Your search keyword '"Servida M"' showing total 31 results

1. Survival gain in glioblastoma patients treated with dendritic cell immunotherapy is associated with increased NK but not CD8+T cell activation in the presence of adjuvant temozolomide

Author

Pellegatta, S, Eoli, M, Cuccarini, V, Anghileri, E, Pollo, B, Pessina, S, Frigerio, S, Servida, M, Cuppini, L, Antozzi, C, Cuzzubbo, S, Corbetta, C, Paterra, R, Acerbi, F, Ferroli, P, Dimeco, F, Fariselli, L, Parati, E, Bruzzone, M, Finocchiaro, G, Pellegatta, Serena, Eoli, Marica, Cuccarini, Valeria, Anghileri, Elena, Pollo, Bianca, Pessina, Sara, Frigerio, Simona, Servida, Maura, Cuppini, Lucia, Antozzi, Carlo, CUZZUBBO, STEFANIA, CORBETTA, CRISTINA, Paterra, Rosina, Acerbi, Francesco, Ferroli, Paolo, DiMeco, Francesco, Fariselli, Laura, Parati, Eugenio A., Bruzzone, Maria Grazia, Finocchiaro, Gaetano, Pellegatta, S, Eoli, M, Cuccarini, V, Anghileri, E, Pollo, B, Pessina, S, Frigerio, S, Servida, M, Cuppini, L, Antozzi, C, Cuzzubbo, S, Corbetta, C, Paterra, R, Acerbi, F, Ferroli, P, Dimeco, F, Fariselli, L, Parati, E, Bruzzone, M, Finocchiaro, G, Pellegatta, Serena, Eoli, Marica, Cuccarini, Valeria, Anghileri, Elena, Pollo, Bianca, Pessina, Sara, Frigerio, Simona, Servida, Maura, Cuppini, Lucia, Antozzi, Carlo, CUZZUBBO, STEFANIA, CORBETTA, CRISTINA, Paterra, Rosina, Acerbi, Francesco, Ferroli, Paolo, DiMeco, Francesco, Fariselli, Laura, Parati, Eugenio A., Bruzzone, Maria Grazia, and Finocchiaro, Gaetano

Abstract

In a two-stage phase II study, 24 patients with first diagnosis of glioblastoma (GBM) were treated with dendritic cell (DC) immunotherapy associated to standard radiochemotherapy with temozolomide (TMZ) followed by adjuvant TMZ. Three intradermal injections of mature DC loaded with autologous GBM lysate were administered before adjuvant TMZ, while 4 injections were performed during adjuvant TMZ. According to a two-stage Simon design, to proceed to the second stage progression-free survival (PFS) 12 months after surgery was expected in at least 8 cases enrolled in the first stage. Evidence of immune response and interaction with chemotherapy were investigated. After a median follow up of 17.4 months, 9 patients reached PFS12. In these patients (responders, 37.5%), DC vaccination induced a significant, persistent activation of NK cells, whose increased response was significantly associated with prolonged survival. CD8+T cells underwent rapid expansion and priming but, after the first administration of adjuvant TMZ, failed to generate a memory status. Resistance to TMZ was associated with robust expression of the multidrug resistance protein ABCC3 in NK but not CD8+T cells. The negative effect of TMZ on the formation of T cell-associated antitumor memory deserves consideration in future clinical trials including immunotherapy

Published

2018

2. Co-existence of amyotrophic lateral sclerosis and polymyositis: a case report

Author

SUSANI, EMANUELA LAURA, TREMOLIZZO, LUCIO, CEREDA, DILETTA, FERRARESE, CARLO, Santarone, ME, Marzorati, L, Messina, S, Servida, M, Moggio, M, Mora, G, Silani, V, Susani, E, Tremolizzo, L, Cereda, D, Santarone, M, Marzorati, L, Messina, S, Servida, M, Moggio, M, Mora, G, Silani, V, and Ferrarese, C

Subjects

MED/26 - NEUROLOGIA, polymyositi, differential diagnosi, amyotrophic lateral sclerosi, muscle biopsy

Abstract

Background: The diagnosis of amyotrophic lateral sclerosis (ALS) requires the careful exclusion of mimic syndromes in presence of involvement of both upper and lower motor neurons progressing over time. In the differential diagnosis myopathic processes must be considered. In particular, inclusion body myositis patients are often misdiagnosed as having ALS, due to the fact that these two conditions share some clinical and serological similarities. Other myopathies, such as polymyositis are even rarer and, as a general rule, a diagnosis of inflammatory myopathy tends to exclude ALS. Aim: Describe the case of an ALS patient that was subsequently co-diagnosed with polymyositis. Case Report: A 51-year-old woman with a 4-month history of distal muscle weakness and progressive hypotrophy at the upper limbs came to our attention. Her past medical history was significant for hypothyroidism. Neurological examination showed intact cranial nerves, diffuse mild bilateral weakness with wasting of the interossei muscles at the hands and evident fasciculations; deep tendon reflexes were increased at the upper limbs and decreased at the lower ones. Both brain and spinal cord MRI were normal, as it was the exam of the CSF. An EMG study revealed signs of acute denervation and fasciculations in both distal and proximal muscle of the arms; myopathic changes were not reported. Due to the unexpected bilateral worsening of proximal weakness at the lower limbs, the patient underwent a muscle biopsy (vastus lateralis), which revealed the coexistence of neurogenic alterations and myopathic features, compatible with an inflammatory myopathy. An oral steroid course was started but the patient failed to respond, deteriorating further until tracheostomy. Discussion: Polymyositis can rarely mimic ALS but this is, to our knowledge, the first report of cooccurrence of these two disorders. Muscle biopsy is required in order to confirm or discard this hypothesis. Moreover, albeit our case did not respond to treatment, a correct diagnosis could be extremely important due to the possible favourable response of polymyositis to steroids.

Published

2012

3. D4Z4 reduced allele in myopathic subjects with no FSHD phenotype: why inconsistency between molecular and clinical data should prompt us to further investigations

Author

Daolio, Jessica, Nikolic, Ana, Ricci, Giulia, Govi, Monica, Mele, Fabiano, Carra, Serena, Vercelli, L., Antonini, G., Berardinelli, Maria Angela, Mongini, T., Servida, M., Ruggiero, L., Angelini, C., Cao, M., D’Angelo, G., Muzio, A. Di, Moggio, M., Morandi, L., Ricci, Eusebio, Rodolico, C., Santoro, Luisa, Siciliano, G., Tomelleri, G., and Tupler, Rossella

Subjects

FSHD, myopathy, genetic, FSHD, genetic, myopathy

Published

2013

4. A standardized clinical evaluation of patients affected by facioscapulohumeralmuscular dystrophy: The FSHD clinical score

Author

Lamperti, C, Fabbri, G, Vercelli, L, D'Amico, R, Frusciante, R, Bonifazi, E, Fiorillo, C, Borsato, C, Cao, M, Servida, M, Greco, F, DI LEO, Rita, Volpi, L, Manzoli, C, Cudia, P, Pastorello, E, Ricciardi, L, Siciliano, G, Galluzzi, G, Rodolico, Carmelo, Santoro, L, Tomelleri, G, Angelini, C, Ricci, E, Palmucci, L, Moggio, M, and Tupler, R.

