concetta, additional, Cantoresi, Franca, additional, Fargnoli, Maria Concetta, additional, Trevisini, Sara, additional, Brianti, Pina, additional, Pescitelli, Leonardo, additional, Gigante, Giovanni, additional, Bartezaghi, Marta, additional, Caputo, Luisa, additional, Aloisi, Elisabetta, additional, and Costanzo, Antonio, additional

Published
2023
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8. Efficacy of Secukinumab in Psoriasis: Post Hoc Gender-Wise Analysis of the SUPREME Study

Author

Stingeni, Luca, primary, Malara, Giovanna, additional, Conti, Andrea, additional, Di Costanzo, Luisa, additional, Carrera, Carlo Giovanni, additional, Burlando, Martina, additional, Malagoli, Piergiorgio, additional, Musumeci, Maria Letizia, additional, Bardazzi, Federico, additional, Brazzelli, Valeria, additional, Amerio, Paolo, additional, De Simone, Clara, additional, Trevisini, Sara, additional, Balato, Anna, additional, Megna, Matteo, additional, Loconsole, Francesco, additional, De Felice, Catia, additional, Bartezaghi, Marta, additional, Rausa, Alice, additional, Aloisi, Elisabetta, additional, Orsenigo, Roberto, additional, and Costanzo, Antonio, additional

Published
2023
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9. Secukinumab Exhibits Sustained and Stable Response in Patients with Moderate-to-Severe Psoriasis: Results from the SUPREME Study

Author

Costanzo, Antonio, primary, Russo, Filomena, additional, Galluzzo, Marco, additional, Stingeni, Luca, additional, Scuderi, Roberta, additional, Zichichi, Leonardo, additional, Papini, Manuela, additional, Di Costanzo, Luisa, additional, Conti, Andrea, additional, Burlando, Martina, additional, Chiricozzi, Andrea, additional, Gaiani, Francesca Maria, additional, Mugheddu, Cristina, additional, Musumeci, Maria Letizia, additional, Gisondi, Paolo, additional, Piaserico, Stefano, additional, Dapavo, Paolo, additional, Venturini, Marina, additional, Pagnanelli, Gianluca, additional, Amerio, Paolo, additional, Potenza, Concetta, additional, Peris, Ketty, additional, Cantoresi, Franca, additional, Trevisini, Sara, additional, Loconsole, Francesco, additional, Offidani, Annamaria, additional, Mercuri, Santo Raffaele, additional, Lora, Viviana, additional, Prignano, Francesca, additional, Bartezaghi, Marta, additional, Oliva, Giovanni, additional, Aloisi, Elisabetta, additional, and Orsenigo, Roberto, additional

Published
2021
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11. Altered surface mGluR5 dynamics provoke synaptic NMDAR dysfunction and cognitive defects in Fmr1 knockout mice

Author

Aloisi, Elisabetta, primary, Le Corf, Katy, additional, Dupuis, Julien, additional, Zhang, Pei, additional, Ginger, Melanie, additional, Labrousse, Virginie, additional, Spatuzza, Michela, additional, Georg Haberl, Matthias, additional, Costa, Lara, additional, Shigemoto, Ryuichi, additional, Tappe-Theodor, Anke, additional, Drago, Filippo, additional, Vincenzo Piazza, Pier, additional, Mulle, Christophe, additional, Groc, Laurent, additional, Ciranna, Lucia, additional, Catania, Maria Vincenza, additional, and Frick, Andreas, additional

Published
2017
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12. Potential Involvement of Impaired BKCa Channel Function in Sensory Defensiveness and Some Behavioral Disturbances Induced by Unfamiliar Environment in a Mouse Model of Fragile X Syndrome

Author

Carreno-Munoz, Maria Isabel, primary, Martins, Fabienne, additional, Medrano, Maria Carmen, additional, Aloisi, Elisabetta, additional, Pietropaolo, Susanna, additional, Dechaud, Corentin, additional, Subashi, Enejda, additional, Bony, Guillaume, additional, Ginger, Melanie, additional, Moujahid, Abdelmalik, additional, Frick, Andreas, additional, and Leinekugel, Xavier, additional

Published
2017
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13. Involvement of mGluR5/Homer crosstalk disruption in the pathophysiology of Fragile X Syndrome

Author

Aloisi, Elisabetta Gabriella

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, nervous system, Fragile X Syndrome, mGluR5, Homer, Area 06 - Scienze mediche, animal diseases, mental disorders
Abstract

