Centre for Eye Research Australia (CERA) - Research Publications

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Author: Mackey, David × End date: 2013 × Start date: 2010 ×

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    Large scale international replication and meta-analysis study confirms association of the 15q14 locus with myopia. The CREAM consortium
    Verhoeven, VJM ; Hysi, PG ; Saw, S-M ; Vitart, V ; Mirshahi, A ; Guggenheim, JA ; Cotch, MF ; Yamashiro, K ; Baird, PN ; Mackey, DA ; Wojciechowski, R ; Ikram, MK ; Hewitt, AW ; Duggal, P ; Janmahasatian, S ; Khor, C-C ; Fan, Q ; Zhou, X ; Young, TL ; Tai, E-S ; Goh, L-K ; Li, Y-J ; Aung, T ; Vithana, E ; Teo, Y-Y ; Tay, W ; Sim, X ; Rudan, I ; Hayward, C ; Wright, AF ; Polasek, O ; Campbell, H ; Wilson, JF ; Fleck, BW ; Nakata, I ; Yoshimura, N ; Yamada, R ; Matsuda, F ; Ohno-Matsui, K ; Nag, A ; McMahon, G ; St Pourcain, B ; Lu, Y ; Rahi, JS ; Cumberland, PM ; Bhattacharya, S ; Simpson, CL ; Atwood, LD ; Li, X ; Raffel, LJ ; Murgia, F ; Portas, L ; Despriet, DDG ; van Koolwijk, LME ; Wolfram, C ; Lackner, KJ ; Toenjes, A ; Maegi, R ; Lehtimaki, T ; Kahonen, M ; Esko, T ; Metspalu, A ; Rantanen, T ; Parssinen, O ; Klein, BE ; Meitinger, T ; Spector, TD ; Oostra, BA ; Smith, AV ; de Jong, PTVM ; Hofman, A ; Amin, N ; Karssen, LC ; Rivadeneira, F ; Vingerling, JR ; Eiriksdottir, G ; Gudnason, V ; Doering, A ; Bettecken, T ; Uitterlinden, AG ; Williams, C ; Zeller, T ; Castagne, R ; Oexle, K ; van Duijn, CM ; Iyengar, SK ; Mitchell, P ; Wang, JJ ; Hoehn, R ; Pfeiffer, N ; Bailey-Wilson, JE ; Stambolian, D ; Wong, T-Y ; Hammond, CJ ; Klaver, CCW (SPRINGER, 2012-09)
    Myopia is a complex genetic disorder and a common cause of visual impairment among working age adults. Genome-wide association studies have identified susceptibility loci on chromosomes 15q14 and 15q25 in Caucasian populations of European ancestry. Here, we present a confirmation and meta-analysis study in which we assessed whether these two loci are also associated with myopia in other populations. The study population comprised 31 cohorts from the Consortium of Refractive Error and Myopia (CREAM) representing 4 different continents with 55,177 individuals; 42,845 Caucasians and 12,332 Asians. We performed a meta-analysis of 14 single nucleotide polymorphisms (SNPs) on 15q14 and 5 SNPs on 15q25 using linear regression analysis with spherical equivalent as a quantitative outcome, adjusted for age and sex. We calculated the odds ratio (OR) of myopia versus hyperopia for carriers of the top-SNP alleles using a fixed effects meta-analysis. At locus 15q14, all SNPs were significantly replicated, with the lowest P value 3.87 × 10(-12) for SNP rs634990 in Caucasians, and 9.65 × 10(-4) for rs8032019 in Asians. The overall meta-analysis provided P value 9.20 × 10(-23) for the top SNP rs634990. The risk of myopia versus hyperopia was OR 1.88 (95 % CI 1.64, 2.16, P < 0.001) for homozygous carriers of the risk allele at the top SNP rs634990, and OR 1.33 (95 % CI 1.19, 1.49, P < 0.001) for heterozygous carriers. SNPs at locus 15q25 did not replicate significantly (P value 5.81 × 10(-2) for top SNP rs939661). We conclude that common variants at chromosome 15q14 influence susceptibility for myopia in Caucasian and Asian populations world-wide.
