Your search keyword '"Longman C"' showing total 12 results

1. Congenital muscular dystrophies in the UK population: Clinical and molecular spectrum of a large cohort diagnosed over a 12-year period.

Author

Sframeli M, Sarkozy A, Bertoli M, Astrea G, Hudson J, Scoto M, Mein R, Yau M, Phadke R, Feng L, Sewry C, Fen ANS, Longman C, McCullagh G, Straub V, Robb S, Manzur A, Bushby K, and Muntoni F

Subjects

Adaptor Proteins, Signal Transducing, Cell Cycle Proteins, Cohort Studies, Dystroglycans genetics, Dystroglycans metabolism, Female, Genetic Testing, Humans, Male, Muscular Dystrophies classification, N-Acetylgalactosaminyltransferases genetics, Nuclear Proteins metabolism, Nucleotidyltransferases genetics, Sclerosis epidemiology, Sclerosis genetics, Trans-Activators metabolism, United Kingdom epidemiology, Laminin genetics, Muscular Dystrophies epidemiology, Muscular Dystrophies genetics, Mutation genetics, Nuclear Proteins genetics, Trans-Activators genetics

Abstract

Congenital muscular dystrophies (CMDs) are clinically and genetically heterogeneous conditions; some fatal in the first few years of life and with central nervous system involvement, whereas others present a milder course. We provide a comprehensive report of the relative frequency and clinical and genetic spectrum of CMD in the UK. Genetic analysis of CMD genes in the UK is centralised in London and Newcastle. Between 2001 and 2013, a genetically confirmed diagnosis of CMD was obtained for 249 unrelated individuals referred to these services. The most common CMD subtype was laminin-α2 related CMD (also known as MDC1A, 37.4%), followed by dystroglycanopathies (26.5%), Ullrich-CMD (15.7%), SEPN1 (11.65%) and LMNA (8.8%) gene related CMDs. The most common dystroglycanopathy phenotype was muscle-eye-brain-like disease. Fifteen patients carried mutations in the recently discovered ISPD, GMPPB and B3GALNT2 genes. Pathogenic allelic mutations in one of the CMD genes were also found in 169 unrelated patients with milder phenotypes, such as limb girdle muscular dystrophy and Bethlem myopathy. In all, we identified 362 mutations, 160 of which were novel. Our results provide one of the most comprehensive reports on genetics and clinical features of CMD subtypes and should help diagnosis and counselling of families with this group of conditions., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

2. Recessive desmin-null muscular dystrophy with central nuclei and mitochondrial abnormalities.

Author

Henderson M, De Waele L, Hudson J, Eagle M, Sewry C, Marsh J, Charlton R, He L, Blakely EL, Horrocks I, Stewart W, Taylor RW, Longman C, Bushby K, and Barresi R

Subjects

Child, Child, Preschool, Desmin genetics, Female, Humans, Intermediate Filaments metabolism, Intermediate Filaments pathology, Male, Mitochondria, Muscle metabolism, Mitochondria, Muscle pathology, Muscular Dystrophies genetics, Muscular Dystrophies metabolism, Desmin metabolism, Muscular Dystrophies diagnosis

Published

2013

3. ISPD gene mutations are a common cause of congenital and limb-girdle muscular dystrophies.

Author

Cirak S, Foley AR, Herrmann R, Willer T, Yau S, Stevens E, Torelli S, Brodd L, Kamynina A, Vondracek P, Roper H, Longman C, Korinthenberg R, Marrosu G, Nürnberg P, Michele DE, Plagnol V, Hurles M, Moore SA, Sewry CA, Campbell KP, Voit T, and Muntoni F

Subjects

Adolescent, Child, Child, Preschool, Dystroglycans genetics, Dystroglycans metabolism, Female, Glycosylation, Humans, Magnetic Resonance Imaging, Male, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Muscular Dystrophies metabolism, Muscular Dystrophies pathology, Muscular Dystrophies, Limb-Girdle genetics, Muscular Dystrophies, Limb-Girdle metabolism, Muscular Dystrophies, Limb-Girdle pathology, Young Adult, Muscular Dystrophies congenital, Muscular Dystrophies genetics, Mutation, Nucleotidyltransferases genetics

