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2. POS1264 PULMONARY PROGRESSIVE FIBROSIS IN RHEUMATOID ARTHRITIS AND PRIMARY SJOGREN SYNDROME: SIMILARITIES AND DIFFERENCES

Author

Manfredi, A., primary, Rai, A., additional, Venerito, V., additional, Cazzato, M., additional, Sambataro, G., additional, Gentileschi, S., additional, Canofari, C., additional, Atzeni, F., additional, Cerri, S., additional, Andrisani, D., additional, Vacchi, C., additional, Cassone, G., additional, and Cozzini, F., additional

Published
2024
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3. Rheumatoid arthritis extra-articular lung disease: new insights on pathogenesis and experimental drugs

Author

Sebastiani, M, Manfredi, A, Croci, S, Faverio, P, Cassone, G, Vacchi, C, Salvarani, C, Luppi, F, Sebastiani, Marco, Manfredi, Andreina, Croci, Stefania, Faverio, Paola, Cassone, Giulia, Vacchi, Caterina, Salvarani, Carlo, Luppi, Fabrizio, Sebastiani, M, Manfredi, A, Croci, S, Faverio, P, Cassone, G, Vacchi, C, Salvarani, C, Luppi, F, Sebastiani, Marco, Manfredi, Andreina, Croci, Stefania, Faverio, Paola, Cassone, Giulia, Vacchi, Caterina, Salvarani, Carlo, and Luppi, Fabrizio

Abstract

Introduction: Pulmonary involvement is one of the most common extra-articular manifestations of rheumatoid arthritis (RA), a systemic inflammatory disease characterized by joint swelling and tenderness. All lung compartments can be interested in the course of RA, including parenchyma, airways, and, more rarely, pleura and vasculature. Areas covered: The aim of this paper is to review the main RA lung manifestations, focusing on pathogenesis, clinical and therapeutic issues of RA-related interstitial lung disease (ILD). Despite an increasing number of studies in the last years, pathogenesis of RA-ILD remains largely debated and the treatment of RA patients with lung involvement is still challenging in these patients. Expert opinion: Management of RA-ILD is largely based on expert-opinion. Due to the broad clinical manifestations, including both joints and pulmonary involvement, multidisciplinary discussion, including rheumatologist and pulmonologist, is essential, not only for diagnosis, but also to evaluate the best therapeutic approach and follow-up. In fact, the coexistence of different lung manifestations may influence the treatment response and safety. The identification of biomarkers and risk-factors for an early identification of RA patients at risk of developing ILD remains a need that still needs to be fulfilled, and that will require further investigation in the next years.

Published
2024

6. Pneumopathie interstitielle fibrosante dans le syndrome de Gougerot-Sjögren primitif

Author

Manfredi, A, Vacchi, C, Della Casa, G, Cerri, S, Cassone, G, Di Cecco, G, Luppi, F, Salvarani, C, Sebastiani, M, Manfredi A., Vacchi C., Della Casa G., Cerri S., Cassone G., Di Cecco G., Luppi F., Salvarani C., Sebastiani M., Manfredi, A, Vacchi, C, Della Casa, G, Cerri, S, Cassone, G, Di Cecco, G, Luppi, F, Salvarani, C, Sebastiani, M, Manfredi A., Vacchi C., Della Casa G., Cerri S., Cassone G., Di Cecco G., Luppi F., Salvarani C., and Sebastiani M.

Abstract

Objectifs: La pneumopathie interstitielle (PI) représente la principale atteinte pulmonaire dans le syndrome de Gougerot-Sjögren primitif (SGSp). Un certain nombre de patients atteints de SGSp développent une forme fibrosante progressive de PI, mais il n'existe aucune donnée sur la prévalence de telles présentations.L'objectif de cette étude transversale monocentrique était d'explorer la prévalence des formes fibrosantes chez les patients atteints de SGSp présentant une PI. Méthodes: Tous les patients consécutifs remplissant les critères de classification du SGSp et présentant une PI existante ou nouvellement diagnostiquée ont été inclus dans l’étude. Le diagnostic de PI était toujours établi par TDM-HR et les différentes formes ont été déterminées sur la base des critères de classification en vigueur et réparties dans deux groupes selon qu'une forme fibrosante était détectée ou non. Résultats: Trente-quatre patients présentant un SGSp avec PI ont été inclus dans l’étude (3 hommes et 31 femmes, âge médian 69,5 ans, durée moyenne du SGSp 47,5 mois). Une forme fibrosante a été identifiée chez 52,9 % des patients (groupe 1) : pneumopathie interstitielle commune (PIC) chez 13 patients (38,2 %), pneumopathie interstitielle non spécifique (PINS) fibrosante chez 4 patients (11,8 %) et pneumopathie organisée (PO) fibrosante chez 1 patient (2,9 %). Le groupe 2 (16 patients, 47,1 %) comprenait la PINS chez 6 patients (17,6 %), la PO chez 4 patients (11,8 %), la PIL chez 2 patients (5,9 %) et la pneumopathie interstitielle inclassable chez 4 patients (11,8 %). Dans le groupe 1, les patients étaient plus jeunes et la durée du SGSp au moment du diagnostic de PI plus courte. Notamment, la PI a été diagnostiquée avant ou en même temps que le SGSp dans 83,3 % des cas, contre 62,5 % dans le groupe 2 de forme non fibrosante (p < 0,05). Conclusion: Nos données suggèrent une forte prévalence de ce phénotype clinique pulmonaire che

Published
2022

7. A 2D imager for X-ray FELs with a 65 nm CMOS readout based on per-pixel signal compression and 10 bit A/D conversion

Author

Ratti, L., Comotti, D., Fabris, L., Grassi, M., Lodola, L., Malcovati, P., Manghisoni, M., Re, V., Traversi, G., Vacchi, C., Rizzo, G., Batignani, G., Bettarini, S., Casarosa, G., Forti, F., Giorgi, M., Morsani, F., Paladino, A., Paoloni, E., Pancheri, L., Dalla Betta, G.-F., Mendicino, R., Verzellesi, G., Xu, H., and Benkechkache, M.A.

Published
2016
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9. In-pixel conversion with a 10 bit SAR ADC for next generation X-ray FELs

Author

Lodola, L., Batignani, G., Benkechkache, M.A., Bettarini, S., Casarosa, G., Comotti, D., Dalla Betta, G.F., Fabris, L., Forti, F., Grassi, M., Latreche, S., Malcovati, P., Manghisoni, M., Mendicino, R., Morsani, F., Paladino, A., Pancheri, L., Paoloni, E., Ratti, L., Re, V., Rizzo, G., Traversi, G., Vacchi, C., Verzellesi, G., and Xu, H.

Published
2016
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10. Online Dark Count Rate Measurements in 150 nm CMOS SPADs Exposed to Low Neutron Fluxes

Author

Ratti, L., Brogi, P., Collazuol, G., Betta, G. -F. Dalla, Delgado, J. C., Marrocchesi, P. S., MInga, J., Morsani, F., Pancheri, Lucio, Pino, F., Selva, A., Stolzi, F., Torilla, G., and Vacchi, C.

Abstract

Arrays of single photon avalanche diodes (SPADs) fabricated in a 150 nm CMOS technology have been exposed to neutrons up to fluences of about $4.3 \times 10^{10}~1$ MeV neutron equivalent cm $^{-2}$ , with fluxes around $3 \times 10^{6}~1$ MeV neutron equivalent cm $^{-2}\text{s}^{-1}$ . Dark count rate (DCR) was monitored during irradiation and for some time, from 5 to 23 min, depending on the irradiation step, at the end of the irradiation interval to investigate the dynamics of defect formation and short-term annealing. Measurements were performed both on single- and on dual-layer devices, where SPAD arrays are face to face bonded and read out in coincidence. A range of different DCR behaviors were detected after single neutron interaction with the device substrate, including in particular partial performance recovery following a logarithmic relaxation process, but also damped oscillation phenomena, sudden step-shaped changes, and the emergence of RTS-like fluctuations, pointing to different defect reordering dynamics.

