Your search keyword '"Kamron N. Khan"' showing total 47 results

1. Panel‐based genetic testing for inherited retinal disease screening 176 genes

Author

Leo H. N. Sheck, Simona D. Esposti, Omar A. Mahroo, Gavin Arno, Nikolas Pontikos, Genevieve Wright, Andrew R. Webster, Kamron N. Khan, and Michel Michaelides

Subjects

Genetics, QH426-470

Abstract

Abstract Background This case series reports the performance of a next‐generation sequencing (NGS) panel of 176 retinal genes (NGS 176) in patients with inherited retinal disease (IRD). Methods Subjects are patients who underwent genetic testing between 1 August 2016 and 1 January 2018 at Moorfields Eye Hospital, London, UK. Panel‐based genetic testing was performed unless a specific gene (e.g., RS1) or small group of genes (e.g., ABCA4, PRPH2) were suspected. If a novel variant was identified, a further comment on their predicted pathogenicity and evolutionary conservation was offered and segregation studies performed. The main outcome measure is the likelihood of obtaining a genetic diagnosis using NGS 176. Results 488 patients were included. A molecular diagnosis was obtained for 59.4% of patients. Younger patients were more likely to receive a molecular diagnosis; with 92% of children under the age of 6 years receiving a conclusive result. There was a change in their initially assigned inheritance pattern in 8.4% of patients following genetic testing. Selected IRD diagnoses (e.g., achromatopsia, congenital stationary night blindness) were associated with high diagnostic yields. Conclusion This study confirms that NGS 176 is a useful first‐tier genetic test for most IRD patients. Age and initial clinical diagnosis were strongly associated with diagnostic yield.

Published

2021

2. Outcome of Cataract Surgery in Patients With Retinitis Pigmentosa

Author

Xuan-Thanh-An Nguyen, Alberta A.H.J. Thiadens, Marta Fiocco, Weijen Tan, Martin McKibbin, Caroline C.W. Klaver, Magda A. Meester-Smoor, Caroline Van Cauwenbergh, Ine Strubbe, Andrea Vergaro, Jan-Willem R. Pott, Carel B. Hoyng, Bart P. Leroy, Reda Zemaitiene, Kamron N. Khan, Camiel J.F. Boon, Ophthalmology, and ANS - Complex Trait Genetics

Subjects

Ophthalmology, All institutes and research themes of the Radboud University Medical Center, Medicine and Health Sciences, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12]

Abstract

Contains fulltext : 290816.pdf (Publisher’s version ) (Open Access) PURPOSE: To assess the visual outcome of cataract surgery in patients with retinitis pigmentosa (RP). DESIGN: Retrospective, noncomparative clinical study. METHODS: Preoperative, intraoperative, and postoperative data of patients with RP who were undergoing cataract surgery were collected from several expertise centers across Europe. RESULTS: In total, 295 eyes of 226 patients were included in the study. The mean age at surgery of the first eye was 56.1 ± 17.9 years. Following surgery, best-corrected visual acuity (BCVA) improved significantly from 1.03 to 0.81 logMAR (ie, 20/214 to 20/129 Snellen) in the first treated eye (-0.22 logMAR; 95% CI = -0.31 to -0.13; P < .001) and from 0.80 to 0.56 logMAR (ie, 20/126 to 20/73 Snellen) in the second treated eye (-0.24 logMAR; 95% CI = -0.32 to -0.15; P < .001). Marked BCVA improvements (postoperative change in BCVA of ≥0.3 logMAR) were observed in 87 of 226 patients (39%). Greater odds for marked visual improvements were observed in patients with moderate visual impairment or worse. The most common complications were zonular dialysis (n = 15; 5%) and (exacerbation of) cystoid macular edema (n = 14; 5%), respectively. Postoperative posterior capsular opacifications were present in 111 of 295 eyes (38%). CONCLUSION: Significant improvements in BCVA are observed in most patients with RP following cataract surgery. Baseline BCVA is a predictor of visual outcome. Preoperative evaluation should include the assessment of potential zonular insufficiency and the presence of CME, as they are relatively common and may increase the risk of complications. 01 februari 2023

Published

2023

3. Spatial distribution of metabolites in the retina and its relevance to studies of metabolic retinal disorders

Author

Roberto Bonelli, Sasha M. Woods, Sarah Lockwood, Paul N. Bishop, Kamron N. Khan, Melanie Bahlo, Brendan R. E. Ansell, and Marcus Fruttiger

Subjects

Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Biochemistry

Abstract

Introduction The primate retina has evolved regional specialisations for specific visual functions. The macula is specialised towards high acuity vision and is an area that contains an increased density of cone photoreceptors and signal processing neurons. Different regions in the retina display unique susceptibility to pathology, with many retinal diseases primarily affecting the macula. Objectives To better understand the properties of different retinal areas we studied the differential distribution of metabolites across the retina. Methods We conducted an untargeted metabolomics analysis on full-thickness punches from three different regions (macula, temporal peri-macula and periphery) of healthy primate retina. Results Nearly half of all metabolites identified showed differential abundance in at least one comparison between the three regions. Furthermore, mapping metabolomics results from macula-specific eye diseases onto our region-specific metabolite distributions revealed differential abundance defining systemic metabolic dysregulations that were region specific. Conclusions The unique metabolic phenotype of different retinal regions is likely due to the differential distribution of different cell types in these regions reflecting the specific metabolic requirements of each cell type. Our results may help to better understand the pathobiology of retinal diseases with region specificity.

Published

2023

4. Spatial distribution of metabolites in primate retina and its relevance to studies of human metabolic retinal disorders

Author

Roberto Bonelli, Brendan R E Ansell, Sasha M Woods, Sarah Lockwood, Paul N Bishop, Kamron N Khan, Melanie Bahlo, and Marcus Fruttiger

Abstract

The primate retina has evolved regional specialisations for specific visual functions. The macula is specialised towards high acuity vision and is an area that contains an increased density of cone photoreceptors and signal processing neurons. Different regions in the retina display unique susceptibility to pathology, with many retinal diseases primarily affecting the macula. To better understand the properties of different retinal areas we conducted an untargeted metabolomics analysis on full thickness punches from three different regions (macula, temporal peri-macula and periphery) of primate retina. Half of all metabolites identified showed differential abundance in at least one comparison between the three regions. The unique metabolic phenotype of different retinal regions is likely due to the differential distribution of different cell types in these regions reflecting the specific metabolic requirements of each cell type. Furthermore, mapping metabolomics results from macula-specific eye diseases onto the region-specific distributions of healthy primate retina revealed differential abundance defining systemic metabolic dysregulations that were region specific, highlighting how our results may help to better understand the pathobiology of retinal diseases with region specificity.

Published

2022

5. Novel disease-causing variant in RDH12 presenting with autosomal dominant retinitis pigmentosa

Author

Michel Michaelides, Gavin Arno, Manickam Nick Muthiah, Kamron N. Khan, Navjit Singh, Kate Oprych, Anthony G. Robson, Genevieve A. Wright, Angelos Kalitzeos, and Michaelis Georgiou

Subjects

Retina, medicine.medical_specialty, Visual acuity, genetic structures, medicine.diagnostic_test, business.industry, Fundus photography, Penetrance, Sensory Systems, Ophthalmoscopy, Cellular and Molecular Neuroscience, Ophthalmology, medicine.anatomical_structure, Meridian (perimetry, visual field), medicine, medicine.symptom, business, Retinal thinning, Electroretinography

Abstract

AimTo describe the clinical and molecular features of a novel, autosomal dominant RDH12-retinopathy.MethodsRetrospective cross-sectional study. Twelve individuals from a four-generation British pedigree underwent ophthalmic examination, genotyping using next generation sequencing, including whole genome sequencing and multimodal retinal imaging including fundus photography, optical coherence tomography (OCT), autofluorescence imaging and adaptive optics (AO) scanning light ophthalmoscopy were performed. Visual electrophysiology was performed in a subset.ResultsEight family members were confirmed as affected by genotyping heterozygous for RDH12 c.763delG. Visual acuity ranged from −0.1 to 0.2 logMAR. Affected individuals had constricted visual fields. A parafoveal and peripapillary ring of hyper-autofluorescence was seen initially, and with progression the area of perifoveal hypo-autofluorescence increased to involve the parafoveal area. Mild retinal thinning was identified on OCT imaging with reduction in both foveal total retinal and outer nuclear layer thickness. Cone densities along the temporal meridian were reduced in affected individuals compared with normative values at all temporal eccentricities studied. One individual with incomplete penetrance, was identified as clinically affected primarily on the basis of AO imaging. Full-field electroretinography demonstrated a rod-cone pattern of dysfunction and large-field pattern electroretinography identified peripheral macular dysfunction.ConclusionsThis novel heterozygous variant RDH12 c.763delG is associated with a rod-cone dystrophy with variable expression. Determination of the degree of penetrance may depend on the modality employed to phenotypically characterise an individual. This rare and specific heterozygous (dominant) variant is predicted to result in a gain of function, that causes disease in a gene typically associated with biallelic (recessive) variants.

Published

2021

6. Autosomal Recessive Bestrophinopathy

Author

Nikolas Pontikos, Kamron N. Khan, Genevieve A. Wright, Michalis Georgiou, Monica Armengol, Giuseppe Casalino, Michel Michaelides, Parampal S. Grewal, Andrew R. Webster, and Anthony G. Robson

Subjects

Male, Visual acuity, ADB, autosomal dominant Best disease, genetic structures, DA, dark-adapted, ARB, autosomal recessive bestrophinopathy, Visual Acuity, SRF, subretinal fluid, Compound heterozygosity, chemistry.chemical_compound, 0302 clinical medicine, BEST1, Medicine, Bestrophins, Child, 0303 health sciences, Clinical Trials as Topic, logMAR, logarithm of the minimum angle of resolution, Optical Imaging, Retinal imaging, Eye Diseases, Hereditary, IRF, intraretinal fluid, Middle Aged, Autosomal recessive bestrophinopathy, Natural history, Electrophysiology, Phenotype, Child, Preschool, Female, medicine.symptom, Tomography, Optical Coherence, Adult, medicine.medical_specialty, RPE, retinal pigment epithelium, Adolescent, Genes, Recessive, Article, LA, light-adapted, FCE, focal choroidal excavation, 03 medical and health sciences, Gene therapy, Retinal Diseases, Ophthalmology, Genetics, VA, visual acuity, Humans, Allele, Molecular Biology, CNV, choroidal neovascularization, 030304 developmental biology, Retrospective Studies, FAF, fundus autofluorescence, CRT, central retinal thickness, NIR, near-infrared reflectance, business.industry, Genetic heterogeneity, Retinal, eye diseases, Clinical trial, chemistry, 030221 ophthalmology & optometry, sense organs, business, Cone-Rod Dystrophies

Abstract

Purpose To investigate the clinical course, genetic findings, and phenotypic spectrum of autosomal recessive bestrophinopathy (ARB) in a large cohort of children and adults. Design Retrospective case series. Participants Patients with a detailed clinical phenotype consistent with ARB, biallelic likely disease-causing sequence variants in the BEST1 gene, or both identified at a single tertiary referral center. Methods Review of case notes, retinal imaging (color fundus photography, fundus autofluorescence, OCT), electrophysiologic assessment, and molecular genetic testing. Main Outcome Measures Visual acuity (VA), retinal imaging, and electrophysiologic changes over time. Results Fifty-six eyes of 28 unrelated patients were included. Compound heterozygous variants were detected in most patients (19/27), with 6 alleles recurring in apparently unrelated individuals, the most common of which was c.422G→A, p.(Arg141His; n = 4 patients). Mean presenting VA was 0.52 ± 0.36 logarithm of the minimum angle of resolution (logMAR), and final VA was 0.81 ± 0.75 logMAR (P = 0.06). The mean rate of change in VA was 0.05 ± 0.13 logMAR/year. A significant change in VA was detected in patients with a follow-up of 5 years or more (n = 18) compared with patients with a follow-up of 5 years or less (n = 10; P = 0.001). Presence of subretinal fluid and vitelliform material were early findings in most patients, and this did not change substantially over time. A reduction in central retinal thickness was detected in most eyes (80.4%) over the course of follow-up. Many patients (10/26) showed evidence of generalized rod and cone system dysfunction. These patients were older (P < 0.001) and had worse VA (P = 0.02) than those with normal full-field electroretinography results. Conclusions Although patients with ARB are presumed to have no functioning bestrophin channels, significant phenotypic heterogeneity is evident. The clinical course is characterized by a progressive loss of vision with a slow rate of decline, providing a wide therapeutic window for anticipated future treatment strategies.

