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51. Comparison of fingolimod, dimethyl fumarate and teriflunomide for multiple sclerosis.

Author

Spelman T., Karabudak R., Butler E., Vucic S., Jokubaitis V., Butzkueven H., Kalincik T., Kubala Havrdova E., Horakova D., Izquierdo G., Prat A., Girard M., Duquette P., Grammond P., Onofrj M., Lugaresi A., Ozakbas S., Kappos L., Kuhle J., Terzi M., Lechner-Scott J., Boz C., Grand'maison F., Prevost J., Sola P., Ferraro D., Granella F., Trojano M., Bergamaschi R., Pucci E., Turkoglu R., McCombe P.A., Pesch V.V., Van Wijmeersch B., Solaro C., Ramo-Tello C., Slee M., Alroughani R., Yamout B., Shaygannejad V., Spitaleri D., Sanchez-Menoyo J.L., Ampapa R., Hodgkinson S., Spelman T., Karabudak R., Butler E., Vucic S., Jokubaitis V., Butzkueven H., Kalincik T., Kubala Havrdova E., Horakova D., Izquierdo G., Prat A., Girard M., Duquette P., Grammond P., Onofrj M., Lugaresi A., Ozakbas S., Kappos L., Kuhle J., Terzi M., Lechner-Scott J., Boz C., Grand'maison F., Prevost J., Sola P., Ferraro D., Granella F., Trojano M., Bergamaschi R., Pucci E., Turkoglu R., McCombe P.A., Pesch V.V., Van Wijmeersch B., Solaro C., Ramo-Tello C., Slee M., Alroughani R., Yamout B., Shaygannejad V., Spitaleri D., Sanchez-Menoyo J.L., Ampapa R., and Hodgkinson S.

Abstract

Objective Oral immunotherapies have become a standard treatment in relapsing-remitting multiple sclerosis. Direct comparison of their effect on relapse and disability is needed. Methods We identified all patients with relapsing-remitting multiple sclerosis treated with teriflunomide, dimethyl fumarate or fingolimod, with minimum 3-month treatment persistence and disability follow-up in the global MSBase cohort study. Patients were matched using propensity scores. Three pairwise analyses compared annualised relapse rates and hazards of disability accumulation, disability improvement and treatment discontinuation (analysed with negative binomial models and weighted conditional survival models, with pairwise censoring). Results The eligible cohorts consisted of 614 (teriflunomide), 782 (dimethyl fumarate) or 2332 (fingolimod) patients, followed over the median of 2.5 years. Annualised relapse rates were lower on fingolimod compared with teriflunomide (0.18 vs 0.24; p=0.05) and dimethyl fumarate (0.20 vs 0.26; p=0.01) and similar on dimethyl fumarate and teriflunomide (0.19 vs 0.22; p=0.55). No differences in disability accumulation (p>=0.59) or improvement (p>=0.14) were found between the therapies. In patients with >=3-month treatment persistence, subsequent discontinuations were less likely on fingolimod than teriflunomide and dimethyl fumarate (p<0.001). Discontinuation rates on teriflunomide and dimethyl fumarate were similar (p=0.68). Conclusion The effect of fingolimod on relapse frequency was superior to teriflunomide and dimethyl fumarate. The effect of the three oral therapies on disability outcomes was similar during the initial 2.5 years on treatment. Persistence on fingolimod was superior to the two comparator drugs.Copyright © 2019 Author(s) (or their employer(s)). No commercial re-use. See rights and permissions. Published by BMJ.

Published
2019

52. Anti-inflammatory disease-modifying treatment and disability progression in primary progressive multiple sclerosis: a cohort study

Author

Lorscheider, J, Kuhle, J, Izquierdo, G, Lugaresi, A, Havrdova, E, Horakova, D, Hupperts, R, Duquette, P, Girard, M, Prat, A, Grand'Maison, F, Grammond, P, Sola, P, Ferraro, D, Trojano, M, Ramo-Tello, C, Lechner-Scott, J, Pucci, E, Solaro, C, Slee, M, Van Pesch, V, Sanchez Menoyo, JL, van der Walt, A, Butzkueven, H, Kappos, L, Kalincik, T, Lorscheider, J, Kuhle, J, Izquierdo, G, Lugaresi, A, Havrdova, E, Horakova, D, Hupperts, R, Duquette, P, Girard, M, Prat, A, Grand'Maison, F, Grammond, P, Sola, P, Ferraro, D, Trojano, M, Ramo-Tello, C, Lechner-Scott, J, Pucci, E, Solaro, C, Slee, M, Van Pesch, V, Sanchez Menoyo, JL, van der Walt, A, Butzkueven, H, Kappos, L, and Kalincik, T

Abstract

BACKGROUND AND PURPOSE: Treatment options in primary progressive multiple sclerosis (PPMS) are scarce and, with the exception of ocrelizumab, anti-inflammatory agents have failed to show efficacy in ameliorating disability progression. The aim of this study was to investigate a potential effect of anti-inflammatory disease-modifying treatment on disability outcomes in PPMS. METHODS: Using MSBase, a large, international, observational database, we identified patients with PPMS who were either never treated or treated with a disease-modifying agent. Propensity score matching was used to select subpopulations with similar baseline characteristics. Expanded Disability Status Scale (EDSS) outcomes were compared with an intention-to-treat and an as-treated approach in paired, pairwise-censored analyses. RESULTS: Of the 1284 included patients, 533 were matched (treated, n = 195; untreated n = 338). Median on-study pairwise-censored follow-up was 3.4 years (quartiles 1.2-5.5). No difference in the hazard of experiencing 3-month confirmed EDSS progression events was observed between the groups [hazard ratio (HR), 1.0; 95% confidence interval (CI), 0.6-1.7, P = 0.87]. We did not find significant differences in the hazards of confirmed EDSS improvement (HR, 1.0; 95% CI, 0.6-1.6, P = 0.91) or reaching a confirmed EDSS step ≥7 (HR, 1.1; 95% CI, 0.7-1.6, P = 0.69). CONCLUSION: Our pooled analysis of disease-modifying agents suggests that these therapies have no substantial effect on short- to medium-term disability outcomes in PPMS.

Published
2019

60. The Italian dementia with Lewy bodies study group (DLB-SINdem): toward a standardization of clinical procedures and multicenter cohort studies design

Author

Bonanni, L, Cagnin, A., Agosta, F., Babiloni, C., Borroni, B., Bozzali, M., Bruni, A. C., Filippi, M., Galimberti, D., Monastero, R., Muscio, C., Parnetti, L., Perani, D., Serra, L., Silani, V., Tiraboschi, P., Padovani, A., On behalf of DLB SINdem study group, Null, Alberici, A., Alberoni, M., Amici, S., Appollonio, I., Arena, M. G., Arighi, A., Avanzi, S., Bagella, C. F., Baglio, F., Barocco, F., Belardinelli, N., Bonuccelli, U., Bottini, G., Bruno Bossio, R., Bruno, G., Buccomino, D., Cacchiò, G., Calabrese, E., Campanelli, A., Canevelli, M., Canu, E. D. G., Cappa, A., Capra, C., Carapelle, E., Caratozzolo, S., Carbone, G. F. S., Cattaruzza, T., Cerami, C., Cester, A., Cheldi, A., Cherchi, R., Chiari, A., Cirafisi, C., Colao, R., Confaloni, A., Conti, M. Z., Costa, A., Costa, B., Cotelli, M. S., Cova, I., Cravello, L., Cumbo, E., Cupidi, C., De Togni, L., Del Din, G., Del Re, M. L., Dentizzi, C., Di Lorenzo, F., Di Stefano, F., Dikova, N., Farina, E., Floris, G., Foti, A., Franceschi, M., Fumagalli, G. G., Gabelli, C., Ghidoni, E., Giannandrea, D., Giordana, M. T., Giorelli, M., Giubilei, F., Grimaldi, L., Grimaldi, R., Guglielmi, V., Lanari, A., Le Pira, F., Letteri, F., Levi Minzi, G. V., Lorusso, S., Ludovico, L., Luzzi, S., Maggiore, L., Magnani, G., Mancini, G., Manconi, F. M., Manfredi, L., Maniscalco, M., Marano, P., Marcon, M., Marcone, A., Marra, C., Martorana, A., Mascia, M. G., Mascia, V., Mauri, M., Mazzei, B., Meloni, M., Merlo, P., Messa, G., Milia, A., Monacelli, F., Montecalvo, G., Moschella, V., Mura, G., Nemni, R., Nobili, F., Notarelli, A., Di Giacomo, R., Onofrj, M., Paci, C., Padiglioni, C., Perini, M., Perotta, D., Perri, Formenti A., Perri, R., Piccininni, C., Piccoli, T., Pilia, G., Pilotto, A., Poli, S., Pomati, S., Pompanin, S., Pucci, E., Puccio, G., Quaranta, D., Rainero, I., Rea, G., Realmuto, S., Riva, M., Rizzetti, M. C., Rolma, G., Rozzini, L., Sacco, L., Saibene, F. L., Scarpini, E., Sensi, S., Seripa, D., Sinforiani, E., Sorbi, S., Sorrentino, Giuseppe, Spallazzi, M., Stracciari, A., Talarico, G., Tassinari, T., Thomas, A., Tiezzi, A., Tomassini, P. F., Trebbastoni, A., Tremolizzo, L., Tripi, G., Ursini, F., Vaianella, L., Valluzzi, F., Vezzadini, G., Vista, M., Volontè, M. A., Bonanni, L, Cagnin, A, Agosta, F, Babiloni, C, Borroni, B, Bozzali, M, Bruni, A, Filippi, M, Galimberti, D, Monastero, R, Muscio, C, Parnetti, L, Perani, D, Serra, L, Silani, V, Tiraboschi, P, Padovani, A, Alberici, A, Alberoni, M, Amici, S, Appollonio, I, Arena, M, Arighi, A, Avanzi, S, Bagella, C, Baglio, F, Barocco, F, Belardinelli, N, Bonuccelli, U, Bottini, G, Bruno Bossio, R, Bruno, G, Buccomino, D, Cacchiò, G, Calabrese, E, Campanelli, A, Canevelli, M, Canu, E, Cappa, A, Capra, C, Carapelle, E, Caratozzolo, S, Carbone, G, Cattaruzza, T, Cerami, C, Cester, A, Cheldi, A, Cherchi, R, Chiari, A, Cirafisi, C, Colao, R, Confaloni, A, Conti, M, Costa, A, Costa, B, Cotelli, M, Cova, I, Cravello, L, Cumbo, E, Cupidi, C, de Togni, L, Del Din, G, Del Re, M, Dentizzi, C, Di Lorenzo, F, Di Stefano, F, Dikova, N, Farina, E, Floris, G, Foti, A, Franceschi, M, Fumagalli, G, Gabelli, C, Ghidoni, E, Giannandrea, D, Giordana, M, Giorelli, M, Giubilei, F, Grimaldi, L, Grimaldi, R, Guglielmi, V, Lanari, A, Le Pira, F, Letteri, F, Levi Minzi, G, Lorusso, S, Ludovico, L, Luzzi, S, Maggiore, L, Magnani, G, Mancini, G, Manconi, F, Manfredi, L, Maniscalco, M, Marano, P, Marcon, M, Marcone, A, Marra, C, Martorana, A, Mascia, M, Mascia, V, Mauri, M, Mazzei, B, Meloni, M, Merlo, P, Messa, G, Milia, A, Monacelli, F, Montecalvo, G, Moschella, V, Mura, G, Nemni, R, Nobili, F, Notarelli, A, Di Giacomo, R, Onofrj, M, Paci, C, Padiglioni, C, Perini, M, Perotta, D, Perri, F, Perri, R, Piccininni, C, Piccoli, T, Pilia, G, Pilotto, A, Poli, S, Pomati, S, Pompanin, S, Pucci, E, Puccio, G, Quaranta, D, Rainero, I, Rea, G, Realmuto, S, Riva, M, Rizzetti, M, Rolma, G, Rozzini, L, Sacco, L, Saibene, F, Scarpini, E, Sensi, S, Seripa, D, Sinforiani, E, Sorbi, S, Sorrentino, G, Spallazzi, M, Stracciari, A, Talarico, G, Tassinari, T, Thomas, A, Tiezzi, A, Tomassini, P, Trebbastoni, A, Tremolizzo, L, Tripi, G, Ursini, F, Vaianella, L, Valluzzi, F, Vezzadini, G, Vista, M, Volontè, M, Bruni, Ac, DLB-SINdem study, Group, Bruni, AC, and Padovani, A - On behalf of DLB-SINdem study group

Subjects
Lewy Body Disease, medicine.medical_specialty, Pediatrics, Dementia with Lewy bodie, Dementia with Lewy bodies, Dermatology, Cohort Studies, Diagnosis, Differential, 03 medical and health sciences, 0302 clinical medicine, Quality of life, Alzheimer Disease, Surveys and Questionnaires, mental disorders, Standardization of diagnostic procedures, Diagnosis, Survey, Disease Management, Humans, Italy, Research Design, 2708, Neurology (clinical), Psychiatry and Mental Health, medicine, Dementia, 030212 general & internal medicine, MED/01 - STATISTICA MEDICA, MED/26 - NEUROLOGIA, business.industry, Standardization of diagnostic procedure, General Medicine, medicine.disease, Settore MED/26 - NEUROLOGIA, Cohort, Differential, Physical therapy, Delirium, Alzheimer's disease, medicine.symptom, business, 030217 neurology & neurosurgery, Frontotemporal dementia, Cohort study
Abstract

Dementia with Lewy bodies (DLB) causes elevated outlays for the National Health Systems due to high institutionalization rate and patients' reduced quality of life and high mortality. Furthermore, DLB is often misdiagnosed as Alzheimer's disease. These data motivate harmonized multicenter longitudinal cohort studies to improve clinical management and therapy monitoring. The Italian DLB study group of the Italian Neurological Society for dementia (SINdem) developed and emailed a semi-structured questionnaire to 572 national dementia centers (from primary to tertiary) to prepare an Italian large longitudinal cohort. The questionnaire surveyed: (1) prevalence and incidence of DLB; (2) clinical assessment; (3) relevance and availability of diagnostic tools; (4) pharmacological management of cognitive, motor, and behavioural disturbances; (5) causes of hospitalization, with specific focus on delirium and its treatment. Overall, 135 centers (23.6 %) contributed to the survey. Overall, 5624 patients with DLB are currently followed by the 135 centers in a year (2042 of them are new patients). The percentage of DLB patients was lower (27 ± 8 %) than that of Alzheimer's disease and frontotemporal dementia (56 ± 27 %) patients. The majority of the centers (91 %) considered the clinical and neuropsychological assessments as the most relevant procedure for a DLB diagnosis. Nonetheless, most of the centers has availability of magnetic resonance imaging (MRI; 95 %), electroencephalography (EEG; 93 %), and FP-CIT single photon emission-computerized tomography (SPECT; 75 %) scan for clinical applications. It will be, therefore, possible to recruit a large harmonized Italian cohort of DLB patients for future cross-sectional and longitudinal multicenter studies.

