Abstract

Development of the vertebrate embryo depends on intercellular signaling to specify the fate of cells comprising the embryonic body. Although many of the intercellular inducing factors involved in these signaling events have now been identified (e.g. FCF, Vg1, Xwnt, noggin), it is not known how intracellular signals triggered by these factors mediate cell fate. Toward this end, we have isolated a SER/THR kinase, Xgsk-3, from the amphibian, Xenopus laevis. Inhibition of Xgsk-3 activity on the ventral side of the embryo with a dominant-negative mutant of Xgsk-3, leads to embryos with completely twinned axes, including secondary heads. This result indicates that Xgsk-3 actively represses axis formation in the early embryo, and that axal development requires the repression of Xgsk-3 activity within the future Spemann organizer, establishing Xgsk-3 as a major intracellular regulator of early axis formation in the Xenopus embryo. In addition, genetic evidence from DrosophiLa, together with localization of the Xgsk-3 gene in Xenopus, suggests that it may also be an important regulator of the neuroectoderm. Three major areas will be pursued: 1. The regulation of Xgsk-3 in early axial patterning will be investigated, by developing biochemical assays for Xgsk-3 function. These experiments will determine which inducing factors have the ability to regulate Xgsk-3, and will ultimately elucidate the mechanism for Xgsk-3 inhibition during early development 2. The role of Xgsk-3 in later axial development and neural development will be determined, using the dominant-negative mutant of Xgsk-3 to block its function during different stages of embryogenesis. 3. A search for the proteins that regulate Xgsk-3 and that are regulated by Xgsk-3 during different developmental stages will be conducted in order to elucidate the intracellular signaling pathway that regulates axis development in the Xenopus embryo. The ultimate goal of this proposal is to provide a dear mechanistic understanding of the intracellular signaling processes that underlie vertebrate embryonic development. Since birth defects are due to a failure in the normal processes of embryogenesis, these studies will delineate the processes that can be perturbed by dysmorphogenic agents and genetic abnormalities.

  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 #
2R01HD027262-06
Application #
2200335
Study Section
Special Emphasis Panel (ZRG2-HED-2 (01))
Project Start
1990-08-01
Project End
1999-07-31
Budget Start
1995-08-01
Budget End
1996-07-31
Support Year
6
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Washington
Department
Biochemistry
Type
Schools of Medicine
DUNS #
135646524
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Weiser, Douglas C; Kimelman, David (2012) Analysis of cell shape and polarity during zebrafish gastrulation. Methods Mol Biol 839:53-68
Kimelman, David (2010) On the fast track to organizer gene expression. Dev Cell 19:190-2
Dahlberg, Caroline Lund; Nguyen, Elizabeth Z; Goodlett, David et al. (2009) Interactions between Casein kinase Iepsilon (CKIepsilon) and two substrates from disparate signaling pathways reveal mechanisms for substrate-kinase specificity. PLoS One 4:e4766
Martin, Benjamin L; Kimelman, David (2008) Regulation of canonical Wnt signaling by Brachyury is essential for posterior mesoderm formation. Dev Cell 15:121-33
Weiser, Douglas C; St Julien, Krystal R; Lang, James S et al. (2008) Cell shape regulation by Gravin requires N-terminal membrane effector domains. Biochem Biophys Res Commun 375:512-6
Weiser, Douglas C; Pyati, Ujwal J; Kimelman, David (2007) Gravin regulates mesodermal cell behavior changes required for axis elongation during zebrafish gastrulation. Genes Dev 21:1559-71
Xu, Wenqing; Kimelman, David (2007) Mechanistic insights from structural studies of beta-catenin and its binding partners. J Cell Sci 120:3337-44
Sampietro, James; Dahlberg, Caroline L; Cho, Uhn Soo et al. (2006) Crystal structure of a beta-catenin/BCL9/Tcf4 complex. Mol Cell 24:293-300
Kimelman, D; Xu, W (2006) beta-catenin destruction complex: insights and questions from a structural perspective. Oncogene 25:7482-91
Clements, Wilson K; Kimelman, David (2005) LZIC regulates neuronal survival during zebrafish development. Dev Biol 283:322-34

Showing the most recent 10 out of 37 publications