Published
2024
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13. Usefulness of digital velcro crackles detection in identification of interstitial lung disease in patients with connective tissue diseases

Author

Manfredi, A, Cassone, G, Vacchi, C, Pancaldi, F, Casa, G, Cerri, S, De Pasquale, L, Luppi, F, Salvarani, C, Sebastiani, M, Manfredi A., Cassone G., Vacchi C., Pancaldi F., Casa G. D., Cerri S., De Pasquale L., Luppi F., Salvarani C., Sebastiani M., Manfredi, A, Cassone, G, Vacchi, C, Pancaldi, F, Casa, G, Cerri, S, De Pasquale, L, Luppi, F, Salvarani, C, Sebastiani, M, Manfredi A., Cassone G., Vacchi C., Pancaldi F., Casa G. D., Cerri S., De Pasquale L., Luppi F., Salvarani C., and Sebastiani M.

Abstract

Objectives: This study aims to evaluate the diagnostic accuracy of the VECTOR software in patients with connective tissue diseases (CTDs), compared with the reference standard of high-resolution computed tomography (HRCT). Patients and methods: The study included 98 consecutive patients of CTD (24 males, 74 females; median age: 66 years; range, 24 to 85 years) with a recent HRCT. Patients were evaluated in a blindly manner by VECTOR and the results obtained by the algorithm were compared with the presence of interstitial lung disease (ILD) according to HRCT. Results: Interstitial lung disease was detected in 42.8% of subjects. VECTOR correctly classified 81/98 patients, with a diagnostic accuracy of 82.6%; sensitivity and specificity were 88.1% and 78.6%, respectively. Only 5/42 patients with ILD were not correctly classified by VECTOR, while false positive cases were 21.4%. No significant differences were observed according to the radiologic pattern of ILD. Conclusion: VECTOR showed high sensitivity, specificity and diagnostic accuracy, allowing selecting patients to be investigated with HRCT. The relatively high frequency rate of false positive results is acceptable if compared with the lack of effective screening methods for this complication of CTDs.

Published
2021

14. Interstitial pneumonia with autoimmune features: A single center prospective follow-up study

Author

Sebastiani, M, Cassone, G, De Pasquale, L, Cerri, S, Della Casa, G, Vacchi, C, Luppi, F, Salvarani, C, Manfredi, A, Sebastiani M., Cassone G., De Pasquale L., Cerri S., Della Casa G., Vacchi C., Luppi F., Salvarani C., Manfredi A., Sebastiani, M, Cassone, G, De Pasquale, L, Cerri, S, Della Casa, G, Vacchi, C, Luppi, F, Salvarani, C, Manfredi, A, Sebastiani M., Cassone G., De Pasquale L., Cerri S., Della Casa G., Vacchi C., Luppi F., Salvarani C., and Manfredi A.

Abstract

Background and objective: Recently the term “interstitial pneumonia with autoimmune features” (IPAF) has been proposed to identify patients with interstitial lung disease and autoimmune characteristics, not fulfilling the criteria for specific connective tissue diseases (CTD). Only few data are available about the clinical and serological features of IPAF patients, their survival and the possible evolution in a CTD. The aims of the study were to investigate the demographic and clinico-serologic features of patients with IPAF, their relationship to survival, and the possible evolution in a definite CTD. Patients and methods: Fifty-two patients were consecutively enrolled and prospectively followed for 45 ± 31.6 months. Data about disease onset, serological, clinical and therapeutic features, pulmonary function tests and high-resolution computed tomography were periodically repeated. The survival of patients with IPAF was compared with that of 104 patients with idiopathic pulmonary fibrosis (IPF). Results: The clinical domain for IPAF was satisfied in 44 patients, serological domain in 49 and the morphological domain in 29 patients. During the follow-up, a definite CTD was diagnosed in 7 patients, in particular Sjogren's syndrome in 4 patients, rheumatoid arthritis in 2, and polymyositis in the last. The estimated 5-year survival of IPAF patients 69.5 ± 7.8%, significantly higher than survival observed in IPF patients, and the baseline value of FVC and DLCO were the only factors associated to death. Conclusions: IPAF seems to a distinct entity, with a low tendency to evolve in a definite CTD. Nevertheless, further studies are needed to better define the clinical evolution and the outcome of IPAF.

Published
2020

15. Erratum: Acute exacerbation of interstitial lung diseases secondary to systemic rheumatic diseases: A prospective study and review of the literature (Journal of Thoracic Disease (2019) 11 (1621-1628) DOI: 10.21037/jtd.2019.03.28)

Author

Manfredi A., Manfredi, A, Sebastiani, M, Cerri, S, Vacchi, C, Tonelli, R, Della Casa, G, Cassone, G, Spinella, A, Pancaldi, F, Luppi, F, Salvarani, C, Manfredi A., Sebastiani M., Cerri S., Vacchi C., Tonelli R., Della Casa G., Cassone G., Spinella A., Pancaldi F., Luppi F., Salvarani C., Manfredi A., Manfredi, A, Sebastiani, M, Cerri, S, Vacchi, C, Tonelli, R, Della Casa, G, Cassone, G, Spinella, A, Pancaldi, F, Luppi, F, Salvarani, C, Manfredi A., Sebastiani M., Cerri S., Vacchi C., Tonelli R., Della Casa G., Cassone G., Spinella A., Pancaldi F., Luppi F., and Salvarani C.

Abstract

In the article that appeared on Page 1621-1628, Vol 11, No 4 (April 2019) Issue of the Journal of Thoracic Disease (1), the given and family names of author “Fabrizio Pancaldi” was incorrectly published in the original. The author's name should be corrected as Fabrizio Pancaldi, instead of Pancaldi Fabrizio. The authors regret the error.

Published
2020

16. Estimated 10-year cardiovascular risk in a large Italian cohort of rheumatoid arthritis patients: Data from the Cardiovascular Obesity and Rheumatic DISease (CORDIS) Study Group

Author

Cacciapaglia, F., Spinelli, F. R., Piga, M., Erre, G. L., Sakellariou, G., Manfredi, A., Viapiana, O., Fornaro, M., Colella, S., Floris, A., Mangoni, A. A., Castagna, F., Vacchi, Caterina, Orsolini, G., Bugatti, S., Cafaro, G., Cauli, A., Gremese, Elisa, Atzeni, F., Bartoloni, E., Vacchi C., Gremese E. (ORCID:0000-0002-2248-1058), Cacciapaglia, F., Spinelli, F. R., Piga, M., Erre, G. L., Sakellariou, G., Manfredi, A., Viapiana, O., Fornaro, M., Colella, S., Floris, A., Mangoni, A. A., Castagna, F., Vacchi, Caterina, Orsolini, G., Bugatti, S., Cafaro, G., Cauli, A., Gremese, Elisa, Atzeni, F., Bartoloni, E., Vacchi C., and Gremese E. (ORCID:0000-0002-2248-1058)

