Your search keyword '"Berge A. Minassian"' showing total 23 results

1. Assessment of burden and segregation profiles of CNVs in patients with epilepsy

Author

Claudia Moreau, Frédérique Tremblay, Stefan Wolking, Alexandre Girard, Catherine Laprise, Fadi F. Hamdan, Jacques L. Michaud, Berge A. Minassian, Patrick Cossette, and Simon L. Girard

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Objective Microdeletions are associated with different forms of epilepsy but show incomplete penetrance, which is not well understood. We aimed to assess whether unmasked variants or double CNVs could explain incomplete penetrance. Methods We analyzed copy number variants (CNVs) in 603 patients with four different subgroups of epilepsy and 945 controls. CNVs were called from genotypes and validated on whole‐genome (WGS) or whole‐exome sequences (WES). CNV burden difference between patients and controls was obtained by fitting a logistic regression. CNV burden was assessed for small and large (>1 Mb) deletions and duplications and for deletions overlapping different gene sets. Results Large deletions were enriched in genetic generalized epilepsies (GGE) compared to controls. We also found enrichment of deletions in epilepsy genes and hotspots for GGE. We did not find truncating or functional variants that could have been unmasked by the deletions. We observed a double CNV hit in two patients. One patient also carried a de novo deletion in the 22q11.2 hotspot. Interpretation We could corroborate previous findings of an enrichment of large microdeletions and deletions in epilepsy genes in GGE. We could also replicate that microdeletions show incomplete penetrance. However, we could not validate the hypothesis of unmasked variants nor the hypothesis of double CNVs to explain the incomplete penetrance. We found a de novo CNV on 22q11.2 that could be of interest. We also observed GGE families carrying a deletion on 15q13.3 hotspot that could be investigated in the Quebec founder population.

Published

2022

2. GYS1 or PPP1R3C deficiency rescues murine adult polyglucosan body disease

Author

Erin E. Chown, Peixiang Wang, Xiaochu Zhao, Justin J. Crowder, Jordan W. Strober, Mitchell A. Sullivan, Yunlin Xue, Cody S. Bennett, Ami M. Perri, Bret M. Evers, Peter J. Roach, Anna A. Depaoli‐Roach, H. Orhan Akman, Bartholomew A. Pederson, and Berge A. Minassian

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Objective Adult polyglucosan body disease (APBD) is an adult‐onset neurological variant of glycogen storage disease type IV. APBD is caused by recessive mutations in the glycogen branching enzyme gene, and the consequent accumulation of poorly branched glycogen aggregates called polyglucosan bodies in the nervous system. There are presently no treatments for APBD. Here, we test whether downregulation of glycogen synthesis is therapeutic in a mouse model of the disease. Methods We characterized the effects of knocking out two pro‐glycogenic proteins in an APBD mouse model. APBD mice were crossed with mice deficient in glycogen synthase (GYS1), or mice deficient in protein phosphatase 1 regulatory subunit 3C (PPP1R3C), a protein involved in the activation of GYS1. Phenotypic and histological parameters were analyzed and glycogen was quantified. Results APBD mice deficient in GYS1 or PPP1R3C demonstrated improvements in life span, morphology, and behavioral assays of neuromuscular function. Histological analysis revealed a reduction in polyglucosan body accumulation and of astro‐ and micro‐gliosis in the brains of GYS1‐ and PPP1R3C‐deficient APBD mice. Brain glycogen quantification confirmed the reduction in abnormal glycogen accumulation. Analysis of skeletal muscle, heart, and liver found that GYS1 deficiency reduced polyglucosan body accumulation in all three tissues and PPP1R3C knockout reduced skeletal muscle polyglucosan bodies. Interpretation GYS1 and PPP1R3C are effective therapeutic targets in the APBD mouse model. These findings represent a critical step toward the development of a treatment for APBD and potentially other glycogen storage disease type IV patients.

Published

2020

3. Epilepsy phenotype in individuals with chromosomal duplication encompassing FGF12

Author

Marjolein H. Willemsen, Himanshu Goel, Judith S. Verhoeven, Hilde M. H. Braakman, Nicole deLeeuw, Alison Freeth, and Berge A. Minassian

Subjects

developmental regression, epilepsy, FGF12, intellectual disability, LINE, microduplication 3q28q29, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Intragenic mutations in FGF12 are associated with intractable seizures, developmental regression, intellectual disability, ataxia, hypotonia, and feeding difficulties. FGF12 duplications are rarely reported, but it was suggested that those might have a similar gain‐of‐function effect and lead to a more or less comparable phenotype. A favorable response to the sodium blocker phenytoin was reported in several cases, both in patients with an intragenic mutation and in patients with a duplication of FGF12. We report three individuals from two families with FGF12 duplications. The duplications are flanked and probably mediated by two long interspersed nuclear elements (LINEs). The duplication cases show phenotypic overlap with the cases with intragenic mutations. Though the onset of epilepsy might be later, after the onset of seizures both groups show developmental stagnation and regression in several cases. This illustrates and further confirms that chromosomal FGF12 duplications and intragenic gain‐of‐function mutations yield overlapping phenotypes.

