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3. Correction: Clinical and laboratory features associated with macrophage activation syndrome in Still’s disease: data from the international AIDA Network Still’s Disease Registry

Author

Triggianese, Paola, Vitale, Antonio, Lopalco, Giuseppe, Mayrink Giardini, Henrique Ayres, Ciccia, Francesco, Al-Maghlouth, Ibrahim, Ruscitti, Piero, Sfikakis, Petros Paul, Iannone, Florenzo, de Brito Antonelli, Isabele Parente, Patrone, Martina, Asfina, Kazi Nur, Di Cola, Ilenia, Laskari, Katerina, Gaggiano, Carla, Tufan, Abdurrahman, Sfriso, Paolo, Dagna, Lorenzo, Giacomelli, Roberto, Hinojosa-Azaola, Andrea, Ragab, Gaafar, Fotis, Lampros, Direskeneli, Haner, Spedicato, Veronica, Dagostin, Marilia Ambiel, Iacono, Daniela, Ali, Hebatallah Hamed, Cipriani, Paola, Sota, Jurgen, Kardas, Riza Can, Bindoli, Sara, Campochiaro, Corrado, Navarini, Luca, Gentileschi, Stefano, Martín-Nares, Eduardo, Torres-Ruiz, Jiram, Saad, Moustafa Ali, Kourtesi, Katerina, Alibaz-Oner, Fatma, Sevik, Gizem, Iagnocco, Annamaria, Makowska, Joanna, Govoni, Marcello, Monti, Sara, Maggio, Maria Cristina, La Torre, Francesco, Del Giudice, Emanuela, Hernández-Rodríguez, José, Bartoloni, Elena, Emmi, Giacomo, Chimenti, Maria Sole, Maier, Armin, Simonini, Gabriele, Conti, Giovanni, Olivieri, Alma Nunzia, Tarsia, Maria, De Paulis, Amato, Lo Gullo, Alberto, Więsik-Szewczyk, Ewa, Viapiana, Ombretta, Ogunjimi, Benson, Tharwat, Samar, Erten, Sukran, Nuzzolese, Rossana, Karamanakos, Anastasios, Frassi, Micol, Conforti, Alessandro, Caggiano, Valeria, Marino, Achille, Sebastiani, Gian Domenico, Gidaro, Antonio, Tombetti, Enrico, Carubbi, Francesco, Rubegni, Giovanni, Cartocci, Alessandra, Balistreri, Alberto, Fabiani, Claudia, Frediani, Bruno, and Cantarini, Luca

Published
2024
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4. Clinical and laboratory features associated with macrophage activation syndrome in Still’s disease: data from the international AIDA Network Still’s Disease Registry

Author

Triggianese, Paola, Vitale, Antonio, Lopalco, Giuseppe, Mayrink Giardini, Henrique Ayres, Ciccia, Francesco, Al-Maghlouth, Ibrahim, Ruscitti, Piero, Sfikakis, Petros Paul, Iannone, Florenzo, de Brito Antonelli, Isabele Parente, Patrone, Martina, Asfina, Kazi Nur, Di Cola, Ilenia, Laskari, Katerina, Gaggiano, Carla, Tufan, Abdurrahman, Sfriso, Paolo, Dagna, Lorenzo, Giacomelli, Roberto, Hinojosa-Azaola, Andrea, Ragab, Gaafar, Fotis, Lampros, Direskeneli, Haner, Spedicato, Veronica, Dagostin, Marilia Ambiel, Iacono, Daniela, Ali, Hebatallah Hamed, Cipriani, Paola, Sota, Jurgen, Kardas, Riza Can, Bindoli, Sara, Campochiaro, Corrado, Navarini, Luca, Gentileschi, Stefano, Martín-Nares, Eduardo, Torres-Ruiz, Jiram, Saad, Moustafa Ali, Kourtesi, Katerina, Alibaz-Oner, Fatma, Sevik, Gizem, Iagnocco, Annamaria, Makowska, Joanna, Govoni, Marcello, Monti, Sara, Maggio, Maria Cristina, La Torre, Francesco, Del Giudice, Emanuela, Hernández-Rodríguez, José, Bartoloni, Elena, Emmi, Giacomo, Chimenti, Maria Sole, Maier, Armin, Simonini, Gabriele, Conti, Giovanni, Olivieri, Alma Nunzia, Tarsia, Maria, De Paulis, Amato, Lo Gullo, Alberto, Więsik-Szewczyk, Ewa, Viapiana, Ombretta, Ogunjimi, Benson, Tharwat, Samar, Erten, Sukran, Nuzzolese, Rossana, Karamanakos, Anastasios, Frassi, Micol, Conforti, Alessandro, Caggiano, Valeria, Marino, Achille, Sebastiani, Gian Domenico, Gidaro, Antonio, Tombetti, Enrico, Carubbi, Francesco, Rubegni, Giovanni, Cartocci, Alessandra, Balistreri, Alberto, Fabiani, Claudia, Frediani, Bruno, and Cantarini, Luca

Published
2023
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5. Orbital/ocular inflammatory involvement in VEXAS syndrome: Data from the international AIDA network VEXAS registry

Author

Vitale, Antonio, Caggiano, Valeria, Martin-Nares, Eduardo, Frassi, Micol, Dagna, Lorenzo, Hissaria, Pravin, Sfriso, Paolo, Hernández-Rodríguez, José, Ruiz-Irastorza, Guillermo, Monti, Sara, Tufan, Abdurrahman, Piga, Matteo, Giardini, Henrique A Mayrink, Lopalco, Giuseppe, Viapiana, Ombretta, De Paulis, Amato, Triggianese, Paola, Vitetta, Rosetta, de-la-Torre, Alejandra, Fonollosa, Alex, Caroni, Federico, Sota, Jurgen, Conticini, Edoardo, Sbalchiero, Jessica, Renieri, Alessandra, Casamassima, Giulia, Wiesik-Szewczyk, Ewa, Yildirim, Derya, Hinojosa-Azaola, Andrea, Crisafulli, Francesca, Franceschini, Franco, Campochiaro, Corrado, Tomelleri, Alessandro, Callisto, Alicia, Beecher, Mark, Bindoli, Sara, Baggio, Chiara, Gómez-Caverzaschi, Verónica, Pelegrín, Laura, Soto-Peleteiro, Adriana, Milanesi, Alessandra, Vasi, Ibrahim, Cauli, Alberto, Antonelli, Isabele Parente de Brito, Iannone, Florenzo, Bixio, Riccardo, Casa, Francesca Della, Mormile, Ilaria, Gurnari, Carmelo, Fiorenza, Alessia, Mejia-Salgado, Germán, Kawakami-Campos, Perla Ayumi, Ragab, Gaafar, Ciccia, Francesco, Ruscitti, Piero, Bocchia, Monica, Balistreri, Alberto, Tosi, Gian Marco, Frediani, Bruno, Cantarini, Luca, and Fabiani, Claudia

Published
2024
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6. Expert consensus on the treatment of patients with adult-onset still's disease with the goal of achieving an early and long-term remission

