Abstract

The development of techniques which allow the efficient introduction of foreign genetic material into the germ line of animals has made it possible to analyze controls of mammalian development by a combined molecular and genetic approach. In this research proposal previously established methods will be used to introduce genes or cells into the developing mouse embryo. The main goals of these experiments are (1) identification and characterization of genes which are crucial for early development; (2) understanding the function protooncogenes may have in mammalian embryogenesis and the effect of oncogene expression on the developing mouse embryo; (3) The study of patterns of migration and homing of normal and transformed cells in the developing mouse embryo. 1) Insertional mutations will be induced by inserting retroviruses into the germ line of mice by an experimental approach which was successful previously in derivating a lethal mutation of the a1(1) collagen gene. Furthermore, procedures will be established for genetically rescuing mice carrying lethal mutations. As a first approach we will attempt to rescue the collagen mutation on the germ line level by microinjection of the wild type gene into mouse zygotes and on the somatic level by microinjection of a vector transducing the gene into mutant embryos prior to their developmental arrest. 2) Protooncogenes, oncogenes or temperature sensitive mutants of oncogenes will be introduced into the developing mouse embryo by retrovirus infection or by microinjection in the zygote. The expression of the inserted genes will be controlled by tissue specific or inducible promoters. These experiments are designed to test the normal function of protooncogenes in mammalian development and to determine the oncogenic potential of oncogenes. 3) Previous experiments have shown that neural crest cells can be introduced into midgestation embryos and participate in normal morphogenesis. We will use this approach of introducing cells into the developing embryo in an effort to define the parameters that determine the migration and homing of normal and transformed cells in n embryonic environment.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Unknown (R35)
Project #
5R35CA044339-06
Application #
3479503
Study Section
Special Emphasis Panel (SRC (88))
Project Start
1987-06-01
Project End
1994-05-31
Budget Start
1992-06-01
Budget End
1993-05-31
Support Year
6
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Whitehead Institute for Biomedical Research
Department
Type
DUNS #
076580745
City
Cambridge
State
MA
Country
United States
Zip Code
02142

  Publications

Hochedlinger, Konrad; Blelloch, Robert; Brennan, Cameron et al. (2004) Reprogramming of a melanoma genome by nuclear transplantation. Genes Dev 18:1875-85
Humpherys, David; Eggan, Kevin; Akutsu, Hidenori et al. (2002) Abnormal gene expression in cloned mice derived from embryonic stem cell and cumulus cell nuclei. Proc Natl Acad Sci U S A 99:12889-94
Biniszkiewicz, Detlev; Gribnau, Joost; Ramsahoye, Bernard et al. (2002) Dnmt1 overexpression causes genomic hypermethylation, loss of imprinting, and embryonic lethality. Mol Cell Biol 22:2124-35
Eggan, Kevin; Rode, Anja; Jentsch, Isabell et al. (2002) Male and female mice derived from the same embryonic stem cell clone by tetraploid embryo complementation. Nat Biotechnol 20:455-9
Akbarian, Schahram; Rios, Maribel; Liu, Rong-Jian et al. (2002) Brain-derived neurotrophic factor is essential for opiate-induced plasticity of noradrenergic neurons. J Neurosci 22:4153-62
Bates, Brian; Hirt, Lorenz; Thomas, Sunu S et al. (2002) Neurotrophin-3 promotes cell death induced in cerebral ischemia, oxygen-glucose deprivation, and oxidative stress: possible involvement of oxygen free radicals. Neurobiol Dis 9:24-37
Fan, G; Beard, C; Chen, R Z et al. (2001) DNA hypomethylation perturbs the function and survival of CNS neurons in postnatal animals. J Neurosci 21:788-97
Haase, V H; Glickman, J N; Socolovsky, M et al. (2001) Vascular tumors in livers with targeted inactivation of the von Hippel-Lindau tumor suppressor. Proc Natl Acad Sci U S A 98:1583-8
Akbarian, S; Chen, R Z; Gribnau, J et al. (2001) Expression pattern of the Rett syndrome gene MeCP2 in primate prefrontal cortex. Neurobiol Dis 8:784-91
Csankovszki, G; Nagy, A; Jaenisch, R (2001) Synergism of Xist RNA, DNA methylation, and histone hypoacetylation in maintaining X chromosome inactivation. J Cell Biol 153:773-84

Showing the most recent 10 out of 88 publications