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1. Myogenic Cell Transplantation in Genetic and Acquired Diseases of Skeletal Muscle.

Author

Boyer, O, Butler-Browne, G, Chinoy, H, Cossu, G, Galli, F, Lilleker, JB, Magli, A, Mouly, V, Perlingeiro, RCR, Previtali, SC, Sampaolesi, M, Smeets, H, Schoewel-Wolf, V, Spuler, S, Torrente, Y, Van Tienen, F, Study Group, Boyer, O, Butler-Browne, G, Chinoy, H, Cossu, G, Galli, F, Lilleker, JB, Magli, A, Mouly, V, Perlingeiro, RCR, Previtali, SC, Sampaolesi, M, Smeets, H, Schoewel-Wolf, V, Spuler, S, Torrente, Y, Van Tienen, F, and Study Group

Abstract

This article will review myogenic cell transplantation for congenital and acquired diseases of skeletal muscle. There are already a number of excellent reviews on this topic, but they are mostly focused on a specific disease, muscular dystrophies and in particular Duchenne Muscular Dystrophy. There are also recent reviews on cell transplantation for inflammatory myopathies, volumetric muscle loss (VML) (this usually with biomaterials), sarcopenia and sphincter incontinence, mainly urinary but also fecal. We believe it would be useful at this stage, to compare the same strategy as adopted in all these different diseases, in order to outline similarities and differences in cell source, pre-clinical models, administration route, and outcome measures. This in turn may help to understand which common or disease-specific problems have so far limited clinical success of cell transplantation in this area, especially when compared to other fields, such as epithelial cell transplantation. We also hope that this may be useful to people outside the field to get a comprehensive view in a single review. As for any cell transplantation procedure, the choice between autologous and heterologous cells is dictated by a number of criteria, such as cell availability, possibility of in vitro expansion to reach the number required, need for genetic correction for many but not necessarily all muscular dystrophies, and immune reaction, mainly to a heterologous, even if HLA-matched cells and, to a minor extent, to the therapeutic gene product, a possible antigen for the patient. Finally, induced pluripotent stem cell derivatives, that have entered clinical experimentation for other diseases, may in the future offer a bank of immune-privileged cells, available for all patients and after a genetic correction for muscular dystrophies and other myopathies.

Published
2021

2. Estimating the impact of COVID-19 pandemic on services provided by Italian Neuromuscular Centers: an Italian Association of Myology survey of the acute phase

Author

Mauri, E, Abati, E, Musumeci, O, Rodolico, C, D'Angelo, Mg, Mirabella, M, Lucchini, M, Bello, L, Pegoraro, E, Maggi, L, Manneschi, L, Gemelli, C, Grandis, M, Zuppa, A, Massucco, S, Benedetti, L, Caponnetto, C, Schenone, A, Prelle, A, Previtali, Sc, Scarlato, M, D'Amico, A, Bertini, E, Pennisi, Em, De Giglio, L, Pane, M, Mercuri, E, Mongini, T, Ricci, F, Berardinelli, A, Astrea, G, Lenzi, S, Battini, R, Ricci, G, Torri, F, Siciliano, G, Santorelli, Fm, Ariatti, A, Filosto, M, Passamano, L, Politano, L, Scutifero, M, Tonin, P, Fossati, B, Panicucci, C, Bruno, C, Ravaglia, S, Monforte, M, Tasca, G, Ricci, E, Petrucci, A, Santoro, L, Ruggiero, L, Barp, A, Albamonte, E, Sansone, V, Gagliardi, D, Costamagna, G, Govoni, A, Magri, F, Brusa, R, Velardo, D, Meneri, M, Sciacco, M, Corti, S, Bresolin, N, Moroni, I, Messina, S, Di Muzio, A, Nigro, V, Liguori, R, Antonini, G, Toscano, A, Minetti, C, Comi, Gp, Italian Association of, Myology., Mauri, Eleonora, Abati, Elena, Musumeci, Olimpia, Rodolico, Carmelo, D'Angelo, Maria Grazia, Mirabella, Massimiliano, Lucchini, Matteo, Bello, Luca, Pegoraro, Elena, Maggi, Lorenzo, Manneschi, Letizia, Gemelli, Chiara, Grandis, Marina, Zuppa, Angela, Massucco, Sara, Benedetti, Luana, Caponnetto, Claudia, Schenone, Angelo, Prelle, Alessandro, Previtali, Stefano C, Scarlato, Marina, D'Amico, Adele, Bertini, Enrico, Pennisi, Elena M, De Giglio, Laura, Pane, Marika, Mercuri, Eugenio, Mongini, Tiziana, Ricci, Federica, Berardinelli, Angela, Astrea, Guja, Lenzi, Sara, Battini, Roberta, Ricci, Giulia, Torri, Francesca, Siciliano, Gabriele, Santorelli, Filippo M, Ariatti, Alessandra, Filosto, Massimiliano, Passamano, Luigia, Politano, Luisa, Scutifero, Marianna, Tonin, Paola, Fossati, Barbara, Panicucci, Chiara, Bruno, Claudio, Ravaglia, Sabrina, Monforte, Mauro, Tasca, Giorgio, Ricci, Enzo, Petrucci, Antonio, Santoro, Lucio, Ruggiero, Lucia, Barp, Andrea, Albamonte, Emilio, Sansone, Valeria, Gagliardi, Delia, Costamagna, Gianluca, Govoni, Alessandra, Magri, Francesca, Brusa, Roberta, Velardo, Daniele, Meneri, Megi, Sciacco, Monica, Corti, Stefania, Bresolin, Nereo, Moroni, Isabella, Messina, Sonia, Di Muzio, Antonio, Nigro, Vincenzo, Liguori, Rocco, Antonini, Giovanni, Toscano, Antonio, Minetti, Carlo, Comi, Giacomo Pietro, Mauri E., Abati E., Musumeci O., Rodolico C., D'Angelo M.G., Mirabella M., Lucchini M., Bello L., Pegoraro E., Maggi L., Manneschi L., Gemelli C., Grandis M., Zuppa A., Massucco S., Benedetti L., Caponnetto C., Schenone A., Prelle A., Previtali S.C., Scarlato M., D'Amico A., Bertini E., Pennisi E.M., de Giglio L., Pane M., Mercuri E., Mongini T., Ricci F., Berardinelli A., Astrea G., Lenzi S., Battini R., Ricci G., Torri F., Siciliano G., Santorelli F.M., Ariatti A., Filosto M., Passamano L., Politano L., Scutifero M., Tonin P., Fossati B., Panicucci C., Bruno C., Ravaglia S., Monforte M., Tasca G., Ricci E., Petrucci A., Santoro L., Ruggiero L., Barp A., Albamonte E., Sansone V., Gagliardi D., Costamagna G., Govoni A., Magri F., Brusa R., Velardo D., Meneri M., Sciacco M., Corti S., Bresolin N., Moroni I., Messina S., Muzio A.D., Nigro V., Liguori R., Antonini G., Toscano A., Minetti C., Comi G.P., Mauri, E., Abati, E., Musumeci, O., Rodolico, C., D'Angelo, M. G., Mirabella, M., Lucchini, M., Bello, L., Pegoraro, E., Maggi, L., Manneschi, L., Gemelli, C., Grandis, M., Zuppa, A., Massucco, S., Benedetti, L., Caponnetto, C., Schenone, A., Prelle, A., Previtali, S. C., Scarlato, M., D'Amico, A., Bertini, E., Pennisi, E. M., de Giglio, L., Pane, M., Mercuri, E., Mongini, T., Ricci, F., Berardinelli, A., Astrea, G., Lenzi, S., Battini, R., Ricci, G., Torri, F., Siciliano, G., Santorelli, F. M., Ariatti, A., Filosto, M., Passamano, L., Politano, L., Scutifero, M., Tonin, P., Fossati, B., Panicucci, C., Bruno, C., Ravaglia, S., Monforte, M., Tasca, G., Ricci, E., Petrucci, A., Santoro, L., Ruggiero, L., Barp, A., Albamonte, E., Sansone, V., Gagliardi, D., Costamagna, G., Govoni, A., Magri, F., Brusa, R., Velardo, D., Meneri, M., Sciacco, M., Corti, S., Bresolin, N., Moroni, I., Messina, S., Muzio, A. D., Nigro, V., Liguori, R., Antonini, G., Toscano, A., Minetti, C., and Comi, G. P.

Subjects
COVID-19, Myastenia gravis, Myopathies, Neuromuscular diseases, Neuromuscular services, Neuropathies, SARS-CoV-2, neuropathies, Ambulatory Care, Coronavirus Infections, Cross-Sectional Studies, Health Services Accessibility, Hospitalization, Humans, Italy, Neuromuscular Diseases, Pandemics, Pneumonia, Viral, Referral and Consultation, Surveys and Questionnaires, Telemedicine, Betacoronavirus, neuromuscular diseases, myastenia gravis, neuromuscular services, neuromuscular service, Surveys and Questionnaire, Viral, myopathie, Cross-Sectional Studie, Pandemic, Coronavirus Infection, Pneumonia, neuromuscular disease, myastenia gravi, Settore MED/26 - NEUROLOGIA, neuropathie, myopathies, Original Article, Human
Abstract

Introduction. Since February 2020, the outbreak of COVID-19 in Italy has forced the health care system to undergo profound rearrangements in its services and facilities, especially in the worst-hit areas in Northern Italy. In this setting, inpatient and outpatient services had to rethink and reorganize their activities to meet the needs of patients during the “lockdown”. The Italian Association of Myology developed a survey to estimate the impact of these changes on patients affected by neuromuscular disorders and on specialized neuromuscular centers during the acute phase of COVID-19 pandemic. Methods. We developed an electronic survey that was sent to neuromuscular centers affiliated with the Italian Association of Myology, assessing changes in pharmacological therapies provision, outpatient clinical and instrumental services, support services (physiotherapy, nursing care, psychological support) and clinical trials. Results. 40% of surveyed neuromuscular centers reported a reduction in outpatient visit and examinations (44.5% of centers in Northern regions; 25% of centers in Central regions; 50% of centers in Southern regions). Twenty-two% of centers postponed in-hospital administration of therapies for neuromuscular diseases (23.4% in Northern regions; 13.0% in Central regions; 20% in Southern regions). Diagnostic and support services (physiotherapy, nursing care, psychological support) were suspended in 57% of centers (66/43/44% in Northern, Central and Southern centers respectively) Overall, the most affected services were rehabilitative services and on-site outpatient visits, which were suspended in 93% of centers. Strategies adopted by neuromuscular centers to overcome these changes included maintaining urgent on-site visits, addressing patients to available services and promoting remote contact and telemedicine. Conclusions. Overall, COVID-19 pandemic resulted in a significant disruption of clinical and support services for patients with neuromuscular diseases. Despite the efforts to provide telemedicine consults to patients, this option could be promoted and improved further. A close collaboration between the different neuromuscular centers and service providers as well as further implementation of telehealth platforms are necessary to ensure quality care to NMD patients in the near future and in case of recurrent pandemic waves.

Published
2020

3. Expanding the spectrum of genes responsible for hereditary motor neuropathies

Author

Previtali, Sc, Zhao, E, Lazarevic, D, Pipitone, Gb, Fabrizi, Gm, Manganelli, F, Mazzeo, A, Pareyson, D, Schenone, A, Taroni, F, Vita, G, Bellone, E, Ferrarini, M, Garibaldi, M, Magri, S, Padua, Luca, Pennisi, E, Pisciotta, C, Riva, N, Scaioli, V, Scarlato, M, Tozza, S, Geroldi, A, Jordanova, A, Ferrari, M, Molineris, I, Reilly, Mm, Comi, G, Carrera, P, Devoto, M, Bolino, A., Padua L (ORCID:0000-0003-2570-9326), Previtali, Sc, Zhao, E, Lazarevic, D, Pipitone, Gb, Fabrizi, Gm, Manganelli, F, Mazzeo, A, Pareyson, D, Schenone, A, Taroni, F, Vita, G, Bellone, E, Ferrarini, M, Garibaldi, M, Magri, S, Padua, Luca, Pennisi, E, Pisciotta, C, Riva, N, Scaioli, V, Scarlato, M, Tozza, S, Geroldi, A, Jordanova, A, Ferrari, M, Molineris, I, Reilly, Mm, Comi, G, Carrera, P, Devoto, M, Bolino, A., and Padua L (ORCID:0000-0003-2570-9326)

Abstract

BACKGROUND: Inherited peripheral neuropathies (IPNs) represent a broad group of genetically and clinically heterogeneous disorders, including axonal Charcot-Marie-Tooth type 2 (CMT2) and hereditary motor neuropathy (HMN). Approximately 60%-70% of cases with HMN/CMT2 still remain without a genetic diagnosis. Interestingly, mutations in HMN/CMT2 genes may also be responsible for motor neuron disorders or other neuromuscular diseases, suggesting a broad phenotypic spectrum of clinically and genetically related conditions. Thus, it is of paramount importance to identify novel causative variants in HMN/CMT2 patients to better predict clinical outcome and progression. METHODS: We designed a collaborative study for the identification of variants responsible for HMN/CMT2. We collected 15 HMN/CMT2 families with evidence for autosomal recessive inheritance, who had tested negative for mutations in 94 known IPN genes, who underwent whole-exome sequencing (WES) analyses. Candidate genes identified by WES were sequenced in an additional cohort of 167 familial or sporadic HMN/CMT2 patients using next-generation sequencing (NGS) panel analysis. RESULTS: Bioinformatic analyses led to the identification of novel or very rare variants in genes, which have not been previously associated with HMN/CMT2 (ARHGEF28, KBTBD13, AGRN and GNE); in genes previously associated with HMN/CMT2 but in combination with different clinical phenotypes (VRK1 and PNKP), and in the SIGMAR1 gene, which has been linked to HMN/CMT2 in only a few cases. These findings were further validated by Sanger sequencing, segregation analyses and functional studies. CONCLUSIONS: These results demonstrate the broad spectrum of clinical phenotypes that can be associated with a specific disease gene, as well as the complexity of the pathogenesis of neuromuscular disorders.