Fragile X Syndrome (FXS) is the most common inherited form of intellectual disability and autism. FXS is caused by a mutation in the fragile X mental retardation 1 (Fmr1) gene which leads to the lack of the encoded FMRP protein. FMRP is an RNA binding protein involved in protein synthesis regulation at synapses. Many evidences suggest a central role of the Group-I metabotropic glutamate receptor subtype 5 (mGluR5) in the FXS pathophysiology. In particular, an exaggerated signaling response following mGluR5 activation may underlie synaptic dysfunction in this disorder. Although much work has focused on the dysregulation of synaptic protein synthesis as a consequence of this enhanced mGluR5 signaling, it becomes clear that in FXS there is also an altered balance of mGluR5 association with Homer scaffolding proteins, which are postsynaptic density (PSD) partners of mGluR5. Although an extensive literature describes the mGluR5/Homer association, very little is known about the consequences of the disruption of this interaction in the FXS context. Therefore, the goal of my thesis was to study the consequences of mGluR5/Homer crosstalk disruption in the Fmr1 knockout (KO) mouse model of FXS in term of properties and functions of mGluR5, such as expression during development, surface expression and axonal/dendritic targeting, agonist-induced internalization, surface dynamics and mGluR5-mediated modulation of NMDA receptor (NMDAR) currents. In a first set of experiments we investigated the mGluR5 surface expression in cultured hippocampal neurons from WT and Fmr1 KO mice by using immunofluorescence techniques and biotinylation assay. We found that mGluR5 was more expressed on the neuronal surface and was differently distributed in dendrites and axons of Fmr1 KO cultured neurons. We then hypothesized that these alterations were a direct consequence of the mGluR5/Homer crosstalk disruption. We demonstrated that these altered expression and targeting of mGluR5 were critically dependent on mGluR5/Homer crosstalk disruption. We also observed that mGluR5 did not undergo internalization upon sustained mGluR5 activation with DHPG in Fmr1 KO neurons. This latter phenotype, however, was not dependent on the disruption of the mGluR5/Homer crosstalk. Altogether, these results demonstrate that mGluR5/Homer crosstalk disruption contributes to the pathophysiology of FXS altering expression and targeting of mGluR5 on the surface of Fmr1 KO neurons. In the second part of my study we investigated the consequences of the disrupted mGluR5/Homer crosstalk for the mGluR5 surface dynamics, and consequently for NMDAR function in Fmr1 KO neurons. Using a combination of live-cell imaging and single-molecule tracking, we found that mGluR5/Homer crosstalk disruption specifically increased the mGluR5 lateral diffusion at the synapse of cultured Fmr1 KO hippocampal neurons. The higher mGluR5 mobility resulted in an increased probability of transient physical interaction with NMDAR in the PSD of Fmr1 KO. This interaction altered the mGluR5-mediated modulation of NMDAR currents as evidenced by the two following changes. First, using patch-clamp recordings from CA1 pyramidal neurons, we found that NMDAR-mediated excitatory postsynaptic currents (NMDAR-EPSCs) evoked by Schaffer collateral stimulation showed lower amplitudes in Fmr1 KO neurons. Second, the postsynaptic expression of mGluR5 mediated long term depression (LTD) of NMDAR-EPSCs was reduced in Fmr1 KO neurons. Finally, we demonstrated that these defects in NMDA currents were strongly dependent on the mGluR5/Homer crosstalk disruption and altered mGluR5 dynamics. Our results show that mGluR5/Homer disruption contributes to the mGluR5 dysregulation in Fmr1 KO neurons. This study might have implication for the treatment of mGluR5 synaptic dysfunctions in FXS by targeting mGluR5/Homer interaction and provide new suggestions to correct the defective signaling underlying cognitive impairment and autism.

Published
2015

14. Involvement of mGluR5/Homer crosstalk disruption in the pathophysiology of Fragile X Syndrome

Author

ALOISI, Elisabetta, Physiopathologie de la plasticité neuronale, Université Bordeaux Segalen - Bordeaux 2, Université de Bordeaux, Università degli studi (Catane, Italie), Pier Vincenzo Piazza, Maria Vincenza Catania, STAR, ABES, Piazza, Pier Vincenzo, Catania, Maria Vincenza, Perciavalle, Vincenzo, Renato, Coradetti, and Pierangelo, Gepetti

Subjects
Fragile X Syndrom, Protéines Homer, Syndrome de l'X Fragile, MGluR5, [SDV.NEU]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], [SDV.NEU] Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Homer proteins
Abstract

