Your search keyword '"Devery S"' showing total 69 results

51. A detailed phenotypic assessment of individuals affected by MFRP-related oculopathy

Author

Mukhopadhyay R, Pi, Sergouniotis, Ds, Mackay, Ac, Day, Wright G, Devery S, Bp, Leroy, Anthony Robson, Ge, Holder, Li Z, and Ar, Webster

52. Birt-Hogg-Dube Syndrome: A Two Case Study.

Author

Durell, Sarah, Butler, E., Devery, S., Price, S., and Side, L.

Subjects

INTESTINAL cancer

Abstract

Presents an abstract of the article "Birt-Hogg-Dube Syndrome: A Two Case Study," by Sarah Durell, E. Butler, S. Devery, S. Price, and L. Side.

Published

2005

53. Informing a value care model: lessons from an integrated adult neurogenomics clinic.

Author

McLean A, Tchan M, Devery S, Smyth R, Shrestha R, Kumar KR, Tomlinson S, Tisch S, and Wu KHC

Subjects

Adult, Humans, Retrospective Studies, Exome, Referral and Consultation, Genetic Testing, Ambulatory Care Facilities

Abstract

Background: Advances in genomics provide improved opportunities for diagnosis of complex neurogenetic disorders, yet the optimal approach to translate these benefits to the outpatient clinic is unclear., Aims: We retrospectively reviewed referral indications and outcomes of an integrated multidisciplinary team (MDT) clinic pathway for adults with suspected neurogenetic disorders. The associated cost implications were estimated., Methods: Consecutive patients who attended the neurogenomics clinic from January 2017 to April 2020 were included. The clinic comprised neurologists, clinical geneticists and genetic counsellors, who assessed each patient concurrently., Results: Ninety-nine new patients were referred spanning 45 different clinical diagnoses. Following MDT clinical assessment, 23% (23/99) of referral diagnoses were revised prior to molecular testing. Eighty-one patients (82%) underwent genetic testing, including 43 exome-based panels, 15 whole-genome sequencing, 14 single gene tests, 27 repeat-primed polymerase chain reaction testing and two chromosomal microarrays. Overall, 33/99 patients (33%) received a diagnosis, either a molecular diagnosis (n = 24, of which 22 were diagnostic and two were predictive) or a clinical diagnosis (n = 9). Of the clinical diagnosis cohort, five patients received a diagnosis without molecular testing and four patients whose negative testing (one diagnostic and three predictive) allowed exclusion of genetic differentials and, hence, confirmation of clinical diagnoses. The diagnostic rate following MDT and diagnostic testing was 30% (28/94), excluding the five predictive testing cases. MDT assessment aligned with eventual molecular diagnoses in 96% of cases. The estimated average costs were AU$1386 per patient undergoing MDT assessment and AU$4159 per diagnosis achieved., Conclusions: We present an integrated multidisciplinary neurogenomics clinic pathway providing a diagnostic yield of 33% (30% excluding predictive testing cases), with costing implications. The relatively high diagnostic yield may be attributed to multidisciplinary input integrating accurate phenotyping of complex disorders and interpretation of genomic findings., (© 2023 The Authors. Internal Medicine Journal published by John Wiley & Sons Australia, Ltd on behalf of Royal Australasian College of Physicians.)

Published

2023

54. A novel synonymous KMT2B variant in a patient with dystonia causes aberrant splicing.

Author

Grosz BR, Tisch S, Tchan MC, Fung VSC, Darveniza P, Fellner A, Kurian MA, McLean A, Tomlinson SE, Smyth R, Devery S, Wu KHC, Kennerson ML, and Kumar KR

Subjects

Animals, Child, HeLa Cells, Humans, Mutation, Phenotype, RNA Splice Sites, Rats, Dystonia genetics, Dystonic Disorders genetics, Histone-Lysine N-Methyltransferase genetics

