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Expression dynamics of repetitive DNA in early human embryonic development

机译:早期人胚胎发育中重复DNA的表达动态

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The last decade witnessed a number of genome-wide studies on human pre-implantation, which mostly focused on genes and provided only limited information on repeats, excluding the satellites. Considering the fact that repeats constitute a large portion of our genome with reported links to human physiology and disease, a thorough understanding of their spatiotemporal regulation during human embryogenesis will give invaluable clues on chromatin dynamics across time and space. Therefore, we performed a detailed expression analysis of all repetitive DNA elements including the satellites across stages of human pre-implantation and embryonic stem cells. We uncovered stage-specific expressions of more than a thousand repeat elements whose expressions fluctuated with a mild global decrease at the blastocyst stage. Most satellites were highly expressed at the 4-cell level and expressions of ACRO1 and D20S16 specifically peaked at this point. Whereas all members of the SVA elements were highly upregulated at 8-cell and morula stages, other transposons and small RNA repeats exhibited a high level of variation among their specific subtypes. Our repeat enrichment analysis in gene promoters coupled with expression correlations highlighted potential links between repeat expressions and nearby genes, emphasising mostly 8-cell and morula specific genes together with SVA_D, LTR5_Hs and LTR70 transposons. The DNA methylation analysis further complemented the understanding on the mechanistic aspects of the repeatome's regulation per se and revealed critical stages where DNA methylation levels are negatively correlating with repeat expression. Taken together, our study shows that specific expression patterns are not exclusive to genes and long?non-coding?RNAs but the repeatome also exhibits an intriguingly dynamic pattern at the global scale. Repeats identified in this study; particularly satellites, which were historically associated with heterochromatin, and those with potential links to nearby gene expression provide valuable insights into the understanding of key events in genomic regulation and warrant further research in epigenetics, genomics and developmental biology.
机译:最后十年目睹了许多关于人类预植入的全基因组研究,该研究主要集中在基因上,并仅提供有关卫星的重复的有限信息。考虑到重复的事实构成我们基因组的大部分与人体生理学和疾病的联系,对人类胚胎发生期间的彻底了解它们的时空调节将在时间和空间中给出染色质动力学的宝贵线索。因此,我们对跨植入阶段和胚胎干细胞的阶段的卫星进行了详细的表达分析。我们未发现阶段特异性表达超过一千多个重复元素,其表达在胚泡阶段的温和全局降低的情况下波动。大多数卫星在4细胞水平和acro1和D20s16的表达上高度表达,在此时特异性达到峰值。虽然SVA元素的所有成员在8个细胞和割球菌阶段高度上调,但其他转座子和小RNA重复在其特定亚型中表现出高度的变化。我们在基因启动子的重复浓缩分析与表达相关性突出显示重复表达和附近基因之间的潜在联系,并强调了与SVA_D,LTR5_HS和LTR70转座一起的8细胞和森仑特定基因。 DNA甲基化分析进一步互补了对重复的调节的机械方面的理解,并揭示了DNA甲基化水平与重复表达呈负相关的关键阶段。我们的研究表明,特定的表达模式不是基因和长期的特异性的表达模式?RNA,但重复在全球范围内也表现出一种有趣的动态模式。在本研究中确定的重复;特别是诸如历史上与异铬胺酸相关的卫星,以及附近基因表达的潜在链接的卫星提供了有价值的见解,以了解基因组调控中的关键事件和担保外观遗传学,基因组学和发育生物学的进一步研究。

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