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6. 262P A global analysis of the CMT1A locus: implications for the origin and susceptibility to Charcot-Marie-Tooth disease type 1A across populations.

Author

Cruz, P. Rodriguez, Alitsiou, A., Diagne, R., Lia-Baldini, A., Ghorab, K., Diop, A. Gallo, Ndiaye, M., Beltran, S., and Lao, O.

Subjects
*HOMOLOGOUS recombination, *WHOLE genome sequencing, *GENETIC recombination, *GENETIC variation, *CHARCOT-Marie-Tooth disease, *DISEASE susceptibility
Abstract

Charcot-Marie-Tooth type 1A (CMT1A) is an inherited neuropathy with an estimated prevalence of 1/5000 in the general population. CMT1A results from abnormal dosage of the PMP22 gene, arising from non-allelic homologous recombination (NAHR) events between paralogous sequences called CMT1A-REPs, flanking the gene. While extensively documented in Caucasian individuals, CMT1A is under-reported in individuals of African genetic ancestry. We hypothesize that this is due to differences in the CMT1A-REPs between individuals of African and non-African genetic background. Our aim is to study the variability of CMT1A-REPs between populations using available genetic data and in silico analyses. Here, we have built a combined dataset from previous whole genome sequencing efforts (1KGP, HGDP and other available datasets at EGA) with a focus on capturing African genetic variation. Leveraging this data, we explore haplotypes based on both common and rare SNPs, structural variants in CMT1A-REP regions, recombination-related elements, and their potential interactions, as well as their distribution across different populations. We find that individuals of African genetic ancestry harbour distinct CMT1A-REP haplotypes with lower recombination rates and reduced sequence similarity compared to other ethnicities. This suggests potential genetic variation protective against NAHR-mediated events causing CMT1A. Additionally, recombination regulators like PRDM9 might differ between African and non-African ethnicities, hinting at distinct mechanisms at play. In conclusion, our study shows genetic differences in the CMT1A locus between African and non-African ancestries, which may account to the under-reporting of CMT1A in individuals of African genetic origin. However, further research is needed to better understand the epidemiology of inherited neuropathies and CMT1A in the African continent and how CMT1A-REP variations influence disease risk. [ABSTRACT FROM AUTHOR]

Published
2024
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7. The First Large Deletion of ATL3 Identified in a Patient Presenting with a Sensory Polyneuropathy.

Author

Pyromali I, Richard L, Derouault P, Vallat JM, Ghorab K, Magdelaine C, Sturtz F, Favreau F, and Lia AS

Abstract

Hereditary sensory neuropathies (HSN) are a heterogenous group of sensory neuropathies. Mutations in ATL3 have been described in patients presenting with hereditary sensory neuropathy IF (HSN1F), a subtype of HSN. Herein, by analyzing targeted-NGS data of a patient presenting with sensory neuropathy symptoms using the CovCopCan bioinformatic tool, we discovered the presence of a deletion of around 3kb in ATL3 from Chr11:63,401,422 to Chr11:63,398,182. This deletion affects ATL3 exons 11 and 12 and could lead to the mutation c.(1036-861_1539+329del), p.(Ala346_Gln513del). In addition, an analysis of the breakpoints' sequences revealed the presence of Alu transposable elements at the position of the breakpoints, which pointed to a possible erroneous recombination event following a non-allelic-homologous-recombination mechanism in this area. Moreover, electronic microscopy analysis of the patient's nerve biopsy revealed a severe rarefaction of the myelinated fibers, a demyelinating-remyelinating process, and an abnormal aspect of the endoplasmic reticulum. These findings suggest that this structural variation could potentially be responsible for the HSN symptoms of the patient. Research of structural variations in ATL3 in numerous other patients presenting similar symptoms should be broadly investigated in order to improve patients' diagnoses.

Published
2023
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8. GM2 gangliosidosis AB variant: first case of late onset and review of the literature.

Author

Ganne B, Dauriat B, Richard L, Lamari F, Ghorab K, Magy L, Benkirane M, Perani A, Marquet V, Calvas P, Yardin C, and Bourthoumieu S

Subjects
Humans, Male, Young Adult, G(M2) Activator Protein genetics, G(M2) Ganglioside metabolism, Gangliosides, Mutation genetics, Gangliosidoses, GM2 genetics
Abstract

AB variant is the rarest form of GM2 gangliosidosis, neurodegenerative diseases caused by lysosomal accumulation of GM2 gangliosides. Less than thirty cases are referenced in the literature, and to date, no late-onset form has been described. Our proband is a 22-year-old male with spinocerebellar ataxia and lower limbs motor deficiency. His symptoms started at the age of 10. A genetic analysis revealed two mutations in the GM2A gene encoding the GM2 activator protein (GM2-AP), an essential co-factor of hexosaminidase A. Both mutations, GM2A:c.79A > T:p.Lys27* and GM2A:c.415C > T:p.Pro139Ser, were inherited respectively from his father and his mother. The nonsense mutation was predicted to be likely pathogenic, but the missense mutation was of unknown significance. To establish the pathogenicity of this variant, we studied GM2 accumulation and GM2A gene expression. Electron microscopy and immunofluorescence performed on patient's fibroblasts did not reveal any lysosomal accumulation of GM2. There was also no difference in GM2A gene expression using RT-qPCR, and both mutations were found on cDNA Sanger sequencing. Measurement of plasma gangliosides by liquid-phase chromatography-tandem mass spectrometry showed an accumulation of GM2 in our patient's plasma at 83.5 nmol/L, and a GM2/GM3 ratio at 0.066 (median of negative control at 30.2 nmol/L [19.7-46.8] and 0.019 respectively). Therefore, the association of both p.Lys27* and p.Pro169Ser mutations leads to a GM2-AP functional deficiency. Whereas the first mutation is more likely to be linked with infantile form of GM2 gangliosidosis, the hypomorphic p.Pro169Ser variant may be the first associated with a late-onset form of AB variant., (© 2022. Fondazione Società Italiana di Neurologia.)

Published
2022
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9. CIDP and hemopathies, an underestimated association.

