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1. Delineating the autistic phenotype in children with neurofibromatosis type 1.

Author

Chisholm A.K., Haebich K.M., Pride N.A., Walsh K.S., Lami F., Ure A., Maloof T., Brignell A., Rouel M., Granader Y., Maier A., Barton B., Darke H., Dabscheck G., Anderson V.A., Williams K., North K.N., Payne J.M., Chisholm A.K., Haebich K.M., Pride N.A., Walsh K.S., Lami F., Ure A., Maloof T., Brignell A., Rouel M., Granader Y., Maier A., Barton B., Darke H., Dabscheck G., Anderson V.A., Williams K., North K.N., and Payne J.M.

Abstract

Background: Existing research has demonstrated elevated autistic behaviours in children with neurofibromatosis type 1 (NF1), but the autistic phenotype and its relationship to other neurodevelopmental manifestations of NF1 remains unclear. To address this gap, we performed detailed characterisation of autistic behaviours in children with NF1 and investigated their association with other common NF1 child characteristics. Method(s): Participants were drawn from a larger cross-sectional study examining autism in children with NF1. The population analysed in this study scored above threshold on the Social Responsiveness Scale-Second Edition (T-score >= 60; 51% larger cohort) and completed the Autism Diagnostic Interview-Revised (ADI-R) and/or the Autism Diagnostic Observation Schedule-Second Edition (ADOS-2). All participants underwent evaluation of their intellectual function, and behavioural data were collected via parent questionnaires. Result(s): The study cohort comprised 68 children (3-15 years). Sixty-three per cent met the ADOS-2 'autism spectrum' cut-off, and 34% exceeded the more stringent threshold for 'autistic disorder' on the ADI-R. Social communication symptoms were common and wide-ranging, while restricted and repetitive behaviours (RRBs) were most commonly characterised by 'insistence on sameness' (IS) behaviours such as circumscribed interests and difficulties with minor changes. Autistic behaviours were weakly correlated with hyperactive/impulsive attention deficit hyperactivity disorder (ADHD) symptoms but not with inattentive ADHD or other behavioural characteristics. Language and verbal IQ were weakly related to social communication behaviours but not to RRBs. Limitation(s): Lack of genetic validation of NF1, no clinical diagnosis of autism, and a retrospective assessment of autistic behaviours in early childhood. Conclusion(s): Findings provide strong support for elevated autistic behaviours in children with NF1. While these behaviours were relati

Published
2022

2. Cerebrovascular dysplasia in neurofibromatosis type 1

Author

Cairns, A.G. and North, K.N.

Subjects
Neurofibromatosis -- Complications and side effects, Neurofibromatosis -- Research, Cerebrovascular disease -- Distribution, Cerebrovascular disease -- Research, Company distribution practices, Health, Psychology and mental health
Published
2008

3. A gene for speed: contractile properties of isolated whole EDL muscle from an [alpha]-actinin-3 knockout mouse

Author

Chan, S., Seto, J.T., MacArthur, D.G., Yang, N., North, K.N., and Head, S.I.

Subjects
Binding proteins -- Physiological aspects, Binding proteins -- Health aspects, Genes -- Health aspects, Biological sciences
Abstract

The actin-binding protein [alpha]-actinin-3 is one of the two isoforms of [alpha]-actinin that are found in the Z-discs of skeletal muscle. [alpha]-Actinin-3 is exclusively expressed in fast glycolytic muscle fibers. Homozygosity for a common polymorphism in the ACTN3 gene results in complete deficiency of [alpha]-actinin-3 in about 1 billion individuals worldwide. Recent genetic studies suggest that the absence of [alpha]-actinin-3 is detrimental to sprint and power performance in elite athletes and in the general population. In contrast, [alpha]-actinin-3 deficiency appears to be beneficial for endurance athletes. To determine the effect of [alpha]-actinin-3 deficiency on the contractile properties of skeletal muscle, we studied isolated extensor digitorum longus (fast-twitch) muscles from a specially developed [alpha]-actinin-3 knockout (KO) mouse, [alpha]-Actinin-3-deficient muscles showed similar levels of damage to wild-type (WT) muscles following lengthening contractions of 20% strain, suggesting that the presence or absence of [alpha]-actinin-3 does not significantly influence the mechanical stability of the sarcomere in the mouse. [alpha]-Actinin-3 deficiency does not result in any change in myosin heavy chain expression. However, compared with [alpha]-actinin-3-positive muscles, [alpha]-actinin-3-deficient muscles displayed longer twitch half-relaxation times, better recovery from fatigue, smaller cross-sectional areas, and lower twitch-to-tetanus ratios. We conclude that [alpha]-actinin-3 deficiency results in fast-twitch, glycolytic fibers developing slower-twitch, more oxidative properties. These changes in the contractile properties of fast-twitch skeletal muscle from [alpha]-actinin-3-deficient individuals would be detrimental to optimal sprint and power performance, but beneficial for endurance performance. extensor digitorum longus

