Your search keyword '"Mark R, Davis"' showing total 3 results

1. Two New Families and a Literature Review of ELOVL4-Associated Spinocerebellar Ataxia Type 34

Author

Masahiro Nishide, Kathleen Le Marquand, Mark R. Davis, Gábor M. Halmágyi, Avi Fellner, Ramesh K. Narayanan, Marina L. Kennerson, Stephen W. Reddel, Lisa Worgan, Peter K. Panegyres, and Kishore R. Kumar

Subjects

Neurology, Neurology (clinical)

Abstract

Autosomal dominant variants in ELOVL4 cause spinocerebellar ataxia type 34 (SCA34; ATX-ELOVL4), classically associated with a skin condition known as erythrokeratoderma. Here, we report a large Italian-Maltese-Australian family with spinocerebellar ataxia. Notably, while there were dermatological manifestations (eczema), erythrokeratoderma was not present. Using a next-generation sequencing panel, we identified a previously reported ELOVL4 variant, NM_022726.4: c.698C > T p.(Thr233Met). The variant was initially classified as a variant of uncertain significance; however, through segregation studies, we reclassified the variant as likely pathogenic. We next identified an individual from another family (Algerian-Maltese-Australian) with the same ELOVL4 variant with spinocerebellar ataxia but without dermatological manifestations. We subsequently performed the first dedicated literature review of ELOVL4-associated ataxia to gain further insights into genotype–phenotype relationships. We identified a total of 60 reported cases of SCA34 to date. The majority had gait ataxia (88.3%), limb ataxia (76.7%), dysarthria (63.3%), and nystagmus (58.3%). Of note, skin lesions related to erythrokeratoderma were seen in a minority of cases (33.3%). Other extracerebellar manifestations included pyramidal tract signs, autonomic disturbances, retinitis pigmentosa, and cognitive impairment. For brain MRI data, cerebellar atrophy was seen in all cases (100%), whereas the hot cross bun sign (typically associated with multiple system atrophy type C) was seen in 32.4% of cases. Our family study and literature review highlight the variable phenotypic spectrum of SCA34. Importantly, it shows that erythrokeratoderma is not found in most cases and that, while a dermatological assessment may be helpful in these patients, SCA34 diagnosis should be considered irrespective of dermatological manifestations.

Published

2023

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. Next generation sequencing in a large cohort of patients presenting with neuromuscular disease before or at birth

Author

Royston Ong, Richard J.N. Allcock, Anita Cairns, George McGillivray, Monique M. Ryan, Emily J. Todd, Cathy Kiraly-Borri, David Beeson, Nigel G. Laing, Nigel F. Clarke, Susan Maxwell, Padma Sivadorai, Mark R. Davis, Goknur Haliloglu, Alison Colley, Kyle S. Yau, Ariana Kariminejad, Jennie Slee, Zuhal Akçören, Norma B. Romero, Beril Talim, Gianina Ravenscroft, Caroline Sewry, Mary-Louise Freckmann, Denise Williams, Christopher P. Barnett, and Çocuk Sağlığı ve Hastalıkları

Subjects

Male, Neuromuscular disease, Molecular Sequence Data, Prenatal diagnosis, Biology, DNA sequencing, Cohort Studies, symbols.namesake, Next generation sequencing, Prenatal Diagnosis, medicine, Humans, Genetics(clinical), Pharmacology (medical), Amino Acid Sequence, Child, Nemaline myopathy, Genetics (clinical), Exome sequencing, Arthrogryposis, Medicine(all), Genetics, Sanger sequencing, Congenital myopathy, Genetic heterogeneity, Research, Infant, Newborn, High-Throughput Nucleotide Sequencing, Infant, Neuromuscular Diseases, General Medicine, Fetal hypokinesia, medicine.disease, Pedigree, 3. Good health, Child, Preschool, symbols, Female, medicine.symptom

Abstract

Background Fetal akinesia/hypokinesia, arthrogryposis and severe congenital myopathies are heterogeneous conditions usually presenting before or at birth. Although numerous causative genes have been identified for each of these disease groups, in many cases a specific genetic diagnosis remains elusive. Due to the emergence of next generation sequencing, virtually the entire coding region of an individual’s DNA can now be analysed through “whole” exome sequencing, enabling almost all known and novel disease genes to be investigated for disorders such as these. Methods Genomic DNA samples from 45 patients with fetal akinesia/hypokinesia, arthrogryposis or severe congenital myopathies from 38 unrelated families were subjected to next generation sequencing. Clinical features and diagnoses for each patient were supplied by referring clinicians. Genomic DNA was used for either whole exome sequencing or a custom-designed neuromuscular sub-exomic supercapture array containing 277 genes responsible for various neuromuscular diseases. Candidate disease-causing variants were investigated and confirmed using Sanger sequencing. Some of the cases within this cohort study have been published previously as separate studies. Results A conclusive genetic diagnosis was achieved for 18 of the 38 families. Within this cohort, mutations were found in eight previously known neuromuscular disease genes (CHRND, CHNRG, ECEL1, GBE1, MTM1, MYH3, NEB and RYR1) and four novel neuromuscular disease genes were identified and have been published as separate reports (GPR126, KLHL40, KLHL41 and SPEG). In addition, novel mutations were identified in CHRND, KLHL40, NEB and RYR1. Autosomal dominant, autosomal recessive, X-linked, and de novo modes of inheritance were observed. Conclusions By using next generation sequencing on a cohort of 38 unrelated families with fetal akinesia/hypokinesia, arthrogryposis, or severe congenital myopathy we therefore obtained a genetic diagnosis for 47 % of families. This study highlights the power and capacity of next generation sequencing (i) to determine the aetiology of genetically heterogeneous neuromuscular diseases, (ii) to identify novel disease genes in small pedigrees or isolated cases and (iii) to refine the interplay between genetic diagnosis and clinical evaluation and management. Electronic supplementary material The online version of this article (doi:10.1186/s13023-015-0364-0) contains supplementary material, which is available to authorized users.

Published

2015