Published

2021

7. DYNC2H1 hypomorphic or retina-predominant variants cause nonsyndromic retinal degeneration

Author

Anjali Vig, James A. Poulter, Daniele Ottaviani, Erika Tavares, Katerina Toropova, Anna Maria Tracewska, Antonio Mollica, Jasmine Kang, Oshini Kehelwathugoda, Tara Paton, Jason T. Maynes, Gabrielle Wheway, Gavin Arno, J.C. Ambrose, P. Arumugam, E.L. Baple, M. Bleda, F. Boardman-Pretty, J.M. Boissiere, C.R. Boustred, H. Brittain, M.J. Caulfield, G.C. Chan, C.E.H. Craig, L.C. Daugherty, A. de Burca, A. Devereau, G. Elgar, R.E. Foulger, T. Fowler, P. Furió-Tarí, J.M. Hackett, D. Halai, A. Hamblin, S. Henderson, J.E. Holman, T.J.P. Hubbard, K. Ibáñez, R. Jackson, L.J. Jones, D. Kasperaviciute, M. Kayikci, L. Lahnstein, K. Lawson, S.E.A. Leigh, I.U.S. Leong, F.J. Lopez, F. Maleady-Crowe, J. Mason, E.M. McDonagh, L. Moutsianas, M. Mueller, N. Murugaesu, A.C. Need, C.A. Odhams, C. Patch, D. Perez-Gil, D. Polychronopoulos, J. Pullinger, T. Rahim, A. Rendon, P. Riesgo-Ferreiro, T. Rogers, M. Ryten, K. Savage, K. Sawant, R.H. Scott, A. Siddiq, A. Sieghart, D. Smedley, K.R. Smith, A. Sosinsky, W. Spooner, H.E. Stevens, A. Stuckey, R. Sultana, E.R.A. Thomas, S.R. Thompson, C. Tregidgo, A. Tucci, E. Walsh, S.A. Watters, M.J. Welland, E. Williams, K. Witkowska, S.M. Wood, M. Zarowiecki, Kamron N. Khan, Martin McKibbin, Carmel Toomes, Manir Ali, Matteo Di Scipio, Shuning Li, Jamie Ellingford, Graeme Black, Andrew Webster, Małgorzata Rydzanicz, Piotr Stawiński, Rafał Płoski, Ajoy Vincent, Michael E. Cheetham, Chris F. Inglehearn, Anthony Roberts, and Elise Heon

Subjects

0301 basic medicine, Proband, Retinal degeneration, intraflagellar transport (IFT), Cytoplasmic Dyneins, Ellis-Van Creveld Syndrome, 030105 genetics & heredity, Biology, Article, Retina, 03 medical and health sciences, Exon, chemistry.chemical_compound, primary cilia, medicine, Organoid, Missense mutation, Humans, Induced pluripotent stem cell, Genetics (clinical), Exome sequencing, Retinal Degeneration, Retinal, Exons, DYNC2H1, medicine.disease, Molecular biology, retinitis pigmentosa (RP), Pedigree, inherited retinal disease (IRD), 030104 developmental biology, chemistry, Mutation

Abstract

Purpose Determining the role of DYNC2H1 variants in nonsyndromic inherited retinal disease (IRD). Methods Genome and exome sequencing were performed for five unrelated cases of IRD with no identified variant. In vitro assays were developed to validate the variants identified (fibroblast assay, induced pluripotent stem cell [iPSC] derived retinal organoids, and a dynein motility assay). Results Four novel DYNC2H1 variants (V1, g.103327020_103327021dup; V2, g.103055779A>T; V3, g.103112272C>G; V4, g.103070104A>C) and one previously reported variant (V5, g.103339363T>G) were identified. In proband 1 (V1/V2), V1 was predicted to introduce a premature termination codon (PTC), whereas V2 disrupted the exon 41 splice donor site causing incomplete skipping of exon 41. V1 and V2 impaired dynein-2 motility in vitro and perturbed IFT88 distribution within cilia. V3, homozygous in probands 2–4, is predicted to cause a PTC in a retina-predominant transcript. Analysis of retinal organoids showed that this new transcript expression increased with organoid differentiation. V4, a novel missense variant, was in trans with V5, previously associated with Jeune asphyxiating thoracic dystrophy (JATD). Conclusion The DYNC2H1 variants discussed herein were either hypomorphic or affecting a retina-predominant transcript and caused nonsyndromic IRD. Dynein variants, specifically DYNC2H1 variants are reported as a cause of non syndromic IRD.

Published

2020

8. Systemic lipid dysregulation is a risk factor for macular neurodegenerative disease

Author

Martin Friedlander, Robyn H. Guymer, Kamron N. Khan, Roberto Bonelli, Sasha Woods, Jennifer K Trombley, Tjebo F. C. Heeren, Brendan R E Ansell, Catherine A Egan, Melanie Bahlo, and Marcus Fruttiger

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Carbamoyl-Phosphate Synthase (Ammonia), Glycine, lcsh:Medicine, Disease, Biology, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Metabolomics, Internal medicine, Diabetes mellitus, medicine, Metabolome, Serine, Humans, lcsh:Science, Phosphoglycerate Dehydrogenase, Aged, Multidisciplinary, Phosphatidylethanolamines, lcsh:R, Case-control study, Genetic Variation, Lipid metabolism, Retinal, Diagnostic markers, Middle Aged, medicine.disease, Retinal diseases, Phosphoric Monoester Hydrolases, Sphingomyelins, Data processing, 030104 developmental biology, Endocrinology, chemistry, Risk factors, Diabetes Mellitus, Type 2, Case-Control Studies, 030221 ophthalmology & optometry, Female, lcsh:Q, Sphingomyelin, Metabolic Networks and Pathways

Abstract

Macular Telangiectasia type 2 (MacTel) is an uncommon bilateral retinal disease, in which glial cell and photoreceptor degeneration leads to central vision loss. The causative disease mechanism is largely unknown, and no treatment is currently available. A previous study found variants in genes associated with glycine–serine metabolism (PSPH, PHGDH and CPS1) to be associated with MacTel, and showed low levels of glycine and serine in the serum of MacTel patients. Recently, a causative role of deoxysphingolipids in MacTel disease has been established. However, little is known about possible other metabolic dysregulation. Here we used a global metabolomics platform in a case–control study to comprehensively profile serum from 60 MacTel patients and 58 controls. Analysis of the data, using innovative computational approaches, revealed a detailed, disease-associated metabolic profile with broad changes in multiple metabolic pathways. This included alterations in the levels of several metabolites that are directly or indirectly linked to glycine–serine metabolism, further validating our previous genetic findings. We also found changes unrelated to PSPH, PHGDH and CPS1 activity. Most pronounced, levels of several lipid groups were altered, with increased phosphatidylethanolamines being the most affected lipid group. Assessing correlations between different metabolites across our samples revealed putative functional connections. Correlations between phosphatidylethanolamines and sphingomyelin, and glycine–serine and sphingomyelin, observed in controls, were reduced in MacTel patients, suggesting metabolic re-wiring of sphingomyelin metabolism in MacTel patients. Our findings provide novel insights into metabolic changes associated with MacTel and implicate altered lipid metabolism as a contributor to this retinal neurodegenerative disease.

Published

2020

9. Panel‐based genetic testing for inherited retinal disease screening 176 genes

Author

Omar A. Mahroo, Kamron N. Khan, Michel Michaelides, Leo Sheck, Gavin Arno, Nikolas Pontikos, Simona Degli Esposti, Andrew R. Webster, and Genevieve A. Wright

Subjects

Male, 0301 basic medicine, Pediatrics, Achromatopsia, ABCA4, Disease, 030105 genetics & heredity, QH426-470, Disease Screening, Odds Ratio, Mass Screening, Medical diagnosis, Child, Genetics (clinical), Aged, 80 and over, Congenital stationary night blindness, medicine.diagnostic_test, biology, High-Throughput Nucleotide Sequencing, Middle Aged, Phenotype, Child, Preschool, Female, Original Article, Adult, medicine.medical_specialty, Adolescent, Diagnosis, Differential, Young Adult, 03 medical and health sciences, Retinal Diseases, medicine, Genetics, Humans, Genetic Predisposition to Disease, Genetic Testing, Molecular Biology, Gene, Genetic Association Studies, Aged, Retrospective Studies, Genetic testing, business.industry, Genetic Diseases, Inborn, Infant, Newborn, Infant, Original Articles, medicine.disease, United Kingdom, 030104 developmental biology, biology.protein, business, Biomarkers

Abstract

Background This case series reports the performance of a next‐generation sequencing (NGS) panel of 176 retinal genes (NGS 176) in patients with inherited retinal disease (IRD). Methods Subjects are patients who underwent genetic testing between 1 August 2016 and 1 January 2018 at Moorfields Eye Hospital, London, UK. Panel‐based genetic testing was performed unless a specific gene (e.g., RS1) or small group of genes (e.g., ABCA4, PRPH2) were suspected. If a novel variant was identified, a further comment on their predicted pathogenicity and evolutionary conservation was offered and segregation studies performed. The main outcome measure is the likelihood of obtaining a genetic diagnosis using NGS 176. Results 488 patients were included. A molecular diagnosis was obtained for 59.4% of patients. Younger patients were more likely to receive a molecular diagnosis; with 92% of children under the age of 6 years receiving a conclusive result. There was a change in their initially assigned inheritance pattern in 8.4% of patients following genetic testing. Selected IRD diagnoses (e.g., achromatopsia, congenital stationary night blindness) were associated with high diagnostic yields. Conclusion This study confirms that NGS 176 is a useful first‐tier genetic test for most IRD patients. Age and initial clinical diagnosis were strongly associated with diagnostic yield., A retrospective study of 488 patients with inherited retinal dystrophy confirms that NGS 176 is a useful first tier genetic test, achieving a molecular diagnosis in 59.4% of those tested. Age and initial clinical diagnosis were strongly associated with diagnostic yield.

Published

2021

10. Phenotype and genotype of 197 British patients with McArdle disease: An observational single-centre study

Author

Maria Patasin, Rosaline Quinlivan, Chiara Pizzamiglio, Kamron N Khan, and Omar A. Mahroo

Subjects

Adult, Male, medicine.medical_specialty, Genotype, Exercise intolerance, Rhabdomyolysis, Papillary thyroid cancer, Ptosis, Internal medicine, Retinal Dystrophies, Genetics, medicine, Humans, Muscle, Skeletal, Genetics (clinical), Retrospective Studies, Muscle Weakness, business.industry, Thyroid disease, Muscle weakness, Retrospective cohort study, Middle Aged, medicine.disease, Thyroid Diseases, United Kingdom, Phenotype, Mutation, Glycogen Phosphorylase, Muscle Form, Glycogen Storage Disease Type V, Female, medicine.symptom, business, Acute rhabdomyolysis, Glycogen

Abstract

McArdle disease is caused by recessive mutations in PYGM gene. The condition is considered to cause a "pure" muscle phenotype with symptoms including exercise intolerance, inability to perform isometric activities, contracture, and acute rhabdomyolysis leading to acute renal failure. This is a retrospective observational study aiming to describe phenotypic and genotypic features of a large cohort of patients with McArdle disease between 2011 and 2019. Data relating to genotype and phenotype, including frequency of rhabdomyolysis, fixed muscle weakness, gout and comorbidities, inclusive of retinal disease (pattern retinal dystrophy) and thyroid disease, were collected. Data from 197 patients are presented. Seven previously unpublished PYGM mutations are described. Exercise intolerance (100%) and episodic rhabdomyolysis (75.6%) were the most common symptoms. Fixed muscle weakness was present in 82 (41.6%) subjects. Unexpectedly, ptosis was observed in 28 patients (14.2%). Hyperuricaemia was a common finding present in 88 subjects (44.7%), complicated by gout in 25% of cases. Thyroid dysfunction was described in 30 subjects (15.2%), and in 3 cases, papillary thyroid cancer was observed. Pattern retinal dystrophy was detected in 15 out of the 41 subjects that underwent an ophthalmic assessment (36.6%). In addition to fixed muscle weakness, ptosis was a relatively common finding. Surprisingly, dysfunction of thyroid and retinal abnormalities were relatively frequent comorbidities. Further studies are needed to better clarify this association, although our finding may have important implication for patient management.

Published

2021

11. Macular dystrophies: clinical and imaging features, molecular genetics and therapeutic options

Author

Najiha Rahman, Kamron N. Khan, Michalis Georgiou, and Michel Michaelides

Subjects

0301 basic medicine, retina, pattern dystrophy, TIMP3, RS1, XLRS, ABCA4, Review, Disease, Bioinformatics, Macular Degeneration, 0302 clinical medicine, BEST1, Medicine, Medical diagnosis, macular dystrophy, biology, medicine.diagnostic_test, Macular dystrophy, gene therapy, Sensory Systems, Stargardt disease, X-linked retinoschisis, Diagnostic Imaging, Therapeutics, Drusen, 03 medical and health sciences, Cellular and Molecular Neuroscience, stem cells, Humans, Molecular Biology, Genetic testing, EFEMP1, business.industry, medicine.disease, Clinical trial, Ophthalmology, 030104 developmental biology, autosomal dominant drusen, PRPH2, Best disease, 030221 ophthalmology & optometry, biology.protein, Sorsby fundus dystrophy, ADD, business, pharmacological therapy, STGD

Abstract

Macular dystrophies (MDs) consist of a heterogeneous group of disorders that are characterised by bilateral symmetrical central visual loss. Advances in genetic testing over the last decade have led to improved knowledge of the underlying molecular basis. The developments in high-resolution multimodal retinal imaging have also transformed our ability to make accurate and more timely diagnoses and more sensitive quantitative assessment of disease progression, and allowed the design of optimised clinical trial endpoints for novel therapeutic interventions. The aim of this review was to provide an update on MDs, including Stargardt disease, Best disease, X-linked r etinoschisis, pattern dystrophy, Sorsby fundus dystrophy and autosomal dominant drusen. It highlights the range of innovations in retinal imaging, genotype–phenotype and structure–function associations, animal models of disease and the multiple treatment strategies that are currently in clinical trial or planned in the near future, which are anticipated to lead to significant changes in the management of patients with MDs.