Author

Deschamps N, Mathis S, Duchesne M, Ghorab K, Gallouedec G, Richard L, Boulesteix JM, Corcia P, Magy L, and Vallat JM

Subjects
Biopsy, Humans, Peripheral Nerves, Peripheral Nervous System, Retrospective Studies, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating diagnosis, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating epidemiology, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating therapy
Abstract

Chronic inflammatory demyelinating polyradiculoneuropathy (CIDP) is an immune-mediated and treatable disease that may be associated with various systemic conditions. Our objective is to describe the clinical, electrophysiological and pathological data of a series of patients with both CIDP and hemopathy. In this retrospective study, we analyzed 21 patients with CIDP and various hemopathies (malignant or not), consecutively observed for almost five years. In this particular context (with a risk of neurological complications of the hemopathy), a nerve biopsy was taken from each patient (after written consent). All the patients fulfilled the EAN/PNS electrodiagnostic criteria (2021) of CIDP: 16 with 'CIDP' and 2 with 'possible CIDP' (no data for 3 patients). For each patient, pathological analysis of nerve biopsy was compatible with the diagnosis of CIDP, and there was no evidence for hematological complication of the peripheral nervous system. In cases of peripheral neuropathy and malignant hemopathy, the possibility that the peripheral neuropathy is CIDP should not be overlooked because CIDP is clearly accessible to appropriate therapies, with high potential for a positive clinical response. If the diagnosis of CIDP is usually suspected clinically and electrophysiologically, it should be confirmed by pathological study (nerve biopsy) in certain cases. The management of such patients benefits from the collaboration of neurologists, hematologists and oncologists., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published
2021
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10. The Wide Spectrum of Pathophysiologic Mechanisms of Paraproteinemic Neuropathy.

Author

Vallat JM, Duchesne M, Corcia P, Richard L, Ghorab K, Magy L, and Mathis S

Subjects
Anemia, Hemolytic, Autoimmune diagnosis, Anemia, Hemolytic, Autoimmune etiology, Anemia, Hemolytic, Autoimmune pathology, Anemia, Hemolytic, Autoimmune physiopathology, Ataxia diagnosis, Ataxia etiology, Ataxia pathology, Ataxia physiopathology, Autoantibodies immunology, Biopsy, Decision Trees, Electrodiagnosis, Humans, Immunoglobulin A, Immunoglobulin G, Immunoglobulin Light-chain Amyloidosis complications, Immunoglobulin Light-chain Amyloidosis diagnosis, Immunoglobulin Light-chain Amyloidosis physiopathology, Immunoglobulin M, Monoclonal Gammopathy of Undetermined Significance, Myelin-Associated Glycoprotein immunology, Neural Conduction physiology, Ophthalmoplegia diagnosis, Ophthalmoplegia etiology, Ophthalmoplegia pathology, Ophthalmoplegia physiopathology, POEMS Syndrome diagnosis, POEMS Syndrome etiology, POEMS Syndrome pathology, POEMS Syndrome physiopathology, Paraproteinemias complications, Paraproteinemias diagnosis, Peripheral Nerves pathology, Peripheral Nerves ultrastructure, Peripheral Nervous System Diseases diagnosis, Peripheral Nervous System Diseases etiology, Peripheral Nervous System Diseases pathology, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating diagnosis, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating etiology, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating pathology, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating physiopathology, Primary Dysautonomias diagnosis, Primary Dysautonomias etiology, Primary Dysautonomias pathology, Primary Dysautonomias physiopathology, Small Fiber Neuropathy diagnosis, Small Fiber Neuropathy etiology, Small Fiber Neuropathy pathology, Small Fiber Neuropathy physiopathology, Waldenstrom Macroglobulinemia, Paraproteinemias physiopathology, Peripheral Nervous System Diseases physiopathology
Abstract

Monoclonal gammopathy is encountered quite frequently in the general population. This type of hematologic abnormality may be mild, referred to as monoclonal gammopathy of undetermined significance or related to different types of hematologic malignancies. The association of a peripheral neuropathy with monoclonal gammopathy is also fairly common, and hemopathy may be discovered in an investigation of peripheral neuropathy. In such a situation, it is essential to determine the exact nature of the hematologic process in order not to miss a malignant disease and thus initiate the appropriate treatment (in conjunction with hematologists and oncologists). In this respect, nerve biopsy (discussed on a case-by-case basis) is of great value in the management of such patients. We therefore propose to present the objectives and main interests of nerve biopsy in this situation., (© 2020 American Academy of Neurology.)

Published
2021
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11. A novel pathogenic variant in DYNC1H1 causes various upper and lower motor neuron anomalies.

Author

Viollet LM, Swoboda KJ, Mao R, Best H, Ha Y, Toutain A, Guyant-Marechal L, Laroche-Raynaud C, Ghorab K, Barthez MA, Pedespan JM, Hernandorena X, Lia AS, Deleuze JF, Masson C, Nelson I, Nectoux J, and Si Y

Subjects
Adolescent, Adult, Child, Child, Preschool, Female, Heterozygote, Humans, Lower Extremity physiopathology, Male, Middle Aged, Motor Neurons physiology, Muscle, Skeletal physiopathology, Muscular Atrophy, Spinal pathology, Pedigree, Phenotype, Reflex, Upper Extremity physiopathology, Cytoplasmic Dyneins genetics, Muscular Atrophy, Spinal genetics, Mutation, Missense
Abstract

Objective: To perform genotype-phenotype, clinical and molecular analysis in a large 3-generation family with autosomal dominant congenital spinal muscular atrophy., Methods: Using a combined genetic approach including whole genome scanning, next generation sequencing-based multigene panel, whole genome sequencing, and targeted variant Sanger sequencing, we studied the proband and multiple affected individuals of this family who presented bilateral proximal lower limb muscle weakness and atrophy., Results: We identified a novel heterozygous variant, c.1826T > C; p.Ile609Thr, in the DYNC1H1 gene localized within the common haplotype in the 14q32.3 chromosomal region which cosegregated with disease in this large family. Within the family, affected individuals were found to have a wide array of clinical variability. Although some individuals presented the typical lower motor neuron phenotype with areflexia and denervation, others presented with muscle weakness and atrophy, hyperreflexia, and absence of denervation suggesting a predominant upper motor neuron disease. In addition, some affected individuals presented with an intermediate phenotype characterized by hyperreflexia and denervation, expressing a combination of lower and upper motor neuron defects., Conclusion: Our study demonstrates the wide clinical variability associated with a single disease causing variant in DYNC1H1 gene and this variant demonstrated a high penetrance within this large family., (Copyright © 2020. Published by Elsevier Masson SAS.)