Published

2010

5. A standardized clinical evaluation of patients affected by facioscapulohumeral muscular dystrophy: The FSHD clinical score

Author

Lamperti, C, Fabbri, G, Vercelli, L, D'Amico, R, Frusciante, Roberto, Bonifazi, E, Fiorillo, C, Borsato, C, Cao, C, Servida, M, Greco, F, Di Leo, R, Volpi, L, Manzoli, C, Cudia, P, Pastorelo, E, Ricciardi, L, Siciliano, G, Galluzzi, G, Rodolico, C, Santoro, L, Tomelleri, G, Ricci, Enzo, Palmucci, L, Moggio, M, and Tupler, R.

Subjects

fshd, Settore MED/26 - NEUROLOGIA

Published

2010

6. Unexpected high percentage of asymptomatic subjects carrying the FSHD molecular defect: Which factors contribute to the disease mechanism?

Author

Bonifazi, E, Lamperti, C, Fiorillo, C, Vercelli, L, Borsato, C, Frusciante, R, Servida, M, Greco, F, Frambolli, I, Colantoni, L, Ricci, G, Volpi, L, DI LEO, R, Manzoli, C, Cudia, P, Pastorello, E, Ricciardi, L, Govi, M, Scionti, I, Cao, M, Siciliano, G, Galluzzi, G, Morandi, L, DI MUZIO, A, Trevisan, Cp, Ricci, E, Rodolico, C, Santoro, L, Tomelleri, G, Angelini, Corrado, Palmucci, L, Moggio, M, and Tupler, Rg

Published

2009

7. A robust tool to quantify disability in patients affected by facioscapulohumeral muscular dystrophy

Author

Lamperti, C, Fabbri, G, Greco, F, Servida, M, Vercelli, L, Fiorillo, C, Borsato, C, Cao, M, Cudia, P, Frusciante, R, DI LEO, R, Volpi, L, D'Amico, R, Pastorello, E, Ricciardi, L, Galluzzi, G, Siciliano, G, Muzio, A, D'Angelo, G, Rodolico, C, Morandi, L, Tomelleri, G, Trevisan, C, Angelini, Corrado, Santoro, L, Ricci, E, Palmucci, L, Moggio, M, and Tupler, Rg

Published

2008

8. P17.79 * A MELANOMA-ASTROCYTOMA SYNDROME ASSOCIATED TO A CONSTITUTIVE MICRODUPLICATION ON 5P15.33, CONTAINING THE TERT GENE

Author

Servida, M., primary, Sciacca, F., additional, Paterra, R., additional, and Finocchiaro, G., additional

Published

2014

9. Clinical evaluation and cellular electrophysiology of a recessive clcn1 patient

Author

Lucchiari, S, Ulzi, G, Magri, F, Bucchia, M, Corbetta, F, Servida, M, Moggio, M, Comi, G, Lecchi, M, LECCHI, MARZIA MARIA, Lucchiari, S, Ulzi, G, Magri, F, Bucchia, M, Corbetta, F, Servida, M, Moggio, M, Comi, G, Lecchi, M, and LECCHI, MARZIA MARIA

Abstract

Here we present the case of a 32-year-old female patient with myotonia congenita. She carried two mutations in the CLCN1 gene that encodes the chloride channel ClC-1: p.Phe167Leu, which was previously identified in several families, and p.Val536Leu, which has been previously reported but not yet characterized by electrophysiological investigations. The patient's symptoms included generalized stiffness, myotonia, and muscle cramps mostly localized in the lower limbs. These symptoms started during childhood and worsened over the following years. The symptoms were exacerbated by low outside temperature, rest, stress, and fasting and were improved by mild exercise, suggesting a warm-up phenomenon. The mutation p.Phe167Leu has previously been associated with a slight shift in the overall open probability. Here we further analysed this mutation to extrapolate the voltage-dependence of the fast and slow gates. In our experimental conditions, p.Phe167Leu exclusively affected the slow gate, increasing the minimum open probability and displacing the voltage-dependence toward depolarized potentials. p.Val536Leu showed more severe effects, dramatically influencing the slow gate as well as modifying properties of the fast gate. Co-expression of the mutants in a human cell line to reproduce the compound heterozygous condition of the patient produced channels with altered voltage-dependence of the slow gate but a restored fast gate. The alteration of the slow mechanism was reflected by the relative open probability, reducing the contribution of ClC-1 channels in maintaining the resting membrane potential of skeletal muscles and thus explaining the myotonic phenotype of the patient.

Published

2013

10. Large scale genotype-phenotype analyses indicate that novel prognostic tools are required for families with facioscapulohumeral muscular dystrophy

Author

Ricci, G, Scionti, I, Sera, F, Govi, M, D'Amico, R, Frambolli, I, Mele, F, Filosto, M, Vercelli, L, Ruggiero, L, Berardinelli, A, Angelini, C, Antonini, G, Bucci, E, Cao, M, Daolio, J, Di Muzio, A, Di Leo, R, Galluzzi, G, Iannaccone, E, Maggi, L, Maruotti, V, Moggio, M, Mongini, T, Morandi, L, Nikolic, A, Pastorello, E, Ricci, Enzo, Rodolico, C, Santoro, L, Servida, M, Siciliano, G, Tomelleri, G, Tupler, R., Ricci, Enzo (ORCID:0000-0003-3092-3597), Ricci, G, Scionti, I, Sera, F, Govi, M, D'Amico, R, Frambolli, I, Mele, F, Filosto, M, Vercelli, L, Ruggiero, L, Berardinelli, A, Angelini, C, Antonini, G, Bucci, E, Cao, M, Daolio, J, Di Muzio, A, Di Leo, R, Galluzzi, G, Iannaccone, E, Maggi, L, Maruotti, V, Moggio, M, Mongini, T, Morandi, L, Nikolic, A, Pastorello, E, Ricci, Enzo, Rodolico, C, Santoro, L, Servida, M, Siciliano, G, Tomelleri, G, Tupler, R., and Ricci, Enzo (ORCID:0000-0003-3092-3597)

