Your search keyword '"Servidei S."' showing total 32 results

1. Novel TNNT1 mutation and mild nemaline myopathy phenotype in an Italian patient.

Author

Petrucci A, Primiano G, Savarese M, Sancricca C, Udd B, and Servidei S

Subjects

Female, Humans, Italy, Middle Aged, Myopathies, Nemaline diagnosis, Respiratory Insufficiency etiology, Mutation genetics, Myopathies, Nemaline genetics, Phenotype, Troponin T genetics

Abstract

Mutations in the TNNT1 gene cause an infantile, lethal form of myopathy named "Amish" Nemaline Myopathy. Adult patients are very rarely described. We report a 49-year-old patient who presented a slowly progressive phenotype characterized by myalgia, exercise intolerance and dyspnea since infancy. In adult life she lapsed into a coma as a result of acute respiratory failure, with the need of tracheostomy, subsequently removed once her respiratory condition improved. Afterwards, non-invasive ventilation was started. Short stature, contractures, a small size posterior cranial fossa and osteonecrosis were additional clinical findings. Muscle MRI showed minor hypotrophy and degenerative changes of the muscles of the posterior thigh compartment and involvement of the paraspinal, medial gastrocnemius and soleus muscles with sparing of the gracilis muscle. Muscle biopsy revealed multiminicores and nemaline rods. Genetic analysis identified a new pathogenetic biallelic deletion c.786delG p.(Lys263Serfs*36) in exon 13 of TNNT1 gene. This case confirms that recessive mutations in TNNT1 gene can manifest mainly with respiratory failure in adult life., Competing Interests: Declaration of Competing Interest Nothing to declare, (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

2. Novel KCND3 Variant Underlying Nonprogressive Congenital Ataxia or SCA19/22 Disrupt K V 4.3 Protein Expression and K+ Currents with Variable Effects on Channel Properties.

Author

Zanni G, Hsiao CT, Fu SJ, Tang CY, Capuano A, Bosco L, Graziola F, Bellacchio E, Servidei S, Primiano G, Soong BW, and Jeng CJ

Subjects

Amino Acid Sequence, Animals, Child, Female, HEK293 Cells, Humans, Magnetic Resonance Imaging, Male, Middle Aged, Proteostasis, Spinocerebellar Ataxias diagnostic imaging, Xenopus laevis, Ion Channel Gating, Mutation genetics, Shal Potassium Channels genetics, Spinocerebellar Ataxias genetics, Spinocerebellar Ataxias physiopathology

Abstract

KCND3 encodes the voltage-gated potassium channel K V 4.3 that is highly expressed in the cerebellum, where it regulates dendritic excitability and calcium influx. Loss-of-function K V 4.3 mutations have been associated with dominant spinocerebellar ataxia (SCA19/22). By targeted NGS sequencing, we identified two novel KCND3 missense variants of the K V 4.3 channel: p.S347W identified in a patient with adult-onset pure cerebellar syndrome and p.W359G detected in a child with congenital nonprogressive ataxia. Neuroimaging showed mild cerebellar atrophy in both patients. We performed a two-electrode voltage-clamp recording of K V 4.3 currents in Xenopus oocytes: both the p.G345V (previously reported in a SCA19/22 family) and p.S347W mutants exhibited reduced peak currents by 50%, while no K+ current was detectable for the p.W359G mutant. We assessed the effect of the mutations on channel gating by measuring steady-state voltage-dependent activation and inactivation properties: no significant alterations were detected in p.G345V and p.S347W disease-associated variants, compared to controls. K V 4.3 expression studies in HEK293T cells showed 53% (p.G345V), 45% (p.S347W) and 75% (p.W359G) reductions in mutant protein levels compared with the wildtype. The present study broadens the spectrum of the known phenotypes and identifies additional variants for KCND3 -related disorders, outlining the importance of SCA gene screening in early-onset and congenital ataxia.

Published

2021

3. Neuroacanthocytosis Syndromes in an Italian Cohort: Clinical Spectrum, High Genetic Variability and Muscle Involvement.

Author

Vaisfeld A, Bruno G, Petracca M, Bentivoglio AR, Servidei S, Vita MG, Bove F, Straccia G, Dato C, Di Iorio G, Sampaolo S, Peluso S, De Rosa A, De Michele G, Barghigiani M, Galatolo D, Tessa A, Santorelli F, Chiurazzi P, and Melone MAB

Subjects

Adult, Child, Cohort Studies, Erythrocytes metabolism, Erythrocytes pathology, Female, Humans, Italy, Male, Muscular Diseases genetics, Muscular Diseases metabolism, Muscular Diseases pathology, Neuroacanthocytosis genetics, Neuroacanthocytosis metabolism, Neuroacanthocytosis pathology, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Mutation, Vesicular Transport Proteins genetics, Vesicular Transport Proteins metabolism

Abstract

Neuroacanthocytosis (NA) syndromes are a group of genetically defined diseases characterized by the association of red blood cell acanthocytosis, progressive degeneration of the basal ganglia and neuromuscular features with characteristic persistent hyperCKemia. The main NA syndromes include autosomal recessive chorea-acanthocytosis (ChAc) and X-linked McLeod syndrome (MLS). A series of Italian patients selected through a multicenter study for these specific neurological phenotypes underwent DNA sequencing of the VPS13A and XK genes to search for causative mutations. Where it has been possible, muscle biopsies were obtained and thoroughly investigated with histochemical assays. A total of nine patients from five different families were diagnosed with ChAC and had mostly biallelic changes in the VPS13A gene (three nonsense, two frameshift, three splicing), while three patients from a single X-linked family were diagnosed with McLeod syndrome and had a deletion in the XK gene. Despite a very low incidence (only one thousand cases of ChAc and a few hundred MLS cases reported worldwide), none of the 8 VPS13A variants identified in our patients is shared by two families, suggesting the high genetic variability of ChAc in the Italian population. In our series, in line with epidemiological data, McLeod syndrome occurs less frequently than ChAc, although it can be easily suspected because of its X-linked mode of inheritance. Finally, histochemical studies strongly suggest that muscle pathology is not simply secondary to the axonal neuropathy, frequently seen in these patients, but primary myopathic alterations can be detected in both NA syndromes.

Published

2021

4. Clinical utility of genetic testing in the early diagnosis of Danon disease mimicking hypertrophic cardiomyopathy: a case report.

Author

Novelli V, Bisignani A, Pelargonio G, Primiano G, Narducci ML, Palmieri V, Tiziano FD, Zeppilli P, Servidei S, Crea F, and Genuardi M

Subjects

Adolescent, Diagnostic Errors, Early Diagnosis, Genetic Predisposition to Disease, Glycogen Storage Disease Type IIb diagnostic imaging, Glycogen Storage Disease Type IIb genetics, Humans, Male, Phenotype, Predictive Value of Tests, Cardiomyopathy, Hypertrophic diagnosis, DNA Mutational Analysis, Genetic Testing, Glycogen Storage Disease Type IIb diagnosis, Lysosomal-Associated Membrane Protein 2 genetics, Mutation

Abstract

Background: Danon disease (OMIM 300257) is an X-linked lysosomal storage disorder, characterized by hypertrophic cardiomyopathy (HCM), skeletal myopathy, variable intellectual disability, and other minor clinical features. This condition accounts for ~ 4% of HCM patients, with a more severe and early onset phenotype in males, causing sudden cardiac death (SCD) in the first three decades of life. Genetic alterations in the LAMP2 gene are the main cause of this inherited fatal condition. Up to date, more than 100 different pathogenic variants have been reported in the literature. However, the majority of cases are misdiagnosed as HCM or have a delay in the diagnosis., Case Presentation: Here, we describe a young boy with an early diagnosis of HCM. After 2 episodes of ventricular fibrillation within 2 years, genetic testing identified a novel LAMP2 pathogenic variant. Subsequently, further clinical evaluations showing muscle weakness and mild intellectual disability confirmed the diagnosis of Danon disease., Conclusions: This report highlights the role of genetic testing in the rapid diagnosis of Danon disease, underscoring the need to routinely consider the inclusion of LAMP2 gene in the genetic screening for HCM, since an early diagnosis of Danon disease in patients with a phenotype mimicking HCM is essential to plan appropriate treatment, ie cardiac transplantation.

