Genetic Variants in the Vitamin D Pathway, 25(OH)D Levels, and Mortality in a Large Population-Based Cohort Study

J. Ordóñez-Mena, H. Maalmi, B. Schöttker, K. Saum, B. Holleczek, Thomas J. Wang, B. Burwinkel, H. Brenner
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引用次数: 12

Abstract

Context: Low 25-hydroxyvitamin D [25(OH)D] concentrations have been consistently associated with excess mortality in epidemiological studies, but this association could be due to confounding by health impairments associated with low 25(OH)D levels. An association of vitamin D–related genetic variants with all-cause mortality could strengthen the claims of causality, because this association is assumed to be unaffected by confounding. Objective: To assess the associations of low 25(OH)D with mortality in the presence or absence of genetic variants in the vitamin D pathway. Design, Setting, and Participants: The study consisted of a population-based cohort of 8417 German older adults in whom genetic variants were genotyped. Main Outcome Measures: The primary outcome measure was all-cause mortality. Results: Two single nucleotide polymorphisms (SNPs), rs3755967 (GC) and rs11603330 (DHCR7), were associated with higher risk of low vitamin D status [odds ratio (95% confidence interval) per minor allele, 1.27 (1.18 to 1.36) and 1.16 (1.08 to 1.25), respectively]. Low 25(OH)D (less than the season-specific 33rd percentile) was associated with increased mortality. However, none of the SNPs was associated with increased mortality. Furthermore, the increase in mortality for those with low 25(OH)D was generally smaller in the presence of the risk alleles for low 25(OH)D [“genetically low 25(OH)D”] than in the absence of those risk alleles [“otherwise low 25(OH)D”]. Conclusions: Although we may have been limited by a low statistical power to detect small associations, our study showed that the strong relationship between low 25(OH)D and increased mortality may be at least partly due to other factors related to low 25(OH)D levels.
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一项大型人群队列研究中维生素D途径、25(OH)D水平和死亡率的遗传变异
背景:在流行病学研究中,低25-羟基维生素D [25(OH)D]浓度一直与高死亡率相关,但这种关联可能是由于与低25(OH)D水平相关的健康损害混淆所致。维生素d相关基因变异与全因死亡率的关联可能会加强因果关系的主张,因为这种关联被认为不受混淆的影响。目的:评估在维生素D途径中存在或不存在遗传变异的情况下,低25(OH)D与死亡率的关系。设计、环境和参与者:该研究包括一个以人群为基础的队列,包括8417名德国老年人,他们的遗传变异被基因分型。主要结局指标:主要结局指标为全因死亡率。结果:两个单核苷酸多态性(SNPs) rs3755967 (GC)和rs11603330 (DHCR7)与维生素D低状态的高风险相关[每个小等位基因的优势比(95%置信区间)分别为1.27(1.18至1.36)和1.16(1.08至1.25)]。低25(OH)D(低于特定季节的第33百分位数)与死亡率增加有关。然而,没有一个snp与死亡率增加有关。此外,低25(OH)D风险等位基因(“基因上低25(OH)D”)存在时,低25(OH)D死亡率的增加通常小于不存在这些风险等位基因(“其他方面低25(OH)D”)的人。结论:虽然我们可能受到检测小关联的低统计能力的限制,但我们的研究表明,低25(OH)D与死亡率增加之间的密切关系可能至少部分归因于与低25(OH)D水平相关的其他因素。
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