Your search keyword '"Maselli RA"' showing total 79 results

1. Mutations in LAMB2 causing a severe form of synaptic congenital myasthenic syndrome

Author

Maselli, RA, Ng, JJ, Anderson, JA, Cagney, O, Arredondo, J, Williams, C, Wessel, HB, Abdel-Hamid, H, and Wollmann, RL

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Rare Diseases, Neurosciences, Pediatric, Clinical Research, Genetics, Aetiology, 2.1 Biological and endogenous factors, DNA Mutational Analysis, Eye Diseases, Hereditary, Female, Humans, Laminin, Mutation, Myasthenic Syndromes, Congenital, Neuromuscular Junction, Young Adult, Biological Sciences, Medical and Health Sciences, Genetics & Heredity, Clinical sciences

Abstract

BackgroundWe describe a severe form of congenital myasthenic syndrome (CMS) associated with congenital nephrosis and ocular malformations caused by two truncating mutations in the gene encoding the laminin beta2 subunit (LAMB2).Methods and resultsMutational analysis in the affected patient, who has a history of a serious untoward reaction to treatment with acetylcholinesterase inhibition, revealed two frame-shifting heteroallelic mutations, a maternally inherited 1478delG and a paternally inherited 4804delC. An anconeus muscle biopsy demonstrated a profound distortion of the architecture and function of the neuromuscular junction, which was strikingly similar to that seen in mice lacking laminin beta2 subunit. The findings included: pronounced reduction of the axon terminal size with encasement of the nerve endings by Schwann cells, severe widening of the primary synaptic cleft and invasion of the synaptic space by the processes of Schwann cells, and moderate simplification of postsynaptic folds and intact expression of the endplate acetylcholinesterase. The endplate potential quantal content was notably reduced, while the frequencies and amplitudes of miniature endplate potentials were only moderately diminished and the decay phases of miniature endplate potentials were normal. Western blot analysis of muscle and kidney tissue and immunohistochemistry of kidney tissue showed no laminin beta2 expression.ConclusionThis case, which represents a new type of synaptic CMS, exemplifies the wide variability of phenotypes associated with LAMB2 mutations and underscores the fundamental role that laminin beta2 plays in the development of the human neuromuscular junction.

Published

2009

2. Congenital myasthenic syndrome associated with epidermolysis bullosa caused by homozygous mutations in PLEC1 and CHRNE

Author

Maselli, RA, Arredondo, J, Cagney, O, Mozaffar, T, Skinner, S, Yousif, S, Davis, RR, Gregg, JP, Sivak, M, Konia, TH, Thomas, K, and Wollmann, RL

Published

2011

3. Congenital myasthenic syndrome associated with epidermolysis bullosa caused by homozygous mutations in PLEC1 and CHRNE

Author

Maselli, RA, primary, Arredondo, J, additional, Cagney, O, additional, Mozaffar, T, additional, Skinner, S, additional, Yousif, S, additional, Davis, RR, additional, Gregg, JP, additional, Sivak, M, additional, Konia, TH, additional, Thomas, K, additional, and Wollmann, RL, additional

Published

2010

4. Congenital myasthenic syndrome caused by two non‐N88K rapsyn mutations

Author

Maselli, RA, primary, Dris, H, additional, Schnier, J, additional, Cockrell, JL, additional, and Wollmann, RL, additional

Published

2007

5. Missense variants in CMS22 patients reveal that PREPL has both enzymatic and nonenzymatic functions.

Author

Monnens Y, Theodoropoulou A, Rosier K, Bhalla K, Mahy A, Vanhoutte R, Meulemans S, Cavani E, Antanasijevic A, Lemmens I, Lee JA, Spellicy CJ, Schroer RJ, Maselli RA, Laverty CG, Agostinis P, Pagliarini DJ, Verhelst S, Marcaida MJ, Rochtus A, Dal Peraro M, and Creemers JW

Subjects

Female, Humans, Male, Mitochondria metabolism, Mitochondria genetics, Phenotype, Serine Endopeptidases genetics, Serine Endopeptidases metabolism, Mutation, Missense, Myasthenic Syndromes, Congenital genetics, Myasthenic Syndromes, Congenital metabolism, Prolyl Oligopeptidases metabolism

Abstract

Congenital myasthenic syndrome-22 (CMS22, OMIM 616224) is a rare genetic disorder caused by deleterious genetic variation in the prolyl endopeptidase-like (PREPL) gene. Previous reports have described patients with deletions and nonsense variants in PREPL, but nothing is known about the effect of missense variants in the pathology of CMS22. In this study, we have functionally characterized missense variants in PREPL from 3 patients with CMS22, all with hallmark phenotypes. Biochemical evaluation revealed that these missense variants do not impair hydrolase activity, thereby challenging the conventional diagnostic criteria and disease mechanism. Structural analysis showed that the variants affect regions most likely involved in intraprotein or protein-protein interactions. Indeed, binding to a selected group of known interactors was differentially reduced for the 3 variants. The importance of nonhydrolytic functions of PREPL was investigated in catalytically inactive PREPL p.Ser559Ala cell lines, which showed that hydrolytic activity of PREPL is needed for normal mitochondrial function but not for regulating AP1-mediated transport in the transgolgi network. In conclusion, these studies showed that CMS22 can be caused not only by deletion and truncation of PREPL but also by missense variants that do not necessarily result in a loss of hydrolytic activity of PREPL.

Published

2024

6. Congenital myasthenic syndrome secondary to pathogenic variants in the SLC5A7 gene: report of two cases.

Author

Muntadas JA, Hyland MR, Martínez MDRO, Young JN, Chong JX, Bamshad MJ, and Maselli RA

Subjects

Humans, Male, Mutation, Symporters genetics, Child, Child, Preschool, Myasthenic Syndromes, Congenital genetics

Abstract

Background: Congenital Myasthenic Syndromes (CMS) are rare genetic diseases, which share as a common denominator muscle fatigability due to failure of neuromuscular transmission. A distinctive clinical feature of presynaptic CMS variants caused by defects of the synthesis of acetylcholine is the association with life-threatening episodes of apnea. One of these variants is caused by mutations in the SLC5A7 gene, which encodes the sodium-dependent HC-3 high-affinity choline transporter 1 (CHT1). To our knowledge there are no published cases of this CMS type in Latin America., Case Presentation: We present two cases of CHT1-CMS. Both patients were males presenting with repeated episodes of apnea, hypotonia, weakness, ptosis, mild ophthalmoparesis, and bulbar deficit. The first case also presented one isolated seizure, while the second case showed global developmental delay. Both cases, exhibited incomplete improvement with treatment with pyridostigmine., Conclusions: This report emphasizes the broad incidence of CMS with episodic apnea caused by mutations in the SLC5A7 gene and the frequent association of this condition with serious manifestations of central nervous system involvement., (© 2024. The Author(s).)

Published

2024

7. Adeno-Associated Virus Type 9-Mediated Gene Therapy of Choline Acetyltransferase-Deficient Mice.

Author

Lin CV, Thomas CAD, Huynh TL, Wei DT, Young JN, Aivazian AS, McInnes A, Xu J, Cook SE, Vazquez J, and Maselli RA

Subjects

Mice, Humans, Animals, Tissue Distribution, Mice, Knockout, Genetic Therapy, Choline O-Acetyltransferase genetics, Choline O-Acetyltransferase metabolism, Dependovirus genetics, Dependovirus metabolism

Abstract

The enzyme choline acetyltransferase (ChAT) synthesizes acetylcholine from acetyl-CoA and choline at the neuromuscular junction and at the nerve terminals of cholinergic neurons. Mutations in the ChAT gene ( CHAT ) result in a presynaptic congenital myasthenic syndrome (CMS) that often associates with life-threatening episodes of apnea. Knockout mice for Chat (Chat -/- ) die at birth. To circumvent the lethality of this model, we crossed mutant mice possessing loxP sites flanking Chat exons 4 and 5 with mice that expressed Cre-ER T2 . Injection of tamoxifen (Tx) at postnatal (P) day 11 in these mice induced downregulation of Chat , autonomic failure, weakness, and death. However, a proportion of Chat flox/flox -Cre-ER T2 mice receiving at birth an intracerebroventricular injection of 2 × 10 13 vg/kg adeno-associated virus type 9 (AAV9) carrying human CHAT (AAV9- CHAT ) survived a subsequent Tx injection and lived to adulthood without showing signs of weakness. Likewise, injection of AA9- CHAT by intracisternal injection at P28 after the onset of weakness also resulted in survival to adulthood. The expression of Chat in spinal motor neurons of Chat flox/flox -Cre-ER T2 mice injected with Tx was markedly reduced, but AAV-injected mice showed a robust recovery of ChAT expression, which was mainly translated by the human CHAT RNA. The biodistribution of the viral genome was widespread but maximal in the spinal cord and brain of AAV-injected mice. No significant histopathological changes were observed in the brain, liver, and heart of AAV-injected mice after 1 year follow-up. Thus, AAV9-mediated gene therapy may provide an effective and safe treatment for patients severely affected with CHAT- CMS.

Published

2024

8. Intravenous immunoglobulin is safe and effective in controlling pre-existing paraneoplastic neuromuscular diseases in cancer patients treated with immune checkpoint inhibitors: two case reports and literature review.

Author

Xiong G, Young RB, Chow H, Maverakis E, Maselli RA, Richman DP, and Li T

Abstract

Immune checkpoint inhibitors cause rare but potentially fatal neuromuscular complications, leading to a concern to use these agents in cancer patients with pre-existing autoimmune or inflammatory neuromuscular diseases. We report two such patients with paraneoplastic dermatomyositis and "seronegative" paraneoplastic demyelinating neuropathy, respectively, who have been successfully treated with immune checkpoint inhibitor monotherapy as well as maintenance intravenous immunoglobulin. While controlling the paraneoplastic or autoimmune neuromuscular diseases, the use of intravenous immunoglobulin did not compromise the anti-cancer effect of immune checkpoint inhibitor., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Xiong, Young, Chow, Maverakis, Maselli, Richman and Li.)

Published

2023

9. Atypical Case of POEMS Presented as Demyelinating Polyneuropathy With Motor Conduction Block.

Author

Guo SY, Duffy AO, Maselli RA, and Xiong G

Subjects

Humans, Neural Conduction, POEMS Syndrome complications, POEMS Syndrome diagnosis, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating complications, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating diagnosis

Abstract

Competing Interests: The authors report no conflicts of interest.

