Global mapping of DNA methylation in mouse promoters reveals epigenetic reprogramming of pluripotency genes.

Global mapping of DNA methylation in mouse promoters reveals epigenetic reprogramming of pluripotency genes.

DNA methylation patterns are reprogrammed in primordial germ cells and in preimplantation embryos by demethylation and subsequent de novo methylation. It has been suggested that epigenetic reprogramming may be necessary for the embryonic genome to return to a pluripotent state. We have carried out a...

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Main Authors: Cassandra R Farthing, Gabriella Ficz, Ray Kit Ng, Chun-Fung Chan, Simon Andrews, Wendy Dean, Myriam Hemberger, Wolf Reik
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2008-06-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC2432031?pdf=render
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spelling doaj-b8d268cc47a6442887af4f80e33407ce2020-11-25T01:22:53ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042008-06-0146e100011610.1371/journal.pgen.1000116Global mapping of DNA methylation in mouse promoters reveals epigenetic reprogramming of pluripotency genes.Cassandra R FarthingGabriella FiczRay Kit NgChun-Fung ChanSimon AndrewsWendy DeanMyriam HembergerWolf ReikDNA methylation patterns are reprogrammed in primordial germ cells and in preimplantation embryos by demethylation and subsequent de novo methylation. It has been suggested that epigenetic reprogramming may be necessary for the embryonic genome to return to a pluripotent state. We have carried out a genome-wide promoter analysis of DNA methylation in mouse embryonic stem (ES) cells, embryonic germ (EG) cells, sperm, trophoblast stem (TS) cells, and primary embryonic fibroblasts (pMEFs). Global clustering analysis shows that methylation patterns of ES cells, EG cells, and sperm are surprisingly similar, suggesting that while the sperm is a highly specialized cell type, its promoter epigenome is already largely reprogrammed and resembles a pluripotent state. Comparisons between pluripotent tissues and pMEFs reveal that a number of pluripotency related genes, including Nanog, Lefty1 and Tdgf1, as well as the nucleosome remodeller Smarcd1, are hypomethylated in stem cells and hypermethylated in differentiated cells. Differences in promoter methylation are associated with significant differences in transcription levels in more than 60% of genes analysed. Our comparative approach to promoter methylation thus identifies gene candidates for the regulation of pluripotency and epigenetic reprogramming. While the sperm genome is, overall, similarly methylated to that of ES and EG cells, there are some key exceptions, including Nanog and Lefty1, that are highly methylated in sperm. Nanog promoter methylation is erased by active and passive demethylation after fertilisation before expression commences in the morula. In ES cells the normally active Nanog promoter is silenced when targeted by de novo methylation. Our study suggests that reprogramming of promoter methylation is one of the key determinants of the epigenetic regulation of pluripotency genes. Epigenetic reprogramming in the germline prior to fertilisation and the reprogramming of key pluripotency genes in the early embryo is thus crucial for transmission of pluripotency.http://europepmc.org/articles/PMC2432031?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Cassandra R Farthing
Gabriella Ficz
Ray Kit Ng
Chun-Fung Chan
Simon Andrews
Wendy Dean
Myriam Hemberger
Wolf Reik
spellingShingle Cassandra R Farthing
Gabriella Ficz
Ray Kit Ng
Chun-Fung Chan
Simon Andrews
Wendy Dean
Myriam Hemberger
Wolf Reik
Global mapping of DNA methylation in mouse promoters reveals epigenetic reprogramming of pluripotency genes.
PLoS Genetics
author_facet Cassandra R Farthing
Gabriella Ficz
Ray Kit Ng
Chun-Fung Chan
Simon Andrews
Wendy Dean
Myriam Hemberger
Wolf Reik
author_sort Cassandra R Farthing
title Global mapping of DNA methylation in mouse promoters reveals epigenetic reprogramming of pluripotency genes.
title_short Global mapping of DNA methylation in mouse promoters reveals epigenetic reprogramming of pluripotency genes.
title_full Global mapping of DNA methylation in mouse promoters reveals epigenetic reprogramming of pluripotency genes.
title_fullStr Global mapping of DNA methylation in mouse promoters reveals epigenetic reprogramming of pluripotency genes.
title_full_unstemmed Global mapping of DNA methylation in mouse promoters reveals epigenetic reprogramming of pluripotency genes.
title_sort global mapping of dna methylation in mouse promoters reveals epigenetic reprogramming of pluripotency genes.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2008-06-01
description DNA methylation patterns are reprogrammed in primordial germ cells and in preimplantation embryos by demethylation and subsequent de novo methylation. It has been suggested that epigenetic reprogramming may be necessary for the embryonic genome to return to a pluripotent state. We have carried out a genome-wide promoter analysis of DNA methylation in mouse embryonic stem (ES) cells, embryonic germ (EG) cells, sperm, trophoblast stem (TS) cells, and primary embryonic fibroblasts (pMEFs). Global clustering analysis shows that methylation patterns of ES cells, EG cells, and sperm are surprisingly similar, suggesting that while the sperm is a highly specialized cell type, its promoter epigenome is already largely reprogrammed and resembles a pluripotent state. Comparisons between pluripotent tissues and pMEFs reveal that a number of pluripotency related genes, including Nanog, Lefty1 and Tdgf1, as well as the nucleosome remodeller Smarcd1, are hypomethylated in stem cells and hypermethylated in differentiated cells. Differences in promoter methylation are associated with significant differences in transcription levels in more than 60% of genes analysed. Our comparative approach to promoter methylation thus identifies gene candidates for the regulation of pluripotency and epigenetic reprogramming. While the sperm genome is, overall, similarly methylated to that of ES and EG cells, there are some key exceptions, including Nanog and Lefty1, that are highly methylated in sperm. Nanog promoter methylation is erased by active and passive demethylation after fertilisation before expression commences in the morula. In ES cells the normally active Nanog promoter is silenced when targeted by de novo methylation. Our study suggests that reprogramming of promoter methylation is one of the key determinants of the epigenetic regulation of pluripotency genes. Epigenetic reprogramming in the germline prior to fertilisation and the reprogramming of key pluripotency genes in the early embryo is thus crucial for transmission of pluripotency.
url http://europepmc.org/articles/PMC2432031?pdf=render
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