Your search keyword '"Carbogno, Simone"' showing total 4 results

1. RISK SCORE OF MACROPHAGE ACTIVATION SYNDROME IN PATIENTS WITH SYSTEMIC JUVENILE IDIOPATHIC ARTHRITIS

Author

Carbogno, Simone Marafon, Denise Pires Marucci, Giulia and Pardeo, Manuela Insalaco, Antonella Messia, Virginia Sacco, Emanuela Demir, Ferhat Sozeri, Betul Gagro, Alenka and Kifer, Nastasia Jelusic, Marija Minoia, Francesca Kostik, Mikhail Vougiouka, Olga De Benedetti, Fabrizio Bracaglia, Claudia MAS sJIA PReS Working Party

Published

2019

2. THU0527 RISK SCORE OF MACROPHAGE ACTIVATION SYNDROME IN PATIENTS WITH SYSTEMIC JUVENILE IDIOPATHIC ARTHRITIS

Author

Carbogno, Simone, Pires Marafon, Denise, Marucci, Giulia, Pardeo, Manuela, Insalaco, Antonella, Messia, Virginia, Sacco, Emanuela, Demir, Ferhat, Sözeri, Betül, Gagro, Alenka, Kifer, Nastasia, Jelusic, Marija, Minoia, Francesca, Kostik, Mikhail, Vougiouka, Olga, De Benedetti, Fabrizio, Bracaglia, Claudia, and MAS/sJIA PReS working party

Subjects

musculoskeletal diseases, medicine.medical_specialty, education.field_of_study, Framingham Risk Score, business.industry, Significant difference, Population, fungi, Arthritis, medicine.disease, Rheumatology, body regions, Internal medicine, Macrophage activation syndrome, sJIA, MAS, score, validation, Medicine, In patient, lipids (amino acids, peptides, and proteins), business, Complication, education, hormones, hormone substitutes, and hormone antagonists

Abstract

Background: Macrophage Activation Syndrome (MAS) is a severe, life-threatening, complication of rheumatic diseases in childhood, particularly of systemic Juvenile Idiopathic Arthritis (sJIA), occurring in approximately 25% of the patients with sJIA. A score that identifies sJIA patients who are at high risk to develop MAS would be useful in clinical practice. Objectives: To evaluate whether routine laboratory parameters at disease onset may predict the development of MAS in patients with active sJIA. To define a risk score of MAS for sJIA patients using these parameters. Methods: Laboratory parameters of disease activity and severity (WBC, N, PLT, Hb, ferritin, AST, ALT, gGT, LDH, TGL, fibrinogen, D-dimer and CRP), were retrospectively evaluated in 86 sJIA patients referred to our Division of Rheumatology from 1998 to 2017 with at least one year of follow-up. Laboratory parameters were evaluated during active sJIA, without MAS, at time of hospitalization (T1) and before treatment for sJIA was started (T2). Patients were divided in two groups: group 1 (patients without history of MAS), group 2 (patients with at least one MAS episode during disease course). To calculate a MAS risk score, laboratory parameters, collected at T2, with a statistical significant difference between the two groups of patients were selected. Results: Thirty-three patients, who fulfilled the 2016 classification criteria for MAS [1] at time of sampling, were excluded from the analysis. Therefore, we analysed laboratory parameters of 53 patients with sJIA, 33 of whom without history of MAS (group 1) and 20 who developed at least one episode of MAS during disease course (group 2). Levels of ferritin, AST, LDH, gGT and TGL, collected at T2, were statistically significant higher in patients with a history of MAS compared to those without a history of MAS. For each of these parameters an arbitrary cut-off was defined. In order to define the final score an arbitrary rate was attributed to each parameter. Sensitivity (Se), specificity (Sp), positive predictive value (PPV) and negative predictive value (NPV) were calculated to define the best scoring system. The scoring system with the best sensitivity was chosen (Table 1). A MAS risk score >3 identified 19 out of 20 sJIA patients with a history of MAS and 4 out of 33 sJIA patients without history of MAS. In order to validate the MAS risk score on a different population, we applied it on 53 patients from other paediatric Rheumatologic centres. Thirty-seven of these patients without history of MAS while 16 with at least one episode of MAS. Sensitivity and specificity were 0.750 and 0.784 respectively. Conclusion: In conclusion we developed a MAS risk score based on routine laboratory parameters that are available worldwide, that can help clinicians to identify patients at higher risk to develop MAS. A validation on a larger population is necessary. References: [1] Ravelli A et al. Ann Rheum Dis. 2016 Mar;75(3):481-9. Disclosure of Interests: Simone Carbogno: None declared, Denise Pires Marafon: None declared, Giulia Marucci: None declared, Manuela Pardeo: None declared, Antonella Insalaco: None declared, Virginia Messia: None declared, Emanuela Sacco: None declared, Ferhat Demir: None declared, Betul Sozeri: None declared, Alenka Gagro: None declared, Nastasia Kifer: None declared, Marija Jelusic: None declared, Francesca Minoia: None declared, Mikhail Kostik: None declared, Olga Vougiouka: None declared, Fabrizio De Benedetti Grant/research support from: Abbvie, SOBI, Novimmune, Roche, Novartis, Sanofi, Pfizer, Claudia Bracaglia: None declared