Abstract

Background: Heterozygous KMT2B variants are a common cause of dystonia. A novel synonymous KMT2B variant, c.5073C>T (p.Gly1691=) was identified in an individual with childhood-onset progressive dystonia., Methods: The splicing impact of c.5073C>T was assessed using an in vitro exon-trapping assay. The genomic region of KMT2B exons 23-26 was cloned into the pSpliceExpress plasmid between exon 2 and 3 of the rat Ins2 gene. The c.5073C>T variant was then introduced through site-directed mutagenesis. The KMT2B wild-type and c.5073C>T plasmids were transfected separately into HeLa cells and RNA was extracted 48 hours after transfection. The RNA was reverse transcribed to produce cDNA, which was PCR amplified using primers annealing to the flanking rat Ins2 sequences., Results: Sanger sequencing of the PCR products revealed that c.5073C>T caused a novel splice donor site and therefore a 5-bp deletion of KMT2B exon 23 in mature mRNA, leading to a coding frameshift and premature stop codon (p.Lys1692AsnfsTer7)., Conclusion: To our knowledge, this is the first report of a KMT2B synonymous variant associated with dystonia. Reassessment of synonymous variants may increase diagnostic yield for inherited disorders including monogenic dystonia. This is of clinical importance, given the generally favourable response to deep brain stimulation for KMT2B-related dystonia., (© 2022 The Authors. Molecular Genetics & Genomic Medicine published by Wiley Periodicals LLC.)

Published

2022

55. Investigation of current models of care for genetic heart disease in Australia: A national clinical audit.

Author

Austin R, Quinn MCJ, Afoakwah C, Metke-Jimenez A, Leroux H, Atherton J, Brown JS, Wornham LJ, Macciocca I, de Silva MG, Thompson T, Martin EM, Hilton D, Devery S, Wu KHC, Jackson MR, Correnti G, Overkov A, Elbracht-Leong S, Ingles J, Scuffham P, Semsarian C, and McGaughran J

Subjects

Australia epidemiology, Clinical Audit, Humans, Queensland epidemiology, Heart Diseases diagnosis, Heart Diseases epidemiology, Heart Diseases genetics, Telemedicine

Abstract

Background: This sub-study of the Australian Genomics Cardiovascular Genetic Disorders Flagship sought to conduct the first nation-wide audit in Australia to establish the current practices across cardiac genetics clinics., Method: An audit of records of patients with a suspected genetic heart disease (cardiomyopathy, primary arrhythmia, autosomal dominant congenital heart disease) who had a cardiac genetics consultation between 1st January 2016 and 31 July 2018 and were offered a diagnostic genetic test., Results: This audit included 536 records at multidisciplinary cardiac genetics clinics from 11 public tertiary hospitals across five Australian states. Most genetic consultations occurred in a clinic setting (90%), followed by inpatient (6%) and Telehealth (4%). Queensland had the highest proportion of Telehealth consultations (9% of state total). Sixty-six percent of patients had a clinical diagnosis of a cardiomyopathy, 28% a primary arrhythmia, and 0.7% congenital heart disease. The reason for diagnosis was most commonly as a result of investigations of symptoms (73%). Most patients were referred by a cardiologist (85%), followed by a general practitioner (9%) and most genetic tests were funded by the state Genetic Health Service (73%). Nationally, 29% of genetic tests identified a pathogenic or likely pathogenic gene variant; 32% of cardiomyopathies, 26% of primary arrhythmia syndromes, and 25% of congenital heart disease., Conclusion: We provide important information describing the current models of care for genetic heart diseases throughout Australia. These baseline data will inform the implementation and impact of whole genome sequencing in the Australian healthcare landscape., Competing Interests: Declaration of Competing Interest JI receives research grant support from Myokardia, Inc. No additional conflicts of interest to declare., (Crown Copyright © 2021. Published by Elsevier B.V. All rights reserved.)