Fragile X Syndrome (FXS) is the most common inherited form of intellectual disability and autism. FXS is caused by a mutation in the fragile X mental retardation 1(Fmr1) gene which leads to the lack of the encoded FMRP protein. FMRP is an RNA binding protein involved in protein synthesis regulation at synapses. Many evidences suggest a central role of the Group-I metabotropic glutamate receptor subtype 5(mGluR5) in the FXS pathophysiology. In particular, an exaggerated signaling response following mGluR5 activation may underlie synaptic dysfunction in this disorder. Although much work has focused on the dysregulation of synaptic protein synthesis as aconsequence of this enhanced mGluR5 signaling, it becomes clear that in FXS there is also an altered balance of mGluR5 association with Homer scaffolding proteins, whichare postsynaptic density (PSD) partners of mGluR5. Although an extensive literature describes the mGluR5/Homer association, very little is known about the consequences of the disruption of this interaction in the FXS context. Therefore, the goal of my thesis was to study the consequences of mGluR5/Homer crosstalk disruption in the Fmr1 knockout(KO) mouse model of FXS in terms of properties and functions of mGluR5, such as expression during development, surface expression and axonal/dendritic targeting, agonist-induced internalization, surface dynamics and mGluR5-mediated modulation ofNMDA receptor (NMDAR) currents. In a first set of experiments we investigated the mGluR5 surface expression incultured hippocampal neurons from WT and Fmr1 KO mice by using immunofluorescence techniques and biotinylation assay. We found that mGluR5 was more expressed on the neuronal surface and was differently distributed in dendrites andaxons of Fmr1 KO cultured neurons. We then hypothesized that these alterations were adirect consequence of the mGluR5/Homer crosstalk disruption. We demonstrated that the altered expression and targeting of mGluR5 were critically dependent on mGluR5/Homer crosstalk disruption. We also observed that mGluR5 did not undergo internalization upon sustained mGluR5 activation with DHPG in Fmr1 KO neurons. This latter phenotype, however, was not dependent on the disruption of the mGluR5/Homer crosstalk. Altogether, these results demonstrate that mGluR5/Homer crosstalk disruption contributes to the pathophysiology of FXS altering expression and targeting of mGluR5 on the surface of Fmr1 KO neurons. In the second part of my study we investigated the consequences of the disrupted mGluR5/Homer crosstalk for the mGluR5 surface dynamics, and consequently for NMDAR function in Fmr1 KO neurons. Using a combination of live-cell imaging and single-molecule tracking, we found that mGluR5/Homer crosstalk disruption specifically increased the mGluR5 lateral diffusion at the synapse of cultured Fmr1 KO hippocampal neurons. The higher mGluR5 mobility resulted in an increased probability of transient physical interaction with NMDAR in the PSD of Fmr1 KO. This interaction altered the mGluR5-mediated modulation of NMDAR currents as evidenced by the two following changes. First, using patch-clamp recordings from CA1 pyramidal neurons, we found that NMDAR-mediated excitatory postsynaptic currents (NMDAR-EPSCs) evoked by Schaffer collateral stimulation showed lower amplitudes in Fmr1 KO neurons. Second, the postsynaptic expression of mGluR5 mediated long term depression (LTD) of NMDAR-EPSCs was reduced in Fmr1 KO neurons. Finally, we demonstrated that these defects in NMDA currents were strongly dependent on the mGluR5/Homer crosstalk disruption and altered mGluR5 dynamics. Altogether, our results show that mGluR5/Homer disruption contributes to the mGluR5 dysregulation in Fmr1 KO neurons. This study might have implication for the treatment of mGluR5 synaptic dysfunctions in FXS by targeting mGluR5/Homer interaction and provide new suggestions to correct the defective signaling underly ingcognitive impairment and autism., Le Syndrome de l'X Fragile (FXS) est la forme héréditaire majoritaire de déficience intellectuelle et la cause monogénique de l'autisme. Le FXS est causé par une mutation du gène Fragile X Mental Retardation 1 (Fmr1), qui entraîne son inactivation et l'absence d’expression de la protéine codée: Fragile X Mental Retardation Protein(FMRP). FMRP est une protéine de liaison à l’ARN, impliquée dans la régulation de la synthèse protéiques à la synapse. Un rôle central est attribué au sous-type 5 des récepteurs métabotropiques au glutamate du groupe I (mGluR5) dans la physiopathologie du FXS. En effet, une réponse exagérée suite à l'activation de mGluR5 pourrait expliquer le dysfonctionnement synaptique dans ce syndrôme. Bien que de nombreux travaux aient mis l'accent sur la dérégulation de la synthèse des protéines synaptiques comme une conséquence de cette signalisation accrue du mGluR5, il y a aussi un équilibre altéré dans l'association de mGluR5 avec les différentes isoformes des protéines Homer, partenaires de densité post-synaptique (PSD) du mGluR5. Bien qu'une abondante littérature décrit l'association mGluR5/Homer, les conséquences de la perturbation de cette interaction dans le contexte du FXS sont peu connues. Par conséquent, l'objectif de ma thèse était d'étudier les conséquences de la perturbation de l’interaction mGluR5/Homer au niveau des propriétés et des fonctions de mGluR5, telles que l'expression durant le développement, l'expression de surface et le ciblage axonal/dendritique, l’internalisation déclenchée par l'agoniste, les dynamiques de surface, et la modulation des courants NMDAR induite par mGluR5. Dans un premier temps, nous avons étudié l’expression de surface de mGluR5 dans des neurones hippocampiques in vitro issus de souris sauvages et Fmr1 KO, par des techniques d’immunofluorescence et de biotinylation. Nous avons constaté que mGluR5 est plus exprimé à la surface neuronale et est différemment distribué dans les dendrites et les axones des neurones Fmr1 KO. Puis, nous avons démontré que cette altération d’expression et de ciblage est une conséquence directe de l’altération de l’interaction mGluR5/Homer. Nous avons aussi observé que mGluR5, indépendamment de l’altération de l’interaction mGluR5/Homer, ne subit pas d’internalisation suite son activation soutenue par DHPG dans les neurones Fmr1 KO. Dans la seconde partie de mon étude, nous avons étudié les conséquences de la perturbation de l’interaction mGluR5/Homer dans les dynamiques de surface de mGluR5 et par conséquent pour la fonction du NMDAR dans les neurones Fmr1 KO. Par des techniques d'imagerie et de pistage moléculaire, nous avons constaté que l’altération du complexe mGluR5/Homer augmente spécifiquement la diffusion latérale à la synapse des neurones hippocampiques Fmr1 KO in vitro. La mobilité élevée du mGluR5 conduit à une probabilité accrue d'une interaction physique transitoire avec NMDAR dans la PSD du Fmr1 KO. Cette interaction altère la modulation, induite par mGluR5, des courants NMDAR. En effet, en utilisant des enregistrements en patch-clamp de neurones pyramidaux de CA1 sur tranches couplés à la stimulation des fibres collatérales de Schaffer, nous avons constaté que les courants excitateurs post-synaptiques induits par NMDAR (NMDAR-EPSCs) présentent des amplitudes plus faibles dans les neurones Fmr1 KO. De plus, l'expression post-synaptique de mGluR5, induite par la dépression à long-terme de NMDAR-EPSCs est réduite dans les neurones Fmr1 KO. Finalement, nous avons démontré que ces défauts des courants NMDAR sont dépendants de la perturbation de l’interaction mGluR5/Homer et altèrent les dynamiques de mGluR5. Cette étude pourrait avoir des conséquences dans le traitement des dysfonctionnements synaptiques du mGluR5 dans le FXS, en ciblant l’interactionmGluR5/Homer, et offre de nouvelles suggestions pour corriger la signalisation défectueuse sous-jacente aux troubles du spectre autistique.