Published
2019

5. 6 Min walk test 12 month changes in DMD: correlation with the genotype

Author

Pane M, Mazzone E, Sormani MP, Scalise R, Berardinelli A, Messina S, Torrente Y, D'amico A, Doglio L, Viggiano E, D'Ambrosio P, Cavallaro P, Frosini S, Bello L, De Sanctis R, Fanelli L, Rolle E, Bianco F, Magri F, Vita GL, Motta MC, Donati MA, Mongini T, Pini a, Battini R, Pegoraro E, Previtali SC, Napolitano S, Bruno C, Comi GP, Bertini E, Mercuri E., POLITANO, Luisa, Pane, M, Mazzone, E, Sormani, Mp, Scalise, R, Berardinelli, A, Messina, S, Torrente, Y, D'Amico, A, Doglio, L, Viggiano, E, D'Ambrosio, P, Cavallaro, P, Frosini, S, Bello, L, De Sanctis, R, Fanelli, L, Rolle, E, Bianco, F, Magri, F, Vita, Gl, Motta, Mc, Donati, Ma, Mongini, T, Pini, A, Battini, R, Pegoraro, E, Previtali, Sc, Napolitano, S, Bruno, C, Politano, Luisa, Comi, Gp, Bertini, E, and Mercuri, E.

Published
2013

6. Brain connectivity abnormalities extend beyond the sensorimotor network in peripheral neuropathy

Author

Rocca MA, Valsasina P, Fazio R, Previtali SC, Messina R, FALINI , ANDREA, COMI , GIANCARLO, FILIPPI , MASSIMO, Rocca, Ma, Valsasina, P, Fazio, R, Previtali, Sc, Messina, R, Falini, Andrea, Comi, Giancarlo, and Filippi, Massimo

Subjects
Adult, Male, Analysis of Variance, Brain Mapping, Brain, Peripheral Nervous System Diseases, Middle Aged, Magnetic Resonance Imaging, Oxygen, Case-Control Studies, Neural Pathways, Image Processing, Computer-Assisted, Humans, Female, Nerve Net, Gait Disorders, Neurologic, Research Articles, Aged
Abstract

OBJECTIVES: To investigate, using resting state (RS) functional connectivity (FC), the selectivity of involvement of the sensorimotor network in patients with acquired (A) and with hereditary (H) peripheral neuropathies (PN) and the correlations of RS FC abnormalities with clinical impairment and structural brain damage. Temporal associations among RS networks were also explored. Experimental design: RS fMRI scans were acquired from 13 APN, 12 HPN, and 18 age‐ and sex‐matched healthy controls. Independent component analysis and functional network connectivity were used to investigate RS FC within and among RS networks with potential functional relevance. PRINCIPAL OBSERVATIONS: Compared to controls, patients had a decreased FC of the right precentral gyrus and an increased RS FC of the precuneus within the sensorimotor network. Both decreased and increased RS FC also involved the visual and auditory networks, which additionally had an increased coherence of function with the sensorimotor network (more pronounced in HPN). RS FC modifications in patients extended to several cognitive networks and were correlated with disease duration. In APN, they were also correlated with the severity of clinical impairment and corpus callosum atrophy. CONCLUSIONS: In PN, RS FC modifications extend beyond the sensorimotor network and involve other sensory and cognitive networks. The correlations between RS FC patterns and disease duration in patients as well as with clinical impairment in patients with APN suggest that modifications of FC might reflect an adaptive mechanism, which takes time to occur and helps to limit the clinical consequences of peripheral damage. Hum Brain Mapp 35:513–526, 2014. © 2012 Wiley Periodicals, Inc.

Published
2012

7. The exctracellular matrix affects axonal regeneration in peripheral neuropathies

Author

PREVITALI SC, MALAGUTI MC, RIVA N, SCARLATO M, DACCI P. DINA G, TRIOLO D, PORRELLO E, LORENZETTI I, FAZIO F, BOLINO A, QAUTTRINI A., COMI , GIANCARLO, Previtali, Sc, Malaguti, Mc, Riva, N, Scarlato, M, DACCI P., DINA G, Triolo, D, Porrello, E, Lorenzetti, I, Fazio, F, Comi, Giancarlo, Bolino, A, and Qauttrini, A.

Published
2008

8. Phenotypic clustering of lamin A/C mutations in neuromuscolar patients

Author

BENEDETTI S, MENDITTO I, DEGANO M, RODOLICO C, MERLINI L, D'AMICO A, PALMUCCI L, BERARDINELLI A, PEGORARO E, TREVISAN CP, MORANDI L, MORONI I, GALLUZZI G, BESTINI E, TOSCANO A, OLIVE M, BONNE G, MARI F, CALDARA R, FAZIO R, MAMMI I, CARRERA P, TONIOLO D, QUATTRINI A, FERRAI M, PREVITALI SC, COMI , GIANCARLO, Benedetti, S, Menditto, I, Degano, M, Rodolico, C, Merlini, L, D'Amico, A, Palmucci, L, Berardinelli, A, Pegoraro, E, Trevisan, Cp, Morandi, L, Moroni, I, Galluzzi, G, Bestini, E, Toscano, A, Olive, M, Bonne, G, Mari, F, Caldara, R, Fazio, R, Mammi, I, Carrera, P, Toniolo, D, Comi, Giancarlo, Quattrini, A, Ferrai, M, and Previtali, Sc

Published
2007

9. Autoimmunity in the peripheral nervous system

Author

QUATTRINI A, PREVITALI SC, KIESEIER BC, KIEFER R, HARTUNG HP, COMI , GIANCARLO, Quattrini, A, Previtali, Sc, Kieseier, Bc, Kiefer, R, Comi, Giancarlo, and Hartung, Hp

Published
2003

10. Autocrine and immune cell-derived BDNF in human skeletal muscle: implications for myogenesis and tissue regeneration

Author

Colombo, E, Bedogni, F, Lorenzetti, I, Landsberger, Nicoletta, Previtali, Sc, and Farina, C.

Subjects
Inflammation, Male, Myositis, Brain-Derived Neurotrophic Factor, Macrophages, T-Lymphocytes, Fluorescent Antibody Technique, Nerve Tissue Proteins, Receptors, Nerve Growth Factor, Flow Cytometry, Muscle Development, Real-Time Polymerase Chain Reaction, Immunohistochemistry, Cell Line, Autocrine Communication, Humans, Regeneration, Female, RNA Interference, Muscle, Skeletal, In Situ Hybridization, Aged
Abstract

The neurotrophin system has a role in skeletal muscle biology. Conditional depletion of BDNF in mouse muscle precursor cells alters myogenesis and regeneration in vivo. However, the expression, localization and function of BDNF in human skeletal muscle tissue is not known, so the relevance of the rodent findings for human muscle are unknown. Here we address this by combining ex vivo histological investigations on human biopsies with in vitro analyses of human primary myocytes. We found that BDNF was expressed by precursor and differentiated cells both in vitro and in vivo. Differential analysis of BDNF receptors showed expression of p75NTR and not of TrkB in myocytes, suggesting that the BDNF-p75NTR axis is predominant in human skeletal muscle cells. Several in vitro functional experiments demonstrated that BDNF gene silencing or protein blockade in myoblast cultures hampered myogenesis. Finally, histological investigations of inflammatory myopathy biopsies revealed that infiltrating immune cells localized preferentially near p75NTR-positive regenerating fibres and that they produced BDNF. In conclusion, BDNF is an autocrine factor for skeletal muscle cells and may regulate human myogenesis. Furthermore, the preferential localization of BDNF-producing immune cells near p75NTR-positive regenerating myofibres suggests that immune cell-derived BDNF may sustain tissue repair in inflamed muscle.

Published
2013

11. 6 minute walk test in duchenne MD patients with different mutations:12 month changes

Author

Pane, Marika, Mazzone, Elena Stacy, Sormani, Mp, Messina, S, Vita, Gl, Fanelli, L, Berardinelli, A, Torrente, Y, D'Amico, A, Lanzillotta, V, Viggiano, E, D'Ambrosio, P, Cavallaro, Fabio, Frosini, S, Bello, L, Bonfiglio, S, Scalise, Roberta, De Sanctis, R, Rolle, E, Bianco, F, Van der Haawue, M, Magri, F, Palermo, C, Rossi, F, Donati, Ma, Alfonsi, C, Sacchini, M, Arnoldi, Mt, Baranello, Giovanni, Mongini, T, Pini, A, Battini, Roberta, Pegoraro, E, Previtali, Sc, Napolitano, S, Bruno, C, Politano, L, Comi, Gp, Bertini, Enrico Silvio, Morandi, Laura, Gualandi, F, Ferlini, A, Goemans, N, Mercuri, Eugenio Maria, Pane, Marika (ORCID:0000-0002-4851-6124), Mercuri, Eugenio Maria (ORCID:0000-0002-9851-5365), Pane, Marika, Mazzone, Elena Stacy, Sormani, Mp, Messina, S, Vita, Gl, Fanelli, L, Berardinelli, A, Torrente, Y, D'Amico, A, Lanzillotta, V, Viggiano, E, D'Ambrosio, P, Cavallaro, Fabio, Frosini, S, Bello, L, Bonfiglio, S, Scalise, Roberta, De Sanctis, R, Rolle, E, Bianco, F, Van der Haawue, M, Magri, F, Palermo, C, Rossi, F, Donati, Ma, Alfonsi, C, Sacchini, M, Arnoldi, Mt, Baranello, Giovanni, Mongini, T, Pini, A, Battini, Roberta, Pegoraro, E, Previtali, Sc, Napolitano, S, Bruno, C, Politano, L, Comi, Gp, Bertini, Enrico Silvio, Morandi, Laura, Gualandi, F, Ferlini, A, Goemans, N, Mercuri, Eugenio Maria, Pane, Marika (ORCID:0000-0002-4851-6124), and Mercuri, Eugenio Maria (ORCID:0000-0002-9851-5365)

Abstract

OBJECTIVE: In the last few years some of the therapeutical approaches for Duchenne muscular dystrophy (DMD) are specifically targeting distinct groups of mutations, such as deletions eligible for skipping of individual exons. The aim of this observational study was to establish whether patients with distinct groups of mutations have different profiles of changes on the 6 minute walk test (6MWT) over a 12 month period. METHODS: The 6MWT was performed in 191 ambulant DMD boys at baseline and 12 months later. The results were analysed using a test for heterogeneity in order to establish possible differences among different types of mutations (deletions, duplications, point mutations) and among subgroups of deletions eligible to skip individual exons. RESULTS: At baseline the 6MWD ranged between 180 and 560,80 metres (mean 378,06, SD 74,13). The 12 month changes ranged between -325 and 175 (mean -10.8 meters, SD 69.2). Although boys with duplications had better results than those with the other types of mutations, the difference was not significant. Similarly, boys eligible for skipping of the exon 44 had better baseline results and less drastic changes than those eligible for skipping exon 45 or 53, but the difference was not significant. CONCLUSIONS: even if there are some differences among subgroups, the mean 12 month changes in each subgroup were all within a narrow Range: from the mean of the whole DMD cohort. This information will be of help at the time of designing clinical trials with small numbers of eligible patients.

Published
2014

12. LMNA-associated myopathies: the Italian experience in a large cohort of patients

Author

Maggi, L, D'Amico, A, Pini, A, Sivo, S, Pane, M, Ricci, G, Vercelli, L, D'Ambrosio, P, Travaglini, L, Sala, S, Brenna, G, Kapetis, D, Scarlato, M, Pegoraro, E, Ferrari, M, Toscano, A, Benedetti, S, Bernasconi, P, Colleoni, L, Lattanzi, G, Bertini, E, Mercuri, Eugenio Maria, Siciliano, G, Rodolico, C, Mongini, T, Politano, L, Previtali, Sc, Carboni, N, Mantegazza, R, Morandi, L., Mercuri, Eugenio Maria (ORCID:0000-0002-9851-5365), Maggi, L, D'Amico, A, Pini, A, Sivo, S, Pane, M, Ricci, G, Vercelli, L, D'Ambrosio, P, Travaglini, L, Sala, S, Brenna, G, Kapetis, D, Scarlato, M, Pegoraro, E, Ferrari, M, Toscano, A, Benedetti, S, Bernasconi, P, Colleoni, L, Lattanzi, G, Bertini, E, Mercuri, Eugenio Maria, Siciliano, G, Rodolico, C, Mongini, T, Politano, L, Previtali, Sc, Carboni, N, Mantegazza, R, Morandi, L., and Mercuri, Eugenio Maria (ORCID:0000-0002-9851-5365)

Abstract

Our aim was to conduct a comparative study in a large cohort of myopathic patients carrying LMNA gene mutations to evaluate clinical and molecular features associated with different phenotypes.

Published
2014

13. Importance of SPP1 genotype as a covariate in clinical trials in Duchenne muscular dystrophy

Author

Bello, L, Piva, L, Barp, A, Taglia, Andrea, Picillo, E, Vasco, Gessica, Pane, Marika, Previtali, Sc, Torrente, Y, Gazzerro, E, Motta, Mario, Grieco, Giovanni, Napolitano, S, Magri, F, D'Amico, Adele, Astrea, G, Messina, S, Sframeli, M, Vita, Gl, Boffi, Pietro, Mongini, T, Ferlini, A, Gualandi, F, Soraru', G, Ermani, M, Vita, G, Battini, R, Bertini, Enrico Silvio, Comi, Gp, Berardinelli, A, Minetti, C, Bruno, Carmelina, Mercuri, Eugenio Maria, Politano, L, Angelini, Carlo, Hoffman, Ep, Pegoraro, E., Pane, Marika (ORCID:0000-0002-4851-6124), Mercuri, Eugenio Maria (ORCID:0000-0002-9851-5365), Bello, L, Piva, L, Barp, A, Taglia, Andrea, Picillo, E, Vasco, Gessica, Pane, Marika, Previtali, Sc, Torrente, Y, Gazzerro, E, Motta, Mario, Grieco, Giovanni, Napolitano, S, Magri, F, D'Amico, Adele, Astrea, G, Messina, S, Sframeli, M, Vita, Gl, Boffi, Pietro, Mongini, T, Ferlini, A, Gualandi, F, Soraru', G, Ermani, M, Vita, G, Battini, R, Bertini, Enrico Silvio, Comi, Gp, Berardinelli, A, Minetti, C, Bruno, Carmelina, Mercuri, Eugenio Maria, Politano, L, Angelini, Carlo, Hoffman, Ep, Pegoraro, E., Pane, Marika (ORCID:0000-0002-4851-6124), and Mercuri, Eugenio Maria (ORCID:0000-0002-9851-5365)

Abstract

To test the effect of the single nucleotide polymorphism -66 T>G (rs28357094) in the osteopontin gene (SPP1) on functional measures over 12 months in Duchenne muscular dystrophy (DMD).