Published

2021

56. RFC1 expansions can mimic hereditary sensory neuropathy with cough and Sjögren syndrome.

Author

Kumar KR, Cortese A, Tomlinson SE, Efthymiou S, Ellis M, Zhu D, Stoll M, Dominik N, Tisch S, Tchan M, Wu KHC, Devery S, Spring PJ, Hawke S, Cremer P, Ng K, Reilly MM, Nicholson GA, Houlden H, and Kennerson M

Subjects

Cough, Humans, Cerebellar Ataxia, Hereditary Sensory and Autonomic Neuropathies, Sjogren's Syndrome complications, Sjogren's Syndrome diagnosis, Sjogren's Syndrome genetics, Vestibular Neuronitis

Published

2020

57. Multisystem Progeroid Syndrome With Lipodystrophy, Cardiomyopathy, and Nephropathy Due to an LMNA p.R349W Variant.

Author

Hussain I, Jin RR, Baum HBA, Greenfield JR, Devery S, Xing C, Hegele RA, Carranza-Leon BG, Linton MF, Vuitch F, Wu KHC, Precioso DR, Oshima J, Agarwal AK, and Garg A

Abstract

Background: Pathogenic variants in lamin A/C ( LMNA ) cause a variety of progeroid disorders including Hutchinson-Gilford progeria syndrome, mandibuloacral dysplasia, and atypical progeroid syndrome. Six families with 11 patients harboring a pathogenic heterozygous LMNA c.1045C>T; p.R349W variant have been previously reported to have partial lipodystrophy, cardiomyopathy, and focal segmental glomerulosclerosis (FSGS), suggesting a distinct progeroid syndrome., Methods: We report 6 new patients with a heterozygous LMNA p.R349W variant and review the phenotype of previously reported patients to define their unique characteristics. We also performed functional studies on the skin fibroblasts of a patient to seek the underlying mechanisms of various clinical manifestations., Results: Of the total 17 patients, all 14 adults with the heterozygous LMNA p.R349W variant had peculiar lipodystrophy affecting the face, extremities, palms, and soles with variable gain of subcutaneous truncal fat. All of them had proteinuric nephropathy with FSGS documented in 7 of them. Ten developed cardiomyopathy, and 2 of them died early at ages 33 and 45 years. Other common features included premature graying, alopecia, high-pitched voice, micrognathia, hearing loss, and scoliosis. Metabolic complications, including diabetes mellitus, hypertriglyceridemia, and hepatomegaly, were highly prevalent. This variant did not show any abnormal splicing, and no abnormal nuclear morphology was noted in the affected fibroblasts., Conclusions: The heterozygous LMNA p.R349W variant in affected individuals has several distinct phenotypic features, and these patients should be classified as having multisystem progeroid syndrome (MSPS). MSPS patients should undergo careful assessment at symptom onset and yearly metabolic, renal, and cardiac evaluation because hyperglycemia, hypertriglyceridemia, FSGS, and cardiomyopathy cause major morbidity and mortality., (© Endocrine Society 2020.)

Published

2020

58. KBG syndrome presenting with brachydactyly type E.

Author

Libianto R, Wu KH, Devery S, Eisman JA, and Center JR

Subjects

Facies, Female, Humans, Karyotype, Mutation genetics, Repressor Proteins genetics, Whole Genome Sequencing, Abnormalities, Multiple genetics, Abnormalities, Multiple pathology, Bone Diseases, Developmental genetics, Bone Diseases, Developmental pathology, Brachydactyly genetics, Brachydactyly pathology, Intellectual Disability genetics, Intellectual Disability pathology, Tooth Abnormalities genetics, Tooth Abnormalities pathology

Abstract

We report the case of a young woman who presented at age 10 years with height on the tenth centile, brachydactyly type E and mild developmental delay. Biochemistry and hormonal profiles were normal. Differential diagnoses considered included Albright hereditary osteodystrophy without hormone resistance (a.k.a pseudopseudohypoparathyroidism), 2q37 microdeletion syndrome and acrodysostosis. She had a normal karyotype and normal FISH of 2q37. Whole genome sequencing (WGS) identified a mutation in the ANKRD11 gene associated with KBG syndrome. We review the clinical features of the genetic syndromes considered, and suggest KBG syndrome be considered in patients presenting with syndromic brachydactyly type E, especially if short stature and developmental delay are also present., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