Published

2019

12. Loss-of-Function Mutations in the CFH Gene Affecting Alternatively Encoded Factor H-like 1 Protein Cause Dominant Early-Onset Macular Drusen

Author

Rachel L. Taylor, James A. Poulter, Susan M. Downes, Martin McKibbin, Kamron N. Khan, Chris F. Inglehearn, Andrew R. Webster, Alison J. Hardcastle, Michel Michaelides, Paul N. Bishop, Simon J. Clark, Graeme C. Black, Graeme Black, Georgina Hall, Stuart Ingram, Rachel Taylor, Forbes Manson, Panagiotis Sergouniotis, Andrew Webster, Alison Hardcastle, Vincent Plagnol, Nikolas Pontikos, Michael Cheetham, Gavin Arno, Alessia Fiorentino, Chris Inglehearn, Carmel Toomes, Manir Ali, Claire Smith, Kamron Khan, Susan Downes, Jing Yu, Stephanie Halford, Suzanne Broadgate, and Veronica van Heyningen

Subjects

Male, Muscle Proteins, Retinal Drusen, Drusen, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Exome sequencing, Aged, Retrospective Studies, 030304 developmental biology, Genetics, 0303 health sciences, Mutation, biology, business.industry, Intracellular Signaling Peptides and Proteins, Genetic Variation, LIM Domain Proteins, Middle Aged, Macular degeneration, medicine.disease, eye diseases, 3. Good health, Complement system, Ophthalmology, Complement Factor H, Factor H, 030221 ophthalmology & optometry, biology.protein, Female, sense organs, Haploinsufficiency, business, Complement control protein

Abstract

Purpose To characterize the molecular mechanism underpinning early-onset macular drusen (EOMD), a phenotypically severe subtype of age-related macular degeneration (AMD), in a subgroup of patients. Design Multicenter case series, in vitro experimentation, and retrospective analysis of previously reported variants. Participants Seven families with apparently autosomal dominant EOMD. Methods Patients underwent a comprehensive ophthalmic assessment. Affected individuals from families A, B, and E underwent whole exome sequencing. The probands from families C, D, F, and G underwent Sanger sequencing analysis of the complement factor H (CFH) gene. Mutant recombinant factor H like-1 (FHL-1) proteins were expressed in HEK293 cells to assess the impact on FHL-1 expression and function. Previously reported EOMD-causing variants in CFH were reviewed. Main Outcome Measures Detailed clinical phenotypes, genomic findings, in vitro characterization of mutation effect on protein function, and postulation of the pathomechanism underpinning EOMD. Results All affected participants demonstrated bilateral drusen. The earliest reported age of onset was 16 years (median, 46 years). Ultra-rare (minor allele frequency [MAF], ≤0.0001) CFH variants were identified as the cause of disease in each family: CFH c.1243del, p.(Ala415ProfsTer39) het; c.350+1G→T het; c.619+1G→A het, c.380G→A, p.(Arg127His) het; c.694C→T p.(Arg232Ter) het (identified in 2 unrelated families in this cohort); and c.1291T→A, p.(Cys431Ser). All mutations affect complement control protein domains 2 through 7, and thus are predicted to impact both FHL-1, the predominant isoform in Bruch’s membrane (BrM) of the macula, and factor H (FH). In vitro analysis of recombinant proteins FHL-1R127H, FHL-1A415f/s, and FHL-1C431S demonstrated that they are not secreted, and thus are loss-of-function proteins. Review of 29 previously reported EOMD-causing mutations found that 75.8% (22/29) impact FHL-1 and FH. In total, 86.2% (25/29) of EOMD-associated variants cause haploinsufficiency of FH or FHL-1. Conclusions Early-onset macular drusen is an underrecognized, phenotypically severe subtype of AMD. We propose that haploinsufficiency of FHL-1, the main regulator of the complement pathway in BrM, where drusen develop, is an important mechanism underpinning the development of EOMD in a number of cases. Understanding the molecular basis of EOMD will shed light on AMD pathogenesis given their pathologic similarities.

Published

2019

13. New variants and in silico analyses in GRK1 associated Oguchi disease

Author

James A. Poulter, Elfride De Baere, Kaoru Fujinami, Andrew R. Webster, Atta Ur Rehman, Gavin Arno, Abdur Rehman, Rachel L. Taylor, Sarah A. Harris, Graeme C.M. Black, James Bellingham, Julie De Zaeytijd, Martin McKibbin, Chris F. Inglehearn, Molly S. C. Gravett, Kamron N. Khan, Muhammad Ansar, Takaaki Hayashi, Robert H. Henderson, Manir Ali, Nigel P. Davies, Dan Donnelly, Mineo Kondo, Omar A. Mahroo, Carmel Toomes, Bart P. Leroy, Carlo Rivolta, and UK Inherited Retinal Disease Consortium, Genomics England Research Consortium

Subjects

MECHANISM, G-Protein-Coupled Receptor Kinase 1, In silico, PROTEIN, GRK1, PHOTOTRANSDUCTION, Disease, Biology, Genome, ACTIVATION, 03 medical and health sciences, Night Blindness, Medicine and Health Sciences, Genetics, medicine, Missense mutation, Humans, Genetics(clinical), CSNB, MUTATION, Exome, Genetics (clinical), Exome sequencing, Research Articles, 030304 developmental biology, 0303 health sciences, DELETION, Oguchi disease, 030305 genetics & heredity, Eye Diseases, Hereditary, DEFECTS, Eye Diseases, Hereditary/genetics, G-Protein-Coupled Receptor Kinase 1/genetics, Night Blindness/genetics, rhodopsin, medicine.disease, genomic DNA, RHODOPSIN KINASE GENE, FORM, PATHOGENICITY, Research Article

Abstract

Biallelic mutations in G‐Protein coupled receptor kinase 1 (GRK1) cause Oguchi disease, a rare subtype of congenital stationary night blindness (CSNB). The purpose of this study was to identify disease causing GRK1 variants and use in‐depth bioinformatic analyses to evaluate how their impact on protein structure could lead to pathogenicity. Patients’ genomic DNA was sequenced by whole genome, whole exome or focused exome sequencing. Disease associated variants, published and novel, were compared to nondisease associated missense variants. The impact of GRK1 missense variants at the protein level were then predicted using a series of computational tools. We identified twelve previously unpublished cases with biallelic disease associated GRK1 variants, including eight novel variants, and reviewed all GRK1 disease associated variants. Further structure‐based scoring revealed a hotspot for missense variants in the kinase domain. In addition, to aid future clinical interpretation, we identified the bioinformatics tools best able to differentiate disease associated from nondisease associated variants. We identified GRK1 variants in Oguchi disease patients and investigated how disease‐causing variants may impede protein function in‐silico., In this study, Poulter et al. expand the number of mutations in Rhodopsin Kinase (GRK1), associated with Oguchi disease, from 13 to 21. The authors compare disease associated mutations with likely nonpathogenic variants in a range of bioinformatic prediction software. In silico analyses of the mutations, using a homology model, suggest mutations result in one of three potential mechanisms of disease: loss of protein, loss of kinase function or a failure of prenylation leading to mislocalisation of the protein.

Published

2020

14. New pathogenic variants and insights into pathogenic mechanisms in GRK1-related Oguchi disease

Author

Chris F. Inglehearn, Nigel P. Davies, Gavin Arno, Robert H. Henderson, Kamron N. Khan, Rachel L. Taylor, Omar A. Mahroo, James Bellingham, Manir Ali, James A. Poulter, Molly S. C. Gravett, Elfride De Baere, Dan Donnelly, Atta Ur Rehman, Abdur Rehman, Carlo Rivolta, Kaoru Fujinami, Graeme C.M. Black, Julie De Zaeytijd, Mineo Kondo, Sarah A. Harris, Martin McKibbin, Andrew R. Webster, Takaaki Hayashi, Muhammad Ansar, Bart P. Leroy, and Carmel Toomes

Subjects

Genetics, 0303 health sciences, Oguchi disease, Biology, medicine.disease, Genome, 3. Good health, 03 medical and health sciences, genomic DNA, 0302 clinical medicine, 030221 ophthalmology & optometry, medicine, Missense mutation, Leiden Open Variation Database, Exome, Gene, Exome sequencing, 030304 developmental biology

Abstract

PurposeBiallelic mutations in G-Protein coupled receptor kinase 1 (GRK1) cause Oguchi disease, a rare subtype of congenital stationary night blindness (CSNB). The purpose of this study was to identify pathogenic GRK1 variants and use in-depth bioinformatic analyses to evaluate how their impact on protein structure could lead to pathogenicity.MethodsPatients’ genomic DNA was sequenced by whole genome, whole exome or focused exome sequencing. Pathogenic variants, published and novel, were compared to nondisease associated missense variants. The impact of GRK1 missense variants at the protein level were then predicted using a series of computational tools.ResultsWe identified eleven previously unpublished cases with biallelic pathogenic GRK1 variants, including seven novel variants, and reviewed all GRK1 pathogenic variants. Further structure-based scoring revealed a hotspot for missense variants in the kinase domain. Additionally, to aid future clinical interpretation, we identified the bioinformatics tools best able to differentiate pathogenic from non-pathogenic variants.ConclusionWe identified new GRK1 pathogenic variants in Oguchi disease patients and investigated how disease-causing variants may impede protein function, giving new insights into the mechanisms of pathogenicity. All pathogenic GRK1 variants described to date have been collated into a Leiden Open Variation Database (http://dna2.leeds.ac.uk/GRK1_LOVD/genes/GRK1).

Published

2020

15. Clinical Course of Autosomal Recessive Bestrophinopathy Complicated by Choroidal Neovascularization

Author

Ugo Introini, Giuseppe Casalino, Francesco Bandello, Chiara M. Eandi, Kamron N. Khan, Michel Michaelides, Camilla Alovisi, Introini, Ugo, Casalino, Giuseppe, Khan, Kamron N., Eandi, Chiara, Alovisi, Camilla, Michaelides, Michel, and Bandello, Francesco

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, genetic structures, Fundus Oculi, Visual Acuity, 03 medical and health sciences, 0302 clinical medicine, Retinal Diseases, Ophthalmology, Electroretinography, medicine, Humans, Bestrophins, Fluorescein Angiography, Child, Retina, Choroid, business.industry, Clinical course, Eye Diseases, Hereditary, DNA, Optical coherence tomography angiography, Response to treatment, Choroidal Neovascularization, eye diseases, 030104 developmental biology, medicine.anatomical_structure, Choroidal neovascularization, 030221 ophthalmology & optometry, Female, sense organs, Subretinal fibrosis, medicine.symptom, business, Tomography, Optical Coherence, Autosomal recessive bestrophinopathy

Abstract

The authors report the clinical course of two cases of autosomal recessive bestrophinopathy (ARB) complicated by choroidal neovascularization (CNV). One patient presenting with a novel BEST1 mutation (c.658 C>T, p.Gln220*) underwent anti-vascular endothelial growth factor therapy. Response to treatment was documented on optical coherence tomography angiography (OCTA). Despite initial response to treatment, recurrent CNV exudation with progressive subretinal fibrosis was observed. In the second patient, the CNV was not treated and spontaneous regression was observed. This report indicates that the clinical course of CNV in ARB may vary considerably, ranging from spontaneous regression to progressive subretinal fibrosis despite intervention. [ Ophthalmic Surg Lasers Imaging Retina. 2018;49:888–892.]

Published

2018

16. Quantifying the Separation Between the Retinal Pigment Epithelium and Bruch's Membrane using Optical Coherence Tomography in Patients with Inherited Macular Degeneration

Author

Michel Michaelides, Shyamanga Borooah, Martin McKibbin, Kamron N. Khan, Anthony T. Moore, William R. Freeman, Andrew R. Webster, Amit Meshi, Angelos Kalitzeos, Sasan Moghimi, Leonardo Lando, Omar A. Mahroo, Kunny Dans, and Georgios Agorogiannis

Subjects

0301 basic medicine, Retinal degeneration, medicine.medical_specialty, genetic structures, inherited macular degeneration, Biomedical Engineering, Retinal Pigment Epithelium, Drusen, Asymptomatic, Bruch's membrane, Nyctalopia, Article, 03 medical and health sciences, Macular Degeneration, 0302 clinical medicine, Optical coherence tomography, Ophthalmology, Medicine, Humans, retinal dystrophy, Retrospective Studies, Retinal pigment epithelium, optical coherence tomography, medicine.diagnostic_test, business.industry, Reproducibility of Results, Macular degeneration, medicine.disease, eye diseases, 030104 developmental biology, medicine.anatomical_structure, 030221 ophthalmology & optometry, sense organs, Bruch Membrane, medicine.symptom, business, Tomography, Optical Coherence

Abstract

Author(s): Khan, Kamron N; Borooah, Shyamanga; Lando, Leonardo; Dans, Kunny; Mahroo, Omar A; Meshi, Amit; Kalitzeos, Angelos; Agorogiannis, Georgios; Moghimi, Sasan; Freeman, William R; Webster, Andrew R; Moore, Anthony T; McKibbin, Martin; Michaelides, Michel | Abstract: PurposeTo describe and quantify Bruch's membrane (BM) and retinal pigment epithelium (RPE) separation using spectral-domain (SD) optical coherence tomography (OCT) in patients affected by inherited macular degenerations associated with BM thickening.MethodsPatients with molecularly confirmed Sorsby fundus dystrophy (SFD), dominant drusen (DD), and late-onset retinal degeneration (L-ORD) were included in this retrospective study. Each disease was classed as early stage if subjects were asymptomatic, intermediate stage if they had nyctalopia alone, and late stage if they described loss of central vision. The main outcome was measurement of BM-RPE separation on SD-OCT. The BM-RPE separation measurements were compared against those in normal age-matched controls.ResultsSeventeen patients with SFD, 22 with DD, and eight with L-ORD were included. BM-RPE separation on SD-OCT demonstrated a high test-retest and interobserver reproducibility (intraclass correlation coefficients g0.9). BM-RPE separation was not identified in normal subjects. In SFD, there was greater BM-RPE separation in late-stage disease compared with intermediate-stage patients both at subfoveal (P l 0.05) and juxtafoveal (P l 0.01) locations. In DD, there was increased BM-RPE separation in late-stage disease compared with early stage at subfoveal (P l 0.001) and juxtafoveal (P l 0.05) topographies. There was no significant difference in BM-RPE separation between disease stages in L-ORD.ConclusionsBM-RPE separation is a novel, quantifiable phenotype in the three monogenic macular dystrophies studied, and may be an optical correlate of the histopathological thickening in BM that is known to occur. BM-RPE separation, as measured by OCT, varies with stage of disease in SFD and DD, but not in L-ORD.Translational relevanceSFD, DD, and L-ORD are associated with BM thickening. In this group of patients, OCT assessment of macular structure identifies a separation of the usually single, hyperreflective line thought to represent BM and the overlying RPE. This separation is a novel and quantifiable feature of disease staging in SFD and DD.