Published
2020
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12. Hearing loss in inherited peripheral neuropathies: Molecular diagnosis by NGS in a French series.

Author

Lerat J, Magdelaine C, Roux AF, Darnaud L, Beauvais-Dzugan H, Naud S, Richard L, Derouault P, Ghorab K, Magy L, Vallat JM, Cintas P, Bieth E, Arne-Bes MC, Goizet C, Espil-Taris C, Journel H, Toutain A, Urtizberea JA, Boespflug-Tanguy O, Laffargue F, Corcia P, Pasquier L, Fradin M, Napuri S, Ciron J, Boulesteix JM, Sturtz F, and Lia AS

Subjects
Adult, Age of Onset, Aged, Aged, 80 and over, Alleles, Computational Biology, Female, France epidemiology, Genetic Testing, Genotype, Hearing Loss epidemiology, High-Throughput Nucleotide Sequencing, Humans, Inheritance Patterns, Male, Middle Aged, Mutation, Pedigree, Peripheral Nervous System Diseases epidemiology, Phenotype, Genetic Association Studies methods, Genetic Predisposition to Disease, Hearing Loss diagnosis, Hearing Loss genetics, Peripheral Nervous System Diseases diagnosis, Peripheral Nervous System Diseases genetics
Abstract

Background: The most common inherited peripheral neuropathy is Charcot-Marie-Tooth disease (CMT), with a prevalence of 1/2500. Other symptoms can be associated to the condition, such as hearing loss. Currently, no global hearing impairment assessment has been determined, and the physiopathology is not well known., Methods: The aim of the study was to analyze among a French series of 3,412 patients with inherited peripheral neuropathy (IPN), the ones who also suffer from hearing loss, to establish phenotype-genotype correlations. An NGS strategy for IPN one side and nonsyndromic hearing loss (NSHL) on the other side, were performed., Results: Hearing loss (HL) was present in only 44 patients (1.30%). The clinical data of 27 patients were usable. Demyelinating neuropathy was diagnosed in 15 cases and axonal neuropathy in 12 cases. HL varied from mild to profound. Five cases of auditory neuropathy were noticed. Diagnosis was made for 60% of these patients. Seven novel pathogenic variants were discovered in five different genes: PRPS1; MPZ; SH3TC2; NEFL; and ABHD12. Two patients with PMP22 variant, had also an additional variant in COCH and MYH14 respectively. No pathogenic variant was found at the DFNB1 locus. Genotype-phenotype correlations do exist, especially with SH3TC2, PRPS1, ABHD12, NEFL, and TRPV4., Conclusion: Involvement of PMP22 is not enough to explain hearing loss in patients suffering from IPN. HL can be due to cochlear impairment and/or auditory nerve dysfunction. HL is certainly underdiagnosed, and should be evaluated in every patient suffering from IPN., (© 2019 The Authors. Molecular Genetics & Genomic Medicine published by Wiley Periodicals, Inc.)

Published
2019
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13. A novel pathogenic variant of NEFL responsible for deafness associated with peripheral neuropathy discovered through next-generation sequencing and review of the literature.

Author

Lerat J, Magdelaine C, Beauvais-Dzugan H, Espil C, Ghorab K, Latour P, Derouault P, Sturtz F, and Lia AS

Subjects
Aged, Female, High-Throughput Nucleotide Sequencing, Humans, Review Literature as Topic, Charcot-Marie-Tooth Disease genetics, Hearing Loss, Sensorineural genetics, Neurofilament Proteins genetics
Abstract

Neurofilaments are neuron-specific intermediate filaments essential for the radial growth of axons during development and the maintenance of axonal diameter. Pathogenic variants of Neurofilament Light (NEFL) are associated with CMT1F, CMT2E, and CMTDIG and have been observed in less than 1% of Charcot-Marie-Tooth (CMT) cases, resulting in the reporting of 35 variants in 173 CMT patients to date. However, only six variants have been reported in 17 patients with impaired hearing. No genotype-phenotype correlations have yet been established. Here, we report an additional case: a 69-year-old female, who originally presented with axonal sensory and motor neuropathy at the age of 45, associated with moderate sensorineural hearing loss, with a slight slope at high frequencies. Next-generation sequencing identified a novel pathogenic variant: c.269A > G, p.(Glu90Gly). Hearing impairment is often linked to CMT due to pathogenic variants of NEFL, especially p.(Glu90Lys) and p.(Asn98Ser), and in our case p.(Glu90Gly). These pathogenic variants are all located at hot spots, in the head domain and the two ends of the rod domain of the protein., (© 2019 Peripheral Nerve Society.)

Published
2019
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15. Value of nerve biopsy in the management of peripheral neuropathies.

Author

Mathis S, Magy L, Le Masson G, Richard L, Soulages A, Solé G, Duval F, Ghorab K, Vallat JM, and Duchesne M

Subjects
Humans, Peripheral Nervous System Diseases complications, Peripheral Nervous System Diseases diagnosis, Vasculitis complications, Biopsy, Peripheral Nervous System Diseases etiology, Peripheral Nervous System Diseases pathology
Abstract

Introduction: Peripheral neuropathy is a common symptom throughout the population, with numerous possible etiologies. The diagnosis of peripheral neuropathies (and their causes) is mainly based on clinical, electrophysiological, biological, and imaging features. Areas covered: This paper reviews the main causes of neuropathy and discusses the usefulness of nerve biopsy (NB) in such cases. Expert commentary: In most cases, NB is not mandatory in the diagnostic work-up of a peripheral neuropathy. However, NB is clearly an indication in cases of vasculitis. It is also valuable in peripheral neuropathies with severe and rapid worsening (without clear cause) in order to uncover a pathological hallmark (amyloid deposits). Although NB is considered an invasive method, it may be useful in the management of peripheral neuropathy, especially to guide treatment in certain cases. In summary, although NB is not a systematic procedure, it is a useful tool that should be discussed on a case-by-case basis within the clinical context.