59. Factors associated with uterine endometrial hyperplasia and pyometra in wild canids: implications for fertility.

Author

Asa CS, Bauman KL, Devery S, Zordan M, Camilo GR, Boutelle S, and Moresco A

Subjects

Animals, Breeding, Contraception veterinary, Contraceptive Agents pharmacology, Endometrial Hyperplasia prevention & control, Female, Fertility drug effects, Male, Pyometra prevention & control, Retrospective Studies, Animals, Zoo physiology, Canidae physiology, Endometrial Hyperplasia veterinary, Fertility physiology, Pyometra veterinary

Abstract

The ability to safely and effectively manage reproduction is central to the success of AZA captive-breeding programs. Although the AZA Wildlife Contraception Center routinely monitors contraceptive safety, there have been no studies that compare the effects of contraceptive use to separation of males from females, the other option for preventing reproduction. We used retrospective medical records and pathology reports submitted by AZA and related facilities for the seven AZA-managed canid species to assess rates of uterine pathology relative to female reproductive life histories. Our results showed that the prevalence of both pyometra and endometrial hyperplasia (EH) was associated not only with treatment with the two most common contraceptives (Suprelorin® and MGA implants) but also with the number of years barren (i.e., not producing a litter and not contracepted). Rates of pyometra and EH were especially high in African painted dogs and red wolves, but lowest in swift and fennec foxes. The number of years producing a litter had a low association, suggesting it could be protective against uterine pathology. A more recently developed Suprelorin® protocol using Ovaban® to prevent the initial stimulation phase, followed by implant removal when reversal is desired, may be a safer contraceptive option. These results concerning the relationship between reproductive management and uterine health have important implications for AZA-managed programs, since the unsustainability of many captive populations may be due at least in part to infertility. Managing a female's reproductive lifespan to optimize or maintain fertility will require a reconsideration of how breeding recommendations are formulated., (© 2013 Wiley Periodicals, Inc.)

Published

2014

60. Understanding the impact of genetic testing for inherited retinal dystrophy.

Author

Combs R, McAllister M, Payne K, Lowndes J, Devery S, Webster AR, Downes SM, Moore AT, Ramsden S, Black G, and Hall G

Subjects

Female, Health Knowledge, Attitudes, Practice, Humans, Male, Retinal Dystrophies diagnosis, Genetic Predisposition to Disease, Genetic Testing, Inheritance Patterns genetics, Retinal Dystrophies genetics

Abstract

The capability of genetic technologies is expanding rapidly in the field of inherited eye disease. New genetic testing approaches will deliver a step change in the ability to diagnose and extend the possibility of targeted treatments. However, evidence is lacking about the benefits of genetic testing to support service planning. Here, we report qualitative data about retinal dystrophy families' experiences of genetic testing in United Kingdom. The data were part of a wider study examining genetic eye service provision. Twenty interviewees from families in which a causative mutation had been identified by a genetic eye clinic were recruited to the study. Fourteen interviewees had chosen to have a genetic test and five had not; one was uncertain. In-depth telephone interviews were conducted allowing a thorough exploration of interviewees' views and experiences of the benefits of genetic counselling and testing. Transcripts were analysed using thematic analysis. Both affected and unaffected interviewees expressed mainly positive views about genetic testing, highlighting benefits such as diagnostic confirmation, risk information, and better preparation for the future. Negative consequences included the burden of knowledge, moral dilemmas around reproduction, and potential impact on insurance. The offer of genetic testing was often taken up, but was felt unnecessary in some cases. Interviewees in the study reported many benefits, suggesting genetic testing should be available to this patient group. The benefits and risks identified will inform future evaluation of models of service delivery. This research was part of a wider study exploring experiences of families with retinal dystrophy.