Published
2015

15. Participation de la perturbation de l'interaction entre mGluR5 et Homer dans la physiopathologie du Syndrome de l'X Fragile

Author

Aloisi, Elisabetta, Physiopathologie de la plasticité neuronale, Université Bordeaux Segalen - Bordeaux 2, Université de Bordeaux, Università degli studi (Catane, Italie), Pier Vincenzo Piazza, Maria Vincenza Catania, and STAR, ABES

Subjects
Fragile X Syndrom, Protéines Homer, Syndrome de l'X Fragile, MGluR5, [SDV.NEU]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], [SDV.NEU] Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Homer proteins
Abstract

Fragile X Syndrome (FXS) is the most common inherited form of intellectual disability and autism. FXS is caused by a mutation in the fragile X mental retardation 1(Fmr1) gene which leads to the lack of the encoded FMRP protein. FMRP is an RNA binding protein involved in protein synthesis regulation at synapses. Many evidences suggest a central role of the Group-I metabotropic glutamate receptor subtype 5(mGluR5) in the FXS pathophysiology. In particular, an exaggerated signaling response following mGluR5 activation may underlie synaptic dysfunction in this disorder. Although much work has focused on the dysregulation of synaptic protein synthesis as aconsequence of this enhanced mGluR5 signaling, it becomes clear that in FXS there is also an altered balance of mGluR5 association with Homer scaffolding proteins, whichare postsynaptic density (PSD) partners of mGluR5. Although an extensive literature describes the mGluR5/Homer association, very little is known about the consequences of the disruption of this interaction in the FXS context. Therefore, the goal of my thesis was to study the consequences of mGluR5/Homer crosstalk disruption in the Fmr1 knockout(KO) mouse model of FXS in terms of properties and functions of mGluR5, such as expression during development, surface expression and axonal/dendritic targeting, agonist-induced internalization, surface dynamics and mGluR5-mediated modulation ofNMDA receptor (NMDAR) currents. In a first set of experiments we investigated the mGluR5 surface expression incultured hippocampal neurons from WT and Fmr1 KO mice by using immunofluorescence techniques and biotinylation assay. We found that mGluR5 was more expressed on the neuronal surface and was differently distributed in dendrites andaxons of Fmr1 KO cultured neurons. We then hypothesized that these alterations were adirect consequence of the mGluR5/Homer crosstalk disruption. We demonstrated that the altered expression and targeting of mGluR5 were critically dependent on mGluR5/Homer crosstalk disruption. We also observed that mGluR5 did not undergo internalization upon sustained mGluR5 activation with DHPG in Fmr1 KO neurons. This latter phenotype, however, was not dependent on the disruption of the mGluR5/Homer crosstalk. Altogether, these results demonstrate that mGluR5/Homer crosstalk disruption contributes to the pathophysiology of FXS altering expression and targeting of mGluR5 on the surface of Fmr1 KO neurons. In the second part of my study we investigated the consequences of the disrupted mGluR5/Homer crosstalk for the mGluR5 surface dynamics, and consequently for NMDAR function in Fmr1 KO neurons. Using a combination of live-cell imaging and single-molecule tracking, we found that mGluR5/Homer crosstalk disruption specifically increased the mGluR5 lateral diffusion at the synapse of cultured Fmr1 KO hippocampal neurons. The higher mGluR5 mobility resulted in an increased probability of transient physical interaction with NMDAR in the PSD of Fmr1 KO. This interaction altered the mGluR5-mediated modulation of NMDAR currents as evidenced by the two following changes. First, using patch-clamp recordings from CA1 pyramidal neurons, we found that NMDAR-mediated excitatory postsynaptic currents (NMDAR-EPSCs) evoked by Schaffer collateral stimulation showed lower amplitudes in Fmr1 KO neurons. Second, the postsynaptic expression of mGluR5 mediated long term depression (LTD) of NMDAR-EPSCs was reduced in Fmr1 KO neurons. Finally, we demonstrated that these defects in NMDA currents were strongly dependent on the mGluR5/Homer crosstalk disruption and altered mGluR5 dynamics. Altogether, our results show