Identifying proteins bound to native mitotic ESC chromosomes reveals chromatin repressors are important for compaction

Author:

Djeghloul DouniaORCID,Patel Bhavik,Kramer HolgerORCID,Dimond AndrewORCID,Whilding Chad,Brown Karen,Kohler Anne-Céline,Feytout Amelie,Veland NicolasORCID,Elliott James,Bharat Tanmay A. M.ORCID,Tarafder Abul K.,Löwe JanORCID,Ng Bee L.ORCID,Guo Ya,Guy JackyORCID,Huseyin Miles K.ORCID,Klose Robert J.,Merkenschlager MatthiasORCID,Fisher Amanda G.ORCID

Abstract

AbstractEpigenetic information is transmitted from mother to daughter cells through mitosis. Here, to identify factors that might play a role in conveying epigenetic memory through cell division, we report on the isolation of unfixed, native chromosomes from metaphase-arrested cells using flow cytometry and perform LC-MS/MS to identify chromosome-bound proteins. A quantitative proteomic comparison between metaphase-arrested cell lysates and chromosome-sorted samples reveals a cohort of proteins that were significantly enriched on mitotic ESC chromosomes. These include pluripotency-associated transcription factors, repressive chromatin-modifiers such as PRC2 and DNA methyl-transferases, and proteins governing chromosome architecture. Deletion of PRC2, Dnmt1/3a/3b or Mecp2 in ESCs leads to an increase in the size of individual mitotic chromosomes, consistent with de-condensation. Similar results were obtained by the experimental cleavage of cohesin. Thus, we identify chromosome-bound factors in pluripotent stem cells during mitosis and reveal that PRC2, DNA methylation and Mecp2 are required to maintain chromosome compaction.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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