Published

2019

17. THE FUNDUS PHENOTYPE ASSOCIATED WITH THE p.Ala243Val BEST1 MUTATION

Author

Michel Michaelides, Kamron N. Khan, Anthony T. Moore, and Farrah Islam

Subjects

Adult, Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Genotype, Fundus Oculi, Vitelliform macular dystrophy, Fundus (eye), 03 medical and health sciences, 0302 clinical medicine, Interquartile range, Electroretinography, Humans, Medicine, Bestrophins, Family history, Aged, Retrospective Studies, Genetic testing, medicine.diagnostic_test, business.industry, General Medicine, Middle Aged, medicine.disease, Vitelliform Macular Dystrophy, Ophthalmology, Phenotype, 030104 developmental biology, Mutation, Mutation (genetic algorithm), 030221 ophthalmology & optometry, Maculopathy, Female, business

Abstract

To describe a highly recognizable and reproducible retinal phenotype associated with a specific BEST1 mutation-p.Ala243Val.Retrospective review of consecutive cases where genetic testing has identified p.Ala243Val BEST1 as the cause of disease. Electronic patient records were used to extract demographic, as well as functional and anatomical data. These data were compared with those observed with the most common BEST1 genotype, p.Arg218Cys.Eight individuals (six families) were identified with the p.Ala243Val BEST1 mutation and seven patients with the pathologic variant p.Arg218Cys. No patients with mutation of codon 243 knowingly had a family history of retinal disease, whereas all patients with the p.Arg218Cys variant did. The maculopathy was bilateral in all cases. The p.Ala243Val mutation was associated with a pattern dystrophy-type appearance, most visible with near-infrared reflectance and fundus autofluorescence imaging. This phenotype was never observed with any other genotype. This mutation was associated with an older median age of symptom onset (median = 42, interquartile range = 22) compared with those harboring the p.Arg218Cys mutation (median = 18, interquartile range = 12; Mann-Whitney U test; P0.05). Despite their older age, the final recorded acuity seemed to be better in the p.Ala243Val group (median = 0.55, interquartile range = 0.6475; median = 0.33, interquartile range = 0.358), although this did not reach statistical significance (Mann-Whitney U test; P0.05).The mutation p.Ala243Val is associated with highly recognizable and reproducible pattern dystrophy-like phenotype. Patients develop symptoms at a later age and tend to have better preservation of electrooculogram amplitudes.

Published

2018

18. NORMAL ELECTROOCULOGRAPHY IN BEST DISEASE AND AUTOSOMAL RECESSIVE BESTROPHINOPATHY

Author

Kamron N. Khan, Michel Michaelides, Graham E. Holder, Anthony G. Robson, Andrew R. Webster, Farrah Islam, and Anthony T. Moore

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Eye Movements, genetic structures, DNA Mutational Analysis, Dark Adaptation, Fundus (eye), Young Adult, 03 medical and health sciences, 0302 clinical medicine, Retinal Diseases, Reference Values, Ophthalmology, Genotype, Electroretinography, Humans, Medicine, Macula Lutea, Bestrophins, Best disease, medicine.diagnostic_test, business.industry, Arden ratio, Eye Diseases, Hereditary, DNA, General Medicine, Electrooculography, eye diseases, Phenotype, 030104 developmental biology, Intracellular calcium homeostasis, Mutation, 030221 ophthalmology & optometry, Female, sense organs, business, Autosomal recessive bestrophinopathy

Abstract

Purpose To evaluate the electrooculogram (EOG) in a large series of patients with Best disease and autosomal recessive bestrophinopathy. Methods A retrospective review of consecutive cases at Moorfields Eye Hospital, London, United Kingdom. Patients with Best disease or autosomal recessive bestrophinopathy who, after electrophysiologic testing, had a normal or atypical EOG light rise were identified. Main outcome measure was EOG amplitude, clinical phenotype and genotype. Results One hundred thirteen patients were identified with likely disease-causing sequence variants in BEST1 (99 Best disease and 14 autosomal recessive bestrophinopathy). Electrooculograms had been performed in 75 patients. Twenty patients (27%) had no detectable light rise (Arden ratio of 100%) and 49 (65%) had Arden ratios of between 100% to 165%. Six patients (8%) were found to have an EOG light rise of >165%. No cases demonstrated significant interocular asymmetry in EOG amplitude. Conclusion The current work provides significant clinical evidence that the EOG phenotype in Best disease and autosomal recessive bestrophinopathy is more variable than currently appreciated. As a normal EOG may occur in the presence of a classical fundus appearance, the consequences of BEST1 mutation may be independently expressed, possibly mediated through differential effects on intracellular calcium homeostasis.

Published

2018

19. CNGB3 mutations cause severe rod dysfunction

Author

Martin McKibbin, Declan J. McKeefry, Kamron N. Khan, James H. Maguire, Susanne Kohl, and Manir Ali

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Achromatopsia, genetic structures, Cyclic Nucleotide-Gated Cation Channels, Rod monochromatism, Color Vision Defects, Dark Adaptation, 030105 genetics & heredity, Consanguinity, Macular Degeneration, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Retinal Rod Photoreceptor Cells, Ophthalmology, Electroretinography, medicine, Humans, Scotopic vision, Genetics (clinical), medicine.diagnostic_test, business.industry, Siblings, Retinal, Full field, medicine.disease, eye diseases, chemistry, Mutation, Pediatrics, Perinatology and Child Health, 030221 ophthalmology & optometry, Clinical electrophysiology, Female, sense organs, business, Erg, Photic Stimulation

Abstract

Congenital achromatopsia or rod monochromatism is a rare autosomal recessive condition defined by a severe loss of cone photoreceptor function in which rods purportedly retain normal or near-to-normal function. This report describes the results of electroretinography in two siblings with CNGB3-associated achromatopsia.Full field light- and dark-adapted electroretinograms (ERGs) were recorded using standard protocols detailed by the International Society for Clinical Electrophysiology of Vision (ISCEV). We also examined rod-mediated ERGs using series of stimuli that varied over a 6 log unit range of retinal illuminances (-1.9-3.5 log scotopic trolands).Dark-adapted ERGs in achromatopsia patients exhibited severely reduced b-wave amplitudes with abnormal b:a ratios (1.3 and 0.6). In comparison, the reduction in a-wave amplitude was less marked. The rod-mediated ERG took on an electronegative appearance at high-stimulus illuminances.Although the defect that causes achromatopsia is primarily in the cone photoreceptors, our results reveal an accompanying disruption of rod function that is more severe than has previously been reported. The differential effects on the b-wave relative to the a-wave points to an inner-retinal locus for the disruption of rod function in these patients.

Published

2017

20. FUNCTIONAL AND ANATOMICAL OUTCOMES OF CHOROIDAL NEOVASCULARIZATION COMPLICATING BEST1-RELATED RETINOPATHY

Author

Kamron N. Khan, Andrew R. Webster, Omar A. Mahroo, Michel Michaelides, Anthony T. Moore, and Farrah Islam

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Time Factors, Visual acuity, Adolescent, genetic structures, Fundus Oculi, Visual Acuity, Vitelliform macular dystrophy, Retina, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Ophthalmology, Humans, Medicine, Fluorescein Angiography, Child, Aged, Retrospective Studies, medicine.diagnostic_test, Choroid, business.industry, Retrospective cohort study, General Medicine, Middle Aged, Prognosis, medicine.disease, Fluorescein angiography, Choroidal Neovascularization, eye diseases, Vitelliform Macular Dystrophy, 030104 developmental biology, Choroidal neovascularization, medicine.anatomical_structure, Disease Progression, 030221 ophthalmology & optometry, Female, sense organs, medicine.symptom, business, Tomography, Optical Coherence, Autosomal recessive bestrophinopathy, Follow-Up Studies, Retinopathy

Abstract

To describe the presenting features and functional outcomes in a series of patients with choroidal neovascular membrane complicating BEST1-related retinopathy (Best disease and autosomal recessive bestrophinopathy).Retrospective review of consecutive cases at a tertiary care eye hospital. Patients were identified retrospectively over an 11-year period. Records were reviewed to extract demographic as well as functional and anatomical outcome data.Fourteen eyes of 12 patients were identified (11 Best disease and 1 autosomal recessive bestrophinopathy). Median follow-up was 2.8 years (range 0.8-6). The median age at choroidal neovascular membrane discovery was 15.5 years (range 6-72). Choroidal neovascular membranes were active early in the disease course before vitelliruption. Seven eyes were treated with intravitreal bevacizumab, 7 eyes were monitored by observation alone. On average, patients required a single treatment (median = 1, range 1-10). The median gain in visual acuity was greater in the treated versus the observed group-0.46 versus 0.17 decimalized units of Snellen acuity, respectively (P0.05 Mann-Whitney U test). Although a significant reduction in central macular thickness was evident in both groups, 150 μm (treated) and 104 μm (observed), active treatment was not associated with greater thinning than observation (P0.05 Mann-Whitney U test).There is a high rate of spontaneous recovery of BEST1-related choroidal neovascular membrane, and overall the authors observed a gain in visual acuity associated with a reduction in central macular thickness. Active treatment, here with intravitreal bevacizumab, is associated with better functional outcomes than observation alone.

Published

2017

21. Correction: Biallelic sequence and structural variants in RAX2 are a novel cause for autosomal recessive inherited retinal disease

Author

Stijn Van de Sompele, Claire Smith, Marianthi Karali, Marta Corton, Kristof Van Schil, Frank Peelman, Timothy Cherry, Toon Rosseel, Hannah Verdin, Julien Derolez, Thalia Van Laethem, Kamron N. Khan, Martin McKibbin, Carmel Toomes, Manir Ali, Annalaura Torella, Francesco Testa, Belen Jimenez, Francesca Simonelli, Julie De Zaeytijd, Jenneke Van den Ende, Bart P. Leroy, Frauke Coppieters, Carmen Ayuso, Chris F. Inglehearn, Sandro Banfi, and Elfride De Baere

Subjects

Adult, Male, Genotype, DNA Mutational Analysis, Mutation, Missense, Genes, Recessive, Retina, White People, Article, Retinal Diseases, retinitis pigmentosa, Humans, Eye Proteins, Genetic Association Studies, Genetics (clinical), Homeodomain Proteins, novel ARRP gene, Correction, RAX2, Middle Aged, Pedigree, Phenotype, Haplotypes, loss of function, Mutation, Female, homeobox-containing transcription factor, Transcription Factors

Abstract

Purpose RAX2 encodes a homeobox-containing transcription factor, in which four monoallelic pathogenic variants have been described in autosomal dominant cone-dominated retinal disease. Methods Exome sequencing in a European cohort with inherited retinal disease (IRD) (n = 2086) was combined with protein structure modeling of RAX2 missense variants, bioinformatics analysis of deletion breakpoints, haplotyping of RAX2 variant c.335dup, and clinical assessment of biallelic RAX2-positive cases and carrier family members. Results Biallelic RAX2 sequence and structural variants were found in five unrelated European index cases, displaying nonsyndromic autosomal recessive retinitis pigmentosa (ARRP) with an age of onset ranging from childhood to the mid-40s (average mid-30s). Protein structure modeling points to loss of function of the novel recessive missense variants and to a dominant-negative effect of the reported dominant RAX2 alleles. Structural variants were fine-mapped to disentangle their underlying mechanisms. Haplotyping of c.335dup in two cases suggests a common ancestry. Conclusion This study supports a role for RAX2 as a novel disease gene for recessive IRD, broadening the mutation spectrum from sequence to structural variants and revealing a founder effect. The identification of biallelic RAX2 pathogenic variants in five unrelated families shows that RAX2 loss of function may be a nonnegligible cause of IRD in unsolved ARRP cases.

