Your search keyword '"Francesco Muntoni"' showing total 25 results

1. Disease Progression in Charcot–Marie–Tooth Disease Related to <scp> MPZ </scp> Mutations: A Longitudinal Study

Author

Vera, Fridman, Stefan, Sillau, Jacob, Bockhorst, Kaitlin, Smith, Isabella, Moroni, Emanuela, Pagliano, Chiara, Pisciotta, Guiseppe, Piscosquito, Matilde, Laurá, Francesco, Muntoni, Chelsea, Bacon, Shawna, Feely, Tiffany, Grider, Laurie, Gutmann, Rosemary, Shy, Janel, Wilcox, David N, Herrmann, Jun, Li, Sindhu, Ramchandren, Charlotte J, Sumner, Thomas E, Lloyd, John, Day, Carly E, Siskind, Sabrina W, Yum, Reza, Sadjadi, Richard S, Finkel, Steven S, Scherer, Davide, Pareyson, Mary M, Reilly, and Michael E, Shy

Subjects

Neurology, Neurology (clinical)

Abstract

The paucity of longitudinal natural history studies in MPZ neuropathy remains a barrier to clinical trials. We have completed a longitudinal natural history study in patients with MPZ neuropathies across 13 sites of the Inherited Neuropathies Consortium.Change in Charcot-Marie-Tooth Examination Score (CMTES) and Rasch modified CMTES (CMTES-R) were evaluated using longitudinal regression over a 5-year period in subjects with MPZ neuropathy. Data from 139 patients with MPZ neuropathy were examined.The average baseline CMTES and CMTES-R were 10.84 (standard deviation [SD] = 6.0, range = 0-28) and 14.60 (SD = 7.56, range = 0-32), respectively. A mixed regression model showed significant change in CMTES at years 2-5 (mean change from baseline of 0.87 points at 2 years, p = 0.008). Subgroup analysis revealed greater change in CMTES at 2 years in subjects with axonal as compared to demyelinating neuropathy (mean change of 1.30 points [p = 0.016] vs 0.06 points [p = 0.889]). Patients with a moderate baseline neuropathy severity also showed more notable change, by estimate, than those with mild or severe neuropathy (mean 2-year change of 1.14 for baseline CMTES 8-14 [p = 0.025] vs -0.03 for baseline CMTES 0-7 [p = 0.958] and 0.25 for baseline CMTES ≥ 15 [p = 0.6897]). The progression in patients harboring specific MPZ mutations was highly variable.CMTES is sensitive to change over time in adult patients with axonal but not demyelinating forms of MPZ neuropathy. Change in CMTES was greatest in patients with moderate baseline disease severity. These findings will inform future clinical trials of MPZ neuropathies. ANN NEUROL 2022.

Published

2022

2. Clinical Variability in Spinal Muscular Atrophy Type <scp>III</scp>

Author

Claudio Bruno, Gian Luca Vita, Jacqueline Montes, Maria Sframeli, Tina Duong, Valeria Sansone, Annalia Frongia, Mariacristina Scoto, John W. Day, Francesco Muntoni, Giorgia Coratti, Enrico Bertini, Jessica Exposito Escudero, Simona Lucibello, Marika Pane, Sonia Messina, Allan M. Glanzman, Eugenio Mercuri, Roberto De Sanctis, Elena S. Mazzone, Anna Mayhew, Laura Antonaci, Francesca Bovis, Andrés Nascimento Osorio, Matthew Civitello, Sara Carnicella, Rachel Salazar, Richard S. Finkel, Chiara Marini Bettolo, Adele D'Amico, Nathalie Goemans, Robert Muni Lofra, Darryl C. De Vivo, Marleen Van den Hauwe, Maria Carmela Pera, Evelin Milev, Amy Pasternak, Sally Dunaway Young, Emilio Albamonte, and Basil T. Darras

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Longitudinal study, Adolescent, Models, Neurological, Gene Dosage, Spinal Muscular Atrophies of Childhood, Young Adult, 03 medical and health sciences, Settore MED/39 - NEUROPSICHIATRIA INFANTILE, 0302 clinical medicine, Age of Onset, Child, Child, Preschool, Disease Progression, Female, Humans, Survival of Motor Neuron 2 Protein, Models, Internal medicine, medicine, Preschool, business.industry, Repeated measures design, Retrospective cohort study, Spinal muscular atrophy, medicine.disease, SMA, 030104 developmental biology, Neurology, Neurological, Cohort, Neurology (clinical), sma, Age of onset, business, 030217 neurology & neurosurgery, Cohort study

Abstract

OBJECTIVE: We report natural history data in a large cohort of 199 patients with spinal muscular atrophy (SMA) type III assessed using the Hammersmith Functional Motor Scale Expanded (HFMSE). The aim of the study was to establish the annual rate and possible patterns of progression according to a number of variables, such as age of onset, age at assessment, SMN2 copy number, and functional status. METHODS: HFMSE longitudinal changes were assessed using piecewise linear mixed-effects models. The dependency in the data due to repeated measures was accounted for by a random intercept per individual and an unstructured covariance R matrix was used as correlation structure. An additional descriptive analysis was performed for 123 patients, for a total of 375 12-month assessments. RESULTS: A break point at age 7 years was set for the whole cohort and for SMA IIIA and IIIB. Age, SMA type, and ambulatory status were significantly associated with changes in mean HFMSE score, whereas gender and SMN2 copy number were not. The increase in response before the break point of age 7 years is significant only for SMA IIIA (ß = 1.79, p < 0.0001). After the break point, the change in the rate of HFMSE score significantly decrease for both SMA IIIA (ß = -1.15, p < 0.0001) and IIIB (ß = -0.69, p = 0.002). INTERPRETATION: Our findings contribute to the understanding of the natural history of SMA type III and will be helpful in the interpretation of the real-world data of patients treated with commercially available drugs. ANN NEUROL 2020;88:1109-1117.