Published
2008

7. Congenital Titinopathy: Comprehensive characterization and pathogenic insights

Author

Oates, E.C., Jones, K.J., Donkervoort, S., Charlton, A., Brammah, S., Smith, J.E., Ware, J.S., Yau, K.S., Swanson, L.C., Whiffin, N., Peduto, A.J., Bournazos, A., Waddell, L.B., Farrar, M.A., Sampaio, H.A., Teoh, H.L., Lamont, P.J., Mowat, D., Fitzsimons, R.B., Corbett, A.J., Ryan, M.M., O'Grady, G.L., Sandaradura, S.A., Ghaoui, R., Joshi, H., Marshall, J.L., Nolan, M.A., Kaur, S., Punetha, J., Topf, A., Harris, E., Bakshi, M., Genetti, C.A., Marttila, M., Werlauff, U., Streichenberger, N., Pestronk, A., Mazanti, I., Pinner, J.R., Vuillerot, C., Grosmann, C., Camacho, A., Mohassel, P., Leach, M.E., Foley, A.R., Bharucha-Goebel, D., Collins, J., Connolly, A.M., Gilbreath, H.R., Iannaccone, S.T., Castro, D., Cummings, B.B., Webster, R.I., Lazaro, L., Vissing, J., Coppens, S., Deconinck, N., Luk, H.M., Thomas, N.H., Foulds, N.C., Illingworth, M.A., Ellard, S., McLean, C.A., Phadke, R., Ravenscroft, G., Witting, N., Hackman, P., Richard, I., Cooper, S.T., Kamsteeg, E.J., Hoffman, E.P., Bushby, K., Straub, V., Udd, B., Ferreiro, A., North, K.N., Clarke, N.F., Lek, M., Beggs, A.H., Bonnemann, C.G., MacArthur, D.G., Granzier, H., Davis, M.R., Laing, N.G., Oates, E.C., Jones, K.J., Donkervoort, S., Charlton, A., Brammah, S., Smith, J.E., Ware, J.S., Yau, K.S., Swanson, L.C., Whiffin, N., Peduto, A.J., Bournazos, A., Waddell, L.B., Farrar, M.A., Sampaio, H.A., Teoh, H.L., Lamont, P.J., Mowat, D., Fitzsimons, R.B., Corbett, A.J., Ryan, M.M., O'Grady, G.L., Sandaradura, S.A., Ghaoui, R., Joshi, H., Marshall, J.L., Nolan, M.A., Kaur, S., Punetha, J., Topf, A., Harris, E., Bakshi, M., Genetti, C.A., Marttila, M., Werlauff, U., Streichenberger, N., Pestronk, A., Mazanti, I., Pinner, J.R., Vuillerot, C., Grosmann, C., Camacho, A., Mohassel, P., Leach, M.E., Foley, A.R., Bharucha-Goebel, D., Collins, J., Connolly, A.M., Gilbreath, H.R., Iannaccone, S.T., Castro, D., Cummings, B.B., Webster, R.I., Lazaro, L., Vissing, J., Coppens, S., Deconinck, N., Luk, H.M., Thomas, N.H., Foulds, N.C., Illingworth, M.A., Ellard, S., McLean, C.A., Phadke, R., Ravenscroft, G., Witting, N., Hackman, P., Richard, I., Cooper, S.T., Kamsteeg, E.J., Hoffman, E.P., Bushby, K., Straub, V., Udd, B., Ferreiro, A., North, K.N., Clarke, N.F., Lek, M., Beggs, A.H., Bonnemann, C.G., MacArthur, D.G., Granzier, H., Davis, M.R., and Laing, N.G.

Abstract

Contains fulltext : 196367.pdf (Publisher’s version ) (Open Access), OBJECTIVE: Comprehensive clinical characterization of congenital titinopathy to facilitate diagnosis and management of this important emerging disorder. METHODS: Using massively parallel sequencing we identified 30 patients from 27 families with 2 pathogenic nonsense, frameshift and/or splice site TTN mutations in trans. We then undertook a detailed analysis of the clinical, histopathological and imaging features of these patients. RESULTS: All patients had prenatal or early onset hypotonia and/or congenital contractures. None had ophthalmoplegia. Scoliosis and respiratory insufficiency typically developed early and progressed rapidly, whereas limb weakness was often slowly progressive, and usually did not prevent independent walking. Cardiac involvement was present in 46% of patients. Relatives of 2 patients had dilated cardiomyopathy. Creatine kinase levels were normal to moderately elevated. Increased fiber size variation, internalized nuclei and cores were common histopathological abnormalities. Cap-like regions, whorled or ring fibers, and mitochondrial accumulations were also observed. Muscle magnetic resonance imaging showed gluteal, hamstring and calf muscle involvement. Western blot analysis showed a near-normal sized titin protein in all samples. The presence of 2 mutations predicted to impact both N2BA and N2B cardiac isoforms appeared to be associated with greatest risk of cardiac involvement. One-third of patients had 1 mutation predicted to impact exons present in fetal skeletal muscle, but not included within the mature skeletal muscle isoform transcript. This strongly suggests developmental isoforms are involved in the pathogenesis of this congenital/early onset disorder. INTERPRETATION: This detailed clinical reference dataset will greatly facilitate diagnostic confirmation and management of patients, and has provided important insights into disease pathogenesis. Ann Neurol 2018;83:1105-1124.

Published
2018

8. The Future of Genomic Research in Athletic Performance and Adaptation to Training

Author

Wang, G. Tanaka, M. Eynon, N. North, K.N. Williams, A.G. Collins, M. Moran, C.N. Britton, S.L. Fuku, N. Ashley, E.A. Klissouras, V. Lucia, A. Ahmetov, I.I. De Geus, E. Alsayrafi, M. Pitsiladis, Y.P.

Abstract

Despite numerous attempts to discover genetic variants associated with elite athletic performance, an individual's trainability and injury predisposition, there has been limited progress to date. Past reliance on candidate gene studies focusing predominantly on genotyping a limited number of genetic variants in small, often heterogeneous cohorts has not generated results of practical significance. Hypothesis-free genome-wide approaches will in the future provide more comprehensive coverage and in-depth understanding of the biology underlying sports-related traits and related genetic mechanisms. Large, collaborative projects with sound experimental designs (e.g. clearly defined phenotypes, considerations and controls for sources of variability, and necessary replications) are required to produce meaningful results, especially when a hypothesis-free approach is used. It remains to be determined whether the novel approaches under current implementation will result in findings with real practical significance. This review will briefly summarize current and future directions in exercise genetics and genomics. © 2016 S. Karger AG, Basel.

