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Differential Histone Distribution Patterns in Induced Asymmetrically Dividing Mouse Embryonic Stem Cells

机译:诱导不对称分裂小鼠胚胎干细胞的差分组蛋白分布图

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Wnt3a-coated beads can induce asymmetric divisions of mouse embryonic stem cells (mESCs), resulting in one self-renewed mESC and one differentiating epiblast stem cell. This provides an opportunity for studying histone inheritance pattern at a single-cell resolution in cell culture. Here, we report that mESCs with Wnt3a-bead induction display nonoverlapping preexisting (old) versus newly synthesized (new) histone H3 patterns, but mESCs without Wnt3a beads have largely overlapping patterns. Furthermore, H4K20me2/3, an old histone-enriched modification, displays a higher instance of asymmetric distribution on chromatin fibers from Wnt3a-induced mESCs than those from non-induced mESCs. These locally distinct distributions between old and new histones have both cellular specificity in Wnt3a-induced mESCs and molecular specificity for histones H3 and H4. Given that post-translational modifications at H3 and H4 carry the major histone modifications, our findings provide a mammalian cell culture system to study histone inheritance for maintaining stem cell fate and for resetting it during differentiation.
机译:WNT3A涂层珠子可以诱导小鼠胚胎干细胞(MESCS)的不对称分裂,导致一个自我更新的母体和一个差异化的表血管干细胞。这提供了在细胞培养中以单细胞分辨率研究组蛋白遗传模式的机会。在这里,我们报告了使用Wnt3a-bead诱导显示器的MESCS,其与新合成的(新)组蛋白H3图案相比,但没有Wnt3a珠子的MESCs具有很大程度上重叠的图案。此外,H4K20ME2 / 3是一种古老的组蛋白富集的修饰,在WNT3A诱导的MESCS上显示出染色质纤维上的不对称分布的更高实例,而不是来自非诱导的MESC。这些古老和新的组蛋白之间的局部不同的分布在Wnt3a诱导的MESC中具有细胞特异性和组蛋白H3和H4的分子特异性。鉴于H3和H4的翻译后修饰携带主要的组蛋白修饰,我们的研究结果提供了哺乳动物细胞培养系统,以研究维持干细胞命运的组蛋白遗传和用于在分化期间重新复位。

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