Published

2020

3. Natural history of Charcot-Marie-Tooth disease during childhood

Author

Manoj P. Menezes, Mary M. Reilly, Michael E. Shy, Matilde Laura, David N. Herrmann, R Shy, Francesco Muntoni, Emanuela Pagliano, Isabella Moroni, Paula Bray, T Estilow, T Bhandari, Kate Eichinger, Richard S. Finkel, Joshua Burns, Kayla M.D. Cornett, Mark Halaki, Davide Pareyson, and Sabrina W. Yum

Subjects

0301 basic medicine, medicine.medical_specialty, Disease progression, Disease, Anthropometry, Confidence interval, Developmental psychology, Natural history, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Neurology, Internal medicine, medicine, Neurology (clinical), Early childhood, Young adult, Psychology, 030217 neurology & neurosurgery, Natural history study

Abstract

Objective To determine the rate of disease progression in a longitudinal natural history study of children with Charcot-Marie-Tooth (CMT) disease. Methods Two hundred six (103 female) participants aged 3 to 20 years enrolled in the Inherited Neuropathies Consortium were assessed at baseline and 2 years. Demographic, anthropometric, and diagnostic information were collected. Disease progression was assessed with the CMT Pediatric Scale (CMTPedS), a reliable Rasch-built linearly weighted disability scale evaluating fine and gross motor function, strength, sensation, and balance. Results On average, CMTPedS Total scores progressed at a rate of 2.4 ± 4.9 over 2 years (14% change from baseline; p

Published

2017

4. Diagnosis and etiology of congenital muscular dystrophy: We are halfway there

Author

Sandra T. Cooper, Mark R. Davis, Kathryn N. North, Nigel G. Laing, Nigel F. Clarke, Roula Ghaoui, Heather A. Best, Sarah A. Sandaradura, Emily C. Oates, Gina L. O'Grady, Monkol Lek, Simranpreet Kaur, Jaya Punetha, Daniel G. MacArthur, Francesco Muntoni, Leigh B. Waddell, Eric P. Hoffman, and Shireen R. Lamandé

Subjects

0301 basic medicine, Proband, Sanger sequencing, Candidate gene, Pathology, medicine.medical_specialty, Muscle biopsy, medicine.diagnostic_test, business.industry, Congenital myasthenic syndrome, medicine.disease, 03 medical and health sciences, symbols.namesake, 030104 developmental biology, 0302 clinical medicine, Neurology, Collagen VI, symbols, Etiology, Congenital muscular dystrophy, Medicine, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

Objective To evaluate the diagnostic outcomes in a large cohort of congenital muscular dystrophy (CMD) patients using traditional and next generation sequencing (NGS) technologies. Methods A total of 123 CMD patients were investigated using the traditional approaches of histology, immunohistochemical analysis of muscle biopsy, and candidate gene sequencing. Undiagnosed patients available for further testing were investigated using NGS. Results Muscle biopsy and immunohistochemical analysis found deficiencies of laminin α2, α-dystroglycan, or collagen VI in 50% of patients. Candidate gene sequencing and chromosomal microarray established a genetic diagnosis in 32% (39 of 123). Of 85 patients presenting in the past 20 years, 28 of 51 who lacked a confirmed genetic diagnosis (55%) consented to NGS studies, leading to confirmed diagnoses in a further 11 patients. Using the combination of approaches, a confirmed genetic diagnosis was achieved in 51% (43 of 85). The diagnoses within the cohort were heterogeneous. Forty-five of 59 probands with confirmed or probable diagnoses had variants in genes known to cause CMD (76%), and 11 of 59 (19%) had variants in genes associated with congenital myopathies, reflecting overlapping features of these conditions. One patient had a congenital myasthenic syndrome, and 2 had microdeletions. Within the cohort, 5 patients had variants in novel (PIGY and GMPPB) or recently published genes (GFPT1 and MICU1), and 7 had variants in TTN or RYR1, large genes that are technically difficult to Sanger sequence. Interpretation These data support NGS as a first-line tool for genetic evaluation of patients with a clinical phenotype suggestive of CMD, with muscle biopsy reserved as a second-tier investigation. Ann Neurol 2016;80:101–111

Published

2016

5. Vascular Defects and Spinal Cord Hypoxia in Spinal Muscular Atrophy

Author

Francesco Muntoni, Robert D. Lees, James N. Sleigh, Thomas H. Gillingwater, Simon H. Parson, Haiyan Zhou, Eilidh Somers, Katie Hoban, and Kevin Talbot

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Cord, business.industry, Skeletal muscle, Spinal muscular atrophy, SMN1, Hypoxia (medical), Motor neuron, medicine.disease, Spinal cord, SMA, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Neurology, medicine, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Objective Spinal muscular atrophy (SMA) is a major inherited cause of infant death worldwide. It results from mutations in a single, ubiquitously expressed gene (SMN1), with loss of lower motor neurons being the primary pathological signature. Systemic defects have also been reported in SMA patients and animal models. We investigated whether defects associated with the vasculature contribute to motor neuron pathology in SMA. Methods Development and integrity of the capillary bed was examined in skeletal muscle and spinal cord of SMA mice, and muscle biopsies from SMA patients and controls, using quantitative morphometric approaches on immunohistochemically labeled tissue. Pimonidazole hydrochloride–based assays were used to identify functional hypoxia. Results The capillary bed in muscle and spinal cord was normal in presymptomatic SMA mice (postnatal day 1), but failed to match subsequent postnatal development in control littermates. At mid- and late-symptomatic time points, the extent of the vascular architecture observed in two distinct mouse models of SMA was ∼50% of that observed in control animals. Skeletal muscle biopsies from human patients confirmed the presence of developmentally similar, significant vascular depletion in severe SMA. Hypovascularity in SMA mouse spinal cord was accompanied by significant functional hypoxia and defects in the blood–spinal cord barrier. Interpretation Our results indicate that vascular defects are a major feature of severe forms of SMA, present in both mouse models and patients, resulting in functional hypoxia of motor neurons. Thus, abnormal vascular development and resulting hypoxia may contribute to the pathogenesis of SMA. Ann Neurol 2016;79:217–230

Published

2016

6. Natural history of Charcot-Marie-Tooth disease during childhood

Author

Kayla M D, Cornett, Manoj P, Menezes, Rosemary R, Shy, Isabella, Moroni, Emanuela, Pagliano, Davide, Pareyson, Timothy, Estilow, Sabrina W, Yum, Trupti, Bhandari, Francesco, Muntoni, Matilde, Laura, Mary M, Reilly, Richard S, Finkel, Kate J, Eichinger, David N, Herrmann, Paula, Bray, Mark, Halaki, Michael E, Shy, and Joshua, Burns

Subjects

Male, Young Adult, Adolescent, Charcot-Marie-Tooth Disease, Child, Preschool, Mutation, Disease Progression, Humans, Female, Longitudinal Studies, Child, Myelin Proteins, Article