Published
2016

9. Athlome project consortium: A concerted effort to discover genomic and other 'omic' markers of athletic performance

Author

Pitsiladis, Y.P. Tanaka, M. Eynon, N. Bouchard, C. North, K.N. Williams, A.G. Collins, M. Moran, C.N. Britton, S.L. Fuku, N. Ashley, E.A. Klissouras, V. Lucia, A. Ahmetov, I.I. De Geus, E. Alsayrafi, M. Webborn, N. Wang, G. Bishop, D.J. Papadimitriou, I. Yan, X. Tirosh, O. Kuang, J. Rankinen, T. Sarzinsky, M. Mikael Mattsson, C. Wheeler, M. Waggott, D. Byrne, N.M. Artioli, G.G. September, A. Posthumus, M. Van der Merwe, W. Cieszczyk, P. Leonska-Duniec, A. Ficek, K. Maciejewska-Karlowska, A. Sawczuk, M. Stepien-Slodkowska, M. Feller, J. Dijkstra, P. Chmutov, A.M. Dyatlov, D.A. Orekhov, E.F. Pushkareva, Y.E. Shvedkaya, I.A. Massidda, M. Calò, C.M. Day, S.H. Stebbings, G.K. Erskine, R.M. Montgomery, H.E. Garton, F.C. Houweling, P. Derave, W. Baguet, A. Muniesa, C.A. Sessa, F. Petito, A. Sale, C. Hughes, D.C. Varley, I. Boomsma, D. Bartels, M. Davies, G.E. Ginevičienė, V. Jakaitienė, A. Kučinskas, V. Tubelis, L. Utkus, A. Milašius, K. Venckunas, T. Skurvydas, A. Stasiulis, A. Malkova, D. Wilson, R. Koch, L.G. Zempo, H. Naito, H. Kikuchi, N. Miyamoto-Mikami, E. Murakami, H. Miyachi, M. Takahashi, H. Ohiwa, N. Kawahara, T. Tsuchie, H. Tobina, T. Ichinoseki-Sekine, N. Tanaka, H. Kaneoka, K. Nakazato, K. Egorova, E.S. Gabdrakhmanova, L.J. Arkhipova, A.A. Borisova, A.V. Gabbasov, R.T. Stepanova, A.A. Kashapov, R.I. Rogozkin, V.A. Astratenkova, I.V. Druzhevskaya, A.M. Fedotovskaya, O.N. Golberg, N.D. Hakimullina, A.M. Kostryukova, E.S. Alexeev, D.G. Generozov, E.V. Ischenko, D.S. Kulemin, N.A. Larin, A.K. Ospanova, E.A. Pavlenko, A.V. Govorun, V.M. Gilep, A.A. Gilep, I.L. Haidukevich, I.V. Rybina, I.L. Drozdovska, S.B. Docenko, V.E. Ilyin, V.N. Lekontsev, E. Akimov, E.B. El-Rayess, M. Georgakopoulos, C. Botre, F. Suhre, K. Hubank, M. Wolfarth, B. Greeves, J.P. Stellingwerff, T. Ranson, C. Fraser, W.D. Grealy, R. Griffiths, L. Scott, R. Pushkarev, V.P. Athlome Project Consortium

Abstract

Despite numerous attempts to discover genetic variants associated with elite athletic performance, injury predisposition, and elite/world-class athletic status, there has been limited progress to date. Past reliance on candidate gene studies predominantly focusing on genotyping a limited number of single nucleotide polymorphisms or the insertion/deletion variants in small, often heterogeneous cohorts (i.e., made up of athletes of quite different sport specialties) have not generated the kind of results that could offer solid opportunities to bridge the gap between basic research in exercise sciences and deliverables in biomedicine. A retrospective view of genetic association studies with complex disease traits indicates that transition to hypothesis-free genome-wide approaches will be more fruitful. In studies of complex disease, it is well recognized that the magnitude of genetic association is often smaller than initially anticipated, and, as such, large sample sizes are required to identify the gene effects robustly. A symposium was held in Athens and on the Greek island of Santorini from 14 -17 May 2015 to review the main findings in exercise genetics and genomics and to explore promising trends and possibilities. The symposium also offered a forum for the development of a position stand (the Santorini Declaration). Among the participants, many were involved in ongoing collaborative studies (e.g., ELITE, GAMES, Gene SMART, GENESIS, and POWERGENE). A consensus emerged among participants that it would be advantageous to bring together all current studies and those recently launched into one new large collaborative initiative, which was subsequently named the Athlome Project Consortium. © 2016 the American Physiological Society.

Published
2016

10. The Future of Genomic Research in Athletic Performance and Adaptation to Training

Author

Wang, G., Tanaka, M., Eynon, N., North, K.N., Williams, A.G., Collins, M., Moran, C.M., Britton, S.L., Fuku, N., Ashley, E.A., Klissouras, V., Lucia, A., Ahmetov, I.I., de Geus, E.J.C., Alsayrafi, M., Pitsiladis, Y.P., Posthumus, M., Biological Psychology, Amsterdam Global Change Institute, EMGO+ - Lifestyle, Overweight and Diabetes, Posthumus, M., and Collins, M.

Subjects
0301 basic medicine, Genetics, Candidate gene, Physical conditioning, Genomic research, Genetic variants, Physical activity, Genomics, 030229 sport sciences, Biology, Data science, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Adaptation (computer science)
Abstract

Despite numerous attempts to discover genetic variants associated with elite athletic performance, an individual's trainability and injury predisposition, there has been limited progress to date. Past reliance on candidate gene studies focusing predominantly on genotyping a limited number of genetic variants in small, often heterogeneous cohorts has not generated results of practical significance. Hypothesis-free genome-wide approaches will in the future provide more comprehensive coverage and in-depth understanding of the biology underlying sports-related traits and related genetic mechanisms. Large, collaborative projects with sound experimental designs (e.g. clearly defined phenotypes, considerations and controls for sources of variability, and necessary replications) are required to produce meaningful results, especially when a hypothesis-free approach is used. It remains to be determined whether the novel approaches under current implementation will result in findings with real practical significance. This review will briefly summarize current and future directions in exercise genetics and genomics.

Published
2016
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11. Genotype-phenotype correlation in nemaline myopathy

Author

Ryan, M.M., Schnell, C., Strickland, C.D., Shield, L.K., Morgan, G., Iannaccone, S.T., Laing, N.G., North, K.N., and Beggs, A.H.

Subjects
Genetic disorders -- Research, Human chromosome abnormalities -- Research, Human genetics -- Research, Muscle diseases -- Genetic aspects, Gene mutations -- Physiological aspects, Biological sciences
Published
2001

13. Direct-to-consumer genetic testing for predicting sports performance and talent identification: Consensus statement

Author

Webborn, N. Williams, A. McNamee, M. Bouchard, C. Pitsiladis, Y. Ahmetov, I. Ashley, E. Byrne, N. Camporesi, S. Collins, M. Dijkstra, P. Eynon, N. Fuku, N. Garton, F.C. Hoppe, N. Holm, S. Kaye, J. Klissouras, V. Lucia, A. Maase, K. Moran, C. North, K.N. Pigozzi, F. Wang, G.

Abstract

The general consensus among sport and exercise genetics researchers is that genetic tests have no role to play in talent identification or the individualised prescription of training to maximise performance. Despite the lack of evidence, recent years have witnessed the rise of an emerging market of direct-toconsumer marketing (DTC) tests that claim to be able to identify children's athletic talents. Targeted consumers include mainly coaches and parents. There is concern among the scientific community that the current level of knowledge is being misrepresented for commercial purposes. There remains a lack of universally accepted guidelines and legislation for DTC testing in relation to all forms of genetic testing and not just for talent identification. There is concern over the lack of clarity of information over which specific genes or variants are being tested and the almost universal lack of appropriate genetic counselling for the interpretation of the genetic data to consumers. Furthermore independent studies have identified issues relating to quality control by DTC laboratories with different results being reported from samples from the same individual. Consequently, in the current state of knowledge, no child or young athlete should be exposed to DTC genetic testing to define or alter training or for talent identification aimed at selecting gifted children or adolescents. Large scale collaborative projects, may help to develop a stronger scientific foundation on these issues in the future.

