中国人群中肌纤蛋白(MYOC)基因多态性与高度近视的连锁及关联研究
Linkage and association of myocilin (MYOC) polymorphisms with high myopia in a Chinese population.
作者信息
Tang Wing Chun, Yip Shea Ping, Lo Ka Kin, Ng Po Wah, Choi Pik Shan, Lee Sau Yin, Yap Maurice K H
机构信息
School of Optometry, The Hong Kong Polytechnic University, Hung Hom, Kowloon, Hong Kong SAR, China.
出版信息
Mol Vis. 2007 Apr 4;13:534-44.
PURPOSE
To test the association between myocilin gene (MYOC) polymorphisms and high myopia in Hong Kong Chinese by using family-based association study.
METHODS
A total of 162 Chinese nuclear families, consisting of 557 members, were recruited from an optometry clinic. Each family had two parents and at least one offspring with high myopia (defined as -6.00D or less for both eyes). All offspring were healthy with no clinical evidence of syndromic disease and other ocular abnormality. Genotyping was performed for two MYOC microsatellites (NGA17 and NGA19) and five tag single nucleotide polymorphisms (SNPs) spreading across the gene. The genotype data were analyzed with Family-Based Association Test (FBAT) software to check linkage and association between the genetic markers and myopia, and with GenAssoc to generate case and pseudocontrol subjects for investigating main effects of genetic markers and calculating the genotype relative risks (GRR).
RESULTS
FBAT analysis showed linkage and association with high myopia for two microsatellites and two SNPs under one to three genetic models after correction for multiple comparisons by false discovery rate. NGA17 at the promoter was significant under an additive model (p=0.0084), while NGA19 at the 3' flanking region showed significant results under both additive (p=0.0172) and dominant (p=0.0053) models. SNP rs2421853 (C>T) exhibited both linkage and association under additive (p=0.0009) and dominant/recessive (p=0.0041) models. SNP rs235858 (T>C) was also significant under additive (p=4.0E-6) and dominant/recessive (p=2.5E-5) models. Both SNPs were downstream of NGA19 at the 3' flanking region. Positive results for these SNPs were novel findings. A stepwise conditional logistic regression analysis of the case-pseudocontrol dataset generated by GenAssoc from the families showed that both SNPs could separately account for the association of NGA17 or NGA19, and that both SNPs contributed separate main effects to high myopia. For rs2421853 and with C/C as the reference genotype, the GRR increased from 1.678 for G/A to 2.738 for A/A (p=9.0E-4, global Wald test). For rs235858 and with G/G as the reference, the GRR increased 2.083 for G/A to 3.931 for A/A (p=2.0E-2, global Wald test). GRR estimates thus suggested an additive model for both SNPs, which was consistent with the finding that, of the three models tested, the additive model gave the lowest p values in FBAT analysis.
CONCLUSIONS
Linkage and association was shown between the MYOC polymorphisms and high myopia in our family-based association study. The SNP rs235858 at the 3' flanking region showed the highest degree of confidence for association.
目的
通过基于家系的关联研究,检测香港华人中肌纤蛋白基因(MYOC)多态性与高度近视之间的关联。
方法
从一家验光诊所招募了总共162个中国核心家庭,共557名成员。每个家庭有两名父母和至少一名患有高度近视的后代(定义为双眼近视度数≤-6.00D)。所有后代均健康,无综合征性疾病及其他眼部异常的临床证据。对两个MYOC微卫星(NGA17和NGA19)以及分布于该基因的五个标签单核苷酸多态性(SNP)进行基因分型。使用基于家系的关联检验(FBAT)软件分析基因型数据,以检查遗传标记与近视之间的连锁和关联,并使用GenAssoc生成病例和假对照个体,以研究遗传标记的主要效应并计算基因型相对风险(GRR)。
结果
在通过错误发现率进行多重比较校正后,FBAT分析显示,在一至三种遗传模型下,两个微卫星和两个SNP与高度近视存在连锁和关联。启动子处的NGA17在加性模型下具有显著性(p = 0.0084),而3'侧翼区域的NGA19在加性(p = 0.0172)和显性(p = 0.0053)模型下均显示出显著结果。SNP rs2421853(C>T)在加性(p = 0.0009)和显性/隐性(p = 0.0041)模型下均表现出连锁和关联。SNP rs235858(T>C)在加性(p = 4.0E-6)和显性/隐性(p = 2.5E-5)模型下也具有显著性。这两个SNP均位于3'侧翼区域NGA19的下游。这些SNP的阳性结果是新发现。对GenAssoc从这些家庭生成的病例-假对照数据集进行的逐步条件逻辑回归分析表明,这两个SNP均可分别解释NGA17或NGA19的关联,且这两个SNP对高度近视均有独立的主要效应。对于rs2421853,以C/C作为参考基因型,GRR从G/A的1.678增加到A/A的2.738(p = 9.0E-4,全局Wald检验)。对于rs235858,以G/G作为参考,GRR从G/A的2.083增加到A/A的3.931(p = 2.0E-2,全局Wald检验)。GRR估计表明这两个SNP均呈现加性模型,这与在FBAT分析中测试的三种模型中加性模型给出最低p值的发现一致。
结论
在我们基于家系的关联研究中,显示出MYOC多态性与高度近视之间存在连锁和关联。3'侧翼区域的SNP rs235858显示出最高的关联可信度。
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