Published

2020

4. GYS1 or PPP1R3C deficiency rescues murine adult polyglucosan body disease

Author

Justin J. Crowder, Erin E. Chown, Bret M. Evers, Mitchell A. Sullivan, Jordan W. Strober, Bartholomew A. Pederson, Peter J. Roach, Berge A. Minassian, Cody S. Bennett, Xiaochu Zhao, Anna A. DePaoli-Roach, H. Orhan Akman, Ami M. Perri, Yunlin Xue, and Peixiang Wang

Subjects

0301 basic medicine, medicine.medical_specialty, Neurosciences. Biological psychiatry. Neuropsychiatry, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Downregulation and upregulation, Internal medicine, medicine, Glycogen branching enzyme, Animals, Glycogen storage disease type IV, Glycogen synthase, RC346-429, Research Articles, Mice, Knockout, biology, Glycogen, Behavior, Animal, business.industry, General Neuroscience, Intracellular Signaling Peptides and Proteins, Skeletal muscle, Protein phosphatase 1, Adult polyglucosan body disease, medicine.disease, Glycogen Storage Disease, Disease Models, Animal, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Glycogen Synthase, chemistry, biology.protein, Neurology (clinical), Neurology. Diseases of the nervous system, Nervous System Diseases, business, 030217 neurology & neurosurgery, Research Article, RC321-571

Abstract

Objective Adult polyglucosan body disease (APBD) is an adult‐onset neurological variant of glycogen storage disease type IV. APBD is caused by recessive mutations in the glycogen branching enzyme gene, and the consequent accumulation of poorly branched glycogen aggregates called polyglucosan bodies in the nervous system. There are presently no treatments for APBD. Here, we test whether downregulation of glycogen synthesis is therapeutic in a mouse model of the disease. Methods We characterized the effects of knocking out two pro‐glycogenic proteins in an APBD mouse model. APBD mice were crossed with mice deficient in glycogen synthase (GYS1), or mice deficient in protein phosphatase 1 regulatory subunit 3C (PPP1R3C), a protein involved in the activation of GYS1. Phenotypic and histological parameters were analyzed and glycogen was quantified. Results APBD mice deficient in GYS1 or PPP1R3C demonstrated improvements in life span, morphology, and behavioral assays of neuromuscular function. Histological analysis revealed a reduction in polyglucosan body accumulation and of astro‐ and micro‐gliosis in the brains of GYS1‐ and PPP1R3C‐deficient APBD mice. Brain glycogen quantification confirmed the reduction in abnormal glycogen accumulation. Analysis of skeletal muscle, heart, and liver found that GYS1 deficiency reduced polyglucosan body accumulation in all three tissues and PPP1R3C knockout reduced skeletal muscle polyglucosan bodies. Interpretation GYS1 and PPP1R3C are effective therapeutic targets in the APBD mouse model. These findings represent a critical step toward the development of a treatment for APBD and potentially other glycogen storage disease type IV patients.

Published

2020

5. Both gain‐of‐function and loss‐of‐functionde novo<scp>CACNA</scp>1Amutations cause severe developmental epileptic encephalopathies in the spectrum of Lennox‐Gastaut syndrome

Author

Nazzareno D'Avanzo, Tyler Mark Pierson, Elsa Rossignol, Mathieu Lachance, Berge A. Minassian, Julie Pepin, Praveen K. Raju, Jean-Claude Lacaille, François Dubeau, Xiao Jiang, Luis Bello-Espinosa, and Wendy G. Mitchell

Subjects

Male, 0301 basic medicine, Patch-Clamp Techniques, Mutant, Biology, Immunofluorescence, Cav2.1, Mice, 03 medical and health sciences, Epilepsy, 0302 clinical medicine, Loss of Function Mutation, medicine, Animals, Humans, Cells, Cultured, Loss function, Genetics, Brain Diseases, medicine.diagnostic_test, Lennox Gastaut Syndrome, Genetic heterogeneity, HEK 293 cells, Infant, Newborn, Infant, medicine.disease, HEK293 Cells, Phenotype, 030104 developmental biology, Neurology, Gain of Function Mutation, biology.protein, Female, Calcium Channels, Neurology (clinical), Spasms, Infantile, 030217 neurology & neurosurgery, Lennox–Gastaut syndrome

