Your search keyword '"Phillipa J. Lamont"' showing total 32 results

1. A novel RFC1 repeat motif (ACAGG) in two Asia-Pacific CANVAS families

Author

Mark R. Davis, Henry Houlden, Roisin Sullivan, Andrea Cortese, Sarah J. Beecroft, Richard Roxburgh, Carolin K. Scriba, Wai Yan Yau, Natalia Dominik, Teddy Y. Wu, Mary M. Reilly, Zoe Dyer, Gianina Ravenscroft, Miriam Rodrigues, Phillipa J. Lamont, Joshua S. Clayton, Ben Weisburd, David Chandler, Nigel G. Laing, and Elizabeth B. Walker

Subjects

0301 basic medicine, Genetics, Vestibular areflexia, Cerebellar ataxia, Haplotype, Intron, Biology, Phenotype, law.invention, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, law, Report, medicine, Neurology (clinical), Allele, medicine.symptom, Trinucleotide repeat expansion, 030217 neurology & neurosurgery, Polymerase chain reaction

Abstract

Cerebellar ataxia, neuropathy and vestibular areflexia syndrome (CANVAS) is a progressive late-onset, neurological disease. Recently, a pentanucleotide expansion in intron 2 of RFC1 was identified as the genetic cause of CANVAS. We screened an Asian-Pacific cohort for CANVAS and identified a novel RFC1 repeat expansion motif, (ACAGG)exp, in three affected individuals. This motif was associated with additional clinical features including fasciculations and elevated serum creatine kinase. These features have not previously been described in individuals with genetically-confirmed CANVAS. Haplotype analysis showed our patients shared the same core haplotype as previously published, supporting the possibility of a single origin of the RFC1 disease allele. We analysed data from >26 000 genetically diverse individuals in gnomAD to show enrichment of (ACAGG) in non-European populations.

Published

2020

2. The Impact of Next-Generation Sequencing on the Diagnosis, Treatment, and Prevention of Hereditary Neuromuscular Disorders

Author

Nigel G. Laing, Mark R. Davis, Samantha Edwards, Phillipa J. Lamont, Sarah J. Beecroft, Hayley Goullee, and Gianina Ravenscroft

Subjects

0301 basic medicine, Pharmacology, Neuromuscular disease, business.industry, Genetic counseling, General Medicine, Consanguinity, Disease, Computational biology, medicine.disease, Human genetics, DNA sequencing, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Genetics, Molecular Medicine, Medicine, business, Gene, Exome sequencing

Abstract

The impact of high-throughput sequencing in genetic neuromuscular disorders cannot be overstated. The ability to rapidly and affordably sequence multiple genes simultaneously has enabled a second golden age of Mendelian disease gene discovery, with flow-on impacts for rapid genetic diagnosis, evidence-based treatment, tailored therapy development, carrier-screening, and prevention of disease recurrence in families. However, there are likely many more neuromuscular disease genes and mechanisms to be discovered. Many patients and families remain without a molecular diagnosis following targeted panel sequencing, clinical exome sequencing, or even genome sequencing. Here we review how massively parallel, or next-generation, sequencing has changed the field of genetic neuromuscular disorders, and anticipate future benefits of recent technological innovations such as RNA-seq implementation and detection of tandem repeat expansions from short-read sequencing.

Published

2020

3. Partial loss-of-function variant in neuregulin 1 identified in family with heritable peripheral neuropathy

Author

Daniel E. Lysko, Ana M. Meireles, Chiara Folland, Elyshia McNamara, Nigel G. Laing, Phillipa J. Lamont, Gianina Ravenscroft, and William S. Talbot

Subjects

Charcot-Marie-Tooth Disease, Neuregulin-1, Genetics, Animals, Humans, Schwann Cells, Genetics (clinical), Axons, Myelin Sheath, Zebrafish

Abstract

Neuregulin 1 signals are essential for the development and function of Schwann cells, which form the myelin sheath on peripheral axons. Disruption of myelin in the peripheral nervous system can lead to peripheral neuropathy, which is characterized by reduced axonal conduction velocity and sensorimotor deficits. Charcot-Marie-Tooth disease is a group of heritable peripheral neuropathies that may be caused by variants in nearly 100 genes. Despite the evidence that Neuregulin 1 is essential for many aspects of Schwann cell development, previous studies have not reported variants in the neuregulin 1 gene (NRG1) in patients with peripheral neuropathy. We have identified a rare missense variant in NRG1 that is homozygous in a patient with sensory and motor deficits consistent with mixed axonal and de-myelinating peripheral neuropathy. Our in vivo functional studies in zebrafish indicate that the patient variant partially reduces NRG1 function. This study tentatively suggests that variants at the NRG1 locus may cause peripheral neuropathy and that NRG1 should be investigated in families with peripheral neuropathy of unknown cause.

Published

2022

4. Genomic sequencing highlights the diverse molecular causes of Perrault syndrome: a peroxisomal disorder (PEX6), metabolic disorders (CLPP, GGPS1), and mtDNA maintenance/translation disorders (LARS2, TFAM)

Author

Sandra Whalen, Juliette Dupont, Sandrine Vuillaumier-Barrot, Chloe Hanna, Gorjana Robevska, Phillipa J. Lamont, Lurdes Sampaio, John Christodoulou, Rocio Rius, Elena J. Tucker, André Travessa, Jocelyn van den Bergen, Andrew H. Sinclair, Arnaud Isapof, Katrina M. Bell, Andrea Simpson, Jérôme Dulon, Sylvie Jaillard, Tanya Stojkovic, Susana Quijano-Roy, David R. Thorburn, Katie L. Ayers, Philippe Touraine, Murdoch Children's Research Institute (MCRI), University of Melbourne, CHU Pontchaillou [Rennes], Institut de recherche en santé, environnement et travail (Irset), Université d'Angers (UA)-Université de Rennes (UR)-École des Hautes Études en Santé Publique [EHESP] (EHESP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique ), Sorbonne Université (SU), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), AP-HP - Hôpital Bichat - Claude Bernard [Paris], Filière Neuromusculaire (FILNEMUS), Université de Versailles Saint-Quentin-en-Yvelines (UVSQ), National Health and Medical Research Council (NHMRC)National Health and Medical Research Council of Australia [1113531], NHMRCNational Health and Medical Research Council of Australia [1074258, 1054432, 1062854, 1155244], CONACYTConsejo Nacional de Ciencia y Tecnologia (CONACyT), Victorian Government's Operational Infrastructure Support Program, Université d'Angers (UA)-Université de Rennes 1 (UR1), and Université de Rennes (UNIV-RENNES)-Université de Rennes (UNIV-RENNES)-École des Hautes Études en Santé Publique [EHESP] (EHESP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique )

Subjects

Adult, Male, Candidate gene, Adolescent, Mitochondrial translation, Hearing Loss, Sensorineural, [SDV]Life Sciences [q-bio], Gene Expression, Biology, DNA, Mitochondrial, Amino Acyl-tRNA Synthetases, Mitochondrial Proteins, 03 medical and health sciences, Peroxisomal disorder, Genetics, medicine, Peroxisomes, Farnesyltranstransferase, Humans, Genetic Predisposition to Disease, Child, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Base Sequence, 030305 genetics & heredity, Ovary, High-Throughput Nucleotide Sequencing, Geranyltranstransferase, Endopeptidase Clp, TFAM, medicine.disease, Dimethylallyltranstransferase, Human genetics, Premature ovarian failure, Gonadal Dysgenesis, 46,XX, Pedigree, DNA-Binding Proteins, Protein prenylation, ATPases Associated with Diverse Cellular Activities, Female, PEX6, Transcription Factors

Abstract

International audience; Perrault syndrome is a rare heterogeneous condition characterised by sensorineural hearing loss and premature ovarian insufficiency. Additional neuromuscular pathology is observed in some patients. There are six genes in which variants are known to cause Perrault syndrome; however, these explain only a minority of cases. We investigated the genetic cause of Perrault syndrome in seven affected individuals from five different families, successfully identifying the cause in four patients. This included previously reported and novel causative variants in known Perrault syndrome genes, CLPP and LARS2, involved in mitochondrial proteolysis and mitochondrial translation, respectively. For the first time, we show that pathogenic variants in PEX6 can present clinically as Perrault syndrome. PEX6 encodes a peroxisomal biogenesis factor, and we demonstrate evidence of peroxisomal dysfunction in patient serum. This study consolidates the clinical overlap between Perrault syndrome and peroxisomal disorders, and highlights the need to consider ovarian function in individuals with atypical/mild peroxisomal disorders. The remaining patients had variants in candidate genes such as TFAM, involved in mtDNA transcription, replication, and packaging, and GGPS1 involved in mevalonate/coenzyme Q(10) biosynthesis and whose enzymatic product is required for mouse folliculogenesis. This genomic study highlights the diverse molecular landscape of this poorly understood syndrome.