Published
2017

61. Development of new multipurpose-reference materials of rice grains and rice flour

Author

Pucci, E., Zoani, C., Zappa, G., Pucci, E., Zoani, C., and Zappa, G.

Subjects
METROFOOD-RI, Characterization, Reference material, Rice, Pilot study
Abstract

This paper details with the preparation of new Multipurpose-Reference Materials (RMs) of rice grains and rice flour performed as a pilot study within the PRO-METROFOOD-RI project. RMs will be characterized for different parameters including contaminants, biomarkers, stable isotopes and markers of origin/authenticity. These RMs will also have a major role in quality control and quality assurance of other food products. Copyright� (2017) by the International Measurement Confederation (IMEKO). All rights reserved.

Published
2017

63. Disability outcomes in patients with early cerebellar symptoms in multiple sclerosis

Author

Le, M. V. H., Malpas, C., Sharmin, S., Horakova, D., Havrdova, E. K., Trojano, M., Izquierdo, G., Eichau, S., Ozakbas, S., Lugaresi, A., Prat, A., Girard, M., Duquette, P., Alroughani, R., Bergamaschi, R., Sola, P., Grammond, P., Grand Maison, F., Terzi, M., Boz, C., Hupperts, R., Butzkueven, H., Walt, A., Pucci, E., Granella, F., Pesch, V., Soysa, A., Yamout, B., Lechner-Scott, J., Spitaleri, D., Ampapa, R., Recai Turkoglu, Iuliano, G., Ramo-Tello, C., Sanchez-Menoyo, J. L., Gouider, R., Shaygannejad, V., Prevost, J., Altintas, A., Fragoso, Y., Mccombe, P., Petersen, T., Slee, M., Barnett, M., Vucic, S., and Kalincik, T.

Published
2018

64. Familial multiple sclerosis: comparing demographic and clinical characteristics with sporadic form

Author

Rojas, I., Sirbu-Adella, C., Ferraro, D., Luliano, G., Van Pesch, V., Izquierdo, G., Spelman, T., Eichau, S., Alroughani, R., Boz, C., Larochelle, C., Sanchez Menoyo, J. L., Butzkueven, H., Oreja-Guevara, C., Cartechini, E., Duquette, P., Girard, M., Trojano, M., Sola, P., Pucci, E., Vella, N., Castillo Trivino, T., Frogoso, Y., Petkovska-Boskova, T., Laffaldano, P., Terzi, M., and Ozakbas, SERKAN

Published
2018

65. No evidence of disease activity (NEDA-3) and disability improvement after alemtuzumab treatment for multiple sclerosis: a 36-month real-world study

Author

Prosperini, L, Annovazzi, P, Boffa, L, Buscarinu, Mc, Gallo, A, Matta, M, Moiola, L, Musu, L, Perini, P, Avolio, C, Barcella, V, Bianco, A, Farina, D, Ferraro, E, Pontecorvo, S, Granella, F, Grimaldi, Lme, Laroni, A, Lus, G, Patti, F, Pucci, E, Pasca, M, Sarchielli, P, Ghezzi, A, Zaffaroni, M, Baroncini, D, Buttari, F, Centonze, D, Fornasiero, A, Salvetti, M, Docimo, R, Signoriello, E, Tedeschi, G, Bertolotto, A, Capobianco, M, Comi, G, Cocco, E, Gallo, P, Puthenparampil, M, Grasso, R, Di Francescantonio, V, Rottoli, Mr, Mirabella, M, Lugaresi, A, De Luca, G, Di Ioia, M, Di Tommaso, V, Mancinelli, L, Di Battista, G, Francia, A, Ruggieri, S, Pozzilli, C, Curti, E, Tsantes, E, Palmeri, B, Lapucci, C, Mancardi, Gl, Uccelli, A, Chisari, C, D'Amico, E, Cartechini, E, Repice, Am, Magnani, E, Massaccesi, L, Calabresi, P, Di Filippo, M, Di Gregorio, M, Italian Alemtuzumab Study, Group., Prosperini, Luca, Annovazzi, Pietro, Boffa, Laura, Buscarinu, Maria Chiara, Gallo, Antonio, Matta, Manuela, Moiola, Lucia, Musu, Luigina, Perini, Paola, Avolio, Carlo, Barcella, Valeria, Bianco, Assunta, Farina, Deborah, Ferraro, Elisabetta, Pontecorvo, Simona, Granella, Franco, Grimaldi, Luigi M E, Laroni, Alice, Lus, Giacomo, Patti, Francesco, Pucci, Eugenio, Pasca, Matteo, and Sarchielli, Paola

Subjects
Adult, Male, medicine.medical_specialty, Neurology, Outcome measurement, Relapsing-Remitting, Follow-Up Studie, Multiple sclerosis, 03 medical and health sciences, Immunologic Factor, 0302 clinical medicine, Multiple Sclerosis, Relapsing-Remitting, Alemtuzumab, Multiple sclerosis, Outcome measurement, Retrospective Studie, Alemtuzumab, Internal medicine, Medicine, Humans, Immunologic Factors, Multiple sclerosi, 030212 general & internal medicine, Female, Follow-Up Studies, Magnetic Resonance Imaging, Retrospective Studies, Treatment Outcome, Neurology (clinical), Expanded Disability Status Scale, medicine.diagnostic_test, business.industry, Retrospective cohort study, Magnetic resonance imaging, Odds ratio, medicine.disease, alemtuzumab, multiple sclerosis, outcome measurement, neurology, Clinical trial, Settore MED/26 - NEUROLOGIA, business, 030217 neurology & neurosurgery, Human, medicine.drug
Abstract

In this retrospective, multicenter, real-world study we collected clinical and magnetic resonance imaging (MRI) data of all patients (n = 40) with relapsing-remitting multiple sclerosis (RRMS) treated with alemtuzumab according to a "free-of-charge" protocol available before the drug marketing approval in Italy. Almost all (39/40) started alemtuzumab after discontinuing multiple disease-modifying treatments (DMTs) because of either lack of response or safety concerns. We considered the proportion of alemtuzumab-treated patients who had no evidence of disease activity (NEDA-3) and disability improvement over a 36-month follow-up period. NEDA-3 was defined as absence of relapses, disability worsening, and MRI activity. Disability improvement was defined as a sustained reduction of ≥ 1-point in Expanded Disability Status Scale (EDSS) score. At follow-up, 18 (45%) patients achieved NEDA-3, 30 (75%) were relapse-free, 33 (82.5%) were EDSS worsening-free, and 25 (62.5%) were MRI activity-free. Eleven (27.5%) patients had a sustained disability improvement. We found no predictor for the NEDA-3 status, while the interaction of higher EDSS score by higher number of pre-alemtuzumab relapses was associated with a greater chance of disability improvement (odds ratio 1.10, p = 0.049). Our study provides real-world evidence that alemtuzumab can promote clinical and MRI disease remission, as well as disability improvement, in a significant proportion of patients with RRMS despite prior multiple DMT failures. The drug safety profile was consistent with data available from clinical trials.

Published
2018

66. Participant perspectives of a home-based palliative approach for people with severe multiple sclerosis: A qualitative study

Author

Giovannetti, A. M., Borreani, C., Bianchi, E., Giordano, A., Cilia, S., Cipollari, S., Rossi, I., Cavallaro, C., Clerici, V. T., Rossetti, E., Stefanelli, M. C., Totis, A., Pappalardo, A., Occhipinti, G., Confalonieri, P., Veronese, S., Grasso, M. G., Patti, F., Zaratin, P., Battaglia, M. A., Solari, A., Amadeo, R., Ponzio, M., Lugaresi, A., Martino, G., Palmisano, L., Pagano, E., Radice, D., Farinotti, M., Ferrari, G., Rosato, R., Oliver, D. J., Pucci, E., Tesio, L., Pietrolongo, E., Giuntoli, M., Fittipaldo, A., Cugno, C., Causarano, R., Morino, P., Campanella, A., Mantegazza, R., Tucci, L., Ippoliti, F., Morone, G., Fusco, A., Cascio, V., Cimino, V., Zagari, F., Lopes de Carvalho, M. L., Motta, R., Onofrj, M., Da Col, D., and Casale, G.

Subjects
Male, Genetics and Molecular Biology (all), Palliative care, Medical Doctors, Psychologists, Team Role Inventories, Health Care Providers, medicine.medical_treatment, Nurses, Social Sciences, lcsh:Medicine, Referring Physician, Severity of Illness Index, Biochemistry, law.invention, 0302 clinical medicine, Sociology, Randomized controlled trial, Biochemistry, Genetics and Molecular Biology (all), Agricultural and Biological Sciences (all), law, Medicine and Health Sciences, Medical Personnel, 030212 general & internal medicine, Human Families, lcsh:Science, Aged, 80 and over, Multidisciplinary, Rehabilitation, Palliative Care, Neurodegenerative Diseases, Qualitative Studies, Middle Aged, Home Care Services, Professions, Neurology, Research Design, Female, Psychology, Research Article, Adult, Multiple Sclerosis, Drug Research and Development, Patients, Immunology, Research and Analysis Methods, Autoimmune Diseases, 03 medical and health sciences, Nursing, Physicians, Intervention (counseling), medicine, Humans, Clinical Trials, Aged, Pharmacology, lcsh:R, Biology and Life Sciences, Demyelinating Disorders, Focus group, Randomized Controlled Trials, Health Care, People and Places, Population Groupings, Clinical Immunology, lcsh:Q, Clinical Medicine, 030217 neurology & neurosurgery, Qualitative research
Abstract

Background We performed a qualitative study to investigate the experiences of participants in a multicentre randomized controlled trial on a home-based palliative approach (HPA) for adults with severe multiple sclerosis (MS) and their caregivers. Our aim was to explore the strengths and challenges of the intervention, and circumstances that may have influenced its efficacy. Methods Participants to the qualitative study were the patients, their caregivers, patient referring physicians, and the teams who delivered the HPA intervention. We performed semi-structured one-on-one interviews with 12 patients and 15 informal caregivers chosen using a maximum variation strategy, two focus group meetings with patient referring physicians (4 participants each), and one with the HPA teams (9 participants). Results From data analysis (framework method) 38 sub-categories emerged, which were grouped into 10 categories and 3 themes: 'expectations,' 'met and unmet needs', and 'barriers’. Intervention benefits were improved control of symptoms and reduced sense of isolation of the patient-caregiver dyads. Limitations were: factors related to experimental design (difficulty of dyads in identifying examiner and team roles, additional burden for caregivers); team issues (insufficient team building /supervision, competing priorities); limitations of the intervention itself (insufficient length, lack of rehabilitation input); and external factors (resource limitations, under-responsive services/professionals). The referring physician focus groups provided little experiential data. Conclusions The HPA reduced patient symptoms and sense of isolation in patients and caregivers. The indirect role of the HPA teams, and insufficient length of the intervention were key limitations. The experimental design imposed additional burdens on the dyads. Key barriers were the paucity of available services, the demanding administrative procedures, and lack of networking facilities. These findings suggest that two major requirements are necessary for home palliative care to be effective in this patient population: HPA teams well-connected with MS rehabilitation services, and care delivered over the long-term, with variable intensity. Trial registration Current Controlled Trials ISRCTN73082124 (Registered 19/06/2014).

Published
2018

67. Management of psychogenic nonepileptic seizures (PNES): a multidisciplinary approach

Author

Gasparini S 1, 2, Beghi E 3, Ferlazzo E 1, 4, Beghi M 5, Belcastro V 6, Biermann KP 7, Bottini G 8, Capovilla G 9, Cervellione RA 10, Cianci V 2, Coppola G 11, Cornaggia CM 12, De Fazio P 13, De Masi S 7, De Sarro G 14, Elia M 15, Erba G 16, Fusco L 17, Gambardella A 1, Gentile V 18, Giallonardo AT 19, Guerrini R 20, Ingravallo F 22, Iudice A 23, Labate A 1, Lucenteforte E 21, Magaudda A 24, Mumoli L 1, Papagno C 25, Pesce GB 26, Pucci E 27, Ricci P 28, Romeo A 29, Quintas R 30, Sueri C 2, Vitaliti G 31, Zoia R 32, Aguglia U 1, and 33.

Subjects
EEG, conversion disorder, epilepsy
Abstract

BACKGROUND: The International League Against Epilepsy (ILAE) proposed a diagnostic scheme for psychogenic nonepileptic seizures (PNES). The debate on ethical aspects of the diagnostic procedures is ongoing, the treatment is not standardized, and management might differ according to the age groups. OBJECTIVE: To reach an expert and stakeholder consensus on PNES management. METHODS: A board comprising adult and child neurologists, neuropsychologists, psychiatrists, pharmacologists, experts in forensic medicine and bioethics as well as patients' representatives was formed. The board chose five main topics regarding PNES: "diagnosis"; "ethical issues"; "psychiatric comorbidities"; "psychological treatment"; "pharmacological treatment". After a systematic review of the literature, the board met in a Consensus Conference in Catanzaro (Italy). Further consultations using the model of Delphi panel were held. RESULTS: The global level of evidence for all topics was low. Even though most questions were formulated separately for children/adolescents and adults, no major age-related differences emerged. The board established that the approach to PNES diagnosis should comply with ILAE recommendations. Seizures' induction was considered ethical, preferring the least invasive techniques. The board recommended: to carefully look for mood disturbances, personality disorders and psychic trauma in persons with PNES; to consider cognitive-behavioural therapy as first line psychological approach and pharmacological treatment to manage comorbid conditions, namely anxiety and depression. CONCLUSIONS: PNES management should be multidisciplinary. High-quality, long-term studies are needed to standardize PNES management. This article is protected by copyright. All rights reserved.