Abstract

Dystroglycanopathies are a clinically and genetically diverse group of recessively inherited conditions ranging from the most severe of the congenital muscular dystrophies, Walker-Warburg syndrome, to mild forms of adult-onset limb-girdle muscular dystrophy. Their hallmark is a reduction in the functional glycosylation of α-dystroglycan, which can be detected in muscle biopsies. An important part of this glycosylation is a unique O-mannosylation, essential for the interaction of α-dystroglycan with extracellular matrix proteins such as laminin-α2. Mutations in eight genes coding for proteins in the glycosylation pathway are responsible for ∼50% of dystroglycanopathy cases. Despite multiple efforts using traditional positional cloning, the causative genes for unsolved dystroglycanopathy cases have escaped discovery for several years. In a recent collaborative study, we discovered that loss-of-function recessive mutations in a novel gene, called isoprenoid synthase domain containing (ISPD), are a relatively common cause of Walker-Warburg syndrome. In this article, we report the involvement of the ISPD gene in milder dystroglycanopathy phenotypes ranging from congenital muscular dystrophy to limb-girdle muscular dystrophy and identified allelic ISPD variants in nine cases belonging to seven families. In two ambulant cases, there was evidence of structural brain involvement, whereas in seven, the clinical manifestation was restricted to a dystrophic skeletal muscle phenotype. Although the function of ISPD in mammals is not yet known, mutations in this gene clearly lead to a reduction in the functional glycosylation of α-dystroglycan, which not only causes the severe Walker-Warburg syndrome but is also a common cause of the milder forms of dystroglycanopathy.

Published

2013

4. Brain involvement in muscular dystrophies with defective dystroglycan glycosylation.

Author

Clement E, Mercuri E, Godfrey C, Smith J, Robb S, Kinali M, Straub V, Bushby K, Manzur A, Talim B, Cowan F, Quinlivan R, Klein A, Longman C, McWilliam R, Topaloglu H, Mein R, Abbs S, North K, Barkovich AJ, Rutherford M, and Muntoni F

Subjects

Adolescent, Brain metabolism, Child, Child, Preschool, Genetic Predisposition to Disease genetics, Glycosylation, Humans, Infant, Infant, Newborn, Magnetic Resonance Imaging, Mannosyltransferases genetics, Membrane Proteins genetics, Muscular Dystrophies metabolism, Mutation genetics, N-Acetylglucosaminyltransferases genetics, Nervous System Malformations metabolism, Phenotype, Brain abnormalities, Dystroglycans metabolism, Muscular Dystrophies complications, Muscular Dystrophies genetics, Nervous System Malformations diagnosis, Nervous System Malformations genetics

Abstract

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

Published

2008

5. Localisation of merosin-positive congenital muscular dystrophy to chromosome 4p16.3.

Author

Sellick GS, Longman C, Brockington M, Mahjneh I, Sagi L, Bushby K, Topaloğlu H, Muntoni F, and Houlston RS

Subjects

Chromosome Mapping methods, Female, Humans, Male, Middle Aged, Muscular Dystrophies congenital, Oligonucleotide Array Sequence Analysis methods, Pedigree, Quantitative Trait Loci genetics, Chromosome Disorders genetics, Chromosomes, Human, Pair 4 genetics, Laminin metabolism, Lod Score, Muscular Dystrophies genetics, Polymorphism, Single Nucleotide

Abstract

The congenital muscular dystrophies (CMD) are a heterogeneous group of autosomal recessive disorders, which present within the first 6 months of life with hypotonia, muscle weakness and contractures, associated with dystrophic changes on skeletal muscle biopsy. We have previously reported a large consanguineous family segregating merosin-positive congenital muscular dystrophy, in which involvement of known CMD loci was excluded. A genome-wide linkage search of the family conducted using microsatellite markers spaced at 10-Mb intervals failed to identify a disease locus. A second scan using a high-density SNP array, however, permitted a novel CMD locus on 4p16.3 to be identified (multipoint LOD score 3.4). Four additional consanguineous CMD families with a similar phenotype were evaluated for linkage to a 4.14-Mb interval on 4p16.3; however, none showed any evidence of linkage to the region. Our findings further illustrate the utility of highly informative SNP arrays compared with standard panels of microsatellite markers for the mapping of recessive disease loci.