Abstract

To determine the rate of disease progression in a longitudinal natural history study of children with Charcot-Marie-Tooth (CMT) disease.Two hundred six (103 female) participants aged 3 to 20 years enrolled in the Inherited Neuropathies Consortium were assessed at baseline and 2 years. Demographic, anthropometric, and diagnostic information were collected. Disease progression was assessed with the CMT Pediatric Scale (CMTPedS), a reliable Rasch-built linearly weighted disability scale evaluating fine and gross motor function, strength, sensation, and balance.On average, CMTPedS Total scores progressed at a rate of 2.4 ± 4.9 over 2 years (14% change from baseline; p 0.001). There was no difference between males and females (mean difference, 0.5; 95% confidence interval [CI], -0.9 to 1.9; p = 0.49). The most responsive CMTPedS items were dorsiflexion strength (z-score change, -0.3; 95% CI, -0.6 to -0.05; p = 0.02), balance (z-score change, -1.0; 95% CI, -1.9 to -0.09; p = 0.03), and long jump (z-score change, -0.4; 95% CI, -0.7 to -0.02; p = 0.04). Of the most common genetic subtypes, 111 participants with CMT1A/PMP22 duplication progressed by 1.8 ± 4.2 (12% change from baseline; p 0.001), 9 participants with CMT1B/MPZ mutation progressed by 2.2 ± 5.1 (11% change), 6 participants with CMT2A/MFN2 mutation progressed by 6.2 ± 7.9 (23% change), and 7 participants with CMT4C/SH3TC2 mutations progressed by 3.0 ± 4.5 (12% change). Participants with CMT2A progressed faster than CMT1A (mean difference, -4.4; 95% CI, -8.1 to -0.8; p = 0.02). Children with CMT1A progressed consistently through early childhood (3-10 years) and adolescence (11-20 years; mean difference, 1.1; 95% CI, -0.6 to 2.7; p = 0.19), whereas CMT2A appeared to progress faster during early childhood than adolescence (mean difference, 10.0; 95% CI, -2.2 to 22.2; p = 0.08).Using the CMTPedS as an outcome measure of disease severity, children with CMT progress at a significant rate over 2 years. Understanding the rate at which children with CMT deteriorate is essential for adequately powering trials of disease-modifying interventions. Ann Neurol 2017;82:353-359.

Published

2017

7. Diagnosis and etiology of congenital muscular dystrophy: We are halfway there

Author

Gina L, O'Grady, Monkol, Lek, Shireen R, Lamande, Leigh, Waddell, Emily C, Oates, Jaya, Punetha, Roula, Ghaoui, Sarah A, Sandaradura, Heather, Best, Simranpreet, Kaur, Mark, Davis, Nigel G, Laing, Francesco, Muntoni, Eric, Hoffman, Daniel G, MacArthur, Nigel F, Clarke, Sandra, Cooper, and Kathryn, North

Subjects

Adult, Adolescent, Genetic Variation, High-Throughput Nucleotide Sequencing, Infant, Collagen Type VI, Muscular Dystrophies, Young Adult, Child, Preschool, Humans, Genetic Predisposition to Disease, Laminin, Child, Dystroglycans, Muscle, Skeletal

Abstract

To evaluate the diagnostic outcomes in a large cohort of congenital muscular dystrophy (CMD) patients using traditional and next generation sequencing (NGS) technologies.A total of 123 CMD patients were investigated using the traditional approaches of histology, immunohistochemical analysis of muscle biopsy, and candidate gene sequencing. Undiagnosed patients available for further testing were investigated using NGS.Muscle biopsy and immunohistochemical analysis found deficiencies of laminin α2, α-dystroglycan, or collagen VI in 50% of patients. Candidate gene sequencing and chromosomal microarray established a genetic diagnosis in 32% (39 of 123). Of 85 patients presenting in the past 20 years, 28 of 51 who lacked a confirmed genetic diagnosis (55%) consented to NGS studies, leading to confirmed diagnoses in a further 11 patients. Using the combination of approaches, a confirmed genetic diagnosis was achieved in 51% (43 of 85). The diagnoses within the cohort were heterogeneous. Forty-five of 59 probands with confirmed or probable diagnoses had variants in genes known to cause CMD (76%), and 11 of 59 (19%) had variants in genes associated with congenital myopathies, reflecting overlapping features of these conditions. One patient had a congenital myasthenic syndrome, and 2 had microdeletions. Within the cohort, 5 patients had variants in novel (PIGY and GMPPB) or recently published genes (GFPT1 and MICU1), and 7 had variants in TTN or RYR1, large genes that are technically difficult to Sanger sequence.These data support NGS as a first-line tool for genetic evaluation of patients with a clinical phenotype suggestive of CMD, with muscle biopsy reserved as a second-tier investigation. Ann Neurol 2016;80:101-111.

Published

2016

8. Validation of the Charcot-Marie-Tooth disease pediatric scale as an outcome measure of disability

Author

R Shy, Robert A. Ouvrier, Mary M. Reilly, Richard S. Finkel, Gyula Acsadi, Matilde Laura, Joshua Burns, Davide Pareyson, Monkol Lek, Francesco Muntoni, Michael E. Shy, T Estilow, and Julie F Pallant

Subjects

Male, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, MEDLINE, Disease, Sensitivity and Specificity, Article, Disability Evaluation, Tooth disease, Charcot-Marie-Tooth Disease, Rating scale, Humans, Medicine, Child, business.industry, Outcome measures, medicine.disease, nervous system diseases, Clinical trial, Peripheral neuropathy, Neurology, Child, Preschool, Scale (social sciences), Physical therapy, Female, Neurology (clinical), Factor Analysis, Statistical, business

Abstract

Charcot-Marie-Tooth disease (CMT) is a common heritable peripheral neuropathy. There is no treatment for any form of CMT, although clinical trials are increasingly occurring. Patients usually develop symptoms during the first 2 decades of life, but there are no established outcome measures of disease severity or response to treatment. We identified a set of items that represent a range of impairment levels and conducted a series of validation studies to build a patient-centered multi-item rating scale of disability for children with CMT.As part of the Inherited Neuropathies Consortium, patients aged 3 to 20 years with a variety of CMT types were recruited from the USA, United Kingdom, Italy, and Australia. Initial development stages involved definition of the construct, item pool generation, peer review, and pilot testing. Based on data from 172 patients, a series of validation studies were conducted, including item and factor analysis, reliability testing, Rasch modeling, and sensitivity analysis.Seven areas for measurement were identified (strength, dexterity, sensation, gait, balance, power, endurance), and a psychometrically robust 11-item scale was constructed (CMT Pediatric Scale [CMTPedS]). Rasch analysis supported the viability of the CMTPedS as a unidimensional measure of disability in children with CMT. It showed good overall model fit, no evidence of misfitting items, and no person misfit, and it was well targeted for children with CMT.The CMTPedS is a well-tolerated outcome measure that can be completed in 25 minutes. It is a reliable, valid, and sensitive global measure of disability for children with CMT from the age of 3 years.