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    Genetic Loci for Retinal Arteriolar Microcirculation
    Sim, X ; Jensen, RA ; Ikram, MK ; Cotch, MF ; Li, X ; MacGregor, S ; Xie, J ; Smith, AV ; Boerwinkle, E ; Mitchell, P ; Klein, R ; Klein, BEK ; Glazer, NL ; Lumley, T ; McKnight, B ; Psaty, BM ; de Jong, PTVM ; Hofman, A ; Rivadeneira, F ; Uitterlinden, AG ; van Duijn, CM ; Aspelund, T ; Eiriksdottir, G ; Harris, TB ; Jonasson, F ; Launer, LJ ; Attia, J ; Baird, PN ; Harrap, S ; Holliday, EG ; Inouye, M ; Rochtchina, E ; Scott, RJ ; Viswanathan, A ; Li, G ; Smith, NL ; Wiggins, KL ; Kuo, JZ ; Taylor, KD ; Hewitt, AW ; Martin, NG ; Montgomery, GW ; Sun, C ; Young, TL ; Mackey, DA ; van Zuydam, NR ; Doney, ASF ; Palmer, CNA ; Morris, AD ; Rotter, JI ; Tai, ES ; Gudnason, V ; Vingerling, JR ; Siscovick, DS ; Wang, JJ ; Wong, TY ; Wallace, GR (PUBLIC LIBRARY SCIENCE, 2013-06-12)
    Narrow arterioles in the retina have been shown to predict hypertension as well as other vascular diseases, likely through an increase in the peripheral resistance of the microcirculatory flow. In this study, we performed a genome-wide association study in 18,722 unrelated individuals of European ancestry from the Cohorts for Heart and Aging Research in Genomic Epidemiology consortium and the Blue Mountain Eye Study, to identify genetic determinants associated with variations in retinal arteriolar caliber. Retinal vascular calibers were measured on digitized retinal photographs using a standardized protocol. One variant (rs2194025 on chromosome 5q14 near the myocyte enhancer factor 2C MEF2C gene) was associated with retinal arteriolar caliber in the meta-analysis of the discovery cohorts at genome-wide significance of P-value <5×10(-8). This variant was replicated in an additional 3,939 individuals of European ancestry from the Australian Twins Study and Multi-Ethnic Study of Atherosclerosis (rs2194025, P-value = 2.11×10(-12) in combined meta-analysis of discovery and replication cohorts). In independent studies of modest sample sizes, no significant association was found between this variant and clinical outcomes including coronary artery disease, stroke, myocardial infarction or hypertension. In conclusion, we found one novel loci which underlie genetic variation in microvasculature which may be relevant to vascular disease. The relevance of these findings to clinical outcomes remains to be determined.
