首页> 外文期刊>Journal of bone and mineral research: the official journal of the American Society for Bone and Mineral Research >Childhood bone mineral content is associated with methylation status of the RXRA promoter at birth
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Childhood bone mineral content is associated with methylation status of the RXRA promoter at birth

机译:儿童骨骼矿物质含量与出生时RXRA启动子的甲基化状态有关

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Maternal vitamin D deficiency has been associated with reduced offspring bone mineral accrual. Retinoid-X receptor-alpha (RXRA) is an essential cofactor in the action of 1,25-dihydroxyvitamin D (1,25[OH]2-vitamin D), and RXRA methylation in umbilical cord DNA has been associated with later offspring adiposity. We tested the hypothesis that RXRA methylation in umbilical cord DNA collected at birth is associated with offspring skeletal development, assessed by dual-energy X-ray absorptiometry, in a population-based mother-offspring cohort (Southampton Women's Survey). Relationships between maternal plasma 25-hydroxyvitamin D (25[OH]-vitamin D) concentrations and cord RXRA methylation were also investigated. In 230 children aged 4 years, a higher percent methylation at four of six RXRA CpG sites measured was correlated with lower offspring bone mineral content (BMC) corrected for body size (β = -2.1 to -3.4 g/SD, p = 0.002 to 0.047). In a second independent cohort (n = 64), similar negative associations at two of these CpG sites, but positive associations at the two remaining sites, were observed; however, none of the relationships in this replication cohort achieved statistical significance. The maternal free 25(OH)-vitamin D index was negatively associated with methylation at one of these RXRA CpG sites (β = -3.3 SD/unit, p = 0.03). Thus, perinatal epigenetic marking at the RXRA promoter region in umbilical cord was inversely associated with offspring size-corrected BMC in childhood. The potential mechanistic and functional significance of this finding remains a subject for further investigation.
机译:孕产妇维生素D缺乏与后代骨骼矿物质的积累减少有关。维甲酸-X受体-α(RXRA)是1,25-二羟基维生素D(1,25 [OH] 2-维生素D)作用中的重要辅助因子,并且脐带DNA中的RXRA甲基化与后来的后代肥胖相关。我们测试了一个假设,即在以人口为基础的母亲-后代队列中,出生时收集的脐带DNA中的RXRA甲基化与后代骨骼发育有关(通过双能X线吸收法评估)(南安普敦妇女调查)。还研究了孕妇血浆25-羟基维生素D(25 [OH]-维生素D)浓度与脐带RXRA甲基化之间的关系。在230岁的4岁儿童中,所测量的六个RXRA CpG位点中的四个位点的甲基化百分比较高,与较低的后代骨骼矿物质含量(BMC)校正了体重相关(β= -2.1至-3.4 g / SD,p = 0.002至0.047)。在第二个独立队列中(n = 64),在这些CpG位点的两个位点出现了相似的负关联,但在其余两个位点出现了正关联。但是,该复制队列中的任何关系均未达到统计学意义。产妇的游离25(OH)-维生素D指数与这些RXRA CpG位点之一的甲基化呈负相关(β= -3.3 SD /单位,p = 0.03)。因此,在儿童时期,脐带RXRA启动子区域的围生期表观遗传标记与后代大小校正的BMC呈负相关。这一发现的潜在机制和功能意义仍然是有待进一步研究的主题。

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