Maintenance of Self-renewal Ability of Mouse Embryonic Stem Cells in the Absence of DNA Methyltransferases Dnmt1, Dnmt3a and Dnmt3b

Overview

Journal Genes Cells

Specialties Cell Biology
Molecular Biology

Date 2006 Jul 11

PMID 16824199

Citations 303

Authors

Akiko Tsumura

Tomohiro Hayakawa

Yuichi Kumaki

Shin-Ichiro Takebayashi

Morito Sakaue

Chisa Matsuoka

Kunitada Shimotohno

Fuyuki Ishikawa

En Li

Hiroki R Ueda

Jun-Ichi Nakayama

Masaki Okano

Affiliations

Soon will be listed here.

Abstract

DNA methyltransferases Dnmt1, Dnmt3a and Dnmt3b cooperatively regulate cytosine methylation in CpG dinucleotides in mammalian genomes, providing an epigenetic basis for gene silencing and maintenance of genome integrity. Proper CpG methylation is required for the normal growth of various somatic cell types, indicating its essential role in the basic cellular function of mammalian cells. Previous studies using Dnmt1(-/-) or Dnmt3a(-/-)Dnmt3b(-/-) ES cells, however, have shown that undifferentiated embryonic stem (ES) cells can tolerate hypomethylation for their proliferation. In an attempt to investigate the effects of the complete loss of CpG DNA methyltransferase function, we established mouse ES cells lacking all three of these enzymes by gene targeting. Despite the absence of CpG methylation, as demonstrated by genome-wide methylation analysis, these triple knockout (TKO) ES cells grew robustly and maintained their undifferentiated characteristics. TKO ES cells retained pericentromeric heterochromatin domains marked with methylation at Lys9 of histone H3 and heterochromatin protein-1, and maintained their normal chromosome numbers. Our results indicate that ES cells can maintain stem cell properties and chromosomal stability in the absence of CpG methylation and CpG DNA methyltransferases.

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