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斑马鱼胚胎发生过程中新兴的 H3K9me3 染色质景观。

The emerging H3K9me3 chromatin landscape during zebrafish embryogenesis.

机构信息

Department of Genetics, University of Georgia, Athens, GA, 30602, USA.

出版信息

Genetics. 2024 Oct 7;228(2). doi: 10.1093/genetics/iyae138.

Abstract

The structural organization of eukaryotic genomes is contingent upon the fractionation of DNA into transcriptionally permissive euchromatin and repressive heterochromatin. However, we have a limited understanding of how these distinct states are first established during animal embryogenesis. Histone 3 lysine 9 trimethylation (H3K9me3) is critical to heterochromatin formation, and bulk establishment of this mark is thought to help drive large-scale remodeling of an initially naive chromatin state during animal embryogenesis. However, a detailed understanding of this process is lacking. Here, we leverage CUT&RUN to define the emerging H3K9me3 landscape of the zebrafish embryo with high sensitivity and temporal resolution. Despite the prevalence of DNA transposons in the zebrafish genome, we found that LTR transposons are preferentially targeted for embryonic H3K9me3 deposition, with different families exhibiting distinct establishment timelines. High signal-to-noise ratios afforded by CUT&RUN revealed new, emerging sites of low-amplitude H3K9me3 that initiated before the major wave of zygotic genome activation (ZGA). Early sites of establishment predominated at specific subsets of transposons and were particularly enriched for transposon sequences with maternal piRNAs and pericentromeric localization. Notably, the number of H3K9me3 enriched sites increased linearly across blastula development, while quantitative comparison revealed a >10-fold genome-wide increase in H3K9me3 signal at established sites over just 30 min at the onset of major ZGA. Continued maturation of the H3K9me3 landscape was observed beyond the initial wave of bulk establishment.

摘要

真核基因组的结构组织取决于将 DNA 分成转录允许的常染色质和抑制的异染色质。然而,我们对这些不同状态如何在动物胚胎发生过程中首先建立的知之甚少。组蛋白 3 赖氨酸 9 三甲基化 (H3K9me3) 对异染色质的形成至关重要,并且认为这种标记的大量建立有助于在动物胚胎发生过程中驱动最初幼稚染色质状态的大规模重塑。然而,对这个过程的详细了解是缺乏的。在这里,我们利用 CUT&RUN 以高灵敏度和时间分辨率定义斑马鱼胚胎的新兴 H3K9me3 景观。尽管 DNA 转座子在斑马鱼基因组中普遍存在,但我们发现 LTR 转座子优先被靶向用于胚胎 H3K9me3 沉积,不同家族表现出不同的建立时间线。CUT&RUN 提供的高信噪比揭示了新的、低幅度 H3K9me3 的新兴起始位点,这些起始位点发生在合子基因组激活 (ZGA) 的主要波之前。建立的早期位点主要集中在特定的转座子子集上,并且特别富含具有母体 piRNA 和着丝粒定位的转座子序列。值得注意的是,H3K9me3 富集位点的数量在原肠胚发育过程中呈线性增加,而定量比较显示,在主要 ZGA 开始时,仅 30 分钟内,建立的位点的 H3K9me3 信号在整个基因组范围内增加了 10 多倍。在初始批量建立波之后,还观察到 H3K9me3 景观的持续成熟。

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