Abstract

Background: Several cardiovascular (CV) risk algorithms are available to predict CV events in the general population. However, their performance in patients with rheumatoid arthritis (RA) might differ from the general population. This cross-sectional multicentre study aimed to estimate the 10-year CV risk using two different algorithms in a large RA cohort and in patients with osteoarthritis (OA). Methods: In a consecutive series of RA patients and matched OA controls without prior CV events, clinical and serologic data and traditional CV risk factors were recorded. The 10-year CV risk was assessed with the Systematic COronary Risk Evaluation (SCORE) and the “Progetto Cuore” algorithms. Results: 1,467 RA patients and 342 OA subjects were included. RA patients were more frequently diabetic (9.9% vs 6.4%; p=0.04) and smokers (20.4% vs 12.5%; p=0.002) but had lower prevalence of obesity (15% vs 21%; p=0.003). Dyslipidaemia was more prevalent in OA (32.5% vs 21.7%; p<0.0001). The 10-year estimated CV risk was 1.6% (95%CI 1.3-1.9) in RA and 1.4% (95%CI 1.3-1.6) in OA (p=0.002) according to SCORE and 6.5% (95%CI 6.1-6.9) in RA and 4.4% (95%CI 3.9-5.1) in OA (p<0.001) according to “Progetto Cuore”. Regardless of the score used, RA patients had a 3- to-4-fold increased 10-year risk of CV events compared to OA subjects. Conclusion: RA patients have a significantly higher 10-year risk of CV events than OA subjects. In addition to effective disease control and joint damage prevention, specific protective measures targeting modifiable traditional CV risk factors should be implemented in RA.

Published
2022

17. POS0919 MOLECULAR AND BIOLOGICAL PATHWAYS OF BREAST CANCER IN PATIENTS WITH SYSTEMIC SCLEROSIS: IMMUNOHISTOCHEMICAL INVESTIGATIONS FROM THE SCLERO-BREAST STUDY

Author

Spinella, A., primary, Toss, A., additional, Isca, C., additional, De Pinto, M., additional, Vacchi, C., additional, Magnani, L., additional, Lumetti, F., additional, Macripo’, P., additional, Ficarra, G., additional, Fabbiani, L., additional, Iannone, A., additional, Gasparini, E., additional, Piana, S., additional, Cortesi, L., additional, De Santis, G., additional, Maiorana, A., additional, Dominici, M., additional, Salvarani, C., additional, and Giuggioli, D., additional

Published
2022
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18. POS1214 COVID-19 VACCINATION RATE AND SAFETY PROFILE IN PATIENTS AFFECTED BY MIXED CRYOGLOBULINEMIC VASCULITIS.

Author

Vacchi, C., primary, Testoni, S., additional, Visentini, M., additional, Zani, R., additional, Lauletta, G., additional, Gragnani, L., additional, Filippini, D. A., additional, Mazzaro, C., additional, Fraticelli, P., additional, Quartuccio, L., additional, Padoan, R., additional, Castelnovo, L., additional, Zignego, A. L., additional, Ferri, C., additional, Hoxha, A., additional, Salvarani, C., additional, Monti, G., additional, Galli, M., additional, and Sebastiani, M., additional

Published
2022
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20. Italian consensus recommendations for the management of hepatitis C infection in patients with rheumatoid arthritis

Author

Sebastiani, M, Milazzo, L, Atzeni, F, Vacchi, C, Manfredi, A, Quartuccio, L, Scire, C, Gaeta, G, Lapadula, G, Armignacco, O, Tavio, M, D'Angelo, S, Meroni, P, Bazzichi, L, Grassi, W, Mathieu, A, Mastroianni, C, Sagnelli, E, Santantonio, T, Foppa, C, Puoti, M, Sarmati, L, Airo, P, Epis, O, Scrivo, R, Gargiulo, M, Riva, A, Ciancio, G, Zehender, G, Taliani, G, Meroni, L, Sollima, S, Sarzi-Puttini, P, Galli, M, Sebastiani M., Milazzo L., Atzeni F., Vacchi C., Manfredi A., Quartuccio L., Scire C., Gaeta G. B., Lapadula G., Armignacco O., Tavio M., D'Angelo S., Meroni P., Bazzichi L., Grassi W., Mathieu A., Mastroianni C., Sagnelli E., Santantonio T., Foppa C. U., Puoti M., Sarmati L., Airo P., Epis O. M., Scrivo R., Gargiulo M., Riva A., Ciancio G., Zehender G., Taliani G., Meroni L., Sollima S., Sarzi-Puttini P., Galli M., Sebastiani, M, Milazzo, L, Atzeni, F, Vacchi, C, Manfredi, A, Quartuccio, L, Scire, C, Gaeta, G, Lapadula, G, Armignacco, O, Tavio, M, D'Angelo, S, Meroni, P, Bazzichi, L, Grassi, W, Mathieu, A, Mastroianni, C, Sagnelli, E, Santantonio, T, Foppa, C, Puoti, M, Sarmati, L, Airo, P, Epis, O, Scrivo, R, Gargiulo, M, Riva, A, Ciancio, G, Zehender, G, Taliani, G, Meroni, L, Sollima, S, Sarzi-Puttini, P, Galli, M, Sebastiani M., Milazzo L., Atzeni F., Vacchi C., Manfredi A., Quartuccio L., Scire C., Gaeta G. B., Lapadula G., Armignacco O., Tavio M., D'Angelo S., Meroni P., Bazzichi L., Grassi W., Mathieu A., Mastroianni C., Sagnelli E., Santantonio T., Foppa C. U., Puoti M., Sarmati L., Airo P., Epis O. M., Scrivo R., Gargiulo M., Riva A., Ciancio G., Zehender G., Taliani G., Meroni L., Sollima S., Sarzi-Puttini P., and Galli M.

Abstract

Objectives: The recent introduction of direct-acting antiviral agents (DAAs) which can eliminate Hepatitis C virus (HCV) had revolutionized the treatment of HCV infections also in a complex clinical setting such as the patients with rheumatoid arthritis (RA). HCV elimination is also opportune due to the availability of more efficient immunosuppressive drugs, whose effect on the course of HCV infection is largely unknown. Methods: Consensus process was endorsed by the Italian Society of Rheumatology (SIR) and the Italian Society of Infectious and Tropical Diseases (SIMIT) to review the available evidence and produce practical, hospital-wide recommendations. The consensus panel consisted of 18 infectious diseases consultants, 20 rheumatologists and one clinical epidemiologist, who used the criteria of the Oxford Centre for Evidence-based Medicine to assess the quality of the evidence and the strength of their recommendations. Results: A core-set of statements about management of patients with RA and infection by HCV have been developed to help clinicians in their clinical practice. Conclusions: A screening for HCV should be performed in all RA patients and it is mandatory before starting an immunosuppressive therapy. Finally, a DAA treatment should be considered in all HCV-infected patients.Significance and Innovations HCV antibodies should be investigated at the time of diagnosis of RA and, in any case, before starting immunosuppressive therapy with disease-modifying antirheumatic drugs (DMARDs). HCV eradication with DAA should be attempted as soon as possible, depending on patient conditions allowing a continuous oral treatment lasting 8–12 weeks Conventional and biological DMARDs are allowed in patients with HCV infection, but they should be used cautiously in presence of advanced liver disease.