Published

2021

10. Dominant and recessive congenital myasthenic syndromes caused by SYT2 mutations.

Author

Maselli RA, Wei DT, Hodgson TS, Sampson JB, Vazquez J, Smith HL, Pytel P, and Ferns M

Subjects

Adult, Child, Preschool, Female, Humans, Lambert-Eaton Myasthenic Syndrome genetics, Lambert-Eaton Myasthenic Syndrome physiopathology, Male, Muscle Weakness genetics, Muscle Weakness physiopathology, Myasthenic Syndromes, Congenital diagnosis, Neuromuscular Junction physiopathology, Mutation genetics, Myasthenic Syndromes, Congenital genetics, Neuromuscular Junction genetics, Synaptotagmin II genetics

Abstract

Introduction/aims: We studied a patient with a congenital myasthenic syndrome (CMS) caused by a dominant mutation in the synaptotagmin 2 gene (SYT2) and compared the clinical features of this patient with those of a previously described patient with a recessive mutation in the same gene., Methods: We performed electrodiagnostic (EDX) studies, genetic studies, muscle biopsy, microelectrode recordings and electron microscopy (EM)., Results: Both patients presented with muscle weakness and bulbar deficits, which were worse in the recessive form. EDX studies showed presynaptic failure, which was more prominent in the recessive form. Microelectrode studies in the dominant form showed a marked reduction of the quantal content, which increased linearly with higher frequencies of nerve stimulation. The MEPP frequencies were normal at rest but increased markedly with higher frequencies of nerve stimulation. The EM demonstrated overdeveloped postsynaptic folding, and abundant endosomes, multivesicular bodies and degenerative lamellar bodies inside small nerve terminals., Discussion: The recessive form of CMS caused by a SYT2 mutation showed far more severe clinical manifestations than the dominant form. The pathogenesis of the dominant form likely involves a dominant-negative effect due to disruption of the dual function of synaptotagmin as a Ca 2+ -sensor and modulator of synaptic vesicle exocytosis., (© 2021 Wiley Periodicals LLC.)

Published

2021

11. Recessive congenital myasthenic syndrome caused by a homozygous mutation in SYT2 altering a highly conserved C-terminal amino acid sequence.

Author

Maselli RA, van der Linden H Jr, and Ferns M

Subjects

Amino Acid Sequence genetics, Child, Preschool, Female, Genes, Recessive genetics, Humans, Mutation, Myasthenic Syndromes, Congenital pathology, Genetic Predisposition to Disease, Myasthenic Syndromes, Congenital genetics, Synaptotagmin II genetics

Abstract

Defects in the gene encoding synaptotagmin 2 (SYT2) have been linked to a presynaptic congenital myasthenic syndrome (CMS) and motor neuropathies. However, to date only dominant forms of the disease have been described. We report here a consanguineous patient with a severe recessive form of presynaptic CMS and denervation atrophy caused by the homozygous mutation c.1191delG, p.Arg397Serfs*37 in SYT2. The affected 2-year-old girl had profound weakness and areflexia with moderate bulbar deficit. Repetitive nerve stimulation revealed an extreme reduction of compound muscle action potential amplitudes at rest, with a striking facilitation followed by a progressive decline at fast stimulation rates. These findings were reminiscent, but not identical to those seen in the Lambert-Eaton myasthenic syndrome. 3,4 diaminopyridine and pyridostigmine were effective to ameliorate muscle fatigue, but albuterol was ineffective. Modeling of the mutation using the rat Syt1 C2B x-ray structure revealed that Arg397Serfs*37 disrupts a highly conserved amino acid sequence at the bottom face of the C2B domain not directly involved in calcium binding, but crucial for synaptotagmin-SNARE interaction and exocytosis. Thus, this report describes a recessive form of synaptotagmin 2-CMS and highlights the importance of the synaptotagmin C-terminal on synaptic vesicle fusion and exocytosis., (© 2020 Wiley Periodicals, Inc.)

Published

2020

12. Phenotypic Differences in 2 Unrelated Cases Carrying Identical DOK7 Mutations.

Author

Bissay V and Maselli RA

Subjects

Adult, Humans, Male, Myasthenic Syndromes, Congenital genetics, Phenotype, Muscle Proteins genetics, Myasthenic Syndromes, Congenital physiopathology

Abstract

Introduction: Mutations in the Dok-7 gene (DOK7) underlie a congenital myasthenic syndrome (CMS) with a characteristic limb-girdle (LG) pattern of muscle weakness. Multiple clinical findings and a wide clinical heterogeneity have been identified in this form of CMS., Methods: We describe here 2 unrelated adult patients who presented with a LG CMS, caused by 2 compound heterozygous pathogenic sequence variants in DOK7: c.1124_1127dupTGCC (P.Ala378Serfs*30) and c.480C> A (p.Tyr160*)., Results: Although both patients presented with severe proximal weakness consistent with LG myasthenia, one of the patients presented with additional distal muscle involvement in the lower extremities. By contrast, the other patient had severe bulbar and respiratory deficit requiring gastric tube feeding and mechanical ventilatory support for most parts of the day., Discussion: These 2 cases illustrate the lack of phenotype-genotype correlation and the absence of geographic, genetic, and ethnic association in cases of LG CMS caused by DOK7 mutations.

Published

2019

13. Pathogenic effects of agrin V1727F mutation are isoform specific and decrease its expression and affinity for HSPGs and LRP4.

Author

Rudell JB, Maselli RA, Yarov-Yarovoy V, and Ferns MJ

Subjects

Agrin chemistry, Alleles, Alternative Splicing, Cell Line, Heparan Sulfate Proteoglycans chemistry, Humans, Immunohistochemistry, LDL-Receptor Related Proteins chemistry, Models, Biological, Models, Molecular, Protein Binding, Protein Conformation, Protein Isoforms, Structure-Activity Relationship, Agrin genetics, Agrin metabolism, Amino Acid Substitution, Gene Expression Regulation, Heparan Sulfate Proteoglycans metabolism, LDL-Receptor Related Proteins metabolism, Mutation

Abstract

Agrin is a large extracellular matrix protein whose isoforms differ in their tissue distribution and function. Motoneuron-derived y+z+ agrin regulates the formation of the neuromuscular junction (NMJ), while y-z- agrin is widely expressed and has diverse functions. Previously we identified a missense mutation (V1727F) in the second laminin globular (LG2) domain of agrin that causes severe congenital myasthenic syndrome. Here, we define pathogenic effects of the agrin V1727F mutation that account for the profound dysfunction of the NMJ. First, by expressing agrin variants in heterologous cells, we show that the V1727F mutation reduces the secretion of y+z+ agrin compared to wild type, whereas it has no effect on the secretion of y-z- agrin. Second, we find that the V1727F mutation significantly impairs binding of y+z+ agrin to both heparin and the low-density lipoprotein receptor-related protein 4 (LRP4) coreceptor. Third, molecular modeling of the LG2 domain suggests that the V1727F mutation primarily disrupts the y splice insert, and consistent with this we find that it partially occludes the contribution of the y splice insert to agrin binding to heparin and LRP4. Together, these findings identify several pathogenic effects of the V1727F mutation that reduce its expression and ability to bind heparan sulfate proteoglycan and LRP4 coreceptors involved in the muscle-specific kinase signaling pathway. These defects primarily impair the function of neural y+z+ agrin and combine to cause a severe CMS phenotype, whereas y-z- agrin function in other tissues appears preserved., (© The Author(s) 2019. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2019

14. Presynaptic congenital myasthenic syndrome with altered synaptic vesicle homeostasis linked to compound heterozygous sequence variants in RPH3A.

Author

Maselli RA, Vázquez J, Schrumpf L, Arredondo J, Lara M, Strober JB, Pytel P, Wollmann RL, and Ferns M

Subjects

Adaptor Proteins, Signal Transducing physiology, Child, Female, Heterozygote, Homeostasis, Humans, Microscopy, Electron, Nerve Tissue Proteins physiology, Synaptic Transmission genetics, Synaptic Vesicles genetics, Synaptic Vesicles metabolism, Vesicular Transport Proteins physiology, Rabphilin-3A, Adaptor Proteins, Signal Transducing genetics, Myasthenic Syndromes, Congenital genetics, Myasthenic Syndromes, Congenital metabolism, Nerve Tissue Proteins genetics, Vesicular Transport Proteins genetics

Abstract

Background: Monogenic defects of synaptic vesicle (SV) homeostasis have been implicated in many neurologic diseases, including autism, epilepsy, and movement disorders. In addition, abnormal vesicle exocytosis has been associated with several endocrine dysfunctions., Methods: We report an 11 year old girl with learning disabilities, tremors, ataxia, transient hyperglycemia, and muscle fatigability responsive to albuterol sulfate. Failure of neuromuscular transmission was confirmed by single fiber electromyography. Electron microscopy of motor nerve terminals revealed marked reduction in SV density, double-membrane-bound sacs containing SVs, abundant endosomes, and degenerative lamellar bodies. The patient underwent whole exome sequencing (WES) and relevant sequence variants were expressed and studied in a mammalian cell line., Results: Chromosomal microarray studies and next generation sequencing (NGS) of mitochondrial DNA were unrevealing; however, NGS of genomic DNA showed two rare sequence variants in the gene encoding rabphilin 3a (RPH3A). The paternally inherited variant c.806 G>A (p.Arg269Gln) involves a substitution of a conserved residue in the linker region, while the maternally inherited variant c.1390 G>T (p.Val464Leu) involves a conserved amino acid substitution in the highly conserved C2A region. Expression studies revealed that p.Arg269Gln strongly impairs the binding of rabphilin 3a to 14-3-3, which is a proposed regulator of synaptic transmission and plasticity. In contrast, the binding of rabphilin 3a to 14-3-3 is only marginally impaired by p.Val464Leu; thus, the pathogenic role of p.Val464Leu remains unclear., Conclusion: In summary, we report a patient with a multisystem neurologic disorder and altered SV regulation attributed to defects in RPH3A, which grants further studies of this gene in human disorders of synaptic transmission., (© 2018 The Authors. Molecular Genetics & Genomic Medicine published by Wiley Periodicals, Inc.)

Published

2018

15. A presynaptic congenital myasthenic syndrome attributed to a homozygous sequence variant in LAMA5.

Author

Maselli RA, Arredondo J, Vázquez J, Chong JX, Bamshad MJ, Nickerson DA, Lara M, Ng F, Lo VL, Pytel P, and McDonald CM

Subjects

Adult, Female, Humans, Motor Endplate physiology, Lambert-Eaton Myasthenic Syndrome genetics, Lambert-Eaton Myasthenic Syndrome pathology, Laminin genetics, Myasthenic Syndromes, Congenital genetics, Myasthenic Syndromes, Congenital pathology, Synaptic Transmission physiology

Abstract

We report a severe defect of neuromuscular transmission in a consanguineous patient with a homozygous variant in the laminin α5 subunit gene (LAMA5). The variant c.8046C > T (p.Arg2659Trp) is rare and has a predicted deleterious effect. The affected individual, who also carries a rare homozygous sequence variant in LAMA1, had normal cognitive function, but magnetic resonance brain imaging showed mild volume loss and periventricular T2 prolongation. Repetitive nerve stimulation at 2 Hz showed 50% decrement of compound muscle action potential amplitudes but 250% facilitation immediately after exercise, similar to that seen in Lambert-Eaton myasthenic syndrome. Endplate studies demonstrated a profound reduction of the endplate potential quantal content but normal amplitudes of miniature endplate potentials. Electron microscopy showed endplates with increased postsynaptic folding that were denuded or only partially occupied by small nerve terminals. Expression studies revealed that p.Arg2659Trp caused decreased binding of laminin α5 to SV2A and impaired laminin-521 cell adhesion and cell projection support in primary neuronal cultures. In summary, this report describing severe neuromuscular transmission failure in a patient with a LAMA5 mutation expands the list of phenotypes associated with defects in genes encoding α-laminins., (© 2018 New York Academy of Sciences.)

