Abstract

The role of the major histocompatibility complex (MHC) in early mammalian development will be investigated. A key factor in preimplantation embryonic development is the timing of the early cleavage divisions. We have recently discovered a gene, Ped (Preimplantation embryo development), associated with the H-2 complex, which influences the time of the first cleavage division and the subsequent rate of mouse embryonic development. Analysis of congenic strains has shown that embryos of certain haplotypes (k and r) exhibit a slow rate of development, whereas embryos of other haplotypes (b,d,q,a,s,u) develop at a fast rate. Further genetic analysis of Ped gene expression is proposed. First, linkage of the H-2 associated Ped gene to the H-2 complex will be tested by analysis of backcross embryos. Next, it will be determined whether the Ped gene affects the time of implantation or length of gestation. These data are important because there may be Ped genes in humans, associated with the HLA complex, that influence the timing of human development. Another important aspect of early embryonic development is the structure and function of cell surface proteins found on embryos. One class of cell surface molecules, the H-2 antigens, have been shown to be crucially important to a variety of cell-cell interactions between adult cells. However, the detection of H-2 antigens on early mouse embryos has been difficult and controversial. Using a highly sensitive cytotoxicity technique developed in our laboratory, we have been able to show the presence of H-2 antigens on embryos of the k, b, and d haplotypes. Further analysis of the types of H-2 antigens expressed on mouse embryos is proposed. Both conventional antisera and monoclonal antibodies will be used, and positive results will be confirmed by blocking studies with purified H-2 antigens. Finally, the question of whether H-2 antigens on mouse embryos are biologically functional will be probed by attempting to kill mouse embryos with cytotoxic T lymphocytes (CTL's). Since CTL's must recognize H-2 antigens in order to kill their targets, killing of the embryos by CTL's will be excellent evidence that H-2 antigens on mouse embryos are not only serologically detectable, but biologically functional, as well.

  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 #
5R01HD013748-07
Application #
3312296
Study Section
Mammalian Genetics Study Section (MGN)
Project Start
1979-12-01
Project End
1987-11-30
Budget Start
1985-12-01
Budget End
1986-11-30
Support Year
7
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Iowa State University
Department
Type
Schools of Arts and Sciences
DUNS #
City
Ames
State
IA
Country
United States
Zip Code
50011

  Publications

Xu, Y; Jin, P; Mellor, A L et al. (1994) Identification of the Ped gene at the molecular level: the Q9 MHC class I transgene converts the Ped slow to the Ped fast phenotype. Biol Reprod 51:695-9
Warner, C M; Gollnick, S O (1993) Expression of H-2K major histocompatibility antigens on preimplantation mouse embryos. Biol Reprod 48:1082-7
Xu, Y; Jin, P; Warner, C M (1993) Modulation of preimplantation embryonic development by antisense oligonucleotides to major histocompatibility complex genes. Biol Reprod 48:1042-6
Warner, C M; Panda, P; Almquist, C D et al. (1993) Preferential survival of mice expressing the Qa-2 antigen. J Reprod Fertil 99:145-7
Warner, C M; Almquist, C D; Toulimat, M H et al. (1993) Induction of embryonic major histocompatibility complex antigen expression by gamma-IFN. J Reprod Immunol 24:111-21
Tian, Z; Xu, Y; Warner, C M (1992) Removal of Qa-2 antigen alters the Ped gene phenotype of preimplantation mouse embryos. Biol Reprod 47:271-6
Warner, C M; Brownell, M S; Rothschild, M F (1991) Analysis of litter size and weight in mice differing in Ped gene phenotype and the Q region of the H-2 complex. J Reprod Immunol 19:303-13
Brownell, M S; Warner, C M (1988) Ped gene expression by embryos cultured in vitro. Biol Reprod 39:806-11
Warner, C M; Brownell, M S; Ewoldsen, M A (1988) Why aren't embryos immunologically rejected by their mothers? Biol Reprod 38:17-29
Warner, C M; Gollnick, S O; Goldbard, S B (1987) Linkage of the preimplantation-embryo-development (Ped) gene to the mouse major histocompatibility complex (MHC). Biol Reprod 36:606-10

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