Abstract

Objective Developmental epileptic encephalopathies (DEEs) are genetically heterogeneous severe childhood-onset epilepsies with developmental delay or cognitive deficits. In this study, we explored the pathogenic mechanisms of DEE-associated de novo mutations in the CACNA1A gene. Methods We studied the functional impact of four de novo DEE-associated CACNA1A mutations, including the previously described p.A713T variant and three novel variants (p.V1396M, p.G230V, and p.I1357S). Mutant cDNAs were expressed in HEK293 cells, and whole-cell voltage-clamp recordings were conducted to test the impacts on CaV 2.1 channel function. Channel localization and structure were assessed with immunofluorescence microscopy and three-dimensional (3D) modeling. Results We find that the G230V and I1357S mutations result in loss-of-function effects with reduced whole-cell current densities and decreased channel expression at the cell membrane. By contrast, the A713T and V1396M variants resulted in gain-of-function effects with increased whole-cell currents and facilitated current activation (hyperpolarized shift). The A713T variant also resulted in slower current decay. 3D modeling predicts conformational changes favoring channel opening for A713T and V1396M. Significance Our findings suggest that both gain-of-function and loss-of-function CACNA1A mutations are associated with similarly severe DEEs and that functional validation is required to clarify the underlying molecular mechanisms and to guide therapies.

Published

2019

6. MYORG is associated with recessive primary familial brain calcification

Author

Vardiella Meiner, Alexander Lossos, David Arkadir, Muneer Abu Snineh, Dolev Rahat, Silvia Nitschke, Ora Schueler-Furman, Yuval Tabach, Israela Lerer, Yair Sadaka, and Berge A. Minassian

Subjects

0301 basic medicine, Genetics, Candidate gene, Mutation, business.industry, General Neuroscience, medicine.disease, medicine.disease_cause, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Protein sequencing, Anion transmembrane transport, medicine, Phylogenetic profiling, Neurology (clinical), business, Gene, Research Articles, 030217 neurology & neurosurgery, Exome sequencing, Research Article, Calcification

Abstract

Objective To investigate the genetic basis of the recessive form of primary familial brain calcification and study pathways linking a novel gene with known dominant genes that cause the disease. Methods Whole exome sequencing and Sanger‐based segregation analysis were used to identify possible disease causing mutations. Mutation pathogenicity was validated by structural protein modeling. Functional associations between the candidate gene, MYORG, and genes previously implicated in the disease were examined through phylogenetic profiling. Results We studied nine affected individuals from two unrelated families of Middle Eastern origin. The median age of symptom onset was 29.5 years (range 21–57 years) and dysarthria was the most common presenting symptom. We identified in the MYORG gene, a homozygous c.1233delC mutation in one family and c.1060_1062delGAC mutation in another. The first mutation results in protein truncation and the second in deletion of a highly conserved aspartic acid that is likely to disrupt binding of the protein with its substrate. Phylogenetic profiling analysis of the MYORG protein sequence suggests co‐evolution with a number of calcium channels as well as other proteins related to regulation of anion transmembrane transport (False Discovery Rate, FDR < 10−8) and with PDCD6IP, a protein interacting with PDGFR β which is known to be involved in the disease. Interpretation MYORG mutations are linked to a recessive form of primary familial brain calcification. This association was recently described in patients of Chinese ancestry. We suggest the possibility that MYORG mutations lead to calcification in a PDGFR β‐related pathway.

Published

2018

7. Extraneurological sparing in long-lived typical Lafora disease

Author

Berge A. Minassian and Danielle Goldsmith

Subjects

0301 basic medicine, Adult polyglucosan disease, Pediatrics, medicine.medical_specialty, Genetic enhancement, Central nervous system, Lafora disease, 03 medical and health sciences, Epilepsy, Gene therapy, 0302 clinical medicine, Neurological Damage, Gene replacement, medicine, Short Research Article, Dementia, business.industry, medicine.disease, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Neurology, Neurology (clinical), medicine.symptom, business, Myoclonus, 030217 neurology & neurosurgery

Abstract

Summary Lafora disease (LD) clinically appears in previously healthy teenagers as progressively worsening seizures, myoclonus, dementia, and ultimately a vegetative state leading to death within a decade of its onset. Here we present a typical case of LD in which the patient survived until the age of 40. Although the patient's brain was severely affected, other organs remained functional until her death. The field of LD research is approaching potentially curative therapies (eg, with antisense oligonucleotides or gene replacement) targeting only the central nervous system (CNS). Our case provides anecdotal evidence suggesting that a patient with typical LD can retain full bodily health aside from the effects of neurological damage.

Published

2018

8. Neuronal ceroid lipofuscinoses

Author

Berge A. Minassian, Dragos A. Nita, and Sara E. Mole

Subjects

0301 basic medicine, Batten disease, KCTD7, PPT1, General Medicine, Biology, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, nervous system, Neurology, Neuronal Ceroid-Lipofuscinoses, CLN8, medicine, DNAJC5, Humans, Myoclonic epilepsy, Cerebellar atrophy, Neurology (clinical), Cognitive decline, Neuroscience, 030217 neurology & neurosurgery

Abstract

The neuronal ceroid lipofuscinoses (NCL) are neurodegenerative conditions that associate cognitive decline, progressive cerebellar atrophy, retinopathy, and myoclonic epilepsy. NCL result from the excessive accumulation of neuronal and extraneuronal lipopigments, despite having diverse underlying biochemical aetiologies. Here we review the clinical presentation, pathophysiology and genetics of these conditions as well as the approach to diagnosis and management.

