Common variants on chromosome 2 and risk of primary open-angle glaucoma in the Afro-Caribbean population of Barbados

Jiao, Xiaodong; Yang, Zhenglin; Yang, Xian; Chen, Yuhong; Tong, Zongzhong; Zhao, Chao; Zeng, Junjie; Chen, Haoyu; Gibbs, Daniel; Sun, Xufang; Li, Bei; Wakins, W. Scott; Meyer, Cynthia; Wang, Xiaolei; Kasuga, Daniel; Bedell, Matthew; Pearson, Erik; Weinreb, Robert N.; Leske, M. Cristina; Hennis, Anselm; DeWan, Andrew T.; Nemesure, Barbara; Jorde, Lynn B.; Hoh, Josephine; Hejtmancik, J. Fielding; Zhang, Kang

doi:10.1073/pnas.0907564106

Cited by 38 publications

(44 citation statements)

References 31 publications

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“…There was no significant association of either of these two SNPs with HTG and NTG in the present cohort (Tables 1 and 2), and this locus was not associated with POAG in the Japanese population. These two SNPs are common variants in the Japanese population as well as in the Afro-Caribbean population, and the present results indicate that these two SNPs are markers of a neighboring susceptible gene polymorphism responsible for POAG in the Afro-Caribbean population, although Jiao et al (1) reported that they may perform a regulatory role influencing the neighboring gene expression and that, alternatively, one cannot exclude the possibility that they are located within a yet-to-beannotated gene. A variety of genetic factors would contribute to optic neuropathy in POAG.…”

contrasting

confidence: 51%

“…Primary open-angle glaucoma (POAG) is the most common form of glaucoma, and it is clinically classified into high-tension glaucoma (HTG), in which an elevated intraocular pressure (IOP) is a major feature, and normal-tension glaucoma (NTG), in which the IOPs are consistently within the statistically normal population range. Jiao et al (1) performed linkage analyses in 146 multiplex families and identified a locus with a major impact on the susceptibility to POAG in the Afro-Caribbean population in Barbados, West Indies. They demonstrated a strong association of rs12994401 and rs1533428 on chromosomes 2p with POAG, according to the findings of subsequent case-control analyses.…”

mentioning

confidence: 99%

“…It is presumed that non-IOP-related genetic factors would predominate in patients with NTG and that, conversely, high IOP-related genetic factors would predominate in patients with HTG. Although it is not yet clear how this locus might act in the Afro-Caribbean population, it is thought that it contributes to optic neuropathy as a high IOPrelated genetic factor, because the mean IOP (26.7 mm Hg) of affected individuals is higher than that (17.0 mm Hg) of unaffected individuals ascertained from the family study (1). A direct comparison of the epidemiologic data between different ethnic populations may be difficult, because the diagnostic criteria are not always the same among the epidemiologic studies of glaucoma.…”

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confidence: 99%

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Lack of association of common variants on chromosome 2p with primary open-angle glaucoma in the Japanese population

Mabuchi¹,

Sakurada²,

Kashiwagi³

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

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confidence: 51%

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confidence: 99%

mentioning

confidence: 99%

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Lack of association of common variants on chromosome 2p with primary open-angle glaucoma in the Japanese population

Mabuchi¹,

Sakurada²,

Kashiwagi³

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

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“…We observed no linkage disequilibrium (LD) between the three SNPs in either population based on r 2 (r 2 < 0.35 for all SNP pairs in the respective cases and controls). Although we identified a modest association with POAG risk in the African-American population, risk was conferred by the C allele at rs12994401 rather than the T allele as reported by Jiao et al (1). T allele frequencies in our African-American controls and the Barbados controls were nearly identical.…”

supporting

confidence: 67%

Association between chromosome 2p16.3 variants and glaucoma in populations of African descent

Liu

Qin

Schmidt

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

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Jiao et al. (1) recently reported significant association of three SNPs on chromosome 2p16.3 (rs12994401, rs10202118, and rs1533428) with an increased risk of primary open-angle glaucoma (POAG) in the Barbados population. In an effort to replicate these findings, we genotyped these three SNPs in our African-American and Ghanaian (West African) datasets. The research was reviewed and approved by the Institutional Review Board of Duke University Medical Center and for Ghanaian subjects, by the Noguchi Memorial Institute of Medical Research of the College of Health Sciences at the University of Ghana.The African-American dataset included 382 cases and 275 controls, and the Ghanaian dataset contained 170 cases and 132 controls as previously described (2).Genotyping of blood DNA was performed with TaqMan allelic discrimination assays according to the standard protocols (Applied Biosystems). We required 95% genotyping efficiency and matching genotypes of quality-control samples within and across all plates to include samples in the statistical analysis. Within each population, genotype frequencies of cases and controls were compared by logistic regression with adjustment for gender using SAS software (SAS Institute).All markers were in Hardy-Weinberg equilibrium (P > 0.05) in cases and controls from both populations. Only rs12994401 was significantly associated with an increased risk of POAG in the African-American population (P = 0.003) ( Table 1). We observed no linkage disequilibrium (LD) between the three SNPs in either population based on r 2 (r 2 < 0.35 for all SNP pairs in the respective cases and controls). Although we identified a modest association with POAG risk in the African-American population, risk was conferred by the C allele at rs12994401 rather than the T allele as reported by Jiao et al. (1). T allele frequencies in our African-American controls and the Barbados controls were nearly identical. Thus, this discrepancy may be attributed to population differences in the POAG cases. The Barbados population is believed to be fairly homogenous with only 10% European admixture (3), whereas African Americans have ∼21% European admixture (4). Lack of LD between rs12994401 and rs1533428 in our datasets strongly contrasts with a D′ value of 0.72 between these SNPs in the Barbados population. The lack of an observed association in the Ghanaian population may be because of population differences or reduced statistical power, because this smaller dataset had only 42% power (at 5% significance level) to detect an odds ratio of 0.5 for a minor allele frequency of 6%. In summary, we identified a significant association between SNP rs12994401 and POAG in the North Carolina African-American population with a different risk allele than reported for Barbados. As previously discussed (5), this suggests that the as yet unidentified causal variant in this region of chromosome 2 has different levels of LD with the genotyped SNP in these distinct populations of African descent. More studies will be necessary to identify the ...

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“…There is a correlation between IOP and the likelihood of development of glaucoma and its progression (Boland and Quigley, 2007). Other risk factors are age (Tschumper and Johnson, 1990); family history, ethnicity or genetic variation (Jiao et al, 2009;Rao et al, 2011); other ocular or systemic disease, such as myopia, uveitis, decreased corneal or choroidal thickness, thyroid abnormality, sleep apnea, migraine (Boland and Quigley, 2007;Foster et al, 2002); vacular factors (Yanagi et al, 2011) and others. Age plays an important role in the development of glaucoma.…”

Section: Causes Of Glaucomamentioning

confidence: 99%

Mechanism of Aqueous Humor Secretion, Its Regulation and Relevance to Glaucoma

Shahidullah¹,

Almalki²,

Delamere³

2011

Glaucoma - Basic and Clinical Concepts

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Common variants on chromosome 2 and risk of primary open-angle glaucoma in the Afro-Caribbean population of Barbados

Cited by 38 publications

References 31 publications

Lack of association of common variants on chromosome 2p with primary open-angle glaucoma in the Japanese population

Lack of association of common variants on chromosome 2p with primary open-angle glaucoma in the Japanese population

Association between chromosome 2p16.3 variants and glaucoma in populations of African descent

Mechanism of Aqueous Humor Secretion, Its Regulation and Relevance to Glaucoma

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