Published
2018
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68. Randomized controlled trial of a home-based palliative approach for people with severe multiple sclerosis

Author

Solari, A., Giordano, A., Patti, F., Grasso, M. G., Confalonieri, P., Palmisano, L., Ponzio, M., Borreani, C., Rosato, R., Veronese, S., Zaratin, P., Battaglia, M. A., Amadeo, R., Lugaresi, A., Martino, G., Pagano, E., Radice, D., Farinotti, M., Ferrari, G., Oliver, D. J., Pucci, E., Tesio, L., Pietrolongo, E., Giuntoli, M., Fittipaldo, A., Cugno, C., Causarano, R., Morino, P., Campanella, A., Mantegazza, R., Tucci, L., Ippoliti, F., Morone, G., Fusco, A., Cascio, V., Cimino, V., Zagari, F., Lopes de Carvalho, M. L., Motta, R., Onofrj, M., Da Col, D., and Casale, G.

Subjects
Male, medicine.medical_specialty, caregivers, symptom burden, Palliative care, Aftercare, Severity of Illness Index, law.invention, Multiple sclerosis, 03 medical and health sciences, 0302 clinical medicine, Quality of life (healthcare), Randomized controlled trial, law, Activities of Daily Living, medicine, Humans, 030212 general & internal medicine, palliative care, quality of life, randomized controlled trial, Aged, business.industry, Symptom burden, Middle Aged, medicine.disease, Home based, Home Care Services, Treatment Outcome, Neurology, Italy, Multivariate Analysis, Physical therapy, Disease Progression, Female, Neurology (clinical), Homebound Persons, business, Original Research Papers, 030217 neurology & neurosurgery
Abstract

Background: Evidence on the efficacy of palliative care in persons with severe multiple sclerosis (MS) is scarce. Objective: To assess the efficacy of a home-based palliative approach (HPA) for adults with severe MS and their carers. Methods: Adults with severe MS-carer dyads were assigned (2:1 ratio) to either HPA or usual care (UC). At each center, a multi-professional team delivered the 6-month intervention. A blind examiner assessed dyads at baseline, 3 months, and 6 months. Primary outcome measures were Palliative care Outcome Scale-Symptoms-MS (POS-S-MS) and Schedule for the Evaluation of Individual Quality of Life-Direct Weighting (SEIQoL-DW, not assessed in severely cognitively compromised patients). Results: Of 78 dyads randomized, 76 (50 HPA, 26 UC) were analyzed. Symptom burden (POS-S-MS) significantly reduced in HPA group compared to UC ( p = 0.047). Effect size was 0.20 at 3 months and 0.32 at 6 months, and statistical significance was borderline in per-protocol analysis ( p = 0.062). Changes in SEIQoL-DW index did not differ in the two groups, as changes in secondary patient and carer outcomes. Conclusion: HPA slightly reduced symptoms burden. We found no evidence of HPA efficacy on patient quality of life and on secondary outcomes.

Published
2018

70. Contributors

Author

Albrecht, D., primary, Angeleri, F., additional, Arcelli, P., additional, Asanuma, C., additional, Avanzini, G., additional, Bal, T., additional, Battaglia, G., additional, Belardinelli, N., additional, Bentivoglio, M., additional, Bertini, G., additional, Burman, K., additional, Campbell, G., additional, Casas-Puig, R., additional, Chen, S., additional, Colacitti, C., additional, Contreras, D., additional, Crunelli, V., additional, Ralston, D. Daly, additional, Darian-Smith, C., additional, Darian-Smith, I., additional, Davidowa, H., additional, De Biasi, S., additional, DeBoom, T., additional, De Curtis, M., additional, Dell'Anna, M.E., additional, Diamond, I.T., additional, Diamond, M.E., additional, Fenelon, G., additional, Fitzpatrick, D., additional, Françis, C., additional, Frassoni, C., additional, Frost, S.B., additional, Futami, T., additional, Galea, M., additional, Gambetti, P., additional, Giannetti, S., additional, Granato, A., additional, Hendry, S.H.C., additional, Humphrey, A.L., additional, Ilinsky, I.A., additional, Jones, E.G., additional, Kakei, S., additional, Killackey, H.P., additional, Kultas-Ilinsky, K., additional, Leggio, M.G., additional, Leresche, N., additional, Lieberman, A.R., additional, Lizier, C., additional, Lugaresi, E., additional, Luppino, G., additional, Macchi, G., additional, Mancia, M., additional, Marini, G., additional, Masterton, R.B., additional, Matelli, M., additional, McCormick, D.A., additional, Meder, J.F., additional, Minciacchi, D., additional, Molinari, M., additional, Montagna, P., additional, Nolfe, G., additional, Peng, Z.-C., additional, Percheron, G., additional, Persson, H., additional, Pucci, E., additional, Quattrini, A., additional, Ralston, H.J., additional, Rausell, E., additional, Regondi, M.C., additional, Reinoso-Suarez, F., additional, Ringstedt, T., additional, Rustioni, A., additional, Salt, T.E., additional, Santarelli, M., additional, Saul, A.B., additional, Sbriccoli, A., additional, Sherman, S.M., additional, Shinoda, Y., additional, Signorino, M., additional, Soltesz, I., additional, Spreafico, R., additional, Steriade, M., additional, Sugiuchi, Y., additional, Talbi, B., additional, Tippayatorn, N., additional, Toga, A.W., additional, Toth, T.I., additional, Turner, J., additional, Usrey, W.M., additional, Vaudano, E., additional, Velayos, J.L., additional, von Krosigk, M., additional, Wannier, T., additional, Yelnik, J., additional, and Zippel, U., additional

Published
1993
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71. Natalizumab in pediatric multiple sclerosis: results of a cohort of 55 cases

Author

Ghezzi, A, Zaffaroni, M, Bianchi, A, Pozzilli, C, Prosperini, L, Borriello, G, Filippi, M, Moiola, L, Gerevini, S, Rocca, MA, Martinelli, V, Comi, G, Grimaldi, LM, Bucello, S, Lus, G, Rinaldi, F, Gallo, P, Trojano, M, Provinciali, L, Pucci, E, Bortolon, F, Capra, R, Coniglio, G, Gasperini, C, Lugaresi, A, Pietrolongo, E, Farina, D, Di Ioia, M, Milani, N, Rottoli, MR, Sarchielli, P., BRESCIA MORRA, VINCENZO, LANZILLO, ROBERTA, Ghezzi, A, Zaffaroni, M, Bianchi, A, Pozzilli, C, Prosperini, L, Borriello, G, Filippi, M, Moiola, L, Gerevini, S, Rocca, Ma, Martinelli, V, Comi, G, BRESCIA MORRA, Vincenzo, Lanzillo, Roberta, Grimaldi, Lm, Bucello, S, Lus, G, Rinaldi, F, Gallo, P, Trojano, M, Provinciali, L, Pucci, E, Bortolon, F, Capra, R, Coniglio, G, Gasperini, C, Lugaresi, A, Pietrolongo, E, Farina, D, Di Ioia, M, Milani, N, Rottoli, Mr, Sarchielli, P., Brescia Morra, V, Comi, Giancarlo, Filippi, Massimo, Italian MS Study, Group, Ghezzi A, Pozzilli C, Grimaldi L, Moiola L, Brescia-Morra V, Lugaresi A, Lus G, Rinaldi F, Rocca M, Trojano M, Bianchi A, Comi G, Filippi M, the Italian MS Study Group, and Lus, Giacomo

Subjects
Male, medicine.medical_specialty, Pediatrics, Adolescent, Antibodies, Monoclonal, Humanized, adolescence, childhood, Multiple sclerosis, natalizumab, Brain, Child, Cohort Studies, Female, Humans, Magnetic Resonance Imaging, Multiple Sclerosis, Relapsing-Remitting, Natalizumab, Neurology, Neurology (clinical), Female patient, Medicine, Multiple sclerosi, Cognitive skill, Expanded Disability Status Scale, medicine.diagnostic_test, business.industry, Magnetic resonance imaging, Mean age, medicine.disease, Surgery, Cohort, business, medicine.drug
Abstract

Background: Limited information is available on the use of natalizumab (NA) in pediatric multiple sclerosis (ped-MS) patients. Objective: The purpose of this study was to describe the long-term effects of NA in a large cohort of active ped-MS patients. Methods: Patients with definite ped-MS were treated with NA if in the previous year they had experienced at least two relapses or a severe relapse with incomplete recovery while on immunomodulating treatment, or at least two relapses and new magnetic resonance imaging (MRI) lesions regardless of any prior treatment. Results: The study included 55 patients (mean age: 14.4 years, mean number of relapses: 4.4, pre-treatment mean disease duration: 25.5 months). They received a median number of 26 infusions. Three relapses occurred during the follow-up, one female patient continued to deteriorate in cognitive functioning. Mean Expanded Disability Status Scale (EDSS) scores decreased from 2.7 to 1.9 at the last visit ( pConclusions: NA was well tolerated in all patients. A strong suppression of disease activity was observed in the majority of patients during the follow-up.

Published
2013

72. Fully-metallic, Low-dispersive, Leaky-wave Fed Lens Antenna for 60 GHz Base Station Applications

Author

Dahlberg, Oskar, Pucci, E., Wang, L., Quevedo-Teruel, Oscar, Dahlberg, Oskar, Pucci, E., Wang, L., and Quevedo-Teruel, Oscar

Abstract

The guiding structure commonly employed in leaky-wave antennas is dispersive, resulting in beam-steering with frequency. This behavior reduces operational bandwidth in point-to-point communication applications. In this work, we present an approach that aims at increasing the operational bandwidth of leaky-wave antennas by the employment of a metasur-face lens., QC 20190121

Published
2018
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73. Anti-inflammatory disease-modifying treatment and disability progression in primary progressive multiple sclerosis: a cohort study.

Author

UCL - SSS/IONS/CEMO - Pôle Cellulaire et moléculaire, Lorscheider, J, Kuhle, J, Izquierdo, G, Lugaresi, A, Havrdova, E, Horakova, D, Hupperts, R, Duquette, P, Girard, M, Prat, A, Grand'Maison, F, Grammond, P, Sola, P, Ferraro, D, Trojano, M, Ramo-Tello, C, Lechner-Scott, J, Pucci, E, Solaro, C, Slee, M, Van Pesch, Vincent, Sanchez Menoyo, J L, van der Walt, A, Butzkueven, H, Kappos, L, Kalincik, T, MSBase Study Group, UCL - SSS/IONS/CEMO - Pôle Cellulaire et moléculaire, Lorscheider, J, Kuhle, J, Izquierdo, G, Lugaresi, A, Havrdova, E, Horakova, D, Hupperts, R, Duquette, P, Girard, M, Prat, A, Grand'Maison, F, Grammond, P, Sola, P, Ferraro, D, Trojano, M, Ramo-Tello, C, Lechner-Scott, J, Pucci, E, Solaro, C, Slee, M, Van Pesch, Vincent, Sanchez Menoyo, J L, van der Walt, A, Butzkueven, H, Kappos, L, Kalincik, T, and MSBase Study Group

Abstract

Treatment options in primary progressive multiple sclerosis (PPMS) are scarce and, with the exception of ocrelizumab, anti-inflammatory agents have failed to show efficacy in ameliorating disability progression. The aim of this study was to investigate a potential effect of anti-inflammatory disease-modifying treatment on disability outcomes in PPMS. Using MSBase, a large, international, observational database, we identified patients with PPMS who were either never treated or treated with a disease-modifying agent. Propensity score matching was used to select subpopulations with similar baseline characteristics. Expanded Disability Status Scale (EDSS) outcomes were compared with an intention-to-treat and an as-treated approach in paired, pairwise-censored analyses. Of the 1284 included patients, 533 were matched (treated, n = 195; untreated n = 338). Median on-study pairwise-censored follow-up was 3.4 years (quartiles 1.2-5.5). No difference in the hazard of experiencing 3-month confirmed EDSS progression events was observed between the groups [hazard ratio (HR), 1.0; 95% confidence interval (CI), 0.6-1.7, P = 0.87]. We did not find significant differences in the hazards of confirmed EDSS improvement (HR, 1.0; 95% CI, 0.6-1.6, P = 0.91) or reaching a confirmed EDSS step ≥7 (HR, 1.1; 95% CI, 0.7-1.6, P = 0.69). Our pooled analysis of disease-modifying agents suggests that these therapies have no substantial effect on short- to medium-term disability outcomes in PPMS.