Author

Belfiore, Norma, Bernardi, Cristina, Gabini, Marco, Bettio, Silvano, Brucato, Antonio, Italiano, Giovanni, Cantatore, Francesco Paolo, Iacono, Daniela, Pantano, Ilenia, Tirri, Enrico, Ursini, Francesco, Monaco, Andrea Lo, Caso, Francesco, Quartuccio, Luca, Chimenti, Maria Sole, Gattamelata, Angelica, Gremese, Elisa, Paroli, Marino, Picchianti-Diamanti, Andrea, Sebastiani, Gian Domenico, Favalli, Ennio, Sulli, Alberto, Frassi, Micol, Faggioli, Paola, Foti, Rosario, Campochiaro, Corrado, Cavalli, Giulio, Tomelleri, Alessandro, Manara, Maria, De Stefano, Ludovico, De Angelis, Rossella, Parisi, Simone, Lopalco, Giuseppe, Piga, Matteo, Marotto, Daniela, Colaci, Michele, Padula, Angela, Guggino, Giuliana, Emmi, Giacomo, Baldini, Chiara, Sota, Jurgen, Vitale, Antonio, Berti, Alvise, Bartoloni, Elena, Grava, Chiara, Bindoli, Sara, Vitetta, Rosetta, Giacomelli, Roberto, Caporali, Roberto, Ciccia, Francesco, Colafrancesco, Serena, Dagna, Lorenzo, Govoni, Marcello, Iannone, Florenzo, Leccese, Pietro, Montecucco, Carlomaurizio, Pappagallo, Giovanni, Pistone, Giovanni, Priori, Roberta, Ruscitti, Piero, Sfriso, Paolo, and Cantarini, Luca

Published
2023
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7. Expanding the VEXAS diagnostic workup: the role of peripheral blood cytological analysis.

Author

Baggio, Chiara, Oliviero, Francesca, Padoan, Roberto, Iorio, Luca, Bixio, Riccardo, Orsolini, Giovanni, Bertoldo, Eugenia, Bernardi, Cristina, Colavito, Davide, Paiero, Barbara, Pregnolato, Giovanna, Ramonda, Roberta, Doria, Andrea, Bindoli, Sara, and Sfriso, Paolo

Subjects
BONE marrow cells, SOMATIC mutation, FAMILIAL Mediterranean fever, PROGENITOR cells, CELL death
Abstract

VEXAS syndrome is a newly described autoinflammatory entity characterized by somatic mutations in the UBA1 X-linked gene in hematopoietic progenitor cells. Several studies have demonstrated that the presence of vacuoles in progenitor cells from bone marrow aspirates is a hallmark finding for this syndrome. Therefore, this study aimed to characterize leukocytes from VEXAS patients versus patients with ANCA-associated vasculitis (AAV), familial Mediterranean fever (FMF), and healthy donors (HD) to define a specific cytological pattern that can support VEXAS diagnosis. Twelve VEXAS patients were included in the study. Blood samples from FMF (n = 16), AAV (n = 16) and HDs (n = 20) acted as controls. May-Grünwald Giemsa (MGG) staining was used for studying cellular morphology, including cytoplasm, granules, and vacuoles and to perform a cytogenic evaluation of leucocytes. Plasma IL-1b, IL-1a, TNFa, IL-18 and IL-8 were measured using ELISA assay. The cytological analysis from blood smears confirmed the presence of immature neutrophils in VEXAS patients. We found a greater number of vacuoles in VEXAS patients vs. FMF, AAV and HD. Micronuclei (MNi) and cell death rate were higher in VEXAS patients vs. HD. Cell death correlated with IL-1b and IL-8 levels. MNi were positively associated with IL-8 and IL-1b levels, and with the percentage of immature neutrophils and vacuoles. In conclusion, our findings suggested that cytological test may be supportive for VEXAS diagnosis, despite genetical analysis is mandatory for confirming the disease. Finally, we identified several cytological hallmarks that may distinguish the VEXAS “cytotype” not only from HD but also from other inflammatory diseases. [ABSTRACT FROM AUTHOR]

Published
2024
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8. Proteomic Profiling of Tears in Blau Syndrome Patients in Identification of Potential Disease Biomarkers.

Author

Galozzi, Paola, Bindoli, Sara, Baggio, Chiara, Battisti, Ilaria, Leonardi, Andrea, Basso, Daniela, Arrigoni, Giorgio, and Sfriso, Paolo

Subjects
*PROTEIN binding, *PROTEIN expression, *BIOMARKERS, *AUTOINFLAMMATORY diseases, *MASS spectrometry
Abstract

Blau syndrome (BS) is a rare autoinflammatory granulomatosis characterized by granulomatous arthritis, uveitis, and dermatitis. Ocular complications are particularly severe in BS, significantly contributing to morbidity. This study aims to identify potential biomarkers for BS ocular degeneration through proteomic profiling of tear samples from affected patients. Seven subjects from the same family, including four carriers of the BS-associated NOD2 mutation (p.E383K), were recruited alongside healthy controls. Tear samples were collected using Schirmer strips and analyzed via mass spectrometry. A total of 387 proteins were identified, with significant differences in protein expression between BS patients, healthy familial subjects, and healthy controls. Key findings include the overexpression of alpha-2-macroglobulin (A2M) and immunoglobulin heavy constant gamma 4 (IGHG4) in BS patients. Bioinformatic analysis revealed that differentially expressed proteins are involved in acute-phase response, extracellular exosome formation, and protein binding. Notably, neutrophils' azurophilic granule components, as azurocidin (AZU1), myeloperoxidases (MPO), and defensins (DEFA3), were highly expressed in the most severely affected subject, suggesting a potential role of neutrophils in BS ocular severity. These proteins might be promising biomarkers for ocular involvement in BS, facilitating early detection and tailored treatment strategies. [ABSTRACT FROM AUTHOR]

Published
2024
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9. Fertility issues in women of childbearing age with spondyloarthritis.

Author

Bindoli, Sara, Cozzi, Giacomo, Lorenzin, Mariagrazia, Sfriso, Paolo, Doria, Andrea, Scagnellato, Laura, and Ramonda, Roberta

Subjects
CHILDBEARING age, FERTILITY, SPONDYLOARTHROPATHIES, OVARIAN reserve, HUMAN fertility, INFERTILITY
Abstract

The topic of fertility in women with spondyloarthritis (SpA) has been scarcely investigated to date. Recent systematic reviews and registry studies have brought renewed attention to the plight of women of childbearing age with rheumatic diseases, in particular SpA. Fertility may be impacted by physical impairment, hormonal imbalances and psychological distress. Several studies observed a reduction in anti-Müllerian hormone in women with SpA, reflecting a reduced ovarian reserve (OR). Furthermore, disease activity and the use of certain therapies can alter fertility, and this is reflected in a prolonged time-topregnancy (TTP), a validated outcome measure that can evaluate the status of subfertility. The employment of glucocorticoids or non-steroidal antiinflammatory drugs has also been linked to reduced fertility, whereas the use of biologics, especially tumour necrosis factor inhibitors (TNFi), is not associated with a prolonged TTP. In all women of childbearing age with rheumatic diseases, preconception counselling is paramount, and a referral to a reproductive specialist should be considered in the presence of multiple factors that may influence fertility. A comprehensive evaluation involving a multidisciplinary team of rheumatologists, gynaecologists, and often psychologists is warranted. In this narrative review, we collected the currently available literature focusing on fertility issues in women affected by SpA, providing data on fertility outcomes, hormonal imbalance, and therapeutic concerns. [ABSTRACT FROM AUTHOR]

Published
2024
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10. Correction: Clinical and laboratory features associated with macrophage activation syndrome in Still’s disease: data from the international AIDA Network Still’s Disease Registry