Published

2020

5. Sudoscan in the evaluation and follow-up of patients and carriers with TTR mutations: experience from an Italian Centre.

Author

Luigetti M, Bisogni G, Romano A, Di Paolantonio A, Barbato F, Primicerio G, Rossini PM, Servidei S, and Sabatelli M

Subjects

Adult, Aged, Female, Follow-Up Studies, Galvanic Skin Response, Humans, Italy, Male, Middle Aged, Neural Conduction, Prognosis, Prospective Studies, Severity of Illness Index, Amyloid Neuropathies, Familial diagnosis, Amyloid Neuropathies, Familial genetics, Electrodiagnosis methods, Mutation, Prealbumin genetics

Abstract

Objective: To evaluate the utility of Sudoscan as possible marker of disease progression and disease onset in a cohort of hereditary ATTR amyloidosis (hATTR amyloidosis) polyneuropathy patients and carriers., Patients and Methods: We regularly performed different clinical scales, nerve conductions studies (NCS), and Sudoscan on a cohort of hATTR amyloidosis patients and carriers from a single centre of central Italy, a non-endemic area, in the last 2 years., Results: About 18 hATTR amyloidosis patients and 8 asymptomatic carriers were enrolled. All patients had a neuropathy affecting large fibres, small fibres or both. Two subjects developed symptoms and neurophysiological alterations during follow-up. Sudoscan data from hand and feet inversely correlated with neuropathy severity and with disease duration. Moreover, global disease status, expressed by Kumamoto scale also inversely correlated with Sudoscan values., Conclusions: We confirmed that Sudoscan is a reliable marker of disease progression in late-onset hATTR amyloidosis patients and we suggest its possible utility in early detection of disease in this population.

Published

2018

6. Biallelic SQSTM1 mutations in early-onset, variably progressive neurodegeneration.

Author

Muto V, Flex E, Kupchinsky Z, Primiano G, Galehdari H, Dehghani M, Cecchetti S, Carpentieri G, Rizza T, Mazaheri N, Sedaghat A, Vahidi Mehrjardi MY, Traversa A, Di Nottia M, Kousi MM, Jamshidi Y, Ciolfi A, Caputo V, Malamiri RA, Pantaleoni F, Martinelli S, Jeffries AR, Zeighami J, Sherafat A, Di Giuda D, Shariati GR, Carrozzo R, Katsanis N, Maroofian R, Servidei S, and Tartaglia M

Subjects

Adolescent, Adult, Age of Onset, Animals, Female, Humans, Male, Pedigree, Exome Sequencing methods, Young Adult, Zebrafish, Alleles, Disease Progression, Mutation genetics, Neurodegenerative Diseases diagnostic imaging, Neurodegenerative Diseases genetics, Sequestosome-1 Protein genetics

Abstract

Objective: To characterize clinically and molecularly an early-onset, variably progressive neurodegenerative disorder characterized by a cerebellar syndrome with severe ataxia, gaze palsy, dyskinesia, dystonia, and cognitive decline affecting 11 individuals from 3 consanguineous families., Methods: We used whole-exome sequencing (WES) (families 1 and 2) and a combined approach based on homozygosity mapping and WES (family 3). We performed in vitro studies to explore the effect of the nontruncating SQSTM1 mutation on protein function and the effect of impaired SQSTM1 function on autophagy. We analyzed the consequences of sqstm1 down-modulation on the structural integrity of the cerebellum in vivo using zebrafish as a model., Results: We identified 3 homozygous inactivating variants, including a splice site substitution (c.301+2T>A) causing aberrant transcript processing and accelerated degradation of a resulting protein lacking exon 2, as well as 2 truncating changes (c.875_876insT and c.934_936delinsTGA). We show that loss of SQSTM1 causes impaired production of ubiquitin-positive protein aggregates in response to misfolded protein stress and decelerated autophagic flux. The consequences of sqstm1 down-modulation on the structural integrity of the cerebellum in zebrafish documented a variable but reproducible phenotype characterized by cerebellum anomalies ranging from depletion of axonal connections to complete atrophy. We provide a detailed clinical characterization of the disorder; the natural history is reported for 2 siblings who have been followed up for >20 years., Conclusions: This study offers an accurate clinical characterization of this recently recognized neurodegenerative disorder caused by biallelic inactivating mutations in SQSTM1 and links this phenotype to defective selective autophagy., (© 2018 American Academy of Neurology.)

Published

2018

7. The Bacterial Protein CNF1 as a Potential Therapeutic Strategy against Mitochondrial Diseases: A Pilot Study.

Author

Fabbri A, Travaglione S, Maroccia Z, Guidotti M, Pierri CL, Primiano G, Servidei S, Loizzo S, and Fiorentini C

Subjects

Bacterial Toxins isolation & purification, DNA, Mitochondrial metabolism, Electron Transport Complex IV genetics, Electron Transport Complex IV metabolism, Escherichia coli chemistry, Escherichia coli Proteins isolation & purification, Fibroblasts metabolism, Fibroblasts pathology, Gene Expression, Humans, MERRF Syndrome drug therapy, MERRF Syndrome genetics, MERRF Syndrome metabolism, MERRF Syndrome pathology, Male, Membrane Transport Proteins genetics, Membrane Transport Proteins metabolism, Middle Aged, Mitochondria genetics, Mitochondria metabolism, Mitochondria ultrastructure, Mitochondrial Precursor Protein Import Complex Proteins, Pilot Projects, Primary Cell Culture, Receptors, Cell Surface genetics, Receptors, Cell Surface metabolism, Stress Fibers drug effects, Stress Fibers metabolism, Stress Fibers ultrastructure, Adenosine Triphosphate biosynthesis, Bacterial Toxins pharmacology, DNA, Mitochondrial genetics, Escherichia coli Proteins pharmacology, Fibroblasts drug effects, Mitochondria drug effects, Mutation

Abstract

The Escherichia coli protein toxin cytotoxic necrotizing factor 1 (CNF1), which acts on the Rho GTPases that are key regulators of the actin cytoskeleton, is emerging as a potential therapeutic tool against certain neurological diseases characterized by cellular energy homeostasis impairment. In this brief communication, we show explorative results on the toxin’s effect on fibroblasts derived from a patient affected by myoclonic epilepsy with ragged-red fibers (MERRF) that carries a mutation in the m.8344A>G gene of mitochondrial DNA. We found that, in the patient’s cells, besides rescuing the wild-type-like mitochondrial morphology, CNF1 administration is able to trigger a significant increase in cellular content of ATP and of the mitochondrial outer membrane marker Tom20. These results were accompanied by a profound F-actin reorganization in MERRF fibroblasts, which is a typical CNF1-induced effect on cell cytoskeleton. These results point at a possible role of the actin organization in preventing or limiting the cell damage due to mitochondrial impairment and at CNF1 treatment as a possible novel strategy against mitochondrial diseases still without cure.

Published

2018

8. "Myo-cardiomyopathy" is commonly associated with the A8344G "MERRF" mutation.