Published
2012

14. Expression of laminin receptors in schwann cell differentiation: evidence for distinct roles

Author

Previtali, S, Nodari, A, Taveggia, C, Pardini, C, Dina, G, Villa, A, Wrabetz, L, Quattrini, A, Feltri, M, Previtali, SC, Feltri, ML, VILLA, ANTONELLO, Previtali, S, Nodari, A, Taveggia, C, Pardini, C, Dina, G, Villa, A, Wrabetz, L, Quattrini, A, Feltri, M, Previtali, SC, Feltri, ML, and VILLA, ANTONELLO

Abstract

Schwann cells require laminin-2 throughout nerve development, because mutations in the alpha2 chain in dystrophic mice interfere with sorting of axons before birth and formation of myelin internodes after birth. Mature Schwann cells express several laminin receptors, but their expression and roles in development are poorly understood. Therefore, we correlated the onset of myelination in nerve and synchronized myelinating cultures to the appearance of integrins and dystroglycan in Schwann cells. Only alpha6beta1 integrin is expressed before birth, whereas dystroglycan and alpha6beta4 integrin appear perinatally, just before myelination. Although dystroglycan is immediately polarized to the outer surface of Schwann cells, alpha6beta4 appears polarized only after myelination. We showed previously that Schwann cells lacking beta1 integrin do not relate properly to axons before birth. Here we show that the absence of beta1 before birth is not compensated by other laminin receptors, whereas coexpression of both dystroglycan and beta4 integrin is likely required for beta1-null Schwann cells to myelinate after birth. Finally, both beta1-null and dystrophic nerves contain bundles of unsorted axons, but they are predominant in different regions: in spinal roots in dystrophic mice and in nerves in beta1-null mice. We show that differential compensation by laminin-1, but not laminin receptors may partially explain this. These data suggest that the action of laminin is mediated by beta1 integrins during axonal sorting and by dystroglycan, alpha6beta1, and alpha6beta4 integrins during myelination.

Published
2003

15. Autoantibodies to amphiphysin I and amphiphysin II in a patient with sensory-motor neuropathy

Author

Perego, L, Previtali, S, Nemni, R, Longhi, R, Carandente, O, Saibene, A, Sciolla, R, Villa, A, Gai, P, Panzeri, C, Dell'Antonio, G, Quattrini, A, Folli, F, Previtali, SC, Folli, F., VILLA, ANTONELLO, Perego, L, Previtali, S, Nemni, R, Longhi, R, Carandente, O, Saibene, A, Sciolla, R, Villa, A, Gai, P, Panzeri, C, Dell'Antonio, G, Quattrini, A, Folli, F, Previtali, SC, Folli, F., and VILLA, ANTONELLO

Abstract

A proportion of patients with peripheral neuropathies has circulating autoantibodies directed against neural antigens. In some cases, autoantibodies may play a pathogenic role. We studied a patient with a progressive sensory-motor axonal neuropathy of unknown etiology, looking for circulating autoantibodies against neural antigens and we showed that the patient's serum contained anti-amphiphysin I (AMP I) and amphiphysin II (AMP II) autoantibodies. A sural nerve biopsy revealed an axonal neuropathy. Indirect immunofluorescence experiments with the patient's serum showed a staining of rat axons due to alpha-AMP I autoantibodies and a specific labelling of cytoplasm and Schmidt-Lanterman incisures of Schwann cells due to alpha-AMP II autoantibodies. In conclusion we identified a patient affected by a sensory-motor neuropathy with autoantibodies against both AMP I and AMP II.

Published
2002

17. Epitope-tagged P-0 glycoprotein causes Charcot-Marie-Tooth-like neuropathy in transgenic mice

Author

Previtali, S, Quattrini, A, Fasolini, M, Panzeri, M, Villa, A, Filbin, M, Li, W, Chiu, S, Messing, A, Wrabetz, L, Feltri, M, Previtali, SC, Panzeri, MC, Filbin, MT, Li, WH, Chiu, SY, Feltri, ML, VILLA, ANTONELLO, Previtali, S, Quattrini, A, Fasolini, M, Panzeri, M, Villa, A, Filbin, M, Li, W, Chiu, S, Messing, A, Wrabetz, L, Feltri, M, Previtali, SC, Panzeri, MC, Filbin, MT, Li, WH, Chiu, SY, Feltri, ML, and VILLA, ANTONELLO

Abstract

In peripheral nerve myelin, the intraperiod line results from compaction of the extracellular space due to homophilic adhesion between extracellular domains (ECD) of the protein zero (P-0) glycoprotein. Point mutations in this region of P-0 cause human hereditary demyelinating neuropathies such as Charcot-Marie-Tooth. We describe transgenic mice expressing a full-length P-0 modified in the ECD with a myc epitope tag. The presence of the myc sequence caused a dysmyelinating peripheral neuropathy similar to two distinct subtypes of Charcot-Marie-Tooth. with hypomyelination, altered intraperiod lines, and tomacula (thickened myelin). The tagged protein was incorporated into myelin and was associated with the morphological abnormalities. In vivo and in vitro experiments showed that P(0)myc retained partial adhesive function, and suggested that the transgene inhibits P-0-mediated adhesion in a dominant-negative fashion. These mice suggest new mechanisms underlying both the pathogenesis of P-0 ECD mutants and the normal interactions of P-0 in the myelin sheath.

Published
2000

23. Long-term natural history data in Duchenne muscular dystrophy ambulant patients with mutations amenable to skip exons 44, 45, 51 and 53

Author

Brogna, Claudia, Coratti, Giorgia, Pane, Marika, Ricotti, Valeria, Messina, Sonia, D'Amico, Adele, Bruno, Claudio, Vita, Gianluca, Berardinelli, Angela, Mazzone, Elena, Magri, Francesca, Ricci, Federica, Mongini, Tiziana, Battini, Roberta, Bello, Luca, Pegoraro, Elena, Baranello, Giovanni, Previtali, Stefano C, Politano, Luisa, Comi, Giacomo P, Sansone, Valeria A, Donati, Alice, Bertini, Enrico, Muntoni, Francesco, Goemans, Nathalie, Mercuri, Eugenio, Lanzillotta, Valentina, Viggiano, Emanuela, Frosini, Silvia, Barp, Andrea, Rolle, Enrica, Rossi, Francesca, Arnoldi, Maria Teresa, Fanelli, Lavinia, Forcina, Nicola, Salmin, Francesca, Albamonte, Emilio, Gorni, Ksenija, Dominges, Joana Pisco, van der Hauwe, Marleen, Consulo, Chiara, Di Bella, Vincenzo, Rossi, Marta, Gardani, Alice, Colia, Giulia, Carlesi, Adelina, Brogna, C, Coratti, G, Pane, M, Ricotti, V, Messina, S, D'Amico, A, Bruno, C, Vita, G, Berardinelli, A, Mazzone, E, Magri, F, Ricci, F, Mongini, T, Battini, R, Bello, L, Pegoraro, E, Baranello, G, Previtali, Sc, Politano, L, Comi, Gp, Sansone, Va, Donati, A, Bertini, E, Muntoni, F, Goemans, N, Mercuri, E, and on behalf on the International DMD, Group.

Subjects
Male, 0301 basic medicine, Heredity, Physiology, Epidemiology, Genetic Linkage, Duchenne muscular dystrophy, Walking, Gene mutation, Bioinformatics, Settore MED/03 - GENETICA MEDICA, Biochemistry, Muscular Dystrophies, Cohort Studies, Dystrophin, 6-MINUTE WALK TEST, Exon, 0302 clinical medicine, Medicine and Health Sciences, Longitudinal Studies, Muscular Dystrophy, Prospective Studies, Muscular dystrophy, Child, Sequence Deletion, Multidisciplinary, biology, Settore MED/48 - SCIENZE INFERMIERISTICHE E TECNICHE NEURO-PSICHIATRICHE E RIABILITATIVE, Organic Compounds, Exons, Multidisciplinary Sciences, Child, Preschool, Disease Progression, Humans, Muscular Dystrophy, Duchenne, Mutation, Chemistry, Settore MED/26 - NEUROLOGIA, Neurology, X-Linked Traits, Sex Linkage, Physical Sciences, Science & Technology - Other Topics, Medicine, Steroids, Exon skipping, Research Article, Science, Patient Advocacy, 03 medical and health sciences, Settore MED/39 - NEUROPSICHIATRIA INFANTILE, Genetics, medicine, Medical history, Preschool, Clinical Genetics, Science & Technology, DMD, exon skipping , exon 44, exon 45, Biological Locomotion, business.industry, Duchenne Muscular Dystrophy, Dystrophin, Antisense Oligonucleotide, Organic Chemistry, Chemical Compounds, Correction, Biology and Life Sciences, Proteins, Human Genetics, QUANTIFICATION, Duchenne, medicine.disease, Human genetics, Health Care, Cytoskeletal Proteins, Natural History of Disease, 030104 developmental biology, biology.protein, business, 030217 neurology & neurosurgery
Abstract

INTRODUCTION: The aim of this international collaborative effort was to report 36-month longitudinal changes using the 6MWT in ambulant patients affected by Duchenne muscular dystrophy amenable to skip exons 44, 45, 51 or 53. MATERIALS AND METHODS: Of the 92 patients included in the study, 24 had deletions amenable to skip exon 44, 27 exon 45, 18 exon 51, and 28 exon 53. Five patients with a single deletion of exon 52 were counted in both subgroups skipping exon 51 and 53. RESULTS: The difference between subgroups amenable to skip different exons was not significant at 12 months but became significant at both 24 (p≤0.05) and 36 months (p≤0.01). DISCUSSION: Mutations amenable to skip exon 53 had lower baseline values and more negative changes than the other subgroups while those amenable to skip exon 44 had better results both at baseline and at follow up. Deletions amenable to skip exon 45 were associated with a more variable pattern of progression. Single exon deletions were more often associated with less drastic changes but this was not always true in individual cases. CONCLUSION: Our results confirm that the progression of disease can differ between patients with different deletions, although the changes only become significant from 24 months onwards. This information is relevant because there are current clinical trials specifically targeting patients with these subgroups of mutations. ispartof: PLOS ONE vol:14 issue:6 ispartof: location:United States status: published

Published
2019

24. Muscle MRI findings in facioscapulohumeral muscular dystrophy

Author

Lucia Morandi, Lorenzo Maggi, Giandomenico Caliendo, Barbara Pasanisi, Simonetta Gerevini, Stefano C. Previtali, Andrea Falini, Mariangela Cava, Marina Scarlato, Gerevini, S, Scarlato, M, Maggi, L, Cava, M, Caliendo, G, Pasanisi, B, Falini, Andrea, Previtali, Sc, and Morandi, L.

Subjects
musculoskeletal diseases, Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Pathology, Adolescent, Subcutaneous Fat, Intermediate Back Muscles, Muscle disorder, Muscular Dystrophies, 030218 nuclear medicine & medical imaging, Diagnosis, Differential, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Atrophy, medicine, Facioscapulohumeral muscular dystrophy, Edema, Humans, Radiology, Nuclear Medicine and imaging, Whole Body Imaging, Muscular dystrophy, Muscle, Skeletal, Muscle contracture, Aged, Muscle Weakness, medicine.diagnostic_test, business.industry, Muscle weakness, Magnetic resonance imaging, General Medicine, Middle Aged, medicine.disease, Magnetic Resonance Imaging, Muscular Dystrophy, Facioscapulohumeral, nervous system diseases, Adipose Tissue, Lower Extremity, Superficial Back Muscles, Female, Radiology, medicine.symptom, business, 030217 neurology & neurosurgery
Abstract

Facioscapulohumeral muscular dystrophy (FSHD) is characterized by extremely variable degrees of facial, scapular and lower limb muscle involvement. Clinical and genetic determination can be difficult, as molecular analysis is not always definitive, and other similar muscle disorders may have overlapping clinical manifestations. Whole-body muscle MRI examination for fat infiltration, atrophy and oedema was performed to identify specific patterns of muscle involvement in FSHD patients (30 subjects), and compared to a group of control patients (23) affected by other myopathies (NFSHD). In FSHD patients, we detected a specific pattern of muscle fatty replacement and atrophy, particularly in upper girdle muscles. The most frequently affected muscles, including paucisymptomatic and severely affected FSHD patients, were trapezius, teres major and serratus anterior. Moreover, asymmetric muscle involvement was significantly higher in FSHD as compared to NFSHD patients. In conclusion, muscle MRI is very sensitive for identifying a specific pattern of involvement in FSHD patients and in detecting selective muscle involvement of non-clinically testable muscles. Muscle MRI constitutes a reliable tool for differentiating FSHD from other muscular dystrophies to direct diagnostic molecular analysis, as well as to investigate FSHD natural history and follow-up of the disease. • Muscle MRI identifies a specific pattern of muscle involvement in FSHD patients. • Muscle MRI may predict FSHD in asymptomatic and severely affected patients. • Muscle MRI of upper girdle better predicts FSHD. • Muscle MRI may differentiate FSHD from other forms of muscular dystrophy. • Muscle MRI may show the involvement of non-clinical testable muscles.