Published
2015

14. Clinical characterisation of a large international congenital titinopathy cohort

Author

Oates, E.C., primary, Yau, K.S., additional, Jones, K., additional, Smith, J.E., additional, Donkervoort, S., additional, Swanson, L., additional, Charlton, A., additional, Brammah, S., additional, Peduto, A.J., additional, Richard, I., additional, Ferreiro, A., additional, Hoffman, E., additional, Bushby, K., additional, Straub, V., additional, Udd, B., additional, Lek, M., additional, MacArthur, D.G., additional, Granzier, H., additional, Beggs, A., additional, Bönnemann, C.G., additional, North, K.N., additional, Davis, M.R., additional, and Laing, N.G., additional

Published
2017
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15. Variants in SLC18A3, vesicular acetylcholine transporter, cause congenital myasthenic syndrome

Author

O'Grady, G.L., Verschuuren, C., Yuen, M., Webster, R., Menezes, M., Fock, J.M., Pride, N., Best, H.A., Benavides Damm, T., Turner, C., Lek, M., Engel, A.G., North, K.N., Clarke, N.F., MacArthur, D.G., Kamsteeg, E.J., Cooper, S.T., O'Grady, G.L., Verschuuren, C., Yuen, M., Webster, R., Menezes, M., Fock, J.M., Pride, N., Best, H.A., Benavides Damm, T., Turner, C., Lek, M., Engel, A.G., North, K.N., Clarke, N.F., MacArthur, D.G., Kamsteeg, E.J., and Cooper, S.T.

Abstract

Item does not contain fulltext, OBJECTIVE: To describe the clinical and genetic characteristics of presynaptic congenital myasthenic syndrome secondary to biallelic variants in SLC18A3. METHODS: Individuals from 2 families were identified with biallelic variants in SLC18A3, the gene encoding the vesicular acetylcholine transporter (VAChT), through whole-exome sequencing. RESULTS: The patients demonstrated features seen in presynaptic congenital myasthenic syndrome, including ptosis, ophthalmoplegia, fatigable weakness, apneic crises, and deterioration of symptoms in cold water for patient 1. Both patients demonstrated moderate clinical improvement on pyridostigmine. Patient 1 had a broader phenotype, including learning difficulties and left ventricular dysfunction. Electrophysiologic studies were typical for a presynaptic defect. Both patients showed profound electrodecrement on low-frequency repetitive stimulation followed by a prolonged period of postactivation exhaustion. In patient 1, this was unmasked only after isometric contraction, a recognized feature of presynaptic disease, emphasizing the importance of activation procedures. CONCLUSIONS: VAChT is responsible for uptake of acetylcholine into presynaptic vesicles. The clinical and electrographic characteristics of the patients described are consistent with previously reported mouse models of VAChT deficiency. These findings make it very likely that defects in VAChT due to variants in SLC18A3 are a cause of congenital myasthenic syndrome in humans.

Published
2016

16. Prominent scapulae mimicking an inherited myopathy expands the phenotype of CHD7-related disease

Author

O'Grady, G.L., Ma, A., Sival, D., Wong, M.T.Y., Peduto, T., Menezes, M.P., Young, H., Waddell, L., Ghaoui, R., Needham, M., Lek, M., North, K.N., MacArthur, D.G., van Ravenswaaij-Arts, C.M.A., Clarke, N.F., O'Grady, G.L., Ma, A., Sival, D., Wong, M.T.Y., Peduto, T., Menezes, M.P., Young, H., Waddell, L., Ghaoui, R., Needham, M., Lek, M., North, K.N., MacArthur, D.G., van Ravenswaaij-Arts, C.M.A., and Clarke, N.F.

Abstract

CHD7 variants are a well-established cause of CHARGE syndrome, a disabling multi-system malformation disorder that is often associated with deafness, visual impairment and intellectual disability. Less severe forms of CHD7-related disease are known to exist, but the full spectrum of phenotypes remains uncertain. We identified a de novo missense variant in CHD7 in a family presenting with musculoskeletal abnormalities as the main manifestation of CHD7-related disease, representing a new phenotype. The proband presented with prominent scapulae, mild shoulder girdle weakness and only subtle dysmorphic features. Investigation revealed hypoplasia of the trapezius and sternocleidomastoid muscles and semicircular canal defects, but he did not fulfill diagnostic criteria for CHARGE syndrome. Although the shoulders are often sloping and anteverted in CHARGE syndrome, the underlying neuromuscular cause has never been investigated. This report expands the phenotypes associated with CHD7 mutations to include a musculoskeletal presentation, with hypoplasia of the shoulder and neck muscles. CHD7 should be considered in patients presenting in childhood with stable scapular winging, particularly if accompanied by dysmorphic features and balance difficulties.

Published
2016

17. Use of whole-exome sequencing for diagnosis of Limb-Girdle muscular dystrophy

Author

Ghaoui, R., Cooper, S.T., Lek, M., Jones, K., Corbett, A., Reddel, S.W., Needham, M., Liang, C., Waddell, L.B., Nicholson, G., O’Grady, G., Kaur, S., Ong, R., Davis, M., Sue, C.M., Laing, N.G., North, K.N., MacArthur, D.G., Clarke, N.F., Ghaoui, R., Cooper, S.T., Lek, M., Jones, K., Corbett, A., Reddel, S.W., Needham, M., Liang, C., Waddell, L.B., Nicholson, G., O’Grady, G., Kaur, S., Ong, R., Davis, M., Sue, C.M., Laing, N.G., North, K.N., MacArthur, D.G., and Clarke, N.F.

