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Joint Effect of CFH and ARMS2/HTRA1 Polymorphisms on Neovascular Age-Related Macular Degeneration in Chinese Population

机译:CFH和ARMS2 / HTRA1多态性对中国人群新血管性年龄黄斑变性的联合作用

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摘要

Purpose. The etiology of neovascular age-related macular degeneration (nAMD) cannot be completely explained by identified environmental risk factors or single-locus gene variants. This study was to explore the potential interactions among gene variants on nAMD in Chinese population. Methods. 43 SNPs located in different genes were genotyped in 932 Chinese individuals (464 nAMD patients and 468 controls). We explored the potential interactions among gene variants using generalized multifactor dimensionality reduction (GMDR) algorithm and the method to measure the departure from the additivity model. Results. The joint effect that involved CFH rs1061170 and HTRA1 rs3793917 was shown statistically significant (P < 0.001) with the highest cross-validation consistency (10/10) and the best testing balanced accuracy (64.50%). In addition, based on the method to measure the departure from the additivity model, the synergy index (S) was 2.63 (1.09–6.38) and the attributable proportion due to interaction (AP) was 55.7% (21.4%–89.9%), which suggested that a common pathway may exist for these genes for nAMD. Those who carried CC for rs3793917 and TC/CC for rs1061170 were at the highest risk of nAMD (OR: 9.76, 95% CI: 4.65–20.51). Conclusions. Evidence that the joint effect that involved CFH and ARMS2/HTRA1 may contribute to the risk of neovascular AMD in Chinese population was obtained.
机译:目的。新血管性年龄相关性黄斑变性(nAMD)的病因不能完全通过已确定的环境危险因素或单基因座基因变异来解释。本研究旨在探讨中国人群nAMD基因变异之间的潜在相互作用。方法。对932名中国人(464名nAMD患者和468名对照)中位于不同基因的43个SNP进行了基因分型。我们使用广义多因素降维(GMDR)算法和测量与可加性模型的偏离的方法探索了基因变异之间的潜在相互作用。结果。涉及CFH rs1061170和HTRA1 rs3793917的联合效应具有统计学显着性(P <0.001),具有最高的交叉验证一致性(10/10)和最佳的测试平衡准确性(64.50%)。此外,根据衡量与可加性模型偏离的方法,协同指数(S)为2.63(1.09–6.38),归因于交互作用的比例(AP)为55.7%(21.4%–89.9%),这表明nAMD的这些基因可能存在一个共同的途径。那些携带rs3793917的CC和rs1061170的TC / CC的患nAMD的风险最高(或:9.76,95%CI:4.65–20.51)。结论。获得的证据表明,涉及CFH和ARMS2 / HTRA1的联合效应可能导致中国人群发生新血管性AMD的风险。

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