Published
2016

25. Importance of SPP1 genotype as a covariate in clinical trials in Duchenne muscular dystrophy

Author

P Boffi, Corrado Angelini, Luisa Politano, Guja Astrea, Eugenio Mercuri, Adele D'Amico, Tiziana Mongini, Marika Pane, Alessandra Ferlini, Giuseppe Vita, Sara Napolitano, Mario Ermani, Yvan Torrente, Francesca Gualandi, Antonella Taglia, Gaetano S. Grieco, Gian Luca Vita, Gianni Sorarù, Eric P. Hoffman, Angela Berardinelli, Andrea Barp, Esther Picillo, Gessica Vasco, Claudio Bruno, Roberta Battini, Stefano C. Previtali, Enrico Bertini, Giacomo P. Comi, Francesca Magri, Sonia Messina, Luca Bello, Luisa Piva, Maria Chiara Motta, Maria Sframeli, Carlo Minetti, Elisabetta Gazzerro, Elena Pegoraro, Bello, L, Piva, L, Barp, A, Taglia, A, Picillo, E, Vasco, G, Pane, M, Previtali, Sc, Torrente, Y, Gazzerro, E, Motta, Mc, Grieco, G, Napolitano, S, Magri, F, D'Amico, A, Astrea, G, Messina, S, Sframeli, M, Vita, Gl, Boffi, P, Mongini, T, Ferlini, A, Gualandi, F, Soraru', G, Ermani, M, Vita, G, Battini, R, Bertini, E, Comi, Gp, Berardinelli, A, Minetti, C, Bruno, C, Mercuri, E, Politano, Luisa, Angelini, C, Hoffman, Ep, and Pegoraro, E.

Subjects
Adult, medicine.medical_specialty, Adolescent, Duchenne muscular dystrophy, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, Settore MED/39 - NEUROPSICHIATRIA INFANTILE, Internal medicine, Genotype, medicine, Humans, Multicenter Studies as Topic, Longitudinal Studies, Muscular Dystrophy, Polymorphism, Child, Preschool, Retrospective Studies, Clinical Trials as Topic, business.industry, Genetic Variation, Retrospective cohort study, Articles, Single Nucleotide, Duchenne, medicine.disease, Muscular Dystrophy, Duchenne, Clinical trial, Child, Preschool, Ambulatory, Cohort, Physical therapy, Osteopontin, Neurology (clinical), business, Student's t-test
Abstract

Objective: To test the effect of the single nucleotide polymorphism −66 T>G (rs28357094) in the osteopontin gene ( SPP1 ) on functional measures over 12 months in Duchenne muscular dystrophy (DMD). Methods: This study was conducted on a cohort of ambulatory patients with DMD from a network of Italian neuromuscular centers, evaluated longitudinally with the North Star Ambulatory Assessment (NSAA) and the 6-Minute Walk Test (6MWT) at study entry and after 12 months. Genotype at rs28357094 was determined after completion of the clinical evaluations. Patients were stratified in 2 groups according to a dominant model (TT homozygotes vs TG heterozygotes and GG homozygotes) and clinical data were retrospectively compared between groups. Results: Eighty patients were selected (age 4.1–19.3 years; mean 8.3 ± 2.7 SD). There were no differences in age or steroid treatment between the 2 subgroups. Paired t test showed a significant difference in both NSAA ( p = 0.013) and 6MWT ( p = 0.03) between baseline and follow-up after 12 months in patients with DMD carrying the G allele. The difference was not significant in the T subgroup. The analysis of covariance using age and baseline values as covariate and SPP1 genotype as fixed effect showed that these parameters are significantly correlated with the 12-month values. Conclusions: These data provide evidence of the role of SPP1 genotype as a disease modifier in DMD and support its relevance in the selection of homogeneous groups of patients for future clinical trials.

Published
2012

26. Protein profiling reveals energy metabolism and cytoskeletal protein alterations in LMNA mutation carriers

Author

Angela Bachi, Stefano C. Previtali, Elena Fattore, M. Ferrari, Gianpaolo Zerbini, Sara Benedetti, Isabella Fermo, Cinzia Magagnotti, Michela Riba, Annapaola Andolfo, Magagnotti, C, Bachi, A, Zerbini, G, Fattore, E, Fermo, I, Riba, M, Previtali, Sc, Ferrari, Maurizio, Andolfo, A, and Benedetti, S.

Subjects
Adult, Male, Proteomics, Nuclear Envelope, Protein Array Analysis, Skin fibroblasts, Biology, medicine.disease_cause, LMNA, medicine, Humans, Muscular dystrophy, Gene, Molecular Biology, Skin, Genetics, Mutation, Mass spectrometry, Laminopathies, Nuclear Proteins, Neuromuscular Diseases, Fibroblasts, Middle Aged, Familial partial lipodystrophy, medicine.disease, Lamin Type A, Phenotype, Muscular Dystrophy, Emery-Dreifuss, LMNA mutation carriers, Cytoskeletal Proteins, Oxidative Stress, Molecular Medicine, Female, Energy Metabolism, Lamin
Abstract

Nuclear envelope-related muscular dystrophies, in particular those referred to as laminopathies, are relatively novel and unclear diseases, also considering the increasing number of mutations identified so far in genes of the nuclear envelope. As regard LMNA gene, only tentative relations between phenotype, type and localization of the mutations have been established in striated muscle diseases, while laminopathies affecting adipose tissue, peripheral nerves or progerioid syndromes could be linked to specific genetic variants. This study describes the biochemical phenotype of neuromuscular laminopathies in samples derived from LMNA mutant patients. Since it has been reported that nuclear alterations, due to LMNA defects, are present also in fibroblasts from Emery–Dreifuss muscular dystrophy and familial partial lipodystrophy patients, we analyzed 2D-maps of skin fibroblasts of patients carrying 12 different LMNA mutations spread along the entire gene. To recognize distinctive proteins underlying affected biochemical pathways, we compared them with fibroblasts from healthy controls and, more importantly, fibroblasts from patients with non-lamin related neuromuscular disorders. We found less abundance of cytoskeletal/structural proteins, confirming a dominant role for Lamin A/C in structural support of nuclear architecture. Interestingly, we also established significant changes in the expression of proteins involved in cellular energy production and oxidative stress response. To our knowledge, this is the first report where proteomics was applied to characterize ex-vivo cells from LMNA patients, suggesting that this may represent a new approach to better understand the molecular mechanisms of these rare diseases and facilitate the development of novel therapeutic treatments.

Published
2012
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27. Motor nerve biopsy: Clinical usefulness and histopathological criteria

Author

Stefano C. Previtali, Angelo Quattrini, B. Sferrazza, C. Casellato, Sandro Iannaccone, Marina Scarlato, Eduardo Nobile-Orazio, Nilo Riva, Massimo Corbo, Giancarlo Comi, A. Lazzerini, Federica Cerri, Riva, N, Iannaccone, S, Corbo, M, Casellato, C, Sferrazza, B, Lazzerini, A, Scarlato, M, Cerri, F, Previtali, Sc, Nobile Orazio, E, Comi, Giancarlo, and Quattrini, A.

Subjects
medicine.medical_specialty, medicine.diagnostic_test, business.industry, Biopsy, Neuromuscular Junction, Motor nerve, Efferent Pathways, Lower motor neuron, Surgery, medicine.anatomical_structure, Neurology, Peripheral nervous system, Peripheral Nervous System, medicine, Humans, Gracilis muscle, Obturator nerve, Neurology (clinical), Motor Neuron Disease, Differential diagnosis, Muscle, Skeletal, Obturator Nerve, business
Abstract

Early differential diagnosis of motor neuropathies (MN) and lower motor neuron diseases (LMND) is important, as prognosis and therapeutic approaches are different. We evaluated the diagnostic contribution of the biopsy of the motor branch of the obturator nerve and gracilis muscle in 21 consecutive patients in which, after proper clinical and neurophysiological studies, the differential diagnosis was still open. At baseline, motor biopsy was performed; diagnostic confirmation was obtained by 2-year clinical follow-up. Our results support the usefulness of this diagnostic procedure for selected cases of MN and LMND.

Published
2010

28. Intra-arterial transplantation of HLA-matched donor mesoangioblasts in Duchenne muscular dystrophy

Author

Cossu, Giulio, Previtali, Stefano C, Napolitano, Sara, Cicalese, Maria Pia, Tedesco, Francesco Saverio, Nicastro, Francesca, Noviello, Maddalena, Roostalu, Urmas, Natali Sora, Maria Grazia, Scarlato, Marina, De Pellegrin, Maurizio, Godi, Claudia, Giuliani, Serena, Ciotti, Francesca, Tonlorenzi, Rossana, Lorenzetti, Isabella, Rivellini, Cristina, Benedetti, Sara, Gatti, Roberto, Marktel, Sarah, Mazzi, Benedetta, Tettamanti, Andrea, Ragazzi, Martina, Imro, Maria Adele, Marano, Giuseppina, Ambrosi, Alessandro, Fiori, Rossana, Sormani, Maria Pia, Bonini, Chiara, Venturini, Massimo, Politi, Letterio S, Torrente, Yvan, Ciceri, Fabio, Cossu, G, Previtali, Sc, Napolitano, S, Cicalese, Mp, Tedesco, F, Nicastro, F, Noviello, M, Roostalu, U, Natali Sora, Mg, Scarlato, M, De Pellegrin, M, Godi, C, Giuliani, S, Ciotti, F, Tonlorenzi, R, Lorenzetti, I, Rivellini, C, Benedetti, S, Gatti, R, Marktel, S, Mazzi, B, Tettamanti, A, Ragazzi, M, Imro, Ma, Marano, G, Ambrosi, Alessandro, Fiori, R, Sormani, Mp, Bonini, MARIA CHIARA, Venturini, M, Politi, L, Torrente, Y, and Ciceri, Fabio

Subjects
medicine.medical_specialty, Duchenne muscular dystrophy, Cell- and Tissue-Based Therapy, dystrophin, 03 medical and health sciences, 0302 clinical medicine, Clinical endpoint, Humans, Infusions, Intra-Arterial, Medicine, mesoangioblast, MRI, Duchenne, cell therapy, Muscular dystrophy, Cell therapy, Dystrophin, Mesoangioblast, 030304 developmental biology, 0303 health sciences, Muscle biopsy, medicine.diagnostic_test, biology, business.industry, Histocompatibility Testing, medicine.disease, 3. Good health, Surgery, Muscular Dystrophy, Duchenne, Clinical trial, Transplantation, biology.protein, Molecular Medicine, Corrigendum, business, 030217 neurology & neurosurgery
Abstract

Intra-arterial transplantation of mesoangioblasts proved safe and partially efficacious in preclinical models of muscular dystrophy. We now report the first-in-human, exploratory, non-randomized open-label phase I-IIa clinical trial of intra-arterial HLA-matched donor cell transplantation in 5 Duchenne patients. We administered escalating doses of donor-derived mesoangioblasts in limb arteries under immunosuppressive therapy (tacrolimus). Four consecutive infusions were performed at 2-month intervals, preceded and followed by clinical, laboratory, and muscular MRI analyses. Two months after the last infusion, a muscle biopsy was performed. Safety was the primary endpoint. The study was relatively safe: One patient developed a thalamic stroke with no clinical consequences and whose correlation with mesoangioblast infusion remained unclear. MRI documented the progression of the disease in 4/5 patients. Functional measures were transiently stabilized in 2/3 ambulant patients, but no functional improvements were observed. Low level of donor DNA was detected in muscle biopsies of 4/5 patients and donor-derived dystrophin in 1. Intra-arterial transplantation of donor mesoangioblasts in human proved to be feasible and relatively safe. Future implementation of the protocol, together with a younger age of patients, will be needed to approach efficacy.

Published
2015

29. LMNA-associated myopathies: the Italian experience in a large cohort of patients

Author

Lorena Travaglini, Tiziana Mongini, Elena Pegoraro, Giulia Ricci, Pia Bernasconi, Paola D'Ambrosio, Liliana Vercelli, Dimos Kapetis, Nicola Carboni, Antonio Toscano, Renato Mantegazza, Enrico Bertini, Sara Benedetti, Maurizio Ferrari, Stefano C. Previtali, Lucia Morandi, Simone Sala, Greta Brenna, Giovanna Lattanzi, Luisa Politano, Carmelo Rodolico, Antonella Pini, Adele D'Amico, Serena Sivo, Lorenzo Maggi, Marika Pane, Eugenio Mercuri, Gabriele Siciliano, Marina Scarlato, Lara Colleoni, Maggi, L, D'Amico, A, Pini, A, Sivo, S, Pane, M, Ricci, G, Vercelli, L, D'Ambrosio, P, Travaglini, L, Sala, S, Brenna, G, Kapetis, D, Scarlato, M, Pegoraro, E, Ferrari, Maurizio, Toscano, A, Benedetti, S, Bernasconi, P, Colleoni, L, Lattanzi, G, Bertini, E, Mercuri, E, Siciliano, G, Rodolico, C, Mongini, T, Politano, L, Previtali, Sc, Carboni, N, Mantegazza, R, Morandi, L., Ferrari, M, and Politano, Luisa

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, Mutation, Missense, Aged, Aged, 80 and over, Child, Child, Preschool, Cohort Studies, Female, Humans, Italy, Lamin Type A, Middle Aged, Muscular Dystrophies, Limb-Girdle, Muscular Dystrophy, Emery-Dreifuss, Pedigree, Phenotype, Young Adult, Cardiomyopathies, Muscular Diseases, Muscular Dystrophies, Gene mutation, Gastroenterology, Frameshift mutation, LMNA, Limb-Girdle, Settore MED/39 - NEUROPSICHIATRIA INFANTILE, Internal medicine, medicine, 80 and over, Missense mutation, Muscular Dystrophy, Muscular dystrophy, Myopathy, Preschool, business.industry, Emery-Dreifuss, Retrospective cohort study, medicine.disease, Mutation, Congenital muscular dystrophy, Physical therapy, Neurology (clinical), medicine.symptom, Missense, business
Abstract

Objectives: Our aim was to conduct a comparative study in a large cohort of myopathic patients carrying LMNA gene mutations to evaluate clinical and molecular features associated with different phenotypes. Methods: We performed a retrospective cohort study of 78 myopathic patients with LMNA mutation and 30 familial cases with LMNA mutation without muscle involvement. We analyzed features characterizing the various forms of LMNA -related myopathy through correlation statistics. Results: Of the 78 patients, 37 (47%) had limb-girdle muscular dystrophy 1B (LGMD1B), 18 (23%) congenital muscular dystrophy (MDCL), 17 (22%) autosomal dominant Emery-Dreifuss muscular dystrophy 2 (EDMD2), and 6 (8%) an atypical myopathy. The myopathic phenotypes shared a similar cardiac impairment. Cardioverter defibrillator or pacemaker was implanted in 41 (53%) myopathic patients compared to 7 (23%) familial cases without muscle involvement ( p = 0.005). Heart transplantation was performed in 8 (10.3%) myopathic patients and in none of the familial cases. Ten (12.8%) myopathic patients died; there were no deaths among the familial cases ( p = 0.032). Missense mutations were found in 14 patients (82%) with EDMD2 and 14 patients (78%) with MDCL compared to 17 patients (45%) with LGMD1B and 4 (67%) atypical patients. Frameshift mutations were detected in 17 (45%) LGMD1B compared to 3 (18%) EDMD2, 1 (6%) MDCL, and 2 (33%) with atypical myopathy ( p = 0.021). Furthermore, frameshift mutations were found in 30 of 73 patients (41%) with heart involvement compared to 4 of 35 (11%) without heart involvement ( p = 0.004). Conclusions: Our data provided new insights in LMNA -related myopathies, whose natural history appears to be dominated by cardiac involvement and related complications.