Published

2016

9. Diagnostic yield of genetic testing in epileptic encephalopathy in childhood

Author

O. Carter Snead, Jeff Kobayashi, Berge A. Minassian, Dawn Cordeiro, David F. Callen, Cecil D. Hahn, Stacy Hewson, Saadet Mercimek-Mahmutoglu, Jaina Patel, Mahendranath Moharir, Rosanna Weksberg, Komudi Siriwardena, Shelly K. Weiss, Elizabeth J. Donner, and Peter Kannu

Subjects

Male, Pathology, medicine.medical_specialty, Sodium-Hydrogen Exchangers, Adolescent, Methylenetetrahydrofolate reductase deficiency, Developmental Disabilities, Biology, Glycine encephalopathy, Bioinformatics, Cohort Studies, Epilepsy, Munc18 Proteins, Molecular genetics, medicine, Humans, KCNQ2 Potassium Channel, Genetic Predisposition to Disease, Global developmental delay, Child, Pyridoxine-dependent epilepsy, Genetic testing, NAV1.2 Voltage-Gated Sodium Channel, medicine.diagnostic_test, Infant, Cadherins, medicine.disease, Protocadherins, Neurology, Child, Preschool, Mutation, Female, Menkes disease, Neurology (clinical), Cognition Disorders, Spasms, Infantile

Abstract

SummaryObjective Epilepsy is a common neurologic disorder of childhood. To determine the genetic diagnostic yield in epileptic encephalopathy, we performed a retrospective cohort study in a single epilepsy genetics clinic. Methods We included all patients with intractable epilepsy, global developmental delay, and cognitive dysfunction seen between January 2012 and June 2014 in the Epilepsy Genetics Clinic. Electronic patient charts were reviewed for clinical features, neuroimaging, biochemical investigations, and molecular genetic investigations including targeted next-generation sequencing of epileptic encephalopathy genes. Results Genetic causes were identified in 28% of the 110 patients: 7% had inherited metabolic disorders including pyridoxine dependent epilepsy caused by ALDH7A1 mutation, Menkes disease, pyridox(am)ine-5-phosphate oxidase deficiency, cobalamin G deficiency, methylenetetrahydrofolate reductase deficiency, glucose transporter 1 deficiency, glycine encephalopathy, and pyruvate dehydrogenase complex deficiency; 21% had other genetic causes including genetic syndromes, pathogenic copy number variants on array comparative genomic hybridization, and epileptic encephalopathy related to mutations in the SCN1A, SCN2A, SCN8A, KCNQ2, STXBP1, PCDH19, and SLC9A6 genes. Forty-five percent of patients obtained a genetic diagnosis by targeted next-generation sequencing epileptic encephalopathy panels. It is notable that 4.5% of patients had a treatable inherited metabolic disease. Significance To the best of our knowledge, this is the first study to combine inherited metabolic disorders and other genetic causes of epileptic encephalopathy. Targeted next-generation sequencing panels increased the genetic diagnostic yield from 25% in patients with epileptic encephalopathy.

Published

2015

10. NHLRC1 repeat expansion in two beagles with Lafora disease

Author

Peixiang Wang, Clare Rusbridge, I. Hajek, F. Kettner, V. Simerdova, Berge A. Minassian, and V. Palus

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Pathology, medicine.medical_specialty, 040301 veterinary sciences, business.industry, Repeat sequence, Genetic disorder, Genetic variants, 04 agricultural and veterinary sciences, Disease, medicine.disease, Lafora disease, 0403 veterinary science, 03 medical and health sciences, 030104 developmental biology, Carrier protein, Mutation (genetic algorithm), Medicine, Small Animals, business, Trinucleotide repeat expansion

Abstract

Lafora disease is a fatal genetic disorder characterised by neurotoxic deposits of malformed insoluble glycogen. In humans it is caused by mutation in the EPM2A or NHLRC1 genes. There is a known mutation in miniature wirehaired dachshunds which has not been documented in other dog breeds, including beagles, in which the disease is relatively commonly reported. This case report describes the causative defect in two affected beagles, namely the same massive expansion as in miniature wirehaired dachshunds of a 12-nucleotide repeat sequence that is unique to the canine NHLRC1 gene. This is the first mutation described in beagles with Lafora disease, and so far the only Lafora disease genetic variant in dogs.

