Ophthalmology (Eye & Ear Hospital) - Research Publications

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    Diagnostic yield of candidate genes in an Australian corneal dystrophy cohort
    Souzeau, E ; Siggs, OM ; Mullany, S ; Schmidt, JM ; Hassall, MM ; Dubowsky, A ; Chappell, A ; Breen, J ; Bae, H ; Nicholl, J ; Hadler, J ; Kearns, LS ; Staffieri, SE ; Hewitt, AW ; Mackey, DA ; Gupta, A ; Burdon, KP ; Klebe, S ; Craig, JE ; Mills, RA (WILEY, 2022-10)
    Corneal dystrophies describe a clinically and genetically heterogeneous group of inherited disorders. The International Classification of Corneal Dystrophies (IC3D) lists 22 types of corneal dystrophy, 17 of which have been demonstrated to result from pathogenic variants in 19 identified genes. In this study, we investigated the diagnostic yield of genetic testing in a well-characterised cohort of 58 individuals from 44 families with different types of corneal dystrophy. Individuals diagnosed solely with Fuchs endothelial corneal dystrophy were excluded. Clinical details were obtained from the treating ophthalmologist. Participants and their family members were tested using a gene candidate and exome sequencing approach. We identified a likely molecular diagnosis in 70.5% families (31/44). The detection rate was significantly higher among probands with a family history of corneal dystrophy (15/16, 93.8%) than those without (16/28, 57.1%, p = .015), and among those who had undergone corneal graft surgery (9/9, 100.0%) compared to those who had not (22/35, 62.9%, p = .041). We identified eight novel variants in five genes and identified five families with syndromes associated with corneal dystrophies. Our findings highlight the genetic heterogeneity of corneal dystrophies and the clinical utility of genetic testing in reaching an accurate clinical diagnosis.
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    Attitudes Toward Glaucoma Genetic Risk Assessment in Unaffected Individuals
    Hollitt, GL ; Siggs, OM ; Ridge, B ; Keane, MC ; Mackey, DA ; MacGregor, S ; Hewitt, AW ; Craig, JE ; Souzeau, E (ASSOC RESEARCH VISION OPHTHALMOLOGY INC, 2022-10)
    PURPOSE: Integrating polygenic risk scores (PRS) into healthcare has the potential to stratify an individual's risk of glaucoma across a broad population. Glaucoma is the most common cause of irreversible blindness worldwide, therefore effective screening for glaucoma endorsed by the population is highly important. This study assessed the attitude of unaffected individuals toward PRS testing for glaucoma, and sought to identify factors associated with interest in testing. METHODS: We surveyed 418 unaffected individuals including 193 with a first-degree relative with glaucoma, 117 who had a recent eye examination, and 108 general members of the community. RESULTS: Overall, 71.3% of the individuals indicated an interest in taking a polygenic risk test for glaucoma. Interest was more likely in those who believed glaucoma to be a severe medical condition (odds ratio [OR] = 14.58, 95% confidence interval [CI] = 1.15-185.50, P = 0.039), those concerned about developing glaucoma (OR = 4.37, 95% CI = 2.32-8.25, P < 0.001), those with an intention to take appropriate measures regarding eye health (OR = 2.39, 95% CI = 1.16-4.95, P = 0.019), and those preferring to know if considered to be at-risk or not (OR = 4.52, 95% CI = 2.32-8.83, P < 0.001). CONCLUSIONS: Our results show strong interest in genetic risk assessment for glaucoma among unaffected individuals in Australia. TRANSLATIONAL RELEVANCE: These findings represent a valuable assessment of interest in glaucoma polygenic risk testing among potential target populations, which will be integral to the implementation and uptake of novel PRS-based tests into clinical practice.