Published
2018
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16. History and current difficulties in classifying inherited myopathies and muscular dystrophies.

Author

Mathis S, Tazir M, Magy L, Duval F, Le Masson G, Duchesne M, Couratier P, Ghorab K, Solé G, Lacoste I, Goizet C, and Vallat JM

Subjects
History, 19th Century, History, 20th Century, History, 21st Century, Humans, Muscular Diseases genetics, Muscular Diseases history, Muscular Diseases physiopathology, Muscular Diseases classification
Abstract

The wide spectrum of hereditary muscular disorders leads to unavoidable difficulties in their classification, even for specialists. For this reason, new proposals are required that would ultimately replace our current rather complex classifications by a simpler structure. Our proposal will be limited to dystrophic and non-dystrophic myopathies (excluding metabolic disorders, mitochondriopathies, and channelopathies) for which similar proposals would also be relevant. Various genes (encoding structural proteins associated with the sarcolemma, nuclear membrane proteins, and proteins involved in myofiber metabolism have now been sequenced and mutations ascribed to specific forms of inherited muscular disorders. Based on our observations and our recent proposals in other neurogenetic conditions and informal discussions with specialists of neuromuscular disorders, the prerequisite for a simple and sound classification for inherited muscular disorders should encompass the clinical and pathological phenotypes (described in a simple and clear manner), the mode of inheritance, and the mutated gene. We think that the denomination of the different subtypes could be simplified considerably, although any new proposal of classification of muscular disorders will need to be discussed in the neurological and genetic communities., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published
2018
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17. Erratum to: An exploratory randomised double-blind and placebo-controlled phase 2 study of a combination of baclofen, naltrexone and sorbitol (PXT3003) in patients with Charcot-Marie-Tooth disease type 1A.

Author

Attarian S, Vallat JM, Magy L, Funalot B, Gonnaud PM, Lacour A, Péréon Y, Dubourg O, Pouget J, Micallef J, Franques J, Lefebvre MN, Ghorab K, Al-Moussawi M, Tiffreau V, Preudhomme M, Magot A, Leclair-Visonneau L, Stojkovic T, Bossi L, Lehert P, Gilbert W, Bertrand V, Mandel J, Milet A, Hajj R, Boudiaf L, Scart-Grès C, Nabirotchkin S, Guedj M, Chumakov I, and Cohen D

Published
2016
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18. Variations in multiple sclerosis practice within Europe - Is it time for a new treatment guideline?

Author

Marziniak M, Ghorab K, Kozubski W, Pfleger C, Sousa L, Vernon K, Zaffaroni M, and Meuth SG

Subjects
Europe, Humans, Multiple Sclerosis diagnosis, Practice Patterns, Physicians', Healthcare Disparities, Multiple Sclerosis therapy, Practice Guidelines as Topic
Abstract

In the past 5 years, the combination of developments in diagnostic strategy and approval of new disease-modifying therapies has provided an opportunity to achieve dramatic improvements in patient outcomes in multiple sclerosis (MS). However, across Europe there are several factors that may prevent patients from receiving the best therapy at the appropriate time, and there is variation among countries in terms of which of these factors are most relevant. Here, we review current MS clinical practices in a number of countries in the European Union to identify differences regarding initiation of treatment in patients with clinically isolated syndrome or relapsing-remitting MS, and differences in the timing of treatment switch or escalation. While recognizing that policy is not static in any country, we believe that patients' interests would be better served if a European treatment guideline was developed. Such a guideline could both inform and be informed by national policies, facilitating the dissemination of best clinical practice internationally., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published
2016
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19. Gender as a Modifying Factor Influencing Myotonic Dystrophy Type 1 Phenotype Severity and Mortality: A Nationwide Multiple Databases Cross-Sectional Observational Study.

Author

Dogan C, De Antonio M, Hamroun D, Varet H, Fabbro M, Rougier F, Amarof K, Arne Bes MC, Bedat-Millet AL, Behin A, Bellance R, Bouhour F, Boutte C, Boyer F, Campana-Salort E, Chapon F, Cintas P, Desnuelle C, Deschamps R, Drouin-Garraud V, Ferrer X, Gervais-Bernard H, Ghorab K, Laforet P, Magot A, Magy L, Menard D, Minot MC, Nadaj-Pakleza A, Pellieux S, Pereon Y, Preudhomme M, Pouget J, Sacconi S, Sole G, Stojkovich T, Tiffreau V, Urtizberea A, Vial C, Zagnoli F, Caranhac G, Bourlier C, Riviere G, Geille A, Gherardi RK, Eymard B, Puymirat J, Katsahian S, and Bassez G

Subjects
Adult, Cross-Sectional Studies, Female, Humans, Male, Myotonic Dystrophy mortality, Sex Distribution, Socioeconomic Factors, Databases, Factual, Myotonic Dystrophy epidemiology, Phenotype
Abstract

Background: Myotonic Dystrophy type 1 (DM1) is one of the most heterogeneous hereditary disease in terms of age of onset, clinical manifestations, and severity, challenging both medical management and clinical trials. The CTG expansion size is the main factor determining the age of onset although no factor can finely predict phenotype and prognosis. Differences between males and females have not been specifically reported. Our aim is to study gender impact on DM1 phenotype and severity., Methods: We first performed cross-sectional analysis of main multiorgan clinical parameters in 1409 adult DM1 patients (>18 y) from the DM-Scope nationwide registry and observed different patterns in males and females. Then, we assessed gender impact on social and economic domains using the AFM-Téléthon DM1 survey (n = 970), and morbidity and mortality using the French National Health Service Database (n = 3301)., Results: Men more frequently had (1) severe muscular disability with marked myotonia, muscle weakness, cardiac, and respiratory involvement; (2) developmental abnormalities with facial dysmorphism and cognitive impairment inferred from low educational levels and work in specialized environments; and (3) lonely life. Alternatively, women more frequently had cataracts, dysphagia, digestive tract dysfunction, incontinence, thyroid disorder and obesity. Most differences were out of proportion to those observed in the general population. Compared to women, males were more affected in their social and economic life. In addition, they were more frequently hospitalized for cardiac problems, and had a higher mortality rate., Conclusion: Gender is a previously unrecognized factor influencing DM1 clinical profile and severity of the disease, with worse socio-economic consequences of the disease and higher morbidity and mortality in males. Gender should be considered in the design of both stratified medical management and clinical trials.