Published

2005

6. Congenital muscular dystrophy.

Author

Mercuri E and Longman C

Subjects

Adaptor Proteins, Signal Transducing, Cell Cycle Proteins, Child, Collagen Type VI genetics, DNA-Binding Proteins genetics, Diagnosis, Differential, Education, Medical, Continuing, Humans, Laminin deficiency, Laminin genetics, Membrane Proteins, Muscle Proteins genetics, Muscular Dystrophies diagnosis, Mutation, N-Acetylglucosaminyltransferases genetics, Nuclear Proteins genetics, Pentosyltransferases, Proteins genetics, Selenoproteins genetics, Trans-Activators genetics, Muscular Dystrophies classification, Muscular Dystrophies genetics, Pediatrics education

Published

2005

7. Localization and functional analysis of the LARGE family of glycosyltransferases: significance for muscular dystrophy.

Author

Brockington M, Torelli S, Prandini P, Boito C, Dolatshad NF, Longman C, Brown SC, and Muntoni F

Subjects

Animals, Brain metabolism, Cricetinae, Dystroglycans metabolism, Fibroblasts enzymology, Glycosyltransferases genetics, Golgi Apparatus enzymology, Golgi Apparatus metabolism, Humans, Laminin metabolism, Mice, Multigene Family, Muscular Dystrophies genetics, Mutation, Myoblasts enzymology, Protein Structure, Tertiary, Glycosyltransferases metabolism, Muscular Dystrophies enzymology

Abstract

The dystroglycanopathies are a novel group of human muscular dystrophies due to mutations in known or putative glycosyltransferase enzymes. They share the common pathological feature of a hypoglycosylated form of alpha-dystroglycan, diminishing its ability to bind extracellular matrix ligands. The LARGE glycosyltransferase is mutated in both the myodystrophy mouse and congenital muscular dystrophy type 1D (MDC1D). We have transfected various cell lines with a variety of LARGE expression constructs in order to characterize their subcellular localization and effect on alpha-dystroglycan glycosylation. Wild-type LARGE co-localized with the Golgi marker GM130 and stimulated the production of highly glycosylated alpha-dystroglycan (hyperglycosylation). MDC1D mutants had no effect on alpha-dystroglycan glycosylation and failed to localize correctly, confirming their pathogenicity. The two predicted catalytic domains of LARGE contain three conserved DxD motifs. Systematically mutating each of these motifs to NNN resulted in the mislocalization of one construct, while all failed to have any effect on alpha-dystroglycan glycosylation. A construct lacking the transmembrane domain also failed to localize at the Golgi apparatus. These results indicate that LARGE needs to both physically interact with alpha-dystroglycan and function as a glycosyltransferase in order to stimulate alpha-dystroglycan hyperglycosylation. We have also cloned and overexpressed a homologue of LARGE, glycosyltransferase-like 1B (GYLTL1B). Like LARGE it localized to the Golgi apparatus and stimulated alpha-dystroglycan hyperglycosylation. These results suggest that GYLTL1B may be a candidate gene for muscular dystrophy and that its overexpression could compensate for the deficiency of both LARGE and other glycosyltransferases.