Author

Triggianese, Paola, primary, Vitale, Antonio, additional, Lopalco, Giuseppe, additional, Mayrink Giardini, Henrique Ayres, additional, Ciccia, Francesco, additional, Al-Maghlouth, Ibrahim, additional, Ruscitti, Piero, additional, Sfikakis, Petros Paul, additional, Iannone, Florenzo, additional, de Brito Antonelli, Isabele Parente, additional, Patrone, Martina, additional, Asfina, Kazi Nur, additional, Di Cola, Ilenia, additional, Laskari, Katerina, additional, Gaggiano, Carla, additional, Tufan, Abdurrahman, additional, Sfriso, Paolo, additional, Dagna, Lorenzo, additional, Giacomelli, Roberto, additional, Hinojosa-Azaola, Andrea, additional, Ragab, Gaafar, additional, Fotis, Lampros, additional, Direskeneli, Haner, additional, Spedicato, Veronica, additional, Dagostin, Marilia Ambiel, additional, Iacono, Daniela, additional, Ali, Hebatallah Hamed, additional, Cipriani, Paola, additional, Sota, Jurgen, additional, Kardas, Riza Can, additional, Bindoli, Sara, additional, Campochiaro, Corrado, additional, Navarini, Luca, additional, Gentileschi, Stefano, additional, Martín-Nares, Eduardo, additional, Torres-Ruiz, Jiram, additional, Saad, Moustafa Ali, additional, Kourtesi, Katerina, additional, Alibaz-Oner, Fatma, additional, Sevik, Gizem, additional, Iagnocco, Annamaria, additional, Makowska, Joanna, additional, Govoni, Marcello, additional, Monti, Sara, additional, Maggio, Maria Cristina, additional, La Torre, Francesco, additional, Del Giudice, Emanuela, additional, Hernández-Rodríguez, José, additional, Bartoloni, Elena, additional, Emmi, Giacomo, additional, Chimenti, Maria Sole, additional, Maier, Armin, additional, Simonini, Gabriele, additional, Conti, Giovanni, additional, Olivieri, Alma Nunzia, additional, Tarsia, Maria, additional, De Paulis, Amato, additional, Lo Gullo, Alberto, additional, Więsik-Szewczyk, Ewa, additional, Viapiana, Ombretta, additional, Ogunjimi, Benson, additional, Tharwat, Samar, additional, Erten, Sukran, additional, Nuzzolese, Rossana, additional, Karamanakos, Anastasios, additional, Frassi, Micol, additional, Conforti, Alessandro, additional, Caggiano, Valeria, additional, Marino, Achille, additional, Sebastiani, Gian Domenico, additional, Gidaro, Antonio, additional, Tombetti, Enrico, additional, Carubbi, Francesco, additional, Rubegni, Giovanni, additional, Cartocci, Alessandra, additional, Balistreri, Alberto, additional, Fabiani, Claudia, additional, Frediani, Bruno, additional, and Cantarini, Luca, additional

Published
2023
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11. Efficacy of canakinumab in patients with Still’s disease across different lines of biologic therapy: real-life data from the International AIDA Network Registry for Still’s Disease

Author

Vitale, Antonio, primary, Caggiano, Valeria, additional, Sfikakis, Petros P., additional, Dagna, Lorenzo, additional, Lopalco, Giuseppe, additional, Ragab, Gaafar, additional, La Torre, Francesco, additional, Almaghlouth, Ibrahim A., additional, Maggio, Maria Cristina, additional, Sota, Jurgen, additional, Tufan, Abdurrahman, additional, Hinojosa-Azaola, Andrea, additional, Iannone, Florenzo, additional, Loconte, Roberta, additional, Laskari, Katerina, additional, Direskeneli, Haner, additional, Ruscitti, Piero, additional, Morrone, Maria, additional, Mayrink Giardini, Henrique A., additional, Panagiotopoulos, Alexandros, additional, Di Cola, Ilenia, additional, Martín-Nares, Eduardo, additional, Monti, Sara, additional, De Stefano, Ludovico, additional, Kardas, Rıza Can, additional, Duran, Rahime, additional, Campochiaro, Corrado, additional, Tomelleri, Alessandro, additional, Alabdulkareem, Abdulaziz Mohammed, additional, Gaggiano, Carla, additional, Tarsia, Maria, additional, Bartoloni, Elena, additional, Romeo, Mery, additional, Hussein, Mohamed A., additional, Laymouna, Ahmed Hatem, additional, Parente de Brito Antonelli, Isabele, additional, Dagostin, Marilia Ambiel, additional, Fotis, Lampros, additional, Bindoli, Sara, additional, Navarini, Luca, additional, Alibaz-Oner, Fatma, additional, Sevik, Gizem, additional, Frassi, Micol, additional, Ciccia, Francesco, additional, Iacono, Daniela, additional, Crisafulli, Francesca, additional, Portincasa, Piero, additional, Jaber, Nour, additional, Kawakami-Campos, Perla Ayumi, additional, Wiesik-Szewczyk, Ewa, additional, Iagnocco, Annamaria, additional, Simonini, Gabriele, additional, Sfriso, Paolo, additional, Balistreri, Alberto, additional, Giacomelli, Roberto, additional, Conti, Giovanni, additional, Frediani, Bruno, additional, Fabiani, Claudia, additional, and Cantarini, Luca, additional

Published
2023
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19. Progress in Biological Therapies for Adult-Onset Still’s Disease

Author

Galozzi,Paola, Bindoli,Sara, Doria,Andrea, and Sfriso,Paolo

Subjects
Targets and Therapy [Biologics]
Abstract

Paola Galozzi, Sara Bindoli, Andrea Doria, Paolo Sfriso Rheumatology Unit, Department of Medicine DIMED, University of Padova, Padova, ItalyCorrespondence: Paola Galozzi, Rheumatology Unit, Department of Medicine DIMED, University of Padova, via Giustiniani, 2, Padova, 35128, Italy, Tel +39 049 821 8654, Email paola.galozzi@unipd.itAbstract: Adult-onset Still’s disease (AOSD) is a rare multifactorial autoinflammatory disorder of unknown etiology, characterized by an excessive release of cytokines triggered by dysregulated inflammation and articular and systemic manifestations. The clinical spectrum of AOSD ranges from self-limiting forms with mild symptoms to life-threatening cases and presents clinical and biological similarities with the juvenile form (sJIA). Nowadays, the advances in biologic agents no longer limit the treatment to NSAIDs, glucocorticoids, or conventional synthetic DMARDs. The blockade of IL-1 and IL-6 is effective in the treatment of systemic and articular inflammation of AOSD patients; however, novel compounds with different properties and targets are now available and others are being studied. In this review, starting from the pathogenesis of AOSD, we summarized the current and emerging biological therapies, possible effective agents for achieving AOSD control and remission.Keywords: biologics, AOSD, IL-1 inhibitors, IL-6 inhibitors, small molecules, new treatment

Published
2022

22. New onset and flare of rheumatic diseases following COVID-19 vaccination are mild and respond well to treatment: 9-month follow-up data from a single centre cohort

Author

Gasparotto, Michela, primary, Bindoli, Sara, additional, Padoan, Roberto, additional, Cozzi, Giacomo, additional, Depascale, Roberto, additional, Zanatta, Elisabetta, additional, Giollo, Alessandro, additional, Gatto, Mariele, additional, Zen, Margherita, additional, Schiavon, Franco, additional, Ramonda, Roberta, additional, Sfriso, Paolo, additional, Doria, Andrea, additional, and Iaccarino, Luca, additional

Published
2021
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24. EVALUATION OF SERUM LEVELS OF ASC FOR THE DIAGNOSIS AND MONITORING OF CRYOPYRIN ASSOCIATED PERIODIC SYNDROMES (CAPS)

