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Assessing DNA methylation in the developing human intestinal epithelium: potential link to inflammatory bowel disease

机译:评估人类肠道上皮细胞中的DNA甲基化:与炎症性肠病的潜在联系

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摘要

DNA methylation is one of the major epigenetic mechanisms implicated in regulating cellular development and cell-type-specific gene expression. Here we performed simultaneous genome-wide DNA methylation and gene expression analysis on purified intestinal epithelial cells derived from human fetal gut, healthy pediatric biopsies, and children newly diagnosed with inflammatory bowel disease (IBD). Results were validated using pyrosequencing, real-time PCR, and immunostaining. The functional impact of DNA methylation changes on gene expression was assessed by employing in-vitro assays in intestinal cell lines. DNA methylation analyses allowed identification of 214 genes for which expression is regulated via DNA methylation, i.e. regulatory differentially methylated regions (rDMRs). Pathway and functional analysis of rDMRs suggested a critical role for DNA methylation in regulating gene expression and functional development of the human intestinal epithelium. Moreover, analysis performed on intestinal epithelium of children newly diagnosed with IBD revealed alterations in DNA methylation within genomic loci, which were found to overlap significantly with those undergoing methylation changes during intestinal development. Our study provides novel insights into the physiological role of DNA methylation in regulating functional maturation of the human intestinal epithelium. Moreover, we provide data linking developmentally acquired alterations in the DNA methylation profile to changes seen in pediatric IBD.
机译:DNA甲基化是涉及调控细胞发育和细胞类型特异性基因表达的主要表观遗传机制之一。在这里,我们对源自人类胎儿肠道,健康的儿科活组织检查和刚被诊断出患有炎症性肠病(IBD)的儿童的肠道上皮细胞进行了全基因组DNA甲基化和基因表达分析。使用焦磷酸测序,实时PCR和免疫染色验证了结果。 DNA甲基化变化对基因表达的功能影响通过在肠道细胞系中进行体外测定来评估。 DNA甲基化分析可以鉴定214个基因,这些基因的表达受DNA甲基化调节,即调节差异甲基化区域(rDMR)。 rDMR的途径和功能分析表明,DNA甲基化在调节人肠上皮的基因表达和功能发育中起着至关重要的作用。此外,对新诊断为IBD的儿童的肠上皮进行的分析显示,基因组位点内DNA甲基化的变化与肠道发育过程中发生甲基化变化的那些显着重叠。我们的研究为DNA甲基化在调节人肠上皮功能成熟中的生理作用提供了新的见解。此外,我们提供的数据将DNA甲基化配置文件中的发育性获得的变化与儿科IBD的变化联系起来。

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