Published

2019

22. Biallelic sequence and structural variants in RAX2 are a novel cause for autosomal recessive inherited retinal disease

Author

Julien Derolez, Hannah Verdin, Carmen Ayuso, Frauke Coppieters, Marta Corton, Frank Peelman, Marianthi Karali, Francesca Simonelli, Thalia Van Laethem, Kamron N. Khan, Julie De Zaeytijd, Jenneke van den Ende, Belen Jimenez, Sandro Banfi, Manir Ali, Francesco Testa, Elfride De Baere, Claire E. L. Smith, Martin McKibbin, Annalaura Torella, Timothy J. Cherry, Bart P. Leroy, Carmel Toomes, Chris F. Inglehearn, Toon Rosseel, Kristof Van Schil, Stijn Van De Sompele, Van de Sompele, Stijn, Smith, Claire, Karali, Marianthi, Corton, Marta, Van Schil, Kristof, Peelman, Frank, Cherry, Timothy, Rosseel, Toon, Verdin, Hannah, Derolez, Julien, Van Laethem, Thalia, Khan, Kamron N., Mckibbin, Martin, Toomes, Carmel, Ali, Manir, Torella, Annalaura, Testa, Francesco, Jimenez, Belen, Simonelli, Francesca, De Zaeytijd, Julie, Van den Ende, Jenneke, Leroy, Bart P., Coppieters, Frauke, Ayuso, Carmen, Inglehearn, Chris F., Banfi, Sandro, and De Baere, Elfride

Subjects

0301 basic medicine, EXPRESSION, CRX, PROTEIN, Disease, 030105 genetics & heredity, Biology, 03 medical and health sciences, chemistry.chemical_compound, retinitis pigmentosa, Retinitis pigmentosa, medicine, Medicine and Health Sciences, Genetics (clinical), Loss function, Sequence (medicine), HOMEOBOX GENE [novel ARRP gene KeyWords Plus], Genetics, MUTATIONS, novel ARRP gene, Biology and Life Sciences, Retinal, RAX2, medicine.disease, 030104 developmental biology, chemistry, loss of function, homeobox-containing transcription factor, Human medicine, NRL

Abstract

Purpose: RAX2 encodes a homeobox-containing transcription factor, in which four monoallelic pathogenic variants have been described in autosomal dominant cone-dominated retinal disease. Methods: Exome sequencing in a European cohort with inherited retinal disease (IRD) (n = 2086) was combined with protein structure modeling of RAX2 missense variants, bioinformatics analysis of deletion breakpoints, haplotyping of RAX2 variant c.335dup, and clinical assessment of biallelic RAX2-positive cases and carrier family members. Results: Biallelic RAX2 sequence and structural variants were found in five unrelated European index cases, displaying nonsyndromic autosomal recessive retinitis pigmentosa (ARRP) with an age of onset ranging from childhood to the mid-40s (average mid-30s). Protein structure modeling points to loss of function of the novel recessive missense variants and to a dominant-negative effect of the reported dominant RAX2 alleles. Structural variants were fine-mapped to disentangle their underlying mechanisms. Haplotyping of c.335dup in two cases suggests a common ancestry. Conclusion: This study supports a role for RAX2 as a novel disease gene for recessive IRD, broadening the mutation spectrum from sequence to structural variants and revealing a founder effect. The identification of biallelic RAX2 pathogenic variants in five unrelated families shows that RAX2 loss of function may be a nonnegligible cause of IRD in unsolved ARRP cases. Purpose: RAX2 encodes a homeobox-containing transcription factor, in which four monoallelic pathogenic variants have been described in autosomal dominant cone-dominated retinal disease. Methods: Exome sequencing in a European cohort with inherited retinal disease (IRD) (n = 2086) was combined with protein structure modeling of RAX2 missense variants, bioinformatics analysis of deletion breakpoints, haplotyping of RAX2 variant c.335dup, and clinical assessment of biallelic RAX2-positive cases and carrier family members. Results: Biallelic RAX2 sequence and structural variants were found in five unrelated European index cases, displaying nonsyndromic autosomal recessive retinitis pigmentosa (ARRP) with an age of onset ranging from childhood to the mid-40s (average mid-30s). Protein structure modeling points to loss of function of the novel recessive missense variants and to a dominant-negative effect of the reported dominant RAX2 alleles. Structural variants were fine-mapped to disentangle their underlying mechanisms. Haplotyping of c.335dup in two cases suggests a common ancestry. Conclusion: This study supports a role for RAX2 as a novel disease gene for recessive IRD, broadening the mutation spectrum from sequence to structural variants and revealing a founder effect. The identification of biallelic RAX2 pathogenic variants in five unrelated families shows that RAX2 loss of function may be a nonnegligible cause of IRD in unsolved ARRP cases.

Published

2019

23. Clinical and Genetic Features of Choroideremia in Childhood

Author

Kamron N. Khan, Michel Michaelides, Anthony T. Moore, and Farrah Islam

Subjects

0301 basic medicine, medicine.medical_specialty, Visual acuity, Fundus (eye), Choroideremia, Peripapillary chorioretinal atrophy, Ophthalmoscopy, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Ophthalmology, Medicine, Retinal pigment epithelium, medicine.diagnostic_test, business.industry, Retinal, medicine.disease, eye diseases, 030104 developmental biology, medicine.anatomical_structure, chemistry, 030221 ophthalmology & optometry, sense organs, medicine.symptom, business, Retinopathy

Abstract

Purpose To review the functional and anatomic characteristics of choroideremia in the pediatric population, aiming to describe the earliest features of the disease and to identify biomarkers useful for monitoring disease progression. Design Retrospective case series. Participants Children diagnosed with choroideremia at a single institution. Methods Patients were identified using an electronic patient record system. Case notes and retinal imaging (color fundus photography [CFP], spectral-domain [SD] optical coherence tomography [OCT], and fundus autofluorescence [FAF]) then were reviewed. The results of genetic testing also were recorded. Main Outcome Measures Presenting symptoms, visual acuity, fundus changes (CFP, SD OCT, FAF), and CHM sequencing results. Results Twenty-nine patients were identified with a mean age at referral of 9 years (range, 3–16 years). CHM mutations were identified in 15 of 19 patients tested. Nyctalopia was the predominant symptom (66%). Five of 29 patients were asymptomatic at presentation. At the final follow-up visit (mean age, 16 years; range, 7–26 years), most maintained excellent visual acuity (mean, 0.98±0.13 decimalized Snellen acuity). The first sign of retinopathy was widespread pigment clumping at the level of the retinal pigment epithelium (RPE). This later evolved to chorioretinal atrophy, most marked in the mid-peripheral retina. Peripapillary atrophy also was an early feature and was progressive in nature. Three different zones of FAF change were visible. Persistence of the inner retinal layers, detected by SD OCT, was visible at presentation in 15 of 27 patients. Subfoveal choroidal thickness decreased with age, whereas central retinal thickness increased over a similar interval. Four patients in whom visual acuity decreased over the follow-up period recorded a reduction in central retinal thickness. Conclusions Progressive structural changes occur at a time when central visual function is maintained. Pigmentary changes at the level of the RPE occur early in the disease course. Peripapillary chorioretinal atrophy, central retinal thickness, and subfoveal choroidal thickness are likely to be valuable in monitoring disease progression and should be considered as potential biomarkers in future therapeutic trials.

Published

2016

24. Advanced diagnostic genetic testing in inherited retinal disease: experience from a single tertiary referral centre in the UK National Health Service

Author

Genevieve A. Wright, Andrew R. Webster, Michel Michaelides, Kamron N. Khan, A. T. Moore, Naser Ali, and Ravinder K. Chana

Subjects

0301 basic medicine, medicine.medical_specialty, medicine.diagnostic_test, Retinal dystrophy, business.industry, Tertiary referral centre, Physical examination, Retinal, Disease, 030105 genetics & heredity, Bioinformatics, National health service, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Internal medicine, 030221 ophthalmology & optometry, Genetics, medicine, Retinal imaging, business, Genetics (clinical), Genetic testing

Abstract

In 2013, as part of our genetic investigation of patients with inherited retinal disease, we utilized multigene panel testing of 105 genes known to cause retinal disease in our patient cohorts. This test was performed in a UK National Health Service (NHS) accredited laboratory. The results of all multigene panel tests requested between 1.4.13 and 31.8.14 were retrospectively reviewed. All patients had been previously seen at Moorfields Eye Hospital, London, UK and diagnosed with an inherited retinal dystrophy after clinical examination and detailed retinal imaging. The results were categorized into three groups: (i) Testing helped establish a certain molecular diagnosis in 45 out of 115 (39%). Variants in USH2A (n = 6) and RP1 (n = 4) were most common. (ii) Definitive conclusions could not be drawn from molecular testing alone in 13 out of 115 (11%) as either insufficient pathogenic variants were discovered or those identified were not consistent with the phenotype. (iii) Testing did not identify any pathogenic variants responsible for the phenotype in 57 out of 115 (50%). Multigene panel testing performed in an NHS setting has enabled a molecular diagnosis to be confidently made in 40% of cases. Novel variants accounted for 38% of all identified variants. Detailed retinal phenotyping helped the interpretation of specific variants. Additional care needs to be taken when assessing polymorphisms in genes that have been infrequently associated with disease, as historical techniques were not as rigorous as contemporary ones. Future iterations of sequencing are likely to offer higher sensitivity, testing a broader range of genes, more rapidly and at a reduced cost.

Published

2016

25. Early Patterns of Macular Degeneration in ABCA4-Associated Retinopathy

Author

Kamron N, Khan, Melissa, Kasilian, Omar A R, Mahroo, Preena, Tanna, Angelos, Kalitzeos, Anthony G, Robson, Kazushige, Tsunoda, Takeshi, Iwata, Anthony T, Moore, Kaoru, Fujinami, and Michel, Michaelides

Subjects

Male, RPE, retinal pigment epithelium, genetic structures, Adolescent, DA, dark-adapted, Visual Acuity, PERG, pattern electroretinography, ONL, outer nuclear layer, Retina, Article, LA, light-adapted, Macular Degeneration, cd.s.m−2, candela seconds per meter squared, AOSLO, adaptive optics scanning laser ophthalmoscope, Exome Sequencing, Electroretinography, Humans, Stargardt Disease, Macula Lutea, Fluorescein Angiography, BM, Bruch membrane, Child, Retrospective Studies, FAF, fundus autofluorescence, logMAR, logarithm of the minimum angle of resolution, MEH, Moorfields Eye Hospital, ABCA4, ATP binding cassette, subfamily A, member 4, eye diseases, Ophthalmoscopy, Phenotype, ISCEV, International Society for Clinical Electrophysiology of Vision, Child, Preschool, STGD1, Stargardt disease, ATP-Binding Cassette Transporters, Female, sense organs, Atrophy, ELM, external limiting membrane, Tomography, Optical Coherence

Abstract

Purpose To describe the earliest features of ABCA4-associated retinopathy. Design Case series. Participants Children with a clinical and molecular diagnosis of ABCA4-associated retinopathy without evidence of macular atrophy. Methods The retinal phenotype was characterized by color fundus photography, OCT, fundus autofluorescence (FAF) imaging, electroretinography, and in 2 patients, adaptive optics scanning laser ophthalmoscopy (AOSLO). Sequencing of the ABCA4 gene was performed in all patients. Main Outcome Measures Visual acuity, OCT, FAF, electroretinography, and AOSLO results. Results Eight children with ABCA4-associated retinopathy without macular atrophy were identified. Biallelic variants in ABCA4 were identified in all patients. Four children were asymptomatic, and 4 reported loss of VA. Patients were young (median age, 8.5 years; interquartile range, 6.8 years) with good visual acuity (median, 0.155 logarithm of the minimum angle of resolution [logMAR]; interquartile range, 0.29 logMAR). At presentation, the macula appeared normal (n = 3), had a subtly altered foveal reflex (n = 4), or demonstrated manifest fine yellow dots (n = 1). Fundus autofluorescence identified hyperautofluorescent dots in the central macula in 3 patients, 2 of whom showed a normal fundus appearance. Only 1 child had widespread hyperautofluorescent retinal flecks at presentation. OCT imaging identified hyperreflectivity at the base of the outer nuclear layer in all 8 patients. Where loss of outer nuclear volume was evident, this appeared to occur preferentially at a perifoveal locus. Longitudinal split-detector AOSLO imaging in 2 individuals confirmed that the greatest change in cone spacing occurred in the perifoveal, and not foveolar, photoreceptors. Electroretinography showed a reduced B-wave–to–A-wave ratio in 3 of 5 patients tested; in 2 children, recordings clearly showed electronegative results. Conclusions In childhood-onset ABCA4-associated retinopathy, the earliest stages of macular atrophy involve the parafovea and spare the foveola. In some cases, these changes are predated by tiny, foveal, yellow, hyperautofluorescent dots. Hyperreflectivity at the base of the outer nuclear layer, previously described as thickening of the external limiting membrane, is likely to represent a structural change at the level of the foveal cone nuclei. Electroretinography suggests that the initial site of retinal dysfunction may occur after phototransduction.