Published

2016

11. Infantile spasms with periventricular nodular heterotopia, unbalanced chromosomal translocation 3p26.2 ‐10p15.1 and 6q22.31 duplication

Author

Kevin Jones, Berge A. Minassian, and Shelly K. Weiss

Subjects

0301 basic medicine, Candidate gene, Pathology, medicine.medical_specialty, Infantile spasms, Microarray, business.industry, Periventricular Nodular Heterotopia, periventricular nodular heterotopia, Case Report, Chromosomal translocation, Case Reports, personalized medicine, General Medicine, Disease, 030105 genetics & heredity, 03 medical and health sciences, 0302 clinical medicine, Gene duplication, Medicine, Personalized medicine, Copy-number variation, business, 030217 neurology & neurosurgery

Abstract

Key Clinical Message Patients presenting with infantile spasms, dysmorphic features, and periventricular nodular heterotopia may benefit from genetic copy number variation microarray, or whole‐exome sequencing to identify candidate genes. This will allow personalized diagnosis and prognostication and the eventual understanding of single and combined gene functions in brain health and disease.

Published

2016

12. Absent CNKSR2 causes seizures and intellectual, attention, and language deficits

Author

Tove B. Haaland, Mary Lou Smith, Sarah Bowdin, Katja S. Brocke-Holmefjord, Gunnar Houge, Stephen W. Scherer, Katia J. Sinopoli, Brigitte Gilbert-Dussardier, Emmanuelle Lagrue, Christian R. Marshall, Catherine Vincent-Delorme, Susan Walker, Berge A. Minassian, Vera M. Kalscheuer, Andrea K. Vaags, Cindy Gilles, and Radu Harbuz

Subjects

Disease, medicine.disease, Synapse, Epilepsy, Synaptic function, Neurology, Intellectual disability, medicine, CNKSR2, Neurology (clinical), Early childhood, Psychology, Neuroscience, Brain function

Abstract

Synaptic function is central to brain function. Understanding the synapse is aided by studies of patients lacking individual synaptic proteins. Common neurological diseases are genetically complex. Their understanding is likewise simplified by studies of less common monogenic forms. We detail the disease caused by absence of the synaptic protein CNKSR2 in 8 patients ranging from 6 to 62 years old. The disease is characterized by intellectual disability, attention problems, and abrupt lifelong language loss following a brief early childhood epilepsy with continuous spike-waves in sleep. This study describes the phenotype of CNKSR2 deficiency and its involvement in systems underlying common neurological disorders. Ann Neurol 2014;76:758–764

Published

2014

13. Late adult-onset of X-linked myopathy with excessive autophagy

Author

Cameron D. Crockett, Alessandra Ruggieri, Berge A. Minassian, Christopher M. Zallek, Nivetha Ramachandran, Steven A. Moore, and Meena Gujrati

Subjects

Autophagosome, Pathology, medicine.medical_specialty, Muscle biopsy, medicine.diagnostic_test, Physiology, Autophagy, Muscle weakness, Anatomy, Biology, Cellular and Molecular Neuroscience, X-linked myopathy with excessive autophagy, medicine.anatomical_structure, Physiology (medical), Lysosome, medicine, Progressive proximal muscle weakness, Neurology (clinical), medicine.symptom, Myopathy

Abstract

Introduction: X-linked myopathy with excessive autophagy (XMEA) is characterized by autophagic vacuoles with sarcolemmal features. Mutations in VMA21 result in insufficient lysosome acidification, causing progressive proximal weakness with onset before age 20 years and loss of ambulation by middle age. Methods: We describe a patient with onset of slowly progressive proximal weakness of the lower limbs after age 50, who maintains ambulation with the assistance of a cane at age 71. Results: Muscle biopsy at age 66 showed complex muscle fiber splitting, internalized capillaries, and vacuolar changes characteristic of autophagic vacuolar myopathy. Vacuoles stained positive for sarcolemmal proteins, LAMP2, and complement C5b-9. Ultrastructural evaluation further revealed basal lamina reduplication and extensive autophagosome extrusion. Sanger sequencing identified a known pathologic splice site mutation in VMA21 (c.164–7T>G). Conclusions: This case expands the clinical phenotype of XMEA and suggests VMA21 sequencing be considered in evaluating men with LAMP2-positive autophagic vacuolar myopathy. Muscle Nerve 50: 138–144, 2014

Published

2014

14. Novel exon 1 mutations in MECP2 implicate isoform MeCP2_e1 in classical Rett syndrome

Author

Carol J Saunders, Eva W.C. Chow, John B. Vincent, Weiwei Zhao, and Berge E. Minassian

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Methyl-CpG-Binding Protein 2, Mutation, Missense, Codon, Initiator, Rett syndrome, Biology, medicine.disease_cause, Frameshift mutation, MECP2, Young Adult, Exon, Start codon, Rett Syndrome, Genetics, medicine, Humans, Protein Isoforms, Missense mutation, Child, Genetics (clinical), Mutation, Splice site mutation, Exons, medicine.disease, Female