Published

2012

9. Oxidative stress inSEPN1-related myopathy: From pathophysiology to treatment

Author

Bodvael Fraysse, S. Arbogast, Haiyan Zhou, Francesco Muntoni, Ana Ferreiro, and Maud Beuvin

Subjects

Male, medicine.medical_specialty, Adolescent, Muscle Proteins, Oxidative phosphorylation, Biology, Muscle disorder, medicine.disease_cause, Antioxidants, Muscular Diseases, Internal medicine, medicine, Homeostasis, Humans, Child, Selenoproteins, education, Myopathy, Cells, Cultured, chemistry.chemical_classification, education.field_of_study, Reactive oxygen species, Selenoprotein N, Ryanodine receptor, Oxidative Stress, Endocrinology, Neurology, chemistry, Child, Preschool, Gene Targeting, Mutation, Female, Neurology (clinical), medicine.symptom, Oxidation-Reduction, Intracellular, Oxidative stress

Abstract

Objective: Mutations of the selenoprotein N gene (SEPN1) cause SEPN1-relaced myopathy (SEPN1-RM), a novel early-onset muscle disorder formerly divided into four different nosological categories. Selenoprorein N (SelN) is the only selenoprotein involved in a genetic disease; its function being Unknown, no treatment is available for this potentially lethal disorder. Our objective was to clarify the role of SelN and the pathophysiology of SEPN1-RM to identify therapeutic targets.Methods: We established and analyzed an ex vivo model of SelN deficiency using Fibroblast and myoblast primary Cultures from patients with null SEPN1 Mutations. DCFH assay, OxyBlot, Western blot, Fura-2, and cell survival studies were performed to measure intracellular oxidant activity, oxidative stress markets, calcium handling, and response to exogenous treatments.Results: SelN-depleted cells showed oxidative/nitrosative stress manifested by increased intracellular oxidant activity (reactive oxygen species and nitric oxide) and/or excessive oxidation of proteins, including the contractile proteins actin and myosin heavy chain II in myotubes. SelN-devoid myotubes showed also Ca2+ homeostasis abnormalities suggesting dysfunction of the redox-sensor Ca2+ channel ryanodine receptor type 1. Furthermore, absence of SelN was associated with abnormal susceptibility to H2O2-induced oxidative stress, demonstrated by increased cell death. This cell phenotype was restored by pretreatment with the antioxidant N-acetylcysteine.Interpretation: SelN plays a key role in redox homeostasis and human cell protection against oxidative stress. Oxidative/nitrosative stress is a primary pathogenic mechanism in SEPN1-RM, which call be effectively targeted ex vivo by antioxidants. These Findings pave the way to SEPN1-RM treatment, which would represent a First specific pharmacological treatment for a congenital myopathy.

Published

2009

10. Mutation in BAG3 causes severe dominant childhood muscular dystrophy

Author

Duygu Selcen, Francesco Muntoni, Elena Pegoraro, Anna V. Bite, Andrew G. Engel, Barbara K. Burton, and Caroline Sewry

Subjects

Male, Pathology, medicine.medical_specialty, Adolescent, DNA Mutational Analysis, Muscle Fibers, Skeletal, Cardiomyopathy, Muscle Proteins, Biology, Transfection, medicine.disease_cause, Article, Muscular Dystrophies, Microscopy, Electron, Transmission, Chlorocebus aethiops, In Situ Nick-End Labeling, medicine, Animals, Humans, Myotilin, Missense mutation, Muscular dystrophy, Child, Myopathy, Adaptor Proteins, Signal Transducing, Mutation, Genetic heterogeneity, medicine.disease, Crystallins, Neurology, COS Cells, Female, Desmin, Neurology (clinical), medicine.symptom, Apoptosis Regulatory Proteins

Abstract

Myofibrillar myopathies (MFMs) are morphologically distinct but genetically heterogeneous muscular dystrophies in which disintegration of Z disks and then of myofibrils is followed by ectopic accumulation of multiple proteins. Cardiomyopathy, neuropathy, and dominant inheritance are frequent associated features. Mutations in alphaB-crystallin, desmin, myotilin, Zasp, or filamin-C can cause MFMs and were detected in 32 of 85 patients of the Mayo MFM cohort. Bag3, another Z-disk-associated protein, has antiapoptotic properties, and its targeted deletion in mice causes fulminant myopathy with early lethality. We therefore searched for mutations in BAG3 in 53 unrelated MFM patients.We searched for mutations in BAG3 by direct sequencing. We analyzed structural changes in muscle by histochemistry, immunocytochemistry, and electron microscopy, examined mobility of the mutant Bag3 by nondenaturing electrophoresis, and searched for abnormal aggregation of the mutant protein in COS-7 (SV-40 transformed monkey kidney fibroblast-7) cells.We identified a heterozygous p.Pro209Leu mutation in three patients. All presented in childhood, had progressive limb and axial muscle weakness, and experienced development of cardiomyopathy and severe respiratory insufficiency in their teens; two had rigid spines, and one a peripheral neuropathy. Electron microscopy showed disintegration of Z disks, extensive accumulation of granular debris and larger inclusions, and apoptosis of 8% of the nuclei. On nondenaturing electrophoresis of muscle extracts, the Bag3 complex migrated faster in patient than control extracts, and expression of FLAG-labeled mutant and wild-type Bag3 in COS cells showed abnormal aggregation of the mutant protein.We conclude mutation in Bag3 defines a novel severe autosomal dominant childhood muscular dystrophy.

Published

2008

11. Brain involvement in muscular dystrophies with defective dystroglycan glycosylation

Author

Haluk Topaloglu, Mary A. Rutherford, Adnan Y. Manzur, Robert McWilliam, Ros Quinlivan, Eugenio Mercuri, Andrea Klein, Cheryl Longman, Maria Kinali, Volker Straub, Janine Smith, Kathryn N. North, Emma Clement, Beril Talim, Stephanie A. Robb, Frances M. Cowan, Francesco Muntoni, Caroline Godfrey, Stephen Abbs, A. James Barkovich, Kate Bushby, R. Mein, University of Zurich, and Muntoni, F

Subjects

Pathology, medicine.medical_specialty, Glycosylation, Adolescent, Clinical Neurology, Lissencephaly, 610 Medicine & health, N-Acetylglucosaminyltransferases, Nervous System Malformations, Mannosyltransferases, Muscular Dystrophies, medicine, Polymicrogyria, Dystroglycan, Humans, Genetic Predisposition to Disease, Muscular dystrophy, Child, Dystroglycans, Walker–Warburg syndrome, biology, business.industry, fungi, Infant, Newborn, Brain, Infant, Membrane Proteins, Cortical dysplasia, medicine.disease, Magnetic Resonance Imaging, Fukutin, Hypoplasia, 2728 Neurology (clinical), Phenotype, Neurology, 10036 Medical Clinic, 2808 Neurology, Child, Preschool, Mutation, biology.protein, Neurology (clinical), business

Abstract

Objective: To assess the range and severity of brain involvement, as assessed by magnetic resonance imaging, in 27 patients with mutations in POMT1 (4), POMT2 (9), POMGnT1 (7), Fukutin (4), or LARGE (3), responsible for muscular dystrophies with abnormal glycosylation of dystroglycan (dystroglycanopathies). Methods: Blinded review of magnetic resonance imaging brain scans from 27 patients with mutations in 1 of these 5 genes. Results: Brain magnetic resonance images were normal in 3 of 27 patients; in another 5, only nonspecific abnormalities (ventricular dilatation, periventricular white matter abnormalities, or both) were seen. The remaining 19 patients had a spectrum of structural defects, ranging from complete lissencephaly in patients with Walker–Warburg syndrome to isolated cerebellar involvement. Cerebellar cysts and/or dysplasia and hypoplasia were the predominant features in four patients. Polymicrogyria (11/27) was more severe in the frontoparietal regions in 6, and had an occipitofrontal gradient in 2. Pontine clefts, with an unusual appearance to the corticospinal tracts, were seen in five patients with a muscle-eye-brain–like phenotype, three patients with POMGnT1, one with LARGE, and one with POMT2 mutations. Prominent cerebellar cysts were always seen with POMGnT1 mutations, but rarely seen in POMT1 and POMT2. Brainstem and pontine abnormalities were common in patients with POMT2, POMGnT1, and LARGE mutations. Interpretation: Our results expand the spectrum of brain involvement associated with mutations in LARGE, POMGnT1, POMT1, and POMT2. Pontine clefts were visible in some dystroglycanopathy patients. Infratentorial structures were often affected in isolation, highlighting their susceptibility to involvement in these conditions. Ann Neurol 2008;64:573–582

