Your search keyword '"Sean Ennis"' showing total 4 results

1. Intra-familial variability associated with recessive RYR1 mutation diagnosed prenatally by exome sequencing

Author

Jillian P. Casey, Michael Farrell, Karen Flood, Sean Ennis, Sally Ann Lynch, and Emma Doyle

Subjects

0301 basic medicine, Genetics, Mutation, medicine.diagnostic_test, business.industry, Obstetrics and Gynecology, medicine.disease_cause, Compound heterozygosity, Frameshift mutation, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Missense mutation, Medicine, medicine.symptom, business, Myopathy, Exome, 030217 neurology & neurosurgery, Genetics (clinical), Exome sequencing, Genetic testing

Abstract

OBJECTIVE To determine the underlying molecular aetiology in a non-consanguineous Irish family who have had three fetal losses because of a primary myopathy characterised by fetal akinesia, arthrogryposis multiplex, bilateral pulmonary hypoplasia and reduced muscle bulk. METHODS Fetal DNA extracted from amniotic cells was whole genome amplified and subjected to whole exome sequencing. RESULTS Whole exome sequencing identified compound heterozygous variants in RYR1 as the cause of the lethal myopathy in this family. All three fetuses were compound heterozygous for a paternally inherited missense variant (c.2113G > A; p.Gly705Arg) and a novel maternally inherited truncating frameshift deletion (c.8843delC; p.Ser2948Cysfs*58). This family did not have the classic cores and fibre type disproportion typically associated with RYR1 mutation. The RYR1 exome finding was made during the couple's third pregnancy and enabled prenatal genetic testing to be undertaken. CONCLUSION We show that recessive RYR1 mutations can be associated with significant intra-familial variability in clinical presentation which can complicate prediction of clinical outcome. RYR1 mutations can also cause diverse muscle pathologies which thwarts diagnosis. This study demonstrates the impact that exome-based diagnoses can have for families with lethal disorders. © 2016 John Wiley & Sons, Ltd.

Published

2016

2. <scp>NAPB</scp> – a novel <scp>SNARE</scp> ‐associated protein for early‐onset epileptic encephalopathy

Author

Amre Shahwan, Mary D. King, Sean Ennis, Judith Conroy, Sally Ann Lynch, Nicholas M. Allen, and Kathleen M. Gorman

Subjects

0301 basic medicine, Genetics, Epilepsy, Biology, Bioinformatics, medicine.disease, 03 medical and health sciences, 030104 developmental biology, Synaptic vesicle docking, Knockout mouse, medicine, Humans, Exome, Female, Global developmental delay, Age of Onset, Child, SNARE Proteins, SNARE complex, Receptor, Gene, Genetics (clinical), Exome sequencing

Abstract

Next-generation sequencing has accelerated the identification of disease genes in many rare genetic disorders including early-onset epileptic encephalopathies (EOEEs). While many of these disorders are caused by neuronal channelopathies, the role of synaptic and related neuronal proteins are increasingly being described. Here, we report a 6-year-old girl with unexplained EOEE characterized by multifocal seizures and profound global developmental delay. Recessive inheritance was considered due to parental consanguinity and Irish Traveller descent. Exome sequencing was performed. Variant prioritization identified a homozygous nonsense variant in the N-ethylmaleimide-sensitive factor attachment protein, beta (NAPB) gene resulting in a premature stop codon and 46% loss of the protein. NAPB plays a role in soluble N-ethylmaleimide-sensitive fusion attachment protein receptor (SNARE)-complex dissociation and recycling (synaptic vesicle docking). Knockout mouse models of the murine ortholog Napb have been previously reported. These mice develop recurrent post-natal epileptic seizures in the absence of structural brain changes. The identification of a disease-causing variant in NAPB further recognizes the importance of the SNARE complex in the development of epilepsy and suggests that this gene should be considered in patients with unexplained EOEE.

Published

2015

3. A chromosomal 5q31.1 gain involvingPITX1causes Liebenberg syndrome

Author

Clare Brenner, Sally Ann Lynch, Jennifer McDaid, David R. Betts, Deirdre Máire Seoighe, Sean Ennis, Regina Regan, Patricia A. Eadie, and Veselina G. Gadancheva

Subjects

Hand deformity, Genetics, medicine, Liebenberg syndrome, Biology, medicine.disease, Phenotype, Genetics (clinical)

Published

2014

4. Genome-wide SNP association-based localization of a dwarfism gene in Friesian dwarf horses

Author

Preethi Govindarajan, Willem Back, Emmeline W. Hill, Pieter A.J. Brama, Judith Conroy, Sean Ennis, B.J. Ducro, Jingjing Gu, Nick Orr, J.A.M. van Arendonk, David E. MacHugh, and Peter A. J. Leegwater

Subjects

Genetics, Dwarfism, Single-nucleotide polymorphism, Genome-wide association study, General Medicine, Biology, medicine.disease, Genome, SNP genotyping, Horse genome, medicine, SNP, Animal Science and Zoology, Gene

Abstract

Summary The recent completion of the horse genome and commercial availability of an equine SNP genotyping array has facilitated the mapping of disease genes. We report putative localization of the gene responsible for dwarfism, a trait in Friesian horses that is thought to have a recessive mode of inheritance, to a 2- MB region of chromosome 14 using just 10 affected animals and 10 controls. We successfully genotyped 34 429 SNPs that were tested for association with dwarfism using chi-square tests. The most significant SNP in our study, BIEC2-239376 (P2df = 4.54 · 10 )5 , Prec = 7.74 · 10 )6 ), is located close to a gene implicated in human dwarfism. Fine-mapping and resequencing analyses did not aid in further localization of the causative variant, and replication of our findings in independent sample sets will be necessary to confirm these results.

Published

2010