Abstract

Importance To our knowledge, the efficacy of transferring next-generation sequencing from a research setting to neuromuscular clinics has never been evaluated. Objective To translate whole-exome sequencing (WES) to clinical practice for the genetic diagnosis of a large cohort of patients with limb-girdle muscular dystrophy (LGMD) for whom protein-based analyses and targeted Sanger sequencing failed to identify the genetic cause of their disorder. Design, Setting, and Participants We performed WES on 60 families with LGMDs (100 exomes). Data analysis was performed between January 6 and December 19, 2014, using the xBrowse bioinformatics interface (Broad Institute). Patients with LGMD were ascertained retrospectively through the Institute for Neuroscience and Muscle Research Biospecimen Bank between 2006 and 2014. Enrolled patients had been extensively investigated via protein studies and candidate gene sequencing and remained undiagnosed. Patients presented with more than 2 years of muscle weakness and with dystrophic or myopathic changes present in muscle biopsy specimens. Main Outcomes and Measures The diagnostic rate of LGMD in Australia and the relative frequencies of the different LGMD subtypes. Our central goals were to improve the genetic diagnosis of LGMD, investigate whether the WES platform provides adequate coverage of known LGMD-related genes, and identify new LGMD-related genes. Results With WES, we identified likely pathogenic mutations in known myopathy genes for 27 of 60 families. Twelve families had mutations in known LGMD-related genes. However, 15 families had variants in disease-related genes not typically associated with LGMD, highlighting the clinical overlap between LGMD and other myopathies. Common causes of phenotypic overlap were due to mutations in congenital muscular dystrophy–related genes (4 families) and collagen myopathy–related genes (4 families). Less common myopathies included metabolic myopathy (2 families), congenital myasthenic s

Published
2015

18. Expanding the phenotype of GMPPB mutations

Author

Cabrera-Serrano, M., Ghaoui, R., Ravenscroft, G., Johnsen, R.D., Davis, M.R., Corbett, A., Reddel, S., Sue, C.M., Liang, C., Waddell, L.B., Kaur, S., Lek, M., North, K.N., MacArthur, D.G., Lamont, P.J., Clarke, N.F., Laing, N.G., Cabrera-Serrano, M., Ghaoui, R., Ravenscroft, G., Johnsen, R.D., Davis, M.R., Corbett, A., Reddel, S., Sue, C.M., Liang, C., Waddell, L.B., Kaur, S., Lek, M., North, K.N., MacArthur, D.G., Lamont, P.J., Clarke, N.F., and Laing, N.G.

Abstract

Dystroglycanopathies are a heterogeneous group of diseases with a broad phenotypic spectrum ranging from severe disorders with congenital muscle weakness, eye and brain structural abnormalities and intellectual delay to adult-onset limb-girdle muscular dystrophies without mental retardation. Most frequently the disease onset is congenital or during childhood. The exception is FKRP mutations, in which adult onset is a common presentation. Here we report eight patients from five non-consanguineous families where next generation sequencing identified mutations in the GMPPB gene. Six patients presented as an adult or adolescent-onset limb-girdle muscular dystrophy, one presented with isolated episodes of rhabdomyolysis, and one as a congenital muscular dystrophy. This report expands the phenotypic spectrum of GMPPB mutations to include limb-girdle muscular dystrophies with adult onset with or without intellectual disability, or isolated rhabdomyolysis.

Published
2015

20. G.O.2: Mutations in LMOD3 cause severe nemaline myopathy by disrupting thin filament organisation in skeletal muscle

Author

UCL - SSS/IONS/NEUR - Clinical Neuroscience, UCL - (SLuc) Service de neurologie, Kreissl, M., Sandaradura, S.A., Dowling, J.J., Kostyukova, A.S., Moroz, N., Quinlan, K.G., Lehtokari, V., Ravenscroft, G., Todd, E.J., Ceyhan-Birsoy, O., Gokhin, D.S., Maluenda, J., Lek, M., Nolent, F., Pappas, C.T., Novak, S.M., D’Amico, A., Malfatti, E., Thomas, B.P., Gabriel, S.B., Gupta, N., Daly, M.J., Ilkovski, B., Houweling, P.J., Swanson, L.C., Brownstein, C.A., Gupta, V.A., Medne, L., Shannon, P., Flisberg, A., Holmberg, E., Van den Bergh, Peter, Lapunzina, P., Waddell, L.B., Sloboda, D.D., Bertini, E., Chitayat, D., Telfer, W.R., Laquerrière, A., Gregorio, C.C., Ottenheijm, C.A.C., Bönnemann, C.G., Pelin, K., Beggs, A.H., Hayashi, Y.K., Romero, N.B., Laing, N.G., Nishino, I., Wallgren-Pettersson, C., Melki, J., Fowler, V.M., MacArthur, D.G., North, K.N., Clarke, N.F., UCL - SSS/IONS/NEUR - Clinical Neuroscience, UCL - (SLuc) Service de neurologie, Kreissl, M., Sandaradura, S.A., Dowling, J.J., Kostyukova, A.S., Moroz, N., Quinlan, K.G., Lehtokari, V., Ravenscroft, G., Todd, E.J., Ceyhan-Birsoy, O., Gokhin, D.S., Maluenda, J., Lek, M., Nolent, F., Pappas, C.T., Novak, S.M., D’Amico, A., Malfatti, E., Thomas, B.P., Gabriel, S.B., Gupta, N., Daly, M.J., Ilkovski, B., Houweling, P.J., Swanson, L.C., Brownstein, C.A., Gupta, V.A., Medne, L., Shannon, P., Flisberg, A., Holmberg, E., Van den Bergh, Peter, Lapunzina, P., Waddell, L.B., Sloboda, D.D., Bertini, E., Chitayat, D., Telfer, W.R., Laquerrière, A., Gregorio, C.C., Ottenheijm, C.A.C., Bönnemann, C.G., Pelin, K., Beggs, A.H., Hayashi, Y.K., Romero, N.B., Laing, N.G., Nishino, I., Wallgren-Pettersson, C., Melki, J., Fowler, V.M., MacArthur, D.G., North, K.N., and Clarke, N.F.

Abstract

Nemaline myopathy (NM) is a disorder of the skeletal muscle thin filament characterised by muscle dysfunction and electron-dense protein accumulations (nemaline bodies). Pathogenic mutations have been described in nine genes to date, but the genetic basis remains unknown in many cases. We used whole exome sequencing (WES) in two families with NM and subsequent gene sequencing in over 540 additional genetically unresolved NM patients to identify and characterise a new genetic cause of NM. We developed a knock-down zebrafish model of this condition and used immunohistochemistry, western blotting, single-fibre contractility studies and recombinant protein studies to characterise the expression, localisation and biochemical functions of the new disease-related protein. We identified homozygous or compound heterozygous variants in LMOD3, which encodes leiomodin-3 (Lmod3) in 21 patients from 14 families. Affected individuals had severe generalised weakness and hypotonia, and most affected individuals died in the neonatal period. We demonstrated that Lmod3 is expressed from early muscle differentiation, localises to thin filaments with enrichment at the pointed ends, and has strong actin nucleating activity. Loss of Lmod3 in patient muscle results in shortening and disorganisation of thin filaments. Knockdown of lmod3 in the zebrafish replicates this phenotype. These findings define a new genetic subtype of congenital myopathy and demonstrate an essential, previously unrecognised role for Lmod3 in the regulation of sarcomeric thin filaments in skeletal muscle.