Abstract

Facioscapulohumeral muscular dystrophy has been genetically linked to reduced numbers (≤ 8) of D4Z4 repeats at 4q35 combined with 4A(159/161/168) DUX4 polyadenylation signal haplotype. However, we have recently reported that 1.3% of healthy individuals carry this molecular signature and 19% of subjects affected by facioscapulohumeral muscular dystrophy do not carry alleles with eight or fewer D4Z4 repeats. Therefore, prognosis for subjects carrying or at risk of carrying D4Z4 reduced alleles has become more complicated. To test for additional prognostic factors, we measured the degree of motor impairment in a large group of patients affected by facioscapulohumeral muscular dystrophy and their relatives who are carrying D4Z4 reduced alleles. The clinical expression of motor impairment was assessed in 530 subjects, 163 probands and 367 relatives, from 176 unrelated families according to a standardized clinical score. The associations between clinical severity and size of D4Z4 allele, degree of kinship, gender, age and 4q haplotype were evaluated. Overall, 32.2% of relatives did not display any muscle functional impairment. This phenotype was influenced by the degree of relation with proband, because 47.1% of second- through fifth-degree relatives were unaffected, whereas only 27.5% of first-degree family members did not show motor impairment. The estimated risk of developing motor impairment by age 50 for relatives carrying a D4Z4 reduced allele with 1-3 repeats or 4-8 repeats was 88.7% and 55%, respectively. Male relatives had a mean score significantly higher than females (5.4 versus 4.0, P = 0.003). No 4q haplotype was exclusively associated with the presence of disease. In 13% of families in which D4Z4 alleles with 4-8 repeats segregate, the diagnosis of facioscapulohumeral muscular dystrophy was reported only in one generation. In conclusion, this large-scale analysis provides further information that should be taken into account when counselling families in whic

Published

2013

11. Co-existence of amyotrophic lateral sclerosis and polymyositis: a case report

Author

Susani, E, Tremolizzo, L, Cereda, D, Santarone, ME, Marzorati, L, Messina, S, Servida, M, Moggio, M, Mora, G, Silani, V, Ferrarese, C, Susani, E, Tremolizzo, L, Cereda, D, Santarone, ME, Marzorati, L, Messina, S, Servida, M, Moggio, M, Mora, G, Silani, V, and Ferrarese, C

Abstract

Background: The diagnosis of amyotrophic lateral sclerosis (ALS) requires the careful exclusion of mimic syndromes in presence of involvement of both upper and lower motor neurons progressing over time. In the differential diagnosis myopathic processes must be considered. In particular, inclusion body myositis patients are often misdiagnosed as having ALS, due to the fact that these two conditions share some clinical and serological similarities. Other myopathies, such as polymyositis are even rarer and, as a general rule, a diagnosis of inflammatory myopathy tends to exclude ALS. Aim: Describe the case of an ALS patient that was subsequently co-diagnosed with polymyositis. Case Report: A 51-year-old woman with a 4-month history of distal muscle weakness and progressive hypotrophy at the upper limbs came to our attention. Her past medical history was significant for hypothyroidism. Neurological examination showed intact cranial nerves, diffuse mild bilateral weakness with wasting of the interossei muscles at the hands and evident fasciculations; deep tendon reflexes were increased at the upper limbs and decreased at the lower ones. Both brain and spinal cord MRI were normal, as it was the exam of the CSF. An EMG study revealed signs of acute denervation and fasciculations in both distal and proximal muscle of the arms; myopathic changes were not reported. Due to the unexpected bilateral worsening of proximal weakness at the lower limbs, the patient underwent a muscle biopsy (vastus lateralis), which revealed the coexistence of neurogenic alterations and myopathic features, compatible with an inflammatory myopathy. An oral steroid course was started but the patient failed to respond, deteriorating further until tracheostomy. Discussion: Polymyositis can rarely mimic ALS but this is, to our knowledge, the first report of cooccurrence of these two disorders. Muscle biopsy is required in order to confirm or discard this hypothesis. Moreover, albeit our case did not resp

Published

2012

12. Colocalization of ribonuclear inclusions with muscle blind like-proteins in a family with myotonic dystrophy type 2 associated with a short CCTG expansion

Author

Lucchiari, S., Pagliarani, S., Corti, S., Mancinelli, E., Servida, M., Fruguglietti, E., Sansone, V., Moggio, M., Bresolin, N., Comi, G.P., and Meola, G.

Published

2008

13. G.P.15.09 Unexpected high percentage of asymptomatic subjects carrying the FSHD molecular defect: Which factors contribute to the disease mechanism?

Author

Bonifazi, E., primary, Lamperti, C., additional, Fiorillo, C., additional, Vercelli, L., additional, Borsato, C., additional, Frusciante, R., additional, Servida, M., additional, Greco, F., additional, Frambolli, I., additional, Colantoni, L., additional, Ricci, G., additional, Volpi, L., additional, Di Leo, R., additional, Manzoli, C., additional, Cudia, P., additional, Pastorello, E., additional, Ricciardi, L., additional, Govi, M., additional, Scionti, I., additional, Cao, M., additional, Siciliano, G., additional, Galluzzi, G., additional, Morandi, L., additional, Di Muzio, A., additional, Trevisan, C.P., additional, Ricci, E., additional, Rodolico, C., additional, Santoro, L., additional, Tomelleri, G., additional, Angelini, C., additional, Palmucci, L., additional, Moggio, M., additional, and Tupler, R.G., additional

Published

2009

14. D.P.1.08 Morphological pattern of muscle biopsy in a large cohort of FSHD patients

Author

Crugnola, V., primary, Ghiaroni, V., additional, Ciscato, P., additional, Servida, M., additional, Prelle, A., additional, Sciacco, M., additional, Tiberio, F., additional, Borsa, S., additional, Tupler, R.G., additional, Bresolin, N., additional, Moggio, M., additional, and Lamperti, C., additional

Published

2008

15. D.P.1.02 A robust tool to quantify disability in patients affected by facioscapulohumeral muscular dystrophy

Author

Lamperti, C., primary, Fabbri, G., additional, Greco, F., additional, Servida, M., additional, Vercelli, L., additional, Fiorillo, C., additional, Borsato, C., additional, Cao, M., additional, Cudia, P., additional, Frusciante, R., additional, Leo, R. Di, additional, Volpi, L., additional, d’Amico, R., additional, Pastorello, E., additional, Ricciardi, L., additional, Galluzzi, G., additional, Siciliano, G., additional, Muzio, A., additional, D’Angelo, G., additional, Rodolico, C., additional, Morandi, L., additional, Tomelleri, G., additional, Trevisan, C., additional, Angelini, C., additional, Santoro, L., additional, Ricci, E., additional, Palmucci, L., additional, Moggio, M., additional, and Tupler, R.G., additional

