Abstract

The primary goal of this research is to understand the cause of the abnormal phenotypes in mouse embryos developing in the absence of the Dnmt1o form of the Dnmt1 cytosine methyltransferase. The central premise to be tested is that the majority of Dnmt1o-deficient embryos die because they are epigenetic mosaics of cells that have defective imprints. Consequently, they do not develop normally. This model system will allow a detailed examination of the effect of epigenetic variation on phenotype and pregnancy outcome.
Aim 1 : Determine the nature of the epigenetic mosaicism in embryos derived from Dnmt1o-deficient oocytes. An embryo derived from a Dnmt1(delta1o) homozygous female develops in the absence of maternally supplied Dnmt1o and exhibits a loss of DNA methylation from 50% of the normally methylated alleles of imprinted genes. Each embryo is a mosaic, and should be comprised of many different epigenetic cell types, ranging from cells with mostly normal methylation on imprinted genes to cells with nearly no methylation on imprinted genes. This prediction will be tested by measuring imprinted methylation patterns in clones of embryonic stem (ES) and embryonic fibroblast (EF) cells derived from Dnmt1o-deficient embryos.
Aim 2 : Establish the source of the epigenetic mosaicism in embryos derived from Dnmt1o-deficient oocytes. The loss of Dnmt1o-dependent maintenance methylation probably occurs at the fourth embryonic S phase. This hypothesis will be tested by measuring imprinted methylation patterns in pools of Dnmt1o-deficient embryos at each preimplantation stage, and in cloned embryos derived using donor nuclei from each Dnmt1o-deficient preimplantation stage.
Aim 3 : Determine the cause of the variable, abnormal phenotypes of Dnmt1o-deficient embryos. Dnmt1o-deficient embryos die, most likely because their imprint-defective cells are unable to contribute to normal development. This hypothesis will be tested by first defining the morphological abnormalities present in Dnmt1o-deficient embryos and extraembryonic tissues. Afterwards, clones of Dnmt1o-deficient ES cells, each a self-renewing population with a unique pattern of normal and defective imprints, will be tested for their ability to contribute to embryonic development in ES-blastocyst and ES-tetraploid chimeras.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD044133-04
Application #
7235989
Study Section
Reproductive Biology Study Section (REB)
Program Officer
Coulombe, James N
Project Start
2004-05-15
Project End
2009-03-31
Budget Start
2007-04-01
Budget End
2009-03-31
Support Year
4
Fiscal Year
2007
Total Cost
$289,781
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Genetics
Type
Schools of Medicine
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Shaffer, Ben; McGraw, Serge; Xiao, Siyu C et al. (2015) The DNMT1 intrinsically disordered domain regulates genomic methylation during development. Genetics 199:533-41
McGraw, Serge; Zhang, Jacques X; Farag, Mena et al. (2015) Transient DNMT1 suppression reveals hidden heritable marks in the genome. Nucleic Acids Res 43:1485-97
Balakrishnan, Ashwini; Chaillet, J Richard (2013) Role of the inositol polyphosphate-4-phosphatase type II Inpp4b in the generation of ovarian teratomas. Dev Biol 373:118-29
McGraw, Serge; Oakes, Christopher C; Martel, Josée et al. (2013) Loss of DNMT1o disrupts imprinted X chromosome inactivation and accentuates placental defects in females. PLoS Genet 9:e1003873
Epperly, Michael W; Chaillet, J Richard; Kalash, Ronny et al. (2013) Conditional radioresistance of Tet-inducible manganese superoxide dismutase bone marrow stromal cell lines. Radiat Res 180:189-204
Himes, K P; Koppes, E; Chaillet, J Richard (2013) Generalized disruption of inherited genomic imprints leads to wide-ranging placental defects and dysregulated fetal growth. Dev Biol 373:72-82
Ackerman 4th, W E; Bulmer, J N; Carter, A M et al. (2012) IFPA Meeting 2011 workshop report III: Placental immunology; epigenetic and microRNA-dependent gene regulation; comparative placentation; trophoblast differentiation; stem cells. Placenta 33 Suppl:S15-22
Rugo, R E; Mutamba, J T; Mohan, K N et al. (2011) Methyltransferases mediate cell memory of a genotoxic insult. Oncogene 30:751-6
Mohan, K Naga; Ding, Feng; Chaillet, J Richard (2011) Distinct roles of DMAP1 in mouse development. Mol Cell Biol 31:1861-9
D'Aiuto, Leonardo; Di Maio, Roberto; Mohan, K Naga et al. (2011) Mouse ES cells overexpressing DNMT1 produce abnormal neurons with upregulated NMDA/NR1 subunit. Differentiation 82:9-17

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