Abstract

Rett syndrome (RTT) is a neurodevelopmental disorder caused by mutations in the X-linked MECP2 gene. Recently, a new MeCP2 isoform was described, MeCP2_e1, which skips exon 2 and has an alternative N-terminus, translated from exon 1, whereas MeCP2_e2 is translated from a start codon in exon 2. Since the incorporation of exon 1 into standard sequencing protocols for RTT, few exon 1 mutations have been described and are thus assumed to be only rare causes of RTT. Also, studies have suggested that the frameshift mutations identified in exon 1 affect both isoforms. Our aim in this study was to assess the frequency of mutations in exon 1, their relationship to phenotype, and the implications on the etiological role for the isoform MeCP2_e1 in RTT, versus the previously described isoform, MeCP2_e2. We sequenced MECP2 in 51 females with various clinical presentations, including developmental delay, autism, atypical and classical RTT, referred to our laboratories for testing. In patients with identified mutations, X-chromosome inactivation was analyzed. We identified four patients with exon 1 mutations; three were novel (c.1A > T; c.1A > G; c.5C > T), two of which affected the start codon, one a missense change, and one patient had a previously reported splice site mutation, c.62 + 1delGT. The four patients fit criteria for classical RTT, and thus these findings add support to previous reports that exon 1 mutations may be associated with a severe phenotype. Also, these findings add significant weight to the mounting evidence suggesting that the MeCP2_e1 isoform is the etiologically relevant form of the protein.

Published

2009

15. Sequence variants within exon 1 ofMECP2 occur in females with mental retardation

Author

Chris G, Harvey, Sailesh D, Menon, Beata, Stachowiak, Abdul, Noor, Adam, Proctor, Albert K, Mensah, Gevork N, Mnatzakanian, Simon E, Alfred, Ray, Guo, Stephen W, Scherer, James L, Kennedy, Wendy, Roberts, Anand K, Srivastava, Anand K, Srivistava, Berge A, Minassian, and John B, Vincent

Subjects

Adult, Male, Methyl-CpG-Binding Protein 2, DNA Mutational Analysis, Molecular Sequence Data, Rett syndrome, Biology, Polymorphism, Single Nucleotide, MECP2, Cellular and Molecular Neuroscience, Exon, Trinucleotide Repeats, Intellectual Disability, medicine, Humans, Coding region, Amino Acid Sequence, Autistic Disorder, Gene, Genetics (clinical), Sequence (medicine), Genetics, Sex Characteristics, Alanine, Base Sequence, Alternative splicing, Exons, medicine.disease, Psychiatry and Mental health, Case-Control Studies, Female, Trinucleotide repeat expansion

Abstract

A new splice variant of the Rett syndrome gene, MECP2, was recently identified, that includes coding sequence from exon 1, and is the predominant transcript in the central nervous system. This sequence encodes polyalanine and polyglycine stretches within the N-terminal portion of MeCP2, and may confer novel functional properties to the protein. We screened autism, mental retardation (MR), and control populations for sequence variation within this region, and identified variation in ∼1% of MR cases screened (N = 1,410). No variants were identified in the autism sample (N = 401). Most of these variants occur within a trinucleotide repeat region and result in change in number of alanine or glycine residues within the repeat stretches. We suggest some of these variants may be a relatively frequent cause of non-specific MR or developmental delay. © 2006 Wiley-Liss, Inc.

Published

2007

16. Electrophysiological findings in X-linked myopathy with excessive autophagy

Author

Satu K. Jääskeläinen, Hannu Kalimo, Berge A. Minassian, Bjarne Udd, Marcello Villanova, Rocco Liguori, Pekka Niemi, Vern C. Juel, and Björn Falck

Subjects

Pathology, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Myotonic discharges, Autophagy, Magnetic resonance imaging, Electromyography, X-linked myopathy with excessive autophagy, Electrophysiology, Neurology, Electroneuronography, medicine, Neurology (clinical), medicine.symptom, Myopathy, business

Abstract

We report electrophysiological features and magnetic resonance imaging muscle findings in 4 patients and 1 female carrier of X-linked myopathy with excessive autophagy. Motor units were polyphasic with high mean amplitude and normal duration. The thigh muscles were most severely involved, but myotonic discharges were abundant in both clinically affected and unaffected muscles. Along with the clinicopathological features, these electrophysiological findings distinguish X-linked myopathy with excessive autophagy from other limb-girdle myopathies.