Published
2019

23. Interstitial Pneumonia with Autoimmune Features: Why Rheumatologist-Pulmonologist Collaboration Is Essential

Author

Sebastiani, M, Faverio, P, Manfredi, A, Cassone, G, Vacchi, C, Stainer, A, Pozzi, M, Salvarani, C, Pesci, A, Luppi, F, Sebastiani, Marco, Faverio, Paola, Manfredi, Andreina, Cassone, Giulia, Vacchi, Caterina, Stainer, Anna, Pozzi, Maria Rosa, Salvarani, Carlo, Pesci, Alberto, Luppi, Fabrizio, Sebastiani, M, Faverio, P, Manfredi, A, Cassone, G, Vacchi, C, Stainer, A, Pozzi, M, Salvarani, C, Pesci, A, Luppi, F, Sebastiani, Marco, Faverio, Paola, Manfredi, Andreina, Cassone, Giulia, Vacchi, Caterina, Stainer, Anna, Pozzi, Maria Rosa, Salvarani, Carlo, Pesci, Alberto, and Luppi, Fabrizio

Abstract

In 2015 the European Respiratory Society (ERS) and the American Thoracic Society (ATS) “Task Force on Undifferentiated Forms of Connective Tissue Disease-associated Interstitial Lung Disease” proposed classification criteria for a new research category defined as “Interstitial Pneumonia with Autoimmune Features” (IPAF), to uniformly define patients with interstitial lung disease (ILD) and features of autoimmunity, without a definite connective tissue disease. These classification criteria were based on a variable combination of features obtained from three domains: a clinical domain consisting of extra-thoracic features, a serologic domain with specific autoantibodies, and a morphologic domain with imaging patterns, histopathological findings, or multicompartment involvement. Features suggesting a systemic vasculitis were excluded. Since publication of ERS/ATS IPAF research criteria, various retrospective studies have been published focusing on prevalence; clinical, morphological, and serological features; and prognosis of these patients showing a broad heterogeneity in the results. Recently, two prospective, cohort studies were performed, confirming the existence of some peculiarities for this clinical entity and the possible progression of IPAF to a defined connective tissue disease (CTD) in about 15% of cases. Moreover, a non-specific interstitial pneumonia pattern, an anti-nuclear antibody positivity, and a Raynaud phenomenon were the most common findings. In comparison with idiopathic pulmonary fibrosis (IPF), IPAF patients showed a better performance in pulmonary function tests and less necessity of oxygen delivery. However, at this stage of our knowledge, we believe that further prospective studies, possibly derived from multicenter cohorts and through randomized control trials, to further validate the proposed classification criteria are needed.

Published
2021

24. Fibrosing interstitial lung disease in primary Sjogren syndrome

Author

Manfredi, A, Vacchi, C, Casa, G, Cerri, S, Cassone, G, Cecco, G, Luppi, F, Salvarani, C, Sebastiani, M, Manfredi, Andreina, Vacchi, Caterina, Casa, Giovanni Della, Cerri, Stefania, Cassone, Giulia, Cecco, Giovanna Di, Luppi, Fabrizio, Salvarani, Carlo, Sebastiani, Marco, Manfredi, A, Vacchi, C, Casa, G, Cerri, S, Cassone, G, Cecco, G, Luppi, F, Salvarani, C, Sebastiani, M, Manfredi, Andreina, Vacchi, Caterina, Casa, Giovanni Della, Cerri, Stefania, Cassone, Giulia, Cecco, Giovanna Di, Luppi, Fabrizio, Salvarani, Carlo, and Sebastiani, Marco

Abstract

Objectives: Interstitial lung disease (ILD) represents the main pulmonary involvement in primary Sjogren syndrome (pSS). A proportion of patients with pSS develop a progressive fibrosing form of ILD, but no data are available about the prevalence of these patterns in pSS patients. Aim of this monocentric, cross-sectional study was to investigate the prevalence of fibrosing patterns in pSS patients with ILD. Methods: All consecutive patients fulfilling classification criteria for pSS with a new or previous diagnosis of ILD were enrolled in the study. Diagnosis of ILD was always performed by mean of HRCT and specific patterns were identified according to current classification criteria and divided in two groups according to the detection of a fibrotic pattern. Results: Thirty-four pSS-ILD patients were enrolled in the study (males/females 3/31, median age 69.5 years, median pSS duration 47.5 months). Fibrotic pattern was detected in 52.9% of patients, namely: UIP (13 patients, 38.2%), fibrotic NSIP (4, 11.8%), fibrotic OP (1 2.9%) and group 2 (16 pts, 47.1%) including NSIP (6, 17.6%), OP (4, 11.8%), LIP (2, 5.9%) and unclassifiable (4, 11.8%). These patients were younger and with a shorter pSS duration at ILD diagnosis, in particular ILD diagnosis was prior or concurrent to pSS in 83.3% of cases compared to 62.5% in the group of nonfibrotic pattern (P < 0.05). Conclusion: Our data suggest a high prevalence of this pulmonary clinical phenotype in pSS-ILD patients. Since the course of progressive fibrosing pneumonia generally results in respiratory failure, this result could be worthy of further studies.

Published
2021

25. Correction

Author

Sebastiani, M, Milazzo, L, Atzeni, F, Vacchi, C, Manfredi, A, Quartuccio, L, Scire, C, Gaeta, GB, Lapadula, G, Armignacco, O, Tavio, M, D'Angelo, S, Meroni, P, Bazzichi, L, Grassi, W, Mathieu, A, Mastroianni, C, Sagnelli, E, Santantonio, T, Uberti Foppa, C, Puoti, M, Sarmati, L, Airo, P, Epis, OM, Scrivo, R, Gargiulo, M, Riva, A, Ciancio, G, Zehender, G, Taliani, G, Meroni, L, Sollima, S, Sarzi-Puttini, P, Galli, M, Sebastiani, M, Milazzo, L, Atzeni, F, Vacchi, C, Manfredi, A, Quartuccio, L, Scire, C, Gaeta, Gb, Lapadula, G, Armignacco, O, Tavio, M, D'Angelo, S, Meroni, P, Bazzichi, L, Grassi, W, Mathieu, A, Mastroianni, C, Sagnelli, E, Santantonio, T, Uberti Foppa, C, Puoti, M, Sarmati, L, Airo, P, Epis, Om, Scrivo, R, Gargiulo, M, Riva, A, Ciancio, G, Zehender, G, Taliani, G, Meroni, L, Sollima, S, Sarzi-Puttini, P, and Galli, M

Published
2019

26. POS0214 ASSOCIATION BETWEEN C-REACTIVE PROTEIN AND 10-YEAR RISK OF CARDIOVASCULAR DISEASE IN RHEUMATOID ARTHRITIS USING THE ERS-RA SCORE: A CROSS-SECTIONAL ANALYSIS OF THE CORDIS COHORT

Author

Erre, G. L., primary, Cacciapaglia, F., additional, Sakellariou, G., additional, Manfredi, A., additional, Bartoloni Bocci, E., additional, Viapiana, O., additional, Fornaro, M., additional, Dessì, M., additional, Mangoni, A. A., additional, Palermo, B. L., additional, Gremese, E., additional, Cafaro, G., additional, Nucera, V., additional, Vacchi, C., additional, Spinelli, F. R., additional, Atzeni, F., additional, and Piga, M., additional

Published
2021
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29. Pathogenesis and treatment of idiopathic and rheumatoid arthritis-related interstitial pneumonia. The possible lesson from COVID-19 pneumonia

Author

Manfredi, A, Luppi, F, Cassone, G, Vacchi, C, Salvarani, C, Sebastiani, M, Manfredi, A, Luppi, F, Cassone, G, Vacchi, C, Salvarani, C, and Sebastiani, M

Abstract

Introduction: Main clinical manifestations of SARS-CoV-2 infection are characterized by fever, dyspnea, and interstitial pneumonia, frequently evolving in acute respiratory distress syndrome (ARDS). Areas covered: Features of coronavirus disease 2019 (COVID-19) presents some common points with interstitial lung disease (ILD) both idiopathic and related to rheumatoid arthritis (RA), typically characterized by a chronic progression over time and possibly complicated by acute exacerbation (AE). The study of common pathogenetic mechanisms, such as the involvement of toll-like receptor 4, could contribute to the knowledge and treatment of idiopathic and RA-ILD. Moreover, hyperinflammation, mainly characterized by increase of effector T-cells and inflammatory cytokines, and activation of coagulation cascade, observed in COVID-19 related ARDS have been already shown in patients with AE of idiopathic and RA-ILD. A literature search was performed in PubMed, Embase, Scopus, and Web of Science, together with a manual search in COVID-resource centers of the main journals. Expert opinion: Despite the uncertainty about pathogenetic aspects about COVID-19- pneumonia, it could be a possible model for other forms of ILD and AE. The great amount of data from studies on COVID-19 could be helpful in proposing safe therapeutic approaches for RA-ILD, in understanding pathogenesis of usual interstitial pneumonia and to develop new therapeutic strategies for AE.