Published
2018

75. Long-term disability trajectories in primary progressive MS patients: A latent class growth analysis

Author

Signori, A, Izquierdo, G, Lugaresi, A, Hupperts, R, Grand'Maison, F, Sola, P, Horakova, D, Havrdova, E, Prat, A, Girard, M, Duquette, P, Boz, C, Grammond, P, Terzi, M, Singhal, B, Alroughani, R, Petersen, T, Ramo, C, Oreja-Guevara, C, Spitaleri, D, Shaygannejad, V, Butzkueven, H, Kalincik, T, Jokubaitis, V, Slee, M, Fernandez Bolanos, R, Luis Sanchez-Menoyo, J, Pucci, E, Granella, F, Lechner-Scott, J, Iuliano, G, Hughes, S, Bergamaschi, R, Taylor, B, Verheul, F, Rio, ME, Amato, MP, Sajedi, SA, Majdinasab, N, Van Pesch, V, Sormani, MP, Trojano, M, Signori, A, Izquierdo, G, Lugaresi, A, Hupperts, R, Grand'Maison, F, Sola, P, Horakova, D, Havrdova, E, Prat, A, Girard, M, Duquette, P, Boz, C, Grammond, P, Terzi, M, Singhal, B, Alroughani, R, Petersen, T, Ramo, C, Oreja-Guevara, C, Spitaleri, D, Shaygannejad, V, Butzkueven, H, Kalincik, T, Jokubaitis, V, Slee, M, Fernandez Bolanos, R, Luis Sanchez-Menoyo, J, Pucci, E, Granella, F, Lechner-Scott, J, Iuliano, G, Hughes, S, Bergamaschi, R, Taylor, B, Verheul, F, Rio, ME, Amato, MP, Sajedi, SA, Majdinasab, N, Van Pesch, V, Sormani, MP, and Trojano, M

Abstract

BACKGROUND: Several natural history studies on primary progressive multiple sclerosis (PPMS) patients detected a consistent heterogeneity in the rate of disability accumulation. OBJECTIVES: To identify subgroups of PPMS patients with similar longitudinal trajectories of Expanded Disability Status Scale (EDSS) over time. METHODS: All PPMS patients collected within the MSBase registry, who had their first EDSS assessment within 5 years from onset, were included in the analysis. Longitudinal EDSS scores were modeled by a latent class mixed model (LCMM), using a nonlinear function of time from onset. LCMM is an advanced statistical approach that models heterogeneity between patients by classifying them into unobserved groups showing similar characteristics. RESULTS: A total of 853 PPMS (51.7% females) from 24 countries with a mean age at onset of 42.4 years (standard deviation (SD): 10.8 years), a median baseline EDSS of 4 (interquartile range (IQR): 2.5-5.5), and 2.4 years of disease duration (SD: 1.5 years) were included. LCMM detected three different subgroups of patients with a mild ( n = 143; 16.8%), moderate ( n = 378; 44.3%), or severe ( n = 332; 38.9%) disability trajectory. The probability of reaching EDSS 6 at 10 years was 0%, 46.4%, and 81.9% respectively. CONCLUSION: Applying an LCMM modeling approach to long-term EDSS data, it is possible to identify groups of PPMS patients with different prognosis.

Published
2018

76. No evidence of disease activity (NEDA-3) and disability improvement after alemtuzumab treatment for multiple sclerosis: a 36-month real-world study

Author

Prosperini, L., Annovazzi, P., Boffa, L., Buscarinu, M. C., Gallo, A., Matta, M., Moiola, L., Musu, L., Perini, P., Avolio, C., Barcella, V., Bianco, Assunta, Farina, D., Ferraro, E., Pontecorvo, S., Granella, F., Grimaldi, L. M. E., Laroni, A., Lus, G., Patti, F., Pucci, E., Pasca, M., Sarchielli, P., Ghezzi, A., Zaffaroni, M., Baroncini, D., Buttari, F., Centonze, D., Fornasiero, A., Salvetti, M., Docimo, R., Signoriello, E., Tedeschi, G., Bertolotto, A., Capobianco, M., Comi, G., Cocco, E., Gallo, P., Puthenparampil, M., Grasso, R., Di Francescantonio, V., Rottoli, M. R., Mirabella, Massimiliano, Lugaresi, A., De Luca, G., Di Ioia, M., Di Tommaso, V., Mancinelli, L., Di Battista, G., Francia, A., Ruggieri, S., Pozzilli, C., Curti, E., Tsantes, E., Palmeri, B., Lapicci, C., Mancardi, G. L., Uccelli, A., Chisari, C., D'Amico, E., Cartechini, E., Repice, A. M., Magnani, E., Massaccesi, L., Calabresi, Paolo, Di Filippo, Mario, Di Gregorio, M., Bianco A., Mirabella M. (ORCID:0000-0002-7783-114X), Calabresi P. (ORCID:0000-0003-0326-5509), Di Filippo M., Prosperini, L., Annovazzi, P., Boffa, L., Buscarinu, M. C., Gallo, A., Matta, M., Moiola, L., Musu, L., Perini, P., Avolio, C., Barcella, V., Bianco, Assunta, Farina, D., Ferraro, E., Pontecorvo, S., Granella, F., Grimaldi, L. M. E., Laroni, A., Lus, G., Patti, F., Pucci, E., Pasca, M., Sarchielli, P., Ghezzi, A., Zaffaroni, M., Baroncini, D., Buttari, F., Centonze, D., Fornasiero, A., Salvetti, M., Docimo, R., Signoriello, E., Tedeschi, G., Bertolotto, A., Capobianco, M., Comi, G., Cocco, E., Gallo, P., Puthenparampil, M., Grasso, R., Di Francescantonio, V., Rottoli, M. R., Mirabella, Massimiliano, Lugaresi, A., De Luca, G., Di Ioia, M., Di Tommaso, V., Mancinelli, L., Di Battista, G., Francia, A., Ruggieri, S., Pozzilli, C., Curti, E., Tsantes, E., Palmeri, B., Lapicci, C., Mancardi, G. L., Uccelli, A., Chisari, C., D'Amico, E., Cartechini, E., Repice, A. M., Magnani, E., Massaccesi, L., Calabresi, Paolo, Di Filippo, Mario, Di Gregorio, M., Bianco A., Mirabella M. (ORCID:0000-0002-7783-114X), Calabresi P. (ORCID:0000-0003-0326-5509), and Di Filippo M.

Abstract

In this retrospective, multicenter, real-world study we collected clinical and magnetic resonance imaging (MRI) data of all patients (n = 40) with relapsing-remitting multiple sclerosis (RRMS) treated with alemtuzumab according to a “free-of-charge” protocol available before the drug marketing approval in Italy. Almost all (39/40) started alemtuzumab after discontinuing multiple disease-modifying treatments (DMTs) because of either lack of response or safety concerns. We considered the proportion of alemtuzumab-treated patients who had no evidence of disease activity (NEDA-3) and disability improvement over a 36-month follow-up period. NEDA-3 was defined as absence of relapses, disability worsening, and MRI activity. Disability improvement was defined as a sustained reduction of ≥ 1-point in Expanded Disability Status Scale (EDSS) score. At follow-up, 18 (45%) patients achieved NEDA-3, 30 (75%) were relapse-free, 33 (82.5%) were EDSS worsening-free, and 25 (62.5%) were MRI activity-free. Eleven (27.5%) patients had a sustained disability improvement. We found no predictor for the NEDA-3 status, while the interaction of higher EDSS score by higher number of pre-alemtuzumab relapses was associated with a greater chance of disability improvement (odds ratio 1.10, p = 0.049). Our study provides real-world evidence that alemtuzumab can promote clinical and MRI disease remission, as well as disability improvement, in a significant proportion of patients with RRMS despite prior multiple DMT failures. The drug safety profile was consistent with data available from clinical trials.

Published
2018

77. Effectiveness of fingolimod, dimethyl fumarate and teriflunomide in relapsing-remitting multiple sclerosis: a comparative longitudinal study

Author

Kalincik, T., Spelman, T., Jokubaitis, V., Horakova, D., Havrdova, E., Izquierdo, G., Prat, A., Girard, M., Duquette, P., Lugaresi, A., Grammond, P., Alroughani, R., Lechner-Scott, J., Prevost, J., Terzi, M., Grand Maison, F., Boz, C., Trojano, M., Wijmeersch, B., Pucci, E., Granella, F., Recai Turkoglu, Sola, P., Ferraro, D., Mccombe, P., Solaro, C., Pesch, V., Ozakbas, S., Slee, M., Spitaleri, D., Sanchez-Menoyo, J. L., Ampapa, R., Hodgkinson, S., Karabudak, R., Vucic, S., and Butzkueven, H.

Published
2017

78. Prognostic value of MRI activity in treatment failure

Author

Grammond, P., Alroughani, R., Sola, P., Ferraro, D., Ozakbas, S., Lugaresi, A., Lechner-Scott, J., Kalincik, T., Butzkueven, H., Sormani, M. P., Jokubaitis, V., Vucic, S., Spitaleri, D., Grand'Maison, F., Pucci, E., Boz, C., Van Wijmeersch, B., Sanchez-Menoyo, J. L., Trojano, M., Izquierdo, G., Kunchok, A. C., and Granella, F.

Published
2017

79. Timing of high-efficacy disease modifying therapies for relapsing-remitting multiple sclerosis

Author

Merkel, B., Jokubaitis, V., Spelman, T., Horakova, D., Havrdova, E., Trojano, M., Izquierdo, G., Lugaresi, A., Prat, A., Girard, M., Duquette, P., Sola, P., Ferraro, D., Grammond, P., Hupperts, R., Bergamaschi, R., Alroughani, R., Boz, C., Terzi, M., Pucci, E., Pesch, V., Grand Maison, F., Fernandez-Bolanos, R., Lechner-Scott, J., Spitaleri, D., Shaygannejad, V., Iuliano, G., Granella, F., Solaro, C., Prevost, J., Petersen, T., Olascoaga, J., Cristina Ramo-Tello, Verheul, F., Mccombe, P., Slee, M., Sanchez-Menoyo, J. L., Cristiano, E., Ozakbas, S., Saladino, M. L., Ampapa, R., Vucic, S., Moore, F., Deri, N., Alkhaboori, J., Barnett, M., Walt, A., Butzkueven, H., and Kalincik, T.

Published
2017

80. Disease modifying therapy improves disability outcomes in relapsing-remitting multiple sclerosis over 22 years

Author

Kalincik, T., Spelman, T., Jokubaitis, V., Horakova, D., Havrdova, E., Trojano, M., Pucci, E., and Ondokuz Mayıs Üniversitesi

Abstract

7th Joint European-Committee-for-Treatment-and-Research-in-Multiple-Sclerosis (ECTRIMS)-Americas-Committee-for-Treatment-and-Research-in-Multiple-Sclerosis (ACTRIMS) -- OCT 25-28, 2017 -- Paris, FRANCE Ramo-Tello, Cristina M/0000-0001-8643-5053; Ferraro, Diana/0000-0003-4818-3806; Lugaresi, Alessandra/0000-0003-2902-5589; WOS: 000413730202120 … European Comm Treatment & Res Multiple Sclerosis, Americas Comm Treatment & Res Multiple Sclerosis BiogenBiogen; MerckMerck & Company; Teva; NovartisNovartis; Charles University in Prague [PRVOUK-P26/LF1/4]; Czech Ministry of HealthMinistry of Health, Czech Republic [NT13237-4/2012]; Actelion; Celgene; RocheRoche Holding; SanofiSanofi-Aventis; Czech Ministry of EducationMinistry of Education, Youth & Sports - Czech Republic [Q27/LF1]; Biogen-IdecBiogen; Biogen IdecBiogen; Sanofi Genzyme; BayerBayer AG; Sanofi-Genzyme; Fondazione Italiana Sclerosi Multipla (FISM)Fondazione Italiana Sclerosi Multipla (FISM); Almirall; Bayer ScheringBayer AG; Sanofi-AventisSanofi-Aventis; GenzymeGenzyme Corporation; Teva-Neuroscience; Canadian Multiple sclerosis society; Mitsubishi; ONO Pharmaceuticals; Teva Canada Innovation; Genzyme SanofiGenzyme Corporation; EMD; Canadian Institutes of Health ResearchCanadian Institutes of Health Research (CIHR); CIHRCanadian Institutes of Health Research (CIHR); MS Society of Canada; Sanofi AventisSanofi-Aventis; Bayer-ScheringBayer AG; Novartis Pharma; UCBUCB Pharma SA; LundbeckLundbeck Corporation; Associazione Marchigiana Sclerosi Multipla e altre malattie neurologiche Dana Horakova received speaker honoraria and consulting fees from Biogen, Merck, Teva and Novartis, as well as support for research activities from Biogen and research grants from Charles University in Prague (PRVOUK-P26/LF1/4 and Czech Ministry of Health (NT13237-4/2012).; Eva Havrdova received speaker honoraria and consultant fees from Actelion, Biogen, Celgene, Merck, Novartis, Roche, Sanofi and Teva, and support for research activities from Czech Ministry of Education, project Progres Q27/LF1.; Maria Trojano received speaker honoraria from Biogen-Idec, Bayer-Schering, Sanofi Aventis, Merck, Teva, Novartis and Almirall; has received research grants for her Institution from Biogen-Idec, Merck, and Novartis.; Patrizia Sola served on scientific advisory boards for Biogen Idec and TEVA, she has received funding for travel and speaker honoraria from Biogen Idec, Merck, Teva, Sanofi Genzyme, Novartis and Bayer and research grants for her Institution from Bayer, Biogen, Merck, Novartis, Sanofi, Teva.; Diana Ferraro received travel grants and/or speaker honoraria from Merck, TEVA, Novartis, Biogen and Sanofi-Genzyme.; Alessandra Lugaresi is a Bayer, Biogen, Genzyme, Merck Advisory Board Member. She received travel grants and honoraria from Bayer, Biogen, Merck, Novartis, Sanofi, Teva and Fondazione Italiana Sclerosi Multipla (FISM). Her institution received research grants from Bayer, Biogen, Merck, Novartis, Sanofi, Teva and Fondazione Italiana Sclerosi Multipla (FISM). Guillermo Izquierdo received speaking honoraria from Biogen, Novartis, Sanofi, Merck and Teva.; Franco Granella served on scientific advisory boards for Biogen Idec, Novartis and Sanofi Aventis and received funding for travel and speaker honoraria from Biogen Idec, Merck, and Almirall.; Roberto Bergamaschi received speaker honoraria from Bayer Schering, Biogen, Genzyme, Merck, Novartis, Sanofi-Aventis, Teva; research grants from Bayer Schering, Biogen, Merck, Novartis, Sanofi-Aventis, Teva; congress and travel/accommodation expense compensations by Almirall, Bayer Schering, Biogen, Genzyme, Merck, Novartis, Sanofi-Aventis, Teva.; Helmut Butzkueven served on scientific advisory boards for Biogen, Novartis and Sanofi-Aventis and has received conference travel support from Novartis, Biogen and Sanofi Aventis. He serves on steering committees for trials conducted by Biogen and Novartis, and has received research support from Merck, Novartis and Biogen.; Tomas Kalincik served on scientific advisory boards for Roche, Genzyme-Sanofi, Novartis, Merck and Biogen, steering committee for Brain Atrophy Initiative by Genzyme, received conference travel support and/or speaker honoraria from WebMD Global, Novartis, Biogen, Genzyme-Sanofi, Teva, BioCSL and Merck and received research support from Biogen.; Pierre Grammond is a Merck, Novartis, Teva-neuroscience, Biogen and Genzyme advisory board member, consultant for Merck, received payments for lectures by Merck, Teva-Neuroscience and Canadian Multiple sclerosis society, and received grants for travel from Teva-Neuroscience and Novartis.; Raymond Hupperts received honoraria as consultant on scientific advisory boards from Merck, Biogen, Genzyme-Sanofi and Teva, research funding from Merck and Biogen, and speaker honoraria from Sanofi-Genzyme and Novartis.; Francois Grand'Maison received honoraria or research funding from Biogen, Genzyme, Novartis, Teva Neurosciences, Mitsubishi and ONO Pharmaceuticals.; Marc Girard received consulting fees from Teva Canada Innovation, Biogen, Novartis and Genzyme Sanofi; lecture payments from Teva Canada Innovation, Novartis and EMD. He has also received a research grant from Canadian Institutes of Health Research.; Pierre Duquette served on editorial boards and has been supported to attend meetings by EMD, Biogen, Novartis, Genzyme, and TEVA Neuroscience. He holds grants from the CIHR and the MS Society of Canada and has received funding for investigator-initiated trials from Biogen, Novartis, and Genzyme.; Daniele Spitaleri received honoraria as a consultant on scientific advisory boards by Bayer- Schering, Novartis and Sanofi-Aventis and compensation for travel from Novartis, Biogen, Sanofi Aventis, Teva and Merck.; Murat Terzi received travel grants from Merck, Novartis, Bayer-Schering, Merck and Teva; has participated in clinical trials by Sanofi Aventis, Roche and Novartis.; Vincent Van Pesch received travel grants from Biogen, Bayer Schering, Genzyme, Merck, Teva and Novartis Pharma. His institution receives honoraria for consultancy and lectures from Biogen, Bayer Schering, Genzyme, Merck, Roche, Teva and Novartis Pharma as well as research grants from Novartis Pharma and Bayer Schering.; Eugenio Pucci served on scientific advisory boards for Merck, Genzyme and Biogen; he has received honoraria and travel grants from Sanofi Aventis, UCB, Lundbeck, Novartis, Bayer Schering, Biogen, Merck, Genzyme and Teva; he has received travel grants and equipment from "Associazione Marchigiana Sclerosi Multipla e altre malattie neurologiche".; Gerardo Iuliano had travel/accommodations/meeting expenses funded by Bayer Schering, Biogen, Merck, Novartis, Sanofi Aventis, and Teva.; Helmut Butzkueven served on scientific advisory boards for Biogen, Novartis and Sanofi-Aventis and has received conference travel support from Novartis, Biogen and Sanofi Aventis. He serves on steering committees for trials conducted by Biogen and Novartis, and has received research support from Merck, Novartis and Biogen.; Thor Petersen received funding or speaker honoraria from Biogen, Merck, Novartis, Bayer Schering, Sanofi-Aventis, Roche, and Genzyme.; Julie Prevost accepted travel compensation from Novartis, Biogen, Genzyme, Teva, and speaking honoraria from Biogen, Novartis, Genzyme and Teva.; Fraser Moore participated in clinical trials sponsored by EMD and Novartis.; Tatjana Petkovska-Boskova received congress and travel expense compensations from Biogen Idec and Teva.; Cristina Ramo-Tello received research funding, compensation for travel or speaker honoraria from Biogen, Novartis, Genzyme and Almirall.