Published

2008

16. Clinical evaluation and cellular electrophysiology of a recessive clcn1 patient

Author

Lucchiari S, Ulzi G, Francesca Magri, Bucchia M, Corbetta F, Servida M, Moggio M, Gp, Comi, Lecchi M, Lucchiari, S, Ulzi, G, Magri, F, Bucchia, M, Corbetta, F, Servida, M, Moggio, M, Comi, G, and Lecchi, M

Subjects

Adult, Myotonia Congenita, Chloride Channels, BIO/09 - FISIOLOGIA, Mutation, Humans, channelopathy, CLCN1 gene, skeletal muscle, myotonia congenita, Becker’s generalized myotonia, electrophysiology, Female, Cell Line

Abstract

Here we present the case of a 32-year-old female patient with myotonia congenita. She carried two mutations in the CLCN1 gene that encodes the chloride channel ClC-1: p.Phe167Leu, which was previously identified in several families, and p.Val536Leu, which has been previously reported but not yet characterized by electrophysiological investigations. The patient's symptoms included generalized stiffness, myotonia, and muscle cramps mostly localized in the lower limbs. These symptoms started during childhood and worsened over the following years. The symptoms were exacerbated by low outside temperature, rest, stress, and fasting and were improved by mild exercise, suggesting a warm-up phenomenon. The mutation p.Phe167Leu has previously been associated with a slight shift in the overall open probability. Here we further analysed this mutation to extrapolate the voltage-dependence of the fast and slow gates. In our experimental conditions, p.Phe167Leu exclusively affected the slow gate, increasing the minimum open probability and displacing the voltage-dependence toward depolarized potentials. p.Val536Leu showed more severe effects, dramatically influencing the slow gate as well as modifying properties of the fast gate. Co-expression of the mutants in a human cell line to reproduce the compound heterozygous condition of the patient produced channels with altered voltage-dependence of the slow gate but a restored fast gate. The alteration of the slow mechanism was reflected by the relative open probability, reducing the contribution of ClC-1 channels in maintaining the resting membrane potential of skeletal muscles and thus explaining the myotonic phenotype of the patient.

17. IMCT-06SURVIVAL GAIN AND IMMUNE RESPONSE IN GLIOBLASTOMA PATIENTS TREATED WITH DENDRITIC CELL IMMUNOTHERAPY BEFORE AND DURING ADJUVANT TEMOZOLOMIDE

Author

Finocchiaro G, Eoli M, Pellegatta S, Anghileri E, Frigerio S, Bianca Pollo, Cuccarini V, Antozzi C, Acerbi F, Cuppini L, Porrati P, Pessina S, Servida M, and Parati E

18. Adult brainstem glioma: a multicentre retrospective analysis of 47 Italian patients

Author

Giorgia Simonetti, Andrea Salmaggi, Giulia Berzero, Roberta Rudà, R. Merli, Federica Franchino, Antonio Silvani, Ivano Chiarotti, Andrea Pace, Giannantonio Spena, Maura Servida, Alfonso Cerase, Veronica Villani, Andrea Rigamonti, Alberto Picca, Rigamonti, A., Simonetti, G., Silvani, A., Ruda, R., Franchino, F., Villani, V., Pace, A., Merli, R., Servida, M., Picca, A., Berzero, G., Cerase, A., Chiarotti, I., Spena, G., and Salmaggi, A.

Subjects

Oncology, Adult, Male, medicine.medical_specialty, Survival, Dermatology, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Glioma, Biopsy, medicine, Brain Stem Neoplasms, Humans, 030212 general & internal medicine, Neuroradiology, Retrospective Studies, Univariate analysis, Performance status, medicine.diagnostic_test, business.industry, Brain Neoplasms, Retrospective cohort study, General Medicine, medicine.disease, Prognosis, Management, Brainstem gliomas, Clinical trial, Psychiatry and Mental health, Italy, Female, Neurology (clinical), Neurosurgery, business, 030217 neurology & neurosurgery

Abstract

Background and purpose: Adult brainstem gliomas are rare primary brain tumours with heterogeneous clinical course. The low frequency of these tumours makes it difficult to achieve high-quality evidence regarding prognostic factors, adequate therapeutic approach and outcome in such patients. Methods: In this retrospective study, we analysed clinical, radiological, molecular, prognostic and therapeutic factors in a series of 47 histologically proven adult brainstem gliomas recruited over a 20-year period (1998–2018). Results: Twenty-two patients were male, 25 female with median age of 39 years. The tumour involved one brainstem segment in 20 cases and 2 or more segments in 27. Contrast enhancement was reported in 28 cases. Surgical procedures included biopsy in 26 cases and partial/total resection in the remaining 21. Histological diagnosis was of low-grade glioma in 23 patients, high-grade glioma in 22 and non-diagnostic in 2 cases. Data regarding molecular biology were available for 22 patients. Median overall survival was 35 months, in particular 16 months in high-grade glioma and 84 months in low-grade glioma. At univariate analysis, tumour grade was the only factor with a statistically significant impact on survival time (p = 0,003), whereas younger age, better performance status and total/subtotal resection showed a trend to more prolonged survival. This study also confirms safety of biopsy/surgery in adult brainstem glioma patients and shows a clear trend to a more frequent assessment of molecular biology data. Conclusions: Further prospective multicentre efforts, and hopefully clinical trials, are necessary to improve outcome in this neglected glioma patient population.