Published

2020

5. Mutations in ATP1A1 Cause Dominant Charcot-Marie-Tooth Type 2

Author

Dana Šafka Brožková, Rene Barro-Soria, H. Peter Larsson, Petra Laššuthová, Shawna M. E. Feely, Pavel Seeman, Eric Powell, Yi-Chung Lee, Elena Buglo, Daniel G. Isom, Cima Saghira, Feifei Tao, Royston Ong, Yunhong Bai, Steven S. Scherer, Lorna Marns, Chelsea Bacon, Gianina Ravenscroft, Megan F. Baxter, Lisa Abreu, Stephan Züchner, Jana Haberlová, Phillipa J. Lamont, Adriana P. Rebelo, Fiore Manganelli, Mark R. Davis, Lucio Santoro, Steve Courel, Ki Wha Chung, Dana M. Bis, Radim Mazanec, Michael E. Shy, Byung Ok Choi, Nigel G. Laing, Lassuthova, Petra, Rebelo, Adriana P., Ravenscroft, Gianina, Lamont, Phillipa J., Davis, Mark R., Manganelli, Fiore, Feely, Shawna M., Bacon, Chelsea, Brožková, Dana Šafka, Haberlova, Jana, Mazanec, Radim, Tao, Feifei, Saghira, Cima, Abreu, Lisa, Courel, Steve, Powell, Eric, Buglo, Elena, Bis, Dana M., Baxter, Megan F., Ong, Royston W., Marns, Lorna, Lee, Yi-Chung, Bai, Yunhong, Isom, Daniel G., Barro-Soria, René, Chung, Ki W., Scherer, Steven S., Larsson, H. Peter, Laing, Nigel G., Choi, Byung-Ok, Seeman, Pavel, Shy, Michael E., Santoro, Lucio, and Zuchner, Stephan

Subjects

Adult, Male, 0301 basic medicine, Charcot-Marie-Tooth, axonal neuropathy, Protein subunit, Mutant, Xenopus, Biology, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Genetic, Charcot-Marie-Tooth Disease, Report, Genetics, Humans, Missense mutation, Family, Amino Acid Sequence, Na+,K+ATPase, Na+/K+-ATPase, Child, Gene, Genetics (clinical), Aged, Genes, Dominant, Aged, 80 and over, CMT, genetic matchmaking, ATP1A1, Middle Aged, biology.organism_classification, Molecular biology, Axolemma, Pedigree, 030104 developmental biology, Mutation, Female, Mendelian disease, Sodium-Potassium-Exchanging ATPase, 030217 neurology & neurosurgery, Immunostaining

Abstract

Although mutations in more than 90 genes are known to cause CMT, the underlying genetic cause of CMT remains unknown in more than 50% of affected individuals. The discovery of additional genes that harbor CMT2-causing mutations increasingly depends on sharing sequence data on a global level. In this way—by combining data from seven countries on four continents—we were able to define mutations in ATP1A1, which encodes the alpha1 subunit of the Na+,K+-ATPase, as a cause of autosomal-dominant CMT2. Seven missense changes were identified that segregated within individual pedigrees: c.143T>G (p.Leu48Arg), c.1775T>C (p.Ile592Thr), c.1789G>A (p.Ala597Thr), c.1801_1802delinsTT (p.Asp601Phe), c.1798C>G (p.Pro600Ala), c.1798C>A (p.Pro600Thr), and c.2432A>C (p.Asp811Ala). Immunostaining peripheral nerve axons localized ATP1A1 to the axolemma of myelinated sensory and motor axons and to Schmidt-Lanterman incisures of myelin sheaths. Two-electrode voltage clamp measurements on Xenopus oocytes demonstrated significant reduction in Na+ current activity in some, but not all, ouabain-insensitive ATP1A1 mutants, suggesting a loss-of-function defect of the Na+,K+ pump. Five mutants fall into a remarkably narrow motif within the helical linker region that couples the nucleotide-binding and phosphorylation domains. These findings identify a CMT pathway and a potential target for therapy development in degenerative diseases of peripheral nerve axons.

Published

2018

6. New era in genetics of early-onset muscle disease: Breakthroughs and challenges

Author

Phillipa J. Lamont, Alistair R. R. Forrest, Gianina Ravenscroft, Mark R. Davis, and Nigel G. Laing

Subjects

0301 basic medicine, Genetics, Genetic heterogeneity, Genetic counseling, Cell Biology, Disease, Geneticist, Biology, medicine.disease, Congenital myopathy, Hypotonia, 3. Good health, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Congenital muscular dystrophy, medicine, Centronuclear myopathy, medicine.symptom, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Early-onset muscle disease includes three major entities that present generally at or before birth: congenital myopathies, congenital muscular dystrophies and congenital myasthenic syndromes. Almost exclusively there is weakness and hypotonia, although cases manifesting hypertonia are increasingly being recognised. These diseases display a wide phenotypic and genetic heterogeneity, with the uptake of next generation sequencing resulting in an unparalleled extension of the phenotype-genotype correlations and "diagnosis by sequencing" due to unbiased sequencing. Perhaps now more than ever, detailed clinical evaluations are necessary to guide the genetic diagnosis; with arrival at a molecular diagnosis frequently occurring following dialogue between the molecular geneticist, the referring clinician and the pathologist. There is an ever-increasing blurring of the boundaries between the congenital myopathies, dystrophies and myasthenic syndromes. In addition, many novel disease genes have been described and new insights have been gained into skeletal muscle development and function. Despite the advances made, a significant percentage of patients remain without a molecular diagnosis, suggesting that there are many more human disease genes and mechanisms to identify. It is now technically- and clinically-feasible to perform next generation sequencing for severe diseases on a population-wide scale, such that preconception-carrier screening can occur. Newborn screening for selected early-onset muscle diseases is also technically and ethically-achievable, with benefits to the patient and family from early management of these diseases and should also be implemented. The need for world-wide Reference Centres to meticulously curate polymorphisms and mutations within a particular gene is becoming increasingly apparent, particularly for interpretation of variants in the large genes which cause early-onset myopathies: NEB, RYR1 and TTN. Functional validation of candidate disease variants is crucial for accurate interpretation of next generation sequencing and appropriate genetic counseling. Many published "pathogenic" variants are too frequent in control populations and are thus likely rare polymorphisms. Mechanisms need to be put in place to systematically update the classification of variants such that accurate interpretation of variants occurs. In this review, we highlight the recent advances made and the challenges ahead for the molecular diagnosis of early-onset muscle diseases.