Published
2014

30. 6 minute walk test in Duchenne MD patients with different mutations: 12 month changes

Author

Claudio Bruno, Tiziana Mongini, Silvia Frosini, Sonia Messina, Enrica Rolle, Stefano C. Previtali, Francesca Gualandi, Roberto De Sanctis, Marika Pane, Gian Luca Vita, Filippo Cavallaro, Adele D'Amico, Paola D'Ambrosio, Angela Berardinelli, Roberta Battini, Luca Bello, Giovanni Baranello, Lucia Morandi, Giacomo P. Comi, Luisa Politano, Maria Teresa Arnoldi, Enrico Bertini, Elena S. Mazzone, Francesca Rossi, Concetta Palermo, Nathalie Goemans, Marlene Van der Haawue, Antonella Pini, Maria Alice Donati, Alessandra Ferlini, Yvan Torrente, Elena Pegoraro, Chiara Alfonsi, Roberta Scalise, Maria Pia Sormani, Eugenio Mercuri, Francesca Magri, Serena Bonfiglio, Michele Sacchini, Valentina Lanzillotta, Sara Napolitano, Lavinia Fanelli, Flaviana Bianco, Emanuela Viggiano, Pane, M, Mazzone, E, Sormani, Mp, Messina, S, Vita, Gl, Fanelli, L, Berardinelli, A, Torrente, Y, D'Amico, A, Lanzillotta, V, Viggiano, E, D'Ambrosio, P, Cavallaro, F, Frosini, S, Bello, L, Bonfiglio, S, Scalise, R, De Sanctis, R, Rolle, E, Bianco, F, Van der Haawue, M, Magri, F, Palermo, C, Rossi, F, Donati, Ma, Alfonsi, C, Sacchini, M, Arnoldi, Mt, Baranello, G, Mongini, T, Pini, A, Battini, R, Pegoraro, E, Previtali, Sc, Napolitano, S, Bruno, C, Politano, Luisa, Comi, Gp, Bertini, E, Morandi, L, Gualandi, F, Ferlini, A, Goemans, N, and Mercuri, E.

Subjects
Male, Time Factors, Duchenne muscular dystrophy, Muscular Dystrophies, Cohort Studies, Dystrophin, inglese, Muscular dystrophy, Child, Multidisciplinary, Statistics, Neuromuscular Diseases, Neurology, Child, Preschool, Cohort, Observational Studies, Medicine, Cohort study, Research Article, Test Evaluation, medicine.medical_specialty, Adolescent, Clinical Research Design, Science, Nonsense mutation, changes, Biostatistics, walking, Settore MED/39 - NEUROPSICHIATRIA INFANTILE, Genetic Mutation, Diagnostic Medicine, Internal medicine, medicine, Genetics, Humans, Biology, Clinical Genetics, business.industry, Point mutation, Human Genetics, X-Linked, medicine.disease, Clinical trial, Muscular Dystrophy, Duchenne, Mutation, Physical therapy, Observational study, business, Mathematics
Abstract

ObjectiveIn the last few years some of the therapeutical approaches for Duchenne muscular dystrophy (DMD) are specifically targeting distinct groups of mutations, such as deletions eligible for skipping of individual exons. The aim of this observational study was to establish whether patients with distinct groups of mutations have different profiles of changes on the 6 minute walk test (6MWT) over a 12 month period.MethodsThe 6MWT was performed in 191 ambulant DMD boys at baseline and 12 months later. The results were analysed using a test for heterogeneity in order to establish possible differences among different types of mutations (deletions, duplications, point mutations) and among subgroups of deletions eligible to skip individual exons.ResultsAt baseline the 6MWD ranged between 180 and 560,80 metres (mean 378,06, SD 74,13). The 12 month changes ranged between -325 and 175 (mean -10.8 meters, SD 69.2). Although boys with duplications had better results than those with the other types of mutations, the difference was not significant. Similarly, boys eligible for skipping of the exon 44 had better baseline results and less drastic changes than those eligible for skipping exon 45 or 53, but the difference was not significant.Conclusionseven if there are some differences among subgroups, the mean 12 month changes in each subgroup were all within a narrow Range: from the mean of the whole DMD cohort. This information will be of help at the time of designing clinical trials with small numbers of eligible patients.

Published
2014

31. Analyzing histopathological features of rare charcot-marie-tooth neuropathies to unravel their pathogenesis

Author

Luigi M.E. Grimaldi, Elisabetta Munerati, Sara Benedetti, Maurizio Ferrari, Angelo Quattrini, Lara Piantoni, Maria Chiara Malaguti, Nilo Riva, Silvia Coviello, Marina Scarlato, Ivana Spiga, Federica Cerri, Maurizio De Pellegrin, Alessandra Bolino, Maria Giovanna Marrosu, Patrizia Dacci, Raffaella Fazio, Emanuela Di Pierri, Giancarlo Comi, Maria Grazia Natali Sora, Stefano C. Previtali, Benedetti, S, Previtali, Sc, Coviello, S, Scarlato, M, Cerri, F, DI PIERRI, E, Piantoni, L, Spiga, I, Fazio, R, Riva, N, NATALI SORA, Mg, Dacci, P, Malaguti, Mc, Munerati, E, Grimaldi, Lm, Marrosu, Mg, DE PELLEGRIN, M, Ferrari, Maurizio, Comi, Giancarlo, Quattrini, A, and Bolino, A.

Subjects
Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Pathology, medicine.medical_specialty, Adolescent, DNA Mutational Analysis, MFN2, HSP27 Heat-Shock Proteins, Sural nerve, medicine.disease_cause, Connexins, GTP Phosphohydrolases, Central nervous system disease, Pathogenesis, Cohort Studies, Mitochondrial Proteins, Young Adult, Degenerative disease, Arts and Humanities (miscellaneous), Sural Nerve, Charcot-Marie-Tooth Disease, Biopsy, medicine, Humans, Child, Pathological, Heat-Shock Proteins, Aged, Retrospective Studies, Aged, 80 and over, Mutation, medicine.diagnostic_test, business.industry, Intracellular Signaling Peptides and Proteins, Membrane Proteins, Middle Aged, medicine.disease, Phosphoproteins, Ether-A-Go-Go Potassium Channels, nervous system diseases, Female, Neurology (clinical), business, Demyelinating Diseases, Molecular Chaperones, Transcription Factors
Abstract

Background Charcot-Marie-Tooth (CMT) neuropathies are very heterogeneous disorders from both a clinical and genetic point of view. The CMT genes identified so far encode different proteins that are variably involved in regulating Schwann cells and/or axonal functions. However, the function of most of these proteins still remains to be elucidated. Objective To characterize a large cohort of patients with demyelinating, axonal, and intermediate forms of CMT neuropathy. Design A cohort of 131 unrelated patients were screened for mutations in 12 genes responsible for CMT neuropathies. Demyelinating, axonal, and intermediate forms of CMT neuropathy were initially distinguished as usual on the basis of electrophysiological criteria and clinical evaluation. A sural nerve biopsy was also performed for selected cases. Accordingly, patients underwent first-level analysis of the genes most frequently mutated in each clinical form of CMT neuropathy. Results Although our cohort had a particularly high percentage of cases of rare axonal and intermediate CMT neuropathies, we found mutations in 40% of patients. Among identified changes, 7 represented new mutations occurring in the MPZ , GJB1 , EGR2 , MFN2 , NEFL , and HSBP1/HSP27 genes. Histopathological analysis performed in selected cases revealed morphological features, which correlated with the molecular diagnosis and provided evidence of the underlying pathogenetic mechanism. Conclusion Clinical and pathological analysis of patients with CMT neuropathies contributes to our understanding of the molecular mechanisms of CMT neuropathies.

Published
2010

32. Foot pad skin biopsy in mouse models of hereditary neuropathy

Author

Maria Laura Feltri, Angelo Quattrini, Ignazio Diego Lopez, Alessandra Bolino, Stefano C. Previtali, Lawrence Wrabetz, Giuseppe Lauria, Federica Cerri, Giancarlo Comi, Patrizia Dacci, Giorgia Dina, Dacci, P, Dina, G, Cerri, F, Previtali, Sc, Lopez, Id, Lauria, G, Feltri, Ml, Bolino, A, Comi, Giancarlo, Wrabetz, L, and Quattrini, A.

Subjects
Biopsy, Sural nerve, Nerve Fibers, Myelinated, dermal nerve, epidermal nerve, Cellular and Molecular Neuroscience, Myelin, Mice, Mice, Neurologic Mutants, Sural Nerve, Charcot-Marie-Tooth Disease, medicine, Animals, Humans, Myelin Sheath, medicine.diagnostic_test, business.industry, Foot, CMT, Anatomy, Dermis, medicine.disease, Sciatic Nerve, Axons, Disease Models, Animal, medicine.anatomical_structure, Neurology, nervous system, Peripheral nervous system, Knockout mouse, Skin biopsy, Congenital muscular dystrophy, Sciatic nerve, Epidermis, business, Research Article
Abstract

Numerous transgenic and knockout mouse models of human hereditary neuropathies have become available over the past decade. We describe a simple, reproducible, and safe biopsy of mouse skin for histopathological evaluation of the peripheral nervous system (PNS) in models of hereditary neuropathies. We compared the diagnostic outcome between sciatic nerve and dermal nerves found in skin biopsy (SB) from the hind foot. A total of five animal models of different Charcot-Marie-Tooth neuropathies, and one model of congenital muscular dystrophy associated neuropathy were examined. In wild type mice, dermal nerve fibers were readily identified by immunohistochemistry, light, and electron microscopy and they appeared similar to myelinated fibers in sciatic nerve. In mutant mice, SB manifested myelin abnormalities similar to those observed in sciatic nerves, including hypomyelination, onion bulbs, myelin outfolding, redundant loops, and tomacula. In many strains, however, SB showed additional abnormalities—fiber loss, dense neurofilament packing with lower phosphorylation status, and axonal degeneration—undetected in sciatic nerve, possibly because SB samples distal nerves. SB, a reliable technique to investigate peripheral neuropathies in human beings, is also useful to investigate animal models of hereditary neuropathies. Our data indicate that SB may reveal distal axonal pathology in mouse models and permits sequential follow-up of the neuropathy in an individual mouse, thereby reducing the number of mice necessary to document pathology of the PNS. © 2010 Wiley-Liss, Inc.

Published
2010

33. HIGH POROSITY COLLAGEN TUBE: AN INNOVATIVE MEDICAL DEVICE FOR NERVE REGENERATION

Author

Cerri, F., Lopez, I. D., Sannino, A., Del Carro, U., Previtali, S. C., Mortini, P., LUCA SALVATORE, Comi, G. C., Quattrini, A., Cerri, F, Lopez, Id, Sannino, A, Del Carro, U, Previtali, Sc, Mortini, Pietro, Salvatore, L, Comi, Gc, Quattrini, A., Lopez I., D, Sannino, Alessandro, Previtali S., C, Mortini, P, Salvatore, Luca, and Comi G., C

Abstract

Bridging the gap after a nerve transection has always been a top challenge in the field of neuroscience. The peripheral nervous system can regenerate after injury but to fill a gap needs to find a proper guide directing the axonal elongation. Many techniques and devices have been studied in order to promote nerve regeneration but are still inade- quate. The aim of this work is validating an innovative high porosity collagen tube (medical devices, MD) and comparing the nerve outgrowth through this MD to the already avail- able in clinical practice NeuroGen IntegraÒ collagen and the silicone tubes, as a standard control, in an animal model of traumatic injury. The conduits were implanted in a 10 mm- gap in rat sciatic nerve and retrieved at different time points for morphological and ultrastructural analysis. Nerve conduc- tion studies were also evaluated. Nerve outgrowth through the NeuroGen IntegraÒ devices appeared to be similar to the one in the silicone tubes, being characterized by mini- fascicles containing less small axons with thin myelin and without a well-organized blood vessels distribution in the en- doneurium. In contrast, our MD showed, in the regenerated mid-graft, a normal size and number of nerve fibers with a normal myelination (G-ratio), already evident at 60 days postoperatively. Moreover, perineurium and blood vessels appeared absolutely normal with tight junction by EM. At 90 days postoperatively a nerve action potential was recordable distally, at the paw, in the sciatic nerves of the rats implanted with our MD or with the NeuroGen ones whereas was absent in the silicon group. Overall the neurophysiologi- cal and neuropathological data demonstrate the terrific qual- ity of nerve regeneration using our MD. These results make us confident in proposing our MD in the clinical practice to treat injury of the PNS.

Published
2009

34. Diffuse intraneural leiomyoma in a case of sensorimotor neuropathy

Author

Ignazio Diego Lopez, Massimo Franceschi, Armando Gavazzi, Paola Podini, Marina Scarlato, Giancarlo Comi, Stefano C. Previtali, Federica Cerri, Angelo Quattrini, Cerri, F, Gavazzi, A, Previtali, Sc, Franceschi, M, Lopez, Id, Scarlato, M, Podini, P, Comi, Giancarlo, and Quattrini, A.