Author

Catteruccia M, Sauchelli D, Della Marca G, Primiano G, Cuccagna C, Bernardo D, Leo M, Camporeale A, Sanna T, Cianfoni A, and Servidei S

Subjects

Adolescent, Adult, Aged, Aspartic Acid analogs & derivatives, Aspartic Acid metabolism, Brain metabolism, Brain pathology, Cardiomyopathies complications, Cardiomyopathies pathology, Female, Humans, MERRF Syndrome complications, Magnetic Resonance Imaging, Male, Middle Aged, Muscle, Skeletal pathology, Spectrum Analysis, Cardiomyopathies genetics, DNA, Mitochondrial genetics, MERRF Syndrome genetics, Mutation genetics

Abstract

The objective of the study was to better characterize the clinical phenotype associated with the A8344G "MERRF" mutation of mitochondrial DNA. Fifteen mutated patients were extensively investigated. The frequency of main clinical features was: exercise intolerance and/or muscle weakness 67 %, respiratory involvement 67 %, lactic acidosis 67 %, cardiac abnormalities 53 %, peripheral neuropathy 47 %, myoclonus 40 %, epilepsy 40 %, ataxia 13 %. A restrictive respiratory insufficiency requiring ventilatory support was observed in about half of our patients. One patient developed a severe and rapidly progressive cardiomyopathy requiring cardioverter-defibrillator implantation. Five patients died of overwhelming, intractable lactic acidosis. Serial muscle MRIs identified a consistent pattern of muscle involvement and progression. Cardiac MRI showed non-ischemic late gadolinium enhancement in the left ventricle inferolateral part as early sign of myocardial involvement. Brain spectroscopy demonstrated increased peak of choline and reduction of N-acetylaspartate. Lactate was never detected in brain areas, while it could be documented in ventricles. We confirm that muscle involvement is the most frequent clinical feature associated with A8443G mutation. In contrast with previous reports, however, about half of our patients did not develop signs of CNS involvement even in later stages of the disease. The difference may be related to the infrequent investigation of A8344G mutation in 'pure' mitochondrial myo-cardiomyopathy, representing a bias and a possible cause of syndrome's underestimation. Our study highlights the importance of lactic acidosis and respiratory muscle insufficiency as critical prognostic factors. Muscle and cardiac MRI and brain spectroscopy may be useful tools in diagnosis and follow-up of MERRF.

Published

2015

9. Phenotypic heterogeneity of the 8344A>G mtDNA "MERRF" mutation.

Author

Mancuso M, Orsucci D, Angelini C, Bertini E, Carelli V, Comi GP, Minetti C, Moggio M, Mongini T, Servidei S, Tonin P, Toscano A, Uziel G, Bruno C, Caldarazzo Ienco E, Filosto M, Lamperti C, Martinelli D, Moroni I, Musumeci O, Pegoraro E, Ronchi D, Santorelli FM, Sauchelli D, Scarpelli M, Sciacco M, Spinazzi M, Valentino ML, Vercelli L, Zeviani M, and Siciliano G

Subjects

Adult, Age of Onset, Databases, Genetic, Disease Progression, Female, Humans, MERRF Syndrome pathology, Magnetic Resonance Imaging, Male, Middle Aged, Retrospective Studies, DNA, Mitochondrial genetics, MERRF Syndrome genetics, MERRF Syndrome physiopathology, Mutation genetics, Phenotype

Abstract

Objectives: Myoclonic epilepsy with ragged-red fibers (MERRF) is a rare mitochondrial syndrome, mostly caused by the 8344A>G mitochondrial DNA mutation. Most of the previous studies have been based on single case/family reports or series with few patients. The primary aim of this study was the characterization of a large cohort of patients with the 8344A>G mutation. The secondary aim was revision of the previously published data., Methods: Retrospective, database-based study (Nation-wide Italian Collaborative Network of Mitochondrial Diseases) and systematic revision., Results: Forty-two patients carrying the mutation were identified. The great majority did not have full-blown MERRF syndrome. Myoclonus was present in 1 of 5 patients, whereas myopathic signs and symptoms, generalized seizures, hearing loss, eyelid ptosis, and multiple lipomatosis represented the most common clinical features. Some asymptomatic mutation carriers have also been observed. Myoclonus was more strictly associated with ataxia than generalized seizures in adult 8344A>G subjects. Considering all of the 321 patients so far available, including our dataset and previously published cases, at the mean age of approximately 35 years, the clinical picture was characterized by the following signs/symptoms, in descending order: myoclonus, muscle weakness, ataxia (35%-45% of patients); generalized seizures, hearing loss (25%-34.9%); cognitive impairment, multiple lipomatosis, neuropathy, exercise intolerance (15%-24.9%); and increased creatine kinase levels, ptosis/ophthalmoparesis, optic atrophy, cardiomyopathy, muscle wasting, respiratory impairment, diabetes, muscle pain, tremor, migraine (5%-14.9%)., Conclusions: Our results showed higher clinical heterogeneity than commonly thought. Moreover, MERRF could be better defined as a myoclonic ataxia rather than a myoclonic epilepsy.

Published

2013

10. Spinal muscular atrophy associated with progressive myoclonic epilepsy is caused by mutations in ASAH1.

Author

Zhou J, Tawk M, Tiziano FD, Veillet J, Bayes M, Nolent F, Garcia V, Servidei S, Bertini E, Castro-Giner F, Renda Y, Carpentier S, Andrieu-Abadie N, Gut I, Levade T, Topaloglu H, and Melki J

Subjects

Adolescent, Animals, Child, Child, Preschool, Female, Gene Knockdown Techniques, Humans, Male, Myoclonic Epilepsies, Progressive genetics, Pedigree, Zebrafish, Acid Ceramidase genetics, Mutation, Spinal Muscular Atrophies of Childhood genetics

Abstract

Spinal muscular atrophy (SMA) is a clinically and genetically heterogeneous disease characterized by the degeneration of lower motor neurons. The most frequent form is linked to mutations in SMN1. Childhood SMA associated with progressive myoclonic epilepsy (SMA-PME) has been reported as a rare autosomal-recessive condition unlinked to mutations in SMN1. Through linkage analysis, homozygosity mapping, and exome sequencing in three unrelated SMA-PME-affected families, we identified a homozygous missense mutation (c.125C>T [p.Thr42Met]) in exon 2 of ASAH1 in the affected children of two families and the same mutation associated with a deletion of the whole gene in the third family. Expression studies of the c.125C>T mutant cDNA in Farber fibroblasts showed that acid-ceramidase activity was only 32% of that generated by normal cDNA. This reduced activity was able to normalize the ceramide level in Farber cells, raising the question of the pathogenic mechanism underlying the CNS involvement in deficient cells. Morpholino knockdown of the ASAH1 ortholog in zebrafish led to a marked loss of motor-neuron axonal branching, a loss that is associated with increased apoptosis in the spinal cord. Our results reveal a wide phenotypic spectrum associated with ASAH1 mutations. An acid-ceramidase activity below 10% results in Farber disease, an early-onset disease starting with subcutaneous lipogranulomata, joint pain, and hoarseness of the voice, whereas a higher residual activity might be responsible for SMA-PME, a later-onset phenotype restricted to the CNS and starting with lower-motor-neuron disease., (Copyright © 2012 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2012

11. P525L FUS mutation is consistently associated with a severe form of juvenile amyotrophic lateral sclerosis.

Author

Conte A, Lattante S, Zollino M, Marangi G, Luigetti M, Del Grande A, Servidei S, Trombetta F, and Sabatelli M

Subjects

Child, DNA Mutational Analysis, Female, Humans, Phenotype, Amyotrophic Lateral Sclerosis genetics, Mutation genetics, RNA-Binding Protein FUS genetics

Abstract

Some FUS mutations have been observed in patients with the juvenile form of Amyotrophic Lateral Sclerosis starting before 25 years. We report an 11-year-old girl affected by sporadic juvenile ALS with a rapid course resulting in tracheostomy after 14 months from the onset. Sequencing FUS gene revealed a de novo P525L mutation. Our findings, together with literature data, indicate that this mutation is consistently associated with a specific phenotype characterized by juvenile onset, severe course and high proportion of de novo mutations in sporadic cases., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2012

12. Identification of novel and recurrent CACNA1A gene mutations in fifteen patients with episodic ataxia type 2.

Author

Mantuano E, Romano S, Veneziano L, Gellera C, Castellotti B, Caimi S, Testa D, Estienne M, Zorzi G, Bugiani M, Rajabally YA, Barcina MJ, Servidei S, Panico A, Frontali M, and Mariotti C