Published

2017

26. A clinical and molecular characterisation of CRB1-associated maculopathy

Author

Kamron N, Khan, Anthony, Robson, Omar A R, Mahroo, Gavin, Arno, Chris F, Inglehearn, Monica, Armengol, Naushin, Waseem, Graham E, Holder, Keren J, Carss, Lucy F, Raymond, Andrew R, Webster, Anthony T, Moore, Martin, McKibbin, Maria M, van Genderen, James A, Poulter, and Michel, Michaelides

Subjects

Adult, Male, Adolescent, Infant, Newborn, Infant, Membrane Proteins, Nerve Tissue Proteins, Retinal Photoreceptor Cell Outer Segment, Article, Macular Degeneration, Young Adult, Child, Preschool, Electronic Health Records, Humans, Female, Genetic Predisposition to Disease, Genetic Testing, Child, Eye Proteins, Alleles, Genetic Association Studies

Abstract

To date, over 150 disease-associated variants in CRB1 have been described, resulting in a range of retinal disease phenotypes including Leber congenital amaurosis and retinitis pigmentosa. Despite this, no genotype–phenotype correlations are currently recognised. We performed a retrospective review of electronic patient records to identify patients with macular dystrophy due to bi-allelic variants in CRB1. In total, seven unrelated individuals were identified. The median age at presentation was 21 years, with a median acuity of 0.55 decimalised Snellen units (IQR = 0.43). The follow-up period ranged from 0 to 19 years (median = 2.0 years), with a median final decimalised Snellen acuity of 0.65 (IQR = 0.70). Fundoscopy revealed only a subtly altered foveal reflex, which evolved into a bull’s-eye pattern of outer retinal atrophy. Optical coherence tomography identified structural changes—intraretinal cysts in the early stages of disease, and later outer retinal atrophy. Genetic testing revealed that one rare allele (c.498_506del, p.(Ile167_Gly169del)) was present in all patients, with one patient being homozygous for the variant and six being heterozygous. In trans with this, one variant recurred twice (p.(Cys896Ter)), while the four remaining alleles were each observed once (p.(Pro1381Thr), p.(Ser478ProfsTer24), p.(Cys195Phe) and p.(Arg764Cys)). These findings show that the rare CRB1 variant, c.498_506del, is strongly associated with localised retinal dysfunction. The clinical findings are much milder than those observed with bi-allelic, loss-of-function variants in CRB1, suggesting this in-frame deletion acts as a hypomorphic allele. This is the most prevalent disease-causing CRB1 variant identified in the non-Asian population to date.

Published

2017

27. DETAILED RETINAL IMAGING IN CARRIERS OF OCULAR ALBINISM

Author

Emma C. Lord, James A. Poulter, Keren J. Carss, Andrew R. Webster, Kamron N. Khan, Gavin Arno, Farrah Islam, Michel Michaelides, FLucy Raymond, Chris F. Inglehearn, Anthony T. Moore, Manir Ali, and Carmel Toomes

Subjects

0301 basic medicine, Ocular albinism, Adult, medicine.medical_specialty, Heterozygote, genetic structures, Retinal Pigment Epithelium, Fundus (eye), Retina, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Ophthalmology, Medicine, Humans, Macula Lutea, Prospective Studies, Eye Proteins, Hypopigmentation, Retinal pigment epithelium, Membrane Glycoproteins, medicine.diagnostic_test, business.industry, Fundus photography, Retinal, General Medicine, Middle Aged, medicine.disease, Albinism, Ocular, eye diseases, 3. Good health, Autofluorescence, 030104 developmental biology, medicine.anatomical_structure, chemistry, 030221 ophthalmology & optometry, Albinism, Female, sense organs, medicine.symptom, business

Abstract

BACKGROUND: Albinism refers to a group of disorders primarily characterized by hypopigmentation. Affected individuals usually manifest both ocular and cutaneous features of the disease, but occasionally hair and skin pigmentation may appear normal. This is the case in ocular albinism, an X chromosome linked disorder resulting from mutation of GPR143. Female carriers may be recognized by a "mud-splatter" appearance in the peripheral retina. The macula is thought to be normal, however. METHODS: Obligate female carriers of pathogenic GPR143 alleles were recruited. Molecular confirmation of disease was performed only for atypical cases. Detailed retinal imaging was performed (colour fundus photography, optical coherence tomography, fundus autofluorescence. RESULTS: Eight individuals were ascertained. A novel GPR143 mutation was identified in one family (p.Gln328Ter). Foveal fundus autofluorescence was subjectively reduced in 6/6 patients imaged. A "tapetal-like" pattern of autofluorescence was visible at the macula in 3/6. Persistence of the inner retinal layers at the fovea was observed in 6/8 females. CONCLUSION: Female carriers of ocular albinism may manifest signs of retinal pigment epithelium mosaicism at the macula and the peripheral fundus. A tapetal-like reflex on fundus autofluorescence may be considered the macular correlate of "mud-splatter."

Published

2017

28. Recessive Mutations in SLC38A8 Cause Foveal Hypoplasia and Optic Nerve Misrouting without Albinism

Author

Eamonn Sheridan, Chris F. Inglehearn, Murugan Saktivel, Phillis Lakeman, Rohit Shetty, Anandula Venkataramana, Manir Ali, Sabrina Carrella, Bishwanath Pal, Ian M. Carr, Alex W. Hewitt, James A. Poulter, Maria M. van Genderen, Musallam Al-Araimi, Govindasamy Kumaramanickavel, Vedam L. Ramprasad, Mike Shires, David A. Mackey, David A. Parry, Carmel Toomes, Kamron N. Khan, Andrew R. Webster, Panagiotis I. Sergouniotis, Anthony T. Moore, Sandro Banfi, Moin Mohamed, Alex Tai Loong Tan, Ivan Conte, John Bradbury, Poulter, J. A., Al-Araimi, M., Conte, I., Van Genderen, M. M., Sheridan, E., Carr, I. M., Parry, D. A., Shires, M., Carrella, S., Bradbury, J., Khan, K., Lakeman, P., Sergouniotis, P. I., Webster, A. R., Moore, A. T., Pal, B., Mohamed, M. D., Venkataramana, A., Ramprasad, V., Shetty, R., Saktivel, M., Kumaramanickavel, G., Tan, A., Mackey, D. A., Hewitt, A. W., Banfi, S., Ali, M., Inglehearn, C. F., Toomes, C., Human Genetics, Human genetics, Other Research, Poulter, Ja, Al Araimi, M, Conte, I, van Genderen, Mm, Sheridan, E, Carr, Im, Parry, Da, Shires, M, Carrella, S, Bradbury, J, Khan, K, Lakeman, P, Sergouniotis, Pi, Webster, Ar, Moore, At, Pal, B, Mohamed, Md, Venkataramana, A, Ramprasad, V, Shetty, R, Saktivel, M, Kumaramanickavel, G, Tan, A, Mackey, Da, Hewitt, Aw, Banfi, Sandro, Ali, M, and Inglehearn, Cf

Subjects

Male, Fovea Centralis, Amino Acid Transport Systems, genetic structures, Neutral, DNA Mutational Analysis, Neurodegenerative, Medical and Health Sciences, Consanguinity, 0302 clinical medicine, Foveal, 2.1 Biological and endogenous factors, Genetics(clinical), Aetiology, Child, Genetics (clinical), Pediatric, Genetics & Heredity, Genetics, 0303 health sciences, education.field_of_study, Homozygote, Syndrome, Biological Sciences, Hypoplasia, Pedigree, Phenotype, Optic nerve, Albinism, Female, Human, Population, Single-nucleotide polymorphism, Locus (genetics), Genes, Recessive, Biology, DNA Mutational Analysi, 03 medical and health sciences, Clinical Research, medicine, Recessive, Animals, Humans, education, Eye Disease and Disorders of Vision, 030304 developmental biology, Fovea Centrali, Animal, Neurosciences, Optic Nerve, medicine.disease, eye diseases, Amino Acid Transport Systems, Neutral, Genes, Mutation, 030221 ophthalmology & optometry, Congenital Structural Anomalies, sense organs

Abstract

Foveal hypoplasia and optic nerve misrouting are developmental defects of the visual pathway and only co-occur in connection with albinism; to date, they have only been associated with defects in the melanin-biosynthesis pathway. Here, we report that these defects can occur independently of albinism in people with recessive mutations in the putative glutamine transporter gene SLC38A8. Nine different mutations were identified in seven Asian and European families. Using morpholino-mediated ablation of Slc38a8 in medaka fish, we confirmed that pigmentation is unaffected by loss of SLC38A8. Furthermore, by undertaking an association study with SNPs at the SLC38A8 locus, we showed that common variants within this gene modestly affect foveal thickness in the general population. This study reveals a melanin-independent component underpinning the development of the visual pathway that requires a functional role for SLC38A8.

Published

2013

29. Characterization of CDH3-Related Congenital Hypotrichosis With Juvenile Macular Dystrophy

Author

Michel Michaelides, Stephanie Halford, Kamron N. Khan, Gavin Arno, Anthony T. Moore, Sarah Hull, Andrew R. Webster, Martin McKibbin, Vincent Plagnol, Graham E. Holder, Anthony G. Robson, and Suzanne Broadgate

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Visual acuity, genetic structures, Adolescent, Fundus Oculi, Posterior pole, DNA Mutational Analysis, Visual Acuity, Retinal Pigment Epithelium, Fundus (eye), Hypotrichosis, Retina, 030207 dermatology & venereal diseases, 03 medical and health sciences, Macular Degeneration, Young Adult, 0302 clinical medicine, Atrophy, Ophthalmology, medicine, Electroretinography, Humans, Fluorescein Angiography, Child, Retinal pigment epithelium, business.industry, DNA, Macular degeneration, Macular dystrophy, Middle Aged, medicine.disease, Cadherins, eye diseases, medicine.anatomical_structure, Child, Preschool, Mutation, 030221 ophthalmology & optometry, Disease Progression, Female, sense organs, medicine.symptom, business, Tomography, Optical Coherence

Abstract

Congenital hypotrichosis with juvenile macular dystrophy (HJMD) is a rare disorder presenting in childhood and adolescence with central visual disturbance and sparse scalp hair. Reported retinal imaging is lacking, and whether the condition is progressive remains unclear.To investigate a series of patients with HJMD due to biallelic mutations in CDH3 and thereby characterize the disorder.Ten patients from 10 families underwent detailed clinical assessment, including serial retinal imaging and electrophysiologic evaluation, at Moorfields Eye Hospital, St James's University Hospital, and Calderdale Royal Infirmary. Patients ranged in age from 3 to 17 years at onset and 5 to 57 years at last assessment. The molecular genetic investigation included bidirectional Sanger sequencing of all exons and intron-exon boundaries of CDH3 and whole-exome sequencing in 2 patients. The study was conducted from June 5, 2013, to January 15, 2016, with final follow-up completed on December 15, 2015.Results of clinical assessment and molecular genetic testing.All 10 patients (7 male and 3 female) presented with central visual disturbance in childhood and had lifelong sparse scalp hair with normal facial hair. Fundus examination revealed chorioretinal atrophy of the posterior pole contiguous with the disc in all but 1 patient that was associated with marked loss of autofluorescence on fundus autofluorescence imaging. Optical coherence tomography (OCT) demonstrated variable degrees of atrophy of the outer retina, retinal pigment epithelium, and choroid, with outer retinal tubulations frequently observed. One patient had mild disruption of the inner segment ellipsoid band on OCT and additional mild digit abnormalities. Electrophysiologic evaluation in 5 patients demonstrated macular dysfunction with additional mild, generalized retinal dysfunction in 2 patients. Eight patients had more than 1 evaluation; of these, 5 patients showed deterioration of visual acuity over time, 1 patient remained stable, and 2 patients had severe visual loss at presentation that precluded assessment of visual deterioration. The area of atrophy did not progress with time, but retinal thickness decreased on OCT. Electrophysiologic evaluation in 1 patient found deterioration of macular function after 13 years of follow-up, but the mild, generalized photoreceptor dysfunction remained stable. Biallelic mutations were identified in all patients, including 6 novel mutations.These results suggest that CDH3-related disease is characterized by a childhood-onset, progressive chorioretinal atrophy confined to the posterior pole. The disease is readily distinguished from other juvenile macular dystrophies by the universally thin and sparse scalp hair. Patients may have additional limb abnormalities.

Published

2016

30. Differentiating drusen: Drusen and drusen-like appearances associated with ageing, age-related macular degeneration, inherited eye disease and other pathological processes

Author

Moin D. Mohamed, Michel Michaelides, Kamron N. Khan, Alan C. Bird, Rehna Khan, Adnan Tufail, Omar A. Mahroo, Martin McKibbin, and Anthony T. Moore

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Aging, genetic structures, Eye disease, Context (language use), Retinal Drusen, Retinal Pigment Epithelium, Drusen, Biology, Retina, 03 medical and health sciences, Macular Degeneration, 0302 clinical medicine, medicine, Animals, Humans, Pathological, Retinal pigment epithelium, Macular degeneration, Retinal dystrophy, Eye Diseases, Hereditary, Anatomy, medicine.disease, Sensory Systems, eye diseases, Ophthalmology, 030104 developmental biology, medicine.anatomical_structure, Retinal drusen, 030221 ophthalmology & optometry, Eye disorder, sense organs

Abstract

Drusen are discussed frequently in the context of their association with age-related macular degeneration (AMD). Some types may, however, be regarded as a normal consequence of ageing; others may be observed in young age groups. They also occur in a number of inherited disorders and some systemic conditions. Whilst drusen are classically located external (sclerad) to the retinal pigment epithelium, accumulations of material internal (vitread to) this layer can display a drusen-like appearance, having been variously termed pseudodrusen or subretinal drusenoid deposits. This review first briefly presents an overview of drusen biogenesis and subclinical deposit. The (frequently overlapping) subtypes of clinically detectable deposit, seen usually in the context of ageing or AMD, are then described in more detail, together with appearance on imaging modalities: these include hard and soft drusen, cuticular drusen, reticular pseudodrusen and “ghost drusen”. Eye disorders other than AMD which may exhibit drusen or drusen-like features are subsequently discussed: these include monogenic conditions as well as conditions with undefined inheritance, the latter including some types of early onset drusen such as large colloid drusen. A number of systemic conditions in which drusen-like deposits may be seen are also considered. Throughout this review, high resolution images are presented for most of the conditions discussed, particularly the rarer ones, providing a useful reference library for images of the range of conditions associated with drusen-like appearances. In the final section, some common themes are highlighted, as well as a brief discussion of some future avenues for research.

