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

AI Article Synopsis

  • - Epigenetic information is passed from mother cells to daughter cells during cell division, and researchers are investigating the factors involved in this process using flow cytometry to isolate native chromosomes.
  • - A study compared proteins found on metaphase-arrested embryonic stem cell (ESC) chromosomes with those in cell lysates, identifying important proteins that help maintain pluripotency and chromosome structure.
  • - The research shows that certain proteins, like PRC2 and DNA methyl-transferases, are crucial for keeping chromosomes compact during mitosis, as their deletion results in larger, de-condensed chromosomes.

Article Abstract

Epigenetic 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.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7431861PMC
http://dx.doi.org/10.1038/s41467-020-17823-zDOI Listing

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