Published
2014

21. G.P.219: Diagnosing the limb-girdle muscular dystrophies using whole exome sequencing: An Australian cohort

Author

Ghaoui, R., Corbett, A., Needham, M., Farrar, M., Sampaio, H., Mowat, D., Rajagopalan, S., Liang, C., Kaur, S., Waddell, L., Daly, K., Thomas, B.P., Lek, M., Daly, M.J., North, K.N., MacArthur, D.G., Sue, C.M., Clarke, N.F., Ghaoui, R., Corbett, A., Needham, M., Farrar, M., Sampaio, H., Mowat, D., Rajagopalan, S., Liang, C., Kaur, S., Waddell, L., Daly, K., Thomas, B.P., Lek, M., Daly, M.J., North, K.N., MacArthur, D.G., Sue, C.M., and Clarke, N.F.

Abstract

Limb-girdle muscular dystrophies (LGMDs) are a heterogeneous group of genetic disorders associated with proximal muscle weakness that begins after 2 years of age and dystrophic changes on muscle biopsy. The genetic cause of LGMD in Australia remains uncertain in approximately 40% of patients resulting in uncertainty about reproductive risks for patients and long term prognosis. We reviewed the clinical information in a large cohort of patients with LGMD who lacked a genetic diagnosis, usually after extensive previous investigations (n = 50). We first screened patients for myotonic dystrophy type 2 and then performed whole exome sequencing (WES), analysing data using the ‘xBrowse’ web interface (Broad Institute). Testing for myotonic dystrophy type 2 (DM2) identified 2 families in our LGMD cohort. Using WES we identified likely pathogenic mutations in known myopathy genes in 20 families, often in genes not typically associated with LGMD. Two families were diagnosed with dominant LGMD, 9 families with recessive LGMD, 3 with mutations congenital muscular dystrophy genes, 3 with collagen myopathies, 2 with metabolic myopathies and 1 in ACTA1. In addition one family had a mutation CHD7, a gene usually associated with CHARGE syndrome. Our overall diagnostic success rate was 46% in our LGMD cohort of patients most of whom had been extensively investigated previously and who remained without a genetic diagnosis. The diversity of genetic causes that we identified supports the clinical observation of that LGMD is highly heterogeneous and shares clinical features with many other forms of myopathy. Our study emphasises the challenges that clinicians face making a genetic diagnosis in all families. Whole exome sequencing and similar next-generation sequencing are likely to be efficient and cost-effective methods for identifying the genetic basis of LGMD but clinicians must remember that some disorders in the differential diagnosis, such as DM2, are routinely missed by WES.

Published
2014

23. G.P.271

Author

Marttila, M., primary, Lehtokari, V.L., additional, Marston, S.B., additional, Nyman, T.A., additional, Barnerias, C., additional, Beggs, A.H., additional, Bertin, E., additional, Ceyhan-Birsoy, Ö., additional, Cintas, P., additional, Gerard, M., additional, Gilbert-Dussardier, B., additional, Hogue, J.S., additional, Longman, C., additional, Eymard, B., additional, Frydman, M., additional, Kang, P.B., additional, Klinge, L., additional, Kolski, H., additional, Lochmüller, H., additional, Magy, L., additional, Manel, V., additional, Mayer, M., additional, North, K.N., additional, Peudenier-Robert, S., additional, Pihko, H., additional, Probst, F.J., additional, Reisin, R., additional, Stewart, W., additional, Taratuto, A.L., additional, de Visser, M., additional, Wilichowski, E., additional, Winer, J., additional, Nowak, K., additional, Lain, N.G., additional, Winder, T.L., additional, Monnier, N., additional, Clarke, N.F., additional, Pelin, K., additional, Grönholm, M., additional, and Wallgren-Pettersson, C., additional

Published
2014
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24. G.O.2

Author

Kreissl, M., primary, Sandaradura, S.A., additional, Dowling, J.J., additional, Kostyukova, A.S., additional, Moroz, N., additional, Quinlan, K.G., additional, Lehtokari, V., additional, Ravenscroft, G., additional, Todd, E.J., additional, Ceyhan-Birsoy, O., additional, Gokhin, D.S., additional, Maluenda, J., additional, Lek, M., additional, Nolent, F., additional, Pappas, C.T., additional, Novak, S.M., additional, D’Amico, A., additional, Malfatti, E., additional, Thomas, B.P., additional, Gabriel, S.B., additional, Gupta, N., additional, Daly, M.J., additional, Ilkovski, B., additional, Houweling, P.J., additional, Swanson, L.C., additional, Brownstein, C.A., additional, Gupta, V.A., additional, Medne, L., additional, Shannon, P., additional, Flisberg, A., additional, Holmberg, E., additional, den Bergh, P. Van, additional, Lapunzina, P., additional, Waddell, L.B., additional, Sloboda, D.D., additional, Bertini, E., additional, Chitayat, D., additional, Telfer, W.R., additional, Laquerrière, A., additional, Gregorio, C.C., additional, Ottenheijm, C.A.C., additional, Bönnemann, C.G., additional, Pelin, K., additional, Beggs, A.H., additional, Hayashi, Y.K., additional, Romero, N.B., additional, Laing, N.G., additional, Nishino, I., additional, Wallgren-Pettersson, C., additional, Melki, J., additional, Fowler, V.M., additional, MacArthur, D.G., additional, North, K.N., additional, and Clarke, N.F., additional

Published
2014
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25. G.P.219

Author

Ghaoui, R., primary, Corbett, A., additional, Needham, M., additional, Farrar, M., additional, Sampaio, H., additional, Mowat, D., additional, Rajagopalan, S., additional, Liang, C., additional, Kaur, S., additional, Waddell, L., additional, Daly, K., additional, Thomas, B.P., additional, Lek, M., additional, Daly, M.J., additional, North, K.N., additional, MacArthur, D.G., additional, Sue, C.M., additional, and Clarke, N.F., additional

Published
2014
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26. Mutations in GDP-mannose pyrophosphorylase B cause congenital and limb-girdle muscular dystrophies associated with hypoglycosylation of alpha-dystroglycan