that mGluR5/Homer disruption contributes to the mGluR5 dysregulation in Fmr1 KO neurons. This study might have implication for the treatment of mGluR5 synaptic dysfunctions in FXS by targeting mGluR5/Homer interaction and provide new suggestions to correct the defective signaling underly ingcognitive impairment and autism., Le Syndrome de l'X Fragile (FXS) est la forme héréditaire majoritaire de déficience intellectuelle et la cause monogénique de l'autisme. Le FXS est causé par une mutation du gène Fragile X Mental Retardation 1 (Fmr1), qui entraîne son inactivation et l'absence d’expression de la protéine codée: Fragile X Mental Retardation Protein(FMRP). FMRP est une protéine de liaison à l’ARN, impliquée dans la régulation de la synthèse protéiques à la synapse. Un rôle central est attribué au sous-type 5 des récepteurs métabotropiques au glutamate du groupe I (mGluR5) dans la physiopathologie du FXS. En effet, une réponse exagérée suite à l'activation de mGluR5 pourrait expliquer le dysfonctionnement synaptique dans ce syndrôme. Bien que de nombreux travaux aient mis l'accent sur la dérégulation de la synthèse des protéines synaptiques comme une conséquence de cette signalisation accrue du mGluR5, il y a aussi un équilibre altéré dans l'association de mGluR5 avec les différentes isoformes des protéines Homer, partenaires de densité post-synaptique (PSD) du mGluR5. Bien qu'une abondante littérature décrit l'association mGluR5/Homer, les conséquences de la perturbation de cette interaction dans le contexte du FXS sont peu connues. Par conséquent, l'objectif de ma thèse était d'étudier les conséquences de la perturbation de l’interaction mGluR5/Homer au niveau des propriétés et des fonctions de mGluR5, telles que l'expression durant le développement, l'expression de surface et le ciblage axonal/dendritique, l’internalisation déclenchée par l'agoniste, les dynamiques de surface, et la modulation des courants NMDAR induite par mGluR5. Dans un premier temps, nous avons étudié l’expression de surface de mGluR5 dans des neurones hippocampiques in vitro issus de souris sauvages et Fmr1 KO, par des techniques d’immunofluorescence et de biotinylation. Nous avons constaté que mGluR5 est plus exprimé à la surface neuronale et est différemment distribué dans les dendrites et les axones des neurones Fmr1 KO. Puis, nous avons démontré que cette altération d’expression et de ciblage est une conséquence directe de l’altération de l’interaction mGluR5/Homer. Nous avons aussi observé que mGluR5, indépendamment de l’altération de l’interaction mGluR5/Homer, ne subit pas d’internalisation suite son activation soutenue par DHPG dans les neurones Fmr1 KO. Dans la seconde partie de mon étude, nous avons étudié les conséquences de la perturbation de l’interaction mGluR5/Homer dans les dynamiques de surface de mGluR5 et par conséquent pour la fonction du NMDAR dans les neurones Fmr1 KO. Par des techniques d'imagerie et de pistage moléculaire, nous avons constaté que l’altération du complexe mGluR5/Homer augmente spécifiquement la diffusion latérale à la synapse des neurones hippocampiques Fmr1 KO in vitro. La mobilité élevée du mGluR5 conduit à une probabilité accrue d'une interaction physique transitoire avec NMDAR dans la PSD du Fmr1 KO. Cette interaction altère la modulation, induite par mGluR5, des courants NMDAR. En effet, en utilisant des enregistrements en patch-clamp de neurones pyramidaux de CA1 sur tranches couplés à la stimulation des fibres collatérales de Schaffer, nous avons constaté que les courants excitateurs post-synaptiques induits par NMDAR (NMDAR-EPSCs) présentent des amplitudes plus faibles dans les neurones Fmr1 KO. De plus, l'expression post-synaptique de mGluR5, induite par la dépression à long-terme de NMDAR-EPSCs est réduite dans les neurones Fmr1 KO. Finalement, nous avons démontré que ces défauts des courants NMDAR sont dépendants de la perturbation de l’interaction mGluR5/Homer et altèrent les dynamiques de mGluR5. Cette étude pourrait avoir des conséquences dans le traitement des dysfonctionnements synaptiques du mGluR5 dans le FXS, en ciblant l’interactionmGluR5/Homer, et offre de nouvelles suggestions pour corriger la signalisation défectueuse sous-jacente aux troubles du spectre autistique.