Published

2018

16. Congenital Myasthenic Syndrome due to DOK7 mutations in a family from Chile.

Author

Bevilacqua JA, Lara M, Díaz J, Campero M, Vázquez J, and Maselli RA

Abstract

Congenital myasthenic syndromes (CMS) are neuromuscular transmission disorders caused by mutations in genes encoding neuromuscular junction proteins. A 61-year-old female and her older sister showed bilateral ptosis, facial and proximal limb weakness, and scoliosis since childhood. Another female sibling had milder signs, while other family members were asymptomatic. Facial nerve repetitive stimulation in the proband showed decrement of muscle responses. Single fiber EMG revealed increased jitter and blocking. Muscle biopsy showed type 2-fiber atrophy, without tubular aggregates. Mutational analysis in the three affected siblings revealed two compound heterozygous mutations in DOK7 : c.1457delC, that predicts p.Pro486Argfs*13 and truncates the protein C-terminal domain, and c.473G>A, that predicts p.Arg158Gln and disruption of the dok7-MuSK interaction in the phosphotyrosine binding (PTB) domain. Unaffected family members carried only one or neither mutation., Discussion: Two of the affected sisters showed marked improvement with salbutamol treatment, which illustrates the benefits of a correct diagnosis and treatment of DOK7-CMS., (This article is distributed under the terms of the Creative Commons Attribution Noncommercial License (by-nc 4.0) which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and source are credited.)

Published

2017

17. Presynaptic congenital myasthenic syndrome with a homozygous sequence variant in LAMA5 combines myopia, facial tics, and failure of neuromuscular transmission.

Author

Maselli RA, Arredondo J, Vázquez J, Chong JX, Bamshad MJ, Nickerson DA, Lara M, Ng F, Lo VL, Pytel P, and McDonald CM

Subjects

Adult, Face diagnostic imaging, Face physiopathology, Female, Homozygote, Humans, Myasthenic Syndromes, Congenital complications, Myasthenic Syndromes, Congenital diagnostic imaging, Myasthenic Syndromes, Congenital physiopathology, Myopia complications, Myopia diagnostic imaging, Myopia genetics, Myopia physiopathology, Neuromuscular Junction Diseases complications, Neuromuscular Junction Diseases diagnostic imaging, Neuromuscular Junction Diseases physiopathology, Tics complications, Tics diagnostic imaging, Tics genetics, Tics physiopathology, Young Adult, Laminin genetics, Myasthenic Syndromes, Congenital genetics, Neuromuscular Junction Diseases genetics

Abstract

Defects in genes encoding the isoforms of the laminin alpha subunit have been linked to various phenotypic manifestations, including brain malformations, muscular dystrophy, ocular defects, cardiomyopathy, and skin abnormalities. We report here a severe defect of neuromuscular transmission in a consanguineous patient with a homozygous variant in the laminin alpha-5 subunit gene (LAMA5). The variant c.8046C>T (p.Arg2659Trp) is rare and has a predicted deleterious effect. The affected individual, who also carries a rare homozygous sequence variant in LAMA1, had muscle weakness, myopia, and facial tics. Magnetic resonance imaging of brain showed mild volume loss and periventricular T2 prolongation. Repetitive nerve stimulation revealed 50% decrement of compound muscle action potential amplitudes and 250% facilitation immediately after exercise, Endplate studies identified a profound reduction of the endplate potential quantal content and endplates with normal postsynaptic folding that were denuded or partially occupied by small nerve terminals. Expression studies revealed that p.Arg2659Trp caused decreased binding of laminin alpha-5 to SV2A and impaired laminin-521 cell-adhesion and cell projection support in primary neuronal cultures. In summary, this report describing severe neuromuscular transmission failure in a patient with a LAMA5 mutation expands the list of phenotypes associated with defects in genes encoding alpha-laminins., (© 2017 Wiley Periodicals, Inc.)

Published

2017

18. Effect of 3,4-diaminopyridine at the murine neuromuscular junction.

Author

Ng F, Lee DC, Schrumpf LA, Mazurek ME, Lee Lo V, Gill SK, and Maselli RA

Subjects

4-Aminopyridine pharmacology, Acetamides pharmacology, Amifampridine, Animals, Calcium metabolism, Dose-Response Relationship, Drug, Female, In Vitro Techniques, Membrane Potentials drug effects, Mice, Mice, Inbred C57BL, Synaptic Transmission drug effects, 4-Aminopyridine analogs & derivatives, Diaphragm drug effects, Neuromuscular Junction drug effects, Potassium Channel Blockers pharmacology

Abstract

Introduction: We investigated the effects of 3,4-diaminopyridine (3,4-DAP) and its acetylated metabolite, N-(4-amino-pyridin-3-yl) acetamide (3-Ac), at the mammalian neuromuscular junction., Methods: Quantal release of acetylcholine was studied in diaphragm muscles of mice, using in vitro intracellular microelectrode recordings., Results: Under conditions of low probability of release, 3,4-DAP produced a 1,000% increase in quantal release, but 3-Ac had no effect. Under conditions of normal probability of release, the effect of 3,4-DAP was modest and limited by concurrent depletion of synaptic vesicles, especially with high concentrations of 3,4-DAP and high frequencies of nerve stimulation., Conclusions: These findings predict 3,4-DAP is most effective in conditions with low probability of quantal release, such as Lambert-Eaton myasthenic syndrome. A beneficial effect is also expected in disorders of neuromuscular transmission in which the effect of 3,4-DAP on quantal release is not limited by depletion of synaptic vesicles, such as postsynaptic congenital myasthenic syndromes. Muscle Nerve, 2016 Muscle Nerve 55: 223-231, 2017., (© 2016 Wiley Periodicals, Inc.)

Published

2017

19. Choline Acetyltransferase Mutations Causing Congenital Myasthenic Syndrome: Molecular Findings and Genotype-Phenotype Correlations.

Author

Arredondo J, Lara M, Gospe SM Jr, Mazia CG, Vaccarezza M, Garcia-Erro M, Bowe CM, Chang CH, Mezei MM, and Maselli RA

Subjects

Adolescent, Alleles, Amino Acid Substitution, Binding Sites, Catalytic Domain, Child, Preschool, Choline O-Acetyltransferase chemistry, Choline O-Acetyltransferase metabolism, DNA Mutational Analysis, Enzyme Activation, Female, Gene Expression, Genotype, HEK293 Cells, Humans, Hydrogen Bonding, Male, Models, Molecular, Myasthenic Syndromes, Congenital diagnosis, Phosphorylation, Protein Conformation, Substrate Specificity, Choline O-Acetyltransferase genetics, Genetic Association Studies, Mutation, Myasthenic Syndromes, Congenital genetics

Abstract

Choline acetyltransferase catalyzes the synthesis of acetylcholine at cholinergic nerves. Mutations in human CHAT cause a congenital myasthenic syndrome due to impaired synthesis of ACh; this severe variant of the disease is frequently associated with unexpected episodes of potentially fatal apnea. The severity of this condition varies remarkably, and the molecular factors determining this variability are poorly understood. Furthermore, genotype-phenotype correlations have been difficult to establish in patients with biallelic mutations. We analyzed the protein expression of phosphorylated ChAT of seven CHAT mutations, p.Val136Met, p.Arg207His, p.Arg186Trp, p.Val194Leu, p.Pro211Ala, p.Arg566Cys, and p.Ser694Cys, in HEK-293 cells to phosphorylated ChAT, determined their enzyme kinetics and thermal stability, and examined their structural changes. Three mutations, p.Arg207His, p.Arg186Trp, and p.Arg566Cys, are novel, and p.Val136Met and p.Arg207His are homozygous in three families and associated with severe disease. The characterization of mutants showed a decrease in the overall catalytic efficiency of ChAT; in particular, those located near the active-site tunnel produced the most seriously disruptive phenotypic effects. On the other hand, p.Val136Met, which is located far from both active and substrate-binding sites, produced the most drastic reduction of ChAT expression. Overall, CHAT mutations producing low enzyme expression and severe kinetic effects are associated with the most severe phenotypes., (© 2015 WILEY PERIODICALS, INC.)

Published

2015

20. Axonal neuropathy in female carriers of the fragile X premutation with fragile x-associated tremor ataxia syndrome.

Author

Ram S, Devapriya IA, Fenton G, Mcvay L, Nguyen DV, Tassone F, Maselli RA, and Hagerman RJ

Subjects

Aged, Ataxia epidemiology, Cohort Studies, Female, Fragile X Syndrome epidemiology, Humans, Male, Middle Aged, Mutation genetics, Neural Conduction physiology, Peripheral Nervous System Diseases epidemiology, Tremor epidemiology, Ataxia diagnosis, Ataxia genetics, Axons pathology, Fragile X Syndrome diagnosis, Fragile X Syndrome genetics, Heterozygote, Peripheral Nervous System Diseases diagnosis, Peripheral Nervous System Diseases genetics, Tremor diagnosis, Tremor genetics

Abstract

Introduction: In this study we examined whether females with the fragile X-associated tremor ataxia syndrome (FXTAS) and non-FXTAS premutation carriers have electrophysiological signs of underlying peripheral neuropathy., Methods: Nerve conduction studies (NCS) were performed on 19 women with FXTAS, 20 non-FXTAS carriers, and 26 age-matched controls. The results were compared with existing data on corresponding male carriers., Results: Women with FXTAS and non-FXTAS carriers had reduced sensory nerve action potential amplitudes. Also, there was a strong trend for reduced compound muscle action potential amplitudes in women with FXTAS, but not in non-FXTAS carriers. No significant slowing of nerve conduction velocities, prolongation of F-wave latencies, or associations with molecular measures was observed., Conclusions: This study suggests an underlying axonal neuropathy in women with FXTAS. However, in comparison to men with FXTAS, the NCS abnormalities in women were less severe, possibly due to the effect of a normal X chromosome., (© 2014 Wiley Periodicals, Inc.)

