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High histone variant H3.3 content in mouse prospermatogonia suggests a role in epigenetic reformatting

机译:小鼠ProsingMatogonia中的高组蛋白变体H3.3含量表明了表观遗传重新制作中的作用

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摘要

Histone variants can incorporate into the nucleosome outside of S-phase. Some are known to play important roles in mammalian germ cell development, this cell lineage being characterized by long phases of quiescence, a protracted meiotic phase, and genome-wide epigenetic reformatting events. The best known example of such an event is the global-scale erasure of DNA methylation in sexually indifferent primordial germ cells, then its re-establishment in fetal prospermatogonia and growing oocytes. Histone H3 and its post-translationally modified forms provide important waypoints in the establishment of epigenetic states. Using mass spectrometry and immunoblotting, we show that the H3.3 replacement variant is present at an unusually high amount in mouse prospermatogonia at the peak stage of global DNA methylation re-establishment. We speculate that H3.3 facilitates this process through achieving a greater level of accessibility of chromatin modifiers to DNA.
机译:组蛋白变体可以包含在S阶段之外的核小体中。 有人众所周知,在哺乳动物生殖细胞发育中发挥重要作用,这种细胞谱系的特征在于静态阶段的长阶段,长期的减数分子相和基因组的表观遗传重整事件。 这种事件的最着名的例子是性无关紧要的原始生殖细胞中DNA甲基化的全球范围擦除,然后其在胎儿Prospermatogonia和生长卵母细胞中重新建立。 组蛋白H3及其翻译后修改的形式在建立表观遗传状态下提供了重要的航路点。 使用质谱和免疫印迹,我们表明H3.3更换变体在全球DNA甲基化重建的峰值阶段以小鼠Protformmatogonia在小鼠ProsperMatogonia中存在异常高。 我们推测H3.3通过实现染色质调节剂的较大水平的染色质调节剂至DNA的可用性促进该过程。

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