Subjects

Adolescent, Adult, Aged, Child, Child, Preschool, DNA Mutational Analysis, Female, Humans, Infant, Male, Middle Aged, Models, Genetic, Phenotype, Young Adult, Ataxia genetics, Calcium Channels genetics, Mutation

Abstract

Episodic ataxia type 2 is a rare autosomal dominant disease characterized by recurrent attacks of vertigo and cerebellar ataxia. The disease was caused by mutations in the CACNA1A gene, on chromosome 19p. We perform a mutational screening in a group of 43 unrelated patients. Forty-two patients presented episodes of disequilibrium and ataxia, and one child was studied because of the occurrence of episodic torticollis. The genetic analysis showed 15 mutated patients (35%). In 13 cases we found novel CACNA1A gene mutations, including missense, protein truncating, and aberrant splicing mutations. Two truncating mutations lead to the uppermost premature stop so far reported, challenging recent hypotheses on dominant negative effect. In patients without CACNA1A mutations, molecular testing for CACNB4 gene mutations excluded this genetic subtype. Clinical features of mutated subjects mostly confirmed previous sign and symptoms associated with EA2, including paroxysmal torticollis and mental retardation. CACNA1A mutated patients have an earlier age at onset, interictal nystagmus, and abnormalities of ocular movements. A review of all CACNA1A mutations so far reported showed that they are mainly located downstream exon 18. Our data substantially increase the number of the described CACNA1A mutations, and propose clinical and molecular criteria for a more focused genetic screening., (Copyright 2010 Elsevier B.V. All rights reserved.)

Published

2010

13. Rippling muscle disease and cardiomyopathy associated with a mutation in the CAV3 gene.

Author

Catteruccia M, Sanna T, Santorelli FM, Tessa A, Di Giacopo R, Sauchelli D, Verbo A, Lo Monaco M, and Servidei S

Subjects

Adult, Alanine genetics, Cardiomyopathies complications, Cardiomyopathies pathology, Electrocardiography methods, Electromyography methods, Family Health, Female, Humans, Magnetic Resonance Imaging methods, Male, Middle Aged, Muscle, Skeletal pathology, Muscular Diseases complications, Valine genetics, Young Adult, Cardiomyopathies genetics, Caveolin 3 genetics, Genetic Predisposition to Disease, Muscular Diseases genetics, Mutation genetics

Abstract

Caveolin-3, the myocyte-specific isoform of caveolins, is preferentially expressed in skeletal, cardiac and smooth muscles. Mutations in the CAV3 gene cause clinically heterogeneous neuromuscular disorders, including rippling muscle disease, or cardiopathies. The same mutation may lead to different phenotypes, but cardiac and muscle involvement rarely coexists suggesting that the molecular network acting with caveolin-3 in skeletal muscle and heart may differ. Here we describe an Italian family (a father and his two sons) with clinical and neurophysiological features of rippling muscle disease and heart involvement characterized by atrio-ventricular conduction defects and dilated cardiomyopathy. Muscle biopsy showed loss of caveolin-3 immunosignal. Molecular studies identified the p.A46V mutation in CAV3 previously reported in a German family with autosomal dominant rippling muscle disease and sudden death in few individuals. We suggest that cardiac dysfunction in myopathic patients with CAV3 mutations may be underestimated and recommend a more thorough evaluation for the presence of cardiomyopathy and potentially lethal arrhythmias.

Published

2009

14. Genotype-phenotype correlation of paroxysmal nonkinesigenic dyskinesia.

Author

Bruno MK, Lee HY, Auburger GW, Friedman A, Nielsen JE, Lang AE, Bertini E, Van Bogaert P, Averyanov Y, Hallett M, Gwinn-Hardy K, Sorenson B, Pandolfo M, Kwiecinski H, Servidei S, Fu YH, and Ptácek L

Subjects

Adolescent, Adult, Age of Onset, Caffeine adverse effects, Child, Child, Preschool, Chorea metabolism, DNA Mutational Analysis, Dystonia genetics, Dystonia metabolism, Dystonia physiopathology, Ethanol adverse effects, Female, Genetic Markers genetics, Genetic Testing, Genotype, Humans, Male, Pedigree, Penetrance, Stress, Psychological complications, Chorea genetics, Chorea physiopathology, Genetic Predisposition to Disease genetics, Muscle Proteins genetics, Mutation genetics

Abstract

Background: Paroxysmal nonkinesigenic dyskinesia (PNKD) is a rare disorder characterized by episodic hyperkinetic movement attacks. We have recently identified mutations in the MR-1 gene causing familial PNKD., Methods: We reviewed the clinical features of 14 kindreds with familial dyskinesia that was not clearly induced by movement or during sleep. Of these 14 kindreds, 8 had MR-1 mutations and 6 did not., Results: Patients with PNKD with MR-1 mutations had their attack onset in youth (infancy and early childhood). Typical attacks consisted of a mixture of chorea and dystonia in the limbs, face, and trunk, and typical attack duration lasted from 10 minutes to 1 hour. Caffeine, alcohol, and emotional stress were prominent precipitants. Attacks had a favorable response to benzodiazepines, such as clonazepam and diazepam. Attacks in families without MR-1 mutations were more variable in their age at onset, precipitants, clinical features, and response to medications. Several were induced by persistent exercise., Conclusions: Paroxysmal nonkinesigenic dyskinesia (PNKD) should be strictly defined based on age at onset and ability to precipitate attacks with caffeine and alcohol. Patients with this clinical presentation (which is similar to the phenotype initially reported by Mount and Reback) are likely to harbor myofibrillogenesis regulator 1 (MR-1) gene mutations. Other "PNKD-like" families exist, but atypical features suggests that these subjects are clinically distinct from PNKD and do not have MR-1 mutations. Some may represent paroxysmal exertional dyskinesia.

Published

2007

15. McArdle disease: the mutation spectrum of PYGM in a large Italian cohort.

Author

Bruno C, Cassandrini D, Martinuzzi A, Toscano A, Moggio M, Morandi L, Servidei S, Mongini T, Angelini C, Musumeci O, Comi GP, Lamperti C, Filosto M, Zara F, and Minetti C

Subjects

Adolescent, Adult, Aged, Alleles, Amino Acid Sequence, Child, Cohort Studies, DNA Mutational Analysis, Female, Glycogen Storage Disease Type V epidemiology, Humans, Italy epidemiology, Male, Middle Aged, Molecular Sequence Data, Sequence Alignment, Sequence Analysis, Protein, Glycogen Phosphorylase, Muscle Form genetics, Glycogen Storage Disease Type V genetics, Mutation

Abstract

Deficiency of the muscle isozyme of glycogen phosphorylase is causative of McArdle disease or Glycogen storage disease type V (GSD-V), the most common autosomal recessive disorder of glycogen metabolism. The typical clinical presentation is characterized by exercise intolerance with cramps, and recurrent myoglobinuria. To date, 46 mutations in the PYGM gene have been detected in GSD-V patients. We report the mutational spectrum in 68 Italian patients. We identified 30 different mutations in the PYGM gene, including 19 mutations that have not been reported previously. The novel mutations include: eight missense mutations (c.475G>A, p.G159R; c.689C>G, p.P230R; c.1094C>T, p.A365E; c.1151C>A, p.A384D; c.1182C>T, p.R428C; c.1471C>T, p.R491C; c.2444A>C, p.D815A; c.2477G>C, p.W826S), two nonsense mutations (c.1475G>A, p.W492X; c.1627A>T, p.K543X), five splice site mutations (c.855 +1G>C; c.1092 +1G>A; c. 1093-1G>T; c.1239 +1G>A; c.2380 +1G>A), and four deletions (c.715_717delGTC, p.V239del; c.304delA, p.N102DfsX4; c.1970_2177del, p.V657_G726; c.2113_2114delGG, p.G705RfsX16). Whereas we confirmed lack of direct correlation between the clinical phenotype and the genotype, we also found that the so-called 'common mutation' (p.R50X) accounted for about 43% of alleles in our cohort and that no population-related mutations are clearly identified in Italian patients., (Copyright 2006 Wiley-Liss, Inc.)

