血清维生素 D 与维生素 D 通路中遗传变异与欧洲眼部研究中的年龄相关性黄斑变性的关系。
Associations between Serum Vitamin D and Genetic Variants in Vitamin D Pathways and Age-Related Macular Degeneration in the European Eye Study.
机构信息
Centre for Public Health, Queen's University Belfast, Belfast, United Kingdom.
School of Environmental Sciences, University of East Anglia, Norwich, United Kingdom.
出版信息
Ophthalmology. 2017 Jan;124(1):90-96. doi: 10.1016/j.ophtha.2016.09.007. Epub 2016 Oct 28.
PURPOSE
To study associations between early and late age-related macular degeneration (AMD) and neovascular AMD (nvAMD) with serum 25-hydroxy vitamin D (25(OH)D) and genetic variants in vitamin D pathway genes.
DESIGN
Population-based, cross-sectional study in a random sample aged 65 years or older from 7 European countries.
PARTICIPANTS
Of 4753 participants, 4496 (2028 men and 2468 women), with a mean age of 73 years, provided a blood sample; 2137 had no signs of AMD, 2209 had early AMD, and 150 had late AMD, of whom 104 had nvAMD.
METHODS
Participants were interviewed to determine smoking and alcohol use, sunlight exposure, and diet; underwent fundus photography. Fundus images were graded using the International Classification System for Age-Related Maculopathy. The 25(OH)D was measured by liquid chromatography-tandem mass spectrometry and categorized as deficient (<30 nmol/l), insufficient (30-50 nmol/l), or adequate (≥50 nmol/l). Genotyping was performed on a subsample of 1284 AMD cases and controls for 93 single nucleotide polymorphisms (SNPs) from 7 genes. Associations were investigated by linear or logistic regression adjusted for potential confounders.
MAIN OUTCOME MEASURES
Adjusted odds ratio (OR) for 3 outcomes (early AMD, late AMD, nvAMD).
RESULTS
No linear association was found with 25(OH)D and early or late AMD or nvAMD. There was no association between insufficient or deficient status with early or late AMD. Deficient status was associated with nvAMD (adjusted OR, 1.27; 95% confidence interval, 1.1-1.45; P < 0.0001). Significant (P < 0.05) associations with 25(OH)D were found for SNPs in genes GC, VDR, CYP2R1, and CYP27B1. Two SNPs (VDR) were associated with early AMD, 4 SNPs (RXRA) and 1 SNP (VDR) were associated with nvAMD, and 1 SNP (RXRA), 2 SNPs (VDR), and 1 SNP (CYP2R1) were associated with late AMD. After Bonferroni correction, no SNPs were associated with early AMD, late AMD, or nvAMD.
CONCLUSIONS
Deficiency in 25(OH)D was associated with nvAMD, but the adjusted OR was small, and we cannot exclude residual confounding. The hypothesis of a causal association of vitamin D with AMD is not supported by clear evidence for an association of vitamin D SNPs with early AMD, late AMD, or nvAMD.
目的
研究血清 25-羟维生素 D(25(OH)D)和维生素 D 途径基因中的遗传变异与年龄相关性黄斑变性(AMD)和新生血管性 AMD(nvAMD)的早发和晚发年龄之间的相关性。
设计
这是一项在 7 个欧洲国家的随机抽样中,针对 65 岁及以上人群进行的基于人群的横断面研究。
参与者
在 4753 名参与者中,有 4496 名(2028 名男性和 2468 名女性),平均年龄为 73 岁,提供了血液样本;2137 名无 AMD 迹象,2209 名有早期 AMD,150 名有晚期 AMD,其中 104 名有 nvAMD。
方法
对参与者进行访谈,以确定吸烟和饮酒、阳光暴露和饮食情况;进行眼底摄影。使用国际年龄相关性黄斑变性分类系统对眼底图像进行分级。通过液相色谱-串联质谱法测量 25(OH)D,并分为缺乏(<30 nmol/L)、不足(30-50 nmol/L)和充足(≥50 nmol/L)。对 1284 名 AMD 病例和对照组的 1284 名 AMD 病例和对照组进行了 1284 名 AMD 病例和对照组的基因分型,用于来自 7 个基因的 93 个单核苷酸多态性(SNP)。通过线性或逻辑回归调整潜在混杂因素后,研究了与 3 个结局(早期 AMD、晚期 AMD 和 nvAMD)相关的调整后比值比(OR)。
主要结果
与早期或晚期 AMD 或 nvAMD 无线性关联。早期或晚期 AMD 与不足或缺乏状态无关。缺乏状态与 nvAMD 相关(调整后的 OR,1.27;95%置信区间,1.1-1.45;P<0.0001)。在 GC、VDR、CYP2R1 和 CYP27B1 基因中的 SNP 与 25(OH)D 之间存在显著(P<0.05)的关联。2 个 SNP(VDR)与早期 AMD 相关,4 个 SNP(RXRA)和 1 个 SNP(VDR)与 nvAMD 相关,1 个 SNP(RXRA)、2 个 SNP(VDR)和 1 个 SNP(CYP2R1)与晚期 AMD 相关。经 Bonferroni 校正后,没有 SNP 与早期 AMD、晚期 AMD 或 nvAMD 相关。
结论
25(OH)D 缺乏与 nvAMD 相关,但调整后的 OR 较小,我们不能排除残余混杂。维生素 D 与 AMD 之间因果关系的假设没有明确证据支持维生素 D SNP 与早期 AMD、晚期 AMD 或 nvAMD 之间的关联。
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