Author

Carbone, Fortunata, Micillo, Teresa, Cantarini, Luca, Alessio, Maria, Olivieri, Alma Nunzia, Gicchino, Maria Francesca, Insalaco, Antonella, Maggio, Maria Cristina, Lucherini, Orso Maria, Scarpioni, Roberto, Piga, Matteo, Angioni, Maria Maddalena, Obici, Laura, Simpatico, Antonella, Leccese, Pietro, Consolini, Rita, Manna, Raffaele, Sfriso, Paolo, Bindoli, Sara, Galozzi, Paola, Orlando, Ida, Chiesa, Sabrina, Gattorno, Marco, Matarese, Giuseppe, Carbone, Fortunata, Micillo, Teresa, Cantarini, Luca, Alessio, Maria, Olivieri, Alma Nunzia, Gicchino, Maria Francesca, Insalaco, Antonella, Maggio, Maria Cristina, Lucherini, Orso Maria, Scarpioni, Roberto, Piga, Matteo, Angioni, Maria Maddalena, Obici, Laura, Simpatico, Antonella, Leccese, Pietro, Consolini, Rita, Manna, Raffaele, Sfriso, Paolo, Bindoli, Sara, Galozzi, Paola, Orlando, Ida, Chiesa, Sabrina, Gattorno, Marco, and Matarese, Giuseppe

Subjects
Settore MED/38 - Pediatria Generale E Specialistica, CAPS, ASC, IL-1 beta, IL-18
Abstract

Background: Dominantly gain-of-function mutations in the NLRP3 gene lead to Cryopyrin associated periodic syndromes (CAPS) characterized by constitutive activation of the inflammasome, increased secretion of interleukin (IL)-1beta and IL-18, and systemic inflammation. IL-1beta and active caspase-1 subunits are released in the serum together with the oligomeric particles of the adaptor ASC (apoptosis-associated Speck-like protein with a caspase-recruitment domain) after activation of the inflammosome complex and, as a consequence, patients with CAPS show an increased serum concentration of ASC+ particles. Objectives: Patients suffering from CAPS are characterized by clinical manifestation similar to other autoinflammatory diseases. This phenomenon together with the lack of specific laboratory tests makes difficult the diagnosis of CAPS. In this context the development of a test for the evaluation of serum ASC levels could provide novel biomarkers facilitating early disease diagnosis and able to monitor treatment responses. Methods: We analysed, with a novel ELISA assay, the levels of ASC particles in serum and plasma of normal subjects, CAPS patients and patients with autoimmune disorders (Multiple Sclerosis (MS), Type 1 Diabetes (T1D) and juvenile idiopathic arthritis), to confirm that ASC presence in the serum is not due to other chronic inflammatory processes characterizing autoimmunity. To evaluate the specificity of this biomarker in CAPS patients and not in individuals suffering from others inflammatory disorders, we also analysed sera from TNF receptor–associated periodic syndrome (TRAPS) patients. Results: ASC particles were higher in untreated CAPS patients with respect to healthy controls and patients suffering from MS and T1D. This tendency was also evident in patients with arthritis and TRAPS even if the difference was not statistically significant due to the small number of samples. In addition after pharmacological treatment there is a tendency to be confirmed through a reduction of ASC levels in CAPS patients. Conclusion: These data suggest that ELISA quantitation of ASC protein could represent a novel and additional strategy for the diagnosis and monitoring of CAPS.

Published
2019

33. AB1305 EVALUATION OF SERUM LEVELS OF ASC FOR THE DIAGNOSIS AND MONITORING OF CRYOPYRIN ASSOCIATED PERIODIC SYNDROMES (CAPS)

Author

Carbone, Fortunata, primary, Micillo, Teresa, additional, Cantarini, Luca, additional, Alessio, Maria, additional, Olivieri, Alma Nunzia, additional, Gicchino, Maria Francesca, additional, Insalaco, Antonella, additional, Maggio, Maria Cristina, additional, Lucherini, Orso Maria, additional, Scarpioni, Roberto, additional, Piga, Matteo, additional, Angioni, Maria Maddalena, additional, Obici, Laura, additional, Simpatico, Antonella, additional, Leccese, Pietro, additional, Consolini, Rita, additional, Manna, Raffaele, additional, Sfriso, Paolo, additional, Bindoli, Sara, additional, Galozzi, Paola, additional, Orlando, Ida, additional, Chiesa, Sabrina, additional, Gattorno, Marco, additional, and Matarese, Giuseppe, additional

Published
2019
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37. Response to interleukin-1 inhibitors in 140 Italian patients with adult-onset still's disease: A multicentre retrospective observational study

Author

Colafrancesco, Serena, Priori, Roberta, Valesini, Guido, Argolini, Lorenza, Baldissera, Elena, Bartoloni, Elena, Cammelli, Daniele, Canestrari, Giovanni Battista, Cantarini, Luca, Cavallaro, Elena, Cavalli, Giulio, Cerrito, Lucia, Cipriani, Paola, Dagna, Lorenzo, De Marchi, Ginevra, De Vita, Salvatore, Emmi, Giacomo, Ferraccioli, Gianfranco, Frassi, Micol, Galeazzi, Mauro, Gerli, Roberto, Giacomelli, Roberto, Gremese, Elisa, Iannone, Florenzo, Lapadula, Giovanni, Lopalco, Giuseppe, Manna, Raffaele, Mathieu, Alessandro, Montecucco, Carlomaurizio, Mosca, Marta, Piazza, Ilaria, Piga, Matteo, Pontikaki, Irene, Romano, Micol, Rossi, Silvia, Rossini, Maurizio, Ruscitti, Piero, Silvestri, Elena, Stagnaro, Chiara, Talarico, Rosaria, Tincani, Angela, Viapiana, Ombretta, Vitiello, Gianfranco, Fabris, Francesca, Bindoli, Sara, Punzi, Leonardo, Galozzi, Paola, Sfriso, Paolo, Canestrari, Giovanni, Ferraccioli, Gianfranco (ORCID:0000-0001-6246-2428), Gremese, Elisa (ORCID:0000-0002-2248-1058), Manna, Raffaele (ORCID:0000-0003-1560-3907), Colafrancesco, Serena, Priori, Roberta, Valesini, Guido, Argolini, Lorenza, Baldissera, Elena, Bartoloni, Elena, Cammelli, Daniele, Canestrari, Giovanni Battista, Cantarini, Luca, Cavallaro, Elena, Cavalli, Giulio, Cerrito, Lucia, Cipriani, Paola, Dagna, Lorenzo, De Marchi, Ginevra, De Vita, Salvatore, Emmi, Giacomo, Ferraccioli, Gianfranco, Frassi, Micol, Galeazzi, Mauro, Gerli, Roberto, Giacomelli, Roberto, Gremese, Elisa, Iannone, Florenzo, Lapadula, Giovanni, Lopalco, Giuseppe, Manna, Raffaele, Mathieu, Alessandro, Montecucco, Carlomaurizio, Mosca, Marta, Piazza, Ilaria, Piga, Matteo, Pontikaki, Irene, Romano, Micol, Rossi, Silvia, Rossini, Maurizio, Ruscitti, Piero, Silvestri, Elena, Stagnaro, Chiara, Talarico, Rosaria, Tincani, Angela, Viapiana, Ombretta, Vitiello, Gianfranco, Fabris, Francesca, Bindoli, Sara, Punzi, Leonardo, Galozzi, Paola, Sfriso, Paolo, Canestrari, Giovanni, Ferraccioli, Gianfranco (ORCID:0000-0001-6246-2428), Gremese, Elisa (ORCID:0000-0002-2248-1058), and Manna, Raffaele (ORCID:0000-0003-1560-3907)