Published

2013

61. Understanding the expectations of patients with inherited retinal dystrophies.

Author

Combs R, Hall G, Payne K, Lowndes J, Devery S, Downes SM, Moore AT, Ramsden S, Black GC, and McAllister M

Subjects

Female, Health Services Research, Humans, Male, Ophthalmology organization & administration, Retinal Dystrophies genetics, Retinal Dystrophies therapy, Surveys and Questionnaires, Genetic Services statistics & numerical data, Genetic Testing, Patient Preference psychology, Patient Satisfaction, Quality of Health Care, Retinal Dystrophies diagnosis

Abstract

Background: UK genetic ophthalmology services for patients with retinal dystrophy (RD) are variable. Little research exists to define service requirements, or expectations, of patients and their families. This study aimed to explore the views and perceived benefits of genetic ophthalmology services among members of families with RD., Methods: Twenty participants with known RD mutations were recruited through UK genetic ophthalmic clinics. Semistructured qualitative interviews explored interviewees' perceptions of the role of these services. Interviews were transcribed verbatim and analysed using inductive thematic analysis., Results: Interviewees' expectations and requirements of genetic ophthalmology services were wide-ranging and often perceived to be unmet. Participant expectations were classified in three groups: (1) Medical expectations included obtaining a diagnosis and information about disease/prognosis, genetic risks and research (2) Psychosocial expectations related to participants' need for support in adjusting to RD (3) Practical expectations included the desire for information about welfare and support., Conclusions: Expectations of RD families for clinical services are complex, encompassing a range of healthcare specialties. Services that align to these expectations will need to reach beyond the diagnostic arena and provide practical and psychosocial support. The identification of measurable outcomes will facilitate future development and evaluation of service delivery models. Many of the expectations identified here map to an existing, previously validated, outcomes framework for clinical genetic services. However, an additional outcome domain, labelled 'Independence' was also identified; this could either be specific to vision loss or relate generally to disability caused by genetic conditions.

Published

2013

62. A phenotypic study of congenital stationary night blindness (CSNB) associated with mutations in the GRM6 gene.

Author

Sergouniotis PI, Robson AG, Li Z, Devery S, Holder GE, Moore AT, and Webster AR

Subjects

Adolescent, Adult, Aged, Child, Dark Adaptation, Electroretinography, Exons genetics, Eye Diseases, Hereditary, Female, Genetic Diseases, X-Linked, Humans, Introns genetics, Male, Middle Aged, Myopia physiopathology, Night Blindness physiopathology, Phenotype, Photic Stimulation, Retinal Bipolar Cells physiology, Vision, Ocular, Visual Acuity physiology, Mutation, Myopia genetics, Night Blindness genetics, Receptors, Metabotropic Glutamate genetics

Abstract

Purpose: To describe the clinical phenotype and the molecular pathology in a group of patients with congenital stationary night blindness due to mutations in GRM6, a gene encoding the ON bipolar metabotropic glutamate receptor 6 (mGluR6)., Methods: Nine patients from seven families (age range, 7-75; median, 10 years) with a clinical diagnosis of autosomal recessive complete congenital stationary night blindness were ascertained. Clinical examination, imaging and electrophysiological assessment were performed. The coding region and intron-exon boundaries of GRM6 were sequenced., Results: The median visual acuity for the cohort was 0.2 logMAR (range 0-3). Most patients had myopic astigmatism with the median spherical equivalent being -5.375 dioptres (-0.125 to -18.75). Fundoscopy was within normal limits in 15 eyes; there was severe myopic maculopathy in three eyes. Other secondary complications included face turn because of nystagmus and strabismic amblyopia. All patients had electronegative dark-adapted bright white flash electroretinograms (ERGs) consistent with dysfunction occurring postphototransduction. In the two oldest subjects (aged 75 and 58 years), there was additional photoreceptor dysfunction in keeping with myopic degeneration. ON-OFF ERGs showed generalized cone ON bipolar system dysfunction in all five patients tested. Pattern ERG P50 was normal (Ν = 1), subnormal (N = 2) or undetectable (N = 2). Nine mutations in GRM6 were detected in all seven families; six of these changes were novel., Conclusions: The phenotype associated with GRM6 mutation is variable in terms of presentation, refractive error, visual acuity and macular function. ERGs are electronegative and suggest ON-pathway dysfunction., (© 2011 The Authors. Acta Ophthalmologica © 2011 Acta Ophthalmologica Scandinavica Foundation.)