Published

2020

19. Survival gain in glioblastoma patients treated with dendritic cell immunotherapy is associated with increased NK but not CD8+ T cell activation in the presence of adjuvant temozolomide

Author

Rosina Paterra, Francesco DiMeco, Eugenio Parati, Laura Fariselli, Francesco Acerbi, Marica Eoli, Paolo Ferroli, Gaetano Finocchiaro, Bianca Pollo, Maria Grazia Bruzzone, Simona Frigerio, Carlo Antozzi, Cristina Corbetta, Valeria Cuccarini, Maura Servida, Sara Pessina, Stefania Cuzzubbo, Serena Pellegatta, Lucia Cuppini, Elena Anghileri, Pellegatta, S, Eoli, M, Cuccarini, V, Anghileri, E, Pollo, B, Pessina, S, Frigerio, S, Servida, M, Cuppini, L, Antozzi, C, Cuzzubbo, S, Corbetta, C, Paterra, R, Acerbi, F, Ferroli, P, Dimeco, F, Fariselli, L, Parati, E, Bruzzone, M, and Finocchiaro, G

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, Oncology, medicine.medical_specialty, dendritic cell, medicine.medical_treatment, Immunology, Phases of clinical research, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Immunology and Allergy, Cytotoxic T cell, dendritic cells, Chemotherapy, natural killer cells, Temozolomide, business.industry, Dendritic cell, Immunotherapy, natural killer cell, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, adjuvant chemotherapy, 030104 developmental biology, 030220 oncology & carcinogenesis, immunotherapy, lcsh:RC581-607, Glioblastoma, business, Adjuvant, CD8, medicine.drug

Abstract

In a two-stage phase II study, 24 patients with first diagnosis of glioblastoma (GBM) were treated with dendritic cell (DC) immunotherapy associated to standard radiochemotherapy with temozolomide (TMZ) followed by adjuvant TMZ. Three intradermal injections of mature DC loaded with autologous GBM lysate were administered before adjuvant TMZ, while 4 injections were performed during adjuvant TMZ. According to a two-stage Simon design, to proceed to the second stage progression-free survival (PFS) 12 months after surgery was expected in at least 8 cases enrolled in the first stage. Evidence of immune response and interaction with chemotherapy were investigated. After a median follow up of 17.4 months, 9 patients reached PFS12. In these patients (responders, 37.5%), DC vaccination induced a significant, persistent activation of NK cells, whose increased response was significantly associated with prolonged survival. CD8+ T cells underwent rapid expansion and priming but, after the first administration of adjuvant TMZ, failed to generate a memory status. Resistance to TMZ was associated with robust expression of the multidrug resistance protein ABCC3 in NK but not CD8+ T cells. The negative effect of TMZ on the formation of T cell-associated antitumor memory deserves consideration in future clinical trials including immunotherapy.

Published

2018

20. A standardized clinical evaluation of patients affected by facioscapulohumeral muscular dystrophy: The FSHD clinical score

Author

Costanza, Lamperti, Greta, Fabbri, Liliana, Vercelli, Roberto, D'Amico, Roberto, Frusciante, Emanuela, Bonifazi, Chiara, Fiorillo, Carlo, Borsato, Michelangelo, Cao, Maura, Servida, Francesca, Greco, Rita, Di Leo, Leda, Volpi, Claudia, Manzoli, Paola, Cudia, Ebe, Pastorello, Leopoldo, Ricciardi, Gabriele, Siciliano, Giuliana, Galluzzi, Carmelo, Rodolico, Lucio, Santoro, Giuliano, Tomelleri, Corrado, Angelini, Enzo, Ricci, Laura, Palmucci, Maurizio, Moggio, Rossella, Tupler, Lamperti, C, Fabbri, G, Vercelli, L, D'Amico, R, Frusciante, R, Bonifazi, E, Fiorillo, C, Borsato, C, Cao, M, Servida, M, Greco, F, Di Leo, R, Volpi, L, Manzoli, C, Cudia, P, Pastorello, E, Ricciardi, L, Siciliano, G, Galluzzi, G, Rodolico, C, Santoro, Lucio, Tomelleri, G, Angelini, C, Ricci, E, Palmucci, L, Moggio, M, and Tupler, R.

Subjects

Adult, Aged, 80 and over, Male, clinical evaluation form, FSHD, Muscle Weakness, severity score, facioscapulohumeral muscular dystrophy, Adolescent, clinical severity score, Reproducibility of Results, Middle Aged, Severity of Illness Index, Muscular Dystrophy, Facioscapulohumeral, muscle weakness distribution, Kappa-statistic, Humans, Female, Aged

Abstract

To define numerically the clinical severity of facioscapulohumeral muscular dystrophy (FSHD), we developed a protocol that quantifies muscle weakness by combining the functional evaluation of six muscle groups affected in this disease. To validate reproducibility of the protocol, 69 patients were recruited. Each patient was evaluated by at least five neurologists, and an FSHD severity score was given by each examiner. The degree of agreement among clinicians' evaluations was measured by kappa-statistics. Nineteen subjects received a score between 0 and 1, 9 had a score between 2 and 4, 20 received a score between 5 and 10, and 8 had a score between 11 and 15. Of the 13 subjects with D4Z4 alleles within the normal range (ranging from 10 to 150 repeats), 12 obtained a score of 0 and only 1 had a score of 1. Kappa-statistics showed a very high concordance for all muscle groups. We developed a simple, reliable, easily used tool to define the clinical expression of FSHD. Longitudinal studies will assess its sensitivity and utility in measuring changes for widespread use.

Published

2010

21. Adult brainstem glioma: a multicentre retrospective analysis of 47 Italian patients.

Author

Rigamonti A, Simonetti G, Silvani A, Rudà R, Franchino F, Villani V, Pace A, Merli R, Servida M, Picca A, Berzero G, Cerase A, Chiarotti I, Spena G, and Salmaggi A

Subjects

Adult, Female, Humans, Italy epidemiology, Male, Prognosis, Retrospective Studies, Brain Neoplasms diagnostic imaging, Brain Neoplasms genetics, Brain Neoplasms therapy, Brain Stem Neoplasms diagnostic imaging, Brain Stem Neoplasms genetics, Brain Stem Neoplasms therapy, Glioma diagnostic imaging, Glioma genetics, Glioma therapy

Abstract

Background and Purpose: Adult brainstem gliomas are rare primary brain tumours with heterogeneous clinical course. The low frequency of these tumours makes it difficult to achieve high-quality evidence regarding prognostic factors, adequate therapeutic approach and outcome in such patients., Methods: In this retrospective study, we analysed clinical, radiological, molecular, prognostic and therapeutic factors in a series of 47 histologically proven adult brainstem gliomas recruited over a 20-year period (1998-2018)., Results: Twenty-two patients were male, 25 female with median age of 39 years. The tumour involved one brainstem segment in 20 cases and 2 or more segments in 27. Contrast enhancement was reported in 28 cases. Surgical procedures included biopsy in 26 cases and partial/total resection in the remaining 21. Histological diagnosis was of low-grade glioma in 23 patients, high-grade glioma in 22 and non-diagnostic in 2 cases. Data regarding molecular biology were available for 22 patients. Median overall survival was 35 months, in particular 16 months in high-grade glioma and 84 months in low-grade glioma. At univariate analysis, tumour grade was the only factor with a statistically significant impact on survival time (p = 0,003), whereas younger age, better performance status and total/subtotal resection showed a trend to more prolonged survival. This study also confirms safety of biopsy/surgery in adult brainstem glioma patients and shows a clear trend to a more frequent assessment of molecular biology data., Conclusions: Further prospective multicentre efforts, and hopefully clinical trials, are necessary to improve outcome in this neglected glioma patient population.