Published

2017

7. The genetic landscape of axonal neuropathies in the middle-aged and elderly: Focus on MME

Author

Julia Wanschitz, Manuela Wiessner, Rebecca Schüle, Royston Ong, Jennefer N. Kohler, Katharina Kinslechner, Pavel Seeman, Katja Eggermann, Bruno Francou, Marina L. Kennerson, Sabine Rudnik-Schöneborn, Garth Nicholson, Lois Dankwa, Jochen Weishaupt, Wilson Marques, T Deconinck, Tanya Stojkovic, Lisa Abreu, Anja Schirmacher, Jan Senderek, Christian Beetz, Matthis Synofzik, Stephan Iglseder, Susanne Petri, Michaela Auer-Grumbach, Nigel G. Laing, Rita Horvath, Geir J. Braathen, Reinhard Windhager, Petra Lassuthova, Jonathan Baets, Albert Ludolph, Peter De Jonghe, David N. Herrmann, Ingo Kurth, Bianca Dräger, Gianina Ravenscroft, Adriana P. Rebelo, Beate Schlotter-Weigel, Tim M. Strom, Phillipa J. Lamont, Stefan Toegel, Daniela Weinmann, David A. Brenner, Andrzej Kochański, Dagmara Kabzińska, Joline Dalton, David Walk, Carina Fischer, Giulia Ricci, Helle Høyer, Ludger Schoels, Stephan Züchner, Peter Young, Löscher Wolfgang N, Johannes Wagner, Melina Ellis, Dankwa, Lois [0000-0002-0259-9550], Kurth, Ingo [0000-0002-5642-8378], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Male, Aging, Population, blood [Neprilysin], Disease, Genetic analysis, Whole Exome Sequencing, genetics [Neprilysin], 03 medical and health sciences, 0302 clinical medicine, blood [Hereditary Sensory and Motor Neuropathy], Charcot-Marie-Tooth Disease, blood [Charcot-Marie-Tooth Disease], Exome Sequencing, blood [Aging], Medicine, Humans, Genetic Predisposition to Disease, ddc:610, genetics [Genetic Predisposition to Disease], Allele, Age of Onset, education, Neprilysin, Exome sequencing, Aged, Genetics, education.field_of_study, business.industry, genetics [Hereditary Sensory and Motor Neuropathy], High-Throughput Nucleotide Sequencing, Middle Aged, Phenotype, 030104 developmental biology, Female, Neurology (clinical), genetics [Charcot-Marie-Tooth Disease], Age of onset, business, Hereditary Sensory and Motor Neuropathy, 030217 neurology & neurosurgery

Abstract

ObjectiveTo test the hypothesis that monogenic neuropathies such as Charcot-Marie-Tooth disease (CMT) contribute to frequent but often unexplained neuropathies in the elderly, we performed genetic analysis of 230 patients with unexplained axonal neuropathies and disease onset ≥35 years.MethodsWe recruited patients, collected clinical data, and conducted whole-exome sequencing (WES; n = 126) and MME single-gene sequencing (n = 104). We further queried WES repositories for MME variants and measured blood levels of the MME-encoded protein neprilysin.ResultsIn the WES cohort, the overall detection rate for assumed disease-causing variants in genes for CMT or other conditions associated with neuropathies was 18.3% (familial cases 26.4%, apparently sporadic cases 12.3%). MME was most frequently involved and accounted for 34.8% of genetically solved cases. The relevance of MME for late-onset neuropathies was further supported by detection of a comparable proportion of cases in an independent patient sample, preponderance of MME variants among patients compared to population frequencies, retrieval of additional late-onset neuropathy patients with MME variants from WES repositories, and low neprilysin levels in patients' blood samples. Transmission of MME variants was often consistent with an incompletely penetrant autosomal-dominant trait and less frequently with autosomal-recessive inheritance.ConclusionsA detectable fraction of unexplained late-onset axonal neuropathies is genetically determined, by variants in either CMT genes or genes involved in other conditions that affect the peripheral nerves and can mimic a CMT phenotype. MME variants can act as completely penetrant recessive alleles but also confer dominantly inherited susceptibility to axonal neuropathies in an aging population.

Published

2020

8. A mutation in MT-TW causes a tRNA processing defect and reduced mitochondrial function in a family with Leigh syndrome

Author

Rachael M. Duff, Judith A. Ermer, Aleksandra Filipovska, Tara R. Richman, Shanti Balasubramaniam, Rebecca Gooding, Oliver Rackham, David R. Thorburn, Phillipa J. Lamont, Anne-Marie J. Shearwood, and Giulia Rossetti

Subjects

Male, Mitochondrial disease, TRNA processing, Biology, Mitochondrion, medicine, Humans, Point Mutation, RNA Processing, Post-Transcriptional, Leigh disease, Child, Molecular Biology, Cells, Cultured, Family Health, Genetics, Siblings, Point mutation, Infant, Newborn, Infant, Cell Biology, Fibroblasts, RNA, Transfer, Trp, medicine.disease, Molecular biology, MT-TW, Mitochondria, Child, Preschool, Lactic acidosis, Transfer RNA, Molecular Medicine, Female, Leigh Disease

Abstract

Leigh syndrome (LS) is a progressive mitochondrial neurodegenerative disorder, whose symptoms most commonly include psychomotor delay with regression, lactic acidosis and a failure to thrive. Here we describe three siblings with LS, but with additional manifestations including hypertrophic cardiomyopathy, hepatosplenomegaly, cholestatic hepatitis, and seizures. All three affected siblings were found to be homoplasmic for an m. 5559A>G mutation in the T stem of the mitochondrial DNA-encoded MT-TW by next generation sequencing. The m.5559A>G mutation causes a reduction in the steady state levels of tRNA(Trp) and this decrease likely affects the stability of other mitochondrial RNAs in the patient fibroblasts. We observe accumulation of an unprocessed transcript containing tRNA(Trp), decreased de novo protein synthesis and consequently lowered steady state levels of mitochondrial DNA-encoded proteins that compromise mitochondrial respiration. Our results show that the m.5559A>G mutation at homoplasmic levels causes LS in association with severe multi-organ disease (LS-plus) as a consequence of dysfunctional mitochondrial RNA metabolism.

Published

2015

9. Adult onset distal and proximal myopathy with complete ophthalmoplegia associated with a novelde novop.(Leu1877Pro) mutation inMYH2

Author

J. Boutilier, Nigel G. Laing, Phillipa J. Lamont, Fathimath Faiz, Victoria A. Fabian, Cheryl A Wise, and Macarena Cabrera-Serrano

Subjects

Genetics, Pathology, medicine.medical_specialty, Complete ophthalmoplegia, business.industry, Bulbar involvement, Oculopharyngodistal Myopathy, medicine.disease, Congenital myopathy, Phenotype, Multiple congenital contractures, Proximal myopathy, Mutation (genetic algorithm), Medicine, business, Genetics (clinical)

Abstract

An MYH2 mutation p.(Glu706Lys) was originally described in a family with autosomal dominant inheritance, where the affected family members presented with multiple congenital contractures and ophthalmoplegia, progressing to a proximal myopathy in adulthood. Another patient with a dominant mutation p.(Leu1870Pro) was described, presenting as a congenital myopathy with ophthalmoplegia. Here, we present a patient with symptoms beginning at age 16 years, of prominent distal but also proximal weakness, bulbar involvement and ophthalmoplegia. Initially, clinically classified as oculopharyngodistal myopathy, the patient was found to carry a novel, de novo MYH2 mutation c.5630T>C p.(Leu1877Pro). This expands the phenotype of dominant MYH2 myopathies with the clinical phenotype overlapping the oculopharyngodistal myopathy spectrum.