Published

2012

63. Unilateral vitelliform maculopathy: a comprehensive phenotype study with molecular screening of BEST1 and PRPH2.

Author

Subash M, Rotsos T, Wright GA, Devery S, Holder GE, Robson AG, Pal B, Tufail A, Webster AR, Moore AT, and Michaelides M

Subjects

Adult, Aged, Bestrophins, DNA Mutational Analysis, Electrooculography, Electroretinography, Female, Fluorescein Angiography, Humans, Male, Middle Aged, Mutation genetics, Peripherins, Phenotype, Polymerase Chain Reaction, Retrospective Studies, Tomography, Optical Coherence, Visual Acuity physiology, Vitelliform Macular Dystrophy diagnosis, Vitelliform Macular Dystrophy physiopathology, Chloride Channels genetics, Eye Proteins genetics, Intermediate Filament Proteins genetics, Membrane Glycoproteins genetics, Nerve Tissue Proteins genetics, Vitelliform Macular Dystrophy genetics

Abstract

Aim: To describe the clinical features of a case series of patients with unilateral vitelliform maculopathy and the results of screening BEST1 and PRPH2 for disease-causing mutations., Design/methods: This was a retrospective case series study of six patients ascertained over a 2-year period. Ophthalmological examination, fundus photography, autofluorescence imaging, optical coherence tomography and detailed electrophysiological assessment were undertaken. Blood samples were taken for DNA extraction and mutation screening of BEST1 and PRPH2 was performed., Results: Six patients (3 men and 3 women) with unilateral vitelliform maculopathy were identified, ranging in age from 30 to 68 years. Vision in the affected eye ranged from 20/10 to 20/100. There was no clinical, retinal imaging or electrophysiological evidence of fellow eye involvement. Direct sequencing of BEST1 and PRPH2 did not reveal any disease-causing variants., Conclusions: A case series of patients is reported with an unusual unilateral vitelliform phenotype, often associated with good visual function. The patients do not have the typical characteristics associated with age-related maculopathy or any inherited macular disorders, such as Best vitelliform macular dystrophy. Molecular screening of the candidate genes BEST1 and PRPH2 revealed no mutations.

Published

2012

64. Mutations in KIF11 cause autosomal-dominant microcephaly variably associated with congenital lymphedema and chorioretinopathy.

Author

Ostergaard P, Simpson MA, Mendola A, Vasudevan P, Connell FC, van Impel A, Moore AT, Loeys BL, Ghalamkarpour A, Onoufriadis A, Martinez-Corral I, Devery S, Leroy JG, van Laer L, Singer A, Bialer MG, McEntagart M, Quarrell O, Brice G, Trembath RC, Schulte-Merker S, Makinen T, Vikkula M, Mortimer PS, Mansour S, and Jeffery S

Subjects

Abnormalities, Multiple genetics, Cohort Studies, Exome, Facies, Female, Heterozygote, Humans, Lymphedema genetics, Male, Pedigree, Phenotype, Retinal Dysplasia genetics, Cholestasis genetics, Congenital Abnormalities genetics, Kinesins genetics, Lymphedema congenital, Microcephaly genetics, Mutation

Abstract

We have identified KIF11 mutations in individuals with syndromic autosomal-dominant microcephaly associated with lymphedema and/or chorioretinopathy. Initial whole-exome sequencing revealed heterozygous KIF11 mutations in three individuals with a combination of microcephaly and lymphedema from a microcephaly-lymphedema-chorioretinal-dysplasia cohort. Subsequent Sanger sequencing of KIF11 in a further 15 unrelated microcephalic probands with lymphedema and/or chorioretinopathy identified additional heterozygous mutations in 12 of them. KIF11 encodes EG5, a homotetramer kinesin motor. The variety of mutations we have found (two nonsense, two splice site, four missense, and six indels causing frameshifts) are all predicted to have an impact on protein function. EG5 has previously been shown to play a role in spindle assembly and function, and these findings highlight the critical role of proteins necessary for spindle formation in CNS development. Moreover, identification of KIF11 mutations in patients with chorioretinopathy and lymphedema suggests that EG5 is involved in the development and maintenance of retinal and lymphatic structures., (Copyright © 2012 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2012

