TRIM28 represses transcription of endogenous retroviruses in neural progenitor cells. - Literature - Data resources

25543143

TRIM28 represses transcription of endogenous retroviruses in neural progenitor cells.

Cell Rep, 2015/1/06;10(1):20-8.

Fasching L^[1], Kapopoulou A^[2], Sachdeva R^[1], Petri R^[1], Jönsson ME^[1], Männe C^[1], Turelli P^[2], Jern P^[3], Cammas F^[4], Trono D^[2], Jakobsson J^[5]

Affiliations

PMID: 25543143

Impact factor: 9.995

Abstract

TRIM28 is a corepressor that mediates transcriptional silencing by establishing local heterochromatin. Here, we show that deletion of TRIM28 in neural progenitor cells (NPCs) results in high-level expression of two groups of endogenous retroviruses (ERVs): IAP1 and MMERVK10C. We find that NPCs use TRIM28-mediated histone modifications to dynamically regulate transcription and silencing of ERVs, which is in contrast to other somatic cell types using DNA methylation. We also show that derepression of ERVs influences transcriptional dynamics in NPCs through the activation of nearby genes and the expression of long noncoding RNAs. These findings demonstrate a unique dynamic transcriptional regulation of ERVs in NPCs. Our results warrant future studies on the role of ERVs in the healthy and diseased brain.

MeSH terms

Animals; DNA Methylation; Embryonic Stem Cells; Endogenous Retroviruses; Gene Expression Regulation, Developmental; Heterochromatin; Histones; Humans; Mice; Neurons; Nuclear Proteins; Repressor Proteins; Stem Cells; Transcription, Genetic; Tripartite Motif-Containing Protein 28

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