Published

2015

21. Defective fast inactivation recovery of Nav 1.4 in congenital myasthenic syndrome.

Author

Arnold WD, Feldman DH, Ramirez S, He L, Kassar D, Quick A, Klassen TL, Lara M, Nguyen J, Kissel JT, Lossin C, and Maselli RA

Subjects

Amino Acid Sequence, Female, HEK293 Cells, Humans, Ion Channel Gating genetics, Middle Aged, Molecular Sequence Data, Myasthenic Syndromes, Congenital diagnosis, Myasthenic Syndromes, Congenital genetics, NAV1.4 Voltage-Gated Sodium Channel genetics, Recovery of Function genetics

Abstract

Objective: To describe the unique phenotype and genetic findings in a 57-year-old female with a rare form of congenital myasthenic syndrome (CMS) associated with longstanding muscle fatigability, and to investigate the underlying pathophysiology., Methods: We used whole-cell voltage clamping to compare the biophysical parameters of wild-type and Arg1457His-mutant Nav 1.4., Results: Clinical and neurophysiological evaluation revealed features consistent with CMS. Sequencing of candidate genes indicated no abnormalities. However, analysis of SCN4A, the gene encoding the skeletal muscle sodium channel Nav 1.4, revealed a homozygous mutation predicting an arginine-to-histidine substitution at position 1457 (Arg1457His), which maps to the channel's voltage sensor, specifically D4/S4. Whole-cell patch clamp studies revealed that the mutant required longer hyperpolarization to recover from fast inactivation, which produced a profound use-dependent current attenuation not seen in the wild type. The mutant channel also had a marked hyperpolarizing shift in its voltage dependence of inactivation as well as slowed inactivation kinetics., Interpretation: We conclude that Arg1457His compromises muscle fiber excitability. The mutant fast-inactivates with significantly less depolarization, and it recovers only after extended hyperpolarization. The resulting enhancement in its use dependence reduces channel availability, which explains the patient's muscle fatigability. Arg1457His offers molecular insight into a rare form of CMS precipitated by sodium channel inactivation defects. Given this channel's involvement in other muscle disorders such as paramyotonia congenita and hyperkalemic periodic paralysis, our study exemplifies how variations within the same gene can give rise to multiple distinct dysfunctions and phenotypes, revealing residues important in basic channel function., (© 2015 American Neurological Association.)

Published

2015

22. COOH-terminal collagen Q (COLQ) mutants causing human deficiency of endplate acetylcholinesterase impair the interaction of ColQ with proteins of the basal lamina.

Author

Arredondo J, Lara M, Ng F, Gochez DA, Lee DC, Logia SP, Nguyen J, and Maselli RA

Subjects

Acetylcholinesterase metabolism, Animals, Base Sequence, COS Cells, Chlorocebus aethiops, Chromatography, Liquid, Collagen metabolism, DNA Primers, HEK293 Cells, Humans, Muscle Proteins metabolism, Protein Binding, Reverse Transcriptase Polymerase Chain Reaction, Tandem Mass Spectrometry, Acetylcholinesterase genetics, Basement Membrane metabolism, Collagen genetics, Membrane Proteins metabolism, Muscle Proteins genetics, Mutation, Myasthenic Syndromes, Congenital genetics

Abstract

Collagen Q (ColQ) is a key multidomain functional protein of the neuromuscular junction (NMJ), crucial for anchoring acetylcholinesterase (AChE) to the basal lamina (BL) and accumulating AChE at the NMJ. The attachment of AChE to the BL is primarily accomplished by the binding of the ColQ collagen domain to the heparan sulfate proteoglycan perlecan and the COOH-terminus to the muscle-specific receptor tyrosine kinase (MuSK), which in turn plays a fundamental role in the development and maintenance of the NMJ. Yet, the precise mechanism by which ColQ anchors AChE at the NMJ remains unknown. We identified five novel mutations at the COOH-terminus of ColQ in seven patients from five families affected with endplate (EP) AChE deficiency. We found that the mutations do not affect the assembly of ColQ with AChE to form asymmetric forms of AChE or impair the interaction of ColQ with perlecan. By contrast, all mutations impair in varied degree the interaction of ColQ with MuSK as well as basement membrane extract (BME) that have no detectable MuSK. Our data confirm that the interaction of ColQ to perlecan and MuSK is crucial for anchoring AChE to the NMJ. In addition, the identified COOH-terminal mutants not only reduce the interaction of ColQ with MuSK, but also diminish the interaction of ColQ with BME. These findings suggest that the impaired attachment of COOH-terminal mutants causing EP AChE deficiency is in part independent of MuSK, and that the COOH-terminus of ColQ may interact with other proteins at the BL.

Published

2014

23. Exome sequencing detection of two untranslated GFPT1 mutations in a family with limb-girdle myasthenia.

Author

Maselli RA, Arredondo J, Nguyen J, Lara M, Ng F, Ngo M, Pham JM, Yi Q, Stajich JM, McDonald K, Hauser MA, and Wollmann RL

Subjects

4-Aminopyridine analogs & derivatives, 4-Aminopyridine therapeutic use, Aged, Amifampridine, Base Sequence, DNA Mutational Analysis, Electromyography, Female, High-Throughput Nucleotide Sequencing, Humans, Molecular Sequence Data, Myasthenia Gravis drug therapy, Myasthenia Gravis pathology, Myasthenic Syndromes, Congenital drug therapy, Myasthenic Syndromes, Congenital pathology, Neostigmine therapeutic use, Neuromuscular Junction ultrastructure, Pedigree, Reverse Transcriptase Polymerase Chain Reaction, Exome genetics, Glutamine-Fructose-6-Phosphate Transaminase (Isomerizing) genetics, Myasthenia Gravis genetics, Myasthenic Syndromes, Congenital genetics

Abstract

The term 'limb-girdle myasthenia' (LGM) was first used to describe three siblings with proximal limb weakness without oculobulbar involvement, but with EMG decrement and responsiveness to anticholinesterase medication. We report here that exome sequencing in the proband of this family revealed several sequence variations in genes linked to proximal limb weakness. However, the only mutations that cosegregated with disease were an intronic IVS7-8A>G mutation and the previously reported 3'-UTR c.*22C>A mutation in GFPT1, a gene linked to LGM. A minigene assay showed that IVS7-8A>G activates an alternative splice acceptor that results in retention of the last seven nucleotides of intron 7 and a frameshift leading to a termination codon 13 nucleotides downstream from the new splice site. An anconeus muscle biopsy revealed mild reduction of the axon terminal size and postsynaptic fold simplification. The amplitudes of miniature endplate potentials and quantal release were also diminished. The DNA of the mildly affected father of the proband showed only the intronic mutation along with sequence variations in other genes potentially relevant to LGM. Thus, this study performed in the family originally described with LGM showed two GFPT1 untranslated mutations, which may cause disease by reducing GFPT1 expression and ultimately impairing protein glycosylation., (© 2013 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2014

24. Dominantly inherited myotonia congenita resulting from a mutation that increases open probability of the muscle chloride channel CLC-1.

Author

Richman DP, Yu Y, Lee TT, Tseng PY, Yu WP, Maselli RA, Tang CY, and Chen TY

Subjects

Adult, Animals, Child, Chloride Channels chemistry, Chloride Channels physiology, Chlorides metabolism, Disease Progression, Female, Genes, Dominant, HEK293 Cells physiology, Humans, Ion Channel Gating genetics, Male, Models, Molecular, Muscle Cramp genetics, Oocytes physiology, Pedigree, Protein Conformation, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins physiology, Transfection, Xenopus laevis, Chloride Channels genetics, Mutation, Missense, Myotonia Congenita genetics, Point Mutation

Abstract

Myotonia congenita-inducing mutations in the muscle chloride channel CLC-1 normally result in reduced open probability (P (o)) of this channel. One well-accepted mechanism of the dominant inheritance of this disease involves a dominant-negative effect of the mutation on the function of the common-gate of this homodimeric, double-barreled molecule. We report here a family with myotonia congenita characterized by muscle stiffness and clinical and electrophysiologic myotonic phenomena transmitted in an autosomal dominant pattern. DNA sequencing of DMPK and ZNF9 genes for myotonic muscular dystrophy types I and II was normal, whereas sequencing of CLC-1 encoding gene, CLCN1, identified a single heterozygous missense mutation, G233S. Patch-clamp analyses of this mutant CLC-1 channel in Xenopus oocytes revealed an increased P (o) of the channel's fast-gate, from ~0.4 in the wild type to >0.9 in the mutant at -90 mV. In contrast, the mutant exhibits a minimal effect on the P (o) of the common-gate. These results are consistent with the structural prediction that the mutation site is adjacent to the fast-gate of the channel. Overall, the mutant could lead to a significantly reduced dynamic response of CLC-1 to membrane depolarization, from a fivefold increase in chloride conductance in the wild type to a twofold increase in the mutant-this might result in slower membrane repolarization during an action potential. Since expression levels of the mutant and wild-type subunits in artificial model cell systems were unable to explain the disease symptoms, the mechanism leading to dominant inheritance in this family remains to be determined.

Published

2012

25. Animal models of antimuscle-specific kinase myasthenia.

Author

Richman DP, Nishi K, Ferns MJ, Schnier J, Pytel P, Maselli RA, and Agius MA

Subjects

Animals, Immunoglobulin G immunology, Immunoglobulin G metabolism, Mice, Myasthenia Gravis, Autoimmune, Experimental metabolism, Neuromuscular Junction metabolism, Rabbits, Rats, Receptor Protein-Tyrosine Kinases immunology, Muscle, Skeletal enzymology, Myasthenia Gravis, Autoimmune, Experimental immunology, Receptor Protein-Tyrosine Kinases metabolism

Abstract

Antimuscle-specific kinase (anti-MuSK) myasthenia (AMM) differs from antiacetylcholine receptor myasthenia gravis in exhibiting more focal muscle involvement (neck, shoulder, facial, and bulbar muscles) with wasting of the involved, primarily axial, muscles. AMM is not associated with thymic hyperplasia and responds poorly to anticholinesterase treatment. Animal models of AMM have been induced in rabbits, mice, and rats by immunization with purified xenogeneic MuSK ectodomain, and by passive transfer of large quantities of purified serum IgG from AMM patients into mice. The models have confirmed the pathogenic role of the MuSK antibodies in AMM and have demonstrated the involvement of both the presynaptic and postsynaptic components of the neuromuscular junction. The observations in this human disease and its animal models demonstrate the role of MuSK not only in the formation of this synapse but also in its maintenance., (© 2012 New York Academy of Sciences.)

