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基因组和代谢组模式与钙和维生素 D 补充的反应分离。

Genomic and metabolomic patterns segregate with responses to calcium and vitamin D supplementation.

机构信息

Clinical Biochemistry Department, King's College Hospital, Denmark Hill, London SE5 9RS, UK.

出版信息

Br J Nutr. 2011 Jan;105(1):71-9. doi: 10.1017/S0007114510003065. Epub 2010 Aug 23.

DOI:10.1017/S0007114510003065
PMID:20727239
Abstract

Inter-individual response differences to vitamin D and Ca supplementation may be under genetic control through vitamin D and oestrogen receptor genes, which may influence their absorption and/or metabolism. Metabolomic studies on blood and urine from subjects supplemented with Ca and vitamin D reveal different metabolic profiles that segregate with genotype. Genotyping was performed for oestrogen receptor 1 gene (ESR1) and vitamin D receptor gene (VDR) in fifty-six postmenopausal women. Thirty-six women were classified as low bone density as determined by a heel ultrasound scan and twenty women had normal bone density acting as 'controls'. Those with low bone density (LBD) were supplemented with oral Ca and vitamin D and were classified according to whether they were 'responders' or 'non-responders' according to biochemical results before and after therapy compared to controls receiving no supplementation. Metabolomic studies on serum and urine were done for the three groups at 0 and 3 months of therapy using NMR spectroscopy with pattern recognition. The 'non-responder' group showed a higher frequency of polymorphisms in the ESR1 (codons 10 and 325) and VDR (Bsm1 and Taq1), compared with to the 'responders'. The wild-type genotype for Fok1 was more frequent in those with LBD (70 %) compared with the control group (10 %). Distinctive patterns of metabolites were displayed by NMR studies at baseline and 3 months of post-treatment, segregating responders from non-responders and controls. Identification of potential 'non-responders' to vitamin D and Ca, before therapy, based on a genomic and/or metabolomic profile would allow targeted selection of optimal therapy on an individual basis.

摘要

个体对维生素 D 和钙补充的反应差异可能受基因控制,这些基因可能影响它们的吸收和/或代谢。对补充钙和维生素 D 的受试者的血液和尿液进行代谢组学研究显示,不同的代谢谱与基因型分离。对 56 名绝经后妇女的雌激素受体 1 基因 (ESR1) 和维生素 D 受体基因 (VDR) 进行了基因分型。36 名妇女被确定为足跟超声扫描的低骨密度,20 名妇女具有正常骨密度作为“对照”。那些低骨密度(LBD)的人接受口服钙和维生素 D 补充,并根据治疗前后与未接受补充的对照相比的生化结果分为“反应者”或“非反应者”。在治疗 0 和 3 个月时,使用 NMR 光谱和模式识别对三组血清和尿液进行代谢组学研究。与“反应者”相比,“非反应者”组在 ESR1(密码子 10 和 325)和 VDR(Bsm1 和 Taq1)中显示出更高频率的多态性。与对照组(10%)相比,LBD 中 Fok1 的野生型基因型更为常见(70%)。在基线和治疗后 3 个月的 NMR 研究中显示出不同的代谢物模式,将反应者与非反应者和对照组区分开来。在治疗前根据基因组和/或代谢组学特征识别潜在的“非反应者”对维生素 D 和钙,可以根据个体情况选择最佳治疗方案。

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