A cis-acting mechanism mediates transcriptional memory at Polycomb target genes in mammals

被引:0
作者
Daniel Holoch
Michel Wassef
Cecilia Lövkvist
Dina Zielinski
Setareh Aflaki
Bérangère Lombard
Tiphaine Héry
Damarys Loew
Martin Howard
Raphaël Margueron
机构
[1] Sorbonne University,Institut Curie, Paris Sciences et Lettres Research University
[2] INSERM U934/CNRS UMR 3215,Biotech Research and Innovation Centre
[3] John Innes Centre,undefined
[4] Norwich Research Park,undefined
[5] INSERM U900,undefined
[6] Mines ParisTech,undefined
[7] Proteomics Mass Spectrometry Laboratory,undefined
[8] University of Copenhagen,undefined
来源
Nature Genetics | 2021年 / 53卷
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摘要
Epigenetic inheritance of gene expression states enables a single genome to maintain distinct cellular identities. How histone modifications contribute to this process remains unclear. Using global chromatin perturbations and local, time-controlled modulation of transcription, we establish the existence of epigenetic memory of transcriptional activation for genes that can be silenced by the Polycomb group. This property emerges during cell differentiation and allows genes to be stably switched after a transient transcriptional stimulus. This transcriptional memory state at Polycomb targets operates in cis; however, rather than relying solely on read-and-write propagation of histone modifications, the memory is also linked to the strength of activating inputs opposing Polycomb proteins, and therefore varies with the cellular context. Our data and computational simulations suggest a model whereby transcriptional memory arises from double-negative feedback between Polycomb-mediated silencing and active transcription. Transcriptional memory at Polycomb targets thus depends not only on histone modifications but also on the gene-regulatory network and underlying identity of a cell.
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页码:1686 / 1697
页数:11
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