Published

2008

12. De novoLMNAmutations cause a new form of congenital muscular dystrophy

Author

Pascale Guicheney, Nigel F. Clarke, L. Demay, Helen Roper, Norma B. Romero, Enrico Bertini, Carsten G. Bönnemann, Monique M. Ryan, Rabah Ben Yaou, Brigitte Estournet, Linda De Meirleir, Pierre Yves Jeannet, Caroline Sewry, Pascale Richard, B. Mbieleu, Susana Quijano-Roy, A. Barois, Andrés Nascimento, Ana Ferreiro, Francesco Muntoni, Gisèle Bonne, Adele D'Amico, Jaume Colomer, Jean Marie Cuisset, and Pediatrics

Subjects

Adult, Genetic Markers, Male, medicine.medical_specialty, Pathology, Cardiomyopathy, LMNA, Humans, Medicine, Muscular dystrophy, Child, Myopathy, Muscle contracture, congenital muscular dystrophy, biology, business.industry, Muscle weakness, Lamin Type A, medicine.disease, Surgery, Muscular Dystrophies, Limb-Girdle, Neurology, Child, Preschool, Mutation, Congenital muscular dystrophy, biology.protein, Female, Creatine kinase, Neurology (clinical), medicine.symptom, business

Abstract

Objective: To describe a new entity of congenital muscular dystrophies caused by de novo LMNA mutations. Methods: Fifteen patients presenting with a myopathy of onset in the first year of life were subjected to neurological and genetic evaluation. Histopathological and immunohistochemical analyses were performed for all patients. Results: The 15 patients presented with muscle weakness in the first year of life, and all had de novo heterozygous LMNA mutations. Three of them had severe early-onset disease, no motor development, and the rest experienced development of a “dropped head” syndrome phenotype. Despite variable severity, there was a consistent clinical pattern. Patients typically presented with selective axial weakness and wasting of the cervicoaxial muscles. Limb involvement was predominantly proximal in upper extremities and distal in lower extremities. Talipes feet and a rigid spine with thoracic lordosis developed early. Proximal contractures appeared later, most often in lower limbs, sparing the elbows. Ten children required ventilatory support, three continuously through tracheotomy. Cardiac arrhythmias were observed in four of the oldest patients but were symptomatic only in one. Creatine kinase levels were mild to moderately increased. Muscle biopsies showed dystrophic changes in nine children and nonspecific myopathic changes in the remaining. Markedly atrophic fibers were common, most often type 1, and a few patients showed positive inflammatory markers. Interpretation: The LMNA mutations identified appear to correlate with a relatively severe phenotype. Our results further broaden the spectrum of laminopathies and define a new disease entity that we suggest is best classified as a congenital muscular dystrophy (LMNA-related congenital muscular dystrophy, or L-CMD). Ann Neurol 2008;64:177–186

Published

2008

13. Nemaline myopathy caused by absence of α-skeletal muscle actin

Author

A. Barois, Norma B. Romero, Waney Squier, Caroline Sewry, J. Angus Dobbie, Carmen Navarro, Anne-Marie Childs, J.R. Ricoy, Cristina Reina, Francesco Muntoni, Sandeep Jayawant, Richard Appleton, Kristen J. Nowak, Nigel G. Laing, K.R. Walker, Sophie Clément, and Roger C. Mountford

Subjects

Male, Pathology, medicine.medical_specialty, Blotting, Western, Biology, Arginine, Myopathies, Nemaline, Nemaline myopathy, Biopsy, medicine, Humans, Muscle, Skeletal, Nemaline bodies, Actin, Aspartic Acid, Fetus, medicine.diagnostic_test, Myocardium, Homozygote, Infant, Skeletal muscle, medicine.disease, Immunohistochemistry, Congenital myopathy, Actins, Microscopy, Electron, medicine.anatomical_structure, Neurology, Child, Preschool, Mutation, Tyrosine, Neurology (clinical)

Abstract

Objective To investigate seven congenital myopathy patients from six families: one French Gypsy, one Spanish Gypsy, four British Pakistanis, and one British Indian. Three patients required mechanical ventilation from birth, five died before 22 months, one is ventilator-dependent, but one, at 30 months, is sitting with minimal support. All parents were unaffected. Methods The α-skeletal muscle actin gene (ACTA1) was sequenced. Available muscle biopsies were investigated by standard histological and electron microscopic techniques. The expression of various proteins was determined by immunohistochemistry, western blotting, or both. Results Three homozygous ACTA1 null mutations were identified: p.Arg41X in the French patient, p.Tyr364fsX in the Spanish patient, and p.Asp181fsX10 in all five British patients. An absence of α-skeletal muscle actin protein but presence of α-cardiac actin was shown in all muscle biopsies examined, with more α-cardiac actin in the biopsy from the child with the greatest muscle function. Muscle biopsies from all patients exhibited nemaline bodies whereas three also contained zebra bodies. Interpretation The seven patients have recessive nemaline myopathy caused by absence of α-skeletal muscle actin. The level of retention of α-cardiac actin, the skeletal muscle fetal actin isoform, may determine α-skeletal muscle actin disease severity. This has implications for possible future therapy. Ann Neurol 2006

Published

2007

14. Infantile spinal muscular atrophy with respiratory distress type 1 (SMARD1)

Author

Christoph Hübner, Robert A. Ouvrier, Haluk Topaloglu, Heidemarie Neitzel, Nathalie Goemans, Christina Steglich, Carmen Navarro, Piroschka Stolz, Francesco Muntoni, Friedrich Bosch, Enrico Bertini, Kate Bushby, Ulf-Peter Guenther, Hanns Lochmüller, Katja Grohmann, Stephan Eichholz, Padraic Grattan-Smith, Sabine Rudnik-Schöneborn, Markus Schuelke, Raymonda Varon, Coleen Adams, Lionel Van Maldergem, Tilman Polster, Catrin Janetzki, and Klaus Zerres