Published

2012

26. Synaptic basal lamina-associated congenital myasthenic syndromes.

Author

Maselli RA, Arredondo J, Ferns MJ, and Wollmann RL

Subjects

Acetylcholinesterase genetics, Acetylcholinesterase metabolism, Agrin genetics, Animals, Basement Membrane metabolism, Collagen genetics, Humans, Laminin genetics, Mice, Motor Endplate enzymology, Muscle Proteins genetics, Mutation, Myasthenic Syndromes, Congenital genetics, Myasthenic Syndromes, Congenital metabolism, Neuromuscular Junction metabolism, Protein Binding, Basement Membrane physiopathology, Myasthenic Syndromes, Congenital physiopathology, Synapses metabolism

Abstract

Proteins associated with the basal lamina (BL) participate in complex signal transduction processes that are essential for the development and maintenance of the neuromuscular junction (NMJ). Most important junctional BL proteins are collagens, such as collagen IV (α3-6), collagen XIII, and ColQ; laminins; nidogens; and heparan sulfate proteoglycans, such as perlecan and agrin. Mice lacking Colq (Colq(-/-)), laminin β2 (Lamb2(-/-)), or collagen XIII (Col13a1(-/-)) show immature nerve terminals enwrapped by Schwann cell projections that invaginate into the synaptic cleft and decrease contact surface for neurotransmission. Human mutations in COLQ, LAMB2, and AGRN cause congenital myasthenic syndromes (CMSs) owing to deficiency of ColQ, laminin-β2, and agrin, respectively. In these syndromes the NMJ ultrastructure shows striking resemblance to that of mice lacking the corresponding protein; furthermore, the extracellular localization of mutant proteins may provide favorable conditions for replacement strategies based on gene therapy and stem cells., (© 2012 New York Academy of Sciences.)

Published

2012

27. LG2 agrin mutation causing severe congenital myasthenic syndrome mimics functional characteristics of non-neural (z-) agrin.

Author

Maselli RA, Fernandez JM, Arredondo J, Navarro C, Ngo M, Beeson D, Cagney O, Williams DC, Wollmann RL, Yarov-Yarovoy V, and Ferns MJ

Subjects

Acetylcholinesterase metabolism, Adult, Agrin chemistry, Agrin metabolism, Base Sequence, Cell Line, Dystroglycans metabolism, Female, HEK293 Cells, Humans, Male, Models, Molecular, Muscle Fibers, Skeletal metabolism, Muscle Fibers, Skeletal pathology, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Muscle, Skeletal physiopathology, Myasthenic Syndromes, Congenital metabolism, Neuromuscular Junction metabolism, Neuromuscular Junction pathology, Pedigree, Receptors, Cholinergic genetics, Receptors, Cholinergic metabolism, Sequence Analysis, DNA, Agrin genetics, Codon, Nonsense, Mutation, Missense, Myasthenic Syndromes, Congenital genetics

Abstract

We describe a severe form of congenital myasthenic syndrome (CMS) caused by two heteroallelic mutations: a nonsense and a missense mutation in the gene encoding agrin (AGRN). The identified mutations, Q353X and V1727F, are located at the N-terminal and at the second laminin G-like (LG2) domain of agrin, respectively. A motor-point muscle biopsy demonstrated severe disruption of the architecture of the neuromuscular junction (NMJ), including: dispersion and fragmentation of endplate areas with normal expression of acetylcholinesterase; simplification of postsynaptic membranes; pronounced reduction of the axon terminal size; widening of the primary synaptic cleft; and, collection of membranous debris material in the primary synaptic cleft and in the subsynaptic cytoplasm. Expression studies in heterologous cells revealed that the Q353X mutation abolished expression of full-length agrin. Moreover, the V1727F mutation decreased agrin-induced clustering of the acetylcholine receptor (AChR) in cultured C2 muscle cells by >100-fold, and phosphorylation of the MuSK receptor and AChR beta subunit by ~tenfold. Surprisingly, the V1727F mutant also displayed increased binding to α-dystroglycan but decreased binding to a neural (z+) agrin-specific antibody. Our findings demonstrate that agrin mutations can associate with a severe form of CMS and cause profound distortion of the architecture and function of the NMJ. The impaired ability of V1727F agrin to activate MuSK and cluster AChRs, together with its increased affinity to α-dystroglycan, mimics non-neural (z-) agrin and are important determinants of the pathogenesis of the disease.

Published

2012

28. Acute severe animal model of anti-muscle-specific kinase myasthenia: combined postsynaptic and presynaptic changes.

Author

Richman DP, Nishi K, Morell SW, Chang JM, Ferns MJ, Wollmann RL, Maselli RA, Schnier J, and Agius MA

Subjects

Action Potentials physiology, Animals, Autoantibodies blood, Bungarotoxins pharmacokinetics, Cholinesterases metabolism, Diaphragm drug effects, Disease Models, Animal, Dose-Response Relationship, Immunologic, Electric Stimulation methods, Female, Hindlimb physiopathology, Median Nerve physiology, Microscopy, Electron, Transmission, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Muscle, Skeletal physiopathology, Myasthenia Gravis immunology, Myasthenia Gravis metabolism, Neuromuscular Junction metabolism, Neuromuscular Junction ultrastructure, Presynaptic Terminals ultrastructure, Protein Binding drug effects, Rats, Rats, Inbred Lew, Myasthenia Gravis chemically induced, Myasthenia Gravis pathology, Neuromuscular Junction pathology, Presynaptic Terminals pathology, Receptor Protein-Tyrosine Kinases adverse effects, Receptor Protein-Tyrosine Kinases immunology, Receptors, Cholinergic immunology

Abstract

Objectives: To determine the pathogenesis of anti-muscle-specific kinase (MuSK) myasthenia, a newly described severe form of myasthenia gravis associated with MuSK antibodies characterized by focal muscle weakness and wasting and absence of acetylcholine receptor antibodies, and to determine whether antibodies to MuSK, a crucial protein in the formation of the neuromuscular junction (NMJ) during development, can induce disease in the mature NMJ. Design, Setting, and, Participants: Lewis rats were immunized with a single injection of a newly discovered splicing variant of MuSK, MuSK 60, which has been demonstrated to be expressed primarily in the mature NMJ. Animals were assessed clinically, serologically, and by repetitive stimulation of the median nerve. Muscle tissue was examined immunohistochemically and by electron microscopy., Results: Animals immunized with 100 μg of MuSK 60 developed severe progressive weakness starting at day 16, with 100% mortality by day 27. The weakness was associated with high MuSK antibody titers, weight loss, axial muscle wasting, and decrementing compound muscle action potentials. Light and electron microscopy demonstrated fragmented NMJs with varying degrees of postsynaptic muscle end plate destruction along with abnormal nerve terminals, lack of registration between end plates and nerve terminals, local axon sprouting, and extrajunctional dispersion of cholinesterase activity., Conclusions: These findings support the role of MuSK antibodies in the human disease, demonstrate the role of MuSK not only in the development of the NMJ but also in the maintenance of the mature synapse, and demonstrate involvement of this disease in both presynaptic and postsynaptic components of the NMJ.

Published

2012

29. Protection of human muscle acetylcholinesterase from soman by pyridostigmine bromide.

Author

Maselli RA, Henderson JD, Ng J, Follette D, Graves G, and Wilson BW

Subjects

Dose-Response Relationship, Drug, Humans, Organ Culture Techniques, Protective Agents pharmacology, Acetylcholinesterase metabolism, Cholinesterase Inhibitors pharmacology, Intercostal Muscles drug effects, Intercostal Muscles enzymology, Pyridostigmine Bromide pharmacology, Soman toxicity

Abstract

Introduction: Pretreatment with pyridostigmine bromide (PB) of human intercostal muscle fibers exposed to the irreversible acetylcholinesterase (AChE) inhibitor soman was investigated., Methods: Muscles were pretreated with 3 × 10(-6) M PB or saline for 20 minutes, then exposed to 10(-7) M soman for 10 minutes., Results: AChE of muscles treated with soman alone was inhibited >95%. In contrast, PB pretreatment of soman-exposed bundles protected 20% of AChE activity. AChE of bundles exposed to PB alone recovered after 4 hours, but bundles exposed to both PB and soman did not. Soman-induced reduction of resting membrane potentials and increment of amplitudes and decay times of miniature endplate potentials (MEPPs) were partially corrected by PB pretreatment., Conclusions: In vitro pretreatment of human muscles with PB protected up to 20% of muscle AChE and ameliorated some deleterious effects on endplate physiology induced by soman., (Copyright © 2011 Wiley Periodicals, Inc.)

Published

2011

30. Mutations in MUSK causing congenital myasthenic syndrome impair MuSK-Dok-7 interaction.

Author

Maselli RA, Arredondo J, Cagney O, Ng JJ, Anderson JA, Williams C, Gerke BJ, Soliven B, and Wollmann RL

Subjects

Agrin metabolism, Animals, Cell Line, Female, HSP40 Heat-Shock Proteins metabolism, Humans, Mice, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Muscle, Skeletal physiology, Mutation, Missense, Myasthenic Syndromes, Congenital metabolism, Myasthenic Syndromes, Congenital pathology, Neuromuscular Junction metabolism, Neuromuscular Junction ultrastructure, Protein Structure, Secondary, Receptor Protein-Tyrosine Kinases chemistry, Receptor Protein-Tyrosine Kinases metabolism, Receptors, Cholinergic chemistry, Receptors, Cholinergic metabolism, Receptors, Growth Factor metabolism, Young Adult, Muscle Proteins metabolism, Myasthenic Syndromes, Congenital genetics, Receptor Protein-Tyrosine Kinases genetics, Receptors, Cholinergic genetics

Abstract

We describe a severe congenital myasthenic syndrome (CMS) caused by two missense mutations in the gene encoding the muscle specific receptor tyrosine kinase (MUSK). The identified MUSK mutations M605I and A727V are both located in the kinase domain of MuSK. Intracellular microelectrode recordings and microscopy studies of the neuromuscular junction conducted in an anconeus muscle biopsy revealed decreased miniature endplate potential amplitudes, reduced endplate size and simplification of secondary synaptic folds, which were consistent with postsynaptic deficit. The study also showed a striking reduction of the endplate potential quantal content, consistent with additional presynaptic failure. Expression studies in MuSK deficient myotubes revealed that A727V, which is located within the catalytic loop of the enzyme, caused severe impairment of agrin-dependent MuSK phosphorylation, aggregation of acetylcholine receptors (AChRs) and interaction of MuSK with Dok-7, an essential intracellular binding protein of MuSK. In contrast, M605I, resulted in only moderate impairment of agrin-dependent MuSK phosphorylation, aggregation of AChRs and interaction of MuSK with Dok-7. There was no impairment of interaction of mutants with either the low-density lipoprotein receptor-related protein, Lrp4 (a co-receptor of agrin) or with the mammalian homolog of the Drosophila tumorous imaginal discs (Tid1). Our findings demonstrate that missense mutations in MUSK can result in a severe form of CMS and indicate that the inability of MuSK mutants to interact with Dok-7, but not with Lrp4 or Tid1, is a major determinant of the pathogenesis of the CMS caused by MUSK mutations.

