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Loss of DNMT1o Disrupts Imprinted X Chromosome Inactivation and Accentuates Placental Defects in Females
Authors
A Wagschal
AL Fowden
+74 more
AS Doherty
B Lehnertz
BK Sun
C Beard
C Mertineit
Christoph Plass
Christopher C. Oakes
CM Disteche
CP Walsh
CY Howell
D Bourc'his
DE Cohen
DJ Smiraglia
E Borowczyk
E Heard
EJ Michaud
H Barr
I Hatada
I Okamoto
I Zvetkova
J Chaumeil
J Silva
J. Richard Chaillet
JA Bailey
Jacquetta M. Trasler
JC Chow
JD West
Jeannie T. Lee
JM Trasler
Josée Martel
JT Lee
JT Lee
K Hata
KD Huynh
KD Huynh
KL Tucker
KP Himes
L Yu
LL Carlson
M Ehrich
M Hemberger
M Kaneda
M Toppings
M. Cecilia Cirio
Marisa S. Bartolomei
MC Cardoso
MC Cirio
MC Cirio
MF Lyon
N Stavropoulos
N Takagi
Pauline de Zeeuw
RJ Klose
RM Boumil
S Ratnam
Serge McGraw
SH Namekawa
T Ohhata
T Ohhata
T Sado
T Sado
T Sado
T Sado
TH Bestor
W Mak
W Mak
W Reik
W Reik
WA Schulz
Winifred Mak
Y Kurihara
Y Marahrens
Y Ogawa
Y Okazaki
Publication date
1 January 2013
Publisher
'Public Library of Science (PLoS)'
Doi
View
on
PubMed
Abstract
The maintenance of key germline derived DNA methylation patterns during preimplantation development depends on stores of DNA cytosine methyltransferase-1o (DNMT1o) provided by the oocyte. Dnmt1omat-/- mouse embryos born to Dnmt1Δ1o/Δ1o female mice lack DNMT1o protein and have disrupted genomic imprinting and associated phenotypic abnormalities. Here, we describe additional female-specific morphological abnormalities and DNA hypomethylation defects outside imprinted loci, restricted to extraembryonic tissue. Compared to male offspring, the placentae of female offspring of Dnmt1Δ1o/Δ1o mothers displayed a higher incidence of genic and intergenic hypomethylation and more frequent and extreme placental dysmorphology. The majority of the affected loci were concentrated on the X chromosome and associated with aberrant biallelic expression, indicating that imprinted X-inactivation was perturbed. Hypomethylation of a key regulatory region of Xite within the X-inactivation center was present in female blastocysts shortly after the absence of methylation maintenance by DNMT1o at the 8-cell stage. The female preponderance of placental DNA hypomethylation associated with maternal DNMT1o deficiency provides evidence of additional roles beyond the maintenance of genomic imprints for DNA methylation events in the preimplantation embryo, including a role in imprinted X chromosome inactivation. © 2013 McGraw et al
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