Published
2020

30. Epidemiology and management of interstitial lung disease in ANCA-associated vasculitis

Author

Sebastiani, M, Manfredi, A, Vacchi, C, Cassone, G, Faverio, P, Cavazza, A, Sverzellati, N, Salvarani, C, Luppi, F, M. Sebastiani, A. Manfredi, C. Vacchi, G. Cassone, P. Faverio, A. Cavazza, N. Sverzellati, C. Salvarani, F. Luppi, Sebastiani, M, Manfredi, A, Vacchi, C, Cassone, G, Faverio, P, Cavazza, A, Sverzellati, N, Salvarani, C, Luppi, F, M. Sebastiani, A. Manfredi, C. Vacchi, G. Cassone, P. Faverio, A. Cavazza, N. Sverzellati, C. Salvarani, and F. Luppi

Abstract

Antineutrophil cytoplasmic antibodies (ANCA)-associated vasculitis (AAV) is a group of systemic vasculitides that predominantly affect small vessels, including granulomatosis with polyangiitis (GPA), microscopic polyangiitis (MPA), and eosinophilic granulomatosis with polyangiitis (EGPA). Pulmonary involvement is frequently observed in AAV patients, with various possible phenotypes in the different diseases. In the last years, among the possible types of lung involvement, a growing interest has been addressed to the interstitial lung disease (ILD). Prevalence of ILD is higher in MPA than in GPA; in fact, ILD has been reported in up to 45% of MPA patients and in 23% of GPA. Anti-MPO antibodies are the main ANCA subtype associated to ILD, in about 46-71% of cases, while anti-PR3 antibodies are reported in 0-29% of patients. High resolution computed tomography (HRCT) frequently detects interstitial lung abnormalities in AAV, up to 66% of patients with MPA, even if with an unclear clinical relevance, specifically in asymptomatic patients. Ground glass opacities, mainly consistent with diffuse alveolar hemorrhage (DAH), are the most frequent finding in MPA patients, but reticulations, interlobular septal thickening and honeycombing are also reported. ILD significantly affects quality of life and survival, with mortality increased 2 to 4 times, particularly higher in MPA patients with pulmonary fibrosis. Currently, immunosuppressive therapy is considered also as a possible treatment of ILD. However, a careful evaluation of progression and severity of lung involvement, should guide the treatment decision in the single patient. In this review, we discuss the available evidence on clinical features, diagnostic work-up, prognosis and management of AAV-ILD.

Published
2020

31. Treatment of Rheumatoid Arthritis-Associated Interstitial Lung Disease: Lights and Shadows

Author

Cassone, G, Manfredi, A, Vacchi, C, Luppi, F, Coppi, F, Salvarani, C, Sebastiani, M, Cassone, Giulia, Manfredi, Andreina, Vacchi, Caterina, Luppi, Fabrizio, Coppi, Francesca, Salvarani, Carlo, Sebastiani, Marco, Cassone, G, Manfredi, A, Vacchi, C, Luppi, F, Coppi, F, Salvarani, C, Sebastiani, M, Cassone, Giulia, Manfredi, Andreina, Vacchi, Caterina, Luppi, Fabrizio, Coppi, Francesca, Salvarani, Carlo, and Sebastiani, Marco

Abstract

Rheumatoid arthritis (RA) is a chronic and systemic inflammatory disease affecting 0.5-1% of the population worldwide. Interstitial lung disease (ILD) is a serious pulmonary complication of RA and it is responsible for 10-20% of mortality, with a mean survival of 5-8 years. However, nowadays there are no therapeutic recommendations for the treatment of RA-ILD. Therapeutic options for RA-ILD are complicated by the possible pulmonary toxicity of many disease modifying anti-rheumatic drugs (DMARDs) and by their unclear efficacy on pulmonary disease. Therefore, joint and lung involvement should be evaluated independently of each other for treatment purposes. On the other hand, some similarities between RA-ILD and idiopathic pulmonary fibrosis and the results of the recent INBIULD trial suggest a possible future role for antifibrotic agents. From this perspective, we review the current literature describing the pulmonary effects of drugs (immunosuppressants, conventional, biological and target synthetic DMARDs and antifibrotic agents) in patients with RA and ILD. In addition, we suggest a framework for the management of RA-ILD patients and outline a research agenda to fill the gaps in knowledge about this challenging patient cohort.

Published
2020

35. THU0127 Estimated cardiovascular risk in a large cohort of rheumatoid arthritis patients from the “Cardiovascular Obesity and Rheumatic DISease (CORDIS)” Study Group of the Italian Society of Rheumatology.

Author

Cacciapaglia, F., primary, Piga, M., additional, Erre, G., additional, Manfredi, A., additional, Bartoloni Bocci, E., additional, Sakellariou, G., additional, Viapiana, O., additional, Colella, S., additional, Abbruzzese, A., additional, Dessì, M., additional, Vacchi, C., additional, Castagna, F., additional, Cafaro, G., additional, Palermo, B. L., additional, Giollo, A., additional, Fornaro, M., additional, Gremese, E., additional, Spinelli, F. R., additional, and Atzeni, F., additional

Published
2020
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36. AB0528 CHARACTERIZATION OF ANTI-MPO POSITIVE INTERSTITIAL LUNG DISEASE. CLINICAL-SEROLOGIC AND RADIOLOGIC FEATURES AND SURVIVAL

Author

Cassone, G., primary, Dei, G., additional, Sambataro, G., additional, Manfredi, A., additional, Cerri, S., additional, Vacchi, C., additional, Faverio, P., additional, Sambataro, D., additional, Gozzi, F., additional, Vancheri, C., additional, Salvarani, C., additional, Luppi, F., additional, and Sebastiani, M., additional

Published
2020
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38. THU0150 INTERSTITIAL LUNG DISEASE RELATED TO RHEUMATOID ARTHRITIS. WHAT DO WE DON’T KNOW? THE LIRA STUDY (LUNG INVOLVEMENT IN RHEUMATOID ARTHRITIS).