Published
2017

81. Contribution of inflammation to disability accrual in primary progressive multiple sclerosis

Author

Hughes, J, Jokubaitis, V, Spelman, T, Lugaresi, A, Hupperts, R, Izquierdo, G, Prat, A, Girard, M, Duquette, P, Grand'Maison, F, Grammond, P, Sola, P, Ferraro, D, Ramo, C, Trojano, M, Slee, M, Shaygannejad, V, Boz, C, Lechner-Scott, J, Van Pesch, V, Pucci, E, Solaro, C, Verheul, F, Terzi, M, Granella, F, Spitaleri, D, Alroughani, R, van der Walt, A, Butzkueven, H, and Kalincik, T

Published
2017

82. Clausola di coscienza e cura nell’assistenza al fine vita

Author

De Panfilis, L, Cattaneo, D, Cola, L, Gasparini, M, Porteri, C, Tarquini, D, Tiezzi, A, Veronese, S, Zullo, S, Pucci, E, per il Gruppo di Studio in Bioetica, e Cure Palliative della Società Italiana di Neurologia, Alberti, F, Belardinelli, N, Bologna, F, Borasio, Gd, Caraceni, A, Causarano, Ir, Colombi, L, Congedo, M, Conte, A, Crespi, V, Defanti, Ca, Gasperini, M, Giordano, A, Inghilleri, M, Ingravallo, F, Lugaresi, A, Mandrioli, J, Marogna, M, Maschio, M, Mori, M, Neri, W, Moretto, G, Nichelli, P, Pace, A, Pietrolongo, E, Pistollato, L, Primavera, A, Solari, A, Solaro, C, and Tola, Mr

Published
2017

83. Management of psychogenic non‐epileptic seizures: a multidisciplinary approach

Author

Gasparini, S., primary, Beghi, E., additional, Ferlazzo, E., additional, Beghi, M., additional, Belcastro, V., additional, Biermann, K. P., additional, Bottini, G., additional, Capovilla, G., additional, Cervellione, R. A., additional, Cianci, V., additional, Coppola, G., additional, Cornaggia, C. M., additional, De Fazio, P., additional, De Masi, S., additional, De Sarro, G., additional, Elia, M., additional, Erba, G., additional, Fusco, L., additional, Gambardella, A., additional, Gentile, V., additional, Giallonardo, A. T., additional, Guerrini, R., additional, Ingravallo, F., additional, Iudice, A., additional, Labate, A., additional, Lucenteforte, E., additional, Magaudda, A., additional, Mumoli, L., additional, Papagno, C., additional, Pesce, G. B., additional, Pucci, E., additional, Ricci, P., additional, Romeo, A., additional, Quintas, R., additional, Sueri, C., additional, Vitaliti, G., additional, Zoia, R., additional, and Aguglia, U., additional

Published
2018
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86. Contribution of different relapse phenotypes to disability in multiple sclerosis

Author

Stewart, T., Spelman, T., Havrdova, E., Horakova, D., Trojano, M., Izquierdo, G., Duquette, P., Girard, M., Prat, A., Lugaresi, A., Grand’Maison, F., Grammond, P., Sola, P., Shaygannejad, V., Hupperts, R., Alroughani, R., Oreja-Guevara, C., Pucci, E., Boz, C., Lechner-Scott, J., Bergamaschi, R., van Pesch, V., Iuliano, G., Ramo, C., Taylor, B., Slee, M., Spitaleri, D., Granella, F., Verheul, F., McCombe, P., Hodgkinson, S., Amato, M.P., Vucic, S., Gray, O., Cristiano, E., Barnett, M., Sanchez Menoyo, J.L., van Munster, E., Saladino, M.L., Olascoaga, J., Prevost, J., Deri, N., Shaw, C., Singhal, B., Moore, F., Rózsa, C., Shuey, N., Skibina, O., Kister, I., Petkovska-Boskova, T., Ampapa, R., Kermode, A., Butzkueven, H., Jokubaitis, V., Kalincik, T., Stewart, T., Spelman, T., Havrdova, E., Horakova, D., Trojano, M., Izquierdo, G., Duquette, P., Girard, M., Prat, A., Lugaresi, A., Grand’Maison, F., Grammond, P., Sola, P., Shaygannejad, V., Hupperts, R., Alroughani, R., Oreja-Guevara, C., Pucci, E., Boz, C., Lechner-Scott, J., Bergamaschi, R., van Pesch, V., Iuliano, G., Ramo, C., Taylor, B., Slee, M., Spitaleri, D., Granella, F., Verheul, F., McCombe, P., Hodgkinson, S., Amato, M.P., Vucic, S., Gray, O., Cristiano, E., Barnett, M., Sanchez Menoyo, J.L., van Munster, E., Saladino, M.L., Olascoaga, J., Prevost, J., Deri, N., Shaw, C., Singhal, B., Moore, F., Rózsa, C., Shuey, N., Skibina, O., Kister, I., Petkovska-Boskova, T., Ampapa, R., Kermode, A., Butzkueven, H., Jokubaitis, V., and Kalincik, T.

Abstract

Objective: This study evaluated the effect of relapse phenotype on disability accumulation in multiple sclerosis. Methods: Analysis of prospectively collected data was conducted in 19,504 patients with relapse-onset multiple sclerosis and minimum 1-year prospective follow-up from the MSBase cohort study. Multivariable linear regression models assessed associations between relapse incidence, phenotype and changes in disability (quantified with Expanded Disability Status Scale and its Functional System scores). Sensitivity analyses were conducted. Results: In 34,858 relapses recorded during 136,462 patient-years (median follow-up 5.9 years), higher relapse incidence was associated with greater disability accumulation (β = 0.16, p < 0.001). Relapses of all phenotypes promoted disability accumulation, with the most pronounced increase associated with pyramidal (β = 0.27 (0.25–0.29)), cerebellar (β = 0.35 (0.30–0.39)) and bowel/bladder (β = 0.42 (0.35–0.49)) phenotypes (mean (95% confidence interval)). Higher incidence of each relapse phenotype was associated with an increase in disability in the corresponding neurological domain, as well as anatomically related domains. Conclusion: Relapses are associated with accumulation of neurological disability. Relapses in pyramidal, cerebellar and bowel/bladder systems have the greatest association with disability change. Therefore, prevention of these relapses is an important objective of disease-modifying therapy. The differential impact of relapse phenotypes on disability outcomes could influence management of treatment failure in multiple sclerosis.

Published
2017

87. Treatment effectiveness of alemtuzumab compared with natalizumab, fingolimod, and interferon beta in relapsing-remitting multiple sclerosis: a cohort study

Author

Kalincik, T, Brown, JWL, Robertson, N, Willis, M, Scolding, N, Rice, CM, Wilkins, A, Pearson, O, Ziemssen, T, Hutchinson, M, McGuigan, C, Jokubaitis, V, Spelman, T, Horakova, D, Havrdova, E, Trojano, M, Izquierdo, G, Lugaresi, A, Prat, A, Girard, M, Duquette, P, Grammond, P, Alroughani, R, Pucci, E, Sola, P, Hupperts, R, Lechner-Scott, J, Terzi, M, Van Pesch, V, Rozsa, C, Grand'Maison, F, Boz, C, Granella, F, Slee, M, Spitaleri, D, Olascoaga, J, Bergamaschi, R, Verheul, F, Vucic, S, McCombe, P, Hodgkinson, S, Sanchez-Menoyo, JL, Ampapa, R, Simo, M, Csepany, T, Ramo, C, Cristiano, E, Barnett, M, Butzkueven, H, Coles, A, Kalincik, T, Brown, JWL, Robertson, N, Willis, M, Scolding, N, Rice, CM, Wilkins, A, Pearson, O, Ziemssen, T, Hutchinson, M, McGuigan, C, Jokubaitis, V, Spelman, T, Horakova, D, Havrdova, E, Trojano, M, Izquierdo, G, Lugaresi, A, Prat, A, Girard, M, Duquette, P, Grammond, P, Alroughani, R, Pucci, E, Sola, P, Hupperts, R, Lechner-Scott, J, Terzi, M, Van Pesch, V, Rozsa, C, Grand'Maison, F, Boz, C, Granella, F, Slee, M, Spitaleri, D, Olascoaga, J, Bergamaschi, R, Verheul, F, Vucic, S, McCombe, P, Hodgkinson, S, Sanchez-Menoyo, JL, Ampapa, R, Simo, M, Csepany, T, Ramo, C, Cristiano, E, Barnett, M, Butzkueven, H, and Coles, A

Abstract

BACKGROUND: Alemtuzumab, an anti-CD52 antibody, is proven to be more efficacious than interferon beta-1a in the treatment of relapsing-remitting multiple sclerosis, but its efficacy relative to more potent immunotherapies is unknown. We compared the effectiveness of alemtuzumab with natalizumab, fingolimod, and interferon beta in patients with relapsing-remitting multiple sclerosis treated for up to 5 years. METHODS: In this international cohort study, we used data from propensity-matched patients with relapsing-remitting multiple sclerosis from the MSBase and six other cohorts. Longitudinal clinical data were obtained from 71 MSBase centres in 21 countries and from six non-MSBase centres in the UK and Germany between Nov 1, 2015, and June 30, 2016. Key inclusion criteria were a diagnosis of definite relapsing-remitting multiple sclerosis, exposure to one of the study therapies (alemtuzumab, interferon beta, fingolimod, or natalizumab), age 65 years or younger, Expanded Disability Status Scale (EDSS) score 6·5 or lower, and no more than 10 years since the first multiple sclerosis symptom. The primary endpoint was annualised relapse rate. The secondary endpoints were cumulative hazards of relapses, disability accumulation, and disability improvement events. We compared relapse rates with negative binomial models, and estimated cumulative hazards with conditional proportional hazards models. FINDINGS: Patients were treated between Aug 1, 1994, and June 30, 2016. The cohorts consisted of 189 patients given alemtuzumab, 2155 patients given interferon beta, 828 patients given fingolimod, and 1160 patients given natalizumab. Alemtuzumab was associated with a lower annualised relapse rate than interferon beta (0·19 [95% CI 0·14-0·23] vs 0·53 [0·46-0·61], p<0·0001) and fingolimod (0·15 [0·10-0·20] vs 0·34 [0·26-0·41], p<0·0001), and was associated with a similar annualised relapse rate as natalizumab (0·20 [0·14-0·26] vs 0·19 [0·15-0·23], p=0·78). For the disability outcome

