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Association analysis of exome variants and refraction, axial length, and corneal curvature in a European–American population

机译:欧美人口中全体变体和折射,轴向长度和角膜曲率的关联分析

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Abstract Refractive errors, myopia, and hyperopia are common visual disorders greatly affecting older individuals. Refraction is determined by genetic factors but only a small percentage of its variation has been explained. We performed a genetic association analysis with three ocular phenotypes: spherical equivalent (a continous measure of refraction), axial length, and corneal curvature in 1,871 European–Americans from the Beaver Dam Eye Study. Individuals were genotyped on the Illumina exome array and imputed to the Haplotype Reference Consortium reference panel. After increasing the number of analyzed variants in targeted protein‐coding regions 10‐fold via imputation, we confirmed associations for two previously known loci with corneal curvature (chr4q12, rs2114039; g.55092626T??C, β ?=??0.03 (95% confidence interval [CI]): ?0.06, ?0.01, P value?=?0.01) and spherical equivalent (chr15q14, rs634990; g.35006073T??C, β ?=??0.27, 95% CI: ?0.45, ?0.09, P value?=?3.79?×?10 ?3 ). Despite increased single nucleotide polymorphism (SNP) density, we did not detect any novel significant variants after correction for multiple comparisons. In summary, we confirmed two previous loci associated with corneal curvature and spherical equivalent in a European–American population highlighting the potential biological role of those regions in these traits.
机译:摘要屈光畸形,近视和远视是常见的视觉障碍,极大地影响了老年人。折射由遗传因子决定,但已经解释了其变异的小百分比。我们进行了具有三种眼部表型的遗传关联分析:球形当量(连续折射率),轴向长度和来自Beaver Dam眼睛研究的1,871名欧洲人的角膜曲率。个体在Illumina Exome阵列上进行基因分型,归功于单倍型参考联盟参考板。在通过归纳增加靶向蛋白质编码区10倍的分析变体的数量之后,我们确认了两种先前已知的基因率与角膜曲率(CHR4Q12,RS2114039; G.55092626T的关联。&β?= ?? 0.03 (95%置信区间[CI]):?0.06,?0.01,p值?=?0.01)和球形等同物(CHR15Q14,RS634990; G.5006073T?β-C,β= ?? 0.27,95%CI :?0.45,?0.09,P值?=?3.79?×10?3)。尽管单核苷酸多态性(SNP)密度增加,但我们在校正后没有检测到多种比较后的任何新的显着变体。总之,我们确认了与角膜曲率和球形等同于欧美人口的球形等同物相关的两个基因座,突出这些地区在这些特征中的潜在生物学作用。

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