ZFP57 maintains the parent-of-origin-specific expression of the imprinted genes and differentially affects non-imprinted targets in mouse embryonic stem cells
Academic Article
Publication Date:
2016
abstract:
ZFP57 is necessary for maintaining repressive epigenetic
modifications at Imprinting control regions
(ICRs). In mouse embryonic stem cells (ESCs), ZFP57
binds ICRs (ICRBS) and many other loci (non-ICRBS).
To address the role of ZFP57 on all its target sites,
we performed high-throughput and multi-locus analyses
of inbred and hybrid mouse ESC lines carrying
different gene knockouts. By using an allele-specific
RNA-seq approach, we demonstrate that ZFP57 loss
results in derepression of the imprinted allele of multiple
genes in the imprinted clusters. We also find
marked epigenetic differences between ICRBS and
non-ICRBS suggesting that different cis-acting regulatory
functions are repressed by ZFP57 at these
two classes of target loci. Overall, these data demonstrate
that ZFP57 is pivotal to maintain the allelespecific
epigenetic modifications of ICRs that in turn
are necessary for maintaining the imprinted expression
over long distances. At non-ICRBS, ZFP57 inactivation
results in acquisition of epigenetic features
that are characteristic of poised enhancers, suggesting
that another function of ZFP57 in early embryogenesis
is to repress cis-acting regulatory elements
whose activity is not yet required.
Iris type:
01.01 Articolo in rivista
Keywords:
Epigenetics-Imprinting-Zfp57-DNA methylation
List of contributors:
Riccio, Andrea; Grimaldi, Giovanna; Angelini, Claudia; Fico, Annalisa
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