Published
2015

17. Potential Involvement of Impaired BKCaChannel Function in Sensory Defensiveness and Some Behavioral Disturbances Induced by Unfamiliar Environment in a Mouse Model of Fragile X Syndrome

Author

Carreno-Munoz, Maria Isabel, Martins, Fabienne, Medrano, Maria Carmen, Aloisi, Elisabetta, Pietropaolo, Susanna, Dechaud, Corentin, Subashi, Enejda, Bony, Guillaume, Ginger, Melanie, Moujahid, Abdelmalik, Frick, Andreas, and Leinekugel, Xavier

Abstract

In fragile X syndrome (FXS), sensory hypersensitivity and impaired habituation is thought to result in attention overload and various behavioral abnormalities in reaction to the excessive and remanent salience of environment features that would normally be ignored. This phenomenon, termed sensory defensiveness, has been proposed as the potential cause of hyperactivity, hyperarousal, and negative reactions to changes in routine that are often deleterious for FXS patients. However, the lack of tools for manipulating sensory hypersensitivity has not allowed the experimental testing required to evaluate the relevance of this hypothesis. Recent work has shown that BMS-204352, a BKCachannel agonist, was efficient to reverse cortical hyperexcitability and related sensory hypersensitivity in the Fmr1-KO mouse model of FXS. In the present study, we report that exposing Fmr1-KO mice to novel or unfamiliar environments resulted in multiple behavioral perturbations, such as hyperactivity, impaired nest building and excessive grooming of the back. Reversing sensory hypersensitivity with the BKCachannel agonist BMS-204352 prevented these behavioral abnormalities in Fmr1-KO mice. These results are in support of the sensory defensiveness hypothesis, and confirm BKCaas a potentially relevant molecular target for the development of drug medication against FXS/ASD.

Published
2018
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18. Efficacy of Secukinumab in Psoriasis: Post Hoc Gender-Wise Analysis of the SUPREME Study

Author

Luca Stingeni, Giovanna Malara, Andrea Conti, Luisa Di Costanzo, Carlo Giovanni Carrera, Martina Burlando, Piergiorgio Malagoli, Maria Letizia Musumeci, Federico Bardazzi, Valeria Brazzelli, Paolo Amerio, Clara De Simone, Sara Trevisini, Anna Balato, Matteo Megna, Francesco Loconsole, Catia De Felice, Marta Bartezaghi, Alice Rausa, Elisabetta Aloisi, Roberto Orsenigo, Antonio Costanzo, Stingeni, Luca, Malara, Giovanna, Conti, Andrea, Di Costanzo, Luisa, Carrera, Carlo Giovanni, Burlando, Martina, Malagoli, Piergiorgio, Musumeci, Maria Letizia, Bardazzi, Federico, Brazzelli, Valeria, Amerio, Paolo, De Simone, Clara, Trevisini, Sara, Balato, Anna, Megna, Matteo, Loconsole, Francesco, De Felice, Catia, Bartezaghi, Marta, Rausa, Alice, Aloisi, Elisabetta, Orsenigo, Roberto, and Costanzo, Antonio

Subjects
Hospital Anxiety and Depression Scale, Clinical, Cosmetic and Investigational Dermatology, patient-reported outcomes, Dermatology Quality of Life Index, PASI, Dermatology, patient-reported outcome, plaque psoriasis
Abstract