Published

2021

22. Biopsy-proven primary angiitis of the central nervous system mimicking leukodystrophy: A case report and review of the literature.

Author

Caputi L, Erbetta A, Marucci G, Pareyson D, Eoli M, Servida M, Parati E, and Salsano E

Subjects

Biopsy, Female, Humans, Immunosuppressive Agents therapeutic use, Leukoencephalopathies diagnosis, Leukoencephalopathies pathology, Middle Aged, Vasculitis, Central Nervous System drug therapy, Vasculitis, Central Nervous System diagnosis

Abstract

Primary Angiitis of the Central Nervous System (PACNS) is a rare form of idiopathic CNS vasculitis. Neuroimaging is often abnormal and characterized by multifocal brain lesions, but brain biopsy definitely confirms the diagnosis. We report the rare case of a 45-year-old female presenting with symptoms of intracranial hypertension and leukodystrophy-like neuroimaging findings. A comprehensive diagnostic work-up led to the unexpected diagnosis of a definite PACNS which was successfully treated by immunosuppressive treatment. Although rarely, PACNS can present as diffuse leukoencephalopathy on neuroimaging, and mimic even an inherited leukodystrophy. Therefore, in adults with leukodystrophy-like neuroimaging findings, careful examination of clinical and non-clinical features is mandatory to avoid missing the diagnosis of a treatable acquired disease., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

23. Survival gain in glioblastoma patients treated with dendritic cell immunotherapy is associated with increased NK but not CD8 + T cell activation in the presence of adjuvant temozolomide.

Author

Pellegatta S, Eoli M, Cuccarini V, Anghileri E, Pollo B, Pessina S, Frigerio S, Servida M, Cuppini L, Antozzi C, Cuzzubbo S, Corbetta C, Paterra R, Acerbi F, Ferroli P, DiMeco F, Fariselli L, Parati EA, Bruzzone MG, and Finocchiaro G

Abstract

In a two-stage phase II study, 24 patients with first diagnosis of glioblastoma (GBM) were treated with dendritic cell (DC) immunotherapy associated to standard radiochemotherapy with temozolomide (TMZ) followed by adjuvant TMZ. Three intradermal injections of mature DC loaded with autologous GBM lysate were administered before adjuvant TMZ, while 4 injections were performed during adjuvant TMZ. According to a two-stage Simon design, to proceed to the second stage progression-free survival (PFS) 12 months after surgery was expected in at least 8 cases enrolled in the first stage. Evidence of immune response and interaction with chemotherapy were investigated. After a median follow up of 17.4 months, 9 patients reached PFS12. In these patients (responders, 37.5%), DC vaccination induced a significant, persistent activation of NK cells, whose increased response was significantly associated with prolonged survival. CD8 + T cells underwent rapid expansion and priming but, after the first administration of adjuvant TMZ, failed to generate a memory status. Resistance to TMZ was associated with robust expression of the multidrug resistance protein ABCC3 in NK but not CD8 + T cells. The negative effect of TMZ on the formation of T cell-associated antitumor memory deserves consideration in future clinical trials including immunotherapy.

Published

2018

24. Fluorescein-Guided Surgery for Resection of High-Grade Gliomas: A Multicentric Prospective Phase II Study (FLUOGLIO).

Author

Acerbi F, Broggi M, Schebesch KM, Höhne J, Cavallo C, De Laurentis C, Eoli M, Anghileri E, Servida M, Boffano C, Pollo B, Schiariti M, Visintini S, Montomoli C, Bosio L, La Corte E, Broggi G, Brawanski A, and Ferroli P

Subjects

Adult, Aged, Brain Neoplasms, Disease Management, Female, Glioma diagnostic imaging, Glioma mortality, Humans, Kaplan-Meier Estimate, Magnetic Resonance Imaging methods, Male, Middle Aged, Neoplasm Grading, Neoplasm Staging, Treatment Outcome, Fluorescent Dyes, Glioma pathology, Glioma surgery, Surgery, Computer-Assisted adverse effects, Surgery, Computer-Assisted methods

Abstract

Purpose: Sodium fluorescein is a dye that, intravenously injected, selectively accumulates in high-grade glioma (HGG) tissue through a damaged blood-brain barrier. In this article, the final results of a multicentric prospective phase II trial (FLUOGLIO) on fluorescein-guided HGG resection through a dedicated filter on the surgical microscope were reported. Methods: Patients with suspected HGGs considered suitable for removal were eligible to participate in this trial. Fluorescein was intravenously injected at a dose of 5 to 10 mg/kg. The primary endpoint was the percentage of patients with histologically confirmed HGGs, without contrast-enhancing tumor at the immediate postoperative MRI. Secondary endpoints were PFS, residual tumor on postoperative MRI, overall survival, neurologic deficits, and fluorescein-related toxicity. The sensitivity and specificity of fluorescein in identifying tumor tissue were estimated by fluorescent and nonfluorescent biopsies at the tumor margin. The study was registered on the European Regulatory Authorities website (EudraCT 2011-002527-18). Results: Fifty-seven patients aged 45 to 75 years were screened for participation, and 46 were considered for primary and secondary endpoints. Mean preoperative tumor volume was 28.75 cm 3 (range, 1.3-87.8 cm 3 ). Thirty-eight patients (82.6%) underwent a complete tumor removal. Median follow-up was 11 months. PFS-6 and PFS-12 were 56.6% and 15.2%. Median survival was 12 months. No adverse reaction related to SF administration was recorded. The sensitivity and specificity of fluorescein in identifying tumor tissue were respectively 80.8% and 79.1%. Conclusions: Fluorescein-guided technique with a dedicated filter on the surgical microscope is safe and enables a high percentage of contrast-enhancing tumor in patients with HGGs. Clin Cancer Res; 24(1); 52-61. ©2017 AACR ., (©2017 American Association for Cancer Research.)

