Gene expression programs determine cell fate in embryonic development and their dysregulation results in disease. Transcription factors (TFs) control gene expression by binding to enhancers, but how TFs select and activate their target enhancers is still unclear. HOX TFs share conserved homeodomains with highly similar sequence recognition properties, yet they impart the identity of different animal body parts. To understand how HOX TFs control their specific transcriptional programs in vivo, we compared HOXA2 and HOXA3 binding profiles in the mouse embryo. HOXA2 and HOXA3 directly cooperate with TALE TFs and selectively target different subsets of a broad TALE chromatin platform. Binding of HOX and tissue-specific TFs convert low affinity TALE binding into high confidence, tissue-specific binding events, which bear the mark of active enhancers. We propose that HOX paralogs, alone and in combination with tissue-specific TFs, generate tissue-specific transcriptional outputs by modulating the activity of TALE TFs at selected enhancers.
HOX paralogs selectively convert binding of ubiquitous transcription factors into tissue-specific patterns of enhancer activation.
HOX旁系同源物选择性地将普遍存在的转录因子的结合转化为组织特异性的增强子激活模式
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作者:Bridoux Laure, Zarrineh Peyman, Mallen Joshua, Phuycharoen Mike, Latorre Victor, Ladam Frank, Losa Marta, Baker Syed Murtuza, Sagerstrom Charles, Mace Kimberly A, Rattray Magnus, Bobola Nicoletta
| 期刊: | PLoS Genetics | 影响因子: | 3.700 |
| 时间: | 2020 | 起止号: | 2020 Dec 14; 16(12):e1009162 |
| doi: | 10.1371/journal.pgen.1009162 | 研究方向: | 其它 |
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