Sun Cong, Tikellis Gabriella, Liew Gerald, Klein Ronald, Larsen Emily K Marino, Wong Tien Y
Centre for Eye Research Australia, University of Melbourne, VIC, Australia.
Mol Vis. 2007 Nov 12;13:2105-11.
To examine the association between apolipoprotein E (APOE) gene polymorphism and retinal microvascular signs in an older population.
Retinal photographs were taken of 2,152 participants (1,831 whites, and 321 African-Americans), aged 69-96 years, who were participating in a population-based study of four United States communities. We used standardized protocols to assess photographs for the presence of retinal microvascular signs (retinopathy, arterio-venous nicking, and focal arteriolar narrowing) and a computer-assisted method to measure retinal vessel diameters. We analyzed DNA extracted from blood samples of participants for common allelic variants of the APOE gene.
After adjusting for age, gender, systolic blood pressure, smoking, total serum cholesterol, and other risk factors, we found white participants carrying the epsilon2 and epsilon4 alleles were more likely to have arterio-venous nicking than the epsilon3/epsilon3 homozygotes, with odds ratio (OR) of 1.70 and confidence interval (CI) 95% (1.03-2.83) for the epsilon2 carriers and OR 1.74 (95% CI 1.06-2.84) for the epsilon4 carriers. Among white participants without hypertension, the associations remained significant for the epsilon4 carriers (OR 2.32, 95% CI 1.18-4.57). Whites, normotensive carriers of the epsilon2 allele had significantly narrower retinal arteriolar diameters (adjusted mean arteriolar diameter of 163.5 mum, 95% CI 160.1-167.0, p=0.03) compared to the epsilon3/epsilon3 homozygotes (167.8 mum, 95% CI 166.0-169.6). APOE gene polymorphism was not associated with retinopathy, focal narrowing, or retinal venular diameters in white participants. There were insufficient numbers of African-Americans for separate multivariate analysis.
This study provides little evidence that the APOE gene polymorphism plays a significant role in the pathogenesis of retinal microvascular changes in the general population. In the older white population, APOE epsilon2 and epsilon4 allele carriers were more likely to have arterio-venous nicking. Other retinal signs, however, were not related to APOE gene polymorphism.
研究老年人群中载脂蛋白E(APOE)基因多态性与视网膜微血管体征之间的关联。
对参加美国四个社区基于人群研究的2152名参与者(1831名白人,321名非裔美国人)进行视网膜拍照,这些参与者年龄在69 - 96岁。我们使用标准化方案评估照片中视网膜微血管体征(视网膜病变、动静脉交叉征和局灶性小动脉狭窄)的存在情况,并采用计算机辅助方法测量视网膜血管直径。我们分析了从参与者血液样本中提取的DNA,以检测APOE基因的常见等位基因变异。
在对年龄、性别、收缩压、吸烟、总血清胆固醇和其他危险因素进行校正后,我们发现携带ε2和ε4等位基因的白人参与者比ε3/ε3纯合子更易出现动静脉交叉征,ε2携带者的比值比(OR)为1.70,95%置信区间(CI)为(1.03 - 2.83),ε4携带者的OR为1.74(95% CI 1.06 - 2.84)。在无高血压的白人参与者中,ε4携带者的这种关联仍然显著(OR 2.32,95% CI 1.18 - 4.57)。与ε3/ε3纯合子(167.8μm,95% CI 166.0 - 169.6)相比,携带ε2等位基因的血压正常的白人视网膜小动脉直径显著更窄(调整后的平均小动脉直径为163.5μm,95% CI 160.1 - 167.0,p = 0.03)。APOE基因多态性与白人参与者的视网膜病变、局灶性狭窄或视网膜静脉直径无关。非裔美国人数量不足,无法进行单独的多变量分析。
本研究几乎没有证据表明APOE基因多态性在一般人群视网膜微血管变化的发病机制中起重要作用。在老年白人人群中,APOE ε2和ε4等位基因携带者更易出现动静脉交叉征。然而,其他视网膜体征与APOE基因多态性无关。
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