Published

2018

25. Vaccination recommendations for patients with neuromuscular disease.

Author

Esposito S, Bruno C, Berardinelli A, Filosto M, Mongini T, Morandi L, Musumeci O, Pegoraro E, Siciliano G, Tonin P, Marrosu G, Minetti C, Servida M, Fiorillo C, Conforti G, Scapolan S, Ansaldi F, Vianello A, Castaldi S, Principi N, Toscano A, and Moggio M

Subjects

Contraindications, Humans, Vaccination, Vaccines, Attenuated therapeutic use, Immunocompromised Host, Influenza Vaccines therapeutic use, Neuromuscular Diseases immunology, Pneumococcal Vaccines therapeutic use

Abstract

Neuromuscular diseases (NMDs) encompass a broad spectrum of conditions. Because infections may be relevant to the final prognosis of most NMDs, vaccination appears to be the simplest and most effective solution for protecting NMD patients from vaccine-preventable infections. However, very few studies have evaluated the immunogenicity, safety, tolerability, and efficacy of different vaccines in NMD patients; therefore, detailed vaccination recommendations for NMD patients are not available. Here, we present vaccination recommendations from a group of Italian Scientific Societies for optimal disease prevention in NMD patients that maintain high safety levels. We found that NMD patients can be classified into two groups according to immune function: patients with normal immunity and patients who are immunocompromised, including those who intermittently or continuously take immunosuppressive therapy. Patients with normal immunity and do not take immunosuppressive therapy can be vaccinated as healthy subjects. In contrast, immunocompromised patients, including those who take immunosuppressive therapy, should receive all inactivated vaccines as well as influenza and pneumococcal vaccines; these patients should not be administered live attenuated vaccines. In all cases, the efficacy and long-term persistence of immunity from vaccination in NMD patients can be lower than in normal subjects. Household contacts of immunocompromised NMD patients should also be vaccinated appropriately., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

26. Large scale genotype-phenotype analyses indicate that novel prognostic tools are required for families with facioscapulohumeral muscular dystrophy.

Author

Ricci G, Scionti I, Sera F, Govi M, D'Amico R, Frambolli I, Mele F, Filosto M, Vercelli L, Ruggiero L, Berardinelli A, Angelini C, Antonini G, Bucci E, Cao M, Daolio J, Di Muzio A, Di Leo R, Galluzzi G, Iannaccone E, Maggi L, Maruotti V, Moggio M, Mongini T, Morandi L, Nikolic A, Pastorello E, Ricci E, Rodolico C, Santoro L, Servida M, Siciliano G, Tomelleri G, and Tupler R

Subjects

Adolescent, Adult, Aged, Chromosome Deletion, Chromosome Disorders physiopathology, Chromosomes, Human, Pair 4 genetics, Female, Genetic Predisposition to Disease genetics, Haplotypes genetics, Humans, Male, Middle Aged, Muscular Dystrophy, Facioscapulohumeral physiopathology, Pedigree, Prognosis, Young Adult, Chromosome Disorders genetics, Genetic Association Studies methods, Homeodomain Proteins genetics, Muscular Dystrophy, Facioscapulohumeral genetics, Registries

Abstract

Facioscapulohumeral muscular dystrophy has been genetically linked to reduced numbers (≤ 8) of D4Z4 repeats at 4q35 combined with 4A(159/161/168) DUX4 polyadenylation signal haplotype. However, we have recently reported that 1.3% of healthy individuals carry this molecular signature and 19% of subjects affected by facioscapulohumeral muscular dystrophy do not carry alleles with eight or fewer D4Z4 repeats. Therefore, prognosis for subjects carrying or at risk of carrying D4Z4 reduced alleles has become more complicated. To test for additional prognostic factors, we measured the degree of motor impairment in a large group of patients affected by facioscapulohumeral muscular dystrophy and their relatives who are carrying D4Z4 reduced alleles. The clinical expression of motor impairment was assessed in 530 subjects, 163 probands and 367 relatives, from 176 unrelated families according to a standardized clinical score. The associations between clinical severity and size of D4Z4 allele, degree of kinship, gender, age and 4q haplotype were evaluated. Overall, 32.2% of relatives did not display any muscle functional impairment. This phenotype was influenced by the degree of relation with proband, because 47.1% of second- through fifth-degree relatives were unaffected, whereas only 27.5% of first-degree family members did not show motor impairment. The estimated risk of developing motor impairment by age 50 for relatives carrying a D4Z4 reduced allele with 1-3 repeats or 4-8 repeats was 88.7% and 55%, respectively. Male relatives had a mean score significantly higher than females (5.4 versus 4.0, P = 0.003). No 4q haplotype was exclusively associated with the presence of disease. In 13% of families in which D4Z4 alleles with 4-8 repeats segregate, the diagnosis of facioscapulohumeral muscular dystrophy was reported only in one generation. In conclusion, this large-scale analysis provides further information that should be taken into account when counselling families in which a reduced allele with 4-8 D4Z4 repeats segregates. In addition, the reduced expression of disease observed in distant relatives suggests that a family's genetic background plays a role in the occurrence of facioscapulohumeral muscular dystrophy. These results indicate that the identification of new susceptibility factors for this disease will require an accurate classification of families.

Published

2013

27. Clinical evaluation and cellular electrophysiology of a recessive CLCN1 patient.

Author

Lucchiari S, Ulzi G, Magri F, Bucchia M, Corbetta F, Servida M, Moggio M, Comi GP, and Lecchi M

Subjects

Adult, Cell Line, Chloride Channels genetics, Female, Humans, Mutation, Myotonia Congenita genetics, Chloride Channels physiology, Myotonia Congenita physiopathology

Abstract

Here we present the case of a 32-year-old female patient with myotonia congenita. She carried two mutations in the CLCN1 gene that encodes the chloride channel ClC-1: p.Phe167Leu, which was previously identified in several families, and p.Val536Leu, which has been previously reported but not yet characterized by electrophysiological investigations. The patient's symptoms included generalized stiffness, myotonia, and muscle cramps mostly localized in the lower limbs. These symptoms started during childhood and worsened over the following years. The symptoms were exacerbated by low outside temperature, rest, stress, and fasting and were improved by mild exercise, suggesting a warm-up phenomenon. The mutation p.Phe167Leu has previously been associated with a slight shift in the overall open probability. Here we further analysed this mutation to extrapolate the voltage-dependence of the fast and slow gates. In our experimental conditions, p.Phe167Leu exclusively affected the slow gate, increasing the minimum open probability and displacing the voltage-dependence toward depolarized potentials. p.Val536Leu showed more severe effects, dramatically influencing the slow gate as well as modifying properties of the fast gate. Co-expression of the mutants in a human cell line to reproduce the compound heterozygous condition of the patient produced channels with altered voltage-dependence of the slow gate but a restored fast gate. The alteration of the slow mechanism was reflected by the relative open probability, reducing the contribution of ClC-1 channels in maintaining the resting membrane potential of skeletal muscles and thus explaining the myotonic phenotype of the patient.