Abstract

Background: Interleukin (IL)-1 plays a crucial role in the pathogenesis of Adult onset Still's disease (AOSD). Objectives: To evaluate the efficacy and safety of anakinra (ANA) and canakinumab (CAN) in a large group of AOSD patients. Methods: Data on clinical, serological features, and concomitant treatments were retrospectively collected at baseline and after 3, 6, and 12 months from AOSD patients (Yamaguchi criteria) referred by 18 Italian centers. Pouchot's score was used to evaluate disease severity. Results: One hundred forty patients were treated with ANA; 4 were subsequently switched to CAN after ANA failure. The systemic pattern of AOSD was identified in 104 (74.2%) of the ANA-treated and in 3 (75%) of the CAN-treated groups; the chronic-articular type of AOSD was identified in 48 (25.8%) of the ANA-treated and in 1 (25%) of the CAN-treated groups. Methotrexate (MTX) was the most frequent disease modifying anti-rheumatic drug (DMARD) used before beginning ANA or CAN [91/140 (75.8%), 2/4 (50%), respectively]. As a second-line biologic DMARD therapy in 29/140 (20.7%) of the patients, ANA was found effective in improving all clinical and serological manifestations (p < 0.0001), and Pouchot's score was found to be significantly reduced at all time points (p < 0.0001). No differences in treatment response were identified in the ANA-group when the patients were stratified according to age, sex, disease pattern or mono/combination therapy profile. ANA primary and secondary inefficacy at the 12-month time point was 15/140 (10.7%) and 11/140 (7.8%), respectively. Adverse events (AEs) [mainly represented by in situ (28/47, 59.5%) or diffuse (12/47, 25.5%) skin reactions and infections (7/47, 14.8%)] were the main causes for discontinuation. Pouchot's score and clinical and serological features were significantly ameliorated at all time points (p < 0.0001) in the CAN-group, and no AEs were registered during CAN therapy. Treatment was suspended for loss of effi

Published
2017

38. Response to Interleukin-1 Inhibitors in 140 Italian Patients with Adult-Onset Still’s Disease: A Multicentre Retrospective Observational Study

Author

Colafrancesco, Serena, primary, Priori, Roberta, additional, Valesini, Guido, additional, Argolini, Lorenza, additional, Baldissera, Elena, additional, Bartoloni, Elena, additional, Cammelli, Daniele, additional, Canestrari, Giovanni, additional, Cantarini, Luca, additional, Cavallaro, Elena, additional, Cavalli, Giulio, additional, Cerrito, Lucia, additional, Cipriani, Paola, additional, Dagna, Lorenzo, additional, Marchi, Ginevra De, additional, Vita, Salvatore De, additional, Emmi, Giacomo, additional, Ferraccioli, Gianfranco, additional, Frassi, Micol, additional, Galeazzi, Mauro, additional, Gerli, Roberto, additional, Giacomelli, Roberto, additional, Gremese, Elisa, additional, Iannone, Florenzo, additional, Lapadula, Giovanni, additional, Lopalco, Giuseppe, additional, Manna, Raffaele, additional, Mathieu, Alessandro, additional, Montecucco, Carlomaurizio, additional, Mosca, Marta, additional, Piazza, Ilaria, additional, Piga, Matteo, additional, Pontikaki, Irene, additional, Romano, Micol, additional, Rossi, Silvia, additional, Rossini, Maurizio, additional, Ruscitti, Piero, additional, Silvestri, Elena, additional, Stagnaro, Chiara, additional, Talarico, Rosaria, additional, Tincani, Angela, additional, Viapiana, Ombretta, additional, Vitiello, Gianfranco, additional, Fabris, Francesca, additional, Bindoli, Sara, additional, Punzi, Leonardo, additional, Galozzi, Paola, additional, and Sfriso, Paolo, additional

Published
2017
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41. Response to Interleukin-1 Inhibitors in 140 Italian Patients with Adult-Onset Still's Disease: A Multicentre Retrospective Observational Study

Author

Serena Colafrancesco, Roberta Priori, Guido Valesini, Lorenza Argolini, Elena Baldissera, Elena Bartoloni, Daniele Cammelli, Giovanni Canestrari, Luca Cantarini, Elena Cavallaro, Giulio Cavalli, Lucia Cerrito, Paola Cipriani, Lorenzo Dagna, Ginevra De Marchi, Salvatore De Vita, Giacomo Emmi, Gianfranco Ferraccioli, Micol Frassi, Mauro Galeazzi, Roberto Gerli, Roberto Giacomelli, Elisa Gremese, Florenzo Iannone, Giovanni Lapadula, Giuseppe Lopalco, Raffaele Manna, Alessandro Mathieu, Carlomaurizio Montecucco, Marta Mosca, Ilaria Piazza, Matteo Piga, Irene Pontikaki, Micol Romano, Silvia Rossi, Maurizio Rossini, Piero Ruscitti, Elena Silvestri, Chiara Stagnaro, Rosaria Talarico, Angela Tincani, Ombretta Viapiana, Gianfranco Vitiello, Francesca Fabris, Sara Bindoli, Leonardo Punzi, Paola Galozzi, Paolo Sfriso, Colafrancesco, Serena, Priori, Roberta, Valesini, Guido, Argolini, Lorenza, Baldissera, Elena, Bartoloni, Elena, Cammelli, Daniele, Canestrari, Giovanni, Cantarini, Luca, Cavallaro, Elena, Cavalli, Giulio, Cerrito, Lucia, Cipriani, Paola, Dagna, Lorenzo, De Marchi, Ginevra, De Vita, Salvatore, Emmi, Giacomo, Ferraccioli, Gianfranco, Frassi, Micol, Galeazzi, Mauro, Gerli, Roberto, Giacomelli, Roberto, Gremese, Elisa, Iannone, Florenzo, Lapadula, Giovanni, Lopalco, Giuseppe, Manna, Raffaele, Mathieu, Alessandro, Montecucco, Carlomaurizio, Mosca, Marta, Piazza, Ilaria, Piga, Matteo, Pontikaki, Irene, Romano, Micol, Rossi, Silvia, Rossini, Maurizio, Ruscitti, Piero, Silvestri, Elena, Stagnaro, Chiara, Talarico, Rosaria, Tincani, Angela, Viapiana, Ombretta, Vitiello, Gianfranco, Fabris, Francesca, Bindoli, Sara, Punzi, Leonardo, Galozzi, Paola, and Sfriso, Paolo

Subjects
musculoskeletal diseases, 0301 basic medicine, medicine.medical_specialty, Combination therapy, Canakinumab, Interleukin (IL)-1, Adult-onset Still's disease, canakinumab, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Pharmacology (medical), Adverse effect, Original Research, Adult-onset Still’s disease, 030203 arthritis & rheumatology, Pharmacology, Anakinra, treatment, business.industry, Treatment, Settore MED/09 - MEDICINA INTERNA, lcsh:RM1-950, Retrospective cohort study, Surgery, Discontinuation, interleukin (IL)-1, anakinra, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, Concomitant, Methotrexate, business, medicine.drug
Abstract