Published

2010

31. Variable phenotypes associated with mutations in DOK7.

Author

Anderson JA, Ng JJ, Bowe C, McDonald C, Richman DP, Wollmann RL, and Maselli RA

Subjects

Adolescent, Adult, Biopsy, DNA Mutational Analysis, Evoked Potentials, Motor, Female, Haplotypes, Humans, Male, Middle Aged, Muscle, Skeletal pathology, Muscle, Skeletal physiopathology, Myasthenic Syndromes, Congenital pathology, Phenotype, Muscle Proteins genetics, Myasthenic Syndromes, Congenital genetics, Myasthenic Syndromes, Congenital physiopathology

Abstract

Many patients with the limb-girdle variant of congenital myasthenic syndrome (CMS) possess mutations in the human Dok-7 gene (DOK7). We identified six unrelated CMS patients with DOK7 mutations. Two patients, one mildly and the other moderately affected, were homozygous for the previously described 1263insC mutation. The common 1124_1127dupTGCC mutation was detected in the other four patients, whose clinical phenotypes range from mildly to severely affected. This striking phenotypic heterogeneity found both within and between mutational classes is made more compelling by data from our electrophysiological studies and electron microscopy of the neuromuscular junction (NMJ). Indeed, several aspects of the physiological and morphometric data do not correlate with genotype or severity of clinical phenotype. Overall, our study corroborates the findings of others and provides an additional demonstration of the considerable phenotypic variability associated with CMS due to DOK7 mutations.

Published

2008

32. High throughput genetic analysis of congenital myasthenic syndromes using resequencing microarrays.

Author

Denning L, Anderson JA, Davis R, Gregg JP, Kuzdenyi J, and Maselli RA

Subjects

Humans, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Myasthenic Syndromes, Congenital genetics, Oligonucleotide Array Sequence Analysis

Abstract

Background: The use of resequencing microarrays for screening multiple, candidate disease loci is a promising alternative to conventional capillary sequencing. We describe the performance of a custom resequencing microarray for mutational analysis of Congenital Myasthenic Syndromes (CMSs), a group of disorders in which the normal process of neuromuscular transmission is impaired., Methodology/principal Findings: Our microarray was designed to assay the exons and flanking intronic regions of 8 genes linked to CMSs. A total of 31 microarrays were hybridized with genomic DNA from either individuals with known CMS mutations or from healthy controls. We estimated an overall microarray call rate of 93.61%, and we found the percentage agreement between the microarray and capillary sequencing techniques to be 99.95%. In addition, our microarray exhibited 100% specificity and 99.99% reproducibility. Finally, the microarray detected 22 out of the 23 known missense mutations, but it failed to detect all 7 known insertion and deletion (indels) mutations, indicating an overall sensitivity of 73.33% and a sensitivity with respect to missense mutations of 95.65%., Conclusions/significance: Overall, our microarray prototype exhibited strong performance and proved highly efficient for screening genes associated with CMSs. Until indels can be efficiently assayed with this technology, however, we recommend using resequencing microarrays for screening CMS mutations after common indels have been first assayed by capillary sequencing.

Published

2007

33. Novel beta subunit mutation causes a slow-channel syndrome by enhancing activation and decreasing the rate of agonist dissociation.

Author

Navedo MF, Lasalde-Dominicci JA, Báez-Pagán CA, Díaz-Pérez L, Rojas LV, Maselli RA, Staub J, Schott K, Zayas R, and Gomez CM

Subjects

Aged, Amino Acid Substitution, Animals, Calcium Signaling genetics, Cell Membrane Permeability genetics, Excitatory Postsynaptic Potentials genetics, Female, Humans, Ion Channels genetics, Ion Channels metabolism, Kinetics, Male, Muscle, Skeletal innervation, Muscle, Skeletal physiopathology, Myasthenic Syndromes, Congenital metabolism, Myasthenic Syndromes, Congenital physiopathology, Neuromuscular Junction metabolism, Neuromuscular Junction physiopathology, Oocytes, Pedigree, Xenopus laevis, Acetylcholine metabolism, Mutation genetics, Myasthenic Syndromes, Congenital genetics, Neuromuscular Junction genetics, Receptors, Nicotinic genetics, Synaptic Transmission genetics

Abstract

We traced the cause of a slow-channel syndrome (SCS) in a patient with progressive muscle weakness, repetitive compound muscle action potential and prolonged low amplitude synaptic currents to a V --> F substitution in the M1 domain of the beta subunit (betaV229F) of the muscle acetylcholine receptor (AChR). In vitro expression studies in Xenopus oocytes indicated that the novel mutation betaV229F expressed normal amounts of AChRs and decreased the ACh EC50 by 10-fold compared to wild type. Kinetic analysis indicated that the mutation displayed prolonged mean open duration and repeated openings during activation. Prolonged openings caused by the betaV229F mutation were due to a reduction in the channel closing rate and an increase in the effective channel opening rate. Repeated openings of the channel during activation were caused by a significant reduction in the agonist dissociation constant. In addition, the betaV229F mutation produced an increase in calcium permeability. The kinetic and permeation studies presented in this work are sufficient to explain the consequences of the betaV229F mutation on the miniature endplate currents and thus are direct evidence that the betaV229F mutation is responsible for compromising the safety margin of neuromuscular transmission in the patient.

Published

2006

34. Focal caspase activation underlies the endplate myopathy in slow-channel syndrome.

Author

Vohra BP, Groshong JS, Maselli RA, Verity MA, Wollmann RL, and Gomez CM

Subjects

Age of Onset, Aminophenols metabolism, Apoptosis physiology, Bungarotoxins metabolism, Calcium metabolism, Cholinesterases metabolism, DNA Mutational Analysis methods, Enzyme Activation, Family Health, Humans, Immunohistochemistry methods, In Situ Nick-End Labeling methods, Microscopy, Electron methods, Motor Endplate ultrastructure, Muscles ultrastructure, Mutation, Myasthenic Syndromes, Congenital pathology, Myasthenic Syndromes, Congenital ultrastructure, Neurologic Examination methods, Oligodeoxyribonucleotides, Antisense metabolism, Protein Subunits genetics, Receptors, Cholinergic genetics, Caspases metabolism, Motor Endplate pathology, Muscles pathology, Myasthenic Syndromes, Congenital enzymology

Abstract

Slow-channel syndrome (SCS) is a progressive neuromuscular disorder caused by abnormal gating of mutant acetylcholine receptors (AChRs) in the neuromuscular junction (NMJ). The pathological hallmark is selective degeneration of the NMJ termed endplate myopathy. Endplate myopathy consists of a combination of ultrastructural abnormalities, including degenerating subsynaptic nuclei, mitochondria, and postsynaptic folds, caused by localized cation overload through mutant AChRs. Because some of these changes resemble those seen in programmed cell death, we evaluated SCS muscle for evidence of focal activation of apoptotic pathways. Using antisera specific for the activated forms of caspases, the family of cysteine proteases that underlies apoptosis, we demonstrated that active forms of initiator and effector caspases are selectively localized at the NMJ in SCS. In comparison with an electron microscopic assessment of the abnormalities seen in endplate myopathy, we found that activated caspases were present at between 15 and 57% of endplates, similar to the proportion of endplates with degenerating mitochondria or vacuoles. This greatly exceeds the number of NMJs exhibiting nuclear degeneration. These findings provide the first evidence supporting the view that caspase activation in human disease can play a prominent role in localized cellular degenerative processes without causing nuclear or cell death.

Published

2004

35. Common founder effect of rapsyn N88K studied using intragenic markers.

Author

Dunne V and Maselli RA

Subjects

Alleles, DNA Restriction Enzymes pharmacology, Family Health, Female, Genes, Recessive, Genotype, Haplotypes, Heterozygote, Homozygote, Humans, Male, Microsatellite Repeats, Models, Genetic, Pedigree, Phenotype, Polymorphism, Single Nucleotide, Recombination, Genetic, Sequence Analysis, DNA, Founder Effect, Genetic Markers, Muscle Proteins genetics, Mutation, Myasthenic Syndromes, Congenital genetics

Abstract

Mutations in the human gene encoding rapsyn have been linked to a recessive form of postsynaptic congenital myasthenic syndrome due to deficient clustering of acetylcholine receptors at the endplate. All patients reported to date carry the N88K mutation, suggesting a possible common founder effect. To decrease the likelihood of a recombination event occurring within the span of neighboring microsatellite markers, we used seven intragenic single nucleotide polymorphisms (SNPs) spanning 8 kb to characterize the haplotype associated with N88K. In three affected N88K homozygous individuals, we identified a common haplotype present in all heterozygous carriers of N88K. Of note, in two asymptomatic N88K homozygous individuals, a second haplotype was present that differed at three SNP sites downstream from the N88K mutation. Our findings of a common haplotype associated with the N88K mutation support a founder effect. The discordant haplotype found in homozygous individuals suggests that recombination events may have occurred within the rapsyn gene and that this may have implications in the phenotypic expression of the disease.

Published

2004

36. Presynaptic failure of neuromuscular transmission and synaptic remodeling in EA2.

Author

Maselli RA, Wan J, Dunne V, Graves M, Baloh RW, Wollmann RL, and Jen J

Subjects

Acetylcholinesterase metabolism, Adult, Ataxia complications, Binding, Competitive, Biopsy, Calcium Channel Blockers, Calcium Channels drug effects, Calcium Channels genetics, Electric Stimulation, Electromyography, Humans, Male, Middle Aged, Motor Endplate enzymology, Motor Endplate physiopathology, Muscle, Skeletal innervation, Muscle, Skeletal pathology, Muscle, Skeletal physiopathology, Mutation, Myasthenic Syndromes, Congenital complications, Neuromuscular Junction pathology, Neuromuscular Junction physiopathology, Neuromuscular Junction ultrastructure, Synapses ultrastructure, Ataxia diagnosis, Ataxia physiopathology, Myasthenic Syndromes, Congenital diagnosis, Myasthenic Syndromes, Congenital physiopathology, Synapses pathology, Synaptic Transmission genetics

Abstract

Objective: To further investigate the basis of abnormal neuromuscular transmission in two patients with congenital myasthenic syndrome associated with episodic ataxia type 2 (EA2) using stimulated single fiber EMG (SFEMG) and in vitro microelectrode studies., Methods: Two patients with genetically characterized EA2 previously shown to have abnormal neuromuscular transmission by voluntary SFEMG were studied with stimulated SFEMG and anconeus muscle biopsy with microelectrode studies and electron microscopy of the neuromuscular junction., Results: In vivo stimulated SFEMG showed signs of presynaptic failure, with jitter and blocking that improved with increased stimulation frequency. Additional evidence of presynaptic failure was provided by the in vitro microelectrode studies, which showed marked reduction of the end plate potential quantal content in both patients. Of note, the end plate potentials showed high sensitivity to N-type blockade with omega-conotoxin not seen in controls. The ultrastructural studies revealed some evidence of small nerve terminals apposed to normal or mildly overdeveloped postsynaptic membranes, suggesting an ongoing degenerative process., Conclusions: The authors demonstrated presynaptic failure of neurotransmission in patients with heterozygous nonsense mutations in CACNA1A. The contribution of non-P-type calcium channels to the process of neurotransmitter release in these patients likely represents a compensatory mechanism, which is insufficient to restore normal neuromuscular transmission.