65. A novel missense mutation in both OPN1LW and OPN1MW cone opsin genes causes X-linked cone dystrophy (XLCOD5).

Author

Gardner JC, Webb TR, Kanuga N, Robson AG, Holder GE, Stockman A, Ripamonti C, Ebenezer ND, Ogun O, Devery S, Wright GA, Maher ER, Cheetham ME, Moore AT, Michaelides M, and Hardcastle AJ

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Chromosomes, Human, X genetics, Color Vision Defects pathology, Family Health, Humans, Male, Middle Aged, Phenotype, Retinal Cone Photoreceptor Cells pathology, Retinal Dystrophies pathology, Young Adult, Color Vision Defects genetics, Mutation, Missense genetics, Retinal Dystrophies genetics, Rod Opsins genetics

Published

2012

66. X-linked cone dystrophy caused by mutation of the red and green cone opsins.

Author

Gardner JC, Webb TR, Kanuga N, Robson AG, Holder GE, Stockman A, Ripamonti C, Ebenezer ND, Ogun O, Devery S, Wright GA, Maher ER, Cheetham ME, Moore AT, Michaelides M, and Hardcastle AJ

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Amino Acid Sequence, Chromosomes, Human, X genetics, Female, Genetic Association Studies, Genetic Linkage, Genetic Loci, Haplotypes, Humans, Lod Score, Male, Middle Aged, Molecular Sequence Data, Mutation, Missense, Pedigree, Protein Structure, Secondary, Retinal Diseases pathology, Retinal Diseases physiopathology, Cone Opsins genetics, Genetic Diseases, X-Linked genetics, Retinal Cone Photoreceptor Cells pathology, Retinal Diseases genetics

Abstract

X-linked cone and cone-rod dystrophies (XLCOD and XLCORD) are a heterogeneous group of progressive disorders that solely or primarily affect cone photoreceptors. Mutations in exon ORF15 of the RPGR gene are the most common underlying cause. In a previous study, we excluded RPGR exon ORF15 in some families with XLCOD. Here, we report genetic mapping of XLCOD to Xq26.1-qter. A significant LOD score was detected with marker DXS8045 (Z(max) = 2.41 [theta = 0.0]). The disease locus encompasses the cone opsin gene array on Xq28. Analysis of the array revealed a missense mutation (c. 529T>C [p. W177R]) in exon 3 of both the long-wavelength-sensitive (LW, red) and medium-wavelength-sensitive (MW, green) cone opsin genes that segregated with disease. Both exon 3 sequences were identical and were derived from the MW gene as a result of gene conversion. The amino acid W177 is highly conserved in visual and nonvisual opsins across species. We show that W177R in MW opsin and the equivalent W161R mutation in rod opsin result in protein misfolding and retention in the endoplasmic reticulum. We also demonstrate that W177R misfolding, unlike the P23H mutation in rod opsin that causes retinitis pigmentosa, is not rescued by treatment with the pharmacological chaperone 9-cis-retinal. Mutations in the LW/MW cone opsin gene array can, therefore, lead to a spectrum of disease, ranging from color blindness to progressive cone dystrophy (XLCOD5)., (Copyright 2010 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2010

67. A detailed phenotypic assessment of individuals affected by MFRP-related oculopathy.

Author

Mukhopadhyay R, Sergouniotis PI, Mackay DS, Day AC, Wright G, Devery S, Leroy BP, Robson AG, Holder GE, Li Z, and Webster AR

Subjects

Adult, Base Sequence, Electrophysiological Phenomena, Electroretinography, Eye Diseases physiopathology, Female, Fluorescence, Fundus Oculi, Humans, Male, Membrane Proteins chemistry, Middle Aged, Molecular Sequence Data, Mutation genetics, Pedigree, Phenotype, Tomography, Optical Coherence, Eye Diseases genetics, Membrane Proteins genetics