Published

2002

17. Laforin is a cell membrane and endoplasmic reticulum-associated protein tyrosine phosphatase

Author

Cameron Ackerley, Danielle M. Andrade, Edwin J. Young, Stephen W. Scherer, Leonarda Ianzano, Elayne Chan, and Berge A. Minassian

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Endoplasmic reticulum, Protein tyrosine phosphatase, Progressive myoclonus epilepsy, Biology, medicine.disease, Lafora disease, Cell biology, Cell membrane, medicine.anatomical_structure, nervous system, Neurology, Biochemistry, Gene expression, medicine, Neurology (clinical), medicine.symptom, Laforin, Myoclonus

Abstract

Lafora disease (LD) is the only progressive myoclonus epilepsy with polyglucosan bodies. Among conditions with polyglucosan bodies, LD is unique for the subcellular location of its polyglucosans in neuronal perikarya and dendrites and not in axons. Here we report that the protein encoded by the EPM2A gene, which is mutated in LD, localizes at the plasma membrane and the endoplasmic reticulum and that it is a functional protein tyrosine phosphatase. The significance of these findings in the epilepsy of LD and in the origin and characteristic subcellular location of Lafora bodies is discussed.

Published

2001

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

Author

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

Subjects

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

Abstract

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

Published

2000

19. Magnetoencephalographic localization in pediatric epilepsy surgery: Comparison with invasive intracranial electroencephalography

Author

James T. Rutka, Hiroshi Otsubo, Irene Elliott, Berge A. Minassian, Shelly K. Weiss, and O. Carter Snead

Subjects

medicine.medical_specialty, Anatomical location, medicine.diagnostic_test, Magnetoencephalography, Electroencephalography, medicine.disease, nervous system diseases, Surgery, Central nervous system disease, Epilepsy, medicine.anatomical_structure, nervous system, Neurology, Cortex (anatomy), medicine, Epilepsy surgery, Ictal, Neurology (clinical), Psychology

Abstract

The object of this study was to determine the concordance of the anatomical location of interictal magnetoencephalographic (MEG) spike foci with the location of ictal onset zones identified by invasive ictal intracranial electroencephalographic recordings in children undergoing evaluation for epilepsy surgery. MEG was performed in 11 children with intractable, nonlesional, extratemporal, localization-related epilepsy. Subsequently, chronic invasive intracranial electroencephalographic monitoring was performed by using subdural electrodes to localize the ictal onset zone and eloquent cortex. Based on the invasive monitoring data, all children had excision of, or multiple subpial transections through, ictal onset cortex and surrounding irritative zones. In 10 of 11 patients, the anatomical location of the epileptiform discharges as determined by MEG corresponded to the ictal onset zone established by ictal intracranial recordings. In all children, the anatomical location of the somatosensory hand area, determined by functional mapping through the subdural electrode array, was the same as that delineated by MEG. Nine of 11 patients became either seizure-free or had a greater than 90% reduction in seizures after surgery, with a mean follow-up of 24 months. MEG is a powerful and accurate tool in the presurgical evaluation of children with refractory nonlesional extratemporal epilepsy.

Published

1999

20. Genetic locus heterogeneity in Lafora's progressive myoclonus epilepsy

Author

Cathy L. Barr, Antonio V. Delgado-Escueta, Steve W. Scherer, A. V. Sanghvi, Saeed Bohlega, José M. Serratosa, Manyee N. Gee, Berge A. Minassian, Stirling Carpenter, Guy Geoffroy, Lise M. Sakamoto, Jesús Sainz, Karen Wigg, and Uwamie Tomiyasu

Subjects

Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Pathology, medicine.medical_specialty, business.industry, Haplotype, Protein Tyrosine Phosphatase Gene, Locus (genetics), Progressive myoclonus epilepsy, medicine.disease, Degenerative disease, Neurology, medicine, Neurology (clinical), business, Gene, Lafora body, Lod scores

Abstract

In 1995, we mapped a gene for Lafora's progressive myoclonus epilepsy in chromosome 6q23-25. In 1997 and 1998, we reduced the size of the locus to 300 kb, and an international collaboration identified mutations in the protein tyrosine phosphatase gene. Here, we examine for heterogeneity through the admixture test in 22 families and estimate the proportion of linked families to be 75 to 85%. Extremely low posterior probabilities of linkage (Wi), exclusionary LOD scores, and haplotypes identify 4 families unlikely to be linked to chromosome 6q24.

Published

1999

21. Inhibiting glycogen synthesis prevents lafora disease in a mouse model

Author

Paul W. Frankland, Xiaochu Zhao, Staci A. Weaver, Nela Pencea, Berge A. Minassian, Bartholomew A. Pederson, Peter J. Roach, Julie Turnbull, Jonathan R. Epp, and Cameron Ackerley

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Mice, 129 Strain, Progressive myoclonus epilepsy, Biology, Article, Lafora disease, Gene Knockout Techniques, Mice, Glycogen phosphorylase, chemistry.chemical_compound, Internal medicine, medicine, Animals, Glycogen synthase, Mice, Knockout, Glycogen, Kinase, Neurodegeneration, Protein Tyrosine Phosphatases, Non-Receptor, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Glycogen Synthase, Endocrinology, Lafora Disease, Neurology, chemistry, biology.protein, Dual-Specificity Phosphatases, Neurology (clinical), Laforin

