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哺乳动物着床前胚胎中可及染色质的全景。

The landscape of accessible chromatin in mammalian preimplantation embryos.

出版信息

Nature. 2016 Jun 30;534(7609):652-7. doi: 10.1038/nature18606. Epub 2016 Jun 15.

Abstract

In mammals, extensive chromatin reorganization is essential for reprogramming terminally committed gametes to a totipotent state during preimplantation development. However, the global chromatin landscape and its dynamics in this period remain unexplored. Here we report a genome-wide map of accessible chromatin in mouse preimplantation embryos using an improved assay for transposase-accessible chromatin with high throughput sequencing (ATAC-seq) approach with CRISPR/Cas9-assisted mitochondrial DNA depletion. We show that despite extensive parental asymmetry in DNA methylomes, the chromatin accessibility between the parental genomes is globally comparable after major zygotic genome activation (ZGA). Accessible chromatin in early embryos is widely shaped by transposable elements and overlaps extensively with putative cis-regulatory sequences. Unexpectedly, accessible chromatin is also found near the transcription end sites of active genes. By integrating the maps of cis-regulatory elements and single-cell transcriptomes, we construct the regulatory network of early development, which helps to identify the key modulators for lineage specification. Finally, we find that the activities of cis-regulatory elements and their associated open chromatin diminished before major ZGA. Surprisingly, we observed many loci showing non-canonical, large open chromatin domains over the entire transcribed units in minor ZGA, supporting the presence of an unusually permissive chromatin state. Together, these data reveal a unique spatiotemporal chromatin configuration that accompanies early mammalian development.

摘要

在哺乳动物中,广泛的染色质重排对于在植入前发育过程中将终末定型的配子重新编程为全能状态至关重要。然而,在此期间,全局染色质景观及其动态仍未被探索。在这里,我们使用改进的转座酶可及染色质高通量测序(ATAC-seq)方法和 CRISPR/Cas9 辅助的线粒体 DNA 耗竭,报道了小鼠植入前胚胎中可及染色质的全基因组图谱。我们表明,尽管在 DNA 甲基组中存在广泛的亲本不对称性,但在主要合子基因组激活(ZGA)后,亲本基因组之间的染色质可及性在全球范围内是可比的。早期胚胎中的可及染色质广泛受转座元件的影响,并与假定的顺式调控序列广泛重叠。出乎意料的是,可及染色质也存在于活性基因的转录末端附近。通过整合顺式调控元件和单细胞转录组图谱,我们构建了早期发育的调控网络,这有助于识别谱系特化的关键调节剂。最后,我们发现顺式调控元件的活性及其相关的开放染色质在主要 ZGA 之前减少。令人惊讶的是,我们在次要 ZGA 期间观察到许多位点在整个转录单位上显示出非典型的、大的开放染色质域,这支持了异常允许的染色质状态的存在。总之,这些数据揭示了伴随早期哺乳动物发育的独特的时空染色质构象。

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