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    Four Novel Loci (19q13, 6q24, 12q24, and 5q14) Influence the Microcirculation In Vivo
    Ikram, MK ; Xueling, S ; Jensen, RA ; Cotch, MF ; Hewitt, AW ; Ikram, MA ; Wang, JJ ; Klein, R ; Klein, BEK ; Breteler, MMB ; Cheung, N ; Liew, G ; Mitchell, P ; Uitterlinden, AG ; Rivadeneira, F ; Hofman, A ; de Jong, PTVM ; van Duijn, CM ; Kao, L ; Cheng, C-Y ; Smith, AV ; Glazer, NL ; Lumley, T ; McKnight, B ; Psaty, BM ; Jonasson, F ; Eiriksdottir, G ; Aspelund, T ; Harris, TB ; Launer, LJ ; Taylor, KD ; Li, X ; Iyengar, SK ; Xi, Q ; Sivakumaran, TA ; Mackey, DA ; MacGregor, S ; Martin, NG ; Young, TL ; Bis, JC ; Wiggins, KL ; Heckbert, SR ; Hammond, CJ ; Andrew, T ; Fahy, S ; Attia, J ; Holliday, EG ; Scott, RJ ; Islam, FMA ; Rotter, JI ; McAuley, AK ; Boerwinkle, E ; Tai, ES ; Gudnason, V ; Siscovick, DS ; Vingerling, JR ; Wong, TY ; McCarthy, MI (PUBLIC LIBRARY SCIENCE, 2010-10)
    There is increasing evidence that the microcirculation plays an important role in the pathogenesis of cardiovascular diseases. Changes in retinal vascular caliber reflect early microvascular disease and predict incident cardiovascular events. We performed a genome-wide association study to identify genetic variants associated with retinal vascular caliber. We analyzed data from four population-based discovery cohorts with 15,358 unrelated Caucasian individuals, who are members of the Cohort for Heart and Aging Research in Genomic Epidemiology (CHARGE) consortium, and replicated findings in four independent Caucasian cohorts (n  =  6,652). All participants had retinal photography and retinal arteriolar and venular caliber measured from computer software. In the discovery cohorts, 179 single nucleotide polymorphisms (SNP) spread across five loci were significantly associated (p<5.0×10(-8)) with retinal venular caliber, but none showed association with arteriolar caliber. Collectively, these five loci explain 1.0%-3.2% of the variation in retinal venular caliber. Four out of these five loci were confirmed in independent replication samples. In the combined analyses, the top SNPs at each locus were: rs2287921 (19q13; p  =  1.61×10(-25), within the RASIP1 locus), rs225717 (6q24; p = 1.25×10(-16), adjacent to the VTA1 and NMBR loci), rs10774625 (12q24; p  =  2.15×10(-13), in the region of ATXN2,SH2B3 and PTPN11 loci), and rs17421627 (5q14; p = 7.32×10(-16), adjacent to the MEF2C locus). In two independent samples, locus 12q24 was also associated with coronary heart disease and hypertension. Our population-based genome-wide association study demonstrates four novel loci associated with retinal venular caliber, an endophenotype of the microcirculation associated with clinical cardiovascular disease. These data provide further insights into the contribution and biological mechanisms of microcirculatory changes that underlie cardiovascular disease.
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    Mitochondrial Oxidative Phosphorylation Compensation May Preserve Vision in Patients with OPA1-Linked Autosomal Dominant Optic Atrophy
    Van Bergen, NJ ; Crowston, JG ; Kearns, LS ; Staffieri, SE ; Hewitt, AW ; Cohn, AC ; Mackey, DA ; Trounce, IA ; Santos, J (PUBLIC LIBRARY SCIENCE, 2011-06-22)
    Autosomal Dominant Optic Atrophy (ADOA) is the most common inherited optic atrophy where vision impairment results from specific loss of retinal ganglion cells of the optic nerve. Around 60% of ADOA cases are linked to mutations in the OPA1 gene. OPA1 is a fission-fusion protein involved in mitochondrial inner membrane remodelling. ADOA presents with marked variation in clinical phenotype and varying degrees of vision loss, even among siblings carrying identical mutations in OPA1. To determine whether the degree of vision loss is associated with the level of mitochondrial impairment, we examined mitochondrial function in lymphoblast cell lines obtained from six large Australian OPA1-linked ADOA pedigrees. Comparing patients with severe vision loss (visual acuity [VA]<6/36) and patients with relatively preserved vision (VA>6/9) a clear defect in mitochondrial ATP synthesis and reduced respiration rates were observed in patients with poor vision. In addition, oxidative phosphorylation (OXPHOS) enzymology in ADOA patients with normal vision revealed increased complex II+III activity and levels of complex IV protein. These data suggest that OPA1 deficiency impairs OXPHOS efficiency, but compensation through increases in the distal complexes of the respiratory chain may preserve mitochondrial ATP production in patients who maintain normal vision. Identification of genetic variants that enable this response may provide novel therapeutic insights into OXPHOS compensation for preventing vision loss in optic neuropathies.