Subjects

Pediatrics, medicine.medical_specialty, Pathology, Respiratory distress, business.industry, Respiratory disease, Muscle weakness, Prenatal diagnosis, Spinal muscular atrophy, Sudden infant death syndrome, medicine.disease, Central nervous system disease, Degenerative disease, Neurology, medicine, Neurology (clinical), medicine.symptom, business

Abstract

Autosomal recessive spinal muscular atrophy with respiratory distress type 1 (SMARD1) is the second anterior horn cell disease in infants in which the genetic defect has been defined. SMARD1 results from mutations in the gene encoding the immunoglobulin mu-binding protein 2 (IGHMBP2) on chromosome 11q13. Our aim was to review the clinical features of 29 infants affected with SMARD1 and report on 26 novel IGHMBP2 mutations. Intrauterine growth retardation, weak cry, and foot deformities were the earliest symptoms of SMARD1. Most patients presented at the age of 1 to 6 months with respiratory distress due to diaphragmatic paralysis and progressive muscle weakness with predominantly distal lower limb muscle involvement. Sensory and autonomic nerves are also affected. Because of the poor prognosis, there is a demand for prenatal diagnosis, and clear diagnostic criteria for infantile SMARD1 are needed. The diagnosis of SMARD1 should be considered in infants with non-5q spinal muscular atrophy, neuropathy, and muscle weakness and/or respiratory distress of unclear cause. Furthermore, consanguineous parents of a child with sudden infant death syndrome should be examined for IGHMBP2 mutations.

Published

2003

15. X-linked vacuolar myopathies: Two separate loci and refined genetic mapping

Author

Michel Fardeau, Francesco Muntoni, Mari Auranen, Marcello Villanova, Stephen W. Scherer, Berge A. Minassian, and Hannu Kalino

Subjects

Genetics, Cardiomyopathy, Chromosome, Biology, medicine.disease, Xq28, Neurology, Gene mapping, medicine, Neurology (clinical), Muscular dystrophy, Allele, medicine.symptom, Myopathy, X chromosome

Abstract

X-linked vacuolar myopathies can be divided into two forms: one that is associated with cardiomyopathy and mental retardation (XVCM-MR) and a second form, termed X-linked myopathy with excessive autophagy (XMEA), that spares cardiac muscle and has no central nervous system involvement. In this article, we demonstrate linkage between XMEA and markers on chromosome Xq28 and assign the XMEA gene locus to the most telomeric 10.5 cM of chromosome X. We also show that XVCM-MR is not allelic to XMEA.

Published

2000

16. The ever-expanding spectrum of congenital muscular dystrophies

Author

Eugenio Mercuri and Francesco Muntoni

Subjects

Heterogeneous group, Glycosyltransferases, Biology, Muscular Dystrophies, Clinical neurology, Settore MED/39 - NEUROPSICHIATRIA INFANTILE, Neurology, Alpha-Dystroglycan, inglese, Humans, Identification (biology), Neurology (clinical), Dystroglycans, Muscle, Skeletal, Neuroscience

Abstract

Congenital muscular dystrophies are a highly heterogeneous group of conditions. In the last few years the identification of several new genes encoding for both glycosyltransferases and structural proteins has expanded the spectrum of the known forms. New classifications based on combined clinical, genetic and pathological data include all the recently discovered genes and allow an easier identification of the different forms and insight on pathogenetic mechanisms. The aim of this review is to discuss the most recent advances in this field, providing a conceptual framework to help the understanding of the responsible mechanisms and, when available, an update on the therapeutic perspectives.

Published

2012

17. RYR1 mutations are a common cause of congenital myopathies with central nuclei

Author

Wolfram Kress, Komala Pillay, Stephen Abbs, V cloke, Caroline Sewry, Haiyan Zhou, Howard E. Henderson, CG Boennemann, Clemens R. Müller, Enrico Bertini, Heinz Jungbluth, Francesco Muntoni, Jo M. Wilmshurst, Alvin Ndondo, James J. Dowling, S. Lillis, Susan Treves, Volker Straub, Ros Quinlivan, Adnan Y. Manzur, Thomas Cullup, and Safa Al-Sarraj

Subjects

Male, Pathology, medicine.medical_specialty, Heterozygote, Adolescent, Genotype, Biology, Compound heterozygosity, South Africa, medicine, Humans, Centronuclear myopathy, Myopathy, Child, Muscle, Skeletal, Genetics, RYR1, Muscle biopsy, medicine.diagnostic_test, Ryanodine Receptor Calcium Release Channel, medicine.disease, Congenital myopathy, Europe, DNM2, Phenotype, Neurology, Child, Preschool, Mutation, Neurology (clinical), medicine.symptom, Central core disease, Myopathies, Structural, Congenital

Abstract

Objective: Centronuclear myopathy (CNM) is a rare congenital myopathy characterized by prominence of central nuclei on muscle biopsy. CNM has been associated with mutations in MTM1, DNM2, and BIN1 but many cases remain genetically unresolved. RYR1 encodes the principal sarcoplasmic reticulum calcium release channel and has been implicated in various congenital myopathies. We investigated whether RYR1 mutations cause CNM. Methods: We sequenced the entire RYR1 coding sequence in 24 patients with a diagnosis of CNM from South Africa (n ¼ 14) and Europe (n ¼ 10) and identified mutations in 17 patients. The most common genotypes featured compound heterozygosity for RYR1 missense mutations and mutations resulting in reduced protein expression, including intronic splice site and frameshift mutations. Results: The high incidence in South African patients (n ¼ 12/14) in conjunction with recurrent RYR1 mutations associated with common haplotypes suggested the presence of founder effects. In addition to central nuclei, prominent histopathological findings included (often multiple) internalized nuclei and t ype 1f iber predominance and hypotrophy with relative type 2 hypertrophy. Although cores were not typically seen on oxidative stains, electron microscopy revealed subtle abnormalities in most cases. External ophthalmoplegia, proximal weakness, and bulbar involvement were prominent clinical findings. Interpretation: Our findings expand the range of RYR1-related phenotypes and suggest RYR1 mutations as a common cause of congenital myopathies with central nuclei. Corresponding to recent observations in X-linked CNM, these findings indicate disturbed assembly and/or malfunction of the excitation-contraction machinery as a key mechanism in CNM and related myopathies. ANN NEUROL 2010;68:717–726

Published

2010

18. Fukutin gene mutations in steroid-responsive limb girdle muscular dystrophy

Author

Lucy Feng, Cecilia Jimenez-Mallebrera, Susan C. Brown, Martin Brockington, Francesco Muntoni, Yehuda Shapira, Mary A. Rutherford, Diana M. Escolar, Silvia Torelli, Caroline Godfrey, Stephen Abbs, R. Mein, Emma Clement, and Caroline Sewry

