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Epigenomic Reorganization of the Clustered Hox Genes in Embryonic Stem Cells Induced by Retinoic Acid

机译:维甲酸诱导胚胎干细胞中簇状Hox基因的表观基因组重组

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摘要

Retinoic acid (RA) regulates clustered Hox gene expression during embryogenesis and is required to establish the anterior-posterior body plan. Using mutant embryonic stem cell lines deficient in the RA receptor γ (RARγ) or Hoxa1 3′-RA-responsive element, we studied the kinetics of transcriptional and epigenomic patterning responses to RA. RARγ is essential for RA-induced Hox transcriptional activation, and deletion of its binding site in the Hoxa1 enhancer attenuates transcriptional and epigenomic activation of both Hoxa and Hoxb gene clusters. The kinetics of epigenomic reorganization demonstrate that complete erasure of the polycomb repressive mark H3K27me3 is not necessary to initiate Hox transcription. RARγ is not required to establish the bivalent character of Hox clusters, but RA/RARγ signaling is necessary to erase H3K27me3 from activated Hox genes during embryonic stem cell differentiation. Highly coordinated, long range epigenetic Hox cluster reorganization is closely linked to transcriptional activation and is triggered by RARγ located at the Hoxa1 3′-RA-responsive element.
机译:维甲酸(RA)调节胚胎发生过程中成簇的Hox基因表达,是建立前后身体计划所必需的。使用缺乏RA受体γ(RARγ)或Hoxa1 3'-RA反应元件的突变胚胎干细胞系,我们研究了对RA的转录和表观基因组模式反应的动力学。 RARγ对于RA诱导的Hox转录激活是必不可少的,在Hoxa1增强子中删除其结合位点会减弱Hoxa和Hoxb基因簇的转录和表观基因组激活。表观基因组重组的动力学表明,完全擦除多梳抑制标记H3K27me3对于启动Hox转录不是必需的。 RARγ不是建立Hox簇的二价特征所必需的,但是在胚胎干细胞分化过程中,RA /RARγ信号传导对于从激活的Hox基因中清除H3K27me3是必需的。高度协调的远距离表观遗传Hox簇重组与转录激活密切相关,并由位于Hoxa1 3'-RA反应元件上的RARγ触发。

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