Author

Sebastiani, M., primary, Vacchi, C., additional, Cassone, G., additional, Atzeni, F., additional, Biggioggero, M., additional, Carriero, A., additional, Erre, G. L., additional, Fedele, A. L., additional, Furini, F., additional, Tomietto, P., additional, Venerito, V., additional, Atienza-Mateo, B., additional, Della Casa, G., additional, Cerri, S., additional, Sandri, G., additional, Palermo, A., additional, Galli, E., additional, Pancaldi, F., additional, González-Gay, M. A., additional, Salvarani, C., additional, and Manfredi, A., additional

Published
2020
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39. Test results and prospects for RD53A, a large scale 65 nm CMOS chip for pixel readout at the HL-LHC

Author

Gaioni, (Gaioni, L, Luigi), Barbero, (Barbero, Mb, ( 1 ), M. B., Fougeron, (Fougeron, D, ( 1 ), D., Godiot, (Godiot, S, ( 1 ), S., Menouni, (Menouni, M, ( 1 ), M., Pangaud, (Pangaud, P, ( 1 ), P., Rozanov, (Rozanov, A, ( 1 ), A., Breugnon, (Breugnon, P, Bomben, (Bomben, M, ( 2 ), M., Calderini, (Calderini, G, ( 2 ), G., Crescioli, (Crescioli, F, ( 2 ), F., Dortz, Le, O (Le Dortz, ( 2 ), O., Marchiori, (Marchiori, G, Dzahini, (Dzahini, D, ( 3 ), D., Rarbi, (Rarbi, Fe, ( 3 ), F. E., Gaglione, (Gaglione, R, ( 4 ), R., Kruger, (Krueger, H, ( 5 ), H., Daas, (Daas, M, ( 5 ), M., Dieter, (Dieter, Y, ( 5 ), Y., Hemperek, (Hemperek, T, ( 5 ), T., Hugging, (Huegging, F, ( 5 ), F., Moustakas, (Moustakas, K, ( 5 ), K., Pohl, (Pohl, D, ( 5 ), D., Rymaszewski, (Rymaszewski, P, ( 5 ), P., Standke, (Standke, M, Vogt, (Vogt, M, Wang, (Wang, T, Wermes, (Wermes, N, ( 5 ), N., Karagounis, (Karagounis, M, Stiller, (Stiller, A, ( 6 ), A., Marzocca, (Marzocca, C, ( 7 ), C., Robertis, De, G (De Robertis, ( 8 ), G., Loddo, (Loddo, F, ( 8 ), F., Licciulli, (Licciulli, F, Andreazza, (Andreazza, A, ( 9, A., 10, ), Liberali, (Liberali, V, V)(, 9, Stabile, (Stabile, A, Frontini, (Frontini, L, ( 9, L., Bagatin, (Bagatin, M, ( 11, M., 12, ), Bisello, (Bisello, D, ( 11, D., Gerardin, (Gerardin, S, ( 11, S., Mattiazzo, (Mattiazzo, S, Paccagnella, (Paccagnella, A, ( 11, A., Vogrig, (Vogrig, D, Bonaldo, (Bonaldo, S, Bacchetta, (Bacchetta, N, ( 11 ), N., ( 13, L., 14, ), Canio, De, F (De Canio, ( 13, F., Manghisoni, (Manghisoni, M, ( 13, M., (Re, V, V)(, 13, Riceputi, (Riceputi, E, ( 13, E., Traversi, (Traversi, G, ( 13, G., Ratti, (Ratti, L, ( 15, L., 16, ), Vacchi, (Vacchi, C, ( 15, C., Androsov, (Androsov, K, ( 18, K., 19, ), Beccherle, (Beccherle, R, ( 17 ), R., Magazzu, (Magazzu, G, ( 17 ), G., Minuti, (Minuti, M, ( 17 ), M., Morsani, (Morsani, F, ( 17 ), F., Palla, (Palla, F, Poulios, (Poulios, S, ( 17 ), S., Bilei, (Bilei, Gm, ( 20 ), G. M., Menichelli, (Menichelli, M, ( 20 ), M., Marconi, S., Placidi, P., Dellacasa, (Dellacasa, G, ( 22 ), G., Demaria, (Demaria, N, ( 22 ), N., Mazza, (Mazza, G, Monteil, (Monteil, E, ( 22 ), E., Pacher, (Pacher, L, ( 22 ), L., Paterno, (Paterno, A, ( 22, A., 23, ), Rivetti, (Rivetti, A, ( 22 ), A., Rolo, Mdd, (Rolo, Da Rocha)( 22 ), M. D., Gajanana, (Gajanana, D, ( 24 ), D., Gromov, (Gromov, V, V)( 24, ), Van, Eijk, B (van Eijk, ( 24 ), B., Kluit, (Kluit, R, ( 24 ), R., Vitkovskiy, (Vitkovskiy, A, ( 24 ), A., Benka, (Benka, T, ( 25 ), T., Havranek, (Havranek, M, ( 25 ), M., Janoska, (Janoska, Z, ( 25 ), Z., Marcisovsky, (Marcisovsky, M, Neue, (Neue, G, ( 25 ), G., Tomasek, (Tomasek, L, ( 25 ), L., Kafka, (Kafka, V, V)( 26, ), Vrba, (Vrba, V, ( 28 ), V., Lopez-Morillo, (Lopez-Morillo, E, ( 28 ), E., Palomo, (Palomo, Fr, ( 28 ), F. R., Munoz, (Munoz, F, ( 28 ), F., Vila, (Vila, I, I)( 27, ), Jimenez, Ems, (Jimenez, ( 27 ), E. M. S., Abbaneo, (Abbaneo, D, ( 29 ), D., Christiansen, (Christiansen, J, ( 29 ), J., Orfanelli, (Orfanelli, S, ( 29 ), S., Casas, Lmj, (Casas, Jara)( 29 ), L. M., Conti, (Conti, E, ( 29 ), E., Bell, (Bell, S, ( 30 ), S., Prydderch, (Prydderch, Ml, ( 30 ), M. L., Thomas, (Thomas, S, Christian, (Christian, Dc, ( 31 ), D. C., Deptuch, (Deptuch, G, ( 31 ), G., Fahim, (Fahim, F, ( 31 ), F., Hoff, (Hoff, J, ( 31 ), J., Lipton, (Lipton, R, ( 31 ), R., Liu, (Liu, T, ( 31 ), T., Zimmerman, (Zimmerman, T, Miryala, (Miryala, S, ( 31 ), S., Garcia-Sciveres, (Garcia-Sciveres, M, ( 32 ), M., Gnani, (Gnani, D, ( 32 ), D., Krieger, (Krieger, A, ( 32 ), A., Papadopoulou, (Papadopoulou, K, ( 32 ), K., Heim, (Heim, T, ( 32 ), T., Carney, (Carney, R, ( 32 ), R., Nachman, (Nachman, B, ( 32 ), B., Renteira, (Renteira, C, ( 32 ), C., Wallangen, (Wallangen, V, V)( 32, ), Hoeferkamp, (Hoeferkamp, M, ( 33 ), M., Seidel, (Seidel, S, ( 33 ), S., Centre de Physique des Particules de Marseille (CPPM), Aix Marseille Université (AMU)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Centre National de la Recherche Scientifique (CNRS), Laboratoire de Physique Nucléaire et de Hautes Énergies (LPNHE (UMR_7585)), Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)-Université de Paris (UP), Laboratoire de Physique Subatomique et de Cosmologie (LPSC), Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Centre National de la Recherche Scientifique (CNRS)-Université Grenoble Alpes (UGA)-Institut polytechnique de Grenoble - Grenoble Institute of Technology (Grenoble INP ), Université Grenoble Alpes (UGA), Laboratoire d'Annecy de Physique des Particules (LAPP), Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Université Savoie Mont Blanc (USMB [Université de Savoie] [Université de Chambéry])-Centre National de la Recherche Scientifique (CNRS), RD53, and Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)

Subjects
Cmos chip, Nuclear and High Energy Physics, Scale (ratio), BitTorrent tracker, High-luminosity LHC, Low noise analog front-end, 01 natural sciences, Settore ING-INF/01 - Elettronica, 030218 nuclear medicine & medical imaging, 03 medical and health sciences, 0302 clinical medicine, semiconductor detector: pixel, ATLAS, CMS, Pixel readout chip, RD53, Micro-electronics and interconnections [4], 0103 physical sciences, [PHYS.PHYS.PHYS-INS-DET]Physics [physics]/Physics [physics]/Instrumentation and Detectors [physics.ins-det], Detectors and Experimental Techniques, Instrumentation, activity report, radiation: damage, Physics, Large Hadron Collider, Pixel, 010308 nuclear & particles physics, business.industry, radiation: effect, Emphasis (telecommunications), Mixed-signal integrated circuit, Chip, business, Computer hardware, performance, semiconductor detector: design
Abstract

International audience; The CERN RD53 collaboration was founded to tackle the extraordinary challenges associated with the design of pixel readout chips for the innermost layers of particle trackers at future high energy physics experiments. Around 20 institutions are involved in the collaboration, which has the support of both ATLAS and CMS experiments. The goals of the collaboration include the comprehensive understanding of radiation effects in the 65 nm technology, the development of tools and methodology to efficiently design large complex mixed signal chips and, ultimately, the development of a full size readout chip featuring a 400 × 400 pixel array with 50μm pitch. In August 2017, the collaboration submitted the large scale chip RD53A, integrating a matrix of 400 × 192 pixels and embodying three different analog front-end designs. This work discusses the characteristic of the RD53A chip, with some emphasis on the analog processors, and presents the first test results on the pixel array.