Subjects
Leiomyosarcoma, Pathology, medicine.medical_specialty, Nerve biopsy, medicine.diagnostic_test, business.industry, Sural nerve, Schwannoma, medicine.disease, Pathology and Forensic Medicine, Cellular and Molecular Neuroscience, medicine.anatomical_structure, Epineurium, Peripheral nervous system, Smooth Muscle Tumor, medicine, Neurology (clinical), Endoneurium, business
Abstract

Leiomyomas are benign smooth muscle tumors, usually characterized by well-deWned Wbrous pseudocapsule and intersecting fascicles of spindle cells [3]. Few cases of leiomyomas in the peripheral nervous system (PNS) causing external nerve compression have been described [1, 7]. We report the case of a 71-year-old man who was referred for a 2 years history of burning pain and paresthesias associated with slowly progressive weakness of the lower limbs. He underwent total colectomy for diVuse polyposis 2 years before. Neurological examination and nerve conduction studies revealed symmetric sensorimotor axonal neuropathy of the lower limbs. Since all immunological, hematological and cerebrospinal Xuid examinations were negative, a sural nerve biopsy was performed. On semithin plastic sections, a mild degree of endoneurial Wbrosis, reduction of myelinated Wbers and signs of acute axonal degeneration were evident. Some fascicles had greater myelinated Wber loss than others, primarily in the center of the fascicles. Interestingly, paraYn-embedded, hematoxylin and eosinstained sections showed in epineurial and endoneurial perivascular spaces atypical large cells with abundant eosinophilic cytoplasm. Upon electron microscopy, these cells exhibited a basement membrane and prominent pinocytotic vesicles at the periphery (Fig. 1). The cytoplasm was Wlled with actin and myosin Wlaments, aggregates of glycogen particles and few organelles. Some cells showed oval and centrally located nuclei. Immunohistochemically, they were positive for smooth muscle actin, desmin and calponin (Fig. 2), but negative for CD31, cytokeratin and S-100 protein, demonstrating that they were smooth muscle cells (SMC). These cells did not show proliferative activity (negativity for Ki-67). Neither necrosis nor a deWnite capsule were present. The morphological and immunohistochemical data suggested a diagnosis of leiomyoma. This is the Wrst description of a diVuse SMC inWltrate of the PNS, both in the endoneurium and epineurium, whereas well circumscribed and encapsulated leiomyomas have occasionally been reported in the PNS. Other potential tumors such as leiomyosarcoma, schwannoma and hemangioma have to be considered in the diVerential diagnosis, but can be excluded based on immunoproWle [2]. Several hypotheses can be envisaged for the possible cellular origin of this unique tumor in the PNS, including pluripotential mesenchymal cells, perivascular connective tissue elements or SMC of blood vessels [6]. Epineurial proliferation of SMC in sural nerve biopsies indicating inXammatory or non-inXammatory angiopathy has been described before [5]. However, our patient’s sural nerve biopsy revealed SMC also in the endoneurium without signs of angiopathy, suggesting a diVerent origin of SMC. How this inWltrate caused damage of peripheral nerve Wbers remains unclear. Our patient’s clinical presentation suggests a diVuse damage of the PNS, while nerve biopsy Wndings associated with F. Cerri (&) Department of Neurology and INSPE, San RaVaele ScientiWc Institute, Via Olgettina, 6

Published
2009

35. Lymphomatous neuropathy in cold agglutinin disease

Author

Raffaello Nemni, M. Ponzoni, Nilo Riva, Angelo Quattrini, G. Comi, R. Epis, Federica Cerri, Stefano C. Previtali, G. Bezzi, Riva, N, Bezzi, G, Ponzoni, Maurilio, Epis, R, Previtali, Sc, Cerri, F, Nemni, R, Comi, Giancarlo, and Quattrini, A.

Subjects
Hemolytic anemia, Male, medicine.medical_specialty, Cold agglutinin disease, Anemia, Biopsy, Plasma cell dyscrasia, Neural Conduction, Gastroenterology, Fatal Outcome, Drug Therapy, Sural Nerve, Bone Marrow, Internal medicine, medicine, Humans, Lymphocytes, Treatment Failure, Acrocyanosis, business.industry, Peripheral Nervous System Diseases, Hyporeflexia, Plasmapheresis, Middle Aged, medicine.disease, Cold Agglutinin, Lymphoproliferative Disorders, Peripheral neuropathy, Disease Progression, Neurology (clinical), Anemia, Hemolytic, Autoimmune, medicine.symptom, Waldenstrom Macroglobulinemia, business, Wallerian Degeneration
Abstract

Cold agglutinin disease (CAD) is characterized by the production of cold agglutinins (CAs), usually IgMk autoantibodies, causing chronic hemolytic anemia and cold induced acrocyanosis (reported in 90% of cases). CAD has traditionally been classified into a primary type (pCAD) and a secondary type accompanied by malignant disease, most often lymphoma. PCAD is considered a stable or slowly progressive disease with good prognosis (median survival: 12.5 years from onset). It has recently been shown that even pCAD frequently associates with an underlying lymphoproliferative disorder characterized by clonal expansion of B cells.1 Peripheral neuropathy (PN) is a rare complication of CAD, with isolated cases reported, but the pathogenetic mechanisms are still object of debate.2–4 ### Case report. A 58-year-old man was admitted to the hospital because of asymmetric motor and sensory impairment of limbs. Three years before he had developed cold-induced acrocyanosis and pCAD had been diagnosed. At that time, two bone marrow biopsies showed no evidence of lymphoma or plasma cell dyscrasia. Six months before admission, the patient developed progressive weakness, sensory loss, and paresthesias in the right foot; 3 months later, the same symptoms appeared in the left foot and the right hand. On admission, neurologic examination showed asymmetric (right>left) weakness in distal muscles of lower limbs and in the right hand, sensory loss with the same distribution, absent tendon reflexes at lower limbs, and hyporeflexia in the arms. Laboratory investigations showed mild anemia (hemoglobin 10 g/dL), …

Published
2008

36. Phenotypic clustering of lamin A/C mutations in neuromuscular patients

Author

Sara Benedetti, Maurizio Ferrari, Isabella Mammi, M. Olivè, Isabella Moroni, Laura Palmucci, Angela Berardinelli, Stefano C. Previtali, I. Menditto, Adele D'Amico, Carmelo Rodolico, Giuliana Galluzzi, G. Comi, Enrico Bertini, Carlo P. Trevisan, Raffaella Fazio, Massimo Degano, Elena Pegoraro, Luciano Merlini, Angelo Quattrini, Francesca Mari, R. Caldara, Gisèle Bonne, Paola Carrera, A. Toscano, D. Toniolo, Lucia Morandi, Benedetti, S, Menditto, I, Degano, M, Rodolico, C, Merlini, L, D'Amico, A, Palmucci, L, Berardinelli, A, Pegoraro, E, Trevisan, Cp, Morandi, L, Moroni, I, Galluzzi, G, Bertini, E, Toscano, A, Olive, M, Bonne, G, Mari, F, Caldara, R, Fazio, R, Mammi, I, Carrera, P, Toniolo, D, Comi, Giancarlo, Quattrini, A, Ferrari, Maurizio, and Previtali, Sc

Subjects
Adult, Genetic Markers, Heart Diseases, DNA Mutational Analysis, Mutation, Missense, lamin A/C, neuromuscular disorders, LMNA gene, Biology, medicine.disease_cause, Frameshift mutation, LMNA, Cohort Studies, medicine, Missense mutation, Cluster Analysis, Humans, Genetic Predisposition to Disease, Age of Onset, Myopathy, Child, Frameshift Mutation, Muscle, Skeletal, Loss function, Genetics, Mutation, Myocardium, Neuromuscular Diseases, Lamin Type A, Lamins, Phenotype, Haplotypes, Child, Preschool, Disease Progression, Neurology (clinical), Age of onset, medicine.symptom, Haploinsufficiency
Abstract

Background: Mutations in the LMNA gene, encoding human lamin A/C, have been associated with an increasing number of disorders often involving skeletal and cardiac muscle, but no clear genotype/phenotype correlation could be established to date. Methods: We analyzed the LMNA gene in a large cohort of patients mainly affected by neuromuscular or cardiac disease and clustered mutated patients in two groups to unravel possible correlations. Results: We identified 28 variants, 9 of which reported for the first time. The two groups of patients were characterized by clinical and genetic differences: 1) patients with childhood onset displayed skeletal muscle involvement with predominant scapuloperoneal and facial weakness associated with missense mutations; 2) patients with adult onset mainly showed cardiac disorders or myopathy with limb girdle distribution, often associated with frameshift mutations presumably leading to a truncated protein. Conclusions: Our findings, supported by meta-analysis of previous literature, suggest the presence of two different pathogenetic mechanisms: late onset phenotypes may arise through loss of function secondary to haploinsufficiency, while dominant negative or toxic gain of function mechanisms may explain the severity of early phenotypes. This model of patient stratification may help patient management and facilitate future studies aimed at deciphering lamin A/C pathogenesis.

Published
2007

37. Loss of glial fibrillary acidic protein (GFAP) impairs Schwann cell proliferation and delays nerve regeneration after damage

Author

Daniela Triolo, Stefano C. Previtali, Maria Chiara Malaguti, Giorgia Dina, Paolo Morana, Giancarlo Comi, Isabella Lorenzetti, Albee Messing, Angelo Quattrini, Ubaldo Del Carro, Triolo, D, Dina, G, Lorenzetti, I, Malaguti, Mc, Morana, P, DEL CARRO, U, Comi, Giancarlo, Mesing, A, Quattrini, A, and Previtali, Sc

Subjects
Integrins, Nerve Crush, Integrin, Nerve guidance conduit, Axonal loss, Intermediate Filaments, Vimentin, macromolecular substances, Schwann cell proliferation, Mice, Glial Fibrillary Acidic Protein, Peripheral Nervous System, Animals, Cytoskeleton, Cell Proliferation, Mice, Knockout, Neurons, Glial fibrillary acidic protein, biology, Regeneration (biology), Cell Differentiation, Cell Biology, Sciatic Nerve, Cell biology, Extracellular Matrix, Nerve Regeneration, Mice, Inbred C57BL, nervous system, Immunology, biology.protein, Schwann Cells, Signal transduction
Abstract

Axonal loss causes disabling and permanent deficits in many peripheral neuropathies, and may result from inefficient nerve regeneration due to a defective relationship between Schwann cells, axons and the extracellular matrix. These interactions are mediated by surface receptors and transduced by cytoskeletal molecules. We investigated whether peripheral nerve regeneration is perturbed in mice that lack glial fibrillary acidic protein (GFAP), a Schwann-cell-specific cytoskeleton constituent upregulated after damage. Peripheral nerves develop and function normally in GFAP-null mice. However, axonal regeneration after damage was delayed. Mutant Schwann cells maintained the ability to dedifferentiate but showed defective proliferation, a key event for successful nerve regeneration. We also showed that GFAP and the other Schwann-cell-intermediate filament vimentin physically interact in two distinct signaling pathways involved in proliferation and nerve regeneration. GFAP binds integrin αvβ8, which initiates mitotic signals soon after damage by interacting with fibrin. Consistently, ERK phosphorylation was reduced in crushed GFAP-null nerves. Vimentin instead binds integrin α5β1, which regulates proliferation and differentiation later in regeneration, and may compensate for the absence of GFAP in mutant mice. GFAP might contribute to form macro-complexes to initiate mitogenic and differentiating signaling for efficient nerve regeneration.

Published
2006

38. Dominant LMNA mutations can cause combined muscular dystrophy and peripheral neuropathy

Author

Corrado Angelini, D. Toniolo, M. Trisciani, B. Sferrazza, Enrico Bertini, G. Comi, Angelo Quattrini, Paola Carrera, Stefano C. Previtali, Sandro Iannaccone, Sara Benedetti, Maurizio Ferrari, Benedetti, S, Bertini, E, Iannaccone, S, Angelini, C, Trisciani, M, Toniolo, D, Sferrazza, B, Carrera, P, Comi, Giancarlo, Ferrari, Maurizio, Quattrini, A, and Previtali, Sc

Subjects
Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Pathology, medicine.medical_specialty, Neuromuscular disease, Adolescent, Biopsy, DNA Mutational Analysis, Short Report, medicine.disease_cause, LMNA, Sural Nerve, medicine, Humans, Muscular dystrophy, Myopathy, Muscle, Skeletal, Genes, Dominant, Neurologic Examination, Mutation, integumentary system, business.industry, Genetic heterogeneity, Peripheral Nervous System Diseases, Anatomy, medicine.disease, Lamin Type A, Lamins, Muscular Dystrophy, Emery-Dreifuss, Pedigree, Psychiatry and Mental health, Muscular Atrophy, Peripheral neuropathy, Phenotype, embryonic structures, Surgery, Female, Neurology (clinical), medicine.symptom, business, Lamin
Abstract

The coexistence of neurogenic and myogenic features in scapuloperoneal syndrome is rarely ascribed to a single gene. Defects in the nuclear envelope protein lamin A/C, encoded by the LMNA gene, have been shown to be associated with a variety of disorders affecting mainly the muscular and adipose tissues and, more recently, with autosomal recessive Charcot-Marie-Tooth type 2 neuropathy. This report is about a patient presenting features of myopathy and neuropathy due to a dominant LMNA mutation, suggesting that the peripheral nerve might be affected in primary LMNA myopathy. Our observations further support the marked intrafamilial and interfamilial phenotypic heterogeneity associated with lamin A/C defects.

Published
2005

39. A GENOMIC APPROACH TO IDENTIFY NEW GENES RESPONSIBLE FOR INHERITED MOTOR AND CMT2 NEUROPATHIES: A COLLABORATIVE STUDY

Author

Previtali, S. C., Fabrizi, G. M., Manganelli, F., Mazzeo, A., Davide Pareyson, Schenone, A., Taroni, F., Vita, G., Bellone, E., Ferrarini, M., Magri, S., Scarlato, M., Riva, N., Lunetta, C., Carrera, P., Bucci, G., Mandich, P., Penco, S., Lazarevic, D., Cittaro, D., Jordanova, A., Reilly, M. M., Casari, G., Ferrari, M., Comi, G., Bolino, A., Previtali, Sc, Fabrizi, Gm, Manganelli, F, Mazzeo, A, Pareyson, D, Schenone, A, Taroni, F, Vita, G, Bellone, E, Ferrarini, M, Magri, S, Scarlato, M, Riva, N, Lunetta, C, Carrera, P, Bucci, G, Mandich, P, Penco, S, Lazarevic, D, Cittaro, D, Jordanova, A, Reilly, Mm, Casari, GIORGIO NEVIO, Ferrari, M, Comi, Giancarlo, and Bolino, A.

