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A poised chromatin platform for TGF-β access to master regulators

机译:用于TGF-β进入主调节器的平衡染色质平台

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Specific chromatin marks keep master regulators of differentiation silent yet poised for activation by extracellular signals. We report that nodal TGF-β signals use the poised histone mark H3K9me3 to trigger differentiation of mammalian embryonic stem cells. Nodal receptors induce the formation of companion Smad4-Smad2/3 and TRIM33-Smad2/3 complexes. The PHD-Bromo cassette of TRIM33 facilitates binding of TRIM33-Smad2/3 to H3K9me3 and H3K18ac on the promoters of mesendoderm regulators Gsc and Mixl1. The crystal structure of this cassette, bound to histone H3 peptides, illustrates that PHD recognizes K9me3, and Bromo binds an adjacent K18ac. The interaction between TRIM33-Smad2/3 and H3K9me3 displaces the chromatin-compacting factor HP1γ, making nodal response elements accessible to Smad4-Smad2/3 for Pol II recruitment. In turn, Smad4 increases K18 acetylation to augment TRIM33-Smad2/3 binding. Thus, nodal effectors use the H3K9me3 mark as a platform to switch master regulators of stem cell differentiation from the poised to the active state.
机译:特定的染色质标记使分化的主要调节剂保持沉默,并准备被细胞外信号激活。我们报告说,节点TGF-β信号使用平衡的组蛋白标记H3K9me3来触发哺乳动物胚胎干细胞的分化。节点受体诱导伴侣Smad4-Smad2 / 3和TRIM33-Smad2 / 3复合物的形成。 TRIM33的PHD-Bromo盒可促进TRIM33-Smad2 / 3与中胚层调节子Gsc和Mix11的启动子上的H3K9me3和H3K18ac结合。该盒的晶体结构与组蛋白H3肽结合,说明PHD识别K9me3,而Bromo结合相邻的K18ac。 TRIM33-Smad2 / 3与H3K9me3之间的相互作用取代了染色质紧缩因子HP1γ,使Smad4-Smad2 / 3可以利用节点响应元件进行Pol II募集。反过来,Smad4增加K18乙酰化以增强TRIM33-Smad2 / 3结合。因此,淋巴结效应子使用H3K9me3标记作为平台,将干细胞分化的主要调节因子从平衡状态切换到激活状态。

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