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首页> 外文期刊>BMC Rheumatology >Vitamin D in individuals before onset of rheumatoid arthritis - relation to vitamin D binding protein and its associated genetic variants
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Vitamin D in individuals before onset of rheumatoid arthritis - relation to vitamin D binding protein and its associated genetic variants

机译:类风湿关节炎发作前个体中的维生素D-与维生素D结合蛋白及其相关遗传变异的关系

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摘要

Vitamin D has been implicated as being involved in the aetio-pathogenesis of several autoimmune diseases including rheumatoid arthritis (RA). Previous studies present contradictory results. Vitamin D binding protein (DBP), the major transport protein, is also involved in various inflammatory processes. The aim of this study was to investigate the relationship between circulating levels of 25-hydroxyvitamin D [25(OH) D], DBP and polymorphisms in group-specific component (GC) in pre-symptomatic individuals and matched controls within prospective cohorts of the Northern Sweden. Blood samples donated to the Medical Biobank prior to the onset of symptoms of RA (n = 515, mean [SD] time before the onset of symptoms 6.2 [9.3] years) and from matched (2:1) population-based controls (n = 267) were used. Plasma 25(OH) vitamin D levels were analyzed using liquid chromatography tandem-mass spectrometry and DBP levels were analyzed using enzyme-linked immunosorbent assay. GC polymorphisms (rs4588 and rs7041) were analyzed with TaqMan assays (Applied Biosystems). Levels of 25(OH) D or DBP were not statistically different between pre-symptomatic individuals and controls in a crude, or a multiple-adjusted logistic regression model. However, an increased risk for future RA was found in females of DBP (OR 1.014 [95%CI 1.001–1.028]) per 10 mg/L adjusted for carriage of the minor allele of rs4588, in a multiple-adjusted model (p  0.05). This study indicated that vitamin D is not associated with the future risk of RA although increasing levels of DBP were however, associated with an increased risk of disease in females carrying the minor allele of a DBP encoding SNP.
机译:维生素D被认为与包括风湿性关节炎(RA)在内的几种自身免疫疾病的发病机理有关。先前的研究提出了矛盾的结果。维生素D结合蛋白(DBP)是主要的转运蛋白,也参与各种炎症过程。这项研究的目的是调查有症状的前瞻性人群中的25-羟基维生素D [25(OH)D],DBP的循环水平与组特异性成分(GC)多态性之间的关系,以及该人群预期队列中的匹配对照。瑞典北部。在RA症状发作之前将血液样本捐赠给Medical Biobank(n = 515,在症状发作6.2 [9.3]年之前的平均[SD]时间),并从匹配的(2:1)人群中进行对照(n = 267)。使用液相色谱串联质谱法分析血浆25(OH)维生素D水平,并使用酶联免疫吸附法分析DBP水平。使用TaqMan分析(Applied Biosystems)分析了GC多态性(rs4588和rs7041)。有症状的个体与对照组之间的25(OH)D或DBP的水平在统计学上无差异,或者是经过多因素调整的logistic回归模型。然而,在多校正模型中,每10 mg / L DBP雌性(OR 1.014 [95%CI 1.001–1.028])每10 mg / L因携带rs4588的次要等位基因而进行了校正(p RA < 0.05)。这项研究表明,维生素D与RA的未来风险无关,尽管DBP的水平升高与携带编码SNP的DBP的次要等位基因的女性患病的风险增加相关。

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