Published

2015

31. Next generation sequencing identifies mutations in Atonal homolog 7 (ATOH7) in families with global eye developmental defects

Author

Eamonn Sheridan, Graham R. Taylor, Joanne E. Morgan, Narcis Fernandez-Fuentes, Hussain Jafri, Ahmed Al-Maskari, Özlem Yenice, Colin A. Johnson, Clare V. Logan, Carmel Toomes, Nursel Elcioglu, Manir Ali, Yasmin Raashid, David A. Parry, Martin McKibbin, Chris F. Inglehearn, Kamron N. Khan, Moin Mohamed, Zakia Abdelhamed, James A. Poulter, Ian M. Carr, Khan, Kamron, Logan, Clare V., McKibbin, Martin, Sheridan, Eamonn, Elcioglu, Nursel H., Yenice, Ozlem, Parry, David A., Fernandez-Fuentes, Narcis, Abdelhamed, Zakia I. A., Al-Maskari, Ahmed, Poulter, James A., Mohamed, Moin D., Carr, Ian M., Morgan, Joanne E., Jafri, Hussain, Raashid, Yasmin, Taylor, Graham R., Johnson, Colin A., Inglehearn, Chris F., Toomes, Carmel, and Ali, Manir

Subjects

Male, Eye Diseases, genetic structures, DNA Mutational Analysis, Nerve Tissue Proteins, Biology, Eye, Microphthalmia, Retina, Consanguinity, 03 medical and health sciences, 0302 clinical medicine, NORRIE-DISEASE, VASCULATURE, Basic Helix-Loop-Helix Transcription Factors, Genetics, medicine, Humans, Eye Abnormalities, GENOME-WIDE ASSOCIATION, Eye Proteins, FZD4 MUTATIONS, Persistent fetal vasculature, Molecular Biology, beta Catenin, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Optic nerve hypoplasia, Articles, General Medicine, EXUDATIVE VITREORETINOPATHY, medicine.disease, eye diseases, ATONAL HOMOLOG, Microcornea, medicine.anatomical_structure, Persistent hyperplastic primary vitreous, Mutation, 030221 ophthalmology & optometry, Congenital cataracts, Optic nerve, RETINAL GANGLION-CELL, FATE DETERMINATION, sense organs, OPEN-ANGLE GLAUCOMA, OPTIC-NERVE

Abstract

The atonal homolog 7 (ATOH7) gene encodes a transcription factor involved in determining the fate of retinal progenitor cells and is particularly required for optic nerve and ganglion cell development. Using a combination of autozygosity mapping and next generation sequencing, we have identified homozygous mutations in this gene, p.E49V and p.P18RfsX69, in two consanguineous families diagnosed with multiple ocular developmental defects, including severe vitreoretinal dysplasia, optic nerve hypoplasia, persistent fetal vasculature, microphthalmia, congenital cataracts, microcornea, corneal opacity and nystagmus. Most of these clinical features overlap with defects in the Norrin/beta-catenin signalling pathway that is characterized by dysgenesis of the retinal and hyaloid vasculature. Our findings document Mendelian mutations within ATOH7 and imply a role for this molecule in the development of structures at the front as well as the back of the eye. This work also provides further insights into the function of ATOH7, especially its importance in retinal vascular development and hyaloid regression.

Published

2011

32. Homozygous Mutations in PXDN Cause Congenital Cataract, Corneal Opacity, and Developmental Glaucoma

Author

Ngy Meng, Robert J Casson, Martin McKibbin, Eamonn Sheridan, Carmel Toomes, Michael Hammerton, Clare V. Logan, Colin A. Johnson, James Muecke, David A. Parry, Chris F. Inglehearn, Kathryn P. Burdon, Graham R. Taylor, Kate J. Laurie, Yasmin Raashid, Manir Ali, Ian M. Carr, Adam K Rudkin, Rhys Fogarty, Narcis Fernandez-Fuentes, Zakia Abdelhamed, Hussain Jafri, Kamron N. Khan, Horm Piseth, Mike Shires, Joanne E. Morgan, James A. Poulter, Jamie E Craig, and Moin Mohamed

Subjects

Models, Molecular, medicine.medical_specialty, genetic structures, Molecular Sequence Data, Glaucoma, medicine.disease_cause, Cataract, Cornea, Extracellular matrix, Mice, 03 medical and health sciences, Dysgenesis, Corneal Opacity, 0302 clinical medicine, Report, Ophthalmology, medicine, Genetics, Animals, Humans, Genetic Predisposition to Disease, Genetics(clinical), Genetics (clinical), Peroxidase, 030304 developmental biology, Extracellular Matrix Proteins, 0303 health sciences, Mutation, Base Sequence, business.industry, Sequence Analysis, DNA, medicine.disease, Phenotype, eye diseases, Pedigree, medicine.anatomical_structure, Microscopy, Fluorescence, Lens (anatomy), 030221 ophthalmology & optometry, Trabecular meshwork, sense organs, business

Abstract

Anterior segment dysgenesis describes a group of heterogeneous developmental disorders that affect the anterior chamber of the eye and are associated with an increased risk of glaucoma. Here, we report homozygous mutations in peroxidasin (PXDN) in two consanguineous Pakistani families with congenital cataract-microcornea with mild to moderate corneal opacity and in a consanguineous Cambodian family with developmental glaucoma and severe corneal opacification. These results highlight the diverse ocular phenotypes caused by PXDN mutations, which are likely due to differences in genetic background and environmental factors. Peroxidasin is an extracellular matrix-associated protein with peroxidase catalytic activity, and we confirmed localization of the protein to the cornea and lens epithelial layers. Our findings imply that peroxidasin is essential for normal development of the anterior chamber of the eye, where it may have a structural role in supporting cornea and lens architecture as well as an enzymatic role as an antioxidant enzyme in protecting the lens, trabecular meshwork, and cornea against oxidative damage.

Published

2011

33. Vitamin A deficiency due to bi-allelic mutation of RBP4: There’s more to it than meets the eye

Author

Michel Michaelides, F. Lucy Raymond, Anthony T. Moore, Keren J. Carss, Gavin Arno, Kamron N. Khan, and Farrah Islam

Subjects

Adult, 0301 basic medicine, Pediatrics, medicine.medical_specialty, Retinal dystrophy, Iris, Disease, Biology, medicine.disease_cause, Microphthalmia, Consanguinity, 03 medical and health sciences, medicine, Humans, Microphthalmos, Allele, Vitamin A, Alleles, Genetics (clinical), Whole genome sequencing, Genetics, Mutation, Whole Genome Sequencing, Vitamin A Deficiency, medicine.disease, Phenotype, Coloboma, Vitamin A deficiency, Ophthalmology, 030104 developmental biology, Pediatrics, Perinatology and Child Health, Female, Retinol-Binding Proteins, Plasma, Retinitis Pigmentosa, Tomography, Optical Coherence

Abstract

Vitamin A deficiency is the leading cause of preventable blindness in children worldwide and results in a well-recognized ocular phenotype. Herein we describe a patient presenting to the eye clinic with a retinal dystrophy and ocular colobomata. This combination of clinical signs and consanguineous pedigree structure suggested a genetic basis for the disease, a hypothesis that was tested using whole genome sequencing. Bi-allelic mutations in RBP4 were identified (c.248+1G>A), consistent with a diagnosis of inherited vitamin A deficiency. We describe a constellation of signs that appear to be characteristic for this disease, increasing clinical awareness of this rare condition.

Published

2016

34. Association of Steroid 5α-Reductase Type 3 Congenital Disorder of Glycosylation With Early-Onset Retinal Dystrophy

Author

Carmel Toomes, Gavin Arno, Anthony T. Moore, Martin McKibbin, Andrew R. Webster, Manir Ali, Nikolas Pontikos, Katherine R. Smith, Jill Clayton-Smith, James A. Poulter, Jiten Morarji, Alison J. Hardcastle, Rachel L. Taylor, Chris F. Inglehearn, Michel Michaelides, Graeme C.M. Black, Sarah Hull, Stephanie Grunewald, Antonio Rueda Martin, and Kamron N. Khan

Subjects

Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Visual acuity, Adolescent, Genetic counseling, DNA Mutational Analysis, Vision Disorders, Visual Acuity, Disease, Nyctalopia, Young Adult, 03 medical and health sciences, chemistry.chemical_compound, Congenital Disorders of Glycosylation, 3-Oxo-5-alpha-Steroid 4-Dehydrogenase, Ophthalmology, Retinal Dystrophies, Electroretinography, medicine, Humans, Exome, Fluorescein Angiography, Exome sequencing, Genome, business.industry, Membrane Proteins, Retinal, Sequence Analysis, DNA, medicine.disease, Pedigree, Phenotype, 030104 developmental biology, chemistry, Mutation, Visual Field Tests, Female, Visual Fields, medicine.symptom, business, Congenital disorder of glycosylation

Abstract

Importance: Steroid 5α-reductase type 3 congenital disorder of glycosylation (SRD5A3-CDG) is a rare disorder of N-linked glycosylation. Its retinal phenotype is not well described but could be important for disease recognition because it appears to be a consistent primary presenting feature. Objective: To investigate a series of patients with the same mutation in the SRD5A3 gene and thereby characterize its retinal manifestations and other associated features. Design, Setting and Participants: Seven affected individuals from 4 unrelated families with early-onset retinal dystrophy as a primary manifestation underwent comprehensive ophthalmic assessment, including retinal imaging and electrodiagnostic testing. Developmental and systemic findings were also recorded. Molecular genetic approaches, including targeted next-generation sequencing, autozygosity mapping, and apex microarray, were tried to reach a diagnosis; all participants were mutation negative. Whole-exome sequencing or whole-genome sequencing was used to identify the causative variant. Biochemical profiling was conducted to confirm a CDG type I defect. Patient phenotype data were collected over the course of ophthalmic follow-up, spanning a period of 20 years, beginning March 20, 1997, through September 15, 2016. Main Outcomes and Measures: Detailed clinical phenotypes as well as genetic and biochemical results. Results: The cohort consisted of 7 participants (5 females and 2 males) whose mean (SD) age at the most recent examination was 17.1 (3.9) years and who were all of South Asian ethnicity. Whole-exome sequencing and whole-genome sequencing identified the same homozygous SRD5A3 c.57G>A, p.(Trp19Ter) variant as the underlying cause of early-onset retinal dystrophy in each family. Detailed ocular phenotyping identified early-onset (aged ≤3 years) visual loss (mean [SD] best-corrected visual acuity, +0.95 [0.34] logMAR [20/180 Snellen]), childhood-onset nyctalopia, myopia (mean [SD] refractive error, -6.71 [-4.22]), and nystagmus. Six of the 7 patients had learning difficulties and psychomotor delay. Fundus autofluorescence imaging and optical coherence tomographic scans were abnormal in all patients, and electrodiagnostic testing revealed rod and cone dysfunction in the 5 patients tested. Conclusions and Relevance: Mutations in the SRD5A3 gene may cause early-onset retinal dystrophy, a previously underdescribed feature of the SRD5A3-CDG disorder that is progressive and may lead to serious visual impairment. SRD5A3 and other glycosylation disorder genes should be considered as a cause of retinal dystrophy even when systemic features are mild. Further delineation of SRD5A3-associated eye phenotypes can help inform genetic counseling for prognostic estimation of visual loss and disease progression.

Published

2017

35. [Untitled]

Author

Christopher L.-H. Huang, Anthony J. Burgess, Kamron N. Khan, Austin R. Hockaday, and Jeremy N. Skepper

Subjects

Osmotic shock, Physiology, medicine.drug_class, Furosemide, Cell Biology, Vacuole, Distension, Loop diuretic, Biochemistry, chemistry.chemical_compound, chemistry, Glycerol, medicine, Biophysics, Extracellular, Bumetanide, medicine.drug

Abstract

The effect of loop diuretics at concentrations known to influence cellular water entry coupled to Na-K-Cl co-transport, upon the vacuolation and detubulation following osmotic shock, was investigated in amphibian skeletal muscles. These were exposed to a glycerol-Ringer solution (18 min), an isotonic Ca2+/Mg2+ Ringer solution and cooling. Adding bumetanide (1.0 and 2.0 μM) to these solutions sharply reduced the incidence of detubulation, assessed by abolition or otherwise of action potential after-depolarisations, from 93.9 ± 4.7% (n = 6) to 5.0 ± 1.1% (n = 4: mean ± SEM: 2.0 μM bumetanide). It dramatically reduced the number and fraction of muscle volume occupied by tubular vacuoles, measured using confocal microscopy, from 60.3 ± 4.3% (n = 10) to 9.0 ± 1.1% (n = 35). The incidence of large horseradish peroxidase-lined tubular vacuoles, viewed using electronmicroscopy, similarly was reduced with 2 μM bumetanide in the glycerol-Ringer solution. Bumetanide acted through cellular volume adjustments early in the detubulation protocol. Thus, it exerted its maximum effect when added to the glycerol-Ringer, rather than the Ca2+/Mg2+ Ringer solution. Furthermore, whereas fibre diameters measured using scanning electron microscopy returned to normal during glycerol treatment relative to those of control fibres left in isotonic Ringer, addition of 2.0 μM bumetanide in the glycerol Ringer left markedly smaller fibre diameters. Finally equipotent concentrations of the chemically distinct loop diuretics, furosemide and ethacrynic acid similarly influenced detubulation. These findings implicate Na-K-Cl co-transport in the water entry into muscle fibres that would be expected following introduction of extracellular glycerol. This might then enable the subsequent Na-K-ATPase dependent water extrusion that produces the tubular distension (vacuolation) and detachment (detubulation) following glycerol withdrawal, phenomena also observed in muscular dystrophy.