Published

2005

8. Antenatal and postnatal brain magnetic resonance imaging in muscle-eye-brain disease.

Author

Longman C, Mercuri E, Cowan F, Allsop J, Brockington M, Jimenez-Mallebrera C, Kumar S, Rutherford M, Toda T, and Muntoni F

Subjects

Brain abnormalities, Child, Preschool, Eye Abnormalities genetics, Eye Abnormalities pathology, Humans, Male, Muscular Dystrophies genetics, Muscular Dystrophies pathology, Nervous System Malformations diagnosis, Nervous System Malformations genetics, Nervous System Malformations pathology, Brain pathology, Eye Abnormalities diagnosis, Magnetic Resonance Imaging methods, Muscular Dystrophies diagnosis, Prenatal Diagnosis methods

Abstract

Background: Muscle-eye-brain disease (MEB) is a rare autosomal recessive disorder characterized by congenital muscular dystrophy, structural eye abnormalities, and type II lissencephaly. Previous reports of brain abnormalities on magnetic resonance images (MRIs) in MEB have been in children older than 1 year., Objective: To describe serial antenatal and postnatal brain MRIs in a child with MEB., Design: Case report., Patient: We report a 2-year-old white boy with genetically confirmed MEB. Antenatal MRIs at 25 and 35 weeks' gestation showed posterior ventriculomegaly but no cortical dysplasia. A postnatal brain MRI at age 1 week showed frontal cortical dysplasia and abnormal signal intensity within the frontal white matter. A brain MRI at 8 months showed bilateral frontoparietal polymicrogyria. All images demonstrated flattening of the pons and mild hypoplasia of the inferior vermis. The child had no weakness, and muscle involvement was only suspected when the serum creatine kinase level was found to be elevated at age 8 months., Conclusion: Cortical dysplasia in MEB may not be evident until several postnatal months; therefore, if MEB is suspected, brain MRI performed in the first few months of life should be interpreted with caution.

Published

2004

9. Congenital muscular dystrophy with short stature, proximal contractures and distal laxity.

Author

Mercuri E, Lampe A, Straub V, Yuva Y, Longman C, Wright M, Brown S, Sewry C, Bonnemann C, Kinali M, Brockington M, Hausser I, Hilton Jones D, Voit T, Bushby K, and Muntoni F

Subjects

Adolescent, Adult, Child, Humans, Intellectual Disability complications, Pedigree, Respiratory Insufficiency complications, Spinal Diseases complications, Body Height, Contracture complications, Joint Instability complications, Muscular Dystrophies complications, Muscular Dystrophies congenital

Abstract

We report 5 cases (2 familial and 3 sporadic) who share a diagnosis of congenital muscular dystrophy (CMD) in association with short stature, proximal contractures, rigidity of the spine and distal joint laxity as well as early respiratory failure and mild to moderate mental retardation. The expression of collagen VI was confirmed to be normal on muscle biopsies of all 5 patients and in the informative family linkage to any of the three COL6 A loci was excluded. These findings extend the phenotypes within the CMD classification.

Published

2004

10. Mutations in the FKRP gene can cause muscle-eye-brain disease and Walker-Warburg syndrome.

Author

Beltran-Valero de Bernabé D, Voit T, Longman C, Steinbrecher A, Straub V, Yuva Y, Herrmann R, Sperner J, Korenke C, Diesen C, Dobyns WB, Brunner HG, van Bokhoven H, Brockington M, and Muntoni F

Subjects

Brain pathology, Child, Female, Genetic Predisposition to Disease, Humans, Infant, Newborn, Magnetic Resonance Imaging, Male, Muscle, Skeletal, Muscular Dystrophies diagnosis, Pentosyltransferases, Syndrome, Brain abnormalities, Eye Abnormalities genetics, Muscular Dystrophies genetics, Mutation, Missense, Proteins genetics

Published

2004

11. A novel form of recessive limb girdle muscular dystrophy with mental retardation and abnormal expression of alpha-dystroglycan.