Published

2015

10. STRetch: detecting and discovering pathogenic short tandem repeat expansions

Author

Andrew Lonsdale, Nigel G. Laing, Alicia Oshlack, Joshua S. Clayton, Belinda Phipson, Harriet Dashnow, Daniel G. MacArthur, Simon Sadedin, Andreas Halman, Mark R. Davis, Phillipa J. Lamont, and Monkol Lek

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, lcsh:QH426-470, STR multiplex system, Sequencing data, Method, Computational biology, Biology, Polymerase Chain Reaction, Genome, law.invention, Structural variation, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, law, Genotype, Chromosomes, Human, Humans, lcsh:QH301-705.5, Polymerase chain reaction, Alleles, 030304 developmental biology, Whole genome sequencing, Genetics, 0303 health sciences, DNA Repeat Expansion, Genome, Human, social sciences, Short read, Human genetics, humanities, eye diseases, 3. Good health, lcsh:Genetics, 030104 developmental biology, lcsh:Biology (General), Genetic Loci, Mendelian inheritance, symbols, Microsatellite, Human genome, Software, geographic locations, 030217 neurology & neurosurgery, Microsatellite Repeats

Abstract

Short tandem repeat (STR) expansions have been identified as the causal DNA mutation in dozens of Mendelian diseases. Historically, pathogenic STR expansions could only be detected by single locus techniques, such as PCR and electrophoresis. The ability to use short read sequencing data to screen for STR expansions has the potential to reduce both the time and cost to reaching diagnosis and enable the discovery of new causal STR loci. Most existing tools detect STR variation within the read length, and so are unable to detect the majority of pathogenic expansions. Those tools that can detect large expansions are limited to a set of known disease loci and as yet no new disease causing STR expansions have been identified with high-throughput sequencing technologies.Here we address this by presenting STRetch, a new genome-wide method to detect STR expansions at all loci across the human genome. We demonstrate the use of STRetch for detecting pathogenic STR expansions in short-read whole genome sequencing data with a very low false discovery rate. We further demonstrate the application of STRetch to solve cases of patients with undiagnosed disease and apply STRetch to the analysis of 97 whole genomes to reveal variation at STR loci. STRetch assesses expansions at all STR loci in the genome and allows screening for novel disease-causing STRs.STRetch is open source software, available fromgithub.com/Oshlack/STRetch.

Published

2017

11. NovelCHKBmutation expands the megaconial muscular dystrophy phenotype

Author

Macarena Cabrera-Serrano, Vanessa Atkinson, Nigel G. Laing, Padma Sivadorai, Phillipa J. Lamont, Reimar Junckerstorff, and Richard J.N. Allcock

Subjects

Genetics, Pathology, medicine.medical_specialty, Muscle biopsy, medicine.diagnostic_test, Physiology, Nonsense mutation, Biology, medicine.disease, Hypotonia, Choline kinase beta, Cellular and Molecular Neuroscience, Mitochondrial myopathy, Physiology (medical), Utrophin, medicine, Congenital muscular dystrophy, Neurology (clinical), medicine.symptom, Muscular dystrophy

Abstract

Introduction: Mutations in the choline kinase beta (CHKB) gene are associated with a congenital muscular dystrophy with giant mitochondria at the periphery of muscle fibers. Methods: We describe a patient of Italian origin in whom whole-exome sequencing revealed a novel homozygous nonsense mutation, c.648C>A, p.(Tyr216*), in exon 5 of CHKB. Results: The patient presented with limb-girdle weakness and hypotonia from birth with mental retardation, and had sudden and transient deteriorations of muscle strength with acute intercurrent illnesses. Previously undescribed sarcolemmal overexpression of utrophin was noted in the muscle biopsy. Conclusions: Pathological features broaden the description of the entity and provide new insight in the pathogenic mechanisms. This case highlights the usefulness of next-generation sequencing in the diagnosis of rare and incompletely understood conditions. Muscle Nerve 51: 140–143, 2015

Published

2014

12. EP.114A CMT family with AD and AR inheritance of a MME variant

Author

Gianina Ravenscroft, Royston Ong, Nigel G. Laing, and Phillipa J. Lamont

Subjects

Genetics, Inheritance (object-oriented programming), Neurology, Pediatrics, Perinatology and Child Health, Neurology (clinical), Biology, Genetics (clinical)

Published

2019

13. Dominant Mutations in KBTBD13, a Member of the BTB/Kelch Family, Cause Nemaline Myopathy with Cores

Author

Kyle S. Yau, Nyamkhishig Sambuughin, Baziel G.M. van Engelen, Montse Olivé, Martin Lammens, Munkhuu Bayarsaikhan, Biljana Ilkovski, Frank L. Mastaglia, Rachael M. Duff, Shajia Lu, Vicki Fabian, Kristen J. Nowak, Phillipa J. Lamont, Padma Sivadorai, Gianina Ravenscroft, Kathryn N. North, Nigel G. Laing, Hannie Kremer, Mark R. Davis, Laura Gonzalez-Mera, and Lev G. Goldfarb

Subjects

Myofibril assembly, Genetics and epigenetic pathways of disease [NCMLS 6], Molecular Sequence Data, Mutation, Missense, Muscle Proteins, Functional Neurogenomics Human Movement & Fatigue [DCN 2], Biology, Myopathies, Nemaline, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Nemaline myopathy, Report, Perception and Action [DCN 1], Genetics, medicine, Animals, Humans, Missense mutation, Genetics(clinical), Amino Acid Sequence, Age of Onset, Child, Nemaline bodies, Kelch protein, Genetics (clinical), Genes, Dominant, 030304 developmental biology, Functional Neurogenomics Renal disorder [DCN 2], Chromosomes, Human, Pair 15, 0303 health sciences, Mutation, Sequence Homology, Amino Acid, Gigaxonin, medicine.disease, Immunohistochemistry, Congenital myopathy, Genetics and epigenetic pathways of disease Functional Neurogenomics [NCMLS 6], Erratum, Functional Neurogenomics [DCN 2], 030217 neurology & neurosurgery

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

14. Clinical utility gene card for: Nemaline myopathy – update 2015

Author

Mark R. Davis, Kristen J. Nowak, Nigel G. Laing, Carina Wallgren-Pettersson, and Phillipa J. Lamont

Subjects

business.industry, Cap Disease, Muscle Proteins, Tropomyosin, medicine.disease, Bioinformatics, Myopathies, Nemaline, Congenital myopathy, Nemaline myopathy, Mutation, Genetics, Medicine, Fiber-type disproportion, Humans, Genetic Predisposition to Disease, Genetic Testing, business, Muscle, Skeletal, Gene, Genetics (clinical), Clinical Utility Gene Card Update

Published

2015

15. Expanding the phenotype of GMPPB mutations

Author

Phillipa J. Lamont, Monkol Lek, Nigel F. Clarke, Kathryn N. North, Stephen W. Reddel, Nigel G. Laing, Christina Liang, Roula Ghaoui, Simranpreet Kaur, Macarena Cabrera-Serrano, Alastair Corbett, Daniel G. MacArthur, Mark R. Davis, Leigh B. Waddell, Carolyn M. Sue, Gianina Ravenscroft, and Russell D. Johnsen

Subjects

Adult, Male, Pediatrics, medicine.medical_specialty, Adolescent, medicine.disease_cause, Young Adult, Fatal Outcome, Genotype, Intellectual disability, medicine, Humans, Muscular dystrophy, Child, Dystroglycans, Aged, Genetics, Mutation, business.industry, Muscle weakness, Middle Aged, medicine.disease, Nucleotidyltransferases, Pedigree, Phenotype, Muscular Dystrophies, Limb-Girdle, Child, Preschool, Congenital muscular dystrophy, Female, Neurology (clinical), medicine.symptom, business, Rhabdomyolysis, Limb-girdle muscular dystrophy

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

16. Mutations in the Slow Skeletal Muscle Fiber Myosin Heavy Chain Gene (MYH7) Cause Laing Early-Onset Distal Myopathy (MPD1)

Author

Elizabeth M. Petty, Marianne de Visser, Ralf Herrmann, Khema Liyanage, Danielle E. Dye, Peter Hedera, Thomas Voit, Rachael M. Duff, Phillipa J. Lamont, Christopher Meredith, Nigel G. Laing, Frank L. Mastaglia, Vicki Fabian, John K. Fink, Cheryl Parry, Maaike M. van der Graaff, Kaye Beckman, Leslie R. Bridges, Hayley J. Durling, Neurology, and Faculteit der Geneeskunde

Subjects

Candidate gene, DNA, Complementary, Medizin, Biology, medicine.disease_cause, 03 medical and health sciences, Exon, 0302 clinical medicine, Report, Myosin, medicine, Genetics, Humans, Genetics(clinical), Myopathy, Child, Muscle, Skeletal, Genetics (clinical), 030304 developmental biology, Chromosomes, Human, Pair 14, 0303 health sciences, Mutation, Myosin Heavy Chains, Skeletal muscle, Sequence Analysis, DNA, Molecular biology, Distal Myopathies, medicine.anatomical_structure, Muscle Fibers, Slow-Twitch, Haplotypes, MYH7, sense organs, medicine.symptom, 030217 neurology & neurosurgery