Published
2019
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42. Acute exacerbation of interstitial lung diseases secondary to systemic rheumatic diseases: A prospective study and review of the literature

Author

Manfredi, A, Sebastiani, M, Cerri, S, Vacchi, C, Tonelli, R, Della Casa, G, Cassone, G, Spinella, A, Pancaldi, F, Luppi, F, Salvarani, C, Manfredi, A, Sebastiani, M, Cerri, S, Vacchi, C, Tonelli, R, Della Casa, G, Cassone, G, Spinella, A, Pancaldi, F, Luppi, F, and Salvarani, C

Abstract

Acute exacerbation (AE) is a possible manifestation of interstitial lung diseases (ILD) associated to very high mortality. It’s defined as clinically significant respiratory deterioration with evidence of new widespread alveolar abnormalities on computed tomography scan. AE is better described in idiopathic pulmonary fibrosis (IPF) but also reported in ILD secondary to connective tissue diseases (CTD) and vasculitis. The main features and the real clinical impact of this severe complication in these patients are not well defined. Aim of our study was to prospectively investigate the incidence, clinical features and outcome of AE in a population of patients with ILD related to CTD and vasculitis. We consecutively enrolled all patients, with ILD secondary to rheumatic systemic diseases, referring to our multidisciplinary outpatient clinic for rare lung diseases. All patients were followed for at least 12 months (range, 12–36 months). At baseline, all patients underwent to a core set of laboratory investigations and periodically followed; data about demographic, disease onset, clinical, serological and therapeutic features were also recorded. AE occurred in 9/78 patients, with an incidence of 5.77/100 patients/year, and 5/9 patients died because of AE. The baseline value of DLCO was significantly associated to the risk of AE at Cox regression. In patients with ILD related to rheumatic systemic diseases AE can occur with an incidence similar to IPF. Rheumatologists should carefully consider this life-threatening complication as a possible natural course of all patients with ILD secondary to systemic rheumatic disease.

Published
2019

44. Radiation tolerance characterization of Geiger-mode CMOS avalanche diodes for a dual-layer particle detector

Author

Musacci, M., primary, Bigongiari, G., additional, Brogi, P., additional, Checchia, C., additional, Collazuol, G., additional, Dalla Betta, G.-F., additional, Ficorella, A., additional, Marrocchesi, P.S., additional, Mattiazzo, S., additional, Morsani, F., additional, Noli, S., additional, Pancheri, L., additional, Ratti, L., additional, Savoy Navarro, A., additional, Silvestrin, L., additional, Stolzi, F., additional, Suh, J., additional, Sulaj, A., additional, Vacchi, C., additional, and Zarghami, M., additional

Published
2019
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45. RD53A: a large scale prototype for HL-LHC silicon pixel detector phase 2 upgrades

Author

Monteil, Ennio, primary, Barbero, M., additional, Fougeron, D., additional, Godiot, S., additional, Menouni, M., additional, Pangaud, P., additional, Rozanov, A., additional, Breugnon, P., additional, Bomben, Marco, additional, Calderini, G., additional, Crescioli, F., additional, Marchiori, G., additional, Dzahini, D., additional, Rarbi, F.E., additional, Gaglione, R., additional, Krueger, H., additional, Hemperek, T., additional, Huegging, F., additional, Rymazewski, P., additional, Vogt, M., additional, Wang, T., additional, Wermes, N., additional, Karagounis, M., additional, Marzocca, C., additional, Loddo, F., additional, Licciulli, F., additional, Andreazza, A., additional, Liberali, V., additional, Stabile, A., additional, Frontini, L., additional, Bagatin, M., additional, Bisello, D., additional, Gerardin, S., additional, Mattiazzo, S., additional, Paccagnella, A., additional, Vogrig, D., additional, Bonaldo, S., additional, Bacchetta, N., additional, Gaioni, L., additional, Manghisoni, M., additional, Re, V., additional, Riceputi, E., additional, Traversi, G., additional, Ratti, L., additional, Vacchi, C., additional, Androsov, K., additional, Beccherle, R., additional, Magazzù, G., additional, Minuti, M., additional, Morsani, F., additional, Palla, F., additional, Poulios, S., additional, Bilei, G.M., additional, Menichelli, M., additional, Placidi, P., additional, Marconi, S., additional, Dellacasa, G., additional, Demaria, N., additional, Mazza, G., additional, Monteil, E., additional, Pacher, L., additional, Rivetti, A., additional, Paternò, A., additional, Gajanna, D., additional, Gromov, V., additional, Kluit, R., additional, Vitkovskiy, A., additional, Benka, T., additional, Havranek, M., additional, Janoska, Z., additional, Marcisovsky, M., additional, Neue, G., additional, Tomasek, L., additional, Kafka, V., additional, Vrba, V., additional, Lopez-Morillo, E., additional, Palomo, F.R., additional, Munoz, F., additional, Vila, Ivan, additional, Jiménez, E., additional, Abbaneo, D., additional, Christiansen, J., additional, Orfanelli, S., additional, Bell, S.J.M., additional, Prydderch, M., additional, Thomas, S., additional, Christian, D.C., additional, Deptuch, G., additional, Fahim, F., additional, Hoff, J., additional, Zimmerman, T., additional, Miryala, S., additional, Garcia-Sciveres, M., additional, Gnani, D., additional, Krieger, A., additional, Papadopoulou, K., additional, Heim, T., additional, Carney, R., additional, Nachman, Benjamin, additional, Renteira, C., additional, Wallangen, V., additional, Hoeferkamp, M.R., additional, Seidel, S., additional, Daas, M., additional, Dieter, Y., additional, Moustakas, K., additional, Stiller, A., additional, Lipton, R., additional, and Liu, T. C., additional

Published
2019
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46. Dark Count Rate Degradation in CMOS SPADs Exposed to X-Rays and Neutrons

Author

Ratti, Lodovico, primary, Brogi, P., additional, Collazuol, G., additional, Dalla Betta, G.-F., additional, Ficorella, A., additional, Lodola, L., additional, Marrocchesi, P. S., additional, Mattiazzo, S., additional, Morsani, F., additional, Musacci, M., additional, Pancheri, L., additional, and Vacchi, C., additional

Published
2019
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47. A Case of Refractory Dysphagia in the Context of Polymyositis Treated with Subcutaneous Immunoglobulin and Review of the Literature

Author

Vacchi C

Subjects
030203 arthritis & rheumatology, 0301 basic medicine, medicine.medical_specialty, business.industry, Context (language use), General Medicine, Subcutaneous immunoglobulin, medicine.disease, Dysphagia, Polymyositis, Surgery, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Refractory, medicine, medicine.symptom, business
Published
2017
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48. Design of analog front-ends for the RD53 demonstrator chip