Published

2003

37. Rapsyn mutations in myasthenic syndrome due to impaired receptor clustering.

Author

Maselli RA, Dunne V, Pascual-Pascual SI, Bowe C, Agius M, Frank R, and Wollmann RL

Subjects

Adolescent, Child, Preschool, Excitatory Postsynaptic Potentials genetics, Female, Genetic Testing, Genotype, Heterozygote, Homozygote, Humans, Male, Microscopy, Electron, Muscle, Skeletal innervation, Muscle, Skeletal pathology, Muscle, Skeletal physiopathology, Myasthenic Syndromes, Congenital metabolism, Myasthenic Syndromes, Congenital physiopathology, Neuromuscular Junction pathology, Neuromuscular Junction ultrastructure, Pedigree, Phenotype, Receptors, Cholinergic genetics, Receptors, Cholinergic metabolism, Receptors, Cholinergic ultrastructure, Synaptic Membranes genetics, Synaptic Membranes pathology, Synaptic Membranes ultrastructure, Synaptic Transmission genetics, Genetic Predisposition to Disease genetics, Muscle Proteins deficiency, Muscle Proteins genetics, Mutation genetics, Myasthenic Syndromes, Congenital genetics, Neuromuscular Junction genetics

Abstract

Rapsyn, a 43-kDa postsynaptic protein, is essential for anchoring and clustering acetylcholine receptors (AChRs) at the endplate (EP). Mutations in the rapsyn gene have been found to cause a postsynaptic congenital myasthenic syndrome (CMS). We detected six patients with CMS due to mutations in the rapsyn gene (RAPSN). In vitro studies performed in the anconeus muscle biopsies of four patients showed severe reduction of miniature EP potential amplitudes. Electron microscopy revealed various degrees of impaired development of postsynaptic membrane folds. All patients carried the N88K mutation. Three patients were homozygous for N88K and had less severe phenotypes and milder histopathologic abnormalities than the three patients who were heterozygous and carried a second mutation (either L14P, 46insC, or Y269X). Surprisingly, two N88K homozygous patients had one asymptomatic relative each who carried the same genotype, suggesting that additional genetic factors to RAPSN mutations are required for disease expression.

Published

2003

38. Effect of inherited abnormalities of calcium regulation on human neuromuscular transmission.

Author

Maselli RA, Books W, and Dunne V

Subjects

Action Potentials, Adolescent, Adult, Ataxia complications, Ataxia genetics, Ataxia physiopathology, Base Sequence, Calcium Channel Blockers pharmacology, Calcium Channels genetics, Calcium Channels, L-Type genetics, DNA Mutational Analysis, Electrophysiology, Humans, In Vitro Techniques, Membrane Glycoproteins genetics, Membrane Proteins genetics, Microelectrodes, Microscopy, Electron, Myasthenic Syndromes, Congenital classification, Myasthenic Syndromes, Congenital genetics, Myasthenic Syndromes, Congenital ultrastructure, Nerve Tissue Proteins genetics, Neuromuscular Junction drug effects, Neuromuscular Junction physiopathology, Neuromuscular Junction ultrastructure, Qa-SNARE Proteins, Sequence Alignment, Synapses drug effects, Synapses genetics, Synapses physiology, Synapses ultrastructure, Synaptotagmins, Syntaxin 1, Calcium deficiency, Calcium-Binding Proteins, Myasthenic Syndromes, Congenital physiopathology, Neuromuscular Junction genetics, Synaptic Transmission

Abstract

Synaptotagmins are abundant synaptic proteins that represent the best candidate for the calcium sensor at the nerve terminal. The pore-forming, voltage-sensing transmembrane alpha-1 subunit of the P/Q voltage-gated calcium channel (or Ca(v)2.1) encoded by the CACNA1A gene is another major component of the process of action potential-evoked exocytosis at the adult mammalian neuromuscular junction. Defects of these proteins, in nonhuman species, result in severe disruption of rapid synaptic transmission. This paper investigates the molecular bases of inherited presynaptic deficits of neuromuscular transmission in humans. Patients with congenital presynaptic failure, including two patients with episodic ataxia type 2 (EA-2) due to CACNA1A mutations, were studied with muscle biopsy, microelectrode studies, electron microscopy, DNA amplification, and sequencing. All patients, including EA-2 patients, showed selective failure of the action potential-dependent release without reduction of the spontaneous release of neurotransmitter. In addition, patients with EA-2 showed partial blockade of neuromuscular transmission with the N-type blocker omega-conotoxin not seen in controls. The EM showed a varied degree of increased complexity of postsynaptic folds. Mutational analysis in candidate genes, including human synaptotagmin II, syntaxin 1A, synaptobrevin I, SNAP 25, CACNA1A, CACNB2, and Rab3A, was unrevealing. Although no mutations in candidate genes were found in patients with inborn presynaptic failure, functional and structural similarities between this group and patients with EA-2 due to CACNA1A mutations suggest a common pathogenic mechanism.

Published

2003

39. Choline acetyltransferase mutations in myasthenic syndrome due to deficient acetylcholine resynthesis.

Author

Maselli RA, Chen D, Mo D, Bowe C, Fenton G, and Wollmann RL

Subjects

Adolescent, Biopsy, Bungarotoxins metabolism, Bungarotoxins pharmacology, Child, Child, Preschool, DNA Mutational Analysis, Electromyography, Female, Heterozygote, Humans, Iodine Radioisotopes, Male, Microscopy, Electron, Muscle Fibers, Slow-Twitch enzymology, Muscle Fibers, Slow-Twitch pathology, Muscle Fibers, Slow-Twitch ultrastructure, Muscle, Skeletal enzymology, Muscle, Skeletal pathology, Mutation, Missense, Myasthenic Syndromes, Congenital pathology, Neural Conduction, Acetylcholine biosynthesis, Choline O-Acetyltransferase genetics, Choline O-Acetyltransferase metabolism, Myasthenic Syndromes, Congenital enzymology, Myasthenic Syndromes, Congenital genetics

Abstract

The myasthenic syndrome due to abnormal acetylcholine resynthesis is characterized by early onset, recessive inheritance, and recurrent episodes of potentially fatal apnea. Mutations in the gene encoding choline acetyltransferase (CHAT) have been found to account for this condition. We have identified five patients from three independent families with features of this disease including, in four patients, a paradoxical worsening of symptoms with cold temperatures. Electrodiagnostic studies demonstrated impaired neuromuscular transmission in all patients. In vitro microelectrode studies performed in the anconeus muscle biopsies of two patients showed moderate reduction of quantal release. Electron microscopy of the neuromuscular junction was normal in both patients. Each patient had two heterozygous CHAT mutations including L210P and P211A (family 1), V194L and V506L (family 2), and R548stop and S694C (family 3). Three of these mutations have previously been reported and suggest that, in this syndrome, some molecular defects may be more prevalent than others.

Published

2003

40. Identification of pathogenic mutations in the human rapsyn gene.

Author

Dunne V and Maselli RA

Subjects

Adolescent, Adult, Child, Preschool, DNA Mutational Analysis, Female, Humans, Male, Pedigree, Restriction Mapping, Muscle Proteins genetics, Mutation genetics, Myasthenic Syndromes, Congenital genetics

Abstract

Rapsyn, a complex postsynaptic protein of the striated muscle, assembles acetylcholine receptors (AChR) at high density at the motor endplate (EP). Neuromuscular junctions of mice lacking rapsyn show no clusters of AChRs or other structural postsynaptic proteins such as beta-dystroglycan and utrophin. Humans with mutations in the rapsyn gene ( RAPSN) are affected with a postsynaptic form of congenital myasthenic syndrome (CMS) characterized by impairment of the morphologic development of the postsynaptic region. We have identified four patients from four different families with RAPSNmutations and CMS, confirmed in two cases by microelectrode and electron microscopy studies. The N88K mutation was present in all patients. One patient who was homozygous for N88K was only mildly affected, while the other three patients who were heterozygous for N88K and a second mutation (either L14P, 46insC, or Y269X) were severely affected. Mutations 46insC and Y269X predicts truncation of the protein. L14P predicts a conformational change at the N-terminus that may disrupt membrane association. N88K occurs within the putative leucine zipper motif potentially important for AChR clustering. These findings may explain the severe clinical involvement of compound heterozygous patients.

Published

2003

41. Active calcium accumulation underlies severe weakness in a panel of mice with slow-channel syndrome.

Author

Gomez CM, Maselli RA, Groshong J, Zayas R, Wollmann RL, Cens T, and Charnet P

Subjects

Animals, Disease Models, Animal, Electromyography, Gene Targeting, Mice, Mice, Transgenic, Motor Endplate metabolism, Motor Endplate pathology, Muscle Contraction genetics, Mutation, Neuromuscular Junction metabolism, Neuromuscular Junction pathology, Oocytes metabolism, Patch-Clamp Techniques, Permeability, Protein Subunits, RNA, Messenger biosynthesis, Receptors, Cholinergic genetics, Receptors, Cholinergic metabolism, Transfection, Transgenes, Xenopus, Calcium metabolism, Muscle Weakness etiology, Muscle Weakness metabolism, Myasthenic Syndromes, Congenital etiology, Myasthenic Syndromes, Congenital physiopathology

Abstract

Mutations affecting the gating and channel properties of ionotropic neurotransmitter receptors in some hereditary epilepsies, in familial hyperekplexia, and the slow-channel congenital myasthenic syndrome (SCCMS) may perturb the kinetics of synaptic currents, leading to significant clinical consequences. Although at least 12 acetylcholine receptor (AChR) mutations have been identified in the SCCMS, the altered channel properties critical for disease pathogenesis in the SCCMS have not been identified. To approach this question, we investigated the effect of different AChR subunit mutations on muscle weakness and the function and viability of neuromuscular synapses in transgenic mice. Targeted expression of distinct mutant AChR subunits in skeletal muscle prolonged the decay phases of the miniature endplate currents (MEPCs) over a broad range. In addition, both muscle strength and the amplitude of MEPCs were lower in transgenic lines with greater MEPC duration. SCCMS is associated with calcium overload of the neuromuscular junctional sarcoplasm. We found that the extent of calcium overload of motor endplates in the panel of transgenic mice was influenced by the relative permeability of the mutant AChRs to calcium, on the duration of MEPCs, and on neuromuscular activity. Finally, severe degenerative changes at the motor endplate (endplate myopathy) were apparent by electron microscopy in transgenic lines that displayed the greatest activity-dependent calcium overload. These studies demonstrate the importance of control of the kinetics of AChR channel gating for the function and viability of the neuromuscular junction.