Abstract

We previously linked Laing-type early-onset autosomal dominant distal myopathy (MPD1) to a 22-cM region of chromosome 14. One candidate gene in the region, MYH7, which is mutated in cardiomyopathy and myosin storage myopathy, codes for the myosin heavy chain of type I skeletal muscle fibers and cardiac ventricles. We have identified five novel heterozygous mutations - Arg1500Pro, Lys1617del, Ala1663Pro, Leu1706Pro, and Lys1729del in exons 32, 34, 35, and 36 of MYH7 - in six families with early-onset distal myopathy. All five mutations are predicted, by in silico analysis, to locally disrupt the ability of the myosin tail to form the coiled coil, which is its normal structure. These findings demonstrate that heterozygous mutations toward the 3' end of MYH7 cause Laing-type early-onset distal myopathy. MYH7 is the fourth distal-myopathy gene to have been identified

Published

2004

17. Principal mutation hotspot for central core disease and related myopathies in the C-terminal transmembrane region of the RYR1 gene

Author

Kathryn N. North, Nigel G. Laing, Alison Colley, Ros Quinlivan, Thierry Kuntzer, D. James, Heinz Jungbluth, Mark R. Davis, P. Tomlinson, Joanne Dixon, Agi K. Gedeon, Caroline Sewry, A. Sanchez, Eric Haan, Clemens R. Müller, P. Walsh, L. Nagarajan, Christine Oley, Phillipa J. Lamont, Agnes Bankier, and Francesco Muntoni

Subjects

Genotype, Genetic Linkage, DNA Mutational Analysis, Molecular Sequence Data, Mutation, Missense, Biology, Exon, Nemaline myopathy, Muscular Diseases, medicine, Humans, Myopathy, Central Core, Polymorphism, Single-Stranded Conformational, Genetics (clinical), DNA Primers, Genes, Dominant, RYR1, Genetics, Sequence Homology, Amino Acid, Reverse Transcriptase Polymerase Chain Reaction, Ryanodine Receptor Calcium Release Channel, Exons, medicine.disease, Penetrance, Molecular biology, Congenital myopathy, Peptide Fragments, Pedigree, Protein Structure, Tertiary, Transmembrane domain, Haplotypes, Neurology, Pediatrics, Perinatology and Child Health, Neurology (clinical), Central core disease

Abstract

The congenital myopathies are a group of disorders characterised by the predominance of specific histological features observed in biopsied muscle. Central core disease and nemaline myopathy are examples of congenital myopathies that have specific histological characteristics but significantly overlapping clinical pictures. Central core disease is an autosomal dominant disorder with variable penetrance which has been linked principally to the gene for the skeletal muscle calcium release channel (RYR1). Two recent reports have identified the 3' transmembrane domain of this gene as a common site for mutations. Two other studies have reported single families that have features of both central core disease and nemaline myopathy (core/rod disease) caused by mutations in RYR1. Screening of the 3' region (exons 93-105) of the RYR1 gene for mutations in 27 apparently unrelated patients with either central core disease or core/rod disease by single strand conformation polymorphism analysis and DNA sequencing identified three described and nine novel mutations in 15 patients.

Published

2003

18. Novel mutations widen the phenotypic spectrum of slow skeletal/β-cardiac myosin (MYH7) distal myopathy

Author

Nuria Muelas, Zohar Argov, Juan J. Vílchez, Sini Penttilä, Volker Straub, Carsten Bonneman, Patricia G. Wheeler, Kathryn R. Wagner, Phillipa J. Lamont, Rebecca Gooding, Kym M. Boycott, Gerald F. Cox, Alan H. Beggs, Jahannaz Dastgir, Alexandru Barboi, Anne M. Connolly, David Hilton-Jones, E. Schmedding, Johanna Palmio, Elizabeth T. DeChene, NP Davies, Heinz Jungbluth, Tiina Suominen, Bjarne Udd, Kate Bushby, Peter Van den Bergh, William Wallefeld, Nigel G. Laing, Elizabeth Wraige, Christopher Staples, and Neuroprotection & Neuromodulation

Subjects

Proband, Adult, Male, Pathology, medicine.medical_specialty, Adolescent, Child, preschool, Biopsy, DNA Mutational Analysis, Cardiomyopathy, Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Myosin, Genetics, medicine, Missense mutation, Humans, Myopathy, Child, Muscle, Skeletal, Genetics (clinical), 030304 developmental biology, Aged, 0303 health sciences, Myosin Heavy Chains, Infant, Newborn, Skeletal muscle, Infant, Middle Aged, medicine.disease, Immunohistochemistry, 3. Good health, Distal Myopathies, medicine.anatomical_structure, Phenotype, young adult, MYH7, Female, medicine.symptom, mutation, Cardiac Myosins, 030217 neurology & neurosurgery

Abstract

Laing early onset distal myopathy and myosin storage myopathy are caused by mutations of slow skeletal/β-cardiac myosin heavy chain encoded by the gene MYH7, as is a common form of familial hypertrophic/dilated cardiomyopathy. The mechanisms by which different phenotypes are produced by mutations in MYH7, even in the same region of the gene, are not known. To explore the clinical spectrum and pathobiology, we screened the MYH7 gene in 88 patients from 21 previously unpublished families presenting with distal or generalized skeletal muscle weakness, with or without cardiac involvement. Twelve novel mutations have been identified in thirteen families. In one of these families, the father of the proband was found to be a mosaic for the MYH7 mutation. In eight cases, de novo mutation appeared to have occurred, which was proven in four. The presenting complaint was footdrop, sometimes leading to delayed walking or tripping, in members of 17 families (81%), with other presentations including cardiomyopathy in infancy, generalized floppiness, and scoliosis. Cardiac involvement as well as skeletal muscle weakness was identified in nine of 21 families. Spinal involvement such as scoliosis or rigidity was identified in 12 (57%). This report widens the clinical and pathological phenotypes, and the genetics of MYH7 mutations leading to skeletal muscle diseases.

Published

2014

19. An mtDNA Mutation in the Initiation Codon of the Cytochrome C Oxidase Subunit II Gene Results in Lower Levels of the Protein and a Mitochondrial Encephalomyopathy

Author

Michael G. Hanna, Kim M. Clark, Richard M. Andrews, Isobel P. Nelson, Patrick F. Chinnery, Douglass M. Turnbull, Robert W. Taylor, Margaret A. Johnson, Robert N. Lightowlers, Zofia M.A. Chrzanowska-Lightowlers, Phillipa J. Lamont, and Nicholas W. Wood

Subjects

Mitochondrial encephalomyopathy, Adult, Male, Mitochondrial DNA, Mitochondrial disease, Codon, Initiator, Biology, Heteroplasmy, DNA, Mitochondrial, Mitochondrial cytopathy, Electron Transport Complex IV, 03 medical and health sciences, 0302 clinical medicine, Mitochondrial myopathy, Mitochondrial Encephalomyopathies, medicine, Genetics, Cytochrome c oxidase, Humans, Point Mutation, Genetics(clinical), RNA, Messenger, Genetics (clinical), RNA, Transfer, Ser, 030304 developmental biology, Molecular pathology, 0303 health sciences, RNA, Transfer, Asp, Translation inhibition, mtDNA, Cytochrome c oxidase subunit II, Point mutation, Middle Aged, medicine.disease, Protein Biosynthesis, biology.protein, COX deficiency, Female, 030217 neurology & neurosurgery, Research Article

Abstract

SummaryA novel heteroplasmic 7587T→C mutation in the mitochondrial genome which changes the initiation codon of the gene encoding cytochrome c oxidase subunit II (COX II), was found in a family with mitochondrial disease. This T→C transition is predicted to change the initiating methionine to threonine. The mutation load was present at 67% in muscle from the index case and at 91% in muscle from the patient's clinically affected son. Muscle biopsy samples revealed isolated COX deficiency and mitochondrial proliferation. Single-muscle-fiber analysis revealed that the 7587C copy was at much higher load in COX-negative fibers than in COX-positive fibers. After microphotometric enzyme analysis, the mutation was shown to cause a decrease in COX activity when the mutant load was >55%–65%. In fibroblasts from one family member, which contained >95% mutated mtDNA, there was no detectable synthesis or any steady-state level of COX II. This new mutation constitutes a new mechanism by which mtDNA mutations can cause disease-defective initiation of translation.