Abstract

Lafora disease (LD) is the major teenage-onset progressive myoclonus epilepsy (PME). Insidious cognitive decline and escalating myoclonic, visual, convulsive, and other seizures follow an initial decade of normal development. Within a few years, seizures are intractable, myoclonic absences are near constant, and a disinhibited dementia has set in. A vegetative state with continuous myoclonus characterizes the final stage and most patients die in status epilepticus before age 301. The neuropathology of LD is characterized by progressive formation and growth of Lafora bodies (LB) in neuronal somata and processes, and by neurodegeneration1. LB are composed of aggregates of a variety of proteins and an abnormal form of glycogen that lacks normal glycogen’s normal branching and spherical structure essential to its solubility. The abnormal glycogen, called polyglucosan, makes up over 70% of a LB2. Whether LB are pathogenic, or a mere epiphenotype, remains uncertain. LD is caused by loss of function of either of two interacting enzymes, malin, a ubiquitin E3 ligase, and laforin, a phosphatase3. Malin regulates the amount of laforin, and laforin regulates glycogen phosphorylation. The latter is essential to normal glycogen structure, through mechanisms that remain poorly defined3–5. Based mostly on cell culture experiments, several additional functions, unrelated to glycogen metabolism, have been tentatively attributed to laforin and malin, including tau kinase dephosphorylation, Wnt signaling regulation, and others6–9. It is possible that loss of one or more of these functions, rather than effects on glycogen metabolism and LB formation, underlie the neurodegeneration and PME of LD. PTG is an adaptor protein that mediates dephosphorylation of the glycogen synthesizing (glycogen synthase; GS) and degrading (glycogen phosphorylase; GP) enzymes by the pleiotropic phosphatase PP1, which activates GS, inactivates GP, and thus increases glycogen production10. We recently hypothesized that, malstructured though they are, polyglucosans are glycogen, and reducing glycogen synthesis might reduce LB formation, which, if LB cause the disease, might prevent LD. As a test of this hypothesis, we removed PTG from the laforin-deficient mouse model of LD (laforin knockout; LKO) by crossing PTG knockout mice with the LD mice. This resulted in drastic reduction of LB and rescued the neurodegeneration of the LD mice11. While these results supported the view that LB are pathogenic, there remained the possibility that PTG has adaptor or other functions outside of glycogen metabolism and that its removal prevented neurodegeneration through pathways unrelated to glycogen metabolism and LB. Furthermore, the study was of short duration and did not assess whether the correction of the neurodegeneration is maintained. To address these two issues, we removed GS itself from LKO mice and found that the absence of glycogen synthesis alone was sufficient to prevent LB formation, neurodegeneration, and seizure susceptibility, and do so long-term.

Published

2013

22. Gene defects in progressive myoclonus epilepsy

Author

Subramaniam Ganesh, José M. Serratosa, and Berge A. Minassian

Subjects

Genetics, Pathology, medicine.medical_specialty, business.industry, Respiratory chain, Progressive myoclonus epilepsy, medicine.disease, Myoclonus epilepsy, Lafora disease, Atrophy, Degenerative disease, Neurology, Ragged-red fibers, medicine, Neurology (clinical), business, Gene

Abstract

Lafora disease (EPM2A and EPM2B genes); myoclonus epilepsy with ragged red fibers; or MERRF (mtDNA tRNA genes), and Dentatorubral-pallidoluysian atrophy or DRPLA (ATNI gene) are three severe forms of progressive myoclonus epilepsy. The corresponding gene defects have been identified and molecular diagnosis is now widely available. Recent advances in genetics and molecular biology offer promising venues toward the development of new therapies. For an expanded treatment of this topic see Jasper's Basic Mechanisms of the Epilepsies, Fourth Edition (Noebels JL, Avoli M, Rogawski MA, Olsen RW, Delgado-Escueta AV, eds) published by Oxford University Press (available on the National Library of Medicine Bookshelf [NCBI] at www.ncbi.nlm.nih.gov/ books).

Published

2010

23. Sequence variants within exon 1 of MECP2 occur in females with mental retardation. Am J Medical Genetics Part B (Neuropsychiatric Genetic) 144B:355–360 (2007)

Author

Abdul Noor, Gevork N. Mnatzakanian, Stephen W. Scherer, James L. Kennedy, Anand K. Srivastava, John B. Vincent, Ray Guo, Wendy Roberts, Sailesh D. Menon, Beata Stachowiak, Chris G. Harvey, Simon E. Alfred, Adam Proctor, Albert K. Mensah, and Berge A. Minassian

Subjects

Genetics, Cellular and Molecular Neuroscience, Psychiatry and Mental health, medicine.medical_specialty, Exon, medicine, Medical genetics, Biology, Genetics (clinical), MECP2, Sequence (medicine)

Published

2007