Published
2016
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20. Simultaneous Combined Myositis, Inflammatory Polyneuropathy, and Overlap Myasthenic Syndrome.

Author

Mathis S, Magy L, Corcia P, Ghorab K, Richard L, Ciron J, Duchesne M, and Vallat JM

Abstract

Immune-mediated neuromuscular disorders include pathologies of the peripheral nervous system, neuromuscular junction, and muscles. If overlap syndromes (or the association of almost two autoimmune disorders) are recognized, the simultaneous occurrence of several autoimmune neuromuscular disorders is rare. We describe two patients presenting the simultaneous occurrence of inflammatory neuropathy, myositis, and myasthenia gravis (with positive acetylcholine receptor antibodies). For each patient, we carried out a pathological analysis (nerve and muscle) and an electrophysiological study (and follow-up). To our knowledge, this is the first description of such a triple immune-mediated neuromuscular syndrome. We compared our observations with a few other cases of simultaneous diagnosis of two inflammatory neuromuscular disorders., Competing Interests: The authors declare that they have no competing interests.

Published
2016
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21. Natalizumab as a Disease-Modifying Therapy in Chronic Inflammatory Demyelinating Polyneuropathy - A Report of Three Cases.

Author

Vallat JM, Mathis S, Ghorab K, Milor MA, Richard L, and Magy L

Subjects
Adult, Aged, Female, Humans, Male, Middle Aged, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating pathology, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating physiopathology, Immunologic Factors therapeutic use, Natalizumab therapeutic use, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating drug therapy
Abstract

Background: Several treatments are available to treat the immune-mediated chronic inflammatory demyelinating polyneuropathy (CIDP). Among these treatments, intravenous immunoglobulins, corticosteroids and plasma exchanges are validated and widely used. A few immunosuppressive drugs have been tried, but they had little efficiency., Methods: We describe three CIDP patients treated by Natalizumab (acting against cellular adhesion and T-cell migration) after a failure of the validated treatments., Results: We observed a long-term improvement in one patient, a dramatic improvement over a significant duration in another patient and stabilization in the last one., Conclusion: This open label study provides evidence for the value of Natalizumab as second-line treatment for individual patients with a high dependency on waning efficacy of first-line therapies. CIDP is characterized by heterogeneity of clinical phenotypes, electrophysiological and pathological features, and various variable courses types of evolution. The different responses to drugs of our patients are consistent with some reported cases and may reflect the spectrum of lesional mechanisms and the molecular dysfunctions in CIDP., (© 2015 S. Karger AG, Basel.)

Published
2015
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22. Value of nerve biopsy in patients with latent malignant hemopathy and peripheral neuropathy: a case series.

Author

Duchesne M, Mathis S, Corcia P, Richard L, Ghorab K, Jaccard A, Magy L, and Vallat JM

Subjects
Aged, Biopsy, Female, Hematologic Neoplasms pathology, Humans, Leukemia, Lymphocytic, Chronic, B-Cell diagnosis, Leukemia, Lymphocytic, Chronic, B-Cell pathology, Leukemia, Lymphocytic, Chronic, B-Cell therapy, Lymphoma, B-Cell diagnosis, Lymphoma, B-Cell pathology, Lymphoma, B-Cell therapy, Lymphoma, Non-Hodgkin diagnosis, Lymphoma, Non-Hodgkin pathology, Lymphoma, Non-Hodgkin therapy, Male, Middle Aged, Peripheral Nervous System Diseases pathology, Disease Management, Hematologic Neoplasms diagnosis, Hematologic Neoplasms therapy, Peripheral Nerves pathology, Peripheral Nervous System Diseases diagnosis
Abstract

Hematological malignancies include several diseases that may affect the peripheral nervous system (PNS) through various mechanisms. A common and challenging situation is represented by the occurrence of an active peripheral neuropathy in a patient with a supposed inactive hematological disorder.We report clinical, electrophysiological, biological, and pathological data of 8 patients with latent malignant hemopathies (most were considered in remission): B-cell chronic lymphocytic leukemia in 3 patients, B-cell lymphoma in 1 patient, low-grade non-Hodgkin's lymphoma in 1 patient, Waldenström's macroglobulinemia in 1 patient, smoldering multiple myeloma in 1 patient, and monoclonal gammopathy of undetermined significance in 1 patient.In all these cases, the nerve biopsy (NB) helped to diagnose the hematological relapse or detect a pathological mechanism linked to the hematological disorder: epineurial lymphocytic infiltration in 5 patients (including one with antimyelin-associated glycoprotein antibodies), cryoglobulin deposits in 1 patient, chronic inflammatory demyelinating polyneuropathy in 1 patient, and necrotizing vasculitis in 1 patient. In each case, pathological findings were crucial to select the adequate treatment, leading to an improvement in the neurological and biological manifestations.These observations illustrate the value of NB and the need for active collaboration between neurologists and hematologists in such cases.

Published
2015
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23. Heterogeneity of Polyneuropathy Associated with Anti-MAG Antibodies.