Published

1999

20. Genetics of Muscle Disease

Author

Kristen J. Nowak, Nigel G. Laing, and Phillipa J. Lamont

Subjects

Genetics, Skeletal muscle disease, Muscle disease, business.industry, Genetic counseling, Medicine, Dystrophy, Mutation detection, medicine.symptom, business, Myopathy, DNA sequencing, Gene Discovery

Published

2013

21. Respiratory chain complex I deficiency caused by mitochondrial DNA mutations

Author

Helen Swalwell, Canny Sugiana, Emma L. Blakely, Robert McFarland, Phillipa J. Lamont, David R. Thorburn, Renato Salemi, Elena J. Tucker, Douglass M. Turnbull, Alison G. Compton, Bi-Xia Ke, Denise M. Kirby, Robert W. Taylor, and Anna L. Mitchell

Subjects

Adult, Mitochondrial DNA, Nuclear gene, Mitochondrial Diseases, Adolescent, Mitochondrial disease, Genetic counseling, Respiratory chain, Inheritance Patterns, Biology, medicine.disease_cause, DNA, Mitochondrial, Article, Young Adult, Genetics, medicine, Humans, Age of Onset, Child, Gene, Genetics (clinical), Cell Nucleus, Mutation, Electron Transport Complex I, Infant, Newborn, Infant, medicine.disease, Molecular biology, Survival Analysis, Enzyme Activation, Mitochondrial respiratory chain, Phenotype, Child, Preschool

Abstract

Defects of the mitochondrial respiratory chain are associated with a diverse spectrum of clinical phenotypes, and may be caused by mutations in either the nuclear or the mitochondrial genome (mitochondrial DNA (mtDNA)). Isolated complex I deficiency is the most common enzyme defect in mitochondrial disorders, particularly in children in whom family history is often consistent with sporadic or autosomal recessive inheritance, implicating a nuclear genetic cause. In contrast, although a number of recurrent, pathogenic mtDNA mutations have been described, historically, these have been perceived as rare causes of paediatric complex I deficiency. We reviewed the clinical and genetic findings in a large cohort of 109 paediatric patients with isolated complex I deficiency from 101 families. Pathogenic mtDNA mutations were found in 29 of 101 probands (29%), 21 in MTND subunit genes and 8 in mtDNA tRNA genes. Nuclear gene defects were inferred in 38 of 101 (38%) probands based on cell hybrid studies, mtDNA sequencing or mutation analysis (nuclear gene mutations were identified in 22 probands). Leigh or Leigh-like disease was the most common clinical presentation in both mtDNA and nuclear genetic defects. The median age at onset was higher in mtDNA patients (12 months) than in patients with a nuclear gene defect (3 months). However, considerable overlap existed, with onset varying from 0 to >60 months in both groups. Our findings confirm that pathogenic mtDNA mutations are a significant cause of complex I deficiency in children. In the absence of parental consanguinity, we recommend whole mitochondrial genome sequencing as a key approach to elucidate the underlying molecular genetic abnormality.

Published

2011

22. G.P.18

Author

Richard J.N. Allcock, K. Mina, Mark M. Davis, Rachael M. Duff, C. Wise, S. Wagner, D. Trajanoski, Padma Sivadorai, M. Cabrera, Kyle S. Yau, Gianina Ravenscroft, Kristen J. Nowak, Phillipa J. Lamont, Vanessa Atkinson, Rebecca Gooding, and Nigel G. Laing

Subjects

Genetics, Sanger sequencing, Proband, Genetic heterogeneity, Biology, DNA sequencing, symbols.namesake, Exon, Neurology, Pediatrics, Perinatology and Child Health, Gene duplication, symbols, Neurology (clinical), Diagnostic laboratory, Gene, Genetics (clinical)

Abstract

Two problems for molecular diagnosis of neurogenetic disorders are high levels of genetic heterogeneity and involvement of large genes, e.g. titin. These problems result in many patients not being diagnosed by current Sanger-sequencing based diagnostics. To offset these problems we have developed a TargetSeq (Life Technologies) capture panel consisting of 335 disease genes with mutations detectable by next generation sequencing (NGS). The genes were 276 neurogenetic and 59 cardiomyopathy genes, targeted together because of clinical overlap. The 335 panel genes were captured from pools of 16 bar-coded patient DNA samples and sequenced 16 patients at a time using Ion Proton™ (Life Technologies) sequencing. Variant analysis was by either custom Annovar or Cartagenia (Cartagenia, Inc.) based pipelines. Testing the panel identified 88% of the known small-scale mutations in 28 positive controls. Known mutations deliberately chosen in regions not sequenced well by NGS were not detected. Using the FishingCNV package, we identified 90% of CNV controls, including 100% of CMT1A/HNPP duplication/deletion controls. Although one single exon CNV was detected, not all small CNVs were detected. We have screened >300 molecularly undiagnosed probands, identifying mutations in 59 disease genes, many of which were not previously analysed by the diagnostic laboratory due to Sanger sequencing costs. Using the targeted panel is not ethically different to traditional sequential Sanger sequencing diagnostics. The panel needs updating regularly with new disease gene discoveries. We now receive samples from all round Australasia for analysis of the 335-gene panel, which is cheaper than Sanger.

Published

2014

23. G.P.197

Author

J.P. Bouchard, Marie-Pierre Dubé, J. Mathieu, Erin K. O'Ferrall, Marie-Josée Dicaire, N. Al-Bustani, Nigel G. Laing, V. Bolduc, Bernard Brais, Talita C. Conte, B. Beland, Sylvie Provost, Phillipa J. Lamont, Martine Tétreault, R.T. Hepple, G. Ravenscroft, and Myriam Srour

Subjects

Genetics, RYR1, Weakness, CLCN1, biology, Skeletal muscle, Myostatin, Muscle hypertrophy, medicine.anatomical_structure, Neurology, Pediatrics, Perinatology and Child Health, medicine, biology.protein, Myocyte, Neurology (clinical), medicine.symptom, Genetics (clinical), Muscle cramp

Abstract

Muscle mass and strength are variable traits in humans. Many French Canadians (FC) became international celebrities because of their exceptional strength. Though muscle hypertrophy has been associated in many mammals with myostatin mutations, to date only a single pediatric case has been reported in humans. Dominant pathological mutations in the CLCN1, SCN4A, CAV3, ATP2A1, LPIN1, LMNA and RYR1 gene have been known to lead to muscle hypertrophy in humans, in particular selective muscle hypertrophy in certain myopathies. These conditions are associated with either weakness or increased strength. We recruited a cohort of more than 115 cases belonging to more than 65 families of a heterogeneous dominant condition that we refer to as: “Strongman syndrome” (SM). In all families, the most affected case suffers from incapacitating myalgias with variable degree of muscle cramps, and they also have a personal and familial history of above average strength. On examination these patients have large well defined muscles, above average strength, non-electric prolonged muscle contractions and progressive weakness on repeated contractions. Exome sequencing of a large FC family identified a single segregating variant predicted to be damaging in the DCST2 gene shared also by two other FC families. The DCST2 gene is expressed in skeletal muscle and is predicted to code for a six transmembrane domains channel-like protein. To better characterize the herculean strength we assesses different biometric variables in a subset of cases with and without DCST2 mutations and investigated if myofiber hypertrophy is present. Results of quantifiable methods to evaluate the clinical and pathological phenotype of strongman cases will be presented, as well as functional data about DCST2. The uncovering of the function of DCST2 and other strongman genes will contribute to a better understanding of pathways important for muscle hypertrophy and strength in health and disease.