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    Retinal ganglion cell-specific genetic regulation in primary open-angle glaucoma
    Daniszewski, M ; Senabouth, A ; Liang, HH ; Han, X ; Lidgerwood, GE ; Hernandez, D ; Sivakumaran, P ; Clarke, JE ; Lim, SY ; Lees, JG ; Rooney, L ; Gulluyan, L ; Souzeau, E ; Graham, SL ; Chan, C-L ; Nguyen, U ; Farbehi, N ; Gnanasambandapillai, V ; Mccloy, RA ; Clarke, L ; Kearns, LS ; Mackey, DA ; Craig, JE ; Macgregor, S ; Powell, JE ; Pebay, A ; Hewitt, AW (ELSEVIER, 2022-06-08)
    To assess the transcriptomic profile of disease-specific cell populations, fibroblasts from patients with primary open-angle glaucoma (POAG) were reprogrammed into induced pluripotent stem cells (iPSCs) before being differentiated into retinal organoids and compared with those from healthy individuals. We performed single-cell RNA sequencing of a total of 247,520 cells and identified cluster-specific molecular signatures. Comparing the gene expression profile between cases and controls, we identified novel genetic associations for this blinding disease. Expression quantitative trait mapping identified a total of 4,443 significant loci across all cell types, 312 of which are specific to the retinal ganglion cell subpopulations, which ultimately degenerate in POAG. Transcriptome-wide association analysis identified genes at loci previously associated with POAG, and analysis, conditional on disease status, implicated 97 statistically significant retinal ganglion cell-specific expression quantitative trait loci. This work highlights the power of large-scale iPSC studies to uncover context-specific profiles for a genetically complex disease.
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    The Relationship Between Fetal Growth and Retinal Nerve Fiber Layer Thickness in a Cohort of Young Adults
    Dyer, KIC ; Sanfilippo, PG ; Yazar, S ; Craig, JE ; Hewitt, AW ; Newnham, JP ; Mackey, DA ; Lee, SSY (ASSOC RESEARCH VISION OPHTHALMOLOGY INC, 2022-07)
    PURPOSE: To explore relationships between patterns of fetal anthropometric growth, as reflective of fetal wellbeing, and global retinal nerve fiber layer (RNFL) thickness measured in young adulthood. METHODS: Participants (n = 481) from within a Western Australian pregnancy cohort study underwent five serial ultrasound scans during gestation, with fetal biometry measured at each scan. Optic disc parameters were measured via spectral-domain optical coherence tomography imaging at a 20-year follow-up eye examination. Generalized estimating equations were used to evaluate differences in global RNFL thickness between groups of participants who had undergone similar growth trajectories based on fetal head circumference (FHC), abdominal circumference (FAC), femur length (FFL), and estimated fetal weight (EFW). RESULTS: Participants with consistently large FHCs throughout gestation had significantly thicker global RNFLs than those with any other pattern of FHC growth (P = 0.023), even after adjustment for potential confounders (P = 0.037). Based on model fit statistics, FHC growth trajectory was a better predictor of global RNFL thickness than birth weight or head circumference at birth. RNFL thickness did not vary significantly between groups of participants with different growth trajectories based on FAC, FFL, or EFW. CONCLUSIONS: FHC growth is associated with RNFL thickness in young adulthood and, moreover, is a better predictor than either birth weight or head circumference at birth. TRANSLATIONAL RELEVANCE: This research demonstrates an association between intrauterine growth and long-term optic nerve health, providing a basis for further exploring the extent of the influence of fetal wellbeing on clinical conditions linked to RNFL thinning.
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    Comparison of Anterior Segment Abnormalities in Individuals With FOXC1 and PITX2 Variants
    Prem Senthil, M ; Knight, LSW ; Taranath, D ; Mackey, DA ; Ruddle, JB ; Chiang, MY ; Siggs, OM ; Souzeau, E ; Craig, JE (LIPPINCOTT WILLIAMS & WILKINS, 2022-08)
    PURPOSE: Axenfeld-Rieger syndrome encompasses a group of developmental disorders affecting the anterior chamber structures of the eye, with associated systemic features in some cases. This study aims to compare the difference in anterior segment phenotypes such as those involving the cornea, iris, lens, and anterior chamber angle between cases with disease-causing sequence variations in FOXC1 and PITX2 . METHODS: This cross-sectional study involved 61 individuals, from 32 families with pathogenic FOXC1 or PITX2 variants, who were registered with the Australian and New Zealand Registry of Advanced Glaucoma. RESULTS: The median age of the cohort was 39 years at the time of last assessment (range 3-85 years; females, 54%). Thirty-two patients had pathogenic variants in the FOXC1 gene, and 29 patients had pathogenic variants in the PITX2 gene. Corneal abnormalities were more common in individuals with FOXC1 variants (18/36, 50%) than those with PITX2 variants (4/25, 16%; P = 0.007). Iris abnormalities such as hypoplasia ( P = 0.008) and pseudopolycoria ( P = 0.001) were more common in individuals with PITX2 variants than those with FOXC1 variants. Glaucoma was present in 72% of participants. Corneal decompensation was positively associated with corneal abnormalities ( P < 0.001), glaucoma surgery ( P = 0.025), and cataract surgery ( P = 0.002). CONCLUSIONS: Corneal abnormalities were more common in individuals with FOXC1 than in those with PITX2 variants and were often associated with early onset glaucoma. These findings highlight that patients with FOXC1 variations require close follow-up and monitoring throughout infancy and into adulthood.