Author

Magy L, Kaboré R, Mathis S, Lebeau P, Ghorab K, Caudie C, and Vallat JM

Subjects
Aged, Aged, 80 and over, Female, Humans, Immunoglobulin M immunology, Male, Middle Aged, Myelin Sheath immunology, Peripheral Nerves immunology, Retrospective Studies, Antibodies, Monoclonal immunology, Autoantibodies immunology, Myelin-Associated Glycoprotein immunology, Polyneuropathies immunology, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating immunology
Abstract

Polyneuropathy associated with IgM monoclonal gammopathy and anti-myelin associated glycoprotein (MAG) antibodies is an immune-mediated demyelinating neuropathy. The pathophysiology of this condition is likely to involve anti-MAG antibody deposition on myelin sheaths of the peripheral nerves and it is supposed to be distinct from chronic inflammatory demyelinating neuropathy (CIDP), another immune-mediated demyelinating peripheral neuropathy. In this series, we have retrospectively reviewed clinical and laboratory findings from 60 patients with polyneuropathy, IgM gammopathy, and anti-MAG antibodies. We found that the clinical picture in these patients is highly variable suggesting a direct link between the monoclonal gammopathy and the neuropathy. Conversely, one-third of patients had a CIDP-like phenotype on electrodiagnostic testing and this was correlated with a low titer of anti-MAG antibodies and the absence of widening of myelin lamellae. Our data suggest that polyneuropathy associated with anti-MAG antibodies is less homogeneous than previously said and that the pathophysiology of the condition is likely to be heterogeneous as well with the self-antigen being MAG in most of the patients but possibly being another component of myelin in the others.

Published
2015
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24. An exploratory randomised double-blind and placebo-controlled phase 2 study of a combination of baclofen, naltrexone and sorbitol (PXT3003) in patients with Charcot-Marie-Tooth disease type 1A.

Author

Attarian S, Vallat JM, Magy L, Funalot B, Gonnaud PM, Lacour A, Péréon Y, Dubourg O, Pouget J, Micallef J, Franques J, Lefebvre MN, Ghorab K, Al-Moussawi M, Tiffreau V, Preudhomme M, Magot A, Leclair-Visonneau L, Stojkovic T, Bossi L, Lehert P, Gilbert W, Bertrand V, Mandel J, Milet A, Hajj R, Boudiaf L, Scart-Grès C, Nabirotchkin S, Guedj M, Chumakov I, and Cohen D

Subjects
Adult, Double-Blind Method, Drug Therapy, Combination, Female, Humans, Male, Middle Aged, Baclofen administration & dosage, Charcot-Marie-Tooth Disease diagnosis, Charcot-Marie-Tooth Disease drug therapy, Naltrexone administration & dosage, Sorbitol administration & dosage
Abstract

Background: Charcot-Marie-Tooth type 1A disease (CMT1A) is a rare orphan inherited neuropathy caused by an autosomal dominant duplication of a gene encoding for the structural myelin protein PMP22, which induces abnormal Schwann cell differentiation and dysmyelination, eventually leading to axonal suffering then loss and muscle wasting. We favour the idea that diseases can be more efficiently treated when targeting multiple disease-relevant pathways. In CMT1A patients, we therefore tested the potential of PXT3003, a low-dose combination of three already approved compounds (baclofen, naltrexone and sorbitol). Our study conceptually builds on preclinical experiments highlighting a pleiotropic mechanism of action that includes downregulation of PMP22. The primary objective was to assess safety and tolerability of PXT3003. The secondary objective aimed at an exploratory analysis of efficacy of PXT3003 in CMT1A, to be used for designing next clinical development stages (Phase 2b/3)., Methods: 80 adult patients with mild-to-moderate CMT1A received in double-blind for 1 year Placebo or one of the three increasing doses of PXT3003 tested, in four equal groups. Safety and tolerability were assessed with the incidence of related adverse events. Efficacy was assessed using the Charcot-Marie-Tooth Neuropathy Score (CMTNS) and the Overall Neuropathy Limitations Scale (ONLS) as main endpoints, as well as various clinical and electrophysiological outcomes., Results: This trial confirmed the safety and tolerability of PXT3003. The highest dose (HD) showed consistent evidence of improvement beyond stabilization. CMTNS and ONLS, with a significant improvement of respectively of 8% (0.4% - 16.2%) and 12.1% (2% - 23.2%) in the HD group versus the pool of all other groups, appear to be the most sensitive clinical endpoints to treatment despite their quasi-stability over one year under Placebo. Patients who did not deteriorate over one year were significantly more frequent in the HD group., Conclusions: These results confirm that PXT3003 deserves further investigation in adults and could greatly benefit CMT1A-diagnosed children, usually less affected than adults., Trial Registration: EudraCT Number: 2010-023097-40. ClinicalTrials.gov Identifier: NCT01401257. The Committee for Orphan Medicinal Products issued in February 2014 a positive opinion on the application for orphan designation for PXT3003 (EMA/OD/193/13).

Published
2014
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25. Constitutive activation of the calcium sensor STIM1 causes tubular-aggregate myopathy.

Author

Böhm J, Chevessier F, Maues De Paula A, Koch C, Attarian S, Feger C, Hantaï D, Laforêt P, Ghorab K, Vallat JM, Fardeau M, Figarella-Branger D, Pouget J, Romero NB, Koch M, Ebel C, Levy N, Krahn M, Eymard B, Bartoli M, and Laporte J

Subjects
Adolescent, Adult, Aged, Amino Acid Sequence, Animals, Base Sequence, Cell Line, Child, Female, Homeostasis, Humans, Male, Membrane Proteins chemistry, Membrane Proteins genetics, Mice, Middle Aged, Molecular Sequence Data, Muscles pathology, Muscles ultrastructure, Mutation genetics, Myoblasts metabolism, Myoblasts pathology, Myopathies, Structural, Congenital genetics, Neoplasm Proteins chemistry, Neoplasm Proteins genetics, Pedigree, Phenotype, Stromal Interaction Molecule 1, Young Adult, Calcium metabolism, Membrane Proteins metabolism, Myopathies, Structural, Congenital pathology, Neoplasm Proteins metabolism
Abstract