Published

2014

24. Clinical utility gene card for: Laing distal myopathy

Author

William Wallefeld, Phillipa J. Lamont, Bjarne Udd, Nigel G. Laing, and Mark R. Davis

Subjects

0303 health sciences, LAING DISTAL MYOPATHY, medicine.diagnostic_test, Myosin Heavy Chains, business.industry, Anatomy, Sensitivity and Specificity, Distal Myopathies, 03 medical and health sciences, 0302 clinical medicine, Cardiac Myosins, Myosin, Clinical Utility Gene Card, Genetics, medicine, Humans, Genetic Testing, business, Gene, 030217 neurology & neurosurgery, Genetics (clinical), 030304 developmental biology, Genetic testing

Published

2010

25. Alzheimer's disease with spastic paraparesis and 'cotton wool' plaques: two pedigrees with PS-1 exon 9 deletions

Author

John B.J. Kwok, Peter R. Schofield, A. E. G. Tannenberg, G. Anthony Broe, William S. Brooks, Peter C. Blumbergs, Jillian J. Kril, Phillipa J. Lamont, and Philippa Hedges

Subjects

Adult, Neuropathology, Biology, Exon, Degenerative disease, Alzheimer Disease, medicine, Presenilin-1, Dementia, Humans, Cotton wool plaques, Spasticity, Age of Onset, Genetics, Membrane Proteins, Exons, Middle Aged, medicine.disease, Pedigree, Mutation, Paraparesis, Spastic, Neurology (clinical), Alzheimer's disease, medicine.symptom, Age of onset, Gene Deletion

Abstract

Several pedigrees have recently been reported in which dominantly inherited familial Alzheimer's disease is associated in some family members with spastic paraparesis and non-neuritic 'cotton wool' plaques. Here we report clinical, genetic and neuropathological findings in two further large pedigrees in which this combination of phenotypes is associated with a deletion of exon 9 of the presenilin-1 (PS-1) gene caused by mutations at the splice acceptor site. In both pedigrees, individuals with paraparesis at presentation had a later than average age at onset of symptoms. In addition, one subject with paraparesis had a much less prominent dementia syndrome than his dementia-affected siblings. As PS-1 mutations are almost always associated with a particularly aggressive form of presenile dementia, these findings suggest the existence of a protective or delaying factor in individuals with spastic paraparesis.

Published

2003

26. A locus on chromosome 15q for a dominantly inherited nemaline myopathy with core-like lesions

Author

I.M.P. Gommans, Mark M. Davis, Kathrin Saar, B.G.M. van Engelen, Francis Mastaglia, André Reis, H.J. ter Laak, Hubertus P. H. Kremer, Phillipa J. Lamont, G. Van Duijnhoven, Nigel G. Laing, Martin Lammens, and O.J.M. Vogels

Subjects

Adult, Male, Candidate gene, Adolescent, Genotype, Genetic Linkage, Tropomyosin, Myopathies, Nemaline, TPM2, Congenital neuromuscular disorder, Nebulin, Chromosome 15, Nemaline myopathy, medicine, Humans, Neurosensory disorders [UMCN 3.3], Muscle, Skeletal, Myopathy, RYR1, Genetics, Chromosomes, Human, Pair 15, biology, medicine.disease, Neuromuscular development and genetic disorders [UMCN 3.1], Pedigree, Renal disorders [UMCN 5.4], Phenotype, Haplotypes, Genetic defects of metabolism [UMCN 5.1], biology.protein, Female, Neurology (clinical), Lod Score, medicine.symptom, Microsatellite Repeats

Abstract

Item does not contain fulltext Nemaline myopathy is a congenital neuromuscular disorder characterized by muscle weakness and the presence of nemaline rods. Five genes have now been associated with nemaline myopathy: alpha-tropomyosin-3 (TPM3), alpha-actin (ACTA1), nebulin (NEB), beta-tropomysin (TPM2) and troponin T (TNNT1). In addition, mutations in the ryanodine receptor gene (RYR1) have been associated with core-rod myopathy. Here we report linkage in two unrelated families, with a variant of nemaline myopathy, with associated core-like lesions. The clinical phenotype consists of muscle weakness in addition to a peculiar kind of muscle slowness. A genome-wide scan revealed a locus for nemaline myopathy with core-like lesions on chromosome 15q21-q23 for both families. Combining the two families gave a two-point LOD score of 10.65 for D15S993. The alpha-tropomyosin-1 gene (TPM1) located within this region is the strongest candidate gene. However, no mutations were found in the protein-coding region of TPM1, although small deletions or mutations in an intron cannot be excluded. The critical region contains few other candidate genes coding for muscle proteins and several genes of unknown function, and has not yet been sequenced completely. The novel phenotype of nemaline myopathy in the two presented families corresponds to an also novel, as yet uncharacterized, genotype.

Published

2003

27. D.P.5 Whole exome sequencing applied to Charcot–Marie–Tooth (CMT) disease

Author

Kyle S. Yau, Phillipa J. Lamont, Richard J.N. Allcock, Mark R. Davis, Nigel G. Laing, Nina Kresoje, and Royston Ong

Subjects

Proband, Sanger sequencing, Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Pes cavus, Mutation, business.industry, medicine.disease, Bioinformatics, medicine.disease_cause, Disease gene identification, nervous system diseases, symbols.namesake, Chromosome 16, Neurology, Genetic linkage, Pediatrics, Perinatology and Child Health, symbols, medicine, Neurology (clinical), business, Genetics (clinical), Exome sequencing

Abstract

Charcot–Marie–Tooth disease (CMT) is a common inherited peripheral neuropathy associated with mutations in 54 known genes. CMT is characterized by distal wasting of the legs and later hands. Skeletal deformations are frequent including pes cavus and hammer toes. CMT is subdivided into three subtypes: CMT1 is demyelinating, CMT2 axonal, and intermediate CMT mixed. The clinical and molecular heterogeneity of this disease means many families remain without a molecular diagnosis. This proof of principal study aimed to investigate the use of whole exome sequencing (WES), allied with linkage analysis, to detect known or novel mutations in CMT families in which CMT1A had been excluded. We looked at three families, two dominant and one consanguineous. All other known CMT regions were excluded by linkage analysis in one dominant family; all CMT regions except MPZ, by homozygosity mapping in the consanguineous family. In both these families, WES excluded all known CMT genes including MPZ in the consanguineous family. This suggests the CMT genes in these two families are novel. The second dominant family presented with pes cavus and hammer toes in the first decade followed by difficulty in participation in sports in the second decade. Nerve conduction studies showed a severe sensorimotor axonal peripheral neuropathy. Linkage analysis excluded all known CMT genes except a 65 Mbp region on chromosome 16 including three known CMT genes. One of these, AARS (encoding alanyl-tRNA synthetase), fitted with the autosomal dominant inheritance in the family. WES of the proband identified a heterozygous variant, c.G986A (p.R329H) in AARS, which is a known pathogenic mutation. The variant was confirmed by Sanger sequencing in the proband and all other affected family members available, indicating the mutation is the cause of the disease in the family. Our study highlights the potential of WES in diagnostics and that more CMT genes remain to be found.