Background: Interleukin (IL)-1 plays a crucial role in the pathogenesis of Adult onset Still’s disease (AOSD).Objectives: To evaluate the efficacy and safety of anakinra (ANA) and canakinumab (CAN) in a large group of AOSD patients.Methods: Data on clinical, serological features, and concomitant treatments were retrospectively collected at baseline and after 3, 6, and 12 months from AOSD patients (Yamaguchi criteria) referred by 18 Italian centers. Pouchot’s score was used to evaluate disease severity.Results: One hundred forty patients were treated with ANA; 4 were subsequently switched to CAN after ANA failure. The systemic pattern of AOSD was identified in 104 (74.2%) of the ANA-treated and in 3 (75%) of the CAN-treated groups; the chronic-articular type of AOSD was identified in 48 (25.8%) of the ANA-treated and in 1 (25%) of the CAN-treated groups. Methotrexate (MTX) was the most frequent disease modifying anti-rheumatic drug (DMARD) used before beginning ANA or CAN [91/140 (75.8%), 2/4 (50%), respectively]. As a second-line biologic DMARD therapy in 29/140 (20.7%) of the patients, ANA was found effective in improving all clinical and serological manifestations (p < 0.0001), and Pouchot’s score was found to be significantly reduced at all time points (p < 0.0001). No differences in treatment response were identified in the ANA-group when the patients were stratified according to age, sex, disease pattern or mono/combination therapy profile. ANA primary and secondary inefficacy at the 12-month time point was 15/140 (10.7%) and 11/140 (7.8%), respectively. Adverse events (AEs) [mainly represented by in situ (28/47, 59.5%) or diffuse (12/47, 25.5%) skin reactions and infections (7/47, 14.8%)] were the main causes for discontinuation. Pouchot’s score and clinical and serological features were significantly ameliorated at all time points (p < 0.0001) in the CAN-group, and no AEs were registered during CAN therapy. Treatment was suspended for loss of efficacy only in one case (1/4, 25%).Conclusion: This is the largest retrospective observational study evaluating the efficacy and safety of IL-1 inhibitors in AOSD patients. A good response was noted at 3 months after therapy onset in both the ANA- and CAN-groups. Skin reaction may nevertheless represent a non-negligible AE during ANA treatment.

Published
2017

42. Efficacy and safety of therapies for Still's disease and macrophage activation syndrome (MAS): a systematic review informing the EULAR/PReS guidelines for the management of Still's disease.

Author

Bindoli S, De Matteis A, Mitrovic S, Fautrel B, Carmona L, and De Benedetti F

Subjects
Humans, Antirheumatic Agents therapeutic use, Treatment Outcome, Still's Disease, Adult-Onset drug therapy, Practice Guidelines as Topic, Antibodies, Monoclonal, Humanized therapeutic use, Interleukin 1 Receptor Antagonist Protein therapeutic use, Antibodies, Monoclonal therapeutic use, Macrophage Activation Syndrome drug therapy
Abstract

Objectives: To analyse the efficacy and safety of treatments for Still's disease and macrophage activation syndrome (MAS)., Methods: Medline, Embase and Cochrane Library were searched for clinical trials (randomised, randomised controlled trial (RCT), controlled and clinical controlled trial (CCT)), observational studies (retrospective, longitudinal observational retrospective (LOR), prospective and longitudinal observational prospective (LOP)) and systematic reviews (SRs), in which the populations studied were patients with Still's disease and MAS. The intervention was any pharmacological treatment (approved or under evaluation) versus any comparator drug or placebo, and as outcomes, any relevant efficacy and safety event. The risk of bias (RoB) was assessed with the Cochrane RoB and AMSTAR-2 (Assessing the Methodological Quality of Systematic Reviews-2, version 2) for SRs., Results: 128 full texts were included: 25 RCTs, 1 CCT, 11 SRs published after 2013 and 91 LOP/LOR studies. In Still's disease, interleukin (IL)-1 inhibitors (IL-1i) and IL-6R inhibitors (IL-6i) were the most studied drugs. Two meta-analyses on RCTs showed an OR, to achieve an ARC50 response rate, of 6.02 (95% CI 2.24 to 21.36) and 8.08 (95% CI 1.89 to 34.57) for IL-1i and IL-6Ri, respectively. Retrospective studies showed that early initiation of IL-1i or IL-6i was associated with high rates of clinically inactive disease. In MAS, GCs were employed in all patients, often associated with ciclosporin and/or anakinra. Rates of complete response were reported, with a range from 53% to 100%. Emapalumab was the only drug tested in a CCT, with a complete response of 93%., Conclusion: IL-1i and IL-6Ri show the highest level of efficacy in the treatment of Still's disease. For MAS, IL-1 and interferon-γ inhibition appear to be effective on a background of high-dose glucocorticoids., Competing Interests: Competing interests: ADM has no conflict of interest. SB has not received fees or personal grants from any laboratory, but her working group received fees and/or grants from Novartis and SOBI. SM has no permanent financial links but has received consulting fees from BMS, Lilly, Pfizer and SOBI. FDB has received fees and/or unrestricted grants from Abbvie, Novimmune, Novartis, Roche, Sanofi-Aventis, Sobi, Regeneron, Elixiron and Zhydus. BF has received research grants from AbbVie, Lilly, MSD and Pfizer, and consultancy fees from AbbVie, Amgen, Biogen, BMS, Celltrion, Fresenius Kabi, Galapagos, Gilead, Janssen, Lilly, Medac, MSD, NORDIC Pharma, Novartis, Pfizer, Roche, Sandoz, Sanofi-Genzyme, SOBI, UCB and Viatris. LC has not received fees or personal grants from any laboratory, but her institute works by contract for laboratories among other institutions, such as Amgen, Fresenius Kabi España, Galapagos, Gilead, Pfizer, Lilly, Meda Pharma, MSD, Novartis, Roche, Sanofi Aventis, Upjohn, BMS, Novo Nordisk and Sandoz., (© European Alliance of Associations for Rheumatology, EULAR 2024. Re-use permitted under CC BY-NC-ND. No commercial re-use. No derivatives. See rights and permissions. Published by BMJ on behalf of EULAR.)

Published
2024
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43. Systemic juvenile idiopathic arthritis and adult-onset Still's disease are the same disease: evidence from systematic reviews and meta-analyses informing the 2023 EULAR/PReS recommendations for the diagnosis and management of Still's disease.

Author

De Matteis A, Bindoli S, De Benedetti F, Carmona L, Fautrel B, and Mitrovic S

Subjects
Humans, Adult, Practice Guidelines as Topic, Ferritins blood, Diagnosis, Differential, Interleukin-18 blood, Child, Still's Disease, Adult-Onset diagnosis, Arthritis, Juvenile diagnosis, Arthritis, Juvenile blood, Biomarkers blood, Macrophage Activation Syndrome diagnosis
Abstract

Objectives: To analyse the similarity in clinical manifestations and laboratory findings between systemic juvenile idiopathic arthritis (sJIA) and adult-onset Still's disease (AOSD)., Methods: Three systematic reviews (SR) were performed. One included cohort studies comparing sJIA versus AOSD that described clinical and biological manifestations with at least 20 patients in each group (SR1). The second identified studies of biomarkers in both diseases and their diagnostic performance (SR2). The last focused on diagnostic biomarkers for macrophage activation syndrome (MAS, SR3). Medline (PubMed), Embase and Cochrane Library were systematically searched. The risk of bias was assessed with an adapted form of the Hoy scale for prevalence studies in SR1 and the Quality Assessment of Diagnostic Accuracy Studies-2 in SR2 and SR3. We performed meta-analyses of proportions for the qualitative descriptors., Results: Eight studies were included in SR1 (n=1010 participants), 33 in SR2 and 10 in SR3. The pooled prevalence of clinical manifestations did not differ between sJIA and AOSD, except for myalgia, sore throat and weight loss, which were more frequent in AOSD than sJIA because they are likely ascertained incompletely in sJIA, especially in young children. Except for AA amyloidosis, more frequent in sJIA than AOSD, the prevalence of complications did not differ, nor did the prevalence of biological findings. Ferritin, S100 proteins and interleukin-18 (IL-18) were the most frequently used diagnostic biomarkers, with similar diagnostic performance. For MAS diagnosis, novel biomarkers such as IL-18, C-X-C motif ligand 9, adenosine deaminase 2 activity and activated T cells seemed promising., Conclusion: Our results argue for a continuum between sJIA and AOSD., Prospero Registration Number: CRD42022374240 and CRD42024534021., Competing Interests: Competing interests: ADM has no competing interests with this work. SB has not received fees or personal grants from any laboratory, but her working group received fees and/or grants from Novartis and Sobi. FDB has received fees and/or unrestricted grants from AbbVie, Novimmune, Novartis, Roche, Sanofi-Aventis, Sobi, Regeneron, Elixiron and Zydus. BF has received research grants from AbbVie, Lilly, MSD and Pfizer, and consultancy fees from AbbVie, Amgen, Biogen, BMS, Celltrion, Fresenius Kabi, Galapagos, Gilead, Janssen, Lilly, Medac, MSD, Nordic Pharma, Novartis, Pfizer, Roche, Sandoz, Sanofi-Genzyme, Sobi, UCB and Viatris. LC has not received fees or personal grants from any laboratory, but her institute works by contract for laboratories among other institutions, such as Amgen, Fresenius Kabi España, Galapagos, Gilead, Pfizer, Lilly, Meda Pharma, MSD, Novartis, Roche, Sanofi Aventis, Upjohn, BMS, Novo Nordisk and Sandoz. SM has no permanent financial links, but has received consulting fees from BMS, Lilly, Pfizer and SOBI., (© European Alliance of Associations for Rheumatology, EULAR 2024. Re-use permitted under CC BY-NC-ND. No commercial re-use. No derivatives. See rights and permissions. Published by BMJ on behalf of EULAR.)