Tubular aggregates are regular arrays of membrane tubules accumulating in muscle with age. They are found as secondary features in several muscle disorders, including alcohol- and drug-induced myopathies, exercise-induced cramps, and inherited myasthenia, but also exist as a pure genetic form characterized by slowly progressive muscle weakness. We identified dominant STIM1 mutations as a genetic cause of tubular-aggregate myopathy (TAM). Stromal interaction molecule 1 (STIM1) is the main Ca(2+) sensor in the endoplasmic reticulum, and all mutations were found in the highly conserved intraluminal Ca(2+)-binding EF hands. Ca(2+) stores are refilled through a process called store-operated Ca(2+) entry (SOCE). Upon Ca(2+)-store depletion, wild-type STIM1 oligomerizes and thereby triggers extracellular Ca(2+) entry. In contrast, the missense mutations found in our four TAM-affected families induced constitutive STIM1 clustering, indicating that Ca(2+) sensing was impaired. By monitoring the calcium response of TAM myoblasts to SOCE, we found a significantly higher basal Ca(2+) level in TAM cells and a dysregulation of intracellular Ca(2+) homeostasis. Because recessive STIM1 loss-of-function mutations were associated with immunodeficiency, we conclude that the tissue-specific impact of STIM1 loss or constitutive activation is different and that a tight regulation of STIM1-dependent SOCE is fundamental for normal skeletal-muscle structure and function., (Copyright © 2013 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published
2013
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26. Impact of 6-hour sepsis resuscitation bundle compliance on hospital mortality in a saudi hospital.

Author

Memon JI, Rehmani RS, Alaithan AM, El Gammal A, Lone TM, Ghorab K, and Abdulbasir A

Abstract

Purpose. To assess the effect of improved compliance with 6-hour sepsis resuscitation bundle on mortality in patients with severe sepsis and septic shock. Materials and Methods. A quasi-experimental prospective study was conducted at a 10-bedded combined medical and surgical intensive care unit. The historical group included all consecutive patients with severe sepsis and septic shock admitted from January 2008 to March 2009. Intervention included evidence-based written sepsis pathway, antibiotic recommendations, and an educational program.The post-intervention group included all consecutive patients admitted from July 2009 to June 2011. The primary outcome measures were the overall compliance to seven 6-hour sepsis resuscitation bundle elements and 30-day hospital mortality. There were 99 patients in the historical group and 199 in the post-intervention group. Results. The baseline patients' characteristics were similar. Overall compliance to all seven sepsis resuscitation bundle elements in historical group was 5.1% [95% confidence interval (CI), 2.1-11.3] which improved after intervention to 23.6% (95% CI, 17.9-30.1); P < 0.001. The overall compliance to 6-hour sepsis resuscitation bundle elements was associated with improved survival [odds ratio (OR), 5.8 (95% CI, 2.2-15.1; P < 0.001)]. 30-day hospital mortality reduced from 31.3% in the historical group to 21.1% in the intervention group; P = 0.05. Conclusion. Improvement in compliance to 6-hour sepsis resuscitation bundle was associated with a reduction in 30-day hospital mortality.

Published
2012
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27. [Small fibre neuropathy in primary Sjögren syndrome].

Author

Fauchais AL, Richard L, Gondran G, Ghorab K, Palat S, Bezanahary H, Loustaud-Ratti V, Ly K, Jauberteau MO, Vallat JM, Vidal E, and Magy L

Subjects
Chronic Disease, Female, Humans, Middle Aged, Neuralgia etiology, Neuralgia pathology, Sjogren's Syndrome complications
Abstract

Purpose: About forty percent of the patients with primary Sjögren's syndrome (pSS) experience chronic neuropathic pain with normal electrodiagnostic studies. Two previous studies suggest that chronic neuropathic pain in pSS is due to small fiber neuropathy (SFN). Quantification of epidermal nerve fiber density after skin biopsy has been validated to diagnose small fiber neuropathy., Methods: Skin biopsy was performed in 14 consecutive pSS patients (satisfying the american-european classification criteria) with chronic neuropathic pain and normal electrodiagnostic studies suggesting SFN., Results: Fourteen female pSS patients exhibited chronic neuropathic pain [burning sensation (n=14), prickling (n=4), dysesthesia (n=8)] with paroxystic exacerbations (n=10) and allodynia (n=13), for a mean period of 18.4±12.4 months. Neuropathic pain involved mostly hands and feet (n=13), with a distal (n=9) and leg (n=4) predominant distribution. Neurological examination disclosed normal deep tendon responses and absence of motor weakness (n=14). Small fiber neuropathy was confirmed by skin biopsy in 13 cases. Epidermal nerve fiber density was decreased in distal [(n=12), mean 3.5±1.7 fibers/mm (N>6.9)] and proximal site of biopsy [(n=9), mean 7.04±2.63 fibers/mm (N>9.3)]., Conclusion: Small fiber neuropathy is commonly responsible of chronic neuropathic pain in pSS. Prevalence, physiopathology and neurological evolution of such neuropathies still remain unknown., (Copyright © 2010 Société nationale française de médecine interne (SNFMI). Published by Elsevier SAS. All rights reserved.)

Published
2011
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28. Genotype-phenotype correlations in Charcot-Marie-Tooth disease type 2 caused by mitofusin 2 mutations.

Author

Calvo J, Funalot B, Ouvrier RA, Lazaro L, Toutain A, De Mas P, Bouche P, Gilbert-Dussardier B, Arne-Bes MC, Carrière JP, Journel H, Minot-Myhie MC, Guillou C, Ghorab K, Magy L, Sturtz F, Vallat JM, and Magdelaine C

Subjects
Adolescent, Adult, Aged, Charcot-Marie-Tooth Disease classification, Child, Child, Preschool, Female, GTP Phosphohydrolases, Genes, Dominant, Genes, Recessive, Genetic Markers genetics, Genotype, Humans, Male, Middle Aged, Severity of Illness Index, Young Adult, Charcot-Marie-Tooth Disease genetics, Charcot-Marie-Tooth Disease pathology, Membrane Proteins genetics, Mitochondrial Proteins genetics, Mutation, Missense genetics, Phenotype
Abstract

