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Methylation changes in the peripheral blood of Filipinos with type 2 diabetes suggest spurious transcription initiation at TXNIP

机译:2型糖尿病粉丝骨外周血的甲基化变化表明TXNIP的杂散转录起始

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摘要

While much work has been done in associating differentially methylated positions (DMPs) to type 2 diabetes (T2D) across different populations, not much attention has been placed on identifying its possible functional consequences. We explored methylation changes in the peripheral blood of Filipinos with T2D and identified 177 associated DMPs. Most of these DMPs were associated with genes involved in metabolism, inflammation and the cell cycle. Three of these DMPs map to the TXNIP gene body, replicating previous findings from epigenome-wide association studies (EWAS) of T2D. The TXNIP downmethylation coincided with increased transcription at the 3' UTR, H3K36me3 histone markings and Sp1 binding, suggesting spurious transcription initiation at the TXNIP 3' UTR as a functional consequence of T2D methylation changes. We also explored potential epigenetic determinants to increased incidence of T2D in Filipino immigrants in the USA and found three DMPs associated with the interaction of T2D and immigration. Two of these DMPs were located near MAP2K7 and PRMT1, which may point towards dysregulated stress response and inflammation as a contributing factor to T2D among Filipino immigrants.
机译:虽然在将差异甲基化的位置(DMP)与不同群体之间的2型糖尿病(T2D)相关联的情况下,但在识别其可能的功能后果的情况下,并不多。我们用T2D探索了菲律宾脲外周血的甲基化变化,并确定了177个相关的DMP。这些DMP中的大多数与参与代谢,炎症和细胞周期的基因有关。这些DMPS中的三种地图到TXNIP基因体,从外延型关联研究(EWAS)复制了先前的T2D。 TXNIP下甲基化与3'UTR,H3K36ME3组蛋白标记和SP1结合的转录相一致,表明TXNIP 3'UTR处的寄生转录起始作为T2D甲基化变化的功能后果。我们还探讨了潜在的表观遗传决定因素,以增加美国菲律宾移民T2D的发病率,并发现与T2D和移民相互作用相关的三个DMP。这些DMP中的两种位于Map2K7和PRMT1附近,该PRMT1可以指向菲律宾移民中T2D的促成因子的表现症应力反应和炎症。

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