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    Attitudes Towards Polygenic Risk Testing in Individuals with Glaucoma
    Hollitt, GL ; Siggs, OM ; Ridge, B ; Keane, MC ; Mackey, DA ; MacGregor, S ; Hewitt, AW ; Craig, JE ; Souzeau, E (ELSEVIER, 2022-09)
    PURPOSE: Glaucoma is the leading cause of irreversible blindness worldwide; however, vision loss resulting from glaucoma generally can be prevented through early identification and timely implementation of treatment. Recently, polygenic risk scores (PRSs) have shown promise in stratifying individual risk and prognostication for primary open-angle glaucoma (POAG) to reduce disease burden. Integrating PRS testing into clinical practice is becoming increasingly realistic; however, little is known about the attitudes of patients toward such testing. DESIGN: Cross-sectional, questionnaire-based study. PARTICIPANTS: Among the participants in the Australian and New Zealand Registry of Advanced Glaucoma, 2369 were invited to participate who fit the inclusion criteria of adults with a diagnosis of POAG who had not received genetic results that explain their condition, were not known to be deceased, resided in Australia, and had agreed to receive correspondence. METHODS: One thousand one hundred sixty-nine individuals (response rate, 49%) with POAG completed the survey evaluating their attitudes towards polygenic risk testing for glaucoma. MAIN OUTCOME MEASURES: Sociodemographic, health, perception, and emotional factors were examined to assess associations with interest in PRS testing. Interest in PRS testing was evaluated through assessing likelihood to take the test to predict personal risk of disease and disease severity, and whether the individual would recommend the test to family members or others. RESULTS: Our results show strong interest in the test, with 69.4% of individuals (798 of 1150) indicating a keenness in testing before diagnosis, had it been available. In particular, interest was seen in those from an urban area (odds ratio [OR], 1.70; 95% confidence interval [CI], 1.15-2.49; P = 0.007), those who perceived their risk of developing glaucoma as higher (OR, 2.05; 95% CI, 1.28-3.29; P = 0.003), and those who were worried about developing glaucoma (OR, 2.07; 95% CI, 1.27-3.37; P = 0.004). People who were interested in testing were more likely to change their eye health-seeking intentions and to recommend testing to family members and others, as well as to undergo testing for prognostication. CONCLUSIONS: These findings will help to facilitate the clinical implementation of PRS testing for glaucoma to reduce irreversible vision loss.