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    Common Genetic Variants near the Brittle Cornea Syndrome Locus ZNF469 Influence the Blinding Disease Risk Factor Central Corneal Thickness
    Lu, Y ; Dimasi, DP ; Hysi, PG ; Hewitt, AW ; Burdon, KP ; Toh, T ; Ruddle, JB ; Li, YJ ; Mitchell, P ; Healey, PR ; Montgomery, GW ; Hansell, N ; Spector, TD ; Martin, NG ; Young, TL ; Hammond, CJ ; Macgregor, S ; Craig, JE ; Mackey, DA ; Gibson, G (PUBLIC LIBRARY SCIENCE, 2010-05)
    Central corneal thickness (CCT), one of the most highly heritable human traits (h(2) typically>0.9), is important for the diagnosis of glaucoma and a potential risk factor for glaucoma susceptibility. We conducted genome-wide association studies in five cohorts from Australia and the United Kingdom (total N = 5058). Three cohorts were based on individually genotyped twin collections, with the remaining two cohorts genotyped on pooled samples from singletons with extreme trait values. The pooled sample findings were validated by individual genotyping the pooled samples together with additional samples also within extreme quantiles. We describe methods for efficient combined analysis of the results from these different study designs. We have identified and replicated quantitative trait loci on chromosomes 13 and 16 for association with CCT. The locus on chromosome 13 (nearest gene FOXO1) had an overall meta-analysis p-value for all the individually genotyped samples of 4.6x10(-10). The locus on chromosome 16 was associated with CCT with p = 8.95x10(-11). The nearest gene to the associated chromosome 16 SNPs was ZNF469, a locus recently implicated in Brittle Cornea Syndrome (BCS), a very rare disorder characterized by abnormal thin corneas. Our findings suggest that in addition to rare variants in ZNF469 underlying CCT variation in BCS patients, more common variants near this gene may contribute to CCT variation in the general population.
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    Genome-wide association identifies ATOH7 as a major gene determining human optic disc size
    Macgregor, S ; Hewitt, AW ; Hysi, PG ; Ruddle, JB ; Medland, SE ; Henders, AK ; Gordon, SD ; Andrew, T ; McEvoy, B ; Sanfilippo, PG ; Carbonaro, F ; Tah, V ; Li, YJ ; Bennett, SL ; Craig, JE ; Montgomery, GW ; Tran-Viet, K-N ; Brown, NL ; Spector, TD ; Martin, NG ; Young, TL ; Hammond, CJ ; Mackey, DA (OXFORD UNIV PRESS, 2010-07-01)
    Optic nerve assessment is important for many blinding diseases, with cup-to-disc ratio (CDR) assessments commonly used in both diagnosis and progression monitoring of glaucoma patients. Optic disc, cup, rim area and CDR measurements all show substantial variation between human populations and high heritability estimates within populations. To identify loci underlying these quantitative traits, we performed a genome-wide association study in two Australian twin cohorts and identified rs3858145, P=6.2x10(-10), near the ATOH7 gene as associated with the mean disc area. ATOH7 is known from studies in model organisms to play a key role in retinal ganglion cell formation. The association with rs3858145 was replicated in a cohort of UK twins, with a meta-analysis of the combined data yielding P=3.4x10(-10). Imputation further increased the evidence for association for several SNPs in and around ATOH7 (P=1.3x10(-10) to 4.3x10(-11), top SNP rs1900004). The meta-analysis also provided suggestive evidence for association for the cup area at rs690037, P=1.5x10(-7), in the gene RFTN1. Direct sequencing of ATOH7 in 12 patients with optic nerve hypoplasia, one of the leading causes of blindness in children, revealed two novel non-synonymous mutations (Arg65Gly, Ala47Thr) which were not found in 90 unrelated controls (combined Fisher's exact P=0.0136). Furthermore, the Arg65Gly variant was found to have very low frequency (0.00066) in an additional set of 672 controls.