Published

2006

16. Novel GNE mutations in Italian families with autosomal recessive hereditary inclusion-body myopathy.

Author

Broccolini A, Ricci E, Cassandrini D, Gliubizzi C, Bruno C, Tonoli E, Silvestri G, Pescatori M, Rodolico C, Sinicropi S, Servidei S, Zara F, Minetti C, Tonali PA, and Mirabella M

Subjects

DNA Mutational Analysis, Genes, Recessive, Humans, Italy, Myositis, Inclusion Body enzymology, Multienzyme Complexes genetics, Mutation, Myositis, Inclusion Body genetics

Abstract

The most common form of autosomal recessive (AR) hereditary inclusion-body myopathy (HIBM), originally described in Persian-Jewish families, is characterized by onset in early adult life with weakness and atrophy of distal lower limb muscles, which progress proximally and relatively spare the quadriceps. AR HIBM is associated with mutations in the UDP-N-acetylglucosamine 2-epimerase/N-acetylmannosamine kinase gene (GNE) on chromosome 9p12-13. In the present study we have identified seven novel GNE mutations in patients from five unrelated Italian families with clinical and pathologic features indicative of AR HIBM. Four were missense mutations (c.1556A>G [p.N519S], c.79C>T [p.P27S], c.1798G>A [p.A600T] and c.616G>A [p.G206S]), two consisted in a single-base deletion (c.616delG [p.G206fsX4] and c.1130delT [p.I377fsX16]) and one in an intronic single-base insertion (c.1070+2dupT). These latter findings further extend the type of GNE mutations associated with HIBM. Furthermore, in one patient we also identified the c.737G>A [p.R246Q] missense mutation that corresponds to the one previously reported in a family from the Bahamas. Interestingly, in two of our families distinct mutations affected nucleotide c.616 in exon 3 (c.616delG and c.616G>A). The possibility of specific portions of the gene being more prone to mutations remains to be elucidated., (Copyright 2004 Wiley-Liss, Inc.)

Published

2004

17. Mitochondrial encephalomyopathies: gene mutation.

Author

Servidei S

Subjects

Humans, Chromosome Mapping, Mitochondrial Encephalomyopathies genetics, Mutation genetics

Published

2004

18. An Italian family with autosomal recessive inclusion-body myopathy and mutations in the GNE gene.

Author

Broccolini A, Pescatori M, D'Amico A, Sabino A, Silvestri G, Ricci E, Servidei S, Tonali PA, and Mirabella M

Subjects

Chromosomes, Human, Pair 9 genetics, Exons genetics, Genes, Recessive, Humans, Italy, Muscle, Skeletal enzymology, Muscle, Skeletal pathology, Mutation physiology, Myositis, Inclusion Body pathology, Pedigree, Reverse Transcriptase Polymerase Chain Reaction, Carbohydrate Epimerases genetics, Escherichia coli Proteins, Mutation genetics, Myositis, Inclusion Body genetics

Published

2002

19. Mitochondrial encephalomyopathies: gene mutation.

Author

Servidei S

Subjects

Humans, Mitochondrial Encephalomyopathies genetics, Mutation

Published

2002

20. Mitochondrial encephalomyopathies: gene mutation.

Author

Servidei S

Subjects

Humans, Molecular Sequence Data, Mitochondrial Encephalomyopathies genetics, Mutation

Published

2001

21. Mitochondrial encephalomyopathies: gene mutation.

Author

Servidei S

Subjects

Humans, Mitochondrial Encephalomyopathies genetics, Mutation

Published

2000

22. Apoptosis in mitochondrial encephalomyopathies with mitochondrial DNA mutations: a potential pathogenic mechanism.

Author

Mirabella M, Di Giovanni S, Silvestri G, Tonali P, and Servidei S

Subjects

Adolescent, Adult, Aged, Apoptosis, Child, Child, Preschool, Female, Humans, Inclusion Bodies pathology, Inclusion Bodies ultrastructure, MELAS Syndrome genetics, MELAS Syndrome pathology, MERRF Syndrome genetics, MERRF Syndrome pathology, Male, Middle Aged, Mitochondria genetics, Mitochondria pathology, Muscle, Skeletal ultrastructure, Point Mutation, Sequence Deletion, DNA, Mitochondrial genetics, Mitochondrial Encephalomyopathies genetics, Mitochondrial Encephalomyopathies pathology, Muscle, Skeletal pathology, Mutation

Abstract

Mitochondrial encephalomyopathies caused by mitochondrial DNA (mtDNA) defects are a genetically and phenotypically heterogeneous group of disorders. The site, percentage and distribution of mutations do not explain the overall clinical heterogeneity that is found. Apoptosis (programmed cell death) is an evolutionarily conserved mechanism that is essential for tissue development and homeostasis. Dysregulation of apoptosis has been implicated in the pathogenesis of various human diseases, such as cancer and autoimmune and neurodegenerative disorders. Recent in vitro evidence has indicated the central role of mitochondria in the apoptotic process. We investigated the occurrence of apoptosis in muscle biopsies of 36 patients carrying different mtDNA mutations and four patients with inclusion body myositis and mitochondrial abnormalities. Apoptotic features, mainly localized in cytochrome c oxidase-negative fibres, were observed in muscle fibres of patients carrying a high percentage of single mtDNA deletions (>40%) and of tRNA point mutations (>70%). By contrast, no apoptotic changes were observed in inclusion body myositis and in patients carrying mutations of mtDNA structural genes. Our study suggests that apoptosis is not simply a means whereby cells with dysfunctional mitochondria are eliminated, but that it seems to play a role in the pathogenesis of mitochondrial disorders associated with mtDNA defects affecting mitochondrial protein synthesis. The imbalance and relative abundances of nuclear-encoded and mtDNA-encoded subunits may favour cytochrome c inactivation and release. Cytochrome c, together with respiratory chain dysfunction, could activate apoptotic pathways that, in turn, inhibit the rate of mitochondrial translation and the importation of nuclear-encoded mitochondrial protein precursors. This vicious circle may amplify the biochemical defects and tissue damage and contribute to the modulation of clinical features.

Published

2000

23. Mitochondrial encephalomyopathies: gene mutation.

Author

Servidei S

Subjects

Humans, Mitochondrial Encephalomyopathies genetics, Mutation genetics

Published

1999

24. Identification of five new mutations and three novel polymorphisms in the muscle chloride channel gene (CLCN1) in 20 Italian patients with dominant and recessive myotonia congenita. Mutations in brief no. 118. Online.

Author

Sangiuolo F, Botta A, Mesoraca A, Servidei S, Merlini L, Fratta G, Novelli G, and Dallapiccola B

Subjects

Genes, Dominant genetics, Genes, Recessive genetics, Humans, Italy, Chloride Channels genetics, Muscle Proteins genetics, Mutation genetics, Myotonia Congenita genetics, Polymorphism, Genetic genetics

Abstract

Autosomal dominant myotonia congenita or Thomsen's disease and autosomal recessive myotonia congenita or Becker's are rare nondystrophic disorders due to allelic mutations of the muscle chloride channel gene, CLCN1. We have analysed all 24 exons of the CLCN1 gene, in a panel of 20 unrelated patients (9 with dominant and 11 with recessive mytotonia congenita). We have found five novel mutations including two missense (V5631, F708L), one nonsense (C481X), one splicing (IVS19+2T->A), and one frameshift (2264delC), and also detected the recurrent R894X mutation. These account for 10 of the 22 recessive alleles examined, while no mutations were found in the dominant form. We report three novel polymorphisms (-134T/G, 898C/A and 2154T/C). Our results support high molecular heterogeneity of these myotonias in Italian population and provide new insight for the diagnosis and genetic counselling of these diseases.