40. Hypokalemic periodic paralysis in a patient with acquired growth hormone deficiency

Author

M. Fortunato, Roberto Lanzi, Valeria A. Sansone, Marco Losa, Marina Scavini, Stefano C. Previtali, Elisa Gatti, Emanuele Bosi, G. Meola, Lanzi, R, Previtali, Sc, Sansone, V, Scavini, M, Fortunato, M, Gatti, E, Meola, G, Bosi, Emanuele, and Losa, M.

Subjects
Adult, Male, medicine.medical_specialty, Hormone Replacement Therapy, Endocrinology, Diabetes and Metabolism, Hypokalemic Periodic Paralysis, Context (language use), Hypopituitarism, GH deficiency, Hyperinsulinemia, Hypokalemic periodic paralisis, Endocrinology, Hypokalemic periodic paralysis, Internal medicine, medicine, Humans, Dwarfism, Pituitary, Muscle biopsy, medicine.diagnostic_test, business.industry, Human Growth Hormone, Muscles, medicine.disease, Hypokalemia, Diabetes insipidus, Settore MED/26 - Neurologia, Acquired Growth Hormone Deficiency, medicine.symptom, business
Abstract

Context: Hypokalemic periodic paralysis (HypoPP) is a rare disorder consisting of sudden episodes of muscle weakness with areflexia involving all four limbs, which spontaneously resolve within several hours or days. Primary HypoPP is genetically determined, while secondary acquired HypoPP has been described in association with thyreotoxycosis, hyperaldosteronism, kidney diseases, diuretics and liquorice abuse, gastrointestinal potassium loss, or cysplatinum therapy. Objective: To report a case of HypoPP associated with GH deficiency. Patient: A 33 yr-old man with hypopituitarism and diabetes insipidus secondary to pituitary stalk-localized sarcoidosis, and documented HypoPP episodes. Clinical Presentation: Neurologic exam outside HypoPP episodes was normal. Needle electromyography was normal without myotonia or other spontaneous electric activity. Muscle biopsy documented a vacuolar myopathy with tubular aggregates. However, genetic analysis ruled out common mutations of the voltage-gated calcium channel observed in primary HypoPP. Common causes of secondary HypoPP were also ruled out. The patient was diagnosed with severe GH deficiency with modest fasting hyperinsulinemia and insulin resistance and started on GH replacement therapy, an α-glucosidase inhibitor (acarbose) and a diet low in simple carbohydrates. Conclusions: GH replacement therapy, acarbose and a diet low in simple carbohydrates resulted in the complete long-term (>2 yr) remission of HypoPP episodes. This is consistent with the hypothesis that the hyperinsulinemia associated to GH deficiency may trigger HypoPP episodes by increasing Na+/K+ ATPase activity and K+ transport into the intracellular compartment with subsequent hypokalemia.

41. Natural history of Becker muscular dystrophy: DMD gene mutations predict clinical severity.

Author

Gorgoglione D, Sabbatini D, Riguzzi P, Capece G, Pane M, Servidei S, Briganti M, Sancricca C, Bruschi F, Ardissone A, Masson R, Gallone A, Maggi L, Picillo E, Politano L, Petrosino A, Vianello S, Penzo M, Villa M, Sframeli M, Allegra C, Barp A, Di Bari A, Salmin F, Albamonte E, Colacicco G, Panicucci C, Traverso M, Palermo C, Lerario A, Velardo D, D'Angelo MG, Berardinelli A, Gardani A, Nicotra R, Parravicini S, Siciliano G, Ricci G, Torri F, Gadaleta G, Urbano G, Rolle E, Ricci F, D'Amico A, Catteruccia M, Pini A, Giannotta M, Battini R, Marinella G, Previtali SC, Zambon AA, Ferlini A, Fortunato F, Magri F, Mongini TE, Sansone VA, Bruno C, Messina S, Nigro V, Moroni I, Mercuri E, Bello L, and Pegoraro E

Abstract

Background: Becker muscular dystrophy (BMD) is an X-linked neuromuscular disease due to mutations in the DMD gene, leading to a deficient and less functional dystrophin mainly in skeletal and cardiac muscle. Understanding the natural history of BMD is crucial for optimizing patient care and developing targeted treatments., Materials and Methods: Retrospective data were collected from 943 patients diagnosed with BMD based on a combination of clinical, biochemical and genetic criteria followed by 17 Italian neuromuscular centers. Patients' demographics, main signs and symptoms at BMD onset, neuropsychiatric comorbidities, age at loss of ambulation (LoA), cardiac left ventricular ejection fraction (LVEF), pulmonary forced vital capacity (FVC), and DMD mutations were collected. Disease milestones were analysed in specific DMD mutational groups., Results: the median age at the last assessment was 26.0 (16.6-41.9) years, with a median age at diagnosis of 7.5 (4.0-14.0) years. In 55% of patients, the diagnosis was prompted by the incidental finding of hyperCKemia. At the last assessment, 13.5% of patients had lost the ability to walk at a median age estimated by Kaplan-Meier analysis of 69 years. Thirty percent of patients exhibited left ventricular impairment and 2.7% respiratory involvement. Ten percent of patients carried out-of-frame mutations, 4% nonsense mutations, and 86% in-frame deletions/duplications. The subset of in-frame deletions was further classified based on the specific mutations. Patients carrying del45-49 compared to del45-47 were associated with an earlier LoA (P=1×10-4), where patients with del45-55 (P=.005), del48 (P=.02), and del48-49 (P=.02) correlated with a later LoA compared to del45-47. del45-55 (P=.002) and del48 (P=.003) were significantly associated with decreased odds of developing a pathological LVEF% compared to del45-47., Conclusion: Our results contribute to the better understanding of the natural history of BMD and capture precious data in the era of the emerging therapies. The knowledge of the specific DMD mutation may help to define a prognosis in a subset of BMD patients and will serve as a model for the design of future therapies., (© The Author(s) 2024. Published by Oxford University Press on behalf of the Guarantors of Brain. All rights reserved. For commercial re-use, please contact reprints@oup.com for reprints and translation rights for reprints. All other permissions can be obtained through our RightsLink service via the Permissions link on the article page on our site—for further information please contact journals.permissions@oup.com.)

Published
2024
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42. Integrating D4Z4 methylation analysis into clinical practice: improvement of FSHD molecular diagnosis through distinct thresholds for 4qA/4qA and 4qA/4qB patients.

Author

Strafella C, Megalizzi D, Trastulli G, Proietti Piorgo E, Colantoni L, Tasca G, Monforte M, Zampatti S, Primiano G, Sancricca C, Bortolani S, Torchia E, Ravera B, Torri F, Gadaleta G, Risi B, Caria F, Gerardi F, Carraro E, Gioiosa V, Garibaldi M, Tufano L, Frezza E, Massa R, Caltagirone C, Pennisi EM, Petrucci A, Pane M, Frongia A, Gragnani F, Scutifero M, Mandich P, Grandis M, Maioli MA, Casali C, Manfroi E, Politano L, Passamano L, Petillo R, Rodolico C, Pugliese A, Previtali SC, Sansone V, Vercelli L, Mongini TE, Ricci G, Siciliano G, Filosto M, Ricci E, Cascella R, and Giardina E

Subjects
Humans, Male, Female, Adult, Middle Aged, Epigenesis, Genetic genetics, Homeodomain Proteins genetics, Aged, Young Adult, Muscular Dystrophy, Facioscapulohumeral genetics, Muscular Dystrophy, Facioscapulohumeral diagnosis, DNA Methylation genetics, Chromosomes, Human, Pair 4 genetics
Abstract

Background: Facioscapulohumeral dystrophy (FSHD) is a myopathy characterized by the loss of repressive epigenetic features affecting the D4Z4 locus (4q35). The assessment of DNA methylation at two regions (DUX4-PAS and DR1) of D4Z4 locus proved to be an effective method to detect epigenetic signatures compatible with FSHD. The present study aims at validating the employment of this method into clinical practice and improving the protocol by refining the classification thresholds of 4qA/4qA patients. To this purpose, 218 subjects with clinical suspicion of FSHD collected in 2022-2023 were analyzed. Each participant underwent in parallel the traditional FSHD molecular testing (D4Z4 sizing) and the proposed methylation assay. The results provided by both analyses were compared to evaluate the concordance and calculate the performance metrics of the methylation test., Results: Among the 218 subjects, the 4q variant type distribution was 54% 4qA/4qA, 43% 4qA/4qB and 3% 4qB/4qB. The methylation analysis was performed only on carriers of at least one 4qA allele. After refining the classification threshold, the test reached the following performance metrics: sensitivity = 0.90, specificity = 1.00 and accuracy = 0.93. These results confirmed the effectiveness of the methylation assay in identifying patients with genetic signature compatible with FSHD1 and FSHD2 based on their DUX4-PAS and DR1 profile, respectively. The methylation data were also evaluated with respect to the clinical information., Conclusions: The study confirmed the ability of the method to accurately identify methylation profiles compatible with FSHD genetic signatures considering the 4q genotype. Moreover, the test allows the detection of hypomethylated profiles in asymptomatic patients, suggesting its potential application in identifying preclinical conditions in patients with positive family history and FSHD genetic signatures. Furthermore, the present work emphasizes the importance of interpreting methylation profiles considering the patients' clinical data., (© 2024. The Author(s).)

Published
2024
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43. Six-minute walk test as outcome measure of fatigability in adults with spinal muscular atrophy treated with nusinersen.

Author

Govoni A, Ricci G, Bonanno S, Bello L, Magri F, Meneri M, Torri F, Caponnetto C, Passamano L, Grandis M, Trojsi F, Cerri F, Gadaleta G, Capece G, Caumo L, Tanel R, Saccani E, Vacchiano V, Sorarù G, D'Errico E, Tramacere I, Bortolani S, Rolle E, Gellera C, Zanin R, Silvestrini M, Politano L, Schenone A, Previtali SC, Berardinelli A, Turri M, Verriello L, Coccia M, Mantegazza R, Liguori R, Filosto M, Maioli MA, Simone IL, Mongini T, Corti S, Manca ML, Pegoraro E, Siciliano G, Comi GP, and Maggi L

Subjects
Humans, Male, Female, Adult, Retrospective Studies, Middle Aged, Young Adult, Treatment Outcome, Cohort Studies, Adolescent, Outcome Assessment, Health Care, Follow-Up Studies, Oligonucleotides therapeutic use, Walk Test, Fatigue drug therapy, Fatigue etiology, Fatigue physiopathology, Fatigue diagnosis, Muscular Atrophy, Spinal drug therapy, Muscular Atrophy, Spinal physiopathology
Abstract

Introduction/aims: Fatigue (subjective perception) and fatigability (objective motor performance worsening) are relevant aspects of disability in individuals with spinal muscular atrophy (SMA). The effect of nusinersen on fatigability in SMA patients has been investigated with conflicting results. We aimed to evaluate this in adult with SMA3., Methods: We conducted a multicenter retrospective cohort study, including adult ambulant patients with SMA3, data available on 6-minute walk test (6MWT) and Hammersmith Functional Motor Scale-Expanded (HFMSE) at baseline and at least at 6 months of treatment with nusinersen. We investigated fatigability, estimated as 10% or higher decrease in walked distance between the first and sixth minute of the 6MWT, at baseline and over the 14-month follow-up., Results: Forty-eight patients (56% females) were included. The 6MWT improved after 6, 10, and 14 months of treatment (p < 0.05). Of the 27 patients who completed the entire follow-up, 37% improved (6MWT distance increase ≥30 m), 48.2% remained stable, and 14.8% worsened (6MWT distance decline ≥30 m). Fatigability was found at baseline in 26/38 (68%) patients and confirmed at subsequent time points (p < 0.05) without any significant change over the treatment period. There was no correlation between fatigability and SMN2 copy number, sex, age at disease onset, age at baseline, nor with 6MWT total distance and baseline HFMSE score., Discussion: Fatigability was detected at baseline in approximately 2/3 of SMA3 walker patients, without any correlation with clinical features, included motor performance. No effect on fatigability was observed during the 14-month treatment period with nusinersen., (© 2024 The Author(s). Muscle & Nerve published by Wiley Periodicals LLC.)

Published
2024
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44. Clinical, Histopathologic, and Genetic Features of Patients With Myofibrillary and Distal Myopathies: Experience From the Italian Network.