Luca Stingeni,1 Giovanna Malara,2,3 Andrea Conti,4 Luisa Di Costanzo,5 Carlo Giovanni Carrera,6 Martina Burlando,7 Piergiorgio Malagoli,8 Maria Letizia Musumeci,9 Federico Bardazzi,10 Valeria Brazzelli,11 Paolo Amerio,12 Clara De Simone,13,14 Sara Trevisini,15 Anna Balato,16 Matteo Megna,17 Francesco Loconsole,18 Catia De Felice,19 Marta Bartezaghi,20 Alice Rausa,20 Elisabetta Aloisi,20 Roberto Orsenigo,20 Antonio Costanzo21,22 On behalf of the SUPREME Study Group1Dermatology Section, Medical and Surgical Department, University of Perugia, Perugia, Italy; 2Dermatology Unit, Hospital “Bianchi Melacrino Morelli”, Reggio Calabria, Italy; 3Department of Dermatology, Papardo Hospital, Messina, Italy; 4Dermatologic Unit, Department of Surgery, Infermi Hospital, AUSL Romagna, Rimini, Italy; 5Department of Dermatology, “Gaetano Rummo” Hospital, Benevento UOC Dermatologia, AO G. Rummo, Benevento, Italy; 6U.O. Dermatologia, Fondazione IRCCS Ca’ Granda - Ospedale Maggiore Policlinico, Milano, Italy; 7IRCCS San Martino Polyclinic Hospital, Di.S.Sal. Section of Dermatology, Genoa, Italy; 8Dermatology Unit IRCCS Policlinico San Donato, Milan, Italy; 9Dermatology Clinic, University of Catania, Catania, Italy; 10Division of Dermatology, University Hospital Policlinico “S. Orsola-Malpighi”, Bologna, Italy; 11Institute of Dermatology, Foundation IRCCS Policlinico San Matteo and University of Pavia, Pavia, Italy; 12Dermatologic Clinic, G. D’Annunzio University, Chieti, Italy; 13Istituto di Dermatologia, Università Cattolica del Sacro Cuore, Rome, Italy; 14Fondazione Policlinico Universitario A. Gemelli – IRCCS, Rome, Italy; 15Dermatology Department, University of Trieste, Trieste, Italy; 16Dermatology Unit, University of Campania “Luigi Vanvitelli”, Naples, Italy; 17Section of Dermatology, Department of Clinical Medicine and Surgery, University of Naples Federico II, Naples, Italy; 18Department of Biomedical Sciences and Human Oncology, University of Bari, Bari, Italy; 19Department of Clinical Dermatology, Centre for the Study and Treatment of Psoriasis, San Gallicano Dermatological Institute, IRCCS, Rome, Italy; 20Novartis Farma SpA, Origgio, Italy; 21Unit of Dermatology, IRCCS Humanitas Research Hospital, Milan, Italy; 22Department of Biomedical Sciences, Humanitas University, Milan, ItalyCorrespondence: Luca Stingeni, Dermatology Section, Medical and Surgical Department, University of Perugia, Perugia, Italy, Tel +39075-5783881, Email luca.stingeni@unipg.itPurpose: Psoriasis, a common systemic inflammatory disorder, presents with gender-related differences in the quality of life (QoL) and treatment outcomes. This post hoc analysis from the Phase 3b SUPREME study explored gender-related differences in patient characteristics and efficacy of secukinumab 300 mg on Psoriasis Area and Severity Index (PASI) 75/90/100 and impact on QoL using the Dermatology Life Quality Index (DLQI) in patients with moderate to severe psoriasis through week 24.Patients and Methods: The proportion of patients achieving PASI 75/90/100 was computed using a nonresponder imputation approach. Differences between cohorts were analyzed using a logistic regression model. The mean change from baseline in DLQI was computed using the Wilcoxon test.Results: Among the 433 patients (males: 71.6%), females had a higher DLQI than males at baseline (13.1 vs 9.5; P< 0.0001). Males had a slightly higher response for PASI 90 than females at week 16 (80.7% vs 78.1%; P=0.0779) and 24 (83.2% vs 79.7%; P=0.0319). No differences were observed between genders in PASI 100/75 responses at week 24. Both genders showed an improvement in DLQI with secukinumab at week 24 (− 10.9 vs − 8.1, respectively, in females vs males; P=0.0004).Conclusion: In summary, secukinumab was effective in the treatment of psoriasis, irrespective of gender.Keywords: plaque psoriasis, PASI, patient-reported outcomes, Dermatology Quality of Life Index, Hospital Anxiety and Depression Scale

Published
2023

19. Secukinumab Improves Patient Perception of Anxiety and Depression in Patients with Moderate to Severe Psoriasis: A Post hoc Analysis of the SUPREME Study

Author

M Talamonti, G Malara, Y Natalini, F Bardazzi, A Conti, A Chiricozzi, C Mugheddu, P Gisondi, S Piaserico, G Pagnanelli, P Amerio, C Potenza, F Cantoresi, M Fargnoli, A Balato, F Loconsole, A Offidani, C Bonifati, F Prignano, M Bartezaghi, A Rausa, E Aloisi, R Orsenigo, A Costanzo, f Group, Talamonti, Marina, Malara, Giovanna, Natalini, Ylenia, Bardazzi, Federico, Conti, Andrea, Chiricozzi, Andrea, Mugheddu, Cristina, Gisondi, Paolo, Piaserico, Stefano, Pagnanelli, Gianluca, Amerio, Paolo, Potenza, Concetta, Cantoresi, Franca, Fargnoli, Maria Concetta, Balato, Anna, Loconsole, Francesco, Offidani, Annamaria, Bonifati, Claudio, Prignano, Francesca, Bartezaghi, Marta, Rausa, Alice, Aloisi, Elisabetta, Orsenigo, Roberto, and Costanzo, Antonio

Subjects
depression, psoriasis, quality of life, secukinumab, anxiety, medicine.medical_specialty, Anxiety, Depression, Psoriasis, Quality of life, Secukinumab, Antibodies, Monoclonal, Antibodies, Monoclonal, Humanized, Double-Blind Method, Humans, Italy, Perception, Prospective Studies, Quality of Life, Severity of Illness Index, Treatment Outcome, Dermatology, Hospital Anxiety and Depression Scale, Antibodies, Settore MED/35, Internal medicine, Post-hoc analysis, Monoclonal, Medicine, Prospective cohort study, Humanized, Depression (differential diagnoses), psoriasi, business.industry, General Medicine, medicine.disease, RL1-803, medicine.symptom, Settore MED/35 - MALATTIE CUTANEE E VENEREE, business
Abstract

This study evaluated whether secukinumab treatment for patients with moderate to severe plaque psoriasis correlates with improvements in symptoms of anxiety and depression. SUPREME was a 24-week, phase IIIb, multicentre, prospective study conducted across 50 centres in Italy with an extension period of up to 72 weeks. Assessments used were: Psoriasis Area Sever-ity Index (PASI), Hospital Anxiety and Depression Scale (HADS) - Anxiety (HADS-A), and HADS - Depression (HADS-D) scores and Dermatology Quality Life Index (DLQI). Compared with baseline, a significantly greater proportion of patients who reported moderate to severe clinical symptoms of anxiety or depression (HADS-A or HADS-D ≥ 11) were free of moderate to severe symptoms at weeks 16 and 48. The PASI and DLQI scores reduced over time with secukinumab treatment. Psoriasis treatment with secukinumab for 48 weeks resulted in significantly improved skin clearance and a parallel improvement in symptoms of anxiety and depression, assessed by HADS.