Subjects

musculoskeletal diseases, Male, Pathology, medicine.medical_specialty, Glycosylation, DNA Mutational Analysis, Anti-Inflammatory Agents, Gene mutation, medicine.disease_cause, Fukuyama congenital muscular dystrophy, medicine, Dystroglycan, Humans, Point Mutation, Muscular dystrophy, Walker–Warburg syndrome, Dystroglycans, Muscle, Skeletal, Genetics, Mutation, biology, Siblings, Infant, Membrane Proteins, Exons, medicine.disease, Fukutin, Immunohistochemistry, Neurology, Muscular Dystrophies, Limb-Girdle, biology.protein, Prednisone, Female, Neurology (clinical), Limb-girdle muscular dystrophy

Abstract

Objective: Defects in glycosylation of -dystroglycan are associated with several forms of muscular dystrophy, often characterized by congenital onset and severe structural brain involvement, collectively known as dystroglycanopathies. Six causative genes have been identified in these disorders including fukutin. Mutations in fukutin cause Fukuyama congenital muscular dystrophy. This is the second most common form of muscular dystrophy in Japan and is invariably associated with mental retardation and structural brain defects. The aim of this study was to determine the genetic defect in two white families with a dystroglycanopathy. Methods: The six genes responsible for dystroglycanopathies were studied in three children with a severe reduction of -dystroglycan in skeletal muscle. Results: We identified pathogenic fukutin mutations in these two families. Affected children had normal intelligence and brain structure and shared a limb girdle muscular dystrophy (LGMD) phenotype, had marked elevation of serum creatine kinase, and were all ambulant with remarkable steroid responsiveness. Interpretation: Our data suggest that fukutin mutations occur outside Japan and can be associated with much milder phenotypes than Fukuyama congenital muscular dystrophy. These findings significantly expand the spectrum of phenotypes associated with fukutin mutations to include this novel form of limb girdle muscular dystrophy that we propose to name LGMD2L. Ann Neurol 2006;60:603– 610

Published

2006

19. Cardiac and respiratory failure in limb-girdle muscular dystrophy 2I

Author

Thomas Voit, Klaus Wrogemann, Kate Bushby, Patrick Frosk, Volker Straub, Cheerag Shirodaria, David Hilton-Jones, Michelle Eagle, Francesco Muntoni, John P. Bourke, Cheryl R. Greenberg, and M Poppe

Subjects

Adult, Male, medicine.medical_specialty, Vital capacity, Heterozygote, Heart disease, Adolescent, Heart Diseases, DNA Mutational Analysis, Vital Capacity, Cardiomyopathy, Medizin, Electrocardiography, Internal medicine, Medicine, Humans, Muscular dystrophy, Child, Retrospective Studies, business.industry, Respiratory disease, Homozygote, Age Factors, Membrane Proteins, Proteins, Middle Aged, medicine.disease, Surgery, Neurology, Respiratory failure, Muscular Dystrophies, Limb-Girdle, Echocardiography, Heart failure, Mutation, Cardiology, Female, Neurology (clinical), business, Respiratory Insufficiency, Limb-girdle muscular dystrophy

Abstract

Mutations in the gene encoding fukutin-related protein cause limb-girdle muscular dystrophy 2I. In this multicenter retrospective analysis of 38 patients, 55.3% had cardiac abnormalities, of which 24% had developed cardiac failure. Heterozygotes for the common C826A mutation developed cardiac involvement earlier than homozygotes. All patients initially improved while receiving standard therapy. Independent of cardiac status, forced vital capacity was below 75% in 44.4% of the patients. There was no absolute correlation between skeletal muscle weakness and cardiomyopathy or respiratory insufficiency. These complications are a primary part of this specific type of limb-girdle muscular dystrophy, with important implications for management.

Published

2004

20. Infantile spinal muscular atrophy with respiratory distress type 1 (SMARD1)

Author

Katja, Grohmann, Raymonda, Varon, Piroschka, Stolz, Markus, Schuelke, Catrin, Janetzki, Enrico, Bertini, Kate, Bushby, Francesco, Muntoni, Robert, Ouvrier, Lionel, Van Maldergem, Nathalie M L A, Goemans, Hanns, Lochmüller, Stephan, Eichholz, Coleen, Adams, Friedrich, Bosch, Padraic, Grattan-Smith, Carmen, Navarro, Heidemarie, Neitzel, Tilman, Polster, Haluk, Topaloğlu, Christina, Steglich, Ulf P, Guenther, Klaus, Zerres, Sabine, Rudnik-Schöneborn, and Christoph, Hübner

Subjects

DNA-Binding Proteins, Male, Respiratory Distress Syndrome, Newborn, Mutation, Infant, Newborn, Humans, Infant, Female, Spinal Muscular Atrophies of Childhood, Carrier Proteins, Transcription Factors

Abstract

Autosomal recessive spinal muscular atrophy with respiratory distress type 1 (SMARD1) is the second anterior horn cell disease in infants in which the genetic defect has been defined. SMARD1 results from mutations in the gene encoding the immunoglobulin micro-binding protein 2 (IGHMBP2) on chromosome 11q13. Our aim was to review the clinical features of 29 infants affected with SMARD1 and report on 26 novel IGHMBP2 mutations. Intrauterine growth retardation, weak cry, and foot deformities were the earliest symptoms of SMARD1. Most patients presented at the age of 1 to 6 months with respiratory distress due to diaphragmatic paralysis and progressive muscle weakness with predominantly distal lower limb muscle involvement. Sensory and autonomic nerves are also affected. Because of the poor prognosis, there is a demand for prenatal diagnosis, and clear diagnostic criteria for infantile SMARD1 are needed. The diagnosis of SMARD1 should be considered in infants with non-5q spinal muscular atrophy, neuropathy, and muscle weakness and/or respiratory distress of unclear cause. Furthermore, consanguineous parents of a child with sudden infant death syndrome should be examined for IGHMBP2 mutations.

Published

2003

21. Phenotypic spectrum associated with mutations in the fukutin-related protein gene

Author

Ralf Herrmann, Francesco Muntoni, Silvia Torelli, Pascale Guicheney, Martin Brockington, Y Yuva, Thomas Voit, Caroline Sewry, Victor Dubowitz, Susana Quijano-Roy, Brigitte Estournet, Derek J. Blake, Norma B. Romero, Susan C. Brown, Eugenio Mercuri, and Volker Straub

Subjects

Adult, Adolescent, Biopsy, Nonsense mutation, Medizin, Mutation, Missense, medicine.disease_cause, Severity of Illness Index, Muscular Dystrophies, Ventricular Dysfunction, Left, Peripheral Nervous System, medicine, Missense mutation, Humans, Pentosyltransferases, Muscular dystrophy, Age of Onset, Child, Dystroglycans, Muscle, Skeletal, Genetics, Mutation, Fukutin-related protein, Membrane Glycoproteins, biology, Brain, Proteins, Hypoventilation, medicine.disease, Fukutin, Muscular Dystrophy, Duchenne, Cytoskeletal Proteins, Phenotype, Neurology, Child, Preschool, biology.protein, Congenital muscular dystrophy, Female, Neurology (clinical), Limb-girdle muscular dystrophy

Abstract

We describe 22 patients with mutations in the fukutin-related protein (FKPR) gene. Four patients had congenital muscular dystrophy (MDC1C), with presentation at birth, severe weakness and inability to stand unsupported. The other 18 had limb girdle muscular dystrophy (LGMD2I). Eleven showed a Duchenne-like course with loss of ambulation in the early teens while 7 had a milder phenotype. Muscle biopsy invariably showed abnormal expression of a-dystroglycan. MDC1C patients either carried 2 missense or 1 missense and 1 nonsense mutations. Patients with LGMD2I shared a common mutation (C826A,Leu276Ileu) and their phenotypic severity was correlated with the second allelic mutation.