Published
2017

88. Towards personalized therapy for multiple sclerosis: prediction of individual treatment response

Author

Kalincik, T, Manouchehrinia, A, Sobisek, L, Jokubaitis, V, Spelman, T, Horakova, D, Havrdova, E, Trojano, M, Izquierdo, G, Lugaresi, A, Girard, M, Prat, A, Duquette, P, Grammond, P, Sola, P, Hupperts, R, Grand'Maison, F, Pucci, E, Boz, C, Alroughani, R, Van Pesch, V, Lechner-Scott, J, Terzi, M, Bergamaschi, R, Iuliano, G, Granella, F, Spitaleri, D, Shaygannejad, V, Oreja-Guevara, C, Slee, M, Ampapa, R, Verheul, F, McCombe, P, Olascoaga, J, Amato, MP, Vucic, S, Hodgkinson, S, Ramo-Tello, C, Flechter, S, Cristiano, E, Rozsa, C, Moore, F, Luis Sanchez-Menoyo, J, Laura Saladino, M, Barnett, M, Hillert, J, Butzkueven, H, Kalincik, T, Manouchehrinia, A, Sobisek, L, Jokubaitis, V, Spelman, T, Horakova, D, Havrdova, E, Trojano, M, Izquierdo, G, Lugaresi, A, Girard, M, Prat, A, Duquette, P, Grammond, P, Sola, P, Hupperts, R, Grand'Maison, F, Pucci, E, Boz, C, Alroughani, R, Van Pesch, V, Lechner-Scott, J, Terzi, M, Bergamaschi, R, Iuliano, G, Granella, F, Spitaleri, D, Shaygannejad, V, Oreja-Guevara, C, Slee, M, Ampapa, R, Verheul, F, McCombe, P, Olascoaga, J, Amato, MP, Vucic, S, Hodgkinson, S, Ramo-Tello, C, Flechter, S, Cristiano, E, Rozsa, C, Moore, F, Luis Sanchez-Menoyo, J, Laura Saladino, M, Barnett, M, Hillert, J, and Butzkueven, H

Abstract

Timely initiation of effective therapy is crucial for preventing disability in multiple sclerosis; however, treatment response varies greatly among patients. Comprehensive predictive models of individual treatment response are lacking. Our aims were: (i) to develop predictive algorithms for individual treatment response using demographic, clinical and paraclinical predictors in patients with multiple sclerosis; and (ii) to evaluate accuracy, and internal and external validity of these algorithms. This study evaluated 27 demographic, clinical and paraclinical predictors of individual response to seven disease-modifying therapies in MSBase, a large global cohort study. Treatment response was analysed separately for disability progression, disability regression, relapse frequency, conversion to secondary progressive disease, change in the cumulative disease burden, and the probability of treatment discontinuation. Multivariable survival and generalized linear models were used, together with the principal component analysis to reduce model dimensionality and prevent overparameterization. Accuracy of the individual prediction was tested and its internal validity was evaluated in a separate, non-overlapping cohort. External validity was evaluated in a geographically distinct cohort, the Swedish Multiple Sclerosis Registry. In the training cohort (n = 8513), the most prominent modifiers of treatment response comprised age, disease duration, disease course, previous relapse activity, disability, predominant relapse phenotype and previous therapy. Importantly, the magnitude and direction of the associations varied among therapies and disease outcomes. Higher probability of disability progression during treatment with injectable therapies was predominantly associated with a greater disability at treatment start and the previous therapy. For fingolimod, natalizumab or mitoxantrone, it was mainly associated with lower pretreatment relapse activity. The probability of disability

Published
2017

89. Prognostic Indicators in Pediatric Clinically Isolated Syndrome

Author

Iaffaldano, P, Simone, M, Lucisano, G, Ghezzi, A, Coniglio, G, Morra, VB, Salemi, G, Patti, F, Lugaresi, A, Izquierdo, G, Bergamaschi, R, Cabrera-Gomez, JA, Pozzilli, C, Millefiorini, E, Alroughani, R, Boz, C, Pucci, E, Zimatore, GB, Sola, P, Lus, G, Maimone, D, Avolio, C, Cocco, E, Sajedi, SA, Costantino, G, Duquette, P, Shaygannejad, V, Petersen, T, Fernandez Bolanos, R, Paolicelli, D, Tortorella, C, Spelman, T, Margari, L, Amato, MP, Comi, G, Butzkueven, H, Trojano, M, Iaffaldano, P, Simone, M, Lucisano, G, Ghezzi, A, Coniglio, G, Morra, VB, Salemi, G, Patti, F, Lugaresi, A, Izquierdo, G, Bergamaschi, R, Cabrera-Gomez, JA, Pozzilli, C, Millefiorini, E, Alroughani, R, Boz, C, Pucci, E, Zimatore, GB, Sola, P, Lus, G, Maimone, D, Avolio, C, Cocco, E, Sajedi, SA, Costantino, G, Duquette, P, Shaygannejad, V, Petersen, T, Fernandez Bolanos, R, Paolicelli, D, Tortorella, C, Spelman, T, Margari, L, Amato, MP, Comi, G, Butzkueven, H, and Trojano, M

Abstract

OBJECTIVE: To assess prognostic factors for a second clinical attack and a first disability-worsening event in pediatric clinically isolated syndrome (pCIS) suggestive of multiple sclerosis (MS) patients. METHODS: A cohort of 770 pCIS patients was followed up for at least 10 years. Cox proportional hazard models and Recursive Partitioning and Amalgamation (RECPAM) tree-regression were used to analyze data. RESULTS: In pCIS, female sex and a multifocal onset were risk factors for a second clinical attack (hazard ratio [HR], 95% confidence interval [CI] = 1.28, 1.06-1.55; 1.42, 1.10-1.84, respectively), whereas disease-modifying drug (DMD) exposure reduced this risk (HR, 95% CI = 0.75, 0.60-0.95). After pediatric onset MS (POMS) diagnosis, age at onset younger than 15 years and DMD exposure decreased the risk of a first Expanded Disability Status Scale (EDSS)-worsening event (HR, 95% CI = 0.59, 0.42-0.83; 0.75, 0.71-0.80, respectively), whereas the occurrence of relapse increased this risk (HR, 95% CI = 5.08, 3.46-7.46). An exploratory RECPAM analysis highlighted a significantly higher incidence of a first EDSS-worsening event in patients with multifocal or isolated spinal cord or optic neuritis involvement at onset in comparison to those with an isolated supratentorial or brainstem syndrome. A Cox regression model including RECPAM classes confirmed DMD exposure as the most protective factor against EDSS-worsening events and relapses as the most important risk factor for attaining EDSS worsening. INTERPRETATION: This work represents a step forward in identifying predictors of unfavorable course in pCIS and POMS and supports a protective effect of early DMD treatment in preventing MS development and disability accumulation in this population. Ann Neurol 2017;81:729-739.

Published
2017

90. Quantifying risk of early relapse in patients with first demyelinating events: Prediction in clinical practice

Author

Spelman, T, Meyniel, C, Ignacio Rojas, J, Lugaresi, A, Izquierdo, G, Grand'Maison, F, Boz, C, Alroughani, R, Havrdova, E, Horakova, D, Iuliano, G, Duquette, P, Terzi, M, Grammond, P, Hupperts, R, Lechner-Scott, J, Oreja-Guevara, C, Pucci, E, Verheul, F, Fiol, M, Van Pesch, V, Cristiano, E, Petersen, T, Moore, F, Kalincik, T, Jokubaitis, V, Trojano, M, Butzkueven, H, Spelman, T, Meyniel, C, Ignacio Rojas, J, Lugaresi, A, Izquierdo, G, Grand'Maison, F, Boz, C, Alroughani, R, Havrdova, E, Horakova, D, Iuliano, G, Duquette, P, Terzi, M, Grammond, P, Hupperts, R, Lechner-Scott, J, Oreja-Guevara, C, Pucci, E, Verheul, F, Fiol, M, Van Pesch, V, Cristiano, E, Petersen, T, Moore, F, Kalincik, T, Jokubaitis, V, Trojano, M, and Butzkueven, H

Abstract

BACKGROUND: Characteristics at clinically isolated syndrome (CIS) examination assist in identification of patient at highest risk of early second attack and could benefit the most from early disease-modifying drugs (DMDs). OBJECTIVE: To examine determinants of second attack and validate a prognostic nomogram for individualised risk assessment of clinical conversion. METHODS: Patients with CIS were prospectively followed up in the MSBase Incident Study. Predictors of clinical conversion were analysed using Cox proportional hazards regression. Prognostic nomograms were derived to calculate conversion probability and validated using concordance indices. RESULTS: A total of 3296 patients from 50 clinics in 22 countries were followed up for a median (inter-quartile range (IQR)) of 1.92 years (0.90, 3.71). In all, 1953 (59.3%) patients recorded a second attack. Higher Expanded Disability Status Scale (EDSS) at baseline, first symptom location, oligoclonal bands and various brain and spinal magnetic resonance imaging (MRI) metrics were all predictors of conversion. Conversely, older age and DMD exposure post-CIS were associated with reduced rates. Prognostic nomograms demonstrated high concordance between estimated and observed conversion probabilities. CONCLUSION: This multinational study shows that age at CIS onset, DMD exposure, EDSS, multiple brain and spinal MRI criteria and oligoclonal bands are associated with shorter time to relapse. Nomogram assessment may be useful in clinical practice for estimating future clinical conversion.

Published
2017

91. Highly active immunomodulatory therapy ameliorates accumulation of disability in moderately advanced and advanced multiple sclerosis

Author

Lizak, N, Lugaresi, A, Alroughani, R, Lechner-Scott, J, Slee, M, Havrdova, E, Horakova, D, Trojano, M, Izquierdo, G, Duquette, P, Girard, M, Prat, A, Grammond, P, Hupperts, R, Grand'Maison, F, Sola, P, Pucci, E, Bergamaschi, R, Oreja-Guevara, C, Van Pesch, V, Ramo, C, Spitaleri, D, Iuliano, G, Boz, C, Granella, F, Olascoaga, J, Verheul, F, Rozsa, C, Cristiano, E, Flechter, S, Hodgkinson, S, Amato, MP, Deri, N, Jokubaitis, V, Spelman, T, Butzkueven, H, Kalincik, T, Lizak, N, Lugaresi, A, Alroughani, R, Lechner-Scott, J, Slee, M, Havrdova, E, Horakova, D, Trojano, M, Izquierdo, G, Duquette, P, Girard, M, Prat, A, Grammond, P, Hupperts, R, Grand'Maison, F, Sola, P, Pucci, E, Bergamaschi, R, Oreja-Guevara, C, Van Pesch, V, Ramo, C, Spitaleri, D, Iuliano, G, Boz, C, Granella, F, Olascoaga, J, Verheul, F, Rozsa, C, Cristiano, E, Flechter, S, Hodgkinson, S, Amato, MP, Deri, N, Jokubaitis, V, Spelman, T, Butzkueven, H, and Kalincik, T

Abstract

OBJECTIVE: To evaluate variability and predictability of disability trajectories in moderately advanced and advanced multiple sclerosis (MS), and their modifiability with immunomodulatory therapy. METHODS: The epochs between Expanded Disability Status Scale (EDSS) steps 3-6, 4-6 and 6-6.5 were analysed. Patients with relapse-onset MS and having reached 6-month confirmed baseline EDSS step (3/4/6) were identified in MSBase, a global observational MS cohort study. We used multivariable survival models to examine the impact of disease-modifying therapy, clinical and demographic factors on progression to the outcome EDSS step (6/6.5). Sensitivity analyses with varying outcome definitions and inclusion criteria were conducted. RESULTS: For the EDSS 3-6, 4-6 and 6-6.5 epochs, 1560, 1504 and 1231 patients were identified, respectively. Disability trajectories showed large coefficients of variance prebaseline (0.92-1.11) and postbaseline (2.15-2.50), with no significant correlations. The probability of reaching the outcome step was not associated with prebaseline variables, but was increased by higher relapse rates during each epoch (HRs 1.58-3.07; p<0.001). A greater proportion of each epoch treated with higher efficacy therapies was associated with lower risk of reaching the outcome disability step (HRs 0.72-0.91 per 25%; p≤0.02). 3 sensitivity analyses confirmed these results. CONCLUSIONS: Disease progression during moderately advanced and advanced MS is highly variable and amnesic to prior disease activity. Lower relapse rates and greater time on higher efficacy immunomodulatory therapy after reaching EDSS steps 3, 4 and 6 are associated with a decreased risk of accumulating further disability. Highly effective immunomodulatory therapy ameliorates accumulation of disability in moderately advanced and advanced relapse-onset MS.

Published
2017

92. Experience of an information aid for newly diagnosed multiple sclerosis patients: A qualitative study on the SIMS-Trial

Author

Borreani, Claudia, Giordano, Andrea, Falautano, Monica, Lugaresi, Alessandra, Martinelli, Vittorio, Granella, Franco, Tortorella, Carla, Plasmati, Imma, Radaelli, Marta, Farina, Deborah, Dalla Bella, Eleonora, Bianchi, Elisabetta, Acquarone, Nicola, Miccinesi, Guido, Solari, Alessandra, D'Alessandro, R., Pucci, E., Uccelli, M. M., Trojano, M., Heesen, C., Mancardi, G. L., Milanese, C., Calabrese, D., Ferrari, G., Mattarozzi, K., Confalonieri, P., Antozzi, C., Maggi, L., Mantegazza, R., Martinelli, V., Colombo, B., Esposito, F., Moiola, L., Rodegher, M., Immovilli, P., De Luca, Giovanna, Di Tommaso, V., Di Ioia, M., Travaglini, D., Pietrolongo, E., Zimatore, G., Borreani, Claudia, Giordano, Andrea, Falautano, Monica, Lugaresi, Alessandra, Martinelli, Vittorio, Granella, Franco, Tortorella, Carla, Plasmati, Imma, Radaelli, Marta, Farina, Deborah, Dalla Bella, Eleonora, Bianchi, Elisabetta, Acquarone, Nicola, Miccinesi, Guido, Solari, Alessandra, D'Alessandro, R., Pucci, E., Uccelli, M. M., Trojano, M., Heesen, C., Mancardi, G. L., Milanese, C., Calabrese, D., Ferrari, G., Mattarozzi, K., Confalonieri, P., Antozzi, C., Maggi, L., Mantegazza, R., Martinelli, V., Colombo, B., Esposito, F., Moiola, L., Rodegher, M., Immovilli, P., De Luca, Giovanna, Di Tommaso, V., Di Ioia, M., Travaglini, D., Pietrolongo, E., and Zimatore, G.