Published
2024
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44. EULAR/PReS recommendations for the diagnosis and management of Still's disease, comprising systemic juvenile idiopathic arthritis and adult-onset Still's disease.

Author

Fautrel B, Mitrovic S, De Matteis A, Bindoli S, Antón J, Belot A, Bracaglia C, Constantin T, Dagna L, Di Bartolo A, Feist E, Foell D, Gattorno M, Georgin-Lavialle S, Giacomelli R, Grom AA, Jamilloux Y, Laskari K, Lazar C, Minoia F, Nigrovic PA, Oliveira Ramos F, Ozen S, Quartier P, Ruscitti P, Sag E, Savic S, Truchetet ME, Vastert SJ, Wilhelmer TC, Wouters C, Carmona L, and De Benedetti F

Subjects
Humans, Adult, Immunosuppressive Agents therapeutic use, Antirheumatic Agents therapeutic use, Cyclosporine therapeutic use, Child, Biomarkers, Still's Disease, Adult-Onset diagnosis, Still's Disease, Adult-Onset drug therapy, Still's Disease, Adult-Onset therapy, Arthritis, Juvenile diagnosis, Arthritis, Juvenile drug therapy, Arthritis, Juvenile therapy, Glucocorticoids therapeutic use, Macrophage Activation Syndrome diagnosis, Macrophage Activation Syndrome therapy, Macrophage Activation Syndrome drug therapy
Abstract

Systemic juvenile idiopathic arthritis (sJIA) and adult-onset Still's disease (AOSD) are considered the same disease, but a common approach for diagnosis and management is still missing., Methods: In May 2022, EULAR and PReS endorsed a proposal for a joint task force (TF) to develop recommendations for the diagnosis and management of sJIA and AOSD. The TF agreed during a first meeting to address four topics: similarity between sJIA and AOSD, diagnostic biomarkers, therapeutic targets and strategies and complications including macrophage activation syndrome (MAS). Systematic literature reviews were conducted accordingly., Results: The TF based their recommendations on four overarching principles, highlighting notably that sJIA and AOSD are one disease, to be designated by one name, Still's disease.Fourteen specific recommendations were issued. Two therapeutic targets were defined: clinically inactive disease (CID) and remission, that is, CID maintained for at least 6 months. The optimal therapeutic strategy relies on early use of interleukin (IL-1 or IL-6 inhibitors associated to short duration glucocorticoid (GC). MAS treatment should rely on high-dose GCs, IL-1 inhibitors, ciclosporin and interferon-γ inhibitors. A specific concern rose recently with cases of severe lung disease in children with Still's disease, for which T cell directed immunosuppressant are suggested. The recommendations emphasised the key role of expert centres for difficult-to-treat patients. All overarching principles and recommendations were agreed by over 80% of the TF experts with a high level of agreement., Conclusion: These recommendations are the first consensus for the diagnosis and management of children and adults with Still's disease., Competing Interests: Competing interests: BF: AbbVie, Amgen, Biogen, BMS, Celltrion, Fresenius Kabi, Galapagos, Gilead, Janssen, Lilly, Medac, MSD, Nordic Pharma, Novartis, Pfizer, Roche-Chugai, Sandoz, Sanofi-Genzyme, SOBI, UCB, Viatris; SM: BMS, Lilly, SOBI; JA: Sobi, Novartis, Roche, Pfizer, AbbVie, Lilly; AB: Boehringer Ingelheim, Novartis, AbbVie, Fresenius Kabi, GlaxoSmithKline; CB: SOBI; TC: AbbVie, Novartis, Roche; LD: AbbVie, Amgen, Astra-Zeneca, Boehringer-Ingelheim, BMS, Lilly, Galapagos, GlaxoSmithKline, Janssen, Kiniksa, Novartis, Pfizer, SOBI; ADB: Lenovo; EF: AbbVie, BMS, Galapagos, Lilly, Medac, Novartis, Sanofi, UCB, Pfizer, Roche, SOBI; DF: Boehringer-Ingelheim, SOBI, Novartis, Werfen Innova; MG, SGL, FM, FOR, SV: Novartis, SOBI; RG, AG: Novartis; IJ: Amgen, Lilly, Novartis, SOBI; PN: BMS, Brickell Bio, Cerecor, Exo Therapeutics, Miach Ortho, Novartis, Pfizer, SOBI, UpToDate, American Academy of Pediatrics; SO: Novartis, SOBI, Pfizer; PQ: Amgen, AbbVie, BMS, Roche-Chugai, Lilly, Novartis, Pfizer, Sanofi, SOBI, Health Events; PR: AbbVie, BMS, Janssen, Novartis, SOBI; SS: Novartis, SOBI, CSL Behring, Takeda, BioCryst, Biotest; M-ET: Boehringer-Ingelheim, Pfizer, Lilly, MSD, SOBI, Janssen, BMS, Fresenius Kabi, Galapagos, AbbVie; CW: Novartis, SOBI, UCB; LC: Meda Pharma, Angelini Pharma, Pfizer, SANOFI-AVENTIS, Fresenius Kabi, Galapagos; FDB: SOBI, Novartis, Apollo, Kiniksa, Sanofi, Roche, Elixiron, Regeneron; ADM, SB, KL, CL, ES, T-CW: none., (© European Alliance of Associations for Rheumatology, EULAR 2024. Re-use permitted under CC BY-NC-ND. No commercial re-use. No derivatives. See rights and permissions. Published by BMJ on behalf of EULAR.)

Published
2024
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46. Diagnostic capabilities, clinical features, and longitudinal UBA1 clonal dynamics of a nationwide VEXAS cohort.