Published

2019

3. Kawasaki facile e difficile: Dieci messaggi attraverso i casi degli specializzandi italiani

Author

Benelli, Elisa, Carbogno, Simone, Carucci, Nicolina Stefania, Gori, Martina, Marrani, Edoardo, Melis, Marta, Pellegrin, MARIA CHIARA, Benelli, Elisa, Carbogno, Simone, Carucci, Nicolina Stefania, Gori, Martina, Marrani, Edoardo, Melis, Marta, and Pellegrin, MARIA CHIARA

Subjects

Retropharyngeal absce, Retropharyngeal abscess, Kawasaki disease, Acetylsalicylic acid, Pediatrics, Perinatology and Child Health, Corticosteroids, Corticosteroid, Febrile cholestatic jaundice, Hemophagocytic syndrome, Perinatology and Child Health, Pediatrics

Abstract

La malattia di Kawasaki (MK) è una vasculite sistemica che di norma colpisce bambini di 2-5 anni: la diagnosi ed il trattamento sono in genere facili, come descritto nel primo caso. Tuttavia, nonostante un'ageguata terapia, il 10-15% dei pazienti sviluppa aneurismi dell'arteria coronarica. I pazienti ad alto rischio sono quelli sotto l'anno di età o con forme incomplete o atipiche. Per questo motivo la tempestività della diagnosi risulta fondamentale per iniziare una terapia adeguata. Questo articolo descrive alcuni casi di forme atipiche di MK: un ascesso retrofaringeo, un ittero colestatico febbrile e una sindrome da attivazione macrofagica. Tuttavia, l'articolo riporta alcuni casi severi di MK come uno shock emodinamico, il caso di un paziente che ha ricevuto una terapia anti-TNF a causa dell'inefficacia della terapia standard ed infine il caso di un adulto che ha subito un intervento di bypass aorto-coronarico dovuto alle conseguenze di un aneurisma gigante sviluppato all'età di 2 anni dopo la MK. Alla fine dell'articolo, i messaggi trasmessi dai casi descritti sono riassunti in 10 punti.

Published

2017

4. Risk Score of Macrophage Activation Syndrome in Patients with Systemic Juvenile Idiopathic Arthritis

Author

Carbogno, Simone, Marafon, Denise Pires, Marucci, Giulia, Pardeo, Manuela, Insalaco, Antonella, Messia, Virginia, Sacco, Emanuela, Demir, Ferhat, Sozeri, Betul, Cekada, Natasia, Marija Jelusic, Vougiouka, Olga, Kostik, Mikhail, Gagro, Alenka, Kessel, Christoph, Minoia, Francesca, Benedetti, Fabrizio, and Bracaglia, Claudia

Subjects

body regions, musculoskeletal diseases, Risk Score, Macrophage Activation Syndrome, Systemic Juvenile Idiopathic Arthritis, fungi, lipids (amino acids, peptides, and proteins), hormones, hormone substitutes, and hormone antagonists

Abstract

Background/Purpose : Macrophage Activation Syndrome (MAS) is a severe, life- threatening, complication of rheumatic diseases in childhood, particularly of systemic Juvenile Idiopathic Arthritis (sJIA), occurring in approximately 25% of the patients with sJIA. The mortality rate of MAS is still signifi cantly high. A score that identify sJIA patients who are at high risk to develop MAS would be useful in clinical practice. There are no parameters available to identify from onset sJIA patients with high risk to develop MAS in their disease course. Methods : We evaluated whether routine laboratory parameters at disease onset may predict the development of MAS in patients with active sJIA and we defi ned a risk score of MAS for sJIA patients using these parameters. Laboratory parameters of disease activity and severity (WBC, N, PLT, Hb, ferritin, AST, ALT, gGT, LDH, TGL, fi brinogen, D- dimer and CRP), were retrospectively evaluated in 85 sJIA patients referred to our Division of Rheumatology from 1998 to 2018 with at least one year of follow- up. Laboratory parameters were evaluated during active sJIA, without MAS, at time of hospitalization (T1) and immediately before treatment for sJIA was started (T2). Patients were divided in two groups: group 1 (sJIA patients without history of MAS), group 2 (sJIA patients with at least one MAS episode during disease course). To calculate a MAS risk score, laboratory parameters, collected at T2, with a statistically signifi cant difference between the two groups of patients were selected. Results : Thirty- two patients, that fulfi lled the 2016 classifi cation criteria for MAS [1] at time of sampling, were excluded from the analysis. Therefore, we analysed laboratory parameters of 53 patients with sJIA, 33 of whom without history of MAS (group 1) and 20 who developed at least one episode of MAS during disease course (group 2). Levels of ferritin, AST, LDH, gGT and TGL, collected at T2, were statistically signifi cant higher in patients with a history of MAS compared to those without a history of MAS. For each of these parameters an arbitrary cut- off was defi ned. In order to define the final score an arbitrary rate was attributed to each parameter (Table1). Sensitivity (Se), specifi city (Sp), positive predictive value (PPV) and negative predictive value (NPV) were calculated to defi ne the best scoring system. The scoring system with the best sensitivity was chosen (Table 2). A MAS risk score >3 identifi ed 19 out of 20 sJIA patients with a history of MAS and 5 out of 33 sJIA patients without history of MAS. In order to validate the MAS risk score on a different population, we applied the score on 47 patients from other Paediatric Rheumatologic centres, 29 without history of MAS and 18 with at least one episode of MAS. Sensitivity and specifi city of the score are reported in table 3. Conclusion : In conclusion we developed a MAS risk score based on routine laboratory parameters, available worldwide, that can help clinicians to identify these patients early in the disease course. The initial validation analysis is promising but we need to validate the score on a larger population.