As the 3D structure of the genome is analysed at ever increasing resolution it is clear that there is considerable variation in the 3D chromatin architecture across different cell types. It has been proposed that this may, in part, be due to increased recruitment of cohesin to activated cis-elements (enhancers and promoters) leading to cell-type specific loop extrusion underlying the formation of new sub-TADs. Here we show that cohesin correlates well with the presence of active enhancers and that this varies in an allele-specific manner with the presence or absence of polymorphic enhancers which vary from one individual to another. Using the alpha globin cluster as a model, we show that when all enhancers are removed, peaks of cohesin disappear from these regions and the erythroid specific sub-TAD is no longer formed. Re-insertion of the major alpha globin enhancer (R2) is associated with re-establishment of recruitment and increased interactions. In complementary experiments insertion of the R2 enhancer element into a "neutral" region of the genome recruits cohesin, induces transcription and creates a new large (75Â kb) erythroid-specific domain. Together these findings support the proposal that active enhancers recruit cohesin, stimulate loop extrusion and promote the formation of cell specific sub-TADs.
Active regulatory elements recruit cohesin to establish cell specific chromatin domains.
活性调控元件募集黏连蛋白以建立细胞特异性染色质结构域
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作者:Georgiades Emily, Harrold Caroline, Roberts Nigel, Kassouf Mira, Riva Simone G, Sanders Edward, Downes Damien, Francis Helena S, Blayney Joseph, Oudelaar A Marieke, Milne Thomas A, Higgs Douglas, Hughes Jim R
| 期刊: | Scientific Reports | 影响因子: | 3.900 |
| 时间: | 2025 | 起止号: | 2025 Apr 6; 15(1):11780 |
| doi: | 10.1038/s41598-025-96248-4 | 研究方向: | 细胞生物学 |
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