Published

1998

25. Genotype-phenotype correlations of DHP receptor alpha 1-subunit gene mutations causing hypokalemic periodic paralysis.

Author

Fouad G, Dalakas M, Servidei S, Mendell JR, Van den Bergh P, Angelini C, Alderson K, Griggs RC, Tawil R, Gregg R, Hogan K, Powers PA, Weinberg N, Malonee W, and Ptácek LJ

Subjects

Adolescent, Adult, Calcium Channels, L-Type, Child, Genotype, Humans, Hypokalemia pathology, Hypokalemia physiopathology, Male, Paralysis pathology, Paralysis physiopathology, Phenotype, Polymorphism, Single-Stranded Conformational, Calcium Channels genetics, Hypokalemia genetics, Muscle Proteins genetics, Mutation, Paralysis genetics, Periodicity

Abstract

Hypokalemic periodic paralysis (hypoKPP) is an autosomal dominant or sporadic disorder characterized by periodic, reversible attacks of muscle weakness. Mutations in the skeletal muscle dihydropyridine receptor alpha 1-subunit that functions as a calcium channel (CACNL1A3) cause hypoKPP. We studied a group of 45 hypoKPP probands and demonstrated mutations in 30 of them. When compared with patients in whom CACNL1A3 mutations were not identified, those with mutations had an earlier age of onset and more often had a family history of hypoKPP. To date, three mutations have been identified. The R1239G mutation has only been found in one family. Of the 30 probands with recognized mutations, R528H accounted for 43% and R1239H was seen in 53%. Age of onset and potassium levels during attacks were lower in patients with the R1239H mutation than those with R528H. Cardiac dysrhythmias co-segregated with hypoKPP in one small kindred with the R528H mutation. No mutations were identified in exons of the gene encoding the S4 segments of domains one and three or the cytoplasmic loop between domains two and three. In addition to the 45 hypoKPP probands, an additional 11 probands with clinical variants of hypoKPP (three thyrotoxic hypoKPP and eight Andersen syndrome patients) were examined for CACNL1A3 mutations and none were found.

Published

1997

26. Fatigue and exercise intolerance in mitochondrial diseases. Literature revision and experience of the Italian Network of mitochondrial diseases

Author

Mancuso, M., Angelini, C., Bertini, E., Carelli, V., Comi, G. P., Minetti, C., Moggio, M., Mongini, T., Servidei, S., Tonin, Paola, Toscano, A., Uziel, G., Zeviani, M., Siciliano, G., Nation wide Italian Collaborative Network of Mitochondrial Diseases, Collaborators: Bruno, C., Filosto, Massimiliano, Lamperti, C., Martinelli, D., Moroni, I., Musumeci, O., Orsucci, D., Pegoraro, E., Santorelli, F. M., Scarpelli, Mauro, Sciacco, M., Spinazzi, M., Valentino, M. L., Vercelli, L., Mancuso M, Angelini C, Bertini E, Carelli V, Comi G P, Minetti C, Moggio M, Mongini T, Servidei S, Tonin P, Toscano A, Uziel G, Zeviani M, Siciliano G, and Nation-wide Italian Collaborative Network of Mitochondrial Diseases

Subjects

Mitochondrial DNA, medicine.medical_specialty, Ubiquinone, Mitochondrial disease, Clinical Neurology, mitochondrial myopathies, Exercise intolerance, Article, chemistry.chemical_compound, Disease registry, Mitochondrial myopathy, Internal medicine, Humans, Medicine, Aerobic exercise, Genetics(clinical), Pediatrics, Perinatology, and Child Health, Exercise physiology, skeletal muscle, Exercise, Genetics (clinical), Coenzyme Q10, mitochondrial diseases, business.industry, mtDNA, medicine.disease, exercise intolerance, mitochondria, Settore MED/26 - NEUROLOGIA, mitochondrial disease, Neurology, chemistry, Mutation, Pediatrics, Perinatology and Child Health, Physical therapy, disease registry, fatigue, Neurology (clinical), medicine.symptom, business

Abstract

Fatigue and exercise intolerance are common symptoms of mitochondrial diseases, but difficult to be clinically assessed. New methods to quantify these rather common complaints are strongly needed in the clinical practice. Coenzyme Q10 administration and aerobic exercise may improve exercise intolerance, but more definite studies are still pending. Herein, we have revised “how to measure” and “how to treat” these symptoms of mitochondrial patients. Subsequently, we reviewed the clinical data of the 1164 confirmed mitochondrial patients present in the Italian nation-wide database of mitochondrial disease, with special regard to exercise intolerance. We observed that more of 20% of mitochondrial patients complain of exercise intolerance. This symptom seems to be frequently associated with specific patient groups and/or genotypes. Ragged red fibers and COX-negative fibers are more often present in subjects with exercise intolerance, whereas lactate levels could not predict this symptom. Multicenter efforts are strongly needed for rare disorders such as mitochondrial diseases, and may represent the basis for more rigorous longitudinal studies.

Published

2012

27. Autosomal dominant hereditary spastic paraplegia: DHPLC-based mutation analysis of SPG4 reveals eleven novel mutations

Author

Patrono, C, Scarano, V, Cricchi, F, Melone, Ma, Chiriaco, M, Napolitano, A, Malandrini, A, DE MICHELE, G, Petrozzi, L, Giraldi, C, Santoro, L, Servidei, S, Casali, Carlo, C, Filla, A, Santorelli, Fm, Patrono, C, Scarano, V, Cricchi, F, Melone, Ma, Chiriaco, M, Napolitano, A, Malandrini, A, DE MICHELE, Giuseppe, Petrozzi, L, Giraldi, C, Santoro, Lucio, Servidei, S, Casali, C, Filla, Alessandro, Santorelli, F. M., Melone, Mariarosa Anna Beatrice, DE MICHELE, G, Santoro, L, and Filla, A

Subjects

Adult, Spastin, Hereditary spastic paraplegia, Genetic counseling, DNA Mutational Analysis, Molecular Sequence Data, Mutation, Missense, Biology, Bioinformatics, medicine.disease_cause, Frameshift mutation, Cohort Studies, Genetics, medicine, Missense mutation, HSP, Humans, Amino Acid Sequence, Genetic Testing, Family history, Frameshift Mutation, Genetics (clinical), Chromatography, High Pressure Liquid, Genes, Dominant, Adenosine Triphosphatases, Mutation, Polymorphism, Genetic, Spastic Paraplegia, Hereditary, Middle Aged, medicine.disease, HSP, DHPLC, Penetrance, Settore MED/26 - NEUROLOGIA, Phenotype, Italy, hereditary spastic paraplegia, SPG4, Sequence Alignment, Polymorphism, Restriction Fragment Length

Abstract

We set up a new denaturing high-performance liquid chromatography (DHPLC)-based protocol to screen patients with autosomal dominant hereditary spastic paraplegia (AD-HSP) for mutations in SPG4. Six patients had a complicated form and 49 a pure HSP phenotype. We also analyzed 19 unrelated patients presenting with an HSP phenotype (pure in 17 and complicated in two subjects) but no clear family history, as such patients may be cases of dominant inheritance with low penetrance. The overall frequency of SPG4 mutations in our study of HSP (in which prior linkage data were unavailable) was 32.4%, rising to 46.9% when only pure AD-HSP patients were considered. This figure falls well within the range reported in different populations. Rather as expected, the clinical data available for the patients did not support an easy genotype-phenotype correlation. Moreover, the clinical picture was not influenced by the length of the predicted residual gene product. As well as identifying novel variants in SPG4, this study constitutes the molecular characterization of the largest cohort of Italian AD-HSP patients studied to date. In addition, it provided an efficient, cost-effective, and reliable detection protocol for mutational screening of SPG4, which might facilitate medical genetic counseling.