Background: Mutations in the gene encoding mitofusin 2 (MFN2) cause Charcot-Marie-Tooth disease type 2 (CMT2), with heterogeneity concerning severity and associated clinical features., Objective: To describe MFN2 mutations and associated phenotypes in patients with hereditary motor and sensory neuropathy (HMSN)., Design: Direct sequencing of the MFN2 gene and clinical investigations of patients with MFN2 mutations., Setting: Molecular genetics laboratory of a university hospital and the Limoges National Referral Center for Rare Peripheral Neuropathies., Patients: One hundred fifty index patients with HMSN and a median motor nerve conduction velocity of 25 m/s or greater and without mutations in the genes encoding connexin 32 and myelin protein zero., Main Outcome Measures: Results of genetic analyses and phenotypic observations., Results: Twenty different missense mutations were identified in 20 index patients. Mutation frequency was 19 of 107 (17.8%) in patients with CMT2 and 1 of 43 (2.3%) in patients with a median motor nerve conduction velocity less than 38 m/s. Four patients had proven de novo mutations, 8 families had autosomal dominant inheritance, and 3 had autosomal recessive inheritance. The remaining 5 patients were sporadic cases with heterozygous mutations. Phenotypes varied from mild forms to early-onset severe forms. Additional features were encountered in 8 patients (32%). Six patients underwent sural nerve biopsy: electronic microscopy showed prominent mitochondrial abnormalities on longitudinal sections., Conclusions: MFN2 mutations are a frequent cause of CMT2, with variable severity and either dominant or recessive inheritance. MFN2 gene testing must be a first-line analysis in axonal HMSN irrespective of the mode of inheritance or the severity of the peripheral neuropathy.

Published
2009
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29. [Hereditary neuropathies].

Author

Vallat JM, Calvo J, Ghorab K, and Tazir M

Subjects
Amyloid Neuropathies, Familial diagnosis, Axons physiology, Charcot-Marie-Tooth Disease classification, Charcot-Marie-Tooth Disease diagnosis, Chromosomes, Human, X genetics, Demyelinating Diseases genetics, Fabry Disease diagnosis, Genes, Dominant genetics, Genes, Recessive genetics, Humans, Porphyrias diagnosis, Hereditary Sensory and Motor Neuropathy diagnosis
Abstract

Although there are many human hereditary neuropathies, most of them with the exception of Charcot-Marie-Tooth disease or hereditary sensorimotor neuropathy, are rare. Irrespective of their type, the mode of transmission may be autosomal dominant or recessive, or X-linked. The most difficult to diagnose, however, are the sporadic forms. It is customary to distinguish the cases in which the neuropathy is the sole clinical expression from multisystemic diseases where neuropathy is one component of multi-organ involvement. The complexity and the multiplicity of genes involved and the lack of understanding of their exact functions hinder logical presentation of these hereditary neuropathies. For understandable technical reasons, the stage of specific treatment, namely the repair of the mutated gene, has yet to be attained.

Published
2008

30. Intranervous immunoglobulin deposits: an underestimated mechanism of neuropathy.

Author

Vallat JM, Magy L, Richard L, Piaser M, Sindou P, Calvo J, Ghorab K, and Cros D

Subjects
Adult, Aged, Biopsy, Cell Count, Cryoglobulins metabolism, Electrodiagnosis, Electrophysiology, Female, Fluorescent Antibody Technique, Humans, Male, Microscopy, Immunoelectron, Middle Aged, Motor Neurons metabolism, Motor Neurons pathology, Nerve Fibers, Myelinated pathology, Neural Conduction physiology, Neurons, Afferent metabolism, Neurons, Afferent pathology, Paraproteinemias metabolism, Paraproteinemias pathology, Immunoglobulins metabolism, Nerve Tissue metabolism, Nerve Tissue pathology, Polyneuropathies metabolism, Polyneuropathies pathology
Abstract

There are several pathogenic mechanisms of peripheral nerve involvement in patients with monoclonal dysglobulinemia. Intranervous proliferation of malignant cells, immunoglobulin, or amyloid deposits in the endoneurial space can only be determined by examination of nerve biopsy specimens. We present clinical, electrophysiological, and histological data from seven patients whose polyneuropathy was induced by immunoglobulin deposits in the endoneurial space. As these lesions cannot be demonstrated on clinical and electrophysiological grounds, the indication for nerve biopsy derives from careful analysis of each patient presenting with a polyneuropathy and a monoclonal dysglobulinemia. To visualize and clearly characterize these deposits, electron microscopic examination is indispensable. Immunocytochemical methods using both light and electron microscopy for ultrastructural analysis are of great value. Demonstration of endoneurial immunoglobulin deposits may have major therapeutic consequences. Indeed, identification of these deposits prompted the use of aggressive treatment, which was quite effective in five of our seven patients., ((c) 2008 Wiley Periodicals, Inc.)

Published
2008
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31. Carotid angioplasty stenting revisited: clinical and radiological (MRI) outcome.

Author

Ghorab K, Macian F, Adoukounou T, Magy L, Chapot R, and Vallat JM

Subjects
Aged, Aged, 80 and over, Carotid Stenosis diagnosis, Carotid Stenosis etiology, Cohort Studies, Contraindications, Diffusion Magnetic Resonance Imaging, Endarterectomy, Carotid, Female, Humans, Male, Middle Aged, Risk Factors, Treatment Outcome, Angioplasty, Carotid Stenosis therapy, Stents
Abstract

Background: Although carotid angioplasty and stenting (CAS) is widely used to treat carotid stenosis, recent studies point to the inferiority of the procedure compared with carotid endarterectomy., Methods: We present 50 consecutive cases of CAS treated in our unit. Endarterectomy was contraindicated in these patients due to high operative risk. All the patients underwent a diffusion-weighted MRI (DWI) before and after the procedure and had a neurological assessment in a stroke unit., Results: No deaths were recorded until 30 days after the procedure. Six patients [12%, confidence interval at 95% (CI(95)) = 3.7-20.2] had a positive DWI MRI after the procedure but only 2 (4%, CI(95) = 0-9.43) had a worse neurological status., Conclusion: This study shows that CAS is feasible with a low morbid-mortality rate in patients with a high surgical risk. DWI is highly sensitive to detect neurological complications after the procedure., ((c) 2007 S. Karger AG, Basel.)

Published
2008
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