Published

2012

28. Identification and sizing of the GAA trinucleotide repeat expansion of Friedreich's ataxia in 56 patients. Clinical and genetic correlates

Author

Phillipa J. Lamont, Nicholas W. Wood, and Mary B. Davis

Subjects

Adult, congenital, hereditary, and neonatal diseases and abnormalities, Heterozygote, Ataxia, Adolescent, Chromosome 9, Locus (genetics), Biology, Polymerase Chain Reaction, Central nervous system disease, medicine, Humans, Allele, Age of Onset, Child, Alleles, Repetitive Sequences, Nucleic Acid, Genetics, Homozygote, Infant, Middle Aged, medicine.disease, Pedigree, Genes, Friedreich Ataxia, Child, Preschool, Spinocerebellar ataxia, Neurology (clinical), medicine.symptom, Age of onset, Trinucleotide repeat expansion, Chromosomes, Human, Pair 9

Abstract

Fifty-six patients with a clinical diagnosis of Friedreich's ataxia were investigated for the GAA trinucleotide repeat expansion recently found within the gene X25 on chromosome 9. All 56 were found to be homozygous for the expansion, with all but two patients having alleles of differing sizes. The expansion size ranged from 2 to 5 kb, with normal alleles around 1.5 kb. Sizing of the single copy of the expansion in eight sets of parents revealed marked instability in the transmission of the expansion, with both increases and decreases in allele size seen. In Friedreich's ataxia patients there was a significant inverse correlation seen between the average of the two expansions sizes and age of onset of symptoms. The GAA repeat expansion was found in the homozygous state in atypical cases of Friedreich's ataxia, such as older age of onset, preservation of lower limb reflexes and cardiac presentations. In three families the father had onset of spinocerebellar ataxia as an adult, and in two the possibility of partial expression in heterozygote carrier fathers has been raised. More importantly, the history of an ataxic syndrome in a parent does not exclude the diagnosis of Friedreich's ataxia in the offspring, and tests for the expansion should be carried out. The third family with an affected father conforms to previously described 'pseudodominant' inheritance.

Published

1997

29. T.P.28 Pseudo-exon inactivation of the dystrophin gene: Ideal candidates for exon skipping

Author

Steve D. Wilton, Sue Fletcher, R. Gooding, Mark R. Davis, S. Krishnaswamy, L. Barrett, Kevin M. Flanigan, and Phillipa J. Lamont

Subjects

musculoskeletal diseases, Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Splice site mutation, biology, Mature messenger RNA, Duchenne muscular dystrophy, Intron, medicine.disease, Molecular biology, Exon skipping, Exon, Neurology, Pediatrics, Perinatology and Child Health, RNA splicing, medicine, biology.protein, Neurology (clinical), Dystrophin, Genetics (clinical)

Abstract

There are many different types of mutations that can inactivate the dystrophin gene and lead to Duchenne muscular dystrophy (DMD). Genomic deletions of one or more exons deletions account for the most common type of dystrophin gene lesion, and a handful of splice switching antisense oligomers could potentially restore the reading frame of some 40% of all DMD mutations. The removal of one or more exons flanking a frame-shifting genomic deletion could restore the reading frame and allow a Becker MD-like gene transcript be generated from a DMD pre-mRNA. Exon 51 skipping trials are showing great promise as a therapy that may reduce the severity in some DMD patients, but regardless of how efficiently exon skipping can be induced, the resultant dystrophin isoforms will be Becker MD like. There is one type of DMD mutation that could be ideally suited to exon skipping, and although pseudo-exon activation is relatively rare, the application of splice switching to these mutations should result in the generation of a normal, not Becker MD-like, dystrophin gene transcript. A BMD patient was recently diagnosed whose dystrophin defect arose from an as yet uncharacterized mutation in intron 62 that led to the retention of 58 bases of intronic sequence being retained in the mature mRNA. While this pseudo-exon disrupts the reading frame and should have led to DMD, there were low levels of normal dystrophin that reduced disease severity. Antisense oligomers can mask normal exons from the splicing machinery, and we have found that some pseudo-exons are even easier to exclude from the mature mRNA. We describe personalized exon skipping strategies to address two different pseudo-exons, one arising from intron 62 and another from intron 47. In both these cases, normal dystrophin mRNA is induced, and unlike all other splice switching oligomers, compounds targeting these pseudo-exons could be tested in healthy volunteers.

Published

2012

30. C.P.6 Study of a novel autosomal recessive minicore disease

Author

Richard J.N. Allcock, Mark R. Davis, Nina Kresoje, Kyle S. Yau, Victoria A. Fabian, Nigel G. Laing, Padma Sivadorai, and Phillipa J. Lamont

Subjects

Genetics, Arthrogryposis, Pathology, medicine.medical_specialty, Biology, medicine.disease, Congenital myopathy, Hypotonia, Neurology, Pediatrics, Perinatology and Child Health, medicine, Respiratory muscle, Neurology (clinical), Muscular dystrophy, medicine.symptom, Genetics (clinical), Exome sequencing, Minicore myopathy, SGCA

Abstract

Minicore disease is a congenital myopathy of early onset, defined pathologically by the presence of multiple areas of reduced mitochondrial oxidative activity in muscle biopsies. There are currently three types of minicore disease defined; minicore myopathy with external ophthalmoplegia, caused by mutations in the RYR1 gene; minicore disease, severe classic form, caused by mutations in the SEPN1 gene and minicore myopathy, antenatal onset with arthrogryposis, with no associated disease gene. A family with three affected sibs was studied. The parents are unaffected and not known to be related, and the phenotype is consistent. The affected sibs presented at birth with extreme generalised hypotonia. There was marked delay in motor milestones, with walking only achieved after 2 years of age. Neck, trunk and facial weakness was moderate, and there was moderate reduction in respiratory muscle strength. The heart was unaffected and intelligence preserved. Muscle biopsy of the quadriceps showed minicores on oxidative stains. This phenotype was not consistent with the described phenotypes of minicore disease, suggesting that this is a novel minicore disease phenotype. We combined linkage analysis with exome capture and next generation sequencing to attempt to identify the causative mutation in this family. SNP linkage analysis under a recessive model eliminated all known congenital myopathy, minicore disease and muscular dystrophy genes except for TTN, POMT1, SGCA, DMN2, and COL6A1. Subsequently, whole exome sequencing data eliminated all genes in the list except for TTN, in which two heterozygous variants were identified. Further investigation of these variants in the family found that both variants were inherited from the unaffected father, suggesting that these variants are not the cause of the disease in this family. Thus, it is suspected that a novel disease gene is the cause of this family’s disease.

Published

2012

31. P5.10. Myotonia congenita and CLCN1 testing in Australia: Novel mutations, racial variation and founder effects

Author

Ichizo Nishino, Phillipa J. Lamont, Nigel G. Laing, Padma Sivadorai, and Mark R. Davis

Subjects

Genetics, CLCN1, Variation (linguistics), Neurology, Myotonia congenita, Pediatrics, Perinatology and Child Health, biology.protein, medicine, Neurology (clinical), Biology, medicine.disease, Genetics (clinical), Founder effect

Published

2011

32. An expansion in the ZNF9 gene causes PROMM in a previously described family with an incidental CLCN1 mutation

Author

R. Jacob, Phillipa J. Lamont, Francis Mastaglia, and Nigel G. Laing

Subjects

Adult, Male, musculoskeletal diseases, Letter, Adolescent, Muscle Proteins, Locus (genetics), Biology, Gene mutation, Myotonic dystrophy, Cataract, Myotonia, Proximal myotonic myopathy, Exon, Chloride Channels, Chromosome 19, medicine, Humans, Abnormalities, Multiple, Genes, Dominant, Genetics, Brain Diseases, CLCN1, Greece, Syndrome, Middle Aged, medicine.disease, Magnetic Resonance Imaging, Psychiatry and Mental health, Mutation, biology.protein, Female, Surgery, Neurology (clinical)

Abstract

In 1997 Mastaglia et al described a two generation family of Macedonian origin with phenotypic features of PROMM and an incidental CLCN1 mutation.1 Affected individuals had mild myotonia, predominantly proximal muscle weakness, and cataracts, compatible with a diagnosis of proximal myotonic myopathy (PROMM). Molecular genetic studies showed that the proposita did not have the chromosome 19 myotonic dystrophy (DM1) CTG expansion, but did have the R894X mutation in exon 23 of the muscle chloride channel gene (CLCN1). However she had only passed the R894X mutation to one of her two affected offspring. Thus the CLCN1 gene mutation did not segregate with the disease. We can now confirm that a definite genetic cause for PROMM has been identified in this family. In 1998 a locus for a second type of myotonic dystrophy (DM2 or PROMM) was mapped to chromosome 3q21.2 In 2001 it was shown that DM2/PROMM was caused by a …

Published

2004