Author

Carss, K.J., Stevens, E., Foley, A.R., Cirak, S., Riemersma, M., Torelli, S., Hoischen, A., Willer, T., Scherpenzeel, M. van, Moore, S.A., Messina, S., Bertini, E., Bonnemann, C.G., Abdenur, J.E., Grosmann, C.M., Kesari, A., Punetha, J., Quinlivan, R., Waddell, L.B., Young, H.K., Wraige, E., Yau, S., Brodd, L., Feng, L., Sewry, C., MacArthur, D.G., North, K.N., Hoffman, E., Stemple, D.L., Hurles, M.E., Bokhoven, H. van, Campbell, K.P., Lefeber, D.J., Lin, Y.Y., Muntoni, F., et al., Carss, K.J., Stevens, E., Foley, A.R., Cirak, S., Riemersma, M., Torelli, S., Hoischen, A., Willer, T., Scherpenzeel, M. van, Moore, S.A., Messina, S., Bertini, E., Bonnemann, C.G., Abdenur, J.E., Grosmann, C.M., Kesari, A., Punetha, J., Quinlivan, R., Waddell, L.B., Young, H.K., Wraige, E., Yau, S., Brodd, L., Feng, L., Sewry, C., MacArthur, D.G., North, K.N., Hoffman, E., Stemple, D.L., Hurles, M.E., Bokhoven, H. van, Campbell, K.P., Lefeber, D.J., Lin, Y.Y., Muntoni, F., and et al.

Abstract

Item does not contain fulltext, Congenital muscular dystrophies with hypoglycosylation of alpha-dystroglycan (alpha-DG) are a heterogeneous group of disorders often associated with brain and eye defects in addition to muscular dystrophy. Causative variants in 14 genes thought to be involved in the glycosylation of alpha-DG have been identified thus far. Allelic mutations in these genes might also cause milder limb-girdle muscular dystrophy phenotypes. Using a combination of exome and Sanger sequencing in eight unrelated individuals, we present evidence that mutations in guanosine diphosphate mannose (GDP-mannose) pyrophosphorylase B (GMPPB) can result in muscular dystrophy variants with hypoglycosylated alpha-DG. GMPPB catalyzes the formation of GDP-mannose from GTP and mannose-1-phosphate. GDP-mannose is required for O-mannosylation of proteins, including alpha-DG, and it is the substrate of cytosolic mannosyltransferases. We found reduced alpha-DG glycosylation in the muscle biopsies of affected individuals and in available fibroblasts. Overexpression of wild-type GMPPB in fibroblasts from an affected individual partially restored glycosylation of alpha-DG. Whereas wild-type GMPPB localized to the cytoplasm, five of the identified missense mutations caused formation of aggregates in the cytoplasm or near membrane protrusions. Additionally, knockdown of the GMPPB ortholog in zebrafish caused structural muscle defects with decreased motility, eye abnormalities, and reduced glycosylation of alpha-DG. Together, these data indicate that GMPPB mutations are responsible for congenital and limb-girdle muscular dystrophies with hypoglycosylation of alpha-DG.

Published
2013

27. Mutations in TPM2 and congenital fibre type disproportion

Author

Clarke, N.F., Waddell, L.B., Sie, L.T.L., van Bon, B.W., McLean, C., Clark, D., Kornberg, A., Lammens, M.M., North, K.N., Clarke, N.F., Waddell, L.B., Sie, L.T.L., van Bon, B.W., McLean, C., Clark, D., Kornberg, A., Lammens, M.M., and North, K.N.

Abstract

Item does not contain fulltext, The main diagnostic feature of congenital fibre type disproportion is that type 1 fibres are consistently smaller than type 2 fibres in the absence of other histological abnormalities. Mutations in the TPM3, RYR1 and ACTA1 genes are the most common established genetic causes. There has been one previous report of congenital fibre type disproportion due to a mutation in TPM2, although some atypical histological features were present. We present two cases in which novel de novo missense mutations in TPM2 are associated with marked fibre size disproportion. The finding of typical histological changes of congenital fibre type disproportion in association with a p.Ser61Pro mutation confirms that TPM2 can cause typical congenital fibre type disproportion. Although not seen on light microscopy studies, protein inclusions typical of small 'caps' were found on electron microscopy in a second patient with a p.Ala155Val mutation in TPM2. This case emphasises the importance of electron microscopy in patients with presumed congenital fibre type disproportion, to exclude the presence of caps, nemaline bodies or minicores, which, if present, may be very helpful in guiding genetic analysis.

Published
2012

28. Mutations in TPM3 are a common cause of congenital fiber type disproportion.

Author

Laing N.G., Lim E., Smith R.L.L., Patel R., Fahey M.C., Bellance R., Romero N.B., Johnson E.S., Labarre-Vila A., Monnier N., North K.N., Clarke N.F., Kolski H., Dye D.E., Laing N.G., Lim E., Smith R.L.L., Patel R., Fahey M.C., Bellance R., Romero N.B., Johnson E.S., Labarre-Vila A., Monnier N., North K.N., Clarke N.F., Kolski H., and Dye D.E.

Abstract

Objective: Congenital fiber type disproportion (CFTD) is a rare form of congenital myopathy in which the principal histological abnormality is hypotrophy of type 1 (slow-twitch) fibers compared with type 2 (fast-twitch) fibers. To date, mutation of ACTA1 and SEPN1 has been associated with CFTD, but the genetic basis in most patients is unclear. The gene encoding alpha-tropomyosinslow (TPM3) is a rare cause of nemaline myopathy, previously reported in only five families. We investigated whether mutation of TPM3 is a cause of CFTD. Methods and Results: We sequenced TPM3 in 23 unrelated probands with CFTD or CFTD-like presentations of unknown cause and identified novel heterozygous missense mutations in five CFTD families (p. Leu100Met, p.Arg168Cys, p.Arg168Gly, p.Lys169Glu, p.Arg245Gly). All affected family members that underwent biopsy had typical histological features of CFTD, with type 1 fibers, on average, at least 50% smaller than type 2 fibers. We also report a sixth family in which a recurrent TPM3 mutation (p.Arg168His) was associated with histological features of CFTD and nemaline myopathy in different family members. We describe the clinical features of 11 affected patients. Typically, there was proximal limb girdle weakness, prominent weakness of neck flexion and ankle dorsiflexion, mild facial weakness, and mild ptosis. The age of onset and severity varied, even within the same family. Many patients required nocturnal noninvasive ventilation despite remaining ambulant. Interpretation(s): Mutation of TPM3 is the most common cause of CFTD reported to date. © 2008 American Neurological Association. Published by Wiley-Liss, Inc.