Published

2003

22. Clinical and molecular genetic spectrum of autosomal dominant Emery-Dreifuss muscular dystrophy due to mutations of the lamin A/C gene

Author

C Pollitt, Lacombe D, Denis Duboc, Manfred Wehnert, Gisèle Bonne, Isabelle Pénisson-Besnier, Francesco Muntoni, Bruno Eymard, Ketty Schwartz, Antoine Muchir, Eugenio Mercuri, D. Recan, Isabelle Desguerre, Boor R, Jean-Marie Cuisset, Luciano Merlini, Kate Bushby, Daniela Toniolo, Matthias Vorgerd, Wicklein Em, Andoni Urtizberea, Michel Fardeau, Xavier Ferrer, H.M. Bécane, and Reuner U

Subjects

Adult, Male, Contracture, Adolescent, Genotype, Biopsy, Nonsense mutation, DNA Mutational Analysis, Emerin, Mutation, Missense, Laminopathy, Biology, LMNA, Cardiovascular Physiological Phenomena, medicine, Missense mutation, Humans, Emery–Dreifuss muscular dystrophy, Muscular dystrophy, Age of Onset, Child, Creatine Kinase, Physical Examination, Muscle contracture, Aged, Genes, Dominant, Genetics, Muscle Weakness, Myocardium, Nuclear Proteins, Heart, Middle Aged, medicine.disease, Lamin Type A, Lamins, Muscular Dystrophy, Emery-Dreifuss, Pedigree, Muscular Atrophy, Phenotype, Neurology, Disease Progression, Female, Neurology (clinical), Gene Deletion

Abstract

Emery-Dreifuss muscular dystrophy (EDMD) is characterized by early contractures of the elbows and Achilles tendons, slowly progressive muscle wasting and weakness, and life-threatening cardiomyopathy with conduction blocks. We recently identified LMNA encoding two nuclear envelope proteins, lamins A and C, to be implicated in the autosomal dominant form of EDMD. Here, we report on the variability of the phenotype and spectrum of LMNA mutations in 53 autosomal dominant EDMD patients (36 members of 6 families and 17 sporadic cases). Twelve of the 53 patients showed cardiac involvement exclusively, although the remaining 41 all showed muscle weakness and contractures. We were able to identify a common phenotype among the patients with skeletal muscle involvement, consisting of humeroperoneal wasting and weakness, scapular winging, rigidity of the spine, and elbow and Achilles tendon contractures. The disease course was generally slow, but we observed either a milder phenotype characterized by late onset and a mild degree of weakness and contractures or a more severe phenotype with early presentation and a rapidly progressive course in a few cases. Mutation analysis identified 18 mutations in LMNA (ie, 1 nonsense mutation, 2 deletions of a codon, and 15 missense mutations). All the mutations were distributed between exons 1 and 9 in the region of LMNA that is common to lamins A and C. LMNA mutations arose de novo in 76% of the cases; 2 of these de novo mutations were typical hot spots, and 2 others were identified in 2 unrelated cases. There was no clear correlation between the phenotype and type or localization of the mutations within the gene. Moreover, a marked inter- and intra-familial variability in the clinical expression of LMNA mutations exists, ranging from patients expressing the full clinical picture of EDMD to those characterized only by cardiac involvement, which points toward a significant role of possible modifier genes in the course of this disease. In conclusion, the high proportion of de novo mutations together with the large spectrum of both LMNA mutations and the expression of the disease should now prompt screening for LMNA in familial and sporadic cases of both EDMD and dilated cardiomyopathy associated with conduction system disease. Ann Neurol 2000;48:170–180

Published

2000

23. Nemaline myopathy caused by absence of α‐skeletal muscle actin.

Author

Kristen J. Nowak, Caroline A. Sewry, Carmen Navarro, Waney Squier, Cristina Reina, Jose R. Ricoy, Sandeep S. Jayawant, Anne‐Marie Childs, J. Angus Dobbie, Richard E. Appleton, Roger C. Mountford, Kendall R. Walker, Sophie Clement, Annie Barois, Francesco Muntoni, Norma B. Romero, and Nigel G. Laing

Abstract

To investigate seven congenital myopathy patients from six families: one French Gypsy, one Spanish Gypsy, four British Pakistanis, and one British Indian. Three patients required mechanical ventilation from birth, five died before 22 months, one is ventilator‐dependent, but one, at 30 months, is sitting with minimal support. All parents were unaffected.The α‐skeletal muscle actin gene (ACTA1) was sequenced. Available muscle biopsies were investigated by standard histological and electron microscopic techniques. The expression of various proteins was determined by immunohistochemistry, western blotting, or both.Three homozygous ACTA1 null mutations were identified: p.Arg41X in the French patient, p.Tyr364fsX in the Spanish patient, and p.Asp181fsX10 in all five British patients. An absence of α‐skeletal muscle actin protein but presence of α‐cardiac actin was shown in all muscle biopsies examined, with more α‐cardiac actin in the biopsy from the child with the greatest muscle function. Muscle biopsies from all patients exhibited nemaline bodies whereas three also contained zebra bodies.The seven patients have recessive nemaline myopathy caused by absence of α‐skeletal muscle actin. The level of retention of α‐cardiac actin, the skeletal muscle fetal actin isoform, may determine α‐skeletal muscle actin disease severity. This has implications for possible future therapy. Ann Neurol 2006 [ABSTRACT FROM AUTHOR]

Published

2007

24. Cardiac and respiratory failure in limb‐girdle muscular dystrophy 2I.

Author

Maja Poppe, John Bourke, Michelle Eagle, Patrick Frosk, Klaus Wrogemann, Cheryl Greenberg, Francesco Muntoni, Thomas Voit, Volker Straub, David Hilton‐Jones, Cheerag Shirodaria, and Kate Bushby

Published

2004

25. Phenotypic spectrum associated with mutations in the fukutin-related protein gene.

Author

Eugenio Mercuri, Martin Brockington, Volker Straub, Susana Quijano-Roy, Yeliz Yuva, Ralf Herrmann, Susan C. Brown, Silvia Torelli, Victor Dubowitz, Derek J. Blake, Norma B. Romero, Brigitte Estournet, Caroline A. Sewry, Pascale Guicheney, Thomas Voit, and Francesco Muntoni

Published

2003