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    Rare variants in optic disc area gene CARD10 enriched in primary open-angle glaucoma
    Zhou, T ; Souzeau, E ; Sharma, S ; Siggs, OM ; Goldberg, I ; Healey, PR ; Graham, S ; Hewitt, AW ; Mackey, DA ; Casson, RJ ; Landers, J ; Mills, R ; Ellis, J ; Leo, P ; Brown, MA ; MacGregor, S ; Burdon, KP ; Craig, JE (WILEY, 2016-11)
    BACKGROUND: Genome-wide association studies (GWAS) have identified association of common alleles with primary open-angle glaucoma (POAG) and its quantitative endophenotypes near numerous genes. This study aims to determine whether rare pathogenic variants in these disease-associated genes contribute to POAG. METHODS: Participants fulfilled strict inclusion criteria of advanced POAG at a young age of diagnosis. Myocilin mutation carriers were excluded using direct sequencing. Whole exome sequencing was performed on 187 glaucoma cases and 103 local screened nonglaucoma controls then joint-called with exomes of 993 previously sequenced Australian controls. GWAS-associated genes were assessed for enrichment of rare predicted pathogenic variants in POAG. Significantly enriched genes were compared against Exome Aggregation Consortium (ExAC) public control. RESULTS: Eighty-six GWAS disease or trait-associated glaucoma genes were captured and sequenced. CARD10 showed enrichment after Bonferroni correction for rare variants in glaucoma cases (OR = 13.2, P = 6.94 × 10-5) with mutations identified in 4.28% of our POAG cohort compared to 0.27% in controls. CARD10 was significantly associated with optic disc parameters in previous GWAS. The whole GWAS gene set showed no enrichment in POAG overall (OR = 1.12, P = 0.51). CONCLUSION: We report here an enrichment of rare predicted pathogenic coding variants within a GWAS-associated locus in POAG (CARD10). These findings indicate that both common and rare pathogenic coding variants in CARD10 may contribute to POAG pathogenesis.
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    Novel pleiotropic risk loci for melanoma and nevus density implicate multiple biological pathways (vol 9, 4774, 2018)
    Duffy, DL ; Zhu, G ; Li, X ; Sanna, M ; Iles, MM ; Jacobs, LC ; Evans, DM ; Yazar, S ; Beesley, J ; Law, MH ; Kraft, P ; Visconti, A ; Taylor, JC ; Liu, F ; Wright, MJ ; Henders, AK ; Bowdler, L ; Glass, D ; Ikram, MA ; Uitterlinden, AG ; Madden, PA ; Heath, AC ; Nelson, EC ; Green, AC ; Chanock, S ; Barrett, JH ; Brown, MA ; Hayward, NK ; MacGregor, S ; Sturm, RA ; Hewitt, AW ; Kayser, M ; Hunter, DJ ; Bishop, JAN ; Spector, TD ; Montgomery, GW ; Mackey, DA ; Smith, GD ; Nijsten, TE ; Bishop, DT ; Bataille, V ; Falchi, M ; Han, J ; Martin, NG ; Lee, JE ; Brossard, M ; Moses, EK ; Song, F ; Kumar, R ; Easton, DF ; Pharoah, PDP ; Swerdlow, AJ ; Kypreou, KP ; Harland, M ; Randerson-Moor, J ; Akslen, LA ; Andresen, PA ; Avril, M-F ; Azizi, E ; Scarra, GB ; Brown, KM ; Debniak, T ; Elder, DE ; Fang, S ; Friedman, E ; Galan, P ; Ghiorzo, P ; Gillanders, EM ; Goldstein, AM ; Gruis, NA ; Hansson, J ; Helsing, P ; Hocevar, M ; Hoiom, V ; Ingvar, C ; Kanetsky, PA ; Chen, WV ; Landi, MT ; Lang, J ; Lathrop, GM ; Lubinski, J ; Mackie, RM ; Mann, GJ ; Molven, A ; Novakovic, S ; Olsson, H ; Puig, S ; Puig-Butille, JA ; Radford-Smith, GL ; van der Stoep, N ; van Doorn, R ; Whiteman, DC ; Craig, JE ; Schadendorf, D ; Simms, LA ; Burdon, KP ; Nyholt, DR ; Pooley, KA ; Orr, N ; Stratigos, AJ ; Cust, AE ; Ward, SV ; Schulze, H-J ; Dunning, AM ; Demenais, F ; Amos, CI (NATURE PUBLISHING GROUP, 2019-01-14)
    The original version of this Article contained errors in the spelling of the authors Fan Liu and M. Arfan Ikram, which were incorrectly given as Fan Lui and Arfan M. Ikram. In addition, the original version of this Article also contained errors in the author affiliations which are detailed in the associated Publisher Correction.