Author

Luigi Gaioni, F. De Canio, Nodari, B, Manghisoni, M, Re, V, Traversi, G, Barbero, M. B, Fougeron, D, Gensolen, F, Godiot M. Menouni, S, Pangaud, P, Rozanov, A, Wang, A, Bomben, M, Calderini, G, Crescioli, F, Le Dortz, O, Marchiori, G, Dzahini, D, Rarbi, F. E, Gaglione, R, Gonella, L, Hemperek, T, Huegging, F, Karagounis, M, Kishishita, T, Krueger, H, Rymaszewski, P, Wermes, N, Ciciriello, F, Corsi, F, Marzocca, C, De Robertis, G, Loddo, F, Licciulli, F, Andreazza, A, Liberali, V, Shojaii, S, Stabile, A, Bagatin, M, Bisello, D, Mattiazzo, S, Ding, L, Gerardin, S, Giubilato, P, Neviani, A, Paccagnella, A, Vogrig, D, Wyss, J, Bacchetta, N, Della Casa, G, Demaria, N, Mazza, G, Rivetti, Angelo, Da Rocha Rolo, M. D, Comotti, D, Ratti, L, Vacchi, C, Beccherle, R, Bellazzini, R, Magazzu, G, Minuti, M, Morsani, F, Palla, F, Poulios, S, Fanucci, L, Rizzi, A, Saponara, S, Androsov, K, Bilei, G. M, Menichelli, M, Conti, E, Marconi, S, Passeri, D, Placidi, P, Monteil, E, Pacher, L, Gajanana, D, Gromov, V, Hessey, N, Kluit, R, Zivkovic, V, Havranek, M, Janoska, Z, Marcisovsky, M, Neue, G, Tomasek, L, Kafka, V, Sicho, P, Vrba, V, Vila, I, Lopez Morillo, E, Aguirre, M. A, Palomo, F. R, Munoz, F, Abbaneo, D, Christiansen, J, Dannheim, D, Dobos, D, Linssen, L, Pernegger, H, Valerio, P, Alipour Tehrani, N, Bell, S, Prydderch, M. L, Thomas, S, Christian, D. C, Fahim, F, Hoff, J, Lipton, R, Liu, T, Zimmerman, T, Garcia Sciveres, M, Gnani, D, Mekkaoui, A, Gorelov, I, Hoeferkamp, M, Seidel, S, Toms, K, De Witt, J. N, and Grillo, A.

Published
2017

49. Haematological Malignancies in Systemic Sclerosis Patients: Case Reports and Review of the World Literature

Author

Colaci, M., Giuggioli, D., Vacchi, C., and Ferri, C.

Subjects
integumentary system, Article Subject, skin and connective tissue diseases
Abstract

Background. The association of systemic sclerosis (SSc) and haematological cancers was reported in a large number of case reports and cohort studies, describing SSc patients with highly heterogeneous clinical pictures. Objective. We reviewed the literature to better describe SSc patients with haematological malignancies. Methods. SSc cases complicated by haematological malignancies described in the world literature were collected; other 2 cases referred to our centre were reported. Results. One hundred-thirty SSc subjects were collected from 1954 up to date. The mean age of patients at cancer diagnosis was 56.1 ± 16.7 years; 72% of patients were females. In 60% of cases, the diagnosis of haematological malignancy was described within 5 years of SSc diagnosis. In 7.8% of cases, coexistence of Sjögren’s syndrome or other autoimmune disorders was cited. Sixty-six cases with lymphoma (in the majority of cases B-cell neoplasms), 28 with leukaemia (chronic lymphocytic form in 9), 14 with multiple myeloma plus one solitary IgM plasmocytoma, and 16 with myeloproliferative disorders were found. No specific SSc subsets seem to be related to haematological malignancies. Conclusions. We remarked the importance of clinical work-up in SSc, in order to early diagnose and treat eventual occult haematological malignancies, especially during the first years of the disease.

Published
2017
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50. Interstiziopatia polmonare non classificabile o secondaria a connettivite indifferenziata. importanza e difficoltà di una diagnosi differenziale

Author

Manfredi, AT, Sebastiani, M, Cerri, S, Della Casa, G, Vacchi, C, Giuggioli, D, Colaci, M, Luppi, F, Ferri, C, Manfredi, A, Sebastiani, M, Cerri, S, Della Casa, G, Vacchi, C, Giuggioli, D, Colaci, M, Luppi, F, and Ferri, C

Subjects
Interstiziopatia polmonare, UCTD
Abstract

Introduzione. Le interstiziopatie polmonari rappresentano un ampio gruppo di malattie che causano fibrosi o infiammazione del parenchima polmonare. Le principali forme sono quelle secondarie ad esposizione ambientale, fibrosi polmonari idiopatiche, polmoniti interstiziali non specifiche (NSIP), forme secondarie a sarcoidosi e quelle secondarie alle connettiviti. Quando per qualche motivo (limiti diagnostici, fattori confondenti, quadri atipici, ecc.) non è possibile classificare un’interstiziopatia nei sottotipi soprariportati, questa viene definita come non classificabile (U-ILD). Le connettiviti indifferenziate (UCTD) sono malattie sistemiche caratterizzate da caratteristiche cliniche e sierologiche tipiche di altre connettiviti definite ma che non ne soddisfano i criteri classificativi esistenti. Il coinvolgimento polmonare è raramente descritto in pazienti affetti da UCTD e non è solitamente considerato a fini diagnostici e classificativi come possibile manifestazione d’esordio. Recentemente alcuni autori hanno suggerito che alcune interstiziopatie non classificabili potrebbero essere meglio inquadrate come secondarie a connettiviti. Nella pratica clinica, soprattutto quando il quadro respiratorio sembra essere il sintomo d’esordio della patologia, la diagnosi differenziale può essere estremamente complessa, eppure di sostanziale importanza alla luce delle implicazioni terapeutiche. Scopo dello studio. Individuare le caratteristiche cliniche e sierologiche che distinguono le U-ILD dalle interstiziopatie secondarie ad UCTD (UCTD-ILD) per migliorare la diagnosi differenziale e individuare pazienti candidati a terapia immunosoppressiva. Metodi. Fra settembre 2011 a novembre 2014, 50 pazienti valutati presso il nostro centro venivano classificati come affetti da UCTD o U-ILD, dopo discussione interdisciplinare, secondo i criteri presenti in letteratura. Il quadro radiologico rilevato alla TC ad alta risoluzione veniva classificato come usual interstitial pneumonia (UIP) definito, possibile o non compatibile, secondo i criteri classificativi della fibrosi polmonare idiopatica. Risultati. Le principali caratteristiche dei pazienti sono riportate nella tabella. Il fenomeno di Raynaud, la xeroftalmia e la positività dell’ANA test risultavano più frequenti nei pazienti con UCTD (rispettivamente p=0.27, p=0-07, p=0.2). Un pattern radiologico non compatibile con UIP veniva rilevato in circa il 70% dei pazienti con UCTD. Un modello predittivo basato su fenomeno di Raynaud, xeroftalmia, positività dell’ANA test mostrava un valore predittivo dell’85,7% (le UCTD venivano classificate nel 90,5% e le U-ILD nel 78,6%). Conclusioni. Il coinvolgimento polmonare è una possibile manifestazione d’esordio delle UCTD. La diagnosi differenziale con le U-ILD può essere problematica ma è assolutamente necessaria per le conseguenti implicazioni nell’approccio terapeutico. A questo scopo, un’attenta valutazione di alcune caratteristiche cliniche e sierologiche può essere di aiuto. Un lavoro in team multidisciplinare che includa reumatologo, pneumologo, radiologo, anatomo-patologo rappresenta l’approccio migliore al paziente con interstiziopatia polmonare da definire.

Published
2015

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