Published

2000

36. A cautious approach to interpreting retrospective data

Author

Rubina Rahman and Kamron N. Khan

Subjects

Male, medicine.medical_specialty, Phacoemulsification, genetic structures, business.industry, medicine.medical_treatment, Epiretinal Membrane, Cataract surgery, medicine.disease, Sensory Systems, Retrospective data, Surgery, Cellular and Molecular Neuroscience, Ophthalmology, Lens Implantation, Intraocular, Retinal Diseases, medicine, Humans, Female, Epiretinal membrane, business, Single session

Abstract

The recent article of Yiu et al 1 aims to compare the functional and anatomical outcomes after idiopathic epiretinal membrane (ERM) surgery either ‘alone’ or when ‘combined’ with a cataract surgery. We feel that the design of this study is fundamentally flawed, however. In order to adequately compare these groups, the ‘alone’ group should remain phakic for the duration of the study. In this paper, the ‘alone’ group were already pseudophakic in 67.5% of cases (27/40) at recruitment, and a further 10% received surgery for lens opacification at a separate date. The authors have, therefore, compared single session combined surgery with sequential individual surgery (primary cataract surgery with late ERM peeling) in 77.5% of cases. Furthermore, all …

Published

2013

37. Defining small eye phenotypes

Author

Osama Giasin and Kamron N. Khan

Subjects

Genetics, musculoskeletal diseases, Male, congenital, hereditary, and neonatal diseases and abnormalities, Eye Diseases, Biology, Phenotype, Article, Craniofacial Abnormalities, Holoprosencephaly, Humans, Female, Small eye, Genetics (clinical)

Abstract

Holosprosencephaly (HPE) is the most common disorder of the developing forebrain in humans, and is characterized by failed or incomplete cleavage of the cerebral hemispheres and deep brain structures. HPE includes wide phenotypic variability, with a continuum of both brain and craniofacial anomalies.

Published

2011

38. Outcomes of sulfur hexafluoride (SF6) versus perfluoroethane (C2F6) gas tamponade for non-posturing macular-hole surgery

Author

Rubina Rahman, Indira Madgula, and Kamron N. Khan

Subjects

Male, medicine.medical_specialty, Visual acuity, genetic structures, Eye disease, Posture, Sulfur Hexafluoride, Vision Disorders, Visual Acuity, Endotamponade, Perfluoroethane, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Lens Implantation, Intraocular, Ophthalmology, Vitrectomy, medicine, Humans, Silicone Oils, Prospective Studies, Macular hole, Aged, Retrospective Studies, Aged, 80 and over, Fluorocarbons, Phacoemulsification, business.industry, Middle Aged, medicine.disease, Retinal Perforations, eye diseases, Sensory Systems, Surgery, Sulfur hexafluoride, Treatment Outcome, chemistry, Maculopathy, Female, Tamponade, medicine.symptom, business, Tomography, Optical Coherence, Retinopathy, Follow-Up Studies

Abstract

Aim To compare the outcomes of non-posturing macular-hole surgery using sulfur hexafluoride (SF 6 ) gas versus perfluoroethane (C 2 F 6 ) for idiopathic macular hole repair. Design Interventional, comparative cohort study. Methods 39 eyes of 38 patients undergoing macular-hole surgery with SF 6 were compared with another consecutive group of 39 eyes (39 patients) in whom C 2 F 6 was used. All patients were operated on by a single surgeon and underwent 23G transconjunctival phakovitrectomy with no prone posturing in the postoperative period. The best-corrected Snellen9s visual acuity (VA) was converted to the logarithm of minimal angle of resolution (logmar) visual acuity for analysis. Optical coherence tomography documentation of anatomical closure and complications of surgery were recorded. Results Primary hole closure was achieved in 89.75% in the C 2 F 6 group and 87.2% in the SF 6 group. Secondary closure after non-posturing redo surgery with heavy oil (Oxane-HD) was 100% in both groups. The mean preoperative VA in the C 2 F 6 group and SF 6 group was 0.81 logMAR and 0.78 respectively. 2 weeks after surgey, SF 6 was completely absorbed in all cases, and the mean VA improved to 0.5 logMAR; however, it remained 1.9 logMAR in the C 2 F 6 group. The final mean VA at 6 months was 0.44 (range 0–0.78) and 0.38 (range 0–1) in the C 2 F 6 and SF 6 group respectively. There were no instances of pupillary capture in the SF 6 group, whereas there were four in the C 2 F 6 group. Conclusion Macular-hole surgery with SF 6 gas achieves similar results to C 2 F 6 and is absorbed faster, allowing quicker visual rehabilitation for the patient.

Published

2011

39. Genetic heterogeneity for recessively inherited congenital cataract microcornea with corneal opacity

Author

Chris F. Inglehearn, Martin McKibbin, Manir Ali, Eamonn Sheridan, Ahmed Al-Maskari, Carmel Toomes, Tehseen Sahi, Aine Rice, Clara V. Logan, Yasmin Raashid, James A. Poulter, Alex F. Markham, Salina Siddiqui, Colin A. Johnson, David A. Parry, Adam Booth, Moin Mohamed, Kamron N. Khan, Ian M. Carr, Hussain Jafri, and Anwar Hashmi

Subjects

Male, Candidate gene, genetic structures, Adolescent, Biology, Cataract, Corneal Diseases, Cornea, Genetic Heterogeneity, Corneal Opacity, SNP, Polymorphic Microsatellite Marker, Humans, Genetic Predisposition to Disease, Pakistan, Child, Genetics, Linkage (software), Genetic heterogeneity, Homozygote, DNA, Sequence Analysis, DNA, Articles, Disease gene identification, eye diseases, Microcornea, Pedigree, Female, sense organs

Abstract

To investigate whether three consanguineous families from the Punjab province of Pakistan, with affected members with recessively inherited congenital cataract microcornea with corneal opacity, are genetically homogeneous.An ophthalmic examination was performed on each family member to establish the diagnosis. The two largest families were analyzed by homozygosity mapping using SNP arrays. Linkage was confirmed using polymorphic microsatellite markers, and logarithm of odds (LOD) scores were calculated. Candidate genes were prioritized using the ENDEAVOUR program.Autosomal recessive congenital cataract-microcornea with corneal opacity mapped to chromosome 10cen for family MEP57 and to either chromosomes 2ptel or 20p for family MEP60. For MEP57, the refined interval was 36.8 Mb flanked by D10S1208 (35.3 Mb) and D10S676 (72.1 Mb). For MEP60, the interval containing the mutation was either 6.7 Mb from the telomere of chromosome 2 to marker D2S281 or 3.8 Mb flanked by D20S906 (1.5 Mb) and D20S835 (5.3 Mb). Maximum multipoint LOD scores of 3.09, 1.94, and 3.09 were calculated at D10S567, D2S281, and D20S473 for families MEP57 and MEP60. Linkage to these loci was excluded for family MEP68. SLC4A11 was excluded as a candidate gene for the observed phenotype in MEP60.The authors have identified two new loci, one on chromosome 10cen and the other on 2ptel or 20p, that are associated with recessively inherited congenital cataract-microcornea with corneal opacity. This phenotype is genetically heterogeneous in the Pakistani population. Further genetic studies of this kind, combined with a detailed phenotypic description, will contribute to more precise classification criteria for anterior segment disease.

Published

2011

40. Macular OCT changes after vitrectomy

Author

S.K. Gibran, Kamron N. Khan, S. Madhusudhan, and R. Jayaswal

Subjects

medicine.medical_specialty, Visual acuity, Eye Diseases, business.industry, medicine.medical_treatment, Visual Acuity, Vitrectomy, Vitreous Body, Ophthalmology, Text mining, Postoperative Complications, Macula Lutea, Retinal Diseases, medicine, Humans, Prospective Studies, medicine.symptom, business, Tomography, Optical Coherence

Published

2007

41. Correspondence

Author

Kamron N, Khan and Rubina, Rahman

Subjects

Male, Ophthalmology, Vitrectomy, Humans, Female, General Medicine, Retinal Perforations

Published

2014

42. Increasing the efficiency of ophthalmic care for all patients during Ramadan

Author

A Al-Maskari, Kamron N. Khan, and R Khan

Subjects

Evening, genetic structures, business.industry, Poor compliance, Glaucoma, Disease monitoring, medicine.disease, humanities, eye diseases, Sensory Systems, Cellular and Molecular Neuroscience, Ophthalmology, chemistry.chemical_compound, Muslim population, chemistry, medicine, Optometry, Latanoprost, business, Patient education

Abstract

Ramadan (the month of fasting for Muslims) is approaching at the end of August 2009. As ophthalmologists in a centre with a large Muslim population, we read Kumar et al 's study with interest.1 We agree that poor compliance with treatment can be improved with patient education. A major proportion of chronic ophthalmological disease monitoring is for glaucoma, first-line treatment for which is guttae latanoprost, administered in the evening. This does not interfere with fasting which ends after sunset. If a Muslim patient has good compliance outside the month of Ramadan, fasting will not be a cause for poor compliance during Ramadan. With the support of the ophthalmologist to remind the patient, drops that require twice-daily use can be instilled before …

Published

2009

43. Rapid Visualisation of Microarray Copy Number Data for the Detection of Structural Variations Linked to a Disease Phenotype

Author

Kamron N. Khan, Christine P. Diggle, Sérgio D.J. Pena, Rashida Anwar, Manir Ali, David T. Bonthron, Ian M. Carr, Angus Dobbie, Alexander F. Markham, Chris F. Inglehearn, Martin McKibbin, and Adamovic, T

Subjects

Male, DNA Copy Number Variations, Microarray, Microarrays, Copy number analysis, lcsh:Medicine, Loss of Heterozygosity, Biology, Polymorphism, Single Nucleotide, Genome, Cytogenetics, Chromosomal Disorders, Genome Analysis Tools, Genetics, Humans, Genetic Predisposition to Disease, Genetic Testing, Genetic variability, Copy-number variation, lcsh:Science, Aniridia, Genotyping, Genetic Association Studies, Oligonucleotide Array Sequence Analysis, Chromosome Aberrations, Family Health, Clinical Genetics, Linkage Maps, Multidisciplinary, Genome, Human, lcsh:R, Chromosome Mapping, Reproducibility of Results, Computational Biology, Chromosomal Deletions and Duplications, Human Genetics, Genomics, Phenotype, Pedigree, Cytogenetic Analysis, Medicine, lcsh:Q, Female, DNA microarray, Software, Research Article

Abstract

Whilst the majority of inherited diseases have been found to be caused by single base substitutions, small insertions or deletions (

Published

2012

44. Corneal Thinning Phenotypes—An Alternative Perspective

Author

Rehna S. Khan, Kamron N. Khan, and Osama Giasin

Subjects

medicine.medical_specialty, medicine.anatomical_structure, business.industry, Ophthalmology, Cornea, Corneal thinning, Perspective (graphical), Medicine, business, Phenotype

Published

2012

45. Changing the status quo bias

Author

Manir Ali, Chris F. Inglehearn, John Bradbury, Carmel Toomes, and Kamron N. Khan

Subjects

Pediatrics, medicine.medical_specialty, Status quo bias, business.industry, Alternative medicine, Retinopathy of prematurity, Retrospective cohort study, medicine.disease, Evidence level, Sensory Systems, Cellular and Molecular Neuroscience, Ophthalmology, medicine, business

Abstract

We read with interest the article by Durnian and Clark who presented a retrospective cohort of infants that fell outside evidence level B guidelines for screening retinopathy of prematurity (ROP) and we wish to discuss some further points.1 The data presented in table 1 highlight that all 11 babies would be missed if screening was according to level B evidence and 2 of these would still be missed using the good practice points evidence. An alternative conclusion would be that if the guidelines had been amended to screen infants under 32 weeks or 1251 g then one extra baby would have been missed (who fortunately did not require treatment). It is also debatable based on the information presented, if any of the babies absolutely required treatment as others …

Published

2011

46. Reply to Papanikolaou et al

Author

Manir Ali, Kamron N. Khan, and Chris F. Inglehearn

Subjects

Cellular and Molecular Neuroscience, Ophthalmology, medicine.medical_specialty, business.industry, Medicine, business, Nodular corneal degeneration, Dermatology, Sensory Systems

Abstract

We read with interest the recent article of Papanikolaou et al 1 describing a possible inherited form of Salzmann's nodular …

Published

2010

47. Changing the status quo bias.

Author

Kamron N Khan

Published

2011