Published

2002

42. Novel delta subunit mutation in slow-channel syndrome causes severe weakness by novel mechanisms.

Author

Gomez CM, Maselli RA, Vohra BP, Navedo M, Stiles JR, Charnet P, Schott K, Rojas L, Keesey J, Verity A, Wollmann RW, and Lasalde-Dominicci J

Subjects

Adolescent, Amino Acid Sequence, Animals, Child, Electromyography, Humans, Male, Molecular Sequence Data, Motor Endplate pathology, Motor Endplate physiology, Muscle Weakness pathology, Mutagenesis, Site-Directed physiology, Myasthenic Syndromes, Congenital pathology, Neuromuscular Junction pathology, Neuromuscular Junction physiology, Oocytes physiology, Patch-Clamp Techniques, Point Mutation physiology, Xenopus, Ion Channel Gating genetics, Muscle Weakness genetics, Muscle Weakness physiopathology, Myasthenic Syndromes, Congenital genetics, Myasthenic Syndromes, Congenital physiopathology, Receptors, Nicotinic genetics

Abstract

We investigated the basis for a novel form of the slow-channel congenital myasthenic syndrome presenting in infancy in a single individual as progressive weakness and impaired neuromuscular transmission without overt degeneration of the motor endplate. Prolonged low-amplitude synaptic currents in biopsied anconeus muscle at 9 years of age suggested a kinetic disorder of the muscle acetylcholine receptor. Ultrastructural studies at 16 months, at 9 years, and at 15 years of age showed none of the typical degenerative changes of the endplate associated with the slow-channel congenital myasthenic syndrome, and acetylcholine receptor numbers were not significantly reduced. We identified a novel C-to-T substitution in exon 8 of the delta-subunit that results in a serine to phenylalanine mutation in the region encoding the second transmembrane domain that lines the ion channel. Using Xenopus oocyte in vitro expression studies we confirmed that the deltaS268F mutation, as with other slow-channel congenital myasthenic syndrome mutations, causes delayed closure of acetylcholine receptor ion channels. In addition, unlike other mutations in slow-channel congenital myasthenic syndrome, this mutation also causes delayed opening of the channel, a finding that readily explains the marked congenital weakness in the absence of endplate degeneration. Finally, we used serial morphometric analysis of electron micrographs to explore the basis for the progressive weakness and decline of amplitude of endplate currents over a period of 14 years. We demonstrated a progressive widening and accumulation of debris in the synaptic cleft, resulting in loss of efficacy of released neurotransmitter and reduced safety factor. These studies demonstrate the role of previously unrecognized mechanisms of impairment of synaptic transmission caused by a novel mutation and show the importance of serial in vitro studies to elucidate novel disease mechanisms.

Published

2002

43. Presynaptic congenital myasthenic syndrome due to quantal release deficiency.

Author

Maselli RA, Kong DZ, Bowe CM, McDonald CM, Ellis WG, Agius MA, Gomez CM, Richman DP, and Wollmann RL

Subjects

Adolescent, Child, Electromyography, Humans, Male, Microscopy, Electron, Muscles physiopathology, Neuromuscular Junction physiopathology, Neuromuscular Junction ultrastructure, Myasthenic Syndromes, Congenital etiology, Myasthenic Syndromes, Congenital physiopathology, Neurotransmitter Agents deficiency, Presynaptic Terminals physiology

Abstract

Objective: To provide clinical, electrophysiologic, and ultrastructural findings in three patients with a presynaptic congenital myasthenic syndrome (CMS)., Background: Familial infantile myasthenia and paucity of synaptic vesicles are the only two fully characterized CMS. We are describing here three patients with another form of presynaptic CMS characterized by deficiency of the action potential-dependent release without reduction of the spontaneous release of neurotransmitter from the nerve terminal., Methods: The authors performed electromyography and anconeus muscle biopsies that included intracellular recordings and electron microscopy of the neuromuscular junction in three patients with presynaptic CMS. They also sequenced part of the P/Q-calcium alpha(1)-subunit gene (CACNA1A) and the acetylcholine receptor subunit (AChR) genes in these patients., Results: In these patients there were additional neurologic findings including nystagmus and ataxia. In all three patients the end-plate potential quantal content (m) was markedly reduced but neither the amplitudes nor the frequencies of miniature end-plate potentials were diminished. Ultrastructurally, postsynaptic end-plate folds, nerve terminal size, and synaptic vesicle number were normal but double-membrane-bound sacs containing synaptic vesicles were present in the nerve terminal of all three patients. The screening of reported pathogenic mutations in the CACNA1A and a mutational analysis of AChR subunit genes were negative., Conclusion: This form of CMS appears to result only from a deficiency of the quantal release of neurotransmitter that may be due to an abnormal calcium mechanism or impaired endocytosis and recycling of synaptic vesicles.

Published

2001

44. Diagnostic difficulties in patients with adul botulism type a.

Author

Bakshi N, Rauf S, Fenton GE, and Maselli RA

Abstract

Although the ekcuodiagnostic abnormalities in botulism have bean well characterized, the expected abnormalities, such as facilitation of compound muscle anion potential amplitudes after sustained activation or with repetitive stimulation at fast tales, may not always be present especially early m the disease. This may lead to etectrodtagnosttc difficulties and sometimes a delay in establishing a diagnosis. We describe four serologically proven cases of type A botulism in adults that illustrate the variability in ekctrodiagnostic findings in this disease.

Published

2000

45. AAEM case report 16. Botulism. American Association of Electrodiagnostic Medicine.

Author

Maselli RA and Bakshi N

Subjects

Adult, Botulism pathology, Botulism physiopathology, Electric Stimulation, Electrodiagnosis, Electromyography, Humans, Male, Membrane Potentials physiology, Motor Endplate physiology, Muscle Fibers, Skeletal physiology, Neural Conduction physiology, Receptors, Cholinergic immunology, Substance Abuse, Intravenous, Treatment Outcome, Botulism diagnosis

Abstract

Early diagnosis of botulism is essential for effective treatment. Electrophysiologic testing can be of major help to establish a prompt diagnosis, but the classic electrodiagnostic features of botulism are often elusive. Decrement or increment of compound muscle action potential (CMAP) amplitudes to slow or fast rates of nerve stimulation are often unimpressive or totally absent. Reduction of CMAP amplitudes, denervation activity, or myopathic-like motor unit potentials in affected muscles are found more frequently but they are less specific. In general, the electrophysiologic findings taken together suggest involvement of the motor nerve terminal, which should raise the possibility of botulism. The case reported here illustrates a common clinical presentation of botulism. This study emphasizes realistic expectations of the electrodiagnostic testing, the differential diagnosis, and the potential pitfalls often encountered in the interpretation of the electrophysiologic data., (Copyright 2000 American Association of Electrodiagnostic Medicine.)

Published

2000

46. Morvan's fibrillary chorea: a paraneoplastic manifestation of thymoma.

Author

Lee EK, Maselli RA, Ellis WG, and Agius MA

Subjects

Biopsy, Chorea diagnosis, Disease Progression, Electromyography methods, Humans, Immunoglobulin G blood, Male, Middle Aged, Muscle Spasticity complications, Muscle, Skeletal innervation, Muscle, Skeletal pathology, Rhinitis, Allergic, Seasonal complications, Chorea complications, Paraneoplastic Syndromes, Thymoma complications, Thymus Neoplasms complications

Abstract

Morvan's fibrillary chorea is a rare disease characterised by symptoms which include neuromyotonia, cramping, weakness, pruritus, hyperhidrosis, insomnia, and delirium. The first case of Morvan's fibrillary chorea to be associated with clinical manifestations of myasthenia gravis with thymoma, psoriasis, and atopic dermatitis is reported. Muscle histopathology disclosed chronic denervation and myopathic changes and in vitro electrophysiology demonstrated both presynaptic and postsynaptic defects in neuromuscular transmission. Serum antibodies to acetylcholine receptors, titin, N-type calcium channels, and voltage gated potassium channels were detected. Plasmapheresis, thymectomy, and long term immunosuppression induced a dramatic resolution of symptoms. The association of thymoma with other autoimmune disorders and autoantibodies, and prolonged and sustained remission with chronic immunosuppression, place Morvan's fibrillary chorea on the range of neurological diseases arising as a paraneoplastic complication of cortical thymomas.

Published

1998

47. Electrodiagnosis of disorders of neuromuscular transmission.

Author

Maselli RA

Subjects

Electric Stimulation, Electromyography, Evoked Potentials, Humans, Lambert-Eaton Myasthenic Syndrome diagnosis, Motor Endplate physiology, Muscle Fibers, Skeletal physiology, Muscle, Skeletal physiopathology, Myasthenia Gravis diagnosis, Neuromuscular Diseases physiopathology, Synaptic Vesicles physiology, Electrodiagnosis, Motor Endplate physiopathology, Neuromuscular Diseases diagnosis

Published

1998

48. Pathogenesis of human botulism.

Author

Maselli RA

Subjects

Adult, Botulinum Toxins pharmacology, Botulism diagnosis, Electric Stimulation, Electrodiagnosis, Electromyography, Evoked Potentials, Female, Humans, Male, Middle Aged, Motor Endplate physiopathology, Neuromuscular Junction drug effects, Botulism physiopathology, Muscle, Skeletal physiopathology, Neuromuscular Junction physiopathology

Published

1998

49. Antibody effector mechanisms in myasthenia gravis. The complement hypothesis.

Author

Richman DP, Agius MA, Kirvan CA, Gomez CM, Fairclough RH, Dupont BL, and Maselli RA

Subjects

Animals, Antibodies immunology, Antibodies, Monoclonal, Humans, Models, Immunological, Myasthenia Gravis physiopathology, Neuromuscular Junction physiopathology, Complement System Proteins immunology, Myasthenia Gravis immunology

Published

1998

50. Rhodamine-labeled alpha-bungarotoxin allows visualization of end plates in congenital end plate acetylcholinesterase deficiency (CEAD).

Author

Agius MA, Maselli RA, Zhu S, Fairclough RH, Lin MY, and Ellis W

Subjects

Adult, Bungarotoxins metabolism, Female, Humans, Neuromuscular Diseases congenital, Receptors, Cholinergic metabolism, Rhodamines, Acetylcholinesterase deficiency, Motor Endplate metabolism, Neuromuscular Diseases enzymology, Receptors, Cholinergic analysis

Published

1998