Published

2005

28. Nucleus-driven multiple large-scale deletions of the human mitochondrial genome: a new autosomal dominant disease

Author

Zeviani, M., Nereo Bresolin, Gellera, C., Bordoni, A., Pannacci, M., Amati, P., Moggio, M., Servidei, S., Scarlato, G., and Didonato, S.

Subjects

Adult, DNA Replication, Male, Adolescent, Molecular Sequence Data, DNA, Mitochondrial, Polymerase Chain Reaction, Chromosomes, Muscular Diseases, Chromosomes, Human, Humans, Dominant, Polymorphism, Southern, Genes, Dominant, Cell Nucleus, Ophthalmoplegia, Base Sequence, Blotting, DNA, Middle Aged, Mitochondria, Muscle, Mitochondrial, Mitochondria, Pedigree, Blotting, Southern, Restriction Fragment Length, Female, Mutation, Polymorphism, Restriction Fragment Length, Chromosome Deletion, Genes, Muscle, Research Article, Human

Abstract

We studied several affected and one nonaffected individuals belonging to three unrelated pedigrees. The pathological trait was an autosomal dominant mitochondrial myopathy due to large-scale multiple deletions of the mitochondrial genome. Clinically, symptomatic patients had progressive external ophthalmoplegia, muscle weakness and wasting, sensorineural hypoacusia, and, in some cases, vestibular areflexia and tremor. The muscle biopsies of all patients examined showed ragged-red fibers, neurogenic changes, and a partially decreased histochemical reaction to cytochrome c oxidase. Multiple mtDNA heteroplasmy was detected in the patients by both Southern blot analysis and PCR amplification, whereas the unaffected individual had the normal homoplasmic hybridization pattern. These findings confirm and add further details to the existence of a new human disease--defined clinically as a mitochondrial myopathy, genetically as a Mendelian autosomal dominant trait, and molecularly by the accumulation of multiple, large-scale deletions of the mitochondrial genome--that is due to impaired nuclear control during mtDNA replication.

Published

1990

29. Identification of five new mutations and three novel polymorphisms in the muscle chloride channel gene (CLCN1) in 20 Italian patients with dominant and recessive myotonia congenita. Mutations in brief no. 118. Online

Author

federica sangiuolo, Botta, A., Mesoraca, A., Servidei, S., Merlini, L., Fratta, G., Novelli, G., and Dallapiccola, B.

Subjects

Polymorphism, Genetic, Myotonia Congenita, Settore MED/46 - Scienze Tecniche di Medicina di Laboratorio, Muscle Proteins, Genes, Recessive, Chloride Channels, Genes, Dominant, Humans, Italy, Mutation, Genes, Genetic, Settore MED/03 - Genetica Medica, Recessive, Dominant, Polymorphism

Abstract

Autosomal dominant myotonia congenita or Thomsen's disease and autosomal recessive myotonia congenita or Becker's are rare nondystrophic disorders due to allelic mutations of the muscle chloride channel gene, CLCN1. We have analysed all 24 exons of the CLCN1 gene, in a panel of 20 unrelated patients (9 with dominant and 11 with recessive mytotonia congenita). We have found five novel mutations including two missense (V5631, F708L), one nonsense (C481X), one splicing (IVS19+2T-A), and one frameshift (2264delC), and also detected the recurrent R894X mutation. These account for 10 of the 22 recessive alleles examined, while no mutations were found in the dominant form. We report three novel polymorphisms (-134T/G, 898C/A and 2154T/C). Our results support high molecular heterogeneity of these myotonias in Italian population and provide new insight for the diagnosis and genetic counselling of these diseases.

30. Revisiting mitochondrial ocular myopathies: a study from the Italian Network

Author

Gabriele Siciliano, Olimpia Musumeci, Tiziana Mongini, Guido Primiano, Isabella Moroni, Corrado Angelini, Liliana Vercelli, Maurizio Moggio, Paola Tonin, Enrico Bertini, Simona Salvatore, S. Servidei, Massimo Zeviani, Daria Diodato, Claudio Bruno, M. Sciacco, Daniele Orsucci, Carlo Minetti, Luca Bello, E. Caldarazzo Ienco, Maria Lucia Valentino, Dario Ronchi, C. Lamperti, Massimiliano Filosto, Michelangelo Mancuso, Giacomo P. Comi, Anna Ardissone, Antonio Toscano, Anna Rubegni, Elena Pegoraro, Valerio Carelli, Antonio Federico, Filippo M. Santorelli, Orsucci, D, Angelini, C, Bertini, E, Carelli, V, Comi, G, Federico, A, Minetti, C, Moggio, M, Mongini, T, Santorelli, F, Servidei, S, Tonin, P, Ardissone, A, Bello, L, Bruno, C, Ienco, E, Diodato, D, Filosto, M, Lamperti, C, Moroni, I, Musumeci, O, Pegoraro, E, Primiano, G, Ronchi, D, Rubegni, A, Salvatore, S, Sciacco, M, Valentino, M, Vercelli, L, Toscano, A, Zeviani, M, Siciliano, G, Mancuso, M, Orsucci, D., Angelini, C., Bertini, E., Carelli, Valerio, Comi, G. P., Federico, A., Minetti, C., Moggio, M., Mongini, T., Santorelli, F. M., Servidei, S., Tonin, P., Ardissone, A., Bello, L., Bruno, C., Ienco, E. Caldarazzo, Diodato, D., Filosto, M., Lamperti, C., Moroni, I., Musumeci, O., Pegoraro, E., Primiano, G., Ronchi, D., Rubegni, A., Salvatore, S., Sciacco, M., Valentino, MARIA LUCIA, Vercelli, L., Toscano, A., Zeviani, M., Siciliano, G., and Mancuso, M.

Subjects

0301 basic medicine, Mitochondrial encephalomyopathy, Male, Pathology, Ophthalmoplegia, Chronic Progressive External, Neurology, CPEO, Mitochondrial disorders, Mitochondrial myopathy, mtDNA, PEO, GTP Phosphohydrolases, GTP Phosphohydrolase, 0302 clinical medicine, Retrospective Studie, Neurology (clinical), Age of Onset, Ophthalmoplegia, Mitochondrial disorder, Mitochondrial, DNA Polymerase gamma, Settore MED/26 - NEUROLOGIA, Phenotype, Italy, Female, Human, Adult, Mitochondrial DNA, medicine.medical_specialty, Mitochondrial disease, Genetic Association Studie, macromolecular substances, Biology, DNA, Mitochondrial, 03 medical and health sciences, Young Adult, medicine, Humans, Genetic Association Studies, Retrospective Studies, External ophthalmoplegia, technology, industry, and agriculture, Retrospective cohort study, DNA, medicine.disease, eye diseases, Mutation, 030104 developmental biology, Chronic Progressive External, Age of onset, 030217 neurology & neurosurgery

Abstract

Ocular myopathy, typically manifesting as progressive external ophthalmoplegia (PEO), is among the most common mitochondrial phenotypes. The purpose of this study is to better define the clinical phenotypes associated with ocular myopathy. This is a retrospective study on a large cohort from the database of the “Nation-wide Italian Collaborative Network of Mitochondrial Diseases”. We distinguished patients with ocular myopathy as part of a multisystem mitochondrial encephalomyopathy (PEO-encephalomyopathy), and then PEO with isolated ocular myopathy from PEO-plus when PEO was associated with additional features of multisystemic involvement. Ocular myopathy was the most common feature in our cohort of mitochondrial patients. Among the 722 patients with a definite genetic diagnosis, ocular myopathy was observed in 399 subjects (55.3%) and was positively associated with mtDNA single deletions and POLG mutations. Ocular myopathy as manifestation of a multisystem mitochondrial encephalomyopathy (PEO-encephalomyopathy, n=131) was linked to the m.3243A>G mutation, whereas the other “PEO” patients (n=268) were associated with mtDNA single deletion and Twinkle mutations. Increased lactate was associated with central neurological involvement. We then defined, among the PEO group, as “pure PEO” the patients with isolated ocular myopathy and “PEO-plus” those with ocular myopathy and other features of neuromuscular and multisystem involvement, excluding central nervous system. The male proportion was significantly lower in pure PEO than PEO-plus. This study reinforces the need for research on the role of gender in mitochondrial diseases. The phenotype definitions here revisited may contribute to a more homogeneous patient categorization, useful in future studies and clinical trials

