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A novel approach identifies new differentially methylated regions (DMRs) associated with imprinted genes.

机译:一种新颖的方法可以识别与印迹基因相关的新的差异甲基化区域(DMR)。

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摘要

Imprinted genes are critical for normal human growth and neurodevelopment. They are characterized by differentially methylated regions (DMRs) of DNA that confer parent of origin-specific transcription. We developed a new strategy to identify imprinted gene-associated DMRs. Using genome-wide methylation profiling of sodium bisulfite modified DNA from normal human tissues of biparental origin, candidate DMRs were identified by selecting CpGs with methylation levels consistent with putative allelic differential methylation. In parallel, the methylation profiles of tissues of uniparental origin, i.e., paternally-derived androgenetic complete hydatidiform moles (AnCHMs), and maternally-derived mature cystic ovarian teratoma (MCT), were examined and then used to identify CpGs with parent of origin-specific DNA methylation. With this approach, we found known DMRs associated with imprinted genomic regions as well as new DMRs for known imprinted genes, NAP1L5 and ZNF597, and novel candidate imprinted genes. The paternally methylated DMR for one candidate, AXL, a receptor tyrosine kinase, was also validated in experiments with mouse embryos that demonstrated Axl was expressed preferentially from the maternal allele in a DNA methylation-dependent manner.
机译:印迹的基因对于正常的人类生长和神经发育至关重要。它们的特征在于赋予来源特异性转录亲本的DNA差异甲基化区域(DMR)。我们开发了一种新的策略来识别与基因相关的印迹DMR。使用双亲起源的正常人组织中的亚硫酸氢钠修饰的DNA进行全基因组甲基化分析,通过选择甲基化水平与推定的等位基因差异甲基化相一致的CpG来鉴定候选DMR。平行地,检查了单亲起源组织的甲基化谱,即,父本衍生的雄激素完全葡萄胎(AnCHMs)和母本衍生的成熟囊性卵巢畸胎瘤(MCT),然后用于鉴定母本为CpGs-特定的DNA甲基化。通过这种方法,我们发现了与印迹基因组区域相关的已知DMR,以及针对已知印迹基因NAP1L5和ZNF597以及新型候选印迹基因的新DMR。还在小鼠胚胎的实验中验证了一种候选物AXL(一种受体酪氨酸激酶)的父本甲基化DMR,该实验证明Axl优先以DNA甲基化依赖性方式从母本等位基因表达。

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