Subjects
Adult, Male, Clinical Trials as Topic, Patient, Time Factor, Public Health, Environmental and Occupational Health, Middle Aged, Diagnosis communication, Complex intervention, Patient Education as Topic, Physician, Multiple Sclerosi, Female, Qualitative study, Shared decision making, Qualitative Research, Human
Abstract

Background The SIMS-Trial (ISRCTN81072971) proved the effectiveness, in terms of patient's knowledge and care satisfaction, of an add-on information aid (personal interview with a physician using a navigable CD and take-home booklet) in 120 newly diagnosed patients with multiple sclerosis (MS) from five Italian centres. Objective To scrutinize the experience of SIMS-Trial participants in order to gain better understanding of the effectiveness of the information aid and its components. Design We performed (i) nine individual semi-structured interviews with a purposeful sample of SIMS-Trial patients who received the information aid, (ii) focus group meeting (FGM) with the physicians who conducted the personal interview, and (iii) FGM with patients' caring neurologists. Results Patients' experience with the information aid was positive as it enhanced their understanding of their disease, being viewed as a guided tour of their medical condition. The physicians who conducted the personal interviews were also positive in their overall evaluation but noted an initial difficulty in using the CD. The caring neurologists had limited direct experience of the aid, and their views were confined to utility of the information aid in general. All participants considered the combination of personal interview, CD navigation and take-home booklet essential, but urged a more flexible scheduling of the personal interview. It also emerged that some content required revision and that the aid was unsuitable for patients with primary progressive MS. Conclusions The results of the study further support the value of the aid and also provide important indications for improving it and refining indications for use. © 2011 John Wiley & Sons Ltd.

Published
2014

93. Design and rationale for the Minimizing Adverse haemorrhagic events by TRansradial access site and systemic Implementation of angioX program

Author

Valgimigli, M, Gagnor, A, Calabrò, P, Rubartelli, P, Garducci, S, Ando', Giuseppe, Santarelli, A, Galli, M, Garbo, R, Bramucci, E, Ierna, S, Briguori, C, Cortese, B, Limbruno, U, Violini, R, Presbitero, P, de Cesare, N, Sganzerla, P, Ausiello, A, Tosi, P, Sardella, G, Sabate, M, Brugaletta, S, Saccone, G, Vandoni, P, Zingarelli, A, Liso, A, Rigattieri, S, Di Lorenzo, E, Vigna, C, Palmieri, C, Falcone, C, De Caterina, R, Caputo, M, Esposito, G, Lupi, A, Mazzarotto, P, Varbella, F, Zaro, T, Nazzaro, M, Rao, Sv, van't Hof, Aw, Omerovic, E, Uguccioni, L, Tamburino, C, Ferrari, F, Ceravolo, R, Tarantino, F, Casu, G, Cremonesi, A, Saia, F, Guiducci, V, Dellavalle, A, Curello, S, Mangiacapra, F, Evola, R, Liistro, F, Creaco, M, Colombo, A, Perkan, A, De Servi, S, Fischetti, D, Pucci, E, Romagnoli, E, Moretti, C, Moretti, L, Turturo, M, Bonmassari, R, Penzo, C, Loi, B, Mauro, C, Gabrielli, G, Micari, A, Petronio, As, Comeglio, M, Fresco, C, Pasquetto, G, Belloni, F, Amico, F., Cardiology, Valgimigli, M, Gagnor, A, Calabrò, P, Rubartelli, P, Garducci, S, Andò, G, Santarelli, A, Galli, M, Garbo, R, Bramucci, E, Ierna, S, Briguori, C, Cortese, B, Limbruno, U, Violini, R, Presbitero, P, de Cesare, N, Sganzerla, P, Ausiello, A, Tosi, P, Sardella, G, Sabate, M, Brugaletta, S, Saccone, G, Vandoni, P, Zingarelli, A, Liso, A, Rigattieri, S, Di Lorenzo, E, Vigna, C, Palmieri, C, Falcone, C, De Caterina, R, Caputo, M, Esposito, G, Lupi, A, Mazzarotto, P, Varbella, F, Zaro, T, Nazzaro, M, Rao, Sv, van't Hof, Aw, Omerovic, E, Uguccioni, L, Tamburino, C, Ferrari, F, Ceravolo, R, Tarantino, F, Casu, G, Cremonesi, A, Saia, F, Guiducci, V, Dellavalle, A, Curello, S, Mangiacapra, F, Evola, R, Liistro, F, Creaco, M, Colombo, A, Perkan, A, De Servi, S, Fischetti, D, Pucci, E, Romagnoli, E, Moretti, C, Moretti, L, Turturo, M, Bonmassari, R, Penzo, C, Loi, B, Mauro, C, Gabrielli, G, Micari, A, Petronio, A, Comeglio, M, Fresco, C, Pasquetto, G, Belloni, F, and Amico, F

Subjects
Male, Hirudin, medicine.medical_treatment, Antithrombin, Myocardial Infarction, Peptide Fragment, Bivalirudin, Myocardial infarction, Stroke, Incidence (epidemiology), Heparin, Hirudins, Middle Aged, Recombinant Protein, Recombinant Proteins, Europe, Femoral Artery, Treatment Outcome, Radial Artery, Cardiology, Female, Survival Analysi, Cardiology and Cardiovascular Medicine, medicine.drug, Human, medicine.medical_specialty, Platelet Glycoprotein GPIIb-IIIa Complex, Postoperative Hemorrhage, Acute Coronary Syndrome, Aged, Antithrombins, Humans, Percutaneous Coronary Intervention, Platelet Aggregation Inhibitors, Survival Analysis, Peptide Fragments, Acute coronary syndromes, Transradial intervention, bivalirudin, Internal medicine, medicine, business.industry, Platelet Aggregation Inhibitor, Percutaneous coronary intervention, medicine.disease, Surgery, Access site, business
Abstract

Background Transradial intervention (TRI) and bivalirudin infusion compared with transfemoral coronary intervention or unfractionated heparin plus glycoprotein IIb/IIIa inhibitors decrease bleeding complications in patients with acute coronary syndromes (ACS). Although bleeding is thought to be associated with worse outcomes, it remains unclear whether TRI and bivalirudin both independently lower ischemic or combined ischemic and bleeding complications in ACS patients undergoing contemporary invasive management. Hypotheses The primary objectives of the MATRIX program are to assess whether TRI or bivalirudin as compared, respectively, with transfemoral coronary intervention (MATRIX access site) or unfractionated heparin plus provisional glycoprotein IIb/IIIa inhibitors, (MATRIX antithrombin) decrease the 30-day incidence of an ischemic (ie, death, myocardial infarction or stroke) or an ischemic and bleeding composite end point across the whole spectrum of ACS patients, including clarifying the optimal duration of bivalirudin infusion after percutaneous coronary intervention (MATRIX treatment duration). Study design The MATRIX (NCT01433627) study, which incorporates 3 randomized comparisons in a nonfactorial manner and primary end points at 30 days and clinical follow-up ≤1 year, is a large-scale, multicenter study with blind event adjudication conducted at approximately 100 European sites. With 8,200 patients in the randomized comparison of access sites and 6,800 individuals participating in the randomized comparison of antithrombin regimens, this study will have ≥85% power for the primary end points. Summary The MATRIX program aims at conclusively ascertaining the role of TRI and bivalirudin infusion in the whole spectrum of ACS patients undergoing contemporary invasive management.

Published
2014

94. Natalizumab treatment in multiple sclerosis patients: a multicenter experience in clinical practice in Italy

Author

Totaro, R., Alessandra Lugaresi, Bellantonio, P., Danni, M., Costantino, G., Gasperini, C., Florio, C., Pucci, E., Maddestra, M., Spitaleri, D., Lus, G., Ardito, B., Farina, D., Rossi, M., Carmine, C. D. I., Altobelli, E., Maccarone, B., Casalena, A., Luca, G., Travaglini, D., Ioia, M. D. I., Tommaso, V. D. I., Fantozzi, R., Ruggieri, S., Provinciali, L., Riso, S., Mundi, C., Fuiani, A., Galgani, S., Maniscalco, G. T., Giuliani, G., Cartechini, E., Petretta, V., Fratta, M., Alfieri, G., Gatto, M., Carolei, A., Totaro, R, Lugaresi, A, Bellantonio, P, Danni, M, Costantino, G, Gasperini, C, Florio, C, Pucci, E, Maddestra, M, Spitaleri, D, Lus, Giacomo, Ardito, B, Farina, D, Rossi, M, Di Carmine, C, Altobelli, E, Maccarone, B, Casalena, A, De Luca, G, Travaglini, D, Di Ioia, M, Di Tommaso, V, Fantozzi, R, Ruggieri, S, Provinciali, L, De Riso, S, Mundi, C, Fuiani, A, Galgani, S, Maniscalco, Gt, Giuliani, G, Cartechini, E, Petretta, V, Fratta, M, Alfieri, G, Gatto, M, Carolei, A., and DIPARTIMENTO DI SCIENZE BIOMEDICHE E NEUROMOTORIE

Subjects
Adult, Male, medicine.medical_specialty, Time Factors, Antibodies, Monoclonal, Humanized, Disability Evaluation, Disease Progression, Disease-Free Survival, Female, Humans, Immunosuppressive Agents, Italy, Kaplan-Meier Estimate, Magnetic Resonance Imaging, Middle Aged, Multiple Sclerosis, Relapsing-Remitting, Natalizumab, Product Surveillance, Postmarketing, Treatment Outcome, Immunology, Relapsing-Remitting, multiple sclerosis, Antibodies, Internal medicine, Monoclonal, medicine, Immunology and Allergy, Humanized, Pharmacology, Expanded Disability Status Scale, medicine.diagnostic_test, treatment, business.industry, Multiple sclerosis, Disease progression, Magnetic resonance imaging, multi center, medicine.disease, Product Surveillance, Postmarketing, Clinical Practice, Physical therapy, Observational study, multiple sclerosis, treatment, natalizumab, multi center, Italy, business, medicine.drug
Abstract

none 39 no Articolo con dati scientifici originali pubblicato nella sezione "Editorial" della rivista We evaluated efficacy of natalizumab in relapsing-remitting multiple sclerosis patients in a clinical practice setting. We report data on the first consecutive 343 patients receiving natalizumab in 12 multiple sclerosis (MS) Italian centers enrolled between April 2007 and November 2010. The main efficacy endpoints were the proportion of patients free from relapses, disease progression, combined clinical activity, defined as presence of relapse or disease progression, from MRI activity, and from any disease activity defined as the absence of any single or combined activity. At the end of follow-up, the cumulative proportion of patients free from relapses was 68%; the proportion of patients free from Expanded Disability Status Scale (EDSS) progression was 93%; the proportion of patients free from combined clinical activity was 65%; the proportion of patients free from MRI activity was 77%; and the proportion of patients free from any disease activity was 53%. Natalizumab was effective in reducing clinical and neuroradiological disease activity. Its effectiveness in clinical practice is higher than that reported in pivotal trials and was maintained over time. none Totaro R; Lugaresi A; Bellantonio P; Danni M; Costantino G; Gasperini C; Florio C; Pucci E; Maddestra M; Spitaleri D; Lus G; Ardito B; Farina D; Rossi M; Di Carmine C; Altobelli E; Maccarone B; Casalena A; De Luca G; Travaglini D; Di Ioia M; Di Tommaso V; Fantozzi R; Ruggieri S; Provinciali L; De Riso S; Mundi C; Fuiani A; Galgani S; Ruggieri S; Maniscalco GT; Giuliani G; Cartechini E; Petretta V; Fratta M; Alfieri G; Gatto M; Carolei A; Natalizumab Long-Term Treatment Study group Totaro R; Lugaresi A; Bellantonio P; Danni M; Costantino G; Gasperini C; Florio C; Pucci E; Maddestra M; Spitaleri D; Lus G; Ardito B; Farina D; Rossi M; Di Carmine C; Altobelli E; Maccarone B; Casalena A; De Luca G; Travaglini D; Di Ioia M; Di Tommaso V; Fantozzi R; Ruggieri S; Provinciali L; De Riso S; Mundi C; Fuiani A; Galgani S; Ruggieri S; Maniscalco GT; Giuliani G; Cartechini E; Petretta V; Fratta M; Alfieri G; Gatto M; Carolei A; Natalizumab Long-Term Treatment Study group

Published
2014

95. The Multiple Sclerosis Knowledge Questionnaire: a self-administered instrument for recently diagnosed patients

Author

Giordano, A, Uccelli, Mm, Pucci, E, Martinelli, V, Borreani, C, Lugaresi, A, Trojano, M, Granella, F, Confalonieri, P, Radice, D, Solari, A, D'Alessandro, R, Heesen, C, Mancardi, Gl, Milanese, C, Galimberti, S, Calabrese, D, Ferrari, G, Mattarozzi, K, Antozzi, C, Lauria, G, La Mantia, L, Pedotti, R, Mantegazza, R, Maggi, L, Colombo, B, Esposito, F, Moiola, L, Rodegher, M, Radaelli, M, Immovilli, P, Dalla Bella, E, De Luca, G, Mattoscio, M, Di Ioia, M, Pace, M, Travaglini, D, Maruotti, V, Farina, D, Zimatore, G, Plasmati, I, Tortorella, C., Giordano A., Uccelli M.M., Pucci E., Martinelli V., Borreani C., Lugaresi A., Trojano M., Granella F., Confalonieri P., Radice D., Solari A., D'Alessandro R., Heesen C., Mancardi G.L., Milanese C., Galimberti S., Calabrese D., Ferrari G., Mattarozzi K., Antozzi C., Lauria G., La Mantia L., Pedotti R., Mantegazza R., Maggi L., Colombo B., Esposito F., Moiola L., Rodegher M., Radaelli M., Immovilli P., Dalla Bella E., De Luca G., Mattoscio M., Di Ioia M., Pace M., Travaglini D., Maruotti V., Farina D., Zimatore G., Plasmati I., Tortorella C., (SIMS-Trial group)., Giordano, A., Uccelli, M. M., Pucci, E., Martinelli, V., Borreani, C., Lugaresi, A., Trojano, M., Granella, F., Confalonieri, P., Radice, D., Solari, A., D'Alessandro, R., Heesen, C., Mancardi, G. L., Milanese, C., Galimberti, S., Calabrese, D., Ferrari, G., Mattarozzi, K., Antozzi, C., Lauria, G., La Mantia, L., Pedotti, R., Mantegazza, R., Maggi, L., Colombo, B., Esposito, F., Moiola, L., Rodegher, M., Radaelli, M., Immovilli, P., Dalla Bella, E., De Luca, G., Mattoscio, M., Di Ioia, M., Pace, M., Travaglini, D., Maruotti, V., Farina, D., Zimatore, G., Plasmati, I., and Tortorella, C.