Author

Dinçer P, Balci B, Yuva Y, Talim B, Brockington M, Dinçel D, Torelli S, Brown S, Kale G, Haliloglu G, Gerçeker FO, Atalay RC, Yakicier C, Longman C, Muntoni F, and Topaloglu H

Subjects

Adolescent, Adult, Age of Onset, Brain metabolism, Brain pathology, Brain physiopathology, Child, Chromosome Mapping, Cytoskeletal Proteins biosynthesis, Cytoskeletal Proteins genetics, DNA Mutational Analysis, Dystroglycans, Female, Genetic Testing, Humans, Immunohistochemistry, Intellectual Disability complications, Intellectual Disability metabolism, Male, Membrane Glycoproteins biosynthesis, Membrane Glycoproteins genetics, Microcephaly genetics, Microcephaly pathology, Muscle Proteins metabolism, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Muscle, Skeletal physiopathology, Muscular Dystrophies metabolism, Turkey, Cytoskeletal Proteins deficiency, Genes, Recessive genetics, Intellectual Disability genetics, Membrane Glycoproteins deficiency, Muscular Dystrophies complications, Muscular Dystrophies genetics

Abstract

The limb girdle muscular dystrophies are a heterogeneous group of conditions characterized by proximal muscle weakness and disease onset ranging from infancy to adulthood. We report here eight patients from seven unrelated families affected by a novel and relatively mild form of autosomal recessive limb girdle muscular dystrophy (LGMD2) with onset in the first decade of life and characterized by severe mental retardation but normal brain imaging. Immunocytochemical studies revealed a significant selective reduction of alpha-dystroglycan expression in the muscle biopsies. Linkage analysis excluded known loci for both limb girdle muscular dystrophy and congenital muscular dystrophies in the consanguineous families. We consider that this represents a novel form of muscular dystrophy with associated brain involvement. The biochemical studies suggest that it may belong to the growing number of muscular dystrophies with abnormal expression of alpha-dystroglycan.

Published

2003

12. Mutations in the human LARGE gene cause MDC1D, a novel form of congenital muscular dystrophy with severe mental retardation and abnormal glycosylation of alpha-dystroglycan.

Author

Longman C, Brockington M, Torelli S, Jimenez-Mallebrera C, Kennedy C, Khalil N, Feng L, Saran RK, Voit T, Merlini L, Sewry CA, Brown SC, and Muntoni F

Subjects

Adolescent, Chromosome Mapping, Dystroglycans, Female, Glycosylation, Humans, Intellectual Disability metabolism, Laminin metabolism, Magnetic Resonance Imaging, Muscular Dystrophies metabolism, Mutation, Cytoskeletal Proteins metabolism, Intellectual Disability genetics, Membrane Glycoproteins metabolism, Muscle, Skeletal metabolism, Muscular Dystrophies genetics

Abstract

The congenital muscular dystrophies (CMD) are a heterogeneous group of autosomal recessive disorders. A new pathomechanism has recently been identified in a group of these disorders in which known or putative glycosyltransferases are defective. Common to all these conditions is the hypoglycosylation of alpha-dystroglycan. Fukuyama CMD, muscle-eye-brain disease and Walker-Warburg syndrome, each associated with eye abnormalities and neuronal migration defects, result from mutations in fukutin, POMGnT1 and POMT1, respectively, while mutations in the fukutin-related protein (FKRP) gene cause congenital muscular dystrophy 1C, typically lacking brain involvement. Another putative glycosyltransferase, Large, is mutated in the myodystrophy mouse. The human homologue of this gene is therefore a strong candidate for involvement in novel forms of muscular dystrophy. We studied 36 patients with muscular dystrophy and either mental retardation, structural brain changes or abnormal alpha-dystroglycan immunolabelling, unlinked to any reported CMD loci. Linkage analysis in seven informative families excluded involvement of LARGE but sequencing of this gene in the remaining 29 families identified one patient with a G1525A (Glu509Lys) missense mutation and a 1 bp insertion, 1999insT. This 17-year-old girl presented with congenital muscular dystrophy, profound mental retardation, white matter changes and subtle structural abnormalities on brain MRI. Her skeletal muscle biopsy showed reduced immunolabelling of alpha-dystroglycan. Immunoblotting with an antibody to a glycosylated epitope demonstrated a reduced molecular weight form of alpha-dystroglycan that retained some laminin binding activity. This is the first description of mutations in the human LARGE gene and we propose to name this new disorder MDC1D.

Published

2003