Abstract

Purpose: To determine the spectrum of mutations and phenotypic variability within patients with mutations in membrane-type frizzled related protein gene (MFRP)., Methods: Individuals were initially ascertained based on a phenotype similar to that previously published in association with MFRP mutations. Affected patients underwent a full ophthalmic examination (best-corrected visual acuity, slit-lamp examination, applanation tonometry, and fundoscopy), color fundus photography, optical coherence tomography, autofluorescence imaging, and electrophysiology. MFRP was identified by a genome-wide scan in the fourth-largest autozygous region in one consanguineous family. Sanger sequencing of all the exons and intron-exon boundaries of MFRP was undertaken in the affected individuals., Results: Seven affected individuals from four families were identified as having mutations in MFRP. Patients from two families were homozygous for mutations already previously described (c.1143_1144 insC and c.492 delC), while those from the other two were compound heterozygous for mutations (c.201G>A and c.491_492 insT, and c.492 delC, and c.1622_1625 delTCTG), three of which were novel. There was considerable phenotypic variability within and among families. Autofluorescence imaging revealed the central macula to be relatively well preserved. Foveal cysts and optic nerve head drusen were present in two of the four families. Electrophysiology results showed rod-cone dystrophy with mild to moderate reduction in macular function in all affected members., Conclusions: We report three novel MFRP mutations and expand the phenotypic data available on patients with MFRP mutations.

Published

2010

68. Recessive mutations of the gene TRPM1 abrogate ON bipolar cell function and cause complete congenital stationary night blindness in humans.

Author

Li Z, Sergouniotis PI, Michaelides M, Mackay DS, Wright GA, Devery S, Moore AT, Holder GE, Robson AG, and Webster AR

Subjects

Amino Acid Sequence, Base Sequence, Case-Control Studies, Chromosome Mapping, Chromosomes, Human, Pair 15, Cohort Studies, Consanguinity, Electroretinography, Female, Heterozygote, Homozygote, Humans, Male, Molecular Sequence Data, Pedigree, Mutation, Night Blindness congenital, Night Blindness genetics, Retinal Rod Photoreceptor Cells physiology, TRPM Cation Channels genetics

Abstract

Complete congenital stationary night blindness (cCSNB) is associated with loss of function of rod and cone ON bipolar cells in the mammalian retina. In humans, mutations in NYX and GRM6 have been shown to cause the condition. Through the analysis of a consanguineous family and screening of nine additional pedigrees, we have identified three families with recessive mutations in the gene TRPM1 encoding transient receptor potential cation channel, subfamily M, member 1, also known as melastatin. A number of other variants of unknown significance were found. All patients had myopia, reduced central vision, nystagmus, and electroretinographic evidence of ON bipolar cell dysfunction. None had abnormalities of skin pigmentation, although other skin conditions were reported. RNA derived from human retina and skin was analyzed and alternate 5' exons were determined. The most 5' exon is likely to harbor an initiation codon, and the protein sequence is highly conserved across vertebrate species. These findings suggest an important role of this specific cation channel for the normal function of ON bipolar cells in the human retina.

Published

2009

69. Familial breast cancer: double heterozygosity for BRCA1 and BRCA2 mutations with differing phenotypes.

Author

Smith M, Fawcett S, Sigalas E, Bell R, Devery S, Andrieska N, and Winship I

Subjects

Adult, Aged, BRCA1 Protein genetics, BRCA2 Protein genetics, Breast Neoplasms diagnosis, Female, Genotype, Humans, Middle Aged, Pedigree, Phenotype, Polymerase Chain Reaction, Population Surveillance, Risk Assessment, Risk Factors, Breast Neoplasms genetics, Founder Effect, Genes, BRCA1, Genes, BRCA2, Heterozygote, Jews genetics, Mutation

Abstract

The co-existence of mutations in the BRCA1 and BRCA2 genes is unusual, and to date almost all cases reported have had at least one of the Ashkenazi founder mutations. We report on a family in whom individuals are double heterozygotes for a mutation in BRCA1 and a novel splice site mutation in BRCA2. The phenotypes are discordant, where one sister has had multiple cancers in the BRCA spectrum, while the other is unaffected at 65 years of age. The utility of testing is discussed, and the completion of diagnostic testing despite the finding of a potentially causal mutation is validated.

Published

2008