Author

Gurnari C, Pascale MR, Vitale A, Diral E, Tomelleri A, Galossi E, Falconi G, Bruno A, Crisafulli F, Frassi M, Cattaneo C, Bertoli D, Bernardi M, Condorelli A, Morsia E, Poloni A, Crisà E, Caravelli D, Triggianese P, Brussino L, Battipaglia G, Bindoli S, Sfriso P, Caroni F, Dragani M, Mallegni F, Pilo F, Firinu D, Curti A, Papayannidis C, Olivieri A, Kordasti S, Albano F, Pane F, Musto P, Bocchia M, Lugli E, Breccia M, Frigeni M, Dagna L, Greco R, Franceschini F, Campochiaro C, Cantarini L, and Voso MT

Subjects
Humans, Male, Aged, Mutation, Hematopoietic Stem Cell Transplantation, Myelodysplastic Syndromes diagnosis, Myelodysplastic Syndromes genetics, Myelodysplastic Syndromes therapy, Leukemia, Arthritis, Rheumatoid, Skin Diseases, Genetic
Abstract

VEXAS is a prototypic hemato-inflammatory disease combining rheumatologic and hematologic disorders in a molecularly defined nosological entity. In this nationwide study, we aimed at screenshotting the current diagnostic capabilities and clinical-genomic features of VEXAS, and tracked UBA1 longitudinal clonal dynamics upon different therapeutics, including allogeneic hematopoietic cell transplant. We leveraged a collaboration between the Italian Society of Experimental Hematology and of Rheumatology and disseminated a national survey to collect clinical and molecular patient information. Overall, 13/29 centers performed UBA1 genomic testing locally, including Sanger sequencing (46%), next-generation sequencing (23%), droplet digital polymerase chain reaction (8%), or combination (23%). A total of 41 male patients were identified, majority (51%) with threonine substitutions at Met41 hotspot, followed by valine and leucine (27% and 8%). Median age at VEXAS diagnosis was 67 years. All patients displayed anemia (median hemoglobin 9.1 g/dL), with macrocytosis. Bone marrow vacuoles were observed in most cases (89%). The most common rheumatologic association was polychondritis (49%). A concomitant myelodysplastic neoplasm/syndrome (MDS) was diagnosed in 71% of patients (n = 28), chiefly exhibiting lower Revised International Prognostic Scoring System risk profiles. Karyotype was normal in all patients, except three MDS cases showing -Y, t(12;16)(q13;q24), and +8. The most frequently mutated gene was DNMT3A (n = 10), followed by TET2 (n = 3). At last follow-up, five patients died and two patients progressed to acute leukemia. Longitudinal UBA1 clonal dynamics demonstrated mutational clearance following transplant. We collected a nationwide interdisciplinary VEXAS patient cohort, characterized by heterogeneous rheumatologic manifestations and treatments used. MDS was diagnosed in 71% of cases. Patients exhibited various longitudinal UBA1 clonal dynamics., (© 2023 Wiley Periodicals LLC.)

Published
2024
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47. New onset and flare of rheumatic diseases following COVID-19 vaccination are mild and respond well to treatment: 9-month follow-up data from a single centre cohort.

Author

Gasparotto M, Bindoli S, Padoan R, Cozzi G, Depascale R, Zanatta E, Giollo A, Gatto M, Zen M, Schiavon F, Ramonda R, Sfriso P, Doria A, and Iaccarino L

Subjects
Adult, Humans, BNT162 Vaccine, Follow-Up Studies, Vaccination adverse effects, Arthritis, Rheumatoid, COVID-19 prevention & control, COVID-19 Vaccines adverse effects, Rheumatic Diseases drug therapy
Abstract

Objectives: Anti-COVID-19 vaccines have proved to be effective and well tolerated. Great attention is now being paid to the characterisation of possible adverse events associated to their administration. We report a case series of suspected rheumatic diseases (RDs) following anti-COVID-19 vaccination., Methods: We included patients evaluated at first-aid rheumatologic consultancy and at rheumatologic outpatient and inpatient clinic at Padova University Hospital between May and September 2021 presenting with a RD within 30 days after an anti-COVID-19 vaccine dose. Our selection was in accordance with the World Health Organisation guidelines for adverse event following immunisation (AEFI) surveillance. Patients were regularly re-evaluated by telemedicine or face-to-face visit., Results: We identified 30 cases of RD following vaccination: 24 (80.0%) new onsets and 6 (20.0%) flares. Most of patients (76.6%) received the BNT162b2 vaccine. The mean time to RD onset/flare was 12±9 days. The most common manifestations were inflammatory arthritis (40.0%), rheumatic polymyalgia (33.3%) and adult-onset Still's disease (13.3%). At the last FU visit (9.6±2.2 months), 83.3% of patients showed complete response to first- or second-line therapy, 13.3% a partial response and one patient (3.3%) was still experiencing an active disease., Conclusions: Considering the amount of vaccine doses administered during the evaluation period we overall detected a limited number of cases. We noted a clear prevalence of autoinflammatory conditions and seronegative manifestations. The great majority of patients had mild features and showed a good response to therapy.

Published
2023
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48. Progress in Biological Therapies for Adult-Onset Still's Disease.

Author

Galozzi P, Bindoli S, Doria A, and Sfriso P

Abstract

Adult-onset Still's disease (AOSD) is a rare multifactorial autoinflammatory disorder of unknown etiology, characterized by an excessive release of cytokines triggered by dysregulated inflammation and articular and systemic manifestations. The clinical spectrum of AOSD ranges from self-limiting forms with mild symptoms to life-threatening cases and presents clinical and biological similarities with the juvenile form (sJIA). Nowadays, the advances in biologic agents no longer limit the treatment to NSAIDs, glucocorticoids, or conventional synthetic DMARDs. The blockade of IL-1 and IL-6 is effective in the treatment of systemic and articular inflammation of AOSD patients; however, novel compounds with different properties and targets are now available and others are being studied. In this review, starting from the pathogenesis of AOSD, we summarized the current and emerging biological therapies, possible effective agents for achieving AOSD control and remission., Competing Interests: The authors report no conflicts of interest in this work., (© 2022 Galozzi et al.)

Published
2022
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49. 18 F-Fluorodeoxyglucose Positron Emission Tomography and Computed Tomography With Magnetic Resonance for Diagnosing Adult-Onset Still's Disease.

Author

Bindoli S, Galozzi P, Magnani F, Rubin L, Campi C, Doria A, Cecchin D, and Sfriso P

Abstract

Objective: The objective of the study was to assess the advantages of 18 F-fluorodeoxyglucose (FDG) positron emission tomography and computed tomography with magnetic resonance (PET/CT-MR) in diagnosing and monitoring patients with adult-onset Still's disease (AOSD). Methods: Participants in this retrospective case-control study underwent whole-body 18 F-FDG-PET/CT-MR imaging. All PET scans were qualitatively and semiquantitatively analyzed using standardized uptake values (SUVs) normalized to liver uptake, i.e., we calculated the ratio (SUVr) between the minimum, maximum, and mean SUVs for different organs and tissues and the mean SUV for the liver. Disease activity scores were assessed using Pouchot's criteria. Results: Eighteen patients diagnosed with AOSD and 24 controls (non-AOSD patients diagnosed with solid tumors, excluding lymphomas) were considered. A total of 38 PET/MR and nine PET/CT scans were analyzed. AOSD patients had higher SUVr than controls. All SUVr differed significantly between the patient and control group for bone marrow, and for the spleen, the only difference lacking statistical significance concerned the ratio of the minimum SUV for spleen to the mean SUV for liver. Though limited in number, AOSD responders to therapy showed lower uptakes during the period monitored. No correlations were found between Pouchot's scores and SUVr. Conclusion: Our data revealed higher spleen and bone marrow 18 F-FDG uptakes on PET/CT and PET/MR images in AOSD patients than in controls. Together with clinical examinations and laboratory data, PET/CT and PET/MR seemed more reliable than Pouchot's score in assessing disease activity., (Copyright © 2020 Bindoli, Galozzi, Magnani, Rubin, Campi, Doria, Cecchin and Sfriso.)

Published
2020
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