Subjects
Questionnaires, Male, law.invention, Disability Evaluation, Randomized controlled trial, Informed consent, law, Surveys and Questionnaires, Multiple Sclerosi, Content validity, Surveys and Questionnaire, Medicine, Young adult, Patient-reported outcome, Informed Consent, Psychiatric Status Rating Scale, Middle Aged, Newly diagnosed, Test (assessment), Knowledge, Neurology, Italy, drug therapy/psychology, Female, Human, Adult, Employment, medicine.medical_specialty, Multiple Sclerosis, Logistic Model, Adolescent, multiple sclerosis, questionnaire, MEDLINE, Reproducibility of Result, Education, Young Adult, Patient Education as Topic, Adolescent, Adult, Disability Evaluation, Education, Employment, Female, Humans, Informed Consent, Italy, Logistic Models, Male, Middle Aged, Multiple Sclerosis, drug therapy/psychology, Patient Education as Topic, Psychiatric Status Rating Scales, Questionnaires, Reproducibility of Results, Young Adult, Humans, Psychiatric Status Rating Scales, Questionnaire, business.industry, Construct validity, Reproducibility of Results, Surgery, Clinical trial, Logistic Models, Measurement development, Physical therapy, Neurology (clinical), business
Abstract

There are few studies on patient knowledge in multiple sclerosis (MS), and only two published questionnaires. The objective of this article was to develop and validate the MS Knowledge Questionnaire (MSKQ), a self-assessed instrument for newly diagnosed MS patients. Thirty multiple-choice statements, conceived to test MS knowledge, were produced by a multidisciplinary panel and pre-tested on three MS patients, resulting in an intermediate 26-item version. This was tested on 54 MS patients for internal consistency, content and construct validity (validation sample I). The final (25-item) MSKQ was a primary outcome measure in the SIMS-Trial on an information aid to newly diagnosed MS patients. Postal responses of SIMS-Trial participants to the MSKQ a month after intervention (validation sample II) were analysed. Median MSKQ scores in validation samples I and II were, respectively, 18 (range 9—23) and 17 (range 3—24). Acceptability, internal consistency (Kuder—Richardson-20 formula 0.76) and content validity were good. Educational attainment and receiving the information aid were the main independent predictors of MS knowledge. Other predictors were female sex (positive association) and disease duration (negative association). In conclusion, the MSKQ has good clinimetric properties and is sensitive to an educational intervention. We propose the MSKQ as a brief instrument for clinical practice and research.

Published
2009

96. Home-based palliative approach for people with severe multiple sclerosis and their carers: Study protocol for a randomized controlled trial

Author

Solari, Alessandra, Giordano, Andrea, Grasso, Maria Grazia, Confalonieri, Paolo, Patti, Francesco, Lugaresi, Alessandra, Palmisano, Lucia, Amadeo, Roberta, Martino, Giovanni, Ponzio, Michela, Casale, Giuseppe, Borreani, Claudia, Causarano, Renzo, Veronese, Simone, Zaratin, Paola, Battaglia, MARIO ALBERTO, Radice, D., Oliver, D. J., Pucci, E., Tesio, L., Cugno, C., Morino, P., Lopes de Carvalho, M. L., Giuntoli, M., Motta, R., Stefanelli, M. C., Bianchi, E., Giovannetti, A., Torri Clerici, V., Rossetti, E., Totis, A., Campanella, A., Martini, F., Fittipaldo, A., Ferrari, G., Mantegazza, R., Rossi, I., Troisi, E., Pompa, A., Tucci, L., Ippoliti, F., Morone, G., Fusco, A., Da Col, D., Lissoni, B., Pietrolongo, E., Onofrj, M., Cilia, S., Leone, C., Cascio, V., Cimino, V., Occhipinti, G., Pappalardo, A., Cavallaro, C., Zagari, F., and Alessandra Solari, Andrea Giordano, Maria Grazia Grasso, Paolo Confalonieri, Francesco Patti, Alessandra Lugaresi, Lucia Palmisano, Roberta Amadeo, Giovanni Martino, Michela Ponzio, Giuseppe Casale, Claudia Borreani, Renzo Causarano, Simone Veronese, Paola Zaratin, Mario Alberto Battaglia, PeNSAMI project

Subjects
Complex intervention, Multiple sclerosis, Palliative care, Qualitative research, Randomized controlled trial, Home Care Service, Pediatrics, medicine.medical_specialty, Medicine (miscellaneous), law.invention, Quality of life (healthcare), law, Intervention (counseling), Multiple Sclerosi, medicine, Single-Blind Method, Pharmacology (medical), Clinical Protocol, business.industry, Caregiver, Focus group, Clinical trial, Mood, Family medicine, business, Human
Abstract

Preliminary evidence suggests that palliative care may be useful for people with severe multiple sclerosis (MS). The aim of this study is to determine the effectiveness of a home-based palliative approach (HPA) for people with severe MS and their carers. This is a single-blind randomized controlled trial with a nested qualitative study. Seventy-five severe MS-carer dyads are being randomized (at three centers, one in each area of Italy) to HPA or usual care (UC) in a 2:1 ratio. Each center has a specially trained team consisting of four professionals (physician, nurse, psychologist, social worker). The team makes a comprehensive assessment of the needs of the dyads. HPA content is then agreed on, discussed with the patient’s caring physician, and delivered over six months. The intervention is not intended to replace existing services. At later visits, the team checks the HPA delivery and reviews/modifies it as necessary. HPA and UC dyads are assessed at home by a blind examiner at baseline, and three and six months later; they also receive monthly telephone interviews. Dyads assigned to UC receive the examiner’s visits and telephone interviews, but not the team visits. Primary outcome measures are changes in symptoms (Palliative care Outcome Scale-Symptoms-MS, POS-S-MS), and quality of life (the Schedule for the Evaluation of Individual Quality of Life-Direct Weighting (SEIQoL-DW), not assessed in patients with severe cognitive compromise) at three and six months. Other outcomes are changes in patient functional status and mood; changes in carer quality of life, mood and caregiving burden; costs; incorporation with standard care; unplanned hospital admissions; referrals to hospice; and deaths. The experience of participants will be evaluated qualitatively by individual semi-structured interviews (HPA patients and carers) and focus group meetings (HPA patients’ caring physicians). The results of our study will show whether the HPA is feasible and beneficial to people with severe MS and their carers living in the three Italian geographic areas. The nested qualitative study will add to the understanding of the strengths and limitations of the intervention. The trial was registered with Current Controlled Trials (identifier: ISRCTN73082124 ) on 19 June 2014.

Published
2015

98. Anti‐inflammatory disease‐modifying treatment and disability progression in primary progressive multiple sclerosis: a cohort study.

Author

Lorscheider, J., Kuhle, J., Izquierdo, G., Lugaresi, A., Havrdova, E., Horakova, D., Hupperts, R., Duquette, P., Girard, M., Prat, A., Grand'Maison, F., Grammond, P., Sola, P., Ferraro, D., Trojano, M., Ramo‐Tello, C., Lechner‐Scott, J., Pucci, E., Solaro, C., and Slee, M.

Subjects
MULTIPLE sclerosis, MEDICAL care, CLINICAL trials, DISEASE progression, DEMYELINATION
Abstract

Background and purpose: Treatment options in primary progressive multiple sclerosis (PPMS) are scarce and, with the exception of ocrelizumab, anti‐inflammatory agents have failed to show efficacy in ameliorating disability progression. The aim of this study was to investigate a potential effect of anti‐inflammatory disease‐modifying treatment on disability outcomes in PPMS. Methods: Using MSBase, a large, international, observational database, we identified patients with PPMS who were either never treated or treated with a disease‐modifying agent. Propensity score matching was used to select subpopulations with similar baseline characteristics. Expanded Disability Status Scale (EDSS) outcomes were compared with an intention‐to‐treat and an as‐treated approach in paired, pairwise‐censored analyses. Results: Of the 1284 included patients, 533 were matched (treated, n = 195; untreated n = 338). Median on‐study pairwise‐censored follow‐up was 3.4 years (quartiles 1.2–5.5). No difference in the hazard of experiencing 3‐month confirmed EDSS progression events was observed between the groups [hazard ratio (HR), 1.0; 95% confidence interval (CI), 0.6–1.7, P = 0.87]. We did not find significant differences in the hazards of confirmed EDSS improvement (HR, 1.0; 95% CI, 0.6–1.6, P = 0.91) or reaching a confirmed EDSS step ≥7 (HR, 1.1; 95% CI, 0.7–1.6, P = 0.69). Conclusion: Our pooled analysis of disease‐modifying agents suggests that these therapies have no substantial effect on short‐ to medium‐term disability outcomes in PPMS. [ABSTRACT FROM AUTHOR]

Published
2019
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99. Defining secondary progressive multiple sclerosis

Author

Lorscheider, J, Buzzard, K, Jokubaitis, V, Spelman, T, Havrdova, E, Horakova, D, Trojano, M, Izquierdo, G, Girard, M, Duquette, P, Prat, A, Lugaresi, A, Grand'Maison, F, Grammond, P, Hupperts, R, Alroughani, R, Sola, P, Boz, C, Pucci, E, Lechner-Scott, J, Bergamaschi, R, Oreja-Guevara, C, Iuliano, G, Van Pesch, V, Granella, F, Ramo-Tello, C, Spitaleri, D, Petersen, T, Slee, M, Verheul, F, Ampapa, R, Amato, MP, McCombe, P, Vucic, S, Sanchez Menoyo, JL, Cristiano, E, Barnett, MH, Hodgkinson, S, Olascoaga, J, Laura Saladino, M, Gray, O, Shaw, C, Moore, F, Butzkueven, H, Kalincik, T, Lorscheider, J, Buzzard, K, Jokubaitis, V, Spelman, T, Havrdova, E, Horakova, D, Trojano, M, Izquierdo, G, Girard, M, Duquette, P, Prat, A, Lugaresi, A, Grand'Maison, F, Grammond, P, Hupperts, R, Alroughani, R, Sola, P, Boz, C, Pucci, E, Lechner-Scott, J, Bergamaschi, R, Oreja-Guevara, C, Iuliano, G, Van Pesch, V, Granella, F, Ramo-Tello, C, Spitaleri, D, Petersen, T, Slee, M, Verheul, F, Ampapa, R, Amato, MP, McCombe, P, Vucic, S, Sanchez Menoyo, JL, Cristiano, E, Barnett, MH, Hodgkinson, S, Olascoaga, J, Laura Saladino, M, Gray, O, Shaw, C, Moore, F, Butzkueven, H, and Kalincik, T

Published
2016

100. The effect of oral immunomodulatory therapy on treatment uptake and persistence in multiple sclerosis

Author

Warrender-Sparkes, M, Spelman, T, Izquierdo, G, Trojano, M, Lugaresi, A, Grand'Maison, F, Havrdova, E, Horakova, D, Boz, C, Oreja-Guevara, C, Alroughani, R, Iuliano, G, Duquette, P, Girard, M, Terzi, M, Hupperts, R, Grammond, P, Petersen, T, Fernandez-Bolanos, R, Fiol, M, Pucci, E, Lechner-Scott, J, Verheul, F, Cristiano, E, Van Pesch, V, Petkovska-Boskova, T, Moore, F, Kister, I, Bergamaschi, R, Laura Saladino, M, Slee, M, Barnett, M, Amato, MP, Shaw, C, Shuey, N, Young, C, Gray, O, Kappos, L, Butzkueven, H, Kalincik, T, Jokubaitis, V, Warrender-Sparkes, M, Spelman, T, Izquierdo, G, Trojano, M, Lugaresi, A, Grand'Maison, F, Havrdova, E, Horakova, D, Boz, C, Oreja-Guevara, C, Alroughani, R, Iuliano, G, Duquette, P, Girard, M, Terzi, M, Hupperts, R, Grammond, P, Petersen, T, Fernandez-Bolanos, R, Fiol, M, Pucci, E, Lechner-Scott, J, Verheul, F, Cristiano, E, Van Pesch, V, Petkovska-Boskova, T, Moore, F, Kister, I, Bergamaschi, R, Laura Saladino, M, Slee, M, Barnett, M, Amato, MP, Shaw, C, Shuey, N, Young, C, Gray, O, Kappos, L, Butzkueven, H, Kalincik, T, and Jokubaitis, V

Abstract

OBJECTIVE: We aimed to analyse the effect of the introduction of fingolimod, the first oral disease-modifying therapy, on treatment utilisation and persistence in an international cohort of patients with multiple sclerosis (MS). METHODS: MSBASIS, a prospective, observational sub-study of the MSBase registry, collects demographic, clinical and paraclinical data on patients followed from MS onset (n=4718). We conducted a multivariable conditional risk set survival analysis to identify predictors of treatment discontinuation, and to assess if the introduction of fingolimod has altered treatment persistence. RESULTS: A total of 2640 patients commenced immunomodulatory therapy. Following the introduction of fingolimod, patients were more likely to discontinue all other treatments (hazard ratio 1.64, p<0.001) while more patients switched to fingolimod than any other therapy (42.3% of switches). Patients switched to fingolimod due to convenience. Patients treated with fingolimod were less likely to discontinue treatment compared with other therapies (p<0.001). Female sex, country of residence, younger age, a high Expanded Disability Status Scale score and relapse activity were all independently associated with higher rates of treatment discontinuation. CONCLUSION: Following the availability of fingolimod, patients were more likely to discontinue injectable treatments. Those who switched to fingolimod were more likely to do so for convenience. Persistence was improved on fingolimod compared to other medications.

Published
2016

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