Published
2012

29. Dominant mutations in KBTBD13, a member of the BTB/Kelch family, cause nemaline myopathy with cores.

Author

Sambuughin, N., Yau, K.S., Duff, R.M., Bayarsaikhan, M., Lu, S.J., Gonzalez-Mera, L., Sivadorai, P., Nowak, K.J., Ravenscroft, G., Mastaglia, F.L., North, K.N., Ilkovski, B., Kremer, H., Lammens, M.M., Engelen, B.G.M. van, Fabian, V., Lamont, P., Davis, M.R., Laing, N.G., Goldfarb, L.G., Sambuughin, N., Yau, K.S., Duff, R.M., Bayarsaikhan, M., Lu, S.J., Gonzalez-Mera, L., Sivadorai, P., Nowak, K.J., Ravenscroft, G., Mastaglia, F.L., North, K.N., Ilkovski, B., Kremer, H., Lammens, M.M., Engelen, B.G.M. van, Fabian, V., Lamont, P., Davis, M.R., Laing, N.G., and Goldfarb, L.G.

Abstract

Item does not contain fulltext

Published
2011

30. Fetal akinesia: review of the genetics of the neuromuscular causes

Author

Ravenscroft, G., Sollis, E., Charles, A.K., North, K.N., Baynam, G., Laing, N.G., Ravenscroft, G., Sollis, E., Charles, A.K., North, K.N., Baynam, G., and Laing, N.G.

Abstract

Fetal akinesia refers to a broad spectrum of disorders in which the unifying feature is a reduction or lack of fetal movement. Fetal akinesias may be caused by defects at any point along the motor system pathway including the central and peripheral nervous system, the neuromuscular junction and the muscle, as well as by restrictive dermopathy or external restriction of the fetus in utero. The fetal akinesias are clinically and genetically heterogeneous, with causative mutations identified to date in a large number of genes encoding disparate parts of the motor system. However, for most patients, the molecular cause remains unidentified. One reason for this is because the tools are only now becoming available to efficiently and affordably identify mutations in a large panel of disease genes. Next-generation sequencing offers the promise, if sufficient cohorts of patients can be assembled, to identify the majority of the remaining genes on a research basis and facilitate efficient clinical molecular diagnosis. The benefits of identifying the causative mutation(s) for each individual patient or family include accurate genetic counselling and the options of prenatal diagnosis or preimplantation genetic diagnosis. In this review, we summarise known single-gene disorders affecting the spinal cord, peripheral nerves, neuromuscular junction or skeletal muscles that result in fetal akinesia. This audit of these known molecular and pathophysiological mechanisms involved in fetal akinesia provides a basis for improved molecular diagnosis and completing disease gene discovery.

Published
2011

31. Dominant mutations in KBTBD13, a member of the BTB/Kelch family, cause nemaline myopathy with cores.

Author

Sambuughin, N., Yau, K.S., Olive, M., Duff, R.M., Bayarsaikhan, M., Lu, S., Gonzalez-Mera, L., Sivadorai, P., Nowak, K.J., Ravenscroft, G., Mastaglia, F.L., North, K.N., Ilkovski, B., Kremer, J.M.J., Lammens, M.M.Y., Engelen, B.G.M. van, Fabian, V., Lamont, P., Davis, M.R., Laing, N.G., Goldfarb, L.G., Sambuughin, N., Yau, K.S., Olive, M., Duff, R.M., Bayarsaikhan, M., Lu, S., Gonzalez-Mera, L., Sivadorai, P., Nowak, K.J., Ravenscroft, G., Mastaglia, F.L., North, K.N., Ilkovski, B., Kremer, J.M.J., Lammens, M.M.Y., Engelen, B.G.M. van, Fabian, V., Lamont, P., Davis, M.R., Laing, N.G., and Goldfarb, L.G.

Abstract

Contains fulltext : 88858.pdf (publisher's version ) (Closed access), We identified a member of the BTB/Kelch protein family that is mutated in nemaline myopathy type 6 (NEM6), an autosomal-dominant neuromuscular disorder characterized by the presence of nemaline rods and core lesions in the skeletal myofibers. Analysis of affected families allowed narrowing of the candidate region on chromosome 15q22.31, and mutation screening led to the identification of a previously uncharacterized gene, KBTBD13, coding for a hypothetical protein and containing missense mutations that perfectly cosegregate with nemaline myopathy in the studied families. KBTBD13 contains a BTB/POZ domain and five Kelch repeats and is expressed primarily in skeletal and cardiac muscle. The identified disease-associated mutations, C.742C>A (p.Arg248Ser), c.1170G>C (p.Lys390Asn), and c.1222C>T (p.Arg408Cys), located in conserved domains of Kelch repeats, are predicted to disrupt the molecule's beta-propeller blades. Previously identified BTB/POZ/Kelch-domain-containing proteins have been implicated in a broad variety of biological processes, including cytoskeleton modulation, regulation of gene transcription, ubiquitination, and myofibril assembly. The functional role of KBTBD13 in skeletal muscle and the pathogenesis of NEM6 are subjects for further studies.

Published
2010

35. O.10 Mutations in a new dynein/dynactin adaptor gene cause Dominant Congenital Spinal Muscular Atrophy (DCSMA) and Hereditary Spastic Paraplegia (HSP)

Author

Oates, E.C., primary, Rosser, A.M., additional, Hafezparast, M., additional, Lek, M., additional, Scoto, M., additional, Greensmith, L., additional, Auer-Grumbach, M., additional, Schule, R., additional, Herrmann, D.N., additional, Clarke, N.F., additional, MacArthur, D.G., additional, Züchner, S., additional, Muntoni, F., additional, Reilly, M.M., additional, and North, K.N., additional

Published
2013
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36. C.P.15 K7del is a recurrent TPM2 nemaline myopathy mutation associated with joint contractures and increased calcium sensitivity

Author

Mokbel, N., primary, Ilkovski, B., additional, Memo, M., additional, Marttila, M., additional, Kreissl, M., additional, Wallgren-Pettersson, C., additional, Menard, D., additional, Marcorelles, P., additional, Echaniz-Laguna, A., additional, Reimann, J., additional, Vainzof, M., additional, Monnier, N., additional, Nowak, K., additional, McNamara, E., additional, Laing, N.G., additional, Trewhella, J., additional, Jeffries, C., additional, Ottenheijm, C., additional, North, K.N., additional, and Clarke, N.F., additional

Published
2012
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49. P1.23 Muscle membrane repair proteins are upregulated in muscular dystrophy and localise to t-tubule membranes following mechanical stretch

Author

Waddell, L.B., primary, Lemckert, F., additional, Tran, J., additional, Zheng, F., additional, Evesson, F.J., additional, Hawkes, J., additional, Lek, A., additional, Street, N., additional, Lin, P., additional, Clarke, N.F., additional, Weisleder, N., additional, Ma, J., additional, North, K.N., additional, and Cooper, S.T., additional

Published
2010
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