Author

Bortolani S, Savarese M, Vattemi G, Bonanno S, Falzone YM, Pugliese A, Primiano G, Sancricca C, Lopergolo D, Greco G, Gemelli C, Ravaglia S, Bencivenga RP, Velardo D, Magri F, Valentino ML, Cheli M, Torchia E, Lucchini M, Petrucci A, Ricci G, Garibaldi M, Astrea G, Rubegni A, Angelini CI, Ariatti A, Santorelli FM, Ruggieri A, Antonini G, Siciliano G, Filosto M, Mirabella M, Liguori R, Comi GP, Ruggiero L, Grandis M, Massa R, Malandrini A, Servidei S, Mongini TE, Rodolico C, Toscano A, Previtali SC, Tonin P, Diaz-Manera J, Monforte M, Ricci E, Maggi L, and Tasca G

Subjects
Humans, Female, Male, Middle Aged, Italy, Adult, Retrospective Studies, Aged, Distal Myopathies genetics, Distal Myopathies pathology, Distal Myopathies epidemiology, Myopathies, Structural, Congenital genetics, Myopathies, Structural, Congenital pathology
Abstract

Background and Objectives: The diagnostic process for myofibrillar myopathies (MFM) and distal myopathies (DM) is particularly complex because of the large number of causative genes, the existence of still molecularly undefined disease entities, and the overlapping features between the 2 categories. This study aimed to characterize a large cohort of patients affected by MFM and DM and identify the most important diagnostic and prognostic aspects of these diseases., Methods: Patients with either a myopathological diagnosis of MFM or a clinical diagnosis of DM were included in this retrospective multicentric national study. Demographic, genetic, clinical, and histopathologic data of anonymized patients were collected from the neuromuscular centers of the Italian Association of Myology network., Results: Data regarding 132 patients with MFM (mean age 57.0 ± 15.8 years, 49% female) and 298 patients with DM (mean age 50.7 ± 15.9 years, 40% female) were gathered from 20 neuromuscular centers. 69 patients fulfilled the criteria for both groups (distal myopathies with myofibrillar pathology, DM-MP). Molecular confirmation was achieved in 63% of the patients. Fifty-two percent of the patients with MFM carried pathogenic variants in either DES (n = 30), MYOT (n = 20), or DNAJB6 (n = 18), which were also the most frequent disease-causing genes in DM-MP, while GNE (n = 44) and MYH7 (n = 23) were the genes most commonly carrying pathogenic variants in DM. The mean age at onset varied from <25 years in patients with causative variants in MYH7 and DYSF to 59 years in patients with myotilinopathies. Cardiac involvement was reported in 29% of patients with MFM and 16% of patients with DM, with DES and MYH7 variants significantly associated with the development of cardiomyopathy. Respiratory impairment was more prevalent in patients with TTN and DES variants and rare in other disorders such as GNE myopathy and dysferlinopathies, which were instead associated, together with DNAJB6 -related and PLIN4 -related myopathies, with the risk of losing ambulation during the disease course., Discussion: The Italian cohort of patients with MFM and DM recapitulates the phenotypic heterogeneity and the partial overlap between the 2 groups. However, in relative contrast to the encountered phenotypic variability, only 5 genes accounted for most of the molecular diagnoses. Specific genetic entities are associated with significantly increased risk of developing cardiorespiratory complications or loss of ambulation, which has relevant prognostic implications.

Published
2024
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45. Muscle hypertrophy following acquired neurogenic injury: systematic review and analysis of existing literature.

Author

Strano CM, Bosco L, Laurini C, Sferruzza G, Butera C, Falzone YM, Sorrenti B, Ratti A, Tufano L, Leonardi L, Merlonghi G, Morino S, Gerevini S, Del Carro U, Garibaldi M, Filippi M, and Previtali SC

Subjects
Humans, Muscle, Skeletal pathology, Muscle, Skeletal physiopathology, Male, Female, Middle Aged, Adult, Hypertrophy etiology
Abstract

Objectives: Neurogenic muscle hypertrophy (NMH) is a rare condition characterized by focal muscle hypertrophy caused by chronic partial nervous injury. Given its infrequency, underlying mechanisms remain poorly understood. Inspired by two clinical cases, we conducted a systematic review to gain insights into the different aspects of NMH., Methods: We systematically searched online databases up until May 30, 2023, for reports of muscle hypertrophy attributed to acquired neurogenic factors. We conducted an exploratory analysis to identify commonly associated features. We also report two representative clinical cases., Results: Our search identified 63 reports, describing 93 NMH cases, to which we added our two cases. NMH predominantly affects patients with compressive radiculopathy (68.4%), negligible muscular weakness (93.3%), and a chronic increase in muscle bulk. A striking finding in most neurophysiological studies (60.0%) is profuse spontaneous discharges, often hindering the analysis of voluntary traces. Some patients exhibited features consistent with more significant muscle damage, including higher creatine phosphokinase levels, muscle pain, and inflammatory muscle infiltration. These patients are sometimes referred to in literature as "focal myositis." Treatment encompassed corticosteroid, Botulinum Toxin A, decompressive surgery, antiepileptic medications, and nerve blocks, demonstrating varying degrees of efficacy. Botulinum Toxin A yielded the most favorable response in terms of reducing spontaneous discharges., Interpretation: This systematic review aims to provide a clear description and categorization of this uncommon presentation of an often-overlooked neurological disorder. Though questions remain about the underlying mechanism, evidence suggests that aberrant fiber overstimulation along with increased workload that promotes focal damage may result in muscle hypertrophy. This may serve as a guide for therapeutic interventions., (© 2024 The Author(s). Annals of Clinical and Translational Neurology published by Wiley Periodicals LLC on behalf of American Neurological Association.)

Published
2024
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47. Overcoming therapeutic challenges: Successful management of a supposedly triple seronegative, refractory generalized myasthenia gravis patient with efgartigimod.

Author

Sorrenti B, Laurini C, Bosco L, Strano CMM, Scarlato M, Gastaldi M, Filippi M, Previtali SC, and Falzone YM

Subjects
Female, Humans, Autoantibodies blood, Receptors, Cholinergic immunology, Receptors, Fc therapeutic use, Myasthenia Gravis drug therapy, Myasthenia Gravis immunology
Abstract

Background and Purpose: This study was undertaken to highlight neonatal Fc receptor inhibition (efgartigimod) as a valuable therapeutic option for patients with refractory seronegative myasthenia gravis (MG) and to emphasize the concept that seronegative MG is greatly constrained by the limitations of currently available diagnostic methods and therapeutic measures., Methods: We describe the first refractory, generalized MG (gMG) patient successfully treated with efgartigimod after testing negative on standard autoantibody detection tests., Results: Our patient presented with severe fluctuating bulbar and generalized weakness, resulting in multiple myasthenic crises requiring intubation. After a 28-year medical history of multiple failed lines of treatment, our patient was started on efgartigimod. Over five treatment cycles, a definite improvement in her clinical condition was observed (Myasthenia Gravis Foundation of America class: IIIb to IIb; MG-Activities of Daily Living score: 11 to 0; MG-Quality of Life 15 score: 30 to 0; Quantitative MG score: 28 to 6). Standard autoantibody detection tests failed to detect known pathogenic autoantibodies, but cell-based assay (CBA) identified autoantibodies against clustered adult acetylcholine receptor (AChR)., Conclusions: In light of recent approvals of efgartigimod by the European Medicines Agency and US Food and Drug Administration exclusively for AChR-positive gMG forms, our case highlights evidence suggesting that such an approach might be shortsighted and could limit therapeutic options for patients with refractory seronegative gMG. Additionally, introducing more sensitive analytical techniques, exemplified by CBA, may help bridge the gap between seronegative and seropositive patients. This represents an urgent unmet need for gMG patients, as the antibody profile dramatically influences the therapeutic approach., (© 2024 The Authors. European Journal of Neurology published by John Wiley & Sons Ltd on behalf of European Academy of Neurology.)

Published
2024
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48. Phenotypic spectrum of myelin protein zero-related neuropathies: a large cohort study from five mutation clusters across Italy.

Author

Bertini A, Gentile L, Cavallaro T, Tozza S, Saveri P, Russo M, Massucco S, Falzone YM, Bellone E, Taioli F, Geroldi A, Occhipinti G, Ferrarini M, Cavalca E, Crivellari L, Mandich P, Balistreri F, Magri S, Taroni F, Previtali SC, Schenone A, Grandis M, Manganelli F, Fabrizi GM, Mazzeo A, Pareyson D, and Pisciotta C

Abstract

Background: We aimed to investigate the clinical features of a large cohort of patients with myelin protein zero ( MPZ )-related neuropathy, focusing on the five main mutation clusters across Italy., Methods: We retrospectively gathered a minimal data set of clinical information in a series of patients with these frequent mutations recruited among Italian Charcot-Marie-Tooth (CMT) registry centres, including disease onset/severity (CMTES-CMT Examination Score), motor/sensory symptoms and use of orthotics/aids., Results: We collected data from 186 patients: 60 had the p.Ser78Leu variant ('classical' CMT1B; from Eastern Sicily), 42 the p.Pro70Ser (CMT2I; mainly from Lombardy), 38 the p.Thr124Met (CMT2J; from Veneto), 25 the p.Ser44Phe (CMT2I; from Sardinia) and 21 the p.Asp104ThrfsX13 (mild CMT1B; from Apulia) mutation. Disease severity (CMTES) was higher (p<0.001) in late-onset axonal forms (p.Thr124Met=9.2±6.6; p.Ser44Phe=7.8±5.7; p.Pro70Ser=7.6±4.8) compared with p.Ser78Leu (6.1±3.5) patients. Disease progression (ΔCMTES/year) was faster in the p.Pro70Ser cohort (0.8±1.0), followed by p.Ser44Phe (0.7±0.4), p.Thr124Met (0.4±0.5) and p.Ser78Leu (0.2±0.4) patients. Disease severity (CMTES=1.2±1.5), progression (ΔCMTES/year=0.1±0.4) and motor involvement were almost negligible in p.Asp104ThrfsX13 patients, who, however, frequently (78%, p<0.001) complained of neuropathic pain. In the other four clusters, walking difficulties were reported by 69-85% of patients, while orthotic and walking aids use ranged between 40-62% and 16-28%, respectively., Conclusions: This is the largest MPZ (and late-onset CMT2) cohort ever collected, reporting clinical features and disease progression of 186 patients from five different clusters across Italy. Our findings corroborate the importance of differentiating between 'classical' childhood-onset demyelinating, late-onset axonal and mild MPZ -related neuropathy, characterised by different pathomechanisms, in view of different therapeutic targets., Competing Interests: Competing interests: GMF acknowledges donations from Pfizer to support research activities of his Research Unit, financial support from Akcea, Kedrion, Pfizer for participation in national and international meetings and from Akcea, Alnylam and Pharnext for participation in Advisory Boards; MG acknowledges donations from Sanofi Genzyme to support research activities of her Research Unit, financial support from Alnylam and Sanofi Genzyme for participation in national and international Meetings, participation in Advisory Board of Pfizer, speaker honorarium from Sanofi Genzyme; AM acknowledges financial support from Pfizer, Alnylam and Akcea for participation in national and international meetings, participation in Advisory Board of Pfizer, Alnylam and Akcea; DP acknowledges participation in Advisory Board of Inflectis, Alnylam, Akcea, Arvinas, Augustine Tx, DTx; ST is supported by the Ministry of University and Research (MUR), National Recovery and Resilience Plan (NRRP), project MNESYS (PE0000006) - A multiscale integrated approach to the study of the nervous system in health and disease (DN. 1553 11.10.2022). AB, LG, TC, PS, MR, SM, YMF, EM, FT, AG, GO, MF, EC, LC, PM, FB, SM, FT, SCP, AS, FM, CP report no disclosure., (© Author(s) (or their employer(s)) 2024. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published
2024
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49. Psychosocial resources and psychopathology among persons with neuromuscular disorders during the COVID-19 pandemic.

Author

Sanzo' S, Tizzoni F, Previtali SC, Berardinelli A, Nobile M, Molteni M, Manzoni M, Tarabelloni A, Russo A, Delle Fave A, and D'Angelo MG

Subjects
Humans, Adult, Male, Female, Middle Aged, Adolescent, Young Adult, Anxiety psychology, Anxiety epidemiology, Depression psychology, Depression epidemiology, Surveys and Questionnaires, SARS-CoV-2, COVID-19 psychology, COVID-19 epidemiology, Resilience, Psychological, Neuromuscular Diseases psychology, Neuromuscular Diseases epidemiology, Social Support
Abstract

Background: The COVID-19 pandemic substantially affected the lives of persons with inherited neuromuscular disorders (INMD), causing disruption in clinical and support services. While several studies have investigated mental health, distress and psychosocial resources in the general population during the pandemic, little is known about the experience of persons with INMD., Methods: This study was aimed to fill this gap by jointly investigating both psychopathological symptoms and psychosocial resources - specifically, resilience and perceived social support - among persons with INMD during the pandemic, taking into account demographic and clinical factors. Between April and December 2020, 59 participants with INMD (aged 15-59, 71.2% M) completed a questionnaire collecting demographic and clinical data, the Multidimensional Scale of Perceived Social Support, the Resilience Scale for Adults, and the Achenbach System of Empirically Based Assessment., Results: Overall, participants showed good levels of resilience and perceived social support. A minority of participants reported clinically relevant psychopathological symptoms, 28.81% for anxiety and depression. Most psychopathological symptoms were negatively correlated with resilience (-0.347 < r < - .420), but not significantly associated with social support. Consistent with previous studies, regression analyses highlighted that participants with Duchenne muscular dystrophy were more prone to report anxious and depressive symptoms (B = 1.748, p = .028, OR = 5.744), and participants with myotonic dystrophy, attention problems (B = 2.339, p = .006, OR = 10.376). Resilience emerged as a potential predictor of lower anxious-depressive symptoms (B=-1.264, p = .012, OR = 0.283)., Conclusions: The findings suggest the importance to investigate psychosocial resources in addition to psychopathology among persons with INMD, and to design interventions supporting resilience as a protective factor for mental health promotion., (© 2024. The Author(s).)

Published
2024
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50. Molecular mechanisms and therapeutic strategies for neuromuscular diseases.

Author

Zambon AA, Falzone YM, Bolino A, and Previtali SC

Subjects
Humans, Animals, Neuromuscular Diseases therapy, Neuromuscular Diseases genetics, Neuromuscular Diseases metabolism, Genetic Therapy methods
Abstract

Neuromuscular diseases encompass a heterogeneous array of disorders characterized by varying onset ages, clinical presentations, severity, and progression. While these conditions can stem from acquired or inherited causes, this review specifically focuses on disorders arising from genetic abnormalities, excluding metabolic conditions. The pathogenic defect may primarily affect the anterior horn cells, the axonal or myelin component of peripheral nerves, the neuromuscular junction, or skeletal and/or cardiac muscles. While inherited neuromuscular disorders have been historically deemed not treatable, the advent of gene-based and molecular therapies is reshaping the treatment landscape for this group of condition. With the caveat that many products still fail to translate the positive results obtained in pre-clinical models to humans, both the technological development (e.g., implementation of tissue-specific vectors) as well as advances on the knowledge of pathogenetic mechanisms form a collective foundation for potentially curative approaches to these debilitating conditions. This review delineates the current panorama of therapies targeting the most prevalent forms of inherited neuromuscular diseases, emphasizing approved treatments and those already undergoing human testing, offering insights into the state-of-the-art interventions., (© 2024. The Author(s).)

Published
2024
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