Published

2013

28. Optic atrophy plus phenotype due to mutations in the OPA1 gene: two more Italian families.

Author

Ranieri M, Del Bo R, Bordoni A, Ronchi D, Colombo I, Riboldi G, Cosi A, Servida M, Magri F, Moggio M, Bresolin N, Comi GP, and Corti S

Subjects

Adolescent, Amino Acid Substitution genetics, Child, Female, Gene Deletion, Humans, Italy, Male, Middle Aged, Pedigree, GTP Phosphohydrolases genetics, Mutation genetics, Optic Atrophy diagnosis, Optic Atrophy genetics, Phenotype

Abstract

Autosomal Dominant Optic Atrophy (ADOA) is characterized by the selective degeneration of retinal ganglion cells. The occurrence of mutations in the gene encoding the dynamin-like GTPase protein Optic Atrophy 1 (OPA1) has been observed in about 60-70% of ADOA cases. A subset of missense mutations, mostly within the GTPase domain, has recently been associated with a syndromic ADOA form called "OPA1 plus" phenotype presenting, at muscle level, mitochondrial DNA (mtDNA) instability. In this study we disclosed two OPA1 gene mutations in independent probands from two families affected by OPA1 plus phenotype: the previously reported c.985-2A>G substitution and a novel microdeletion (c.2819-1_2821del). The correlation between genotype and phenotype and the effects of these variants at the transcript level and in the muscle tissue were investigated, confirming the broad complexity in the phenotypic spectrum associated with these OPA1 mutations., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2012

29. The novel mitochondrial tRNAAsn gene mutation m.5709T>C produces ophthalmoparesis and respiratory impairment.

Author

Ronchi D, Sciacco M, Bordoni A, Raimondi M, Ripolone M, Fassone E, Di Fonzo A, Rizzuti M, Ciscato P, Cosi A, Servida M, Moggio M, Corti S, Bresolin N, and Comi GP

Subjects

Base Sequence, Electron Transport Complex IV genetics, Female, Humans, Middle Aged, Mitochondrial Myopathies diagnosis, Mitochondrial Myopathies genetics, Muscle Fibers, Skeletal enzymology, Ophthalmoplegia diagnosis, Phenotype, RNA, Mitochondrial, Sequence Alignment, Mutation, Ophthalmoplegia genetics, RNA genetics, RNA, Transfer, Asn genetics

Abstract

Although mutations in mitochondrial tRNAs constitute the most common mtDNA defect, the presence of pathological variants in mitochondrial tRNA(Asn) is extremely rare. We were able to identify a novel mtDNA tRNA(Asn) gene pathogenic mutation associated with a myopathic phenotype and a previously unreported respiratory impairment. Our proband is an adult woman with ophthalmoparesis and respiratory impairment. Her muscle biopsy presented several cytochrome c oxidase-negative (COX-) fibres and signs of mitochondrial proliferation (ragged red fibres). Sequence analysis of the muscle-derived mtDNA revealed an m.5709T>C substitution, affecting mitochondrial tRNA(Asn) gene. Restriction-fragment length polymorphism analysis of the mutation in isolated muscle fibres showed that a threshold of at least 91.9% mutated mtDNA results in the COX deficiency phenotype. The new phenotype further increases the clinical spectrum of mitochondrial diseases caused by mutations in the tRNA(Asn) gene.

Published

2012

30. Unusual adult-onset Leigh syndrome presentation due to the mitochondrial m.9176T>C mutation.

Author

Ronchi D, Bordoni A, Cosi A, Rizzuti M, Fassone E, Di Fonzo A, Servida M, Sciacco M, Collotta M, Ronzoni M, Lucchini V, Mattioli M, Moggio M, Bresolin N, Corti S, and Comi GP

Subjects

Adult, Age of Onset, Female, Humans, Leigh Disease pathology, Muscle, Skeletal pathology, Mutation, Pedigree, DNA, Mitochondrial genetics, Genes, Mitochondrial, Leigh Disease genetics

Abstract

Leigh syndrome (LS) is an incurable, nearly always fatal, neurodegenerative, pediatric disorder that results from respiratory chain failure. The most common mitochondrial DNA (mtDNA) mutations that result in LS are m.8993T→C/G and m.9176T→C/G, which were previously found in several patients with early-onset Leigh syndrome. Here, we describe clinical and molecular features of a novel pedigree, where LS developed in two siblings. The proband was a young woman with an unusual adult-onset LS. She harbored a homoplasmic m.9176T→C mutation, based on analysis of a muscle biopsy. In contrast, the brother died at a young age. This novel case report and literature review highlights the variability of phenotypic expression of the m.9176T→C mutation., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

31. A standardized clinical evaluation of patients affected by facioscapulohumeral muscular dystrophy: The FSHD clinical score.

Author

Lamperti C, Fabbri G, Vercelli L, D'Amico R, Frusciante R, Bonifazi E, Fiorillo C, Borsato C, Cao M, Servida M, Greco F, Di Leo R, Volpi L, Manzoli C, Cudia P, Pastorello E, Ricciardi L, Siciliano G, Galluzzi G, Rodolico C, Santoro L, Tomelleri G, Angelini C, Ricci E, Palmucci L, Moggio M, and Tupler R

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Female, Humans, Male, Middle Aged, Muscle Weakness genetics, Muscle Weakness physiopathology, Muscular Dystrophy, Facioscapulohumeral physiopathology, Reproducibility of Results, Severity of Illness Index, Muscle Weakness diagnosis, Muscular Dystrophy, Facioscapulohumeral diagnosis

Abstract

To define numerically the clinical severity of facioscapulohumeral muscular dystrophy (FSHD), we developed a protocol that quantifies muscle weakness by combining the functional evaluation of six muscle groups affected in this disease. To validate reproducibility of the protocol, 69 patients were recruited. Each patient was evaluated by at least five neurologists, and an FSHD severity score was given by each examiner. The degree of agreement among clinicians' evaluations was measured by kappa-statistics. Nineteen subjects received a score between 0 and 1, 9 had a score between 2 and 4, 20 received a score between 5 and 10, and 8 had a score between 11 and 15. Of the 13 subjects with D4Z4 alleles within the normal range (ranging from 10 to 150 repeats), 12 obtained a score of 0 and only 1 had a score of 1. Kappa-statistics showed a very high concordance for all muscle groups. We developed a simple, reliable, easily used tool to define the clinical expression of FSHD. Longitudinal studies will assess its sensitivity and utility in measuring changes for widespread use.

Published

2010