补体因子H基因中的编码变体I62V与息肉状脉络膜血管病变密切相关。
Coding variant I62V in the complement factor H gene is strongly associated with polypoidal choroidal vasculopathy.
作者信息
Kondo Naoshi, Honda Shigeru, Kuno Shin-ichi, Negi Akira
机构信息
Department of Surgery, Division of Ophthalmology, Kobe University Graduate School of Medicine, Kobe, Japan.
出版信息
Ophthalmology. 2009 Feb;116(2):304-10. doi: 10.1016/j.ophtha.2008.11.011.
PURPOSE
To investigate whether variants in the complement factor H (CFH) gene are associated with polypoidal choroidal vasculopathy (PCV).
DESIGN
Cross-sectional study.
PARTICIPANTS
A case-control group of 130 PCV subjects and 173 unrelated controls.
METHODS
We conducted an association analysis between CFH variants and PCV in a Japanese population, genotyping 12 tag single nucleotide polymorphisms (SNPs)-including rs3753394, rs800292 (I62V), and rs1061170 (Y402H)-that are highly representative of the common genetic variation in the CFH region. Genotyping was performed using TaqMan technology.
MAIN OUTCOME MEASURES
Allele and haplotype frequencies of the CFH variants.
RESULTS
A highly significant association with PCV was observed across the CFH region. The strongest association was observed at I62V (P = 1.7 x 10(-7)). Six other SNPs (rs3753394, rs6680396, rs1410996, rs2284664, rs1329428, and rs1065489) also showed significant association (10(-3) < P < 10(-6)). These associations became nonsignificant after accounting for rs800292 in a conditional logistic regression analysis. A significant omnibus haplotype association was detected in the entire CFH region (omnibus P = 1.6 x 10(-5) at 7 degrees of freedom). Conditional haplotype-based likelihood ratio tests revealed that the significant omnibus haplotype association disappeared when it was estimated conditional on I62V (omnibus P = 0.20, 6 degrees of freedom, post-I62V dependency), whereas the omnibus haplotype association remained significant when it was estimated conditional on any SNP other than I62V. These findings indicate that multiple observed effects were caused by linkage disequilibrium with I62V, and that this variant fully accounts for the association signals observed at the set of SNPs examined at this locus.
CONCLUSIONS
The present study provides evidence that the complement pathway plays a substantial role in the pathogenesis of PCV. The nonsynonymous variant I62V is a plausible candidate for a causal polymorphism leading to the development of PCV, given its potential for functional consequences on the CFH protein and our own statistical evidence.
FINANCIAL DISCLOSURE(S): The authors have to proprietary or commercial interest in any materials discussed in this article.
目的
研究补体因子H(CFH)基因变异是否与息肉状脉络膜血管病变(PCV)相关。
设计
横断面研究。
参与者
130例PCV患者和173例无关对照组成的病例对照研究组。
方法
我们在日本人群中对CFH变异与PCV进行关联分析,对12个标签单核苷酸多态性(SNP)进行基因分型,包括rs3753394、rs800292(I62V)和rs1061170(Y402H),这些SNP高度代表CFH区域的常见遗传变异。使用TaqMan技术进行基因分型。
主要观察指标
CFH变异的等位基因和单倍型频率。
结果
在整个CFH区域观察到与PCV有高度显著的关联。在I62V处观察到最强的关联(P = 1.7×10⁻⁷)。其他6个SNP(rs3753394、rs6680396、rs1410996、rs2284664、rs1329428和rs1065489)也显示出显著关联(10⁻³ < P < 10⁻⁶)。在条件逻辑回归分析中考虑rs800292后,这些关联变得不显著。在整个CFH区域检测到显著的总体单倍型关联(自由度为7时,总体P = 1.6×10⁻⁵)。基于条件单倍型的似然比检验显示,当以I62V为条件估计时,显著的总体单倍型关联消失(总体P = 0.20,自由度为6,I62V后依赖性),而当以I62V以外的任何SNP为条件估计时,总体单倍型关联仍然显著。这些发现表明,多个观察到的效应是由与I62V的连锁不平衡引起的,并且该变异完全解释了在该位点检测的一组SNP处观察到的关联信号。
结论
本研究提供了证据表明补体途径在PCV的发病机制中起重要作用。非同义变异I62V是导致PCV发生的因果多态性的一个合理候选者,鉴于其对CFH蛋白的潜在功能影响以及我们自己的统计证据。
财务披露
作者对本文讨论的任何材料均无专有或商业利益。
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