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    Testosterone Pathway Genetic Polymorphisms in Relation to Primary Open-Angle Glaucoma: analysis in Two Large Datasets
    Bailey, JNC ; Gharahkhani, P ; Kang, JH ; Butkiewicz, M ; Sullivan, DA ; Weinreb, RN ; Aschard, H ; Allingham, RR ; Ashley-Koch, A ; Lee, RK ; Moroi, SE ; Brilliant, MH ; Wollstein, G ; Schuman, JS ; Fingert, JH ; Budenz, DL ; Realini, T ; Gaasterland, T ; Scott, WK ; Singh, K ; Sit, AJ ; Igo, RP ; Song, YE ; Hark, L ; Ritch, R ; Rhee, DJ ; Vollrath, D ; Zack, DJ ; Medeiros, F ; Vajaranant, TS ; Chasman, DI ; Christen, WG ; Pericak-Vance, MA ; Liu, Y ; Kraft, P ; Richards, JE ; Rosner, BA ; Hauser, MA ; Craig, JE ; Burdon, KP ; Hewitt, AW ; Mackey, DA ; Haines, JL ; MacGregor, S ; Wiggs, JL ; Pasquale, LR (ASSOC RESEARCH VISION OPHTHALMOLOGY INC, 2018-02)
    PURPOSE: Sex hormones may be associated with primary open-angle glaucoma (POAG), although the mechanisms are unclear. We previously observed that gene variants involved with estrogen metabolism were collectively associated with POAG in women but not men; here we assessed gene variants related to testosterone metabolism collectively and POAG risk. METHODS: We used two datasets: one from the United States (3853 cases and 33,480 controls) and another from Australia (1155 cases and 1992 controls). Both datasets contained densely called genotypes imputed to the 1000 Genomes reference panel. We used pathway- and gene-based approaches with Pathway Analysis by Randomization Incorporating Structure (PARIS) software to assess the overall association between a panel of single nucleotide polymorphisms (SNPs) in testosterone metabolism genes and POAG. In sex-stratified analyses, we evaluated POAG overall and POAG subtypes defined by maximum IOP (high-tension [HTG] or normal tension glaucoma [NTG]). RESULTS: In the US dataset, the SNP panel was not associated with POAG (permuted P = 0.77), although there was an association in the Australian sample (permuted P = 0.018). In both datasets, the SNP panel was associated with POAG in men (permuted P ≤ 0.033) and not women (permuted P ≥ 0.42), but in gene-based analyses, there was no consistency on the main genes responsible for these findings. In both datasets, the testosterone pathway association with HTG was significant (permuted P ≤ 0.011), but again, gene-based analyses showed no consistent driver gene associations. CONCLUSIONS: Collectively, testosterone metabolism pathway SNPs were consistently associated with the high-tension subtype of POAG in two datasets.
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    A 127 kb truncating deletion of PGRMC1 is a novel cause of X-linked isolated paediatric cataract
    Jones, JL ; Corbett, MA ; Yeaman, E ; Zhao, D ; Gecz, J ; Gasperini, RJ ; Charlesworth, JC ; Mackey, DA ; Elder, JE ; Craig, JE ; Burdon, KP (SPRINGERNATURE, 2021-08)
    Inherited paediatric cataract is a rare Mendelian disease that results in visual impairment or blindness due to a clouding of the eye's crystalline lens. Here we report an Australian family with isolated paediatric cataract, which we had previously mapped to Xq24. Linkage at Xq24-25 (LOD = 2.53) was confirmed, and the region refined with a denser marker map. In addition, two autosomal regions with suggestive evidence of linkage were observed. A segregating 127 kb deletion (chrX:g.118373226_118500408del) in the Xq24-25 linkage region was identified from whole-genome sequencing data. This deletion completely removed a commonly deleted long non-coding RNA gene LOC101928336 and truncated the protein coding progesterone receptor membrane component 1 (PGRMC1) gene following exon 1. A literature search revealed a report of two unrelated males with non-syndromic intellectual disability, as well as congenital cataract, who had contiguous gene deletions that accounted for their intellectual disability but also disrupted the PGRMC1 gene. A morpholino-induced pgrmc1 knockdown in a zebrafish model produced significant cataract formation, supporting a role for PGRMC1 in lens development and cataract formation. We hypothesise that the loss of PGRMC1 causes cataract through disrupted PGRMC1-CYP51A1 protein-protein interactions and altered cholesterol biosynthesis. The cause of paediatric cataract in this family is the truncating deletion of PGRMC1, which we report as a novel cataract gene.