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Literature DB >> 33730542

H3K27ac bookmarking promotes rapid post-mitotic activation of the pluripotent stem cell program without impacting 3D chromatin reorganization.

Bobbie Pelham-Webb¹, Alexander Polyzos², Luke Wojenski³, Andreas Kloetgen⁴, Jiexi Li⁵, Dafne Campigli Di Giammartino⁵, Theodore Sakellaropoulos⁶, Aristotelis Tsirigos⁷, Leighton Core⁸, Effie Apostolou⁹.

Abstract

During self-renewal, cell-type-defining features are drastically perturbed in mitosis and must be faithfully reestablished upon G1 entry, a process that remains largely elusive. Here, we characterized at a genome-wide scale the dynamic transcriptional and architectural resetting of mouse pluripotent stem cells (PSCs) upon mitotic exit. We captured distinct waves of transcriptional reactivation with rapid induction of stem cell genes and transient activation of lineage-specific genes. Topological reorganization at different hierarchical levels also occurred in an asynchronous manner and showed partial coordination with transcriptional resetting. Globally, rapid transcriptional and architectural resetting associated with mitotic retention of H3K27 acetylation, supporting a bookmarking function. Indeed, mitotic depletion of H3K27ac impaired the early reactivation of bookmarked, stem-cell-associated genes. However, 3D chromatin reorganization remained largely unaffected, suggesting that these processes are driven by distinct forces upon mitotic exit. This study uncovers principles and mediators of PSC molecular resetting during self-renewal.

Entities: Chemical

Keywords: 3D chromatin organization; H3K27ac; Hi-C; PRO-seq; bookmarking; cell identity; enhancer-promoter interaction; mitosis; pluripotent stem cells; transcription reactivation

Mesh：

Substances：
Chromatin
Histones

Year: 2021 PMID： 33730542 PMCID： PMC8052294 DOI： 10.1016/j.molcel.2021.02.032

Source DB: PubMed Journal: Mol Cell ISSN： 1097-2765 Impact factor: 17.970

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