Histone proteomics implicates H3K36me2 and its regulators in mouse embryonic stem cell pluripotency exit and lineage choice

Sezginmert Dersu; Terzi Cizmecioglu Nihal

doi:10.1515/tjb-2023-0030

Türk Biyokimya Dergisi (Jul 2023)

Histone proteomics implicates H3K36me2 and its regulators in mouse embryonic stem cell pluripotency exit and lineage choice

Sezginmert Dersu,
Terzi Cizmecioglu Nihal

Affiliations

Sezginmert Dersu: Department of Biological Sciences, Faculty of Arts and Sciences, Middle East Technical University, Ankara, Türkiye
Terzi Cizmecioglu Nihal: Department of Biological Sciences, Faculty of Arts and Sciences, Middle East Technical University, Ankara, Türkiye

DOI: https://doi.org/10.1515/tjb-2023-0030
Journal volume & issue: Vol. 48, no. 4
pp. 351 – 361

Abstract

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Gene expression changes during embryonic stem cell (ESC) differentiation is regulated by epigenetic mechanisms. Understanding these can help uncover how cell fate decisions are made during early embryonic development. Comparison of chromatin of ESCs with lineage-committed cells can implicate chromatin factors functional in exit from pluripotency and the choice of proper lineages. Therefore, we quantitatively analyzed histone modifications in mouse ESC differentiation towards neuroectoderm and endoderm.

Published in Türk Biyokimya Dergisi

ISSN: 1303-829X (Online)
Publisher: De Gruyter
Country of publisher: Germany
LCC subjects: Science: Chemistry: Organic chemistry: Biochemistry
Website: https://www.degruyter.com/journal/key/tjb/html

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