Published

2017

31. Neuroacanthocytosis Syndromes in an Italian Cohort: Clinical Spectrum, High Genetic Variability and Muscle Involvement

Author

Melissa Barghigiani, Anna Rita Bentivoglio, Alessandra Tessa, Giorgia Bruno, Giuseppe De Michele, Filippo M. Santorelli, Pietro Chiurazzi, Martina Petracca, Giuseppe Di Iorio, Alessandro Vaisfeld, Daniele Galatolo, Clemente Dato, Giulia Straccia, Mariarosa A. B. Melone, Francesco Bove, Anna De Rosa, Serenella Servidei, Maria Gabriella Vita, Silvio Peluso, Simone Sampaolo, Vaisfeld, A, Bruno, G, Petracca, M, Bentivoglio, Ar, Servidei, S, Vita, Mg, Bove, F, Straccia, G, Dato, C, Di Iorio, G, Sampaolo, S, Peluso, S, De Rosa, A, De Michele, G, Barghigiani, M, Galatolo, D, Tessa, A, Santorelli, F, Chiurazzi, P, Melone, Mab., DE ROSA, Anna, DE MICHELE, Giuseppe, and Peluso, Silvio

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Pathology, Erythrocytes, lcsh:QH426-470, Vesicular Transport Proteins, Settore MED/03 - GENETICA MEDICA, Article, Frameshift mutation, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Muscular Diseases, Neuroacanthocytosis, Epidemiology, Genetics, medicine, Humans, McLeod syndrome, chorea-acanthocytosi, Genetic variability, Child, Muscle, Skeletal, XK gene, Gene, Genetics (clinical), Chorea acanthocytosis, business.industry, Incidence (epidemiology), neuroacanthocytosis syndromes, VPS13A gene, medicine.disease, lcsh:Genetics, 030104 developmental biology, Italy, Mutation, chorea-acanthocytosis, Female, business, 030217 neurology & neurosurgery

Abstract

Neuroacanthocytosis (NA) syndromes are a group of genetically defined diseases characterized by the association of red blood cell acanthocytosis, progressive degeneration of the basal ganglia and neuromuscular features with characteristic persistent hyperCKemia. The main NA syndromes include autosomal recessive chorea-acanthocytosis (ChAc) and X-linked McLeod syndrome (MLS). A series of Italian patients selected through a multicenter study for these specific neurological phenotypes underwent DNA sequencing of the VPS13A and XK genes to search for causative mutations. Where it has been possible, muscle biopsies were obtained and thoroughly investigated with histochemical assays. A total of nine patients from five different families were diagnosed with ChAC and had mostly biallelic changes in the VPS13A gene (three nonsense, two frameshift, three splicing), while three patients from a single X-linked family were diagnosed with McLeod syndrome and had a deletion in the XK gene. Despite a very low incidence (only one thousand cases of ChAc and a few hundred MLS cases reported worldwide), none of the 8 VPS13A variants identified in our patients is shared by two families, suggesting the high genetic variability of ChAc in the Italian population. In our series, in line with epidemiological data, McLeod syndrome occurs less frequently than ChAc, although it can be easily suspected because of its X-linked mode of inheritance. Finally, histochemical studies strongly suggest that muscle pathology is not simply secondary to the axonal neuropathy, frequently seen in these patients, but primary myopathic alterations can be detected in both NA syndromes.

Published

2020

32. The m.3243A>G mitochondrial DNA mutation and related phenotypes. A matter of gender?

Author

Olimpia Musumeci, Dario Ronchi, Graziella Uziel, Tiziana Mongini, Elena Caldarazzo Ienco, Enrico Bertini, Alice Donati, Corrado Angelini, Michela Catteruccia, Antonio Toscano, Paola Tonin, Filippo M. Santorelli, Massimo Zeviani, Mauro Scarpelli, Elena Pegoraro, Gabriele Siciliano, Valerio Carelli, Daniele Orsucci, Maurizio Moggio, M. Sciacco, Serenella Servidei, Giacomo P. Comi, Massimiliano Filosto, Donato Sauchelli, Costanza Lamperti, Liliana Vercelli, Michelangelo Mancuso, Maria Lucia Valentino, Carlo Minetti, Isabella Moroni, Claudio Bruno, Mancuso, M., Orsucci, D., Angelini, C., Bertini, E., Carelli, V., Comi, G.P., Donati, A., Minetti, C., Moggio, M., Mongini, T., Servidei, S., Tonin, P., Toscano, A., Uziel, G., Bruno, C., Ienco, E.C., Filosto, M., Lamperti, C., Catteruccia, M., Moroni, I., Musumeci, O., Pegoraro, E., Ronchi, D., Santorelli, F.M., Sauchelli, D., Scarpelli, M., Sciacco, M., Valentino, M.L., Vercelli, L., Zeviani, M., and Siciliano, G.

Subjects

Male, MELAS syndrome, Bioinformatics, G+mutation%22">mitochondrial m.3243A>G mutation, MIDD, Genotype, Databases, Genetic, MELAS Syndrome, Child, Genetics, mtDNA, Medicine (all), Stroke-like episodes, Middle Aged, Mitochondrial DNA, Mitochondrial, Settore MED/26 - NEUROLOGIA, A3243G, mitochondrial DNA, PEO, stroke-like episodes, Phenotype, phenotypic, Italy, Neurology, Lactic acidosis, Child, Preschool, Mutation (genetic algorithm), MELAS, Female, medicine.symptom, Adult, mitochondrial encephalopathy with lactic acidosis and stroke-like episode, Heterozygote, G+"MELAS%22">m.3243A>G "MELAS, Adolescent, Hearing loss, Mitochondrial disease, Biology, DNA, Mitochondrial, Databases, Young Adult, Sex Factors, Genetic, Mitochondrial Encephalomyopathies, medicine, Humans, Aged, Infant, Mutation, Retrospective Studies, Neurology (clinical), Preschool, DNA, medicine.disease

Abstract

The m.3243A>G "MELAS" (mitochondrial encephalopathy with lactic acidosis and stroke-like episodes) mutation is one of the most common point mutations of the mitochondrial DNA, but its phenotypic variability is incompletely understood. The aim of this study was to revise the phenotypic spectrum associated with the mitochondrial m.3243A>G mutation in 126 Italian carriers of the mutation, by a retrospective, database-based study ("Nation-wide Italian Collaborative Network of Mitochondrial Diseases"). Our results confirmed the high clinical heterogeneity of the m.3243A>G mutation. Hearing loss and diabetes were the most frequent clinical features, followed by stroke-like episodes. "MIDD" (maternally-inherited diabetes and deafness) and "PEO" (progressive external ophthalmoplegia) are nosographic terms without any real prognostic value, because these patients may be even more prone to the development of multisystem complications such as stroke-like episodes and heart involvement. The "MELAS" acronym is convincing and useful to denote patients with histological, biochemical and/or molecular evidence of mitochondrial disease who experience stroke-like episodes. Of note, we observed for the first time that male gender could represent a risk factor for the development of stroke-like episodes in Italian m.3243A>G carriers. Gender effect is not a new concept in mitochondrial medicine, but it has never been observed in MELAS. A better elucidation of the complex network linking mitochondrial dysfunction, apoptosis, estrogen effects and stroke-like episodes may hold therapeutic promises. © 2013 Springer-Verlag Berlin Heidelberg.

Published

2014