TRIM28 is an epigenetic barrier to induced pluripotent stem cell reprogramming

Miles, DC; de Vries, NA; Gisler, S; Lieftink, C; Akhtar, W; Gogola, E; Pawlitzky, I; Hulsman, D; Tanger, E; Koppens, M; Beijersbergen, RL; van Lohuizen, M

Author(s): Miles, DC; de Vries, NA; Gisler, S; Lieftink, C; Akhtar, W; Gogola, E; Pawlitzky, I; Hulsman, D; Tanger, E; Koppens, M; Beijersbergen, RL; van Lohuizen, M;
Details: Publication Year 2017,Volume 35,Issue #1,Page 147-157
Journal Title: Stem Cells
Publication Type: Journal Article
Abstract: Since the discovery of induced pluripotent stem cells there has been intense interest in understanding the mechanisms that allow a somatic cell to be reprogrammed back to a pluripotent state. Several groups have studied the alterations in gene expression that occur as somatic cells modify their genome to that of an embryonic stem cell. Underpinning many of the gene expression changes are modifications to the epigenetic profile of the associated chromatin. We have used a large-scale shRNA screen to identify epigenetic modifiers that act as barriers to reprogramming. We have uncovered an important role for TRIM28 in cells resisting transition between somatic and pluripotent states. TRIM28 achieves this by maintaining the H3K9me3 repressed state and keeping endogenous retroviruses (ERVs) silenced. We propose that knockdown of TRIM28 during reprogramming results in more plastic H3K9me3 domains, dysregulation of genes nearby H3K9me3 marks, and up regulation of ERVs, thus facilitating the transition through reprogramming. Stem Cells 2016.
Publisher: Wiley
Research Division(s): Molecular Medicine
PubMed ID: 27350605
Publisher's Version: https://doi.org/10.1002/stem.2453
NHMRC Grants: NHMRC/1052195,
Terms of Use/Rights Notice: Refer to copyright notice on published article.

Creation Date: 2016-10-25 02:58:28

Last Modified: 2018-07-11 09:31:44