Published
2020

20. Secukinumab Improves Patient Perception of Anxiety and Depression in Patients with Moderate to Severe Psoriasis: A Post hoc Analysis of the SUPREME Study.

Author

Talamonti M, Malara G, Natalini Y, Bardazzi F, Conti A, Chiricozzi A, Mugheddu C, Gisondi P, Piaserico S, Pagnanelli G, Amerio P, Potenza C, Cantoresi F, Fargnoli MC, Balato A, Loconsole F, Offidani A, Bonifati C, Prignano F, Bartezaghi M, Rausa A, Aloisi E, Orsenigo R, and Costanzo A

Subjects
Antibodies, Monoclonal adverse effects, Antibodies, Monoclonal, Humanized, Anxiety diagnosis, Anxiety drug therapy, Double-Blind Method, Humans, Italy, Perception, Prospective Studies, Quality of Life, Severity of Illness Index, Treatment Outcome, Depression diagnosis, Depression drug therapy, Psoriasis diagnosis, Psoriasis drug therapy
Abstract

This study evaluated whether secukinumab treatment for patients with moderate to severe plaque psoriasis correlates with improvements in symptoms of anxiety and depression. SUPREME was a 24-week, phase IIIb, multicentre, prospective study conducted across 50 centres in Italy with an extension period of up to 72 weeks. Assessments used were: Psoriasis Area Sever-ity Index (PASI), Hospital Anxiety and Depression Scale (HADS) - Anxiety (HADS-A), and HADS - Depression (HADS-D) scores and Dermatology Quality Life Index (DLQI). Compared with baseline, a significantly greater proportion of patients who reported moderate to severe clinical symptoms of anxiety or depression (HADS-A or HADS-D ≥ 11) were free of moderate to severe symptoms at weeks 16 and 48. The PASI and DLQI scores reduced over time with secukinumab treatment. Psoriasis treatment with secukinumab for 48 weeks resulted in significantly improved skin clearance and a parallel improvement in symptoms of anxiety and depression, assessed by HADS.

Published
2021
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21. Potential Involvement of Impaired BK Ca Channel Function in Sensory Defensiveness and Some Behavioral Disturbances Induced by Unfamiliar Environment in a Mouse Model of Fragile X Syndrome.

Author

Carreno-Munoz MI, Martins F, Medrano MC, Aloisi E, Pietropaolo S, Dechaud C, Subashi E, Bony G, Ginger M, Moujahid A, Frick A, and Leinekugel X

Subjects
Animals, Anti-Anxiety Agents pharmacology, Diazepam pharmacology, Disease Models, Animal, Environment, Fragile X Mental Retardation Protein genetics, Fragile X Mental Retardation Protein metabolism, Grooming drug effects, Indoles pharmacology, Large-Conductance Calcium-Activated Potassium Channel alpha Subunits agonists, Large-Conductance Calcium-Activated Potassium Channel alpha Subunits metabolism, Male, Mice, Knockout, Motor Activity drug effects, Nesting Behavior drug effects, Neurotransmitter Agents pharmacology, Psychotropic Drugs pharmacology, Recognition, Psychology, Stereotyped Behavior drug effects, Stereotyped Behavior physiology, Fragile X Syndrome physiopathology, Grooming physiology, Motor Activity physiology, Nesting Behavior physiology
Abstract

In fragile X syndrome (FXS), sensory hypersensitivity and impaired habituation is thought to result in attention overload and various behavioral abnormalities in reaction to the excessive and remanent salience of environment features that would normally be ignored. This phenomenon, termed sensory defensiveness, has been proposed as the potential cause of hyperactivity, hyperarousal, and negative reactions to changes in routine that are often deleterious for FXS patients. However, the lack of tools for manipulating sensory hypersensitivity has not allowed the experimental testing required to evaluate the relevance of this hypothesis. Recent work has shown that BMS-204352, a BK Ca channel agonist, was efficient to reverse cortical hyperexcitability and related sensory hypersensitivity in the Fmr1-KO mouse model of FXS. In the present study, we report that exposing Fmr1-KO mice to novel or unfamiliar environments resulted in multiple behavioral perturbations, such as hyperactivity, impaired nest building and excessive grooming of the back. Reversing sensory hypersensitivity with the BK Ca channel agonist BMS-204352 prevented these behavioral abnormalities in Fmr1-KO mice. These results are in support of the sensory defensiveness hypothesis, and confirm BK Ca as a potentially relevant molecular target for the development of drug medication against FXS/ASD.

Published
2018
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